key: cord-0730451-6m1f4q5r authors: Brahier, Thomas; Meuwly, Jean-Yves; Pantet, Olivier; Brochu Vez, Marie-Josée; Gerhard Donnet, Hélène; Hartley, Mary-Anne; Hugli, Olivier; Boillat-Blanco, Noémie title: Lung ultrasonography for risk stratification in patients with COVID-19: a prospective observational cohort study date: 2020-09-17 journal: Clin Infect Dis DOI: 10.1093/cid/ciaa1408 sha: 5b0277f0efa6b0ed8316b6dc80e0d05f7824f72d doc_id: 730451 cord_uid: 6m1f4q5r BACKGROUND: Point-of-care lung ultrasound (LUS) is a promising pragmatic risk stratification tool in COVID-19. This study describes and compares LUS characteristics between patients with different clinical outcomes METHODS: Prospective observational study of PCR-confirmed COVID-19 adults with symptoms of lower respiratory tract infection in the emergency department (ED) of Lausanne University Hospital. A trained physician recorded LUS images using a standardized protocol. Two experts reviewed images blinded to patient outcome. We describe and compare early LUS findings (acquired within 24hours of presentation to the ED) between patient groups based on their outcome at 7 days after inclusion: 1) outpatients, 2) hospitalised and 3) intubated/death. Normalized LUS score was used to discriminate between groups RESULTS: Between March 6 and April 3 2020, we included 80 patients (17 outpatients, 42 hospitalized and 21 intubated/dead). 73 patients (91%) had abnormal LUS (70% outpatients, 95% hospitalised and 100% intubated/death; p=0.003). The proportion of involved zones was lower in outpatients compared with other groups (median 30% [IQR 0-40%], 44% [31-70%] and 70% [50-88%], p<0.001). Predominant abnormal patterns were bilateral and multifocal spread thickening of the pleura with pleural line irregularities (70%), confluent B lines (60%) and pathologic B lines (50%). Posterior inferior zones were more often affected. Median normalized LUS score had a good level of discrimination between outpatients and others with area under the ROC of 0.80 (95% CI 0.68-0.92) CONCLUSIONS: Systematic LUS has potential as a reliable, cheap and easy-to-use triage tool for the early risk stratification in COVID-19 patients presenting in EDs The Coronavirus disease pandemic has overwhelmed the health systems in several high-income settings (1) , and is now spreading in the low-income countries. There is a critical need for accessible and low cost methods to stratify risk for evidence-based resource allocation (2). While the majority of COVID-19 patients have a paucisymptomatic or asymptomatic course, some may rapidly deteriorate leading to hospitalisation and the need for respiratory support. It has been suggested that early identification of patients at high risk of respiratory compromise is associated with lower mortality (3) . Several studies have shown the predictive value of CT imaging, where the extent and patterns of lung involvement correlated well with severity of COVID-19 on admission to hospital. Other studies have described a progression of lung anomalies on consecutive chest CTs during the course of the disease, with rapid evolution from focal unilateral to diffuse bilateral ground-glass opacities and finally, consolidation (7) . However, CT imaging has important limitations in triaging patients during the context of COVID-19, not only due to their limited availability, high cost and exposure to radiation, but more critically, due to their immobile nature, thus necessitating the movement of infectious patients (8) . Point-of-care ultrasound applied to lung is a promising alternative diagnostic tool, which can shorten time-to-diagnosis for the aetiology of acute dyspnoea, as well as stratify severity in the Emergency Department (ED) (9) . It is widely used in routine practice of Swiss EDs, can be performed at the bedside without radiation exposure and is easy-to-use in patients requiring protective isolation. So far, the use of lung ultrasonography (LUS) in COVID-19 has only been described in cohorts of severe hospitalised patients (10) (11) (12) (13) . However, it has already shown excellent performance to detect non-COVID-19 pneumonia, compared to CT as a reference standard (14) , and matches the discriminative power of CT in patients with acute respiratory distress syndrome (ARDS) (15) . A c c e p t e d M a n u s c r i p t LUS has potential in the pragmatic triage of COVID-19 patients especially in low-resource settings. This study aims to describe LUS characteristics in a prospective cohort of patients with COVID-19 and explore their predictive capacity for risk stratification. This study is nested in a prospective cohort study of patients with lower respiratory tract infections, which started on February 6 th , 2020 in the ED of the Lausanne University Hospital, Switzerland. We prospectively screened consecutive adult patients (age ≥ 18 years) presenting in the ED with an acute lower respiratory tract infection (cough, sputum, dyspnoea or chest pain for <21 days) (16) . Patients with COVID-19 confirmed by real time polymerase chain reaction (RT-PCR) for SARS-CoV-2 in a nasopharyngeal swab were included in this study. Patients were excluded if LUS could not be performed within 24 hours of admission or if the patient was receiving therapeutic prone ventilation before the LUS. The study team collected patient's data using a standardized electronic case report form in REDCap® (Research Electronic Data Capture). We assessed day-7 outcome by checking the electronic health record and we classified patients in three groups: group 