Extensive Remodeling of the Immune Microenvironment in B Cell Acute Lymphoblastic Leukemia

Chunxu Qu,William L. Carroll,Philip J. Lupo,Gabriel Robbins ,Joanna Pierro,Sheetal Sreeram,Nikki A. Evensen,Matthew Witkowski ,Marla Daves,Caihong Ma ,Weiqiang Chen,Deqing Pei,Aristotelis Tsirigos,Cheng Cheng,Charles G. Mullighan,Yuling Dai,Anastasia Tikhonova ,Tiffany M. Chambers ,Igor Dolgalev,Karen R. Rabin,Cynthia A. Loomis,Michael E. Scheurer,Valeria Mezzano,Kathryn G. Roberts,Audrey Lasry,Iannis Aifantis,Shanmugapriya Selvaraj

doi:10.1016/j.ccell.2020.04.015

Chunxu Qu, William L. Carroll + Show 25 more

Open Access

https://doi.org/10.1016/j.ccell.2020.04.015

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Abstract

A subset of B cell acute lymphoblastic leukemia (B-ALL) patients will relapse and succumb to therapy-resistant disease. The bone marrow microenvironment may support B-ALL progression and treatment evasion. Utilizing single-cell approaches, we demonstrate B-ALL bone marrow immune microenvironment remodeling upon disease initiation and subsequent re-emergence during conventional chemotherapy. We uncover a role for non-classical monocytes in B-ALL survival, and demonstrate monocyte abundance at B-ALL diagnosis is predictive of pediatric and adult B-ALL patient survival. We show that human B-ALL blasts alter a vascularized microenvironment promoting monocytic differentiation, while depleting leukemia-associated monocytes in B-ALL animal models prolongs disease remission invivo. Our profiling of the B-ALL immune microenvironment identifies extrinsic regulators of B-ALL survival supporting new immune-based therapeutic approaches for high-risk B-ALL treatment.

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