AQUA[1-(2,6-DICHLORO-4-HYDROXYPHENYL)-2-PHENYLETHYLENEDIAMINE]SULFATOPLATINUM(II) COMPLEXES WITH VARIABLE SUBSTITUENTS IN THE 2-PHENYL RING .2. CORRELATION OF MOLECULAR-STRUCTURE AND ESTROGENIC ACTIVITY OF BREAST AND PROSTATE-CANCER INHIBITING [ERYTHRO-1-(2,6-DICHLOR-4-HYDROXY-PHENYL)-2-(2-HALO-4-HYDROXYPHENYL)ETHYLENEDIAMINE]PLATINUM(II) COMPLEXES

GUST, R and SCHONENBERGER, H and KLEMENT, U and RANGE, KJ (1993) AQUA[1-(2,6-DICHLORO-4-HYDROXYPHENYL)-2-PHENYLETHYLENEDIAMINE]SULFATOPLATINUM(II) COMPLEXES WITH VARIABLE SUBSTITUENTS IN THE 2-PHENYL RING .2. CORRELATION OF MOLECULAR-STRUCTURE AND ESTROGENIC ACTIVITY OF BREAST AND PROSTATE-CANCER INHIBITING [ERYTHRO-1-(2,6-DICHLOR-4-HYDROXY-PHENYL)-2-(2-HALO-4-HYDROXYPHENYL)ETHYLENEDIAMINE]PLATINUM(II) COMPLEXES. ARCHIV DER PHARMAZIE, 326 (12). pp. 967-976. ISSN 0365-6233,

Full text not available from this repository.

Abstract

Complete three-dimensional X-ray crystal structure analyses of estrogenic [erythro-1-(2,6-dichloro-4-hydroxyphenyl)-2-(2-halo-4-hydroxyphenyl)ethylenediamine]diiodoplatinum(II) complexes (halo = fluoro:erythro-8-PtI2 and halo = chloro:erythro-9-PtI2) which were synthesized for application in breast and prostate cancer, have been carried out. 6239 as well as 6521 reflexes were measured and refined to an R-value of 0.105 and 0.066, respectively. The molecules of erythro-8-PtI2 are displaced laterally from a possible Pt-Pt-axis separated, alternatingly, by Pt-Pt-distances of 3.62 Angstrom A and 6.27 Angstrom A. a comparable structure possesses erythro-9-PtI2 with Pt-Pt-distances of 3.59 Angstrom A and 6.32 Angstrom A. the ethylenediamine ligands of erythro-8-PtI2 and erythro-9-PtI2 are puckered and exist in half chair conformations. For both complexes the 2,6-dichloro-4- hydroxyphenyl ring is equatorially arranged, while the 2-halo-4-hydroxyphenyl ring is nearly perpendicular to the N-Pt-N plane. The O-O-distance between the phenolic oxygens amounts to 8.1 Angstrom A in erythro-8-PtI2 and to 7.8 Angstrom A in erythro-9-PtI2. Though these O-O-distances differ strongly from that (12.1 Angstrom A), which is considered to be necessary for the binding of an estrogen to its receptor, [1-(2,6-dichloro-4-hydroxyphenyl-2-(2-halo-4-hydroxyphenyl)ethylenediamine)]platinum(II) complexes show estrogenic effects which are, however, strongly reduced compared to that of therapeutically used estrogens like diethylstilbestrol. The relationship between molecular structure and estrogenicity as well as the significance of the latter for antitumor activity and untoward side effects ate thoroughly discussed.

Item Type: Article
Uncontrolled Keywords: DEPENDENT MAMMARY-CARCINOMA; PLATINUM COMPLEX; ANTI-ESTROGENS; SD-RAT; TUMORS; 1,1,2-TRIPHENYLBUT-1-ENES; ZINDOXIFENE; CISPLATIN; ESTRADIOL; MECHANISM;
Depositing User: Dr. Gernot Deinzer
Last Modified: 19 Oct 2022 08:42
URI: https://pred.uni-regensburg.de/id/eprint/53634

Actions (login required)

View Item View Item
pred is powered by EPrints 3.4 which is developed by the School of Electronics and Computer Science at the University of Southampton. More information and software credits.