Recent Advances in Kawasaki Disease

Kyu Yeun Kim; Dong Soo Kim

doi:10.3349/ymj.2016.57.1.15

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Kim and Kim: Recent Advances in Kawasaki Disease

Review Article

Yonsei Medical Journal 2016; 57(1): 15-21.

Published online: 30 November 2015

DOI: https://doi.org/10.3349/ymj.2016.57.1.15

Recent Advances in Kawasaki Disease

Kyu Yeun Kim, Dong Soo Kim

Division of Infectious Disease and Immunology, Department of Pediatrics, Yonsei University College of Medicine, Severance Children's Hospital, Seoul, Korea.

Corresponding author: Dr. Dong Soo Kim, Division of Infectious Disease and Immunology, Department of Pediatrics, Yonsei University College of Medicine, Severance Children's Hospital, 50-1 Yonsei-ro, Seodaemun-gu, Seoul 03722, Korea. Tel: 82-2-2228-2057, Fax: 82-2-393-9118, dskim6634@yuhs.ac

Received 17 June 2015

(open-access):

This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License (http://creativecommons.org/licenses/by-nc/3.0/) which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.

Abstract

Kawasaki disease (KD) is characterized with acute systemic vasculitis, occurs predominantly in children between 6 months to 5 years of age. Patients with this disease recover well and the disease is self-limited in most cases. Since it can lead to devastating cardiovascular complications, KD needs special attention. Recent reports show steady increases in the prevalence of KD in both Japan and Korea. However, specific pathogens have yet to be found. Recent advances in research on KD include searches for genetic susceptibility related to KD and research on immunopathogenesis based on innate and acquired immunity. Also, search for etiopathogenesis and treatment of KD has been actively sought after using animal models. In this paper, the recent progress of research on KD was discussed.

Keywords: Kawasaki disease, genetics, pathogenesis, animal models

INTRODUCTION

Kawasaki disease (KD) was first reported in 1967 by T. Kawasaki, a Japanese pediatrician.1 The first Korean KD patient was reported in 1973.2 Since then, the incidence of this disease has increased continuously. KD is characterized with acute systemic vasculitis that occurs predominantly in children between 6 months to 5 years of age. Although the clinical symptoms of KD are well characterized, the causes of this disease are not yet known. For this reason, KD is usually diagnosed by clinical symptoms, such as a fever for 5 days or more, bilateral nonpurulent conjunctival congestion, changes of the lips and oral mucosa, polymorphous exanthema along the trunk, changes of the peripheral extremities and subsequent desquamation of finger tips, and nonpurulent cervical lymphadenopathy over 1.5 cm in size (Table 1). Other than these criteria, erythema on Bacille Calmette-Guérin (BCG) vaccination sites is also thought to be an important finding in children younger than the age of 2 years.3 This is an especially important finding for KD patients in Korea, since BCG vaccination is included in a national immunization program (NIP) during the neonatal period.

Patients with this disease recover well, and the disease is self-limited in most cases. However, since it can lead to devastating cardiovascular complications, KD carries great clinical importance and needs special attention. Among cardiovascular complications, coronary artery lesions in particular can lead to long term morbidity and mortality. Without proper treatment in a timely manner during the acute phase of coronary artery complications, about 20% of patients develop coronary artery aneurysm. Giant aneurysm, with a diameter exceeding 8 mm, is known to develop in about 0.5-1% of KD patients. Once a giant aneurysm is formed, recovery is almost impossible and can result in coronary stenosis, obstruction, or acute thrombosis. These complications cause ischemic heart disease and/or myocardial infarction later and may also cause rare but fatal sudden cardiac death in children.4 5 In particular, occurrence of myocardial infarction results in poor prognosis with reported mortality after the first myocardial infarction at 22% and with subsequent episodes of myocardial infarction causing 70-80% mortality.6

