Identification of chebulinic acid as potent natural inhibitor of M. tuberculosis DNA gyrase and molecular insights into its binding mode of action. (December 2015)
- Record Type:
- Journal Article
- Title:
- Identification of chebulinic acid as potent natural inhibitor of M. tuberculosis DNA gyrase and molecular insights into its binding mode of action. (December 2015)
- Main Title:
- Identification of chebulinic acid as potent natural inhibitor of M. tuberculosis DNA gyrase and molecular insights into its binding mode of action
- Authors:
- Patel, Kunal
Tyagi, Chetna
Goyal, Sukriti
Jamal, Salma
Wahi, Divya
Jain, Ritu
Bharadvaja, Navneeta
Grover, Abhinav - Abstract:
- Graphical abstract: Highlights: Checking multiple and extensively drug resistant TB by targeting wild type and three mutant variants of DNA gyrase. After exhaustive screening of natural compounds, one compound namely, chebulinic acid (CA) was identified as active against all 4 variants. Molecular dynamics revealed binding stability of CA with DNA gyrase chain A. Two mechanisms are proposed for its antibacterial activity: displacement of crucial residue and steric hindrance due to DNA binding. Abstract: Drug resistant tuberculosis has threatened all the advances that have been made in TB control at the global stage in the last few decades. DNA gyrase enzymes are an excellent target for antibacterial drug discovery as they are involved in essential functions like DNA replication. Here we report, a successful application of high throughput virtual screening (HTVS) to identify an inhibitor of Mycobacterium DNA gyrase targeting the wild type and the most prevalent three double mutants of quinolone resistant DNA gyrase namely A90V + D94G, A74S + D94G and A90V + S91P. HTVS of 179.299 compounds gave five compounds with significant binding affinity. Extra presicion (XP) docking and MD simulations gave a clear view of their interaction pattern. Among them, chebulinic acid (CA), a phytocompound obtained from Terminalia chebula was the most potent inhibitor with significantly high XP docking score, −14.63, −16.46, −15.94 and −15.11 against wild type and three variants respectively.Graphical abstract: Highlights: Checking multiple and extensively drug resistant TB by targeting wild type and three mutant variants of DNA gyrase. After exhaustive screening of natural compounds, one compound namely, chebulinic acid (CA) was identified as active against all 4 variants. Molecular dynamics revealed binding stability of CA with DNA gyrase chain A. Two mechanisms are proposed for its antibacterial activity: displacement of crucial residue and steric hindrance due to DNA binding. Abstract: Drug resistant tuberculosis has threatened all the advances that have been made in TB control at the global stage in the last few decades. DNA gyrase enzymes are an excellent target for antibacterial drug discovery as they are involved in essential functions like DNA replication. Here we report, a successful application of high throughput virtual screening (HTVS) to identify an inhibitor of Mycobacterium DNA gyrase targeting the wild type and the most prevalent three double mutants of quinolone resistant DNA gyrase namely A90V + D94G, A74S + D94G and A90V + S91P. HTVS of 179.299 compounds gave five compounds with significant binding affinity. Extra presicion (XP) docking and MD simulations gave a clear view of their interaction pattern. Among them, chebulinic acid (CA), a phytocompound obtained from Terminalia chebula was the most potent inhibitor with significantly high XP docking score, −14.63, −16.46, −15.94 and −15.11 against wild type and three variants respectively. Simulation studies for a period of 16 ns indicated stable DNA gyrA–CA complex formation. This stable binding would result in inhibition of the enzyme by two mechanisms. Firstly, binding of CA causes displacement of catalytic Tyr129 away from its target DNA-phosphate molecule from 1.6 Å to 3.8–7.3 Å and secondly, by causing steric hindrance to the binding of DNA strand at DNA binding site of enzyme. The combined effect would result in loss of cleavage and religation activity of enzyme leading to bactericidal effect on tuberculosis. This phytocompound displays desirable quality for carrying forward as a lead compound for anti-tuberculosis drug development. The results presented here are solely based on computations and need to be validated experimentally in order to assert the proposed mechanism of action. … (more)
- Is Part Of:
- Computational biology and chemistry. Volume 59:Part A(2015)
- Journal:
- Computational biology and chemistry
- Issue:
- Volume 59:Part A(2015)
- Issue Display:
- Volume 59, Issue 2015 (2015)
- Year:
- 2015
- Volume:
- 59
- Issue:
- 2015
- Issue Sort Value:
- 2015-0059-2015-0000
- Page Start:
- 37
- Page End:
- 47
- Publication Date:
- 2015-12
- Subjects:
- HTVS high throughput virtual screening -- CA chebulinic acid -- XP extra precision -- MDR-TB multiple-drug resistant tuberculosis -- XDR-TB extensively-drug resistant tuberculosis -- QRDR quinolone resistance determining region -- CTD C-terminal domain -- PSVS protein structure validation suite -- MD molecular dynamics
Chebulinic acid -- DNA gyrase -- Multiple drug resistance -- Tuberculosis -- Virtual screening -- Molecular dynamics simulations
Chemistry -- Data processing -- Periodicals
Biology -- Data processing -- Periodicals
Biochemistry -- Data processing
Biology -- Data processing
Molecular biology -- Data processing
Periodicals
Electronic journals
542.85 - Journal URLs:
- http://www.sciencedirect.com/science/journal/14769271 ↗
http://www.elsevier.com/journals ↗ - DOI:
- 10.1016/j.compbiolchem.2015.09.006 ↗
- Languages:
- English
- ISSNs:
- 1476-9271
- Deposit Type:
- Legaldeposit
- View Content:
- Available online (eLD content is only available in our Reading Rooms) ↗
- Physical Locations:
- British Library DSC - 3390.576700
British Library DSC - BLDSS-3PM
British Library STI - ELD Digital store - Ingest File:
- 7817.xml