An In Vivo Inflammatory Loop Potentiates KRAS Blockade

Overview

Journal Biomedicines

Specialty Biomedical Engineering

Date 2022 Mar 25

PMID 35327394

Authors

Kristina A M Arendt

Giannoula Ntaliarda

Vasileios Armenis

Danai Kati

Christin Henning

Georgia A Giotopoulou

Mario A A Pepe

Laura V Klotz

Anne-Sophie Lamort

Rudolf A Hatz

Sebastian Kobold

Andrea C Schamberger

Georgios T Stathopoulos

Affiliations

Soon will be listed here.

Abstract

KRAS (KRAS proto-oncogene, GTPase) inhibitors perform less well than other targeted drugs in vitro and fail clinical trials. To investigate a possible reason for this, we treated human and murine tumor cells with KRAS inhibitors deltarasin (targeting phosphodiesterase-δ), cysmethynil (targeting isoprenylcysteine carboxylmethyltransferase), and AA12 (targeting KRAS), and silenced/overexpressed mutant KRAS using custom-designed vectors. We showed that -mutant tumor cells exclusively respond to KRAS blockade in vivo, because the oncogene co-opts host myeloid cells via a C-C-motif chemokine ligand 2 (CCL2)/interleukin-1 beta (IL-1β)-mediated signaling loop for sustained tumorigenicity. Indeed, -mutant tumors did not respond to deltarasin in C-C motif chemokine receptor 2 and gene-deficient mice, but were deltarasin-sensitive in wild-type and -deficient mice adoptively transplanted with wild-type murine bone marrow. A KRAS-dependent pro-inflammatory transcriptome was prominent in human cancers with high mutation prevalence and poor predicted survival. Our findings support that in vitro cellular systems are suboptimal for anti-KRAS drug screens, as these drugs function to suppress interleukin-1 receptor 1 (IL1R1) expression and myeloid IL-1β-delivered pro-growth effects in vivo. Moreover, the findings support that IL-1β blockade might be suitable for therapy for -mutant cancers.

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