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NCT05606679 Clinical Trial

Maternal KIR and Fetal HLA Influence Reproductive Success in ART-oocyte Donor.

Reproductive Issues Clinical Trial

Official title:
Maternal KIR and Fetal HLA Influence Reproductive Success in ART-oocyte Donor.

Clinical Trial Details — Status: Recruiting

Administrative data
NCT number NCT05606679
Other study ID # 2207-MAD-098-DA
Secondary ID
Status Recruiting
Phase
First received
Last updated
Start date November 1, 2022
Est. completion date December 31, 2025

Study information
Verified date January 2024
Source IVI Madrid
Contact Diana Alecsandru, PhD
Phone +34 91 180 29 00
Email Diana.Alecsandru@ivirma.com
Is FDA regulated No
Health authority
Study type Observational

Clinical Trial Summary

The present project is an ambispective study designed to answer how HLA-F SNPs, as well as KIR-HLA-C compatibility, influence reproductive outcomes in oocyte donation cycles. On the one hand, healthy patients without history of RIF and RM and with indication of egg donation cycle as ART treatment will be genotype for KIR, HLA-C and HLA-F. HLA-C from male partners and egg donors will be also analyzed. No matching based on HLA-C genotypes would be performed and donors would be assigned to recipients following the routine clinical practices. After SET, patients will be followed up until delivery or until the end of treatment. On the other hand, access to data from patients who have equally undergone oocyte-donation cycles, who meet the inclusion criteria and who have been genotyped for KIR and HLA-C as a matter of routine practice, will be requested. For this study, only the first SET of oocyte-donation that patients undergo will be considered. LBR will be the primary endpoint of the study. In addition, secondary endpoints such as embryo development, sustained implantation, progesterone levels, implantation failure, miscarriage rate and unwanted events (preeclampsia, fetal grow restriction, premature birth, low birth weight…) will also be evaluated.

Description:

This is an ambispective study in which healthy patients without history of RIF and RM and with indication of egg donation cycle as ART treatment will be genotyped for KIR, HLA-C and HLA-F. Male partners and egg donors will also be studied for their HLA-C alleles. Patients would be assigned to donors, following routine clinical practice, without matching based on donor's HLA-C genotype. They would undergo SET and be followed up until delivery. In addition to this prospective part, we will request access to data from patients who have equally undergone oocyte donation cycles at the clinic, who meet the inclusion criteria and who have been genotyped for KIR and HLA-C as a matter of routine practice. Combinations of maternal KIR and HLA-C genotypes of the egg donor and fetus (based on the genotypes of the donor and male partner), as well as different HLA-F SNP genotypes of the recipients (form the prospective part of this proyect) will be correlated with reproductive outcomes. LBR will be the primary endpoint of the study. In addition, secondary endpoints such as embryo development, sustained implantation, progesterone leves, implantation failure and miscarriage rate will also be evaluated. Obstetrical complications such as preeclampsia, premature birth (<34 weeks) and low birth weight will also be evaluated.

Recruitment information / eligibility
Status Recruiting
Enrollment 400
Est. completion date December 31, 2025
Est. primary completion date December 1, 2024
Accepts healthy volunteers
Gender All
Age group 18 Years to 45 Years
Eligibility Inclusion Criteria: - Patients who have undergone or are undergoing their first egg donation cycle. - Between 18 and 45 years of age. - BMI between 19 and 25 kg/m2 - Signed written informed consent submitted. - No history of RIF, defined as implantation failure after 4 consecutive blastocysts are transferred. - No history of RM, defined as the presence of 2 or more clinical miscarriages. - Normal blood pressure and viral serology. Exclusion Criteria: - Male partner diagnosed with severe male factor - Patients who test positive for thrombophilic disorders (factor V Leiden, prothrombinG20210A mutation, positive antiphospholipid antibodies) - Participation in a different study or clinical trial with a research drug or device in the last three months prior to recruitment. - Known abnormal karyotype of subject or of her partner - Any known clinically significant systemic disease - Known inherited or acquired thrombophilia disease. - Any known endocrine or metabolic abnormalities with the exception of controlled thyroid function disease. - Severe psychiatric conditions. - Patients with uterine factor/abnormalities (eg. myomas, polyps, adenomyosis, etc), that determines an unsatisfactory ultrasound for their ART. - Patients with PCOS. - Patients diagnosed with autoimmune diseases (eg. Systemic Lupus erythematosus, multiple sclerosis, rheumatoid arthritis). - Patients with recent diagnosis (6 months) of chronic infectious disease (HPV, HBV, HCV, HIV, TBC). - Patients with current treatment of immunosuppressant (eg. corticosteroids, monoclonal antibodies…).

Study Design

Related Conditions & MeSH terms

Intervention

Genetic:
Analysis combinations of maternal KIR and HLA-C genotypes
Analysis of combinations of maternal KIR and HLA-C genotypes of the egg donor and fetus (based on the genotypes of the donor and male partner), as well as different HLA-F SNP genotypes of the recipients

Locations
Country Name City State
Spain Instituto Valenciano de Infertilidad Madrid

Sponsors (2)
Lead Sponsor Collaborator
IVI Madrid Diana Alecsandru

Country where clinical trial is conducted

Spain, 

Outcome
Type Measure Description Time frame Safety issue
Primary To determine if certain combinations of maternal KIR and oocyte donor HLA-C genotypes results in improved outcomes of live birth rate. Principally, to establish whether patients of KIR AA and KIR Bx (2DS1-) genotypes show better outcomes when receiving oocytes from HLA-C1C1 donors than from donors with at least one HLA-C2 allele. 36 months
Secondary To determine if certain combinations of maternal KIR and oocyte donor HLA-C genotypes results in improved outcomes of live birth rate taking into account the extra HLA-C2 alleles of the embryo. To determine if certain combinations of maternal KIR and oocyte donor HLA-C genotypes results in improved outcomes of live birth rathe, in the same way as in the primary target, but taking into account the extra HLA-C2 alleles of the embryo with respect to the mother and the alternative division of the maternal genotypes into KIR AA, AB and BB. 36 months
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