Synthesis, Docking and Biological Activities of Novel Hybrids Celecoxib and Anthraquinone Analogs as Potent Cytotoxic Agents

Synthesis, Docking and Biological Activities of Novel Hybrids Celecoxib and Anthraquinone Analogs as Potent Cytotoxic Agents

Herein, novel hybrid compounds of celecoxib and 2-aminoanthraquinone derivatives have been synthesized using condensation reactions of celecoxib with 2-aminoanthraquinone derivatives or 2-aminoanthraquinon with celecoxib derivatives. Celecoxib was reacted with different acid chlorides, 2-chloroethyl...

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Main Authors: Maha S. Almutairi, Gehan H. Hegazy, Mogedda E. Haiba, Hamed I. Ali, Nagy M. Khalifa, Abd El-mohsen M. Soliman
Format: Article
Language:English
Published: MDPI AG 2014-12-01
Series:International Journal of Molecular Sciences
Subjects:
antitumor
anthraquinone
celecoxib
HEPG2
docking
protein kinase activities
Online Access:http://www.mdpi.com/1422-0067/15/12/22580
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spelling doaj-42922305ee29456f830a5a4af2e838222020-11-24T20:48:25ZengMDPI AGInternational Journal of Molecular Sciences1422-00672014-12-011512225802260310.3390/ijms151222580ijms151222580Synthesis, Docking and Biological Activities of Novel Hybrids Celecoxib and Anthraquinone Analogs as Potent Cytotoxic AgentsMaha S. Almutairi0Gehan H. Hegazy1Mogedda E. Haiba2Hamed I. Ali3Nagy M. Khalifa4Abd El-mohsen M. Soliman5Pharmaceutical Chemistry Department, Faculty of Pharmacy, King Saud University, Riyadh 11451, Saudi ArabiaPharmaceutical Chemistry Department, Faculty of Pharmacy, Cairo University, Cairo 11562, EgyptPharmaceutical Chemistry Department, Faculty of Pharmacy, King Saud University, Riyadh 11451, Saudi ArabiaDepartment of Pharmaceutical Sciences, Irma Lerma Rangel College of Pharmacy, Texas A&M Health Science Center, Kingsville, TX 78363, USAPharmaceutical Chemistry Department, Drug Exploration & Development Chair (DEDC), College of Pharmacy, King Saud University, Riyadh 11451, Saudi ArabiaDepartment of Therapeutical Chemistry, Pharmaceutical and Drug Industries Division, National Research Center, Dokki, Cairo 12622, EgyptHerein, novel hybrid compounds of celecoxib and 2-aminoanthraquinone derivatives have been synthesized using condensation reactions of celecoxib with 2-aminoanthraquinone derivatives or 2-aminoanthraquinon with celecoxib derivatives. Celecoxib was reacted with different acid chlorides, 2-chloroethylisocyanate and bis (2-chloroethyl) amine hydrochloride. These intermediates were then reacted with 2-aminoanthraquinone. Also the same different acid chlorides and 2-chloroethylisocyanate were reacted with 2-aminoanthraquinone and the resulting intermediates were reacted with celecoxib to give isomers for the previous compounds. The antitumor activities against hepatic carcinoma tumor cell line (HEPG2) have been investigated in vitro, and all these compounds showed promising activities, especially compound 3c, 7, and 12. Flexible docking studies involving AutoDock 4.2 was investigated to identify the potential binding affinities and the mode of interaction of the hybrid compounds into two protein tyrosine kinases namely, SRC (Pp60v-src) and platelet-derived growth factor receptor, PDGFR (c-Kit). The compounds in this study have a preferential affinity for the c-Kit PDGFR PTK over the non-receptor tyrosine kinase SRC (Pp60v-src).http://www.mdpi.com/1422-0067/15/12/22580antitumoranthraquinonecelecoxibHEPG2dockingprotein kinase activities
collection DOAJ
language English
format Article
sources DOAJ
author Maha S. Almutairi
Gehan H. Hegazy
Mogedda E. Haiba
Hamed I. Ali
Nagy M. Khalifa
Abd El-mohsen M. Soliman
spellingShingle Maha S. Almutairi
Gehan H. Hegazy
Mogedda E. Haiba
Hamed I. Ali
Nagy M. Khalifa
Abd El-mohsen M. Soliman
Synthesis, Docking and Biological Activities of Novel Hybrids Celecoxib and Anthraquinone Analogs as Potent Cytotoxic Agents
International Journal of Molecular Sciences
antitumor
anthraquinone
celecoxib
HEPG2
docking
protein kinase activities
author_facet Maha S. Almutairi
Gehan H. Hegazy
Mogedda E. Haiba
Hamed I. Ali
Nagy M. Khalifa
Abd El-mohsen M. Soliman
author_sort Maha S. Almutairi
title Synthesis, Docking and Biological Activities of Novel Hybrids Celecoxib and Anthraquinone Analogs as Potent Cytotoxic Agents
title_short Synthesis, Docking and Biological Activities of Novel Hybrids Celecoxib and Anthraquinone Analogs as Potent Cytotoxic Agents
title_full Synthesis, Docking and Biological Activities of Novel Hybrids Celecoxib and Anthraquinone Analogs as Potent Cytotoxic Agents
title_fullStr Synthesis, Docking and Biological Activities of Novel Hybrids Celecoxib and Anthraquinone Analogs as Potent Cytotoxic Agents
title_full_unstemmed Synthesis, Docking and Biological Activities of Novel Hybrids Celecoxib and Anthraquinone Analogs as Potent Cytotoxic Agents
title_sort synthesis, docking and biological activities of novel hybrids celecoxib and anthraquinone analogs as potent cytotoxic agents
publisher MDPI AG
series International Journal of Molecular Sciences
issn 1422-0067
publishDate 2014-12-01
description Herein, novel hybrid compounds of celecoxib and 2-aminoanthraquinone derivatives have been synthesized using condensation reactions of celecoxib with 2-aminoanthraquinone derivatives or 2-aminoanthraquinon with celecoxib derivatives. Celecoxib was reacted with different acid chlorides, 2-chloroethylisocyanate and bis (2-chloroethyl) amine hydrochloride. These intermediates were then reacted with 2-aminoanthraquinone. Also the same different acid chlorides and 2-chloroethylisocyanate were reacted with 2-aminoanthraquinone and the resulting intermediates were reacted with celecoxib to give isomers for the previous compounds. The antitumor activities against hepatic carcinoma tumor cell line (HEPG2) have been investigated in vitro, and all these compounds showed promising activities, especially compound 3c, 7, and 12. Flexible docking studies involving AutoDock 4.2 was investigated to identify the potential binding affinities and the mode of interaction of the hybrid compounds into two protein tyrosine kinases namely, SRC (Pp60v-src) and platelet-derived growth factor receptor, PDGFR (c-Kit). The compounds in this study have a preferential affinity for the c-Kit PDGFR PTK over the non-receptor tyrosine kinase SRC (Pp60v-src).
topic antitumor
anthraquinone
celecoxib
HEPG2
docking
protein kinase activities
url http://www.mdpi.com/1422-0067/15/12/22580
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