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Literature DB >> 33379193

Non-Homologous End Joining Factors XLF, PAXX and DNA-PKcs Maintain the Neural Stem and Progenitor Cell Population.

Raquel Gago-Fuentes^1,2, Valentyn Oksenych^1,3,4.

Abstract

Non-homologous end-joining (NHEJ) is a major DNA repair pathway in mammalian cells that recognizes, processes and fixes DNA damage throughout the cell cycle and is specifically important for homeostasis of post-mitotic neurons and developing lymphocytes. Neuronal apoptosis increases in the mice lacking NHEJ factors Ku70 and Ku80. Inactivation of other NHEJ genes, either Xrcc4 or Lig4, leads to massive neuronal apoptosis in the central nervous system (CNS) that correlates with embryonic lethality in mice. Inactivation of either Paxx, Mri or Dna-pkcs NHEJ gene results in normal CNS development due to compensatory effects of Xlf. Combined inactivation of Xlf/Paxx, Xlf/Mri and Xlf/Dna-pkcs, however, results in late embryonic lethality and high levels of apoptosis in CNS. To determine the impact of NHEJ factors on the early stages of neurodevelopment, we isolated neural stem and progenitor cells from mouse embryos and investigated proliferation, self-renewal and differentiation capacity of these cells lacking either Xlf, Paxx, Dna-pkcs, Xlf/Paxx or Xlf/Dna-pkcs. We found that XRCC4-like factor (XLF), DNA-dependent protein kinase catalytic subunit (DNA-PKcs) and paralogue of XRCC4 and XLF (PAXX) maintain the neural stem and progenitor cell populations and neurodevelopment in mammals, which is particularly evident in the double knockout models.

Entities: CellLine Chemical Disease Gene Mutation Species

Keywords: DNA repair; NHEJ; genetic interaction; synthetic lethality

Mesh：

Substances：

Year: 2020 PMID： 33379193 PMCID： PMC7823790 DOI： 10.3390/biom11010020

Source DB: PubMed Journal: Biomolecules ISSN： 2218-273X

50 in total

1. Transcription-associated processes cause DNA double-strand breaks and translocations in neural stem/progenitor cells.

Authors: Bjoern Schwer; Pei-Chi Wei; Amelia N Chang; Jennifer Kao; Zhou Du; Robin M Meyers; Frederick W Alt
Journal: Proc Natl Acad Sci U S A Date: 2016-02-12 Impact factor: 11.205

2. Cernunnos, a novel nonhomologous end-joining factor, is mutated in human immunodeficiency with microcephaly.

Authors: Dietke Buck; Laurent Malivert; Régina de Chasseval; Anne Barraud; Marie-Claude Fondanèche; Ozden Sanal; Alessandro Plebani; Jean-Louis Stéphan; Markus Hufnagel; Françoise le Deist; Alain Fischer; Anne Durandy; Jean-Pierre de Villartay; Patrick Revy
Journal: Cell Date: 2006-01-27 Impact factor: 41.582

3. Differential phosphorylation of DNA-PKcs regulates the interplay between end-processing and end-ligation during nonhomologous end-joining.

Authors: Wenxia Jiang; Jennifer L Crowe; Xiangyu Liu; Satoshi Nakajima; Yunyue Wang; Chen Li; Brian J Lee; Richard L Dubois; Chao Liu; Xiaochun Yu; Li Lan; Shan Zha
Journal: Mol Cell Date: 2015-03-26 Impact factor: 17.970

4. Requirement for Ku80 in growth and immunoglobulin V(D)J recombination.

Authors: A Nussenzweig; C Chen; V da Costa Soares; M Sanchez; K Sokol; M C Nussenzweig; G C Li
Journal: Nature Date: 1996-08-08 Impact factor: 49.962

5. Growth retardation and leaky SCID phenotype of Ku70-deficient mice.

Authors: Y Gu; K J Seidl; G A Rathbun; C Zhu; J P Manis; N van der Stoep; L Davidson; H L Cheng; J M Sekiguchi; K Frank; P Stanhope-Baker; M S Schlissel; D B Roth; F W Alt
Journal: Immunity Date: 1997-11 Impact factor: 31.745

6. Genome integrity and neurogenesis of postnatal hippocampal neural stem/progenitor cells require a unique regulator Filia.

Authors: Jingzheng Li; Yafang Shang; Lin Wang; Bo Zhao; Chunli Sun; Jiali Li; Siling Liu; Cong Li; Min Tang; Fei-Long Meng; Ping Zheng
Journal: Sci Adv Date: 2020-10-28 Impact factor: 14.136

7. Functional redundancy between the XLF and DNA-PKcs DNA repair factors in V(D)J recombination and nonhomologous DNA end joining.

Authors: Valentyn Oksenych; Vipul Kumar; Xiangyu Liu; Chunguang Guo; Bjoern Schwer; Shan Zha; Frederick W Alt
Journal: Proc Natl Acad Sci U S A Date: 2013-01-23 Impact factor: 11.205

Non-Homologous End Joining Factors XLF, PAXX and DNA-PKcs Maintain the Neural Stem and Progenitor Cell Population.

1. Transcription-associated processes cause DNA double-strand breaks and translocations in neural stem/progenitor cells.

2. Cernunnos, a novel nonhomologous end-joining factor, is mutated in human immunodeficiency with microcephaly.

3. Differential phosphorylation of DNA-PKcs regulates the interplay between end-processing and end-ligation during nonhomologous end-joining.

4. Requirement for Ku80 in growth and immunoglobulin V(D)J recombination.

5. Growth retardation and leaky SCID phenotype of Ku70-deficient mice.

6. Genome integrity and neurogenesis of postnatal hippocampal neural stem/progenitor cells require a unique regulator Filia.

7. Functional redundancy between the XLF and DNA-PKcs DNA repair factors in V(D)J recombination and nonhomologous DNA end joining.

8. Genetic interaction between DNA repair factors PAXX, XLF, XRCC4 and DNA-PKcs in human cells.

9. Leaky severe combined immunodeficiency in mice lacking non-homologous end joining factors XLF and MRI.

10. Lymphocyte-specific compensation for XLF/cernunnos end-joining functions in V(D)J recombination.

1. Acetyltransferases GCN5 and PCAF Are Required for B Lymphocyte Maturation in Mice.