Open access

Gene Therapy in Urology

Written By

Ratha Mahendran, Sin Mun Tham and Kesavan Esuvaranathan

Submitted: 18 November 2010 Published: 23 August 2011

DOI: 10.5772/22235

From the Edited Volume

Gene Therapy Applications

Edited by Chunsheng Kang

Chapter metrics overview

2,963 Chapter Downloads

View Full Metrics

1. Introduction

The application of gene therapy in the field of Urology is not limited to cancer therapy but is also being evaluated for non-cancer related bladder dysfunctions as well as erectile dysfunction (ED). This article will review the use of gene therapy for these conditions; the vectors used and limitations associated with different gene delivery systems and the attempts to overcome these shortcomings.

Advertisement

2. Bladder cancer

Bladder cancer is the 7th most common cancer worldwide. It has a natural history of superficial recurrences and local progression. It is estimated that within 18 months of first diagnosis approximately 50% of patients will have a recurrence (Anderson & Naish 2008). Thus there is a need for frequent monitoring of these patients. In the US the estimated life-time cost of therapy for bladder cancer patients with non-muscle invasive disease was US $21.03 million based on a Medicare database (Cooksley et al. 2008). The majority of this is spent on surveillance and the treatment of recurrences. Tumors occur on the luminal surface of the bladder and the architecture of the bladder permits topical intravesical therapies. The bladder is isolated from other organs and tissues and intravesical therapy permits contact with the entire internal surface of the bladder with minimal systemic side-effects.

The present gold standard therapy for superficial bladder cancers is immunotherapy with Mycobacterium bovis, Bacillus Calmette Guerin (BCG) following local transurethral resection of the bladder tumor (TURBT). BCG induces a mononuclear and neutrophilic infiltrate in the bladder wall which results in an inflammatory response as measured by cytokine production that causes sloughing of both tumor and normal cells (Herr and Morales 2008). The presence of IL-2, IL-8 and IL-18 in the urine of patients has been reported to correlate with response to therapy (Thalmann et al. 1997; Thalmann et al. 2000; Saint et al. 2003). Unfortunately, BCG has several shortcomings: it is a live vaccine and commonly causes side effects and occasionally septicemia. In addition some patients (20-42%) do not respond to therapy (Kamat and Lamm 2000). In place of BCG, recombinant cytokines such as IFN-, TNF-, and IL-2 have been used in a number of clinical trials with encouraging results (Glazier et al. 1995; Den Otter et al. 1998; Stavropoulos et al. 2002). However, recombinant cytokines are costly, unstable in urine and have poor permeability across the glycosaminoglycan (GAG) layer of the urothelium. Gene therapy is a natural alternative approach to ensure cytokine production in the bladder environment.

2.1. Viral transfection systems for bladder cancer

Initially replication defective viruses were generated with the sole purpose of gene delivery (Thomas et al. 2003). The viruses evaluated included: Adenovirus (type 2 and 5), Adeno-associated virus (Parvoviridae family), Herpes simplex virus, Retrovirus (Dumey et al. 2005), Canary pox virus and Vaccinia virus (Lee et al. 1994). Table 1 lists their characteristics.

However, because of the limited transduction capability of some viruses, replicating and conditionally replicating viruses were developed. These viruses amplify the transfection efficiency, as virus transduced cells produce more viruses that can infect the surrounding cells. Replication of wild type viruses also induces cytolysis of infected cells.

2.1.1. Limitations and Improvements

2.1.1.1. Non-specificity of transfection

Siemens et al. compared adeno-, canary pox and vaccinia viruses in terms of their ability to transfect tumor cells after intravesical delivery in a murine model of bladder cancer (Siemens et al. 2003). The vaccinia and avian pox viruses were better at transfecting tumor cells than adenoviruses but all three resulted in transfection of extravesical tissue (e.g. kidney, liver, spleen). In contrast Wood et al reported only sporadic extravesical transfection after intravesical adenovirus instillations (Wood et al. 1999).

To reduce non specific viral transduced gene expression, oncolytic adenoviruses have been engineered to express the E1A and E1B genes under the control of the uroplankin II gene promoter (Zhang et al. 2002; He et al. 2009) which limits expression to urothelial cells. Another strategy to target viral replication to tumor cells is to place the adenovirus E1A gene under the control of the telomerase promoter (Lanson et al. 2003), the midkine gene promoter (Terao et al. 2007) or the Cox-2 promoter (Shirakawa et al. 2004). All these genes are highly expressed in tumor cells.

Bladder cancer cells often over-express the epidermal growth factor receptor (EGFR) and targeting EGFR with bi-specific antibodies improved the delivery of adenovirus to cancer cells (van der Poel et al. 2002). A gammaretrovirus carrying a chimeric envelope protein containing a single chain variable fragment (scFv) antibody to the human epidermal growth factor receptor 2 (HER2) was shown to specifically target cells expressing Her2 (Tsai et al. 2010).

2.1.1.2. Transfection efficiency

The internal surface of the bladder is covered by uroplakin proteins and the GAG layer which together provide a barrier to transfection of urothelial cells. Agents that disrupt this protective layer such as ethanol, HCl, dodecyl-B-d-maltoside and sodium dodecyl sulphate have been shown to improve viral transduction of the bladder (Engler et al. 1999; Lin et al. 2002; Ramesh et al. 2004).

Though adenoviruses are the most popular viruses for gene therapy they require adhesion with the cellular coxsackie-adenoviral receptor (CAR) for transduction of mammalian cells. Neoplastic tissue unlike normal bladder cells have reduced CAR expression (Buscarini et al. 2007) as a result of epigenetic control mechanisms (Pong et al. 2003).

VirusTransfection efficiencyImmunogenicityDNA insertsGene expression
AdenovirusHigh with CAR receptorhigh8kbTransient expression, DNA remains episomal
Adeno-associated virusGood, no receptorlow4.5kbStable, DNA episomes found
Herpes simplex virusHigh in neuronshigh"/>30kbStable in neurons and transient in others, episomal
Moloney murine leukemia virusHigh in dividing cellslow8kbStable expression, DNA integration into host genome
Hematopoietic cells
LentivirusNon dividing cellslow8kbStable expression, Integration in host chromosome,
Canary pox virusMost cellslow25kbTransient expression, Viral DNA limited to cytoplasm
Vaccinia virusMost cellshighUp to 25kbTransient expression, Viral DNA limited to cytoplasm

Table 1.

Characteristics of viral vectors for gene therapy

To circumvent the need for receptor mediated uptake, polymers have been used to enhance adenovirus transfection of bladder cells (Kasman et al. 2009) or even small molecule excipients such as Syn3 (Connor et al. 2001; Yamashita et al. 2002; Nagabhushan et al. 2007). A recent study has shown that CAR receptor expression and thus adenoviral expression can be increased by treatment with histone deacetylase inhibitors (HDACI) such as trichostatin A and sodium phenylbutyrate (Sachs et al. 2004).

2.1.1.3. Previous Immunity

Vaccinia viruses have long been used in man as vaccines against smallpox. This raised the issue of whether previous immunization would block the effectiveness of these viruses as gene delivery vehicles. Intravesical instillation of vaccinia viruses was successfully demonstrated in pre-immunized mice (Lee et al. 1994). The immunogenicity of adenoviruses is a major limitation in most therapeutic strategies. However it may be advantageous in bladder cancer therapy where non-specific inflammation as a consequence of BCG instillation has been associated with tumor removal.

