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由多糖-蛋白结合疫苗引发的针对B族链球菌B族多糖的抗体的功能活性。

Functional activity of antibodies to the group B polysaccharide of group B streptococci elicited by a polysaccharide-protein conjugate vaccine.

作者信息

Marques M B, Kasper D L, Shroff A, Michon F, Jennings H J, Wessels M R

机构信息

Channing Laboratory, Brigham and Women's Hospital, Boston, Massachusetts 02115.

出版信息

Infect Immun. 1994 May;62(5):1593-9. doi: 10.1128/iai.62.5.1593-1599.1994.

Abstract

Group B streptococci (GBS) are a major cause of sepsis and meningitis in infants. While antibodies directed to the type-specific GBS capsule have been shown to be protective, it is less clear whether antibodies to the group B polysaccharide, a noncapsular, cell wall-associated antigen, may play a role in immunity. To investigate the functional activity of group B polysaccharide-specific antibodies, we tested sera from rabbits vaccinated with group B polysaccharide coupled to tetanus toxoid (B-TT). Anti-B-TT was weakly opsonic in vitro for a highly encapsulated type III strain, while antiserum elicited by vaccination with type III capsular polysaccharide linked to tetanus toxoid (III-TT) was a very effective opsonin. In contrast to anti-III-TT, anti-B-TT given before or after bacterial challenge was only marginally effective in protecting newborn mice against lethal infection with type III GBS. The number of C3 molecules bound to type III GBS was augmented by anti-III-TT but not by high antibody concentrations of anti-B-TT. These results suggest that the difference in opsonic activity between anti-B-TT and anti-III-TT may be due to a difference in their ability to deposit C3. In addition, the maximum number of antibody molecules bound to the bacterial surface was greater for anti-III-TT than for anti-B-TT. That anti-B-TT binds to fewer sites than anti-III-TT may explain the differences in complement activation and in opsonic and protective efficacy of antibodies to group B polysaccharide compared with antibodies to the type-specific capsular polysaccharide.

摘要

B族链球菌(GBS)是婴儿败血症和脑膜炎的主要病因。虽然已证明针对GBS型特异性荚膜的抗体具有保护作用,但针对B族多糖(一种非荚膜、与细胞壁相关的抗原)的抗体是否在免疫中发挥作用尚不清楚。为了研究B族多糖特异性抗体的功能活性,我们检测了用与破伤风类毒素偶联的B族多糖(B-TT)免疫的兔血清。抗B-TT对高度荚膜化的III型菌株在体外的调理作用较弱,而用与破伤风类毒素偶联的III型荚膜多糖(III-TT)免疫产生的抗血清是一种非常有效的调理素。与抗III-TT相反,在细菌攻击之前或之后给予的抗B-TT在保护新生小鼠免受III型GBS致死性感染方面仅具有微弱的效果。抗III-TT可增加与III型GBS结合的C3分子数量,但高浓度的抗B-TT抗体则不能。这些结果表明,抗B-TT和抗III-TT在调理活性上的差异可能是由于它们沉积C3的能力不同所致。此外,抗III-TT与细菌表面结合的抗体分子最大数量比抗B-TT更多。抗B-TT比抗III-TT结合的位点更少,这可能解释了与型特异性荚膜多糖抗体相比,B族多糖抗体在补体激活、调理和保护功效方面的差异。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a407/186360/77c1639aa507/iai00005-0105-a.jpg

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