1 (outpatients: absence of admission within 7 days of inclusion); group 2 (hospital admission within 7 days of inclusion); group 3 (intubation and/or death within 7 days of inclusion). A c c e p t e d M a n u s c r i p t A trained physician (TB) in lung ultrasonography performed all LUS at inclusion in the ED. Acquisition was standardized according to the "10-zone method" (17, 18) . Two images (sagittal and transverse) and 5 second videos were systematically recorded in every zone with a Butterfly IQ TM , using the lung preset. The study physician (TB) and an expert radiologist (JYM) standardized the reporting of pathological LUS features based on COVID-19 patterns (Figure 1 ) (e- Figure 1 , e- Figure 2 and Video V1 in the online data supplement) (10, 19) . For every zone, the following patterns were reported: (1) normal appearance (A lines, < 3 B lines), (2) pathologic B lines (≥3 B lines), (3) confluent B lines, (4) thickening of the pleura with pleural line irregularities (subpleural consolidation < 1 cm) or (5) consolidation (≥ 1 cm). The presence of pleural effusion was also recorded. The LUS score, used as a correlate of loss of lung tissue aeration, as well as a normalized LUS score (nLUS score) corrected for the number of examined zone, were calculated in every patient (15, 19, 20) . Blinded to patient outcome, both physicians independently filled the standardized report. Discordance between the two readers was resolved by a third expert (OP). Supplementary table 1 shows the potential correlation of visible features between CT and LUS images based on physical explanations behind their generation in several retrospective human studies (11, (21) (22) (23) (24) an animal study (25) and biomedical analysis (26) . Differences between the three groups was evaluated by one-way ANOVA, Kruskal-Wallis or chi-squared test, as appropriate. A bilateral p value <0.05 was considered indicative of A c c e p t e d M a n u s c r i p t statistical significance. The kappa coefficient was calculated to measure the inter-rater agreement between the two LUS readers. The prognostic accuracy of the LUS score, the nLUS score and the proportion of LUS affected zones to predict outcome was assessed by calculating the area under the receiver operating characteristic curve (AUROC). We determined the optimal nLUS score cut-off by choosing the value with the best sensitivity and a specificity superior to 50%. Ethical approval was granted by the Swiss Ethics Committee of the canton of Vaud (CER-VD 2019-02283). Table 1 shows demographics, clinical characteristics and laboratory results of the study population by group. Overall, the mean age was 62 years (SD 17 years), and 34 (42%) patients were female. Outpatients were significantly younger than patients in the other two groups (mean of 51 years, p=0.002). At inclusion, the median duration of symptoms was 7 days (IQR 6-11) and not different between groups. The most common symptoms were cough (91%), fever (83%) and dyspnoea (75%). Dyspnoea occurred with increasing frequency across severity groups (p=0.014). Heart and respiratory rates were lower in outpatients compared with patients in the other two groups (median 78/min vs 91/min, p=0.002 and 20/min vs 24/min, p=0.002, respectively). Leukocyte count and C-reactive protein were significantly and gradually higher with increasing severity. Overall, eight patients (10%) had a CT scan and 95% had a chest X-ray. X-rays were abnormal in 76% and outpatients had fewer abnormal X-rays than patients in the other two groups (38.5% versus 84%, p<0.001). Among 10 patients with a normal chest X-ray (9 in the hospitalized group, one in the intubated/death group), 9 had LUS abnormalities. At ED inclusion, 73 patients (91%) had an abnormal LUS, the proportion of which increased progressively across severity groups to reach 100% in intubated/death patients (p=0.001) ( Table 2) . A total of 735 lung zones were explored with LUS in all patients. A median of 10 zones were recorded for each patient (IQR 9, 10); 10 zones (IQR 10, 10) in outpatients, 10 zones (IQR 9, With increased severity, lung anomalies affected both apical and basal lung regions (e- Figure 4 in the online data supplement) and were more bilaterally distributed. Figure 3 ). In terms of the predominant abnormal LUS pattern, outpatients mostly had a "non-confluent B lines" pattern, while the other two groups more frequently presented with "thickening of the pleura with pleural line irregularities" pattern (e- Figure 5 in the online data supplement). While the patterns of "pathologic B lines" and "confluent B lines" were more commonly The median LUS score was 10 (IQR 5, 15) and the median nLUS score was 1.1 (IQR 0.5- The optimal nLUS score cut-off to differentiate between outpatients and admitted patients including those who were intubated or died was 0.6 (sensitivity 81%, specificity 59%, positive predictive value 88%, negative predictive value 45%, positive likelihood ratio 1.97, negative likelihood ratio 0.32). If this nLUS score had been used at the first ED visit, it would have correctly recommended primary hospitalisation for the three patients who were initially discharged (later returning for secondary hospitalization). The LUS score, the nLUS score and the proportion of affected zones had a poor level of discrimination between patients who died or were intubated and the other two groups. The two observers showed good reproducibility for all explored zones with a kappa of 0.74 based on the standardized US report. The reproducibility was