2.1.1.4. Promoter inactivation

Adenovirus genes expressed from a CMV promoter induced better gene expression than those expressed using a RSV promoter (Freund et al. 2000). But quite often the CMV promoter is inactivated in vivo. It has been found that adenoviral transfection together with HDAC inhibitor trichostatin or retinoic acid improved CMV promoter activity. Treatment with these drugs could improve and prolong adenoviral transgene expression (Gaetano et al 2000). The development of tissue specific promoters as described above may resolve this problem.

2.2. Non-viral transfection systems for bladder cancer

The strength and weakness of non-viral vectors is the transient expression of the delivered genes. For non-viral gene delivery the genes are encoded on plasmid DNA of bacterial origin. Non-viral delivery agents include liposomes (N-[1-(2,3-Dioleoyloxy)propyl]-N,N,N-trimethylammonium chloride, DOTAP), polyethylenimine (PEI), viral envelopes (with fusogenic properties) conjugated to liposomes (Hemagglutinating Virus of Japan (HVJ) liposomes), chitosans as well as physical means such as the use of an electrogun or ultrasound (Harimoto et al. 1998; Lawrencia et al. 2001; Ogawa et al. 2004; Bonnet et al. 2008; Tsai et al. 2009; Zaharoff et al. 2009). Plasmid DNA delivery systems result in cellular entry via the endosomes (Al-Dosari & Gao 2009). Endosomal escape is often difficult and when successful the plasmid DNA is mainly restricted to the cytoplasm. A small amount may make it to the nucleus and exist as episomal DNA molecules that can be lost during replication (Al-Dosari & Gao 2009). Besides the delivery agents, the plasmid DNA sequence can also modulate the efficiency of transfection as discussed below.

2.2.1. Limitations and Improvements

2.2.1.1. Promoter inactivation

It has been reported that the CMV promoter often used for plasmid gene expression does not always result in good gene expression (Loser et al. 1998) as a consequence of promoter inactivation. This can be overcome by using a HDAC inhibitor, as demonstrated with OSU-HDAC42 (Lai et al. 2010). An alternative strategy is to utilize tissue/cancer cell specific promoters such as the COX-2, H19 and human IGF2-P4 gene promoters (Ohana et al. 2002; Zhang et al. 2008; Amit & Hochberg 2010).

2.2.1.2. Transfection efficiency

The primary focus of improving plasmid DNA transfection is improving escape from the endosomes and this is achieved by developing new additives and lipoplexes or even polyplexes that use either acidification or osmotic pressure changes or membrane fusogenic molecules to allow DNA escape (Al-Dosari and Gao 2009). We developed a formulation comprised of DOTAP and Methyl--cyclodextrin solubilized cholesterol (MBC) that transfects urothelial cells in vivo within 2 hours of exposure. Transfection was confined to the bladder (Lawrencia et al. 2001) and occurred in the superficial and deeper layers of the urothelial tumours (Wu et al. 2003).

2.2.1.3 Specificity of plasmid expression and activity/duration

Antibodies have been used to target delivery of plasmids to tumor cells. ScFv antibody to Her-2 (Tsai et al. 2009) or transferrin have been demonstrated to successfully target plasmids to tumor cells (Pirollo et al. 2008). The latter strategy targets both primary and metastatic disease when delivered systemically. Targeting of plasmid DNA to the nucleus can also be induced by introducing mammalian transcription factor binding sites in the plasmid and this increased the duration of expression (Gill et al. 2009).

Plasmid DNA expression is transient because of the episomal nature of transfected DNA. In bladder cancer therapy this can be overcome by repeated intravesical instillations. Another strategy to improve gene expression is to add a scaffold matrix attachment region (S/MAR) to the plasmid DNA. S/MAR serve both to ensure prolonged gene expression, by reducing the silencing of plasmid DNA as well as to ensure plasmid DNA replication as episomes (Gill et al. 2009).

Integration of plasmid DNA into chromosomal DNA is achievable now. The techniques used include retroviral integrase (Tanaka et al. 1998), sleeping beauty (SB) transposons (Hackett et al. 2010) or phage recombinase mediated integration (Olivares et al. 2002). Thus in the future a single intravesical instillation may be sufficient for prolonged therapeutic effects.

2.2.1.4. Liposome free delivery

For small molecules such as CpG oligodeoxynucleotides (ODN), intravesical delivery to urothelial cells can be achieved without a transfection agent (Ninalga et al. 2005). But plasmid DNA requires a delivery agent. Nanoparticles (10-100nm in size) with bound plasmid DNA are recognized by cell surface nucleolin on HeLa cells and this results in DNA transport to the nucleus (Chen et al. 2008) and avoidance of endosomal entrapment.

2.2.1.5. Inflammation

The CpG sequences on plasmid DNA induce inflammation that could reduce gene expression by either destruction of transfected cells or promoter inactivation (Yew et al. 2000). Minicircle DNA (mcDNA), are supercoiled DNA with only the therapeutic gene cassette. They are generated in vivo by site specific recombination in E coli and exhibit improved gene expression in terms of the level and duration of gene expression (Darquet et al. 1997).

2.3. Preclinical evaluation of genes and evolving gene therapy strategies

The different categories of genes used successfully in animal studies are listed in Table 2. Both Sub-cutaneous (sc) and orthotopic models of bladder cancer have been used to evaluate gene therapy. While the data from sc studies have shown the efficacy of the expressed genes, it is the orthotopic models that best reflect clinical disease and therapeutic gene delivery. In general regardless of the delivery system or gene delivered tumor growth reduction or even eradication has been reported in murine models of bladder cancer. Most therapeutic schedules used in the animal studies require repeated instillations of the gene delivery vehicle whether it is a viral or non-viral vector. However, a recent study of viral gene delivery of IFN indicated that a high dose could reduce the need for increased intravesical instillations (Tao et al. 2006). Transfection using transposons may also reduce the need for repeated transfection of plasmid DNA.

New therapies aim to combine several strategies at once. These include the use of oncolytic viruses and immune modulation using GMCSF (Cozzi et al. 2001; Ramesh et al. 2006); wild type p53 and ribozyme erb-2 (Irie et al. 2006) and Rb94 or oncolytic viruses and chemotherapeutic drugs (Zhang et al. 2002; Pirollo et al. 2008). In vitro studies have shown that combining AdHSVTK, ganciclovir and chemotherapy may have therapeutic benefit (Freund et al. 2003). Further the beneficial effect of 5-FU and adenovirus cytosine deaminase gene therapy could be enhanced by irradiation (Zhang et al. 2003). Such multi-factor therapies may be better at eradicating tumor cells. Another strategy is to modify immune cells in vitro for cancer therapy. Dendritic cell manipulation by transfection with adenovirus carrying the survivin gene has been shown to induce cytotoxic T lymphocytes ( CTLs) (Kikkawa et al. 2009).

2.4. Gene therapy clinical trials

Table 3 lists several Phase I trials that have been carried out for bladder cancer. However, results from only a few of these trials are published.

Table 2.

Genes demonstrated to cause tumor reduction in murine models of bladder cancer.

Table 3.

Clinical trials for bladder cancer gene therapy. NCT designation indicates data obtained from http://www.who.int/ictrp/en/; Other alphabet and number designations are for data obtained from http://www.wiley.com/legacy/wileychi/genmed/clinical where the alphabets indicate country of registration and the numbers only designation are for data obtained from http://www.gemcris.od.nih.gov/Contents/GC_HOME.asp. Note some trials were registered on more than one web-site.

