Lee Moung Young, Lee Donguk, Choi Dayun, Kim Kye S, Kang Peter M
Cardiovascular Institute, Beth Israel Deaconess Medical Center, Harvard Medical School, Boston, MA 02115, USA.
Centers for Research in ICT based Infectious Diseases, Jeonbuk National University, Jeonju 561-756, Republic of Korea.
J Funct Biomater. 2024 Dec 15;15(12):378. doi: 10.3390/jfb15120378.
Reactive oxygen species (ROS) are generated predominantly during cellular respiration and play a significant role in signaling within the cell and between cells. However, excessive accumulation of ROS can lead to cellular dysfunction, disease progression, and apoptosis that can lead to organ dysfunction. To overcome the short half-life of ROS and the relatively small amount produced, various imaging methods have been developed, using both endogenous and exogenous means to monitor ROS in disease settings. In this review, we discuss the molecular mechanisms underlying ROS production and explore the methods and materials that could be used to detect ROS overproduction, including iron-based materials, ROS-responsive chemical bond containing polymers, and ROS-responsive molecule containing biomaterials. We also discuss various imaging and imaging techniques that could be used to target and detect ROS overproduction. We discuss the ROS imaging potentials of established clinical imaging methods, such as magnetic resonance imaging (MRI), sonographic imaging, and fluorescence imaging. ROS imaging potentials of other imaging methods, such as photoacoustic imaging (PAI) and Raman imaging (RI) that are currently in preclinical stage are also discussed. Finally, this paper focuses on various diseases that are associated with ROS overproduction, and the current and the future clinical applications of ROS-targeted imaging. While the most widely used clinical condition is cardiovascular diseases, its potential extends into non-cardiovascular clinical conditions, such as neurovascular, neurodegenerative, and other ROS-associated conditions, such as cancers, skin aging, acute kidney injury, and inflammatory arthritis.
活性氧(ROS)主要在细胞呼吸过程中产生,在细胞内和细胞间信号传导中发挥重要作用。然而,ROS的过度积累会导致细胞功能障碍、疾病进展以及细胞凋亡,进而导致器官功能障碍。为了克服ROS半衰期短和产生量相对较少的问题,人们开发了各种成像方法,利用内源性和外源性手段在疾病环境中监测ROS。在这篇综述中,我们讨论了ROS产生的分子机制,并探索可用于检测ROS过量产生的方法和材料,包括铁基材料、含ROS响应化学键的聚合物以及含ROS响应分子的生物材料。我们还讨论了可用于靶向和检测ROS过量产生的各种成像和成像技术。我们讨论了已确立的临床成像方法的ROS成像潜力,如磁共振成像(MRI)、超声成像和荧光成像。还讨论了目前处于临床前阶段的其他成像方法的ROS成像潜力,如光声成像(PAI)和拉曼成像(RI)。最后,本文重点关注与ROS过量产生相关的各种疾病,以及ROS靶向成像的当前和未来临床应用。虽然最广泛使用的临床情况是心血管疾病,但其潜力扩展到非心血管临床情况,如神经血管、神经退行性疾病以及其他与ROS相关的情况,如癌症、皮肤衰老、急性肾损伤和炎症性关节炎。
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