首页> 外文期刊>Journal of nephrology. >Phosphatemia is related to chromosomal aberrations of parathyroid glands in patients with hyperparathyroidism.
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Phosphatemia is related to chromosomal aberrations of parathyroid glands in patients with hyperparathyroidism.

机译:甲状旁腺功能亢进症患者中,磷酸血症与甲状旁腺的染色体畸变有关。

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BACKGROUND AND AIMS: It has been well documented that gene and DNA alterations occur frequently in benign primary parathyroid adenomas as well as in parathyroid glands with secondary hyperplasia. However, it has not been shown whether a correlation exists between somatic DNA aberrations and clinical data. METHODS: We analyzed the frequency of chromosomal aberrations in adenomas obtained from 25 patients with primary hyperparathyroidism (pHPT) and 60 parathyroid nodules from 20 uremic patients with secondary hyperparathyroidism (sHPT). The relation of chromosomal aberrations to parathyroid hormone, as well as calcium and phosphate serum concentrations, was assessed. Allelic changes were evaluated by microsatellite allelotyping using 105 polymorphic markers. RESULTS: Somatic chromosomal aberrations were found in 23 out of 25 adenomas, in hyperplastic lesions from 16 out of 20 patients. In pHPT as well as in sHPT a positive correlation was found between the number of chromosomal alterations and serum phosphate concentration (tau=0.270, p=0.05; and tau=0.362, p=0.03, respectively). Only in pHPT was a negative correlation of borderline significance between serum parathormone (PTH) and number of aberrated chromosomes noticed (tau=-0.258, p=0.07). There was no correlation between the number of DNA changes and serum concentration of calcium or tumor volume. CONCLUSION: Hyperphosphatemia may increase the risk of specific and random chromosomal aberrations due to increasing proliferation rate of parathyroid cells in patients with sHPT.
机译:背景与目的:已有大量文献证明基因和DNA改变经常在良性原发性甲状旁腺腺瘤以及继发性增生的甲状旁腺中发生。但是,尚未显示体DNA畸变与临床数据之间是否存在相关性。方法:我们分析了从20例尿毒症继发性甲状旁腺功能亢进症(sHPT)患者中获得的25例原发性甲状旁腺功能亢进症(pHPT)和60甲状旁腺结节中腺瘤的染色体畸变频率。评估了染色体畸变与甲状旁腺激素的关系,以及钙和磷酸盐的血清浓度。等位基因的变化通过使用105种多态性标记的微卫星定型分析进行评估。结果:25例腺瘤中有23例发现体细胞染色体畸变,20例患者中有16例出现增生性病变。在pHPT和sHPT中,在染色体改变数量和血清磷酸盐浓度之间发现正相关(分别为tau = 0.270,p = 0.05; tau = 0.362,p = 0.03)。仅在pHPT中,血清副激素(PTH)与发现的畸变染色体数之间的临界显着负相关(tau = -0.258,p = 0.07)。 DNA改变的数量与血清钙浓度或肿瘤体积之间没有相关性。结论:高磷血症可能会增加sHPT患者甲状旁腺细胞的增殖率,从而增加特异性和随机染色体畸变的风险。

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