In developed countries, including South Korea, incidences of congenital heart disease are significantly diminishing, although KD still ranks as the most common cause for acquired heart disease in children. In fact, the prevalence of KD in South Korea is second only to Japan. Recent reports show steady increases in the prevalence of KD per 100000 children less than 5 years old: 86.4 in 2000 to 2002, 105.0 in 2003 to 2005, 113.1 in 2006 to 2008, and 134.4 in 2011. Hence, KD is not regarded as a rare disease.7 Interestingly, while Japan and South Korea show continuous increase in incidence,7 United States and Canada showed constant prevalences without increase.8

The etiology of KD has been studied extensively, and viral or bacterial infections, autoimmune factors, and genetic factors have been suggested. It is noteworthy to mention high prevalence of KD in children between 6 months and 5 years old, when maternal immune function decreases. Other points to note include a self-limited clinical course without specific treatment and the epidemic nature of occurrence patterns. These points raise suspicions of an infectious disease; however, specific pathogens have yet to be found.

Almost 50 years have passed since KD was first recognized. Recent advances in research on KD include searches for genetic susceptibility related to KD and research on immunopathogenesis based on the idea that innate immunity has a more prominent role than the acquired immunity. Also, search for etiopathogenesis and treatment of KD has been actively sought after using animal models. This paper will present the recent progress of research on KD.

GENETIC SUSCEPTIBILITY RELATED TO KD

In understanding the pathophysiology of KD, genetic susceptibility has received much attention owing to the likely occurrence patterns in specific races and families. According to data published in 2005, incidence rates per 100000 children under age of 5 were 134.2 for Japan, 104.6 for Korea, and 66 for Taiwan, compared to reports of 18.5 in US, 8.1 in UK, and 6.2 in Sweden. Also, according to reports of an epidemiological survey in California, US from 1995 to 1999, the incidence rate per 100000 children under the age of 5 years old was 15.3. However, the incidence rates according to ethnic background were as follows: 35.3 for Asians, 24.6 for Blacks, 14.7 for Caucasians, 9.6 for Hispanics, and 8.6 for Native Americans.9 In an epidemiology survey taken in Hawaii from 1996 to 2001, incidence rates per 100000 children under the age of 5 were 35.3 for Caucasians and 197.7 for Japanese living in Hawaii. This incidence rate for Japanese children was even higher than the incidence rate in Japan and shows that prevalence among races is clearly different.10

Reports also have been made on family history. Matsubara, et al.11 have reported KD occurred five times in three siblings among one family within 6 years. Several studies have found incidence rates among siblings to be 1.4 to 2.1%; this is much higher than that for the general population.12 13 Also, as the first generation patients with initial KD go into reproductive years, increasing incidences in their children, a familial incidence rate, have been reported.14 These differences in ethnicity and family suggest genetic factors play a strong role in the development of KD.

Initial research on genetic susceptibility has mainly focused on human leukocyte antigen (HLA) and allotypes of immunoglobulin. HLA-DRB1, HLA B5, Bw51, and Bw4415 16 17 18 and kappachainallotype Km1 and heterozygocity of Km1 with Gm and etc.19 are reported in association with susceptibility to KD. Huang, et al.20 reported HLA-DRB1 is not associated with coronary aneurysm in Taiwanese patients, and Barron, et al.21 reported that no association could be found between HLA class II allele and KD.

Recently, many studies on various genes associated with different immunologic reactions among diverse groups have been undertaken. Associations with ethnicity, region, and gender have shown different results, and have been interpreted as differences in genetic background among ethnic groups.

Searches for genes associated with KD are still ongoing and Table 2 lists the candidate genes that have been studied to date.22 23

Ongoing genetic research has sought to find associations with susceptibility to KD, severity of KD, contraindications to immunoglobulin treatment, and development of coronary artery complications. With the start of genome-wide association studies (GWAS), remarkable progress has been made. Currently, the most interesting candidates of KD-susceptibility genes are the inositol 1,4,5-triphosphate 3-kinase (ITPKC) gene, caspase-3 (CASP3) gene, B lymphocyte kinase (BLK), CD40 gene, Fc fragment of IgG low affinity IIa receptor (FCGR2A), and HLA. Recent reports from meta-analysis of GWASes from Japan, Taiwan, and Korea have shown that the above genes hold significant value within these three countries (Table 3).24 Differences in single nucleotide polymorphisms (SNPs) of genes, excluding previously reported SNPs of ITPKC genes by Onouchi,25 were reported. Onouchi25 also reported different risk allele frequencies among Japan, Taiwan, and Europe populations, which reflect differences between ethnicity.

