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肺部免疫微环境中的性别差异与女性患肺癌风险增加有关。

Sex-based differences in the lung immune microenvironment are associated with an increased risk of lung cancer in women.

作者信息

Smith Randall, Gee Kaylan N, Kalvapudi Sukumar, Pachimatla Akhil, Swamidoss Robert, Vedire Yeshwanth, Washington Deschana, Reid Mary, Barbi Joseph, Yendamuri Sai

机构信息

Department of Thoracic Surgery, Roswell Park Comprehensive Cancer Center, Buffalo, NY; Department of Immunology, Roswell Park Comprehensive Cancer Center, Buffalo, NY.

Department of Thoracic Surgery, Roswell Park Comprehensive Cancer Center, Buffalo, NY; Department of Surgery, University of Tennessee Graduate School of Medicine, Knoxville, Tenn.

出版信息

J Thorac Cardiovasc Surg. 2025 Mar;169(3):764-776.e9. doi: 10.1016/j.jtcvs.2024.07.017. Epub 2024 Jul 15.

Abstract

OBJECTIVE

Lung cancer remains a major cause of mortality worldwide, necessitating further understanding of carcinogenesis and its driving factors, including those influenced by sex-dependent variables. We hypothesized that sex-specific lung immune composition may contribute to a greater risk of lung cancer in women.

METHODS

Data from 1056 lung cancer screenings were examined for an association between sex and lung cancer risk using time-to-event analyses. Immune profiling by flow cytometry was performed on male and female lungs of 3 independent mouse models: nontumor bearing, KRAS mutated, and urethane-exposed carcinogenic. A comparable analysis was performed on human bronchoalveolar lavage samples (n = 81) from patients with lung cancer.

RESULTS

Of the high-risk screening cohort examined, 60 patients (5.7%) developed lung cancer during median follow-up of 43.4 months. Multivariable stepwise modeling retained female sex (hazard ratio, 1.56; P < .01) and age (P < .01) as prognostic indicators for lung cancer development. Female lung immune profiles in patients included T-cell phenotypes consistent with exhaustion (eg, higher proportions of PD-1+ Ki67-; P = .02), an expanded pool of regulatory T-cells (P = .03), reduced effector T-cell frequencies (P = .008), and enhancements in suppressive myeloid populations (P = .02) versus male patients, and this is recapitulated in mouse studies.

CONCLUSIONS

Female smokers display higher risk for lung cancer. In murine models and humans, female sex is associated with robust immunosuppression within the lung. Further examination of this link will be important in developing immune-based approaches to lung cancer interception and their optimal application across the sexes.

摘要

目的

肺癌仍是全球主要死因,因此有必要进一步了解其致癌过程及其驱动因素,包括那些受性别相关变量影响的因素。我们推测,性别特异性的肺部免疫组成可能导致女性患肺癌的风险更高。

方法

使用事件发生时间分析方法,对1056例肺癌筛查数据进行分析,以研究性别与肺癌风险之间的关联。通过流式细胞术对3个独立小鼠模型(未患肿瘤、KRAS突变、暴露于氨基甲酸乙酯致癌物)的雄性和雌性肺部进行免疫分析。对81例肺癌患者的人支气管肺泡灌洗样本进行了类似分析。

结果

在接受检查的高危筛查队列中,60例患者(5.7%)在43.4个月的中位随访期内患上肺癌。多变量逐步建模保留了女性(风险比,1.56;P <.01)和年龄(P <.01)作为肺癌发生的预后指标。与男性患者相比,女性患者肺部免疫图谱包括与耗竭一致的T细胞表型(例如,PD-1+Ki67-比例更高;P =.02)、调节性T细胞池扩大(P =.03)、效应T细胞频率降低(P =.008)以及抑制性髓系细胞群增加(P =.02),小鼠研究也证实了这一点。

结论

女性吸烟者患肺癌的风险更高。在小鼠模型和人类中,女性与肺部强大的免疫抑制有关。进一步研究这种联系对于开发基于免疫的肺癌拦截方法及其在不同性别中的最佳应用非常重要。

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