Evidence-Based Guided Interventions in Acute Leukemia

Ron Ram; Liat Vidal; Ronit Gurion; Pia Raanani; Ofer Shpilberg

doi:10.5772/24055

Author Information

Show +

Ron Ram*
- Institute of Hematology, Davidoff Cancer Center, Beilinson Hospital,Rabin Medical Center and Sackler School of Medicine, Tel- Aviv University, Israel
Liat Vidal
- Institute of Hematology, Davidoff Cancer Center, Beilinson Hospital,Rabin Medical Center and Sackler School of Medicine, Tel- Aviv University, Israel
Ronit Gurion
- Institute of Hematology, Davidoff Cancer Center, Beilinson Hospital,Rabin Medical Center and Sackler School of Medicine, Tel- Aviv University, Israel
Pia Raanani
- Institute of Hematology, Davidoff Cancer Center, Beilinson Hospital,Rabin Medical Center and Sackler School of Medicine, Tel- Aviv University, Israel
Ofer Shpilberg
- Institute of Hematology, Davidoff Cancer Center, Beilinson Hospital,Rabin Medical Center and Sackler School of Medicine, Tel- Aviv University, Israel

*Address all correspondence to:

1. Introduction

Evidence based medicine (EBM) is becoming a cornerstone in the establishment of practical guidelines and is nowadays part of the process of decision making in medicine (Woolf 2000). In evidence based medicine, decision making is based on relevant clinical trials ranked by their relevance and validity according to established criteria. Indeed, well designed randomized controlled trials (RCTs) are considered the "gold standard". However, since hematological disorders such as acute leukemia are rare, RCTs with a large enough sample size are difficult to conduct.

Systematic reviews use a preplanned, explicit methodology to answer a predefined question and evaluate the benefit and harm of healthcare interventions. Meta-analyses quantitatively assemble results from RCTs to increase power when individual studies are too small to detect a statistically significant effect (Gale and Lazarus 2011). The quality of a systematic review reflects the quality of its included studies. Potential sources of bias are heterogeneity between the RCTs included, publication bias and difficulties in accessing data from the original clinical trials.

In this chapter we attempted to assemble the evidence on the available meta-analyses analyzing the data in acute myeloid leukemia (AML) and acute lymphoblastic leukemia (ALL) patients. In certain domains, when no meta-analyses were identified, a literature search was performed and, if applicable, suggestions for future studies were made.

2. Methods

We searched The Cochrane and MEDLINE databases for systematic reviews. In Pubmed we crossed MeSH terms for 'acute myeloid leukemia' or 'acute lymphoblastic leukemia' with Clinical Queries to limit the search for systematic reviews.

We included systematic reviews of RCTs (with or without meta-analyses) assessing the effect of different chemotherapy regimens and supportive care on overall survival of patients with acute leukemia. We included the use of these treatment options in the following clinical settings: remission induction, post remission (consolidation) including autologous and allogeneic stem cell transplantation and maintenance.

We assessed the risk of bias in the systematic reviews by the following domains: use of explicit inclusion/exclusion criteria and a predefined protocol; comprehensive search; whether selection bias was avoided; assessment of risk of bias of original trials; correct statistical methods to pool the data. Assessment of risk of bias in each of the systematic reviews based on the AMSTAR protocol is summarized in tables 1-2 and 4 (Liberati, et al 2009, Oxman and Guyatt 1991, Shea, et al 2007, Shea, et al 2009).

For the evaluation of prospective comparative trials in the transplantation field, we searched for meta-analyses including genetically randomized trials. These trials were defined by patient allocation to an intervention on the basis of sibling donor availability (donor group versus no-donor group) and were evaluated for potential bias as previously discussed (Ram, et al 2011).

3. An overview of systematic reviews in acute myeloid leukemia

Survival of AML patients has constantly been increasing from about 5-10% in 1975 to about 25% of diagnosed patients according to SEER data (1975-2007) in US population. This progress is the result of the progress in supportive care enabling treatment with intensive chemotherapy to induce remission and the use of allogeneic hematopoietic cell transplantation (HCT), as well as the use of prognostic factors in clinical decision making. For the majority of patients with AML this disease still has grave consequences. Our understanding of cytogenetic and molecular factors in the pathogenesis and the prognosis of patients with AML has evolved tremendously during the last decade. Still our ability to cure has remained unsatisfactory.

Treatment of AML with curative intent is generally divided into remission induction and post remission (also referred to as consolidation) courses (Dohner, et al 2010). Management of patients with AML depends mainly on their age, their response to therapy and the cytogenetic and molecular factors of the leukemic clone, stratifying patients into favorable, standard and unfavorable risk groups.

We herein reviewed the results of systematic reviews assessing chemotherapy for patients with AML. For each systematic review we evaluated the methodological quality using the AMSTAR assessment tool (Table 1).

3.1 Induction therapy

For more than 3 decades remission induction treatment consists of anthracyclines administered for 3 days and cytarabine given at a dose of 100-200 mg/m² in continuous infusion for 7 days. Efforts to improve response rate and survival of patients with AML included the addition of other chemotherapeutic drugs to the standard induction regimen, using different types and doses of anthracyclines, as well as different doses of cytarabine.

3.1.1 Does the type of anthracycline affect overall survival of adult patients with AML?

A systematic collaborative overview of individual patient data of RCTs that compared an idarubicin-based induction regimen with a different anthracycline-based regimen included trials from 1984 to 1993 including 1898 patients (AML Collaborative Group, 1998). Compared to daunorubicin, idarubicin improved remission rate (53% vs. 62%, respectively, p = 0.002) and overall survival (14% odds reduction, p = 0.03), however disease free survival (DFS) did not differ significantly (15% odds reduction, p=0.07). This overview fulfilled 4 of 11 criteria of the AMSTAR tool.

Since the publication of this systematic review new data has accumulated (Mandelli, et al 2009, Rowe, et al 2004).

3.1.2 Does the dose of anthracyclines during induction have an effect on survival?

Historically, the conventional induction anthracycline dose was the equivalent of daunorubicin 45-50 mg/m² daily given for 3 days. Large case series and observational studies supported a dose escalation to 60 mg/m². It remained questionable if the dose response curve has reached a plateau and whether the dose amplification benefit can be confirmed in RCTs. A few RCTs evaluated various dosages of anthracyclines. No published systematic review has summarized their findings so far.

Two RCTs evaluated dose intensification of anthracyclines (Fernandez, et al 2009, Lowenberg, et al 2009). Patients <60 years old treated with 90 mg/m² of daunorubicin, as compared with the standard 45 mg/m², achieved a higher rate of complete remission (CR) (70.6% vs. 57.3%; P<0.001) and a better overall survival (P=0.003) (Lowenberg, et al 2009). In another trial, >60 year-old patients treated with higher doses of daunorubicin, i.e. 90 mg/m² as compared to 45 mg/m² daily, for 3 days, had higher CR rates (64% for the high dose vs. 54% for the standard dose; P=0.002) (Pautas, et al 2010). There was no significant difference between the two groups in the incidence of hematological adverse events, 30-day mortality (11% and 12% in the 2 groups, respectively), or the incidence of adverse events (P=0.08). An overall survival benefit was demonstrated only in 2 subgroups: patients aged 60 to 65 years, and those with favorable cytogenetics. Paustas et al. compared 3-days of daunorubicin 80 mg/m²/day with 3 or 4-days of idarubicin 12 mg/m²/day in 468 patients aged 50 to 70 years. While a statistically significant higher rate of CR was demonstrated in patients treated with idarubicin (P =.04), there were no significant differences in the other outcomes.

Thus, conventional dose for remission induction in adult patients < 60 years with AML should be between 60 to 90 mg/m²/day. There is no clear benefit for higher doses (90 mg/m²/day) of daunorubicin compared to 45 mg/m² daily in adults >65 years.

3.1.3. Do higher doses of cytarabine during remission induction treatment improve survival?

Kern and Estey reviewed the literature to examine the effect of high dose cytarabine (≥1000 mg/m²/dose) in induction therapy compared with standard dose (100-200 mg/m²/day) cytarabine (Kern and Estey 2006). The search yielded 3 trials, evaluating 1691 adult AML patients < 60 years. There was no difference between high dose and standard dose cytarabine with regard to CR rate (relative risk 1.00; 95% CI 0.92 to 1.10) or early death rate (RR 1.53; 95% CI 0.84 to 2.78, random-effects model). However, 4-year overall survival was better in patients given high dose cytarabine (weighted mean difference, 6.211; 95% CI, 2.701 to 9.721). In this meta-analysis time to event data was analyzed as continuous data, the assumptions made for converting median to mean and their variance to standard deviation were not described, and weighted mean difference was used to pool results. This review fulfilled 7 of 11 criteria of the AMSTAR criteria.

3.2. Post remission therapy

3.2.1. What is the role of transplantation in patients with AML?

3.2.1.1 .Autologous hematopoietic cell transplantation

Four systematic reviews evaluated the effect of autologous hematopoietic cell transplantation (HCT) in first CR (Ashfaq, et al 2010, Levi, et al 2004, Nathan, et al 2004, Wang, et al 2010).

Nathan et al. compared the efficacy of autologous HCT with chemotherapy (or no further treatment) in patients aged 15 to 55 years (Nathan, et al 2004). Their search yielded 6 trials including 1044 patients. Patients who underwent autologous HCT had a better DFS (probabilities ratio of 1.24, 95% CI 1.06 to 1.44) with similar long term mortality rate (RR 1.01, 95% CI 0.89 to 1.15). This review fulfilled 9 of 11 criteria of the AMSTAR tool. Levi et al performed a systematic review on the same question with similar findings (Levi, et al 2004).

A more recent systematic review included 12 RCTs (Wang, et al 2010). Patients treated with autologous HCT had lower relapse rate,better DFS, but no overall survival benefit probably because of higher treatment related mortality. Of note, at present, transplant related mortality is lower than the estimated 4% reported in these systematic reviews.

3.2.1.2. Allogeneic hematopoietic cell transplantation

Eight reviews and meta-analyses were identified but only three of them were systematic and comprehensive (Ashfaq, et al 2010, Hubel, et al 2011, Koreth, et al 2009). Koreth et al. performed a systematic review comparing allogeneic HCT with conventional consolidation chemotherapy or autologous HCT (Koreth, et al 2009). Patients allocated to the allogeneic HCT arm had an overall survival benefit (HR 0.90 95% CI 0.82 to 0.97, 15 trials), and relapse free survival (HR 0.80 95% CI, 0.74 to 0.86, 18 trials). In an analysis stratified according to the cytogenetic risk groups, only intermediate and poor risk AML patients allocated to the allogeneic HCT arm had improved overall survival, while favorable risk patients had similar overall survival in both allocated arms. This review fulfilled 10 of 11 criteria of the AMSTAR tool.

Another comprehensive systematic review (without a quantitative summary) was done through the National Institute for Health Research Health Technology Assessment (HTA) program in UK (Ashfaq, et al 2010). The results and conclusions of this very detailed review were consistent with those of the previous ones. Other systematic reviews were published earlier and were not as comprehensive (Oliansky, et al 2008, Schlenk, et al 2004, Visani, et al 2006, Yanada, et al 2005).

3.3 Consolidation – dose intensity of cytarabine

A systematic overview without a quantitative analysis of chemotherapy for patients with AML was conducted by The Swedish Council of Technology Assessment in Health Care (Kimby, et al 2001). In one trial consolidation was compared to no further treatment. This trial was closed early due to inferior remission duration in the latter group. In all the trials comparing high dose cytarabine to standard dose or maintenance therapy, high dose cytarabine was shown to be superior to the comparator, though overall survival advantage was not consistently shown. Consolidation with high dose cytarabine seemed to be of value mainly for patients with core binding factor AML and in younger patients, due to a high mortality rate in patients older than 60 years. This overview fulfilled 1 of 10 criteria of the AMSTAR tool.

