Design and development of novel urea, sulfonyltriurea, and sulfonamide derivatives as potential inhibitors of sphingosine kinase 1

Sonam Roy; Amarjyoti Das Mahapatra; Taj Mohammad; Preeti Gupta; Mohamed F. Alajmi; Afzal Hussain; Md Tabish Rehman; Bhaskar Datta; Md Imtaiyaz Hassan

doi:10.3390/ph13060118

Design and development of novel urea, sulfonyltriurea, and sulfonamide derivatives as potential inhibitors of sphingosine kinase 1

Sonam Roy
, Amarjyoti Das Mahapatra
, Taj Mohammad
, Preeti Gupta
, Mohamed F. Alajmi
, Afzal Hussain
, Md Tabish Rehman
, Bhaskar Datta
, Md Imtaiyaz Hassan

Jamia Millia Islamia
Indian Institute of Technology Gandhinagar
King Saud University

Research output: Contribution to journal › Article › peer-review

20 Scopus citations

Abstract

Sphingosine kinase 1 (SphK1) is one of the well-studied drug targets for cancer and inflammatory diseases. Recently discovered small-molecule inhibitors of SphK1 have been recommended in cancer therapeutics; however, selectivity and potency of first-generation inhibitors are great challenge. In search of effective SphK1 inhibitors, a set of small molecules have been designed and synthesized bearing urea, sulfonylurea, sulfonamide, and sulfonyltriurea groups. The binding affinity of these inhibitors was measured by fluorescence-binding assay and isothermal titration calorimetry. Compounds 1, 5, 6, and 7 showed an admirable binding affinity to the SphK1 in the sub-micromolar range and significantly inhibited SphK1 activity with admirable IC₅₀ values. Molecular docking studies revealed that these compounds fit well into the sphingosine binding pocket of SphK1 and formed significant number of hydrogen bonds and van der Waals interactions. These molecules may be exploited as potent and selective inhibitors of SphK1 that could be implicated in cancer therapeutics after the required in vivo validation.

Original language	English
Article number	118
Pages (from-to)	1-22
Number of pages	22
Journal	Pharmaceuticals
Volume	13
Issue number	6
DOIs	https://doi.org/10.3390/ph13060118
State	Published - Jun 2020
Externally published	Yes

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

Keywords

Cancer therapy
Drug design and discovery
Enzyme inhibition
Kinase inhibitors
Molecular docking
Sphingosine kinase-1
Sphingosine-1-phosphate

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10.3390/ph13060118

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title = "Design and development of novel urea, sulfonyltriurea, and sulfonamide derivatives as potential inhibitors of sphingosine kinase 1",

abstract = "Sphingosine kinase 1 (SphK1) is one of the well-studied drug targets for cancer and inflammatory diseases. Recently discovered small-molecule inhibitors of SphK1 have been recommended in cancer therapeutics; however, selectivity and potency of first-generation inhibitors are great challenge. In search of effective SphK1 inhibitors, a set of small molecules have been designed and synthesized bearing urea, sulfonylurea, sulfonamide, and sulfonyltriurea groups. The binding affinity of these inhibitors was measured by fluorescence-binding assay and isothermal titration calorimetry. Compounds 1, 5, 6, and 7 showed an admirable binding affinity to the SphK1 in the sub-micromolar range and significantly inhibited SphK1 activity with admirable IC50 values. Molecular docking studies revealed that these compounds fit well into the sphingosine binding pocket of SphK1 and formed significant number of hydrogen bonds and van der Waals interactions. These molecules may be exploited as potent and selective inhibitors of SphK1 that could be implicated in cancer therapeutics after the required in vivo validation.",

keywords = "Cancer therapy, Drug design and discovery, Enzyme inhibition, Kinase inhibitors, Molecular docking, Sphingosine kinase-1, Sphingosine-1-phosphate",

author = "Sonam Roy and \{Das Mahapatra\}, Amarjyoti and Taj Mohammad and Preeti Gupta and Alajmi, \{Mohamed F.\} and Afzal Hussain and Rehman, \{Md Tabish\} and Bhaskar Datta and Hassan, \{Md Imtaiyaz\}",

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year = "2020",

month = jun,

doi = "10.3390/ph13060118",

language = "English",

volume = "13",

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journal = "Pharmaceuticals",

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AU - Roy, Sonam

AU - Das Mahapatra, Amarjyoti

AU - Mohammad, Taj

AU - Gupta, Preeti

AU - Alajmi, Mohamed F.

AU - Hussain, Afzal

AU - Rehman, Md Tabish

AU - Datta, Bhaskar

AU - Hassan, Md Imtaiyaz

PY - 2020/6

Y1 - 2020/6

N2 - Sphingosine kinase 1 (SphK1) is one of the well-studied drug targets for cancer and inflammatory diseases. Recently discovered small-molecule inhibitors of SphK1 have been recommended in cancer therapeutics; however, selectivity and potency of first-generation inhibitors are great challenge. In search of effective SphK1 inhibitors, a set of small molecules have been designed and synthesized bearing urea, sulfonylurea, sulfonamide, and sulfonyltriurea groups. The binding affinity of these inhibitors was measured by fluorescence-binding assay and isothermal titration calorimetry. Compounds 1, 5, 6, and 7 showed an admirable binding affinity to the SphK1 in the sub-micromolar range and significantly inhibited SphK1 activity with admirable IC50 values. Molecular docking studies revealed that these compounds fit well into the sphingosine binding pocket of SphK1 and formed significant number of hydrogen bonds and van der Waals interactions. These molecules may be exploited as potent and selective inhibitors of SphK1 that could be implicated in cancer therapeutics after the required in vivo validation.

AB - Sphingosine kinase 1 (SphK1) is one of the well-studied drug targets for cancer and inflammatory diseases. Recently discovered small-molecule inhibitors of SphK1 have been recommended in cancer therapeutics; however, selectivity and potency of first-generation inhibitors are great challenge. In search of effective SphK1 inhibitors, a set of small molecules have been designed and synthesized bearing urea, sulfonylurea, sulfonamide, and sulfonyltriurea groups. The binding affinity of these inhibitors was measured by fluorescence-binding assay and isothermal titration calorimetry. Compounds 1, 5, 6, and 7 showed an admirable binding affinity to the SphK1 in the sub-micromolar range and significantly inhibited SphK1 activity with admirable IC50 values. Molecular docking studies revealed that these compounds fit well into the sphingosine binding pocket of SphK1 and formed significant number of hydrogen bonds and van der Waals interactions. These molecules may be exploited as potent and selective inhibitors of SphK1 that could be implicated in cancer therapeutics after the required in vivo validation.

KW - Cancer therapy

KW - Drug design and discovery

KW - Enzyme inhibition

KW - Kinase inhibitors

KW - Molecular docking

KW - Sphingosine kinase-1

KW - Sphingosine-1-phosphate

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DO - 10.3390/ph13060118

M3 - Article

AN - SCOPUS:85086644925

SN - 1424-8247

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JO - Pharmaceuticals

JF - Pharmaceuticals

IS - 6

M1 - 118

ER -

Design and development of novel urea, sulfonyltriurea, and sulfonamide derivatives as potential inhibitors of sphingosine kinase 1

Abstract

UN SDGs

Keywords

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