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首页> 外文期刊>Mechanisms of Ageing and Development >Changes in biological characteristics during the cellular aging of ligament fibroblasts derived from patients with prolapsus uteri.
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Changes in biological characteristics during the cellular aging of ligament fibroblasts derived from patients with prolapsus uteri.

机译:子宫垂体患者韧带成纤维细胞细胞老化过程中生物学特性的变化。

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摘要

Prolapsus uteri in pelvic support disorders are common in elderly women. The etiology is unclear and more likely to be multifactorial. We examined changes in biological characteristics and responsiveness to growth factors during the in vitro cellular aging of cardinal ligamental fibroblasts derived from patients with prolapsus uteri (HPLiF), and compared them with those of cells from age-matched control subjects (HCLiF). HPLiF and HCLiF had almost the same in vitro life span and the age-related patterns of biological parameters were essentially the same. However, the saturation density was significantly higher in HPLiF than in HCLiF. Furthermore, the high proliferative activity of HPLiF to serum mitogens, especially to platelet-derived growth factor, was retained throughout the in vitro life span. p53 protein levels in HPLiF increased at late passages, but were significantly less than in aged HCLiF. These results indicate that the higher proliferative activity in prolapsus fibroblasts may result from the decreased expression of p53 protein and may lead to a decrease in the synthesis and deposition of extracellular matrix components. These results support the hypothesis that functional alterations in ligament fibroblasts are involved in the mechanism of the development of prolapsus uteri.
机译:盆腔支持障碍的子宫溢尿症在老年妇女中很常见。病因尚不清楚,可能是多因素的。我们检查了来自子宫垂体患者(HPLiF)的心脏韧带成纤维细胞的体外细胞衰老过程中生物学特征和对生长因子的反应的变化,并将其与年龄匹配的对照组(HCLiF)的细胞进行了比较。 HPLiF和HCLiF的体外寿命几乎相同,并且与年龄相关的生物学参数模式也基本相同。但是,HPLiF的饱和密度明显高于HCLiF。此外,HPLiF对血清有丝分裂原,特别是对血小板衍生的生长因子的高增殖活性在整个体外寿命中得以保留。 HPLiF中的p53蛋白水平在后期传代时增加,但显着低于老年HCLiF。这些结果表明,成年成纤维细胞中较高的增殖活性可能是由于p53蛋白表达降低,并可能导致细胞外基质成分的合成和沉积减少。这些结果支持以下假设,即韧带成纤维细胞的功能改变参与了子宫垂体发展的机制。

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