1. Introduction
Subclinical hypothyroidism (sHT) is defined as serum thyrotropin-stimulating hormone (TSH) concentration above the statistically defined upper limit of the reference range in the face of serum free T4 (FT4) and free T3 (FT3) concentrations within the normal range (Ross, 2004). sHT is a frequent condition among the general population, especially middle-aged and elderly women (Canaris et al., 2000). Depending on the degree of TSH elevation, sHT has been associated with hyperlipidemia, intermediary metabolism alterations, arterial hypertension and cardiovascular disease (CVD) as well as neuropsychiatric features, including cognitive impairment (Ashizawa et al., 2010; Biondi & Cooper., 2008; Cappola et al., 2006; Ceresini et al., 2010; Mitrou et al., 2011; Monzani et al., 2006; Rodondi et al., 2010; Tan et al., 2008; Tappy, 1987). Interestingly, the analysis of variation in thyroid function tests in healthy volunteers has shown that the physiological individual reference ranges for test results are narrow compared with laboratory references (Andersen et al., 2002). This finding suggests that a test result within laboratory reference limits is not necessarily normal for an individual. Giving that serum TSH responds with logarithmically amplified degree to minor changes in serum T4 and T3, abnormal serum TSH may indicate that T4 and T3 are not normal for an individual although still within the laboratory references. These data point out that the distinction between subclinical and overt thyroid failure (elevated serum TSH and low T4 and/or T3) is somewhat arbitrary. Indeed, for the same degree of thyroid function abnormality, the diagnosis depends to a considerable extent on the position of the patient’s normal set point for T4 and T3 within the laboratory reference range.
Because sHT is mainly detected as a biochemical TSH abnormality, the definition of the TSH reference range represents a critical point, especially in the elderly (Baloch et al., 2003; Olsen, 1978; Dayan et al., 2001). In the past, the upper normal limit of TSH was considered about 10 mIU/L with the first-generation TSH RIA assay while, the current normal reference range of serum TSH concentration is around 0.45 to 4.5 mIU/L (Biondi & Cooper, 2008; Surks et al., 2004). Considering that serum TSH concentrations in a healthy population have a skewed distribution with a "tail" toward higher TSH values, the use of age specific reference limits for TSH has been suggested (Surks et al., 2004). This is especially proper in the elderly, in whom normal TSH is often shifted to a higher level (Mariotti, 1995) and the clinical presentation may differ from that in their younger counterparts (Mohandas, 2003). These considerations outline how making a correct diagnosis of sHT is challenging in the elderly but crucial to avoid significant misclassification of patients with abnormal TSH, who may or may not have thyroid dysfunction and may receive unnecessary or even harmful therapy (Laurberg, 2011). Indeed, the clinical significance of sHT in the elderly should be ascertained also in relation to the physiological changes of thyroid function with ageing (Biondi & Cooper, 2008; Carlè, 2007; Ceresini, 2010; Helfand, 2004; Surks et al., 2004). Therefore, the fundamental clinical question regarding these patients is on the clinical significance of sHT and the actual need of hormone replacement therapy (Villar, 2007).
2. Epidemiology
Several population-based studies have reported that sHT is common in the general population, with a prevalence that increases with increasing age (Gharib et al., 2005a,b; Hollowell et al., 2002; Samuels, 1998; Tunbridge et al., 1977). In interpreting epidemiologic data, it should be taken into account that the ability to identify people with sHT varies by TSH assay and cut-off value, which ranged from >3 to >7 mIU/L (Kanaya et al., 2002; Rivolta et al., 1999). In this setting, it is noteworthy that some investigators suggest that the upper limit of normal for serum TSH level should be 2.5 mIU/L (Spencer et al., 1993). In support of this position is a higher prevalence of anti-thyroid antibodies in subjects with serum TSH levels >2.5 mIU/L (Vanderpump et al., 1995). Reasoning about these considerations, it is not astonishing that the reported prevalence of sHT in the general population ranges widely from 1.3% to 21%, depending on age, gender, and iodine intake (Kanaya et al., 2002; Rivolta et al., 1999; Samuels, 1998; Sawin et al., 1985; Tunbridge et al., 1977; Wang et al., 1997).
In the Wickham survey, the prevalence of sHT (TSH > 6 mIU/L) was 7.5% in women and 2.8% in men (Wickham study). An age dependent increase in serum TSH concentrations was found only when women with high serum anti-thyroid antibody values were included in the analysis; with 17.4% prevalence of sHT in women older than 75 years (Wickham study). Accordingly, in a Dutch study the prevalence of sHT in a group of middle-aged women (mean age 55 years) was 4%, the rate rising to 7.3% 10 years later (Geul et al., 1993). The higher prevalence of sHT in older people was confirmed by data from the Framingham Study, which reported a prevalence of sHT of 8.2% in men and 16.9% in women, older than 60 years and, the Colorado study (16% in men and 21% in women older than 74 yrs) (Sawin et al., 1979, Canaris et al., 2000). Overall these findings demonstrate that ageing is associated with an increased prevalence of positive anti-thyroid antibody titers and mild hypothyroidism (Mariotti et al., 1995). The prevalence of sHT varies also according to iodine intake; being higher in areas with elevated intake with respect to areas with low-normal or deficient intake (Biondi & Cooper, 2012). In this setting, the occurrence of sHT among nursing home elderly residents was 4.2% in an iodine-deficient area (urinary iodine 72 micrograms/g creatinine), 10.4% in region of obligatory iodinated salt prophylaxis (urinary iodine 100 micrograms/g creatinine) and 23.9% in an abundant iodine intake area (urinary iodine 513 micrograms/g creatinine) (Szabolcs et al., 1997).
