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高级别原发性乳腺癌病变中HLA I类抗原及抗原加工相关转运体(TAP1和TAP2)下调

HLA class I antigen and transporter associated with antigen processing (TAP1 and TAP2) down-regulation in high-grade primary breast carcinoma lesions.

作者信息

Vitale M, Rezzani R, Rodella L, Zauli G, Grigolato P, Cadei M, Hicklin D J, Ferrone S

机构信息

Department of Biomedical Sciences and Biotechnologies, University of Brescia, Italy.

出版信息

Cancer Res. 1998 Feb 15;58(4):737-42.

PMID:9485029
Abstract

Five specimens of normal mammary tissue and 53 primary breast carcinoma lesions were tested for expression of HLA antigens and components of the antigen-processing machinery by immunohistochemical staining. The expression of transporter associated with antigen processing (TAP) 1, TAP2, and HLA class I antigens in breast carcinoma lesions was significantly associated with tumor grading. Like normal mammary tissue, the 16 low-grade (G1) breast carcinoma lesions showed strong staining for TAP1, TAP2, and HLA class I antigens. In contrast, only 12 (32%) of 37 high-grade (G2 and G3) breast carcinoma lesions displayed the normal staining pattern. In 14 (38%) of 37 high-grade lesions, HLA class I antigen down-regulation was observed without loss of low molecular mass polypeptide and/or TAP staining. Congruent down-regulation of HLA class I antigen and TAP1 or TAP2 was found in 8 (22%) of 37 high-grade lesions. Complete loss of HLA class I antigens, TAP1, and TAP2 was observed in 3 (8%) of 37 high-grade lesions. No lesion was negative for TAP1 and/or TAP2 staining while positive for HLA class I antigen staining. These data demonstrate an association of HLA class I antigen and TAP down-regulation with tumor progression in breast carcinoma. This association suggests that loss of HLA and/or TAP may represent an escape from the host's immune pressure or may reflect the accumulation of abnormalities associated with neoplastic progression. This accumulation of defects in antigen processing and presentation may in turn be responsible for reduced recognition of malignant cells by putative clinically relevant tumor-specific T cells.

摘要

通过免疫组织化学染色检测了5例正常乳腺组织标本和53例原发性乳腺癌病变组织中HLA抗原及抗原加工机制成分的表达情况。乳腺癌病变组织中抗原加工相关转运体(TAP)1、TAP2和HLAⅠ类抗原的表达与肿瘤分级显著相关。与正常乳腺组织一样,16例低级别(G1)乳腺癌病变组织中TAP1、TAP2和HLAⅠ类抗原呈强染色。相比之下,37例高级别(G2和G3)乳腺癌病变组织中只有12例(32%)呈现正常染色模式。在37例高级别病变组织中的14例(38%)中,观察到HLAⅠ类抗原下调,而低分子量多肽和/或TAP染色未缺失。在37例高级别病变组织中的8例(22%)中发现HLAⅠ类抗原与TAP1或TAP2一致下调。在37例高级别病变组织中的3例(8%)中观察到HLAⅠ类抗原、TAP1和TAP2完全缺失。没有病变组织TAP1和/或TAP2染色阴性而HLAⅠ类抗原染色阳性。这些数据表明HLAⅠ类抗原和TAP下调与乳腺癌肿瘤进展相关。这种关联表明HLA和/或TAP的缺失可能代表逃避宿主免疫压力,或可能反映与肿瘤进展相关的异常积累。抗原加工和呈递中这些缺陷的积累可能反过来导致假定的临床相关肿瘤特异性T细胞对恶性细胞的识别减少。

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