Clinical Trial Details
— Status: Not yet recruiting
Administrative data
| NCT number |
NCT04321551 |
| Other study ID # |
200395 |
| Secondary ID |
|
| Status |
Not yet recruiting |
| Phase |
Phase 4
|
| First received |
|
| Last updated |
|
| Start date |
July 1, 2023 |
| Est. completion date |
December 31, 2028 |
Study information
| Verified date |
June 2022 |
| Source |
University of California, San Diego |
| Contact |
Tracy N Harrison, MD |
| Phone |
858-822-1481 |
| Email |
tnharrison[@]health.ucsd.edu |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
Aim 1 utilizes prospective clinical studies in TGN to test the hypothesis that prolonged
exogenous androgens alter menstrual cyclicity by inhibiting gonadotropin secretion, steroid
hormone release, and ovulation. We will utilize a clinical trial of TRT to evaluate T
suppression of ovarian follicle and hormone dynamics (Aim 1A) and LH pulsatility (Aim 1B).
Description:
We will conduct a prospective, controlled clinical trial of ovarian and menstrual cyclicity
in TGN initiating TRT (Fig. 8). Enrollment will include 20 TGN and 20 cisgender female (CF)
control subjects who report female gender identity congruent with female sex assignment at
birth. All subjects will be age >18 y, with female sex assignment at birth, regular menstrual
cycles, and body mass index 18-35 kg/m2. Subjects with history of prior T use, cancer,
chemotherapy, or radiation of the brain, abdomen, or pelvis, current use of hormonal
medications (including, but not limited to, metformin, insulin, progestins, or estrogenic
medications), current endocrinopathy (including, but not limited to, PCOS, androgen secreting
tumor, diabetes, or pituitary, thyroid, or adrenal disease), and renal, hepatic, cardiac, or
hematologic disease will be excluded. TGN subjects will undergo baseline endocrine and
menstrual cycle evaluation, followed by intramuscular (i.m.) administration of testosterone
cypionate (TC) 50 mg (standard dose) every 7 d for 32 wks (Fig. 8). After 24 wks, an
aromatase inhibitor, letrozole (LET, 2.5 mg/d oral), will be co-administered with TC for 8
wks to block estrogen synthesis and examine whether T's effects are independent of E2
signaling. TGN will collect first morning-voided urine daily at home for assessment of
hormone levels during one complete menstrual cycle before TRT begins and continuing during
TRT. Untreated CF controls will collect urine daily during one menstrual cycle. Urinary
concentrations of LH, FSH, estrone (E1) conjugates, and pregnanediol glucuronide (PdG) will
be measured via ELISA. Studies of steroidogenesis during the menopausal transition have
demonstrated accuracy of monitoring urinary hormone metabolite levels to reconstruct ovarian
cyclicity and ovulatory patterns170-173; we can use this methodology to track progression of
any declining HPG axis output over time. All subjects will complete a daily uterine bleeding
log using REDCap® and undergo weekly measurement of serum FSH, LH, E2, and P4 (ELISA), and T
(LC-MS/MS) for confirmation of hormone dynamics demonstrated by urine hormone metabolite
studies. TGN will also undergo weekly transvaginal ultrasound (US) using a 4- to 9-MHz probe
to obtain three-dimensional (3D) pelvic imaging following initiation of TRT for confirmation
of corpus luteum (CL) formation and regression analysis of hormone secretion patterns,
endometrial thickness, antral follicle count (AFC), and volume of the uterus and ovaries.
Changes in follicle dynamics will be studied with 3D US determination of the mean diameter of
each antral in 1-mm increments from 2 to 9 mm, as in our prior reports174,175.
The primary endpoint will be Evidence of Luteal Activity (ELA), as defined by a 3-fold
increase in urinary PdG level over baseline170,176. Basal urinary PdG levels, normalized to
urinary creatinine excretion, will be determined based upon the minimum daily PdG level
detected per cycle or 4-wk interval, as previously described170,176. Secondary endpoints will
include mean serum FSH and LH levels, peak urinary LH concentration, and cumulative LH surge
count. Follicular phase function will be defined per cycle (or per 4-wk interval in
amenorrheic subjects) by creatinine-adjusted urinary E1 AUC. Five-day moving averages of
creatinine-adjusted urinary FSH and LH levels will be calculated, with LH surge defined as a
3 standard deviation increase in the 5-d moving LH average, as previously described170,176.
The proportion of subjects demonstrating an LH surge will be compared during successive 4-wk
intervals.
We have already demonstrated successful recruitment and retention of TGN and CF participants
in longitudinal studies involving daily urine collection and serial pelvic US (e.g., our
study in Fig. 2 and others)174,175. TGN subjects will be serially evaluated for adverse
effects of TRT per The Endocrine Society recommendations63. Details regarding safety
monitoring are in the Human Subjects Section. We calculate that 15 subjects/group will have
>95% power to detect a 30% decrease in the proportion of subjects with ELA at baseline
compared to the final 4-week TC study interval (wks 21-24). Although we anticipate a larger,
more clinically meaningful decrease, we have utilized a conservative target to maximize the
study's power. Although we have had no dropouts in our current TGN pilot study, we factored a
20% dropout rate into our enrollment target of 20 subjects per group to ensure achieving
sufficient power.
