Name: receptors and other targets for toxic substances: proceedings of the european society of toxicology, meeting held in budapest, june 11 14, 1984 (en Inglés)
Price: 163800.00 CLP
Availability: InStock
Author: Chambers, P. L. ; Cholnoky, E. ; Chambers, C.
ISBN: 9783540136705

portada receptors and other targets for toxic substances: proceedings of the european society of toxicology, meeting held in budapest, june 11 14, 1984 (en Inglés)

Formato

Libro Físico

Ilustrado por

Editorial

Autor

Chambers, P. L. ; Cholnoky, E. ; Chambers, C.

Año

1986

Idioma

Inglés

N° páginas

520

Encuadernación

Tapa Blanda

Dimensiones

24.4 x 17.0 x 2.7 cm

Peso

0.84 kg.

ISBN

3540136703

ISBN13

9783540136705

Categorías

Farmacología
Farmacia y prescripción
Bioquímica

receptors and other targets for toxic substances: proceedings of the european society of toxicology, meeting held in budapest, june 11 14, 1984 (en Inglés)

P. L. Chambers (Ilustrado por) · E. Cholnoky (Ilustrado por) · C. Chambers (Ilustrado por) · Springer · Tapa Blanda

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Reseña del libro "receptors and other targets for toxic substances: proceedings of the european society of toxicology, meeting held in budapest, june 11 14, 1984 (en Inglés)"

Trichloroethylene (TRI), administered orally at high doses for 18 months has been shown to increase the incidence of hepatocellular carcinoma in B6C3F 1 mice but not Osborne-Mendel rats (NCI, 1976). The interpretation of these studies has been confounded due to the presence of epoxide stabilizers in the TRI. However more recent studies have demonstrated that pure TRI also causes hepatocellular carcinoma in B6C3F mice (NTP, 1983) and Aldedey Park (Swiss) mice (Elcombe 1 and Pratt, unpublished data). Furthermore, no increase in the incidence of hepatocellular carcinoma was observed in Fisher 344 rats administered pure TRI (NTP, 1983). TRI has been extensively examined for mutagenic potential, but many studies were bedeviled by the presence of mutagenic epoxide stabilizers. However, in general, TRI has been found to be only 'marginally' mutagenic or non-mutagenic (Greim et ai., 1975; Simmon et ai., 1977; Bronzetti et ai., 1978; Waskell, 1978; Bartsch et ai., 1979; Slacik-Erben et ai., 1980). Covalent binding of trichloroethylene or its metabolites to protein, RNA and DNA has been illustrated in vitro (Van Duuren and Banerjee, 1976; Bolt et ai., 1977; Bolt and Filser, 1977; Uehleke and Poplawski-Tabarelli, 1977; Banerjee and Van Dauren, 1978). However, in vivo, only extremely low (indistinguishable from protein binding) or zero binding of TRI metabolites to DNA has been reported (Parchman and Magee, 1982; Stott et ai., 1982).