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前列腺素E2可增加完整雌性大鼠和去卵巢雌性大鼠的皮质骨量,并激活皮质内骨重塑。

Prostaglandin E2 enhances cortical bone mass and activates intracortical bone remodeling in intact and ovariectomized female rats.

作者信息

Jee W S, Mori S, Li X J, Chan S

机构信息

Radiobilogy Division, University of Utah, Salt Lake City 84412.

出版信息

Bone. 1990;11(4):253-66. doi: 10.1016/8756-3282(90)90078-d.

Abstract

To assess the efficacy of prostaglandin E2 (PGE2) in augmenting cortical bone mass, graded doses of PGE2 were subcutaneously administered for 30 days to seven-month old sham-ovariectomized (SHAM) and ovariectomized (OVX) rats. Both groups were operated at three months of age. Histomorphometric analyses of double fluorescent labeled tibial shafts were performed on basal control, OVX, and SHAM rats treated with 0, 0.3, 1, 3, and 6 mg PGE2/kg/d for 30 days. Baseline aging data showed increased cortical tissue and cortical bone area and reduced bone formation parameters at the periosteal and endocortical bone envelopes between three and eight months of age. The tibial shafts of OVX rats compared to SHAM controls showed elevated periosteal mineral apposition rate and endocortical bone formation parameters. PGE2 administration to OVX and SHAM rats increased cortical bone by the addition of new circumferential bone on the endocortical and periosteal surfaces, as well as woven cancellous bone in the marrow region. Stimulated osteoblastic recruitment and activity enhanced bone formation at all bone surfaces. The new bone was both lamellar and woven in nature. PGE2 treatment also activated intracortical bone remodeling (not seen in untreated eight-month old rats), creating a porous cortex. Thus, PGE2 administration activated cortical bone modeling in the formation mode (A----F), as well as intracortical bone remodeling (A----R----F). PGE2 administration to OVX rats resulted in more intracortical bone remodeling, periosteal bone formation, and new cancellous bone production than observed in PGE2 treated controls. The findings that PGE2 administration to OVX and intact female rats increases cortical bone mass, coupled with observations that mouse, rat, dog, and man respond similarly to PGE2, suggest that PGE2 administration may be useful in the prevention and treatment of postmenopausal osteoporosis.

摘要

为评估前列腺素E2(PGE2)增加皮质骨量的功效,将不同剂量的PGE2皮下注射给7月龄的假去卵巢(SHAM)和去卵巢(OVX)大鼠,持续30天。两组大鼠均在3月龄时进行手术。对基础对照组、OVX组以及用0、0.3、1、3和6mg PGE2/kg/d处理30天的SHAM大鼠的双荧光标记胫骨干进行组织形态计量学分析。基线老化数据显示,在3至8月龄之间,皮质组织和皮质骨面积增加,骨膜和骨内膜骨膜处的骨形成参数降低。与SHAM对照组相比,OVX大鼠的胫骨干显示骨膜矿物质沉积率和骨内膜骨形成参数升高。给OVX和SHAM大鼠施用PGE2可通过在内皮质和骨膜表面添加新的环周骨以及骨髓区域的编织松质骨来增加皮质骨。刺激成骨细胞募集和活性可增强所有骨表面的骨形成。新形成的骨既有板层状的也有编织状的。PGE2处理还激活了皮质内骨重塑(未处理的8月龄大鼠未观察到),形成了多孔皮质。因此,施用PGE2激活了皮质骨在形成模式(A----F)下的建模以及皮质内骨重塑(A----R----F)。与PGE2处理的对照组相比,给OVX大鼠施用PGE2导致更多的皮质内骨重塑、骨膜骨形成和新的松质骨生成。给OVX和完整雌性大鼠施用PGE2可增加皮质骨量,再加上观察到小鼠、大鼠、狗和人类对PGE2的反应相似,这表明施用PGE2可能对预防和治疗绝经后骨质疏松症有用。

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