Quercetin acts as a P-gp modulator via impeding signal transduction from nucleotide-binding domain to transmembrane domain

多重耐药 跨膜结构域 癌细胞 对接(动物) 化学 跨膜蛋白 流出 生物信息学 环核苷酸结合域 槲皮素 生物 生物化学 癌症 核苷酸 受体 医学 基因 遗传学 护理部 抗生素 抗氧化剂
作者
Ashutosh Singh,Sandesh Kumar Patel,Prateek Kumar,Kanhu Charan Das,Deepanshu Verma,Rohit Sharma,Timir Tripathi,Rajanish Giri,Natália Martins,Neha Garg
出处
期刊:Journal of Biomolecular Structure & Dynamics [Taylor & Francis]
卷期号:40 (10): 4507-4515 被引量:37
标识
DOI:10.1080/07391102.2020.1858966
摘要

The inherent ability of the cancer cells to resist chemotherapeutic agents is a major challenge in drug discovery. Chemotherapy is one of the most widely used treatment methods for cancer, but due to multidrug resistance (MDR) development in cancer cells, the healing procedure often fails. Various factors impart cancer resistance to cells; among them, P-glycoprotein (P-gp) overexpression is directly linked to MDR in cancer cells. P-gp leads to the efflux of drug molecules to the extracellular space. Several molecules have been reported to inhibit the P-gp activity. Among them, quercetin has revealed a great potential to modulate P-gp activity. However, the mechanistic understanding of quercetin induced modulation is not entirely elucidated. In the present work, we showed that quercetin binds in the interacting region between the transmembrane domain and nucleotide-binding domain out of the three plausible binding sites of P-gp and restrict the conformational change from inward- to outward-facing conformation of P-gp. Due to the absence of the inward-facing structure of human P-gp, we first modeled an inward-facing P-gp structure. Using molecular docking, the interacting residues of P-gp were identified, and the stability and interaction dynamics of the complex were studied using molecular dynamics simulation. Our work reveals the mechanistic understanding of quercetin induced modulation of P-gp and indicates its importance in cancer treatment.Communicated by Ramaswamy H. Sarma.
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