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通过给予双曲钩端螺旋体非致病菌株的脂多糖来控制免疫交叉反应性钩端螺旋体感染。

Control of immunologically crossreactive leptospiral infection by administration of lipopolysaccharides from a nonpathogenic strain of Leptospira biflexa.

作者信息

Matsuo K, Isogai E, Araki Y

机构信息

Laboratory of Environmental Molecular Biology, Graduate School of Environmental Earth Science, Hokkaido University, Sapporo, Japan.

出版信息

Microbiol Immunol. 2000;44(11):887-90. doi: 10.1111/j.1348-0421.2000.tb02579.x.

Abstract

In our previous paper (Matsuo, K., Isogai, E., and Araki, Y., Carbohydr. Res., 328: 517-524, 2000), antigenic polysaccharides obtained from the lipopolysaccharide (LPS) fraction of a nonpathogenic leptospira, Leptospira biflexa patoc Patoc I, are shown to be broadly crossreactable with most rabbit antisera elicited by immunization with various pathogenic leptospires. The result led us to test a protective effect of the same LPS in a hamster model system by heterologously challenging with a pathogenic leptospira, L. interrogans manilae UP-MMG. Firstly, a similarity in the antigenic epitopes of L. biflexa and L. interrogans was confirmed by the following assays. In the microscopic agglutination test (MAT), a hamster antiserum elicited by immunization with the L. biflexa-LPS preparation was shown to agglutinate cells of L. interrogans. Contrarily, in the enzyme-linked immunosorbent assay (ELISA), the L. biflexa-LPS preparation was shown to crossreact with a hamster antiserum elicited by immunization with whole cells of L. interrogans. These results suggest that the same or closely related antigens may be present on the cell surfaces of both L. biflexa patoc Patoc I and L. interrogans manilae UP-MMG. Furthermore, in a protective assay, the prior administration of a L. biflexa-LPS preparation resulted in raising a protective response in hamsters against challenge by L. interrogans without any side effect. The protective effect was strongly dependent on the dose amounts and/or administration times of L. biflexa-LPS. Thus, L. biflexa-LPS preparations can use as a potent vaccine against leptospirosis caused by various leptospires.

摘要

在我们之前的论文(Matsuo, K., Isogai, E., and Araki, Y., Carbohydr. Res., 328: 517 - 524, 2000)中,从非致病性钩端螺旋体双曲钩端螺旋体帕托克I型(Leptospira biflexa patoc Patoc I)的脂多糖(LPS)组分中获得的抗原性多糖,被证明能与大多数由各种致病性钩端螺旋体免疫诱导产生的兔抗血清发生广泛的交叉反应。该结果促使我们在仓鼠模型系统中通过用致病性钩端螺旋体问号钩端螺旋体马尼拉型(L. interrogans manilae UP - MMG)进行异源攻击来测试相同LPS的保护作用。首先,通过以下试验证实了双曲钩端螺旋体和问号钩端螺旋体抗原表位的相似性。在显微镜凝集试验(MAT)中,用双曲钩端螺旋体 - LPS制剂免疫诱导产生的仓鼠抗血清能凝集问号钩端螺旋体的细胞。相反,在酶联免疫吸附试验(ELISA)中,双曲钩端螺旋体 - LPS制剂能与用问号钩端螺旋体全细胞免疫诱导产生的仓鼠抗血清发生交叉反应。这些结果表明,双曲钩端螺旋体帕托克I型和问号钩端螺旋体马尼拉型UP - MMG的细胞表面可能存在相同或密切相关的抗原。此外,在一项保护试验中,预先给予双曲钩端螺旋体 - LPS制剂可使仓鼠对问号钩端螺旋体的攻击产生保护反应,且无任何副作用。保护作用强烈依赖于双曲钩端螺旋体 - LPS的剂量和/或给药时间。因此,双曲钩端螺旋体 - LPS制剂可作为一种有效的疫苗,用于预防由各种钩端螺旋体引起的钩端螺旋体病。

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