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CXCL10 拮抗作用和血浆 sDPPIV 与慢性 HCV 基因型 4 感染患者的肝病进展相关。

CXCL10 antagonism and plasma sDPPIV correlate with increasing liver disease in chronic HCV genotype 4 infected patients.

机构信息

Laboratory of Dendritic Cell Immunobiology, Institut Pasteur, Paris, France; Faculty of Medicine, Aim Shams University, Cairo, Egypt.

出版信息

Cytokine. 2013 Aug;63(2):105-12. doi: 10.1016/j.cyto.2013.04.016. Epub 2013 May 7.

Abstract

Egypt has the highest prevalence of hepatitis C virus infection worldwide. CXCL10 is a potent chemoattractant that directs effector lymphocytes to sites of inflammation. It has been reported that plasma CXCL10 is processed by dipeptidylpeptidase IV (DPPIV) thus leading to the generation of an antagonist form. Using Luminex-based immunoassays we determined the concentration of different forms of CXCL10 (total, agonist, and antagonist). We also evaluated plasma soluble DPPIV (sDPPIV) concentration and plasma dipeptidylpeptidase (DPP) activity. Using flow cytometry and immunohistochemistry, we analyzed the distribution of lymphocyte subsets. Plasma CXCL10 was elevated in chronic HCV patients, however the agonist form was undetectable. Increased sDPPIV concentration and DPP activity supported the NH2-truncation of CXCL10. Finally, we demonstrated an increased frequency of CXCR3(+) cells in the peripheral blood, and low numbers of CXCR3(+) cells within the lobular regions of the liver. These findings generalize the observation of chemokine antagonism as a mechanism of immune modulation in chronic HCV patients and may help guide the use of new therapeutic immune modulators.

摘要

埃及拥有全世界最高的丙型肝炎病毒感染率。趋化因子 CXCL10 是一种强效趋化因子,可引导效应淋巴细胞向炎症部位移动。据报道,血浆 CXCL10 可被二肽基肽酶 IV(DPPIV)加工,从而产生一种拮抗剂形式。我们使用基于 Luminex 的免疫测定法来确定 CXCL10 的不同形式(总形式、激动剂和拮抗剂)的浓度。我们还评估了血浆可溶性 DPPIV(sDPPIV)浓度和血浆二肽基肽酶(DPP)活性。通过流式细胞术和免疫组织化学,我们分析了淋巴细胞亚群的分布。慢性 HCV 患者的血浆 CXCL10 水平升高,但激动剂形式无法检测到。sDPPIV 浓度和 DPP 活性的增加支持 CXCL10 的 NH2 截断。最后,我们证明外周血中 CXCR3(+)细胞的频率增加,而肝小叶区域内的 CXCR3(+)细胞数量较少。这些发现将趋化因子拮抗作为慢性 HCV 患者免疫调节的一种机制进行了推广,并且可能有助于指导新型治疗性免疫调节剂的使用。

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