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Kawasaki disease

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Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Dildar Hussain, MBBS [2], Arzu Kalayci, M.D. [3]

Synonyms and keywords: Mucocutaneous lymph node syndrome; Lymph node syndrome; Acute febrile vasculitic syndrome

For the heart in Kawasaki disease click here

Overview

Overview

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Dildar Hussain, MBBS [2]

Overview

Kawasaki disease, also known as lymph node syndrome, mucocutaneous node disease, infantile polyarteritis and Kawasaki syndrome, is a poorly understood self-limited vasculitis that affects many organs, including the skin, mucous membranes, lymph nodes, blood vessel walls, and the heart. There is no evidence that Kawasaki disease is contagious. It was first described in 1967 by Dr. Tomisaku Kawasaki in Japan. Kawasaki disease is predominantly a disease of young children, with 80% of patients younger than 5 years of age. Additional risk factors in the United States include Asian race and male sex. Kawasaki disease can cause vasculitic changes (inflammation of blood vessels) in the coronary arteries and subsequent coronary artery aneurysms. Common symptoms of Kawasaki disease include high grade fever, red eyes, bright red and cracked lips, red mucous membranes in the mouth, strawberry tongue, white coating on the tongue or prominent red bumps (papillae) on the back of the tongue, red palms of the hands and soles of the feet, swollen hands and feet, and rash. Intravenous immunoglobulin

(IVIG) and aspirin are indicated in Kawasaki disease.

Historical perspective

Kawasaki disease was first discovered by Dr. Tomisaku Kawasaki when he saw his first case of Kawasaki disease in Japan, in 1961. Later in 1967, Kawasaki published his first report on Kawasaki disease in Japanese. Dr Kawasaki also developed “Japan Kawasaki Disease Research Center” in 1990.

Classification

Patients whose illness does not meet the diagnostic criteria of Kawasaki disease, but who have fever and coronary artery abnormalities are classified as atypical or incomplete Kawasaki disease. For patients of atypical or incomplete Kawasaki disease, an evidence of coronary abnormalities or CAA’s must be shown on the echocardiogram.

Pathophysiology

The exact pathogenesis of Kawasaki disease is not fully understood. However, it is thought that Kawasaki disease is caused by either environmental, viral, or genetic causes. Kawasaki disease is defined as the systemic inflammation of the medium sized arteries and in multiple organs and tissues, which can lead to the associated conditions of hepatitis, interstitial pneumonitis, abdominal pain, vomiting, diarrhea, gallbladder hydrops, aseptic meningitis, irritability, myocarditis, pericarditis, valvulitis, pyuria, pancreatitis, and lymphadenopathy. On gross pathology, large or giant coronary artery aneurysms, thrombi containing aneurysms, decreases in luminal diameter, stenosis of the lumen and chronic inflamation are can be seen. On microscopic histopathological analysis of autopsied cases of Kawasaki disease, intracytoplasmic inclusion bodies are frequently observed in ciliated bronchial epithelial cells.

Causes

The exact cause of Kawasaki disease has not been identified. The current etiological theories center primarily on immunological causes for the disease, much research is being carried out to discover a definitive toxin or antigenic substance, possibly a superantigen, that is the specific cause of the disease. There are several hypothesis for the cause of Kawasaki disease, infectious agents thought to induce Kawasaki disease include, parvovirus B19, meningococcal septicemia, adenovirus, bacterial toxin–mediated, superantigens, cytomegalovirus, Epstein-Barr virus, human lymphotropic virus, klebsiella pneumoniae bacteremia, mycoplasma pneumoniae, mite-associated bacteria, measles, propionibacterium acnes, parainfluenza type 3 virus, rotavirus infection, rickettsia species and tick-borne diseases.

Differentiating Kawasaki disease from other diseases

Kawasaki disease must be differentiated from other diseases that cause different rash-like conditions and can be confused with Kawasaki disease. The various conditions that should be differentiated from Kawasaki disease include; infantile polyarteritis nodosa, juvenile idiopathic arthritis, leptospirosis, lyme disease, measles, mercury toxicity, pediatric rocky mountain spotted fever, toxic epidermal necrolysis, staphylococcal scalded skin syndrome, rheumatic fever, impetigoinsect bites, monkey pox, rubella, atypical measles, coxsackie virus, acne, syphilis, molluscum contagiosum, toxic erythema, rat-bite fever, parvovirus B19, cytomegalovirus, scarlet fever, Stevens-Johnson syndrome, varicella-zoster virus, chicken pox, meningococcemia, rickettsial pox, meningitis, toxic shock syndrome, roseola infantum (exanthem subitum), erythema infectiosum (fifth disease), enterovirus, dengue fever, drug – induced rash, infectious mononucleosis, pharyngoconjunctival fever, herpangina, and primary herpetic gingivostomatitis.

