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载有吲哚菁绿的单核细胞作为主动归巢对比剂可使感染性和非感染性炎症的光学区分成为可能。

Monocytes loaded with indocyanine green as active homing contrast agents permit optical differentiation of infectious and non-infectious inflammation.

机构信息

Department of Plastic and Reconstructive Surgery, Johns Hopkins University School of Medicine, Baltimore, Maryland, United States of America.

出版信息

PLoS One. 2013 Nov 25;8(11):e81430. doi: 10.1371/journal.pone.0081430. eCollection 2013.

Abstract

Distinguishing cutaneous infection from sterile inflammation is a diagnostic challenge and currently relies upon subjective interpretation of clinical parameters, microbiological data, and nonspecific imaging. Assessing characteristic variations in leukocytic infiltration may provide more specific information. In this study, we demonstrate that homing of systemically administered monocytes tagged using indocyanine green (ICG), an FDA-approved near infrared dye, may be assessed non-invasively using clinically-applicable laser angiography systems to investigate cutaneous inflammatory processes. RAW 264.7 mouse monocytes co-incubated with ICG fluoresce brightly in the near infrared range. In vitro, the loaded cells retained the ability to chemotax toward monocyte chemotactic protein-1. Following intravascular injection of loaded cells into BALB/c mice with induced sterile inflammation (Complete Freund's Adjuvant inoculation) or infection (Group A Streptococcus inoculation) of the hind limb, non-invasive whole animal imaging revealed local fluorescence at the inoculation site. There was significantly higher fluorescence of the inoculation site in the infection model than in the inflammation model as early as 2 hours after injection (p<0.05). Microscopic examination of bacterial inoculation site tissue revealed points of near infrared fluorescence, suggesting the presence of ICG-loaded cells. Development of a non-invasive technique to rapidly image inflammatory states without radiation may lead to new tools to distinguish infectious conditions from sterile inflammatory conditions at the bedside.

摘要

从无菌性炎症中区分皮肤感染是一个诊断挑战,目前依赖于对临床参数、微生物学数据和非特异性影像学的主观解释。评估白细胞浸润的特征变化可能提供更具体的信息。在这项研究中,我们证明了使用 FDA 批准的近红外染料吲哚菁绿 (ICG) 标记的系统性给予的单核细胞的归巢可以使用临床应用的激光血管造影系统进行非侵入性评估,以研究皮肤炎症过程。与 ICG 共孵育的 RAW 264.7 小鼠单核细胞在近红外范围内发出明亮的荧光。在体外,负载的细胞保留了向单核细胞趋化蛋白-1趋化的能力。在 BALB/c 小鼠中静脉内注射负载细胞后,诱导无菌性炎症(完全弗氏佐剂接种)或感染(A 组链球菌接种)后,非侵入性全动物成像显示接种部位有局部荧光。与炎症模型相比,感染模型中注射后 2 小时即可观察到接种部位的荧光明显升高(p<0.05)。对细菌接种部位组织的显微镜检查显示出近红外荧光点,表明存在负载 ICG 的细胞。开发一种非侵入性技术来快速成像炎症状态而不使用辐射,可能会导致新的工具来区分感染性疾病和无菌性炎症疾病。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0ea8/3839882/95b2c39eff25/pone.0081430.g001.jpg

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