Evaluation of antiproliferative effect of N- (alkyladamantyl)phthalimides in vitro

Horvat, Margareta; Uzelac, Lidija; Marjanović, Marko; Cindro, Nikola; Franković, Oliver; Mlinarić-Majerski, Kata; Kralj, Marijeta; Basarić, Nikola

izvor podataka: crosbi ✓

Evaluation of antiproliferative effect of N- (alkyladamantyl)phthalimides in vitro (CROSBI ID 180366)

Prilog u časopisu | izvorni znanstveni rad | međunarodna recenzija

Horvat, Margareta ; Uzelac, Lidija ; Marjanović, Marko ; Cindro, Nikola ; Franković, Oliver ; Mlinarić-Majerski, Kata ; Kralj, Marijeta ; Basarić, Nikola Evaluation of antiproliferative effect of N- (alkyladamantyl)phthalimides in vitro // Chemical biology & drug design, 79 (2012), 4; 497-506. doi: 10.1111/j.1747-0285.2011.01305.x

Podaci o odgovornosti

Autori

Horvat, Margareta ; Uzelac, Lidija ; Marjanović, Marko ; Cindro, Nikola ; Franković, Oliver ; Mlinarić-Majerski, Kata ; Kralj, Marijeta ; Basarić, Nikola

Osnovni podaci na izvornom jeziku
Osnovni podaci na ostalim jezicima

Jezik

engleski

Naslov

Evaluation of antiproliferative effect of N- (alkyladamantyl)phthalimides in vitro

Sažetak

A series of (1-adamantyl)phthalimides, 1-4, and (2-adamantyl)phthalimides, 5-8, characterized by different chain length between the adamantyl and the phthalimide moiety were synthesized, as well as 1- and 2-adamantylphthalimides substituted by nitro 9, 10, and amino group 11, 12, and phthalimides bearing homoadamantyl 13 and protoadamantyl substituent 14 and 15. The compounds were tested for antiproliferative activity in vitro on a series of five human cancer lines: MCF-7 (breast carcinoma), SW 620 (colon carcinoma), HCT 116 (colon carcinoma), MOLT-4 (acute lymphoblastic leukemia), H 460 (lung carcinoma) and a non-tumor cell line HaCaT (human keratinocytes). All compounds except nitro derivatives 9 and 10 exhibited antiproliferative activity. The activity was generally better in the 2-adamantyl series 5- 8 and in the compounds having the longest alkyl spacers as in 4 and 8, or with an amino group as in 9 and 10. The most active compounds with the propylene spacer 4 and 8 showed the highest selectivity towards tumor cells. The activity was found to be due to a delay in the progress through the cell cycle at G1/S phase.

Ključne riječi

biological screening ; structure-based drug design ; adamantanes ; antiproliferation ; phthalimides

Napomena

nije evidentirano

Jezik

nije evidentirano

Naslov

nije evidentirano

Sažetak

nije evidentirano

Ključne riječi

nije evidentirano

Napomena

nije evidentirano

Podaci o izdanju

Časopis

Chemical biology & drug design

Volumen (broj)

79 (4)

Godina

2012.

Stranice rada

497-506

Status objave rada

objavljeno

ISSN

1747-0277

DOI

10.1111/j.1747-0285.2011.01305.x

Povezanost rada

Povezane osobe

Marijeta Kralj (autor/i)

Nikola Cindro (autor/i)

Nikola Basarić (autor/i)

Margareta Sohora (autor/i)

Kata Majerski (autor/i)

Marko Marjanović (autor/i)

Lidija Uzelac (autor/i)

Povezane ustanove

Institut Ruđer Bošković (098) (autorova ustanova)

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Područje

Kemija, Temeljne medicinske znanosti

Poveznice

doi.org

onlinelibrary.wiley.com

Indeksiranost

Scopus

Current Contents Connect (CCC)

Medline

Web of Science Core Collection, Science Citation Index Expanded (WoSCC-SCI-Exp)

Web of Science Core Collection, SCI-Exp, SSCI & A&HCI (WoSCC-SCI-Exp, SSCI, A&HCI)