3.4 Maintenance therapy instead of consolidation chemotherapy

This question was reviewed by Kimby et al. who found limited data to indicate that post-remission maintenance therapy with long-term attenuated chemotherapy can prolong remission duration compared to no further therapy (Kimby, et al 2001). However, the data in support of these conclusions are sparse and effect on survival was not shown.

3.5. Role of azacitidine

Azacitidine was not exclusively assessed in AML patients but rather analyzed in a pooled myelodysplasia/AML group of patients (20%- 30% blasts, defined by the WHO as AML)

Table 1.
Assessment of risk of bias using AMSTAR criteria in systematic reviews in the field of AML.

(Edlin, et al 2010). This RCT shows an overall survival benefit for azacytidine compared to best supportive care, low dose cytarabine, or intensive chemotherapy. Two RCTs that evaluated the effect of azacytidine in patients with high risk MDS (including patients with 20%- 30% blasts) showed improved time to transformation or death in patients given azacytidine (Fenaux, et al 2009, Silverman, et al 2002).

Azacytidine was also given as part of post remission chemotherapy: in the MRC AML 9 trial, patients given the azacitidine-chemotherapy arm as consolidation had fewer relapses comparedto patients given only chemotherapy (p = 0.003), but a higher treatment related mortality (4.5% vs. 0%), without a statistically significant improved long term survival (Rees, et al 1996).

In another trial, patients were randomized to post remission consolidation with different chemotherapy regimens: standard dose cytarabine-daunorubicin vs. the same treatment followed by amsacrine and azacytidine vs. thioguanine and standard dose cytarabine-daunorubicin (Volger, et al 1995). The 5-year DFS was 38%, 31%, and 27% (p<0.05), respectively.

4. Acute promyelocytic leukemia

Acute promyelocytic leukemia (APL) is usually characterized by a specific gene rearrangement and the generation of the PML-RARα fusion transcript which results from a translocation between chromosomes 15 and 17. Targeted therapy with all-trans retinoic acid (ATRA) and anthracycline-based chemotherapy results in cure in 70-80% of patients.

Two systematic reviews evaluated the first line treatment of patients with APL (Xu, et al 2009a, Xu, et al 2009b).

The first one includes 7 RCTs (392 patients) comparing ATRA plus arsenic trioxide to other treatments. Compared with arsenic trioxide monotherapy, arsenic trioxide plus ATRA affected neither CR or DFS rates nor mortality of relapsed APL patients. Arsenic trioxide plus ATRA improved CR rate, DFS, mortality rate and adverse reactions compared to the same regimen including also chemotherapy. The review fulfilled 6 of 11 criteria of the AMSTAR tool.

A systematic review and meta-analysis including 5 randomized controlled trials (328 patients) compared ATRA plus arsenic trioxide regimen with ATRA monotherapy in patients with APL showed an improved 2-year DFS rate in the group treated with ATRA arsenic trioxide.

5. An overview of systematic reviews in acute lymphoblastic leukemia

Acute lymphobIastic leukemia (ALL) is the most common acute leukemia in children, while the incidence is much lower in adults (National Cancer Institute. SEER Cancer Statistics Review Available at: http://seer.cancer.gov/csr/1975_2006). The outcome of pediatric ALL patients has evolved from an overall survival of less than 10% in the 1960s to approximately 80% at present (Pui, et al 2008). However, adult patients have a less optimistic prognosis. While the remission rate reaches 90%, the survival rate is only 40%-50% (Fielding 2008). ALL patients are stratified and treated according to algorithms that integrate the presenting features, leukemia features and early response to therapy (Faderl, et al 2003); However the classification to standard and poor risk disease varies among the major studies conducted in adult ALL patients (Hoelzer, et al 1988, Kantarjian, et al 2004, Lazarus, et al 2006, Le, et al 2006, Rowe, et al 2005, Ram, et al 2010).

Treatment of adult ALL patients usually consists of remission induction and consolidation/intensification phases followed by either HCT or maintenance therapy.

As stated above, because the disease is relatively rare in adults, much of the knowledge and protocols have been adopted from pediatric regimens. Although we aim to focus on adult population, a portion of the data is based on evidence from pediatric trials.

For each systematic review we evaluated the methodological quality using the AMSTAR assessment tool (table 2).

5.1. Is there a specific induction regimen which is better?

Different groups use various induction regimens, which have not been compared head to head (Gokbuget and Hoelzer 2009, Kantarjian, et al 2004, Larson, et al 1995, Linker, et al 2002, Thomas, et al 2004b). In adult patients, the use of growth factors such as granulocyte colony-stimulating factor that accelerate hematopoietic recovery has greatly improved the success rate of ALL therapy (Kantarjian, et al 2004) and will be reviewed in a different part of this chapter.

One individual patient data meta-analysis examined the role of incorporating different types of anthracycines into pediatric induction regimens (CALLCG, 2009) and identified 4 trials recruiting 958 patients. They found that there was a borderline significant reduction in bone marrow leukemia relapse rate (OR 0.77, 95% CI 0.60 to 1.00; p=0.05) among patients treated with anthracyclines compared to those not, though there was no difference in non-bone marrow leukemia relapse rate (OR 0.88, 95% CI 0.63 to 1.25; p=0.5). The reduction in relapse rate translated into improved relapse free survival (OR 0.81; 95% CI, 0.66 to 1.00; p=0.05). However, event free survival (EFS) and overall survival were similar between the two groups. No significant differences in outcomes were demonstrated when different anthracyclines or when different adninistration schedules were compared. As this meta-analysis has been solely conducted in a pediatric population, results might not be applicable for adult patients. This systematic review fulfilled 5 of 11 criteria of the AMSTAR tool.

5.2 What is the role of pediatric inspired regimens for adult patients, mainly for the group of adolescents and young adults?

Several recent studies comparing the outcome of adolescents and young adults (AYAs) up to the age of 45 years, treated with pediatric versus adult protocols, demonstrated improved survival for AYAs who were treated by pediatric groups (Boissel, et al 2003, Ramanujachar, et al 2007, Stock, et al 2008). All are non-randomized trials and are therefore prone to significant bias. Thus, these trials are difficult to interpret because of the wide spectrum of patients' age, the small number of patients, the variations in the regimens utilized and the varying application of HCT in different studies. Recently our group completed a systematic review and meta analysis of all published comparative studies. We showed that up to the age of 20 years, pediatric inspired regimens are superior to conveintional afults chemotherapy ( Ram, et al 2011). Currently there are several groups conducting prospective trials (e.g., US AALL0232) to further elucidate which is the best treatment for AYAs. Only then, solid conclusions to tailor the best treatment for AYAs should be drawn.

5.3. What is the role of thyrosine kinase inhibitors in the treatment of Philadelphia positive ALL?

Philadelphia positive ALL is a disease with a historically dismal prognosis in which HCT provided the only chance for cure (Fielding and Goldstone 2008). Recently, the introduction of tyrosine kinase inhibitors (TKIs) has opened wide new perspectives of how to treat these patients (Thomas, et al 2004a). We were not able to identify systematic reviews assessing the

Table 2.
Assessment of risk of bias using AMSTAR criteria in systematic reviews in the field of ALL.

role of the different tyrosine kinase inhibitors. Prospective comparison, for example, by using genetic randomization based on donor availability along with intention-to-treat analysis, is necessary to draw conclusions on the clinical utility of allogeneic HCT for these patients.

5.4 What is the role of allogeneic HCT in first CR?

Allogeneic HCT provides a potential curative approach for patients with ALL, mainly through the anti-leukemic effect of the graft. Nonetheless, the relatively high non-relapse mortality compared to other treatment options limits the widespread use of this approach (Hahn, et al 2006, Ram, et al 2011).

As stated in the Methods section, the preferred way to assess the role of allogeneic HCT is to use a genetic randomization design, allocating patients with a matched sibling donor and those lacking sibling donor to the donor/transplantation arm and the no-donor/alternative treatment arm, respectively (Ram, et al 2011).

Five systematic reviews were conducted (Ashfaq, et al 2010, Hahn, et al 2006, Orsi et al 2007, Ram, et al 2010, Yanada et al 2006), 3 out of which included also a meta analysis (Orsi et al 2007, Ram, et al 2010, Yanada et al 2006). All three meta-analyses showed that overall, for ALL patients achieving first CR, allogeneic HCT carries a survival benefit compared to the other options. While all 3 meta-analyses used similar search criteria, the strict intention to treat (ITT) inclusion criteria were different. Moreover, the two largest trials in the field (Cornelissen et al 2009, Goldstone et al 2008) were included only in the most recently published meta-analysis only (Ram, et al 2010). This meta-analysis included 10 genetically trials, randomizing 2,600 patients for the main comparison of allogeneic HCT vs. other treatments, with only seven trials, randomizing 1,863 patients, following strict ITT criteria (table 2). In this meta-analysis, survival benefit was statistically significant for the standard-risk patients (RR for all-cause mortality 0.80, 95% CI 0.68–0.94), while for the high-risk it it was not (RR 0.88, 95% CI 0.76–1.01) (Ram, et al 2010). As expected, there was a significant increase in non-relapse mortality in the allogeneic HCT arm (RR 2.99; 95% CI, 1.37-6.53) and a significant decrease in the relapse rate (RR 0.52; 95% CI, 0.33-0.83). This systematic review fulfilled 10 of 11 criteria of the AMSTAR tool.

Although a systematic review published by Yanada et al showed a similar survival advantage in favor of the donor group (HR 1.29, 95% CI 1.02 to 1.63, p = 0.037), superiority could be demonstrated for the high-risk patients subgroup only (HR 1.42, 95% CI 1.06 to 1.90; p = 0.019). This systematic review fulfilled 8 of 11 criteria of the AMSTAR tool.

The difference between the two meta-analyses might stem from two main causes: The first is the inclusion of the two recent large trials in the last meta-analysis only (Cornelissen et al 2009, Goldstone et al 2008) and the second from the different methodologies and inclusion criteria used in the various studies (with more emphasis on strict ITT methodology in the recently published meta-analysis).

Orsi et al. conducted an individual patient meta-analysis of four trials (Hunault et al., 2004, Labar et al 2004, Ribera et al 2005, Thomas, et al 2004b). They also showed survival benefit for the donor group (mean EFS was 5.88 years in the donor group and 4.88 years in the no-donor group) with survival rate of 44.2% (± 2.9%) at 7 years in the donor group and 31.6% (± 2.2%) in the non-donor group, log-rank test p = 0.011. Performance of allogeneic HCT in first CR was found to be cost effective. This systematic review fulfilled 9 of 11 criteria of the AMSTAR tool.

To summarize, all meta-analyses suggest overall survival benefit for patients undergoing a matched donor allogeneic HCT in first CR when compared to other modalities. By drawing firm conclusions based on strict ITT trials it is suggested that allogeneic HCT may be more effective for the standard risk group.

5.5 Is there a role for autologous HCT in first CR?

We identified three systematic reviews that reported on the comparison between post remission autologous HCT and maintenance chemotherapy (Ashfaq, et al 2010, Hahn, et al 2006, Ram, et al 2010). One of them also performed a meta-analysis of the available RCTs. Both Hahn et al. and Ashfaq et al. concluded that both autologous HCT and maintenance chemotherapy yield a similar outcome (Ashfaq, et al 2010, Hahn, et al 2006). They also suggested that autologous HCT might be a superior option for high risk patients. In the meta-analysis performed by our group (Ram, et al 2010), five conventionally randomized trials enrolling 963 patients were identified. Similar to previous systematic reviews, survival was comparable between the two arms (RR 1.02, 95%CI, 0.88 to 1.19) for both standard and high risk patients. However there was a significant increase in non-relapse mortality in the autologous HCT arm (RR 1.77; 95% CI, 1.12 to 2.8), though no statistically significant difference was demonstrated in the relapse risk (RR 0.92; 95% CI, 0.73-1.15).

