Link Nils, Aubel Corinne, Kelm Jens M, Marty René R, Greber David, Djonov Valentin, Bourhis Jean, Weber Wilfried, Fussenegger Martin
Institute for Chemical and Bio-Engineering (ICB), Swiss Federal Institute of Technology, ETH Hoenggerberg, HCI F115, Wolfgang-Pauli-Strasse 10, CH-8093 Zurich, Switzerland.
Nucleic Acids Res. 2006 Jan 30;34(2):e16. doi: 10.1093/nar/gnj014.
The straightforward production and dose-controlled administration of protein therapeutics remain major challenges for the biopharmaceutical manufacturing and gene therapy communities. Transgenes linked to HIV-1-derived vpr and pol-based protease cleavage (PC) sequences were co-produced as chimeric fusion proteins in a lentivirus production setting, encapsidated and processed to fusion peptide-free native protein in pseudotyped lentivirions for intracellular delivery and therapeutic action in target cells. Devoid of viral genome sequences, protein-transducing nanoparticles (PTNs) enabled transient and dose-dependent delivery of therapeutic proteins at functional quantities into a variety of mammalian cells in the absence of host chromosome modifications. PTNs delivering Manihot esculenta linamarase into rodent or human, tumor cell lines and spheroids mediated hydrolysis of the innocuous natural prodrug linamarin to cyanide and resulted in efficient cell killing. Following linamarin injection into nude mice, linamarase-transducing nanoparticles impacted solid tumor development through the bystander effect of cyanide.
蛋白质治疗药物的直接生产和剂量可控给药仍然是生物制药制造和基因治疗领域面临的主要挑战。与源自HIV-1的vpr和基于pol的蛋白酶切割(PC)序列相连的转基因作为嵌合融合蛋白在慢病毒生产环境中共同产生,在假型慢病毒颗粒中被包装并加工成无融合肽的天然蛋白,用于细胞内递送并在靶细胞中发挥治疗作用。蛋白质转导纳米颗粒(PTN)不含病毒基因组序列,能够在不进行宿主染色体修饰的情况下,以功能量将治疗性蛋白质瞬时且剂量依赖性地递送至多种哺乳动物细胞中。将木薯亚麻苦苷酶递送至啮齿动物或人类肿瘤细胞系及球体中的PTN介导了无害天然前药亚麻苦苷水解为氰化物,并导致有效的细胞杀伤。在将亚麻苦苷注射到裸鼠体内后,转导亚麻苦苷酶的纳米颗粒通过氰化物的旁观者效应影响实体瘤的发展。
Zotero 插件
