1.Dehydroepiandrosterone-dependent induction of peroxisomal proliferation can be reduced by aspartyl esterification without attenuation of inhibitory bone loss in ovariectomy animal model.
Chung Shil KWAK ; Chang Mo KANG ; Heun Soo KANG ; Kye Yong SONG ; Mee Sook LEE ; Sang Cheol SEONG ; Sang Chul PARK
Journal of Korean Medical Science 2000;15(5):533-541
The purpose of this study was to determine whether esterification of dehydroepiandrosterone with aspartate (DHEA-aspartate) could reduce peroxisomal proliferation induced by DHEA itself, without loss of antiosteoporotic activity. Female Sprague-Dawley rats were ovariectomized, then DHEA or DHEA-aspartate was administered intraperitoneally at 0.34 mmol/kg BW 3 times a week for 8 weeks. DHEA-aspartate treatment in ovariectomized rats significantly increased trabeculae area in tibia as much as DHEA treatment. Urinary Ca excretion was not significantly increased by DHEA or DHEA-aspartate treatment in ovariectomized rats, while it was significantly increased by ovariectomy. Osteocalcin concentration and alkaline phosphatase activity in serum and cross linked N-telopeptide type I collagen level in urine were not significantly different between DHEA-aspartate and DHEA treated groups. DHEA-aspartate treatment significantly reduced liver weight and hepatic palmitoyl-coA oxidase activity compared to DHEA treatment. DHEA-aspartate treatment maintained a nearly normal morphology of peroxisomes, while DHEA treatment increased the number and size of peroxisomes in the liver. According to these results, it is concluded that DHEA-aspartate ester has an inhibitory effect on bone loss in ovariectomized rats with a marked reduction of hepatomegaly and peroxisomal proliferation compared to DHEA.
Adjuvants, Immunologic/pharmacology*
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Adjuvants, Immunologic/metabolism
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Adjuvants, Immunologic/chemistry
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Animal
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Aspartic Acid/pharmacology*
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Aspartic Acid/metabolism
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Aspartic Acid/chemistry
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Biological Markers
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Calcium/urine
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Calcium/blood
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Disease Models, Animal
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Esterification
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Fatty Acid Desaturases/metabolism
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Female
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Injections, Intraperitoneal
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Lipoproteins, HDL Cholesterol/blood
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Lipoproteins, LDL Cholesterol/blood
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Liver/enzymology
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Liver/drug effects
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Organ Weight
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Osteoporosis/pathology
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Osteoporosis/metabolism*
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Osteoporosis/drug therapy*
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Ovariectomy*
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Peroxisomes/metabolism*
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Prasterone/pharmacology*
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Prasterone/metabolism
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Prasterone/chemistry
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Rats
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Rats, Sprague-Dawley
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Tibia/pathology
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Tibia/metabolism
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Triglycerides/blood
Result Analysis
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