Lactate Arterial-Central Venous Gradient among COVID-19 Patients in ICU: A Potential Tool in the Clinical Practice.

IF 1.8 Q3 CRITICAL CARE MEDICINE

Critical Care Research and Practice Pub Date : 2020-09-25 eCollection Date: 2020-01-01 DOI:10.1155/2020/4743904

Giuseppe Nardi, Gianfranco Sanson, Lucia Tassinari, Giovanna Guiotto, Antonella Potalivo, Jonathan Montomoli, Fernando Schiraldi

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引用次数: 12

Abstract

Objective: In physiological conditions, arterial blood lactate concentration is equal to or lower than central venous blood lactate concentration. A reversal in this rate (i.e., higher lactate concentration in central venous blood), which could reflect a derangement in the mitochondrial metabolism of lung cells induced by inflammation, has been previously reported in patients with ARDS but has been never explored in COVID-19 patients. The aim of this study was to explore if the COVID-19-induced lung cell damage was mirrored by an arterial lactatemia higher than the central venous one; then if the administration of anti-inflammatory therapy (i.e., canakinumab 300 mg subcutaneous) could normalize such abnormal lactate a-cv difference.

Methods: A prospective cohort study was conducted, started on March 25, 2020, for a duration of 10 days, enrolling 21 patients affected by severe COVID-19 pneumonia undergoing mechanical ventilation consecutively admitted to the ICU of the Rimini Hospital, Italy. Arterial and central venous blood samples were contemporarily collected to calculate the difference between arterial and central venous lactate (Delta a-cv lactate) concentrations within 24 h from tracheal intubation (T ₀) and 24 hours after canakinumab administration (T ₁).

Results: At T ₀, 19 of 21 (90.5%) patients showed a pathologic Delta a-cv lactate (median 0.15 mmol/L; IQR 0.07-0.25). In the 13 patients undergoing canakinumab administration, at T ₁, Delta a-cv lactate decreased in 92.3% of cases, the decrease being statistically significant (T ₀: median 0.24, IQR 0.09-0.31 mmol/L; T ₁: median -0.01, IQR -0.08-0.04 mmol/L; p=0.002).

Conclusion: A reversed Delta a-cv lactate might be interpreted as one of the effects of COVID-19-related cytokine storm, which could reflect a derangement in the mitochondrial metabolism of lung cells induced by severe inflammation or other uncoupling mediators. In addition, Delta a-cv lactate decrease might also reflect the anti-inflammatory activity of canakinumab. Our preliminary findings need to be confirmed by larger outcome studies.

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COVID-19 ICU患者乳酸动脉-中心静脉梯度:临床应用的潜在工具

目的:在生理条件下，动脉血乳酸浓度等于或低于中心静脉血乳酸浓度。这一比率的逆转(即中心静脉血乳酸浓度升高)可能反映炎症引起的肺细胞线粒体代谢紊乱，此前曾在ARDS患者中报道过，但从未在COVID-19患者中探讨过。本研究的目的是探讨covid -19诱导的肺细胞损伤是否反映为动脉乳酸血症高于中心静脉乳酸血症;然后，如果给予抗炎治疗(即皮下皮下canakinumab 300 mg)可以使这种异常的乳酸a-cv差异正常化。方法:采用前瞻性队列研究，于2020年3月25日开始，为期10天，纳入意大利里米尼医院ICU连续收治的21例机械通气重症COVID-19肺炎患者。同时收集动脉和中心静脉血样本，以计算气管插管后24小时(t0)和给药后24小时(t1)动脉和中心静脉乳酸(Delta a-cv乳酸)浓度的差异。结果:在t0时，21例患者中有19例(90.5%)显示病化性Delta a-cv乳酸(中位数0.15 mmol/L;差0.07 - -0.25)。在13例接受canakinumab治疗的患者中，在t1时，92.3%的病例的δ a-cv乳酸下降，下降具有统计学意义(t0:中位数0.24,IQR 0.09-0.31 mmol/L;t1:中位数-0.01,IQR -0.08-0.04 mmol/L;p = 0.002)。结论:Delta A -cv乳酸逆转可能是covid -19相关细胞因子风暴的影响之一，可能反映了严重炎症或其他解偶联介质诱导的肺细胞线粒体代谢紊乱。此外，δ a-cv乳酸降低可能也反映了canakinumab的抗炎活性。我们的初步发现需要更大规模的结果研究来证实。

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