Information about completed, on-going and planned trials were obtained from the following sources: gene therapy clinical trials world wide web-site http://www.wiley.com /legacy/wileychi/genmed/clinical/; the clinical trials.gov, US National Institutes of Health and the Genetic Modification Clinical research Information System database http://www.gemcris.od.nih.gov/Contents/GC_HOME.asp and the World Health Organization International Clinical Trials registry platform portal http://www.who.int /ictrp/en/.

A Phase I trial on vaccinia virus instillation showed increased lymphocyte recruitment and the induction of an inflammatory response in the bladder (Gomella et al. 2001). There were no clinical manifestations of vaccinia toxicity indicating the safety and therapeutic potential of this virus as a gene therapy vector. Adenovirus delivery of p53 was also shown to successfully deliver p53 gene to bladder cells but there was no change in immunohistochemical detection of p53 in bladder tissue (Pagliaro et al. 2003). However, adenovirus therapy was safe and well tolerated (Pagliaro et al. 2003). Delivery of adenovirus carrying p53 with a transduction enhancing agent improved p53 gene delivery and protein expression was found in patient tissue samples (Kuball et al. 2002). Though higher doses of the virus were administered, no dose toxicity was observed (Kuball et al. 2002). Similarly no serious adverse effects were reported by Malmstrom et al. from a recently concluded Phase I/IIa trial using AdCD40L (Malmstrom et al. 2010). They observed gene transfer in biopsies and the infiltration of T lymphocytes (Malmstrom et al. 2010).

A plasmid was used to deliver the diphtheria toxin gene under the control of the H19 gene regulatory sequence in a Phase I/IIa trial for non–muscle invasive bladder cancer (Sidi et al. 2008). They reported mild toxicity and observed complete and partial response in some patients. Thus based on these Phase I trials, both non viral and viral vectors appear to be well tolerated in man.

Several new trials are either in progress or about to commence. These use non-viral and viral delivery vectors as listed in Table 3. A proposal for a Phase I trial for intravesical therapy in bladder cancer patients using plasmid DNA carrying the IFN- gene and our liposome based delivery system is being evaluated by the Health Sciences Authority, Singapore.

2.5. Other urological malignancies

Though not covered here several clinical trials are on-going, evaluating gene therapy for prostate and renal cancers. In general the vectors and genes used are similar though tissue specific promoters may differ. Information on these trials can be obtained from the web-sites listed above. Unlike bladder cancer however, gene delivery to these tissues is not as simple. Thus tissue specific targeted gene expression has been developed. Another strategy is the use of macrophages transfected ex vivo with a plasmid carrying the E1A/B construct under the control of the hypoxia response element (HRE) as well as a replication competent adenovirus with the E1A under the control of the prostate specific antigen promoter. At the hypoxic tumor site the E1A protein is produced and the adenoviruses released infect tumor cells and cause their lysis (Muthana et al. 2011). Such a strategy prevents virus neutralization in vivo.

Advertisement

3. Non-cancer related urological problems

The bladder is made up of a reservoir and an outlet (bladder neck, urethra and urethral sphincter) whose activities are controlled by smooth and striated muscles. There are more patients with bladder dysfunctions related to its primary function of urine storage and voiding than cancer. These include: lower urinary tract symptoms (LUTS), interstitial cystitis (IC), overactive bladder (OAB), spinal cord injuries affecting micturition and urinary incontinence (UI). It is estimated that by 2018, some 2.3 billion people worldwide will be affected by at least one LUTS, OAB, UI and LUTS suggestive of bladder obstruction (Irwin et al. 2011). LUTS is an umbrella term that encompasses urine storage (increased frequency, at least one episode of nocturia per night, urgency and UI), voiding and post-micturition symptoms (Abrams et al. 2003). Another urological problem is erectile dysfunction (ED). Both LUTS and ED are increased with aging and in patients with diabetes (Brown et al. 2005). With the worldwide increase in the incidence of diabetes the incidence of these urological problems will increase.

Most current therapies for the above mentioned conditions are palliative rather than therapeutic. Gene therapy however, may provide a way to cure the disease and the recent review by Christ lists some of these strategies (Christ 2011). Most of the bladder related problems seem to be linked to muscle and neuronal defects and because of the latter the most common vectors used for animals studies of bladder dysfunctions are HSV vectors.

3.1. Urinary incontinence

Urinary incontinence is a general term used to cover three types of incontinence namely stress, urge and overflow (Chancellor et al. 2001). Stress incontinence occurs when the urinary sphincter muscle is unable to prevent urine leakage following jumping or coughing. This is more common in women than men. Treatment approaches include exercise, surgery and collagen injections into the sphincter muscle. Often multiple injections are required which adds to the cost of treatment and some patients are allergic to bovine collagen. Tissue engineering and ex vivo gene therapy are alternative therapeutic strategies that are being evaluated (Shokeir et al. 2010). Phase I trials of the delivery of autologous myoblasts and fibroblasts from muscle biopsies to female patients with stress incontinence have shown some benefit (Mitterberger et al. 2007). In mice, combining myoblast and gene therapy such as the ex vivo transformation of myoblasts with the VEGF gene resulted in improved volume and function of muscle cells (Delo et al. 2008).

Urge incontinence is characterized by increased urinary urgency and frequency caused by involuntary bladder contractions leading to uncontrollable urine leakage. One study has evaluated intravesical non-viral delivery of a cDNA for the K+ channel and showed that this resulted in increased K+ channels in the smooth muscle of the bladder and amelioration of bladder overactivity (Christ et al. 2001).

Overflow incontinence results from nerve damage such that patients cannot urinate. One common cause is diabetes related neuropathy. Diabetes related cystopathy is often irreversible and restoring bladder functions to diabetic patients is difficult (Sasaki et al. 2002). Animal studies have identified nerve growth factor (NGF) as a good candidate for gene therapy for diabetes induced incontinence (Apfel et al. 1994). HSV delivery of NGF increased NGF in the bladder wall and dorsal root ganglion and improved voiding function in streptozotocin (STZ) induced diabetic rats (Goins et al. 2001; Sasaki et al. 2004).

3.2. Interstitial cystitis/painful bladder syndrome

Interstitial cystitis or painful bladder syndrome occurs predominantly in females (Persu et al. 2010). It is believed to result from underlying inflammation in the bladder. It cannot be adequately treated by drugs and prolonged drug therapy can lead to dependency and tolerance to drugs that may require dose escalation to remain effective. Thus it is a candidate for gene therapy. Delivery of the preproenkephalin gene by HSV (Yokoyama et al. 2009) has been shown to be beneficial in reducing pain. A HSV vector carrying the ionotropic glycine receptor (GlyR) whose expression was induced by glycine had an analgesic effect (Goss et al. 2011). This vector when inoculated into the bladder wall of an inflammation model of IC/PBS in rats was activated by systemic glycine delivery.

3.3. Overactive bladder

Overactive bladder (OAB) is defined as “urinary urgency, usually accompanied by frequency and nocturia, with or without urgency urinary incontinence” (Haylen et al. 2010) Detrusor over activity is considered a single marker for OAB. It can occur as a result of spinal injury and could result in a lack of control of micturition. This has been demonstrated in animal models of spinal injury. HSV vector delivery of glutamic acid decarboxylase has shown benefit in a rat model of spinal injury (Miyazato et al. 2009; Miyazato et al. 2010).

