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基质金属蛋白酶-12 活性形式在炎症和动脉瘤中的光学成像。

Optical imaging of MMP-12 active form in inflammation and aneurysm.

机构信息

Cardiovascular Molecular Imaging Laboratory, Section of Cardiovascular Medicine and Yale Cardiovascular Research Center, Yale University School of Medicine, New Haven, CT USA.

Veterans Affairs Connecticut Healthcare System, West Haven, CT USA.

出版信息

Sci Rep. 2016 Dec 5;6:38345. doi: 10.1038/srep38345.

Abstract

Matrix metalloproteinase (MMP)-12 plays a key role in the development of aneurysm. Like other members of MMP family, MMP-12 is produced as a proenzyme, mainly by macrophages, and undergoes proteolytic activation to generate an active form. Accordingly, molecular imaging of the MMP-12 active form can inform of the pathogenic process in aneurysm. Here, we developed a novel family of fluorescent probes based on a selective MMP-12 inhibitor, RXP470.1 to target the active form of MMP-12. These probes were stable in complex media and retained the high affinity and selectivity of RXP470.1 for MMP-12. Amongst these, probe 3 containing a zwitterionic fluorophore, ZW800-1, combined a favorable affinity profile toward MMP-12 and faster blood clearance. In vivo binding of probe 3 was observed in murine models of sterile inflammation and carotid aneurysm. Binding specificity was demonstrated using a non-binding homolog. Co-immunostaining localized MMP-12 probe binding to MMP-12 positive areas and F4/80 positive macrophages in aneurysm. In conclusion, the active form of MMP-12 can be detected by optical imaging using RXP470.1-based probes. This is a valuable adjunct for pathophysiology research, drug development, and potentially clinical applications.

摘要

基质金属蛋白酶(MMP)-12 在动脉瘤的发展中起着关键作用。与 MMP 家族的其他成员一样,MMP-12 作为一种前酶主要由巨噬细胞产生,并经历蛋白水解激活生成活性形式。因此,MMP-12 活性形式的分子成像可以提示动脉瘤中的发病过程。在这里,我们开发了一系列基于选择性 MMP-12 抑制剂 RXP470.1 的新型荧光探针,以靶向 MMP-12 的活性形式。这些探针在复杂介质中稳定,保留了 RXP470.1 对 MMP-12 的高亲和力和选择性。其中,含有两性离子荧光团 ZW800-1 的探针 3 具有良好的 MMP-12 亲和力和更快的血液清除率。在无菌性炎症和颈动脉动脉瘤的小鼠模型中观察到探针 3 的体内结合。使用非结合同源物证明了结合特异性。共免疫染色将 MMP-12 探针结合定位到动脉瘤中 MMP-12 阳性区域和 F4/80 阳性巨噬细胞上。总之,使用基于 RXP470.1 的探针可以通过光学成像检测 MMP-12 的活性形式。这对于病理生理学研究、药物开发以及潜在的临床应用是一种有价值的辅助手段。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1022/5137160/6399ad689411/srep38345-f1.jpg

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