Synthesis of sulfonamide, amide and amine hybrid pharmacophore, an entry of new class of carbonic anhydrase II inhibitors and evaluation of chemo-informatics and binding analysis

Attique Ahmed; Pervaiz Ali Channar; Aamer Saeed; Markus Kalesse; Mehar Ali Kazi; Fayaz Ali Larik; Qamar Abbas; Mubashir Hassan; Hussain Raza; Sung Yum Seo

doi:10.1016/j.bioorg.2019.01.060

Synthesis of sulfonamide, amide and amine hybrid pharmacophore, an entry of new class of carbonic anhydrase II inhibitors and evaluation of chemo-informatics and binding analysis

Attique Ahmed
, Pervaiz Ali Channar
, Aamer Saeed^*
, Markus Kalesse
, Mehar Ali Kazi
, Fayaz Ali Larik
, Qamar Abbas
, Mubashir Hassan
, Hussain Raza
, Sung Yum Seo

^*Corresponding author for this work

Institute of Organic Chemistry

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

Abstract

Selective inhibition of carbonic anhydrase (CA) enzyme is an active area of research for medicinal chemists. In the current account, a hybrid pharmacophore approach was employed to design sulfonamide, amide and amine containing new series of potent carbonic anhydrase II inhibitors. The aromatic fragment associated with pharmacophore was altered suitably in order to find effective inhibitors of CA-II. All the derivatives 4a-4m showed better inhibition compared to the standard acetazolamide. In particular, compound 4l exhibited significant inhibition with IC ₅₀ value of 0.01796 ± 0.00036 µM. The chemo-informatics analysis justified that all the designed compounds possess <10 HBA and <5 HBD. The ligands-protein binding analyses showed that 4l confined in the active binding pocket with three hydrogen bonds observed with His63, Asn66 and Thr197 residues.

Original language	English
Pages (from-to)	624-630
Number of pages	7
Journal	Bioorganic chemistry
Volume	86
E-pub ahead of print	10 Feb 2019
DOIs	https://doi.org/10.1016/j.bioorg.2019.01.060
Publication status	Published - May 2019

Keywords

Binding analysis
Carbonic anhydrase II inhibition
Chemo-informatics
Hybrid pharmacophore
Synthesis

ASJC Scopus subject areas

Biochemistry
Molecular Biology
Drug Discovery
Organic Chemistry

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10.1016/j.bioorg.2019.01.060

Cite this

Ahmed, A., Channar, P. A., Saeed, A., Kalesse, M., Kazi, M. A., Larik, F. A., Abbas, Q., Hassan, M., Raza, H., & Seo, S. Y. (2019). Synthesis of sulfonamide, amide and amine hybrid pharmacophore, an entry of new class of carbonic anhydrase II inhibitors and evaluation of chemo-informatics and binding analysis. Bioorganic chemistry, 86, 624-630. https://doi.org/10.1016/j.bioorg.2019.01.060

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title = "Synthesis of sulfonamide, amide and amine hybrid pharmacophore, an entry of new class of carbonic anhydrase II inhibitors and evaluation of chemo-informatics and binding analysis",

abstract = " Selective inhibition of carbonic anhydrase (CA) enzyme is an active area of research for medicinal chemists. In the current account, a hybrid pharmacophore approach was employed to design sulfonamide, amide and amine containing new series of potent carbonic anhydrase II inhibitors. The aromatic fragment associated with pharmacophore was altered suitably in order to find effective inhibitors of CA-II. All the derivatives 4a-4m showed better inhibition compared to the standard acetazolamide. In particular, compound 4l exhibited significant inhibition with IC 50 value of 0.01796 ± 0.00036 µM. The chemo-informatics analysis justified that all the designed compounds possess <10 HBA and <5 HBD. The ligands-protein binding analyses showed that 4l confined in the active binding pocket with three hydrogen bonds observed with His63, Asn66 and Thr197 residues. ",

keywords = "Binding analysis, Carbonic anhydrase II inhibition, Chemo-informatics, Hybrid pharmacophore, Synthesis",

author = "Attique Ahmed and Channar, \{Pervaiz Ali\} and Aamer Saeed and Markus Kalesse and Kazi, \{Mehar Ali\} and Larik, \{Fayaz Ali\} and Qamar Abbas and Mubashir Hassan and Hussain Raza and Seo, \{Sung Yum\}",