3.4. Erectile dysfunction

Approximately 150 million men are projected to suffer from ED and the incidence of ED increases with age. Normal erectile function occurs as a result of 3 synergistic events namely: neurological mediated penial arterial inflow increase; cavernosal smooth muscle relaxation and restriction of venous outflow from the penis (Andersson & Wagner 1995). In ED one or more of these events may be impaired. The penis is an excellent candidate for gene therapy because it is easily accessible, has limited blood flow and a slow cellular turnover (Bivalacqua & Hellstrom 2001). Though therapy is available for erectile dysfunction there are a significant number of patients who do not respond to available therapy (Yoshimura et al. 2010). The recent review by Harraz et al. provides an excellent overview of gene therapy strategies used in animal models of ED that have been shown to resolve this problem (Harraz et al. 2010). Rather than reproducing that information only recent publications not included in that review are mentioned here. Over expression of the transient receptor potential (TRP) channels 6 (dominant negative) by transfection with a plasmid caused a decrease in calcium levels in the corporal smooth muscle and improved erectile function in diabetic rats (Jung et al. 2010). Using a STZ induced diabetes model to evaluate erectile dysfunction, it was found that implantation of mesenchymal stem cells transfected with VEGF improved erectile function compared to implantation of mesenchymal stem cells alone (Qiu et al. 2011).

3.5. Clinical trials

Only two clinical trials are listed on the http://www.gemcris.od.nih.gov/Contents /GC_HOME.asp for urological conditions unrelated to cancer. One is the Phase I trial for ED and the other is a trial for overactive bladder syndrome. Both trials used plasmid DNA carrying the calcium activated potassium channel (Melman et al. 2007). The results of the Phase I trial for ED indicate the safety of this delivery system.

Advertisement

4. Major issues and future prospects for gene therapy

One major issue is the safety of gene therapy in terms of its impact on the environment as well as long term safety in patients. Schenk-Braat et al found that only half of all registered clinical trials included viral shedding data (Schenk-Braat et al. 2007) and what data was available was primarily for the time after virus delivery and not at the time of delivery. These questions should also be raised for plasmid based gene therapy. Long term follow-up data on patients who have received gene therapy may further ameliorate the safety concerns of this therapy. This will result in gene therapy being more readily applied to other non-malignant conditions. The development of better plasmids and ways to integrate plasmids into the chromosome may lead to the greater use of plasmid rather than viral vectors for urological gene therapy.

MicroRNAs (MiRNA) are new targets for cancer therapy. These are small non-coding RNA molecules that bind to complementary sequences in the protein coding regions of mRNA and block their translation. Their expression levels vary in cancer and normal tissues (Catto et al. 2011). MiRNA-203 and MiRNA-221 have been shown to modulate the growth and apoptosis of human bladder cancer cell lines (Lu et al. 2010; Bo et al. 2011) and these could be new targets for therapy. Given the function of miRNA it is possible that these molecules could also be targets for non-cancer related bladder dysfunctions. This has not yet been explored and identifying such molecules may improve our knowledge of the development of these conditions.

Advertisement

5. Conclusion

The application of gene therapy for urological conditions is being evaluated in many preclinical disease models. In general the results obtained are encouraging and soon these therapies may move to Phase I trials.