	Yanada, Cancer 2006	Orsi, BMT 2007	Ram, Cancer 2010
Bernasconi 1992*			+
Sebban 1994*	+	+	+
Attal 1995*			+
Takeuchi 2002*	+		+
Dombret 2002,Thomas 2004*	+	+	+
Labar 2004#	+		+
Hunault 2004#	+	+	+
Ribera 2005*	+	+	+
Vey 2006*			+
Cornelissen 2008#			+
Goldstone 2008*			+
Fielding, 2009*			+

Table 3.

Comparisons between 3 meta-analyses assessing the role of allogeneic hematopoietic cell transplantation in first complete remission

*True ITT trial #Not strictly ITT trial – Reasons for the inability to perform ITT analysis: Labar,2004- inclusion of patients with no siblings in the non-donor arm; Hunault, 2004- inclusion of patients>50 years in the non-donor group ; Cornelissen,2008- inclusion of patients who underwent matched unrelated donor transplantation in the nondonor study arm

5.6. Which is the best maintenance therapy?

The post remission high relapse rate of adult ALL patients has encouraged the exploration of various post-remission modalities. The optimal type and duration of maintenance therapy and the value of further intensification are still debated.

We identified 3 relevant systematic reviews (CALLCG et al 1996, Eden, et al 2010, Escherich, et al 2011), reporting on pediatric patients.

The first, evaluating the impact of duration and intensity of the different maintenance regimens, included 16 trials, randomizing 746 patients (CALLCG et al., 1996) showed that maintenance treatment administered for up to 3 years was associated with a significantly lower relapse rate albeit a similar rate of death from leukemia. Of note, maintenance duration beyond 3 years did not yield any superiority. More intensive regimens were associated with significantly fewer relapse events and with prolonged survival (absolute difference in survival of about 3% at 5 years and of 4% at 8 years). This systematic review fulfilled 3 of 11 criteria of the AMSTAR tool.

The second systematic review evaluated the addition of steroids plus vincristine pulses during the maintenance period (Eden, et al). In an individual patient meta-analysis vincristine-prednisone pulses were shown to improves EFS (70.1% vs. 62% at 5 years; OR 0.71, 95% CI 0.61 to 0.84; p = 0.00004), while vincristine - dexamethasone pulses did not have this effect (80.9% vs. 79.9% at 5 year; OR 0.94; 95% CI, 0.8 to 1.11;p = 0.5) Overall survival was not affected by both combinations. (Bostrom, et al 2003). Results of this meta-analysis should be taken with caution as they might be significantly biased by different pre-maintenance induction regimens. This systematic review fulfilled 7 of 11 criteria of the AMSTAR tool.

The third systematic review compared between the various thiopurines (mainly thioguanine and metcaptopurine) as maintenance (Escherich, et al). In a meta-analysis of 3 trials, event-free survival was similar for the two agents (OR 0.89, 95% CI, 0.78 to 1.03). However in a subgroup analysis of males aged<10 years there was a significant benefit for thiogouanine in terms of EFS (OR 0.70, 95% CI, 0.58 to 0.84), although this did not result in a significant difference in overall survival (OR 0.83, 95% CI, 0.62 to 1.10). It was concluded that mercaptopurine, and not thiogouanine, should be the thiopurine drug of choice for maintenance. Although this conclusion is valid for pediatric patients, in the absence of data in adults this may also be applicable for them. This systematic review fulfilled 5 of 11 criteria of the AMSTAR tool.

5.7 What is the role of CNS prophylaxis and is there a “gold-standard” regimen?

CNS involvement at presentation in adult ALL patients is estimated as 5% (Lazarus, et al 2006). Nevertheless, without prophylaxis administration, CNS recurrence occurs in approximately 30% of adult patients in complete response (Omura, et al 1980). There are several options to administer CNS prophylaxis therapy. These include cranial radiotherapy and intrathecal or intraventricular chemotherapy.

One pediatric systematic review with individual patient meta-analysis (Clarke, et al 2003) reported that prophylactic radiotherapy reduced CNS relapse slightly more than long-term intrathecal therapy, however no survival benefit was shown. Also, higher than 21 Gy radiation dose did not correlate with lower relapse risk and, the addition of intravenous methotrexate to regimens containing either radiation and intrathecal therapy led to a better EFS. This systematic review fulfilled 4 of 11 criteria of the AMSTAR tool.

6. An overview of systematic reviews in supportive care for patients with acute leukemia

Supportive care in acute leukemia has improved dramatically during the last decades and contributed to the improved overall survival of AL patients.

7. Myeloid growth factors

The use of G-CSF and GM-CSF results in a dose dependent increase in the levels of circulating neutrophils, mainly as a result of shortening the transit time from stem cell to mature cells (Griffin 2001). During intensive chemotherapy, acute leukemia patients experience prolonged and profound neutropenia, which is a risk factor for bacterial and fungal infections, for increased mortality. Patients with acute leukemia can be treated with myeloid growth factors as primary or secondary prophylaxis (before or after the development of neutropenia, respectively) or for priming (before or concurrent with chemotherapy) with the aim of sensitizing blast cells and recruiting them into cell-cycle, thus enhancing their susceptibility to cytotxic agents like cytarabine.

Five systematic reviews assessed the effect of myeloid growth factors in acute leukemia patients.

The first one is a comprehensive systematic review and meta-analysis, published in 2007 by Sung et al and comprises 148 RCTs, randomizing 16,839 patients with all types of cancer. Patients were randomly assigned to receive chemotherapy with or without prophylaxis with myeloid growth factors (Sung, et al 2007). There was no difference between the two groups in short term all cause mortality and in infection related mortality. However, the use of myeloid-growth factors was associated with reduction of clinically and microbiologically documented infections (RR 0.75, 95% CI 0.62 to 0.92, and RR 0.86, 95% CI, 0.77-0.96, respectively). Subgroup analysis of acute leukemia patients did not show any difference in short term all cause mortality and infection related mortality, as well (Sung, et al 2007). This systematic review fulfilled 9 of 11 criteria of the AMSTAR tool.

The second systematic review and meta-analysis compared the prophylactic use of G-CSF in patients with AML receiving chemotherapy, to placebo/no treatment (control group) (Wang, et al 2009a, Wang, et al 2009b). This review included seven trials with almost 2000 participants, and did not show difference in overall survival between the G-CSF group and the control group (Wang, et al 2009a) This systematic review fulfilled 5 of 11 criteria of the AMSTAR tool.

In a systematic review and meta-analysis recently conducted by our group, we questioned the role of myeloid growth factors administrated to AML patients concurrent with or post chemotherapy (Gurion, et al., 2011). There was no difference in short term and long term all cause mortality, CR rate, DFS and relapse rate between the arm receiving growth factors and the control arm. Furthermore, the use of myeloid growth factors was not associated with a reduction in the incidence of infections. This systematic review fulfilled 10 of the 11 criteria of the AMSTAR tool.

Another recently published systematic review compared the administration of myeloid growth factors in AML patients receiving chemotherapy to control/placebo (Heuser, et al 2011). Among patients receiving primary prophylaxis, time to neutrophil recovery and hospitalization stay were shorter, yet no difference was shown in CR, event and DFS and overall survival, compared to no prophylaxis. Among patients receiving growth factors for priming, there was also no difference in CR, event free and disease free survival overall survival. This review fulfilled 7 of 11 criteria of the AMSTAR tool.

In another meta-analysis, the use of myeloid growth factors for priming did not affect CR rate, DFS or overall survival (Sung, et al 2009). Subgroup analyses according to type of myeloid growth factors, the timing of administration and patients' age did not affect outcomes. The main limitation of these meta-analyses is their heterogeneity in terms of patients’ characteristics, chemotherapy regimens and trial designs.

To conclude, the main beneficial effects of growth factors are acceleration of neutrophil recovery by 2 to 5 days and a reduction in the length of hospitalization.(Griffin 2001, Inoue, et al 1990, Lemoli, et al 1991, Lowenberg, et al 1988, Park, et al 1989). With regard to priming with growth factors in AML, 2 meta-analyses did not demonstrate a statistical significant effect on remission rate and overall survival and therefore do not support their regular use.

7.2. Prophylactic anti-infectious treatment

Two systematic review and meta-analyses assessed the effect of antibacterial and antifungal prophylaxis in neutropenic patients receiving chemotherapy.

Gafter-Gvili et al. evaluated the use of antibacterial prophylaxis for afebrile neuropenic patients (Gafter-Gvili, et al 2005). The administration of antibacterial prophylaxis reduced all-cause mortality by 33% (95% CI 0.55 to 0.81) in neutropenic patients who received any antibiotic prophylaxis and by 48% (95% CI 0.35 to 0.77) in patients who received quinolones for prophylaxis compared to placebo or no intervention. Also, the occurrence of febrile episodes and bacterial infections decreased significantly. This review fulfilled 10 of 11 criteria of the AMSTAR tool.

Robenshtock et al. evaluated antifungal agents for prophylaxis in neutropenic patients following chemotherapy or after allogeneic HCT (Robenshtok, et al 2007). All-cause mortality was reduced significantly in patients receiving antifungal prophylaxis compared with placebo, no treatment, or non-systemic antifungals (RR 0.84, 95% CI, 0.74 to 0.95). In a subgroup analysis of patients with acute leukemia there was a significant reduction in fungal-related mortality and documented invasive fungal infections, yet there was no difference in mortality. This review fulfilled 10 of 11 criteria of the AMSTAR tool.

7.3 Transfusion support

One systematic review and meta-analysis evaluated the prophylactic use of platelets in patients with hematological malignancies(Stanworth, et al 2004). Three studies compared prophylactic with therapeutic use of platelets. There was no difference in all-cause mortality, or mortality due to hemorrhagic cause. Of note, studies were conducted between 1974-1982 and were small with marked heterogeneity, thus the results of this meta-analysis should be taken with caution. Three prospective studies compared the platelet transfusion thresholds of 10 vs. 20x10⁹ /L. There were no statistically significant differences between the groups with regards to mortality, remission rates, number of participants with severe bleeding events or red cell transfusion requirements.

The main limitation of this review is the inclusion of a limited number of small studies in different three meta-analyses, carrying a potential risk for bias, though no publication bias was reported. This review fulfilled 8 of 11 criteria of the AMSTAR tool.

Recently, two published RCTs compared low dose to high dose prophylactic platelets transfusion (Heddle, et al 2009, Slichter, et al). Both showed no difference in grade 2-4 bleeding incidence between patients allocated to low threshold of platelets administration and no difference between different doses of platelet transfusion. However, one of the studies was prematurely stopped because of 5.2% grade 4 bleeding in the lower dose platelets compared to none in the high dose (Heddle, et al 2009).

Table 4.
Assessment of risk of bias using AMSTAR criteria in systematic reviews of supportive care in acute leukemia

8. Conclusions

The progress made in the last 4 decades in the treatment of patients with acute leukemia is the consequence of a constant process of testing, data compilation and re-testing. Data gathering on a specific question using explicit, preplanned scientific methods to identify select and synthesize all relevant studies is the process of systematic review, which provides the clinician with the best evidence, and should form the basis for rational medical decision-making.

