What role for AID: mutator, or assembler of the immunoglobulin mutasome?

1 July 2003

journal article
review article
Published by Springer Nature in Nature Immunology

Vol. 4 (7) , 631-638
https://doi.org/10.1038/ni0703-631

Abstract

Activation-induced cytidine deaminase (AID) has been shown to trigger three mechanisms for diversifying immunoglobulin genes--somatic hypermutation, isotype switch recombination and gene conversion--most probably by initiating cytidine deamination at the immunoglobulin locus. Although this deamination process has been shown to be potentially mutagenic by itself, most of the mutations generated in the physiological hypermutation process seem to be created through the AID-mediated assembly of a mutasome complex involving specific repair activities and error-prone DNA polymerases.

Keywords

This publication has 107 references indexed in Scilit:

The influence of transcriptional orientation on endogenous switch region function
Nature Immunology, 2003
R-loops at immunoglobulin class switch regions in the chromosomes of stimulated B cells
Nature Immunology, 2003
Uracil in DNA – occurrence, consequences and repair
Oncogene, 2002
RNA Editing Enzyme APOBEC1 and Some of Its Homologs Can Act as DNA Mutators
Molecular Cell, 2002
DNA Double-Strand Breaks
The Journal of Experimental Medicine, 2002
AID Is Essential for Immunoglobulin V Gene Conversion in a Cultured B Cell Line
Current Biology, 2002
Mismatch repair and immunoglobulin gene hypermutation: did we learn something?
Immunology Today, 1999
Hypermutation of Immunoglobulin Genes in Memory B Cells of DNA Repair–deficient Mice
The Journal of Experimental Medicine, 1998
Rearrangement/hypermutation/gene conversion: when, where and why?
Immunology Today, 1996
Somatic Hypermutation of Immunoglobulin Genes Is Linked to Transcription Initiation
Immunity, 1996