Japan shows the highest incidence of KD worldwide, and a nationwide GWAS was executed on 78 families with KD among siblings. The results showed the strongest associations in 12q24 and 19q13.2 regions.26 In 2008, this research team surveyed and analyzed 1222 SNPs from 1671 Japanese individuals (KD patients: 637, normal control: 1034) and 209 family members with a family history of KD. In doing so, functional SNPs with highly significant associations with KD were found in ITPKC, which is present in the 19q13.2 region of the human chromosome. This result was also confirmed through family analysis. These results showed similar trends in not only Japanese, but American children as well. Thereafter, the functional SNP found and analyzed by the study has been reported to have a high susceptibility to KD and to increase risk of coronary complications in both Eastern and Western populations.27

ITPKC, which is a secondary messenger molecule involved in the Ca⁺⁺/NFAT signal pathway, acts as a negative regulator of T-cell activation. ITPKC polymorphism results in increased activation of T cells with an increased expression of cytokines.27 This can result in more prolonged expansion of proinflammatory T cells during the acute phase, which may lead to KD susceptibility and disease severity.

However, in Koreas, researchers have yet to find a significant polymorphism of ITPKC genes. Rather, the rs4236089 C allele in chloride intracellular channel 5 (CLIC5), located at 6p21.1, has been reported to be very important.28 This discrepancy may be because Japanese and Americans have different genetic backgrounds than Koreans. Reports from Taiwan also show differences in polymorphism incidences of ITPKC genes attributed to differences in ethnicity.29 Interestingly, Taiwan study results showed an association between ITPKC gene polymorphism and erythema of BCG vaccination sites. This observation requires further investigation to see whether other gene polymorphisms exert synergistic effects.

Onouchi, et al.30 also reported that a SNP within the CASP3 gene located on 4q34-35 was associated with KD susceptibility by a positional candidate gene study. This was significantly associated with KD susceptibility in both Japanese and Euro-American populations. CASP3 is associated with apoptosis of immature cells. The G to A substitution within exon 1 of CASP3 (rs113420705) reduces the binding of NFAT to the DNA surrounding the SNP and then decreases the transcription of CASP3 mRNA, which in turn activates immune cells to increase cytokines expression. This might lead to increased susceptibility of KD. However, CASP3 gene polymorphism has not been shown to be associated with development of coronary arterial lesion (CAL) or inadequate response to IVIG.

Interestingly, functional SNPs in both ITPKC and CASP3 genes confer unresponsiveness of patients to IVIG and risk for CAL.31 This might be from synergistic effects of genetic variants of ITPKC and CASP3, which could be observed in other diseases.32 33 Based on these results, administration of cyclosporine A for the treatment of IVIG-resistant KD patients is theoretically feasible, because cyclosporine A suppresses activation of NFAT. Currently, cyclosporine A is already being used34 in treatment and further research projects are ongoing.

Another study showed a strong association for the susceptibility of KD with rs1801274 on FCGR2A.35 FCGR2A is expressed on the surface of various immune cells, such as dendritic cells, monocytes, macrophages, and neutrophils, and transduces activation signals into the cell when ligated with immune complexes.36 Evidence of immune activation during the acute phase of KD might be activated upon signaling through FCGR2A ligation with circulating immune complex, which can be found in the sera of KD patients.37

In 2012, two GWAS studies35 38 independently reported significant associations with KD that were observed in the FAM167A-BLK region on chromosome 8p23-p22. The association peak in this locus was located at the intergenic region between BLK and FAM167A. BLK is a src family tyrosine kinase expressed mainly in B cells and involved in B cell receptor signal transduction.39 This may indicate possible involvement of B cells for the development of KD.40 41 Moreover, BLK is required in the development of IL-17-producing γδT cells in mice.42 During the acute phase of KD, increased IL-17 levels have been reported,43 which might be associated with polymorphism of BLK. This might be associated with dysregulation of Th17/Treg cell imbalance in patients in patients with KD.44 However, the function of FAM167A molecule is unclear.

