在严重成骨不全症小鼠模型中，骨靶向前列腺素 E2 受体 4 激动剂 C3（Mes-1007）治疗的效果。

Effects of treatment with a bone-targeted prostaglandin E2 receptor 4 agonist C3 (Mes-1007) in a mouse model of severe osteogenesis imperfecta.

机构信息

Shriners Hospital for Children-Canada, Montreal, Quebec, Canada; Department of Pediatrics, McGill University, Montreal, Quebec, Canada.

Department of Chemistry, Simon Fraser University, Burnaby, British Columbia, Canada; Mesentech Inc., Vancouver, British Columbia, Canada.

出版信息

Bone. 2021 Apr;145:115867. doi: 10.1016/j.bone.2021.115867. Epub 2021 Jan 29.

DOI:10.1016/j.bone.2021.115867

PMID:33524637

Abstract

OBJECTIVE

Osteogenesis imperfecta (OI) is a heritable bone fragility disorder that is usually caused by mutations affecting collagen type I synthesis in osteoblasts. Bisphosphonates are widely used to decrease fracture rate but are only partially effective. Bone anabolic compounds, such as prostaglandin E2 receptor 4 (EP4) agonists may be an alternative treatment approach. Here we assessed the effect of Mes-1007, a novel bone-targeted EP4 agonist in Jrt mice, a model of severe OI.

STUDY DESIGN

Experimental study.

RESULTS

Male 8-week old wild type (WT) and OI mice were randomly assigned to 4 weeks of three intraperitoneal injections per week with Mes-1007 (25 mg per kg body mass), phosphate-buffered saline, zoledronate (5 μg per kg), or a combination treatment of zoledronate and Mes-1007. Treatment with Mes-1007 alone did not lead to higher trabecular bone volume per tissue volume (BV/TV) in the distal femur or lumbar vertebra 4 in either WT or OI mice. Treatment with zoledronate alone was associated with a significant increase in distal femur and vertebra BV/TV in both genotypes. In zoledronate-treated WT and OI mice, Mes-1007 increased bone formation rate in vertebral trabecular bone and had an additive effect on BV/TV. Vertebral BV/TV in OI mice that received zoledronate or Mes-1007/zoledronate combination treatment was similar to untreated WT mice (p = 0.25). At the femoral midshaft, Mes-1007/zoledronate combination treatment increased cortical thickness in both genotypes and led to higher periosteal diameter in OI mice. Three-point bending tests of femurs showed that Mes-1007/zoledronate combination treatment increased the stiffness, load at yield and maximal load in WT but not in OI mice.

CONCLUSION

Dosing Mes-1007 in combination with zoledronate improved the bone properties in a manner that is consistent with a mechanism of action of EP4 agonists on bone and additive to effects of anti-resorptives typified by zoledronate.

摘要

目的

成骨不全症（OI）是一种遗传性骨骼脆弱疾病，通常由影响成骨细胞中 I 型胶原合成的突变引起。双膦酸盐被广泛用于降低骨折率，但仅部分有效。骨合成代谢化合物，如前列腺素 E2 受体 4（EP4）激动剂，可能是一种替代治疗方法。在这里，我们评估了新型骨靶向 EP4 激动剂 Mes-1007 在 Jrt 小鼠（一种严重 OI 模型）中的作用。

研究设计

实验研究。

结果

8 周龄雄性野生型（WT）和 OI 小鼠随机分为四组，每周接受三次腹腔内注射，分别给予 Mes-1007（25mg/kg 体重）、磷酸盐缓冲液、唑来膦酸（5μg/kg）或唑来膦酸和 Mes-1007 联合治疗。单独使用 Mes-1007 治疗在 WT 或 OI 小鼠的远端股骨或腰椎 4 处并未导致骨小梁体积与组织体积比（BV/TV）增加。单独使用唑来膦酸治疗在两种基因型中均导致远端股骨和椎体 BV/TV 显著增加。在唑来膦酸治疗的 WT 和 OI 小鼠中，Mes-1007 增加了椎体骨小梁的骨形成率，并对 BV/TV 具有附加作用。接受唑来膦酸或 Mes-1007/唑来膦酸联合治疗的 OI 小鼠的椎体 BV/TV 与未治疗的 WT 小鼠相似（p=0.25）。在股骨中段，Mes-1007/唑来膦酸联合治疗增加了两种基因型的皮质厚度，并导致 OI 小鼠的骨膜直径增加。股骨三点弯曲试验显示，Mes-1007/唑来膦酸联合治疗增加了 WT 小鼠的刚度、屈服载荷和最大载荷，但对 OI 小鼠没有作用。