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衰老小鼠中,骨皮质骨细胞的硬化蛋白免疫反应性增加,而关节软骨软骨细胞的硬化蛋白免疫反应性降低。

Sclerostin Immunoreactivity Increases in Cortical Bone Osteocytes and Decreases in Articular Cartilage Chondrocytes in Aging Mice.

作者信息

Thompson Michelle L, Jimenez-Andrade Juan Miguel, Mantyh Patrick W

机构信息

Department of Pharmacology, University of Arizona, Tucson, Arizona (MLT, JMJA, PWM)

Unidad Académica Multidisciplinaria Reynosa Aztlan, Universidad Autónoma de Tamaulipas, Reynosa, Tamaulipas, Mexico (JMJA)

出版信息

J Histochem Cytochem. 2016 Mar;64(3):179-89. doi: 10.1369/0022155415626499. Epub 2015 Dec 23.

Abstract

Sclerostin is a 24-kDa secreted glycoprotein that has been identified as a negative modulator of new bone formation and may play a major role in age-related decline in skeletal function. Although serum levels of sclerostin markedly increase with age, relatively little is known about whether cells in the skeleton change their expression of sclerostin with aging. Using immunohistochemistry and confocal microscopy, we explored sclerostin immunoreactivity (sclerostin-IR) in the femurs of 4-, 9-, and 24-month-old adult C3H/HeJ male mice. In the femur, the only two cell types that expressed detectable levels of sclerostin-IR were bone osteocytes and articular cartilage chondrocytes. At three different sites along the diaphysis of the femur, only a subset of osteocytes expressed sclerostin-IR and the percentage of osteocytes that expressed sclerostin-IR increased from approximately 36% to 48% in 4- vs. 24-month-old mice. In marked contrast, in the same femurs, there were ~40% fewer hypertrophic chondrocytes of articular cartilage that expressed sclerostin-IR when comparing 24- vs. 4-month-old mice. Understanding the mechanism(s) that drive these divergent changes in sclerostin-IR may provide insight into understanding and treating the age-related decline of the skeleton.

摘要

硬化蛋白是一种24千道尔顿的分泌型糖蛋白,已被确定为新骨形成的负调节因子,可能在与年龄相关的骨骼功能衰退中起主要作用。尽管血清硬化蛋白水平随年龄显著升高,但关于骨骼中的细胞是否会随着衰老而改变其硬化蛋白表达的情况,人们了解得相对较少。我们使用免疫组织化学和共聚焦显微镜,探究了4个月、9个月和24个月大的成年C3H/HeJ雄性小鼠股骨中的硬化蛋白免疫反应性(sclerostin-IR)。在股骨中,仅有的两种表达可检测水平sclerostin-IR的细胞类型是骨细胞和关节软骨软骨细胞。沿着股骨干的三个不同部位,只有一部分骨细胞表达sclerostin-IR,并且在4个月大与24个月大的小鼠中,表达sclerostin-IR的骨细胞百分比从约36%增加到了48%。与之形成显著对比的是,在相同的股骨中,比较24个月大与4个月大的小鼠时,表达sclerostin-IR的关节软骨肥大软骨细胞减少了约40%。了解驱动sclerostin-IR这些不同变化的机制,可能有助于深入理解和治疗与年龄相关的骨骼衰退。

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