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Specificity Evaluation and Disease Monitoring in Arthritis Imaging with Complement Receptor of the Ig superfamily targeting Nanobodies

机译:Ig超家族靶向纳米抗体的补体受体在关节炎成像中的特异性评估和疾病监测

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Single-photon emission computed tomography combined with micro-CT (SPECT/μCT) imaging using Nanobodies against complement receptor of the Ig superfamily (CRIg), found on tissue macrophages such as synovial macrophages, has promising potential to visualize joint inflammation in experimental arthritis. Here, we further addressed the specificity and assessed the potential for arthritis monitoring. Signals obtained with (99m)Tc-labelled NbV4m119 Nanobody were compared in joints of wild type (WT) versus CRIg(-/-) mice with collagen-induced arthritis (CIA) or K/BxN serum transfer-induced arthritis (STIA). In addition, SPECT/μCT imaging was used to investigate arthritis development in STIA and in CIA under dexamethasone treatment. (99m)Tc-NbV4m119 accumulated in inflamed joints of WT, but not CRIg(-/-) mice with CIA and STIA. Development and spontaneous recovery of symptoms in STIA was reflected in initially increased and subsequently reduced joint accumulation of (99m)Tc-NbV4m119. Dexamethasone treatment of CIA mice reduced (99m)Tc-NbV4m119 accumulation as compared to saline control in most joints except knees. SPECT/μCT imaging with (99m)Tc-NbV4m119 allows specific assessment of inflammation in different arthritis models and provides complementary information to clinical scoring for quantitatively and non-invasively monitoring the pathological process and the efficacy of arthritis treatment.
机译:单光子发射计算机断层扫描与微CT(SPECT /μCT)成像结合使用抗Ig超家族(CRIg)补体受体的纳米抗体,发现于组织巨噬细胞(如滑膜巨噬细胞)上,有望在实验性关节炎中可视化关节炎症。在这里,我们进一步探讨了特异性,并评估了关节炎监测的潜力。将(99m)Tc标记的NbV4m119纳米抗体获得的信号在具有胶原蛋白诱导的关节炎(CIA)或K / BxN血清转移诱导的关节炎(STIA)的野生型(WT)与CRIg(-/-)小鼠的关节中进行比较。此外,在地塞米松治疗下,SPECT /μCT成像用于研究STIA和CIA中的关节炎发展。 (99m)Tc-NbV4m119在WT的发炎关节中蓄积,但在CIA和STIA的CRIg(-/-)小鼠中没有蓄积。 (99m)Tc-NbV4m119的关节蓄积最初增加,随后减少,反映出STIA中症状的发展和自发恢复。与生理盐水对照组相比,除膝盖外,地塞米松治疗CIA小鼠减少(99m)Tc-NbV4m119积聚。用(99m)Tc-NbV4m119进行的SPECT /μCT成像可对不同关节炎模型中的炎症进行特异性评估,并为临床评分提供补充信息,以定量和非侵入性地监测关节炎的病理过程和疗效。

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