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首页> 外文期刊>Clinical chemistry and laboratory medicine: CCLM >High biological variation of serum hyaluronic acid and Hepascore, a biochemical marker model for the prediction of liver fibrosis.
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High biological variation of serum hyaluronic acid and Hepascore, a biochemical marker model for the prediction of liver fibrosis.

机译:血清透明质酸和肝纤维的高生物变异,一种用于预测肝纤维化的生化标志模型。

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Serum hyaluronic acid and biochemical models which require hyaluronic acid analysis are commonly used as predictors of liver fibrosis in patients with chronic liver disease, however biological variation data for hyaluronic acid are deficient.Four serial serum samples were obtained at weekly intervals from healthy volunteers and patients with chronic hepatitis B, chronic hepatitis C and non- alcoholic fatty liver disease (NAFLD; 20 in each group). The within-individual week-to-week variation (CVI) and reference change values for hyaluronic acid, α?-macroglobulin and Hepascore were obtained. Hepascore is calculated from hyaluronic acid, α2-macroglobulin, bilirubin and γ-glutamyltransferase activity.Hyaluronic acid displayed large within-individual variation, the CVI values were 62% in healthy subjects, 38% in hepatitis C, 37% in hepatitis B and 36% in NAFLD patients. Hepascore CVIs were 43% in healthy subjects, 24% in hepatitis C, 28% in hepatitis B and 39% in NAFLD patients. α?-Macroglobulin was much less variable with CVIs ranging from 4.4% to 7.6%. Bland-Altman plots of week-to-week variations showed rates of significant disagreement for samples collected in any 2 successive weeks varied from 5% in NAFLD patients to 8.3% in healthy subjects.When using non-fasting serum samples, hyaluronic acid and to a lesser extent, the Hepascore model display large within-individual variations in both health and chronic liver disease. This information is critical for interpreting the significance of both single measurements and changes in serial measurements.
机译:需要透明质酸分析的血清透明质酸和生化模型通常用作慢性肝病患者肝纤维化的预测因子,但透明质酸的生物变异数据是不足的。每周血清样品的血清样本是从健康志愿者和患者的每周间隔获得的。含有慢性乙型肝炎,慢性丙型肝炎和非酒精脂肪肝病(NAFLD;每组20)。获得透明质酸,αα-αα-αα-α-αααααααααααααααααααααααα-克罗葡萄糖蛋白和肝素。从透明质酸,α2-麦克风素,胆红素和γ-谷氨酰转移酶活性计算肝孔。羟基脲在内部变异内显示出大,在健康受试者中,CVI值为62%,丙型肝炎38%,乙型肝炎和36%百分比患者%。 HepaScore CVIS在健康受试者中43%,甲型肝炎24%,乙型肝炎28%和39%的NAFLD患者。 α-α-昔螺胶蛋白的可变变化与CVIS范围为4.4%至7.6%。一周到周的平坦altman图表显示出在任何2个星期内收集的样品的显着分歧的率,从NAFLD患者的5%变化,在健康主题中的8.3%。使用非禁食血清样品,透明质酸和到较小程度,肝脏模型在健康和慢性肝病中显示出大的内部变化。此信息对于解释单次测量和串行测量的变化的重要性至关重要。

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