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Loss of the DNA Repair Gene RNase H2 Identifies a Unique Subset of DDR-Deficient Leiomyosarcomas

核糖核酸酶P 生物 平滑肌肉瘤 免疫组织化学 拷贝数分析 拷贝数变化 微阵列 分子生物学 癌症研究 男科 基因 病理 医学 遗传学 免疫学 基因表达 核糖核酸 基因组
作者
Michael S. Nakazawa,Ian M. Silverman,Victoria Rimkunas,Artur Veloso,Dominik Głodzik,Adrienne Johnson,Toshiro K. Ohsumi,Shreyaskumar Patel,Anthony P. Conley,Christina L. Roland,Pamela T. Soliman,Hannah C. Beird,Chia-Chin Wu,Davis R. Ingram,Rossana Lazcano,Dawon Song,Khalida Wani,Alexander J. Lazar,Timothy A. Yap,Wei‐Lien Wang,J. Andrew Livingston
出处
期刊:Molecular Cancer Therapeutics [American Association for Cancer Research]
卷期号:23 (7): 1057-1065 被引量:1
标识
DOI:10.1158/1535-7163.mct-23-0761
摘要

Targeting the DNA damage response (DDR) pathway is an emerging therapeutic approach for leiomyosarcoma (LMS), and loss of RNase H2, a DDR pathway member, is a potentially actionable alteration for DDR-targeted treatments. Therefore, we designed a protein- and genomic-based RNase H2 screening assay to determine its prevalence and prognostic significance. Using a selective RNase H2 antibody on a pan-tumor microarray (TMA), RNase H2 loss was more common in LMS (11.5%, 9/78) than across all tumors (3.8%, 32/843). In a separate LMS cohort, RNase H2 deficiency was confirmed in uterine LMS (U-LMS, 21%, 23/108) and soft-tissue LMS (ST-LMS; 30%, 39/102). In the TCGA database, RNASEH2B homozygous deletions (HomDels) were found in 6% (5/80) of LMS cases, with a higher proportion in U-LMS (15%; 4/27) compared with ST-LMS (2%; 1/53). Using the SNiPDx targeted-NGS sequencing assay to detect biallelic loss of function in select DDR-related genes, we found RNASEH2B HomDels in 54% (19/35) of U-LMS cases with RNase H2 loss by IHC, and 7% (3/43) HomDels in RNase H2 intact cases. No RNASEH2B HomDels were detected in ST-LMS. In U-LMS patient cohort (n = 109), no significant overall survival difference was seen in patients with RNase H2 loss versus intact, or RNASEH2B HomDel (n = 12) versus Non-HomDel (n = 37). The overall diagnostic accuracy, sensitivity, and specificity of RNase H2 IHC for detecting RNA-SEH2B HomDels in U-LMS was 76%, 93%, and 71%, respectively, and it is being developed for future predictive biomarker driven clinical trials targeting DDR in U-LMS.
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