key: cord-0723713-4bu9b45c
authors: Shahram, Farhad; Esalatmanesh, Kamal; Khabbazi, Alireza; Rezaieyazdi, Zahra; Mirfeizi, Zahra; Sadeghi, Alireza; Soroosh, Mohsen; Kavosi, Hoda; Alikhani, Majid; Mostafaei, Shayan
title: Coronavirus disease 2019 in patients with Behcet’s disease: a report of 59 cases in Iran
date: 2021-11-29
journal: Clin Rheumatol
DOI: 10.1007/s10067-021-06004-y
sha: 472d621e05392d0bcbc491f1ab3ffdeef2fc6616
doc_id: 723713
cord_uid: 4bu9b45c

OBJECTIVES: To present the clinical characteristics, disease course, management, and outcomes of COVID-19 infection in patients with Behcet’s disease (BD). METHODS: In this retrospective cohort study, we retrieved BD patients with definite diagnosis of COVID-19 infection. Demographic data, comorbidities, features related both to BD and COVID-19 infection, treatments, and outcomes were collected. Comparisons between patients with or without hospitalization were performed. All statistical analyzes were performed using SPSS version 25. We considered p < 0.05 statistically significant. RESULTS: We identified 61 episodes of COVID-19 infection in 59 BD patients. The prevalence was 0.69%. The median age was 45 years (IQR = 20), and the median disease duration was 162 months (IQR = 195). BD features were similar except for higher rate of arterial involvement and positive pathergy test in infected patients. Thirty-five episodes (62.5%) happened in non-active patients; 39% had a comorbid disease. COVID manifestations were the same as the general population. Flu-like symptoms were the most common (85%), followed by fever (66%), ageusia/anosmia (56%), headache (51%), and pulmonary involvement (48%). There was no change in BD symptoms in 74%. Fifteen patients (25.4%) were hospitalized, and one patient (1.7%) died. Receiving glucocorticoids (p < 0.03) and cytotoxic drugs (p < 0.02) were associated with an increased rate of hospitalization. CONCLUSION: The incidence of COVID-19 infection in BD patients was not higher than general population in Iran. They showed milder form of disease with lower morbidity and mortality rate. Most were on immunosuppressive drugs, or had a comorbidity apart from BD. No significant effect on BD course was shown.

Since December 2019, a novel infection with severe acute respiratory syndrome coronavirus 2 (SARS-Cov-2) broke out in Wuhan, China, and has transformed into a worldwide challenge. The disease, named coronavirus disease 2019 (COVID- 19) , was officially declared a pandemic by World Health Organization (WHO) on 11 March 2020 [1] .

The risk of COVID-19 and its associated complications is considered to be increased in patients with preexisting medical conditions [2] . Whether patients with autoimmune diseases or vasculitides are at increased risk of COVID-19 is not established yet [3] . In general, immunosuppression and the presence of comorbidities are associated with an increased risk of serious infection in people with rheumatic diseases [4] . However, to date, it has not shown a higher incidence of COVID-19 in these patients [5] , even if receiving biologic disease-modifying antirheumatic drug (b-DMARD) therapy [6, 7] .

It is still unclear, if there is a modified course of COVID-19 in patients with autoimmune and/or auto-inflammatory diseases [3, [8] [9] [10] , and whether they are at higher risk for a more severe course with COVID-19, including hospitalization, complications, and death [4] . In addition, a preliminary survey study showed that patients treated with DMARDs and infected with COVID-19 did not develop lifethreatening complications due to their underlying medication [11] .

During the pandemic of COVID-19, a proportion of the autoimmune disease patients suspended their medication due to fear of the immunosuppressive effect of medications or lack of availabilities [12] , and decreased medical visits because of concerns of the contagious nature of SARS-CoV-2 [13] . Disrupted continuity of medical care and medication non-adherence are associated with rheumatologic disease flares and worsened disease activity [14] .

Behcet's disease (BD) is a chronic multi-system disease [15] , classified as a variable type vasculitis due to affecting vessels of all sizes [16] . Its clinical picture is dominated by recurrent oral and genital ulcers, skin manifestations, and ocular lesions. Other manifestations are related to the involvement of joints, large vessels, the nervous system, and the gastrointestinal tract [15] .

Data on the course of COVID-19 in BD patients remain scarce and limited to small case series [17] .