In this chapter we examined the evidence accumulated in various aspects of leukemia management, based on RCTs and systematic reviews and meta-analyses. While in certain areas such as the role of tyrosine kinase inhibitors in Philadelphia positive ALL or allogeneic transplant in adult patients with ALL a consensus could be reached according to the data published so far, many questions are still open in the field of leukemia which warrant conduction of further clinical trials.

References

1. Anonymous 1998 A systematic collaborative overview of randomized trials comparing idarubicin with daunorubicin (or other anthracyclines) as induction therapy for acute myeloid leukaemia. AML Collaborative Group, 1998. Br J Haematol, 103 100 109 .
2. Ashfaq K. Yahaya I. Hyde C. Andronis L. Barton P. Bayliss S. Chen Y. F. 2010 Clinical effectiveness and cost-effectiveness of stem cell transplantation in the management of acute leukaemia: a systematic review. Health Technol Assess, 14, iii-iv, ix-xi, 1 141 .
3. Boissel N. Auclerc M. F. Lheritier V. Perel Y. Thomas X. Leblanc T. Rousselot P. Cayuela J. M. Gabert J. Fegueux N. Piguet C. Huguet-Rigal F. Berthou C. Boiron J. M. Pautas C. Michel G. Fiere D. Leverger G. Dombret H. Baruchel A. 2003 Should adolescents with acute lymphoblastic leukemia be treated as old children or young adults? Comparison of the French FRALLE-93 and LALA-94 trials. J Clin Oncol, 21 774 780 .
4. Bostrom B. C. Sensel M. R. Sather H. N. Gaynon P. S. La M. K. Johnston K. Erdmann G. R. Gold S. Heerema N. A. Hutchinson R. J. Provisor A. J. Trigg M. E. 2003 Dexamethasone versus prednisone and daily oral versus weekly intravenous mercaptopurine for patients with standard-risk acute lymphoblastic leukemia: a report from the Children’s Cancer Group. Blood, 101 3809 3817 .
5. Br Haematol J. 2009 May;145 3 376 88 . Beneficial and harmful effects of anthracyclines in the treatment of childhood acute lymphoblastic leukaemia: a systematic review and meta-analysis. Childhood Acute Lymphoblastic Leukaemia Collaborative Group (CALLCG).
6. Childhood ALL Collaborative Group 1996 Duration and intensity of maintenance chemotherapy in acute lymphoblastic leukaemia: overview of 42 trials involving 12 000 randomised children. Lancet, 347 1783 1788 .
7. Childhood ALL Collaborative Group 2009 Beneficial and harmful effects of anthracyclines in the treatment of childhood acute lymphoblastic leukaemia: a systematic review and meta-analysis. Br J Haematol, 145 376 388 .
8. Clarke M. Gaynon P. Hann I. Harrison G. Masera G. Peto R. Richards S. 2003 CNS-directed therapy for childhood acute lymphoblastic leukemia: Childhood ALL Collaborative Group overview of 43 randomized trials. J Clin Oncol, 21 1798 1809 .
9. Cornelissen J. J. van der Holt B. Verhoef G. E. van’t Veer. M. B. van Oers M. H. Schouten H. C. Ossenkoppele G. Sonneveld P. Maertens J. van Marwijk Kooy. M. Schaafsma M. R. Wijermans P. W. Biesma D. H. Wittebol S. Voogt P. J. Baars J. W. Zachée P. Verdonck L. F. Löwenberg B. Dekker A. W. 2009 Myeloablative allogeneic versus autologous stem cell transplantation in adult patients with acute lymphoblastic leukemia in first remission: a prospective sibling donor versus no-donor comparison. Blood, 113 1375 1382 .
10. Dohner H. Estey E. H. Amadori S. Appelbaum F. R. Buchner T. Burnett A. K. Dombret H. Fenaux P. Grimwade D. Larson R. A. Lo-Coco F. Naoe T. Niederwieser D. Ossenkoppele G. J. Sanz M. A. Sierra J. Tallman M. S. Lowenberg B. Bloomfield C. D. 2010 Diagnosis and management of acute myeloid leukemia in adults: recommendations from an international expert panel, on behalf of the European LeukemiaNet. Blood, 115 453 474 .
11. Duration and intensity 1996. 42 maintenance chemotherapy in acute lymphoblastic leukaemia: overview of 42 trials involving 12 000 randomised children. Childhood ALL Collaborative Group. Lancet 1996;347 9018 1783 8
12. Eden T. O. Pieters R. Richards S. 2010 Systematic review of the addition of vincristine plus steroid pulses in maintenance treatment for childhood acute lymphoblastic leukaemia- an individual patient data meta-analysis involving 5,659 children. Br J Haematol, 149 722 733 .
13. Edlin R. Connock M. Tubeuf S. Round J. Fry-Smith A. Hyde C. Greenheld W. Azacitidine for the treatment of myelodysplastic syndrome, chronic myelomonocytic leukaemia and acute myeloid leukaemia. Health Technol Assess, 14 Suppl 1 69 74 .
14. Escherich G. M. Richards S. Stork L. C. Vora A. J. Meta-analysis of randomised trials comparing thiopurines in childhood acute lymphoblastic leukaemia. Leukemia.
15. Faderl S. Jeha S. Kantarjian H. M. 2003 The biology and therapy of adult acute lymphoblastic leukemia. Cancer, 98 1337 1354 .
16. Fenaux P. Mufti G. J. Hellstrom-Lindberg E. Santini V. Finelli C. Giagounidis A. Schoch R. Gattermann N. Sanz G. List A. Gore S. D. Seymour J. F. Bennett J. M. Byrd J. Backstrom J. Zimmerman L. Mc Kenzie D. Beach C. Silverman L. R. 2009 Efficacy of azacitidine compared with that of conventional care regimens in the treatment of higher-risk myelodysplastic syndromes: a randomised, open-label, phase III study. Lancet Oncol, 10 223 232 .
17. Fernandez H. F. Sun Z. Yao X. Litzow M. R. Luger S. M. Paietta E. M. Racevskis J. Dewald G. W. Ketterling R. P. Bennett J. M. Rowe J. M. Lazarus H. M. Tallman M. S. 2009 Anthracycline dose intensification in acute myeloid leukemia. N Engl J Med, 361 1249 1259 .
18. Fielding A. 2008 The treatment of adults with acute lymphoblastic leukemia. Hematology Am Soc Hematol Educ Program, 381 389 .
19. Fielding A. K. Goldstone A. H. 2008 Allogeneic haematopoietic stem cell transplant in Philadelphia-positive acute lymphoblastic leukaemia. Bone Marrow Transplant, 41 447 453 .
20. Gafter-Gvili A. Fraser A. Paul M. van de Wetering M. Kremer L. Leibovici L. 2005 Antibiotic prophylaxis for bacterial infections in afebrile neutropenic patients following chemotherapy. Cochrane database of systematic reviews, CD004386.
21. Gale R. P. Lazarus H. M. 2011 How helpful are meta-analyses in determining the best therapy of blood diseases? Acta Haematol, 125 91 101 .
22. Gokbuget N. Hoelzer D. 2009 Treatment of adult acute lymphoblastic leukemia. Semin Hematol, 46 64 75 .
23. Goldstone A. H. Richards S. M. Lazarus H. M. MS Tallman Buck. G. Fielding A. K. Burnett A. K. Chopra R. Wiernik P. H. Foroni L. Paietta E. Litzow M. R. Marks D. I. Durrant J. Mc Millan A. Franklin I. M. Luger S. Ciobanu N. Rowe J. M. 2008 n adults with standard-risk acute lymphoblastic leukemia, the greatest benefit is achieved from a matched sibling allogeneic transplantation in first complete remission, and an autologous transplantation is less effective than conventional consolidation/maintenance chemotherapy in all patients: final results of the International ALL Trial (MRC UKALL XII/ECOG E2993). Blood, 111 1827 1833 .
24. Gurion R. Belnik-Plitman Y. Gafter-Gvili A. Paul M. Vidal L. Ben-Bassat I. Shpilberg O Raanani p 2011 Colony-stimulating factors for prevention and treatment of infectious complications in patients with acute myelogenous leukemia. Cochrane Database 34 Syst Rev. 2011 Sep 7;9:CD008238.
25. Griffin J. D. (ed 2001 Hematopoietic growth factor. Lippincott Wiliams & Wilkins, Philadelphia.
26. Hahn T. Wall D. Camitta B. Davies S. Dillon H. Gaynon P. Larson R. A. Parsons S. Seidenfeld J. Weisdorf D. Mc Carthy P. L. Jr 2006 The role of cytotoxic therapy with hematopoietic stem cell transplantation in the therapy of acute lymphoblastic leukemia in adults: an evidence-based review. Biol Blood Marrow Transplant, 12 1 30 .
27. Heddle N. M. Cook R. J. Tinmouth A. Kouroukis C. T. Hervig T. Klapper E. Brandwein J. M. Szczepiorkowski Z. M. Au Buchon. J. P. Barty R. L. Lee K. A. 2009 A randomized controlled trial comparing standard- and low-dose strategies for transfusion of platelets (SToP) to patients with thrombocytopenia. Blood, 113 1564 1573 .
28. Heuser M. Zapf A. Morgan M. Krauter J. Ganser A. 2011 Myeloid growth factors in acute myeloid leukemia: systematic review of randomized controlled trials. Annals of hematology, 90 273 281 .
29. Hoelzer D. Thiel E. Loffler H. Buchner T. Ganser A. Heil G. Koch P. Freund M. Diedrich H. Ruhl H. et al. 1988 Prognostic factors in a multicenter study for treatment of acute lymphoblastic leukemia in adults. Blood, 71 123 131 .
30. Hubel K. Weingart O. Naumann F. Bohlius J. Fresen M. M. Engert A. Wheatley K. 2011 Allogeneic stem cell transplant in adult patients with acute myelogenous leukemia: a systematic analysis of international guidelines and recommendations. Leuk Lymphoma, 52 444 457 .
31. Hunault M. Harousseau J. L. Delain M. Truchan-Graczyk M. Cahn J. Y. Witz F. Lamy T. Pignon B. Jouet J. P. Garidi R. Caillot D. Berthou C. Guyotat D. Sadoun A. Sotto J. J. Lioure B. Casassus P. Solal-Celigny P. Stalnikiewicz L. Audhuy B. Blanchet O. Baranger L. Béné M. C. Ifrah N. Blood 2004 Better outcome of adult acute lymphoblastic leukemia after early genoidentical allogeneic bone marrow transplantation (BMT) than after late high-dose therapy and autologous BMT: a GOELAMS trial. 104 10 3028 3037 .
32. Inoue C. Murate T. Hotta T. Saito H. 1990 Response of leukemic cells to the sequential combination of GM-CSF and G-CSF. International journal of cell cloning, 8 54 62 .
33. Kantarjian H. Thomas D. O’Brien S. Cortes J. Giles F. Jeha S. Bueso-Ramos C. E. Pierce S. Shan J. Koller C. Beran M. Keating M. Freireich E. J. 2004 Long-term follow-up results of hyperfractionated cyclophosphamide, vincristine, doxorubicin, and dexamethasone (Hyper-CVAD), a dose-intensive regimen, in adult acute lymphocytic leukemia. Cancer, 101 2788 2801 .
34. Kern W. Estey E. H. 2006 High-dose cytosine arabinoside in the treatment of acute myeloid leukemia: Review of three randomized trials. Cancer, 107 116 124 .
35. Kimby E. Nygren P. Glimelius B. 2001 A systematic overview of chemotherapy effects in acute myeloid leukaemia. Acta Oncol, 40 231 252 .
36. Koreth J. Schlenk R. Kopecky K. J. Honda S. Sierra J. Djulbegovic B. J. Wadleigh M. De Angelo D. J. Stone R. M. Sakamaki H. Appelbaum F. R. Dohner H. Antin J. H. Soiffer R. J. Cutler C. 2009 Allogeneic stem cell transplantation for acute myeloid leukemia in first complete remission: systematic review and meta-analysis of prospective clinical trials. Jama, 301 2349 2361 .
37. Labar B. Suciu S. Zittoun R. Muus P. Marie J. P. Fillet G. Peetermans M. Stryckmans P. Willemze R. Feremans W. Jaksic B. Bourhis J. H. Burghouts J. P. de Witte T. 2004 Allogeneic stem cell transplantation in acute lymphoblastic leukemia and non-Hodgkin’s lymphoma for patients <or=50 years old in first complete remission: results of the EORTC ALL-3 trial. Haematologica, 89 809 817 .
38. Larson R. A. Dodge R. K. Burns C. P. Lee E. J. Stone R. M. Schulman P. Duggan D. Davey F. R. Sobol R. E. Frankel S. R. et al. 1995 A five-drug remission induction regimen with intensive consolidation for adults with acute lymphoblastic leukemia: cancer and leukemia group B study 8811. Blood, 85 2025 2037 .
39. Lazarus H. M. Richards S. M. Chopra R. Litzow M. R. Burnett A. K. Wiernik P. H. Franklin I. M. Tallman M. S. Cook L. Buck G. Durrant I. J. Rowe J. M. Goldstone A. H. 2006 Central nervous system involvement in adult acute lymphoblastic leukemia at diagnosis: results from the international ALL trial MRC UKALL XII/ECOG E2993. Blood, 108 465 472 .
40. Le Q. H. Thomas X. Ecochard R. Iwaz J. Lheritier V. Michallet M. Fiere D. 2006 Initial and late prognostic factors to predict survival in adult acute lymphoblastic leukaemia. Eur J Haematol, 77 471 479 .
41. Lemoli R. M. Gulati S. C. Strife A. Lambek C. Perez A. Clarkson B. D. 1991 Proliferative response of human acute myeloid leukemia cells and normal marrow enriched progenitor cells to human recombinant growth factors IL-3, GM-CSF and G-CSF alone and in combination. Leukemia : official journal of the Leukemia Society of America, Leukemia Research Fund, U.K, 5 386 391 .
42. Levi I. Grotto I. Yerushalmi R. Ben-Bassat I. Shpilberg O. 2004 Meta-analysis of autologous bone marrow transplantation versus chemotherapy in adult patients with acute myeloid leukemia in first remission. Leuk Res, 28 605 612 .
