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Use of Mutated Self-Cleaving 2A Peptides as a Molecular Rheostat to Direct Simultaneous Formation of Membrane and Secreted Anti-HIV Immunoglobulins

机译:使用突变的自我切割2A肽作为分子变阻器,直接同时形成膜和分泌的抗HIV免疫球蛋白。

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摘要

In nature, B cells produce surface immunoglobulin and secreted antibody from the same immunoglobulin gene via alternative splicing of the pre-messenger RNA. Here we present a novel system for genetically programming B cells to direct the simultaneous formation of membrane-bound and secreted immunoglobulins that we term a “Molecular Rheostat”, based on the use of mutated “self-cleaving” 2A peptides. The Molecular Rheostat is designed so that the ratio of secreted to membrane-bound immunoglobulins can be controlled by selecting appropriate mutations in the 2A peptide. Lentiviral transgenesis of Molecular Rheostat constructs into B cell lines enables the simultaneous expression of functional b12-based IgM-like BCRs that signal to the cells and mediate the secretion of b12 IgG broadly neutralizing antibodies that can bind and neutralize HIV-1 pseudovirus. We show that these b12-based Molecular Rheostat constructs promote the maturation of EU12 B cells in an in vitro model of B lymphopoiesis. The Molecular Rheostat offers a novel tool for genetically manipulating B cell specificity for B-cell based gene therapy.
机译:实际上,B细胞通过信使前RNA的可变剪接产生表面免疫球蛋白和来自同一免疫球蛋白基因的分泌抗体。在这里,我们介绍了一种新的系统,该系统可通过对B细胞进行遗传编程来指导膜结合和分泌的免疫球蛋白的同时形成,我们称之为“分子变阻器”,这是基于使用突变的“自裂解” 2A肽的。对分子变阻器进行设计,以便可以通过选择2A肽中的适当突变来控制分泌的免疫球蛋白与结合膜的免疫球蛋白的比率。分子变阻器构建体的慢病毒转基因进入B细胞系,使得能够同时表达基于功能性b12的IgM样BCR,这些BCR向细胞发出信号并介导b12 IgG的广泛中和抗体的分泌,该抗体可以结合并中和HIV-1假病毒。我们显示这些基于b12的分子变阻器构建体在B淋巴细胞生成的体外模型中促进EU12 B细胞的成熟。分子变阻器为基于B细胞的基因治疗提供遗传操纵B细胞特异性的新工具。

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