研究生学术报告预告登记(开题、中期、答辩)

       为加强研究生学术交流活动,推进学术创新,特开通“研究生学术报告预告区”。我校研究生和教师可以在预告区及时发布和了解有关研究生学术报告的信息,届时参加。也可就某学术报告展开专题讨论与交流。

报告人: 付艳华
学号: 2015213051
学院: 药物科学与技术学院
报告类型: 第一次学术报告
日期: 6 June 2016
时间: 3:05 PM
地点: 24楼502
导师: Nathaniel Finney
题目: Fluorescence-based assays for disease-related liver transport protein
内容提要:

Numerous disease states are associated with having a fatty liver. These include obesity, atherosclerosis and insulin resistance. Because the liver can make its own fat, dietary restriction does not treat fatty liver diseases. The liver makes fatty acids from simple precursors, such as lactic acid. lactate enter the liver from the bloodstream, through the action of ATP-independent transport (“pump”) proteins..The driving force for the lactate pump is the release of protons. The lactate pump is a member of the monocarboxylate transporter family. Proteins in this family transport  a range of monocarboxylic acids across cell membranes.

Developing small-molecule inhibitors of  lactate pumps could lead to drugs for treating fatty liver diseases. There are no known inhibitors of the pump. This is because there are no know assays for pump protein activity. There are crystal structures of prokaryotic lactate pump proteins. Through a collaborator, we have access to unique, stable human liver cell lines with overexpressed lactate pumps. Structural data are not available. This makes reliable structure-based drug design impossible.

Phosphine-derived fluorescent probes will be used to develop appropriate fluorescence-based assays. When attached to a fluorophore, phosphines quench fluorescence by photoinduced electron transfer (PET) from the phosphorus lone pair. When the phosphine is oxidized to the phosphine oxide, the probes become fluorescent again.

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登记人: 付艳华
登记时间: Monday, 2 April 2018, 11:08 PM