Overall, these data show that sHT is a very frequent condition and raise the question of the opportunity for general population screening programs, although a consensus is still lacking on this topic (Biondi & Cooper, 2012). The above notwithstanding, screening older people for thyroid disorders is still suggested by some authorities, aiming at the discovery of previously undiagnosed cases of overt hypothyroidism and the monitoring of cases with subclinical dysfunction (Ladenson et al., 2000; Surks et al., 2004).
3. Subclinical hypothyrodism: Clinical features and etiology
Hypothyroidism is a graded phenomenon that encompasses a wide variety of clinical conditions from full blown myxedema to sHT, which is characterized by elevated serum TSH concentrations in the face of normal free thyroid hormone levels (Cooper, 2001). Currently, the most widely accepted interpretation of these biochemical findings is that increased TSH is an indication of slightly reduced peripheral thyroid hormone effect, leading to mild hypothyroidism instead of a new steady state of euthyroidism (Karmisholt et al., 2011, Ross, 2004). In a consensus statement of the American Association of Clinical Endocrinologists, sHT was classified in two categories according to TSH level: mildly increased serum TSH levels (4.5–10 mIU/liter), and more severely increased serum TSH value (>10 mIU/liter) (Gharib et al., 2005a,b). However, this classification was not adopted in all clinical investigations, thus making the comparison of different trials quite difficult.
There is scientific consensus that sHT is caused by the same etiology of overt hypothyroidism (Biondi & Cooper, 2008), the most frequent one being Hashimoto’s thyroiditis. This is an autoimmune, inflammatory disorder of the thyroid gland, whose prevalence increases with increasing age, being higher in women (Canaris et al., 2000; Surks et al., 1996). Other causes of primary hypothyroidism may result from therapies that destroy the thyroid tissue such as radioactive iodine treatment, external radiation therapy or partial thyroidectomy (Cooper, 2001). Chemotherapy also was associated to hypothyroidism in patients with cancer or lymphoma (Hancock et al., 2001; Kumar et al., 2004). Moreover, both subclinical and overt hypothyroidism could be induced by many drugs such as amiodarone, lithium carbonate, type I interferons, sulfonamides and several other toxic molecules (Basaria & Cooper, 2004; Caraccio et al., 2005).
Patients with sHT have a different rate of progression to clinically overt hypothyroidism in the presence or not of autoimmunity: 2.6% each year if thyroperoxidase (TPO) antibodies are absent and 4.3% if they are present (Vanderpump et al., 1995). However, a significant number of sHT subjects do not show progression and some experiences normalization. One of the most predictive markers of progression to overt hypothyroidism is serum TSH level higher than 10 mIU/L, by contrast a level less than 6 mIU/L depicts a lower likelihood of progression (Fatourechi, 2009). Accordingly, a clinical study, enrolling men and women older than 55 years with mean follow-up of 32 months, indicated that serum TSH levels normalized in 52% of those with serum TSH value less than 10 mIU/L (Díez & Iglesias, 2004).
The most common symptoms reported by sHT patients are the same although less evident than those observed in overt hypothyroidism: dry skin, poor memory, slow thinking, muscle weakness, fatigue, muscle cramp, cold intolerance, puffy eyes, constipation, and hoarseness (Canaris et al., 2000; Canaris et al., 1997). It is conceivable that clinical symptoms of hypothyroidism are related to the degree of thyroid failure, disease duration, and individual sensitivity to thyroid hormone deficiency (Biondi & Cooper, 2008). However, the presence of typical symptoms in patients with sHT remains controversial considering that many of them are non-specific and shared with many clinical conditions, especially in the elderly. Therefore, it is difficult to distinguish euthyroid subjects from sHT patients only by using clinical symptoms (Biondi & Cooper, 2008). Baseline data from a randomized clinical study confirmed a significant prevalence of hypothyroid symptoms among individuals with sHT (Cooper et al., 1984). Moreover, Canaris et al., (2000) reported fewer symptoms related to hypothyroidism in subclinical than in overt hypothyroid patients, but more frequently than in euthyroid controls. However, this study did not distinguish between treated or untreated subclinical and overt hypothyroid patients. By contrast, other cross-sectional and case-control studies did not confirm these observations, but they were conducted among selected or referred populations often involving old hospitalized patients (Bemben et al., 1994; Zulewski et al., 1997). Age represents a confounding factor that may hinder the identification of symptoms of mild hypothyroidism: the typical findings of hypothyroidism are less common in the elderly and, if present, often either resemble or are attributed to chronic illnesses, drugs, depression or ageing
4. Thyroid function and ageing
The relationship between thyroid function and ageing has been hypothesized more than one decade ago (Mariotti et al., 1995). Human ageing is associated with an increased prevalence of serum anti-thyroid antibodies and overt or mild thyroid dysfunction (Hollowell et al., 2002; Gharib et al., 2005a,b; Samuels, 1998; Tunbridge et al., 1977). Several clinical studies confirmed an age-dependent decrease of thyroid function including iodine uptake and thyroid hormone production (Hollowell et al., 2002; Gharib et al., 2005a,b; Samuels, 1998; Sawin et al., 2009; Tunbridge et al., 1977). Although there is a consensus on the detrimental effects of overt hypothyroidism in older patients, the clinical relevance of mild to moderate thyroid failure remains an uncertain area (Surks et al., 2004) and, animal models indicated that low thyroid hormones are associated to increased life span (Ooka et al., 1983). The relative small number of epidemiological studies with inappropriate statistical power, and the lack of large prospective randomized trials directed to evaluate the therapeutic effect and impact on survival of hormonal