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Exploiting the diphtheria toxin internalization receptor enhances delivery of proteins to lysosomes for enzyme replacement therapy

机译:利用白喉毒素内化受体增强蛋白质的蛋白质递送至酶置换疗法

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Enzyme replacement therapy, in which a functional copy of an enzyme is injected either systemically or directly into the brain of affected individuals, has proven to be an effective strategy for treating certain lysosomal storage diseases. The inefficient uptake of recombinant enzymes via the mannose-6-phosphate receptor, however, prohibits the broad utility of replacement therapy. Here, to improve the efficiency and efficacy of lysosomal enzyme uptake, we exploited the strategy used by diphtheria toxin to enter into the endolysosomal network of cells by creating a chimera between the receptor-binding fragment of diphtheria toxin and the lysosomal hydrolase TPP1. We show that chimeric TPP1 binds with high affinity to target cells and is efficiently delivered into lysosomes. Further, we show superior uptake of chimeric TPP1 over TPP1 alone in brain tissue following intracerebroventricular injection in mice lacking TPP1, demonstrating the potential of this strategy for enhancing lysosomal storage disease therapy.
机译:酶替代疗法,其中酶的功能拷贝以自身或直接注射到受影响个体的大脑中,已被证明是治疗某些溶酶体储存疾病的有效策略。然而,通过甘露糖-6-磷酸受体的重组酶的效率低下禁止替代疗法的广泛效用。在这里,为了提高溶酶体酶摄取的效率和功效,我们利用白喉毒素使用的策略通过在白喉毒素和溶酶体水解酶TPP1的受体结合片段之间产生嵌合体来进入细胞内溶血体网络。我们表明嵌合TPP1与靶细胞高亲和力结合,并有效地递送到溶酶体中。此外,我们在缺乏TPP1的小鼠脑内注射术后脑组织中,在脑组织中,我们在脑组织中展示了优异的嵌合TPP1在TPP1上。展示了这种促进溶酶体储存疾病治疗的策略的潜力。

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