PD-L1⁺ diffuse large B-cell lymphoma with extremely high mutational burden and microsatellite instability due to acquired PMS2 mutation.

IF 1.8 Q3 MEDICINE, RESEARCH & EXPERIMENTAL

Cold Spring Harbor Molecular Case Studies Pub Date : 2024-01-10 Print Date: 2023-12-01 DOI:10.1101/mcs.a006318

Andrew W Allbee, James Gerson, Guang Yang, Adam Bagg

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引用次数: 0

Abstract

We present a unique case of a single patient presenting with two mutationally distinct, PD-L1⁺ diffuse large B-cell lymphomas (DLBCLs). One of these DLBCLs demonstrated exceptionally high mutational burden (eight disease-associated variants and 41 variants of undetermined significance) with microsatellite instability (MSI) and an acquired PMS2 mutation with loss of PMS2 protein expression, detected postchemotherapy. This report, while highlighting the extent of possible tumor heterogeneity across separate clonal expansions as well as possible syndromic B-cell neoplasia, supports the notion that, although rare, PD-L1 expression and associated states permissive of high mutational burden (such as mismatch repair gene loss of function/MSI) should be more routinely considered in DLBCLs. Appropriate testing may be predictive of outcome and inform the utility of targeted therapy in these genetically diverse and historically treatment-refractory malignancies.

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PD-L1+弥漫大 B 细胞淋巴瘤，因获得性 PMS2 基因突变而具有极高的突变负荷和微卫星不稳定性。

我们介绍了一个独特的病例，该病例中的一名患者同时患有两种突变不同的 PD-L1+ 弥漫性大 B 细胞淋巴瘤（DLBCL）。其中一个 DLBCL 的突变负荷特别高（8 个疾病相关变异和 41 个意义未定的变异），伴有微卫星不稳定性（MSI）和获得性 PMS2 突变，化疗后检测到 PMS2 蛋白表达缺失。该报告强调了不同克隆扩增之间可能存在的肿瘤异质性程度以及可能存在的综合征 B 细胞肿瘤，同时也支持这样一种观点，即尽管 PD-L1 表达和允许高突变负荷的相关状态（如错配修复基因功能缺失/MSI）非常罕见，但在 DLBCL 中应更多地予以常规考虑。适当的检测可预测预后，并为靶向治疗在这些基因多样且历来难治的恶性肿瘤中的应用提供信息。

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

Cold Spring Harbor Molecular Case Studies MEDICINE, RESEARCH & EXPERIMENTAL-

CiteScore

3.20

自引率

0.00%

发文量

期刊介绍： Cold Spring Harbor Molecular Case Studies is an open-access, peer-reviewed, international journal in the field of precision medicine. Articles in the journal present genomic and molecular analyses of individuals or cohorts alongside their clinical presentations and phenotypic information. The journal''s purpose is to rapidly share insights into disease development and treatment gained by application of genomics, proteomics, metabolomics, biomarker analysis, and other approaches. The journal covers the fields of cancer, complex diseases, monogenic disorders, neurological conditions, orphan diseases, infectious disease, gene therapy, and pharmacogenomics. It has a rapid peer-review process that is based on technical evaluation of the analyses performed, not the novelty of findings, and offers a swift, clear path to publication. The journal publishes: Research Reports presenting detailed case studies of individuals and small cohorts, Research Articles describing more extensive work using larger cohorts and/or functional analyses, Rapid Communications presenting the discovery of a novel variant and/or novel phenotype associated with a known disease gene, Rapid Cancer Communications presenting the discovery of a novel variant or combination of variants in a cancer type, Variant Discrepancy Resolution describing efforts to resolve differences or update variant interpretations in ClinVar through case-level data sharing, Follow-up Reports linked to previous observations, Plus Review Articles, Editorials, and Position Statements on best practices for research in precision medicine.