therapy in mild thyroid impairment, does not allow to conclude whether mild thyroid impairment is a favorable phenotype or a negative clinical condition, especially in older people. An age-dependent thyroid dysfunction (particularly hypothyroidism) has been well documented in the elderly, including the oldest-old population (>85 yr) (Helfand et al., 2004; Mariotti et al., 1993). An interesting study focused on thyroid function during physiological ageing was carried out by Mariotti et al. (1993). In this study thyroid status was assessed in 41 healthy centenarians and 33 healthy elderly subjects as compared to two control groups: 98 healthy normal adult subjects and 52 patients with miscellaneous non-thyroidal illness. Healthy centenarians showed a lower prevalence of positive anti-thyroid autoantibody titer than elderly controls with a relatively low (7%) prevalence of sHT although the median serum FT3 level was lower than in each other group. Interestingly, median serum TSH level of centenarians was lower than in healthy elderly subjects, in whom however, was significantly lower than in young controls (Mariotti et al., 1993). This study did not resolve the question whether the decreased FT3 and TSH value observed in healthy centenarians, represents an adaptive mechanism to reduced metabolic homeostasis or a protective condition in ageing. At partial odds with these data, a population based survey and one large cross-sectional study (Atzmon et al., 2009; Surks et al., 2007) showed a progressive shift of the normal serum TSH range towards higher values from healthy young individuals up to centenarians. Overall these data seem to suggest that ageing is associated with a certain degree of down regulation of the hypothalamus-pituitary-thyroid-peripheral axis, although the clinical significance of such condition is far to be elucidated. To this regard, Rozing et al. (2010) reported that the offspring of nonagenarian siblings presented a lower thyroidal sensitivity to TSH and a paradoxical beneficial cardiometabolic profile as compared to their partners. The authors concluded that the favorable role of low thyroid hormone metabolism on health and longevity, already observed in animal models, might be applicable to humans as well. However, the study by Rozing et al. (2010) enrolled a specific population in order to identify familial determinants of healthy longevity in nonagenarian siblings. The results might, therefore, be affected by some bias and cannot be extended to the general population. On the other hand, a cross-sectional study by Corsonello et al. (2010) carried out in 604 home-dwelling subjects born in Calabria (southern Italy), with ancestry in the region ascertained up to the grandparents, confirms a declining of serum thyroid hormone levels with ageing. Moreover, lower levels of FT3, FT4 and TSH were found in centenarians’ children and nieces/nephews with respect to age-matched controls. Indeed, the authors conclude that an age-related subtle decline of thyroid function (either due to a familial component or due to a reset of the thyroid function occurring between the sixth and the eighth decade of life) seems to be related to longevity. Two other studies support the hypothesis that mild hypothyroidism in elderly might be associated to a better survival and performance status. In the first, Gussekloo et al. (2006) found lower all-cause and cardiovascular mortality in hypothyroid subjects aged more than 85 years followed for 4 years, when compared with euthyroid individuals. In the second, van den Beld et al. (2005) showed that low-serum T3 (with normal rT3) concentrations were associated with a better survival and physical performance, while subjects with low-serum T3 and high rT3 concentrations (“low T3 syndrome”) did not show any survival advantage and had lower baseline physical activity. The authors suggested that higher serum rT3 concentrations may result from a decreased peripheral metabolism of thyroid hormones due to the ageing process itself and/or disease and may reflect a catabolic state although, a certain degree of lower activity of the thyroid hormone axis might be beneficial during the aging process.
All together, these findings might support the idea that mild physiologically decline of thyroid activity at the tissue level might have favorable effects in the oldest-old subjects. However, the interpretation of the predictive value of thyroid failure in old subjects has to be considered with caution, carefully defining the context and the criteria of analyzed populations. In this setting, the comparison of observational trials is not so easy and the different population analyzed should be taken into account. Indeed, there is not a unique definition of TSH limits for patient classification in the clinical studies or statistical analysis, and the population of published trials is very heterogeneous differing for the age of enrolled patients, life styles, comorbidities, treatments, ethnics etc. Although in some selected elderly subjects (specific ethnic population or very old subjects) (subtle) thyroid failure might be a beneficial factor or a longevity associated character, one of the most debated issues regarding the health consequences of (subclinical) hypothyroidism in the elderly is represented by the potential increase of ischemic heart disease (IHD) or other CVDs as well as cognitive impairment (Mariotti et al., 2005).
5. Subclinical hypothyroidism and cardiovascular diseases
5.1. Pathophysiology
The most characteristic and common symptoms and signs, experienced by patients with thyroid disease, are those related to the cardiovascular (CV) system (Klein & Ojamaa, 2001). Both hyperthyroidism and hypothyroidism produce changes in cardiac contractility, myocardial oxygen consumption, cardiac output, blood pressure, and systemic vascular resistances (SVR) (Dillmann, 2002). Indeed, either hyper or hypothyroidism can produce heart arrhythmias, although it is less well recognized that hypothyroidism may predispose to specific dysrhythmias (Klein & Danzi., 2007). Cardiovascular signs and symptoms of hypothyroidism include bradycardia, mild (diastolic) hypertension, narrowed pulse pressure, cold intolerance, and fatigue (Klein & Ojamaa, 2001).
