Analysis of Concordance Between Next-Generation Sequencing Assessment of Microsatellite Instability and Immunohistochemistry-Mismatch Repair From Solid Tumors.

IF 5.3 2区 医学 Q1 ONCOLOGY
JCO precision oncology Pub Date : 2024-10-01 Epub Date: 2024-11-20 DOI:10.1200/PO.23.00648
Rouba Ali-Fehmi, Harris Benjamin Krause, Robert T Morris, John J Wallbillich, Logan Corey, Sudeshna Bandyopadhyay, Mira Kheil, Leana Elbashir, Fadi Zaiem, M Ruhul Quddus, Evi Abada, Thomas Herzog, Anthony N Karnezis, Emmanuel S Antonarakis, Pashtoon Murtaza Kasi, Shuanzeng Wei, Jeffrey Swensen, Andrew Elliott, Joanne Xiu, Jaclyn Hechtman, David Spetzler, Jim Abraham, Milan Radovich, George Sledge, Matthew J Oberley, David Bryant
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引用次数: 0

Abstract

Purpose: The new CAP guideline published in August 2022 recommends using immunohistochemistry (IHC) to test for mismatch repair defects in gastroesophageal (GE), small bowel (SB), or endometrial carcinoma (EC) cancers over next-generation sequencing assessment of microsatellite instability (NGS-MSI) for immune checkpoint inhibitor (ICI) therapy eligibility and states there is a preference to use IHC over NGS-MSI in colorectal carcinoma (CRC).

Methods: We assessed the concordance of NGS-MSI and IHC-MMR from a very large cohort across the spectrum of solid tumors.

Results: Of the over 190,000 samples with both NGS-MSI and IHC-MMR about 1,160 were initially flagged as discordant. Of those samples initially flagged as discordant, 50.9% remained discordant after being reviewed by an additional pathologist. This resulted in a final discordance rate of 0.31% (590/191,767). Among CRC, GE, SB and EC, 55.4% of mismatch repair proficient/MSI high (MMRp/MSI-H) tumors had at least one somatic pathogenic mutation in an MMR gene or POLE. Mismatch repair deficient/microsatellite stable (MMRd/MSS) tumors had a significantly lower rate of high tumor mutational burden than MMRp/MSI-H tumors. Across all solid tumors, MMRd/MSI-H tumors had significantly longer overall survival (OS; hazard ratio [HR], 1.47, P < .001) and post-ICI survival (HR, 1.82, P < .001) as compared with MMRp/MSS tumors. The OS for the MMRd/MSS group was slightly worse compared to the MMRp/MSI-H tumors, but this difference was not statistically significant (HR, 0.73, P = .058), with a similar pattern when looking at post-ICI survival (HR, 0.43, P = .155).

Conclusion: This study demonstrates that NGS-MSI is noninferior to IHC-MMR and can identify MSI-H tumors that IHC-MMR is unable to detect and conversely IHC-MMR can identify MMRd tumors that NGS-MSI misses.

实体瘤微卫星不稳定性的下一代测序评估与免疫组化-错配修复的一致性分析
目的:2022年8月发布的新版CAP指南建议,在检测胃食管癌(GE)、小肠癌(SB)或子宫内膜癌(EC)的错配修复缺陷时,使用免疫组化(IHC)而非下一代测序评估微卫星不稳定性(NGS-MSI)来确定免疫检查点抑制剂(ICI)的治疗资格,并指出在检测结直肠癌(CRC)的错配修复缺陷时,优先使用IHC而非NGS-MSI:方法: 我们评估了来自实体瘤领域的一个庞大队列的 NGS-MSI 和 IHC-MMR 的一致性:结果:在同时具有 NGS-MSI 和 IHC-MMR 的 190,000 多个样本中,约有 1,160 个样本最初被标记为不一致。在这些最初被标记为不一致的样本中,50.9% 的样本在由另一位病理学家复查后仍不一致。因此,最终的不一致率为 0.31%(590/191,767)。在CRC、GE、SB和EC中,55.4%的错配修复能力强/MSI高(MMRp/MSI-H)肿瘤至少有一个MMR基因或POLE的体细胞致病突变。错配修复缺陷/微卫星稳定(MMRd/MSS)肿瘤的高肿瘤突变负荷率明显低于MMRp/MSI-H肿瘤。在所有实体瘤中,与 MMRp/MSS 肿瘤相比,MMRd/MSI-H 肿瘤的总生存期(OS;危险比 [HR],1.47,P < .001)和 ICI 后生存期(HR,1.82,P < .001)明显更长。与MMRp/MSI-H肿瘤相比,MMRd/MSS组的OS稍差,但差异无统计学意义(HR,0.73,P = .058),ICI后生存率的情况也类似(HR,0.43,P = .155):这项研究表明,NGS-MSI 的效果并不亚于 IHC-MMR,它能发现 IHC-MMR 无法检测到的 MSI-H 型肿瘤,反之,IHC-MMR 也能发现 NGS-MSI 遗漏的 MMRd 型肿瘤。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
9.10
自引率
4.30%
发文量
363
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