Epidemiology and Demographics

Kawasaki disease (KD) occurs worldwide, with the highest incidence in Japan, and it most often affects boys and younger children. KD may have a winter-spring seasonality, and community-wide outbreaks have been reported occasionally. In the continental United States, population-based and hospitalization studies have estimated an incidence of KD ranging from 9 to 19 per 100,000 children younger than 5 years of age. Approximately 4248 hospitalizations for Kawasaki disease, of which 3277 (77%) were for children under 5 years of age, were estimated among children younger than 18 years of age in the United States in the year 2000.

Risk factors

Common risk factors in the development of Kawasaki disease are due to a combination of non-modifiable and modifiable risk factors, that include environmental, genetic, and viral factors.

Screening

There is insufficient evidence to recommend routine screening for Kawasaki disease.

Natural History, Complications, and Prognosis

If left untreated, the symptoms will eventually relent, but coronary artery aneurysms will not improve, resulting in a significant risk of death or disability due to myocardial infarction. If treated in a timely fashion, this risk can be mostly avoided and the course of illness cut short. Patients with Kawasaki disease may progress to develop long term cardiovascular illness such as coronary artery disease, and pre-mature atherosclerosis. Common complications of Kawasaki disease include vasculitis and coronary artery aneurysms. Prognosis is generally excellent and the mortality rate of patients with Kawasaki disease is approximately 2%.

Diagnostic Criteria

Kawasaki disease is diagnosed clinically (by medical signs and symptoms), and there are no specific laboratory tests that can tell if someone has Kawasaki disease. It is normally difficult to establish the diagnosis, especially early in the course of illness, and frequently children are not diagnosed until they have seen a physician several times. Many other serious illnesses can cause similar symptoms, and must be considered in the differential diagnosis, including scarlet fever, toxic shock syndrome, and juvenile idiopathic arthritis. Classically, five days of fever plus four of five diagnostic criteria must be met in order to establish the diagnosis, and include, mucositis (erythema of the palatine mucosa), fissured erythematous lips, “strawberry tongue”, rash (polymorphus, usually urticarial erythematous rash mainly in external extremities. The rash can spread to trunk), extremities changes (edema of hands and feet, erythema of palms & soles, desquamation of fingertips, bilateral non-exudative conjuctival erythema), and cervical lymphadenopathy of at least 15 milimeters.

History and Symptoms

Kawasaki disease often begins with a high and persistent fever that is not very responsive to normal doses of acetaminophen or ibuprofen. The fever may persist and rise steadily for up to two weeks and is normally accompanied by irritability. Affected children develop red eyes, mucous membranes, and lips, a “strawberry tongue“, iritis, keratic precipitates (detectable by an ophthalmologist but usually too small to be seen by the naked eye), and swollen lymph nodes. Skin rashes occur early in the disease, and peeling of the skin in the genital area, hands, and feet may occur in later phases. Some of these symptoms may come and go during the course of the illness.

Physical Examination

Physical examination of patients with Kawasaki disease is usually remarkable for erythematous rash, irritability, and desquamation of skin and mucous membranes.

Laboratory Findings

Kawasaki disease is diagnosed by clinical presentation, although the laboratory findings are non-specific for the diagnosis of Kawasaki disease – normocytic anemia, thrombocytosis, with platelets ≥ 450×103/μL (after first week of acute disease), leucocytosis with white blood cell count ≥ 15,000/μL, elevated erythrocyte sedimentation rate, elevated liver enzyme levels, hypoalbuminemia with ≥ 3.0g/dL, elevated c-reactive protein, hyponatremia and sterile pyuria can be noted on laboratory investigations.

Electrocardiogram

Electrocardiogram in Kawasaki disease may demonstrate evidence of ventricular dysfunction or, occasionally arrhythmia due to myocarditis. However, in acute disease the electrocardiogram may demonstrate prolonged PR interval, non-specific ST changes, T-wave changes and increased Q/R ratio, which are consistent with myocarditis.

