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Sulfate homeostasis, NaSi-1 cotransporter, and SAT-1 exchanger expression in chronic renal failure in rats

机译:硫酸盐稳态,NaSi-1共转运蛋白和SAT-1交换子在大鼠慢性肾衰竭中的表达

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摘要

Background. It is known that hypersulfatemia, like hyperphosphatemia, occurs in chronic renal failure (CRF). The aim of this study was to assess the effects of CRF on sulfate homeostasis and on sodium sulfate cotransport (NaSi-1) and sulfate/ oxalate-bicarbonate exchanger (Sat-1) expression in the kidney. In addition, sulfate homeostasis was compared with phosphate homeostasis. Methods. Experimental studies were performed in adult male rats at three and six weeks after 80% subtotal nephrectomy (Nx) or sham-operation (8) (N = 9 per group). Transporter protein and mRNA expressions were measured by Western blot and RNase protection assay (RPA), respectively. Results were quantitated by densitometric scanning (Western) and electronic autoradiography (RPA), and were expressed in densitometric units (DUs: Western) and cpm (RPA). Results. Creatinine clearance was lower in Nx-3 compared with S-3 rats (0.23 vs. 0.51 mL/min/100 g body weight, P <0.001) and was further impaired in Nx-6 rats (0.15 vs. 0.48, P <0.001). Sulfatemia was significantly higher in Nx-3 rats (1.08 vs. 0.84 mmol/L, P <0.05) and further increased in Nx-6 rats (1.42 vs. 0.90 mmol/L, P <0.01). Fractional sulfate excretion (FESO4) was increased by twofold in Nx-3 and Nx-6 rats compared with corresponding S rats. Phosphatemia did not differ between Nx-3 rats and controls, but was increased in Nx-6 rats (P <0.01). Total amounts of both NaSi-1 and Sat-1 proteins were significantly decreased in both Nx-3 and Nx-6 rats when compared with controls. However, NaSi-1 protein and mRNA densities did not significantly change in Nx-3 rats, but were significantly increased in Nx-6 rats when compared with controls (4.8 vs. 3.7 DU/g protein, P <0.05, and 7.1 vs. 2.8 cpm/g RNA, P <0.01, respectively, for protein and mRNA). In contrast to NaSi-1, Sat-1 protein density was significantly decreased both in Nx-3 (2.9 vs. 3.6 DU/g protein, P <0.05) and Nx-6 rats (2.4 vs. 3.4 DU/g protein, P <0.05), and Sat-1 mRNA density significantly decreased in Nx-6 rats (10.7 vs. 14.7 cpm/g RNA, P <0.05). Na-PO4 cotransporter (NaPi-2) protein total abundance and density were decreased at three and six weeks in Nx rats. Conclusions. These results demonstrate that both NaSi-1 and Sat-1 total protein abundances are decreased in CRF, which may contribute to the increase in fractional sulfate excretion. Strikingly, NaSi-1 density was not decreased in CRF three weeks after Nx, and furthermore, increased six weeks after Nx, in contrast to NaPi-2 density, which was decreased at both times. The significance of this difference remains to be determined, but may explain why hypersulfatemia occurs earlier than hyperphosphatemia in CRF.
机译:背景。众所周知,高磷血症与高磷血症一样,会发生在慢性肾衰竭(CRF)中。这项研究的目的是评估CRF对肾脏中硫酸盐稳态,硫酸钠共转运(NaSi-1)和硫酸盐/草酸盐-碳酸氢盐交换剂(Sat-1)表达的影响。另外,比较了硫酸盐稳态和磷酸盐稳态。方法。在成年雄性大鼠中,进行80%的次全肾切除术(Nx)或假手术(8)(每组N = 9)后的三和六周进行了实验研究。转运蛋白和mRNA表达分别通过蛋白质印迹法和RNase保护测定(RPA)测定。结果通过光密度扫描(Western)和电子放射自显影(RPA)进行定量,并以光密度单位(DUs:Western)和cpm(RPA)表示。结果。与S-3大鼠相比,Nx-3中的肌酐清除率较低(0.23对0.51 mL / min / 100 g体重,P <0.001),而在Nx-6大鼠中进一步受损(0.15对0.48,P <0.001) )。 Nx-3大鼠的血脂异常显着增高(1.08 vs. 0.84 mmol / L,P <0.05),Nx-6大鼠进一步升高(1.42 vs. 0.90 mmol / L,P <0.01)。与相应的S大鼠相比,Nx-3和Nx-6大鼠的硫酸盐分数排泄(FESO4)增加了两倍。 Nx-3大鼠与对照组之间的血磷没有差异,但Nx-6大鼠中的磷酸血症却增加了(P <0.01)。与对照组相比,Nx-3和Nx-6大鼠的NaSi-1和Sat-1蛋白总量均显着降低。但是,与对照组相比,Nx-3大鼠的NaSi-1蛋白和mRNA密度没有显着变化,但在Nx-6大鼠中NaSi-1蛋白和mRNA的密度却显着增加(4.8 vs. 3.7 DU / g蛋白,P <0.05,和7.1 vs. DU / g)。 2.8 cpm / g RNA,蛋白质和mRNA分别为P <0.01)。与NaSi-1相比,Nx-3(2.9 vs. 3.6 DU / g蛋白,P <0.05)和Nx-6大鼠(2.4 vs. 3.4 DU / g蛋白,P)的Sat-1蛋白密度均显着降低。 <0.05),Nx-6大鼠的Sat-1 mRNA密度显着降低(10.7 vs. 14.7 cpm / g RNA,P <0.05)。在Nx大鼠中,第3周和第6周,Na-PO4共转运蛋白(NaPi-2)的总蛋白丰度和密度降低。结论。这些结果表明,CRF中NaSi-1和Sat-1总蛋白丰度均降低,这可能有助于增加硫酸盐排泄分数。引人注目的是,Nx在三周后CRF中NaSi-1密度没有降低,而且在Nx后六周中NaSi-1密度却增加了,而NaPi-2密度却在两个时间中均降低了。这种差异的重要性尚待确定,但可以解释为什么高硫酸血症发生的时间早于CRF中的高磷酸盐血症。

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