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梅毒螺旋体与血清脂蛋白的结合:蛋白聚糖的可能作用。

Serum lipoprotein binding by Treponema pallidum: possible role for proteoglycans.

作者信息

Alderete J F, Baseman J B

机构信息

Department of Microbiology, University of Texas Health Science Center, San Antonio 78284-7758.

出版信息

Genitourin Med. 1989 Jun;65(3):177-82. doi: 10.1136/sti.65.3.177.

Abstract

Acquisition by the syphilis spirochaete, Treponema pallidum, of radioiodinated total human plasma lipoprotein and lipoprotein subfractions was examined. Time dependent and saturation binding kinetics were observed for total lipoproteins and subfractions, including high density lipoproteins, low density lipoproteins (LDL), and very low density lipoproteins. All subfractions competed equally well in binding iodinated total lipoproteins and individual subfractions, but apoproteins common to all subfractions were ineffective in inhibiting lipoprotein acquisition. The interaction of LDL with T pallidum was studied further and, interestingly, the presence of 17% sulphated dextran sulphate (DS) in the reaction mixture containing treponemes and LDL resulted in up to 172 times more LDL being bound by live treponemes. Biological variability was observed in the extent of increased LDL bound in the presence of 17% sulphated DS by preparations of T pallidum isolated from different infected rabbits. Saturation kinetics of iodinated LDL acquisition was obtained in the presence of 17% sulphated DS but not 1% sulphated DS. Other proteoglycan molecules, such as chondroitin sulphate, hyaluronic acid and heparin, and fibronectin, the extracellular matrix protein targeted by treponemes in parasitism of host cells and tissues neither diminished nor enhanced LDL binding by live treponemes. Only 5% and 10% of associated radioactivity was released from treponemal surfaces after T pallidum was incubated with iodinated LDL and 17% sulphated-DS for 15 and 30 minutes, respectively. These data show binding and possible internalisation of host lipoproteins by T pallidum, which may be mediated by sulphated proteoglycan. Sulphated proteoglycans accumulate during T pallidum infections of host cells.

摘要

研究了梅毒螺旋体苍白密螺旋体对放射性碘化人血浆总脂蛋白及脂蛋白亚组分的摄取情况。观察到总脂蛋白和亚组分(包括高密度脂蛋白、低密度脂蛋白(LDL)和极低密度脂蛋白)存在时间依赖性和饱和结合动力学。所有亚组分在结合碘化总脂蛋白和单个亚组分方面竞争效果相同,但所有亚组分共有的载脂蛋白在抑制脂蛋白摄取方面无效。进一步研究了LDL与苍白密螺旋体的相互作用,有趣的是,在含有密螺旋体和LDL的反应混合物中加入17%的硫酸葡聚糖(DS),活的密螺旋体结合的LDL最多可增加172倍。从不同感染兔子分离得到的苍白密螺旋体制剂在17%硫酸化DS存在下结合LDL增加的程度存在生物学差异。在17%硫酸化DS存在下可获得碘化LDL摄取的饱和动力学,但在1%硫酸化DS存在下则不能。其他蛋白聚糖分子,如硫酸软骨素、透明质酸和肝素,以及纤连蛋白(密螺旋体在宿主细胞和组织寄生过程中靶向的细胞外基质蛋白),既不会减少也不会增强活的密螺旋体对LDL的结合。将苍白密螺旋体与碘化LDL和17%硫酸化-DS分别孵育15分钟和30分钟后,只有5%和10%的相关放射性从密螺旋体表面释放。这些数据表明苍白密螺旋体可结合并可能内化宿主脂蛋白,这可能由硫酸化蛋白聚糖介导。硫酸化蛋白聚糖在宿主细胞感染苍白密螺旋体期间会积累。

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