The association KD and SNPs around CD40 located on chromosome 20q12-q13.2 have also been reported in a Japanese GWAS38 and a Taiwanese GWAS.45 CD40 is expressed on B cells, as well as on monocytes/macrophages, endothelial cells, epithelial cells, smooth muscle cells, fibroblasts, and adipocytes. Following activation, its receptor, CD40L is upregulated. Elevated expression of CD40L during the acute phase of KD and significantly higher expression thereof in KD patients with CALs have been reported.46 It is likely that CD40-CD40L signal pathways may play a facilitating role in the disease progression of KD and could be a novel target of molecular therapies.

The association of HLA alleles with susceptibility to diseases, especially autoimmune diseases, is well known. Recently, a significant association of the SNPs in the HLA class II region, HLA-DQB2, and HLA-DOB, with KD was reported.38

IMMUNOPATHOGENESIS

Striking immune derangement has been reported to occur in acute KD, including various changes of immune cells, marked cytokine cascade stimulation, and endothelial cell activation (Table 4).

As shown in Table 4, many kinds of proinflammatory cytokines and chemokines are increased during the acute phase of KD. The key processes leading to coronary arteritis are still being clarified, although endothelial cell activation, activation of CD68+ monocytes/macrophages, CD8+ T lymphocytes, and oligoclonal IgA plasma cells appear to be involved in the development of coronary artery arteritis.48 49 50 The infiltration of IgA plasma cells in the respiratory tract, which is similar to findings in fatal viral respiratory infections, suggests a respiratory portal entry of an etiologic agent or agents.51 Rodó, et al.52 suggested that a KD agent is transported by the wind, possibly from a shared source region, across the Pacific. This hypothesis may support the plausibility of the entry of causative agents through the respiratory tract leading to the development of KD. Enzymes, such as MMPs,53 54 that are capable of damaging arterial cell wall integrity could be important in the development of aneurysmal dilatation of coronary arteries. CD40L, VGEF, MCP-1, and various cytokines also could play important roles in the development of vasculitis.46 55 56 57 58 59 60 With these results, Kim47 proposed important roles of acquired immune events in the development of vasculitis in KD.

Meanwhile, increased expression of toll-like receptor 2 (TLR2) on the peripheral blood monocytes suggests that innate immunity may be involved in the pathogenesis of KD.61 Ikeda, et al.62 also reported that innate immunity may be involved in the pathogenesis or pathophysiology of vasculitis in KD. Nishio, et al.63 reported that the pathological findings of Nod1 ligand-induced coronary arteritis in mice were consistent with those of human coronary artery lesions in the acute phase of KD. With this result, they suggest that the innate immune system could play an important role in the development of KD. Kusuda, et al.64 reported that serum KD-specific molecules possess molecular structures common to microbe-associated molecular pattern (MAMP) from Bacillus cereus, Bacillus subtilis, Yersinia pseudotuberculosis, and Staphylococcus aureus, and these molecules decreased after treatment with IVIG. Dr. Hara65 proposed that increased MAMPS and damage-associated molecular patterns (DAMPs) in the sera of acute phase patients with KD activate the immune system and vascular cells through innate immune pattern recognition receptor (PRR) to release chemokines and cytokines, thereby inducing KD in genetically predisposed individuals.

ANIMAL MODELS OF KD

Researchers have faced some obstacles in outlining the etiopathogenesis and treatment modalities for KD. First, usually KD patients come to the hospital after development of full-blown clinical symptoms. Thus, clinical samples can only be obtained from progressed stages of the disease. Second, tissue biopsy from coronary arteries, in which the most important complication of the disease occurs, cannot be obtained easily. Also, tissue samples of coronaries from autopsy are rare. Third, due to the peak incidence at an early age, collecting blood samples from KD patients and obtaining informed consent from guardians are difficult. For these reasons, development of animal models of KD is needed.

