madman
Super Moderator
Abstract
Introduction: Testosterone therapy (TTH) for testosterone deficiency (TD) may lead to elevated estradiol (E2) levels requiring management to avoid unnecessary adverse effects.
Aim: To examine the impact of aromatase inhibitors, specifically anastrozole (AZ), in men with elevated E2 on TTH.
Methods: All patients on TTH at a high volume sexual medicine practice between 2005 and 2019 were reviewed. Men with E2 levels >60 pg/mL regardless of symptoms or 40−60 pg/mL with subjective symptoms were started on AZ 0.5 mg 3x/week. Routine hormone profile and symptom assessment were completed to ensure symptom resolution, reduction of E2 levels, and maintenance of testosterone levels. Multivariable logistic regression was completed to determine predictors of men more likely to respond to therapy.
Main Outcome Measure: Demographics and hormonal profiles of men on AZ and predictors of response to therapy.
Results: 1708 men with TD were placed on TTH. Of these, 51 (3%) were treated with AZ (AZ+). After exclusions, 44 (2.6%) had elevated estradiol levels >60 pg/mL or >40 pg/mL with symptoms. Demographics were similar between groups. TTH distribution between groups was different with greater rates of topical TTH in the AZ- groups (AZ+:34.1% vs AZ-:53.5%) and greater rates of intramuscular TTH in the AZ+ group (AZ+:38.6% vs AZ-:18.5%) (P=.017 overall). Of the 44 men treated with AZ, 68.0% had pre-AZ E2 levels ≥60 pg/mL and 32.0% had levels between 40 and 60 pg/mL. Median pre-AZ E2 levels were 65 (interquartile range [IQR], 55−94) pg/mL in comparison to 22 (IQR 15−38) pg/mL post-AZ E2 levels (P < .001). Total testosterone levels were similar before and after AZ use (616 (IQR 548−846) ng/dL and 596 (IQR 419−798) ng/dL, respectively, P=.926). No statistically significant predictive factors of E2 reduction using AZ were found.
Conclusion: While no statistically significant predictors for E2 recovery in men on AZ were found, AZ remains a reasonable option for E2 reduction in men with elevated levels on TTH.
INTRODUCTION
Testosterone deficiency (TD) occurs in 6−25% of men.1,2 As per the American Urological Association guidelines, treatment of low testosterone (T) is indicated if the levels are below the threshold of 300 ng/dL associated with signs or symptoms.2 TTH may increase estradiol (E2) levels via aromatase enzyme activity (aromatization), which converts T to E2.3 Anastrozole (AZ) is an aromatase inhibitor that targets aromatase preventing conversion.4
In general, AZ is indicated to delay epiphyseal maturation in adolescent boys but has been used in infertile males with TD and elevated E2 levels to preserve spermatogenesis.4 The AZ side effect profile has been studied extensively in women and is a well-tolerated medication.4 Elevated E2 level is most commonly associated with gynecomastia but is not the only responsible mechanism.5
*AZ has been used to treat men with elevated E2, but currently, limited evidence and/or guidelines exist for the optimal management of elevated E2 levels in men on TTH.
Given this, we specifically explore if our proposed management strategy for elevated E2 levels with AZ was effective in reducing E2 levels while maintaining appropriate T levels and if we could determine any predictors of those most likely to respond?
METHODS
Study Population: Data were retrospectively reviewed for all TD men at a single center high volume sexual medicine practice between 2005 and 2019. Men were considered to have TD if they had documented T levels <300 ng/dL on two separate occasions with associated signs or symptoms. In the absence of guidelines for the use of AZ in men TD men with elevated E, men with either E2 levels >60 pg/mL or 40−60 pg/mL with subjective symptoms (ie, breast or nipple tenderness) were started on anastrozole 0.5mg three times per week (off-label). Men were excluded if they were started on AZ by an external physician as baseline estradiol levels were unknown, or if they had breast cancer. Demographic comorbidity and TTH modality data were recorded. Study approval was obtained from the Institutional Review Board at Memorial Sloan Kettering Cancer Center (IRB 16-1526).
Laboratory Assessment and Titration: T levels were assessed using liquid chromatography-mass spectrometry (LCMS) (50% pre-AZ and 57% post-AZ) and were completed before 10 AM. E2 levels were assessed similarly by LCMS each time T levels were measured by LCMS. Free T and luteinizing hormone (LH) were also measured. E2 levels were titrated between 20 and 40 pg/mL through either modulation of frequency and/or dosage of AZ. Hormone levels were recorded before (baseline) and after AZ commencement.