Subclinical hypothyroidism might be interpreted as an intermediate alteration between overt dysfunction and euthyroidism, consequently, the modifications of CV system observed in sHT qualitatively resemble those produced by overt hypothyroidism even if less evident. Accordingly, several evidences indicated that there is a direct association between serum TSH value and CV alterations as well as blood pressure, cholesterol level etc. (Biondi & Cooper, 2008; Asvold et al., 2007). There are many evidences that, in major part of the cases of thyroid patients, cardiovascular changes are reversible when the underlying thyroid disorder is recognized and treated (Kahaly et al., 2005). Moreover, there is substantial evidence that overt hypothyroidism and also sHT, although to a lesser extent, may alter several of the traditional risk factors for ischemic CVD.
The effects of thyroid hormone deficiency on the cardiovascular system have been evaluated from many points of view as heart diastolic and systolic dysfunction, endothelial dysfunction, hypertension, metabolic alterations and impaired exercise performance (Biondi & Cooper, 2008). To understand well the impact of sHT on CV system and the consequent increased risk of cardiovascular events, it is necessary to review the molecular effects of T3 and T4, and the modifications that they exert in myocytes, endothelium, vascular muscle cells, intermediate metabolism etc. The decrease of cardiac output associated with hypothyroidism results, in part, from changes in cardiac gene expression, specifically reduced expression of the sarcoplasmic reticulum Ca2-ATPase, and increased expression of its inhibitor, phospholamban (Belke et al., 2007). In addition, these molecular changes explain the prolonged isovolumic relaxation phase of the hypothyroid myocardium and early reversible diastolic impairment (Klein & Danzi, 2007). Interestingly, this mechanism functionally resembles the progressive age related myocardium modification, in which increased fibrosis, myocyte hypertrophy and myocyte loss result in increased myocardial stiffness leading to diastolic heart failure (Biondi & Cooper, 2008).
Triiodothyronine produces a decrease in systemic vascular resistance enhancing arteriole dilatation of the peripheral circulation (Klein & Ojamaa, 2001). The endothelium and smooth muscle cells are biological targets of action of T3 with a vasodilatation effect, also in coronary arteries (Ojamaa et al., 1996). As stated by Klein & Ojamaa (2001), T3 induces in vitro relaxation of smooth muscle cells with a non-genomic effect and independently of nitric oxide production (Klein & Ojamaa, 2001). Indeed, Ojamaa et al. (1996) found that the exposure of primary cultures vascular smooth muscle cells to T3 resulted in cellular relaxation within 10 min while, the exposure of primary cultures of vascular endothelial cells to the same hormone did not induce nitric oxide production, suggesting a direct effect of T3 on vascular smooth muscle cells. By contrast, Colantuoni et al. (2005) showed that
Arterial hypertension related to thyroid hormone deficiency may result in aortic stiffness and early atherosclerosis. In this setting, aortic stiffness was studied in 30 patients who never received treatment for hypertension or hypothyroidism, 15 patients with normal blood pressure and hypothyroidism, and 15 patients with hypertension and normal thyroid function. Aortic diameter, evaluated by M-mode echocardiography and blood pressure measured by sphygmomanometer, were assessed to calculate the aortic stiffness index. Patients with hypertension and hypothyroidism have increased aortic stiffness, which was decreased in all patients by hormone replacement therapy, although hypertension resulted completely reversible in 50% of the patients (Dernellis et al., 2002). In addition, it has been hypothesized that thyroid hormone deficiency might be related to endothelial dysfunction. In this area, Lekakis et al. (1997) enrolled 35 subjects with various serum TSH levels to assess endothelial and smooth muscle responses of the brachial artery by high-resolution ultrasound imaging. Results of this study showed that flow-mediated, endothelium-dependent (FMD) vasodilatation progressively impaired with increasing serum TSH value; the phenomenon appearing still in patients with TSH value within the normal reference range (2.01-4.00 microIU/mL) (Lekakis et al., 1997). Furthermore, in order to assess vascular reactivity and NO availability in patients with sHT and its relation to the serum lipid profile, Taddei et al. (2003) evaluated, by strain-gauge plethysmography, the forearm blood flow response to intrabrachial acetylcoline, an endothelium-dependent vasodilator, at baseline and during infusion of the
Another concurring factor for developing early atherosclerosis in hypothyroidism is represented by the metabolic alterations induced by hormone deficiency. Hypothyroidism is characterized by hypercholesterolaemia with elevation of low-density lipoprotein cholesterol (LDLc) levels because of decreased fractional clearance of LDLc by a reduced number of the receptors in the liver (Duntas et al., 2002; Staub et al., 1992). Early studies in hypothyroid humans, using isotopically labeled LDLc, demonstrated a prolonged half-life of LDLc due to a decreased catabolism; this effect was reversible with LT4 therapy (Walton et al., 1965). Accordingly, the addition of T3 to human fibroblast cultures induced a higher LDLc degradation, through an increase in LDLc receptor number, without any receptor affinity change (Chait et al., 1979). Molecular mapping has revealed functional thyroid response elements in the promoter region of the LDLc receptor. Indeed, specific stimulation by T3 of a chimeric gene resulting from the LDLc receptor promoter linked to a reporter gene, cotransfected with the isoform of the thyroid hormone receptor into a hepatic cell line, has been reported (Bakker et al., 2001). Moreover, the deletion of the upstream thyroid response elements in the LDLc receptor promoter inhibited T3-mediated reporter gene activity (Cappola et al., 2003). Although the relationship between thyroid function and altered lipid profile is well documented in overt hypothyroidism it is still controversial in sHT (Biondi & Cooper, 2012). The conflicting results about lipid profile and sHT might reflect differences in study design as well as in age, gender, and ethnicity of the study cohorts (Palmieri et al., 2002).
