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In Silico Quantitative Structure-Activity Relationship Studies on P-gp Modulators of Tetrahydroisoquinoline-Ethyl-Phenylamine Series

机译：四氢异喹啉-乙基-苯胺系列的P-gp调节剂的计算机定量结构-活性关系的研究

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BackgroundMultidrug resistance (MDR) is a major obstacle in cancer chemotherapy. The drug efflux by a transport protein is the main reason for MDR. In humans, MDR mainly occurs when the ATP-binding cassette (ABC) family of proteins is overexpressed simultaneously. P-glycoprotein (P-gp) is most commonly associated with human MDR; it utilizes energy from adenosine triphosphate (ATP) to transport a number of substrates out of cells against concentration gradients. By the active transport of substrates against concentration gradients, intracellular concentrations of substrates are decreased. This leads to the cause of failure in cancer chemotherapy.

机译：背景多药耐药性（MDR）是癌症化疗的主要障碍。转运蛋白引起的药物外流是发生MDR的主要原因。在人类中，MDR主要是在同时过度表达ATP结合盒（ABC）家族蛋白时发生的。 P-糖蛋白（P-gp）最常见与人类MDR相关；它利用三磷酸腺苷（ATP）的能量将许多底物逆着浓度梯度运出细胞。通过针对浓度梯度主动转运底物，降低了底物的细胞内浓度。这导致癌症化学疗法失败的原因。

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期刊名称 BMC Structural Biology
作者
Changdev G Gadhe; Thirumurthy Madhavan; Gugan Kothandan; Seung Joo Cho;
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年(卷),期 2011(11),-1
年度 2011
页码 5
总页数 15
原文格式 PDF
正文语种
中图分类生物物理学;
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1. In Silico Quantitative Structure-Activity Relationship Studies on P-gp Modulators of Tetrahydroisoquinoline-Ethyl-Phenylamine Series [J] . Changdev G Gadhe, Thirumurthy Madhavan, Gugan Kothandan, BMC Structural Biology . 2011,第1期

机译：四氢异喹啉-乙基-苯胺系列的P-gp调节剂的计算机定量结构-活性关系的研究
2. Biological Evaluation,Structure-Activity Relationships,and Three-Dimensional Quantitative Structure-Activity Relationship Studies of Dihydro-beta-agarofuran Sesquiterpenes as Modulators of P-Glycoprotein-Dependent Multidrug Resistance [J] . Carolina P.Reyes, Francisco Munoz-Martinez, Ivan R.Torrecillas Journal of Medicinal Chemistry . 2007,第20期

机译：二氢-β-agarofuran倍半萜作为P-糖蛋白依赖性多药耐药性调节剂的生物学评估，结构-活性关系和三维定量结构-活性关系研究
3. Quantitative structure-activity relationships for a series of selective estrogen receptor-beta modulators [J] . Salum LB, Polikarpov I, Andricopulo AD SAR and QSAR in Environmental Research . 2007,第7期

机译：一系列选择性雌激素受体-β调节剂的定量构效关系
4. In Silico Toxicology Screening of the Rodent Carcino-genic Potential of Phytochemicals Using Quantitative Structure-Activity Relationship Analysis [C] . Luis G. Valerie Jr., Naomi L. Kruhlak, R. Daniel Benz Symposium on Risk Assessment of Phytochemicals in Food: Novel Approaches . 2010

机译：在硅毒理学筛选植物癌的植物癌潜力使用定量结构 - 活性关系分析
5. In silico approaches for studying transporter and receptor structure-activity relationships. [D] . Chang, Cheng. 2005

机译：用于研究转运蛋白和受体结构-活性关系的计算机方法。
6. Two- and Three-Dimensional Quantitative Structure-Activity Relationships Studies on a Series of Liver X Receptor Ligands [O] . Káthia M Honório, Lívia B Salum, Richard C Garratt, 2008

机译：一系列肝脏X受体配体的二维和三维定量构效关系研究
7. In Silico Quantitative Structure-Activity Relationship Studies on P-gp Modulators of Tetrahydroisoquinoline-Ethyl-Phenylamine Series [O] . Changdev G Gadhe, Thirumurthy Madhavan, Gugan Kothandan, 2011

机译：四氢异喹啉-乙基-苯胺系列的P-gp调节剂的计算机定量结构-活性关系的研究
8. Simplifying Complex QSAR's (Quantitative Structure-Activity Relationships) in Toxicity Studies with Multivariate Statistics [R] . Niemi, G. J. , McKim, J. M. 1988

机译：用多元统计量简化毒性研究中的复杂QsaR（定量构效关系）

In Silico Quantitative Structure-Activity Relationship Studies on P-gp Modulators of Tetrahydroisoquinoline-Ethyl-Phenylamine Series

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