key: cord-292719-n5lg43tr
authors: Chang, Luan-Yin; Lu, Chun-Yi; Shao, Pei-Lan; Lee, Ping-Ing; Lin, Ming-Tai; Fan, Tsui-Yien; Cheng, Ai-Ling; Lee, Wan-Ling; Hu, Jen-Jan; Yeh, Shu-Jen; Chang, Chien-Chih; Chiang, Bor-Luen; Wu, Mei-Hwan; Huang, Li-Min
title: Viral infections associated with Kawasaki disease
date: 2014-02-01
journal: J Formos Med Assoc
DOI: 10.1016/j.jfma.2013.12.008
sha: 
doc_id: 292719
cord_uid: n5lg43tr

BACKGROUND/PURPOSE: Kawasaki disease (KD) is a disease of unknown cause. To investigate the infectious etiology of Kawasaki disease, we initiated a prospective case-control study to investigate possible links between common viral infections and Kawasaki disease. METHODS: We enrolled 226 children with KD and 226 age- and sex-matched healthy children from February 2004 to March 2010. Throat and nasopharyngeal swabs were taken for both viral isolation and polymerase chain reaction (PCR) for various viruses. RESULTS: The mean age of the 226 KD cases was 2.07 years, and the male to female ratio was 1.43 (133 boys to 93 girls). Their mean fever duration was 7.5 days with a mean peak temperature of 39.7°C. In addition to the typical symptoms of fever, neck lymphadenopathy, lip fissure and/or strawberry tongue, skin rash, nonpurulent bulbar conjunctivitis, palm/sole erythema, and induration followed by periungual desquamation, these KD cases also exhibited cough (69%), rhinorrhea (58%), and diarrhea (45%). Cases of KD had a significantly higher positive rate of viral isolation in comparison with the control group (7.5% vs. 2.2%, p = 0.02). Compared with the control group, cases of KD were more likely to have overall positive rates of viral PCR (50.4% vs. 16.4%, p < 0.001) and for various viruses including enterovirus (16.8% vs. 4.4%, p < 0.001), adenovirus (8.0% vs. 1.8%, p = 0.007), human rhinovirus (26.5% vs. 9.7%, p < 0.001), and coronavirus (7.1% vs. 0.9%, p = 0.003). CONCLUSION: We found that some common respiratory viruses, such as adenoviruses, enteroviruses, rhinoviruses, and coronaviruses, were associated with KD cases.

Kawasaki disease (KD) is an acute systemic febrile illness of unknown etiology which predominantly affects children under 5 years of age. Initially described in 1967 by Tomisaku Kawasaki, 1 it is now the most common cause of acquired heart diseases in children in the developed world due to the less frequent occurrence of rheumatic heart disease. There have been reports of differing incidence rates in different countries. Asian countries are supposed to have higher incidences of KD (30e200/per 100,000 children under 5 years of age) than most of the Western countries (3.5e10/per 100,000 children under 5 years of age). 2e10 The etiology of KD is still controversial and infections are considered to be one of the predisposing factors. The infectious evidence of Kawasaki disease includes temporal clustering and marked seasonality, geographic clustering, family clustering, a high association between Kawasaki disease and infectious disease surveillance, and age distribution, for which the highest incidence rates are seen among 6 monthe2-year-old children who have low maternal antibodies and are most susceptible to infections in general. 11e14 We hypothesize that infections with certain viruses may elicit systemic inflammation, and further small and median sized vasculitis, so-called Kawasaki disease, in certain hosts because we found a higher incidence of KD among males, young children, and Asian populations. We thus carried out a prospective case-control study to investigate the association of common viral infections with Kawasaki disease to test the above hypothesis. We enrolled Kawasaki disease cases that had fever for over 5 days and at least four of the following five manifestations: neck lymphadenopathy, lip fissure and/or strawberry tongue, skin rash, nonpurulent bulbar conjunctivitis, palm/sole erythema, and induration followed by periungual desquamation. The onset of KD illness cases was defined as the 1st day of fever onset.

