Shan, Bo (2003). Molecular modelling assisted design and synthesis of cyclothialidine derivatives as DNA gyrase inhibitors. PHD thesis, Aston University.
Abstract
Since cyclothialidine was discovered as the most active DNA gyrase inhibitor in 1994, enormous efforts have been devoted to make it into a commercial medicine by a number of pharmaceutical companies and research groups worldwide. However, no serious breakthrough has been made up to now. An essential problem involved with cyclothialidine is that though it demonstrated the potent inhibition of DNA gyrase, it showed little activity against bacteria. This probably is attributable to its inability to penetrate bacterial cell walls and membranes. We applied the TSAR programme to generate a QSAR equation to the gram-negative organisms. In that equation, LogP is profoundly indicated as the key factor influencing the cyclothialidine activity against bacteria. However, the synthesized new analogues have failed to prove that. In the structure based drug design stage, we designed a group of open chain cyclothialidine derivatives by applying the SPROUT programme and completed the syntheses. Improved activity is found in a few analogues and a 3D pharmacophore of the DNA gyrase B is proposed to lead to synthesis of the new derivatives for development of potent antibiotics.
Divisions: | College of Health & Life Sciences |
---|---|
Additional Information: | Department: Pharmaceutical and Biological Sciences If you have discovered material in AURA which is unlawful e.g. breaches copyright, (either theirs or that of a third party) or any other law, including but not limited to those relating to patent, trademark, confidentiality, data protection, obscenity, defamation, libel, then please read our Takedown Policy and contact the service immediately. |
Institution: | Aston University |
Uncontrolled Keywords: | Molecular modelling,assisted design,synthesis,cyclothialidine derivatives,DNA gyrase inhibitors |
Last Modified: | 30 Sep 2024 08:04 |
Date Deposited: | 21 Dec 2010 14:12 |
Completed Date: | 2003-09 |
Authors: |
Shan, Bo
|