X Ray

Abnormal findings on chest x-ray may be found in Kawasaki disease, however, they are non-specific and may include; peribronchial cuffing, reticulogranular pattern, pleural effusion, atelectasis and air trapping. In rare circumstances, several years after resolution of the first episode within the elderly population, calcifications of the coronary artery will lead to coronary artery aneurysms. These aneurysms may be visualized using a plain radiograph. This presentation is described as an “Aunt Minnie” sequelae of Kawasaki disease.

Echocardiography and ultrasound

An ECG may be helpful in the diagnosis of Kawasaki disease. Findings on an ECG suggestive of Kawasaki disease include coronary artery dilatations, stenosis or aneurysms. Ultrasound may show hydrops (enlargement) of the gallbladder.

CT scan

CT angiography scan may be helpful in the diagnosis of Kawasaki disease. Findings on CT scan suggestive of Kawasaki disease include small coronary artery dilatations, aneurysms or stenoses. Angiography is the most sensitive and specific for assessment of the vessels.

MRI

There are no MRI findings associated with Kawasaki disease, however, magnetic resonance angiography can accurately define coronary artery aneurysms in patients with Kawasaki disease.  

Other Imaging Findings

There are no other imaging findings associated with Kawasaki disease.

Other Diagnostic Studies

Apart from the imaging studies already discussed previously, urinalysis, lumbar puncture, biomarkers and angiography may be helpful in the diagnosis of Kawasaki disease. Findings suggestive of Kawasaki disease include the presence of white blood cells, leukocytosis and coronary artery aneurysms, respectively.

Treatment

Medical Therapy

Intravenous immunoglobulin (IVIG) and aspirin are indicated in the treatment of Kawasaki Disease. It is imperative that treatment be started as soon as the diagnosis is made to prevent damage to the coronary arteries. Kawasaki disease and a couple of other indications are an exception to the use of aspirin in children, aspirin is otherwise normally not recommended for children due to its association with Reye’s syndrome. Children with Kawasaki disease should be hospitalized.

Surgery

Mechanical revascularization may be attempted in patients with coronary artery compromise.

Prevention

Primary prevention for Kawasaki disease is not applicable. Complications of the disease, however, may be prevented through the use of medical prophylaxis.

Historical Perspective

Historical Perspective

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Dildar Hussain, MBBS [2]

Overview

Kawasaki disease was first discovered by Dr. Tomisaku Kawasaki when he saw his first case of Kawasaki disease in Japan, in 1961. Later in 1967, Kawasaki published his first report of Kawasaki disease in Japanese. Dr Kawasaki also established the “Japan Kawasaki Disease Research Center” in 1990.

Historical Perspective

Discovery

The historical timeline on Kawasaki disease is described below:[1][2][3][4][5][6][7]

  • In 1961, Dr. Tomisaku Kawasaki saw his first case of Kawasaki disease.
  • In 1967, Kawasaki published his first report of Kawasaki disease in Japanese.
  • In the 1960s, pathologist Noboru Tanaka and pediatrician Takajiro Yamamoto disputed the early assertion of Kawasaki that Kawasaki disease was a self-limited illness with no sequelae.
  • In 1970, the first Japanese nationwide survey of Kawasaki disease was conducted and 10 autopsy cases of sudden cardiac death after Kawasaki disease were documented.
  • In 1973, at the University of Hawaii hospital, pathologist Eunice Larson, in collaboration with Benjamin Landing at the Los Angeles Children’s Hospital, retrospectively established a diagnosis of Kawasaki disease in a 1971 autopsy case.
  • In 1974, Tomisaku Kawasaki published the first English language report of 50 patients with Kawasaki disease.
  • By 1974, the link between Kawasaki disease and coronary artery vasculitis was definitively established.
  • In 1976, the first cases of Kawasaki disease outside of Japan were reported in Hawaii.
  • In 1988, the Committee on Infectious Diseases of the American Academy of Pediatrics declared IVIG treatment as the recommended therapy for Kawasaki disease.
  • In 1990, Dr Kawasaki established the “Japan Kawasaki Disease Research Center”.

Impact on Cultural History

  • In March 2006, Kawasaki disease was mentioned in the television programs Nip/Tuck and Without a Trace, and in the episode ‘All In” of the TV series House, it was inexplicably mentioned as a possible diagnosis for a 6 year old boy that was admitted with bloody diarrhea and coordination problems, as well as an elderly woman with unexplained respiratory, cardiovascular and neural deficiencies.
  • Maxie Jones, a fictional character on General Hospital suffers from it.
  • According to John Travolta and Kelly Preston, their son Jett Travolta also suffered from the disease.

