The roles and acting mechanism of Caenorhabditis elegans DNase II genes in apoptotic dna degradation and development.

DNase II enzymes are acidic endonucleases that have been implicated in mediating apoptotic DNA degradation, a critical cell death execution event. C. elegans genome contains three DNase II homologues, NUC-1, CRN-6, and CRN-7, but their expression patterns, acting sites, and roles in apoptotic DNA de...

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Main Authors: Huey-Jen Lai, Szecheng J Lo, Eriko Kage-Nakadai, Shohei Mitani, Ding Xue
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2009-10-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC2752799?pdf=render
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spelling doaj-480c19aa0b0b4c45a8f57a4b4c2b9bce2020-11-25T01:48:05ZengPublic Library of Science (PLoS)PLoS ONE1932-62032009-10-01410e734810.1371/journal.pone.0007348The roles and acting mechanism of Caenorhabditis elegans DNase II genes in apoptotic dna degradation and development.Huey-Jen LaiSzecheng J LoEriko Kage-NakadaiShohei MitaniDing XueDNase II enzymes are acidic endonucleases that have been implicated in mediating apoptotic DNA degradation, a critical cell death execution event. C. elegans genome contains three DNase II homologues, NUC-1, CRN-6, and CRN-7, but their expression patterns, acting sites, and roles in apoptotic DNA degradation and development are unclear. We have conducted a comprehensive analysis of three C. elegans DNase II genes and found that nuc-1 plays a major role, crn-6 plays an auxiliary role, and crn-7 plays a negligible role in resolving 3' OH DNA breaks generated in apoptotic cells. Promoter swapping experiments suggest that crn-6 but not crn-7 can partially substitute for nuc-1 in mediating apoptotic DNA degradation and both fail to replace nuc-1 in degrading bacterial DNA in intestine. Despite of their restricted and largely non-overlapping expression patterns, both CRN-6 and NUC-1 can mediate apoptotic DNA degradation in many cells, suggesting that they are likely secreted nucleases that are retaken up by other cells to exert DNA degradation functions. Removal or disruption of NUC-1 secretion signal eliminates NUC-1's ability to mediate DNA degradation across its expression border. Furthermore, blocking cell corpse engulfment does not affect apoptotic DNA degradation mediated by nuc-1, suggesting that NUC-1 acts in apoptotic cells rather than in phagocytes to resolve 3' OH DNA breaks. Our study illustrates how multiple DNase II nucleases play differential roles in apoptotic DNA degradation and development and reveals an unexpected mode of DNase II action in mediating DNA degradation.http://europepmc.org/articles/PMC2752799?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Huey-Jen Lai
Szecheng J Lo
Eriko Kage-Nakadai
Shohei Mitani
Ding Xue
spellingShingle Huey-Jen Lai
Szecheng J Lo
Eriko Kage-Nakadai
Shohei Mitani
Ding Xue
The roles and acting mechanism of Caenorhabditis elegans DNase II genes in apoptotic dna degradation and development.
PLoS ONE
author_facet Huey-Jen Lai
Szecheng J Lo
Eriko Kage-Nakadai
Shohei Mitani
Ding Xue
author_sort Huey-Jen Lai
title The roles and acting mechanism of Caenorhabditis elegans DNase II genes in apoptotic dna degradation and development.
title_short The roles and acting mechanism of Caenorhabditis elegans DNase II genes in apoptotic dna degradation and development.
title_full The roles and acting mechanism of Caenorhabditis elegans DNase II genes in apoptotic dna degradation and development.
title_fullStr The roles and acting mechanism of Caenorhabditis elegans DNase II genes in apoptotic dna degradation and development.
title_full_unstemmed The roles and acting mechanism of Caenorhabditis elegans DNase II genes in apoptotic dna degradation and development.
title_sort roles and acting mechanism of caenorhabditis elegans dnase ii genes in apoptotic dna degradation and development.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2009-10-01
description DNase II enzymes are acidic endonucleases that have been implicated in mediating apoptotic DNA degradation, a critical cell death execution event. C. elegans genome contains three DNase II homologues, NUC-1, CRN-6, and CRN-7, but their expression patterns, acting sites, and roles in apoptotic DNA degradation and development are unclear. We have conducted a comprehensive analysis of three C. elegans DNase II genes and found that nuc-1 plays a major role, crn-6 plays an auxiliary role, and crn-7 plays a negligible role in resolving 3' OH DNA breaks generated in apoptotic cells. Promoter swapping experiments suggest that crn-6 but not crn-7 can partially substitute for nuc-1 in mediating apoptotic DNA degradation and both fail to replace nuc-1 in degrading bacterial DNA in intestine. Despite of their restricted and largely non-overlapping expression patterns, both CRN-6 and NUC-1 can mediate apoptotic DNA degradation in many cells, suggesting that they are likely secreted nucleases that are retaken up by other cells to exert DNA degradation functions. Removal or disruption of NUC-1 secretion signal eliminates NUC-1's ability to mediate DNA degradation across its expression border. Furthermore, blocking cell corpse engulfment does not affect apoptotic DNA degradation mediated by nuc-1, suggesting that NUC-1 acts in apoptotic cells rather than in phagocytes to resolve 3' OH DNA breaks. Our study illustrates how multiple DNase II nucleases play differential roles in apoptotic DNA degradation and development and reveals an unexpected mode of DNase II action in mediating DNA degradation.
url http://europepmc.org/articles/PMC2752799?pdf=render
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