key: cord-0985284-smcybi4a
authors: He, Guiqing; Wu, Jing; Huang, Jianping; Schieffelin, John S.; Dai, Jianyi; Gamber, Michelle; Hu, Xingzhong; Chen, Quelu; Si, Yang; Sun, Wenjie; Cai, Jing
title: Clinical features and viral RNA shedding of imported and local cases with COVID-19 in Wenzhou, China
date: 2021-03-19
journal: Medicine (Baltimore)
DOI: 10.1097/md.0000000000024826
sha: ccf2aeb8fe02ef3fa07706dfb5c68774046c3fe5
doc_id: 985284
cord_uid: smcybi4a

Wenzhou had the highest number of confirmed novel coronavirus 2019 (COVID-19) cases outside the Hubei province. The aim of this study was to identify the difference in clinical features and viral RNA shedding between the imported and local COVID-19 cases in Wenzhou. All patients with confirmed COVID-19 admitted to Wenzhou Sixth People's Hospital, Wenzhou Central Hospital Medical Group, from January 17 to February 11, 2020, were enrolled in this study. Data was analyzed and compared for the imported and local cases with regard to epidemiological, demographic, clinical, radiological features, and laboratory findings. Outcomes for the enrolled participants were followed up until May 7, 2020. Of the 136 cases, 50 were imported from Wuhan. The median age was 45 years and 73 (53.7%) were men. The most common symptoms at onset were fever (104 [76.5%]) and cough (85[62.5%]). Pleural effusion was more common among imported cases compared to local cases. The white blood cell count, neutrophil count, lymphocyte count and platelet count of the imported cases were significantly lower than those of the local cases, while the prothrombin time was significantly longer than that of the local cases. Severe and critically ill patients accounted for 15.4% and 2.9%, respectively. The median duration of SARS-CoV-2 RNA shedding from symptom onset was 26 days (IQR 17–32.3 days) and there were no significant differences in duration of viral RNA shedding between the two groups. The study findings suggest that imported cases from Wuhan were more likely to be severe compared to the local cases in Wenzhou. However, there was no difference between imported and local cases on the viral shedding among the COVID patients.

COVID-19 is a newly emerged infectious disease that began as an outbreak in Wuhan, China in December 2019. The cases are climbing steeply across the world, and as of June 2020, the global number of confirmed COVID-19 cases has reached 6,140,934. These confirmed cases spanned 216 countries, areas or territories and resulted in 373,548 deaths. [1] Global COVID-19 case fatality rates have varied from 0.06% in Qatar to 16 .25% in Belgium. [2] In China, the case fatality rate of COVID-19 in Wuhan was 4.9%, which is much higher than that of other provinces and territories in China (0.16%). [3] This difference could be partly explained by the limited available medical resources in Wuhan. Until now, most studies focused on the clinical features of cases from Wuhan. [4] [5] [6] Interestingly, patients outside Wuhan have shown different clinical symptoms at the time of onset, e.g 8% diarrhea, 34% headache, both of which are higher than those of Wuhan. [4, 7] The comparison of COVID-19 cases from Wuhan and outside Wuhan could contribute to a better understanding of the evolution of symptoms during the outbreak. Wenzhou, with a population of 8 million, has approximately 100 thousand people who routinely travel to Wuhan on business, and who also traveled home for the Chinese Lunar New Year before January 23, 2020. The distances between Wenzhou and Wuhan is about 900 km, and Wenzhou was the most affected city outside Hubei province with 504 confirmed cases. In the present study, we linked the clinical records with epidemiology data from hospitalized, confirmed cases of COVID-19 from Wenzhou to examine this relationship.

