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软骨细胞与骨骼纵向生长:胫骨软骨发育不良的发展

Chondrocytes and longitudinal bone growth: the development of tibial dyschondroplasia.

作者信息

Farquharson C, Jefferies D

机构信息

Division of Integrative Biology, Roslin Institute, Scotland.

出版信息

Poult Sci. 2000 Jul;79(7):994-1004. doi: 10.1093/ps/79.7.994.

Abstract

Growth plate cartilage is central to the process of bone elongation. Chondrocytes originating within the resting zone of the growth plate proceed through a series of intermediate phenotypes: proliferating, prehypertrophic and hypertrophic, before reaching a terminally differentiated state. Disruption of this chondrocyte maturational sequence causes many skeletal abnormalities in poultry such as tibial dyschondroplasia (TD), which is a common cause of deformity and lameness in the broiler chicken. Cell and matrix components of the growth plate have been studied in order to determine the cause(s) of the premature arrest of chondrocyte differentiation and retention of prehypertrophic chondrocytes observed in TD. Chondrocyte proliferation proceeds normally in TD, but markers of the differentiated phenotype, local growth factors, and the vitamin D receptor are abnormally expressed within the prehypertrophic chondrocytes above, and within, the lesion. Tibial dyschondroplasia is also associated with a reduced incidence of apoptosis, suggesting that the lesion contains an accumulation of immature cells that have outlived their normal life span. Immunolocalization studies of matrix components suggest an abnormal distribution within the TD growth plate that is consistent with a failure of the chondrocytes to fully hypertrophy. In addition, the collagen matrix of the TD lesion is highly crosslinked, which may make the formed lesion more impervious to vascular invasion and osteoclastic resorption. Recent studies have applied the techniques of differential display and semiquantitative reverse transcriptase-polymerase chain reaction to RNA obtained from discrete populations of growth plate chondrocytes of different maturational phenotypes. This strategy has allowed us to compare phenotypically identical cell fractions from normal and TD growth plates in an attempt to identify possible candidate genes for TD.

摘要

生长板软骨是骨骼伸长过程的核心。起源于生长板静止区的软骨细胞会经历一系列中间表型:增殖型、前肥大型和肥大型,然后达到终末分化状态。这种软骨细胞成熟序列的破坏会导致家禽出现许多骨骼异常,如胫骨软骨发育不良(TD),这是肉鸡畸形和跛行的常见原因。为了确定在TD中观察到的软骨细胞分化过早停滞和前肥大软骨细胞滞留的原因,人们对生长板的细胞和基质成分进行了研究。在TD中软骨细胞增殖正常进行,但在病变上方和病变内部的前肥大软骨细胞中,分化表型的标志物、局部生长因子和维生素D受体表达异常。胫骨软骨发育不良还与细胞凋亡发生率降低有关,这表明病变中含有寿命超过正常范围的未成熟细胞的积累。对基质成分的免疫定位研究表明,TD生长板内的分布异常,这与软骨细胞未能完全肥大一致。此外,TD病变的胶原基质高度交联,这可能使形成的病变更不易受到血管侵入和破骨细胞吸收的影响。最近的研究将差异显示技术和半定量逆转录-聚合酶链反应应用于从不同成熟表型的生长板软骨细胞离散群体中获得的RNA。这种策略使我们能够比较正常和TD生长板中表型相同的细胞部分,试图确定TD可能的候选基因。

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