Cardiovascular Safety and Benefits of Testosterone Implant Therapy in Postmenopausal Women: Where Are We?
Abstract
:1. Introduction
1.1. The Controversy of T Therapy in Women
1.2. The Challenge of Low T Diagnosis in Women
1.3. Monitoring T Therapy in Women
1.4. The Evolution of STT in Clinical Practice
1.5. T Impact on Cardiovascular Health
1.6. The Benefits and Effectiveness of T Implant Therapy
Author(s), Year, Reference Number | Implant Dose | Characteristic of Study/Participants | Results |
---|---|---|---|
Glaser et al. (2011) [1] | Subcutaneous T implanted ranged between 75 mg and 160 mg. | Prospective study (300 pre and postmenopausal women with symptoms of relative androgen deficiency) | Improvement in total MRS score, as well as psychological, somatic, and urogenital subscale scores. |
Burger et al. (1984) [6] | Combined subcutaneous implants with E2 (40 mg) and T (100 mg) | Prospective study (17 postmenopausal women) | Substantial symptomatic relief, particularly in libido, while causing rises in mid-follicular concentrations of E2 and maximal T levels about three times normal, without significant effects on plasma lipids. |
Gambrell et al. (2006) [7] | Combined subcutaneous implants with E2 (25 to 100 mg) and T (75 to 225 mg) | Prospective study (606 postmenopausal women) | Menopause-symptom-relieving, side-effect-free regimen, treatment continuation rates of 72.1% for 5 years and 53.5% for 10 years. |
Garnett et al. (1991) [8] | Combined subcutaneous implants with E2 (50 to 75 mg) and T (100 mg) | Cross-sectional study (110 postmenopausal women) | Subcutaneous E2 and T prevent postmenopausal osteoporosis and maintain normal bone density for as long as treatment is continued. |
Thom et al. (1981) [9] | Combined subcutaneous implants with E2 (50 to 100 mg) and T (100–200 mg) | Prospective study (24 postmenopausal hysterectomized patients) | Plasma T concentrations rose from a mean concentration of 28.89 ng/dL to 144.45 ng/dL and 193 ng/dL after implants of 100 mg and 200 mg of T, respectively. |
Dimitrakakis et al. (2004) [10] | Combined subcutaneous implants containing T (50 mg to 150 mg) with conventional E2 or E2 plus progestin treatment. | Prospective study (508 postmenopausal women) | The addition of T to conventional hormone therapy for postmenopausal women does not increase and may indeed reduce the hormone-therapy-associated breast cancer risk. |
Donovitz et al. (2021) [29] | T implants (127.2 ± 17.7 mg) or T (127.6 ± 28.7 mg) plus E2 (15.6 ± 6.5 mg) | Retrospective study (2377 postmenopausal women) | Subcutaneous T alone or associated with E2 implants significantly reduced the incidence of breast cancer in pre and postmenopausal women |
Glaser et al. (2019) [70] | T implant dosing was weight-based with an average dose of 2–2.5 mg/kg (minimum dose 120 mg) | Prospective study (1267 pre and postmenopausal women) | 10-year therapy with subcutaneous T, or T combined with anastrozole, did not increase the incidence of breast cancer |
Glaser et al. (2012) [76] | T implants 130 ± 19.7 mg (range 100–160 mg) | Prospective study (27 pre and postmenopausal women previously diagnosed with migraine headache) | Continuous T implants was effective therapy in reducing the severity of migraine headaches in both pre and postmenopausal women |
Glaser et al. (2016) [81] | T implant dosing was weight-based with an average dose of 2–2.5 mg/kg (mean T dose was 138 ± 22.7 mg) | Prospective study (10 postmenopausal women) | Subcutaneous T had no adverse effect on the female voice including lowering or deepening of the voice. |
1.7. T Implant Therapy and Breast Cancer Risk
1.8. New Directions and Future Approaches in STT
2. Conclusions
Author Contributions
Funding
Institutional Review Board Statement
Informed Consent Statement
Data Availability Statement
Conflicts of Interest
References
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Recommend * | Consider with Caution * | Avoid |
---|---|---|
Total testosterone level | Total testosterone level | Total testosterone level |
<45.5 ng/dL (20–29 years) <27.6 ng/dL (20–39 years) <27.0 ng/dL (40–49 years) | >45.5 ng/dL (20–29 years) | >57.5 ng/dL (20–29 years) |
>27.6 ng/dL (20–39 years) | >39.8 ng/dL (20–39 years) | |
>27.0 ng/dL (40–49 years) | >38.6 ng/dL (40–49 years) | |
--------------and---------------- | ---------------or----------------- | ---------------or----------------- |
Carotid artery intima-media thickness < 75th percentiles and the absence of carotid plaque | Carotid artery intima-media thickness > 75th percentiles and the absence of carotid plaque | Carotid artery intima-media thickness > 75th percentiles or the presence of carotid plaque |
-------------and---------------- | ---------------or----------------- | ---------------or----------------- |
Calculated SCORE < 1% for 10-year risk of fatal CVD | Calculated SCORE ≥ 1% and <5% for 10-year risk of fatal CVD | Calculated SCORE ≥ 5% and <10% for 10-year risk of fatal CVD |
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Renke, G.; Tostes, F. Cardiovascular Safety and Benefits of Testosterone Implant Therapy in Postmenopausal Women: Where Are We? Pharmaceuticals 2023, 16, 619. https://doi.org/10.3390/ph16040619
Renke G, Tostes F. Cardiovascular Safety and Benefits of Testosterone Implant Therapy in Postmenopausal Women: Where Are We? Pharmaceuticals. 2023; 16(4):619. https://doi.org/10.3390/ph16040619
Chicago/Turabian StyleRenke, Guilherme, and Francisco Tostes. 2023. "Cardiovascular Safety and Benefits of Testosterone Implant Therapy in Postmenopausal Women: Where Are We?" Pharmaceuticals 16, no. 4: 619. https://doi.org/10.3390/ph16040619
APA StyleRenke, G., & Tostes, F. (2023). Cardiovascular Safety and Benefits of Testosterone Implant Therapy in Postmenopausal Women: Where Are We? Pharmaceuticals, 16(4), 619. https://doi.org/10.3390/ph16040619