References

  1. 1. AbramsP.CardozoL.FallM.GriffithsD.RosierP.UlmstenU.Van KerrebroeckP.VictorA.WeinA.2003The standardisation of terminology in lower urinary tract function: report from the standardisation sub-committee of the International Continence Society. Urology 613749
  2. 2. AkasakaS.SuzukiS.ShimizuH.IgarashiT.AkimotoM.ShimadaT.2001Suicide gene therapy for chemically induced rat bladder tumor entailing instillation of adenoviral vectors. Jpn J Cancer Res 92568575
  3. 3. Al-DosariM. S.GaoX.2009Nonviral gene delivery: principle, limitations, and recent progress. AAPS J 11671681
  4. 4. AmitD.HochbergA.2010Development of targeted therapy for bladder cancer mediated by a double promoter plasmid expressing diphtheria toxin under the control of H19 and IGF2-4regulatory sequences. J Transl Med 8, 134.
  5. 5. AndersonB.NaishW.2008Bladder cancer and smoking. Part 4: efficacy of health promotion. Br J Nurs 1713401344
  6. 6. AnderssonK. E.WagnerG.1995Physiology of penile erection. Physiol Rev 75191236
  7. 7. ApfelS. C.ArezzoJ. C.BrownleeM.FederoffH.KesslerJ. A.1994Nerve growth factor administration protects against experimental diabetic sensory neuropathy. Brain Res 634712
  8. 8. BenedictW. F.TaoZ.KimC. S.ZhangX.ZhouJ. H.AdamL.Mc ConkeyD. J.PapageorgiouA.MunsellM.PhilopenaJ.EnglerH.DemersW.ManevalD. C.DinneyC. P.ConnorR. J.2004Intravesical Ad-IFNalpha causes marked regression of human bladder cancer growing orthotopically in nude mice and overcomes resistance to IFN-alpha protein. Mol Ther 10525532
  9. 9. BivalacquaT. J.HellstromW. J.2001Potential application of gene therapy for the treatment of erectile dysfunction. J Androl 22183190
  10. 10. BoJ.YangG.HuoK.JiangH.ZhangL.LiuD.HuangY.2011microRNA-203 suppresses bladder cancer development by repressing bcl-w expression. FEBS J 278786792
  11. 11. BonnetM. E.ErbacherP.Bolcato-BelleminA. L.2008Systemic delivery of DNA or siRNA mediated by linear polyethylenimine (L-PEI) does not induce an inflammatory response. Pharm Res 2529722982
  12. 12. BrownJ. S.WessellsH.ChancellorM. B.HowardsS. S.StammW. E.StapletonA. E.SteersW. D.Van DenEeden. S. K.Mc VaryK. T.2005Urologic complications of diabetes. Diabetes Care 28177185
  13. 13. BuscariniM.QuekM. L.Gilliam-HegarichS.KasaharaN.BochnerB.2007Adenoviral receptor expression of normal bladder and transitional cell carcinoma of the bladder. Urol Int 78160166
  14. 14. CattoJ. W.AlcarazA.BjartellA. S.De VereWhite. R.EvansC. P.FusselS.HamdyF. C.KallioniemiO.MengualL.SchlommT.VisakorpiT.2011MicroRNA in Prostate, Bladder, and Kidney Cancer: A Systematic Review. Eur Urol.
  15. 15. ChancellorM. B.YoshimuraN.PruchnicR.HuardJ.2001Gene therapy strategies for urological dysfunction. Trends Mol Med 7301306
  16. 16. ChenL.ChenD.BlockE.O’DonnellM.KufeD. W.ClintonS. K.1997Eradication of murine bladder carcinoma by intratumor injection of a bicistronic adenoviral vector carrying cDNAs for the IL-12 heterodimer and its inhibition by the IL-12 40subunit homodimer. J Immunol 159, 351-359.
  17. 17. ChenX.KubeD. M.CooperM. J.DavisP. B.2008Cell surface nucleolin serves as receptor for DNA nanoparticles composed of pegylated polylysine and DNA. Mol Ther 16333342
  18. 18. ChristG. J.2011Potential applications of gene therapy/transfer to the treatment of lower urinary tract diseases/disorders. Handb Exp Pharmacol, 255265
  19. 19. ChristG. J.DayN. S.DayM.SantizoC.ZhaoW.SclafaniT.ZinmanJ.HsiehK.VenkateswarluK.ValcicM.MelmanA.2001Bladder injection of "naked" hSlo/pcDNA3 ameliorates detrusor hyperactivity in obstructed rats in vivo. Am J Physiol Regul Integr Comp Physiol 281, R16991709
  20. 20. ConnorR. J.EnglerH.MachemerT.PhilopenaJ. M.HornM. T.SutjiptoS.ManevalD. C.YoungsterS.ChanT. M.BauschJ.Mc AuliffeJ. P.HindsgaulO.NagabhushanT. L.2001Identification of polyamides that enhance adenovirus-mediated gene expression in the urothelium. Gene Ther 84148
  21. 21. CooksleyC. D.AvritscherE. B.GrossmanH. B.SabichiA. L.DinneyC. P.PettawayC.EltingL. S.2008Clinical model of cost of bladder cancer in the elderly. Urology 71519525
  22. 22. CozziP. J.MalhotraS.Mc AuliffeP.KoobyD. A.FederoffH. J.HurykB.JohnsonP.ScardinoP. T.HestonW. D.FongY.2001Intravesical oncolytic viral therapy using attenuated, replication-competent herpes simplex viruses G207 and Nv1020 is effective in the treatment of bladder cancer in an orthotopic syngeneic model. FASEB J 1513061308
  23. 23. DarquetA. M.CameronB.WilsP.SchermanD.CrouzetJ.1997A new DNA vehicle for nonviral gene delivery: supercoiled minicircle. Gene Ther 413411349
  24. 24. DeloD. M.EberliD.WilliamsJ. K.AnderssonK. E.AtalaA.SokerS.2008Angiogenic gene modification of skeletal muscle cells to compensate for ageing-induced decline in bioengineered functional muscle tissue. BJU Int 102878884
  25. 25. DenOtter. W.DobrowolskiZ.BugajskiA.PaplaB.Van Der MeijdenA. P.KotenJ. W.BoonT. A.SiedlarM.ZembalaM.1998Intravesical interleukin-2 in T1 papillary bladder carcinoma: regression of marker lesion in 8 of 10 patients. J Urol 15911831186
  26. 26. DumeyN.Mongiat-ArtusP.DevauchelleP.LesourdA.CotardJ. P.Le DucA.MartyM.CussenotO.Cohen-HaguenauerO.2005In vivo retroviral mediated gene transfer into bladder urothelium results in preferential transduction of tumoral cells. Eur Urol 47257263
  27. 27. EnglerH.AndersonS. C.MachemerT. R.PhilopenaJ. M.ConnorR. J.WenS. F.ManevalD. C.1999Ethanol improves adenovirus-mediated gene transfer and expression to the bladder epithelium of rodents. Urology 5310491053
  28. 28. FodorI.TimiryasovaT.DenesB.YoshidaJ.RuckleH.LillyM.2005Vaccinia virus mediated 53gene therapy for bladder cancer in an orthotopic murine model. J Urol 173, 604-609.
  29. 29. FreundC. T.TongX. W.BlockA.ContantC. F.KiebackD. G.RowleyD. R.LernerS. P.2000Adenovirus-mediated suicide gene therapy for bladder cancer: comparison of the cytomegalovirus- and Rous sarcoma virus-promoter. Anticancer Res 2028112816
  30. 30. FreundC. T.TongX. W.RowleyD.EngehausenD.FrolovA.KiebackD. G.LernerS. P.2003Combination of adenovirus-mediated thymidine kinase gene therapy with cytotoxic chemotherapy in bladder cancer in vitro. Urol Oncol 21197205
  31. 31. GaetanoC.CatalanoA.PalumboR.IlliB.OrlandoG.VentoruzzoG.SerinoF.CapogrossiM. C.2000Transcriptionally active drugs improve adenovirus vector performance in vitro and in vivo. Gene Ther 716241630
  32. 32. GillD. R.PringleI. A.HydeS. C.2009Progress and prospects: the design and production of plasmid vectors. Gene Ther 16165171
  33. 33. GlazierD. B.BahnsonR. R.Mc LeodD. G.vonRoemeling. R. W.MessingE. M.ErnstoffM. S.1995Intravesical recombinant tumor necrosis factor in the treatment of superficial bladder cancer: an Eastern Cooperative Oncology Group study. J Urol 1546668
