Literature DB >> 23963444

NLRP7 or KHDC3L genes and the etiology of molar pregnancies and recurrent miscarriage.

L Andreasen1, O B Christiansen, I Niemann, L Bolund, L Sunde.   

Abstract

Women with mutation in both alleles of the NLRP7 or C6orf221/KHDC3L genes are predisposed to diploid biparental moles, but it has also been suggested that mutation in these genes can predispose to diploid androgenetic or triploid moles and to other kinds of reproductive wastage. We have investigated the association between molar pregnancy and recurrent miscarriages regarding changes in the NLRP7 and C6orf221/KHDC3L genes. Our study group can be divided into three sub-cohorts: (i) women having had at least one molar pregnancy and at least two non-mole miscarriages, (ii) women having had recurrent androgenetic hydatidiform moles and (iii) women having had one diploid androgenetic hydatidiform mole and a relative having had a hydatidiform mole (familial hydatidiform moles). We observed a statistically non-significant tendency of non-synonymous variants in NLRP7 to be more frequent in women with familial hydatidiform mole and in women with female family members with hydatidiform mole or non-mole miscarriage compared with women with no family history of mole or miscarriage. However, we did not find any unequivocal pathogenic mutations (the term 'unequivocal pathogenic mutations' refers to mutations that indubitably have a pathogenic effect on the affected woman) in NLRP7 or C6orf221/KHDC3L in any of the women in the study group. This indicates that recurrent miscarriages plus hydatidiform mole, recurrent androgenetic hydatidiform moles and familial androgenetic hydatidiform moles in general do not have the same monogenetic etiology as familiar diploid biparental moles.

Entities:  

Keywords:  KHDC3L; NLRP7; familial androgenetic hydatidiform mole; hydatidiform mole; recurrent miscarriages

Mesh:

Substances:

Year:  2013        PMID: 23963444     DOI: 10.1093/molehr/gat056

Source DB:  PubMed          Journal:  Mol Hum Reprod        ISSN: 1360-9947            Impact factor:   4.025


  9 in total

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4.  Hepatic toxicity following actinomycin D chemotherapy in treatment of familial gestational trophoblastic neoplasia: A case report.

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5.  KHDC3L mutation causes recurrent pregnancy loss by inducing genomic instability of human early embryonic cells.

Authors:  Weidao Zhang; Zhongliang Chen; Dengfeng Zhang; Bo Zhao; Lu Liu; Zhengyuan Xie; Yonggang Yao; Ping Zheng
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6.  Refined diagnosis of hydatidiform moles with p57 immunohistochemistry and molecular genotyping: updated analysis of a prospective series of 2217 cases.

Authors:  Deyin Xing; Emily Adams; Jialing Huang; Brigitte M Ronnett
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7.  Loss of p57 Expression in Conceptions Other Than Complete Hydatidiform Mole: A Case Series With Emphasis on the Etiology, Genetics, and Clinical Significance.

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8.  Paternal Hemizygosity in 11p15 in Mole-like Conceptuses: Two Case Reports.

Authors:  Lone Sunde; Helle Lund; Neil J Sebire; Anni Grove; Rosemary A Fisher; Isa Niemann; Eigil Kjeldsen; Lotte Andreasen; Estrid Staehr Hansen; Anders Bojesen; Lars Bolund; Mette Nyegaard
Journal:  Medicine (Baltimore)       Date:  2015-11       Impact factor: 1.889

9.  Risk Factors for Hydatidiform Mole: Is Husband’s Job a Major Risk Factor?

Authors:  Hourieh Shamshiri Milani; Morteza Abdollahi; Sara Torbati; Taha Asbaghi; Eznollah Azargashb
Journal:  Asian Pac J Cancer Prev       Date:  2017-10-26
  9 in total

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