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Trace of Antibody to Myeloperoxidase with Nanocrystal Quantum Dot-Labeled Antibody Recognizing Activating Neutrophils

机译:用纳米晶体点标记的抗体鉴定活化中性粒细胞抗体的抗体群

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It is assumed that activated neutrophils contribute to the development of anti-neutrophil cytoplasmic auto-antibody (ANCA)-associated vasculitis due to the association of myelopeoxidase(MPO)-ANCA with MPO expressed on the surface of activated neutrophils. FITC-labeled antibody (Ab) used widely are not suitable for neutrophil examination because of the labile fluorescence emission of FITC. Therefore, it is necessary to develop specific fluorescent probes for MPO detection in neutrophils in vivo. Recently, fluorescent nanocrystal quantum dots (QDs) have been used for biotechnological and medical applications because of their greater and far longer fluorescence in. QDs have several advantages over organic fluorophores: high luminescence, far longer stability against photobleaching, and a range of fluorescence wavelengths from blue to infrared, depending on particle size. Thus, we examined the role of MPO and the Ab to MPO in the pathogenesis of glomerulonephritis associated with MPO-ANCA in experimental glomerulonephritis mice using QDs. We demonstrated the QD-conjugated anti-MPO Ab visualized the expression of MPO on the neutrophil surface after stimulation with proinflammatory cytokines. In addition, QD immuno-conjugates with anti-recombinant murine MPO (rmMPO) Ab revealed the trafficking of MPO-ANCA in vivo. Deceleration of blood flow in kidney vessels occurred in model mice, in which serum proteins including anti-rmMPO Ab were leaked out from collapsed glomeruli into the proximal tubule. Thus, sustained MPO expression on the neutrophil surface was significantly related to glomerulonephritis. These results indicate that the expressed MPO on the activated neutrophils with anti-MPO Ab may coordinately play essential roles in the initial steps for the development of glomerulonephritis.
机译:假设活化的嗜中性粒细胞有助于发育抗中性粒细胞细胞质自动 - 抗体(ANCA) - 由于骨髓苷酸酶(MPO)-ANCA与在活性中性粒细胞表面上表达的MPO的关联而产生的血管炎。由于FITC的不稳定荧光发射,FITC标记的抗体(AB)不适合中性粒子检查。因此,有必要在体内中嗜中性粒细胞中发育特定的荧光探针进行MPO检测。最近,荧光纳米晶体圆点(QDS)已被用于生物技术和医学应用,因为它们越大,荧光较长。QDS在有机荧光团上具有几个优点:高发光,对光博的稳定性远远较长,以及一系列荧光波长的稳定性从蓝色到红外线,取决于粒径。因此,我们将MPO和AB对使用QDS的实验性肾小球肾炎小鼠相关的肾小球肾炎的发病机制中的作用。我们证明了QD缀合的抗MPO AB在刺激促炎细胞因子刺激后可视化中性粒细胞表面上的MPO表达。此外,QD免疫缀合物与抗重组鼠MPO(RMMPO)AB揭示了体内MPO-ANCA的贩运。在模型小鼠中发生肾脏血管中血流减速,其中包括抗RMMPO AB的血清蛋白从塌陷的肾小球中泄漏到近端小管中。因此,中性粒细胞表面上的持续MPO表达与肾小球肾炎有显着相关。这些结果表明,具有抗MPO AB的活化嗜中性粒细胞上的表达的MPO可以协调在肾小球肾炎的开发的初始步骤中起作用的基本作用。

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