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缺乏磷酸聚糖重复序列的墨西哥利什曼原虫寄生虫对巨噬细胞和小鼠仍具感染性。

Phosphoglycan repeat-deficient Leishmania mexicana parasites remain infectious to macrophages and mice.

作者信息

Ilg T, Demar M, Harbecke D

机构信息

Max-Planck-Institut für Biologie, Corrensstrasse 38, 72076 Tübingen, Germany.

出版信息

J Biol Chem. 2001 Feb 16;276(7):4988-97. doi: 10.1074/jbc.M008030200. Epub 2000 Nov 8.

Abstract

The human pathogen Leishmania synthesizes phosphoglycans (PGs) formed by variably modified phosphodisaccharide [6-Galbeta1-4Manalpha1-PO(4)] repeats and mannooligosaccharide phosphate [(Manalpha1-2)(0-5)Manalpha1-PO(4)] caps that occur lipid-bound on lipophosphoglycan, protein-bound on proteophosphoglycans, and as an unlinked form. PG repeat synthesis has been described as essential for survival and development of Leishmania throughout their life cycle, including for virulence to the mammalian host. In this study, this proposal was investigated in Leishmania mexicana using a spontaneous mutant that was fortuitously isolated from an infected mouse, and by generating a lmexlpg2 gene deletion mutant (Deltalmexlpg2), that lacks a Golgi GDP-Man transporter. The spontaneous mutant lacks PG repeats but synthesizes normal levels of mannooligosaccharide phosphate caps, whereas the Deltalmexlpg2 mutant is deficient in PG repeat synthesis and down-regulates cap expression. In contrast to expectations, both L. mexicana mutants not only retain their ability to bind to macrophages, but are also indistinguishable from wild type parasites with respect to colonization of and multiplication within host cells. Moreover, in mouse infection studies, the spontaneous L. mexicana repeat-deficient mutant and the Deltalmexlpg2 mutant showed no significant difference to a wild type strain with respect to the severity of disease caused by these parasites. Therefore, at least in Leishmania mexicana, PG repeat synthesis is not an absolute requirement for virulence.

摘要

人类病原体利什曼原虫合成磷酸化聚糖(PGs),其由可变修饰的磷酸二糖[6 - 半乳糖β1 - 4 - 甘露糖α1 - PO(4)]重复序列和甘露寡糖磷酸[(甘露糖α1 - 2)(0 - 5)甘露糖α1 - PO(4)]帽组成,这些结构以脂质结合形式存在于脂磷酸化聚糖上、以蛋白质结合形式存在于蛋白磷酸化聚糖上,还有未连接的形式。PG重复序列的合成被认为对利什曼原虫在其整个生命周期中的存活和发育至关重要,包括对哺乳动物宿主的毒力。在本研究中,利用从感染小鼠中偶然分离出的自发突变体以及通过构建缺失高尔基体GDP - 甘露糖转运体的lmexlpg2基因缺失突变体(Deltalmexlpg2),在墨西哥利什曼原虫中对这一观点进行了研究。自发突变体缺乏PG重复序列,但能合成正常水平的甘露寡糖磷酸帽,而Deltalmexlpg2突变体在PG重复序列合成方面存在缺陷且帽表达下调。与预期相反,两种墨西哥利什曼原虫突变体不仅保留了与巨噬细胞结合的能力,而且在宿主细胞内的定植和增殖方面与野生型寄生虫没有区别。此外,在小鼠感染研究中,自发的墨西哥利什曼原虫重复序列缺陷突变体和Deltalmexlpg2突变体在由这些寄生虫引起的疾病严重程度方面与野生型菌株没有显著差异。因此,至少在墨西哥利什曼原虫中,PG重复序列的合成不是毒力的绝对必要条件。

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