DISCUSSION
Men receiving exogenous TTH may experience side effects, including elevations in E2 levels, which may impact libido and cause gynecomastia. AZ is a safe and effective option for men with elevated E2. Our study evaluated men with TD in which a small subset had elevated E2 requiring intervention (AZ). Overall, we demonstrated a statistically significant reduction in E2 levels to normal physiologic levels with the maintenance of T levels but were unable to identify predictors for men most likely to respond to therapy.
Only 2.6% of men had E2 which warranted treatment with AZ. AZ has been used in men with TD in an effort to reduce the conversion to E2 to T while maintaining fertility.6 We employed a cut-off for the use of AZ, but the literature does not support a clear cut-off or indication for the initiation of estradiol-lowering therapy.7 Similar to our series, in a national sample, 3.5% (1,200/34,016) of men were placed on an AI.7
Almost all men had recovery of E2 within normal levels (<40 pg/mL) with simultaneous maintenance of a serum T. This highlights the importance of appropriate regulation given the important physiological processes regulated by E2.
No statistically significant predictors were found in our series to predict E2 recovery in men on AZ. To the best of our knowledge, this has not been previously reported. Furthermore, limited data exists with respect to a clear cut-off or consideration of response to AZ, and therefore our composite cut-off was suggested based on a clinically meaningful response.
*The clinical implications of AZ in men with elevated E2 while on TTH are evident. Given the importance of E2 in male physiology and the impact of TTH on E2, careful monitoring by practitioners providing exogenous therapy is critical.
Limitations to our study include the retrospective design, but all data were collected prospectively. The study does have limited external validity as data were obtained from a single institution and a single provider. We also did not discern nor account for possible physiologic differences in men on AZ on clomiphene citrate versus those on exogenous TTH. We were not able to validate if AZ or clomiphene citrate did not interfere with E2 immunoassay testing. Furthermore, all men did not have measurements completed by LCMS but were included in order to obtain a reasonable sample size. A sensitivity analysis only using LCMS measurements revealed similar results (Supplementary Table 3). Finally, while the number of men on AZ in our series is small which limited statistical analysis for predictors of estradiol recovery, the total number of men assessed with TD was significant and over a large period of time.
CONCLUSION
In patients with elevated E2 on TTH, using AZ 0.5mg TID, results in a statistically significant reduction in E2, with 76% completely normalized with simultaneous maintenance of T levels. No statistically significant predictors were found for the recovery of E2 levels. Further research and larger studies are warranted.
Introduction: Testosterone therapy (TTH) for testosterone deficiency (TD) may lead to elevated estradiol (E2) levels requiring management to avoid unnecessary adverse effects.
Aim: To examine the impact of aromatase inhibitors, specifically anastrozole (AZ), in men with elevated E2 on TTH.
Methods: All patients on TTH at a high volume sexual medicine practice between 2005 and 2019 were reviewed. Men with E2 levels >60 pg/mL regardless of symptoms or 40−60 pg/mL with subjective symptoms were started on AZ 0.5 mg 3x/week. Routine hormone profile and symptom assessment were completed to ensure symptom resolution, reduction of E2 levels, and maintenance of testosterone levels. Multivariable logistic regression was completed to determine predictors of men more likely to respond to therapy.
Main Outcome Measure: Demographics and hormonal profiles of men on AZ and predictors of response to therapy.
Results: 1708 men with TD were placed on TTH. Of these, 51 (3%) were treated with AZ (AZ+). After exclusions, 44 (2.6%) had elevated estradiol levels >60 pg/mL or >40 pg/mL with symptoms. Demographics were similar between groups. TTH distribution between groups was different with greater rates of topical TTH in the AZ- groups (AZ+:34.1% vs AZ-:53.5%) and greater rates of intramuscular TTH in the AZ+ group (AZ+:38.6% vs AZ-:18.5%) (P=.017 overall). Of the 44 men treated with AZ, 68.0% had pre-AZ E2 levels ≥60 pg/mL and 32.0% had levels between 40 and 60 pg/mL. Median pre-AZ E2 levels were 65 (interquartile range [IQR], 55−94) pg/mL in comparison to 22 (IQR 15−38) pg/mL post-AZ E2 levels (P < .001). Total testosterone levels were similar before and after AZ use (616 (IQR 548−846) ng/dL and 596 (IQR 419−798) ng/dL, respectively, P=.926). No statistically significant predictive factors of E2 reduction using AZ were found.
Conclusion: While no statistically significant predictors for E2 recovery in men on AZ were found, AZ remains a reasonable option for E2 reduction in men with elevated levels on TTH.
