Litcius/Paper detail

Inflation of tumor mutation burden by tumor-only sequencing in under-represented groups

Yan W. Asmann, Kaushal Parikh, P. Leif Bergsagel, Haidong Dong, Alex A. Adjei, Mitesh J. Borad, Aaron S. Mansfield

2021npj Precision Oncology33 citationsDOIOpen Access PDF

Abstract

With the recent FDA approval of tumor mutational burden-high (TMB-H) status as a biomarker for treatment with a PD-1 inhibitor regardless of tumor type, accurate assessment of patient-specific TMB is more critical now more than ever. Using paired tumor and germline exome sequencing data from 701 patients newly diagnosed with multiple myeloma, including 575 self-reported White patients and 126 self-reported Black patients, we observed that compared to the gold standard of filtering germline variants with patient-paired germline sequencing data, TMB estimates were significantly higher in both Black and White patients when using public databases for filtering non-somatic mutations; however, TMB was more significantly inflated in Black patients compared to White patients. TMB as a biomarker for patient selection to receive immune checkpoint inhibitors (ICIs) therapy without patient-paired germline sequencing may introduce racial bias due to the under-representation of minority groups in public databases.

Topics & Concepts

GermlineGermline mutationExomeMedicineExome sequencingOncologyInternal medicineBiomarkerMutationBiologyGeneticsGeneCancer Genomics and DiagnosticsMultiple Myeloma Research and TreatmentsRenal Transplantation Outcomes and Treatments