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脂多糖的磷酰胆碱修饰:流感嗜血杆菌的一个相变特征。

Decoration of lipopolysaccharide with phosphorylcholine: a phase-variable characteristic of Haemophilus influenzae.

作者信息

Weiser J N, Shchepetov M, Chong S T

机构信息

Department of Pediatrics, Children's Hospital of Philadelphia, University of Pennsylvania School of Medicine, 19104-4318, USA.

出版信息

Infect Immun. 1997 Mar;65(3):943-50. doi: 10.1128/IAI.65.3.943-950.1997.

Abstract

Choline, although not a nutritional requirement for Haemophilus influenzae, is taken up from the growth medium and incorporated into its lipopolysaccharide (LPS). Incorporated choline is in the form of phosphorylcholine (ChoP) based on the reactivity with the monoclonal antibody with specificity for this structure, TEPC-15. Incorporation of [3H]choline from the growth medium and expression of the TEPC-15 epitope undergo high-frequency phase variation, characteristic of other LPS structures in this species. The expression and phase variation of ChoP require a previously identified locus involved in LPS biosynthesis, lic1. The first gene in lic1, licA, contains a translational switch based on variation in the number of intragenic tandem repeats of the sequence 5'-CAAT-3'. The full-length LicA polypeptide resembles choline kinases of eucaryotes, suggesting that the pathway for choline incorporation into the H. influenzae glycolipid has similarities to the pathway for choline incorporation in eucaryotic lipid synthesis. The display of ChoP, a host-like structure, renders the organism more rather than less susceptible to the bactericidal activity of human serum. The increased serum sensitivity of variants with ChoP correlates with higher serum immunoglobulin G titers to LPS containing this structure. ChoP appears to be a cell surface feature common to a number of pathogens of the human respiratory tract, including Streptococcus pneumoniae and mycoplasmas. In the case of H. influenzae, its primary contribution to pathogenesis does not appear to be antigenic variation to evade host humoral clearance mechanisms.

摘要

胆碱虽不是流感嗜血杆菌生长所需的营养物质,但可从生长培养基中摄取并整合到其脂多糖(LPS)中。基于与针对该结构具有特异性的单克隆抗体TEPC - 15的反应性,整合的胆碱是以磷酸胆碱(ChoP)的形式存在。从生长培养基中摄取[3H]胆碱以及TEPC - 15表位的表达会发生高频相变,这是该物种其他LPS结构的特征。ChoP的表达和相变需要一个先前确定的参与LPS生物合成的基因座lic1。lic1中的第一个基因licA包含一个基于5'-CAAT-3'序列基因内串联重复序列数量变化的翻译开关。全长LicA多肽类似于真核生物的胆碱激酶,这表明胆碱整合到流感嗜血杆菌糖脂中的途径与胆碱整合到真核生物脂质合成中的途径具有相似性。呈现出类似宿主结构的ChoP会使该生物体对人血清的杀菌活性更敏感而非更不敏感。具有ChoP的变体血清敏感性增加与针对含有该结构的LPS的血清免疫球蛋白G滴度升高相关。ChoP似乎是包括肺炎链球菌和支原体在内的多种人类呼吸道病原体共有的细胞表面特征。就流感嗜血杆菌而言,其对发病机制的主要作用似乎不是通过抗原变异来逃避宿主的体液清除机制。

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