43. Liberati A. Altman D. G. Tetzlaff J. Mulrow C. Gotzsche P. C. Ioannidis J. P. Clarke M. Devereaux P. J. Kleijnen J. Moher D. 2009 The PRISMA statement for reporting systematic reviews and meta-analyses of studies that evaluate health care interventions: explanation and elaboration. PLoS Med, 6, e1000100.
44. Linker C. Damon L. Ries C. Navarro W. 2002 Intensified and shortened cyclical chemotherapy for adult acute lymphoblastic leukemia. J Clin Oncol, 20 2464 2471 .
45. Lowenberg B. Ossenkoppele G. J. van Putten W. Schouten H. C. Graux C. Ferrant A. Sonneveld P. Maertens J. Jongen-Lavrencic M. von-Toal Lilienfeld. M. Biemond B. J. Vellenga E. van Marwijk Kooy. M. Verdonck L. F. Beck J. Dohner H. Gratwohl A. Pabst T. Verhoef G. 2009 High-dose daunorubicin in older patients with acute myeloid leukemia. N Engl J Med, 361 1235 1248 .
46. Lowenberg B. Salem M. Delwel R. 1988 Effects of recombinant multi-CSF, GM-CSF, G-CSF and M-CSF on the proliferation and maturation of human AML in vitro. Blood cells, 14 539 549 .
47. Mandelli F. Vignetti M. Suciu S. Stasi R. Petti M. C. Meloni G. Muus P. Marmont F. Marie J. P. Labar B. Thomas X. Di Raimondo F. Willemze R. Liso V. Ferrara F. Baila L. Fazi P. Zittoun R. Amadori S. de Witte T. 2009 Daunorubicin versus mitoxantrone versus idarubicin as induction and consolidation chemotherapy for adults with acute myeloid leukemia: the EORTC and GIMEMA Groups Study AML-10. J Clin Oncol, 27 5397 5403 .
48. Nathan P. C. Sung L. Crump M. Beyene J. 2004 Consolidation therapy with autologous bone marrow transplantation in adults with acute myeloid leukemia: a meta-analysis. J Natl Cancer Inst, 96 38 45 .
49. National Cancer Institute. 2006 SEER Cancer Statistics Review (Available at: http://seer.cancer.gov/csr/1975_2006).
50. Oliansky D. M. Appelbaum F. Cassileth P. A. Keating A. Kerr J. Nieto Y. Stewart S. Stone R. M. Tallman M. S. Mc Carthy P. L. Jr Hahn T. 2008 The role of cytotoxic therapy with hematopoietic stem cell transplantation in the therapy of acute myelogenous leukemia in adults: an evidence-based review. Biol Blood Marrow Transplant, 14 137 180 .
51. Omura G. A. Moffitt S. Vogler W. R. Salter M. M. 1980 Combination chemotherapy of adult acute lymphoblastic leukemia with randomized central nervous system prophylaxis. Blood, 55 199 204 .
52. Orsi C. Bartolozzi B. Messori A. Bosi A. 2007, Event-free survival and cost-effectiveness in adult acute lymphoblastic leukaemia in first remission treated with allogeneic transplantation. Bone Marrow Transplant, 40 643 649 .
53. Oxman A. D. Guyatt G. H. 1991 Validation of an index of the quality of review articles. J Clin Epidemiol, 44 1271 1278 .
54. Park L. S. Waldron P. E. Friend D. Sassenfeld H. M. Price V. Anderson D. Cosman D. Andrews R. G. Bernstein I. D. Urdal D. L. 1989 Interleukin-3, GM-CSF, and G-CSF receptor expression on cell lines and primary leukemia cells: receptor heterogeneity and relationship to growth factor responsiveness. Blood, 74 56 65 .
55. Pautas C. Merabet F. Thomas X. Raffoux E. Gardin C. Corm S. Bourhis J. H. Reman O. Turlure P. Contentin N. de Revel T. Rousselot P. Preudhomme C. Bordessoule D. Fenaux P. Terre C. Michallet M. Dombret H. Chevret S. Castaigne S. 2010 Randomized study of intensified anthracycline doses for induction and recombinant interleukin-2 for maintenance in patients with acute myeloid leukemia age 50 to 70 years: results of the ALFA-9801 study. J Clin Oncol, 28 808 814 .
56. Pui C. H. Robison L. L. Look A. T. 2008 Acute lymphoblastic leukaemia. Lancet, 371 1030 1043 .
57. Ram R. Gafter-Gvili A. Shpilberg O. Raanani P. 2011 Allogeneic hematopoietic cell transplantation for adult patients with acute leukemia: the role of meta-analyses. Acta Haematol, 125 39 46 .
58. Ram R. Gafter-Gvili A. Vidal L. Paul M. Ben-Bassat I. Shpilberg O. Raanani P. 2010 Management of adult patients with acute lymphoblastic leukemia in first complete remission: systematic review and meta-analysis. Cancer, 116 3447 3457 .
59. Ram R. Wolach O. Vidal L. Gafter-Gvili A. Shpilberg O. Raanani P. 2011 Adolescents and Young Adults with Acute Lymphoblastic Leukemia Have Better Outcomes When Treated with Pediatric-Inspired Regimens- Systematic Review and Meta-Analysis of Comparative Trials. American Society of Hematology, 2011 Abstract 2591
60. Ramanujachar R. Richards S. Hann I. Goldstone A. Mitchell C. Vora A. Rowe J. Webb D. 2007 Adolescents with acute lymphoblastic leukaemia: outcome on UK national paediatric (ALL97) and adult (UKALLXII/E2993) trials. Pediatr Blood Cancer, 48 254 261 .
61. Rees J. K. Gray R. G. Wheatley K. 1996 Dose intensification in acute myeloid leukaemia: greater effectiveness at lower cost. Principal report of the Medical Research Council’s AML9 study. MRC Leukaemia in Adults Working Party. Br J Haematol, 94 89 98 .
62. Ribera J. M. Oriol A. Bethencourt C. Parody R. Hernández-Rivas J. M. Moreno M. J. del Potro E. Torm M. Rivas C. Besalduch J. Sanz M. A. Ortega J. J. 2005 Comparison of intensive chemotherapy, allogeneic or autologous stem cell transplantation as post-remission treatment for adult patients with high-risk acute lymphoblastic leukemia. Results of the PETHEMA ALL-93 trial. Haematologica, 90 1346 1356 .
63. Robenshtok E. Gafter-Gvili A. Goldberg E. Weinberger M. Yeshurun M. Leibovici L. Paul M. 2007 Antifungal prophylaxis in cancer patients after chemotherapy or hematopoietic stem-cell transplantation: systematic review and meta-analysis. Journal of clinical oncology : official journal of the American Society of Clinical Oncology, 25 5471 5489 .
64. Rowe J. M. Buck G. Burnett A. K. Chopra R. Wiernik P. H. Richards S. M. Lazarus H. M. Franklin I. M. Litzow M. R. Ciobanu N. Prentice H. G. Durrant J. Tallman M. S. Goldstone A. H. 2005 Induction therapy for adults with acute lymphoblastic leukemia: results of more than 1500 patients from the international ALL trial: MRC UKALL XII/ECOG E2993. Blood, 106 3760 3767 .
65. Rowe J. M. Neuberg D. Friedenberg W. Bennett J. M. Paietta E. Makary A. Z. Liesveld J. L. Abboud C. N. Dewald G. Hayes F. A. Tallman M. S. Wiernik P. H. 2004 A phase 3 study of three induction regimens and of priming with GM-CSF in older adults with acute myeloid leukemia: a trial by the Eastern Cooperative Oncology Group. Blood, 103 479 485 .
66. Schlenk R. F. Benner A. Krauter J. Buchner T. Sauerland C. Ehninger G. Schaich M. Mohr B. Niederwieser D. Krahl R. Pasold R. Dohner K. Ganser A. Dohner H. Heil G. 2004 Individual patient data-based meta-analysis of patients aged 16 to 60 years with core binding factor acute myeloid leukemia: a survey of the German Acute Myeloid Leukemia Intergroup. J Clin Oncol, 22 3741 3750 .
67. Shea B. J. Bouter L. M. Peterson J. Boers M. Andersson N. Ortiz Z. Ramsay T. Bai A. Shukla V. K. Grimshaw J. M. 2007 External validation of a measurement tool to assess systematic reviews (AMSTAR). PLoS One, 2, e1350.
68. Shea B. J. Hamel C. Wells G. A. Bouter L. M. Kristjansson E. Grimshaw J. Henry D. A. Boers M. 2009 AMSTAR is a reliable and valid measurement tool to assess the methodological quality of systematic reviews. J Clin Epidemiol, 62 1013 1020 .
69. Silverman L. R. Demakos E. P. Peterson B. L. Kornblith A. B. Holland J. C. Odchimar-Reissig R. Stone R. M. Nelson D. Powell B. L. De Castro C. M. Ellerton J. Larson R. A. Schiffer C. A. Holland J. F. 2002 Randomized controlled trial of azacitidine in patients with the myelodysplastic syndrome: a study of the cancer and leukemia group B. J Clin Oncol, 20 2429 2440 .
70. Slichter S. J. Kaufman R. M. Assmann S. F. Mc Cullough J. Triulzi D. J. Strauss R. G. Gernsheimer T. B. Ness P. M. Brecher M. E. Josephson C. D. Konkle B. A. Woodson R. D. Ortel T. L. Hillyer C. D. Skerrett D. L. Mc Crae K. R. Sloan S. R. Uhl L. George J. N. Aquino V. M. Manno C. S. Mc Farland J. G. Hess J. R. Leissinger C. Granger S. Dose of prophylactic platelet transfusions and prevention of hemorrhage. N Engl J Med, 362 362 600 613 .
71. Stanworth S. J. Hyde C. Heddle N. Rebulla P. Brunskill S. Murphy M. F. 2004 Prophylactic platelet transfusion for haemorrhage after chemotherapy and stem cell transplantation. Cochrane database of systematic reviews, CD004269.
72. Stock W. La M. Sanford B. Bloomfield C. D. Vardiman J. W. Gaynon P. Larson R. A. Nachman J. 2008 What determines the outcomes for adolescents and young adults with acute lymphoblastic leukemia treated on cooperative group protocols? A comparison of Children’s Cancer Group and Cancer and Leukemia Group B studies. Blood, 112 1646 1654 .
73. Sung L. Alibhai S. M. Beyene J. Gamis A. Almeida R. Smith S. Aplenc R. 2009 Hematopoietic colony-stimulating factor priming does not influence survival in acute myeloid leukemia: a meta-analysis of randomized trials. Leukemia : official journal of the Leukemia Society of America, Leukemia Research Fund, U.K, 23 811 813 .
74. Sung L. Nathan P. C. Alibhai S. M. Tomlinson G. A. Beyene J. 2007 Meta-analysis: effect of prophylactic hematopoietic colony-stimulating factors on mortality and outcomes of infection. Annals of internal medicine, 147 400 411 .
75. Thomas D. A. Faderl S. Cortes J. O’Brien S. Giles F. J. Kornblau S. M. Garcia-Manero G. Keating M. J. Andreeff M. Jeha S. Beran M. Verstovsek S. Pierce S. Letvak L. Salvado A. Champlin R. Talpaz M. Kantarjian H. 2004a Treatment of Philadelphia chromosome-positive acute lymphocytic leukemia with hyper-CVAD and imatinib mesylate. Blood, 103 4396 4407 .
76. Thomas X. Boiron J. M. Huguet F. Dombret H. Bradstock K. Vey N. Kovacsovics T. Delannoy A. Fegueux N. Fenaux P. Stamatoullas A. Vernant J. P. Tournilhac O. Buzyn A. Reman O. Charrin C. Boucheix C. Gabert J. Lheritier V. Fiere D. 2004b Outcome of treatment in adults with acute lymphoblastic leukemia: analysis of the LALA-94 trial. J Clin Oncol, 22 4075 4086 .
77. Visani G. Olivieri A. Malagola M. Brunori M. Piccaluga P. P. Capelli D. Pomponio G. Martinelli G. Isidori A. Sparaventi G. Leoni P. 2006 Consolidation therapy for adult acute myeloid leukemia: a systematic analysis according to evidence based medicine. Leuk Lymphoma, 47 1091 1102 .
78. Volger W. R. Weiner R. S. Moore J. O. Omura G. A. Bartolucci A. A. Stagg M. 1995 Long-term follow-up of a randomized post-induction therapy trial in acute myelogenous leukemia (a Southeastern Cancer Study Group trial). Leukemia, 9 1456 1460 .
79. Wang J. An L. Chen S. Ouyang J. Zhou R. Chen B. Yang Y. 2009a Prophylactic use of granulocyte colony-stimulating factor after chemotherapy does not affect survival rate in acute myeloid leukemia: a meta-analysis. Acta haematologica, 121 223 226 .
80. Wang J. Ouyang J. Zhou R. Chen B. Yang Y. 2010 Autologous hematopoietic stem cell transplantation for acute myeloid leukemia in first complete remission: a meta-analysis of randomized trials. Acta Haematol, 124 61 71 .
81. Wang J. Zhan P. Ouyang J. Chen B. Zhou R. 2009b Prophylactic use of granulocyte colony-stimulating factor after induction chemotherapy in patients with newly diagnosed acute myeloid leukemia may increase the complete remission rate: a meta-analysis of five randomised controlled trials. Leukemia & lymphoma, 50 457 459 .
82. Woolf S. H. 2000 Evidence-based medicine and practice guidelines: an overview. Cancer Control, 7 362 367 .
83. Xu S. N. Chen J. P. Liu J. P. Xia Y. 2009a [Arsenic trioxide in combination with all-trans retinoic acid for acute promyelocytic leukemia: a systematic review and meta-analysis]. Zhong Xi Yi Jie He Xue Bao, 7 1024 1034 .
84. Xu S. N. Chen J. P. Liu J. P. Xia Y. 2009b [Efficacy of arsenic trioxide for acute promyelocytic leukemia: a systematic review and meta-analysis]. Zhong Xi Yi Jie He Xue Bao, 7 801 808 .
85. Yanada M. Matsuo K. Suzuki T. Naoe T. 2006, Allogeneic hematopoietic stem cell transplantation as part of postremission therapy improves survival for adult patients with high-risk acute lymphoblastic leukemia: a metaanalysis. Cancer, 106 2657 2663 .
86. Yanada M. Matsuo K. Emi N. Naoe T. 2005 Efficacy of allogeneic hematopoietic stem cell transplantation depends on cytogenetic risk for acute myeloid leukemia in first disease remission: a metaanalysis. Cancer, 103 1652 1658 .

