Identification of potential dipeptidyl peptidase IV inhibitors from the ConMedNP library by virtual screening, and molecular dynamics methods

Hans Merlin Tsahnang Fofack; Maraf Mbah Bake; Simon Petry; Baruch A. Ateba; Pascal Amoa Onguéné; Haydar Mohammad-Salim; Fidele Ntie-Kang; Luc Meva a. Mbaze; Serhii Vakal; Cyril A. Kenfack

doi:10.1016/j.heliyon.2024.e35191

Identification of potential dipeptidyl peptidase IV inhibitors from the ConMedNP library by virtual screening, and molecular dynamics methods

Hans Merlin Tsahnang Fofack, Maraf Mbah Bake^*, Simon Petry, Baruch A. Ateba, Pascal Amoa Onguéné, Haydar Mohammad-Salim, Fidele Ntie-Kang, Luc Meva a. Mbaze^*, Serhii Vakal^*, Cyril A. Kenfack^*

^*Tämän työn vastaava kirjoittaja

Tutkimustuotos: Lehtiartikkeli › Artikkeli › Tieteellinen › vertaisarvioitu

2 Sitaatiot (Scopus)

2 Lataukset (Pure)

Abstrakti

In this study, we screened novel dipeptidyl peptidase IV (DPP4) inhibitors from the ConMedNP library consisting of 3507 molecules. Interestingly, molecular docking, ADMET, and the anti-diabetic activity predictions suggest that three molecules, namely OTH_UD_XX06_1, GB19, and BMC_000104, have a high binding affinity toward DPP4. The molecular dynamics (MD) simulation results suggest that these hit molecules have a stable binding pose and occupy the binding pockets throughout the 200 ns simulation. The presence of intermolecular H-bonding between the ligands and DPP4 was observed throughout the simulation period. Thus, docking and MD results, predicted that the three compounds were the most potent DPP4 inhibitors that could putatively bind to the DPP4 active site via both conventional H-bonding and hydrophobic interactions. These results could aid the discovery of new drugs to treat type 2 diabetes.

Alkuperäiskieli	Englanti
Artikkeli	e35191
Julkaisu	Heliyon
Vuosikerta	10
Numero	15
DOI - pysyväislinkit	https://doi.org/10.1016/j.heliyon.2024.e35191
Tila	Julkaistu - 15 elok. 2024
OKM-julkaisutyyppi	A1 Julkaistu artikkeli, soviteltu

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10.1016/j.heliyon.2024.e35191

PIIS2405844024112224Lopullinen julkaistu versio, 11 MBLisenssi: CC BY-NC-ND

https://urn.fi/URN:NBN:fi-fe202502018628

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Tsahnang Fofack, H. M., Mbah Bake, M., Petry, S., Ateba, B. A., Amoa Onguéné, P., Mohammad-Salim, H., Ntie-Kang, F., Mbaze, L. M. A., Vakal, S., & Kenfack, C. A. (2024). Identification of potential dipeptidyl peptidase IV inhibitors from the ConMedNP library by virtual screening, and molecular dynamics methods. Heliyon, 10(15), Artikkeli e35191. https://doi.org/10.1016/j.heliyon.2024.e35191

@article{0bf480eb02ca4c83a2cf57c9bfd5fe6c,

title = "Identification of potential dipeptidyl peptidase IV inhibitors from the ConMedNP library by virtual screening, and molecular dynamics methods",

abstract = "In this study, we screened novel dipeptidyl peptidase IV (DPP4) inhibitors from the ConMedNP library consisting of 3507 molecules. Interestingly, molecular docking, ADMET, and the anti-diabetic activity predictions suggest that three molecules, namely OTH_UD_XX06_1, GB19, and BMC_000104, have a high binding affinity toward DPP4. The molecular dynamics (MD) simulation results suggest that these hit molecules have a stable binding pose and occupy the binding pockets throughout the 200 ns simulation. The presence of intermolecular H-bonding between the ligands and DPP4 was observed throughout the simulation period. Thus, docking and MD results, predicted that the three compounds were the most potent DPP4 inhibitors that could putatively bind to the DPP4 active site via both conventional H-bonding and hydrophobic interactions. These results could aid the discovery of new drugs to treat type 2 diabetes.",

keywords = "ConMedNP library, Dipeptidyl peptidase IV (DPP4), Inhibitors, Molecular dynamics, Virtual screening",