Various changes in the coagulation-fibrinolytic system have been described in patients with thyroid dysfunction although, data regarding the association between thyroid failure and modifications of the coagulation-fibrinolytic system are still controversial (Chadarevian et al., 2001; Canturk et al., 2003; Muller et al., 2001). The influence of thyroid hormone on the coagulation fibrinolytic system is mainly mediated by the interaction between the hormone and its receptors (Shih et al., 2004). Various abnormalities have been described, ranging from subclinical laboratory abnormalities to major hemorrhages or fatal thromboembolic events (Squizzato et al. 2007). The relationship between thyroid hormones and the coagulation system is, however, often ignored. One of the reasons could be that, although several in vivo abnormalities have been reported in patients with hypothyroidism and hyperthyroidism, most published studies focus on laboratory measurements, and good studies on the relationship between thyroid dysfunction and clinically manifest bleeding or thrombosis are lacking. However, most studies confirm that both overt hyper- and hypothyroidism modify the coagulation-fibrinolytic balance. Thyroid hormone excess or deficit is the probable main pathophysiological mechanism and, patients with overt hypo- and hyperthyroidism appear to have an increased risk of bleeding and of thrombosis, respectively (Squizzato et al. 2007).
Overall, these findings support a biologically plausible role for hypothyroidism in increasing the risk of atherosclerotic CV disease, via the increase in circulating levels of LDLc, systemic (diastolic) hypertension, diastolic dysfunction and heart failure as well as an imbalance of the coagulation system and direct effects on vascular smooth muscle (Cappola et al., 2003). However, the actual relationship between sHT and increased cardiovascular risk is still unresolved and represents one of the most common topics in endocrinology, leading to several controversies concerning the clinical management of sHT patients (Turemen et al., 2011).
5.2. Clinical evidences
As above described, thyroid hormone deficiency is associated to several cardiovascular and metabolic abnormalities (Biondi & Cooper, 2008; Caraccio et al., 2003; Dardano & Monzani, 2008). Indeed, thyroid failure may favour the onset of several CV risks like diastolic hypertension, hyperlipidemia, vascular stiffness, heart failure etc. However, although the relationship between overt hypothyroidism and coronary heart disease (CHD) as well as increased CHD mortality is widely recognized (Klein, 2004), the clinical significance of sHT is still controversial and conflicting opinions remain on the association between sHT and CVD or mortality, especially in older people (Biondi & Cooper, 2008; Monzani et al., 2006). Indeed, data regarding the association between sHT and CHD or total mortality are contradictory among various population based, observational studies (Aho et al., 1984; Cappola et al., 2004; Hak et al., 2000; Walsh et al., 2005).
One of the first large study (Whickham Survey) that evaluated vascular events over 20 years in community-dwelling subjects stratified by thyroid function and thyroid autoantibody status did not show any association between CHD and sHT (Vanderpump et al., 1995). This result appeared at odds with the findings of other subsequent cohort studies (Hak et al., 2000; Imaizumi et al., 2004; Walsh et al., 2005). However, while reanalyzing incident CHD events and mortality in Whickham participants including LT4 replacement during follow-up as covariate, a significant increment of incident CHD events and mortality was found in individuals with baseline sHT (Razvi et al., 2010). Based on the results of this analysis, it would appear that treatment of sHT might be associated with reduced mortality as well as CHD events. However, besides the small total number of events in each group of sHT participants, there is a potential for bias in this retrospective observational analysis (i.e. sHT patients who were treated may have been more health conscious leading to a healthy user bias). Therefore, these results need to be interpreted with caution until a large prospective, randomized controlled trial will be available. The inconsistency in results among several studies (Aho et al., 1984; Hak et al., 2000; Cappola et al., 2004; Razvi et al., 2010; Walsh et al., 2005) may be due to differences in the enrolled populations as well as the duration either of tissues exposure to sHT or of follow-up of the various studies. Nonetheless, meta-analyses of CHD events and sHT have shown that such an association probably exists (Razvi et al., 2008; Rodondi et al., 2006), especially in younger cohorts. In this regard, to assess the risks of CHD and total mortality for adults with sHT, Rodondi et al. (2010) carried out a large meta-analysis on 11 prospective cohorts, enrolling a total of 55,287 participants. The risk of CHD events was examined in 25,977 participants from 7 cohorts with available data. Among 55,287 adults, 3450 had sHT (6.2%) and 51,837 were euthyroid. The Authors found that the risk of CHD events and mortality increased with higher TSH concentrations. Results were similar after adjustment for traditional cardiovascular risk factors. Moreover, this pooled analysis showed a higher rate of CHD events in sHT patients with higher TSH levels (>10 mIU/L). These data are consistent with most previous meta-analysis and several naturalistic studies, showing an increased risk of CHD events associated with sHT (Hak et al., 2000; Singh et al., 2007; Walsh et al., 2005).
