Comprehensive and definitive structural identities of Pneumocystis carinii sterols

Pneumocystis causes a type of pneumonia in immunodeficient mammals, such as AIDS patients. Mammals cannot alkylate the C-24 position of the sterol side chain, nor can they desaturate C-22. Thus, the reactions leading to these sterol modifications are particularly attractive targets for the developme...

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Published inJournal of lipid research Vol. 43; no. 7; pp. 1114 - 1124
Main Authors Giner, José-Luis, Zhao, Hui, Beach, David H, Parish, Edward J, Jayasimhulu, Koka, Kaneshiro, Edna S
Format Journal Article
LanguageEnglish
Published United States Elsevier 01.07.2002
Subjects
24-alkylsterols
Acquired Immunodeficiency Syndrome - parasitology
AIDS
Animals
Chromatography, Gas
Chromatography, High Pressure Liquid
drug targets
gas-liquid chromatography
Magnetic Resonance Spectroscopy
mass spectrometry
Molecular Structure
opportunistic infections
Pneumocystis - chemistry
Rats
Sterols - chemistry
Sterols - isolation & purification
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Summary:Pneumocystis causes a type of pneumonia in immunodeficient mammals, such as AIDS patients. Mammals cannot alkylate the C-24 position of the sterol side chain, nor can they desaturate C-22. Thus, the reactions leading to these sterol modifications are particularly attractive targets for the development of drugs against fungal and protozoan pathogens that make them. In the present study, the definitive structures of 43 sterol molecular species in rat-derived Pneumocystis carinii were elucidated by nuclear magnetic resonance spectroscopy. Ergosterol, Delta(5,7) sterols, trienes, and tetraenes were not among them. Most (32 of the 43) were 24-alkylsterols, products of S-adenosyl-L-methionine:C-24 sterol methyl transferase (SAM:SMT) enzyme activity. Their abundance is consistent with the suggestion that SAM:SMT is highly active in this organism and that the enzyme is an excellent anti-Pneumocystis drug target. In contrast, the comprehensive analysis strongly suggest that P. carinii does not form Delta(22) sterols, thus C-22 desaturation does not appear to be a drug target in this pathogen. The lanosterol derivatives, 24-methylenelanost-8-en-3 beta-ol and (Z)-24-ethylidenelanost-8-en-3 beta-ol (pneumocysterol), previously identified in human-derived Pneumocystis jiroveci, were also detected among the sterols of the rat-derived P. carinii organisms.
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ISSN:0022-2275
DOI:10.1194/jlr.M200113-JLR200