enoyl acp reductase
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2020 ◽  
Vol 30 (24) ◽  
pp. 127651
Author(s):  
Yogiara ◽  
Elena A. Mordukhova ◽  
Dooil Kim ◽  
Won-Gon Kim ◽  
Jae-Kwan Hwang ◽  
...  

2020 ◽  
Vol 54 (3s) ◽  
pp. s620-s632
Author(s):  
Shrinivas Dattatraya Joshi ◽  
SR Prem Kumar ◽  
Venkatarao H Kulkarni ◽  
Ali Mohamed Alshabi ◽  
Ibrahim Ahmed Shaikh ◽  
...  

Author(s):  
Shuai Li ◽  
Eirik A. Moreb ◽  
Zhixia Ye ◽  
Jennifer N. Hennigan ◽  
Daniel Baez Castellanos ◽  
...  

AbstractWe report improved NADPH flux and xylitol biosynthesis in engineered E. coli. Xylitol is produced from xylose via an NADPH dependent reductase. We utilize two-stage dynamic metabolic control to compare two approaches to optimize xylitol biosynthesis, a stoichiometric approach, wherein competitive fluxes are decreased, and a regulatory approach wherein the levels of key regulatory metabolites are reduced. The stoichiometric and regulatory approaches lead to a 16 fold and 100 fold improvement in xylitol production, respectively. Strains with reduced levels of enoyl-ACP reductase and glucose-6-phosphate dehydrogenase, led to altered metabolite pools resulting in the activation of the membrane bound transhydrogenase and a new NADPH generation pathway, namely pyruvate ferredoxin oxidoreductase coupled with NADPH dependent ferredoxin reductase, leading to increased NADPH fluxes, despite a reduction in NADPH pools. These strains produced titers of 200 g/L of xylitol from xylose at 86% of theoretical yield in instrumented bioreactors. We expect dynamic control over enoyl-ACP reductase and glucose-6-phosphate dehydrogenase to broadly enable improved NADPH dependent bioconversions.HighlightsDecreases in NADPH pools lead to increased NADPH fluxesPyruvate ferredoxin oxidoreductase coupled with NADPH-ferredoxin reductase improves NADPH production in vivo.Dynamic reduction in acyl-ACP/CoA pools alleviate inhibition of membrane bound transhydrogenase and improve NADPH fluxXylitol titers > 200g/L in fed batch fermentations with xylose as a sole feedstock.


Author(s):  
Balakishan Bhukya ◽  
Sarfaraz Alam ◽  
Vinita Chaturvedi ◽  
Priyanka Trivedi ◽  
Shailesh Kumar ◽  
...  

: Brevifoliol is an abeo-taxane isolated from the Taxus wallichiana needles, eighteen semi-synthetic esters derivatives of brevifoliol were prepared by Steglich esterification and screened for their anti-tubercular potential against Mycobacterium tuberculosis H37Ra avirulent strain. The 3-[chloro (7)] and 3, 5-[dinitro (8)] benzoic acid ester derivatives were most active (MIC 25 ug/ml) against the pathogen. Further, in silico docking studies of the active derivative 7 with mycobacterium enzyme inhA (enoyl-ACP reductase) gave a LibDock score of 152.68 and binding energy of -208.62 and formed three hydrogen bonds with SER94, MET98, and SER94. Similarly, when derivative 8 docked with inhA, it gave a LibDock score of 113.55 and binding energy of -175.46 and formed a single hydrogen bond with GLN100 and Pi-interaction with PHE97. On the other hand the known standard drug isoniazid (INH) gave a LibDock score of 61.63, binding energy of -81.25 and formed one hydrogen bond with ASP148. These molecular docking results and the way of binding pattern indicated that compound 7 and 8 bound well within the binding pocket of inhA and showed a higher binding affinity than the known drug Isoniazid. Additionally, both the derivatives (7 and 8) showed no cytotoxicity towards the healthy liver cell lines CHANG.


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