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Tumor antigens and antigen-presenting capacity in breast cancer.

机译:乳腺癌中的肿瘤抗原和抗原呈递能力。

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AIMS: Cancer cells frequently express antigens capable of being recognized by the host immune system; however, any resultant immune response is often ineffective. This may be related in part to tumor-induced defects in antigen presentation. We screened for dendritic cell infiltration, tumor MHC II expression and associated lymphocytic reaction in the context of three established breast tumor antigens. METHODS: Forty primary breast tumors were evaluated by immunohistochemical techniques for expression of her2eu, p53, and MUC1 and MHC class II molecules. Twenty-five samples were further analyzed for p53 mutations by PCR-SSCP analysis and DNA sequencing. The phenotype of tumor-infiltrating inflammatory cells was evaluated using the following markers: CD1a, MHC Class II, CD3, CD45, and CD45RO. RESULTS: Tumors with p53 mutations and overexpression, but not her2eu or MUC1 overexpressing tumors, more frequently harbored marked CD1a+ dendritic cell infiltrates. An overall correlation between CD1a+ cell infiltrates and HLA class II expression on tumor cells (p = 0.0008) was also observed and these tumors had greater CD45RO+ lymphocytic infiltrates. CONCLUSIONS: In breast cancer, p53 mutations may present a more visible signal to the immune system and hence provide a better target for immunotherapy. Infiltrating CD1a positive cells are associated with a more dense tumor lymphocytic infiltrate and tumor cell expression of MHC II molecules.
机译:目的:癌细胞经常表达能够被宿主免疫系统识别的抗原。但是,任何由此产生的免疫反应通常都是无效的。这可能部分与肿瘤诱导的抗原呈递缺陷有关。我们筛选了树突状细胞浸润,肿瘤MHC II表达和相关的三种已确定的乳腺肿瘤抗原的背景下的淋巴细胞反应。方法:通过免疫组织化学技术评估了40例原发性乳腺肿瘤中her2 / neu,p53,MUC1和MHC II类分子的表达。通过PCR-SSCP分析和DNA测序进一步分析了25个样品的p53突变。使用以下标志物评估肿瘤浸润性炎症细胞的表型:CD1a,II类MHC,CD3,CD45和CD45RO。结果:具有p53突变和过度表达但不是her2 / neu或MUC1过度表达的肿瘤更常带有明显的CD1a +树突状细胞浸润。还观察到CD1a +细胞浸润与肿瘤细胞上HLA II类表达之间的总体相关性(p = 0.0008),这些肿瘤具有更大的CD45RO +淋巴细胞浸润。结论:在乳腺癌中,p53突变可能会向免疫系统提供更明显的信号,从而为免疫治疗提供更好的靶标。浸润的CD1a阳性细胞与更密集的肿瘤淋巴细胞浸润和MHC II分子的肿瘤细胞表达有关。

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