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An Overview of Y-Family DNA Polymerases and a Case Study of Human DNA Polymerase η

[Image: see text] Y-Family DNA polymerases specialize in translesion synthesis, bypassing damaged bases that would otherwise block the normal progression of replication forks. Y-Family polymerases have unique structural features that allow them to bind damaged DNA and use a modified template base to...

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Detalles Bibliográficos
Autor principal: Yang, Wei
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Chemical Society 2014
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4018060/
https://www.ncbi.nlm.nih.gov/pubmed/24716551
http://dx.doi.org/10.1021/bi500019s
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author Yang, Wei
author_facet Yang, Wei
author_sort Yang, Wei
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description [Image: see text] Y-Family DNA polymerases specialize in translesion synthesis, bypassing damaged bases that would otherwise block the normal progression of replication forks. Y-Family polymerases have unique structural features that allow them to bind damaged DNA and use a modified template base to direct nucleotide incorporation. Each Y-Family polymerase is unique and has different preferences for lesions to bypass and for dNTPs to incorporate. Y-Family polymerases are also characterized by a low catalytic efficiency, a low processivity, and a low fidelity on normal DNA. Recruitment of these specialized polymerases to replication forks is therefore regulated. The catalytic center of the Y-Family polymerases is highly conserved and homologous to that of high-fidelity and high-processivity DNA replicases. In this review, structural differences between Y-Family and A- and B-Family polymerases are compared and correlated with their functional differences. A time-resolved X-ray crystallographic study of the DNA synthesis reaction catalyzed by the Y-Family DNA polymerase human polymerase η revealed transient elements that led to the nucleotidyl-transfer reaction.
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spelling pubmed-40180602015-04-10 An Overview of Y-Family DNA Polymerases and a Case Study of Human DNA Polymerase η Yang, Wei Biochemistry [Image: see text] Y-Family DNA polymerases specialize in translesion synthesis, bypassing damaged bases that would otherwise block the normal progression of replication forks. Y-Family polymerases have unique structural features that allow them to bind damaged DNA and use a modified template base to direct nucleotide incorporation. Each Y-Family polymerase is unique and has different preferences for lesions to bypass and for dNTPs to incorporate. Y-Family polymerases are also characterized by a low catalytic efficiency, a low processivity, and a low fidelity on normal DNA. Recruitment of these specialized polymerases to replication forks is therefore regulated. The catalytic center of the Y-Family polymerases is highly conserved and homologous to that of high-fidelity and high-processivity DNA replicases. In this review, structural differences between Y-Family and A- and B-Family polymerases are compared and correlated with their functional differences. A time-resolved X-ray crystallographic study of the DNA synthesis reaction catalyzed by the Y-Family DNA polymerase human polymerase η revealed transient elements that led to the nucleotidyl-transfer reaction. American Chemical Society 2014-04-10 2014-05-06 /pmc/articles/PMC4018060/ /pubmed/24716551 http://dx.doi.org/10.1021/bi500019s Text en Copyright © 2014 U.S. Government
spellingShingle Yang, Wei
An Overview of Y-Family DNA Polymerases and a Case Study of Human DNA Polymerase η
title An Overview of Y-Family DNA Polymerases and a Case Study of Human DNA Polymerase η
title_full An Overview of Y-Family DNA Polymerases and a Case Study of Human DNA Polymerase η
title_fullStr An Overview of Y-Family DNA Polymerases and a Case Study of Human DNA Polymerase η
title_full_unstemmed An Overview of Y-Family DNA Polymerases and a Case Study of Human DNA Polymerase η
title_short An Overview of Y-Family DNA Polymerases and a Case Study of Human DNA Polymerase η
title_sort overview of y-family dna polymerases and a case study of human dna polymerase η
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4018060/
https://www.ncbi.nlm.nih.gov/pubmed/24716551
http://dx.doi.org/10.1021/bi500019s
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