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乳腺癌中 HLA I 类分子的改变与染色体 6 和 15 杂合性丢失的高频率相关。

HLA class I alterations in breast carcinoma are associated with a high frequency of the loss of heterozygosity at chromosomes 6 and 15.

机构信息

Servicio de Radiología, UGC de Radiología, Hospital Universitario Virgen de las Nieves, Granada, Spain.

Servicio de Análisis Clínicos e Inmunología, UGC de Laboratorio Clinico, Hospital Universitario Virgen de las Nieves, Granada, Spain.

出版信息

Immunogenetics. 2018 Nov;70(10):647-659. doi: 10.1007/s00251-018-1074-2. Epub 2018 Aug 25.

Abstract

HLA class I (HLA-I) molecules play a crucial role in the presentation of tumor antigenic peptides to CD8+ T cells. Tumor HLA-I loss provides a route of immune escape from T cell-mediated killing. We analyzed HLA-I expression in 98 cryopreserved breast cancer tissues using a broad panel of anti-HLA-I antibodies. Genomic HLA-I typing was performed using DNA obtained from autologous normal breast tissue. Analysis of the loss of heterozygosity (LOH) in the HLA-I region of chromosome 6 (LOH-6) and in the β2-microglobulin (B2M) region of chromosome 15 (LOH-15) was done by microsatellite amplification of DNA isolated from microdissected tumor areas. B2M gene sequencing was done using this DNA form HLA-I-negative tumors. Immunohistological analysis revealed various types of HLA-I alterations in 79 tumors (81%), including total HLA-I loss in 53 cases (54%) and partial loss in 16 samples (14%). In 19 cases (19%), HLA-I expression was positive. Using microsatellite analysis, we detected LOH in 36 cases out of 92 evaluated (39%), including 15 samples with only LOH-6, 14 with LOH-15, and seven tumors with LOH-6 and LOH-15 at the same time. Remarkably, we detected LOH-6 in eight tumors with positive HLA-I immunolabeling. We did not find any B2M mutations in HLA-I-negative breast tumors. In conclusion, LOH at chromosomes 6 and 15 has a high incidence in breast cancer and occurs in tumors with different HLA-I immunophenotypes. This common molecular mechanism of HLA-I alterations may reduce the ability of cytotoxic T lymphocytes  to kill tumor cells and negatively influence the clinical success of cancer immunotherapy.

摘要

HLA-I 类分子在肿瘤抗原肽向 CD8+T 细胞的呈递中发挥着关键作用。肿瘤 HLA-I 缺失为 T 细胞介导的杀伤提供了免疫逃逸途径。我们使用广泛的抗 HLA-I 抗体分析了 98 例冷冻乳腺癌组织中的 HLA-I 表达。使用从自体正常乳腺组织中获得的 DNA 进行 HLA-I 基因分型。通过对 6 号染色体 HLA-I 区(LOH-6)和 15 号染色体β2-微球蛋白(B2M)区(LOH-15)的杂合性丢失(LOH)进行微卫星扩增,对 DNA 进行分析从微切割的肿瘤区域中分离。使用来自 HLA-I 阴性肿瘤的这种 DNA 形式进行 B2M 基因测序。免疫组织化学分析显示 79 例肿瘤(81%)存在各种类型的 HLA-I 改变,包括 53 例(54%)完全 HLA-I 缺失和 16 例(14%)部分缺失。在 19 例(19%)中,HLA-I 表达为阳性。使用微卫星分析,我们在 92 个评估样本中检测到 36 例(39%)存在 LOH,包括 15 例仅存在 LOH-6,14 例存在 LOH-15,7 例同时存在 LOH-6 和 LOH-15。值得注意的是,我们在 8 例 HLA-I 免疫标记阳性的肿瘤中检测到 LOH-6。我们在 HLA-I 阴性乳腺癌肿瘤中未发现任何 B2M 突变。总之,染色体 6 和 15 上的 LOH 在乳腺癌中发生率较高,并且发生在具有不同 HLA-I 免疫表型的肿瘤中。这种 HLA-I 改变的常见分子机制可能会降低细胞毒性 T 淋巴细胞杀伤肿瘤细胞的能力,并对癌症免疫治疗的临床成功产生负面影响。

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