For this retrospective, single-center cohort study, all patients with confirmed COVID-19 admitted to Wenzhou Sixth People's Hospital, Wenzhou Central Hospital Medical Group from January 17 to February 11, 2020, were enrolled and followed until March 7, 2020. Wenzhou Sixth People's Hospital, Wenzhou Central Hospital Medical Group is a designated hospital specializing in infectious diseases and is responsible for the treatment of COVID-19 patients. All patients enrolled in this study were diagnosed based on WHO interim guidance for COVID-19. [8] 

We reviewed medical records, laboratory findings, and chest computed tomography (CT) for all patients with laboratory confirmed SARS-CoV-2 infection who were reported by the Center for Disease Control. Available RNA virologic data was used to estimate the duration of viral shedding. Clinical data was obtained from the hospital electronic medical record and directly communicated with patients or their families to verify these data and histories. Two researchers independently reviewed all data collection forms to double check the data collected.

In the present study, imported cases are defined as a patient who travelled to Wuhan in the two weeks before the onset of symptoms. Local cases are defined as patients with no travel history in the two weeks prior to symptom onset. Clinical classification of disease severity and discharge criteria were defined in accordance with Tentative Sixth Edition of Diagnosis and Treatment Plan Coronavirus Disease 2019 issued by the national health commission. [9] Acute respiratory distress syndrome (ARDS) was defined according to the Berlin definition. [10] Duration of viral shedding was defined as the interval from the date of symptom onset to the date when SARS-CoV-2 RNA was undetectable by RT-PCR of two consecutive nasopharyngeal swabs, or oropharyngeal swabs or sputum specimens (at least 24 h apart), without converting positive thereafter.

Definition of clinical classification of disease severity and discharge criteria are as follows:

Clinical classification 

Continuous variables were described as median and interquartile range (IQR) and compared with the Mann -Whitney U test. Categorical variables were described as number (%) and compared using x 2 test or Fisher's exact test between imported and local cases. Ranked data was used to compare between both groups with the non-parametric rank sum test. Statistical analyses were done using the SPSS software version 19.0 (IBM Corp, Armonk, NY), unless otherwise indicated. The curve of SARS-CoV-2 RNA conversion between imported and local cases was illustrated by GraphPad Prism 5.0 and tested by log-rank. A two-sided a of less than.05 was considered statistically significant. [8.1%] ). However, there were no significant differences between the two groups with respect to underlying diseases or smoking history ( Table 1 ). The most common initial symptoms at onset were respiratory in nature, which accounted for 86% of cases, and 5.9% of patients were asymptomatic ( Table 2 ). The most common symptoms at presentation were fever (104 [76.5%]), cough (85[62.5%]), and fatigue (34[25.0%]). However, a considerable proportion of patients presented initially with asymptomatic or atypical symptoms, such as diarrhea and nausea, vomiting, abdominal pain, hemoptysis, or anorexia. There were no significant differences in initial symptoms between groups, and there were no significant differences in vital signs (including heart rate, respiratory rate, systolic pressure, finger oxygen saturation) on admission between the two groups ( Table 2) .

Significant differences were noted in laboratory findings between the two groups (Table 3) , including lower mean white blood cell, neutrophil counts, lymphocyte and platelet counts, as well as longer prothrombin time among the imported cases. However, no significant differences were found in other laboratory parameters. Chest CT scans demonstrated bilateral involvement, ground glass opacity and consolidation in 85.3%, 91.9% and 61.0% of patients, respectively (Table 3 ; Fig. 1 refer to the CT image). Additionally, pleural effusions were noted in five (3.7%) patients of imported cases, but in none of the local cases. There was no difference in CT imaging between two groups, except for pleural effusion (P = .006).

Most cases were relatively mild, with mild type and moderate type accounting for 84.5% of the total cases. The severe type and critically ill type accounted for 15.4% and 2.9% respectively, with imported cases being more severe than local cases (Table 4 ). In fact, the imported cases were more likely to have severe or critical disease (26.0%), compared to the local cases (14.0%, P = .034) Common complications among the 136 patients included secondary infection (33 [24.3%]) and ARDS (4 [2.9%]). No significant differences in complications were observed among the two groups (Table 4 ). Supplemental oxygen was required by 45.6% of patients and there was no difference in oxygen use Table 1 Baseline characteristics of patients with SARS-CoV-2 infection.

