Proline-specific aminopeptidase P prevents
replication-associated genome instability

SILVA, Nicola, Maikel CASTELLANO-POZO, Kenichiro J. MATSUZAKI, Consuelo BARROSO, Monica P. ROMAN-TRUFERO, Hannah CRAIG, Darren P. BROOKS, R. Elwyn ISAAC, Simon P. BOULTON and Enrique MARTINEZ-PEREZ. Proline-specific aminopeptidase P prevents replication-associated genome instability. PLoS Genetics. San Francisco: Public Library of Science, 2022, vol. 18, No 1, p. 1-25. ISSN 1553-7404. Available from: https://dx.doi.org/10.1371/journal.pgen.1010025.

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TY  - JOUR
ID  - 2249120
AU  - Silva, Nicola - Castellano-Pozo, Maikel - Matsuzaki, Kenichiro J. - Barroso, Consuelo - Roman-Trufero, Monica P. - Craig, Hannah - Brooks, Darren P. - Isaac, R. Elwyn - Boulton, Simon P. - Martinez-Perez, Enrique
PY  - 2022
TI  - Proline-specific aminopeptidase P prevents replication-associated genome instability
JF  - PLoS Genetics
VL  - 18
IS  - 1
SP  - 1-25
EP  - 1-25
PB  - Public Library of Science
SN  - 15537404
KW  - Proline-specific aminopeptidase P
KW  - replication-associated genome instability
UR  - https://journals.plos.org/plosgenetics/article?id=10.1371/journal.pgen.1010025
N2  - Genotoxic stress during DNA replication constitutes a serious threat to genome integrity and causes human diseases. Defects at different steps of DNA metabolism are known to induce replication stress, but the contribution of other aspects of cellular metabolism is less understood. We show that aminopeptidase P (APP1), a metalloprotease involved in the catabolism of peptides containing proline residues near their N-terminus, prevents replication-associated genome instability. Functional analysis of C. elegans mutants lacking APP-1 demonstrates that germ cells display replication defects including reduced proliferation, cell cycle arrest, and accumulation of mitotic DSBs. Despite these defects, app-1 mutants are competent in repairing DSBs induced by gamma irradiation, as well as SPO-11-dependent DSBs that initiate meiotic recombination. Moreover, in the absence of SPO-11, spontaneous DSBs arising in app-1 mutants are repaired as inter-homologue crossover events during meiosis, confirming that APP-1 is not required for homologous recombination. Thus, APP-1 prevents replication stress without having an apparent role in DSB repair. Depletion of APP1 (XPNPEP1) also causes DSB accumulation in mitotically-proliferating human cells, suggesting that APP1's role in genome stability is evolutionarily conserved. Our findings uncover an unexpected role for APP1 in genome stability, suggesting functional connections between aminopeptidase-mediated protein catabolism and DNA replication. Author summaryThe accurate duplication of DNA that occurs before cells divide is an essential aspect of the cell cycle that is also crucial for the correct development of multicellular organisms. Mutations that compromise the normal function of the DNA replication machinery can lead to the accumulation of replication-related DNA damage, a known cause of human disease and a common feature of cancer and precancerous cells. Therefore, identifying factors that prevent replication-related DNA damage is highly relevant for human health. In this manuscript, we identify aminopeptidase P, an enzyme involved in the breakdown of proteins containing the amino acid Proline at their N-terminus, as a novel factor that prevents replication-related DNA damage. Analysis of C. elegans nematodes lacking aminopeptidase P reveals that this protein is required for normal fertility and development, and that in its absence proliferating germ cells display DNA replication defects, including cell cycle arrest and accumulation of extensive DNA damage. We also show that removal of aminopeptidase P induces DNA damage in proliferating human cells, suggesting that its role in preventing replication defects is evolutionarily conserved. These findings uncover functional connections between aminopeptidase-mediated protein degradation and DNA replication.
ER  -

Basic information
Original name	Proline-specific aminopeptidase P prevents replication-associated genome instability
Authors	SILVA, Nicola (380 Italy, belonging to the institution), Maikel CASTELLANO-POZO, Kenichiro J. MATSUZAKI, Consuelo BARROSO, Monica P. ROMAN-TRUFERO, Hannah CRAIG, Darren P. BROOKS, R. Elwyn ISAAC, Simon P. BOULTON and Enrique MARTINEZ-PEREZ (guarantor).
Edition	PLoS Genetics, San Francisco, Public Library of Science, 2022, 1553-7404.

