key: cord-261315-n8tnistv authors: Palomar‐Lever, Andres; Barraza, Gustavo; Galicia‐Alba, Julieta; Echeverri‐Bolaños, Melissa; Escarria‐Panesso, Robert; Padua‐Barrios, Jorge; Halabe‐Cherem, Jose; Hernandez‐Molina, Gabriela; Chargoy‐Loustaunau, Talia Nila; Kimura‐Hayama, Eric title: Hepatic steatosis as an independent risk factor for severe disease in patients with COVID‐19: A computed tomography study date: 2020-08-04 journal: JGH Open DOI: 10.1002/jgh3.12395 sha: doc_id: 261315 cord_uid: n8tnistv BACKGROUND AND AIM: Hepatic steatosis (HS) is associated with diabetes, hypertension, and obesity, comorbidities recently related to COVID‐19 severity. Here, we assessed if tomographic HS is also a risk factor for severe COVID‐19 pneumonia. METHODS: We included 213 patients with a positive real time polymerase chain reaction (RT‐PCR) test and chest computed tomography (CT) from an out‐hospital facility and a hospital. We obtained information on demographics; weight; height; smoking history; diabetes; hypertension; and cardiovascular, lung, and renal disease. Two radiologists scored the CO‐RADs system (COVID‐19 Reporting and Data System) (1 = normal, 2 = inconsistent, 3–4 = indeterminate, and 5 = typical findings) and the chest CT severity index (≥20 of 40 was considered severe disease). They evaluated the liver‐to‐spleen ratio (CT(L/S)) and defined tomographic steatosis as a CT(L/S) index ≤0.9. We used descriptive statistics, χ(2) and t student tests, logistic regression, and reported odds ratio (OR) with 95% confidence interval (CI). RESULTS: Of the patients, 61% were men, with a mean age of 51.2 years, 48.3% were CO‐RADs 1 and 51.7% CO‐RADs 2–5. Severe tomographic disease was present in 103 patients (48.4%), all CO‐RADs 5. This group was older; mostly men; and with a higher prevalence of obesity, hypertension, diabetes, and HS (69.9 vs 29%). On multivariate analysis, age (OR 1.058, 95% CI 1.03–1.086, P < 0.0001), male gender (OR 1.9, 95% CI 1.03–3.8, P = 0.04), and HS (OR 4.9, 95% CI 2.4–9.7, P < 0.0001) remained associated. CONCLUSION: HS was independently associated with severe COVID pneumonia. The physiopathological explanation of this finding remains to be elucidated. CT(L/S) should be routinely measured in thoracic CT scans in patients with COVID‐19 pneumonia. Ever since the first cases of the COVID-19 pandemic began to surface, it was recognized that certain groups were at an increased risk of complications from the viral infection. Risk factors associated with greater incidence of severe/critical illness and mortality are age, diabetes, obesity, hypertension, and metabolic syndrome, among others. [1] [2] [3] On the other hand, it is also well recognized that patients with some of these comorbidities, mainly type 2 diabetes and obesity, are at higher risk for nonalcoholic fatty liver disease (NAFLD), recently renamed metabolic fatty liver disease (MAFLD), which at the same time may worsen these disorders [4] [5] [6] [7] and which has been implicated in the inflammatory response (increased neutrophil-to-lymphocyte ratio [NLR]) with poorer outcomes in patients with COVID-19. 8 Global prevalence of NAFLD has increased in the past two decades, and it has been calculated to be present in up to 24%. 7, 9 Similarly, the estimated prevalence of NAFLD in Mexico and other regions of Latin America is around 20-29.9% and 30.4% respectively. 5 NAFLD is a complex entity with hepatic and extrahepatic pathophysiological and clinical manifestations, which finally result in ectopic deposits of fatty substrates in the liver, with a spectrum ranging from simple hepatic steatosis (HS) without inflammation to steatohepatitis, advanced fibrosis, and cirrhosis. 7 Imaging plays a role in its assessment, and nonenhanced computed tomography (CT) has proven to be a useful and accurate noninvasive method for diagnosing HS and quantifying the severity of liver fat. [10] [11] This is because HS reduces attenuation of the liver, manifesting as a less dense liver parenchyma than expected, which is quantified in Hounsfield Units (HU). In contrast, as the spleen is devoid of fat, it can be used as an internal control, and several methods have shown good correlation to macrovesicular steatosis on biopsy, such as liver attenuation index and liver-to-spleen ratio (CT L/S ), and have been used as markers of HS. 12 Although CT is not accurate in assessing milder forms of HS (≤5% of fat content), it is a reliable method with high specificity in the diagnosis of moderate to severe HS (≥20% of fat infiltration). 