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来自B族V型链球菌的一种保护性表面蛋白与αC蛋白具有N端序列同源性。

A protective surface protein from type V group B streptococci shares N-terminal sequence homology with the alpha C protein.

作者信息

Lachenauer C S, Madoff L C

机构信息

Channing Laboratory, Department of Medicine, Brigham and Women's Hospital, Boston, Massachusetts 02115, USA.

出版信息

Infect Immun. 1996 Oct;64(10):4255-60. doi: 10.1128/iai.64.10.4255-4260.1996.

Abstract

Infection by group B streptococci (GBS) is an important cause of bacterial disease in neonates, pregnant women, and nonpregnant adults. Historically, serotypes Ia, Ib, II, and III have been most prevalent among disease cases; recently, type V strains have emerged as important strains in the United States and elsewhere. In addition to type-specific capsular polysaccharides, many GBS strains possess surface proteins which demonstrate a laddering pattern on sodium dodecyl sulfate-polyacrylamide gel electrophoresis (SDS-PAGE) and resistance to trypsin digestion. These include the alpha C protein, the R proteins, and protein Rib. Some of these proteins elicit protective antibodies in animals. We demonstrate a trypsin-resistant laddering protein purified from a type V GBS strain by mutanolysin extraction and column chromatography. This protein contains a major 90-kDa band and a series of smaller bands spaced approximately 10 kDa apart on SDS-PAGE. Cross-reactivity of the type V protein with the alpha C protein and with R1 was demonstrated on Western blot (immunoblot). N-terminal sequence analysis of the protein revealed residue identity with 17 of 18 residues at corresponding positions on the alpha protein. Western blot of SDS extracts of 41 clinical type V isolates with rabbit antiserum to the protein demonstrated a homologous protein in 25 isolates (61%); two additional strains exhibited a heterologous pattern which was also demonstrated with 4G8, a monoclonal antibody directed to the alpha C protein repeat region. Rabbit antiserum raised to the type V protein conferred protection in neonatal mice against a type V strain bearing a homologous protein. These data support the hypothesis that there exists a family of trypsin-resistant, laddering GBS surface proteins which may play a role in immunity to GBS infection.

摘要

B族链球菌(GBS)感染是新生儿、孕妇和非孕成人细菌性疾病的重要病因。从历史上看,血清型Ia、Ib、II和III在病例中最为普遍;最近,V型菌株在美国和其他地方已成为重要菌株。除了型特异性荚膜多糖外,许多GBS菌株还具有表面蛋白,这些蛋白在十二烷基硫酸钠-聚丙烯酰胺凝胶电泳(SDS-PAGE)上呈现阶梯状模式,并且对胰蛋白酶消化具有抗性。这些包括αC蛋白、R蛋白和Rib蛋白。其中一些蛋白能在动物体内引发保护性抗体。我们通过变溶菌素提取和柱色谱法展示了一种从V型GBS菌株中纯化的抗胰蛋白酶阶梯状蛋白。该蛋白在SDS-PAGE上含有一条主要的90 kDa条带和一系列间隔约10 kDa的较小条带。在蛋白质印迹(免疫印迹)上证明了V型蛋白与αC蛋白和R1的交叉反应性。该蛋白的N端序列分析显示,在α蛋白相应位置的18个残基中有17个残基具有相同性。用针对该蛋白的兔抗血清对41株临床V型分离株的SDS提取物进行蛋白质印迹分析,结果显示25株分离株(61%)中有同源蛋白;另外两株呈现异源模式,用针对αC蛋白重复区域的单克隆抗体4G8也证明了这一点。用针对V型蛋白产生的兔抗血清对新生小鼠提供了针对携带同源蛋白的V型菌株的保护作用。这些数据支持了这样一种假设,即存在一个抗胰蛋白酶、呈阶梯状的GBS表面蛋白家族,它们可能在GBS感染免疫中发挥作用。

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