Total (n = 136) Imported cases (n = 50) Non-imported cases (n = 86) P between the two groups. Non-invasive ventilation was required for 2.9% of the patients. Only one patient in each group was transferred to an ICU of another hospital for invasive mechanical ventilation. Regarding treatment, 99.3% of patients received antiviral therapy including lopinavir/ritonavir (95.6%), interferon alpha-2b (97.8%), and arbidol (79.4%). Nearly a third of the patients received antibacterial therapy, and 12.5% received glucocorticoid therapy. One (0.7%) patient received kidney replacement therapy for uremia. There were no significant differences in treatments between imported cases and local cases ( Table 4 ).

Thirty patients without available complete virological dynamic data were excluded from the analysis. The RT-PCR RNA conversion of the remaining 106 cases (42 imported vs 64 local) was determined. The curve showed there was no significant difference in the proportion of RT-PCR RNA conversion over time between the imported and local cases (P = -.9016) (Fig. 2) . The median duration of SARS-CoV-2 RNA shedding was 26 days (IQR 17-32.3 days) from symptom onset, 20 days (IQR 11-25.3 days) from first RT-PCR RNA positive onset, and 20 days (IQR11.8-25 days) from treatment onset, respectively. However, the median duration of SARS-CoV-2 shedding did not differ significantly between the imported and local cases (Table 4) .

As of March 7, 2020, 134 (98.5%) of 136 patients had met discharge criteria, and two patients were transferred to ICU of another hospital for further treatment due to progressing to critically illness, but eventually recovered and were discharged. Among these 134 discharged patients, the median hospital stay was 23 days (IQR, 18-28.3). There were 9 patients (6.7%) with recurrence of positive RNA during follow-up visit after discharge and there was no significant difference on recurrence rate of positive RNA between imported cases and local cases (6.1% vs 7.1%) ( Table 4 ).

Our findings suggest that the prevalence of the severe cases was significantly higher among the imported cases than that of local cases, but there was no significant difference in conversion of RT-PCR RNA and duration of viral shedding between the two groups. Local cases had significantly higher white blood cell counts as well as neutrophil and lymphocyte count and platelet counts, but the imported cases had significantly higher prothrombin times. Lymphopenia has been previously noted as a clinical feature of severe COVID-19 disease. [11, 12] These features could help to explain the difference in severity of COVID-19 between local and imported cases. However, the pathology COVID-19 in humans is still not fully understood. Neutrophil counts noted during the 2003 epidemic of SARS-CoV were significantly higher among severe patients compared to nonsevere patients. [13] Similar results were observed with COVID-19 caused by SARS-CoV-2. [14] These differences may be related to secondary infections. However, the neutrophils count of the imported cases in this study were significantly lower than that of the local cases. The leukopenia observed by our group may be related to the suppression of bone marrow by the virus itself. Of note, our study is focused on clinical features of the imported and local cases, but not on severe and non-severe cases. Most important, there is no solid evidence to support that the neutrophil levels are the predicator or causal risk factor of the severe cases in those diseases. Among SARS patients, hematological change was associated with severity of the disease. Lymphopenia frequently resolves when the patient improves. [15] Glucocorticoids may be driving circulating T lymphocyte out from the intravascular compartment resulting in lymphopenia. [16] Hence, activation of the hypothalamic-pituitary-adrenal axis during critical disease, could increase adrenocorticotropic hormone (ACTH) and cortisol resulting in T lymphocytes moving out of the peripheral circulation. [16, 17] Also, similar hematological changes (e.g thrombocytopenia) in COVID-19 have been reported in SARS. [18] One proposed biological mechanism of SARSassociated thrombocytopenia is viral infection bone marrow cells. [19, 20] Usually, it is difficult to trace the original source of a pandemic outbreak, and one possible hypothesis is Wuhan Huanan Seafood Wholesale Market was not the original source. [5] Of note, it was the first one reported because it close to the Wuhan hospital where lot of healthcare workers have been infected. There might be other earlier cases which were asymptomatic or had mild clinical symptoms and could have resolved without treatment and may not have been not hospitalization. In the presented study, Tseveral local cases could not be epidemiologically linked. Further, since viral sequencing was not performed in the present study, a genetic comparison of imported and local cases could not be performed.