9, 13 On the other hand, chest CT scans are useful in different scenarios of COVID-19 (i.e. diagnosis and prognosis). 14 Pulmonary involvement is assessed by the chest CT severity score. This score showed a correlation with other paraclinical and clinical scores, including a respiratory rate ≥30/min, resting blood oxygen saturation ≤93%, and partial pressure of arterial blood oxygen (PaO 2 )/oxygen concentration (FiO 2 ) ≤300 mmHg. Indeed, with a cut-off value of ≥19.5/40, it has a sensitivity of 83.3% and a specificity of 94% in the identification of severe infection and an NPV of 96.3% to rule out severe forms. 15 A chest CT severity score above this threshold correlates with parameters of ventilatory impairment (mechanical ventilation risk, respiratory rate, and hypoxemia) and adverse inflammatory response (neutrophilia, lymphopenia, hypersensitive CRP, and procalcitonin). 15 During the CT evaluation of patients with COVID-19 pneumonia, the CT scan volume routinely includes the upper abdomen, and thus, most of the liver and spleen are visualized. Therefore, HS can be assessed in the same dataset. Due to the high worldwide prevalence of HS and its relationship with many disorders associated with the risk of COVID-19 infection, we hypothesize that tomographic liver steatosis could represent an additional independent risk factor for severe SARS-CoV-2 infection according to the CT severity score definition. From 16 March 2020 to 26 May 2020, we conducted a transversal study including 213 consecutive patients from two different institutions, an out-hospital facility (n = 143) and a hospital (n = 70). Inclusion criteria were patients with a positive real time polymerase chain reaction (RT-PCR) test (Extraction kit Pur-eDireX, Bio-Helix, Keelung City, Taiwan) for COVID-19 obtained from a nasopharyngeal and oropharyngeal swab and from whom a chest CT scan was obtained. Clinical records from patients with COVID-19 were reviewed by two third-year radiology residents (Melissa Echeverri-Bolaños and Robert Escarria-Panesso). Data collection included age, gender, weight and height, body mass index (BMI), smoking history (including current and past smokers), and comorbidities (diabetes, hypertension, cardiovascular disease, lung disease, and renal disease). Local Medical Ethics Committee Approval was obtained prior to the study, and informed consent was waived. CT technique and postprocessing. Patients were scanned in two different commercial CT systems of 16-slices (Somatom Sensation 16, Siemens Healthinneers, Erlangen, Germany) and 512-slices (Revolution CT, GE Medical Systems, Milwaukee, WI, USA) with a kV of 100-120, 200-300 mA with automated current modulation, a pitch factor of 1.375, and X-ray rotation speed of 0.5 s in a single breathold at full inspiration. The tube parameters were selected at radiologist discretion (Eric Kimura-Hayama and Julieta Galicia-Alba). Images were reconstructed with a matrix of 512 × 512, a slice thickness of 0.6-1.25 mm with an increment of 0.6-1.25 mm, and a Lung or B46f kernel. The dataset was analyzed in a dedicated workstation (AW 4.7 GE Medical Systems or AW Server GE Medical Systems) by two different body-imaging radiologists with 7 years of experience (Julieta Galicia-Alba and Talia Nila Chargoy-Loustaunau), and final scores were determined by consensus when discrepancy was noted. CT interpretation and analyses included identification of areas of ground-glass opacities, crazy-paving pattern (i.e. ground-glass opacities with interlobular septal thickening), consolidations, and cicatricial bands according to the standard nomenclature of Fleischner Society, 16 and outcomes were classified according to the time course into four categories as previously described by Pan et al. 17 In addition, the presence of air bronchogram, inverse halo or atoll sign, cardiac enlargement, dilatation of main pulmonary artery, mediastinal lymph node enlargement, tree-in-bud nodules, coronary artery calcification, and pleural effusion was also recorded. CT findings were classified into five categories according to the RSNA Expert Consensus criteria, 18 and the CO-RADs (COVID-19 Reporting and Data System) system from the COVID-19 Working Group of the Dutch Radiological Society. 