宫颈癌患者HLA I类和HLA- g表达改变与IL-10表达相关。

Josefa Antonia Rodríguez, Liliana Galeano, Diana María Palacios, Constanza Gómez, Martha Lucía Serrano, María Mercedes Bravo, Alba Lucía Combita
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引用次数: 60

摘要

尽管高危人乳头瘤病毒(HPV)是宫颈癌发病的重要危险因素,但越来越多的证据表明,逃避免疫监视的能力似乎与HPV的转化潜力和快速发展为癌症有关。在其他癌症模型中,IL-10通过下调人白细胞抗原I类(HLA-I)表达或增加HLA-G表达来损害抗肿瘤免疫应答。为了了解这些改变如何有助于逃避宫颈癌的免疫监测,我们通过免疫组织化学分析了63例宫颈上皮内瘤变III (CIN-III)和宫颈癌患者的活组织检查中hla -1、HLA-G和IL-10的表达。免疫组化显示50/59例患者hla - 1表达缺失或弱。在这些病例中,有很高比例的人失去了杂合子。IL-10和HLA-G表达率分别为46.6%和27.6%。87.5%的HLA-G阳性患者IL-10同时上调(p = 0.000)。同样,IL-10表达与hla -1下调之间存在显著关联(p = 0.028)。最后,我们观察到HLA-I下调患者的HLA-G表达高于HLA-I正常表达的患者(p = 0.004)。我们的研究结果表明,在宫颈癌中,IL-10的表达可能通过上调HLA- g表达和下调HLA- I类表达来诱导免疫抑制环境。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Altered HLA class I and HLA-G expression is associated with IL-10 expression in patients with cervical cancer.

Although high-risk human papillomaviruses (HPVs) are an important risk factor in the etiopathogenesis of cervical cancer, increasing evidence suggests that the ability to avoid immune surveillance seems to be linked to the transforming potential of HPV and a rapid progression to cancer. In other cancer models, IL-10 contributes to impair anti-tumor immune response either by downregulating human leukocyte antigen Class I (HLA-I) expression or by increasing HLA-G expression. To comprehend how these alterations could contribute to evasion of immune surveillance in cervical cancer, we analyzed HLA-I, HLA-G and IL-10 expressions by immunohistochemistry in 63 biopsies from patients with cervical intraepithelial neoplasia III (CIN-III) and cervical cancer. Immunohistochemistry showed absent or weak HLA-I expression in 50/59 cases. In these cases, a high percentage had loss of heterozygosis. IL-10 and HLA-G expression were observed in 46.6 and 27.6% of cases, respectively. Concurrent upregulation of IL-10 was found in 87.5% of HLA-G positive cases (p = 0.000). Similarly, a significant association between IL-10 expression and HLA-I downregulation was found (p = 0.028). Finally, we observed higher HLA-G expression in patients with HLA-I downregulation than in those with normal HLA-I expression (p = 0.004). Our results suggest that, in cervical cancer, the IL-10 expression may induce an immunosuppressive environment by upregulating HLA-G expression and downregulating HLA class I expression.

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