| Literature DB >> 21110830 |
John K Morrow1, Lei Du-Cuny, Lu Chen, Emmanuelle J Meuillet, Eugene A Mash, Garth Powis, Shuxing Zhang.
Abstract
The serine/threonine kinase Akt has proven to be a significant signaling target, involved in various biological functions. Because of its cardinal role in numerous cellular responses, Akt has been implicated in many human diseases, particularly cancer. It has been established that Akt is a viable and feasible target for anticancer therapeutics. Analysis of all Akt kinases reveals conserved homology for an N-terminal regulatory domain, which contains a pleckstrin-homology (PH) domain for cellular translocation, a kinase domain with serine/threonine specificity, and a C-terminal extension domain. These well defined regions have been targeted, and various approaches, including in silico methods, have been implemented to develop Akt inhibitors. In spite of unique techniques and a prolific body of knowledge surrounding Akt, no targeted Akt therapeutics have reached the market yet. Here we will highlight successes and challenges to date on the development of anticancer agents modulating the Akt pathway in recent patents as well as discuss the methods employed for this task. Special attention will be given to patents with focus on those discoveries using computer-aided drug design approaches.Entities:
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Year: 2011 PMID: 21110830 PMCID: PMC3784017 DOI: 10.2174/157489211793980079
Source DB: PubMed Journal: Recent Pat Anticancer Drug Discov ISSN: 1574-8928 Impact factor: 4.169