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通过主体 - [2]轮烷对荧光素化肽进行细胞内递送的研究。

Investigation of the intracellular delivery of fluoresceinated peptides by a host-[2]rotaxane.

作者信息

Wang Xiaoyang, Bao Xiaofeng, McFarland-Mancini Molly, Isaacsohn Idit, Drew Angela F, Smithrud David B

机构信息

Department of Chemistry, University of Cincinnati, Cincinnati, Ohio 45221, USA.

出版信息

J Am Chem Soc. 2007 Jun 13;129(23):7284-93. doi: 10.1021/ja067928x. Epub 2007 May 22.

Abstract

The development of methods to transport peptides into cells via a passive mechanism would greatly aid in the development of therapeutic agents. We recently demonstrated that an impermeable fluoresceinated pentapeptide enters the cytoplasm and nucleus of COS 7 cells in the presence of a host-[2]rotaxane by a mechanism that does not depend on an active cell-mediated process. In this report, we further investigate the ability of the host-[2]rotaxane to deliver peptides possessing a wide range of polarities (negatively charged, positively charged, polar, and apolar side chains) into live cells. Only in the presence of the host-[2]rotaxane were the Fl-peptides taken up by COS 7 and ES2 cells. Flow cytometry experiments demonstrated that the level of delivery is largely temperature and adenosine 5'-triphosphate (ATP) independent, and the membranes remain intact. Although the level of transport does depend upon the nature of the side chains, it does not correlate with calculated LogD values, indicating that an additional interaction with the host-[2]rotaxane is modifying the permeability properties of the peptide. The amount of Fl-peptides transported from an aqueous phase into a chloroform phase in the presence of the host-[2]rotaxane correlates with the intensity of cellular fluorescence. Extraction and U-tube studies show that the Fl-peptide can be released from its complex with the host-[2]rotaxane into an aqueous phase, and the host-[2]rotaxane can transport a greater than a stoichiometric amount of an Fl-peptide through a CHCl3 layer. These studies demonstrate the utility of the host-[2]rotaxane in delivering peptides of all polarities across a cell membrane.

摘要

开发通过被动机制将肽转运到细胞内的方法将极大地有助于治疗药物的开发。我们最近证明,一种不可渗透的荧光五肽在存在主体-[2]轮烷的情况下,通过一种不依赖于细胞主动介导过程的机制进入COS 7细胞的细胞质和细胞核。在本报告中,我们进一步研究了主体-[2]轮烷将具有广泛极性(带负电荷、带正电荷、极性和非极性侧链)的肽递送至活细胞的能力。只有在存在主体-[2]轮烷的情况下,荧光肽才会被COS 7和ES2细胞摄取。流式细胞术实验表明,递送水平在很大程度上与温度和腺苷5'-三磷酸(ATP)无关,并且细胞膜保持完整。虽然转运水平确实取决于侧链的性质,但它与计算出的LogD值不相关,这表明与主体-[2]轮烷的额外相互作用正在改变肽的通透性。在存在主体-[2]轮烷的情况下,从水相转运到氯仿相中的荧光肽的量与细胞荧光强度相关。萃取和U型管研究表明,荧光肽可以从其与主体-[2]轮烷的复合物中释放到水相中,并且主体-[2]轮烷可以通过CHCl3层转运超过化学计量的荧光肽。这些研究证明了主体-[2]轮烷在跨细胞膜递送所有极性肽方面的实用性。

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