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新家族史评分与接受新辅助铂类化疗的乳腺癌患者的病理完全缓解、安全性及生存结局的关联:两项前瞻性试验的探索性分析

Association of Neo-Family History Score with pathological complete response, safety, and survival outcomes in patients with breast cancer receiving neoadjuvant platinum-based chemotherapy: An exploratory analysis of two prospective trials.

作者信息

Xu Yaqian, Lin Yanping, Wang Yaohui, Zhou Liheng, Xu Shuguang, Wu Yifan, Peng Jing, Zhang Jie, Yin Wenjin, Lu Jinsong

机构信息

Department of Breast Surgery, Renji Hospital, School of Medicine, Shanghai Jiao Tong University, Shanghai 200127, People's Republic of China.

出版信息

EClinicalMedicine. 2021 Jul 17;38:101031. doi: 10.1016/j.eclinm.2021.101031. eCollection 2021 Aug.

Abstract

BACKGROUND

Homologous recombination deficiency is associated with platinum-based chemosensitivity, whereas few studies reported the predictive value of family history of cancer for breast cancer in the neoadjuvant setting. This study aimed to construct a novel family history scoring system and to explore its association with clinical outcomes for patients with breast cancer receiving neoadjuvant platinum-based chemotherapy.

METHODS

This study included 262 patients with locally advanced breast cancer enrolled in the SHPD001 and SHPD002 trials from October 2013 to June 2018. The Neo-Family History Score (NeoFHS) was calculated according to cancer type, age at diagnosis, kinship, and number of affected relatives.

FINDINGS

Clinical tumor stage (p=0·048), estrogen receptor status (p=0·001), progesterone receptor status (p=0·036), human epidermal growth factor receptor 2 status (p=0·013), and molecular subtype (p=0·016) were significantly related to NeoFHS. NeoFHS could serve as an independent predictive factor of pathological complete response (pCR) (OR=2·262, 95% CI 1·159-4·414, p=0·017) and an independent prognostic factor of relapse-free survival (adjusted HR=0·305, 95% CI 0·102-0·910, p=0·033). Alopecia (p=0·001), nausea (p=0·001), peripheral neuropathy (p=0·018), diarrhea (p=0·026), constipation (p=0·037) of any grade and leukopenia of grade 3 or greater (p=0·005) were more common in patients with higher NeoFHS.

INTERPRETATION

NeoFHS is a practical and effective biomarker for predicting not only pCR and survival outcomes but also chemotherapy-induced adverse events for neoadjuvant platinum-based chemotherapy in breast cancer. It may help screen candidate responders and guide safety managements.

FUNDING

Shanghai Natural Science Foundation [grant number 19ZR1431100], Clinical Research Plan of Shanghai Hospital Development Center [grant numbers SHDC2020CR3003A, 16CR3065B, and 12016231], Shanghai "Rising Stars of Medical Talent" Youth Development Program for Youth Medical Talents - Specialist Program [grant number 2018-15], Shanghai "Rising Stars of Medical Talent" Youth Development Program for Outstanding Youth Medical Talents [grant number 2018-16], Shanghai Collaborative Innovation Center for Translational Medicine [grant number TM201908], Multidisciplinary Cross Research Foundation of Shanghai Jiao Tong University [grant numbers YG2017QN49, ZH2018QNA42, and YG2019QNA28], Nurturing Fund of Renji Hospital [grant numbers PYMDT-002, PY2018-IIC-01, PY2018-III-15, and PYIII20-09], Science and Technology Commission of Shanghai Municipality [grant numbers 20DZ2201600 and 15JC1402700], and Shanghai Municipal Key Clinical Specialty.

摘要

背景

同源重组缺陷与铂类化疗敏感性相关,而在新辅助治疗背景下,很少有研究报道癌症家族史对乳腺癌的预测价值。本研究旨在构建一种新的家族史评分系统,并探讨其与接受新辅助铂类化疗的乳腺癌患者临床结局的关联。

方法

本研究纳入了2013年10月至2018年6月期间参加SHPD001和SHPD002试验的262例局部晚期乳腺癌患者。根据癌症类型、诊断年龄、亲属关系和受影响亲属数量计算新辅助家族史评分(NeoFHS)。

研究结果

临床肿瘤分期(p=0.048)、雌激素受体状态(p=0.001)、孕激素受体状态(p=0.036)、人表皮生长因子受体2状态(p=0.013)和分子亚型(p=0.016)与NeoFHS显著相关。NeoFHS可作为病理完全缓解(pCR)的独立预测因素(OR=2.262,95%CI 1.159-4.414,p=0.017)和无复发生存的独立预后因素(调整后HR=0.305,95%CI 0.102-0.910,p=0.033)。NeoFHS较高的患者中,任何级别的脱发(p=0.001)、恶心(p=0.001)、周围神经病变(p=0.018)、腹泻(p=0.026)、便秘(p=0.037)以及3级或更高级别的白细胞减少(p=0.005)更为常见。

解读

NeoFHS是一种实用且有效的生物标志物,不仅可预测乳腺癌新辅助铂类化疗的pCR和生存结局,还可预测化疗引起的不良事件。它可能有助于筛选候选反应者并指导安全管理。

资助

上海市自然科学基金[项目编号19ZR143110]、上海市医院发展中心临床研究计划[项目编号SHDC2020CR3003A、16CR3065B和12016231]、上海市“医苑新星”青年医学人才培养计划-专科医师培养项目[项目编号2018-15]、上海市“医苑新星”优秀青年医学人才培养计划[项目编号2018-16]、上海市转化医学协同创新中心[项目编号TM201908]、上海交通大学多学科交叉研究基金[项目编号YG2017QN49、ZH2018QNA42和YG2019QNA28]、仁济医院培育基金[项目编号PYMDT-002、PY2018-IIC-01、PY2018-III-15和PYIII20-09]、上海市科学技术委员会[项目编号20DZ2201600和15JC1402700]以及上海市重点临床专科。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4078/8318862/04381683b5ac/gr1.jpg

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