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大鼠十二指肠钙结合蛋白与活性钙转运:它们在功能上相关吗?

Duodenal calcium binding protein and active calcium transport in rats: are they functionally related?

作者信息

Chabanis S, Hanrotel C, Duchambon P, Banide H, Kubrusly M, Aymard P, Lacour B, Drüeke T

机构信息

INSERM U90, Hôpital Necker, Paris, France.

出版信息

Nephrol Dial Transplant. 1994;9(10):1402-7.

PMID:7816252
Abstract

The effects of calcitriol and a novel calcitriol analogue, 22-oxacalcitriol (OCT) on duodenal Ca transport, calbindin-D9k mRNA, and calbindin-D9k content were studied in two animal models reflecting common human pathologies, namely arterial hypertension and chronic renal failure, as well as in normal rats. The hormone or its analogue were administered intraperitoneally to vitamin-D-replete rats. Active Ca transport was increased in both spontaneously hypertensive rats (SHR) and in normotensive control WKY rats 5 h after calcitriol dosing of either 60 and 600 ng per rat. In WKY, calbindin-D9k content was slightly increased after the injection of 60 ng calcitriol, but not of 600 ng calcitriol whereas calbindin-D9k mRNA stayed essentially unchanged. In contrast, active Ca transport was significantly stimulated after the higher dose of 600 ng calcitriol. In SHR, while both doses of calcitriol increased active Ca transport, they had no stimulatory effect on calbindin-D9k mRNA or protein. In chronically uraemic rats, active Ca transport, duodenal calbindin-D9k and calbindin-D9k mRNA were stimulated after the injection of two subsequent doses of 300 ng calcitriol per rat. OCT treatment at same dosage led to a similar stimulation of calbindin-D9k and calbindin-D9k mRNA, but failed to induce an increase in active Ca transport. These results show that the stimulation of intestinal active Ca transport and calbindin-D9k can be entirely dissociated at the protein synthesis and the mRNA expression level (1) after calcitriol administration to normal and hypertensive rats, and (2) after OCT administration to uraemic rats.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

在反映常见人类病理状况的两种动物模型(即动脉高血压和慢性肾衰竭)以及正常大鼠中,研究了骨化三醇和一种新型骨化三醇类似物22-氧杂骨化三醇(OCT)对十二指肠钙转运、钙结合蛋白-D9k mRNA和钙结合蛋白-D9k含量的影响。将该激素或其类似物腹腔注射给维生素D充足的大鼠。在每只大鼠给予60和600 ng骨化三醇后5小时,自发性高血压大鼠(SHR)和血压正常的对照WKY大鼠的活性钙转运均增加。在WKY大鼠中,注射60 ng骨化三醇后钙结合蛋白-D9k含量略有增加,但注射600 ng骨化三醇后未增加,而钙结合蛋白-D9k mRNA基本保持不变。相比之下,较高剂量600 ng骨化三醇后活性钙转运受到显著刺激。在SHR中,虽然两种剂量的骨化三醇均增加了活性钙转运,但对钙结合蛋白-D9k mRNA或蛋白质没有刺激作用。在慢性尿毒症大鼠中,每只大鼠注射两剂300 ng骨化三醇后,活性钙转运、十二指肠钙结合蛋白-D9k和钙结合蛋白-D9k mRNA均受到刺激。相同剂量的OCT处理导致钙结合蛋白-D9k和钙结合蛋白-D9k mRNA受到类似刺激,但未能诱导活性钙转运增加。这些结果表明,(1)在向正常和高血压大鼠给予骨化三醇后,以及(2)在向尿毒症大鼠给予OCT后,肠道活性钙转运和钙结合蛋白-D9k的刺激在蛋白质合成和mRNA表达水平上可完全分离。(摘要截短至250字)

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