Immuno-genomic landscape of osteosarcoma

Author:

Wu Chia-ChinORCID,Beird Hannah C.ORCID,Andrew Livingston J.ORCID,Advani Shailesh,Mitra AkashORCID,Cao Shaolong,Reuben AlexandreORCID,Ingram Davis,Wang Wei-Lien,Ju Zhenlin,Hong Leung Cheuk,Lin Heather,Zheng Youyun,Roszik JasonORCID,Wang Wenyi,Patel Shreyaskumar,Benjamin Robert S.,Somaiah NeetaORCID,Conley Anthony P.,Mills Gordon B.,Hwu Patrick,Gorlick Richard,Lazar AlexanderORCID,Daw Najat C.,Lewis Valerae,Futreal P. AndrewORCID

Abstract

AbstractLimited clinical activity has been seen in osteosarcoma (OS) patients treated with immune checkpoint inhibitors (ICI). To gain insights into the immunogenic potential of these tumors, we conducted whole genome, RNA, and T-cell receptor sequencing, immunohistochemistry and reverse phase protein array profiling (RPPA) on OS specimens from 48 pediatric and adult patients with primary, relapsed, and metastatic OS. Median immune infiltrate level was lower than in other tumor types where ICI are effective, with concomitant low T-cell receptor clonalities. Neoantigen expression in OS was lacking and significantly associated with high levels of nonsense-mediated decay (NMD). Samples with low immune infiltrate had higher number of deleted genes while those with high immune infiltrate expressed higher levels of adaptive resistance pathways. PARP2 expression levels were significantly negatively associated with the immune infiltrate. Together, these data reveal multiple immunosuppressive features of OS and suggest immunotherapeutic opportunities in OS patients.

Funder

A Shelter for Cancer Families

Cancer Prevention and Research Institute of Texas

QuadW Foundation

Publisher

Springer Science and Business Media LLC

Subject

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

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