Your search keyword '"PORTER CW"' showing total 7 results

1. Cationic porphyrin derivatives as inhibitors of polyamine catabolism.

Author

Libby PR, Munson BR, Fiel RJ, and Porter CW

Subjects

Acetyltransferases antagonists & inhibitors, Adenosylmethionine Decarboxylase antagonists & inhibitors, Animals, Biogenic Polyamines biosynthesis, Catalysis, Cations, Chelating Agents pharmacology, Humans, Kinetics, Leukemia L1210 enzymology, Melanoma enzymology, Ornithine Decarboxylase Inhibitors, Oxidoreductases Acting on CH-NH Group Donors antagonists & inhibitors, Tumor Cells, Cultured, Polyamine Oxidase, Biogenic Polyamines metabolism, Enzyme Inhibitors pharmacology, Porphyrins pharmacology

Abstract

The effects of six cationic porphyrins on several enzymes involved in polyamine biosynthesis and catabolism have been examined. Both spermidine and spermine synthase were unaffected by the porphyrins at up to 2 mM. By contrast, ornithine and S-adenosylmethionine decarboxylase were inhibited by the nickel and cobalt derivatives of meso-tetrakis(N-methyl-4-pyridiniumyl)porphyrin (T4MPyP) with IC50 values in the 10-100 microM region. Spermidine/spermine N1-acetyltransferase (SSAT) and polyamine oxidase (PAO) were highly sensitive to the six meso-substituted cationic porphyrins tested, with Ki values as low as 6 nM for SSAT and 85 nM for PAO. These inhibitors may prove useful in defining the structural features of the active site of these enzymes.

Published

1995

2. Use of 4-fluoro-L-ornithine to monitor metabolic flux through the polyamine biosynthetic pathway.

Author

Kramer D, Stanek J, Diegelman P, Regenass U, Schneider P, and Porter CW

Subjects

Adenosylmethionine Decarboxylase biosynthesis, Animals, Biogenic Polyamines metabolism, CHO Cells, Cell Division drug effects, Cell Membrane Permeability, Chromatography, High Pressure Liquid, Cricetinae, Humans, Kinetics, Leukemia L1210, Melanoma metabolism, Mice, Ornithine analysis, Ornithine pharmacokinetics, Ornithine pharmacology, Ornithine Decarboxylase biosynthesis, Spermidine metabolism, Spermine metabolism, Tumor Cells, Cultured, Biogenic Polyamines biosynthesis, Ornithine analogs & derivatives

Abstract

The mechanistic effectiveness of various polyamine analogs and enzyme inhibitors is typically determined by their ability to deplete intracellular polyamine pools. In this study, we describe an assay that may prove useful in augmenting this relatively static assessment of drug action. The assay relies upon the substitution of 4-fluoro-L-ornithine (Fl-Orn) for ornithine as a polyamine precursor to provide a means to measure metabolic flux through polyamine pools. At concentrations up to 500 microM, the analog did not inhibit the growth of L1210 murine leukemia cells during incubations of up to 72 hr. Using HPLC, the analog was processed metabolically over time to what was deduced to be 2-fluoroputrescine, 6-fluorospermidine and 6-fluorospermine. The relative proportion of fluorinated polyamine analog to the natural polyamine increased with time and Fl-Orn concentration. The sum of the two was found to be nearly identical to the respective polyamine pool of control cells exposed instead to 500 microM ornithine. This indicates that Fl-Orn was recognized and utilized as a precursor at a rate very similar to that of ornithine itself. Using L1210 cells at different stages of cell growth, it was determined that the metabolic flux through the pools, as indicated by the rate of appearance of individual fluorinated polyamine species, reflected the proliferation status of the cells--non-growing cells failed to incorporate the analog. Likewise, in cell types with varying polyamine pool profiles, such as polyamine enzyme overproducers or those with constitutively different spermidine of spermine ratios, the incorporation of the fluorinated analogs into pools was found to be proportional to the size to the natural polyamine pool. In cells treated with inhibitors of S-adenosylmethionine decarboxylase, Fl-Orn incorporation indicated a total blockade of polyamine synthesis at that enzyme site. Overall, the Fl-Orn assay has demonstrated that polyamine pool profiles generally reflect the rate of flux through the pathway in proliferating cells, suggesting that most intracellular polyamines are freely exchangeable with those undergoing metabolic flux.