In 1979, Murata66 developed the first animal model of KD in DD and DDY strains of mice induced by Candida albicans water soluble fraction (CAWS). After this report, much effort has been made to develop various animal models of KD (Table 5).67

Taken together with the results of research from murine models of KD, Takahashi, et al.76 suggested a hypothesis for the development of vasculitis. Upon α-mannan binding to Dectin-2, Syk activates NF-kB. The NF-kB activates cytokine genes, including pro-IL-1β, IL-23, and IL-12. These cytokines stimulate differentiation of Th17 cells. Via Th17 cells, neutrophils and macrophages are recruited to inflammatory sites, stimulating the production of various pro-inflammatory cytokines and chemokines. Also, various cytokines and chemokines stimulate the activation of endothelial cells and vascular smooth muscle cells. Inflammatory cells adhere to activated endothelium and migrate within the vascular wall. Thereby, vasculitis develops. Motomura, et al.77 recently reported cardiac CD11_C+ macrophages, especially, play a pivotal role in the development of acute coronary arteritis in FK565-treated mice. This suggests innate immunity is important to the development of coronary vasculitis in KD. Nevertheless, further studies are needed to clarify the etiopathogenesis of KD.

CARDIAC SEQUELAE

Generally, KD patients without known cardiac sequelae during the first month of KD appear to return to their previous (usually excellent) state of health without signs or symptoms of cardiac impairment.78 However, identification of appropriate long term follow-up of these patients has proven difficult, because no clear picture of the potential sequelae of the disease without coronary artery aneurysms has emerged. Some authors have suggested that KD survivors involve increased arterial stiffness and are more likely to develop hypertension.79 80 A Japanese registry study showed that for KD patients, mortality after the acute phase of the disease is increased only in males with early cardiac lesions, such as aneurysms. However, this group had a standardized mortality ratio of 2.6, with the major cause of death arising from noncardiac origins.81 82 Recently, Holve, et al.83 also reported that long-term cardiac outcomes encompass a low rate of adverse cardiovascular events up to age 21. Meaningful knowledge about long-term myocardial function, late-onset valvular regurgitation, and coronary artery status in this population awaits careful surveillance in the future decades.

CONCLUSION

Though almost 50 years has passed since KD was first recognized, many topics remain to be clarified, including etiology, immunopathogenesis, genetics, development of coronary artery aneurysms, treatment of IVIG resistant patients, and long-term cardiac sequelae. In the future, overcoming KD will reflect the efforts of many researchers in various fields.

Figures and Tables

Table 1

Criteria for Diagnosis of KD

Fever for 5 days or more, plus four of the following five
1.	Changes of the peripheral extremities
	Erythema of the palms and soles, diffuse edema of the hands and feet
	Subsequent desquamation of the fingertips
2.	Polymorphous exanthema
3.	Bilateral nonpurulent conjunctival congestion
4.	Changes of the lips and oral mucosa
4.	Red, dry, cracked lips, strawberry tongue, injection of the oral and pharyngeal mucosa
5.	Acute, nonpurulent cervical lymphadenopathy >1.5 cm in size

KD, Kawasaki disease.

Table 2

Candidate Genes Associated with KD22 23

Cytokines

IL-1β, IL-1Ra, IL-4, IL-6, IL-10, IL-18, MCP-1, TGFB2, TGFBR2, SMAD

Chemokines

CXCR1, CXCR2, CX3CR1, CCR2, CCR3, CCR5, CCL3LI

Matrix metallopeptidases

MMP2, MMP3, MMP9, MMP12, MMP13, TIMP2

Fc fragment of IgG, low affinity

FCGR2A, FCGR2B, FCGR3A, FCGR3B

HLA

Bw15, Bw22J, Bw22J2, Bw44, Bw51, B35, B37, Cw09, DRB3^*031⁺

Others

MTHFR, CRP, SLC11A1, UGT1A1, AGTR1, VEGFA, VEGF2, ACE, HMOX1, CD14, CD40, MICA, PAFAH, eNOS, iNOS, MBL

KD, Kawasaki disease.

