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载紫杉醇的透明质酸交联纳米颗粒诱导细胞凋亡及其在调控AKT和RhoA中的作用。

Induction of apoptosis and role of paclitaxel-loaded hyaluronic acid-crosslinked nanoparticles in the regulation of AKT and RhoA.

作者信息

Chaudhry Gul-E-Saba, Akim Abdah, Zafar Muhammad Naveed, Abdullah M A, Sung Yeong Yik, Muhammad Tengku Sifzizul Tengku

机构信息

Institute of Marine Biotechnology, Universiti Malaysia Terengganu, Kuala Terengganu, Malaysia.

Department of Chemical Engineering, Universiti Teknologi Petronas, Perak, Malaysia.

出版信息

J Adv Pharm Technol Res. 2020 Jul-Sep;11(3):101-106. doi: 10.4103/japtr.JAPTR_26_20. Epub 2020 Jul 14.

Abstract

Cancer is a complex multifactorial disease and leading causes of death worldwide. Despite the development of many anticancer drugs, there is a reduced survival rate due to severe side effects. The nontargeted approach of convention drugs is one of the leading players in context to toxicity. Hyaluronan is a versatile bio-polymer and ligand of the receptor (CD44) on cancer cells. The MCF-7 and HT-29 cancer cell lines treated with hyaluronic acid-paclitaxel (HA-PTX) showed the distinguishing morphological features of apoptosis. Flow cytometric analysis showed that HA-PTX induces apoptosis as a significant mode of cell death. The activation level of tumor suppressor protein (p53) increased after PTX treatment in MCF-7, but no changes observed in HT-29 might be due to hereditary mutations. The lack of suppression in AKT and Rho A protein suggest the use of possible inhibitors in future studies which might could play a role in increasing the sensitivity of drug towards mutated cells line and reducing the possibilities for cancer cell survival, migration, and metastasis.

摘要

癌症是一种复杂的多因素疾病,也是全球主要的死亡原因。尽管开发了许多抗癌药物,但由于严重的副作用,生存率仍然降低。传统药物的非靶向方法是导致毒性的主要因素之一。透明质酸是一种多功能生物聚合物,也是癌细胞上受体(CD44)的配体。用透明质酸-紫杉醇(HA-PTX)处理的MCF-7和HT-29癌细胞系显示出凋亡的明显形态特征。流式细胞术分析表明,HA-PTX诱导凋亡作为一种重要的细胞死亡方式。在MCF-7中,紫杉醇治疗后肿瘤抑制蛋白(p53)的激活水平增加,但在HT-29中未观察到变化,这可能是由于遗传突变。AKT和Rho A蛋白缺乏抑制作用表明,在未来的研究中可能需要使用抑制剂,这可能有助于提高药物对突变细胞系的敏感性,并降低癌细胞存活、迁移和转移的可能性。

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