19 In these scoring systems, CT findings are classified from normal or inconsistent findings to typical findings of COVID-19 pneumonia. In addition, the CO-RADs scoring system includes a sixth category for patients with a positive RT-PCR test. According to this, all patients in our study group were categorized as CO-RADs 6. Estimation of pulmonary involvement was obtained through calculation of the chest CT severity index according to the original description of Yang et al. 15 In summary, lungs are divided into 20 segments according to the Boyden bronchial segmentation: 10 segments in the right lung and 10 in the left. If the segment was normal, it was scored with 0, 1 if the abnormal finding represented less than 50% of the segment, or 2 if it involved more than 50% of the segmental area. The total CT score was the sum of the individual segmental scores and ranged from 0 (no involvement) to 40 (i.e. all 20 segments are involved in more than 50% of their extension). A CT score of ≥20/40 was considered to demonstrate severe disease and has been shown to correlate with worse outcomes. 15 Liver density was measured by averaging the HU of a 1.5 cm 2 circular region of interest (ROI) in four different areas of both lobes, each separated by the hepatic veins. Spleen density was obtained from a 1.5-cm 2 ROI placed in the parenchyma. In both cases, the ROIs avoided areas of high density (e.g. calcifications) or low density due to vascular structures, cysts, or vessel entry points at hila. The liver-to-spleen ratio (CT L/S ) was calculated, and steatosis was defined if the CT L/S index was ≤0.9. [20] [21] Statistical analysis. Quantitative data are presented as means and standard deviations, and qualitative data are presented Steatosis a severe COVID-19 risk factor A Palomar-Lever et al. as percentages. We used t-student test and Chi-square test according to the variable distribution. We performed logistic regression analysis and reported odds ratios (OR) with 95% confidence interval (CI). P ≤ 0.05 was indicative of a statistically significant difference. Statistical analyses were performed using software SPSS, version 24 (IBM, New York, NY, USA). Table 1 depicts baseline characteristics of the 213 patients included. There were 131 men and 82 women, with an average age of 51.2 years (±14.8 years). A total of 108 patients (50.7%) had at least one of the studied comorbidities, with overweight being the most prevalent in 36.6%, followed by obesity in 28.6% and hypertension (26.7%). We observed tomographic steatosis in 104 patients (48.8%). Table 1 also shows all the tomographic findings. All patients had the CT L/S ratio available. CT showed normal findings in 48.3% of cases (i.e. CO-RADs 1) and was abnormal in 51.7% of patients (i.e. CO-RADs 2-5). CO-RADs categories 4 and 5 with high and very high probability of viral pneumonia comprised 48.8% of all abnormal scans (4.2 and 44.6%, respectively), and nearly half of all patients had severe disease (i.e. CT score ≥ 20) (48.4%), all of them CO-RADs 5. Nearly two thirds of patients were in tomographic phases 1 and 3, where ground-glass opacities and consolidation are predominant, respectively. When comparing the group with severe tomographic disease (CT score ≥ 20) versus the group with nonsevere pneumonia, the former had a higher prevalence of male gender (71.6 vs 52.3%), obesity (39.8 vs 18.1%), hypertension (40.7 vs 13.6%), diabetes (29.1 vs 12.7%), and HS (69.9 vs 29%); they were also older ( Table 2 and Fig. 1 ). The remaining comorbidities were similar between the groups. At the logistic regression analysis, the only variables that remained associated with CT lung severity ≥20/40 were age (OR 1.058, 95% CI 1.03-1.086, P < 0.0001), male gender (OR 1.9, 95% CI 1.03-3.8, P = 0.04), and HS (OR 4.9, 95% CI 2.4-9.7, P < 0.0001). In another logistic regression model that considered only the variables age, male gender, and a combined variable of obesity/HS, we found similar results for age and gender, whereas the combination of both obesity and HS showed an OR of 5.9 (95% CI 2.6-13.7, P < 0.0001). Here, we evaluated the presence of tomographic HS and its association with the chest CT severity score, a tool that correlates with ventilatory impairment and an intense adverse inflammatory response among patients with SARs-COVID19 pneumonia. 