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Kappa chain maturation helps drive rapid development of an infant HIV-1 broadly neutralizing antibody lineage

机译:κ链成熟有助于推动婴儿HIV-1广泛中和抗体谱系的快速发展

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摘要

HIV-infected infants develop broadly neutralizing plasma responses with more rapid kinetics than adults, suggesting the ontogeny of infant responses could better inform a path to achievable vaccine targets. Here we reconstruct the developmental lineage of BF520.1, an infant-derived HIV-specific broadly neutralizing antibody (bnAb), using computational methods developed specifically for this purpose. We find that the BF520.1 inferred naive precursor binds HIV Env. We also show that heterologous cross-clade neutralizing activity evolved in the infant within six months of infection and that, ultimately, only 2% SHM is needed to achieve the full breadth of the mature antibody. Mutagenesis and structural analyses reveal that, for this infant bnAb, substitutions in the kappa chain were critical for activity, particularly in CDRL1. Overall, the developmental pathway of this infant antibody includes features distinct from adult antibodies, including several that may be amenable to better vaccine responses.
机译:与成人相比,感染了HIV的婴儿发展出广泛的中和血浆反应,并且动力学动力学比成人更快,这表明婴儿反应的个体发育可以更好地为实现可达到的疫苗目标提供一条途径。在这里,我们使用专门为此目的开发的计算方法,重建了BF520.1(一种婴儿来源的HIV特异性广泛中和抗体(bnAb))的发育谱系。我们发现,BF520.1推断的幼稚前体结合了HIV Env。我们还显示,在感染后的六个月内,婴儿体内进化出了异源跨包合物中和活性,最终,仅2%的SHM即可达到成熟抗体的全部广度。诱变和结构分析表明,对于此婴儿bnAb,κ链中的取代对于活性至关重要,特别是在CDRL1中。总体而言,该婴儿抗体的发育途径包括不同于成人抗体的特征,包括可能适合更好的疫苗反应的几种抗体。

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