Circulating ACE2 level and zinc/albumin ratio as potential biomarkers for a precision medicine approach to COVID-19

Q1 Biochemistry, Genetics and Molecular Biology Advances in biological regulation Pub Date : 2023-08-01 DOI:10.1016/j.jbior.2023.100973
Serena Benedetti , Davide Sisti , Daniela Vandini , Simone Barocci , Maurizio Sudano , Eugenio Carlotti , Jade Lee Lee Teng , Loris Zamai
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引用次数: 1

Abstract

Highly mutable influenza is successfully countered based on individual susceptibility and similar precision-like medicine approach should be effective against SARS-COV-2. Among predictive markers to bring precision medicine to COVID-19, circulating ACE2 has potential features being upregulated in both severe COVID-19 and predisposing comorbidities. Spike SARS-CoVs were shown to induce ADAM17-mediated shedding of enzymatic active ACE2, thus accounting for its increased activity that has also been suggested to induce positive feedback loops leading to COVID-19-like manifestations. For this reason, pre-existing ACE2 activity and inhibition of ACE2/ADAM17 zinc-metalloproteases through zinc chelating agents have been proposed to predict COVID-19 outcome before infection and to protect from COVID-19, respectively. Since most diagnostic laboratories are not equipped for enzymatic activity determination, other potential predictive markers of disease progression exploitable by diagnostic laboratories were explored.

Concentrations of circulating albumin, zinc, ACE2 protein and its activity were investigated in healthy, diabetic (COVID-19-susceptible) and SARS-CoV-2-negative COVID-19 individuals.

ACE2 both protein levels and activity significantly increased in COVID-19 and diabetic patients. Abnormal high levels of ACE2 characterised a subgroup (16–19%) of diabetics, while COVID-19 patients were characterised by significantly higher zinc/albumin ratios, pointing to a relative increase of albumin-unbound zinc species, such as free zinc ones.

Data on circulating ACE2 levels are in line with the hypothesis that they can drive susceptibility to COVID-19 and elevated zinc/albumin ratios support the therapeutic use of zinc chelating inhibitors of ACE2/ADAM17 zinc-metalloproteases in a targeted therapy for COVID-19.

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循环ACE2水平和锌/白蛋白比率作为新冠肺炎精准医学方法的潜在生物标志物。
高度变异性流感是基于个体易感性成功对抗的,类似精准药物的方法应该对严重急性呼吸系统综合征冠状病毒2型有效。在为新冠肺炎带来精准医疗的预测标志物中,循环ACE2具有在严重新冠肺炎和易患合并症中上调的潜在特征。尖峰型SARS-CoVs显示可诱导ADAM17介导的酶活性ACE2脱落,从而解释其活性增加的原因,这也被认为可诱导导致COVID-19样表现的正反馈回路。出于这个原因,已经提出了预先存在的ACE2活性和通过锌螯合剂抑制ACE2/ADAM17锌金属蛋白酶,以分别预测感染前的新冠肺炎结果和保护免受新冠肺炎的影响。由于大多数诊断实验室不具备酶活性测定的设备,因此对诊断实验室可利用的其他潜在疾病进展预测标志物进行了探索。研究了健康、糖尿病(COVID-19敏感)和SARS-CoV-2阴性COVID-19]个体的循环白蛋白、锌、ACE2蛋白浓度及其活性。新冠肺炎和糖尿病患者的ACE2蛋白水平和活性均显著升高。ACE2的异常高水平是糖尿病亚组(16-19%)的特征,而新冠肺炎患者的特征是锌/白蛋白比率显著较高,这表明未结合白蛋白的锌物种(如游离锌)相对增加。关于循环ACE2水平的数据与以下假设一致,即它们可以驱动对新冠肺炎的易感性,并且锌/白蛋白比率升高,这支持ACE2/ADAM17锌金属蛋白酶的锌螯合抑制剂在新冠肺炎靶向治疗中的治疗用途。
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来源期刊
Advances in biological regulation
Advances in biological regulation Biochemistry, Genetics and Molecular Biology-Molecular Medicine
CiteScore
8.90
自引率
0.00%
发文量
41
审稿时长
17 days
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