Distinct Requirements of CHD4 during B Cell Development and Antibody Response

Wei-Feng Yen,Rahul Sharma,Montserrat Cols,Colleen M Lau,Ashutosh Chaudhry,Priyanka Chowdhury,William T Yewdell,Bharat Vaidyanathan,Amy Sun,Maryaline Coffre,Joseph N Pucella,Chun-Chin Chen,Maria Jasin,Joseph C Sun,Alexander Y Rudensky,Sergei B Koralov,Jayanta Chaudhuri

doi:10.1016/j.celrep.2019.04.011

Wei-Feng Yen, Rahul Sharma + Show 15 more

Open Access

https://doi.org/10.1016/j.celrep.2019.04.011

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Abstract

SUMMARYThe immunoglobulin heavy chain (Igh) locus features a dynamic chromatin landscape to promote class switch recombination (CSR), yet the mechanisms that regulate this landscape remain poorly understood. CHD4, a component of the chromatin remodeling NuRD complex, directly binds H3K9me3, an epigenetic mark present at the Igh locus during CSR. We find that CHD4 is essential for early B cell development but is dispensable for the homeostatic maintenance of mature, naive B cells. However, loss of CHD4 in mature B cells impairs CSR because of suboptimal targeting of AID to the Igh locus. Additionally, we find that CHD4 represses p53 expression to promote B cell proliferation. This work reveals distinct roles for CHD4 in B cell development and CSR and links the H3K9me3 epigenetic mark with AID recruitment to the Igh locus.

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