In this study, we present a large case series of COVID-19 in patients with BD and describe their clinical characteristics, disease course, management, and outcomes.

This was a retrospective cohort study on BD patients visited between March 2020 and March 2021.

All patients had BD classified by either International Criteria for Behcet's Disease (ICBD) or International Study Group (ISG) criteria [18, 19] . Diagnosis of COVID infection was relied on positive reverse transcription polymerase chain reaction (PCR) test (nasopharyngeal swab samples) and/or typical lesions on the lung high resolution computed tomography (HRCT) in compatible clinical setting [20] .

Demographics, BD characteristics, comorbidities other than BD, and features related to COVID-19 infection were collected for each patient. BD characteristics included disease duration, clinical manifestations, disease activity, and medications used at the time of infection. COVID-19 features included symptoms and signs, pharmacological treatments, and clinical outcomes (including hospitalization, morbidity, and death). We also assessed whether patients had any exacerbation of BD during infection. Finally, we checked the effect of different data on hospitalization of patients.

Number (%) was presented for categorical variables. The mean and the standard deviation (SD) or median and the interquartile range (IQR) were calculated for the continuous normal and non-normal distributed variables respectively. Kolmogorov-Smirnov test was used to check the normality distribution of the continuous variables. Either the independent t test or the Mann-Whitney U test was used to compare the continuous variables, and the chi-square test with Yates correction was used to compare qualitative or categorical variables. Two-tailed p value of less than 0.05 was considered statistically significant. All statistical analyzes were performed using SPSS version 25 (SPSS Inc., Chicago, IL, USA).

The study protocol was approved by the Research Committee of Rheumatology Research Center (RRC) and the Ethics Committee of Tehran University of Medical Sciences. The study was conducted in accordance with the Code of Ethics of the World Medical Association (Helsinki Declaration of 1975/83) for experiments involving humans and Good Clinical Practice guidelines.

We identified 61 episodes of COVID-19 infection in 59 patients with BD (two with recurrence of the infection) in a cohort of 8586 patients. The prevalence rate was 0.69% in our BD cohort. These patients were retrieved from 6 rheumatology academic centers in 5 cities in Iran (Tehran: RRC 33/7773 and AJA University 2/50; Mashhad: 9/186; Tabriz: 6/383; Kashan: 6/74; Zanjan: 3/120). The majority have been diagnosed elsewhere, and contacted us during their routine follow-up visits or for consulting about their disease status and medication after infection. Due to national test shortages, testing was not done systematically for all our BD cohort and it was done only for BD patients complaining of any of the symptoms suggestive of COVID infection. The testing rate was 5.5%, with a test positivity rate of 9.0% in the BD cohort.

All had confirmed BD diagnosis, 56 (95%) were classified by the ICBD criteria and 45 (76.3%) by the ISG criteria. Diagnosis of COVID infection was relied on positive PCR test in 52 (88%) cases, and typical lesions on the lung HRCT with compatible clinical setting in 7 other cases (with positive serum anti-COVID antibody in two of them).

The 

Data regarding disease activity were available for 56 episodes of infection. Twenty-one (37.5%) cases were seen in patients with active BD according to the physician global assessment (14 with mild and 7 with moderate disease activity). Thirtyfive episodes (62.5%) happened in non-active BD patients.

Except 4 patients who were off treatment, the other 55 (93%) were using one of the following drugs either alone or in combination: corticosteroids: 42 (76%); immunomodulators: 33 (60%) (colchicine 30, sulfasalazine 4, mycophenolate 1, levamisole 1); cytotoxic drugs: 35 (64%) (azathioprine 19, methotrexate 15, cyclophosphamide 2); biologic drugs 6 (11%) (four anti-TNFs and two Interferon alpha).

Twenty-three (39%) had a comorbid disease apart from BD, including diabetes mellitus (10), hypertension (7), obesity (7), cardiac (6), pulmonary (3) renal disease (2), malignancy, brain abscess and smoking (each in one). Thirteen patients (56.5%) had single comorbid disease, but 6 had two, 3 had three, and 1 had four concomitant comorbid diseases.

