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肌上皮钙调蛋白-1缺失可作为高危导管原位癌的特征,这些病例还可进一步根据 T 细胞组成进行分层。

Loss of myoepithelial calponin-1 characterizes high-risk ductal carcinoma in situ cases, which are further stratified by T cell composition.

机构信息

Department of Cell, Developmental, and Cancer Biology, Oregon Health and Science University, Portland, Oregon.

Cancer Prevention and Control, Knight Cancer Institute, Oregon Health and Science University, Portland, Oregon.

出版信息

Mol Carcinog. 2020 Jul;59(7):701-712. doi: 10.1002/mc.23171. Epub 2020 Mar 5.

DOI:10.1002/mc.23171
PMID:32134153
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7317523/
Abstract

A hallmark of ductal carcinoma in situ (DCIS) progression is a loss of the surrounding ductal myoepithelium. However, whether compromise in myoepithelial differentiation, rather than overt cellular loss, can be used to predict the risk of DCIS progression is unknown. Here we address this question utilizing pure and mixed DCIS cases (N = 30) as surrogates for DCIS at low and high risk for progression, respectively. We used multiplex immunohistochemical staining to evaluate the relationship between myoepithelial cell differentiation and lymphoid immune cell types associated with poor prognostic DCIS. Our results show that myoepithelial calponin-1 discriminates between pure and mixed DCIS lesions better than histological subtype, presence of necrosis, or nuclear grade. Additionally, focal loss of myoepithelial cells associated with increased PD-1+CD8+ T cells, which suggests a link between the myoepithelium and immune surveillance. To identify associations between calponin-1 expression and immune response, we performed unsupervised hierarchical clustering of myoepithelial and immune cell biomarkers on 219 DCIS lesions from 30 cases. Notably, the majority of pure (low-risk) DCIS lesions clustered in a high calponin-1, T cell low group, whereas the majority of mixed (high-risk) DCIS lesions clustered in a low calponin-1, T cell high group, specifically with CD8+ and PD-1+CD8+ T cells. However, a subset of pure DCIS lesions had a similar calponin-1 and immune signature as the majority of mixed DCIS lesions, which have low calponin-1 and T cell enrichment-raising the possibility that these pure DCIS lesions might be at a high risk for progression.

摘要

导管原位癌 (DCIS) 进展的一个标志是周围导管的肌上皮丧失。然而,肌上皮分化的损害,而不是明显的细胞丢失,是否可以用来预测 DCIS 进展的风险尚不清楚。在这里,我们利用纯和混合 DCIS 病例(N=30)分别作为低风险和高风险进展的 DCIS 替代物来解决这个问题。我们使用多重免疫组织化学染色来评估肌上皮细胞分化与与预后不良的 DCIS 相关的淋巴免疫细胞类型之间的关系。我们的结果表明,肌上皮细胞 calponin-1 比组织学亚型、坏死存在或核级更好地区分纯和混合 DCIS 病变。此外,与 PD-1+CD8+T 细胞增加相关的肌上皮细胞局灶性丧失表明肌上皮细胞与免疫监视之间存在联系。为了确定 calponin-1 表达与免疫反应之间的关联,我们对 30 例 219 例 DCIS 病变的肌上皮细胞和免疫细胞生物标志物进行了无监督层次聚类分析。值得注意的是,大多数纯(低风险)DCIS 病变聚集在高 calponin-1、T 细胞低的组中,而大多数混合(高风险)DCIS 病变聚集在低 calponin-1、T 细胞高的组中,特别是 CD8+和 PD-1+CD8+T 细胞。然而,一部分纯 DCIS 病变具有与大多数混合 DCIS 病变相似的 calponin-1 和免疫特征,这些病变具有低 calponin-1 和 T 细胞富集,这增加了这些纯 DCIS 病变可能具有高进展风险的可能性。

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