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S-S synapsis during class switch recombination is promoted by distantly located transcriptional elements and activation-induced deaminase.


ABSTRACT: Molecular mechanisms underlying synapsis of activation-induced deaminase (AID)-targeted S regions during class switch recombination (CSR) are poorly understood. By using chromosome conformation capture techniques, we found that in B cells, the Emicro and 3'Ealpha enhancers were in close spatial proximity, forming a unique chromosomal loop configuration. B cell activation led to recruitment of the germline transcript (GLT) promoters to the Emicro:3'Ealpha complex in a cytokine-dependent fashion. This structure facilitated S-S synapsis because Smicro was proximal to Emicro and a downstream S region was corecruited with the targeted GLT promoter to Emicro:3'Ealpha. We propose that GLT promoter association with the Emicro:3'Ealpha complex creates an architectural scaffolding that promotes S-S synapsis during CSR and that these interactions are stabilized by AID. Thus, the S-S synaptosome is formed as a result of the self-organizing transcription system that regulates GLT expression and may serve to guard against spurious chromosomal translocations.

SUBMITTER: Wuerffel R 

PROVIDER: S-EPMC4979535 | biostudies-literature | 2007 Nov

REPOSITORIES: biostudies-literature

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S-S synapsis during class switch recombination is promoted by distantly located transcriptional elements and activation-induced deaminase.

Wuerffel Robert R   Wang Lili L   Grigera Fernando F   Manis John J   Selsing Erik E   Perlot Thomas T   Alt Frederick W FW   Cogne Michel M   Pinaud Eric E   Kenter Amy L AL  

Immunity 20071101 5


Molecular mechanisms underlying synapsis of activation-induced deaminase (AID)-targeted S regions during class switch recombination (CSR) are poorly understood. By using chromosome conformation capture techniques, we found that in B cells, the Emicro and 3'Ealpha enhancers were in close spatial proximity, forming a unique chromosomal loop configuration. B cell activation led to recruitment of the germline transcript (GLT) promoters to the Emicro:3'Ealpha complex in a cytokine-dependent fashion.  ...[more]

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