They were the same as seen in the general population. Flulike symptoms (fatigue and myalgia) were the most common, seen in 52 cases (85%), fever in 40 (66%), headache in 31 (51%), loss of taste and anosmia in 34 (56%). Pulmonary involvement was seen in 29 patients (48%), but pulmonaryrelated symptoms were seen more: cough in 36 (59%), dyspnea or chest tightness in 27 (44%) and expectoration in 9 (15%) patients. Gastrointestinal symptoms (nausea, vomiting and diarrhea) were seen in 25 patients (41%). Prevalence of other signs was as follows: cold symptoms (sore throat and nasal congestion) in 12 (20%); shivering in 20 (33%); vertigo in 4 (7%); illusion/restlessness/agitation in 3 (5%); weight loss, sweating, menorrhagia, hypotension, and hypertension each in 1 patient. We had no skin involvement.

There was no change in BD symptoms in 45 cases (74%). Sixteen patients (26%) presented with a disease flare during COVID infection, but only 3 of them needed treatment intensification. In more than 95%, the medications were either not changed (44 cases, 72%) or even decreased or discontinued (14 cases, 23%).

Seven patients (11.5%) received only symptomatic treatments. Thirty patients (49%) received antibiotics (azithromycin: 22, ceftriaxone: 2, ciprofloxacin: 2, doxycycline: 2 co-amoxiclav: 2, penicillin: 1, tazocin: 1). Antiviral drugs were used in 11 patients (18%) (sofosbuvir/daclatasvir: 5, remdesivir: 3, favipiravir: 1, both remdesivir and favipiravir: 1, lopinavir/ritonavir: 1). Corticosteroids was administered in 13 patients (21%), hydroxychloroquine in 10 (16.4%), interferon beta in 4 (6.5%), and anti-TNF in one (1.7%). We did not access to the treatment regimen for 8 episodes of infection.

Fifteen patients (25.4%) were hospitalized, and one patient (1.7%) died due to severe respiratory failure. We had BD flare in 16 patients (27%); one patient developed pulmonary embolism after deep vein thrombosis; COVID re-infection was seen in two cases.

Comparing hospitalized and non-hospitalized BD patients with COVID-19 infection showed no significant difference for age, gender, disease duration, individual clinical features, or comorbid diseases. However, the rate of active disease was significantly higher in the hospitalized patients (58% vs. 32%, p = 0.02). We found that receiving glucocorticoids (100% vs. 59%, p < 0.04) and cytotoxic drugs (87% vs. 48%, p < 0.02) were significantly associated with an increased rate of hospitalization, but not biologic therapies and immunomodulators (Tables 1 and 2) .

Comparison of clinical presentation of COVID-19 in BD patients by hospitalization status showed no significant differences except for pulmonary involvement which was higher in hospitalized patients (87% vs. 35%, p = 0.001). Corticosteroid (58% vs. 15%, p = 0.006), anti-viral (58% vs. 10%, p = 0.001), and anti-inflammatory drugs (75% vs. 39%, p = 0.06) were prescribed more in hospitalized patients, as expected. In addition, COVID-19 infection had less significant effect on BD treatment in higher percentage of nonhospitalized patients (80% vs. 47%, p < 0.03) ( Table 3 ).

The first official report of coronavirus disease in Iran was in February 2020. As of March 21, 2021, according to both Johns Hopkins University and WHO reports Iran (with a population of 84,770,256) was rated as the fifteenth country in the world by the prevalence with the total number of 1,808,422 confirmed cases (21,333/million population) and total death of 61,877 (730/million population). The total tests done was 12,221,274 (144,169/million population) [21, 22] .

In comparison with general population of Iran, both the prevalence and death rate of COVID-19 infection were lower in BD patients (0.69% versus 2.13% and 1.7% versus 3.42% respectively). Lower number of testing in BD patients (5.5% versus 14.4%) may be one of the attributing causes. Test positivity was also lower in BD patients (9.0% versus 14.8%). This was in line with report of the International Society for Behcet's disease in January 2021, showing lower overall prevalence of COVID-19 infection in BD patients throughout the world. It might be due to BD patients having been especially careful with social shielding. However, underestimation is also possible [17] . Patients with COVID infection showed similar BD features to the whole cohort patients except for higher rate of joint involvement and positive pathergy test [23] . This was in accordance with a recent report from Italy showing no significant difference in BD manifestations in those with COVID infection [24] .

