2013
DOI: 10.1186/1758-2946-5-2
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Enhanced ranking of PknB Inhibitors using data fusion methods

Abstract: BackgroundMycobacterium tuberculosis encodes 11 putative serine-threonine proteins Kinases (STPK) which regulates transcription, cell development and interaction with the host cells. From the 11 STPKs three kinases namely PknA, PknB and PknG have been related to the mycobacterial growth. From previous studies it has been observed that PknB is essential for mycobacterial growth and expressed during log phase of the growth and phosphorylates substrates involved in peptidoglycan biosynthesis. In recent years many… Show more

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Cited by 30 publications
(30 citation statements)
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“…concentrated ROC (CROC), Boltzmann-enhanced discrimination of ROC (BEDROC), Guner Henry Score etc.) 71–74 and whether consensus scoring could overcome these.…”
Section: Discussionmentioning
confidence: 99%
“…concentrated ROC (CROC), Boltzmann-enhanced discrimination of ROC (BEDROC), Guner Henry Score etc.) 71–74 and whether consensus scoring could overcome these.…”
Section: Discussionmentioning
confidence: 99%
“…While antibiotic resistance in the model pathogen L. monocytogenes is not a burgeoning issue, we believe that these data act as a proof of principle that specificity in the targeting of bacterial PASTA eSTKs is possible. Prior to our work, pharmacologic inhibitors that target the M. tuberculosis kinase PknB have also been identified, although their development as potential therapeutic agents is still a work in progress (16)(17)(18). Inhibitors of other bacterial PASTA kinases that work in a ␤-lactam-synergistic manner remain to be identified.…”
Section: Discussionmentioning
confidence: 99%
“…While the substrates and function of the PASTA kinases are incompletely defined, they appear to have various functions in different organisms, ranging from playing a role in biofilm formation (Streptococcus mutans) to being essential in some organisms (M. tuberculosis) (14,15). As such, pharmacologic inhibition of PASTA kinases has been preliminarily pursued as a novel antimicrobial therapeutic strategy against the M. tuberculosis kinase PknB (16)(17)(18). Deletion of Stk1, the PASTA kinase in S. aureus, reverses the methicillin-resistant phenotype in MRSA (19,20).…”
mentioning
confidence: 99%
“…Several PknB structures were previously elucidated, but none with a specific kinase inhibitor bound to the active site (Lombana et al, 2010, Ortiz-Lombardia, Pompeo et al, 2003, Wehenkel, Fernandez et al, 2006, Young, Delagoutte et al, 2003. Additionally, several PknB inhibitors were previously modeled in silico, but structural confirmation of these models was not established (Chapman et al, 2012, Lougheed et al, 2011, Naqvi et al, 2014, Seal et al, 2013. To confirm our model and facilitate future drug development insight, we co-crystallized the catalytic domain of PknB with GSK690693, a compound biochemically equivalent to our best drugs and commercially available in large quantities.…”
Section: Ipas Are Potent Biochemical Inhibitors Of Pknb and Require Amentioning
confidence: 99%