首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >PNAS Plus: Peptides of pHLIP family for targeted intracellular and extracellular delivery of cargo molecules to tumors
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PNAS Plus: Peptides of pHLIP family for targeted intracellular and extracellular delivery of cargo molecules to tumors

机译:PNAS Plus:pHLIP家族的肽用于靶向将货物分子细胞内和细胞外递送至肿瘤

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摘要

The pH (low) insertion peptides (pHLIPs) target acidity at the surfaces of cancer cells and show utility in a wide range of applications, including tumor imaging and intracellular delivery of therapeutic agents. Here we report pHLIP constructs that significantly improve the targeted delivery of agents into tumor cells. The investigated constructs include pHLIP bundles (conjugates consisting of two or four pHLIP peptides linked by polyethylene glycol) and Var3 pHLIPs containing either the nonstandard amino acid, γ-carboxyglutamic acid, or a glycine−leucine−leucine motif. The performance of the constructs in vitro and in vivo was compared with previous pHLIP variants. A wide range of experiments was performed on nine constructs including (i) biophysical measurements using steady-state and kinetic fluorescence, circular dichroism, and oriented circular dichroism to study the pH-dependent insertion of pHLIP variants across the membrane lipid bilayer; (ii) cell viability assays to gauge the pH-dependent potency of peptide-toxin constructs by assessing the intracellular delivery of the polar, cell-impermeable cargo molecule amanitin at physiological and low pH (pH 7.4 and 6.0, respectively); and (iii) tumor targeting and biodistribution measurements using fluorophore-peptide conjugates in a breast cancer mouse model. The main principles of the design of pHLIP variants for a range of medical applications are discussed.
机译:pH(低)插入肽(pHLIPs)靶向癌细胞表面的酸度,并在包括肿瘤成像和治疗剂细胞内递送在内的广泛应用中显示出实用性。在这里,我们报道了pHLIP构建体,该构建体显着改善了药物向肿瘤细胞的靶向递送。研究的构建体包括pHLIP束(由聚乙二醇连接的两个或四个pHLIP肽组成的结合物)和含有非标准氨基酸,γ-羧基谷氨酸或甘氨酸-亮氨酸-亮氨酸基序的Var3 pHLIP。将构建体在体外和体内的性能与以前的pHLIP变体进行了比较。在九种构建体上进行了广泛的实验,包括:(i)使用稳态和动力学荧光进行生物物理测量,圆二色性和定向圆二色性,以研究pHLIP变体跨膜脂质双层插入的pH依赖性; (ii)通过评估在生理和低pH值(分别为pH 7.4和6.0)下极性,细胞不渗透性载脂蛋白amanitin在细胞内的传递来评估肽毒素构建物的pH依赖性效价的细胞活力测定; (iii)在乳腺癌小鼠模型中使用荧光团-肽缀合物的肿瘤靶向和生物分布测量。讨论了用于多种医疗应用的pHLIP变体设计的主要原理。

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