Novel Transplatinum(II) Complexes with [N 2 O 2 ] Donor Sets. Cellular Pharmacology and Apoptosis Induction in Pam 212- r as Cells

Artigo Revisado por pares

Novel Transplatinum(II) Complexes with [N 2 O 2 ] Donor Sets. Cellular Pharmacology and Apoptosis Induction in Pam 212- r as Cells

2005; American Chemical Society; Volume: 49; Issue: 1 Linguagem: Inglês

10.1021/jm050804v

ISSN

1520-4804

Autores

Adoración G. Quiroga, Jose M. Pérez, Carlos Alonso‐Moreno, Carmen Navarro‐Ranninger, Nicholas Farrell,

Tópico(s)

Ferrocene Chemistry and Applications

Resumo

Cellular pharmacological properties of eight trans-picoline platinum(II) complexes of formula trans-[PtX2(L)(L')], where X = Cl or CH3COO (OAc) and L = L' = 3-picoline (3-pic), 4-picoline (4-pic) or L = NH3 and L' = 3-pic or 4-pic, were investigated in murine keratinocyte Pam 212 cells and Pam 212-ras cells, murine tumor keratinocytes derived from transformation with a viral vector containing the H-ras oncogene. The derivatives trans-[Pt(OAc)2(L)(L')] (L = L' = 3-pic, 9, and L = L' = 4-pic, 10) were able to circumvent resistance in Pam 212-ras cells. Although all the trans-picoline platinum(II) acetate derivatives showed a similar level of DNA binding, there were remarkable differences in cellular accumulation: the complexes having two picoline ligands (9, 10) had a much higher intracellular accumulation than those having mixed picoline and ammine ligands (11, 12). No significant differences in cellular pharmacological properties have been observed between isomers having 3- or 4-picoline.

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Novel Transplatinum(II) Complexes with [N 2 O 2 ] Donor Sets. Cellular Pharmacology and Apoptosis Induction in Pam 212- r as Cells