Published

1995

3. Inhibition of enzymes of polyamine back-conversion by pentamidine and berenil.

Author

Libby PR and Porter CW

Subjects

Animals, Diminazene pharmacology, Humans, Kinetics, Leukemia L1210 enzymology, Melanoma enzymology, Mice, Polyamine Oxidase, Acetyltransferases antagonists & inhibitors, Diminazene analogs & derivatives, Oxidoreductases Acting on CH-NH Group Donors antagonists & inhibitors, Pentamidine pharmacology

Abstract

Pentamidine and berenil, clinical antiparasitic amidines, have been found to be potent competitive inhibitors of human spermidine/spermine acetyltransferase (SSAT). Ki values were found to be 2.4 and 2 microM, respectively, with spermidine as substrate. A second enzyme of polyamine back-conversion, murine polyamine oxidase (PAO), was found to be competitively inhibited by pentamidine, with a Ki of 7.6 microM when N-acetylspermine was the substrate. Berenil, on the other hand, was an extremely weak inhibitor (Ki = 120 microM). The implication of the effect of inhibition of polyamine back-conversion on the growth of mammalian parasites is discussed.

Published

1992

4. Inhibition of the bioenergetic functions of isolated rat liver mitochondria by polyamines.

Author

Byczkowski JZ, Zychlinski L, and Porter CW

Subjects

Animals, In Vitro Techniques, Kinetics, Liver metabolism, Mitochondria, Liver drug effects, Oxygen Consumption drug effects, Putrescine pharmacology, Rats, Spermidine pharmacology, Spermine pharmacology, Energy Metabolism drug effects, Mitochondria, Liver metabolism, Polyamines pharmacology

Abstract

The abilities of the naturally occurring polyamines, putrescine, spermidine and spermine, to affect variables related to the bioenergetic functions of isolated rat liver mitochondria were studied. At concentrations comparable to those present intracellularly, the polyamines inhibited state 4 respiration, but they had much less effect on state 3 or uncoupled respiration. The concentrations required to produce 25% inhibition (I25) of state 4 respiration varied according to the polyamine, with putrescine being least effective (I25, 20 mM) and spermidine and spermine being more effective and comparable (I25, 7.5 and 7.0 mM respectively). This inhibition was antagonized by 15 mM potassium and enhanced by valinomycin and 4 mM magnesium. Inhibition of monoamine oxidase, an enzyme of outer mitochondrial membrane, was also observed to occur. Addition of polyamines to mitochondrial suspensions caused an increase in the optical density and protected against the swelling effects of sublytic concentrations of Triton X-100. By electron microscopy, polyamines were found to cause the outer mitochondrial compartment to collapse bringing the inner and outer membranes into apparent contact with one another. The electrophoretic mobility of mitochondria toward the anode was markedly slowed by polyamines (i.e. 50% by 1.25 mM spermine), indicating surface binding and neutralization of the negative surface charge. In almost all of the above mitochondrial effects, spermine and spermidine were similar in effectiveness and putrescine was less effective. It is suggested that polyamines may be capable of modulating respiration of isolated mitochondria by binding to non-specific anionic sites at the surface of the inner mitochondrial membrane. Neutralization of the net negative surface potential may interfere with cation fluxes across the membrane, particularly those of potassium.

Published

1982

5. Effects of a membrane sugar analogue, 6-deoxy-6-fluoro-D-galactose, on the L1210 leukemic cell ectosialyltransferase system.