[1] 1. Anonymous 1998 A systematic collaborative overview of randomized trials comparing idarubicin with daunorubicin (or other anthracyclines) as induction therapy for acute myeloid leukaemia. AML Collaborative Group, 1998. Br J Haematol, 103 100 109 .

[2] 2. Ashfaq K. Yahaya I. Hyde C. Andronis L. Barton P. Bayliss S. Chen Y. F. 2010 Clinical effectiveness and cost-effectiveness of stem cell transplantation in the management of acute leukaemia: a systematic review. Health Technol Assess, 14, iii-iv, ix-xi, 1 141 .

[3] 3. Boissel N. Auclerc M. F. Lheritier V. Perel Y. Thomas X. Leblanc T. Rousselot P. Cayuela J. M. Gabert J. Fegueux N. Piguet C. Huguet-Rigal F. Berthou C. Boiron J. M. Pautas C. Michel G. Fiere D. Leverger G. Dombret H. Baruchel A. 2003 Should adolescents with acute lymphoblastic leukemia be treated as old children or young adults? Comparison of the French FRALLE-93 and LALA-94 trials. J Clin Oncol, 21 774 780 .

[4] 4. Bostrom B. C. Sensel M. R. Sather H. N. Gaynon P. S. La M. K. Johnston K. Erdmann G. R. Gold S. Heerema N. A. Hutchinson R. J. Provisor A. J. Trigg M. E. 2003 Dexamethasone versus prednisone and daily oral versus weekly intravenous mercaptopurine for patients with standard-risk acute lymphoblastic leukemia: a report from the Children’s Cancer Group. Blood, 101 3809 3817 .

[5] 5. Br Haematol J. 2009 May;145 3 376 88 . Beneficial and harmful effects of anthracyclines in the treatment of childhood acute lymphoblastic leukaemia: a systematic review and meta-analysis. Childhood Acute Lymphoblastic Leukaemia Collaborative Group (CALLCG).

[6] 6. Childhood ALL Collaborative Group 1996 Duration and intensity of maintenance chemotherapy in acute lymphoblastic leukaemia: overview of 42 trials involving 12 000 randomised children. Lancet, 347 1783 1788 .

[7] 7. Childhood ALL Collaborative Group 2009 Beneficial and harmful effects of anthracyclines in the treatment of childhood acute lymphoblastic leukaemia: a systematic review and meta-analysis. Br J Haematol, 145 376 388 .

[8] 8. Clarke M. Gaynon P. Hann I. Harrison G. Masera G. Peto R. Richards S. 2003 CNS-directed therapy for childhood acute lymphoblastic leukemia: Childhood ALL Collaborative Group overview of 43 randomized trials. J Clin Oncol, 21 1798 1809 .

[9] 9. Cornelissen J. J. van der Holt B. Verhoef G. E. van’t Veer. M. B. van Oers M. H. Schouten H. C. Ossenkoppele G. Sonneveld P. Maertens J. van Marwijk Kooy. M. Schaafsma M. R. Wijermans P. W. Biesma D. H. Wittebol S. Voogt P. J. Baars J. W. Zachée P. Verdonck L. F. Löwenberg B. Dekker A. W. 2009 Myeloablative allogeneic versus autologous stem cell transplantation in adult patients with acute lymphoblastic leukemia in first remission: a prospective sibling donor versus no-donor comparison. Blood, 113 1375 1382 .

[10] 10. Dohner H. Estey E. H. Amadori S. Appelbaum F. R. Buchner T. Burnett A. K. Dombret H. Fenaux P. Grimwade D. Larson R. A. Lo-Coco F. Naoe T. Niederwieser D. Ossenkoppele G. J. Sanz M. A. Sierra J. Tallman M. S. Lowenberg B. Bloomfield C. D. 2010 Diagnosis and management of acute myeloid leukemia in adults: recommendations from an international expert panel, on behalf of the European LeukemiaNet. Blood, 115 453 474 .

[11] 11. Duration and intensity 1996. 42 maintenance chemotherapy in acute lymphoblastic leukaemia: overview of 42 trials involving 12 000 randomised children. Childhood ALL Collaborative Group. Lancet 1996;347 9018 1783 8

[12] 12. Eden T. O. Pieters R. Richards S. 2010 Systematic review of the addition of vincristine plus steroid pulses in maintenance treatment for childhood acute lymphoblastic leukaemia- an individual patient data meta-analysis involving 5,659 children. Br J Haematol, 149 722 733 .

[13] 13. Edlin R. Connock M. Tubeuf S. Round J. Fry-Smith A. Hyde C. Greenheld W. Azacitidine for the treatment of myelodysplastic syndrome, chronic myelomonocytic leukaemia and acute myeloid leukaemia. Health Technol Assess, 14 Suppl 1 69 74 .

[14] 14. Escherich G. M. Richards S. Stork L. C. Vora A. J. Meta-analysis of randomised trials comparing thiopurines in childhood acute lymphoblastic leukaemia. Leukemia.

[15] 15. Faderl S. Jeha S. Kantarjian H. M. 2003 The biology and therapy of adult acute lymphoblastic leukemia. Cancer, 98 1337 1354 .

[16] 16. Fenaux P. Mufti G. J. Hellstrom-Lindberg E. Santini V. Finelli C. Giagounidis A. Schoch R. Gattermann N. Sanz G. List A. Gore S. D. Seymour J. F. Bennett J. M. Byrd J. Backstrom J. Zimmerman L. Mc Kenzie D. Beach C. Silverman L. R. 2009 Efficacy of azacitidine compared with that of conventional care regimens in the treatment of higher-risk myelodysplastic syndromes: a randomised, open-label, phase III study. Lancet Oncol, 10 223 232 .

[17] 17. Fernandez H. F. Sun Z. Yao X. Litzow M. R. Luger S. M. Paietta E. M. Racevskis J. Dewald G. W. Ketterling R. P. Bennett J. M. Rowe J. M. Lazarus H. M. Tallman M. S. 2009 Anthracycline dose intensification in acute myeloid leukemia. N Engl J Med, 361 1249 1259 .

[18] 18. Fielding A. 2008 The treatment of adults with acute lymphoblastic leukemia. Hematology Am Soc Hematol Educ Program, 381 389 .

