Roche Pharmaceutical Research and Early Development Oncology, Roche Innovation Center Basel, Basel, Switzerland.
Roche Pharmaceutical Research and Early Development, Pharmaceutical Sciences - Biomarkers, Bioinformatics and Omics & Pathology, Roche Innovation Center Basel, Basel, Switzerland.
Front Immunol. 2024 Feb 22;15:1285049. doi: 10.3389/fimmu.2024.1285049. eCollection 2024.
Downregulation of MHC class I expression and/or defects in the antigen presentation pathways are commonly reported in human cancers. Numerous studies previously have explored extensively the molecular mechanisms that underlie HLA-class I and Beta2-Microglobulin (B2M) downregulation. However, the techniques presently available to detect expression of MHC class I proteins lack the robustness, specificity and sensitivity needed for systematic integration and analysis in clinical trials. Furthermore, the dynamics of HLA-class I and B2M expression have not been comprehensively studied as a potential biomarker for immunotherapy.
Using novel, validated, immunohistochemistry (IHC)-based methods for quantifying B2M and HLA-A in tumor samples from diverse cancer types, we have determined loss of B2M and HLA-A proteins in 336 archived, primary specimens and 329 biopsies from metastatic patients collected during Roche-sponsored Phase 1 clinical trials investigating novel immunotherapy candidates as monotherapy or in combination with CPI.
Up to 56% of cases with B2M or HLA-A loss were noted in the investigated tumor types. The frequency of loss was dependent on indication and stage of disease and revealed heterogeneous expression patterns across patients. B2M and HLA-A loss was increased in metastatic lesions compared to primary tumors, indicating selection of MHC class I low clones in metastatic and refractory tumor cells. High on-treatment B2M expression correlated with successful clinical outcome (RECIST), while high baseline B2M did not. A treatment-induced increase of B2M expression was noted in most of the patients with low B2M levels at baseline. The triple biomarker combination of B2M, CD8 and PDL1 strongly improved response prediction to cancer immunotherapy.
Our results indicate that B2M and HLA-A loss occurs frequently in tumors and is reversed in most instances following immunotherapy which supports the conclusion that MHC class I loss is not the dominant resistance mechanism to CPI treatment. This investigation reveals a highly dynamic expression of HLA-A and B2M in tumors affected by indication, metastatic status, immunophenotype and immunotherapy treatment. Baseline expression levels of B2M on tumors may be of utility as a constituent of a biomarker panel used for selecting patients for immunotherapy clinical trials.
人类癌症中普遍存在 MHC Ⅰ类分子表达下调和/或抗原呈递途径缺陷。先前已有大量研究广泛探索了 HLA-Ⅰ类和β2-微球蛋白(B2M)下调的分子机制。然而,目前用于检测 MHC Ⅰ类蛋白表达的技术缺乏在临床试验中进行系统整合和分析所需的稳健性、特异性和灵敏度。此外,HLA-Ⅰ类和 B2M 表达的动态变化尚未作为免疫治疗的潜在生物标志物进行全面研究。
我们使用新颖的、经过验证的、基于免疫组织化学(IHC)的方法来定量检测来自不同癌症类型的肿瘤样本中的 B2M 和 HLA-A,我们在罗氏赞助的 1 期临床试验中确定了 336 个存档的原发性标本和 329 个转移性患者的活检中 B2M 和 HLA-A 蛋白的缺失,这些试验旨在研究新型免疫治疗候选药物作为单一药物或与 CPI 联合治疗的效果。
在所研究的肿瘤类型中,高达 56%的病例存在 B2M 或 HLA-A 缺失。缺失的频率取决于适应症和疾病阶段,并在患者之间呈现出异质性表达模式。与原发性肿瘤相比,转移性病变中 B2M 和 HLA-A 的缺失增加,表明 MHC Ⅰ类低克隆在转移性和难治性肿瘤细胞中被选择。高治疗 B2M 表达与成功的临床结果(RECIST)相关,而高基线 B2M 则不相关。在基线 B2M 水平较低的大多数患者中,观察到 B2M 表达的治疗诱导增加。B2M、CD8 和 PDL1 的三重生物标志物组合强烈改善了对癌症免疫治疗的反应预测。
我们的结果表明,B2M 和 HLA-A 的缺失在肿瘤中经常发生,并且在大多数情况下,免疫治疗后会逆转,这支持 MHC Ⅰ类缺失不是 CPI 治疗的主要耐药机制的结论。本研究揭示了受适应症、转移状态、免疫表型和免疫治疗影响的肿瘤中 HLA-A 和 B2M 的高度动态表达。肿瘤 B2M 的基线表达水平可能作为用于选择免疫治疗临床试验患者的生物标志物组合的一部分具有实用性。
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