两种新型ALN-EP4a偶联药物在去卵巢大鼠模型中对骨骼的体内作用,以逆转绝经后骨质流失。
In vivo effects of two novel ALN-EP4a conjugate drugs on bone in the ovariectomized rat model for reversing postmenopausal bone loss.
作者信息
Hu S, Liu C C, Chen G, Willett T, Young R N, Grynpas M D
机构信息
Department of Laboratory Medicine and Pathology, University of Toronto, Toronto, ON, M5S 1A8, Canada.
Lunenfeld-Tanenbaum Research Institute, Mount Sinai Hospital, Toronto, ON, M5G 1X5, Canada.
出版信息
Osteoporos Int. 2016 Feb;27(2):797-808. doi: 10.1007/s00198-015-3284-x. Epub 2015 Aug 14.
UNLABELLED
Two alendronate-EP4 agonist (ALN-EP4a) conjugate drugs, C1 and C2, which differ in structure by a short linker molecule, were evaluated in ovariectomized (OVX) rats for their anabolic effects. We showed that C1 led to significant anabolic effects on cortical and trabecular bone while anabolic effects associated with C2 were minimal.
INTRODUCTION
EP4as were covalently linked to ALN to create ALN-EP4a conjugate anabolic bone drugs, C1 and C2, which differ in structure by a short linker molecule in C1. When administered systemically, C1 and C2 are delivered to bone through targeted binding of ALN, where local hydrolytic enzymes liberate EP4a from ALN to exert anabolic effects. Here, we compare effects of C1 to C2 in a curative in vivo study.
METHODS
Three-month-old female Sprague Dawley rats were OVX or sham operated and allowed to lose bone for 3 months. Animals were then treated via tail vein injections for 3 months and sacrificed. Treatment groups were as follows: C1L (5 mg/kg biweekly), C1H (5 mg/kg weekly), C2L (15 mg/kg monthly), C2H (15 mg/kg biweekly), OVX and sham control (phosphate-buffered saline (PBS) biweekly), and ALN/EP4a-unconjugated mixture (0.75 mg/kg each biweekly).
RESULTS
MicroCT analysis showed that C1H treatment significantly increased vertebral bone mineral density (vBMD) and trabecular bone volume versus OVX controls while C2 treatments did not. Biomechanical testing showed that C1H treatment but not C2 treatments led to significant improvement in the load bearing abilities of the vertebrae compared to OVX controls. C1 stimulated endocortical bone formation and increased load bearing in femurs, while C2 did not.
CONCLUSIONS
We showed that C1 led to significant anabolic effects on cortical and trabecular bone while anabolic effects associated with C2 were minimal. These results led us to hypothesize a mode of action by which presence of a linker is crucial in facilitating the anabolic effects of EP4a when dosed as a prodrug with ALN.
未标记
评估了两种阿仑膦酸盐 - EP4激动剂(ALN - EP4a)偶联药物C1和C2,它们在结构上因一个短连接分子而不同,在去卵巢(OVX)大鼠中评估了它们的合成代谢作用。我们发现C1对皮质骨和小梁骨有显著的合成代谢作用,而与C2相关的合成代谢作用最小。
引言
EP4a与ALN共价连接以创建ALN - EP4a偶联合成代谢骨药物C1和C2,它们在结构上的差异在于C1中有一个短连接分子。全身给药时,C1和C2通过ALN的靶向结合被递送至骨骼,在那里局部水解酶将EP4a从ALN中释放出来以发挥合成代谢作用。在此,我们在一项体内治疗研究中比较了C1和C2的效果。
方法
将3个月大的雌性Sprague Dawley大鼠进行去卵巢或假手术,并使其骨质流失3个月。然后通过尾静脉注射对动物进行3个月的治疗并处死。治疗组如下:C1L(每两周5mg/kg),C1H(每周5mg/kg),C2L(每月15mg/kg),C2H(每两周15mg/kg),OVX和假手术对照组(每两周磷酸盐缓冲盐水(PBS)),以及ALN/EP4a未偶联混合物(每两周各0.75mg/kg)。
结果
MicroCT分析显示,与OVX对照组相比,C1H治疗显著增加了椎体骨矿物质密度(vBMD)和小梁骨体积,而C2治疗则没有。生物力学测试表明,与OVX对照组相比,C1H治疗而非C2治疗导致椎体承重能力有显著改善。C1刺激了股骨内皮质骨形成并增加了承重能力,而C2则没有。
结论
我们发现C1对皮质骨和小梁骨有显著的合成代谢作用,而与C2相关的合成代谢作用最小。这些结果使我们推测一种作用模式,即当与ALN作为前药给药时,连接分子的存在对于促进EP4a的合成代谢作用至关重要。
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