N-(INDAZOLYL)BENZAMIDO DERIVATIVES AS CDK1 INHIBITORS: DESIGN, SYNTHESIS, BIOLOGICAL ACTIVITY, AND MOLECULAR DOCKING STUDIES

Salvatore Plescia; Giuseppe Daidone; Benedetta Maggio; Maria Valeria Raimondi; Demetrio Raffa; Stella Maria Cascioferro; Claudia Colomba; Lucina Titone Lanza Di Scalea; Domenico Schillaci; Maria Grazia Cusimano; Claudia Colomba; Manlio Tolomeo; Lucina Titone

N-(INDAZOLYL)BENZAMIDO DERIVATIVES AS CDK1 INHIBITORS: DESIGN, SYNTHESIS, BIOLOGICAL ACTIVITY, AND MOLECULAR DOCKING STUDIES

Salvatore Plescia, Giuseppe Daidone, Benedetta Maggio, Maria Valeria Raimondi, Demetrio Raffa, Stella Maria Cascioferro, Claudia Colomba, Lucina Titone Lanza Di Scalea, Domenico Schillaci, Maria Grazia Cusimano, Claudia Colomba, Manlio Tolomeo, Lucina Titone

Scienze e Tecnologie Biologiche Chimiche e Farmaceutiche
Promozione della Salute, Materno-Infantile, di Medicina Interna e Specialistica di Eccellenza “G. D’Alessandro”

Risultato della ricerca: Article › peer review

14 Citazioni (Scopus)

Abstract

A series of N-1H-indazole-1-carboxamides have been synthesized and their effects on both CDK1/cyclin B and K-562 (human chronic myelogenus leukemia) cell line were evaluated. Using a computational model we have observed that all the most active compound 9e,f,i-n exhibited the same binding mode of Purvanalol A in the ATP-binding cleft. Although they were able to moderately inhibit the leukemic cell line K-562, and to show inhibitory activity against the Cdc2-Cyclin B kinase in the low micromolar range, they resulted non cytotoxic against HuDe (IZSL), primary cell cultures from human derm. These preliminary results are quite encouraging in view of the low toxicity showed by the above mentioned compounds.

Lingua originale	English
pagine (da-a)	265-273
Numero di pagine	9
Rivista	Archiv der Pharmazie
Volume	342
Stato di pubblicazione	Published - 2009

All Science Journal Classification (ASJC) codes

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title = "N-(INDAZOLYL)BENZAMIDO DERIVATIVES AS CDK1 INHIBITORS: DESIGN, SYNTHESIS, BIOLOGICAL ACTIVITY, AND MOLECULAR DOCKING STUDIES",

abstract = "A series of N-1H-indazole-1-carboxamides have been synthesized and their effects on both CDK1/cyclin B and K-562 (human chronic myelogenus leukemia) cell line were evaluated. Using a computational model we have observed that all the most active compound 9e,f,i-n exhibited the same binding mode of Purvanalol A in the ATP-binding cleft. Although they were able to moderately inhibit the leukemic cell line K-562, and to show inhibitory activity against the Cdc2-Cyclin B kinase in the low micromolar range, they resulted non cytotoxic against HuDe (IZSL), primary cell cultures from human derm. These preliminary results are quite encouraging in view of the low toxicity showed by the above mentioned compounds.",

keywords = "1H-indazole-3-carboxamides, CDK1, Molecular docking, N-(1H-indazolyl)benzamides, 1H-indazole-3-carboxamides, CDK1, Molecular docking, N-(1H-indazolyl)benzamides",

author = "Salvatore Plescia and Giuseppe Daidone and Benedetta Maggio and Raimondi, {Maria Valeria} and Demetrio Raffa and Cascioferro, {Stella Maria} and Claudia Colomba and {Titone Lanza Di Scalea}, Lucina and Domenico Schillaci and Cusimano, {Maria Grazia} and Claudia Colomba and Manlio Tolomeo and Lucina Titone",

year = "2009",

language = "English",

volume = "342",

pages = "265--273",

journal = "Archiv der Pharmazie",

issn = "0365-6233",

publisher = "Wiley-VCH Verlag",

}

TY - JOUR

T1 - N-(INDAZOLYL)BENZAMIDO DERIVATIVES AS CDK1 INHIBITORS: DESIGN, SYNTHESIS, BIOLOGICAL ACTIVITY, AND MOLECULAR DOCKING STUDIES

AU - Plescia, Salvatore

AU - Daidone, Giuseppe

AU - Maggio, Benedetta

AU - Raimondi, Maria Valeria

AU - Raffa, Demetrio

AU - Cascioferro, Stella Maria

AU - Colomba, Claudia

AU - Titone Lanza Di Scalea, Lucina

AU - Schillaci, Domenico

AU - Cusimano, Maria Grazia

AU - Colomba, Claudia

AU - Tolomeo, Manlio

AU - Titone, Lucina

PY - 2009

Y1 - 2009

N2 - A series of N-1H-indazole-1-carboxamides have been synthesized and their effects on both CDK1/cyclin B and K-562 (human chronic myelogenus leukemia) cell line were evaluated. Using a computational model we have observed that all the most active compound 9e,f,i-n exhibited the same binding mode of Purvanalol A in the ATP-binding cleft. Although they were able to moderately inhibit the leukemic cell line K-562, and to show inhibitory activity against the Cdc2-Cyclin B kinase in the low micromolar range, they resulted non cytotoxic against HuDe (IZSL), primary cell cultures from human derm. These preliminary results are quite encouraging in view of the low toxicity showed by the above mentioned compounds.

AB - A series of N-1H-indazole-1-carboxamides have been synthesized and their effects on both CDK1/cyclin B and K-562 (human chronic myelogenus leukemia) cell line were evaluated. Using a computational model we have observed that all the most active compound 9e,f,i-n exhibited the same binding mode of Purvanalol A in the ATP-binding cleft. Although they were able to moderately inhibit the leukemic cell line K-562, and to show inhibitory activity against the Cdc2-Cyclin B kinase in the low micromolar range, they resulted non cytotoxic against HuDe (IZSL), primary cell cultures from human derm. These preliminary results are quite encouraging in view of the low toxicity showed by the above mentioned compounds.

KW - 1H-indazole-3-carboxamides

KW - CDK1

KW - Molecular docking

KW - N-(1H-indazolyl)benzamides

KW - 1H-indazole-3-carboxamides

KW - CDK1

KW - Molecular docking

KW - N-(1H-indazolyl)benzamides

UR - http://hdl.handle.net/10447/39023

M3 - Article

SN - 0365-6233

VL - 342

SP - 265

EP - 273

JO - Archiv der Pharmazie

JF - Archiv der Pharmazie

ER -

N-(INDAZOLYL)BENZAMIDO DERIVATIVES AS CDK1 INHIBITORS: DESIGN, SYNTHESIS, BIOLOGICAL ACTIVITY, AND MOLECULAR DOCKING STUDIES

Abstract

All Science Journal Classification (ASJC) codes

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