Cockayne syndrome group B cellular and biochemical functions

Cecilie Löe Licht; Tinna V. Stevnsner; Vilhelm A Bohr

doi:10.1086/380399

Cockayne syndrome group B cellular and biochemical functions

Cecilie Löe Licht, Tinna V. Stevnsner, Vilhelm A Bohr

Publikation: Bidrag til tidsskrift › Tidsskriftartikel › Forskning › peer review

130 Citationer (Scopus)

Abstract

The devastating genetic disorder Cockayne syndrome (CS) arises from mutations in the CSA and CSB genes. CS is characterized by progressive multisystem degeneration and is classified as a segmental premature-aging syndrome. The CS complementation group B (CSB) protein is at the interface of transcription and DNA repair and is involved in transcription-coupled and global genome-DNA repair, as well as in general transcription. Recent structure-function studies indicate a process-dependent variation in the molecular mechanism employed by CSB and provide a starting ground for a description of the mechanisms and their interplay.

Originalsprog	Engelsk
Tidsskrift	American Journal of Human Genetics
Vol/bind	73
Udgave nummer	6
Sider (fra-til)	1217-39
Antal sider	23
ISSN	0002-9297
DOI	https://doi.org/10.1086/380399
Status	Udgivet - 1 dec. 2003
Udgivet eksternt	Ja

Adgang til dokumentet

10.1086/380399

Citationsformater

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abstract = "The devastating genetic disorder Cockayne syndrome (CS) arises from mutations in the CSA and CSB genes. CS is characterized by progressive multisystem degeneration and is classified as a segmental premature-aging syndrome. The CS complementation group B (CSB) protein is at the interface of transcription and DNA repair and is involved in transcription-coupled and global genome-DNA repair, as well as in general transcription. Recent structure-function studies indicate a process-dependent variation in the molecular mechanism employed by CSB and provide a starting ground for a description of the mechanisms and their interplay.",

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AU - Stevnsner, Tinna V.

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AB - The devastating genetic disorder Cockayne syndrome (CS) arises from mutations in the CSA and CSB genes. CS is characterized by progressive multisystem degeneration and is classified as a segmental premature-aging syndrome. The CS complementation group B (CSB) protein is at the interface of transcription and DNA repair and is involved in transcription-coupled and global genome-DNA repair, as well as in general transcription. Recent structure-function studies indicate a process-dependent variation in the molecular mechanism employed by CSB and provide a starting ground for a description of the mechanisms and their interplay.

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