excellent to differentiate normal and abnormal zones with a kappa of 0.90. Despite the potential of LUS as a cheap, portable and accessible point-of-care triage tool in acute respiratory disease (especially in low resource settings), a multinational consensus recently stated that the lack of studies limited specific recommendations for the management of COVID-19 patients (27) . Using a standardized approach in a prospective ED cohort of 80 patients, we described the characteristics of LUS findings in COVID-19 pneumonia. Most A c c e p t e d M a n u s c r i p t patients presented abnormal LUS with bilateral and multifocal involvement as previously shown in a large CT scan study (28) . The most common patterns seen on LUS in decreasing frequency were thickening of the pleura with pleural line irregularities, confluent B lines, pathologic B lines and rarely, consolidations and minor pleural effusions. Abnormalities affected all lung regions but were more frequent in posterior and inferior zones. LUS findings also evolved with increasing disease severity, both in anatomic scope (progressing from unilateral to bilateral and pan-lung involvement), and pathological type (progressing from the "non-confluent B lines" pattern to "irregular pleural thickening"). We also describe a risk gradient in LUS findings that can be summarised in a simple ordinal scoring system (LUS score) which was able to discriminate between outcome groups in ED A c c e p t e d M a n u s c r i p t triage. The LUS score can be used to quantify the loss of lung aeration and is thus useful for monitoring patients with ARDS. This simple LUS scoring method may help in assessing COVID-19 disease severity and support ED triage to decide on admission or close monitoring. Previous studies have evaluated the LUS score in COVID-19 patients. In the intensive care unit, the LUS score was higher in patients with refractory respiratory failure compared with others (31) . A good correlation existed between the LUS score and a CT scan severity score. Both scores correlated with clinical severity (21, 24). In our study, LUS score also increased progressively according to clinical severity. However, we did not have the power to predict intubation and/or death with a good accuracy. To our knowledge, our study is the first including the complete range of disease severity, i.e.outpatients and patients who were intubated or died. Our findings provide additional evidence that the LUS score could be used as a triage tool to decide on admission. The role of LUS to evaluate several respiratory diseases such as pneumonia and ARDS has been widely documented (14, 15) . LUS has several advantages over chest CT such as its ease-of-use at point-of-care, low cost, absence of radiation, reproducibility and a reduced risk of nosocomial infection through its portability (reducing patient transport to imaging suites and lengthy disinfection protocol for the CT suite) (32, 33). LUS allows a rapid assessment of severity at presentation in the ED. This study also shows that physicians with basic training in US (1-day theoretical course and 20 supervised acquisitions) are able to identify pathology with excellent concordance compared with experts: a critical proof of concept for its rapid deployment in COVID-19 and for its general use in low resource settings. This study does not correlate LUS with chest CT imaging. However, current recommendations specify that CT imaging should not be used for screening and is rather reserved for hospitalised, symptomatic patients, with specific indications (34). Interestingly, two studies showed that the LUS and CT scan scores have good agreement in the assessment A c c e p t e d M a n u s c r i p t of clinical severity (21, 24). Excluding chest CT from the inclusion criteria eliminates a potential selection bias. On the other hand, we cannot propose a direct correlation between CT imaging and LUS. Acquisition of LUS is dependent on the accessibility of anatomic sites, which is sometimes challenging in respiratory patients unable to mobilise. Indeed, this study reported approximately 15% of missing values in posterior lung regions, which were mostly in severely ill patients. We mitigated this bias by normalising our score according to the number of available zones. Regardless the discriminatory power of the score reveals that the predictive capacity of accessible zones is already highly informative. Work is underway to identify the most informative zones and devise personalised imputations for such missing values. LUS image interpretation is operator dependant, which is a potential disadvantage of this technique. However, in our study, we found a good agreement between the two observers. Furthermore, using a standardized procedure and a pre-defined scoring method could minimize this limitation. In conclusion, LUS is a promising tool for early risk stratification in COVID-19. Lung involvement visualized with US correlates with disease severity and summarising this into a simple ordinal scoring system has potential to discriminate patients requiring hospitalisation in the ED and thus better allocate scarce resources. Work is ongoing to confirm these findings in a larger outpatient cohort. Glasgow coma scale < 15; n (%) 2 (2.6) 0 (0) 0 (0) 2 (10) 0.044 Leukocyte count, G/L; Median (IQR) 6.2 (4.9, 8.5) 5 (4.3, 6.0) 6.3 (5.0, 7.3) 8.9 (6.2, 10) <0.001 :m1090. 2. WHO. Home care for patients with COVID-19 presenting with mild symptoms and management of their contact. 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