Sung Hsiao H, Spresser Wyatt J, Hoffmann Joseph P, Dai Zongrui, Van der Kraan Peter M, Caird Michelle S, Davidson Esmeralda Blaney, Kozloff Kenneth M
Orthopaedic Research Laboratories, Department of Orthopaedic Surgery, University of Michigan, Ann Arbor, MI 48109, United States.
Department of Oral and Maxillofacial Surgery, University of Michigan, Ann Arbor, MI 48109, United States.
JBMR Plus. 2024 Jan 4;8(1):ziad004. doi: 10.1093/jbmrpl/ziad004. eCollection 2024 Jan.
Craniofacial and dentoalveolar abnormalities are present in all types of osteogenesis imperfecta (OI). Mouse models of the disorder are critical to understand these abnormalities and underlying OI pathogenesis. Previous studies on severely affected OI mice report a broad spectrum of craniofacial phenotypes, exhibiting some similarities to the human disorder. The Brtl/+ and G610c/+ are moderately severe and mild-type IV OI, respectively. Little is known about the aging effects on the craniofacial bones of these models and their homology to human OI. This study aimed to analyze the Brtl/+ and G610c/+ craniofacial morphometries during aging to establish suitability for further OI craniofacial bone intervention studies. We performed morphological measurements on the micro-CT-scanned heads of 3-wk-old, 3-mo-old, and 6-mo-old female Brtl/+ and G610c/+ mice. We observed that Brtl/+ skulls are shorter in length than WT ( < .05), whereas G610c/+ skulls are similar in length to their WT counterparts. The Brtl/+ mice exhibit alveolar bone with a porotic-like appearance that is not observed in G610c/+. As they age, Brtl/+ mice show severe bone resorption in both the maxilla and mandible ( < .05). By contrast, G610c/+ mice experience mandibular resorption consistently across all ages, but maxillary resorption is only evident at 6 mo ( < .05). Western blot shows high osteoclastic activities in the Brtl/+ maxilla. Both models exhibit delayed pre-functional eruptions of the third molars ( < .05), which are similar to those observed in some bisphosphonate-treated OI subjects. Our study shows that the Brtl/+ and G610c/+ mice display clear features found in type IV OI patients; both show age-related changes in the craniofacial growth phenotype. Therefore, understanding the craniofacial features of these models and how they age will allow us to select the most accurate mouse model, mouse age, and bone structure for the specific craniofacial bone treatment of differing OI groups.
在所有类型的成骨不全症(OI)中均存在颅面和牙槽骨异常。该疾病的小鼠模型对于理解这些异常以及OI的潜在发病机制至关重要。先前对严重受影响的OI小鼠的研究报告了广泛的颅面表型,与人类疾病表现出一些相似之处。Brtl/+和G610c/+分别为中度严重和轻度IV型OI。关于衰老对这些模型颅面骨的影响及其与人类OI的同源性知之甚少。本研究旨在分析Brtl/+和G610c/+在衰老过程中的颅面形态测量结果,以确定其是否适合进一步的OI颅面骨干预研究。我们对3周龄、3月龄和6月龄的雌性Brtl/+和G610c/+小鼠的头部进行了显微CT扫描,并进行了形态学测量。我们观察到,Brtl/+小鼠的颅骨长度比野生型短(<0.05),而G610c/+小鼠的颅骨长度与野生型相似。Brtl/+小鼠的牙槽骨呈现出类似疏松的外观,而G610c/+小鼠则未观察到这种情况。随着年龄增长,Brtl/+小鼠的上颌骨和下颌骨均出现严重的骨吸收(<0.05)。相比之下,G610c/+小鼠在所有年龄段下颌骨均持续出现吸收,但上颌骨吸收仅在6个月时明显(<0.05)。蛋白质免疫印迹显示Brtl/+上颌骨中有高破骨细胞活性。两种模型均表现出第三磨牙功能性萌出延迟(<0.05),这与在一些接受双膦酸盐治疗的OI患者中观察到的情况相似。我们的研究表明,Brtl/+和G610c/+小鼠表现出IV型OI患者中发现的明显特征;两者均显示出颅面生长表型的年龄相关变化。因此,了解这些模型的颅面特征及其衰老方式将使我们能够为不同OI组的特定颅面骨治疗选择最准确的小鼠模型、小鼠年龄和骨结构。
Zotero 插件
