Background: Testosterone replacement therapy (TRT) with transdermal gel is widely used in men with hypogonadism. Guidelines recommend once-daily application with monitoring of serum testosterone at peak levels. However, real-world clinical experience suggests that peak-trough fluctuations in some patients, potentially affecting hormonal stability and treatment tolerability. The impact of dose fractionation remains unclear. Objectives: To compare hormonal profiles and biochemical safety parameters between once-daily and twice-daily (fractionated) testosterone gel administration in hypogonadal men receivingh the same total daily dose. Methods: We retrospectively identified hypogonadal men treated with 2% testosterone gel who transitioned from once-daily to twice-daily dosing, maintaining the same total daily dose. Eligible patients had serum total testosterone (TT) measurements available at both peak (3 h post-application) and nadir (pre-dose). Hormonal and laboratory parameters under the two regimens were compared. Results: Twelve patients met inclusion criteria. Fractionated dosing was associated with lower peak TT levels [9.0 (5.3-13.0) vs. 5.7 (3.6-7.1) ng/mL, paired difference - 3.6 ng/mL (95% CI: -4.9 to - 1.8)] and higher nadir TT levels [1.4 (1.1-1.8) vs. 3.2 (2.6-5.4) ng/mL, paired difference 2.6 ng/mL (95% CI: 1.2 to 5.1)], resulting in a reduced difference between peak-to-pre-dose difference within the observed sampling window. The proportion of patients achieving target TT levels at peak increased (33% vs. 83%). Calculated free testosterone showed a similar pattern. No clinically relevant differences were observed in luteinizing hormone, prostate-specific antigen, haematocrit, or haemoglobin. Conclusion: In this real-world cohort, fractionated testosterone gel administration was associated with a higher proportion of patients achieving biochemical targets and with a reduced peak-to-pre-dose difference within the observed sampling window, without short-term biochemical safety signals. These findings should be considered hypothesis-generating.
Maltese, V., Delbarba, A., Gatta, E., Vetrugno, S., Sansone, A., Cappelli, C. (2026). Fractionated testosterone gel replacement therapy in clinical practice: A real-world exploratory clinical experience. ENDOCRINE, 91, 1-9 [10.1007/s12020-026-04659-8].
Fractionated testosterone gel replacement therapy in clinical practice: A real-world exploratory clinical experience
Sansone, Andrea;
2026-05-23
Abstract
Background: Testosterone replacement therapy (TRT) with transdermal gel is widely used in men with hypogonadism. Guidelines recommend once-daily application with monitoring of serum testosterone at peak levels. However, real-world clinical experience suggests that peak-trough fluctuations in some patients, potentially affecting hormonal stability and treatment tolerability. The impact of dose fractionation remains unclear. Objectives: To compare hormonal profiles and biochemical safety parameters between once-daily and twice-daily (fractionated) testosterone gel administration in hypogonadal men receivingh the same total daily dose. Methods: We retrospectively identified hypogonadal men treated with 2% testosterone gel who transitioned from once-daily to twice-daily dosing, maintaining the same total daily dose. Eligible patients had serum total testosterone (TT) measurements available at both peak (3 h post-application) and nadir (pre-dose). Hormonal and laboratory parameters under the two regimens were compared. Results: Twelve patients met inclusion criteria. Fractionated dosing was associated with lower peak TT levels [9.0 (5.3-13.0) vs. 5.7 (3.6-7.1) ng/mL, paired difference - 3.6 ng/mL (95% CI: -4.9 to - 1.8)] and higher nadir TT levels [1.4 (1.1-1.8) vs. 3.2 (2.6-5.4) ng/mL, paired difference 2.6 ng/mL (95% CI: 1.2 to 5.1)], resulting in a reduced difference between peak-to-pre-dose difference within the observed sampling window. The proportion of patients achieving target TT levels at peak increased (33% vs. 83%). Calculated free testosterone showed a similar pattern. No clinically relevant differences were observed in luteinizing hormone, prostate-specific antigen, haematocrit, or haemoglobin. Conclusion: In this real-world cohort, fractionated testosterone gel administration was associated with a higher proportion of patients achieving biochemical targets and with a reduced peak-to-pre-dose difference within the observed sampling window, without short-term biochemical safety signals. These findings should be considered hypothesis-generating.| File | Dimensione | Formato | |
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