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阿戊聚糖-叶酸-药物偶联物用于靶向递送至叶酸受体过表达细胞和靶激活释放抗癌药物。

Arabinogalactan-folic acid-drug conjugate for targeted delivery and target-activated release of anticancer drugs to folate receptor-overexpressing cells.

机构信息

Laboratory of Biopolymers and Food Nanotechnology, Department of Biotechnology and Food Engineering, The Russell Berrie Nanotechnology Institute, Israel.

出版信息

Biomacromolecules. 2010 Jan 11;11(1):294-303. doi: 10.1021/bm900853z.

Abstract

Folic acid (FA) is a high affinity ligand (K(d) = 0.1-1 nM) of folate receptors (FRs) responsible for cellular uptake of folates via receptor-mediated endocytosis. FRs are frequently overexpressed in malignant epithelial cells including ovary, brain, kidney, breast, colon, and lung. FR has emerged as a target for the differential-delivery of anticancer chemotherapeutics with several FA-linked therapeutic agents currently undergoing clinical trials. Here we show that by tethering both FA and the anticancer drug methotrexate (MTX) to arabinogalactan (AG), a highly branched natural polysaccharide with unusual water solubility, a targeted biomacromolecular nanovehicle is formed, which can differentially deliver a cytotoxic cargo into FR-overexpressing cells. Moreover, by linking MTX via an endosomally cleavable peptide (GFLG), we demonstrate a target-activated release mechanism. This FA-AG-GFLG-MTX drug conjugate displayed 6.3-fold increased cytotoxic activity to FR-overexpressing cells compared to their FR-lacking counterparts. These findings establish a novel FA-tethered polymeric nanoconjugate for the targeted delivery of antitumor agents into cancer cells overexpressing FR.

摘要

叶酸(FA)是叶酸受体(FR)的高亲和力配体(K(d)=0.1-1 nM),负责通过受体介导的内吞作用将叶酸摄取到细胞内。FR 在恶性上皮细胞中经常过度表达,包括卵巢、脑、肾、乳腺、结肠和肺。FR 已成为抗癌化疗药物差异递送的靶点,目前有几种与 FA 相关的治疗剂正在进行临床试验。在这里,我们表明,通过将 FA 和抗癌药物甲氨蝶呤(MTX)连接到阿拉伯半乳聚糖(AG)上,形成一种靶向生物大分子纳米载体,该载体可以将细胞毒性货物差异递送到 FR 过度表达的细胞中。此外,通过将 MTX 通过内体可切割肽(GFLG)连接,我们证明了一种靶向激活的释放机制。与缺乏 FR 的细胞相比,这种 FA-AG-GFLG-MTX 药物偶联物对 FR 过度表达的细胞的细胞毒性活性增加了 6.3 倍。这些发现建立了一种新型的 FA 连接的聚合物纳米偶联物,用于将抗肿瘤剂靶向递送到过度表达 FR 的癌细胞中。

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