USH2A突变和特异性驱动突变亚型与免疫检查点抑制剂治疗肺癌的临床疗效相关。

Journal of Zhejiang University. Science. B Pub Date : 2023-02-15 DOI:10.1631/jzus.B2200292

Dexin Yang, Yuqin Feng, Haohua Lu, Kelie Chen, Jinming Xu, Peiwei Li, Tianru Wang, Dajing Xia, Yihua Wu

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引用次数: 0

摘要

本研究旨在通过在截至2021年5月31日的电子数据库中进行系统文献检索，确定与免疫检查点抑制剂(ICIs)疗效相关的基因组变异亚型。主要结局包括总生存期(OS)、无进展生存期(PFS)、客观缓解率(ORR)和持久临床获益(DCB)与肿瘤基因组特征相关。14项研究共纳入了1546名有基因组变异数据的肺癌患者。Kirsten大鼠肉瘤病毒癌基因同源物G12C (KRASG12C)突变联合肿瘤蛋白P53 (TP53)突变揭示了ICI治疗对这些患者的良好疗效。此外，表皮生长因子受体(EGFR)经典激活突变(包括EGFRL858R和EGFRΔ19)的患者在OS中表现出更差的ICIs结局(校正风险比(HR)， 1.40;95%置信区间(CI)， 1.01‍-‍1.95;P=0.0411)和PFS(调整后HR, 1.98;95% ci, 1.49‍-‍2.63;与没有EGFRT790M的经典激活突变相比，PEGFRT790M在OS中没有差异(调整HR, 0.96;95% ci, 0.48‍-‍1.94;P=0.9157)或PFS(调整HR, 0.72;95% ci, 0.39‍-‍1.35;P = 0.3050)。值得注意的是，对于携带Usher综合征2a型(USH2A)错义突变的患者，在OS中观察到相应更好的结果(调整HR, 0.52;95% ci, 0.32‍-‍0.82;P=0.0077)， PFS(调整HR, 0.51;95% ci, 0.38‍-‍0.69;PPPUSH2A错意突变和krasg12c突变联合TP53突变与更好的疗效和生存结果相关，但EGFR经典突变无论与EGFRT790M联合，在肺癌患者的ICI治疗中表现出相反的作用。我们的发现可能指导临床选择有效免疫治疗的精确靶点。

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USH2A mutation and specific driver mutation subtypes are associated with clinical efficacy of immune checkpoint inhibitors in lung cancer.

This study aimed to identify subtypes of genomic variants associated with the efficacy of immune checkpoint inhibitors (ICIs) by conducting systematic literature search in electronic databases up to May 31, 2021. The main outcomes including overall survival (OS), progression-free survival (PFS), objective response rate (ORR), and durable clinical benefit (DCB) were correlated with tumor genomic features. A total of 1546 lung cancer patients with available genomic variation data were included from 14 studies. The Kirsten rat sarcoma viral oncogene homolog G12C (KRAS^G12C) mutation combined with tumor protein P53 (TP53) mutation revealed the promising efficacy of ICI therapy in these patients. Furthermore, patients with epidermal growth factor receptor (EGFR) classical activating mutations (including EGFR^L858R and EGFR^Δ19) exhibited worse outcomes to ICIs in OS (adjusted hazard ratio (HR), 1.40; 95% confidence interval (CI), 1.01‍‒‍1.95; P=0.0411) and PFS (adjusted HR, 1.98; 95% CI, 1.49‍‒‍2.63; P<0.0001), while classical activating mutations with EGFR^T790M showed no difference compared to classical activating mutations without EGFR^T790M in OS (adjusted HR, 0.96; 95% CI, 0.48‍‒‍1.94; P=0.9157) or PFS (adjusted HR, 0.72; 95% CI, 0.39‍‒‍1.35; P=0.3050). Of note, for patients harboring the Usher syndrome type-2A(USH2A) missense mutation, correspondingly better outcomes were observed in OS (adjusted HR, 0.52; 95% CI, 0.32‍‒‍0.82; P=0.0077), PFS (adjusted HR, 0.51; 95% CI, 0.38‍‒‍0.69; P<0.0001), DCB (adjusted odds ratio (OR), 4.74; 95% CI, 2.75‍‒‍8.17; P<0.0001), and ORR (adjusted OR, 3.45; 95% CI, 1.88‍‒‍6.33; P<0.0001). Our findings indicated that, USH2A missense mutations and the KRAS^G12Cmutation combined with TP53 mutation were associated with better efficacy and survival outcomes, but EGFR classical mutations irrespective of combination with EGFR^T790M showed the opposite role in the ICI therapy among lung cancer patients. Our findings might guide the selection of precise targets for effective immunotherapy in the clinic.

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Journal of Zhejiang University. Science. B

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