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来自鱼精蛋白的无毒膜转位肽,低分子量鱼精蛋白(LMWP),用于增强细胞内蛋白质递送:体外和体内研究。

Nontoxic membrane translocation peptide from protamine, low molecular weight protamine (LMWP), for enhanced intracellular protein delivery: in vitro and in vivo study.

作者信息

Park Yoon Jeong, Chang Li-Chien, Liang Jun Feng, Moon Cheol, Chung Chong-Pyoung, Yang Victor C

机构信息

Craniomaxillofacial Reconstructive Science Major, School of Dentistry and Intellectual Biointerface Engineering Center, Seoul National University, Seoul, South Korea.

出版信息

FASEB J. 2005 Sep;19(11):1555-7. doi: 10.1096/fj.04-2322fje. Epub 2005 Jul 20.

Abstract

Naturally derived, nontoxic peptides from protamine by the authors, termed low molecular weight protamines (LMWPs), possess high arginine content and carry significant sequence similarity to that of TAT, by far the most potent protein transduction domain peptide. Therefore, it was hypothesized that these LMWPs would also inherit the similar translocation activity across the cell membrane, which enables any impermeable species to be transduced into the cells. LMWPs were prepared by enzymatic digestion of protamine, examined their capability of transducing an impermeable protein toxin into the tumor cells by chemical conjugation, and determined cytotoxicity of transduced protein toxin (e.g., gelonin) against cancer cell lines and a tumor-bearing mouse. In vitro results showed that LMWPs could indeed translocate themselves into several mammalian cell lines as efficiently as TAT, thereby transducing impermeable gelonin into the cells by chemical conjugation. In vivo studies further confirmed that LMWP could carry an impermeable gelonin across the tumor mass and subsequently inhibit the tumor growth. In conclusion, the presence of equivalent cell translocation potency, absence of toxicity of peptide itself, and the suitability for low-cost production by simple enzymatic digestion could expand the range of clinical applications of LMWPs, including medical imaging and gene/protein therapies.

摘要

作者从鱼精蛋白中获得的天然衍生无毒肽,称为低分子量鱼精蛋白(LMWP),其精氨酸含量高,与目前最有效的蛋白质转导结构域肽TAT具有显著的序列相似性。因此,有人推测这些LMWP也会继承类似的跨细胞膜转运活性,从而使任何不能渗透的物质能够被转导进入细胞。通过对鱼精蛋白进行酶解制备LMWP,通过化学偶联检测其将一种不能渗透的蛋白毒素转导到肿瘤细胞中的能力,并测定转导的蛋白毒素(如相思豆毒素)对癌细胞系和荷瘤小鼠的细胞毒性。体外实验结果表明,LMWP确实能像TAT一样有效地将自身转运到几种哺乳动物细胞系中,从而通过化学偶联将不能渗透的相思豆毒素转导到细胞中。体内研究进一步证实,LMWP能够携带不能渗透的相思豆毒素穿过肿瘤组织,随后抑制肿瘤生长。总之,LMWP具有同等的细胞转运能力、肽本身无毒以及适合通过简单酶解进行低成本生产等特性,这可能会扩大LMWP在临床应用中的范围,包括医学成像以及基因/蛋白质治疗。

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