Aesif Scott W, Anathy Vikas, Havermans Marije, Guala Amy S, Ckless Karina, Taatjes Douglas J, Janssen-Heininger Yvonne M W
Department of Pathology, University of Vermont College of Medicine, Burlington, VT 05405, USA.
Am J Pathol. 2009 Jul;175(1):36-45. doi: 10.2353/ajpath.2009.080736.
Protein S-glutathionylation (PSSG) is a posttranslational modification that involves the conjugation of the small antioxidant molecule glutathione to cysteine residues and is emerging as a critical mechanism of redox-based signaling. PSSG levels increase under conditions of oxidative stress and are controlled by glutaredoxins (Grx) that, under physiological conditions, preferentially deglutathionylate cysteines and restore sulfhydryls. Both the occurrence and distribution of PSSG in tissues is unknown because of the labile nature of this oxidative event and the lack of specific reagents. The goal of this study was to establish and validate a protocol that enables detection of PSSG in situ, using the property of Grx to deglutathionylate cysteines. Using Grx1-catalyzed cysteine derivatization, we evaluated PSSG content in mice subjected to various models of lung injury and fibrosis. In control mice, PSSG was detectable primarily in the airway epithelium and alveolar macrophages. Exposure of mice to NO(2) resulted in enhanced PSSG levels in parenchymal regions, while exposure to O(2) resulted in minor detectable changes. Finally, bleomycin exposure resulted in marked increases in PSSG reactivity both in the bronchial epithelium as well as in parenchymal regions. Taken together, these findings demonstrate that Grx1-based cysteine derivatization is a powerful technique to specifically detect patterns of PSSG expression in lungs, and will enable investigations into regional changes in PSSG content in a variety of diseases.
蛋白质S-谷胱甘肽化(PSSG)是一种翻译后修饰,涉及小抗氧化分子谷胱甘肽与半胱氨酸残基的缀合,正成为基于氧化还原信号传导的关键机制。在氧化应激条件下,PSSG水平会升高,并受谷氧还蛋白(Grx)控制,在生理条件下,谷氧还蛋白优先使半胱氨酸去谷胱甘肽化并恢复巯基。由于这种氧化事件的不稳定性以及缺乏特异性试剂,PSSG在组织中的发生情况和分布尚不清楚。本研究的目的是建立并验证一种方案,利用谷氧还蛋白使半胱氨酸去谷胱甘肽化的特性,原位检测PSSG。使用Grx1催化的半胱氨酸衍生化,我们评估了遭受各种肺损伤和纤维化模型的小鼠中的PSSG含量。在对照小鼠中,主要在气道上皮和肺泡巨噬细胞中可检测到PSSG。将小鼠暴露于NO(2)会导致实质区域的PSSG水平升高,而暴露于O(2)会导致可检测到的微小变化。最后,博来霉素暴露导致支气管上皮以及实质区域的PSSG反应性显著增加。综上所述,这些发现表明基于Grx1的半胱氨酸衍生化是一种强大的技术,可特异性检测肺中PSSG的表达模式,并将有助于研究各种疾病中PSSG含量的区域变化。