术前化疗前后激素受体阳性乳腺癌的免疫微环境
The Immune Microenvironment in Hormone Receptor-Positive Breast Cancer Before and After Preoperative Chemotherapy.
作者信息
Waks Adrienne G, Stover Daniel G, Guerriero Jennifer L, Dillon Deborah, Barry William T, Gjini Evisa, Hartl Christina, Lo Wesley, Savoie Jennifer, Brock Jane, Wesolowski Robert, Li Zaibo, Damicis Adrienne, Philips Anne V, Wu Yun, Yang Fei, Sullivan Amy, Danaher Patrick, Brauer Heather Ann, Osmani Wafa, Lipschitz Mikel, Hoadley Katherine A, Goldberg Michael, Perou Charles M, Rodig Scott, Winer Eric P, Krop Ian E, Mittendorf Elizabeth A, Tolaney Sara M
机构信息
Department of Medical Oncology, Dana-Farber Cancer Institute, Boston, Massachusetts.
Division of Medical Oncology, Ohio State University College of Medicine, Columbus, Ohio.
出版信息
Clin Cancer Res. 2019 Aug 1;25(15):4644-4655. doi: 10.1158/1078-0432.CCR-19-0173. Epub 2019 May 6.
PURPOSE
Hormone receptor-positive/HER2-negative (HR/HER2) breast cancer is associated with low levels of stromal tumor-infiltrating lymphocytes (sTIL) and PD-L1, and demonstrates poor responses to checkpoint inhibitor therapy. Evaluating the effect of standard chemotherapy on the immune microenvironment may suggest new opportunities for immunotherapy-based approaches to treating HR/HER2 breast tumors.
EXPERIMENTAL DESIGN
HR/HER2 breast tumors were analyzed before and after neoadjuvant chemotherapy. sTIL were assessed histologically; CD8 cells, CD68 cells, and PD-L1 staining were assessed immunohistochemically; whole transcriptome sequencing and panel RNA expression analysis (NanoString) were performed.
RESULTS
Ninety-six patients were analyzed from two cohorts ( = 55, Dana-Farber cohort; = 41, MD Anderson cohort). sTIL, CD8, and PD-L1 on tumor cells were higher in tumors with basal PAM50 intrinsic subtype. Higher levels of tissue-based lymphocyte (sTIL, CD8, PD-L1) and macrophage (CD68) markers, as well as gene expression markers of lymphocyte or macrophage phenotypes (NanoString or CIBERSORT), correlated with favorable response to neoadjuvant chemotherapy, but not with improved distant metastasis-free survival in these cohorts or a large gene expression dataset ( = 302). In paired pre-/postchemotherapy samples, sTIL and CD8 cells were significantly decreased after treatment, whereas expression analyses (NanoString) demonstrated significant increase of multiple myeloid signatures. Single gene expression implicated increased expression of immunosuppressive (M2-like) macrophage-specific genes after chemotherapy.
CONCLUSIONS
The immune microenvironment of HR/HER2 tumors differs according to tumor biology. This cohort of paired pre-/postchemotherapy samples suggests a critical role for immunosuppressive macrophage expansion in residual disease. The role of macrophages in chemoresistance should be explored, and further evaluation of macrophage-targeting therapy is warranted.
目的
激素受体阳性/人表皮生长因子受体2阴性(HR/HER2)乳腺癌与基质肿瘤浸润淋巴细胞(sTIL)和程序性死亡受体配体1(PD-L1)水平较低相关,并且对检查点抑制剂疗法反应不佳。评估标准化疗对免疫微环境的影响可能为基于免疫疗法的HR/HER2乳腺肿瘤治疗方法带来新机遇。
实验设计
对新辅助化疗前后的HR/HER2乳腺肿瘤进行分析。通过组织学评估sTIL;通过免疫组织化学评估CD8细胞、CD68细胞和PD-L1染色;进行全转录组测序和基因表达分析(NanoString)。
结果
对来自两个队列的96例患者进行了分析(n = 55,达纳-法伯癌症研究所队列;n = 41,MD安德森癌症中心队列)。具有基底样PAM50内在亚型的肿瘤中,肿瘤细胞上的sTIL、CD8和PD-L1水平更高。基于组织的淋巴细胞(sTIL、CD8、PD-L1)和巨噬细胞(CD68)标志物的较高水平,以及淋巴细胞或巨噬细胞表型的基因表达标志物(NanoString或CIBERSORT),与对新辅助化疗的良好反应相关,但与这些队列或一个大型基因表达数据集(n = 302)中无远处转移生存期的改善无关。在化疗前后配对的样本中,治疗后sTIL和CD8细胞显著减少,而表达分析(NanoString)显示多种髓系特征显著增加。单基因表达表明化疗后免疫抑制(M2样)巨噬细胞特异性基因的表达增加。
结论
HR/HER2肿瘤的免疫微环境因肿瘤生物学特性而异。这一化疗前后配对样本队列表明免疫抑制性巨噬细胞扩增在残留疾病中起关键作用。应探索巨噬细胞在化疗耐药中的作用,并且有必要进一步评估针对巨噬细胞的疗法。
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