Infertility Clinical Trial
Official title:
Lutropin Alfa (Luveris®) in Mid Follicular Phase for Controlled Ovarian Stimulation (COS) in Advanced Reproductive Age: Phase II Clinical Trial
Ovarian reserve is related to chronological age; 35 years of age is the accepted threshold
for significant decline in assisted reproductive technologies (ART) success with scarce
follicular recruitment and poor oocyte retrieval. New therapeutic schemes are sought to
improve follicular response in ovarian ageing because of the increasing number of infertile
women aged older than 35 years who are trying to get pregnant. The advent of gonadotropin
releasing hormone analogue antagonist (GnRHant) offers new perspectives to address the
issues related to advanced reproductive age since it prevents premature luteinizing hormone
(LH) surges while not causing suppression in the early follicular phase. Gonadotropin
releasing hormone analogue antagonists are administered in the latter stage of the ovarian
stimulation to prevent LH surge by competitive blockade of gonadotropin releasing hormone
(GnRH) receptors, thus producing a marked decrease in LH levels just when the interplay
between follicle stimulating hormone (FSH) and LH becomes important to complete follicular
development and oocyte competence. Some studies in the past have shown the potential of
recombinant human LH (r-hLH) supplementation in women of advanced reproductive age to
improve oocyte quality, but these studies are of small size and did not provide data on the
physiological mechanism behind the benefit obtained.
This randomized, comparative, parallel controlled Phase II study will be conducted in
infertile female subjects aged 35-42 years undergoing in-vitro fertilization (IVF)/intra
cytoplasmic sperm injection (ICSI), to investigate whether the addition of r-hLH (when the
lead follicle is greater than [>] 14 millimeter [mm] in size), to the standard protocol with
recombinant human FSH (r-hFSH) under GnRHant, improves the number and quality of oocytes
retrieved, implantation rate, and pregnancy rate, while assessing the hormonal milieu in the
ovarian follicular fluid. Comparison will be performed against ovarian stimulation without
addition of r-hLH, that is (i.e.) with r-hFSH under GnRHant alone.
Preclinical pharmacology studies have demonstrated that r-hLH has a LH/human chorionic
gonadotropin (hCG) receptor affinity similar to pituitary human luteinizing hormone (p-hLH),
and is biologically active in-vitro in stimulating steroidogenesis and in promoting oocyte
germinal vesicle breakdown. Several clinical studies have investigated the usefulness of
r-hLH supplementation in normal ovulatory women undergoing ART and in almost all of them
sub-populations of subjects have been identified who will benefit, when r-hLH is added to
FSH.
OBJECTIVES
Primary objectives:
- To determine the efficacy of adding r-hLH at mid-follicular phase compared to not
adding r-hLH, in women of 35-42 years of age included in a COS with r-hFSH under
treatment with a GnRHant for IVF/ICSI, assessed by the number and quality of the oocyte
- To determine the safety of using r-hLH combined with r-hFSH in a protocol with a
GnRHant, including incidence of ovarian hyperstimulation syndrome (OHSS) and adverse
events (AEs) as well as local tolerability
Secondary objectives:
- To complete the verification of efficacy with additional assessments such as follicular
growth, oocyte fertilization, embryo quality and pregnancy rates
- To investigate the underlying mechanism of possible improvement in oocyte quality by
means of determining hormone levels (LH, FSH, T, E2, and hCG) levels in follicular
fluid
Tertiary objectives:
- This is a phase-II study that did not aim to carry out assessment of pharmacoeconomics
or quality of life
All subjects will undergo treatment with r-hFSH at a daily dose of 300-450 IU by
subcutaneous route starting on the stimulation Day 1 (S1) until r-hCG administration. Upon
detection of a lead follicle > 14 mm in diameter, GnRHant 0.25 milligram (mg)/day
subcutaneous administration will be initiated and continued up to r-hCG administration day.
Subjects will be then randomly allocated (at any time between S1 and GnRHant initiation day)
either to additional treatment with r-hLH at a daily fixed dose of 150 IU or continue
treatment with r-hFSH alone. Gonadotropin releasing hormone antagonist and combined
treatment with r-hLH plus (+) r-hFSH or r-hFSH alone will be administered until at least one
follicle > 18 mm in diameter and two additional follicles > 16 mm in diameter are present
and E2 levels are commensurate with the number and size of follicles present. A single
injection of 250-500 microgram of r-hCG, will be given to induce final follicular maturation
within 36 hours of the last r-hLH and/or r-hFSH injections and on the same day of the last
GnRHant morning administration. Oocytes will be retrieved 34-38 hours after r-hCG
administration, assessed, and fertilized in-vitro by ICSI. Not more than 3 embryos will be
replaced on day 2 or 3 after OPU. The luteal phase will be supported by a daily vaginal
administration of natural progesterone, starting after OPU and continuing either up to
menstruation or the pregnancy test or, if the subject is pregnant, for at least 30 days
after laboratory evidence of pregnancy. Each subject will be followed-up and the treatment
outcome (pregnancy or menstruation) will be recorded.
For all subjects who received r-hCG and do not menstruate, a blood sample will be collected
for local determination of serum beta-hCG level between post-hCG days 15-20. If positive
(beta-hCG > 10 International Unit/liter [IU/L]), it should be confirmed by performing a
second test within one week later. An ultrasound scan (US) will be performed at post-hCG
days 35-42 on all subjects who will become pregnant provided that no miscarriage has
occurred. The number of fetal sacs and fetal heart activity will be recorded. Active
follow-up of all pregnancies will be performed, including those subjects withdrawn from the
study.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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