It is not yet known whether patients with rheumatic diseases receiving immunosuppressive therapy are more susceptible to SARS-CoV-2 or not [20, 24] . Meta-regression analysis demonstrated that prior glucocorticoid use was associated with the increased risk of SARS-CoV-2 infection [9, 24] . Most of our patients (93%) were on immunomodulator or immunosuppressive drugs, and 68% were on corticosteroids. Dursen et al. reported that none of their 54 BD patients developed COVID-19 infection while 51 were continuing their immunological treatment [25] .

In general, the presence of comorbidities is associated with an increased risk of serious infection in people with rheumatic diseases [11] . Only 39% of our patients had a comorbid disease apart from BD. It is notable that in general population of Iran, around 90% of patients with COVID infection had at least one comorbid disease.

Disease activity did not appear to be associated with an increased risk of COVID infection in BD patients [4] . In this study, most episodes of infection (62.5%) happened in non-active BD patients.

The most common symptoms of COVID-19 are fever and cough, which can progress to pneumonia and acute respiratory distress syndrome (ARDS) or multi-organ failure [26] . Additionally, it may predispose to thrombotic disease, both in the venous and arterial circulations [20] . In accordance with previous reports, COVID symptoms and signs in our BD patients were the same as the general population [2, 17, 27] . Of interest, we had no skin involvement due to COVID infection in BD patients.

As no specific guidelines for the treatment of COVID infection were present for BD patients, the management was done according to the general national guidelines defined by the Ministry of Health. They received symptomatic treatments, antibiotics (mainly azithromycin), antiviral drugs, hydroxychloroquine, corticosteroids, and interferon.

There is a debate on exacerbation of the underlying rheumatic disease during COVID-19 infection [28, 29] . Medication non-adherence and disrupted continuity of medical care are associated with rheumatologic disease flares and worsening disease activity [14] . We had seen no effect on BD symptoms or any need to change the treatment in most cases. We had BD flare only in 26% of infectious episodes.

There are many reports on the development of autoimmune diseases after SARS-CoV-2 infection, such as cold agglutinin syndrome, autoimmune hemolytic anemia [30, 31] , and systemic lupus erythematosus [32] . Interestingly, we had a case with new development of BD after COVID infection. He was a 57-year-old man presented in July 2020 with fever, sore throat, nasal stiffness, cough, fatigue, and myalgia. He developed later mild dyspnea, diarrhea, anosmia, illusion, and restlessness. He had a history of type 2 diabetes and was on glibenclamide. The diagnosis of COVID infection was made clinically without PCR test. Azithromycin was prescribed along with symptomatic treatments at home. All symptoms resolved completely after 4 weeks. Three months later, he developed recurrent oral and genital ulcers, arthralgia, and constitutional symptoms. HLA typing was positive for B51. The diagnosis of BD was reached upon above symptoms and colchicine was started. COVID-19 infection may be suggested as a trigger for the appearance of BD symptoms in this case. As SARS-CoV-2 infection can break immune tolerance and trigger autoimmune responses, it is also likely to induce clinical autoimmunity [13] .

In contrast to the first case series reported from Turkey suggesting that BD patients have increased risk for severe outcome when infected with COVID-19 [20] , the severity of infection was milder in BD patients in Iran. This was in concordance with several reports showing the milder course of COVID infection in inflammatory rheumatologic diseases [9, 29, 33, 34] , and supports the theory that immunosuppression may play a protective role during COVID-19 infection [17] . In general, patients with BD had a COVID-19 clinical picture resembling the general population, and the severity of COVID-19 infection was milder in them [17, 27, 29] . However, the number of reported BD cases had not been high enough to be able to see the effects of the disease subtypes, activity and medications on the outcome [17] . We found a similar risk of hospitalization, with lower morbidity and mortality rate in BD patients. In line with other reports [4, 9, 34, 35] , using glucocorticoids and cytotoxic drugs were associated with an increased rate of hospitalization. We could not identify any other risk factors associated with hospitalization, except for non-significant higher rate of active disease in them, while previous reports showed that older age and the presence of comorbidity in COVID-19 patients with autoimmune diseases are accompanied with a higher risk of hospitalization [9, 34, 35] .

As expected, the main reason for hospitalization was pulmonary involvement. The rate of other clinical features of COVID-19 infection was not different in hospitalized patients. They needed more corticosteroid, anti-viral and anti-inflammatory drugs for their infection management. COVID-19 infection had no effect on the BD treatment in 47% (compared to 80% in ambulatory patients).

