Department of Pediatrics, Louisiana State University Health Sciences Center, 1501 Kings Highway, Shreveport, LA 71130, USA; Center for Cardiovascular Diseases and Sciences, Louisiana State University Health Sciences Center, Shreveport, LA 71130, USA.
Department of Pediatrics, Louisiana State University Health Sciences Center, 1501 Kings Highway, Shreveport, LA 71130, USA; Center for Cardiovascular Diseases and Sciences, Louisiana State University Health Sciences Center, Shreveport, LA 71130, USA.
Free Radic Biol Med. 2020 Dec;161:84-91. doi: 10.1016/j.freeradbiomed.2020.10.002. Epub 2020 Oct 7.
There is a marked variation in mortality risk associated with COVID-19 infection in the general population. Low socioeconomic status and other social determinants have been discussed as possible causes for the higher burden in African American communities compared with white communities. Beyond the social determinants, the biochemical mechanism that predisposes individual subjects or communities to the development of excess and serious complications associated with COVID-19 infection is not clear. Virus infection triggers massive ROS production and oxidative damage. Glutathione (GSH) is essential and protects the body from the harmful effects of oxidative damage from excess reactive oxygen radicals. GSH is also required to maintain the VD-metabolism genes and circulating levels of 25-hydroxyvitamin D (25(OH)VD). Glucose-6-phosphate dehydrogenase (G6PD) is necessary to prevent the exhaustion and depletion of cellular GSH. X-linked genetic G6PD deficiency is common in the AA population and predominantly in males. Acquired deficiency of G6PD has been widely reported in subjects with conditions of obesity and diabetes. This suggests that individuals with G6PD deficiency are vulnerable to excess oxidative stress and at a higher risk for inadequacy or deficiency of 25(OH)VD, leaving the body unable to protect its 'oxidative immune-metabolic' physiological functions from the insults of COVID-19. An association between subclinical interstitial lung disease with 25(OH)VD deficiencies and GSH deficiencies has been previously reported. We hypothesize that the overproduction of ROS and excess oxidative damage is responsible for the impaired immunity, secretion of the cytokine storm, and onset of pulmonary dysfunction in response to the COVID-19 infection. The co-optimization of impaired glutathione redox status and excess 25(OH)VD deficiencies has the potential to reduce oxidative stress, boost immunity, and reduce the adverse clinical effects of COVID-19 infection in the AA population.
普通人群中,COVID-19 感染导致的死亡率存在明显差异。低社会经济地位和其他社会决定因素被认为是导致非裔美国人社区比白人社区负担更重的可能原因。除了社会决定因素外,导致个体或社区易患 COVID-19 感染相关过度和严重并发症的生化机制尚不清楚。病毒感染会引发大量 ROS 产生和氧化损伤。谷胱甘肽 (GSH) 是必不可少的,可保护身体免受过量活性氧自由基引起的氧化损伤的有害影响。GSH 还需要维持 VD 代谢基因和循环 25-羟维生素 D(25(OH)VD)水平。葡萄糖-6-磷酸脱氢酶 (G6PD) 是防止细胞内 GSH 耗尽和枯竭所必需的。X 连锁遗传 G6PD 缺乏在非裔美国人中很常见,主要在男性中。已广泛报道,肥胖和糖尿病患者中存在 G6PD 获得性缺乏。这表明 G6PD 缺乏的个体易受过度氧化应激影响,25(OH)VD 不足或缺乏的风险更高,使身体无法保护其“氧化免疫代谢”生理功能免受 COVID-19 的侵害。先前有报道称,亚临床间质性肺病与 25(OH)VD 缺乏和 GSH 缺乏之间存在关联。我们假设,ROS 过度产生和过量氧化损伤是导致免疫受损、细胞因子风暴分泌以及对 COVID-19 感染发生肺功能障碍的原因。受损谷胱甘肽氧化还原状态和过量 25(OH)VD 缺乏的共同优化有可能降低氧化应激、增强免疫力,并降低非裔美国人 COVID-19 感染的不良临床效果。
Zotero 插件
