by McGill University
Graphical abstract. Credit: Journal of Clinical Investigation (2024). DOI: 10.1172/JCI170669
A molar pregnancy, also known as a hydatidiform mole, is an abnormal human pregnancy with no embryo and an overgrowth of the cells that form the placenta. The common form of molar pregnancy affects one in every 600 pregnancies in Quebec.
Half of these moles are androgenetic, i.e., they contain only the father's chromosomes with no chromosomes from the mother, and their frequency increases 10 times with advanced maternal age. Because of the hyperproliferation of their cells, androgenetic moles may become malignant and lead to a placental cancer in up to 15% of cases.
Scientists at the Research Institute of the McGill University Health Centre (RI-MUHC) recently discovered six new genes—FOXL2, MAJIN, KASH5, SYCP2, HFM1 and MEIOB—that cause recurrent androgenetic moles, recurrent miscarriages and infertility when mutated on both alleles (copies of the same gene) in the patients.
Five of these genes are essential for Meiosis I, the process of cell division necessary for the production of sperm and eggs in humans. Previous studies have linked defects in some of the six genes to premature ovarian failure, a well-known cause of female infertility. In addition, five of these genes have been linked to male infertility.
These findings, just published in the Journal of Clinical Investigation, will improve the molecular diagnosis of recurrent molar pregnancies, premature ovarian failure and infertile women and men.
"Our findings suggest that recurrent androgenetic moles are a sign of ovarian aging. They will change current clinical practice by introducing the evaluation of ovarian reserve for patients with recurrent moles," says Rima Slim, Ph.D., corresponding and co-senior author of the study, Senior Scientist in the Child Health and Human Development Program at the RI-MUHC and Professor in the Department of Human Genetics at McGill University.
The six new genes add to four other genes that are also responsible for recurrent molar pregnancies and that were previously discovered by the same team (NLRP7, discovered in 2006, and MEI1, TOP6BL and REC114, discovered in 2018).
A broad international investigation
In collaboration with Jacek Majewski's team, Investigator at the RI-MUHC and Professor of Human Genetics at McGill, the researchers performed exome sequencing on 75 unrelated patients referred by physicians from around the world. These patients had at least two hydatidiform moles and did not have mutations in the previously described genes associated with the condition.
The researchers then checked whether the patients who were negative for biallelic mutations (on both alleles of a gene), had only one defective allele in genes with roles in Meiosis I and ovarian functions. They added 240 patients with other forms of reproductive failure—referred primarily from the MUHC Repeated Pregnancy Loss clinic, founded by Dr. William Buckett, and the Réseau des Maladies Trophoblastiques du Québec, founded by Dr. Philippe Sauthier. This second group of patients had either a molar pregnancy and at least one miscarriage, or at least two miscarriages without a molar pregnancy.
They found that 14% to 28% of these patients had one defective allele that appeared to be most frequent in patients with at least two molar pregnancies.
"Our data suggest that these monoallelic variants could be contributing, with other factors, to the genetic susceptibility of these patients for reproductive failure. Our study provides an explanation of the increased frequency of androgenetic moles with advanced maternal age," explains Prof. Slim.
The authors of the study explain that "patients with monoallelic variants in these genes can conceive and have healthy children; however, they are at higher risk for infertility, premature ovarian insufficiency and reproductive loss than women from the general population."
Modeling the genesis of moles
In order to better elucidate the mechanisms underlying this health and reproductive problem, the researchers modeled the disease in mice with deficiency in the HFM1 gene.
"We observed several defects that affect the meiotic progression, some of which were previously observed by our team in mice with deficiency in the Mei1 gene, another gene responsible for the causation of recurrent androgenetic moles," explains Teruko Taketo, Ph.D., co-senior author of the study, Senior Scientist in the Child Health and Human Development Program at the RI-MUHC and Professor in the Department of Surgery at McGill University.
"In this study, using live-cell imaging, we were able to visualize and understand for the first time how the eggs from Hfm1 deficient mice lose all their chromosomes."
The authors emphasize that the identification of the same mechanism in two mouse models supports its plausibility at the origin of androgenetic mole formation in humans.
"Androgenetic moles have been described in 1977. Today, we can better explain to the patients the formation of these aberrant conceptions and the genesis of androgenetic moles," says Prof. Slim.
More information: Maryam Rezaei et al, Defects in meiosis I contribute to the genesis of androgenetic hydatidiform moles, Journal of Clinical Investigation (2024). DOI: 10.1172/JCI170669
Journal information: Journal of Clinical Investigation
Provided by McGill University
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