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Cell surface differentiation of Mycoplasma mobile visualized by surface protein localization

机译:通过表面蛋白定位可视化支原体的细胞表面分化

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Mycoplasma mobile has a flask-shaped cell morphology and glides toward its tapered end at a rate of 3–7 cell lengths per s (2·0–4·5?μm?s?1) by an unknown mechanism. Gliding requires that the surface of the cell is in contact with a solid substrate, such as glass or plastic. In order to characterize the nature of the outer surface of M. mobile, monoclonal antibodies were raised against intact cells and screened for their ability to recognize surface proteins. Four antibodies were identified and their protein targets were determined. One antibody recognized the Gli349 protein, which is known to be involved in glass binding and gliding. This antibody was also able to displace attached M. mobile cells from glass, suggesting that Gli349 is the major adhesion protein in M. mobile. The other three antibodies recognized members of the Mvsp family of proteins, which are presumably the major surface antigens of M. mobile. Immunofluorescence studies were performed to localize these proteins on the surface of M. mobile cells. Gli349 localized to the proximal region of the tapered part of the cell (the ‘neck’), while the various Mvsp family members showed several distinct patterns of subcellular localization. MvspN and MvspO localized to the distal end of the tapered part of the cell (the ‘head’), MvspK localized to the main part of the cell (the ‘body’), and MvspI localized to both the head and body but not the neck. This analysis shows that M. mobile surprisingly expresses multiple versions of its major surface antigen at once but differentiates its surface by differential localization of the various paralogues.
机译:支原体移动具有烧瓶形的细胞形态,并且通过未知机制,以3-7个细胞长度的速率(2·0-4·5?μm≤1)以3-7个细胞长度的速度朝向其锥形端。滑动要求电池的表面与固体基质(例如玻璃或塑料)接触。为了表征M.移动的外表面的性质,将单克隆抗体升高,并筛选其识别表面蛋白的能力。鉴定了四种抗体,测定其蛋白质靶标。一抗识别GLI349蛋白,已知参与玻璃结合和滑动。该抗体也能够从玻璃移位的M.移动电池。表明GLI349是M.移动的主要粘合蛋白。另外三种抗体识别MVSP蛋白质的成员,这可能是M. Mobile的主要表面抗原。进行免疫荧光研究以将这些蛋白质定位在M.移动细胞的表面上。 GLI349本地化到细胞锥形部分的近端区域(“颈部”),而各种MVSP家族成员呈现出几种不同的亚细胞定位模式。 MVSPN和MVSPO本地化到电池锥形部分的远端(“头部”),MVSPK本地化为小区的主要部分(“身体”),而MVSPI本地化为头部和身体,但不是脖子。该分析表明,M.移动令人惊讶地表达了其主要表面抗原的多个版本,但通过各种副寄生术的差异定位区分其表面。

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