首页> 美国卫生研究院文献>Infection and Immunity >Combinatorial Library Cloning of Human Antibodies to Streptococcus pneumoniae Capsular Polysaccharides: Variable Region Primary Structures and Evidence for Somatic Mutation of Fab Fragments Specific for Capsular Serotypes 6B 14 and 23F
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Combinatorial Library Cloning of Human Antibodies to Streptococcus pneumoniae Capsular Polysaccharides: Variable Region Primary Structures and Evidence for Somatic Mutation of Fab Fragments Specific for Capsular Serotypes 6B 14 and 23F

机译:人肺炎链球菌荚膜多糖抗体的组合文库克隆:可变区一级结构和特定于荚膜血清型6B14和23F的Fab片段的体细胞突变的证据。

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摘要

Antibodies specific for capsular polysaccharides play a central role in immunity to encapsulated Streptococcus pneumoniae, but little is known about their genetics or the variable (V) region polymorphisms that affect their protective function. To begin to address these issues, we used combinatorial library cloning to isolate pneumococcal polysaccharide (PPS)-specific Fab fragments from two vaccinated adults. We determined complete V region primary structures and performed antigen binding analyses of seven Fab fragments specific for PPS serotype 6B, 14, or 23F. Fabs were of the immunoglobulin G2 or A isotype. Several VHIII gene segments (HV 3-7, 3-15, 3-23, and 3-11) were identified. VL regions were encoded by several κ genes (KV 4-1, 3-15, 2-24, and 2D-29) and a λ gene (LV 1-51). Deviation of the VH and VL regions from their assigned germ line counterparts indicated that they were somatically mutated. Fabs of the same serotype specificity isolated from a single individual differed in affinity, and these differences could be accounted for either by the extent of mutation among clonal relatives or by usage of different V-region genes. Thus, functionally disparate anti-PPS antibodies can arise within individuals both by activation of independent clones and by intraclonal somatic mutation. For one pair of clonally related Fabs, the more extensively mutated VH was associated with lower affinity for PPS 14, a result suggesting that somatic mutation could lead to diminished protective efficacy. These findings indicate that the PPS repertoire in the adult derives from memory B-cell populations that have class switched and undergone extensive hypermutation.
机译:荚膜多糖特异的抗体在对封装的肺炎链球菌的免疫中起着核心作用,但对其遗传学或影响其保护功能的可变(V)区多态性知之甚少。为了开始解决这些问题,我们使用组合文库克隆从两个接种疫苗的成年人中分离出了肺炎球菌多糖(PPS)特异性Fab片段。我们确定了完整的V区一级结构,并对7种对PPS血清型6B,14或23F特异的Fab片段进行了抗原结合分析。 Fab具有免疫球蛋白G2或A同种型。鉴定了几个VHIII基因片段(HV 3-7、3-15、3-23和3-11)。 VL区由几个κ基因(KV 4-1、3-15、2-24和2D-29)和λ基因(LV 1-51)编码。 VH和VL区与指定的种系对应物之间的差异表明它们在体细胞上发生了突变。从单个个体中分离出的具有相同血清型特异性的Fab亲和力有所不同,这些差异可以通过克隆亲属间突变的程度或使用不同的V区基因来解释。因此,功能上不同的抗PPS抗体可通过独立克隆的激活和克隆内体细胞突变而在个体内产生。对于一对克隆相关的Fab,更广泛突变的VH与对PPS 14的较低亲和力相关,这一结果表明体细胞突变可能导致保护功效降低。这些发现表明,成人中的PPS曲目源自记忆B细胞群体,这些群体具有类别转换并经历了广泛的超突变。

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