key: cord-0819405-y9o3kai9
authors: Axelrad, Jordan E; Malter, Lisa; Hong, Simon; Chang, Shannon; Bosworth, Brian; Hudesman, David
title: From the American Epicenter: Coronavirus Disease 2019 in Patients with Inflammatory Bowel Disease in the New York City Metropolitan Area
date: 2020-06-24
journal: Inflamm Bowel Dis
DOI: 10.1093/ibd/izaa162
sha: 4e99c7dc22e8b1abe8f1a93ad6f05d068f6c5945
doc_id: 819405
cord_uid: y9o3kai9

BACKGROUND: We aimed to characterize patients with inflammatory bowel disease (IBD) and novel coronavirus disease 2019 (COVID-19). METHODS: We performed a case series of patients with IBD and confirmed or highly suspected COVID-19 to assess rates of severe outcomes. RESULTS: We identified 83 patients with IBD with confirmed (54%) or highly suspected (46%) COVID-19. The overall hospitalization rate was 6%, generally comprising patients with active Crohn’s disease or older men with comorbidities, and 1 patient expired. DISCUSSION: In this series of patients with IBD, severe outcomes of COVID-19 were rare and comparable to similarly aged individuals in the general population.

In December of 2019, cases of pneumonia of unknown cause were reported in Wuhan, China, leading to the identification of the novel severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), the causative virus of coronavirus disease 2019 (COVID-19). 1 Since then, the COVID-19 pandemic has shifted geographically to Europe and North America, with the New York City (NYC) metropolitan area currently at the epicenter. Despite increasing data regarding the clinical characteristics of affected patients in the general population, 2 data are limited for populations at higher risk of infection, including patients with inflammatory bowel disease (IBD). Moreover, optimal management of immunosuppression in patients with IBD and COVID-19 is currently based on expert opinion. 3, 4 Preliminary evidence suggests that antirheumatic (ie, hydroxychloroquine [HCQ] ) and anticytokine (ie, IL6 inhibitors) therapies may improve the outcomes of COVID-19 by mitigating the cytokine storm syndrome associated with severe COVID-19 and respiratory failure. 5 Therefore, patients receiving immunosuppression for IBD may have partial protection against severe outcomes of COVID-19 (ie, need for hospitalization, ventilation, or death). We aimed to characterize patients with IBD and COVID-19 and investigate the impact of IBD therapies on COVID-19 outcomes.

We performed a case series of patients with IBD (Crohn's disease [CD], ulcerative colitis [UC]) at the IBD Center at NYU Langone Health, NYC, with confirmed or highly suspected COVID-19 from March 3 to May 10, 2020. High suspicion was defined as any patient residing in the NYC area presenting with new fever >99°F or a known contact positive for SARS-CoV-2 plus 1 or more respiratory symptoms (cough, pharyngitis, or shortness of breath) that could not be confirmed given restricted outpatient SARS-Cov-2 testing in NYC. We analyzed demographic, pharmacy, and IBD data with COVID-19 data and outcomes. Inflamatory bowel disease severity was estimated based on routinely measured clinical disease severity indices (eg, partial Mayo score for UC or Harvey-Bradshaw index for CD) documented in the most recent office visit note or routinely measured endoscopic scoring (eg, Mayo endoscopic subscore for UC or simple endoscopic score for CD) documented in the most recent procedure note. Where these data were not available, IBD severity assessment was done by physician global assessment. Severe outcomes of COVID-19 were considered the requirement for an ER visit, hospitalization, ventilation, or death.

We identified 83 patients with IBD (CD [n = 56, 67%] or UC [n = 27, 33%]) with confirmed (n = 45, 54%) or highly suspected (n = 38, 46%) COVID-19 with a median follow-up of 52 days (range 11-72) from the onset of symptoms (Table 1) . At COVID-19 symptom onset, the median age was 35 years (interquartile range [IQR], 27-45), 70% were white (n = 39), 89% were non-Hispanic (n = 74), and few had comorbidities. The majority had mild IBD activity (n = 26, 31%) or were in remission (n = 30, 36%). Few were on an oral corticosteroid (n = 10, 12%) or tofacitinib (n = 4, 7%), with the majority on a biologic (n = 58, 70%), largely an anti-TNF agent (n = 44, 53%). The most frequently reported symptoms were fever (n = 55, 66%) and cough (n = 46, 55%); fewer had new or worsening diarrhea (n = 26, 31%) or anosmia (n = 25, 30%). The overall hospitalization rate was 6% (n = 5; 1 intubation), with an additional Table 2 ). Inflammatory bowel disease therapies were held in 13 (16%), and the dose/frequency of administration was reduced in 3 (4%). Treatment with HCQ or azithromycin was offered for 8 patients (10%). Median duration of symptoms was 11 days (IQR, 5-15). Of 5 patients who required hospitalization, the majority were patients with active CD or older men with comorbidities, and 1 (1%) expired.

