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Antimetabolic activities of 2-fluoro-L-histidine. |
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| Authors: | E De Clercq A Billiau V G Edy K L Kirk L A Cohen |
| Affiliation: | Laboratory of Virology, Rega Institute for Medical Research, University of Leuven, B-3000 Leuven, Belgium;Laboratory of Chemistry, National Institute of Arthritis, Metabolism and Digestive Diseases National Institutes of Health, Bethesda, Maryland 20014 USA |
| Abstract: | 2-Fluoro-L-Histidine inhibits protein synthesis in various cell cultures, as measured by 3H-leucine incorporation. This histidine analog also inhibits the cytopathogenicity of a number of RNA and DNA viruses in primary and continuous cell cultures; it blocks the transformation of normal mouse (MO) cells by murine sarcoma virus, and partially suppresses the release of murine leukemia virus by a continuously infected mouse cell line (JLSV5). In human skin fibroblasts, it reduces the interferon-inducing capacity of poly(I)·poly(C). Inhibition of cell protein synthesis may be the common cause of the various effects. 4-Fluoro-L-histidine is essentially inert in all of the test systems examined. |
| Keywords: | FPhe 2-FHis 2-fluoro-L-histidine 4-FHis 4-fluoro-L-histidine PFU plaque-forming units VSV vesicular stomatitis virus HSV-1 herpes simplex virus (type 1) Coxs. B4 Coxsackie (type B4) MSV murine (Moloney) sarcoma virus PRK primary rabbit kidney VERO African green monkey kidney cell line MO a 3T3 mouse cell line HSF human skin fibroblast JLSV5 |
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