A potential new mechanism for pregnancy loss: considering the role of LINE-1 retrotransposons in early spontaneous miscarriage

Abstract LINE1 retrotransposons are mobile DNA elements that copy and paste themselves into new sites in the genome. To ensure their evolutionary success, heritable new LINE-1 insertions accumulate in cells that can transmit genetic information to the next generation (i.e., germ cells and embryonic...

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Main Authors: Chao Lou, John L. Goodier, Rong Qiang
Format: Article
Language:English
Published: BMC 2020-01-01
Series:Reproductive Biology and Endocrinology
Subjects:
Online Access:https://doi.org/10.1186/s12958-020-0564-x
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spelling doaj-88792cb0a5234dcb9d2f0ec8d90af89a2021-01-24T12:10:03ZengBMCReproductive Biology and Endocrinology1477-78272020-01-0118111010.1186/s12958-020-0564-xA potential new mechanism for pregnancy loss: considering the role of LINE-1 retrotransposons in early spontaneous miscarriageChao Lou0John L. Goodier1Rong Qiang2Department of Genetics, Northwest Women’s and Children’s HospitalMcKusick-Nathans Deartment of Genetic Medicine, Johns Hopkins University School of MedicineDepartment of Genetics, Northwest Women’s and Children’s HospitalAbstract LINE1 retrotransposons are mobile DNA elements that copy and paste themselves into new sites in the genome. To ensure their evolutionary success, heritable new LINE-1 insertions accumulate in cells that can transmit genetic information to the next generation (i.e., germ cells and embryonic stem cells). It is our hypothesis that LINE1 retrotransposons, insertional mutagens that affect expression of genes, may be causal agents of early miscarriage in humans. The cell has evolved various defenses restricting retrotransposition-caused mutation, but these are occasionally relaxed in certain somatic cell types, including those of the early embryo. We predict that reduced suppression of L1s in germ cells or early-stage embryos may lead to excessive genome mutation by retrotransposon insertion, or to the induction of an inflammatory response or apoptosis due to increased expression of L1-derived nucleic acids and proteins, and so disrupt gene function important for embryogenesis. If correct, a novel threat to normal human development is revealed, and reverse transcriptase therapy could be one future strategy for controlling this cause of embryonic damage in patients with recurrent miscarriages.https://doi.org/10.1186/s12958-020-0564-xSpontaneous miscarriageRetrotransposon, LINE-1De novo insertionHuman embryogenesisMutation
collection DOAJ
language English
format Article
sources DOAJ
author Chao Lou
John L. Goodier
Rong Qiang
spellingShingle Chao Lou
John L. Goodier
Rong Qiang
A potential new mechanism for pregnancy loss: considering the role of LINE-1 retrotransposons in early spontaneous miscarriage
Reproductive Biology and Endocrinology
Spontaneous miscarriage
Retrotransposon, LINE-1
De novo insertion
Human embryogenesis
Mutation
author_facet Chao Lou
John L. Goodier
Rong Qiang
author_sort Chao Lou
title A potential new mechanism for pregnancy loss: considering the role of LINE-1 retrotransposons in early spontaneous miscarriage
title_short A potential new mechanism for pregnancy loss: considering the role of LINE-1 retrotransposons in early spontaneous miscarriage
title_full A potential new mechanism for pregnancy loss: considering the role of LINE-1 retrotransposons in early spontaneous miscarriage
title_fullStr A potential new mechanism for pregnancy loss: considering the role of LINE-1 retrotransposons in early spontaneous miscarriage
title_full_unstemmed A potential new mechanism for pregnancy loss: considering the role of LINE-1 retrotransposons in early spontaneous miscarriage
title_sort potential new mechanism for pregnancy loss: considering the role of line-1 retrotransposons in early spontaneous miscarriage
publisher BMC
series Reproductive Biology and Endocrinology
issn 1477-7827
publishDate 2020-01-01
description Abstract LINE1 retrotransposons are mobile DNA elements that copy and paste themselves into new sites in the genome. To ensure their evolutionary success, heritable new LINE-1 insertions accumulate in cells that can transmit genetic information to the next generation (i.e., germ cells and embryonic stem cells). It is our hypothesis that LINE1 retrotransposons, insertional mutagens that affect expression of genes, may be causal agents of early miscarriage in humans. The cell has evolved various defenses restricting retrotransposition-caused mutation, but these are occasionally relaxed in certain somatic cell types, including those of the early embryo. We predict that reduced suppression of L1s in germ cells or early-stage embryos may lead to excessive genome mutation by retrotransposon insertion, or to the induction of an inflammatory response or apoptosis due to increased expression of L1-derived nucleic acids and proteins, and so disrupt gene function important for embryogenesis. If correct, a novel threat to normal human development is revealed, and reverse transcriptase therapy could be one future strategy for controlling this cause of embryonic damage in patients with recurrent miscarriages.
topic Spontaneous miscarriage
Retrotransposon, LINE-1
De novo insertion
Human embryogenesis
Mutation
url https://doi.org/10.1186/s12958-020-0564-x
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