Model studies on the spiro intermediate

Hawker, Craig Jon

January 1988

No description available.

547

Haem and chlorophyll synthesis

Development of biomarkers in Daphnia magna for the detection of sub-lethal toxicity of urban groundwater pollution

Connon, Richard

January 2003

No description available.

363

Haem peroxidase

5-aminolaevulinic acid synthase activity in human erythroblasts

Fitzsimons, E. J.

January 1986

No description available.

572

Hepatic haem biosynthesis

Towards the synthesis of model peroxidases

Varejao, Jorge Manuel Tavares Branco

January 2000

No description available.

572

Haem; Lignin; Porphyrins

Studies on experimental hepatic porphyria

Holley, Ann E.

January 1987

Intraperitoneal administration of 3,5-diethoxy-carbonyl-1,4-dihydrocollidine (DDC) to female C3H/He/01a and NIH/01a inbred mice produced a marked dose-dependent loss of hepatic ferrochelatase (FK) activity, induction of g-aminolaevulinic acid synthetase (ALA-S) and accumulation of protoporphyrin. There was no strain difference in the degree of FK inhibition. However, induction of ALA-S was greater in C3H/He/01a mice. The strain difference in ALA-S response was most marked when inhibition of FK (the "specific" effect of DDC) was maximal and this suggests that a genetic variation exists in the sensitivity of ALA-S to a second, "non-specific" action of DDC, possibly related to its property of lipid-solubility. A sex difference in griseofulvin (GF)-induced porphyria was found with a greater hepatic protoporphyrin accumulation in male mice of all three strains examined. Stimulation of ALA-S activity was slightly greater in males, but when porphyria was very marked, ALA-S levels were significantly lower in this sex. These, and other, results demonstrated a two-way relationship between ALA-S activity and porphyrin accumulation, with a repression of ALA-S activity occuring at high liver protoporphyrin concentrations. Using a new method to add drugs in solution to cultures of chick embryo hepatocytes, the porphyrogenic effects of various drugs was compared. DDC and ISO-griseofulvin markedly inhibited FK activity and caused accumulation of protoporphyrin. In this system, ISO-griseofulvin was a more potent inhibitor of FK activity than either GF or HET-griseofulvin and also produced a greater accumulation of protoporphyrin, as previously reported in rodents. The hepatic green pigment accumulating in DDC, GF and ISO-griseofulvin-treated mice has been isolated, purified and identified as N-MePP, a previously established inhibitor of FK. All four possible structural isomers were demonstrated and each drug produced primarily the same isomer. An additional hepatic green pigment has been isolated from GF-treated mice, and spectral characteristics suggest this pigment is also an N-mono-substituted porphyrin, but its identity has not yet been established.

572

Haem biosynthetic regulation

Studies of haem biosynthesis and metabolism by high-performance liquid chromatography

Li, F.

January 1987

No description available.

572

Haem analysis by HPLC

Structural studies on liganded T state haemoglobin

Paoli, Massimo

January 1995

No description available.

572

Expression and site-directed mutagenesis of a bacterial nitric oxide reductase

Butland, Gareth Paul

January 2000

No description available.

572

Respiratory; Haem-copper; Oxidases

The cytochrome bâ‚… fold : equilibrium and kinetic studies of folding and unfolding reactions in wild type, apo and variant proteins

Manyusa, Susan

January 1999

No description available.

572

X-ray crystallographic studies of enzymes by molecular replacement

Mohammed, Fiyaz

January 2001

No description available.

572