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Determination of the site of metabolism of total, free, and complexed prostate-specific antigen.

机译:确定总的,游离的和复杂的前列腺特异性抗原的代谢部位。

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OBJECTIVES: To determine the site of metabolism of total prostate-specific antigen (tPSA), free PSA (fPSA), and complexed PSA (cPSA). METHODS: A total of 20 male patients, 50 years old or older, having a clinical indication for left and right heart catheterization were enrolled in this study. Selective blood samples were obtained from the infrarenal, infrahepatic, and suprahepatic inferior vena cava, renal vein, hepatic vein, superior vena cava, pulmonary artery, and femoral artery. cPSA concentration was accepted as the difference between tPSA and fPSA concentrations. RESULTS: We found that tPSA and fPSA concentrations in the infrarenal inferior vena cava were significantly higher than in the systemic artery. There was no significant difference between the systemic artery and the infrarenal inferior vena cava for cPSA concentration. Although fPSA concentration decreased significantly across the renal circulation, the decreases in cPSA and tPSA concentrations were statistically insignificant. In the hepatic circulation, we found that tPSA, fPSA, and cPSA concentrations were significantly decreased. No decrease in tPSA, fPSA, and cPSA concentrations were noted across the pulmonary circulation. CONCLUSIONS: Our results indicate that fPSA and tPSA are released into serum from the prostate but the prostate may not have a significant role in complex formation of PSA. In addition, the liver has a significant role in the elimination of tPSA, fPSA, and cPSA. By contrast, the kidneys have a significant role only in the elimination of fPSA. We also found that the lungs did not have a significant role in the elimination of tPSA, fPSA, or cPSA.
机译:目的:确定总前列腺特异性抗原(tPSA),游离PSA(fPSA)和复合PSA(cPSA)的代谢部位。方法:本研究共纳入20例50岁或以上的男性患者,这些患者具有左右心脏导管插入术的临床指征。从肾下,肝下和肝上下腔静脉,肾静脉,肝静脉,上腔静脉,肺动脉和股动脉获取选择性血液样品。 cPSA浓度被认为是tPSA和fPSA浓度之间的差异。结果:我们发现肾下下腔静脉中的tPSA和fPSA浓度显着高于全身动脉。对于cPSA浓度,全身动脉与肾下腔静脉之间无显着差异。尽管整个肾脏循环中fPSA浓度显着降低,但cPSA和tPSA浓度的降低在统计学上并不显着。在肝循环中,我们发现tPSA,fPSA和cPSA浓度显着降低。整个肺循环中未发现tPSA,fPSA和cPSA浓度降低。结论:我们的结果表明fPSA和tPSA从前列腺释放到血清中,但前列腺可能在PSA的复杂形成中没有重要作用。此外,肝脏在消除tPSA,fPSA和cPSA方面具有重要作用。相比之下,肾脏仅在消除fPSA中具有重要作用。我们还发现,肺部在消除tPSA,fPSA或cPSA中没有重要作用。

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