After informed consent was obtained from the parents, a questionnaire-styled interview was carried out to solicit clinical symptoms and previous contact history with ill household members or with ill people from outside of the household. The illness included sore throat, rash, fever, conjunctivitis, cough, rhinorrhea, abdominal pain, and diarrhea. Clinical laboratory data and coronary arterial lesions were collected from the participants, and all received intravenous immunoglobulin 2 g per Kg plus low-dose aspirin (3e5 mg per Kg). If fever persisted for 2 days after use of intravenous immunoglobulin, retreatment with intravenous immunoglobulin was administered.

Two-dimensional echocardiography was performed in all patients during hospitalization and was repeated at convalescence, 2 weeks, and 8 weeks after discharge. Coronary arterial lesions were defined as coronary arterial dilatation/ectasia, aneurysm, and increased echogenecity, irregularity of vascular wall, or coronary artery aneurysm. A coronary artery aneurysm was defined as having a lumen diameter (inner border to inner border) of !3 mm in KD cases less than 5 years old and !4 mm in cases less than 5 years old, and giant aneurysm was defined as a lumen diameter of !8 mm for any one echocardiography. We took nasopharyngeal swabs and throat swabs from KD cases on the 1st day of hospitalization. These swabs were processed for both viral isolation and polymerase chain reaction (PCR) for various viruses.

For the healthy control group, we enrolled children who were age-and sex-matched with the KD cases, and who did not have preceding illness for the 2 weeks prior to enrollment. The preceding illness included sore throat, rash, fever, conjunctivitis, cough, rhinorrhea, abdominal pain, and diarrhea. These children were kindergarteners or children who visited our baby wellness clinics for vaccination. Informed consent was obtained from parents of all children in the control group. We also took throat swabs and nasopharyngeal swabs from the control children for viral isolation and viral PCR.

Throat or nasopharyngeal swabs were submitted for virus isolation. Samples were inoculated into human embryonic fibroblast, LLC-MK2, Hep-2, and rhabdomyosarcoma cell cultures. When a cytopathic effect involved more than 50% of the cell monolayer, cells were scraped and subjected to indirect fluorescent antibody staining with specific antibodies or typed by specific methods according to the suspected types of viruses.

RNA and DNA extraction from throat swabs, and nasopharyngeal swabs were performed using MagNA Pure LC 2.0 System and MagNA Pure LC Total Nucleic Acid Isolation Kit (Roche Applied Science, Roche Diagnostics, Indianapolis, IN, USA). The primers and probes for enterovirus, adenovirus, influenza B, rhinovirus, metapneumovirus real-time PCR, and coronavirus PCR are presented in Table 1 . Primers and probes for pan-enterovirus were selected based on highly conserved regions in the 5 0 -untranslated region of the enterovirus genome, and design of primers of other viruses are also based on their most conserved regions. The detection limitation of each virus was 100 copies for enterovirus, 100 for adenovirus, 60 for influenza B virus, 50 for rhinovirus, 50 for metapneumovirus, and 10,000 for coronavirus.

If the samples had positive viral isolation or PCR, further molecular typing was done. The detailed method of the viral molecular typing is in the Supplementary Material online.

This study was conducted in Taiwan only and institutional review board (IRB) approval was obtained from National Taiwan University Hospital (IRB number 9361700624).

Written informed consent was obtained from the parents of all participants.

The c 2 test was used to compare the rates of viral isolation and PCR of various viruses between KD cases and the control children. A p value < 0.05 was considered statistically significant.