year = "2019",

month = may,

doi = "10.1016/j.bioorg.2019.01.060",

language = "English",

volume = "86",

pages = "624--630",

journal = "Bioorganic chemistry",

issn = "0045-2068",

publisher = "Academic Press Inc.",

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Ahmed, A, Channar, PA, Saeed, A, Kalesse, M, Kazi, MA, Larik, FA, Abbas, Q, Hassan, M, Raza, H & Seo, SY 2019, 'Synthesis of sulfonamide, amide and amine hybrid pharmacophore, an entry of new class of carbonic anhydrase II inhibitors and evaluation of chemo-informatics and binding analysis', Bioorganic chemistry, vol. 86, pp. 624-630. https://doi.org/10.1016/j.bioorg.2019.01.060

Synthesis of sulfonamide, amide and amine hybrid pharmacophore, an entry of new class of carbonic anhydrase II inhibitors and evaluation of chemo-informatics and binding analysis. / Ahmed, Attique; Channar, Pervaiz Ali; Saeed, Aamer et al.
In: Bioorganic chemistry, Vol. 86, 05.2019, p. 624-630.

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

TY - JOUR

T1 - Synthesis of sulfonamide, amide and amine hybrid pharmacophore, an entry of new class of carbonic anhydrase II inhibitors and evaluation of chemo-informatics and binding analysis

AU - Ahmed, Attique

AU - Channar, Pervaiz Ali

AU - Saeed, Aamer

AU - Kalesse, Markus

AU - Kazi, Mehar Ali

AU - Larik, Fayaz Ali

AU - Abbas, Qamar

AU - Hassan, Mubashir

AU - Raza, Hussain

AU - Seo, Sung Yum

PY - 2019/5

Y1 - 2019/5

N2 - Selective inhibition of carbonic anhydrase (CA) enzyme is an active area of research for medicinal chemists. In the current account, a hybrid pharmacophore approach was employed to design sulfonamide, amide and amine containing new series of potent carbonic anhydrase II inhibitors. The aromatic fragment associated with pharmacophore was altered suitably in order to find effective inhibitors of CA-II. All the derivatives 4a-4m showed better inhibition compared to the standard acetazolamide. In particular, compound 4l exhibited significant inhibition with IC 50 value of 0.01796 ± 0.00036 µM. The chemo-informatics analysis justified that all the designed compounds possess <10 HBA and <5 HBD. The ligands-protein binding analyses showed that 4l confined in the active binding pocket with three hydrogen bonds observed with His63, Asn66 and Thr197 residues.

AB - Selective inhibition of carbonic anhydrase (CA) enzyme is an active area of research for medicinal chemists. In the current account, a hybrid pharmacophore approach was employed to design sulfonamide, amide and amine containing new series of potent carbonic anhydrase II inhibitors. The aromatic fragment associated with pharmacophore was altered suitably in order to find effective inhibitors of CA-II. All the derivatives 4a-4m showed better inhibition compared to the standard acetazolamide. In particular, compound 4l exhibited significant inhibition with IC 50 value of 0.01796 ± 0.00036 µM. The chemo-informatics analysis justified that all the designed compounds possess <10 HBA and <5 HBD. The ligands-protein binding analyses showed that 4l confined in the active binding pocket with three hydrogen bonds observed with His63, Asn66 and Thr197 residues.

KW - Binding analysis

KW - Carbonic anhydrase II inhibition

KW - Chemo-informatics

KW - Hybrid pharmacophore

KW - Synthesis

UR - https://www.scopus.com/pages/publications/85061924955

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DO - 10.1016/j.bioorg.2019.01.060

M3 - Article

C2 - 30807935

AN - SCOPUS:85061924955

SN - 0045-2068

VL - 86

SP - 624

EP - 630

JO - Bioorganic chemistry

JF - Bioorganic chemistry

ER -

Synthesis of sulfonamide, amide and amine hybrid pharmacophore, an entry of new class of carbonic anhydrase II inhibitors and evaluation of chemo-informatics and binding analysis

Abstract

Keywords

ASJC Scopus subject areas

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