Anti-osteoporosis Effect of 5-Bromo-2-(4-chlorobenzoyl)-(Z)-3-(2-cyano-3-hydroxybut-2-enonyl)aminobenzo[b]furan: a Novel Selective Estrogen Receptor Modulator

Ryo Fukuyama; Akio Shimokawa; Yasushi Kodama; Mitsugu Fujita; Yoshitaka Ohishi; Yuko Ando; Masao Koida; Hiromichi Nakamuta

Journal of Pharmacological Sciences (Jan 2011)

Anti-osteoporosis Effect of 5-Bromo-2-(4-chlorobenzoyl)-(Z)-3-(2-cyano-3-hydroxybut-2-enonyl)aminobenzo[b]furan: a Novel Selective Estrogen Receptor Modulator

Ryo Fukuyama,
Akio Shimokawa,
Yasushi Kodama,
Mitsugu Fujita,
Yoshitaka Ohishi,
Yuko Ando,
Masao Koida,
Hiromichi Nakamuta

Affiliations

Ryo Fukuyama: Laboratory of Pharmacology, 5-1-1 Hirokoshingai, Kure, Hiroshima 737-0112, Japan
Akio Shimokawa: Department of Pharmacy, National Hospital Organization Kanmon Medical Center, 1-1 Chofusotoura-cho, Shimonoseki, Yamaguchi 752-8510, Japan
Yasushi Kodama: Laboratory of Molecular and Cellular Pharmacology, Department of Pharmaceutical Sciences, Faculty of Pharmaceutical Sciences, Hiroshima International University, 5-1-1 Hirokoshingai, Kure, Hiroshima 737-0112, Japan
Mitsugu Fujita: Laboratory of Pharmacology, 5-1-1 Hirokoshingai, Kure, Hiroshima 737-0112, Japan
Yoshitaka Ohishi: School of Pharmaceutical Sciences, Mukogawa Women’s University, Koshien Kyubancho, Nishinomiya, Hyogo 663-8179, Japan; School of Pharmaceutical Sciences, Doshisha Women’s College of Liberal Arts, Kodo, Kyotanabe, Kyoto 610-0395, Japan
Yuko Ando: School of Pharmaceutical Sciences, Mukogawa Women’s University, Koshien Kyubancho, Nishinomiya, Hyogo 663-8179, Japan
Masao Koida: Department of Pharmacology, Faculty of Pharmaceutical Sciences, Setsunan University, 45-1 Nagaotoge-cho, Hiraka, Osaka 573-0101, Japan
Hiromichi Nakamuta: Laboratory of Pharmacology, 5-1-1 Hirokoshingai, Kure, Hiroshima 737-0112, Japan; Corresponding author. [email protected]

Journal volume & issue: Vol. 116, no. 2
pp. 214 – 220

Abstract

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Abstract.: The benzo[b]furan derivative MU314 inhibits in vitro bone resorption as potently as β-estradiol (E2). Here, we examined the point of action on the anti-osteoporotic effects of MU314. MU314 (10 nM) suppressed lacunae formation by osteoclastic cells and ICI-182,780, a pure E2 antagonist, inhibited this effect. Specifically, we ovariectomized (OVX) Wistar female rats and subcutaneously injected them with either MU314 (30 or 100 μg/kg) or E2 (100 μg/kg) over an 8-week period. Bone mineral content (BMC) in the proximal end of the tibia was significantly decreased (14%) in OVX rats, and MU314 (100 μg/kg) and E2 significantly suppressed the decline in BMC. OVX rats exhibited decreased cancellous bone in the proximal end of the tibia and induced destruction of its trabecular structure. MU314 suppressed these changes. OVX also reduced the mechanical strength of the femoral neck, which was also recovered by MU314 and E2. E2 completely protected against OVX-induced uterine atrophy, but MU314 had no effect. These results strongly indicate that MU314 acts as a selective estrogen receptor modulator. Keywords:: selective estrogen receptor modulator, osteoporosis, osteoclast, ovariectomy, bone resorption

Published in Journal of Pharmacological Sciences

ISSN: 1347-8613 (Print)
Publisher: Elsevier
Country of publisher: Japan
LCC subjects: Medicine: Therapeutics. Pharmacology
Website: http://www.journals.elsevier.com/journal-of-pharmacological-sciences

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