High tumour-infiltrating lymphocytes correlate with distinct gene expression profile and favourable survival in single hormone receptor-positive breast cancer

Aleksandra Ciarka, M. Kunc, M. Popęda, A. Łacko, Barbara Radecka, Marcin Braun, Joanna Pikiel, M. Litwiniuk, Katarzyna Pogoda, Ewa Iżycka-Świeszewska, Anna Zeller, Magdalena Niemira, R. Pęksa, Wojciech Biernat, Elżbieta Senkus
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Abstract

Introduction This study aimed to evaluate the impact of tumour-infiltrating lymphocytes (TILs) on the expression of immune-related genes and prognosis in single hormone receptor-positive breast cancer. Material and methods: Tumour-infiltrating lymphocytes were analysed according to the guidelines of the International TILs Working Group in a cohort of 206 patients with single hormone receptor-positive breast cancer. Of these, 44.7% were classified as ER+/PgR–/HER2–, 18.4% as ER+/PgR–/HER2+, 26.2% as ER–/PgR+/HER2–, and 10.7% as ER–/PgR+/HER2+. Moreover, in 52 samples the analysis of gene expression profiling was performed using nCounter technology. Results Most cases (74.3%) showed at least 1% of stromal TILs, with a median of 4%, mean of 16.3%, and interquartile range of 0–20%. ER–/PgR+ tumours displayed significantly higher TILs density than ER+/PgR– cases (p < 0.001, Wilcoxon test), regardless of HER2 status. The abundance of TILs was positively associated with ER–/PgR+ phenotype, higher Ki-67, and higher grade, but not with age, tumour size, or regional and distant metastases at diagnosis. Additionally, in ER+/PgR– subgroup higher TILs were associated with HER2-positive status. Stromal TILs > 5% were associated with better survival in the whole group, but this effect was less prominent in ER–/PgR+ patients. We identified 50 differentially expressed genes (DEGs) between single hormone receptor-positive breast tumours with high and low TILs, including 39 up-regulated and 11 down-regulated genes in the high TILs group. Conclusions The up-regulated expression of immune-related genes was consistent also among separately analysed single hormone receptor-positive groups (ER+/PgR– and ER–/PgR+).
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高肿瘤浸润淋巴细胞与单个激素受体阳性乳腺癌独特的基因表达谱和良好的生存率有关
导言:本研究旨在评估肿瘤浸润淋巴细胞(TILs)对单个激素受体阳性乳腺癌免疫相关基因表达和预后的影响。材料与方法根据国际TILs工作组的指导方针,对206名单一激素受体阳性乳腺癌患者的肿瘤浸润淋巴细胞进行了分析。其中,44.7%被归类为ER+/PgR-/HER2-,18.4%被归类为ER+/PgR-/HER2+,26.2%被归类为ER-/PgR+/HER2-,10.7%被归类为ER-/PgR+/HER2+。此外,还利用 nCounter 技术对 52 个样本进行了基因表达谱分析。结果 大多数病例(74.3%)显示至少有1%的基质TIL,中位数为4%,平均值为16.3%,四分位距范围为0-20%。ER-/PgR+肿瘤的TILs密度明显高于ER+/PgR-病例(p < 0.001,Wilcoxon检验),与HER2状态无关。TILs的丰富程度与ER-/PgR+表型、较高的Ki-67和较高的分级呈正相关,但与年龄、肿瘤大小或诊断时的区域和远处转移无关。此外,在ER+/PgR-亚组中,较高的TIL与HER2阳性状态相关。基质TILs>5%与全组患者生存率提高有关,但这一效应在ER-/PgR+患者中不太明显。我们在TILs高和TILs低的单个激素受体阳性乳腺肿瘤之间发现了50个差异表达基因(DEGs),其中高TILs组有39个基因上调,11个基因下调。结论 在单独分析的单一激素受体阳性组(ER+/PgR- 和 ER-/PgR+)中,免疫相关基因的上调表达也是一致的。
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