Impaired TGF-β signaling via AHNAK family mutations elicits an esophageal cancer subtype with sensitivities to genotoxic therapy and immunotherapy.

IF 4.6 2区 医学 Q2 IMMUNOLOGY Cancer Immunology, Immunotherapy Pub Date : 2024-09-05 DOI:10.1007/s00262-024-03798-z
Zihang Mai, Luo Kongjia, Xinye Wang, Xiuying Xie, Lanlan Pang, Hong Yang, Jing Wen, Jianhua Fu
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Abstract

Background: Genome instability (GI) is a hallmark of esophageal squamous cell carcinoma (ESCC) while factors affecting GI remain unclear.

Methods: Here, we aimed to characterize genomic events representing specific mechanisms of GI based on 201 ESCC samples and validated our findings at the patient, single-cell and cancer cell-line levels, including a newly generated multi-omics dataset of the trial NCT04006041.

Results: A two-gene (AHNAK and AHNAK2) mutation signature was identified to define the "AHNAK1/2-mutant" cancer subtype. Single-cell-assisted multi-omics analysis showed that this subtype had a higher neoantigen load, active antigen presentation, and proficient CD8 + T cell infiltrations, which were validated at pan-cancer levels. Mechanistically, AHNAK1/2-mutant ESCC was characterized by impaired response of TGF-β and the inefficient alternative end-join repair (Alt-EJ) that might promote GI. Knockdown of AHNAK in ESCC cell lines resulted in more Alt-EJ events and increased sensitivities to cisplatin. Furthermore, this two-gene signature accurately predicted better responses to DNA-damaging therapy in various clinical settings (HR ≈ 0.25). The two-gene signature predicted higher pCR rates in ESCCs receiving neoadjuvant immunotherapy-involved treatment. Finally, a molecular classification scheme was built and outperformed established molecular typing models in the prognosis stratification of ESCC patients.

Conclusion: Our study extended our understanding of the AHNAK family in promoting GI and selecting treatment responders of ESCC.

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通过AHNAK家族突变导致的TGF-β信号传导受损会诱发一种对基因毒性疗法和免疫疗法敏感的食管癌亚型。
背景:基因组不稳定性(GI)是食管鳞状细胞癌(ESCC)的一个特征,而影响GI的因素仍不清楚。方法:在此,我们以201份ESCC样本为基础,旨在描述代表GI特定机制的基因组事件的特征,并在患者、单细胞和癌细胞系水平验证我们的发现,包括NCT04006041试验中新生成的多组学数据集:结果:确定了一个双基因(AHNAK和AHNAK2)突变特征,从而定义了 "AHNAK1/2突变 "癌症亚型。单细胞辅助多组学分析表明,该亚型具有较高的新抗原负荷、活跃的抗原呈递和熟练的CD8 + T细胞浸润,这在泛癌水平上得到了验证。从机理上讲,AHNAK1/2突变型ESCC的特点是对TGF-β的反应受损和替代性末端连接修复(Alt-EJ)效率低下,这可能会促进GI。在ESCC细胞系中敲除AHNAK会导致更多的Alt-EJ事件,并增加对顺铂的敏感性。此外,这两个基因特征还能准确预测各种临床环境中对DNA损伤疗法的更好反应(HR≈0.25)。在接受新辅助免疫疗法治疗的 ESCC 中,该双基因特征预测了更高的 pCR 率。最后,我们建立了一个分子分类方案,该方案在ESCC患者预后分层方面优于已有的分子分型模型:我们的研究拓展了我们对AHNAK家族在促进GI和选择ESCC治疗应答者方面的认识。
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来源期刊
CiteScore
10.50
自引率
1.70%
发文量
207
审稿时长
1 months
期刊介绍: Cancer Immunology, Immunotherapy has the basic aim of keeping readers informed of the latest research results in the fields of oncology and immunology. As knowledge expands, the scope of the journal has broadened to include more of the progress being made in the areas of biology concerned with biological response modifiers. This helps keep readers up to date on the latest advances in our understanding of tumor-host interactions. The journal publishes short editorials including "position papers," general reviews, original articles, and short communications, providing a forum for the most current experimental and clinical advances in tumor immunology.
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