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Human Germinal Center Transcriptional Programs Are De-synchronized in B Cell Lymphoma

Overview
Journal Nat Immunol
Date 2018 Aug 15
PMID 30104629
Citations 78
Authors
Pierre Milpied
Inaki Cervera-Marzal
Marie-Laure Mollichella
Bruno Tesson
Gabriel Brisou
Alexandra Traverse-Glehen
Gilles Salles
Lionel Spinelli
Bertrand Nadel
Affiliations
Soon will be listed here.
Abstract

Most adult B cell lymphomas originate from germinal center (GC) B cells, but it is unclear to what extent B cells in overt lymphoma retain the functional dynamics of GC B cells or are blocked at a particular stage of the GC reaction. Here we used integrative single-cell analysis of phenotype, gene expression and variable-region sequence of the immunoglobulin heavy-chain locus to track the characteristic human GC B cell program in follicular lymphoma B cells. By modeling the cyclic continuum of GC B cell transitional states, we identified characteristic patterns of synchronously expressed gene clusters. GC-specific gene-expression synchrony was lost in single lymphoma B cells. However, distinct follicular lymphoma-specific cell states co-existed within single patient biopsies. Our data show that lymphoma B cells are not blocked in a GC B cell state but might adopt new dynamic modes of functional diversity, which opens the possibility of novel definitions of lymphoma identity.

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