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癌症诱导的神经损伤促进对抗PD-1疗法的耐药性。

Cancer-induced nerve injury promotes resistance to anti-PD-1 therapy.

作者信息

Baruch Erez N, Gleber-Netto Frederico O, Nagarajan Priyadharsini, Rao Xiayu, Akhter Shamima, Eichwald Tuany, Xie Tongxin, Balood Mohammad, Adewale Adebayo, Naara Shorook, Sathishkumar Hinduja N, Islam Shajedul, McCarthy William, Mattson Brandi J, Ferrarotto Renata, Wong Michael K, Davies Michael A, Jindal Sonali, Basu Sreyashi, Roversi Karine, Nikpoor Amin Reza, Ahmadi Maryam, Ahmadi Ali, Harwood Catherine, Leigh Irene, Gong Dennis, Tallón de Lara Paulino, Tao Derrick L, Davidson Tara M, Ajami Nadim J, Futreal Andrew, Rai Kunal, Kochat Veena, Castillo Micah, Gunaratne Preethi, Goepfert Ryan P, Hernandez Sharia D, Khushalani Nikhil I, Wang Jing, Watowich Stephanie S, Calin George A, Migden Michael R, Yuan Mona, Liu Naijiang, Ye Yi, Hwang William L, Vermeer Paola D, D'Silva Nisha J, Bunimovich Yuri L, Yaniv Dan, Burks Jared K, Gomez Javier, Dougherty Patrick M, Tsai Kenneth Y, Allison James P, Sharma Padmanee, Wargo Jennifer A, Myers Jeffrey N, Talbot Sebastien, Gross Neil D, Amit Moran

机构信息

Division of Cancer Medicine, Hematology and Oncology Fellowship program, The University of Texas MD Anderson Cancer Center, Houston, TX, USA.

Platform for Innovative Microbiome and Translational Research, Department of Genomic Medicine, The University of Texas MD Anderson Cancer Center, Houston, TX, USA.

出版信息

Nature. 2025 Aug 20. doi: 10.1038/s41586-025-09370-8.

Abstract

Perineural invasion (PNI) is a well-established factor of poor prognosis in multiple cancer types, yet its mechanism remains unclear. Here we provide clinical and mechanistic insights into the role of PNI and cancer-induced nerve injury (CINI) in resistance to anti-PD-1 therapy. Our study demonstrates that PNI and CINI of tumour-associated nerves are associated with poor response to anti-PD-1 therapy among patients with cutaneous squamous cell carcinoma, melanoma and gastric cancer. Electron microscopy and electrical conduction analyses reveal that cancer cells degrade the nerve fibre myelin sheets. The injured neurons respond by autonomously initiating IL-6- and type I interferon-mediated inflammation to promote nerve healing and regeneration. As the tumour grows, the CINI burden increases, and its associated inflammation becomes chronic and skews the general immune tone within the tumour microenvironment into a suppressive and exhaustive state. The CINI-driven anti-PD-1 resistance can be reversed by targeting multiple steps in the CINI signalling process: denervating the tumour, conditional knockout of the transcription factor mediating the injury signal within neurons (Atf3), knockout of interferon-α receptor signalling (Ifnar1) or by combining anti-PD-1 and anti-IL-6-receptor blockade. Our findings demonstrate the direct immunoregulatory roles of CINI and its therapeutic potential.

摘要

神经周围浸润(PNI)是多种癌症类型中公认的预后不良因素,但其机制仍不清楚。在此,我们提供了关于PNI和癌症诱导的神经损伤(CINI)在抗PD-1治疗耐药中的作用的临床和机制见解。我们的研究表明,肿瘤相关神经的PNI和CINI与皮肤鳞状细胞癌、黑色素瘤和胃癌患者对抗PD-1治疗的不良反应相关。电子显微镜和电传导分析显示,癌细胞会降解神经纤维髓鞘。受损神经元通过自主启动白细胞介素-6和I型干扰素介导的炎症反应来促进神经愈合和再生。随着肿瘤生长,CINI负担增加,其相关炎症变得慢性化,并使肿瘤微环境中的整体免疫状态偏向抑制和耗竭状态。通过靶向CINI信号传导过程中的多个步骤,可以逆转CINI驱动的抗PD-1耐药性:使肿瘤去神经支配、条件性敲除介导神经元损伤信号的转录因子(Atf3)、敲除干扰素-α受体信号(Ifnar1)或联合抗PD-1和抗白细胞介素-6受体阻断。我们的研究结果证明了CINI的直接免疫调节作用及其治疗潜力。

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