Application of Collagen-Model Triple-Helical Peptide-Amphiphiles for CD44-Targeted Drug Delivery Systems.

Journal of drug delivery Pub Date : 2012-01-01 Epub Date: 2012-11-14 DOI:10.1155/2012/592602
Margaret W Ndinguri, Alexander Zheleznyak, Janelle L Lauer, Carolyn J Anderson, Gregg B Fields
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引用次数: 24

Abstract

Cancer treatment by chemotherapy is typically accompanied by deleterious side effects, attributed to the toxic action of chemotherapeutics on proliferating cells from nontumor tissues. The cell surface proteoglycan CD44 has been recognized as a cancer stem cell marker. The present study has examined CD44 targeting as a way to selectively deliver therapeutic agents encapsulated inside colloidal delivery systems. CD44/chondroitin sulfate proteoglycan binds to a triple-helical sequence derived from type IV collagen, α1(IV)1263-1277. We have assembled a peptide-amphiphile (PA) in which α1(IV)1263-1277 was sandwiched between 4 repeats of Gly-Pro-4-hydroxyproline and conjugated to palmitic acid. The PA was incorporated into liposomes composed of DSPG, DSPC, cholesterol, and DSPE-PEG-2000 (1 : 4 : 5 : 0.5). Doxorubicin-(DOX-)loaded liposomes with and without 10% α1(IV)1263-1277 PA were found to exhibit similar stability profiles. Incubation of DOX-loaded targeted liposomes with metastatic melanoma M14#5 and M15#11 cells and BJ fibroblasts resulted in IC(50) values of 9.8, 9.3, and >100 μM, respectively. Nontargeted liposomes were considerably less efficacious for M14#5 cells. In the CD44(+) B16F10 mouse melanoma model, CD44-targeted liposomes reduced the tumor size to 60% of that of the untreated control, whereas nontargeted liposomes were ineffective. These results suggest that PA targeted liposomes may represent a new class of nanotechnology-based drug delivery systems.

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胶原-模型三螺旋肽-两亲体在cd44靶向药物递送系统中的应用
由于化疗药物对来自非肿瘤组织的增殖细胞的毒性作用,化疗治疗癌症通常伴随着有害的副作用。细胞表面蛋白多糖CD44被认为是癌症干细胞的标志物。目前的研究已经检查了CD44靶向作为一种选择性递送包裹在胶体递送系统中的治疗剂的方法。CD44/硫酸软骨素蛋白聚糖结合到源自IV型胶原α1(IV)1263-1277的三螺旋序列。我们组装了一个肽-两亲体(PA),其中α1(IV)1263-1277被夹在gly - pro -4-羟基脯氨酸的4个重复序列之间,并与棕榈酸偶联。将PA掺入由DSPG、DSPC、胆固醇和DSPE-PEG-2000组成的脂质体中(1:1:5:5:0.5)。负载阿霉素(DOX)的脂质体与不含10% α1(IV)1263-1277 PA的脂质体具有相似的稳定性。在转移性黑色素瘤M14#5和M15#11细胞以及BJ成纤维细胞中,负载dox的靶向脂质体的IC(50)值分别为9.8、9.3和>100 μM。非靶向脂质体对M14#5细胞的效果明显较差。在CD44(+) B16F10小鼠黑色素瘤模型中,CD44靶向脂质体将肿瘤大小缩小至未治疗对照组的60%,而非靶向脂质体则无效。这些结果表明,PA靶向脂质体可能代表了一类新的基于纳米技术的药物传递系统。
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来源期刊
Journal of drug delivery
Journal of drug delivery PHARMACOLOGY & PHARMACY-
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