author = "{Tsahnang Fofack}, {Hans Merlin} and {Mbah Bake}, Maraf and Simon Petry and Ateba, {Baruch A.} and {Amoa Ongu{\'e}n{\'e}}, Pascal and Haydar Mohammad-Salim and Fidele Ntie-Kang and Mbaze, {Luc Meva a.} and Serhii Vakal and Kenfack, {Cyril A.}",

note = "Publisher Copyright: {\textcopyright} 2024",

year = "2024",

month = aug,

day = "15",

doi = "10.1016/j.heliyon.2024.e35191",

language = "English",

volume = "10",

journal = "Heliyon",

issn = "2405-8440",

publisher = "Elsevier",

number = "15",

}

Tsahnang Fofack, HM, Mbah Bake, M, Petry, S, Ateba, BA, Amoa Onguéné, P, Mohammad-Salim, H, Ntie-Kang, F, Mbaze, LMA, Vakal, S & Kenfack, CA 2024, 'Identification of potential dipeptidyl peptidase IV inhibitors from the ConMedNP library by virtual screening, and molecular dynamics methods', Heliyon, Vuosikerta 10, Nro 15, e35191. https://doi.org/10.1016/j.heliyon.2024.e35191

TY - JOUR

T1 - Identification of potential dipeptidyl peptidase IV inhibitors from the ConMedNP library by virtual screening, and molecular dynamics methods

AU - Tsahnang Fofack, Hans Merlin

AU - Mbah Bake, Maraf

AU - Petry, Simon

AU - Ateba, Baruch A.

AU - Amoa Onguéné, Pascal

AU - Mohammad-Salim, Haydar

AU - Ntie-Kang, Fidele

AU - Mbaze, Luc Meva a.

AU - Vakal, Serhii

AU - Kenfack, Cyril A.

PY - 2024/8/15

Y1 - 2024/8/15

N2 - In this study, we screened novel dipeptidyl peptidase IV (DPP4) inhibitors from the ConMedNP library consisting of 3507 molecules. Interestingly, molecular docking, ADMET, and the anti-diabetic activity predictions suggest that three molecules, namely OTH_UD_XX06_1, GB19, and BMC_000104, have a high binding affinity toward DPP4. The molecular dynamics (MD) simulation results suggest that these hit molecules have a stable binding pose and occupy the binding pockets throughout the 200 ns simulation. The presence of intermolecular H-bonding between the ligands and DPP4 was observed throughout the simulation period. Thus, docking and MD results, predicted that the three compounds were the most potent DPP4 inhibitors that could putatively bind to the DPP4 active site via both conventional H-bonding and hydrophobic interactions. These results could aid the discovery of new drugs to treat type 2 diabetes.

AB - In this study, we screened novel dipeptidyl peptidase IV (DPP4) inhibitors from the ConMedNP library consisting of 3507 molecules. Interestingly, molecular docking, ADMET, and the anti-diabetic activity predictions suggest that three molecules, namely OTH_UD_XX06_1, GB19, and BMC_000104, have a high binding affinity toward DPP4. The molecular dynamics (MD) simulation results suggest that these hit molecules have a stable binding pose and occupy the binding pockets throughout the 200 ns simulation. The presence of intermolecular H-bonding between the ligands and DPP4 was observed throughout the simulation period. Thus, docking and MD results, predicted that the three compounds were the most potent DPP4 inhibitors that could putatively bind to the DPP4 active site via both conventional H-bonding and hydrophobic interactions. These results could aid the discovery of new drugs to treat type 2 diabetes.

KW - ConMedNP library

KW - Dipeptidyl peptidase IV (DPP4)

KW - Inhibitors

KW - Molecular dynamics

KW - Virtual screening

UR - http://www.scopus.com/inward/record.url?scp=85199713218&partnerID=8YFLogxK

U2 - 10.1016/j.heliyon.2024.e35191

DO - 10.1016/j.heliyon.2024.e35191

M3 - Article

AN - SCOPUS:85199713218

SN - 2405-8440

VL - 10

JO - Heliyon

JF - Heliyon

IS - 15

M1 - e35191

ER -

Identification of potential dipeptidyl peptidase IV inhibitors from the ConMedNP library by virtual screening, and molecular dynamics methods

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