The dipeptidyl peptidase IV inhibitors vildagliptin and K-579 inhibit a phospholipase C: a case of promiscuous scaffolds in proteins [version 3; peer review: 2 approved]

Chakraborty, Sandeep; Rendón-Ramírez, Adela; Ásgeirsson, Bjarni; Dutta, Mouparna; Ghosh, Anindya S.; Oda, Masataka; Venkatramani, Ravindra; Rao, Basuthkar J.; Dandekar, Abhaya M.; Goñi, Félix M.

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dc.contributor	Háskóli Íslands
dc.contributor	University of Iceland
dc.contributor.author	Chakraborty, Sandeep
dc.contributor.author	Rendón-Ramírez, Adela
dc.contributor.author	orcid.org/0000-0002-4275-2732 Ásgeirsson, Bjarni
dc.contributor.author	Dutta, Mouparna
dc.contributor.author	Ghosh, Anindya S.
dc.contributor.author	Oda, Masataka
dc.contributor.author	Venkatramani, Ravindra
dc.contributor.author	Rao, Basuthkar J.
dc.contributor.author	Dandekar, Abhaya M.
dc.contributor.author	Goñi, Félix M.
dc.date.accessioned	2020-08-25T10:28:30Z
dc.date.available	2020-08-25T10:28:30Z
dc.date.issued	2015-01-29
dc.identifier.citation	Chakraborty S, Rendón-Ramírez A, Ásgeirsson B et al. The dipeptidyl peptidase IV inhibitors vildagliptin and K-579 inhibit a phospholipase C: a case of promiscuous scaffolds in proteins [version 3; peer review: 2 approved]. F1000Research 2015, 2:286 (https://doi.org/10.12688/f1000research.2-286.v3)
dc.identifier.issn	2046-1402
dc.identifier.uri	https://hdl.handle.net/20.500.11815/2014
dc.description	Publisher's version (útgefin grein)
dc.description.abstract	The long term side effects of any newly introduced drug is a subject of intense research, and often raging controversies. One such example is the dipeptidyl peptidase-IV (DPP4) inhibitor used for treating type 2 diabetes, which is inconclusively implicated in increased susceptibility to acute pancreatitis. Previously, based on a computational analysis of the spatial and electrostatic properties of active site residues, we have demonstrated that phosphoinositide-specific phospholipase C (PI-PLC) from Bacillus cereus is a prolyl peptidase using in vivo experiments. In the current work, we first report the inhibition of the native activity of PI-PLC by two DPP4 inhibitors - vildagliptin (LAF-237) and K-579. While vildagliptin inhibited PI-PLC at micromolar concentrations, K-579 was a potent inhibitor even at nanomolar concentrations. Subsequently, we queried a comprehensive, non-redundant set of 5000 human proteins (50% similarity cutoff) with known structures using serine protease (SPASE) motifs derived from trypsin and DPP4. A pancreatic lipase and a gastric lipase are among the proteins that are identified as proteins having promiscuous SPASE scaffolds that could interact with DPP4 inhibitors. The presence of such scaffolds in human lipases is expected since they share the same catalytic mechanism with PI-PLC. However our methodology also detects other proteins, often with a completely different enzymatic mechanism, that have significantly congruent domains with the SPASE motifs. The reported elevated levels of serum lipase, although contested, could be rationalized by inhibition of lipases reported here. In an effort to further our understanding of the spatial and electrostatic basis of DPP4 inhibitors, we have also done a comprehensive analysis of all 76 known DPP4 structures liganded to inhibitors till date. Also, the methodology presented here can be easily adopted for other drugs, and provide the first line of filtering in the identification of pathways that might be inadvertently affected due to promiscuous scaffolds in proteins.
dc.description.sponsorship	FMG thanks the Spanish Ministerio de Ciencia e Innovacion for grant No. BFU 2012-36241, and the University of the Basque Country for grant No. IT 849-13. BJ and RV acknowledge financial support from Tata Institute of Fundamental Research (Department of Atomic Energy). Additionally, BJR is thankful to the Department of Science and Technology for the JC Bose Award Grant. BA extends gratitude to the University of Iceland Research Found for supporting the project financially (grant No. 141619). AMD wishes to acknowledge grant #12-0130-SA from California Department of Food and Agriculture CDFA PD/GWSS Board. MO was supported in part by a Grant-in-aid for Scientific Research from the Ministry of Education, Culture, Sports, Science and Technology, Japan; (grant No. 21790431). The work in Liege was supported by an IUAP program funded by the Belgian federal government.
dc.language.iso	en
dc.publisher	F1000Research
dc.relation.ispartofseries	F1000Research;2(286)
dc.rights	info:eu-repo/semantics/openAccess
dc.subject	Diabetes
dc.subject	Bacillus cereus
dc.subject	PI PLC
dc.subject	Serine protease
dc.subject	Lipase
dc.subject	Sykursýki
dc.subject	Lífefnafræði
dc.subject	Lyfhrifafræði
dc.title	The dipeptidyl peptidase IV inhibitors vildagliptin and K-579 inhibit a phospholipase C: a case of promiscuous scaffolds in proteins [version 3; peer review: 2 approved]
dc.type	info:eu-repo/semantics/article
dcterms.license	Copyright: © 2015 Chakraborty S et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited. The author(s) is/are employees of the US Government and therefore domestic copyright protection in USA does not apply to this work. The work may be protected under the copyright laws of other jurisdictions when used in those jurisdictions. Data associated with the article are available under the terms of the Creative Commons Zero "No rights reserved" data waiver (CC0 1.0 Public domain dedication).
dc.description.version	Peer reviewed
dc.identifier.journal	F1000Research
dc.identifier.doi	10.12688/f1000research.2-286.v3
dc.contributor.department	Raunvísindastofnun (HÍ)
dc.contributor.department	Science Institute (UI)
dc.contributor.school	Verkfræði- og náttúruvísindasvið (HÍ)
dc.contributor.school	School of Engineering and Natural Sciences (UI)