In total, 226 KD cases as well as 226 age-and sex-matched control children were enrolled. The demographic characteristics of the KD cases and the control children are shown in Table 2 . The mean age of KD cases was 2.07 AE 1.76 years, the median (range) was 1.57 (0.12e9.43) and the male to female ratio was 1.43 (133 to 93). Their age distribution is shown in Figure 1 ; about 62% were younger than 2 years old. The demographic characteristics of the control children were comparable to those of the KD cases. Table 3 shows the clinical manifestations. Their mean (SD) fever duration was 7.5 (2.4) days with mean peak temperature of 39.7 C. For the typical clinical features of KD, rash was found in 92% of the cases, BCG scar erythema and induration in 44%, palm and/or sole erythema and induration in 72%, desquamation in 96% (96% of periungual desquamation and 24% of peri-anal desquamation) and bulbar conjunctivitis in 97%, red lip with fissure and/or strawberry tongue in 95%, and neck lymphadenopathy in 40% of cases. KD cases also had other clinical features including cough (69%), rhinorrhea (58%), and diarrhea (45%). During the acute stage, 14 (6.2%) children required intravenous immunoglobulin retreatment, 116 (51%) patients had coronary arterial lesions, and 28 (12%) patients had coronary arterial aneurysm.

For the contact history and the rate of household transmission, 60.8% of the cases had positive contact history: 51.7% of cases had contact with ill household members and 9.1% had positive contact with extra-familial ill people 1e10 days prior to their KD illness. In 129 (57%) of the 226 families, at least one of the other family members had an illness after the onset of disease in the KD cases. Table 4 shows the results of viral isolation and Table 5 shows the results of viral PCR between the KD cases and the control participants. KD cases had significantly higher rates of viral isolation (7.5% vs. 2.2%, p Z 0.02) than the control children. They also had significantly higher positive rates of PCR (50.4% vs. 16 Table 6 .

As for further typing, only one case of echovirus 6 and one case of EV71 were identified among the 40 enteroviralpositive KD cases and the other enterovirus serotyping failed due to low viral titer. For adenovirus, six cases of 28 (12) Data are presented as n (%), unless otherwise indicated. KD Z Kawasaki disease; SD Z standard deviation. a Coronary arterial lesions were defined as coronary arterial dilatation/ectasia, aneurysm, increased echogenicity or irregularity, and coronary artery aneurysm. b A coronary artery aneurysm was defined as having a lumen diameter (inner border to inner border) of !3 mm in KD cases <5 years old and !4 mm in cases !5 years old. serotype 3, five cases of serotype 5, three cases of serotype 2, one case of serotype 1, and one case of serotype 4 were identified in KD cases, whereas two cases of adenovirus serotype 2, one case of serotype 3, and one case of serotype 1 were identified in the control children. For coronavirus, 12 cases of human coronavirus NL63, three cases of human coronavirus 229E, and one case of human coronavirus OC43 were identified in KD cases whereas two of human coronavirus 229E were identified in the control children. For rhinovirus, 36 serotypes were identified and type C was the most common (7 cases) in the 60 rhinoviruspositive KD cases whereas 14 serotypes were identified and the Antwerp RV 98/99 type was the most common (5 cases) among the 22 rhinovirus-positive control children.

Overall, 119 (52.7%) KD cases had positive viral results by either viral isolation or PCR. However, KD cases with positive viral results did not have significantly higher percentages of needing intravenous immunoglobulin retreatment (4% vs. 8%, p Z 0.18), coronary arterial lesions (53% vs. 50%, p Z 0.70), or coronary arterial aneurysm (11% vs. 14%, p Z 0.45) than KD cases without positive viral results.

This was a prospective study to investigate the association of common viruses with Kawasaki disease. We found that cases of KD frequently had a cough (69%), rhinorrhea (58%), and diarrhea (51%) in addition to the typical symptoms of KD; several common respiratory viruses were also more frequently detected in cases of KD than in the control children. We propose that heterogeneous infectious agents, such as common viruses found in our study, may trigger Kawasaki disease in young children with certain genetic backgrounds or susceptibility.

