赖氨酰氧化酶样-1突变小鼠的性连锁骨骼表型
Sex-Linked Skeletal Phenotype of Lysyl Oxidase Like-1 Mutant Mice.
作者信息
Alsofi Loai, Daley Eileen, Hornstra Ian, Morgan Elise F, Mason Zachary D, Acevedo Jesus F, Word R Ann, Gerstenfeld Louis C, Trackman Philip C
机构信息
Department of Molecular and Cell Biology, Henry M. Goldman School of Dental Medicine, Boston University, 700 Albany Street, W-201, Boston, MA, 02118, USA.
Department of Endodontics, Faculty of Dentistry, King Abdulaziz University, Jeddah, Saudi Arabia.
出版信息
Calcif Tissue Int. 2016 Feb;98(2):172-85. doi: 10.1007/s00223-015-0076-4. Epub 2015 Nov 5.
Lysyl oxidases are required for collagen and elastin cross-linking and extracellular matrix maturation including in bone. The lysyl oxidase family consists of lysyl oxidase (LOX) and 4 isoforms (LOXL1-4). Here we investigate whether deletion of LOXL1, which has been linked primarily to elastin maturation, leads to skeletal abnormalities. Left femurs (n = 8), L5 vertebrae (n = 8), and tibiae (n = 8) were analyzed by micro-computed tomography in 13-week-old wild-type (WT) and LOXL1-/- male and female mice. Right femurs (n = 8) were subjected to immunohistochemistry for LOXL1, and histochemical/histology analyses of osteoclasts and growth plates. Sera from all mice were analyzed for bone turnover markers. Results indicate strong expression of LOXL1 in wild-type growth plates in femurs. Significant deterioration of trabecular bone structure in long bones and vertebrae from female was observed but not from male, mutant mice compared with WT. Decreases in BV/TV, Conn.D, trabecular thickness, and number in the femoral distal metaphysis were observed in female, but not in male, mutant mice. Trabecular spacing was increased significantly in femurs of female mutant mice. Findings were similar in trabeculae of L5 vertebrae from female mutant mice. The number of TRAP positive osteoclasts at the trabecular bone surface was increased in female mutant mice compared with WT females, consistent with increased serum RANKL and decreased OPG levels. Analysis of bone turnover markers confirmed increased bone resorption as indicated by significantly elevated CTX-1 in the serum of female LOXL1-/- mice compared to their wild-type counterparts, as well as decreased bone formation as measured by decreased serum levels of PINP. Picrosirius red staining revealed a loss of heterogeneity in collagen organization in female LOXL1-/- mice only, with little to no yellow and orange birefringence. Organization was also impaired in chondrocyte columns in both female and male LOXL1-/- mice, but to a greater extent in females. Data indicate that LOXL1-/- mutant mice develop appendicular and axial skeletal phenotypes characterized by decreased bone volume fraction and compromised trabecular microstructure, predominantly in females.
赖氨酰氧化酶对于胶原蛋白和弹性蛋白的交联以及包括骨骼在内的细胞外基质成熟是必需的。赖氨酰氧化酶家族由赖氨酰氧化酶(LOX)和4种同工型(LOXL1 - 4)组成。在此,我们研究主要与弹性蛋白成熟相关的LOXL1缺失是否会导致骨骼异常。对13周龄野生型(WT)和LOXL1基因敲除(LOXL1-/-)的雄性和雌性小鼠的左股骨(n = 8)、L5椎骨(n = 8)和胫骨(n = 8)进行了显微计算机断层扫描分析。对右股骨(n = 8)进行了LOXL1的免疫组织化学分析,以及破骨细胞和生长板的组织化学/组织学分析。对所有小鼠的血清进行了骨转换标志物分析。结果表明,LOXL1在野生型股骨生长板中强烈表达。与WT相比,观察到雌性而非雄性突变小鼠的长骨和椎骨小梁骨结构显著恶化。在雌性而非雄性突变小鼠中,观察到股骨远端干骺端的骨体积分数(BV/TV)、骨小梁连接密度(Conn.D)、骨小梁厚度和数量减少。雌性突变小鼠股骨中的骨小梁间距显著增加。在雌性突变小鼠L5椎骨的小梁中也观察到类似结果。与WT雌性小鼠相比,雌性突变小鼠小梁骨表面TRAP阳性破骨细胞数量增加,这与血清中核因子κB受体活化因子配体(RANKL)增加和骨保护素(OPG)水平降低一致。骨转换标志物分析证实,与野生型对照相比,雌性LOXL1-/-小鼠血清中I型胶原交联C-末端肽(CTX-1)显著升高,表明骨吸收增加,同时血清I型前胶原N-端前肽(PINP)水平降低,表明骨形成减少。天狼星红染色显示,仅在雌性LOXL1-/-小鼠中胶原组织的异质性丧失,几乎没有或没有黄色和橙色双折射。在雌性和雄性LOXL1-/-小鼠的软骨细胞柱中,组织结构也受到损害,但在雌性中程度更大。数据表明,LOXL1-/-突变小鼠出现以骨体积分数降低和小梁微结构受损为特征的附肢和轴向骨骼表型,主要发生在雌性小鼠中。
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