key: cord-267621-oc8bw7ft authors: Kevorkian, Jean-Philippe; Riveline, Jean-Pierre; Vandiedonck, Claire; Girard, Diane; Galland, Joris; Féron, Florine; Gautier, Jean-François; Mégarbane, Bruno title: Early short-course corticosteroids and furosemide combination to treat non-critically ill COVID-19 patients: An observational cohort study date: 2020-09-01 journal: J Infect DOI: 10.1016/j.jinf.2020.08.045 sha: doc_id: 267621 cord_uid: oc8bw7ft nan Availability of data and materials J.P.K. had full access to all of the data in the study and takes responsibility for the integrity of the data and the accuracy of the data analysis. All the authors agree to publish. None. The authors would like to thank Mrs. Alison Good (Scotland, UK) for her helpful review of the manuscript. Acute respiratory distress syndrome (ARDS), a life-threatening complication of coronavirus disease-2019 (COVID-19) is associated with elevated risk of intensive care unit (ICU) admission and death, predominantly in the elderlies. 1 Based on a randomized controlled trial, early dexamethasone was shown effective to reduce mechanical ventilation (MV) duration and overall mortality in moderate-to-severe ARDS patients independently of the etiology. 2 Therefore, since systemic and pulmonary inflammatory cytokine storm and fibrinous and organizing pneumonia are involved in COVID-19 ARDS, early corticosteroid administration has been considered as appropriate to avoid clinical deterioration and need for MV support. 3 However, cautious has been advised due to potential harmful effects of corticosteroids in viral pneumonia such as During COVID-19 epidemic, non-critically ill COVID-19 patients for whom intubation could be an option if worsening and those not eligible for intubation due to refusal, comorbidities and/or advanced age in the context of limited access to ICU beds were referred to our ward. All patients received standard care, i.e. oxygen with adapted flow to oximetry (including high-flow oxygen), antibiotics, anticoagulants, vasopressors and antiviral drugs if needed. Usual monitoring was provided including pulse oximetry, electrocardiogram, finger blood sugar and daily routine chemical tests. Decision to administer corticosteroids was left to physicians in charge due to uncertainties regarding the benefit/risk balance of their use in non-critically ill COVID-19 patients. 5 Interestingly, because pulmonary edema could worsen hypoxemia in patients presenting cardiovascular co-morbidities and/or cardiac involvement in COVID-19 at risk of fluid retention, we decided to co-administer furosemide systematically to corticosteroid-treated patients, with a rationale similar to that of conservative fluid management in ARDS patients. 5 Therefore, to address the effectiveness of early short-course corticosteroid/furosemide treatment in the non-critically ill COVID-19 patient, we designed a retrospective observational cohort study. All successive COVID-19 patients with pneumonia requiring oxygen admitted to our non-critical medical ward from 03/11/2020 to 04/27/2020 were included. Patients who received intravenous or oral corticosteroids plus furosemide for at least once daily three consecutive days were compared to those who did not (usual care group). The primary composite endpoint was invasive MV requirement (corresponding to care escalation from ward to ICU) or 28-day mortality. Data are expressed as median [percentiles 25 th -75 th ] or percentages. Univariate comparisons were performed using Mann-Whitney or Fisher exact tests, as appropriate. A multivariate logistic regression model to explain the outcome was tested with the corticosteroid/furosemide treatment as explanatory variable and adjustment for independent covariates (gender, age, body-mass index and comorbidities). Odds ratios (OR) and their 95%-confidence intervals were determined. P-values ≤0.05 were considered significant. Analyses were preformed using the R3.6 environment. whereas ninety-three patients did not. Noteworthy, 14/24 control patients (58%) at risk of cardiogenic pulmonary edema (serum brain natriuretic peptide (BNP) ≥100ng/mL) received furosemide without corticosteroids. In the corticosteroid/furosemide treatment group, incidence of invasive MV or death given once daily for up to ten days reduced 28-day mortality by one-third among mechanically ventilated COVID-19 patients and by one-fifth among patients treated with oxygen, while no benefit was observed in patients not receiving respiratory support at randomization. 7 In COVID-19 patients, viral shedding is elevated early then declines. Interestingly, low-dose corticosteroids were shown not to delay viral clearance, thus encouraging their safe prescription aiming to limit the excessive systemic and pulmonary inflammation involved in ventilation worsening. 8 However, the best dose regimen and timing of corticosteroids in COVID-19 remain undetermined. Various anti-inflammatory therapies including interleukin-1-receptor and interleukin-6 receptor antagonists were proposed to treat non-critically ill COVID-19 patients. 9 However, availability and cost-effectiveness of corticosteroids/furosemide (~60-fold less expensive than monoclonal antibodies) remain unbeatable. In aged COVID-19 patients with high proportion of cardiac comorbidities, mild-to-moderate pneumonia may be accompanied by some degree of acute heart failure and ischemia, 10 as evidenced in our series by elevations in cardiac biomarkers (BNP, 43 ng/l [16-135] and troponin, 12 ng/ml , respectively). Thus, furosemide administration when prescribing corticosteroids is pertinent, possibly beneficial to limit corticosteroid-induced retention and at least safe if adequately monitored. We observed increase in length of hospital stay, undoubtedly corresponding to increased survival resulting in prolonged medical care and rehabilitation. Our study limitations include the non-randomized single-center design and relatively small number of patients. The brief study duration determined by COVID-19 epidemic duration precluded a more elaborate design. Future trials should determine the most appropriate strategy offering the best risk/benefit ratio. To conclude, our data provides evidence that early short-course of corticosteroids combined to furosemide reduces the risk of invasive MV requirement or 28-day mortality in the non-critically ill COVID-19 patients. In comparison to the RECOVERY trial results, our findings highly suggest the benefits and safety of adding furosemide to corticosteroids, aiming to improve fluid management especially in the aged patients with comorbidities at risk of pulmonary edema (BNP >100ng/mL on admission). The authors declare that they have no competing interests. This study was part of the French COVID-19 cohort registry conducted by the REACTing consortium (REsearch and ACTion targeting emerging infectious diseases) and directed by INSERM (Institut national de la santé et de la recherche médicale) and ISARIC (International Severe Acute Respiratory and Emerging Infection Consortium). Our institutional ethics committee approved the study (N°, IDRCB, 2020-A00256-33; CPP, 11-20 20.02.04.68737). Figure 1 . Impact of the corticosteroid/furosemide treatment in the different patient subgroups defined according to age (using the median value as threshold), gender, presence of diabetes mellitus, serum brain natriuretic peptide (BNP; threshold at 100 ng/mL) and troponin levels (threshold at 16 ng/mL). Odds ratio (OR) and their 95%-confidence intervals were determined. 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