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Palmitoyl derivatives of GpMBP epitopes: T-cell response and peptidases susceptibility.

机译:GpMBP表位的棕榈酰基衍生物:T细胞反应和肽酶敏感性。

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摘要

We report for the first time the immunoadjuvant effects of lipoconjugation of peptide antigens in an in vitro system by using CD4+ T-cells. The lipopeptides obtained by conjugating a palmitoyl moiety at the N(alpha)-terminal of Gln(74) or at the epsilon-NH(2) of Lys(75) of GpMBP(74-85) induced increased T-cell responsiveness compared to the native nonlipidated peptide. On the other hand, lipoderivatives of GpMBP(82-98) did not increase the T-cell response, demonstrating that the superagonist inducing effect of lipoconjugation is epitope-specific. Digestion of the two native peptides with cathepsin D and L, both implicated in antigen processing, and with a complete lysosomal fraction of a EBV-transformed B cell line shows that GpMBP(74-85) is resistant to cellular proteases, while GpMBP(82-98) is easily digested by these enzymes. These results suggest that the first prerequisite for increasing the T-cell response by lipoconjugation is the stability of the native peptide to peptidases, providing an important insight into the understanding of the immunoadjuvant effect of lipoderivative antigens.
机译:我们首次报道了在体外系统中通过使用CD4 + T细胞对肽抗原脂缀合的免疫佐剂作用。通过与GpMBP(74-85)的Lys(75)的Lys(75)的Nln末端或Gln(74)的ε-NH(2)结合的棕榈酰部分获得的脂肽诱导增加的T细胞反应性天然非脂化肽。另一方面,GpMBP(82-98)的脂衍生物没有增加T细胞反应,表明脂结合的超激​​动剂诱导作用是表位特异性的。用组织蛋白酶D和L消化这两个天然肽,都涉及抗原加工,并且具有EBV转化的B细胞系的完整溶酶体级分,表明GpMBP(74-85)对细胞蛋白酶具有抗性,而GpMBP(82 -98)容易被这些酶消化。这些结果表明,通过脂缀合增加T细胞反应的首要前提是天然肽对肽酶的稳定性,为了解脂类衍生抗原的免疫佐剂作用提供了重要的见识。

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