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左西孟旦与新型冠状病毒肺炎:从高血压到炎症反应

Clevidipine and COVID 19: From Hypertension to Inflammatory Response.

作者信息

Guerrero Orriach Jose Luis, Quesada Muñoz Guillermo

机构信息

Institute of Biomedical Research in Malaga, Malaga, Spain.

Department of Anesthesiology, Virgen de la Victoria University Hospital, Malaga, Spain.

出版信息

J Inflamm Res. 2022 Apr 13;15:2383-2386. doi: 10.2147/JIR.S350822. eCollection 2022.

Abstract

Globally, more than 4 million have died from COVID-19, World Health Organization (WHO) to declare COVID-19 a pandemic. The COVID 19 pathology, produced by SARS-COV2, a virus from the coronavirus family, emerged at the end of 2019. The majority of cases usually have a mild or moderate form, characterized by fever, cough, intense asthenia and multiple symptoms derived from the initial replicative effect and subsequent hyperimmune effect. Severe cases present with Acute Respiratory Distress Syndrome (ARDS), due to pneumonia with bilateral involvement, which lead to hospital admission of patients and the need for admission to intensive care units (ICU) of approximately 10‒20%. According to the different series; the mortality of the condition once the patient is admitted to the ICU is close to 35‒45%. Currently, more than 4 million people have died in the world due to this pathology. The volume of infections generated the declaration by the World Health Organization (WHO) of the pandemic situation. Factors associated with a higher risk of progression into severe disease include age and comorbidities, especially systemic arterial hypertension due to its high incidence in the general population. Clevidipine can be rapidly and effectively adjusted to the clinical status of the patient, since it can be withdrawn and its effects reversed in just a few minutes, and contains high concentrations of lipids, and it could reduce the inflammatory response induced by SARS-COV2, which is key to progression into severe disease. However, its application in pro-inflammatory settings has not yet been explored, although it must play a key role in inflammation as a scavenger molecule.

摘要

全球范围内,已有超过400万人死于新冠病毒,世界卫生组织(WHO)宣布新冠疫情为大流行。2019年末出现了由冠状病毒家族中的一种病毒——严重急性呼吸综合征冠状病毒2(SARS-CoV-2)引发的新冠病毒病理学。大多数病例通常为轻症或中症,表现为发热、咳嗽、极度乏力以及由初始复制效应和随后的高免疫效应产生的多种症状。重症病例会出现急性呼吸窘迫综合征(ARDS),这是由于双侧肺炎所致,约10%至20%的患者需要住院并入住重症监护病房(ICU)。根据不同系列的数据,患者一旦入住ICU,该病症的死亡率接近35%至45%。目前,全球已有超过400万人死于这种病理学疾病。感染数量促使世界卫生组织(WHO)宣布疫情大流行。与病情进展为重症风险较高相关的因素包括年龄和合并症,尤其是系统性动脉高血压,因为其在普通人群中发病率较高。克利夫地平可以迅速有效地根据患者的临床状况进行调整,因为它可以在几分钟内停药且效果逆转,并且含有高浓度脂质,它可能会降低由SARS-CoV-2诱导的炎症反应,而这是病情进展为重症的关键。然而,尽管它作为清除分子在炎症中必定发挥关键作用,但其在促炎环境中的应用尚未得到探索。

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