Only one patient in our series of 59 patients died due to severe respiratory failure, and COVID re-infection was seen in two. Very little is known about the outcomes of patients with COVID-19 who have underlying rheumatic disease [10, 20] . People with rheumatic diseases may be at higher risk for a more severe course with COVID-19, including hospitalization, requiring intensive care/mechanical ventilation, or death [4, 10, 34, 36] . When matched for common comorbidities, the population with rheumatic diseases may not have more frequent death [9, 34] . COVID-19 outcomes were worse in those receiving glucocorticoids but not in patients on maintenance anti-cytokine therapy. However, there are reports showing corticosteroid treatment reduce mortality [9, 36] .

To the best of our knowledge, this is the largest collection of COVID-19 infections among patients with BD, with 61 episodes in 59 cases. There had been few small case series reported from Turkey, Spain, and Italy [20, 24, 27] . In most large studies on COVID infection in patients with rheumatic or autoimmune diseases, BD has not been pointed as a distinct disease and has been included under the large group of vasculitides [3, 9, 33, 34] .

There are some limitations in this study. First, it was a retrospective study. Second, we were not able to include all cases of COVID-19 infection with BD, as we did not routinely test our whole BD population for COVID-19 infection, so asymptomatic patients or those with milder infection or those who could not reach us due to quarantine and other restrictions may not be represented. This might cause selection bias due to factors such as geographical location and disease severity.

The incidence of COVID-19 infection among BD patients is not higher than that observed in the general population of Iran. BD patients had a COVID-19 clinical picture similar to the general population, with milder severity of infection. We found a similar risk of hospitalization, with lower morbidity and mortality rate in BD patients. Regarding BD features, there was not any significant difference except for higher rate of joint involvement and positive pathergy test. Most infected patients (92%) were on immunomodulator or immunosuppressive drugs, and near 40% had a comorbid disease apart from BD. In most cases, COVID infection had no effect on BD symptoms or treatment. Of note, there was a case with new development of BD, suggesting COVID infection as a possible trigger for disease presentation.

Acknowledgements The authors acknowledge Asal Salehi MD for her significant cooperation on data collection.

Author contribution Farhad Shahram: conceptualization; data curation; formal analysis; investigation; methodology; project administration; resources; supervision; validation; writing original draft; review and editing.

Kamal Esalatmanesh: data curation; investigation; validation; review and editing.

Alireza Khabbazi: data curation; investigation; validation; review and editing.

Zahra Rezaieyazdi: data curation; investigation; validation; review and editing.

Zahra Mirfeizi: data curation; investigation; validation; review and editing.

Alireza Sadeghi: data curation; investigation; validation; review and editing.

Mohsen Soroosh: data curation; investigation; project administration; validation; review and editing.

Hoda Kavosi: data curation; investigation; validation; review and editing.

Majid Alikhani: data curation; investigation; project administration; validation; review and editing.

Shayan Mostafaei: formal analysis; investigation; methodology; validation; review and editing.

Ethical approval The study protocol was approved by the Research Committee of Rheumatology Research Center and the Ethics Committee of Tehran University of Medical Sciences. The study was conducted in accordance with the Code of Ethics of the World Medical Association (Helsinki Declaration of 1975/83) for experiments involving humans and Good Clinical Practice guidelines.

Consent to participate A written informed consent was obtained from each participant according to the Declaration of Helsinki.

All authors approved the final version to be published and agreed to be accountable for all aspects of the work.

Disclosures None.

The COVID-19 pandemic: a global health crisis

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COVID-19 Global rheumatology alliance. Characteristics associated with hospitalisation for COVID-19

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Incidence of COVID-19 in a cohort of adult and paediatric patients with rheumatic diseases treated with targeted biologic and synthetic diseasemodifying anti-rheumatic drugs

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Behçet's disease

2012 revised international Chapel Hill consensusconference nomenclature of vasculitides

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The international criteria for Behçet's disease (ICBD): a collaborative study of 27 countries on the sensitivity and specifcity of the new criteria

International Study Group for Behçet's Disease (1990) Criteria for diagnosis of Behçet's disease

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Severity of COVID-19 and survival in patients with rheumatic and inflammatory diseases: data from the French RMD COVID-19 cohort of 694 patients

Covid-19 in immunemediated inflammatory diseases -case series from New York

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