Other information
Original language	English
Type of outcome	Article in a journal
Field of Study	10603 Genetics and heredity
Country of publisher	United States of America
Confidentiality degree	is not subject to a state or trade secret
WWW	URL
Impact factor	Impact factor: 4.500
RIV identification code	RIV/00216224:14110/22:00128227
Organization unit	Faculty of Medicine
Doi	http://dx.doi.org/10.1371/journal.pgen.1010025
UT WoS	000748003200001
Keywords in English	Proline-specific aminopeptidase P; replication-associated genome instability
Tags	14110513, rivok
Tags	International impact, Reviewed
Changed by	Changed by: Mgr. Tereza Miškechová, učo 341652. Changed: 20/2/2023 09:15.

Abstract

Genotoxic stress during DNA replication constitutes a serious threat to genome integrity and causes human diseases. Defects at different steps of DNA metabolism are known to induce replication stress, but the contribution of other aspects of cellular metabolism is less understood. We show that aminopeptidase P (APP1), a metalloprotease involved in the catabolism of peptides containing proline residues near their N-terminus, prevents replication-associated genome instability. Functional analysis of C. elegans mutants lacking APP-1 demonstrates that germ cells display replication defects including reduced proliferation, cell cycle arrest, and accumulation of mitotic DSBs. Despite these defects, app-1 mutants are competent in repairing DSBs induced by gamma irradiation, as well as SPO-11-dependent DSBs that initiate meiotic recombination. Moreover, in the absence of SPO-11, spontaneous DSBs arising in app-1 mutants are repaired as inter-homologue crossover events during meiosis, confirming that APP-1 is not required for homologous recombination. Thus, APP-1 prevents replication stress without having an apparent role in DSB repair. Depletion of APP1 (XPNPEP1) also causes DSB accumulation in mitotically-proliferating human cells, suggesting that APP1's role in genome stability is evolutionarily conserved. Our findings uncover an unexpected role for APP1 in genome stability, suggesting functional connections between aminopeptidase-mediated protein catabolism and DNA replication. Author summaryThe accurate duplication of DNA that occurs before cells divide is an essential aspect of the cell cycle that is also crucial for the correct development of multicellular organisms. Mutations that compromise the normal function of the DNA replication machinery can lead to the accumulation of replication-related DNA damage, a known cause of human disease and a common feature of cancer and precancerous cells. Therefore, identifying factors that prevent replication-related DNA damage is highly relevant for human health. In this manuscript, we identify aminopeptidase P, an enzyme involved in the breakdown of proteins containing the amino acid Proline at their N-terminus, as a novel factor that prevents replication-related DNA damage. Analysis of C. elegans nematodes lacking aminopeptidase P reveals that this protein is required for normal fertility and development, and that in its absence proliferating germ cells display DNA replication defects, including cell cycle arrest and accumulation of extensive DNA damage. We also show that removal of aminopeptidase P induces DNA damage in proliferating human cells, suggesting that its role in preventing replication defects is evolutionarily conserved. These findings uncover functional connections between aminopeptidase-mediated protein degradation and DNA replication.

Links
GA20-08819S, research and development project	Name: Pochopení úlohy PARG při podpoře tvorby a oprav dvouřetězcových zlomů DNA v meióze
GA20-08819S, research and development project	Investor: Czech Science Foundation
MUNI/A/1418/2021, interní kód MU	Name: Biomedicínské vědy II (Acronym: BIOMED)
MUNI/A/1418/2021, interní kód MU	Investor: Masaryk University

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Proline-specific aminopeptidase P prevents replication-associated genome instability

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