Fragment-Based Approaches in Drug Discovery and Chemical Biology 论文

2012Biochemistry引用 452
Biochemical and Molecular ResearchComputational Drug Discovery MethodsProtein Structure and Dynamics

详细信息

发表期刊/会议
Biochemistry
发表日期
2012-06-14
发表年份
2012

关键词

Biochemical and Molecular ResearchComputational Drug Discovery MethodsProtein Structure and Dynamics

摘要

Fragment-based approaches to finding novel small molecules that bind to proteins are now firmly established in drug discovery and chemical biology. Initially developed primarily in a few centers in the biotech and pharma industry, this methodology has now been adopted widely in both the pharmaceutical industry and academia. After the initial success with kinase targets, the versatility of this approach has now expanded to a broad range of different protein classes. Herein we describe recent fragment-based approaches to a wide range of target types, including Hsp90, β-secretase, and allosteric sites in human immunodeficiency virus protease and fanesyl pyrophosphate synthase. The role of fragment-based approaches in an academic research environment is also examined with an emphasis on neglected diseases such as tuberculosis. The development of a fragment library, the fragment screening process, and the subsequent fragment hit elaboration will be discussed using examples from the literature.