INTRODUCTION
Testosterone deficiency (TD) occurs in 6−25% of men.1,2 As per the American Urological Association guidelines, treatment of low testosterone (T) is indicated if the levels are below the threshold of 300 ng/dL associated with signs or symptoms.2 TTH may increase estradiol (E2) levels via aromatase enzyme activity (aromatization), which converts T to E2.3 Anastrozole (AZ) is an aromatase inhibitor that targets aromatase preventing conversion.4
In general, AZ is indicated to delay epiphyseal maturation in adolescent boys but has been used in infertile males with TD and elevated E2 levels to preserve spermatogenesis.4 The AZ side effect profile has been studied extensively in women and is a well-tolerated medication.4 Elevated E2 level is most commonly associated with gynecomastia but is not the only responsible mechanism.5
*AZ has been used to treat men with elevated E2, but currently, limited evidence and/or guidelines exist for the optimal management of elevated E2 levels in men on TTH.
Given this, we specifically explore if our proposed management strategy for elevated E2 levels with AZ was effective in reducing E2 levels while maintaining appropriate T levels and if we could determine any predictors of those most likely to respond?
METHODS
Study Population: Data were retrospectively reviewed for all TD men at a single center high volume sexual medicine practice between 2005 and 2019. Men were considered to have TD if they had documented T levels <300 ng/dL on two separate occasions with associated signs or symptoms. In the absence of guidelines for the use of AZ in men TD men with elevated E, men with either E2 levels >60 pg/mL or 40−60 pg/mL with subjective symptoms (ie, breast or nipple tenderness) were started on anastrozole 0.5mg three times per week (off-label). Men were excluded if they were started on AZ by an external physician as baseline estradiol levels were unknown, or if they had breast cancer. Demographic comorbidity and TTH modality data were recorded. Study approval was obtained from the Institutional Review Board at Memorial Sloan Kettering Cancer Center (IRB 16-1526).
Laboratory Assessment and Titration: T levels were assessed using liquid chromatography-mass spectrometry (LCMS) (50% pre-AZ and 57% post-AZ) and were completed before 10 AM. E2 levels were assessed similarly by LCMS each time T levels were measured by LCMS. Free T and luteinizing hormone (LH) were also measured. E2 levels were titrated between 20 and 40 pg/mL through either modulation of frequency and/or dosage of AZ. Hormone levels were recorded before (baseline) and after AZ commencement.
DISCUSSION
Men receiving exogenous TTH may experience side effects, including elevations in E2 levels, which may impact libido and cause gynecomastia. AZ is a safe and effective option for men with elevated E2. Our study evaluated men with TD in which a small subset had elevated E2 requiring intervention (AZ). Overall, we demonstrated a statistically significant reduction in E2 levels to normal physiologic levels with the maintenance of T levels but were unable to identify predictors for men most likely to respond to therapy.
Only 2.6% of men had E2 which warranted treatment with AZ. AZ has been used in men with TD in an effort to reduce the conversion to E2 to T while maintaining fertility.6 We employed a cut-off for the use of AZ, but the literature does not support a clear cut-off or indication for the initiation of estradiol-lowering therapy.7 Similar to our series, in a national sample, 3.5% (1,200/34,016) of men were placed on an AI.7
Almost all men had recovery of E2 within normal levels (<40 pg/mL) with simultaneous maintenance of a serum T. This highlights the importance of appropriate regulation given the important physiological processes regulated by E2.
No statistically significant predictors were found in our series to predict E2 recovery in men on AZ. To the best of our knowledge, this has not been previously reported. Furthermore, limited data exists with respect to a clear cut-off or consideration of response to AZ, and therefore our composite cut-off was suggested based on a clinically meaningful response.
*The clinical implications of AZ in men with elevated E2 while on TTH are evident. Given the importance of E2 in male physiology and the impact of TTH on E2, careful monitoring by practitioners providing exogenous therapy is critical.
Limitations to our study include the retrospective design, but all data were collected prospectively. The study does have limited external validity as data were obtained from a single institution and a single provider. We also did not discern nor account for possible physiologic differences in men on AZ on clomiphene citrate versus those on exogenous TTH. We were not able to validate if AZ or clomiphene citrate did not interfere with E2 immunoassay testing. Furthermore, all men did not have measurements completed by LCMS but were included in order to obtain a reasonable sample size. A sensitivity analysis only using LCMS measurements revealed similar results (Supplementary Table 3). Finally, while the number of men on AZ in our series is small which limited statistical analysis for predictors of estradiol recovery, the total number of men assessed with TD was significant and over a large period of time.
CONCLUSION
In patients with elevated E2 on TTH, using AZ 0.5mg TID, results in a statistically significant reduction in E2, with 76% completely normalized with simultaneous maintenance of T levels. No statistically significant predictors were found for the recovery of E2 levels. Further research and larger studies are warranted.
