Pdap1 protects mature B lymphocytes from stress-induced cell death and promotes antibody gene diversification

Author:

Delgado-Benito Verónica,Berruezo-Llacuna Maria,Altwasser Robert,Winkler Wiebke,Balasubramanian Sandhya,Sundaravinayagam Devakumar,Graf Robin,Rahjouei Ali,Driesner Madlen,Keller Lisa,Janz MartinORCID,Akalin AltunaORCID,Virgilio Michela DiORCID

Abstract

AbstractThe establishment of protective humoral immunity is dependent on the ability of mature B cells to undergo antibody gene diversification while adjusting to the physiological stressors induced by activation with the antigen. Mature B cells diversify their antibody genes by class switch recombination (CSR) and somatic hypermutation (SHM), which are both dependent on efficient induction of activation-induced cytidine deaminase (AID). Here, we identified PDGFA-associated protein 1 (Pdap1) as an essential regulator of cellular homeostasis in mature B cells. Pdap1 deficiency leads to sustained expression of the integrated stress response (ISR) effector activating transcription factor 4 (Atf4) and induction of the ISR transcriptional program, increased cell death, and defective AID expression. As a consequence, loss of Pdap1 reduces germinal center B cell formation and impairs CSR and SHM. Thus, Pdap1 protects mature B cells against chronic ISR activation and ensures efficient antibody diversification by promoting their survival and optimal function.

Publisher

Cold Spring Harbor Laboratory

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