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A群脑膜炎球菌脂寡糖(LOS):血清型相关及保守LOS表位的初步结构研究与特性分析

Meningococcal group A lipooligosaccharides (LOS): preliminary structural studies and characterization of serotype-associated and conserved LOS epitopes.

作者信息

Kim J J, Phillips N J, Gibson B W, Griffiss J M, Yamasaki R

机构信息

Centre for Immunochemistry, University of California, San Francisco 94143.

出版信息

Infect Immun. 1994 May;62(5):1566-75. doi: 10.1128/iai.62.5.1566-1575.1994.

Abstract

Structural studies indicate that the neisserial lipooligosaccharides (LOS) are composed of an oligosaccharide (OS) portion with a phosphorylated diheptose (Hep) core attached to the toxic lipid A moiety. A conserved meningococcal LOS epitope, defined by monoclonal antibody (MAb) D6A, is expressed on group A and many group B and C meningococci of different LOS serotypes (J. J. Kim, R. E. Mandrell, H. Zhen, M. A. Apicella, J. T. Poolman, and J. M. Griffiss, Infect. Immun. 56:2631-2638, 1988). This MAb-defined D6A epitope is immunogenic in humans (M. M. Estabrook, R. E. Mandrell, M. A. Apicella, and J. M. Griffiss, Infect. Immun. 58:2204-2213, 1990; M. M. Estabrook, C. J. Baker, and J. M. Griffiss, J. Infect. Dis. 197:966-970, 1993). In this study, we characterize this important MAb-defined LOS epitope. Serotype L10 and L11 group A meningococal LOS were chemically modified and used to investigate what portion of the LOS molecule is important for expression of the conserved (D6A) epitope and serotype-associated LOS epitopes by use of immunoblotting techniques and selected MAbs as probes. Preliminary structural characterization of the LOS was also accomplished by electrospray ionization-mass spectrometry. Our results indicate the following. (i) Antibodies that recognize the serotype-associated or conserved LOS epitopes recognize the OS portion of the LOS. (ii) The phosphorylated diheptose core region of the OS is essential for expression of the conserved D6A epitope. (iii) The lipid portion of the molecule is important for optimum expression of the LOS epitopes. (iv) The proposed compositions of the O-deacylated LOS are consistent with the presence of a phosphorylated diheptose core and are as follows: for O-deacylated L10 LOS, 3Hex (hexose), 1HexNAc (N-acetylhexosamine), 2KDO (2-keto-3-deoxy-D-manno-octulosonic acid), 2Hep (heptose), 1PEA or 2PEA (phosphoethanolamine), and O-deacylated lipid A; and for O-deacylated L11 LOS, 2Hex, 1HexNAc, 2KDO, 2Hep, 2PEA, and O-deacylated lipid A. Because the phosphorylated diheptose core region of the LOS is essential for the formation of a conserved LOS epitope (D6A) that is immunogenic in humans, care should be taken to maintain stereochemical requirements for the expression of this conserved epitope in the design of effective, nontoxic LOS vaccines.

摘要

结构研究表明,奈瑟氏菌脂寡糖(LOS)由一个寡糖(OS)部分组成,该部分具有一个磷酸化二庚糖(Hep)核心,连接到有毒的脂多糖A部分。一种由单克隆抗体(MAb)D6A定义的保守的脑膜炎球菌LOS表位,在不同LOS血清型的A群以及许多B群和C群脑膜炎球菌上表达(J. J. Kim、R. E. Mandrell、H. Zhen、M. A. Apicella、J. T. Poolman和J. M. Griffiss,《感染与免疫》56:2631 - 2638,1988年)。这种由MAb定义的D6A表位在人类中具有免疫原性(M. M. Estabrook、R. E. Mandrell、M. A. Apicella和J. M. Griffiss,《感染与免疫》58:2204 - 2213,1990年;M. M. Estabrook、C. J. Baker和J. M. Griffiss,《传染病杂志》197:966 - 970,1993年)。在本研究中,我们对这个重要的由MAb定义的LOS表位进行了表征。对血清型L10和L11的A群脑膜炎球菌LOS进行化学修饰,并利用免疫印迹技术和选定的MAb作为探针,研究LOS分子的哪一部分对于保守(D6A)表位和血清型相关LOS表位的表达至关重要。还通过电喷雾电离质谱对LOS进行了初步结构表征。我们的结果表明:(i)识别血清型相关或保守LOS表位的抗体识别LOS的OS部分。(ii)OS的磷酸化二庚糖核心区域对于保守D6A表位的表达至关重要。(iii)分子的脂质部分对于LOS表位的最佳表达很重要。(iv)所提出的O - 脱酰基LOS的组成与磷酸化二庚糖核心的存在一致,如下:对于O - 脱酰基L10 LOS,3己糖(己糖)、1 N - 乙酰己糖胺(N - 乙酰己糖胺)、2 2 - 酮 - 3 - 脱氧 - D - 甘露糖辛酮酸(KDO)、2庚糖(庚糖)、1磷酸乙醇胺或2磷酸乙醇胺(磷酸乙醇胺)以及O - 脱酰基脂多糖A;对于O - 脱酰基L11 LOS,2己糖、1 N - 乙酰己糖胺、2 KDO、2庚糖、2磷酸乙醇胺以及O - 脱酰基脂多糖A。由于LOS的磷酸化二庚糖核心区域对于形成在人类中具有免疫原性的保守LOS表位(D6A)至关重要,在设计有效的无毒LOS疫苗时,应注意维持该保守表位表达的立体化学要求。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/180e/186357/de290f91d0bb/iai00005-0077-a.jpg

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