  34. 34. GoinsW. F.YoshimuraN.PhelanM. W.YokoyamaT.FraserM. O.OzawaH.BennettN. J.de GroatW. C.GloriosoJ. C.ChancellorM. B.2001Herpes simplex virus mediated nerve growth factor expression in bladder and afferent neurons: potential treatment for diabetic bladder dysfunction. J Urol 16517481754
  35. 35. GomellaL. G.MastrangeloM. J.Mc CueP. A.MaguireH. J.MulhollandS. G.LattimeE. C.2001Phase i study of intravesical vaccinia virus as a vector for gene therapy of bladder cancer. J Urol 16612911295
  36. 36. GossJ. R.CascioM.GoinsW. F.HuangS.KriskyD. M.ClarkeR. J.JohnsonJ. W.YokoyamaH.YoshimuraN.GoldM. S.GloriosoJ. C.2011HSV Delivery of a Ligand-regulated Endogenous Ion Channel Gene to Sensory Neurons Results in Pain Control Following Channel Activation. Mol Ther 19500506
  37. 37. HackettP. B.LargaespadaD. A.CooperL. J.2010A transposon and transposase system for human application. Mol Ther 18674683
  38. 38. HarimotoK.SugimuraK.LeeC. R.KuratsukuriK.KishimotoT.1998In vivo gene transfer methods in the bladder without viral vectors. Br J Urol 81870874
  39. 39. HarrazA.ShindelA. W.LueT. F.2010Emerging gene and stem cell therapies for the treatment of erectile dysfunction. Nat Rev Urol 7143152
  40. 40. HaylenB. T.de RidderD.FreemanR. M.SwiftS. E.BerghmansB.LeeJ.MongaA.PetriE.RizkD. E.SandP. K.SchaerG. N.2010An International Urogynecological Association (IUGA)/International Continence Society (ICS) joint report on the terminology for female pelvic floor dysfunction. Neurourol Urodyn 29420
  41. 41. HeX. D.WangZ. P.WeiH. Y.ZhouQ.WangD. G.TianJ. Q.FuS. J.RodriguezR.2009Construction of urothelium-specific recombinant adenovirus and its inhibition in bladder cancer cell. Urol Int 82209213
  42. 42. HerrH. W.MoralesA.2008History of bacillus Calmette-Guerin and bladder cancer: an immunotherapy success story. J Urol 1795356
  43. 43. HoriguchiY.LarchianW. A.KaplinskyR.FairW. R.HestonW. D.2000Intravesical liposome-mediated interleukin-2 gene therapy in orthotopic murine bladder cancer model. Gene Ther 7844851
  44. 44. HorinagaM.HarschK. M.FukuyamaR.HestonW.LarchianW.2005Intravesical interleukin-12 gene therapy in an orthotopic bladder cancer model. Urology 66461466
  45. 45. InoueK.PerrotteP.WoodC. G.SlatonJ. W.SweeneyP.DinneyC. P.2000Gene therapy of human bladder cancer with adenovirus-mediated antisense basic fibroblast growth factor. Clin Cancer Res 644224431
  46. 46. IrieA.MatsumotoK.AndereggB.KurumaH.Kashani-SabetM.ScanlonK. J.UchidaT.BabaS.2006Growth inhibition efficacy of an adenovirus expressing dual therapeutic genes, wild-type 53and anti-erbB2 ribozyme, against human bladder cancer cells. Cancer Gene Ther 13, 298-305.
  47. 47. IrwinD. E.KoppZ. S.AgatepB.MilsomI.AbramsP.2011Worldwide prevalence estimates of lower urinary tract symptoms, overactive bladder, urinary incontinence and bladder outlet obstruction. BJU Int.
  48. 48. JungJ. H.KimB. J.ChaeM. R.KamS. C.JeonJ. H.SoI.ChungK. H.LeeS. W.2010Gene transfer of TRPC6 (dominant negative) restores erectile function in diabetic rats. J Sex Med 711261138
  49. 49. KamatA. M.LammD. L.2000Intravesical therapy for bladder cancer. Urology 55161168
  50. 50. KasmanL. M.BaruaS.LuP.RegeK.Voelkel-JohnsonC.2009Polymer-enhanced adenoviral transduction of CAR-negative bladder cancer cells. Mol Pharm 616121619
  51. 51. KikkawaK.FujiiR.KuramotoT.MoriT.InagakiT.KohjimotoY.IwahashiM.YamaueH.HaraI.2009Dendritic cells with transduced survivin gene induce specific cytotoxic T lymphocytes in human urologic cancer cell lines. Urology 74222228
  52. 52. KuballJ.WenS. F.LeissnerJ.AtkinsD.MeinhardtP.QuijanoE.EnglerH.HutchinsB.ManevalD. C.GraceM. J.FritzM. A.StorkelS.ThuroffJ. W.HuberC.SchulerM.2002Successful adenovirus-mediated wild-type 53gene transfer in patients with bladder cancer by intravesical vector instillation. J Clin Oncol 20, 957-965.
  53. 53. LaiM. D.ChenC. S.YangC. R.YuanS. Y.TsaiJ. J.TuC. F.WangC. C.YenM. C.LinC. C.2010An HDAC inhibitor enhances the antitumor activity of a CMV promoter-driven DNA vaccine. Cancer Gene Ther 17203211
  54. 54. LansonN. A.Jr FriedlanderP. L.SchwarzenbergerP.KollsJ. K.WangG.2003Replication of an adenoviral vector controlled by the human telomerase reverse transcriptase promoter causes tumor-selective tumor lysis. Cancer Res 6379367941
  55. 55. LawrenciaC.MahendranR.EsuvaranathanK.2001Transfection of urothelial cells using methyl-beta-cyclodextrin solubilized cholesterol and Dotap. Gene Ther 8760768
  56. 56. LeeS. S.EisenlohrL. C.Mc CueP. A.MastrangeloM. J.LattimeE. C.1994Intravesical gene therapy: in vivo gene transfer using recombinant vaccinia virus vectors. Cancer Res 5433253328
  57. 57. LinL. F.ZhuG.YooJ. J.SokerS.SukhatmeV. P.AtalaA.2002A system for the enhancement of adenovirus mediated gene transfer to uro-epithelium. J Urol 168813818
  58. 58. LoserP.JenningsG. S.StraussM.SandigV.1998Reactivation of the previously silenced cytomegalovirus major immediate-early promoter in the mouse liver: involvement of NFkappaB. J Virol 72180190
  59. 59. LoskogA. S.FranssonM. E.TottermanT. T.2005AdCD40L gene therapy counteracts T regulatory cells and cures aggressive tumors in an orthotopic bladder cancer model. Clin Cancer Res 1188168821
  60. 60. LuQ.LuC.ZhouG. P.ZhangW.XiaoH.WangX. R.2010MicroRNA-221 silencing predisposed human bladder cancer cells to undergo apoptosis induced by TRAIL. Urol Oncol 28635641
  61. 61. MalmstromP. U.LoskogA. S.LindqvistC. A.MangsboS. M.FranssonM.WandersA.GardmarkT.TottermanT. H.2010AdCD40L immunogene therapy for bladder carcinoma--the first phase I/IIa trial. Clin Cancer Res 1632793287
  62. 62. Mc GarveyT. W.MengR. D.JohnsonO.El -DeiryW.MalkowiczS. B.2001Growth inhibitory effect of 21and p53 containing adenoviruses on transitional cell carcinoma cell lines in vitro and in vivo. Urol Oncol 6, 155-162.
  63. 63. MelmanA.Bar-ChamaN.Mc CulloughA.DaviesK.ChristG.2007Plasmid-based gene transfer for treatment of erectile dysfunction and overactive bladder: results of a phase I trial. Isr Med Assoc J 9143146
  64. 64. MitterbergerM.MarksteinerR.MargreiterE.PinggeraG. M.ColleselliD.FrauscherF.UlmerH.FusseneggerM.BartschG.StrasserH.2007Autologous myoblasts and fibroblasts for female stress incontinence: a 1-year follow-up in 123 patients. BJU Int 10010811085
  65. 65. MiyakeH.HaraI.HaraS.ArakawaS.KamidonoS.2000Synergistic chemosensitization and inhibition of tumor growth and metastasis by adenovirus-mediated 53gene transfer in human bladder cancer model. Urology 56, 332-336.
