Targeting of Colony-stimulating Factor 1 Receptor (CSF1R) in the CLL Microenvironment Yields Antineoplastic Activity in Primary Patient Samples

Overview

Journal Oncotarget

Specialty Oncology

Date 2018 Jun 7

PMID 29872489

Citations 20

Authors

David K Edwards V

David Tyler Sweeney

Hibery Ho

Christopher A Eide

Angela Rofelty

Anupriya Agarwal

Selina Qiuying Liu

Alexey V Danilov

Patrice Lee

David Chantry

Shannon K McWeeney

Brian J Druker

Jeffrey W Tyner

Stephen E Spurgeon

Marc M Loriaux

Affiliations

Soon will be listed here.

Abstract

In many malignancies, the tumor microenvironment includes CSF1R-expressing supportive monocyte/macrophages that promote tumor cell survival. For chronic lymphocytic leukemia (CLL), these supportive monocyte/macrophages are known as nurse-like cells (NLCs), although the potential effectiveness of selective small-molecule inhibitors of CSF1R against CLL is understudied. Here, we demonstrate the preclinical activity of two inhibitors of CSF1R, GW-2580 and ARRY-382, in primary CLL patient samples. We observed at least 25% of CLL samples showed sub-micromolar sensitivity to CSF1R inhibitors. This sensitivity was observed in samples with varying genetic and clinical backgrounds, although higher white cell count and monocyte cell percentage was associated with increased sensitivity. Depleting CD14-expressing monocytes preferentially decreased viability in samples sensitive to CSF1R inhibitors, and treating samples with CSF1R inhibitors eliminated the presence of NLCs in long-term culture conditions. These results indicate that CSF1R small-molecule inhibitors target CD14-expressing monocytes in the CLL microenvironment, thereby depriving leukemia cells of extrinsic support signals. In addition, significant synergy was observed combining CSF1R inhibitors with idelalisib or ibrutinib, two current CLL therapies that disrupt tumor cell intrinsic B-cell receptor signaling. These findings support the concept of simultaneously targeting supportive NLCs and CLL cells and demonstrate the potential clinical utility of this combination.

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