15 We found that HS, defined as the CT L/S index ≤0.9, 20-21 was significantly associated with severe pneumonia with an OR of 4.9. Interestingly, both NAFLD and COVID-19 infection are more prevalent in men and are linked to worst clinical outcomes (case fatality and cirrhosis progression). [22] [23] Furthermore, HS has been also associated with some recognized COVID-19 risk factors such as hypertension, obesity, and diabetes. Despite these facts, our results remained significant after adjusting for likely comorbidities, including obesity and diabetes, as well as for age and gender. This is the first report that considers CT data analysis for both detection of HS and CT severity of COVID-19 pneumonia. In a previous report in Asian populations by Zheng et al., authors suggested that the risk of obesity to COVID-19 severity is significantly greater in those with fatty liver disease. 24 Unlike those results, after adjustment was performed, obesity did not showed a significant association with severe disease, and only age and HS remained significant. This might be the result of a different definition of obesity (BMI ≥25 kg/m 2 in Zheng et al. vs ≥30 kg/ m 2 in our study) due to different ethnicities. According to a study of overweight and obesity in Asian American men, this population may develop health complications at lower BMIs than other racial/ethnic groups and tend to have higher percentages of body fat at lower BMIs. 25 Indeed, BMI cut-off points for overweight and obesity in Asians are lowered to 23-27.4 kg/m 2 and ≥27.5 kg/m 2 , respectively, compared to standard BMI cut-off points for overweight (25-29.9 kg/m 2 ) and obesity (≥30 kg/m 2 ) in other races. 26 However, according to our results, combined obesity/HS resulted in a significant association with severe disease with an OR 6.49, which suggests a synergic interaction between them. In accordance with these findings, Ji et al. also reported a higher risk of progression to severe COVID-19 and longer viral shedding time in patients with NAFLD. 27 The underlying pathophysiologic mechanisms that explain this association are unknown and warrant future research. However, there is evidence of increased hepatic and circulating interleukin-6 levels in patients with NAFLD, [28] [29] which might have an additive/synergistic role in promoting greater severity of COVID-19. Obesity and NAFLD have been associated with increased production of pro-inflammatory cytokines such as TNF-α by adipose cells and Kupffer cells. 27 In a recent metaanalysis, a higher NLR, a well-known marker of systemic inflammation, was significantly associated with poorer outcomes in patients with COVID-19 infection. 30 Also in patients with NAFLD, there is a significant association between this ratio and liver fibrosis severity. Moreover, it has been recently demonstrated that this association contributes to the COVID-19-induced inflammatory storm, carrying a greater risk for severe SARS-CoV-2 illness. 8 In addition, in patients with COVID-19 infection, liver injury ranks second after lung injury. 31 This damage might be associated with overactivation of Kupffer cells, a virally induced cytotoxic T cell response and induction of a dysregulated innate immune response. 32 Furthermore, postmortem liver biopsies in these patients have shown microvesicular steatosis. 27 Our study has some limitations. First, the decision to perform a chest CT relied on the referring physician. Thus, a selection bias might be present as milder cases might not be included, hampering the validity of our results in this subgroup. Second, no histological or liver function tests are available in order to rule out the presence of other forms of NAFLD (i.e. cirrhosis and steatohepatitis), which have been implicated in poorer outcomes in this group of patients, 33 and it is well recognized that the accuracy of CT for detecting liver steatosis depends on the degree of fatty infiltration. The area under the curve (AUCs) of HS defined by CT L/S in diagnosis of ≥5% and ≥30% HS are 0.732 and 0.925, respectively. 20 Thus, according to our results, the presence of HS as a marker of increased risk of CT severity score may be only applied to patients with moderate to severe HS (≥30%). However, further studies are needed to know whether or not milder forms of fatty infiltration leads to an increased risk of severe forms of COVID-19 in this population. In conclusion, our data demonstrated that the risk of COVID-19 pneumonia severity measured with the chest CT severity score is greater in those with HS. CT L/S should be routinely measured using thoracic CT scans in patients with COVID-19 pneumonia. 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