An update on heart disease risk associated with testosterone boosting medications

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Abstract

Introduction: The cardiovascular (CV) safety of testosterone replacement therapy (TRT) remains a crucial issue in the management of subjects with late onset hypogonadism. The authors systematically reviewed and discussed the available evidence focusing our analysis on heart related issues.

Areas covered: All the available data from prospective observational studies evaluating the role endogenous T levels on the risk of acute myocardial infarction (AMI) were collected and analyzed. In addition, the impact of TRT on heart related diseases, as derived from pharmaco-epidemiological studies as well as from randomized placebo controlled trials (RCTs), was also investigated.

Expert opinion:
Available evidence indicates that endogenous low T represents a risk factor of AMI incidence and its related mortality. TRT in hypogonadal patients is able to improve angina symptoms in subjects with ischemic heart diseases and exercise ability in patients with heart failure (HF). In addition, when prescribed according to the recommended dosage, TRT does not increase the risk of heart-related events.




Article highlights

Low endogenous testosterone (T) is associated with an increased risk of acute myocardial infarction (AMI)-related mortality and AMI incidence.

Testosterone replacement therapy (TRT) in hypogonadal patients is able to improve angina symptoms in subjects with ischemic heart diseases and exercise ability in patients with heart failure.

In 2014, the European Medical Agency (EMA) did not share the FDA’s opinion of an increased CV risk linked to T medication, because of the lack of convincing evidence.

The analysis of all randomized placebo controlled controlled trials showed that when prescribed according to the recommended dosage, TRT does not increase the risk of heart-related events.






4.0 Conclusions

The studies critically scrutinized here clearly show that low T is a marker of poor CV outcomes, including CAD. Meta-analysis of retrospective observational studies suggest that correcting T deficiency marginally improves cardiac outcomes. However, many of the weaknesses linked to pharmaco-epidemiological studies, here discussed, hamper confidence in this conclusion. Meta-analysis of interventional studies having cardiac outcomes as a primary end-point suggest an acute and chronic positive effect of TRT on increasing time to ST-segment depression and in some measures of HF. However, all these studies were of short duration and enrolling a limited number of subjects and therefore they are underpowered. In addition, they may have overlooked early positive transient effects. Nevertheless, prospective studies of longer duration enrolling hypogonadal subjects having cardiac safety as a primary end-point are difficult to realize, due to ethical reasons. For all these reasons, we here summarize in Forest plots results from different meta-analyses of available RCTs not having cardiac outcomes as an endpoint, but reporting information on them. Overall, included trials were of low-to-medium quality, enrolling subjects with variable characteristics, using different TRT protocols for various duration and, again, not powered to evaluate cardiac events. Meta-analysis is particularly useful when there are a variety of reports with low statistical power; thus, pooling data can improve power and provide a convincing result. All the different meta-analyses indicate that there is no significant risk for TRT in several cardiac outcomes, including AMI and acute coronary syndrome. It is important to recognize that all the available trials included in the meta-analyses have a relatively short duration, lasting at maximum three years. Therefore, although there is no clear sign of risk in the short term, no information is available on possible long-term effects. Considering that TRT is meant to be a lifelong treatment in the majority of cases the last issue is a relevant point. In conclusion, five years later, we fully endorse the EMA statement concerning TRT saying: “evidence regarding the risk of heart problems was inconsistent” (12). A new trial (TRAVERSE; clinicaltrials.gov, NCT03518034) to evaluate the effect of TRT on the incidence of MACE and efficacy measures in men with hypogonadism is ongoing. This is the first TRT trial with adequate power to assess CV events in hypogonadal population and it will give important information on this topic in the near future.



















Important point for everyone to keep in mind!


* A new trial (TRAVERSE; clinicaltrials.gov, NCT03518034) to evaluate the effect of TRT on the incidence of MACE and efficacy measures in men with hypogonadism is ongoing. This is the first TRT trial with adequate power to assess CV events in hypogonadal population and it will give important information on this topic in the near future.
 

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4. Conclusion

The therapeutic approach for TT for symptomatic hypogonadism and low testosterone levels associated with aging, obesity, and systemic illness presents challenges. These conditions are intricately linked with CVD outcomes and may confound the relationship between low testosterone and CVD. Although observational studies suggest an association between low testosterone and increased risk of CVD, results from testosterone supplementation are inconsistent. RCTs indicate that short-term TT at standard replacement is not associated with increased CVD risk. Nevertheless, the cardiovascular sub-study of T Trials observed increases in NCP and CAC, signaling the need for further investigation into potential long-term implications of TT.

The TRAVERSE trial, a landmark study unique in its capacity to evaluate CVD events, contributes valuable insights into the short-term safety of TT at lower physiological levels. However, the long-term effects and implications of mid to high physiological testosterone levels are not yet fully understood. The trials’ limitations — achievement of only low-normal testosterone levels, high discontinuation rates, brief follow-up period, and high loss to follow-up rate — suggest that the findings should be interpreted with caution. It is important to avoid generalizing the safety of TT based on these results alone and to approach the extrapolation of TRAVERSE’s conclusions to higher dosages or longer-term therapy with caution.

The decision to initiate TT requires a nuanced approach, which must account for current gaps in evidence regarding CV safety. A personalized assessment and management of CVD risk factors is essential for older men with known CVD. The CV effects of exogenous testosterone, when given to maintain physiological levels, remain to be fully explored. In this regard, an important question remains the identification of male patients with symptomatic hypogonadism who may benefit from TT. This topic continues to be the subject of ongoing debate. Hopefully, future trials will provide clarity on whether TT confers beneficial, neutral, or adverse cardiovascular effects in middle-aged and older men. Until definitive evidence surfaces, clinical practice should exercise caution and prioritize individualized care with informed discussions regarding the potential CV implications of TT.
 
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