These studies, however, did not accurately explore potential differences related to participant characteristics like age, even if older people represented large a share of the population. In this setting, the pooled analysis of large cohort of patients may be affected by hypothetical bias and may not investigate specific classes of patients like very old people versus moderate elderly patients or other specific conditions affecting the clinical outcome. Ochs et al. (2008) analysed in a meta-analysis the effect of ageing on sHT associated CV events and total mortality. Similar to previous meta-analysis, they found a pattern of modestly increased risk for CHD and mortality associated with sHT. A weak evidence for statistical heterogeneity among individual study findings was found, and age explained part of the heterogeneity for the association between sHT and CHD, with an increased risk for CHD only in cohorts with a younger mean age. Accordingly, Cappola et al. (2006), in a large population-based, longitudinal study of coronary heart disease and stroke in adults aged 65 years and older, concluded that the results did not support the hypothesis of an association between unrecognized sHT and increased CV events or mortality. On the other hand, one cross-sectional study with subgroup analyses by age found that increased risk for CHD was present in younger sHT participants only (<50 years old) (Kvetny et al. 2004). In this regard, a prospective, observational, population-based follow-up study carried out on 599 participants followed up from age 85 years through age 89 years showed no association between serum TSH and FT4 levels and disability in daily life, depressive symptoms, and cognitive impairment at baseline or during follow-up. Moreover, increasing serum TSH levels were associated with a lower mortality rate that remained after adjustments for baseline disability and health status (Gusseklo et al. 2004). Overall, these data support the hypothesis that in the oldest old population, individuals with abnormally high levels of TSH do not experience adverse effects and may have a prolonged life span. The study focused on a specific class of patients (very older people), for this reason, the results should be rigorously interpreted, also considering the weakness of observational studies. However, these data together with the results obtained by Rozing et al., (2010) that demonstrated a possible genetic predisposition of nonagenarians to a decrease function of hypothalamus-pituitary-thyroid axis, suggest that the oldest old may represent a different population respect to moderate old people or young adults. Potential explanations for these age differences might be competing mortality among older adults (for example, due to cancer) or more competing risk factors for CHD among older adults (for example, age or sex). However, the above reported substantial age differences should be interpreted with caution, given the possibility of ecological fallacy without individual patient data and, should be confirmed by stratified analyses in future prospective cohort studies with a wide age range (Egger et al., 2001).
There are few clinical studies evaluating the effects of hormone replacement in sHT subjects and none aimed to determine the impact of therapy on total mortality especially in older people. Previous research in this area has shown contradictory results, with some randomized, controlled trials (number of patients ranging from 45 to 63) showing an improvement in the atherogenic lipid profile as well as surrogate endpoints of atherosclerosis (Meier et al., 2001; Caraccio et al., 2002; Monzani et al., 2004) but others (number of patients ranging from 17 to 35) showing no difference (Cooper et al., 1984; Jaeschke et al., 1996; Kong et al., 2002; Nystrom et al., 1988). Recently, Razvi et al. (2007) conducted a randomized, double-blind, crossover study to determine the short-term (12 weeks) effect of LT4 replacement therapy in 100 sHT patients (age range 18-80 yrs, mean 53.8) with serum TSH level>4.0 mIU/L. Primary end points included: serum cholesterol level variations along with improvement in flow-mediated dilation (FMD) as a marker of vascular endothelial function. LT4 treatment significantly reduced either TC or LDLc concentrations, and improved FMD, as compared to placebo group. Moreover, multivariate analysis showed that increased serum FT4 level was the most significant variable predicting reduction in TC or FMD improvement. The Authors hypothesized that if the reduction of LDLc level would be long term sustained, this would result in a relative reduction in 10-yr CV mortality of about 10%, thus supporting the use of LT4 replacement therapy also in patients with slightly elevated TSH value. Long-term studies are nonetheless required to confirm whether these apparent short-term benefits will translate into reduction in CV mortality and morbidity. Moreover, notwithstanding the wide age range of the studied patients, these results cannot directly transfer to the elderly, especially the oldest old population.
In summary, conflicting results among large prospective cohort studies regarding the relationship between sHT and cardiovascular disease might reflect differences in participants such as age, gender, TSH value, or pre-existing cardiovascular disease. However, as demonstrated by some meta-analyses, the negative effect of sHT on cardiovascular risk is well established in younger people while in moderately old population (>65 and <85 years) it appears no longer evident. Moreover, in the oldest old people (>85 years) one study suggested that high levels of TSH not only do not exert adverse effects but also may favor a prolonged life span (Fig. 1). In this regard, elderly population can be interpreted as a heterogeneous group, nonagenarians representing a genetically selected cluster. Indeed, these subjects may have a genetic background that protects from CVD and/or thyroid hormone deficiency, thus suggesting an intriguing link between gene, thyroid status and longevity.
6. Thyroid function and cognitive impairment
Thyroid hormones are crucial for brain development and function: thyroid failure at any age causes cognition to deteriorate because thyroid hormones are essential for adequately sustaining the energy (glucose)-consuming processes needed for neurotransmission, memory, and other higher brain functions (Herholz, 2010; Patel et al., 2011). Low brain uptake of glucose is commonly associated with deteriorating cognition and Alzheimer’s disease and can be present decades before clinical evidence of Alzheimer’s disease occurs (Herholz, 2010). Brain hypometabolism therefore appears to be a precursor lesion increasing the risk of at least some forms of cognitive decline. Elevated TSH levels in the range found in patients with overt hypothyroidism have been described to be associated with impaired function in many cognitive domains, but the association between sHT and cognition is less clear (Graham et al., 1997; Gardner, 2004; Chavanne et al., 2011). On the other hand, several cross-sectional studies have observed that high or low TSH levels, still within the normal range (clinically euthyroid), are each related to poor cognitive performance, although some other investigations failed to demonstrate these findings (Prinz et al., 1999; Volpato et al., 2002). It should be underlined, however, that different cognitive deficits possibly related to thyroid failure do not necessarily follow a consistent pattern, and LT4 treatment may not always completely restore normal functioning in patients with hypothyroidism. Giving these premises, we summarize here the growing, conflicting literature on the relationship between cognitive performance and thyroid function from an ageing perspective.
