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带 RGD 序列的两亲性阳离子脂肽作为基因载体。

Amphiphilic cationic lipopeptides with RGD sequences as gene vectors.

机构信息

Key Laboratory of Biomedical Polymers of Ministry of Education & Department of Chemistry, Wuhan University, Wuhan 430072, China.

出版信息

Org Biomol Chem. 2010 Jul 21;8(14):3142-8. doi: 10.1039/c003538f. Epub 2010 May 18.

Abstract

Two kinds of arginine-rich amphiphilic lipopeptides with hydrophobic aliphatic tails (C(12)GR(8)GDS, LP1 and C(18)GR(8)GDS, LP2) were designed and synthesized as functional gene vectors. With hydrophobic tail modification, these amphiphilic lipopeptides could bind DNA more efficiently and form stable spherical complexes in comparison with the control peptide (AcGR(8)GDS, P1). Moreover, the size and zeta potential results demonstrated the charge density and stability of the vector/DNA complexes could be improved with the increasing length of the aliphatic tails. In vitro transfection experiments showed that LP1 and LP2 could induce much higher gene expression level (luciferase expression) as compared with P1. Due to the incorporation of arginine-glycine-aspartic acid (RGD) sequences which could be specifically recognized by integrins alpha(upsilon)beta(3) and alpha(upsilon)beta(5) over-expressed on cancer cells, these lipopeptides could be specifically recognized by cancer cells, i.e. LP1 and LP2 exhibited relatively higher transfection efficiency in HeLa cell line than that of P2 and P3 without RGD sequence. While the transfection efficiencies of LP2 and P2 were similar in 293T cells. Lipopeptides exhibited very low cell cytotoxicity in both HeLa and 293T cell lines even at high concentration.

摘要

两种精氨酸丰富的两亲性脂肽具有疏水性脂肪尾部(C(12)GR(8)GDS,LP1 和 C(18)GR(8)GDS,LP2)被设计和合成作为功能性基因载体。通过疏水尾部修饰,与对照肽(AcGR(8)GDS,P1)相比,这些两亲性脂肽能够更有效地结合 DNA 并形成稳定的球形复合物。此外,尺寸和 zeta 电位结果表明,载体/DNA 复合物的电荷密度和稳定性可以通过增加脂肪尾部的长度来提高。体外转染实验表明,LP1 和 LP2 可诱导比 P1 更高的基因表达水平(荧光素酶表达)。由于掺入精氨酸-甘氨酸-天冬氨酸(RGD)序列,这些序列可以被整合素 alpha(upsilon)beta(3)和 alpha(upsilon)beta(5)特异性识别,这些脂肽可以被癌细胞特异性识别,即 LP1 和 LP2 在 HeLa 细胞系中比没有 RGD 序列的 P2 和 P3 具有相对较高的转染效率。而 LP2 和 P2 在 293T 细胞中的转染效率相似。脂肽在 HeLa 和 293T 细胞系中均表现出非常低的细胞毒性,即使在高浓度下也是如此。

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