  66. 66. MiyazatoM.SugayaK.GoinsW. F.WolfeD.GossJ. R.ChancellorM. B.de GroatW. C.GloriosoJ. C.YoshimuraN.2009Herpes simplex virus vector-mediated gene delivery of glutamic acid decarboxylase reduces detrusor overactivity in spinal cord-injured rats. Gene Ther 16660668
  67. 67. MiyazatoM.SugayaK.SaitoS.ChancellorM. B.GoinsW. F.GossJ. R.de GroatW. C.GloriosoJ. C.YoshimuraN.2010Suppression of detrusor-sphincter dyssynergia by herpes simplex virus vector mediated gene delivery of glutamic acid decarboxylase in spinal cord injured rats. J Urol 18412041210
  68. 68. MuthanaM.GiannoudisA.ScottS. D.FangH. Y.CoffeltS. B.MorrowF. J.MurdochC.BurtonJ.CrossN.BurkeB.MistryR.HamdyF.BrownN. J.GeorgopoulosL.HoskinP.EssandM.LewisC. E.MaitlandN. J.2011Use of Macrophages to Target Therapeutic Adenovirus to Human Prostate Tumors. Cancer Res 7118051815
  69. 69. NagabhushanT. L.ManevalD. C.BenedictW. F.WenS. F.IhnatP. M.EnglerH.ConnorR. J.2007Enhancement of intravesical delivery with Syn3 potentiates interferon-alpha2b gene therapy for superficial bladder cancer. Cytokine Growth Factor Rev 18389394
  70. 70. NinalgaC.LoskogA.KlevenfeldtM.EssandM.TottermanT. H.2005CpG oligonucleotide therapy cures subcutaneous and orthotopic tumors and evokes protective immunity in murine bladder cancer. J Immunother 282027
  71. 71. OgawaR.KagiyaG.FerilL. B.Jr NakayaN.NozakiT.FuseH.KondoT.2004Ultrasound mediated intravesical transfection enhanced by treatment with lidocaine or heat. J Urol 17214691473
  72. 72. OhanaP.BibiO.MatoukI.LevyC.BirmanT.ArielI.SchneiderT.AyeshS.GiladiH.LasterM.de GrootN.HochbergA.2002Use of H19 regulatory sequences for targeted gene therapy in cancer. Int J Cancer 98645650
  73. 73. OlivaresE. C.HollisR. P.ChalbergT. W.MeuseL.KayM. A.CalosM. P.2002Site-specific genomic integration produces therapeutic Factor IX levels in mice. Nat Biotechnol 2011241128
  74. 74. PagliaroL. C.KeyhaniA.WilliamsD.WoodsD.LiuB.PerrotteP.SlatonJ. W.MerrittJ. A.GrossmanH. B.DinneyC. P.2003Repeated intravesical instillations of an adenoviral vector in patients with locally advanced bladder cancer: a phase I study of 53gene therapy. J Clin Oncol 21, 2247-2253.
  75. 75. PanJ. G.ZhouX.ZengG. W.HanR. F.2011Suppression of bladder cancer growth in mice by adeno-associated virus vector-mediated endostatin expression. Tumour Biol 32301310
  76. 76. PersuC.CauniV.GutueS.BlajI.JingaV.GeavleteP.2010From interstitial cystitis to chronic pelvic pain. J Med Life 3167174
  77. 77. PirolloK. F.RaitA.ZhouQ.ZhangX. Q.ZhouJ.KimC. S.BenedictW. F.ChangE. H.2008Tumor-targeting nanocomplex delivery of novel tumor suppressor RB94 chemosensitizes bladder carcinoma cells in vitro and in vivo. Clin Cancer Res 1421902198
  78. 78. PongR. C.LaiY. J.ChenH.OkegawaT.FrenkelE.SagalowskyA.HsiehJ. T.2003Epigenetic regulation of coxsackie and adenovirus receptor (CAR) gene promoter in urogenital cancer cells. Cancer Res 6386808686
  79. 79. QiuX.SunC.YuW.LinH.SunZ.ChenY.WangR.DaiY.2011Combined Strategy of Mesenchymal Stem Cells Injection with VEGF Gene Therapy for the Treatment of Diabetes Associated Erectile Dysfunction. J Androl.
  80. 80. RameshN.GeY.EnnistD. L.ZhuM.MinaM.GaneshS.ReddyP. S.YuD. C.2006CG0070, a conditionally replicating granulocyte macrophage colony-stimulating factor--armed oncolytic adenovirus for the treatment of bladder cancer. Clin Cancer Res 12305313
  81. 81. RameshN.MemarzadehB.GeY.FreyD.Van RoeyM.RojasV.YuD. C.2004Identification of pretreatment agents to enhance adenovirus infection of bladder epithelium. Mol Ther 10697705
  82. 82. SachsM. D.RamamurthyM.PoelH.WickhamT. J.LamfersM.GerritsenW.ChowdhuryW.LiY.SchoenbergM. P.RodriguezR.2004Histone deacetylase inhibitors upregulate expression of the coxsackie adenovirus receptor (CAR) preferentially in bladder cancer cells. Cancer Gene Ther 11477486
  83. 83. SaintF.KurthN.MailleP.VordosD.HoznekA.SoyeuxP.PatardJ. J.AbbouC. C.ChopinD. K.2003Urinary IL-2 assay for monitoring intravesical bacillus Calmette-Guerin response of superficial bladder cancer during induction course and maintenance therapy. Int J Cancer 107434440
  84. 84. SasakiK.ChancellorM. B.GoinsW. F.PhelanM. W.GloriosoJ. C.de GroatW. C.YoshimuraN.2004Gene therapy using replication-defective herpes simplex virus vectors expressing nerve growth factor in a rat model of diabetic cystopathy. Diabetes 5327232730
  85. 85. SasakiK.ChancellorM. B.PhelanM. W.YokoyamaT.FraserM. O.SekiS.KuboK.KumonH.GroatW. C.YoshimuraN.2002Diabetic cystopathy correlates with a long-term decrease in nerve growth factor levels in the bladder and lumbosacral dorsal root Ganglia. J Urol 16812591264
  86. 86. SazawaA.WatanabeT.TanakaM.HagaK.FujitaH.HarabayashiT.ShinoharaN.KoyanagiT.KuzumakiN.2002Adenovirus mediated gelsolin gene therapy for orthotopic human bladder cancer in nude mice. J Urol 16811821187
  87. 87. Schenk-BraatE. A.van MierloM. M.WagemakerG.BangmaC. H.KapteinL. C.2007An inventory of shedding data from clinical gene therapy trials. J Gene Med 9910921
  88. 88. SethS.MatsuiY.FosnaughK.LiuY.VaishN.AdamiR.HarvieP.JohnsR.SeversonG.BrownT.TakagiA.BellS.ChenY.ChenF.ZhuT.FamR.MaciagiewiczI.KwangE.Mc CutcheonM.FarberK.CharmleyP.Houston JrM. E.SoA.TemplinM. V.PoliskyB.2011RNAi-based Therapeutics Targeting Survivin and PLK1 for Treatment of Bladder Cancer. Mol Ther.
  89. 89. ShiauA. L.LinC. Y.TzaiT. S.WuC. L.2001Postoperative immuno-gene therapy of murine bladder tumor by in vivo administration of retroviruses expressing mouse interferon-gamma. Cancer Gene Ther 87381
  90. 90. ShibataM. A.HoriguchiT.MorimotoJ.OtsukiY.2003Massive apoptotic cell death in chemically induced rat urinary bladder carcinomas following in situ HSVtk electrogene transfer. J Gene Med 5219231
  91. 91. ShiehG. S.ShiauA. L.YoY. T.LinP. R.ChangC. C.TzaiT. S.WuC. L.2006Low-dose etoposide enhances telomerase-dependent adenovirus-mediated cytosine deaminase gene therapy through augmentation of adenoviral infection and transgene expression in a syngeneic bladder tumor model. Cancer Res 6699579966
  92. 92. ShirakawaT.HamadaK.ZhangZ.OkadaH.TagawaM.KamidonoS.KawabataM.GotohA.2004A cox-2 promoter-based replication-selective adenoviral vector to target the cox-2-expressing human bladder cancer cells. Clin Cancer Res 1043424348
  93. 93. ShokeirA. A.HarrazA. M.El -DinA. B.2010Tissue engineering and stem cells: basic principles and applications in urology. Int J Urol 17964973
  94. 94. SidiA. A.OhanaP.BenjaminS.ShalevM.RansomJ. H.LammD.HochbergA.LeibovitchI.2008Phase I/II marker lesion study of intravesical BC-819 DNA plasmid in H19 over expressing superficial bladder cancer refractory to bacillus Calmette-Guerin. J Urol 18023792383