Subclinical hypothyroidism and cognitive function have been investigated in several preclinical experiments and clinical trials. To date, the actual relationship between mild thyroid hormone deficiency and cognitive impairment in the elderly is not well understood. In fact, there are several contrasting data resulting from cross-sectional and clinical experiments (Gussekloo et al., 2004; Roberts et al., 2006; Tan et al., 2008; Ceresini et al., 2009). Moreover, the available published data, in many cases, are not easily comparable considering the differences in inclusion criteria of each clinical study. Several small observational and interventional studies have reported an association, although not homogeneously, between cognitive impairment and sHT and, in some cases, it was described a cognitive performance improvement after LT4 replacement (Etgen et al., 2011; Monzani et al., 1993; Osterweil et al., 1992; St. John et al., 2009; Volpato et al., 2002). Moreover, Hogervost et al. (2008) studied the association between TSH and FT4 levels and cognition at baseline and after 2 years of follow-up in 1047 participants over 64 years of age, without physical frailty or severe cognitive impairment. The study showed that elevated TSH levels were associated with lower MMSE performance at baseline, independently of FT4 value, age, sex, education and mood. Interestingly, epidemiological surveys using the revised Wechsler Adult Intelligence Scale (WAIS-R) and the Mini-Mental State Examination (MMSE) showed a relationship between plasma thyroid hormone levels and cognitive status in subjects with thyroid function still within the upper limit of the normal range (Prinz et al., 1999; Volpato et al., 2002). Accordingly, altered plasma thyroid hormone concentrations have been recognized as a risk factor for cognitive impairment or dementia (Bulens, 1981; Kalmijn et al., 2000; Tan et al., 2008). More specifically, with the increasing sensitivity of neuropsychological tools, it has become evident that thyroid hormone deficiency might produce measurable deficits in very specific neuropsychological functions (Zoeller & Rovet 2004). In this regard, in a recent prospective, open-labeled interventional study, cognitive impairment associated with (mild) thyroid failure appeared predominantly mnemonic in nature, suggesting that the etiology is not indicative of general cognitive slowing (Correia et al., 2009).
Conflicting data were obtained by large, population-based studies, leading to uncertain conclusions regarding the association between (mild) thyroid failure and cognition (Gussekloo et al., 2004; Roberts et al., 2006; Tan et al., 2008; Ceresini et al., 2009). In this setting, one critical point that could affect the results of these studies is the diverse age groups of the enrolled patients (moderate or very old) as well as the presence of comorbidity. Cognitive impairment observed in older sHT individuals might be also an epiphenomenon of the increased risk for atherosclerosis or the effect of thyroid hormone on vasculature. Indeed, arterial stiffness is a potential mechanism of advancing cognitive decline in sHT (Yamamoto et al., 2012) and elevated TSH values might negatively affect vascular function through systemic low-grade inflammation (Taddei et al., 2006). Moreover, whereas in moderate older people sHT might produce a detrimental effect on cognitive performance, in very old individuals (mild) thyroid failure might be not associated to a negative outcome (Gussekloo et al., 2004; Tan et al., 2008). To determine whether subclinical thyroid dysfunction should be treated in old age and the long-term impact of thyroid dysfunction on performance and survival in the elderly, a prospective, observational, population-based survey was carried out within the Leiden 85-Plus Study. A total of 599 participants were followed up from age 85 years through age 89 years. Plasma levels of TSH and FT4 were not associated with disability in daily life, depressive symptoms, and cognitive impairment at baseline or during follow-up. Conversely, increasing levels of TSH were associated with a lower mortality rate that remained after adjustments were made for baseline disability and health status (Gussekloo et al., 2004). It is noteworthy, however, that similarly to CHD risk, these results should be confirmed by stratified analyses in future prospective large cohort studies with a wide age range.
