Apoptotic Cell Fragments Locally Activate Tingible Body Macrophages in the Germinal Center

Overview

Journal Cell

Publisher Cell Press

Specialty Cell Biology

Date 2023 Mar 3

PMID 36868219

Authors

Abigail K Grootveld

Wunna Kyaw

Veera Panova

Angelica W Y Lau

Emily Ashwin

Guillaume Seuzaret

Rama Dhenni

Nayan Deger Bhattacharyya

Weng Hua Khoo

Mate Biro

Tanmay Mitra

Michael Meyer-Hermann

Patrick Bertolino

Masato Tanaka

David A Hume

Peter I Croucher

Robert Brink

Akira Nguyen

Oliver Bannard

Tri Giang Phan

Affiliations

Soon will be listed here.

Abstract

Germinal centers (GCs) that form within lymphoid follicles during antibody responses are sites of massive cell death. Tingible body macrophages (TBMs) are tasked with apoptotic cell clearance to prevent secondary necrosis and autoimmune activation by intracellular self antigens. We show by multiple redundant and complementary methods that TBMs derive from a lymph node-resident, CD169-lineage, CSF1R-blockade-resistant precursor that is prepositioned in the follicle. Non-migratory TBMs use cytoplasmic processes to chase and capture migrating dead cell fragments using a "lazy" search strategy. Follicular macrophages activated by the presence of nearby apoptotic cells can mature into TBMs in the absence of GCs. Single-cell transcriptomics identified a TBM cell cluster in immunized lymph nodes which upregulated genes involved in apoptotic cell clearance. Thus, apoptotic B cells in early GCs trigger activation and maturation of follicular macrophages into classical TBMs to clear apoptotic debris and prevent antibody-mediated autoimmune diseases.

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