One possible hypothesis is that most local cases were in the early stage of the disease with only slight symptoms. Typically, Table 3 Baseline laboratory findings, and imaging characteristics of patients with SARS-CoV-2 infection.

Total (n = 136) Imported cases (n = 50) Non-imported cases (n = 86) P Blood routine White blood cell count, Â 10 9 /L 3.5-9.5 4.6 (3.7-6. Table 4 .

Severity, complications, treatment and outcomes of patients with SARS-CoV-2 infection.

Total (n = 136) Imported cases (n = 50) Non-imported cases (n = 86) P the imported cases are likely to be the index in a cluster of infections, while the local cases are more likely to be found through screening of the close contacts. Also, there is a small proportion of asymptotic cases in the general population who are more likely to be identified through screening. Those cases are more likely to resolve quickly if therapy was administered. Thus, the hematological change (e.g lymphocyte count) and clinical features, such as pleural effusion, may reflect the stage of COVID-19 disease. The difference in severity between imported and local COVID-19 cases could be partly due to the differences in time from symptom onset to diagnosis. This difference might contribute to the presentation of symptoms and disease characteristics. However, there was no significant difference in time from symptom onset to admission and in the number of hospital days between the imported and local COVID-19 cases in our cohort. Additionally, there is no standard treatment protocol for the COVID-19 until now. However, patient reporting of time from onset to presentation may be biased and inaccurate. Etro suggested that antibody dependent enhancement (ADE) of SARS-CoV-2 due to prior exposure to other coronaviruses. [21] This immune response could be explained by the severity found between imported and local COVID-19 cases. Because ADE modulates the immune response and can elicit sustained inflammation, lymphopenia, and/or cytokine storm, one or all of which have been documented in severe cases and deaths. [21] However, there is no evidence that imported cases were previously infected by other coronaviruses. Also, most imported cases are residents who had traveled to Wuhan. Theoretically, there should not be a difference between the two group in other characteristics. An alternative explanation is that the virulence of the SARS-CoV-2 virus decreases during the chain of transmission. Future studies on the virulence of the virus, supported by epidemiological data on transmission is warranted.

To date, comparative data on the duration of SARS-CoV-2 RNA shedding between imported and local cases have been limited. Our study found the median duration of viral RNA shedding from symptom on set was up to 26 days, which was significantly longer than those previously reported (less than 20 days). [22] [23] [24] It has been reported that the duration of Middle East Respiratory Syndrome Coronavirus shedding in severe cases was significantly longer than that in non-severe cases. [25] Although our study found that the number of severe or critically ill cases in imported cases was significantly higher than that in local cases, there was no difference in the duration of viral shedding between the two groups.

Recent studies showed that the prolonged viral shedding was not associated with the severity of illness, but with the time of admission to hospital [24] and antiviral treatment. [26] The prolonged SARS-CoV-2 RNA shedding is relevant not only for the control of nosocomial infection, but also for discharge management.

In the initial stages of COVID 19 outbreak in China, the severe rate or mortality of COVID-19 cases in Wuhan was higher than those of cases outside Wuhan. But in Wenzhou, the severe rate of COVID-19 among imported cases from Wuhan was higher than that of the local cases. This could be due to the adequate medical resources and high capacity of therapy available in Wenzhou, which guaranteed zero death case in COVID-19 cases. Hence, there is no significant difference between the two groups being more likely due to the treatment.

