## Abstract Our recent studies have shown that the vitamin D analog Roโ26โ9228 restores bone mineral density without inducing hypercalcemia in osteopenic rats. Our ex vivo experiments demonstrated that the analog upregulated gene expression in trabecular bone but not in the duodenum of female rats.
Rationale for active vitamin D and analogs in the treatment of osteoporosis
โ Scribed by Yasuho Nishii
- Publisher
- John Wiley and Sons
- Year
- 2002
- Tongue
- English
- Weight
- 114 KB
- Volume
- 88
- Category
- Article
- ISSN
- 0730-2312
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โฆ Synopsis
Abstract
In 1981, Chugai Pharmaceutical succeeded in marketing alfacalcidol, a prodrug of calcitriol, as a therapeutic agent for renal osteodystrophy. In 1983, Chugai succeeded in extending the application of alfacalcidol to the treatment of osteoporosis as well. Clinicians in Japan have accepted alfacalcidol as a remedy for osteoporosis. However, the use of calcitriol and its analogs for the treatment of osteoporosis is still controversial. Some misunderstandings exist internationally about the efficacy of the active form of vitamin D for the treatment of osteoporosis. It is important to emphasize that patients with osteoporosis have intestinal calcium malabsorption and dysfunction in renal activation of vitamin D. When massive doses of parent vitamin D were administered to OVX rats, bone mass increased, but surprisingly, many porotic area were observed in the cortical bone. On the other hand, administration of alfacalcidol increased physiological bone without porotic observation. It is necessary to give the active form of vitamin D, Dโhormone, with an RDAโequivalent supply of calcium. Alfacalcidol forms physiological strong bones that are hardly fractured by regulating calcium and bone metabolism. We proposed a new vitamin D analog, 2ฮฒ (3โhydroxypropoxy)calcitriol [EDโ71] as a therapeutic drug for osteoporosis, which is more potent than calcitriol. EDโ71 is now being investigated in phase 2 clinical studies in Japan. EDโ71 will appear as more improved drugs for osteoporosis until 2010. J. Cell. Biochem. 88: 381โ386, 2003. ยฉ 2002 WileyโLiss, Inc.
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