Smc3 Dosage Regulates B Cell Transit Through Germinal Centers and Restricts Their Malignant Transformation

Overview

Journal Nat Immunol

Date 2021 Jan 12

PMID 33432228

Citations 25

Authors

Martin A Rivas

Cem Meydan

Christopher R Chin

Matt F Challman

Daleum Kim

Bhavneet Bhinder

Andreas Kloetgen

Aaron D Viny

Matt R Teater

Dylan R McNally

Ashley S Doane

Wendy Beguelin

Maria Teresa Calvo Fernandez

Hao Shen

Xiang Wang

Ross L Levine

Zhengming Chen

Aristotelis Tsirigos

Olivier Elemento

Christopher E Mason

Ari M Melnick

Affiliations

Soon will be listed here.

Abstract

During the germinal center (GC) reaction, B cells undergo extensive redistribution of cohesin complex and three-dimensional reorganization of their genomes. Yet, the significance of cohesin and architectural programming in the humoral immune response is unknown. Herein we report that homozygous deletion of Smc3, encoding the cohesin ATPase subunit, abrogated GC formation, while, in marked contrast, Smc3 haploinsufficiency resulted in GC hyperplasia, skewing of GC polarity and impaired plasma cell (PC) differentiation. Genome-wide chromosomal conformation and transcriptional profiling revealed defects in GC B cell terminal differentiation programs controlled by the lymphoma epigenetic tumor suppressors Tet2 and Kmt2d and failure of Smc3-haploinsufficient GC B cells to switch from B cell- to PC-defining transcription factors. Smc3 haploinsufficiency preferentially impaired the connectivity of enhancer elements controlling various lymphoma tumor suppressor genes, and, accordingly, Smc3 haploinsufficiency accelerated lymphomagenesis in mice with constitutive Bcl6 expression. Collectively, our data indicate a dose-dependent function for cohesin in humoral immunity to facilitate the B cell to PC phenotypic switch while restricting malignant transformation.

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