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Gas Chromatographic–Mass Spectrometric Analysis for Measurement of p-Cresol and Its Conjugated Metabolites in Uremic and Normal Serum

机译:气相色谱-质谱法测定尿液和正常血清中的对甲酚及其共轭代谢产物

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p -Cresol (4-methylphenol; 108 Da) is a protein-bound solute retained within the body in renal failure (1). p -Cresol is of interest because it has several toxic effects in vitro (2)(3)(4)(5)(6) and clinical correlates have been demonstrated (7)(8). In the absence of external exposure (9), p -cresol originates uniquely from bacterial tyrosine fermentation in the large intestine (10). During passage through the colonic mucosa and liver, it is detoxified by conjugation processes (sulfation and glucuronidation) (11)(12)(13). Thus, one might expect to find p -cresylsulfate and p -cresylglucuronide in the serum, but reports on conjugated p -cresol in renal failure patients are scarce (14)(15)(16). Most techniques to deproteinize serum samples (e.g., heat and acidification) may also partially hydrolyze sulfate esters and glucuronide bonds. Hence, the “total” (i.e., protein-bound and unbound) and “unbound” p -cresol reported in most studies probably reflect both unconjugated and (part of the) conjugated forms of the solute (17)(18)(19)(20)(21). We determined the extent of desulfation and deglucuronidation by deproteinization with heat and acid followed by gas chromatographic–mass spectrometric (GC-MS) analysis (19) with p -nitrophenylglucuronide and p -nitrophenylsulfate as model substrates. We also calculated exact amounts of unconjugated p -cresol, p -cresylsulfate, and p -cresylglucuronide in serum of hemodialysis patients and healthy controls.Percentage desulfation and deglucuronidation by different methods (see below) was determined for random serum samples. Further analyses were performed on 9 serum pools from hemodialysis patients [n = 86; 49 male; mean (SD) age, 69.8 (1.5) years] and 5 serum pools from healthy controls [n = 29; 10 male; 31.0 (1.4) years; creatinine clearance, 87.1 (1.4) mL · min?1 · (1.73 m2)?1]. Serum pools were …
机译:对甲酚(4-甲基苯酚; 108 Da)是一种蛋白质结合的溶质,可保留在肾衰竭患者体内(1)。对甲酚是令人感兴趣的,因为它在体外具有多种毒性作用(2)(3)(4)(5)(6)并已证明其临床相关性(7)(8)。在没有外部暴露的情况下(9),对甲酚独特地起源于大肠中细菌酪氨酸的发酵(10)。在通过结肠粘膜和肝脏的过程中,它通过结合过程(硫酸化和葡萄糖醛酸化)解毒(11)(12)(13)。因此,人们可能期望在血清中发现对-甲苯基硫酸盐和对-甲苯基葡萄糖醛酸苷,但是关于肾衰竭患者中共轭对-甲酚的报道很少(14)(15)(16)。使血清样品脱蛋白的大多数技术(例如加热和酸化)也可以部分水解硫酸酯和葡糖醛酸苷键。因此,大多数研究中报告的“全部”(即蛋白结合的和未结合的)和“未结合的”对甲酚可能反映了溶质的未结合形式和(部分)结合形式(17)(18)(19) (20)(21)。我们确定了先用热和酸脱蛋白,然后用对硝基苯基葡萄糖醛酸和对硝基苯硫酸盐作为模型基质的气相色谱-质谱(GC-MS)分析(19)来确定脱硫和去葡糖醛酸的程度。我们还计算了血液透析患者和健康对照者血清中未结合的对甲酚,对甲酚硫酸盐和对甲酚葡萄糖醛酸的确切含量,并通过不同方法(见下文)确定了脱硫和去葡糖醛酸化的百分比。从血液透析患者的9个血清库中进行了进一步分析[n = 86; 49男;健康对照组的平均(SD)年龄为69.8(1.5)岁]和5个血清库[n = 29; 10男; 31.0(1.4)年;肌酐清除率:87.1(1.4)mL·min?1·(1.73 m2)?1]。血清池...

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