The leading theory of KD etiology is that a ubiquitous infectious etiologic agent, that usually results in asymptomatic or mild infection in most people, causes KD in a small subset of genetically predisposed children. In our study, approximately 60% of KD cases had a preceding contact history with people of febrile, respiratory, or gastrointestinal illness, and KD cases frequently had cough (69%), rhinorrhea (58%), and diarrhea (45%), which supported certain kinds of viral infections. A winterespring predominance of KD cases in non-temperate climates also suggests the association of KD with some kinds of viral infections, 11 particularly a respiratory infection, and this theory is supported by the two articles which reported a preceding history of respiratory illness in some KD patients. 7, 8 The other infectious evidence of Kawasaki disease includes geographic clustering, family clustering, high association between Kawasaki disease and infectious disease surveillance, and age distribution, with the highest incidence rates among children aged from 6 months to 2 years old who have low maternal antibodies and are most susceptible to infections in general. 11e14 Many studies worked on a certain single pathogen to be associated with KD. Various infectious agents including bacterial (Staphylococcus aureus, group A Streptococcus, Yersinia pseudotuberculosis, Klebsiella pneumoniae, Pseudomonas aeruginosa), viral (parvovirus B19, Eps-teineBarr virus, CMV, HHV6, retrovirus, rotavirus, para-influenza virus, New Haven coronavirus, measles, chickenpox, dengue fever), Chlamydiae pneumoniae, Mycoplasma pneumoniae, Rickettsial organisms, and so-called KD agent, a viral etiology characterized by intracytoplasmic inclusion bodies, have been found to be associated with KD. 15e39 However, at present, links between any of these individual agents and KD have not been irrefutably established.

Although KD had temporal clustering, different seasonality was found in different countries. For example, studies from Europe and Canada reported a higher incidence in winter, 40 whereas Taiwan and Korea have the highest incidence rates of KD during the summer, 11, 41 Beijing and Hong Kong in the spring and summer, and Japan in January and summer. 3, 42, 43 Such seasonality and temporal clustering of KD suggests that different infectious diseases in different countries might trigger this clustering presentation. In the summer, enterovirus infection was one of the most common infections in young children in Taiwan. We also detected enterovirus most frequently in KD cases, which links enterovirus with KD in the summer. Other respiratory viruses, such as adenoviruses, may play an important role during other seasons because adenoviruses circulate all year-round in Taiwan. We proposed that it was not the same infectious etiology, but rather heterogeneous infectious agents in different areas and different seasons, which trigger KD; there was no single pathogen reported to be associated with KD worldwide. That is to say, different pathogens might be responsible for KD in different countries or different seasons. This may explain why no single pathogen was consistently found in cases with Kawasaki disease. For example, Jordan-Villegas et al 44 reported that 8.8% of KD patients had documented respiratory viral infections including rhinovirus, adenovirus, influenza, parainfluenza, and respiratory syncytial virus. A recent article also reported a case of KD associated with parainfluenza type 3 viral infection, 45 and another article reported adenovirus detection in some KD cases. 46 However, Kim et al 47 reported that there was no significant association between the presence of any of the 15 respiratory viruses and the incidence of KD. New tests or techniques for specific microorganisms may help us find the etiology of KD. 48, 49 In conclusion, we found that common respiratory viruses, such as enteroviruses, adenoviruses, rhinoviruses, and coronaviruses, were associated with KD. Heterogeneous infectious etiologies may be responsible for KD in different countries as well as during different seasons.

