A single N-terminal amino acid determines the distinct roles of histones H3 and H3.3 in the Drosophila male germline stem cell lineage

Adult stem cells undergo asymmetric cell divisions to produce 2 daughter cells with distinct cell fates: one capable of self-renewal and the other committed for differentiation. Misregulation of this delicate balance can lead to cancer and tissue degeneration. During asymmetric division of Drosophil...

Descripción completa

Detalles Bibliográficos
Autores principales: Chandrasekhara, Chinmayi, Ranjan, Rajesh, Urban, Jennifer A., Davis, Brendon E. M., Ku, Wai Lim, Snedeker, Jonathan, Zhao, Keji, Chen, Xin
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2023
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10174566/
https://www.ncbi.nlm.nih.gov/pubmed/37126497
http://dx.doi.org/10.1371/journal.pbio.3002098
_version_ 1785040060649832448
author Chandrasekhara, Chinmayi
Ranjan, Rajesh
Urban, Jennifer A.
Davis, Brendon E. M.
Ku, Wai Lim
Snedeker, Jonathan
Zhao, Keji
Chen, Xin
author_facet Chandrasekhara, Chinmayi
Ranjan, Rajesh
Urban, Jennifer A.
Davis, Brendon E. M.
Ku, Wai Lim
Snedeker, Jonathan
Zhao, Keji
Chen, Xin
author_sort Chandrasekhara, Chinmayi
collection PubMed
description Adult stem cells undergo asymmetric cell divisions to produce 2 daughter cells with distinct cell fates: one capable of self-renewal and the other committed for differentiation. Misregulation of this delicate balance can lead to cancer and tissue degeneration. During asymmetric division of Drosophila male germline stem cells (GSCs), preexisting (old) and newly synthesized histone H3 are differentially segregated, whereas old and new histone variant H3.3 are more equally inherited. However, what underlies these distinct inheritance patterns remains unknown. Here, we report that the N-terminal tails of H3 and H3.3 are critical for their inheritance patterns, as well as GSC maintenance and proper differentiation. H3 and H3.3 differ at the 31st position in their N-termini with Alanine for H3 and Serine for H3.3. By swapping these 2 amino acids, we generated 2 mutant histones (i.e., H3A31S and H3.3S31A). Upon expressing them in the early-stage germline, we identified opposing phenotypes: overpopulation of early-stage germ cells in the H3A31S-expressing testes and significant germ cell loss in testes expressing the H3.3S31A. Asymmetric H3 inheritance is disrupted in the H3A31S-expressing GSCs, due to misincorporation of old histones between sister chromatids during DNA replication. Furthermore, H3.3S31A mutation accelerates old histone turnover in the GSCs. Finally, using a modified Chromatin Immunocleavage assay on early-stage germ cells, we found that H3A31S has enhanced occupancy at promoters and transcription starting sites compared with H3, while H3.3S31A is more enriched at transcriptionally silent intergenic regions compared to H3.3. Overall, these results suggest that the 31st amino acids for both H3 and H3.3 are critical for their proper genomic occupancy and function. Together, our findings indicate a critical role for the different amino acid composition of the N-terminal tails between H3 and H3.3 in an endogenous stem cell lineage and provide insights into the importance of proper histone inheritance in specifying cell fates and regulating cellular differentiation.
format Online
Article
Text
id pubmed-10174566
institution National Center for Biotechnology Information
language English
publishDate 2023
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-101745662023-05-12 A single N-terminal amino acid determines the distinct roles of histones H3 and H3.3 in the Drosophila male germline stem cell lineage Chandrasekhara, Chinmayi Ranjan, Rajesh Urban, Jennifer A. Davis, Brendon E. M. Ku, Wai Lim Snedeker, Jonathan Zhao, Keji Chen, Xin PLoS Biol Research Article Adult stem cells undergo asymmetric cell divisions to produce 2 daughter cells with distinct cell fates: one capable of self-renewal and the other committed for differentiation. Misregulation of this delicate balance can lead to cancer and tissue degeneration. During asymmetric division of Drosophila male germline stem cells (GSCs), preexisting (old) and newly synthesized histone H3 are differentially segregated, whereas old and new histone variant H3.3 are more equally inherited. However, what underlies these distinct inheritance patterns remains unknown. Here, we report that the N-terminal tails of H3 and H3.3 are critical for their inheritance patterns, as well as GSC maintenance and proper differentiation. H3 and H3.3 differ at the 31st position in their N-termini with Alanine for H3 and Serine for H3.3. By swapping these 2 amino acids, we generated 2 mutant histones (i.e., H3A31S and H3.3S31A). Upon expressing them in the early-stage germline, we identified opposing phenotypes: overpopulation of early-stage germ cells in the H3A31S-expressing testes and significant germ cell loss in testes expressing the H3.3S31A. Asymmetric H3 inheritance is disrupted in the H3A31S-expressing GSCs, due to misincorporation of old histones between sister chromatids during DNA replication. Furthermore, H3.3S31A mutation accelerates old histone turnover in the GSCs. Finally, using a modified Chromatin Immunocleavage assay on early-stage germ cells, we found that H3A31S has enhanced occupancy at promoters and transcription starting sites compared with H3, while H3.3S31A is more enriched at transcriptionally silent intergenic regions compared to H3.3. Overall, these results suggest that the 31st amino acids for both H3 and H3.3 are critical for their proper genomic occupancy and function. Together, our findings indicate a critical role for the different amino acid composition of the N-terminal tails between H3 and H3.3 in an endogenous stem cell lineage and provide insights into the importance of proper histone inheritance in specifying cell fates and regulating cellular differentiation. Public Library of Science 2023-05-01 /pmc/articles/PMC10174566/ /pubmed/37126497 http://dx.doi.org/10.1371/journal.pbio.3002098 Text en https://creativecommons.org/publicdomain/zero/1.0/This is an open access article, free of all copyright, and may be freely reproduced, distributed, transmitted, modified, built upon, or otherwise used by anyone for any lawful purpose. The work is made available under the Creative Commons CC0 (https://creativecommons.org/publicdomain/zero/1.0/) public domain dedication.
spellingShingle Research Article
Chandrasekhara, Chinmayi
Ranjan, Rajesh
Urban, Jennifer A.
Davis, Brendon E. M.
Ku, Wai Lim
Snedeker, Jonathan
Zhao, Keji
Chen, Xin
A single N-terminal amino acid determines the distinct roles of histones H3 and H3.3 in the Drosophila male germline stem cell lineage
title A single N-terminal amino acid determines the distinct roles of histones H3 and H3.3 in the Drosophila male germline stem cell lineage
title_full A single N-terminal amino acid determines the distinct roles of histones H3 and H3.3 in the Drosophila male germline stem cell lineage
title_fullStr A single N-terminal amino acid determines the distinct roles of histones H3 and H3.3 in the Drosophila male germline stem cell lineage
title_full_unstemmed A single N-terminal amino acid determines the distinct roles of histones H3 and H3.3 in the Drosophila male germline stem cell lineage
title_short A single N-terminal amino acid determines the distinct roles of histones H3 and H3.3 in the Drosophila male germline stem cell lineage
title_sort single n-terminal amino acid determines the distinct roles of histones h3 and h3.3 in the drosophila male germline stem cell lineage
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10174566/
https://www.ncbi.nlm.nih.gov/pubmed/37126497
http://dx.doi.org/10.1371/journal.pbio.3002098
work_keys_str_mv AT chandrasekharachinmayi asinglenterminalaminoaciddeterminesthedistinctrolesofhistonesh3andh33inthedrosophilamalegermlinestemcelllineage
AT ranjanrajesh asinglenterminalaminoaciddeterminesthedistinctrolesofhistonesh3andh33inthedrosophilamalegermlinestemcelllineage
AT urbanjennifera asinglenterminalaminoaciddeterminesthedistinctrolesofhistonesh3andh33inthedrosophilamalegermlinestemcelllineage
AT davisbrendonem asinglenterminalaminoaciddeterminesthedistinctrolesofhistonesh3andh33inthedrosophilamalegermlinestemcelllineage
AT kuwailim asinglenterminalaminoaciddeterminesthedistinctrolesofhistonesh3andh33inthedrosophilamalegermlinestemcelllineage
AT snedekerjonathan asinglenterminalaminoaciddeterminesthedistinctrolesofhistonesh3andh33inthedrosophilamalegermlinestemcelllineage
AT zhaokeji asinglenterminalaminoaciddeterminesthedistinctrolesofhistonesh3andh33inthedrosophilamalegermlinestemcelllineage
AT chenxin asinglenterminalaminoaciddeterminesthedistinctrolesofhistonesh3andh33inthedrosophilamalegermlinestemcelllineage
AT chandrasekharachinmayi singlenterminalaminoaciddeterminesthedistinctrolesofhistonesh3andh33inthedrosophilamalegermlinestemcelllineage
AT ranjanrajesh singlenterminalaminoaciddeterminesthedistinctrolesofhistonesh3andh33inthedrosophilamalegermlinestemcelllineage
AT urbanjennifera singlenterminalaminoaciddeterminesthedistinctrolesofhistonesh3andh33inthedrosophilamalegermlinestemcelllineage
AT davisbrendonem singlenterminalaminoaciddeterminesthedistinctrolesofhistonesh3andh33inthedrosophilamalegermlinestemcelllineage
AT kuwailim singlenterminalaminoaciddeterminesthedistinctrolesofhistonesh3andh33inthedrosophilamalegermlinestemcelllineage
AT snedekerjonathan singlenterminalaminoaciddeterminesthedistinctrolesofhistonesh3andh33inthedrosophilamalegermlinestemcelllineage
AT zhaokeji singlenterminalaminoaciddeterminesthedistinctrolesofhistonesh3andh33inthedrosophilamalegermlinestemcelllineage
AT chenxin singlenterminalaminoaciddeterminesthedistinctrolesofhistonesh3andh33inthedrosophilamalegermlinestemcelllineage

Ejemplares similares