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首页> 外文期刊>Applied Microbiology and Biotechnology >Sustained release of PI3K inhibitor from PHA nanoparticles and in vitro growth inhibition of cancer cell lines
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Sustained release of PI3K inhibitor from PHA nanoparticles and in vitro growth inhibition of cancer cell lines

机译:从PHA纳米粒子中持续释放PI3K抑制剂并抑制癌细胞系的体外生长

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The phosphoinositide-3-kinases (PI3Ks) are a conserved family of lipid kinases that phosphorylate the 3-hydroxyl group of phosphatidylinositols in response to extracellular stimuli. PI3K pathway is enrolled in different kinds of human cancer and plays a prominent role in cancer cell growth and survival. Several PI3K inhibitors have been recently identified but some PI3K inhibitors with high potency in vitro do not show satisfactory effects in animal cancer models because of the poor pharmaceutical properties in vivo such as poor solubility, instability, and fast plasma clearance rate. In this study, we developed a sustained release system of PI3K inhibitor (TGX221) based on polyhydroxyalkanoate nanoparticles (NP) and used it to block proliferation of cancer cell lines. TGX221 was gradually released from PHA-based NP and growth of cancer cell lines was significantly slower in NP-TGX221-treated cells than in either negative controls or in cells receiving free TGX221. Since poor bioavailability and limited in vivo half-life are common features of hydrophobic PI3K inhibitors, our results open the way to similar formulation of other PI3K blockers and to new strategies in cancer treatment.
机译:磷酸肌醇-3-激酶(PI3Ks)是脂质激酶的保守家族,其响应于细胞外刺激而磷酸化磷脂酰肌醇的3-羟基基团。 PI3K通路参与了各种人类癌症,并且在癌细胞的生长和存活中起着重要作用。最近已鉴定出几种PI3K抑制剂,但由于具有不良的体内药物特性(如不良的溶解性,不稳定性和快速的血浆清除率),某些在体外具有高效能的PI3K抑制剂在动物癌症模型中未显示令人满意的效果。在这项研究中,我们开发了基于聚羟基链烷酸酯纳米颗粒(NP)的PI3K抑制剂(TGX221)缓释系统,并将其用于阻断癌细胞系的增殖。 TGX221从基于PHA的NP中逐渐释放,并且在NP-TGX221处理的细胞中,癌细胞系的生长明显慢于阴性对照或接受游离TGX221的细胞。由于不良的生物利用度和有限的体内半衰期是疏水性PI3K抑制剂的共同特征,因此我们的结果为其他PI3K阻滞剂的相似制剂和癌症治疗新策略开辟了道路。

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