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首页> 外文期刊>Saudi Pharmaceutical Journal >Design and encapsulation of anticancer dual HSP27 and HER2 inhibitor into low density lipoprotein to target ovarian cancer cells
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Design and encapsulation of anticancer dual HSP27 and HER2 inhibitor into low density lipoprotein to target ovarian cancer cells

机译:将抗癌双HSP27和HER2抑制剂的设计和封装成低密度脂蛋白以靶向卵巢癌细胞

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Tumor cells overexpress low-density lipoprotein (LDL) receptors (LDL-r). Hence, LDL is proposed as a targeting shuttle of anticancer drugs. Therefore, the objective of this study was to synthesize a dual inhibitor of heat shock protein 27 (HSP27) and human epidermal growth factor receptor 2 (HER2) conjugated with cholesterol and encapsulated into LDL for selective targeting of ovarian cancer cells. In the present study, the anticancer agent and its cholesterol conjugate were successfully prepared and characterized physically for color, shape, and melting point. Moreover, the compounds were chemically characterized for 1 H NMR and 13 C NMR spectra using FTIR and LCMS/MS. Our results revealed that the prepared anticancer agent and its cholesterol conjugate elicited dual HSP27 and HER2 inhibition, as confirmed using western blotting. The anticancer agent (compound D) entered cells and targeted the HSP27 function, thereby reducing HER2 expression. However, a cholesterol-conjugated anticancer agent (compound F) had high cellular uptake and inhibited the growth of SKOV3 cells after encapsulation into LDL. The obtained results concluded that the design of an LDL-encapsulated cholesterol-conjugated HSP27-HER2 dual inhibitor may be a promising approach to realize specific targeted achieve killing of ovarian cancer.
机译:肿瘤细胞过表达低密度脂蛋白(LDL)受体(LDL-R)。因此,LDL被提出为抗癌药物的靶向穿梭。因此,本研究的目的是合成与胆固醇缀合的热休克蛋白27(HSP27)和人表皮生长因子受体2(HER2)的双重抑制剂,并将其包封成LDL以选择性靶向卵巢癌细胞。在本研究中,成功​​制备抗癌剂及其胆固醇缀合物,用于物理上以用于颜色,形状和熔点。此外,化学表征使用FTIR和LCMS / MS化学表征1 H NMR和13 C NMR光谱。我们的研究结果表明,使用蛋白质印迹确认,制备的抗癌剂及其胆固醇共轭引发了双HSP27和HER2抑制。抗癌剂(化合物D)进入细胞并靶向HSP27功能,从而减少了HER2表达。然而,胆固醇缀合的抗癌剂(化合物F)具有高细胞摄取,并在包封到LDL后抑制SkoV3细胞的生长。得到的结果得出结论,LDL封装的胆固醇缀合的HSP27-HER2双重抑制剂的设计可能是实现卵巢癌的特定靶向杀伤的有希望的方法。

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