This study systematically compares the clinical features and viral RNA shedding between imported and local cases. However, our study has serval limitations. First, some epidemiological details are missing in the imported cases such as whether they are secondary infectious cases. Second, the RT-PCR testing was not conducted at fixed timepoints during hospitalization. Although we excluded those patients without no available complete virological dynamic data, there might have still been some selection bias in the remaining data. Third, the physical examine results from admission at the hospital could be affected by the timepoints of prognosis because people's admission into the hospital was varied. Also, we did not identify the sub-clinical type for the most non-severe cases. Some potential indices of virus performance (e.g CD4 or CD8 counts or ratio) were not collected in the present study. Forth, as we know COVID-19 is dangerously pathogenic and the currently study was completed in February 2020. Since the outbreak of COVID-19, the state has strictly prohibited the preservation or outward detection of all highly pathogenic samples. Therefore, in the early stages of this study, there was no outward sample gene sequencing to compare the differences between the two groups. In future similar studies, we will compare the differences between the two groups of genetic genes from the perspective of origin. Despite some defects, it is still of good clinical reference significance for COVID-19. Final, other respiratory virus were not tested among the cases.5

Our results suggest that the severity of illness, laboratory test results, and CT scan images of local cases of COVID-19 are less severe than imported cases of COVID-19 from Wenzhou. However, there was no difference between imported and local cases on the viral shedding among the COVID patients. These results could help physicians and other healthcare providers to better understand the pathogenesis and virological dynamics during the process of illness, which should be helpful in the clinical management of patients with COVID-19.

Dr He and Dr Wu conceptualized and designed the study, collected data, drafted the initial manuscript, and reviewed and revised the manuscript. Dr Huang reviewed and revised the manuscript. Prof Schieffelin conceptualized and designed the study, and reviewed and revised the manuscript.

Coronavirus disease (COVID-19) pandemic. Available at

Global Covid-19 Case Fatality Rate

COVID-19) Mortality Rate

Epidemiological and clinical characteristics of 99 cases of 2019 novel coronavirus pneumonia in Wuhan, China: a descriptive study

Clinical features of patients infected with 2019 novel coronavirus in Wuhan, China

Clinical characteristics of 138 hospitalized patients with 2019 novel coronavirus-infected pneumonia in Wuhan, China

Clinical findings in a group of patients infected with the 2019 novel coronavirus (SARS-Cov-2) outside of Wuhan, China: retrospective case series

Clinical management of severe acute respiratory infection when novel coronavirus (nCoV) infection is suspected: interim guidance

Diagnosis and treatment protocols of the novel coronavirus pneumonia (trial version 6)

Acute respiratory distress syndrome: the Berlin Definition

A familial cluster of pneumonia associated with the 2019 novel coronavirus indicating person-to-person transmission: a study of a family cluster

Pathological findings of COVID-19 associated with acute respiratory distress syndrome

A cluster of patients with severe acute respiratory syndrome in a chest ward in southern Taiwan

Dysregulation of immune response in patients with COVID-19 in Wuhan, China

Clinical presentations and outcome of severe acute respiratory syndrome in children

Lymphopenia in SARS

Glucocorticoids and acute lung injury

Thrombocytopenia in patients with severe acute respiratory syndrome (review)

Impaired T and B cell subpopulations involved in a chronic disease induced by mouse hepatitis virus type 3

Impairment of bone marrow pre-B and B cells in MHV3 chronically-infected mice

Is COVID-19 receiving ADE from other coronaviruses?

The clinical dynamics of 18 cases of COVID-19 outside of Wuhan, China

Lopinavir/ritonavir and interferon combination therapy may help shorten the duration of viral shedding in patients with COVID-19: a retrospective study in two designated hospitals in Anhui

Factors associated with prolonged viral RNA shedding in patients with COVID-19

Middle East respiratory syndrome coronavirus transmission

Factors associated with prolonged viral shedding and impact of Lopinavir/Ritonavir treatment in hospitalised non-critically ill patients with SARS-CoV-2 infection

Dr Dai collected data, reviewed and revised the manuscript. Prof Gamber carried out the analyses, critically reviewed the manuscript for important intellectual content, and reviewed and revised the manuscript. Dr Hu was responsible for the laboratory analysis. Dr Chen and Dr Si were responsible for the imaging analysis. Prof Sun and Dr Cai carried out the analyses and reviewed and revised the manuscript. All authors approved the final manuscript as submitted and agree to be accountable for all aspects of the work in ensuring that questions related to the accuracy or integrity of any part of the work are appropriately investigated and resolved.