Another important aspect is the possible relationship between sHT and the risk to develop Alzheimer disease (AD). On this basis, many studies investigated a possible association between AD and thyroid dysfunction. Increasing evidence supports an extensive interrelationship between thyroid hormones and the cholinergic system, which is selectively and early affected in AD. Thyroid hormones negatively regulate expression of the amyloid-beta protein precursor, which plays a key role in the development of AD (Belakavadi et al., 2011). In a study aimed to examine the feasibility of using thyroid hormone as a therapeutic agent for AD, mice were injected intra-hippocampally with aggregated amyloid beta-peptide (Abeta) to produce AD animal model. Intraperitoneal administration of LT4 into Abeta-induced AD model mice prevented their cognitive impairment and improved their memory function. The authors suggested that the mechanisms of LT4 treating AD might be associated with regulating cholinergic function, protecting the brains of AD model mice against damage and rescuing hippocampal neurons from apoptosis. The results of this study seem indicate that the use of thyroid hormone may have some therapeutic potential in AD (Fu et al., 2010). Accordingly, in a post mortem study it was evaluated the brain thyroid hormone levels in AD measured with radioimmunoassay (RIA) samples of prefrontal cortex of patients with pathologically confirmed AD and controls without any primary neurological disease. Thyroxine levels did not differ between groups while T3 levels were significantly lower in Alzheimer’s brains respect to controls. These results suggest that the conversion of T4 to T3 may be altered in advanced AD, perhaps due to modifications in deiodinase activity, and the reduced hormone conversion might be associated with both AD pathology and the clinical presentation of dementia (Davis et al., 2008). Moreover, Tan et al. (2008) related serum TSH concentrations to the risk of Alzheimer disease in 1864 cognitively intact, euthyroid participants of the Framingham original cohort (mean age 71 years). During a mean follow-up of 12.7 years, 209 participants (142 women) developed AD. Women in the lowest (<1.0 mIU/L) and highest (>2.1 mIU/L) tertiles of serum TSH concentration were at increased risk for AD compared with those in the middle tertile while, TSH levels were not related to AD risk in men. On the other hand, at odds with these findings, the InChianti study showed an association between subclinical hyperthyroidism and cognitive impairment without any correlation with mild thyroid failure in a large cohort of older people (Ceresini et al., 2009).
In conclusion, a certain degree of cognitive (mnemonic) impairment is generally recognized in case of overt hypothyroidism while, the relationship between cognition and sHT is still a disputed field, and it remains unclear whether to treat or not this kind of patients. In particular, there is little or no consensus in the literature whether thyroid failure is associated with impaired cognitive performance in the elderly, especially in the oldest old population. While interpreting the above reported conflicting results it should be outlined, however, that thyroid hormone concentrations change with age and cognitive decline is often concomitant with ageing; therefore, a reciprocal relationship could exist between changes of thyroid function and cognitive decline during normal ageing.
7. Conclusions
Levothyroxine replacement therapy for reducing sHT associated CV risk factors is still controversial, especially in the elderly. The lack of specific randomized trials, enrolling either old or very old subjects, aimed to evaluate the efficacy of hormonal replacement on overall survival and cardiovascular risk reduction as well as the possible negative effects of LT4 supplementation, makes the decision to treat elderly people very difficult. Generally, LT4 replacement therapy should be considered for three main reasons: i) to prevent progression of sHT to overt hypothyroidism which, however, is much more important in young patients; ii) to reduce the symptoms associated with mild thyroid failure, which are especially scarce in the elderly; iii) to improve the lipid profile and other risk factors that may contribute to atherosclerosis progression and CV events.
Subclinical thyroid failure causes changes in cardiac function similar to, but less marked than, those occurring in patients with overt hypothyroidism. Diastolic dysfunction both at rest and upon effort is the most consistent cardiac abnormality in patients with sHT, even in those with slightly elevated TSH levels (>6 mIU/L) (Arem et al., 1996; Biondi & Cooper, 2012;). Mild thyroid failure may also increase diastolic blood pressure as a result of increased systemic vascular resistances (Faber et al., 2002; Kahaly, 2000; Luboshitzky et al., 2002). Interestingly, restoration of euthyroidism by LT4 replacement is able to reduce systemic hypertension as well as improve left ventricular myocardial function (Brenta et al., 2003). Moreover, sHT has been claimed to be a risk factor for atherosclerosis and ischemic CVD, therefore, it is appropriate to consider whether treatment confers some protection from such a risk. Although a consensus is still lacking, the strongest evidence for a beneficial effect of levothyroxine replacement therapy is the substantial demonstration that restoration of euthyroidism can lower TC and LDLc levels in most patients with sHT. Besides hypercholesterolemia several emerging risk factors for CHD have been claimed to be associated with sHT. Among them, altered coagulation parameters, endothelial dysfunction, and elevated CRP levels are consistently regarded to combine with the raised LDLc levels of untreated patients with sHT to enhance the cardiovascular risk.
As a whole, these findings suggest that the decision to treat patients with sHT should depend on the presence of risk factors, rather than on a TSH threshold. International organizations and guidelines suggest starting replacement therapy in patients who have TSH concentrations greater than 10 mIU/liter and in those with evidence of autoimmunity, and in symptomatic patients with TSH levels between 4.5 and 10 mIU/L (Gharib et al., 2005a,b; Surks et al., 2004). However, the treatment of sHT patients, especially the elderly, must be individualized once any underlying coexisting morbidity or pharmacologic interference has been excluded. Generally LT4 replacement results effective and safe in young patients, providing that excessive dosing is avoided by monitoring serum TSH level. Indeed, LT4 replacement therapy can always be discontinued if there is no apparent benefit. It is noteworthy that, once a stable, elevated TSH value is detected, the costs of annual follow-up with clinical assessment and laboratory testing are relatively similar whether or not a patient is treated with LT4 (Cooper et al., 2001). On the other hand, the possibility that restoring euthyroidism may be harmful in the older population has been raised, and should be taken into account in making the decision of treating such patients, especially those older than 85 years. In this setting, hormonal replacement might be considered in old patients on the base of a specific evaluation of the possible thyroid dysfunction causes, pre-existent cardiovascular risk including cholesterol level, hearth failure as well as the presence of comorbidities or frailty and the level of TSH. However, until adequate data are accumulated, clinicians should consider each patient a unique situation, and best clinical practice continues to be a combination of clinical judgment and the patient’s preference.
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