Table 3

Novel Susceptibility Locus for KD from the Meta-Analysis of Three GWASes24

Gene	SNP	p value	SNP (Onouchi)25
ITPKC	rs28493229	3.07×10^-9	rs28493229
CASP3	rs2720377	2.66×10^-9	rs113420705
BLK	rs2736340	1.23×10^-16	rs2254546
CD40	rs1883832	1.76×10^-8	rs4813003
HLA class 2	rs189914842	4.57×10^-11	rs2857151

KD, Kawasaki disease; GWASes, genome-wide association studies; SNP, single nucleotide polymorphism; ITPKC, inositol 1,4,5-triphosphate 3-kinase; CASP3, caspase-3; BLK, B lymphocyte kinase; HLA, human leukocyte antigen.

Table 4

Evidence of Derangement of the Immune System in Acute KD (Modified from Kim47)

Cytokines

TNF-α, TNF-β, p60 soluble TNF-R, IL-1β, IL-2, soluble IL-2R, IL-4, IL-6, IL-8, IL-10, IL-15, IL-17, IL-18, IL-20, IFN-α, IFN-γ, TGF-β

Chemokines

MIP-1, MCP-1β, MIF, RANTES

T lymphocytes

DR+ CD4 and CD8, Vβ2 and Vβ8 T cells, CD40L, Imbalance of Th17/Treg cells

B lymphocytes

Activated B cells spontaneously secreting Ig, cytotoxic IgM Ab to endothelial cells

Circulating immune complex, Ab to EBV, Ab to 65kD HSP, Ab to thrombin-III, Ab to ANCA

Oligoclonal expansion of VκIII and VH, CD5+ B cells

Monocytes/macrophages

Increased number of activated cells, TLR2, VEGF

KD, Kawasaki disease; TLR2, toll-like receptor 2.

Table 5

The History of Animal Models of KD (Modified from Chun, et al.67)

Researchers	Animal	Inducers	Results
Murata66	DD an DDY mice	CAWS	Coronary arteritis
Lehman, et al.68	C57BL/6, BALB/c mice	Group B Lactobacillus	Coronary arteritis
Felsburg, et al.69	Young dogs	Naturally occurred	Necrotizing vasculitis
Onouchi, et al.70	Weanling rabbits	Serum sickness	Coronary arteria dilatation
Duong, et al.71	C57BL/6, BALB/c mice	Group B Lactobacillus casei cell wall extract	Coronary arteritis
Takahashi, et al.72	CD-1, C57BL/6N, C3H/HeN, DBA/2N, CBA/JN, BALB/c mice	CAWS	Systemic vasculitis
Ohno73	DBA/2, C3H/HeN mice	CAWS	Coronary arteritis
Nakamura, et al.74	C57BL/6 mice	BCG crude extract of M. intracellulare	Autoimmune vasculitis
Schulte, et al.75	C57BL/6, RAG1-/- B6, B-null mice	Group B Lactobacillus casei cell wall extract	Coronary arteritis
Chun, et al.67	PD-1-/- BALB/c, PD-1-/- C56BL/6	BCG	Coronary arteritis
Chun, et al.67	PD-1-/- BALB/c, PD-1-/- C56BL/6	HSP65	Systemic vasculitis

KD, Kawasaki disease; CAWS, Candida albicans water soluble fraction; BCG, Bacille Calmette-Guérin.

Notes

The authors have no financial conflicts of interest.

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Recent Advances in Kawasaki Disease

Abstract

INTRODUCTION

GENETIC SUSCEPTIBILITY RELATED TO KD

IMMUNOPATHOGENESIS

ANIMAL MODELS OF KD

CARDIAC SEQUELAE

CONCLUSION

Figures and Tables

Table 1

Criteria for Diagnosis of KD

Table 2

Candidate Genes Associated with KD2223

Table 3

Novel Susceptibility Locus for KD from the Meta-Analysis of Three GWASes24

Table 4

Evidence of Derangement of the Immune System in Acute KD (Modified from Kim47)

Table 5

The History of Animal Models of KD (Modified from Chun, et al.67)

Notes

References

Candidate Genes Associated with KD22 23