HLA-A*02:01 allele is associated with decreased risk and a longer survival in pancreatic cancer: Results from an exhaustive analysis of the HLA variation in PDAC

medRxiv - Oncology Pub Date : 2024-08-29 DOI:10.1101/2024.08.29.24312704

Alberto Langtry, Raul Rabadan, Lola Alonso, Casper van Eijck, Teresa Macarulla, Rita T Lawlor, Alfredo Carrato, Rafael Alvarez-Gallego, Mar Iglesias, Xavier Molero, J Matthias Löhr, Christopher W Michalski, José Perea, Michael O’Rorke, Víctor M Barberà, Adonina Tardón, Antoni Farré, Luís Muñoz-Bellvís, Tatjana Crnogorac-Jurcevic, Enrique Domínguez-Muñoz, Thomas Gress, William Greenhalf, Linda Sharp, Sergio Sabroso-Lasa, Ioan Filip, Gaby Strijk, Florian Castet, Joaquim Balsells, Eithne Costello, Jörg Kleeff, Bo Kong, Josefina Mora, Damian O’Driscoll, Aldo Scarpa, Weimin Ye, Francisco X. Real, Núria Malats, Evangelina López de Maturana, PanGenEU Investigators

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Abstract

Genetic susceptibility loci are associated with PDAC risk and survival, but the impact of germline HLA region variation remains largely unexplored. This study examined HLA I-II alleles within the PanGenEU study and validated our findings using external datasets (UK Biobank, TCGA, PAN-NGS trial, and Caris trial). HLA-A*02:01and HLA-B*49 alleles were linked to a decreased risk of PDAC, whereas HLA-B*39, HLA-DPB1*04, and HLA-A*26:01 were directly associated with increased risk. PDAC patients carrying the HLA-A*02:01 allele also showed lower mortality rates, with the effect being more pronounced in those with KRAS^G12V mutations, pointing to a host*tumor genetic interaction. This research highlights HLA-A*02:01, found in 20% of Europeans, as a marker for reduced PDAC risk and mortality, especially in KRAS^G12V mutated tumors. Results from this study could enhance personalized medicine for PDAC by identifying patients who may benefit from regular screenings through tailored risk assessments. Importantly, our findings are crucial for stratifying PDAC patients based on their genetic background and tumor mutational profile, which can guide treatment strategies.

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HLA-A*02:01 等位基因与胰腺癌风险降低和生存期延长有关：对 PDAC 中 HLA 变异的详尽分析结果

遗传易感基因位点与 PDAC 风险和存活率有关，但种系 HLA 区域变异的影响在很大程度上仍未得到探讨。本研究检测了 PanGenEU 研究中的 HLA I-II 等位基因，并利用外部数据集（英国生物库、TCGA、PAN-NGS 试验和 Caris 试验）验证了我们的研究结果。HLA-A*02:01和HLA-B*49等位基因与PDAC风险的降低有关，而HLA-B*39、HLA-DPB1*04和HLA-A*26:01则与风险的增加直接相关。携带HLA-A*02:01等位基因的PDAC患者死亡率也较低，这种效应在KRASG12V突变的患者中更为明显，这表明宿主与肿瘤基因之间存在相互作用。这项研究强调，在20%的欧洲人中发现的HLA-A*02:01是降低PDAC风险和死亡率的标志物，尤其是在KRASG12V突变的肿瘤中。这项研究的结果可以通过量身定制的风险评估确定哪些患者可以从定期筛查中获益，从而加强针对 PDAC 的个性化医疗。重要的是，我们的研究结果对于根据遗传背景和肿瘤突变情况对PDAC患者进行分层至关重要，可为治疗策略提供指导。

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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medRxiv - Oncology

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