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首页> 外文期刊>Clinica chimica acta: International journal of clinical chemistry and applied molecular biology >Establishment of an in-house ELISA and the reference range for serum amyloid A (SAA): complementarity between SAA and C-reactive protein as markers of inflammation.
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Establishment of an in-house ELISA and the reference range for serum amyloid A (SAA): complementarity between SAA and C-reactive protein as markers of inflammation.

机译:建立内部ELISA以及血清淀粉样蛋白A(SAA)的参考范围:SAA和C反应蛋白之间的互补性(作为炎症的标志物)。

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INTRODUCTION: Serum amyloid A (SAA) and C-reactive protein (CRP) are both acute-phase reactants synthesized by the liver upon stimulation by proinflammatory cytokines reflecting both the acute and chronic inflammatory states. METHODS: We have established a one-step, sandwich ELISA on microplate for SAA using commercial antibodies for coating and detection. RESULTS: This in-house ELISA has a sensitivity of 0.12 mg/l. Both within-day and between-day CVs were <10%. The in-house assay correlated well with the commercial ELISA kit from Anogen (r=0.95). We also established the reference range for apparently healthy Chinese. Statistically higher SAA values were found in those >50 years old. No difference was found between genders. We found only slightly increased levels of SAA in early stage of type 2 diabetics, but highly increased levels of SAA were detected in patients with acute myocardial infarction, generally associated with intense inflammation. At the early stage of type 2 diabetes associated with lowinflammation, SAA was found to be complementary to CRP in test sensitivity. CONCLUSIONS: Based on our data and reports from the literature we believe that SAA responds differently than CRP in inflammatory diseases such as in type 2 diabetes and acute myocardial infarction, and is complementary to CRP in test sensitivity.
机译:简介:血清淀粉样蛋白A(SAA)和C反应蛋白(CRP)都是肝脏在受到促炎细胞因子刺激后合成的急性期反应物,反映了急性和慢性炎症状态。方法:我们已经在微孔板上建立了用于SAA的一步一步夹心ELISA,并使用了商用抗体进行包被和检测。结果:这种内部ELISA的灵敏度为0.12 mg / l。日内和日间CV均<10%。内部分析与Anogen的商业ELISA试剂盒密切相关(r = 0.95)。我们还为看似健康的中国人建立了参考范围。在50岁以上的人群中发现SAA值在统计上较高。性别之间没有发现差异。我们发现,在2型糖尿病的早期阶段,SAA的水平仅略有增加,但是在急性心肌梗死(通常与强烈炎症相关)的患者中检测到SAA的水平显着增加。在与低炎症相关的2型糖尿病的早期阶段,发现SAA与CRP的检测敏感性互补。结论:基于我们的数据和文献报道,我们认为SAA在2型糖尿病和急性心肌梗死等炎症性疾病中的反应不同于CRP,并且在测试敏感性方面与CRP互补。

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