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循环中性粒细胞和肿瘤相关髓系细胞是局部晚期宫颈癌放化疗反应的有力生物标志物。

Circulating neutrophils and tumor-associated myeloid cells function as a powerful biomarker for response to chemoradiation in locally advanced cervical cancer.

作者信息

Gjyshi Olsi, Grippin Adam, Andring Lauren, Jhingran Anuja, Lin Lilie L, Bronk Julianna, Eifel Patricia J, Joyner Melissa M, Sastry Jagannadha K, Yoshida-Court Kyoko, Solley Travis N, Napravnik Tatiana Cisneros, O'Hara Madison P, Hegde Venkatesh L, Colbert Lauren E, Klopp Ann H

机构信息

Department of Radiation Oncology, Saint Elizabeth Cancer Center, Edgewood, KY, United States.

Department of Radiation Oncology, The University of Texas MD Anderson Cancer Center, Houston, Texas Department of Medicine, United States.

出版信息

Clin Transl Radiat Oncol. 2023 Jan 11;39:100578. doi: 10.1016/j.ctro.2023.100578. eCollection 2023 Mar.

Abstract

PURPOSE

The immune system's role in mediating the cytotoxic effects of chemoradiotherapy remains not completely understood. The integration of immunotherapies into treatment will require insight into features and timing of the immune microenvironment associated with treatment response. Here, we investigated the role of circulating neutrophils and tumor-associated myeloid cells (TSAMs) as potential agents and biomarkers for disease-related outcomes in locally advanced cervical cancer (LACC).

MATERIAL AND METHODS

Hematologic parameters for two LACC patient cohorts, a retrospective clinical and a prospective translational cohort, were obtained at baseline, weekly during chemoradiotherapy for the retrospective cohort, biweekly during chemoradiotherapy for the prospective cohort, and at the first follow-up visit for both cohorts (mean 14.7 weeks, range 8.1-25.1 weeks for the prospective cohort and 5.3 weeks with a range of 2.7-9.0 weeks for the retrospective cohort). In both cohorts, baseline as well as mean and lowest on-treatment values for platelets, hemoglobin, absolute neutrophil count (ANC), and absolute lymphocyte count (ALC) were analyzed for correlations with disease-related outcomes. In the prospective cohort, circulating myeloid cells were isolated from peripheral blood mononuclear cells (PBMCs), and TSAMs were isolated from tumor tissue via a novel serial cytobrush sampling assay. The samples were analyzed by flow cytometry.

RESULTS

In both cohorts, the only hematologic parameter significantly associated with survival was elevated on-treatment mean ANC (mANC), which was associated with lower local failure-free and overall survival rates in the retrospective and prospective cohorts, respectively. mANC was not associated with a difference in distant metastases. CD11bCD11c TSAMs, which act as a surrogate marker for intratumoral neutrophils, steadily decreased during the course of chemoRT and nadier'd at week 5 of treatment. Conversely, circulating myeloid cells identified from PBMCs steadily increased through week 5 of treatment. Regression analysis confirmed an inverse relationship between circulating myeloid cells and TSAMs at this time point.

CONCLUSIONS

These findings identify on-treatment mean neutrophil count as a predictor of disease-related outcomes, suggest that neutrophils contribute to chemoradiation treatment resistance, and demonstrate the importance of techniques to measure intratumoral immune activity.

摘要

目的

免疫系统在介导放化疗的细胞毒性作用中所扮演的角色仍未完全明确。将免疫疗法整合到治疗中需要深入了解与治疗反应相关的免疫微环境特征及时机。在此,我们研究了循环中性粒细胞和肿瘤相关髓样细胞(TSAMs)作为局部晚期宫颈癌(LACC)疾病相关结局的潜在介质和生物标志物的作用。

材料与方法

获取了两个LACC患者队列的血液学参数,一个是回顾性临床队列,另一个是前瞻性转化队列。回顾性队列在基线时、放化疗期间每周获取一次,前瞻性队列在放化疗期间每两周获取一次,两个队列均在首次随访时获取(前瞻性队列平均14.7周,范围8.1 - 25.1周;回顾性队列5.3周,范围2.7 - 9.0周)。在两个队列中,分析血小板、血红蛋白、绝对中性粒细胞计数(ANC)和绝对淋巴细胞计数(ALC)的基线值以及治疗期间的平均值和最低值与疾病相关结局的相关性。在前瞻性队列中,从外周血单核细胞(PBMCs)中分离循环髓样细胞,通过一种新型的连续细胞刷采样测定法从肿瘤组织中分离TSAMs。样本通过流式细胞术进行分析。

结果

在两个队列中,唯一与生存显著相关的血液学参数是治疗期间平均ANC(mANC)升高,在回顾性队列和前瞻性队列中,mANC分别与较低的局部无复发生存率和总生存率相关。mANC与远处转移的差异无关。作为肿瘤内中性粒细胞替代标志物的CD11bCD11c TSAMs在放化疗过程中稳步下降,并在治疗第5周达到最低点。相反,从PBMCs中鉴定出的循环髓样细胞在治疗第5周前稳步增加。回归分析证实了此时循环髓样细胞与TSAMs之间存在负相关关系。

结论

这些发现确定治疗期间平均中性粒细胞计数是疾病相关结局的预测指标,表明中性粒细胞导致放化疗耐药,并证明了测量肿瘤内免疫活性技术的重要性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5723/10014332/682556f6fd13/gr1.jpg

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