Gene/Protein Disease Symptom Drug Enzyme Compound
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Query: UMLS:C0023418 (leukemia)
 93,477 document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)

The synthesis, characterization and biological activity of the first zinc(II) complexes with potent inhibitors of cyclin-dependent kinases (CDKs) derived from 6-benzylaminopurine are described. Based on the results following from elemental analyses, infrared, NMR and ES+MS (electrospray mass spectra in the positive ion mode) spectroscopies, conductivity data, thermal analysis and X-ray structures, the tetrahedral Zn(II) complexes of the compositions [Zn(Olo)Cl(2)](n) (1), [Zn(iprOlo)Cl(2)](n) (2), [Zn(BohH(+))Cl(3)] x H(2)O (3) and [Zn(iprOloH(+))Cl(3)] x H(2)O (4) have been prepared, where Olo=2-(2-hydroxyethylamino)-6-benzylamino-9-methylpurine (Olomoucine), iprOlo=2-(2-hydroxyethylamino)-6-benzylamino-9-isopropylpurine (i-propyl-Olomoucine), Boh=2-(3-hydroxypropylamino)-6-benzylamino-9-isopropylpurine (Bohemine). The 1D-polymeric chain structure for [Zn(Olo)Cl(2)](n) (1) as well as the monomeric one for [Zn(BohH(+))Cl(3)] x H(2)O (3) and [Zn(iprOloH(+))Cl(3)] x H(2)O (4) have been revealed unambiguously by single crystal X-ray analyses. The 1D-polymeric chain of 1 consists of Zn(Olo)Cl(2) monomeric units in which the Zn(II) ion is coordinated by two chlorine atoms and one oxygen atom of the 2-hydroxyethylamino group of Olomoucine. The next monomeric unit is bonded to Zn(II) through the N7 atom of a purine ring. Thus, each of Zn(II) ions is tetrahedrally coordinated and a ZnCl(2)NO chromophore occurs in the complex 1. The complexes 3 and 4 are mononuclear species with a distorted tetrahedral arrangement of donor atoms around the Zn(II) ion with a ZnCl(3)N chromophore. The corresponding CDK inhibitor, i.e., both Boh and iprOlo, is coordinated to Zn(II) via the N7 atom of the purine ring in 3 and 4. The cytotoxicity of the zinc(II) complexes against human melanoma, sarcoma, leukaemia and carcinoma cell lines has been determined as well as the inhibition of the CDK2/cyclin E kinase. A relationship between the structure and biological activity of the complexes is also discussed.
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PMID:Zinc(II) complexes with potent cyclin-dependent kinase inhibitors derived from 6-benzylaminopurine: synthesis, characterization, X-ray structures and biological activity. 1638 95

Olomoucine (OLO), a substituted purine analogue, is a much weaker inhibitor of cyclin-dependent kinases than other closely related ATP derivatives. It has been recently reported that OLO did not affect the viability of normal human MRC-5 fibroblasts, but it inhibited the proliferation of human HL-60 leukemia cells. Therefore, it was interesting to explore the antiproliferative effect of OLO and to characterize its action on distinct human cancer cells differing in the functional status of the cell cycle. Human HeLa cervical carcinoma and HL-60 leukemia cells were continuously exposed to increasing concentrations of OLO for 24 h and 48 h or alternatively, cells after treatment for 24 h were postincubated in a drug-free medium. Surprisingly, OLO more strongly affected the proliferation of HL-60 cells than that of HeLa cells. Flow cytometric analyses revealed that OLO at higher doses increases the frequency of a hypoploid HL-60 cell population representing cells undergoing apoptosis. These results substantiated the data of the determination of the number of viable cells. Moreover, OLO at higher doses modulates the cell cycle progression of tested cancer cells. Detailed analyses of the DNA concentration in single cells revealed that OLO-mediated reduction of the number of G(1)-phase cells was accompanied by an increase of the frequency of G(2)-phase cells. The kinetics of these changes differed between both tested cancer cell lines, suggesting that some cancer cells exhibit increased susceptibility to OLO action. It remains to clarify whether the strong proapoptotic effect of OLO observed in HL-60 cells depends on their differentiation status.
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PMID:Is olomoucine, a weak CDK2 inhibitor, able to induce apoptosis in cancer cells? 1972 61