Leukaemia exposure alters the transcriptional profile and function of BCR::ABL1 negative macrophages in the bone marrow niche

Author:

Dawson Amy,Zarou Martha M.ORCID,Prasad BodhayanORCID,Bittencourt-Silvestre Joana,Zerbst Désirée,Himonas EkateriniORCID,Hsieh Ya-Ching,van Loon Isabel,Blanco Giovanny Rodriguez,Ianniciello Angela,Kerekes Zsombor,Krishnan VaidehiORCID,Agarwal PuneetORCID,Almasoudi Hassan,McCluskey Laura,Hopcroft Lisa E. M.ORCID,Scott Mary T.ORCID,Baquero Pablo,Dunn KarenORCID,Vetrie DavidORCID,Copland MhairiORCID,Bhatia RaviORCID,Coffelt Seth B.ORCID,Tiong Ong SinORCID,Wheadon HelenORCID,Zanivan Sara,Kirschner KristinaORCID,Helgason G. VignirORCID

Abstract

AbstractMacrophages are fundamental cells of the innate immune system that support normal haematopoiesis and play roles in both anti-cancer immunity and tumour progression. Here we use a chimeric mouse model of chronic myeloid leukaemia (CML) and human bone marrow (BM) derived macrophages to study the impact of the dysregulated BM microenvironment on bystander macrophages. Utilising single-cell RNA sequencing (scRNA-seq) of Philadelphia chromosome (Ph) negative macrophages we reveal unique subpopulations of immature macrophages residing in the CML BM microenvironment. CML exposed macrophages separate from their normal counterparts by reduced expression of the surface marker CD36, which significantly reduces clearance of apoptotic cells. We uncover aberrant production of CML-secreted factors, including the immune modulatory protein lactotransferrin (LTF), that suppresses efferocytosis, phagocytosis, and CD36 surface expression in BM macrophages, indicating that the elevated secretion of LTF is, at least partially responsible for the supressed clearance function of Ph- macrophages.

Funder

Kay Kendall Leukaemia Fund

Cancer Research UK

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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