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感染性阶段的硕大利什曼原虫前鞭毛体的产生与一种发育调控糖脂的细胞表面表达和释放有关。

The generation of infective stage Leishmania major promastigotes is associated with the cell-surface expression and release of a developmentally regulated glycolipid.

作者信息

Sacks D L, da Silva R P

机构信息

Laboratory of Parasitic Diseases, National Institute of Allergy and Infectious Diseases, Bethesda, MD 20892.

出版信息

J Immunol. 1987 Nov 1;139(9):3099-106.

PMID:3312412
Abstract

A monoclonal antibody, 3F12, was generated which reacted specifically against infective or metacyclic stage Leishmania major promastigotes, but not with noninfective promastigotes obtained from log phase cultures. The antibody recognized a cell surface and released molecule that could be metabolically labeled with [14C]glucose, [3H]mannose, [3H]galactose, and [3H]palmitic acid, but not with [35S]methionine or [3H]leucine. The molecule was the major species surface-labeled by [3H]sodium borohydride after periodate treatment. The glycolipid appeared to be shed primarily as free carbohydrate because 70% of the released material partitioned in the aqueous fraction after phase separation in TX-114. The molecule could be distinguished from the L. major glycolipid which has already been extensively described because its migration on sodium dodecyl sulfate-polyacrylamide gel electrophoresis was of higher relative m.w. However, a close relationship between the two molecules was indicated by the finding that another monoclonal antibody, WIC-79.3, recognized both forms of the glycolipid; one produced and released only by log phase promastigotes, and one produced and released only by metacyclic promastigotes. The loss of agglutination with peanut agglutinin which has been shown to accompany metacyclogenesis was found to be caused by the loss of expression of the log form of the glycolipid which in most cases appeared to be the result of the developmental modification of this molecule. A survey of a number of virulent and avirulent. L. major strains and clones reinforced an absolute association between the ability of these promastigotes to initiate infection in BALB/c mice and their expression and release of the 3F12-binding, developmentally regulated form of the glycolipid. Not only does this glycolipid serve as the first well defined molecular marker for infective stage metacyclic promastigotes, but its unique structure is very likely to contribute to the adaptive changes that allow these parasites to survive within the vertebrate host.

摘要

产生了一种单克隆抗体3F12,它能特异性地与感染性或后循环期的硕大利什曼原虫前鞭毛体发生反应,但不与对数期培养物中获得的非感染性前鞭毛体发生反应。该抗体识别一种细胞表面和释放分子,该分子可被[14C]葡萄糖、[3H]甘露糖、[3H]半乳糖和[3H]棕榈酸代谢标记,但不能被[35S]甲硫氨酸或[3H]亮氨酸标记。该分子是高碘酸盐处理后被[3H]硼氢化钠主要标记的物种表面分子。糖脂似乎主要以游离碳水化合物的形式脱落,因为在TX - 114中进行相分离后,70%的释放物质分配在水相中。该分子可以与已经被广泛描述的硕大利什曼原虫糖脂区分开来,因为它在十二烷基硫酸钠 - 聚丙烯酰胺凝胶电泳上的迁移具有更高的相对分子量。然而,另一种单克隆抗体WIC - 79.3能识别这两种形式的糖脂,这一发现表明这两种分子之间存在密切关系;一种仅由对数期前鞭毛体产生和释放,另一种仅由后循环期前鞭毛体产生和释放。已证明与后循环发育相关的花生凝集素凝集作用的丧失,被发现是由于对数期形式糖脂表达的丧失所致,在大多数情况下,这似乎是该分子发育修饰的结果。对许多有毒和无毒的硕大利什曼原虫菌株和克隆的调查进一步证实,这些前鞭毛体在BALB/c小鼠中引发感染的能力与其表达和释放3F12结合的、发育调控形式的糖脂之间存在绝对关联。这种糖脂不仅是感染性后循环期前鞭毛体的第一个明确定义的分子标记,而且其独特的结构很可能有助于这些寄生虫在脊椎动物宿主体内生存的适应性变化。

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