[19] 19. Fielding A. K. Goldstone A. H. 2008 Allogeneic haematopoietic stem cell transplant in Philadelphia-positive acute lymphoblastic leukaemia. Bone Marrow Transplant, 41 447 453 .

[20] 20. Gafter-Gvili A. Fraser A. Paul M. van de Wetering M. Kremer L. Leibovici L. 2005 Antibiotic prophylaxis for bacterial infections in afebrile neutropenic patients following chemotherapy. Cochrane database of systematic reviews, CD004386.

[21] 21. Gale R. P. Lazarus H. M. 2011 How helpful are meta-analyses in determining the best therapy of blood diseases? Acta Haematol, 125 91 101 .

[22] 22. Gokbuget N. Hoelzer D. 2009 Treatment of adult acute lymphoblastic leukemia. Semin Hematol, 46 64 75 .

[23] 23. Goldstone A. H. Richards S. M. Lazarus H. M. MS Tallman Buck. G. Fielding A. K. Burnett A. K. Chopra R. Wiernik P. H. Foroni L. Paietta E. Litzow M. R. Marks D. I. Durrant J. Mc Millan A. Franklin I. M. Luger S. Ciobanu N. Rowe J. M. 2008 n adults with standard-risk acute lymphoblastic leukemia, the greatest benefit is achieved from a matched sibling allogeneic transplantation in first complete remission, and an autologous transplantation is less effective than conventional consolidation/maintenance chemotherapy in all patients: final results of the International ALL Trial (MRC UKALL XII/ECOG E2993). Blood, 111 1827 1833 .

[24] 24. Gurion R. Belnik-Plitman Y. Gafter-Gvili A. Paul M. Vidal L. Ben-Bassat I. Shpilberg O Raanani p 2011 Colony-stimulating factors for prevention and treatment of infectious complications in patients with acute myelogenous leukemia. Cochrane Database 34 Syst Rev. 2011 Sep 7;9:CD008238.

[25] 25. Griffin J. D. (ed 2001 Hematopoietic growth factor. Lippincott Wiliams & Wilkins, Philadelphia.

[26] 26. Hahn T. Wall D. Camitta B. Davies S. Dillon H. Gaynon P. Larson R. A. Parsons S. Seidenfeld J. Weisdorf D. Mc Carthy P. L. Jr 2006 The role of cytotoxic therapy with hematopoietic stem cell transplantation in the therapy of acute lymphoblastic leukemia in adults: an evidence-based review. Biol Blood Marrow Transplant, 12 1 30 .

[27] 27. Heddle N. M. Cook R. J. Tinmouth A. Kouroukis C. T. Hervig T. Klapper E. Brandwein J. M. Szczepiorkowski Z. M. Au Buchon. J. P. Barty R. L. Lee K. A. 2009 A randomized controlled trial comparing standard- and low-dose strategies for transfusion of platelets (SToP) to patients with thrombocytopenia. Blood, 113 1564 1573 .

[28] 28. Heuser M. Zapf A. Morgan M. Krauter J. Ganser A. 2011 Myeloid growth factors in acute myeloid leukemia: systematic review of randomized controlled trials. Annals of hematology, 90 273 281 .

[29] 29. Hoelzer D. Thiel E. Loffler H. Buchner T. Ganser A. Heil G. Koch P. Freund M. Diedrich H. Ruhl H. et al. 1988 Prognostic factors in a multicenter study for treatment of acute lymphoblastic leukemia in adults. Blood, 71 123 131 .

[30] 30. Hubel K. Weingart O. Naumann F. Bohlius J. Fresen M. M. Engert A. Wheatley K. 2011 Allogeneic stem cell transplant in adult patients with acute myelogenous leukemia: a systematic analysis of international guidelines and recommendations. Leuk Lymphoma, 52 444 457 .

[31] 31. Hunault M. Harousseau J. L. Delain M. Truchan-Graczyk M. Cahn J. Y. Witz F. Lamy T. Pignon B. Jouet J. P. Garidi R. Caillot D. Berthou C. Guyotat D. Sadoun A. Sotto J. J. Lioure B. Casassus P. Solal-Celigny P. Stalnikiewicz L. Audhuy B. Blanchet O. Baranger L. Béné M. C. Ifrah N. Blood 2004 Better outcome of adult acute lymphoblastic leukemia after early genoidentical allogeneic bone marrow transplantation (BMT) than after late high-dose therapy and autologous BMT: a GOELAMS trial. 104 10 3028 3037 .

[32] 32. Inoue C. Murate T. Hotta T. Saito H. 1990 Response of leukemic cells to the sequential combination of GM-CSF and G-CSF. International journal of cell cloning, 8 54 62 .

[33] 33. Kantarjian H. Thomas D. O’Brien S. Cortes J. Giles F. Jeha S. Bueso-Ramos C. E. Pierce S. Shan J. Koller C. Beran M. Keating M. Freireich E. J. 2004 Long-term follow-up results of hyperfractionated cyclophosphamide, vincristine, doxorubicin, and dexamethasone (Hyper-CVAD), a dose-intensive regimen, in adult acute lymphocytic leukemia. Cancer, 101 2788 2801 .

[34] 34. Kern W. Estey E. H. 2006 High-dose cytosine arabinoside in the treatment of acute myeloid leukemia: Review of three randomized trials. Cancer, 107 116 124 .

[35] 35. Kimby E. Nygren P. Glimelius B. 2001 A systematic overview of chemotherapy effects in acute myeloid leukaemia. Acta Oncol, 40 231 252 .

[36] 36. Koreth J. Schlenk R. Kopecky K. J. Honda S. Sierra J. Djulbegovic B. J. Wadleigh M. De Angelo D. J. Stone R. M. Sakamaki H. Appelbaum F. R. Dohner H. Antin J. H. Soiffer R. J. Cutler C. 2009 Allogeneic stem cell transplantation for acute myeloid leukemia in first complete remission: systematic review and meta-analysis of prospective clinical trials. Jama, 301 2349 2361 .

[37] 37. Labar B. Suciu S. Zittoun R. Muus P. Marie J. P. Fillet G. Peetermans M. Stryckmans P. Willemze R. Feremans W. Jaksic B. Bourhis J. H. Burghouts J. P. de Witte T. 2004 Allogeneic stem cell transplantation in acute lymphoblastic leukemia and non-Hodgkin’s lymphoma for patients <or=50 years old in first complete remission: results of the EORTC ALL-3 trial. Haematologica, 89 809 817 .

[38] 38. Larson R. A. Dodge R. K. Burns C. P. Lee E. J. Stone R. M. Schulman P. Duggan D. Davey F. R. Sobol R. E. Frankel S. R. et al. 1995 A five-drug remission induction regimen with intensive consolidation for adults with acute lymphoblastic leukemia: cancer and leukemia group B study 8811. Blood, 85 2025 2037 .

[39] 39. Lazarus H. M. Richards S. M. Chopra R. Litzow M. R. Burnett A. K. Wiernik P. H. Franklin I. M. Tallman M. S. Cook L. Buck G. Durrant I. J. Rowe J. M. Goldstone A. H. 2006 Central nervous system involvement in adult acute lymphoblastic leukemia at diagnosis: results from the international ALL trial MRC UKALL XII/ECOG E2993. Blood, 108 465 472 .

[40] 40. Le Q. H. Thomas X. Ecochard R. Iwaz J. Lheritier V. Michallet M. Fiere D. 2006 Initial and late prognostic factors to predict survival in adult acute lymphoblastic leukaemia. Eur J Haematol, 77 471 479 .

[41] 41. Lemoli R. M. Gulati S. C. Strife A. Lambek C. Perez A. Clarkson B. D. 1991 Proliferative response of human acute myeloid leukemia cells and normal marrow enriched progenitor cells to human recombinant growth factors IL-3, GM-CSF and G-CSF alone and in combination. Leukemia : official journal of the Leukemia Society of America, Leukemia Research Fund, U.K, 5 386 391 .

[42] 42. Levi I. Grotto I. Yerushalmi R. Ben-Bassat I. Shpilberg O. 2004 Meta-analysis of autologous bone marrow transplantation versus chemotherapy in adult patients with acute myeloid leukemia in first remission. Leuk Res, 28 605 612 .

[43] 43. Liberati A. Altman D. G. Tetzlaff J. Mulrow C. Gotzsche P. C. Ioannidis J. P. Clarke M. Devereaux P. J. Kleijnen J. Moher D. 2009 The PRISMA statement for reporting systematic reviews and meta-analyses of studies that evaluate health care interventions: explanation and elaboration. PLoS Med, 6, e1000100.

[44] 44. Linker C. Damon L. Ries C. Navarro W. 2002 Intensified and shortened cyclical chemotherapy for adult acute lymphoblastic leukemia. J Clin Oncol, 20 2464 2471 .

[45] 45. Lowenberg B. Ossenkoppele G. J. van Putten W. Schouten H. C. Graux C. Ferrant A. Sonneveld P. Maertens J. Jongen-Lavrencic M. von-Toal Lilienfeld. M. Biemond B. J. Vellenga E. van Marwijk Kooy. M. Verdonck L. F. Beck J. Dohner H. Gratwohl A. Pabst T. Verhoef G. 2009 High-dose daunorubicin in older patients with acute myeloid leukemia. N Engl J Med, 361 1235 1248 .

[46] 46. Lowenberg B. Salem M. Delwel R. 1988 Effects of recombinant multi-CSF, GM-CSF, G-CSF and M-CSF on the proliferation and maturation of human AML in vitro. Blood cells, 14 539 549 .

[47] 47. Mandelli F. Vignetti M. Suciu S. Stasi R. Petti M. C. Meloni G. Muus P. Marmont F. Marie J. P. Labar B. Thomas X. Di Raimondo F. Willemze R. Liso V. Ferrara F. Baila L. Fazi P. Zittoun R. Amadori S. de Witte T. 2009 Daunorubicin versus mitoxantrone versus idarubicin as induction and consolidation chemotherapy for adults with acute myeloid leukemia: the EORTC and GIMEMA Groups Study AML-10. J Clin Oncol, 27 5397 5403 .

[48] 48. Nathan P. C. Sung L. Crump M. Beyene J. 2004 Consolidation therapy with autologous bone marrow transplantation in adults with acute myeloid leukemia: a meta-analysis. J Natl Cancer Inst, 96 38 45 .

[49] 49. National Cancer Institute. 2006 SEER Cancer Statistics Review (Available at: http://seer.cancer.gov/csr/1975_2006).

[50] 50. Oliansky D. M. Appelbaum F. Cassileth P. A. Keating A. Kerr J. Nieto Y. Stewart S. Stone R. M. Tallman M. S. Mc Carthy P. L. Jr Hahn T. 2008 The role of cytotoxic therapy with hematopoietic stem cell transplantation in the therapy of acute myelogenous leukemia in adults: an evidence-based review. Biol Blood Marrow Transplant, 14 137 180 .

[51] 51. Omura G. A. Moffitt S. Vogler W. R. Salter M. M. 1980 Combination chemotherapy of adult acute lymphoblastic leukemia with randomized central nervous system prophylaxis. Blood, 55 199 204 .

[52] 52. Orsi C. Bartolozzi B. Messori A. Bosi A. 2007, Event-free survival and cost-effectiveness in adult acute lymphoblastic leukaemia in first remission treated with allogeneic transplantation. Bone Marrow Transplant, 40 643 649 .

[53] 53. Oxman A. D. Guyatt G. H. 1991 Validation of an index of the quality of review articles. J Clin Epidemiol, 44 1271 1278 .

