B-cell-specific Checkpoint Molecules That Regulate Anti-tumour Immunity

Overview

Journal Nature

Specialty Science

Date 2023 Jun 21

PMID 37344597

Authors

Lloyd Bod

Yoon-Chul Kye

Jingwen Shi

Elena Torlai Triglia

Alexandra Schnell

Johannes Fessler

Stephen M Ostrowski

Max Y Von-Franque

Juhi R Kuchroo

Rocky M Barilla

Sarah Zaghouani

Elena Christian

Toni Marie Delorey

Kanishka Mohib

Sheng Xiao

Nadine Slingerland

Christopher J Giuliano

Orr Ashenberg

Zhaorong Li

David M Rothstein

David E Fisher

Orit Rozenblatt-Rosen

Arlene H Sharpe

Francisco J Quintana

Lionel Apetoh

Aviv Regev

Vijay K Kuchroo

Affiliations

Soon will be listed here.

Abstract

The role of B cells in anti-tumour immunity is still debated and, accordingly, immunotherapies have focused on targeting T and natural killer cells to inhibit tumour growth. Here, using high-throughput flow cytometry as well as bulk and single-cell RNA-sequencing and B-cell-receptor-sequencing analysis of B cells temporally during B16F10 melanoma growth, we identified a subset of B cells that expands specifically in the draining lymph node over time in tumour-bearing mice. The expanding B cell subset expresses the cell surface molecule T cell immunoglobulin and mucin domain 1 (TIM-1, encoded by Havcr1) and a unique transcriptional signature, including multiple co-inhibitory molecules such as PD-1, TIM-3, TIGIT and LAG-3. Although conditional deletion of these co-inhibitory molecules on B cells had little or no effect on tumour burden, selective deletion of Havcr1 in B cells both substantially inhibited tumour growth and enhanced effector T cell responses. Loss of TIM-1 enhanced the type 1 interferon response in B cells, which augmented B cell activation and increased antigen presentation and co-stimulation, resulting in increased expansion of tumour-specific effector T cells. Our results demonstrate that manipulation of TIM-1-expressing B cells enables engagement of the second arm of adaptive immunity to promote anti-tumour immunity and inhibit tumour growth.

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