Abstract
Anaplastic thyroid cancer (ATC) is a clinically aggressive malignancy with a dismal prognosis. Combined BRAF/MEK inhibition offers significant therapeutic benefit in patients with BRAFV600E-mutant ATCs. However, relapses are common and overall survival remains poor. Compared with differentiated thyroid cancer, a hallmark of ATCs is significant infiltration with myeloid cells, particularly macrophages. ATCs are most common in the aging population, which also has an increased incidence of TET2-mutant clonal hematopoiesis (CH). CH-mutant macrophages have been shown to accelerate CH-associated pathophysiology including atherosclerosis. However, the clinical and mechanistic contribution of CH-mutant clones to solid tumour biology, prognosis and therapeutic response has not been elucidated. Here we show that TET2-mutant CH is enriched in the tumour microenvironment of patients with solid tumours and associated with adverse prognosis in ATC patients. We find that Tet2-mutant macrophages selectively infiltrate mouse BrafV600E-mutant ATC and that their overexpression of Tgfβ-family ligands mediates resistance to BRAF/MEK inhibition. Importantly, inhibition of Tgfβ signaling restores sensitivity to MAPK pathway inhibition, opening a path for synergistic strategies to improve outcomes of patients with ATCs and concurrent CH.
Competing Interest Statement
V.T., P.S.V, J.L.Y., B.R.U., L.B., A.B.C., S.F.E., A.S., M.K., J.G, M.W., A.K., K.C., T.Q., A.R.M.B, R.P., M.S., G.P.K., E.D.S., A.Z., R.S., J.K., R.L.B, S.D. declare no relevant conflict of interest. A.J.S. declares spousal employment at Astra Zeneca. M.E. declares past grants from Ferrer International and Incyte, and personal fees from Quimatryx, unrelated to this work. M.F.B. declares consulting positions at AstraZeneca and Paige.AI and intellectual property rights at SOPHiA Genetics. R.P.K. is a co-founder of and consultant for Econic Biosciences. J.A.F. is a co-inventor of intellectual property focused on HRAS as a biomarker for treating cancer using tipifarnib which has been licensed by MSK to Kura Oncology. J.A.F. received prior research funding from Eisai and was a former consultant for LOXO Oncology, both unrelated to this work. R.L.L. is on the Supervisory board of Qiagen, a co-founder/advisor/board member at Ajax, and is a scientific advisor to Mission Bio, Zentalis, Auron, Prelude, Anovia, Bakx, Epiphanes, Kurome, Scorpion, Syndax and C4 Therapeutics; for each of these entities he receives equity. He has received research support from Calico, Zentalis and Ajax, and has consulted Jubilant, Goldman Sachs, Incyte, Astra Zeneca and Janssen.
Footnotes
↵† These authors jointly supervised this work.