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重组转甲状腺素蛋白凝集素:一种用于溶酶体酶替代疗法的新型非受体依赖性递送系统。

RTB Lectin: a novel receptor-independent delivery system for lysosomal enzyme replacement therapies.

作者信息

Acosta Walter, Ayala Jorge, Dolan Maureen C, Cramer Carole L

机构信息

Arkansas Biosciences Institute at Arkansas State University-Jonesboro, State University, Arkansas, USA.

BioStrategies LC, State University, Arkansas, USA.

出版信息

Sci Rep. 2015 Sep 18;5:14144. doi: 10.1038/srep14144.

Abstract

Enzyme replacement therapies have revolutionized patient treatment for multiple rare lysosomal storage diseases but show limited effectiveness for addressing pathologies in "hard-to-treat" organs and tissues including brain and bone. Here we investigate the plant lectin RTB as a novel carrier for human lysosomal enzymes. RTB enters mammalian cells by multiple mechanisms including both adsorptive-mediated and receptor-mediated endocytosis, and thus provides access to a broader array of organs and cells. Fusion proteins comprised of RTB and human α-L-iduronidase, the corrective enzyme for Mucopolysaccharidosis type I, were produced using a tobacco-based expression system. Fusion products retained both lectin selectivity and enzyme activity, were efficiently endocytosed into human fibroblasts, and corrected the disease phenotype of mucopolysaccharidosis patient fibroblasts in vitro. RTB-mediated delivery was independent of high-mannose and mannose-6-phosphate receptors, which are exploited for delivery of currently approved lysosomal enzyme therapeutics. Thus, the RTB carrier may support distinct in vivo pharmacodynamics with potential to address hard-to-treat tissues.

摘要

酶替代疗法彻底改变了多种罕见溶酶体贮积病的患者治疗方式,但在解决包括脑和骨在内的“难治性”器官和组织的病变方面效果有限。在此,我们研究植物凝集素RTB作为人溶酶体酶的新型载体。RTB通过多种机制进入哺乳动物细胞,包括吸附介导的内吞作用和受体介导的内吞作用,从而能够进入更广泛的器官和细胞。使用基于烟草的表达系统生产了由RTB和人α-L-艾杜糖醛酸酶(I型黏多糖贮积症的校正酶)组成的融合蛋白。融合产物保留了凝集素选择性和酶活性,能有效被内吞进入人成纤维细胞,并在体外校正了黏多糖贮积症患者成纤维细胞的疾病表型。RTB介导的递送不依赖于高甘露糖和甘露糖-6-磷酸受体,而目前批准的溶酶体酶疗法的递送则利用这些受体。因此,RTB载体可能支持独特的体内药效学,有潜力解决难治性组织的问题。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2dd1/4585660/6e4a764a2cfd/srep14144-f1.jpg

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