In this case series of patients with IBD and symptomatic COVID-19 in the NYC area, the epicenter of the pandemic in the United States, severe outcomes of COVID-19 were uncommon, with a hospitalization rate of 6% and mortality rate of 1%. With over 2 months of total follow-up, baseline immunosuppression did not appear to modify the risk of severe outcomes. Compared with reports in the general population, patients with IBD may present with a higher burden of gastrointestinal symptoms due to COVID-19, in particular diarrhea and ageusia, although more data are required. 2, 6 According to the NYC Health Department, as of May 15, 2020, there were 187,848 confirmed cases of SARS-CoV-2 and 49,580 COVID-19 hospitalizations in NYC, suggesting a case-hospitalization rate of 26%. 7 This high rate of hospitalization is likely due to restricted outpatient testing in NYC and the relatively older general population with COVID-19, where hospitalization rates are substantially increased. Thus, limiting our population to those with laboratory-confirmed SARS-Cov-2 testing, the hospitalization rate was 11% in patients with IBD. Although limited in sample size, our data reveal a hospitalization rate on par with similarly aged subjects in NYC. 7 Additionally, consistent with reports in the general population, factors such as age, male sex, and comorbidities were associated with COVID-19-related hospitalization in patients with IBD. 8 Hospitalization for COVID-19 was more common in patients with active CD, suggesting uncontrolled CD may be an additional risk factor for severe outcomes. In the ongoing SECURE-IBD registry, COVID-19 is also more common in patients with CD than UC, although the overall hospitalization rate is 33%. 9 This large difference in hospitalization in the SECURE-IBD registry may be due to selection bias toward more severe cases, underreporting of mild cases that may not present to medical care or testing, and perhaps even misclassification of IBD or attribution of a hospitalization to COVID-19 rather than a complication of IBD by referring providers.

A better understanding of the implications of COVID-19 in patients with IBD and the effects of immunosuppressive therapies is urgently needed to guide gastroenterologists in caring for patients with IBD during this pandemic. In our sample, few patients required delay, reduction, or cessation of IBD therapies due to COVID-19 symptoms. For 3 patients on tofacitinib with active IBD, COVID-19 symptoms persisted with dose reduction and required temporary therapy cessation. Although further data are required, similar to recommendations from the CDC for health care providers returning to work, we resumed immunosuppression 72 hours after being afebrile, with near resolution or minimal respiratory symptoms at least 7 days from symptom onset. In those who required an interruption in therapy, all were restarted without adverse outcome. Patient 6 ( Table 2) , an 80-year-old male previously maintained on adalimumab with methotrexate, was not restarted on IBD therapies and expired on hospital day 11. Patient 4 was hospitalized for acute severe UC complicated by COVID-19 in her first trimester of pregnancy. Cyclosporine was given rather than infliximab for its shorter half-life in the event of COVID-19 progression. Though the patient experienced a spontaneous abortion, her colitis and COVID-19 improved, and she was recently initiated on outpatient ustekinumab. In sum, treatment for moderately to severely active IBD and COVID-19 was chosen on a case-by-case basis.

In conclusion, patients with IBD seem to be similarly at risk for COVID-19 and related outcomes to correspondingly aged individuals in the general population. Severe outcomes of COVID-19 were rare and generally limited to older men with comorbidities and/or patients with active CD. All patients who continued or restarted IBD therapies did so without clinical consequence. Although we did not find evidence of an effect of IBD therapies on COVID-19 outcomes, further data are required. The optimal management of IBD and COVID-19 remains undefined but likely requires a multidisciplinary team and a careful, individualized approach.

Genomic characterisation and epidemiology of 2019 novel coronavirus: implications for virus origins and receptor binding

Clinical characteristics of coronavirus disease 2019 in China

Management of patients with Crohn's disease and ulcerative colitis during the COVID-19 pandemic: results of an international meeting

AGA clinical practice update on management of inflammatory bowel disease during the COVID-19 pandemic: expert commentary

19: consider cytokine storm syndromes and immunosuppression

Novel coronavirus infection and gastrointestinal tract

COVID-19: Data -NYC Health website

COVIDView Weekly Summary | Centers for Disease Control and Prevention website

SECURE-IBD Database Public Data Update website