通过α5β1整合素靶向正电子发射断层扫描对类风湿关节炎早期阶段进行体内成像。

In vivo imaging of early stages of rheumatoid arthritis by α5β1-integrin-targeted positron emission tomography.

作者信息

Notni Johannes, Gassert Florian T, Steiger Katja, Sommer Peter, Weichert Wilko, Rummeny Ernst J, Schwaiger Markus, Kessler Horst, Meier Reinhard, Kimm Melanie A

机构信息

Institute of Pathology, Technische Universität München, Trogerstr. 18, 81675, Munich, Germany.

Department of Diagnostic and Interventional Radiology, Technische Universität München, Munich, Germany.

出版信息

EJNMMI Res. 2019 Sep 9;9(1):87. doi: 10.1186/s13550-019-0541-6.

DOI:10.1186/s13550-019-0541-6

PMID:31501931

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6733939/

Abstract

BACKGROUND

Rheumatoid arthritis (RA) is one of the most common rheumatic diseases. Joint inflammation and pathological growth of joint cartilage cause swollen and painful joints, which severely diminishes the patients' life quality. There is no causal treatment. Symptomatic therapies should start as early as possible to take maximal effect. Hence, diagnostic procedures capable of detecting affected joints before the onset of clinical symptoms are highly desirable. We explored the value of PET imaging of integrin subtypes αvβ3 and α5β1 for early detection of RA foci in collagen-induced arthritis (CIA) mouse models.

RESULTS

Development of RA in CIA mice was monitored by paw scoring, and αvβ3- and α5β1-integrin expression was quantified by μPET using Ga-Avebetrin and Ga-Aquibeprin. For consecutive sections of selected decalcified joints (knee, ankle), arthritic degeneration and integrin expression were assessed by MOVAT staining and β3/α5 immunohistochemistry (IHC), respectively. β3- and α5-IHC revealed elevated levels of both αvβ3- and α5β1-integrin in arthritic joints. Unlike αvβ3, α5β1 is strongly expressed in the proliferating synovial lining layer, which suggests that its presence is directly related to RA development. For mice with advanced RA (6 weeks after CIA), PET signals for α5β1-integrin were substantially stronger (> 300% of baseline) than that of αvβ3-integrin (< 200%). A longitudinal PET follow-up revealed that the manifestation of clinical symptoms of RA is preceded by upregulation of α5β1- but not of αvβ3-integrin.

CONCLUSION

α5β1-integrin PET could add a new functional imaging aspect to the portfolio of RA diagnostics because it appears to be a sensitive biomarker for early RA development. We suggest α5β1-integrin PET as a valuable tool to achieve a higher precision for early diagnosis of RA, including initial staging, monitoring of the disease course, and drug treatment, and for planning of radiosynoviorthesis (RSO).

摘要

背景

类风湿关节炎（RA）是最常见的风湿性疾病之一。关节炎症和关节软骨的病理性生长导致关节肿胀和疼痛，严重降低患者的生活质量。目前尚无针对病因的治疗方法。症状性治疗应尽早开始以取得最大效果。因此，非常需要能够在临床症状出现之前检测出受影响关节的诊断程序。我们探讨了整合素亚型αvβ3和α5β1的PET成像在胶原诱导性关节炎（CIA）小鼠模型中早期检测RA病灶的价值。

结果

通过爪部评分监测CIA小鼠中RA的发展，并使用镓-阿韦贝曲林和镓-阿奎贝曲林通过μPET对αvβ3和α5β1整合素表达进行定量。对于选定的脱钙关节（膝盖、脚踝）的连续切片，分别通过MOVAT染色和β3/α5免疫组织化学（IHC）评估关节炎性退变和整合素表达。β3和α5免疫组织化学显示关节炎关节中αvβ3和α5β1整合素水平均升高。与αvβ3不同，α5β1在增殖的滑膜衬里层中强烈表达，这表明其存在与RA发展直接相关。对于患有晚期RA（CIA后6周）的小鼠，α5β1整合素的PET信号比αvβ3整合素（<200%）强得多（>基线的300%）。纵向PET随访显示，RA临床症状的出现之前是α5β1而非αvβ3整合素的上调。

结论

α5β1整合素PET可为RA诊断增加一个新的功能成像方面，因为它似乎是RA早期发展的敏感生物标志物。我们建议将α5β1整合素PET作为一种有价值的工具，以实现更高精度的RA早期诊断，包括初始分期、疾病进程监测和药物治疗，以及放射性滑膜切除术（RSO）的规划。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a577/6733939/1eb01e062b2b/13550_2019_541_Fig1_HTML.jpg

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通过α5β1整合素靶向正电子发射断层扫描对类风湿关节炎早期阶段进行体内成像。

In vivo imaging of early stages of rheumatoid arthritis by α5β1-integrin-targeted positron emission tomography.

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