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与骨关节炎患者相比,类风湿关节炎患者关节周围骨分离出的成骨细胞的细胞活性和复制能力降低。

Decreased cellular activity and replicative capacity of osteoblastic cells isolated from the periarticular bone of rheumatoid arthritis patients compared with osteoarthritis patients.

作者信息

Yudoh K, Matsuno H, Osada R, Nakazawa F, Katayama R, Kimura T

机构信息

Toyama Medical and Pharmaceutical University, Japan.

出版信息

Arthritis Rheum. 2000 Oct;43(10):2178-88. doi: 10.1002/1529-0131(200010)43:10<2178::AID-ANR5>3.0.CO;2-Z.

Abstract

OBJECTIVE

Periarticular osteopenia is frequently observed in rheumatoid arthritis (RA). Bone loss has been considered to be at least partly due to inadequate bone formation, which in turn, is largely dependent on the number of osteoblasts and the osteoblastic activity. Normal human somatic cells undergo a finite number of cell divisions and ultimately enter a nondividing state called replicative senescence. It has been proposed that the telomere, the terminal sequence of chromosomes, is the mitotic clock that triggers senescence. In the present study, we sought to clarify the relationship between periarticular osteopenia and osteoblast replicative senescence in RA.

METHODS

We examined age-related changes in cellular activity (alkaline phosphatase activity, osteocalcin and C-terminal type I procollagen secretion, and cAMP response to parathyroid hormone), replicative capacity, and senescent cell expression in osteoblasts from periarticular bone samples obtained from 15 patients with RA and 15 age-matched patients with osteoarthritis (OA). Cellular replicative capacity was analyzed by the mean telomere length and in vitro remaining replicative lifespan of the cells.

RESULTS

In both OA and RA groups, the cell proliferation rate, the levels of osteoblastic markers, mean telomere length, and replicative lifespan in osteoblastic cells gradually decreased with the increasing age of the donor. The percentage of senescent osteoblastic cells in the periarticular bone increased with age in both groups, and the rate of expression of senescent cells was higher in RA patients than in age-matched OA patients. The osteoblastic activities and replicative capacity of osteoblastic cells from RA patients were lower than those from OA patients at any donor age. The age-related decreases in the osteoblastic activity and replicative capacity of osteoblastic cells from periarticular bone were greater in RA patients than in OA patients.

CONCLUSION

Our results suggest that osteoblast replicative senescence in periarticular bones occurs more rapidly with aging in RA than in OA patients and contributes to periarticular osteopenia in RA.

摘要

目的

类风湿关节炎(RA)患者常出现关节周围骨质减少。骨质流失至少部分归因于骨形成不足,而骨形成很大程度上依赖于成骨细胞数量和成骨细胞活性。正常人体体细胞经历有限次数的细胞分裂,最终进入一种称为复制性衰老的非分裂状态。有人提出,染色体的末端序列端粒是触发衰老的有丝分裂时钟。在本研究中,我们试图阐明RA患者关节周围骨质减少与成骨细胞复制性衰老之间的关系。

方法

我们检测了从15例RA患者和15例年龄匹配的骨关节炎(OA)患者获取的关节周围骨样本中成骨细胞的细胞活性(碱性磷酸酶活性、骨钙素和I型前胶原C端分泌以及对甲状旁腺激素的cAMP反应)、复制能力和衰老细胞表达的年龄相关变化。通过细胞的平均端粒长度和体外剩余复制寿命分析细胞复制能力。

结果

在OA组和RA组中,成骨细胞的细胞增殖率、成骨标志物水平、平均端粒长度和复制寿命均随供体年龄增加而逐渐降低。两组关节周围骨中衰老成骨细胞的百分比均随年龄增加,且RA患者衰老细胞的表达率高于年龄匹配的OA患者。在任何供体年龄,RA患者成骨细胞的成骨活性和复制能力均低于OA患者。RA患者关节周围骨成骨细胞的成骨活性和复制能力随年龄的下降幅度大于OA患者。

结论

我们的结果表明,RA患者关节周围骨的成骨细胞复制性衰老随年龄增长比OA患者更快,且导致RA患者关节周围骨质减少。

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