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Natural Proteolytic Processing of Hemofiltrate Cc Chemokine 1 Generates a Potent Cc Chemokine Receptor (Ccr)1 and Ccr5 Agonist with Anti-HIV Properties

机译:天然的血滤液Cc趋化因子1的蛋白水解过程产生有效的Cc趋化因子受体(Ccr)1和Ccr5激动剂,具有抗HIV特性

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摘要

Hemofiltrate CC chemokine (HCC)-1 is a recently described human chemokine that is constitutively expressed in numerous tissues and is present at high concentrations in normal plasma. Using a cell line expressing CC chemokine receptor (CCR)5 as a bioassay, we isolated from human hemofiltrate an HCC-1 variant lacking the first eight amino acids. HCC-1[9–74] was a potent agonist of CCR1, CCR3, and CCR5 and promoted calcium flux and chemotaxis of T lymphoblasts, monocytes, and eosinophils. It also blocked entry of HIV-1 strains using CCR5 as coreceptor. Limited tryptic digestion of HCC-1 generated the active variant. Conditioned media from several tumor cell lines activated HCC-1 with a high efficiency, and this activity could be inhibited by serine protease inhibitors. Our results indicate that HCC-1 represents a nonfunctional precursor that can be rapidly converted to the active chemokine by proteolytic processing. This process represents an additional mechanism by which tumor cells might generate chemoattractant molecules and recruit inflammatory cells. It might also affect HIV-1 replication in infected individuals and play an important role in AIDS pathogenesis.
机译:血滤液CC趋化因子(HCC)-1是最近描述的人类趋化因子,在许多组织中组成性表达,并在正常血浆中高浓度存在。使用表达CC趋化因子受体(CCR)5的细胞系作为生物测定法,我们从人血液滤过液中分离出缺少前8个氨基酸的HCC-1变体。 HCC-1 [9–74]是CCR1,CCR3和CCR5的有效激动剂,并促进T淋巴细胞,单核细胞和嗜酸性粒细胞的钙通量和趋化性。它还使用CCR5作为共受体来阻止HIV-1菌株的进入。 HCC-1的有限胰蛋白酶消化产生了活性变体。来自几种肿瘤细胞系的条件培养基可以高效激活HCC-1,丝氨酸蛋白酶抑制剂可以抑制这种活性。我们的结果表明,HCC-1代表一种非功能性前体,可以通过蛋白水解过程快速转化为活性趋化因子。该过程代表了肿瘤细胞可能产生趋化分子并募集炎症细胞的另一种机制。它也可能影响感染者的HIV-1复制,并在AIDS发病机理中发挥重要作用。

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