The Identification of Zebrafish Mutants Showing Alterations in Senescence-Associated Biomarkers

There is an interesting overlap of function in a wide range of organisms between genes that modulate the stress responses and those that regulate aging phenotypes and, in some cases, lifespan. We have therefore screened mutagenized zebrafish embryos for the altered expression of a stress biomarker,...

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Autores principales: Kishi, Shuji, Bayliss, Peter E., Uchiyama, Junzo, Koshimizu, Eriko, Qi, Jie, Nanjappa, Purushothama, Imamura, Shintaro, Islam, Asiful, Neuberg, Donna, Amsterdam, Adam, Roberts, Thomas M.
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2008
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2515337/
https://www.ncbi.nlm.nih.gov/pubmed/18704191
http://dx.doi.org/10.1371/journal.pgen.1000152
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author Kishi, Shuji
Bayliss, Peter E.
Uchiyama, Junzo
Koshimizu, Eriko
Qi, Jie
Nanjappa, Purushothama
Imamura, Shintaro
Islam, Asiful
Neuberg, Donna
Amsterdam, Adam
Roberts, Thomas M.
author_facet Kishi, Shuji
Bayliss, Peter E.
Uchiyama, Junzo
Koshimizu, Eriko
Qi, Jie
Nanjappa, Purushothama
Imamura, Shintaro
Islam, Asiful
Neuberg, Donna
Amsterdam, Adam
Roberts, Thomas M.
author_sort Kishi, Shuji
collection PubMed
description There is an interesting overlap of function in a wide range of organisms between genes that modulate the stress responses and those that regulate aging phenotypes and, in some cases, lifespan. We have therefore screened mutagenized zebrafish embryos for the altered expression of a stress biomarker, senescence-associated β-galactosidase (SA-β-gal) in our current study. We validated the use of embryonic SA-β-gal production as a screening tool by analyzing a collection of retrovirus-insertional mutants. From a pool of 306 such mutants, we identified 11 candidates that showed higher embryonic SA-β-gal activity, two of which were selected for further study. One of these mutants is null for a homologue of Drosophila spinster, a gene known to regulate lifespan in flies, whereas the other harbors a mutation in a homologue of the human telomeric repeat binding factor 2 (terf2) gene, which plays roles in telomere protection and telomere-length regulation. Although the homozygous spinster and terf2 mutants are embryonic lethal, heterozygous adult fish are viable and show an accelerated appearance of aging symptoms including lipofuscin accumulation, which is another biomarker, and shorter lifespan. We next used the same SA-β-gal assay to screen chemically mutagenized zebrafish, each of which was heterozygous for lesions in multiple genes, under the sensitizing conditions of oxidative stress. We obtained eight additional mutants from this screen that, when bred to homozygosity, showed enhanced SA-β-gal activity even in the absence of stress, and further displayed embryonic neural and muscular degenerative phenotypes. Adult fish that are heterozygous for these mutations also showed the premature expression of aging biomarkers and the accelerated onset of aging phenotypes. Our current strategy of mutant screening for a senescence-associated biomarker in zebrafish embryos may thus prove to be a useful new tool for the genetic dissection of vertebrate stress response and senescence mechanisms.
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spelling pubmed-25153372008-08-15 The Identification of Zebrafish Mutants Showing Alterations in Senescence-Associated Biomarkers Kishi, Shuji Bayliss, Peter E. Uchiyama, Junzo Koshimizu, Eriko Qi, Jie Nanjappa, Purushothama Imamura, Shintaro Islam, Asiful Neuberg, Donna Amsterdam, Adam Roberts, Thomas M. PLoS Genet Research Article There is an interesting overlap of function in a wide range of organisms between genes that modulate the stress responses and those that regulate aging phenotypes and, in some cases, lifespan. We have therefore screened mutagenized zebrafish embryos for the altered expression of a stress biomarker, senescence-associated β-galactosidase (SA-β-gal) in our current study. We validated the use of embryonic SA-β-gal production as a screening tool by analyzing a collection of retrovirus-insertional mutants. From a pool of 306 such mutants, we identified 11 candidates that showed higher embryonic SA-β-gal activity, two of which were selected for further study. One of these mutants is null for a homologue of Drosophila spinster, a gene known to regulate lifespan in flies, whereas the other harbors a mutation in a homologue of the human telomeric repeat binding factor 2 (terf2) gene, which plays roles in telomere protection and telomere-length regulation. Although the homozygous spinster and terf2 mutants are embryonic lethal, heterozygous adult fish are viable and show an accelerated appearance of aging symptoms including lipofuscin accumulation, which is another biomarker, and shorter lifespan. We next used the same SA-β-gal assay to screen chemically mutagenized zebrafish, each of which was heterozygous for lesions in multiple genes, under the sensitizing conditions of oxidative stress. We obtained eight additional mutants from this screen that, when bred to homozygosity, showed enhanced SA-β-gal activity even in the absence of stress, and further displayed embryonic neural and muscular degenerative phenotypes. Adult fish that are heterozygous for these mutations also showed the premature expression of aging biomarkers and the accelerated onset of aging phenotypes. Our current strategy of mutant screening for a senescence-associated biomarker in zebrafish embryos may thus prove to be a useful new tool for the genetic dissection of vertebrate stress response and senescence mechanisms. Public Library of Science 2008-08-15 /pmc/articles/PMC2515337/ /pubmed/18704191 http://dx.doi.org/10.1371/journal.pgen.1000152 Text en Kishi et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Kishi, Shuji
Bayliss, Peter E.
Uchiyama, Junzo
Koshimizu, Eriko
Qi, Jie
Nanjappa, Purushothama
Imamura, Shintaro
Islam, Asiful
Neuberg, Donna
Amsterdam, Adam
Roberts, Thomas M.
The Identification of Zebrafish Mutants Showing Alterations in Senescence-Associated Biomarkers
title The Identification of Zebrafish Mutants Showing Alterations in Senescence-Associated Biomarkers
title_full The Identification of Zebrafish Mutants Showing Alterations in Senescence-Associated Biomarkers
title_fullStr The Identification of Zebrafish Mutants Showing Alterations in Senescence-Associated Biomarkers
title_full_unstemmed The Identification of Zebrafish Mutants Showing Alterations in Senescence-Associated Biomarkers
title_short The Identification of Zebrafish Mutants Showing Alterations in Senescence-Associated Biomarkers
title_sort identification of zebrafish mutants showing alterations in senescence-associated biomarkers
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2515337/
https://www.ncbi.nlm.nih.gov/pubmed/18704191
http://dx.doi.org/10.1371/journal.pgen.1000152
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