Polyamine metabolism in a member of the phylum Microspora (Encephalitozoon cuniculi): effects of polyamine analogues

Author:

Bacchi Cyrus J.1,Rattendi Donna1,Faciane Evangeline1,Yarlett Nigel21,Weiss Louis M.3,Frydman Benjamin4,Woster Patrick5,Wei Benjamin5,Marton Laurence J.4,Wittner Murray3

Affiliation:

1. Haskins Laboratories and Department of Biology, Pace University, New York, NY 10038, USA

2. Department of Chemistry, Pace University, New York, NY 10038, USA

3. Departments of Medicine and Pathology, Albert Einstein College of Medicine, Bronx, NY 10461, USA

4. SLIL Biomedical Corp., Madison, WI 53711, USA

5. Department of Pharmaceutical Sciences, College of Pharmacy and Health Sciences, Wayne State University, Detroit, MI 48202, USA

Abstract

The uptake, biosynthesis and catabolism of polyamines in the microsporidian parasiteEncephalitozoon cuniculiare detailed with reference to the effects of oligoamine and arylamine analogues of polyamines.Enc. cuniculi, an intracellular parasite of mammalian cells, has both biosynthetic and catabolic enzymes of polyamine metabolism, as demonstrated in cell-free extracts of mature spores. The uptake of polyamines was measured in immature, pre-emergent spores isolated from host cells by Percoll gradient. Spermine was rapidly taken up and metabolized to spermidine and an unknown, possibly acetamidopropanal, by spermidine/spermineN1-acetyltransferase (SSAT) and polyamine oxidase (PAO). Most of the spermidine and the unknown product were found in the cell incubation medium, indicating they were released from the cell. bis(Ethyl) oligoamine analogues of polyamines, such as SL-11144 and SL-11158, as well as arylamine analogues [BW-1, a bis(phenylbenzyl) 3-7-3 analogue] blocked uptake and interconversion of spermine at micromolar levels and, in the case of BW-1, acted as substrate for PAO. TheEnc. cuniculiPAO activity differed from that found in mammalian cells with respect to pH optimum, substrate specificity and sensitivity to known PAO inhibitors. SL-11158 inhibited SSAT activity with a mixed type of inhibition in which the analogue had a 70-fold higher affinity for the enzyme than the natural substrate, spermine. The interest inEnc. cuniculipolyamine metabolism and the biochemical effects of these polyamine analogues is warranted since they cure model infections ofEnc. cuniculiin mice and are potential candidates for human clinical trials.

Publisher

Microbiology Society

Subject

Microbiology

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