Litcius/Paper detail

The microenvironment of DLBCL is characterized by noncanonical macrophages recruited by tumor-derived CCL5

Benoît Manfroi, Maria De Grandis, Jérôme Moreaux, Sébastien P. Tabruyn, Jean-François Mayol, Mélanie Quintero, Christian Righini, Nathalie Stürm, Michel Aurrand‐Lions, Bertrand Huard

2021Blood Advances30 citationsDOIOpen Access PDF

Abstract

Tissue invasion by tumor cells induces a host inflammatory response that variably impacts tumorigenesis. This has been well documented for tumor-associated macrophages (TAMs) that could play a pro/M2- or an anti/M1-tumoral function. TAMs frequently infiltrate diffuse large B-cell lymphoma (DLBCL), an aggressive neoplasm arising from germinal center-experienced B cells. However, the pathway leading to the presence of TAMs in DLBCL remains unknown, and their impact is unclear. Here, we show that some DLBCL tumor cells expressed the chemokine CCL5, enabling the differential recruitment of blood monocytes through their expression of CCR1 and CCR5. CCL5 expression by DLBCL was not related to molecular subtypes, and healthy tonsillar B cells did not produce this chemokine, implying a posttransformation event. A single-cell analysis revealed that most DLBCL TAMs had a noncanonical gene signature with the concomitant expression of M1 and M2 genes. The presence of noncanonical TAMs may explain the lack of impact of macrophages on DLBCL development reported in some survival studies.

Topics & Concepts

CCL5Diffuse large B-cell lymphomaGerminal centerChemokineCancer researchTumor-associated macrophageLymphomaBiologyTumor microenvironmentChemokine receptorImmunologyB cellInflammationT cellAntibodyImmune systemTumor cellsIL-2 receptorImmune Cell Function and InteractionImmune cells in cancerLymphoma Diagnosis and Treatment
The microenvironment of DLBCL is characterized by noncanonical macrophages recruited by tumor-derived CCL5 | Litcius