Department of Clinical Studies-Philadelphia, University of Pennsylvania School of Veterinary Medicine, 312 Hill Pavilion, 380 S. University Ave, Philadelphia, PA, 19104-4539, USA,
Calcif Tissue Int. 2014 Jun;94(6):621-31. doi: 10.1007/s00223-014-9843-x. Epub 2014 Mar 14.
Type III collagen (Col3), a fibril-forming collagen, is a major extracellular matrix component in a variety of internal organs and skin. It is also expressed at high levels during embryonic skeletal development and is expressed by osteoblasts in mature bone. Loss of function mutations in the gene encoding Col3 (Col3a1) are associated with vascular Ehlers-Danlos syndrome (EDS). Although the most significant clinical consequences of this syndrome are associated with catastrophic failure and impaired healing of soft tissues, several studies have documented skeletal abnormalities in vascular EDS patients. However, there are no reports of the role of Col3 deficiency on the murine skeleton. We compared craniofacial and skeletal phenotypes in young (6-8 weeks) and middle-aged (>1 year) control (Col3(+/+)) and haploinsufficient (Col3(+/-)) mice, as well as young null (Col3(-/-)) mice by microcomputed tomography (μCT). Although Col3(+/-) mice did not have significant craniofacial abnormalities based upon cranial morphometrics, μCT analysis of distal femur trabecular bone demonstrated significant reductions in bone volume (BV), bone volume fraction (BV/TV), connectivity density, structure model index and trabecular thickness in young adult female Col3(+/-) mice relative to wild-type littermates. The reduction in BV/TV persisted in female mice at 1 year of age. Next, we evaluated the role of Col3 in vitro. Osteogenesis assays revealed that cultures of mesenchymal progenitors collected from Col3(-/-) embryos display decreased alkaline phosphatase activity and reduced capacity to undergo mineralization. Consistent with this data, a reduction in expression of osteogenic markers (type I collagen, osteocalcin and bone sialoprotein) correlates with reduced bone Col3 expression in Col3(+/-) mice and with age in vivo. A small but significant reduction in osteoclast numbers was found in Col3(+/-) compared to Col3(+/+) bones. Taken together, these findings indicate that Col3 plays a role in development of trabecular bone through its effects on osteoblast differentiation.
III 型胶原(Col3)是一种纤维形成的胶原,是多种内部器官和皮肤的主要细胞外基质成分。它在胚胎骨骼发育过程中也高度表达,并在成熟骨的成骨细胞中表达。编码 Col3(Col3a1)的基因突变与血管性 Ehlers-Danlos 综合征(EDS)有关。尽管该综合征最显著的临床后果与软组织的灾难性破裂和愈合受损有关,但几项研究已经记录了血管性 EDS 患者的骨骼异常。然而,尚无关于 Col3 缺乏对鼠骨骼影响的报道。我们通过微计算机断层扫描(μCT)比较了年轻(6-8 周)和中年(>1 岁)对照组(Col3(+/+))和半合子不足(Col3(+/-))以及年轻的纯合子(Col3(-/-))小鼠的颅面和骨骼表型。尽管 Col3(+/-)小鼠的颅面形态测量学没有明显的颅面异常,但远端股骨小梁骨的μCT 分析显示,年轻成年雌性 Col3(+/-)小鼠的骨体积(BV)、骨体积分数(BV/TV)、连接密度、结构模型指数和小梁厚度与野生型同窝仔鼠相比均显著降低。BV/TV 的减少在 1 岁时的雌性小鼠中仍持续存在。接下来,我们评估了 Col3 在体外的作用。成骨测定显示,从 Col3(-/-)胚胎中收集的间充质祖细胞的培养物显示碱性磷酸酶活性降低,并且矿化能力降低。与这些数据一致,Col3(+/-)小鼠的骨 Col3 表达减少与体内年龄相关,与成骨标志物(I 型胶原、骨钙素和骨涎蛋白)的表达减少相关。在 Col3(+/-)骨中与 Col3(+/+)骨相比,破骨细胞数量略有减少。总之,这些发现表明,Col3 通过对成骨细胞分化的影响,在小梁骨的发育中发挥作用。
