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在体内对天然免疫细胞进行纳米颗粒成像可作为多发性硬化症模型中疾病严重程度的一个标志物。

In vivo nanoparticle imaging of innate immune cells can serve as a marker of disease severity in a model of multiple sclerosis.

作者信息

Kirschbaum Klara, Sonner Jana K, Zeller Matthias W, Deumelandt Katrin, Bode Julia, Sharma Rakesh, Krüwel Thomas, Fischer Manuel, Hoffmann Angelika, Costa da Silva Milene, Muckenthaler Martina U, Wick Wolfgang, Tews Björn, Chen John W, Heiland Sabine, Bendszus Martin, Platten Michael, Breckwoldt Michael O

机构信息

German Cancer Consortium, Clinical Cooperation Unit Neuroimmunology and Brain Tumor Immunology, German Cancer Research Center (DKFZ), 69120 Heidelberg, Germany.

Department of Neuroradiology, University Hospital Heidelberg, 69120 Heidelberg, Germany.

出版信息

Proc Natl Acad Sci U S A. 2016 Nov 15;113(46):13227-13232. doi: 10.1073/pnas.1609397113. Epub 2016 Oct 31.

Abstract

Innate immune cells play a key role in the pathogenesis of multiple sclerosis and experimental autoimmune encephalomyelitis (EAE). Current clinical imaging is restricted to visualizing secondary effects of inflammation, such as gliosis and blood-brain barrier disruption. Advanced molecular imaging, such as iron oxide nanoparticle imaging, can allow direct imaging of cellular and molecular activity, but the exact cell types that phagocytose nanoparticles in vivo and how phagocytic activity relates to disease severity is not well understood. In this study we used MRI to map inflammatory infiltrates using high-field MRI and fluorescently labeled cross-linked iron oxide nanoparticles for cell tracking. We confirmed nanoparticle uptake and MR detectability ex vivo. Using in vivo MRI, we identified extensive nanoparticle signal in the cerebellar white matter and circumscribed cortical gray matter lesions that developed during the disease course (4.6-fold increase of nanoparticle accumulation in EAE compared with healthy controls, P < 0.001). Nanoparticles showed good cellular specificity for innate immune cells in vivo, labeling activated microglia, infiltrating macrophages, and neutrophils, whereas there was only sparse uptake by adaptive immune cells. Importantly, nanoparticle signal correlated better with clinical disease than conventional gadolinium (Gd) imaging (r, 0.83 for nanoparticles vs. 0.71 for Gd-imaging, P < 0.001). We validated our approach using the Food and Drug Administration-approved iron oxide nanoparticle ferumoxytol. Our results show that noninvasive molecular imaging of innate immune responses can serve as an imaging biomarker of disease activity in autoimmune-mediated neuroinflammation with potential clinical applications in a wide range of inflammatory diseases.

摘要

固有免疫细胞在多发性硬化症和实验性自身免疫性脑脊髓炎(EAE)的发病机制中起关键作用。目前的临床成像仅限于可视化炎症的继发性影响,如神经胶质增生和血脑屏障破坏。先进的分子成像,如氧化铁纳米颗粒成像,可以直接对细胞和分子活动进行成像,但体内吞噬纳米颗粒的确切细胞类型以及吞噬活性与疾病严重程度的关系尚不清楚。在本研究中,我们使用磁共振成像(MRI)通过高场MRI和荧光标记的交联氧化铁纳米颗粒来绘制炎症浸润图以进行细胞追踪。我们在体外证实了纳米颗粒的摄取和磁共振可检测性。通过体内MRI,我们在疾病过程中出现的小脑白质和局限性皮质灰质病变中发现了广泛的纳米颗粒信号(与健康对照相比,EAE中纳米颗粒积累增加4.6倍,P<0.001)。纳米颗粒在体内对固有免疫细胞显示出良好的细胞特异性,标记活化的小胶质细胞、浸润的巨噬细胞和中性粒细胞,而适应性免疫细胞的摄取很少。重要的是,纳米颗粒信号与临床疾病的相关性优于传统的钆(Gd)成像(纳米颗粒的r为0.83,Gd成像为0.71,P<0.001)。我们使用美国食品药品监督管理局批准的氧化铁纳米颗粒菲洛施来验证我们的方法。我们的结果表明,固有免疫反应的非侵入性分子成像可作为自身免疫介导的神经炎症中疾病活动的成像生物标志物,在广泛的炎症性疾病中具有潜在的临床应用价值。

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