Author

Morin MJ, Porter CW, Petrie CR 3rd, Korytnyk W, and Bernacki RJ

Subjects

Animals, Cells, Cultured, Fucose pharmacology, Galactose metabolism, Kinetics, Mice, beta-D-Galactoside alpha 2-6-Sialyltransferase, Fucose analogs & derivatives, Leukemia L1210 enzymology, Sialyltransferases metabolism, Transferases metabolism

Abstract

In L1210 leukemia cells, 6-deoxy-6-fluoro-D-galactose specifically inhibited the incorporation of [3H]-D-galactose, while that of other precursors of glycoconjugate biosynthesis, including mannose and glucosamine, was unaffected. The activation of [6-3H]-6-deoxy-6-fluoro-D-galactose to a nucleotide sugar was similar to that found for [3H]-D-galactose. The incorporation of either sugar after 1 hr was visualized by electron microscopic autoradiography to be in the Golgi region. Treatment of L1210 cells with 6-deoxy-6-fluoro-D-galactose in vitro or in vivo resulted in a specific, dose- and time-dependent decrease in the activity of cell surface sialyltransferase (ectosialyltransferase) but not of 5'-nucleotidase, a plasma membrane marker enzyme. The decrease in ectosialyltransferase activity appeared to be selective and is suggested to be due to structural modification of the cell surface galactoprotein acceptors for this enzyme. The data indicate that 6-deoxy-6-fluoro-D-galactose is an effective modifier of cellular glycoconjugate in that its incorporation into certain cell surface components results in a modification of plasma membrane structure and function.

Published

1983

6. Structure-function correlations of polyamine analog-induced increases in spermidine/spermine acetyltransferase activity.

Author

Libby PR, Bergeron RJ, and Porter CW

Subjects

Animals, Eflornithine pharmacology, Enzyme Induction drug effects, Leukemia L1210 enzymology, Mice, Structure-Activity Relationship, Acetyltransferases biosynthesis, Polyamines pharmacology

Abstract

The cytosolic enzyme, spermidine/spermine acetyltransferase (SSAT), is distinguished by its role in polyamine interconversion and by its high inducibility in response to a variety of physiological and pharmacological stimuli. Among a series of fifteen polyamines and polyamine analogs, the most potent inducers of SSAT activity in cultured L1210 cells were found to be N1,N8-bis(ethyl)spermidine (BES) and N1,N12-bis(ethyl)spermine (BESm). Over a 24-hr exposure at 10 microM, enzyme activity rose 13- and 16-fold with BES and BESm, respectively, compared to 2- to 3-fold with the anticancer agent, methylglyoxal bis(guanylhydrazone). The increase in enzyme activity by BESm began rapidly and continued steadily with time so that by 48 hr it increased to about twenty times control. By inhibitor studies, the increase was found to be due to elevated protein synthesis predominantly at the level of translation and to an apparent prolongation of enzyme half-life related to enzyme stabilization. Among the analogs, the structural requirements for maximum enzyme induction were found to be critically dependent on aminopropyl moieties and on the presence, size and location of the alkyl groups. By structure-function comparisons, it was deduced that the known abilities of BES and BESm to regulate ornithine and S-adenosylmethionine decarboxylase activities or to inhibit cell growth occur independently of their effects on SSAT activity in L1210 cells.

Published

1989

7. Actions of bis(guanylhydrazones) on isolated rat liver mitochondria.

Author

Byczkowski JZ, Salamon W, Harlos JP, and Porter CW

Subjects

Adenosine Triphosphate biosynthesis, Animals, Dose-Response Relationship, Drug, Microscopy, Electron, Mitochondria, Liver ultrastructure, Mitochondrial Swelling drug effects, Monoamine Oxidase metabolism, Oxygen Consumption drug effects, Rats, Carbanilides pharmacology, Guanidines pharmacology, Mitochondria, Liver drug effects, Mitochondria, Liver metabolism, Mitoguazone pharmacology

Published

1981