Hypogonadotropic Hypogonadism Clinical Trial
Official title:
Prospective Randomized Open Label Study to Compare the Efficacy and Safety of Ovarian Stimulation With Pergoveris® and Menopur® in Women With Severe Luteinizing Hormone (LH) and Follicular Stimulating Hormone (FSH) Deficiency.
The aim of the study is to compare the efficacy and safety of r-hFSH+r-hLH in a 2:1 ratio
with human Menopausal Gonadotropin Highly Purified (hMG-HP), in WHO type I anovulation, HH
women.
This open-label monocentric, randomized comparative trial, to receive the two different
standard clinical practice treatments:
- 1 vial of Pergoveris: (vial/powder 150 International unit (IU) r-hFSH+ 75IU r-hLH)
- 2 vials of Menopur: (vials/powder hMG 75IU).
Follicular development were monitored until the protocol hCG requirement is met and a single
injection of hCG was administered.
Main Outcome Measures were follicular development i.e. follicle ≥ 17 millimeters (mm),
pre-ovulatory E2 ≥ 400 picomole/Liter (pmol/L) and mid-luteal phase Progesterone (P4) ≥ 25
nanomole/Liter (nmol/L).
World Health Organization (WHO) type I hypogonadotropic anovulation (hypogonadotropic
hypogonadism, HH) is a rare alteration of the reproductive system with absent or decreased
function of the gonads, caused by congenital, including genetic, or acquired reduced
hypothalamic or pituitary activity. This results in abnormally low serum levels of
Follicular Stimulation Hormone (FSH) and Luteinizing Hormone (LH) and negligible oestrogen
(E2) activity.
The most convenient treatment is daily injections of exogenous gonadotropins that has been
proven to be effective.
Patients lacking an effective hypothalamic-pituitary activity (WHO type I anovulation) do
not produce sufficient threshold levels of endogenous LH, which is required to obtain
optimal follicular development and steroidogenesis when treated with FSH alone. Therefore a
combination therapy with adequate doses of both FSH and LH in an optimal ratio is required
in order to restore fertility.
The LH activity could be produced by LH itself or by human Chorionic Gonadotropin (hCG) and
the two gonadotropins are available to be used in the WHO type I patients in two different
formulations both in indication for this type of patients. It would be worth of interest to
assess if these two different formulations could elicit the same clinical outcomes in
standard clinical practice or not.
The aim of the study is to compare the efficacy and safety of recombinant human FSH and
recombinant human LH (r-hFSH+r-hLH) in a 2:1 ratio with human Menopausal Gonadotropin Highly
Purified (hMG-HP), containing LH-like activity, in women with severe LH and FSH deficiency
(WHO type I anovulation, HH).
All patients were diagnosed with HH according to a negative progesterone (P4) challenge
test, serum LH<1.2 IU/L and FSH <5 IU/L, a transvaginal ultrasound showing a uterus with a
midline echo, no ovarian tumor or cyst and ≤ 13 small follicles (mean diameter ≤
10millimeters (mm)) on the largest section through each ovary, a Body Mass Index (BMI)
between 18 and 32 Kilograms for square meters(Kg/m2), and no systemic diseases.
In this open-label monocentric, randomized comparative trial, patients was randomized in two
arms in 1:1 ratio, to receive the two different standard clinical practice treatments:
- 1 vial of Pergoveris: (vial/powder 150 International Units (IU) r-hFSH+ 75IU
r-hLH)stimulation day 1 until required hCG level is met. The dose can be adjusted at
stimulation Day 6 according to subject ovarian response and standard clinical practice
- 2 vials of Menopur: (vial/powder hMG containing 75IU FSH + 75IU LH-like activity).
stimulation day 1 until required hCG level is met. The dose can be adjusted at
stimulation Day 6 according to subject ovarian response and standard clinical practice
Follicular development were monitored according clinical practice by ultrasound (US)
and/or estradiol (E2) levels, until the protocol hCG requirement is met (i.e., at least
one follicle greater than or equal to 17 mm). After this, a single injection of hCG was
administered in order to induce final oocyte maturation.
Main Outcome Measures were ovulation induction as measured by follicular development i.e.
follicle ≥ 17 mm, pre-ovulatory E2 ≥ 400 picomole/Liter (pmol/L) and mid-luteal phase
Progesterone ≥ 25 nanomole/Liter (nmol/L). Secondary efficacy endpoints included estradiol
levels/follicle at mid-cycle, number of follicles at mid-cycle and pregnancy rate (PR).
Drug safety was assessed by monitoring adverse events and the incidence of local reactions
after drug injection at local site. Ovarian hyperstimulation syndrome (OHSS) was assessed
and recorded according to Golan classification According to this protocol, patients were
initially treated for one cycle. If consenting, patients who did not become pregnant during
the first cycle were treated for a further optional one or two series of cycles with the
same criteria of randomization, i.e. maintaining the same treatment as the previous cycle.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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