  95. 95. SiemensD. R.CristS.AustinJ. C.TartagliaJ.RatliffT. L.2003Comparison of viral vectors: gene transfer efficiency and tissue specificity in a bladder cancer model. J Urol 170979984
  96. 96. StavropoulosN. E.HastazerisK.FiliadisI.MihailidisI.IoachimE.LiamisZ.KalomirisP.2002Intravesical instillations of interferon gamma in the prophylaxis of high risk superficial bladder cancer--results of a controlled prospective study. Scand J Urol Nephrol 36218222
  97. 97. SuttonM. A.BerkmanS. A.ChenS. H.BlockA.DangT. D.KattanM. W.WheelerT. M.RowleyD. R.WooS. L.LernerS. P.1997Adenovirus-mediated suicide gene therapy for experimental bladder cancer. Urology 49173180
  98. 98. TanakaA. S.TanakaM.KomuroK.1998A highly efficient method for the site-specific integration of transfected plasmids into the genome of mammalian cells using purified retroviral integrase. Gene 2166776
  99. 99. TanakaM.GrossmanH. B.2003In vivo gene therapy of human bladder cancer with PTEN suppresses tumor growth, downregulates phosphorylated Akt, and increases sensitivity to doxorubicin. Gene Ther 1016361642
  100. 100. TaoZ.ConnorR. J.AshooriF.DinneyC. P.MunsellM.PhilopenaJ. A.BenedictW. F.2006Efficacy of a single intravesical treatment with Ad-IFN/Syn 3 is dependent on dose and urine IFN concentration obtained: implications for clinical investigation. Cancer Gene Ther 13125130
  101. 101. TeraoS.ShirakawaT.KuboS.BishunuA.LeeS. J.GodaK.TsukudaM.HamadaK.TagawaM.TakenakaA.FujisawaM.GotohA.2007Midkine promoter-based conditionally replicative adenovirus for targeting midkine-expressing human bladder cancer model. Urology 7010091013
  102. 102. ThalmannG. N.DewaldB.BaggioliniM.StuderU. E.1997Interleukin-8 expression in the urine after bacillus Calmette-Guerin therapy: a potential prognostic factor of tumor recurrence and progression. J Urol 15813401344
  103. 103. ThalmannG. N.SermierA.RentschC.MohrleK.CecchiniM. G.StuderU. E.2000Urinary Interleukin-8 and 18 predict the response of superficial bladder cancer to intravesical therapy with bacillus Calmette-Guerin. J Urol 16421292133
  104. 104. ThomasC. E.EhrhardtA.KayM. A.2003Progress and problems with the use of viral vectors for gene therapy. Nat Rev Genet 4346358
  105. 105. TsaiY. S.ShiauA. L.ChenY. F.TsaiH. T.LeeH. L.TzaiT. S.WuC. L.2009Enhancement of antitumor immune response by targeted interleukin-12 electrogene transfer through antiHER2 single-chain antibody in a murine bladder tumor model. Vaccine 2753835392
  106. 106. TsaiY. S.ShiauA. L.ChenY. F.TsaiH. T.TzaiT. S.WuC. L.2010Enhancement of antitumor activity of gammaretrovirus carrying IL-12 gene through genetic modification of envelope targeting HER2 receptor: a promising strategy for bladder cancer therapy. Cancer Gene Ther 173748
  107. 107. van der PoelH. G.MolenaarB.van BeusechemV. W.HaismaH. J.RodriguezR.CurielD. T.GerritsenW. R.2002Epidermal growth factor receptor targeting of replication competent adenovirus enhances cytotoxicity in bladder cancer. J Urol 168266272
  108. 108. WangH.SatohM.AbeH.SunamuraM.MoriyaT.IshidoyaS.SaitoS.HamadaH.AraiY.2006Oncolytic viral therapy by bladder instillation using an E1A, E1B double-restricted adenovirus in an orthotopic bladder cancer model. Urology 68674681
  109. 109. WoodM.PerrotteP.OnishiE.HarperM. E.DinneyC.PagliaroL.WilsonD. R.1999Biodistribution of an adenoviral vector carrying the luciferase reporter gene following intravesical or intravenous administration to a mouse. Cancer Gene Ther 6367372
  110. 110. WuQ.EsuvaranathanK.MahendranR.2004Monitoring the response of orthotopic bladder tumors to granulocyte macrophage colony-stimulating factor therapy using the prostate-specific antigen gene as a reporter. Clin Cancer Res 1069776984
  111. 111. WuQ.MahendranR.EsuvaranathanK.2003Nonviral cytokine gene therapy on an orthotopic bladder cancer model. Clin Cancer Res 945224528
  112. 112. XuH. J.ZhouY.SeigneJ.PerngG. S.MixonM.ZhangC.LiJ.BenedictW. F.HuS. X.1996Enhanced tumor suppressor gene therapy via replication-deficient adenovirus vectors expressing an N-terminal truncated retinoblastoma protein. Cancer Res 5622452249
  113. 113. YamashitaM.RosserC. J.ZhouJ. H.ZhangX. Q.ConnorR. J.EnglerH.ManevalD. C.KarashimaT.CzerniakB. A.DinneyC. P.BenedictW. F.2002Syn3 provides high levels of intravesical adenoviral-mediated gene transfer for gene therapy of genetically altered urothelium and superficial bladder cancer. Cancer Gene Ther 9687691
  114. 114. YewN. S.ZhaoH.WuI. H.SongA.TousignantJ. D.PrzybylskaM.ChengS. H.2000Reduced inflammatory response to plasmid DNA vectors by elimination and inhibition of immunostimulatory CpG motifs. Mol Ther 1255262
  115. 115. YokoyamaH.SasakiK.FranksM. E.GoinsW. F.GossJ. R.de GroatW. C.GloriosoJ. C.ChancellorM. B.YoshimuraN.2009Gene therapy for bladder overactivity and nociception with herpes simplex virus vectors expressing preproenkephalin. Hum Gene Ther 206371
  116. 116. YoshimuraN.KatoR.ChancellorM. B.NelsonJ. B.GloriosoJ. C.2010Gene therapy as future treatment of erectile dysfunction. Expert Opin Biol Ther 1013051314
  117. 117. ZaharoffD. A.HoffmanB. S.HooperH. B.BenjaminC. J.Jr KhuranaK. K.HanceK. W.RogersC. J.PintoP. A.SchlomJ.GreinerJ. W.2009Intravesical immunotherapy of superficial bladder cancer with chitosan/interleukin-12. Cancer Res 6961926199
  118. 118. ZangZ.MahendranR.WuQ.YongT.EsuvaranathanK.2004Non-viral tumor necrosis factor-alpha gene transfer decreases the incidence of orthotopic bladder tumors. Int J Mol Med 14713717
  119. 119. ZhangJ.RameshN.ChenY.LiY.DilleyJ.WorkingP.YuD. C.2002Identification of human uroplakin II promoter and its use in the construction of CG8840, a urothelium-specific adenovirus variant that eliminates established bladder tumors in combination with docetaxel. Cancer Res 6237433750
  120. 120. ZhangX.AtalaA.GodbeyW. T.2008Expression-targeted gene therapy for the treatment of transitional cell carcinoma. Cancer Gene Ther 15543552
  121. 121. ZhangX.GodbeyW. T.2010Preclinical evaluation of a gene therapy treatment for transitional cell carcinoma. Cancer Gene Ther.
  122. 122. ZhangZ.ShirakawaT.HinataN.MatsumotoA.FujisawaM.OkadaH.KamidonoS.MatsuoM.GotohA.2003Combination with CD/5-FC gene therapy enhances killing of human bladder-cancer cells by radiation. J Gene Med 5860867
  123. 123. ZhuZ.XingS.LinC.ZhangX.FuM.LiangX.ZengF.LuG.WuM.2003Bladder cancer therapy using combined proliferating cell nuclear antigen antisense oligonucleotides and recombinant adenovirus 53Chin Med J (Engl) 116, 1860-1863.

Written By

Ratha Mahendran, Sin Mun Tham and Kesavan Esuvaranathan

Submitted: 18 November 2010 Published: 23 August 2011