DNA Damaged Induced Cell Death in Oocytes

DNA Damaged Induced Cell Death in Oocytes

The production of haploid gametes through meiosis is central to the principle of sexual reproduction. The genetic diversity is further enhanced by exchange of genetic material between homologous chromosomes by the crossover mechanism. This mechanism not only requires correct pairing of homologous ch...

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Main Authors: Jakob Gebel, Marcel Tuppi, Nicole Sänger, Björn Schumacher, Volker Dötsch
Format: Article
Language:English
Published: MDPI AG 2020-12-01
Series:Molecules
Subjects:
p63
p73
p53 family
CEP-1
tetramerization
transcriptional activity
Online Access:https://www.mdpi.com/1420-3049/25/23/5714
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spelling doaj-863620c8ac3d45a98343cce10296875b2020-12-04T00:04:04ZengMDPI AGMolecules1420-30492020-12-01255714571410.3390/molecules25235714DNA Damaged Induced Cell Death in OocytesJakob Gebel0Marcel Tuppi1Nicole Sänger2Björn Schumacher3Volker Dötsch4Institute of Biophysical Chemistry and Center for Biomolecular Magnetic Resonance, Goethe University, 60438 Frankfurt, GermanyInstitute of Biophysical Chemistry and Center for Biomolecular Magnetic Resonance, Goethe University, 60438 Frankfurt, GermanyDepartment for Gynecological Endocrinology and Reproductive Medicine, University Hospital of Bonn, Venusberg-Campus 1, 53217 Bonn, GermanyInstitute for Genome Stability in Aging and Disease, Cologne Cluster of Excellence in Cellular Stress Responses in Aging-Associated Diseases (CECAD) Research Center, and Center for Molecular Medicine, University of Cologne, Joseph-Stelzmann-Str. 26, 50931 Cologne, GermanyInstitute of Biophysical Chemistry and Center for Biomolecular Magnetic Resonance, Goethe University, 60438 Frankfurt, GermanyThe production of haploid gametes through meiosis is central to the principle of sexual reproduction. The genetic diversity is further enhanced by exchange of genetic material between homologous chromosomes by the crossover mechanism. This mechanism not only requires correct pairing of homologous chromosomes but also efficient repair of the induced DNA double-strand breaks. Oocytes have evolved a unique quality control system that eliminates cells if chromosomes do not correctly align or if DNA repair is not possible. Central to this monitoring system that is conserved from nematodes and fruit fly to humans is the p53 protein family, and in vertebrates in particular p63. In mammals, oocytes are stored for a long time in the prophase of meiosis I which, in humans, can last more than 50 years. During the entire time of this arrest phase, the DNA damage checkpoint remains active. The treatment of female cancer patients with DNA damaging irradiation or chemotherapeutics activates this checkpoint and results in elimination of the oocyte pool causing premature menopause and infertility. Here, we review the molecular mechanisms of this quality control system and discuss potential therapeutic intervention for the preservation of the oocyte pool during chemotherapy.https://www.mdpi.com/1420-3049/25/23/5714p63p73p53 familyCEP-1tetramerizationtranscriptional activity
collection DOAJ
language English
format Article
sources DOAJ
author Jakob Gebel
Marcel Tuppi
Nicole Sänger
Björn Schumacher
Volker Dötsch
spellingShingle Jakob Gebel
Marcel Tuppi
Nicole Sänger
Björn Schumacher
Volker Dötsch
DNA Damaged Induced Cell Death in Oocytes
Molecules
p63
p73
p53 family
CEP-1
tetramerization
transcriptional activity
author_facet Jakob Gebel
Marcel Tuppi
Nicole Sänger
Björn Schumacher
Volker Dötsch
author_sort Jakob Gebel
title DNA Damaged Induced Cell Death in Oocytes
title_short DNA Damaged Induced Cell Death in Oocytes
title_full DNA Damaged Induced Cell Death in Oocytes
title_fullStr DNA Damaged Induced Cell Death in Oocytes
title_full_unstemmed DNA Damaged Induced Cell Death in Oocytes
title_sort dna damaged induced cell death in oocytes
publisher MDPI AG
series Molecules
issn 1420-3049
publishDate 2020-12-01
description The production of haploid gametes through meiosis is central to the principle of sexual reproduction. The genetic diversity is further enhanced by exchange of genetic material between homologous chromosomes by the crossover mechanism. This mechanism not only requires correct pairing of homologous chromosomes but also efficient repair of the induced DNA double-strand breaks. Oocytes have evolved a unique quality control system that eliminates cells if chromosomes do not correctly align or if DNA repair is not possible. Central to this monitoring system that is conserved from nematodes and fruit fly to humans is the p53 protein family, and in vertebrates in particular p63. In mammals, oocytes are stored for a long time in the prophase of meiosis I which, in humans, can last more than 50 years. During the entire time of this arrest phase, the DNA damage checkpoint remains active. The treatment of female cancer patients with DNA damaging irradiation or chemotherapeutics activates this checkpoint and results in elimination of the oocyte pool causing premature menopause and infertility. Here, we review the molecular mechanisms of this quality control system and discuss potential therapeutic intervention for the preservation of the oocyte pool during chemotherapy.
topic p63
p73
p53 family
CEP-1
tetramerization
transcriptional activity
url https://www.mdpi.com/1420-3049/25/23/5714
work_keys_str_mv AT jakobgebel dnadamagedinducedcelldeathinoocytes
AT marceltuppi dnadamagedinducedcelldeathinoocytes
AT nicolesanger dnadamagedinducedcelldeathinoocytes
AT bjornschumacher dnadamagedinducedcelldeathinoocytes
AT volkerdotsch dnadamagedinducedcelldeathinoocytes
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