Pediatric acute febrile mucocutaneous lymph node syndrome with characteristic desquamation of fingers and toes: my clinical observation of fifty cases

Epidemiologic pictures of Kawasaki disease in Japan: from the nationwide incidence survey in 1991 and 1992

Epidemiologic study on Kawasaki disease in Beijing from

Kawasaki syndrome hospitalizations in the United States

Kawasaki syndrome hospitalizations and associated costs in the United States

Incidence of HenocheSchonlein purpura, Kawasaki disease, and rare vasculitides in children of different ethnic origins

Epidemiologic study of Kawasaki disease in Korea, 1997e1999: comparison with previous studies during 1991e1996

Kawasaki disease in Australia

Kawasaki disease in Sweden: incidence and clinical features

Kawasaki disease in Finland in 1982e1992

Epidemiological features of Kawasaki disease in Taiwan from

Changes in epidemic patterns of Kawasaki disease in Japan

Validity of the infectious disease surveillance system on comparison of nationwide surveys of Kawasaki disease during a 10-year period

Temporal and geographic clustering of Kawasaki disease in Japan

The pathogenesis of Kawasaki disease and superantigens

Lack of association between Kawasaki syndrome and Chlamydia pneumoniae infection: an investigation of a Kawasaki syndrome

Lack of association between Kawasaki syndrome and infection with parvovirus B19, human herpesvirus 8, TT virus, GB virus C/hepatitis G virus or Chlamydia pneumoniae

Kawasaki syndrome: description of two outbreaks in the United States

An epidemic of Kawasaki syndrome in Hawaii

Mucocutaneous lymph node syndrome (Kawasaki disease) in Israel. A review of 13 cases: is pseudomonas infection responsible?

Staphylococcal scalded skin syndrome, toxic shock syndrome, and Kawasaki disease

Coronary aneurysms in a patient with atypical Kawasaki syndrome and a streptococcal infection

Trial of isolation of a virus from sera of patients with Kawasaki disease

Kawasaki syndrome: a controlled study of an outbreak in Wisconsin

EpsteineBarr virus genome-positive T lymphocytes in a boy with chronic active EBV infection associated with Kawasaki-like disease

Kawasaki syndrome: issues in etiology and treatment

Human herpesvirus 6 infection and Kawasaki disease

Prevalence of antibodies to human herpesvirus 6 in different age groups, in children with exanthema subitum, other acute exanthematous childhood diseases, Kawasaki syndrome, and acute infections with other herpesviruses and HIV

EpsteineBarr virus and other herpesvirus infections in Kawasaki syndrome

Adenovirus infection in patients with Kawasaki disease

Possible role of Streptococcus pyogenes in mucocutaneous lymph node syndrome. XII. Variable responses of platelets in MCLS seem to be explainable by streptococcal pyrogenic exotoxin

Kawasaki disease and Epstein-Barr virus

Viruslike particles with reverse transcriptase activity associated with Kawasaki disease

Toxic shock syndrome toxin-secreting Staphylococcus aureus in Kawasaki syndrome

Kawasaki disease associated with streptococcal infection within a family

Serologic evidence that streptococcal superantigens are not involved in the pathogenesis of Kawasaki disease

Kawasaki syndrome associated with group A streptococcal and EpsteineBarr virus co-infections

Lack of association between Kawasaki syndrome and infection with Rickettsia conorii, Rickettsia typhi, Coxiella burnetii or Ehrlichia phagocytophila group

Cytoplasmic inclusion bodies are detected by synthetic antibody in ciliated bronchial epithelium during acute Kawasaki disease

Kawasaki syndrome hospitalizations in Ireland

Kawasaki disease in Korea

Kawasaki disease in Hong Kong

Seasonality and temporal clustering of Kawasaki syndrome

Concomitant respiratory viral infections in children with Kawasaki disease

Kawasaki disease associated with parainfluenza type 3 virus infection

Human adenovirus infection in Kawasaki disease: a confounding bystander

Detection rate and clinical impact of respiratory viruses in children with Kawasaki disease

A highly specific ELISA for diagnosis of 2009 influenza A (H1N1) virus infections

Seroprevalence of hepatitis virus infection in men who have sex with men aged 18e40 years in Taiwan

Supplementary data related to this article can be found at http://dx.doi.org/10.1016/j.jfma.2013.12.008.