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基于三嗪的小分子的超分子自组装:靶向癌细胞中的内质网。

Supramolecular self-assembly of triazine-based small molecules: targeting the endoplasmic reticulum in cancer cells.

机构信息

Department of Chemistry, Indian Institute of Science Education and Research (IISER)-Pune, Dr. Homi Bhabha Road, Pashan, Pune, 411008, India.

出版信息

Nanoscale. 2019 Feb 14;11(7):3326-3335. doi: 10.1039/c8nr08682f.

DOI:10.1039/c8nr08682f
PMID:30724283
Abstract

The endoplasmic reticulum (ER) is one of the most important organelles controlling myriads of cellular functions including protein folding/misfolding/unfolding, calcium ion homeostasis and lipid biosynthesis. Subsequently, due to its functional dysregulation in cancer cells, it has emerged as an interesting target for anti-cancer therapy. However, specific targeting of the ER in cancer cells remains a major challenge due to the lack of ER-selective chemical tools. Furthermore, for performing multiple cellular functions the ER is dependent on the nucleus through complicated cross-talk. Herein, we have engineered a supramolecular self-assembled hexameric rosette structure from two small molecules: tri-substituted triazine and 5-fluorouracil (5-FU). This rosette structure consists of an ER-targeting moiety with a fluorescence tag, an ER-stress inducer and a nuclear DNA damaging drug simultaneously, which further self-assembled into an ER-targeting spherical nano-scale particle (ER-NP). These ER-NPs internalized into HeLa cervical cancer cells by macropinocytosis and specifically localized into the ER to induce ER stress and DNA damage leading to cell death through apoptosis. Interestingly, ER-NPs initiated autophagy, inhibited by a combination of ER-NPs and chloroquine (CQ) to augment cancer cell death. This work has the potential to exploit the concept of supramolecular self-assembly into developing novel nano-scale materials for specific sub-cellular targeting of multiple organelles for future anti-cancer therapy.

摘要

内质网(ER)是控制包括蛋白质折叠/错误折叠/展开、钙离子稳态和脂质生物合成在内的多种细胞功能的最重要细胞器之一。随后,由于其在癌细胞中的功能失调,它已成为癌症治疗的一个有趣靶点。然而,由于缺乏 ER 选择性化学工具,癌细胞中 ER 的特异性靶向仍然是一个主要挑战。此外,为了执行多种细胞功能,内质网通过复杂的交叉对话依赖于细胞核。在此,我们设计了一种由两个小分子构建的超分子自组装六聚体蔷薇花结构:三取代三嗪和 5-氟尿嘧啶(5-FU)。这种蔷薇花结构由具有荧光标记的 ER 靶向部分、ER 应激诱导剂和核 DNA 损伤药物组成,它们进一步自组装成 ER 靶向的球形纳米级颗粒(ER-NP)。这些 ER-NP 通过巨胞饮作用进入 HeLa 宫颈癌细胞,并特异性定位于 ER 以诱导 ER 应激和 DNA 损伤,通过细胞凋亡导致细胞死亡。有趣的是,ER-NP 通过自噬启动,通过 ER-NP 和氯喹(CQ)联合抑制以增强癌细胞死亡。这项工作有可能利用超分子自组装的概念来开发新型纳米级材料,用于未来的癌症治疗中针对多个细胞器的特定亚细胞靶向。

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