[54] 54. Park L. S. Waldron P. E. Friend D. Sassenfeld H. M. Price V. Anderson D. Cosman D. Andrews R. G. Bernstein I. D. Urdal D. L. 1989 Interleukin-3, GM-CSF, and G-CSF receptor expression on cell lines and primary leukemia cells: receptor heterogeneity and relationship to growth factor responsiveness. Blood, 74 56 65 .

[55] 55. Pautas C. Merabet F. Thomas X. Raffoux E. Gardin C. Corm S. Bourhis J. H. Reman O. Turlure P. Contentin N. de Revel T. Rousselot P. Preudhomme C. Bordessoule D. Fenaux P. Terre C. Michallet M. Dombret H. Chevret S. Castaigne S. 2010 Randomized study of intensified anthracycline doses for induction and recombinant interleukin-2 for maintenance in patients with acute myeloid leukemia age 50 to 70 years: results of the ALFA-9801 study. J Clin Oncol, 28 808 814 .

[56] 56. Pui C. H. Robison L. L. Look A. T. 2008 Acute lymphoblastic leukaemia. Lancet, 371 1030 1043 .

[57] 57. Ram R. Gafter-Gvili A. Shpilberg O. Raanani P. 2011 Allogeneic hematopoietic cell transplantation for adult patients with acute leukemia: the role of meta-analyses. Acta Haematol, 125 39 46 .

[58] 58. Ram R. Gafter-Gvili A. Vidal L. Paul M. Ben-Bassat I. Shpilberg O. Raanani P. 2010 Management of adult patients with acute lymphoblastic leukemia in first complete remission: systematic review and meta-analysis. Cancer, 116 3447 3457 .

[59] 59. Ram R. Wolach O. Vidal L. Gafter-Gvili A. Shpilberg O. Raanani P. 2011 Adolescents and Young Adults with Acute Lymphoblastic Leukemia Have Better Outcomes When Treated with Pediatric-Inspired Regimens- Systematic Review and Meta-Analysis of Comparative Trials. American Society of Hematology, 2011 Abstract 2591

[60] 60. Ramanujachar R. Richards S. Hann I. Goldstone A. Mitchell C. Vora A. Rowe J. Webb D. 2007 Adolescents with acute lymphoblastic leukaemia: outcome on UK national paediatric (ALL97) and adult (UKALLXII/E2993) trials. Pediatr Blood Cancer, 48 254 261 .

[61] 61. Rees J. K. Gray R. G. Wheatley K. 1996 Dose intensification in acute myeloid leukaemia: greater effectiveness at lower cost. Principal report of the Medical Research Council’s AML9 study. MRC Leukaemia in Adults Working Party. Br J Haematol, 94 89 98 .

[62] 62. Ribera J. M. Oriol A. Bethencourt C. Parody R. Hernández-Rivas J. M. Moreno M. J. del Potro E. Torm M. Rivas C. Besalduch J. Sanz M. A. Ortega J. J. 2005 Comparison of intensive chemotherapy, allogeneic or autologous stem cell transplantation as post-remission treatment for adult patients with high-risk acute lymphoblastic leukemia. Results of the PETHEMA ALL-93 trial. Haematologica, 90 1346 1356 .

[63] 63. Robenshtok E. Gafter-Gvili A. Goldberg E. Weinberger M. Yeshurun M. Leibovici L. Paul M. 2007 Antifungal prophylaxis in cancer patients after chemotherapy or hematopoietic stem-cell transplantation: systematic review and meta-analysis. Journal of clinical oncology : official journal of the American Society of Clinical Oncology, 25 5471 5489 .

[64] 64. Rowe J. M. Buck G. Burnett A. K. Chopra R. Wiernik P. H. Richards S. M. Lazarus H. M. Franklin I. M. Litzow M. R. Ciobanu N. Prentice H. G. Durrant J. Tallman M. S. Goldstone A. H. 2005 Induction therapy for adults with acute lymphoblastic leukemia: results of more than 1500 patients from the international ALL trial: MRC UKALL XII/ECOG E2993. Blood, 106 3760 3767 .

[65] 65. Rowe J. M. Neuberg D. Friedenberg W. Bennett J. M. Paietta E. Makary A. Z. Liesveld J. L. Abboud C. N. Dewald G. Hayes F. A. Tallman M. S. Wiernik P. H. 2004 A phase 3 study of three induction regimens and of priming with GM-CSF in older adults with acute myeloid leukemia: a trial by the Eastern Cooperative Oncology Group. Blood, 103 479 485 .

[66] 66. Schlenk R. F. Benner A. Krauter J. Buchner T. Sauerland C. Ehninger G. Schaich M. Mohr B. Niederwieser D. Krahl R. Pasold R. Dohner K. Ganser A. Dohner H. Heil G. 2004 Individual patient data-based meta-analysis of patients aged 16 to 60 years with core binding factor acute myeloid leukemia: a survey of the German Acute Myeloid Leukemia Intergroup. J Clin Oncol, 22 3741 3750 .

[67] 67. Shea B. J. Bouter L. M. Peterson J. Boers M. Andersson N. Ortiz Z. Ramsay T. Bai A. Shukla V. K. Grimshaw J. M. 2007 External validation of a measurement tool to assess systematic reviews (AMSTAR). PLoS One, 2, e1350.

[68] 68. Shea B. J. Hamel C. Wells G. A. Bouter L. M. Kristjansson E. Grimshaw J. Henry D. A. Boers M. 2009 AMSTAR is a reliable and valid measurement tool to assess the methodological quality of systematic reviews. J Clin Epidemiol, 62 1013 1020 .

[69] 69. Silverman L. R. Demakos E. P. Peterson B. L. Kornblith A. B. Holland J. C. Odchimar-Reissig R. Stone R. M. Nelson D. Powell B. L. De Castro C. M. Ellerton J. Larson R. A. Schiffer C. A. Holland J. F. 2002 Randomized controlled trial of azacitidine in patients with the myelodysplastic syndrome: a study of the cancer and leukemia group B. J Clin Oncol, 20 2429 2440 .

[70] 70. Slichter S. J. Kaufman R. M. Assmann S. F. Mc Cullough J. Triulzi D. J. Strauss R. G. Gernsheimer T. B. Ness P. M. Brecher M. E. Josephson C. D. Konkle B. A. Woodson R. D. Ortel T. L. Hillyer C. D. Skerrett D. L. Mc Crae K. R. Sloan S. R. Uhl L. George J. N. Aquino V. M. Manno C. S. Mc Farland J. G. Hess J. R. Leissinger C. Granger S. Dose of prophylactic platelet transfusions and prevention of hemorrhage. N Engl J Med, 362 362 600 613 .

[71] 71. Stanworth S. J. Hyde C. Heddle N. Rebulla P. Brunskill S. Murphy M. F. 2004 Prophylactic platelet transfusion for haemorrhage after chemotherapy and stem cell transplantation. Cochrane database of systematic reviews, CD004269.

[72] 72. Stock W. La M. Sanford B. Bloomfield C. D. Vardiman J. W. Gaynon P. Larson R. A. Nachman J. 2008 What determines the outcomes for adolescents and young adults with acute lymphoblastic leukemia treated on cooperative group protocols? A comparison of Children’s Cancer Group and Cancer and Leukemia Group B studies. Blood, 112 1646 1654 .

[73] 73. Sung L. Alibhai S. M. Beyene J. Gamis A. Almeida R. Smith S. Aplenc R. 2009 Hematopoietic colony-stimulating factor priming does not influence survival in acute myeloid leukemia: a meta-analysis of randomized trials. Leukemia : official journal of the Leukemia Society of America, Leukemia Research Fund, U.K, 23 811 813 .

[74] 74. Sung L. Nathan P. C. Alibhai S. M. Tomlinson G. A. Beyene J. 2007 Meta-analysis: effect of prophylactic hematopoietic colony-stimulating factors on mortality and outcomes of infection. Annals of internal medicine, 147 400 411 .

[75] 75. Thomas D. A. Faderl S. Cortes J. O’Brien S. Giles F. J. Kornblau S. M. Garcia-Manero G. Keating M. J. Andreeff M. Jeha S. Beran M. Verstovsek S. Pierce S. Letvak L. Salvado A. Champlin R. Talpaz M. Kantarjian H. 2004a Treatment of Philadelphia chromosome-positive acute lymphocytic leukemia with hyper-CVAD and imatinib mesylate. Blood, 103 4396 4407 .

[76] 76. Thomas X. Boiron J. M. Huguet F. Dombret H. Bradstock K. Vey N. Kovacsovics T. Delannoy A. Fegueux N. Fenaux P. Stamatoullas A. Vernant J. P. Tournilhac O. Buzyn A. Reman O. Charrin C. Boucheix C. Gabert J. Lheritier V. Fiere D. 2004b Outcome of treatment in adults with acute lymphoblastic leukemia: analysis of the LALA-94 trial. J Clin Oncol, 22 4075 4086 .

[77] 77. Visani G. Olivieri A. Malagola M. Brunori M. Piccaluga P. P. Capelli D. Pomponio G. Martinelli G. Isidori A. Sparaventi G. Leoni P. 2006 Consolidation therapy for adult acute myeloid leukemia: a systematic analysis according to evidence based medicine. Leuk Lymphoma, 47 1091 1102 .

[78] 78. Volger W. R. Weiner R. S. Moore J. O. Omura G. A. Bartolucci A. A. Stagg M. 1995 Long-term follow-up of a randomized post-induction therapy trial in acute myelogenous leukemia (a Southeastern Cancer Study Group trial). Leukemia, 9 1456 1460 .

[79] 79. Wang J. An L. Chen S. Ouyang J. Zhou R. Chen B. Yang Y. 2009a Prophylactic use of granulocyte colony-stimulating factor after chemotherapy does not affect survival rate in acute myeloid leukemia: a meta-analysis. Acta haematologica, 121 223 226 .

[80] 80. Wang J. Ouyang J. Zhou R. Chen B. Yang Y. 2010 Autologous hematopoietic stem cell transplantation for acute myeloid leukemia in first complete remission: a meta-analysis of randomized trials. Acta Haematol, 124 61 71 .

[81] 81. Wang J. Zhan P. Ouyang J. Chen B. Zhou R. 2009b Prophylactic use of granulocyte colony-stimulating factor after induction chemotherapy in patients with newly diagnosed acute myeloid leukemia may increase the complete remission rate: a meta-analysis of five randomised controlled trials. Leukemia & lymphoma, 50 457 459 .

[82] 82. Woolf S. H. 2000 Evidence-based medicine and practice guidelines: an overview. Cancer Control, 7 362 367 .

[83] 83. Xu S. N. Chen J. P. Liu J. P. Xia Y. 2009a [Arsenic trioxide in combination with all-trans retinoic acid for acute promyelocytic leukemia: a systematic review and meta-analysis]. Zhong Xi Yi Jie He Xue Bao, 7 1024 1034 .

[84] 84. Xu S. N. Chen J. P. Liu J. P. Xia Y. 2009b [Efficacy of arsenic trioxide for acute promyelocytic leukemia: a systematic review and meta-analysis]. Zhong Xi Yi Jie He Xue Bao, 7 801 808 .

[85] 85. Yanada M. Matsuo K. Suzuki T. Naoe T. 2006, Allogeneic hematopoietic stem cell transplantation as part of postremission therapy improves survival for adult patients with high-risk acute lymphoblastic leukemia: a metaanalysis. Cancer, 106 2657 2663 .

[86] 86. Yanada M. Matsuo K. Emi N. Naoe T. 2005 Efficacy of allogeneic hematopoietic stem cell transplantation depends on cytogenetic risk for acute myeloid leukemia in first disease remission: a metaanalysis. Cancer, 103 1652 1658 .