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Development of an anti-microbial peptide-mediated liposomal delivery system: a novel approach towards pH-responsive anti-microbial peptides

机译:抗微生物肽介导的脂质体递送系统的开发:针对pH响应的抗微生物肽的新方法

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Abstract On one hand, the application of anti-microbial peptides (AMPs) in the construction of AMPs-mediated drug delivery system has not yet been fully exploited; on the other hand, its non-selectivity in vivo has also limited its clinical application. In this work, we chose one pH-responsive peptide, [D]-H6L9, and functionalized it onto the surface of liposomes (D-Lip). The protonation of histidines in the sequence of [D]-H6L9 under pH 6.3 could switch the surface charge of D-Lip from negative (under pH 7.4) to positive (under pH 6.3), and the cellular uptake and tumor spheroids uptake were increased accordingly. Lysosome co-localization assay suggested that there was only little overlap of D-Lip with lysosomes in 12?h, which indicated that D-Lip could escape lysosomes effectively. In vivo biodistribution assay on C26 tumor-bearing BALB/C mice showed that DiR-labeled D-Lip could reach tumors as much as PEG-Lip, and both tumor slices and quantitative measurement of dispersed cells of in vivo tumors by flow cytometry demonstrated that D-Lip could be taken up by tumors more efficiently. Therefore, we have established an anti-microbial peptide-mediated liposomal delivery system for tumor delivery.
机译:摘要一方面,抗菌肽(AMPs)在AMPs介导的药物递送系统的构建中尚未得到充分利用。另一方面,其在体内的非选择性也限制了其临床应用。在这项工作中,我们选择了一种pH响应肽[D] -H 6 L 9 ,并将其功能化到脂质体(D-Lip)的表面上。在pH 6.3下,[D] -H 6 L 9 序列中组氨酸的质子化可以使D-Lip的表面电荷从负(pH 7.4)变为阳性(在pH 6.3下),细胞摄取和肿瘤球体摄取相应增加。溶酶体共定位分析表明,D-Lip与溶酶体在12?h内几乎没有重叠,这表明D-Lip可以有效逃逸溶酶体。对带有C26肿瘤的BALB / C小鼠的体内生物分布测定表明,DiR标记的D-Lip可以达到与PEG-Lip一样多的肿瘤,并且通过流式细胞术对肿瘤切片和体内肿瘤分散细胞的定量测量表明: D-Lip可以更有效地被肿瘤吸收。因此,我们建立了抗微生物肽介导的脂质体递送系统用于肿瘤递送。

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