METABOLISM OF AMINO-CHLORAMPHENICOL: POSSIBLE ROLE IN CHLORAMPHENICOL-INDUCED APLASTIC ANEMIA AND LEUKEMIA

Teo, Steve Keng Ong

January 1985

No description available.

Chloramphenicol -- Toxicology.

Aplastic anemia.

Selective inactivation of four rat liver microsomal androstenedione hydroxylases by chloramphenicol analogs

Stevens, Jeffrey Charles, 1963-

January 1988

The steroid androstenedione has been shown to be a valuable tool for the study of selective inactivation of rat liver cytochrome P-450 isozymes. The validity of this method was investigated using microsomes, purified cytochromes P-450, cytochrome P-450 antibodies, and the mechanism-based inactivator chloramphenicol. Enzyme inactivation and antibody inhibition studies show that microsomes from phenobarbital- and non-phenobarbital-treated rats are needed to accurately monitor the inactivation of the major phenobarbital-inducible P-450 isozyme (PB-B) and of the major constitutive androstenedione 16-alpha hydroxylase (UT-A). Enzyme inactivation studies showed that the antibiotic chloramphenicol caused different rates of NADPH-dependent enzyme inactivation among four androstenedione hydroxylases (16-beta > 6-beta > 16-alpha > 7-alpha). The results with twelve chloramphenicol analogs show that their selectivity as cytochrome P-450 inactivators is dependent upon at least three structural features: (1) the number of halogen atoms, (2) the presence of a para-nitro group on the phenyl ring, and (3) substitutions on the ethyl side chain.

Chloramphenicol -- Toxicology.

Isoenzymes -- Effect of drugs on.

Antibiotics -- Toxicology.

Cytochrome P-450.

Chloramphenicol-induced toxicity on haemopoiesis

江卓庭, Kong, Cheuk-ting.

January 1998

published_or_final_version / Pathology / Master / Master of Philosophy

Antibiotics - Side effects.

Chloramphenicol - Toxicology.

Chloramphenicol - Side effects.

Bone marrow cells.

Hematopoiesis.