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Spatial profiling of patient-matched HER2 positive gastric cancer reveals resistance mechanisms to targeted therapy

曲妥珠单抗 医学 靶向治疗 仿形(计算机编程) 后天抵抗 内科学 肿瘤科 临床试验 癌症 癌症研究 生物信息学 抗药性 癌症治疗 乳腺癌
作者
Taotao Sheng,Raghav Sundar,Supriya Srivastava,Xuewen Ong,Su Ting Tay,Haoran Ma,Tomoyuki Uchihara,Benedict Shi Xiang Lian,Takeshi Hagihara,Mei Kong,Chang Xu,Shamaine Wei Ting Ho,Kie Kyon Huang,Angie Lay Keng Tan,Michelle Ng,Jiamin Toh,Clara Shi Ya Ng,Vincenzo Nasca,Chiara Pircher,Giovanni Randon
出处
期刊:Gut [BMJ]
卷期号:75 (4): 733-747 被引量:11
标识
DOI:10.1136/gutjnl-2024-334667
摘要

Background Human epidermal growth factor receptor 2 (HER2; ERBB2 ) is overexpressed or amplified in 15–20% of gastric cancers (HER2+ GC). Within individual HER2+ GCs, HER2/ ERBB2 expression is often variable. Although HER2 therapeutic targeting improves outcomes for HER2+ GC patients, acquired resistance is frequent. Objective To spatially interrogate HER2+ GC interpatient and intrapatient heterogeneity and resistance mechanisms associated with HER2-targeting agents (trastuzumab, trastuzumab deruxtecan (T-DXd)). Design Spatial transcriptomic analysis (GeoMx Digital Spatial Profiler) was applied to >1500 regions of interest in 30 GCs—these contained 15 HER2+ GCs treated with trastuzumab and T-DXd subsequently. Analysis of patient-matched samples with acquired trastuzumab or T-DXd resistance revealed escape mechanisms. Results were validated by immunohistochemistry, independent cohorts and patient-derived xenografts and organoids. Results HER2+ tumours exhibited PD-L1 expression within the spatial tumour microenvironment. We observed increased expression of CLDN18.2, a promising therapeutic target, in trastuzumab-resistant tumours. One-third of HER2+ GC patients developed epithelial-mesenchymal transition (EMT) on trastuzumab resistance, associated with PD-L1 and CCL2 upregulation. Another third of trastuzumab-resistant HER2+ GC patients activated the endoplasmic reticulum-associated degradation (ERAD) pathway including genes such as GOLM1 . HLA loss and increases in oxidative phosphorylation pathways were observed in T-DXd-resistant GCs. Conclusion Our results delineate multiple acquired resistance mechanisms to trastuzumab and T-DXd in HER2+ GC in vivo . This information may guide trials combining trastuzumab or T-DXd with new agents to enhance the efficacy and durability of HER2 blockade.
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