References

  1. Burns, Jane C.; Kushner, Howard I.; Bastian, John F.; Shike, Hiroko; Shimizu, Chisato; Matsubara, Tomoyo; Turner, Christena L. (2000). “Kawasaki Disease: A Brief History”. Pediatrics. 106 (2): e27–e27. doi:10.1542/peds.106.2.e27. ISSN 0031-4005.
  2. Kawasaki Disease. Centers for Disease Control and Prevention (2013). http://www.cdc.gov/kawasaki/ Accessed on July 28, 2016.
  3. Kawasaki T (1967). “[Acute febrile mucocutaneous syndrome with lymphoid involvement with specific desquamation of the fingers and toes in children]”. Arerugi (in Japanese)|format= requires |url= (help). 16 (3): 178–222. PMID 6062087.
  4. Kawasaki T (1967). “[Acute febrile mucocutaneous syndrome with lymphoid involvement with specific desquamation of the fingers and toes in children]”. Arerugi (in Japanese)|format= requires |url= (help). 16 (3): 178–222. PMID 6062087.
  5. Episode 86 (4×16) – The Little Things (2 March, 2006)
  6. Kawasaki T (1967). “[Acute febrile mucocutaneous syndrome with lymphoid involvement with specific desquamation of the fingers and toes in children]”. Arerugi (in Japanese)|format= requires |url= (help). 16 (3): 178–222. PMID 6062087.
  7. Sánchez-Manubens J, Bou R, Anton J (2014). “Diagnosis and classification of Kawasaki disease”. J. Autoimmun. 48-49: 113–7. doi:10.1016/j.jaut.2014.01.010. PMID 24485156.

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Classification

Classification

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Dildar Hussain, MBBS [2]

Overview

Patients whose illness does not meet the diagnostic criteria of Kawasaki disease, but who have fever and coronary artery abnormalities, are classified as atypical or incomplete Kawasaki disease. For patients of atypical or incomplete Kawasaki disease, an evidence of coronary abnormalities or CAAs must be shown on the echocardiogram.

Classification

References

  1. Sánchez-Manubens J, Bou R, Anton J (2014). “Diagnosis and classification of Kawasaki disease”. J. Autoimmun. 48-49: 113–7. doi:10.1016/j.jaut.2014.01.010. PMID 24485156.
  2. Newburger, J. W.; Takahashi, M.; Gerber, M. A.; Gewitz, M. H.; Tani, L. Y.; Burns, J. C.; Shulman, S. T.; Bolger, A. F.; Ferrieri, P.; Baltimore, R. S.; Wilson, W. R.; Baddour, L. M.; Levison, M. E.; Pallasch, T. J.; Falace, D. A.; Taubert, K. A. (2004). “Diagnosis, Treatment, and Long-Term Management of Kawasaki Disease: A Statement for Health Professionals From the Committee on Rheumatic Fever, Endocarditis, and Kawasaki Disease, Council on Cardiovascular Disease in the Young, American Heart Association”. PEDIATRICS. 114 (6): 1708–1733. doi:10.1542/peds.2004-2182. ISSN 0031-4005.

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Pathophysiology

Pathophysiology

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Dildar Hussain, MBBS [2], Sabawoon Mirwais, M.B.B.S, M.D.[3]

Overview

The exact pathogenesis of Kawasaki disease is not fully understood. However, it is thought that Kawasaki disease is caused by either environmental, genetic, or viral causes. Kawasaki disease is defined as the systemic inflammation of the medium sized arteries and in multiple organs and tissues, which can lead to associated conditions such as hepatitis, interstitial pneumonitis, abdominal pain, vomiting, diarrhea, gallbladder hydrops, aseptic meningitis, irritability, myocarditis, pericarditis, valvulitis, pyuria, pancreatitis, and lymphadenopathy. On gross pathology, large or giant coronary artery aneurysms, thrombi containing aneurysms, decreases in luminal diameter, stenosis of the lumen and chronic inflamation are noted. On microscopic histopathological analysis of autopsied cases of Kawasaki disease, intracytoplasmic inclusion bodies are frequently observed in ciliated bronchial epithelial cells.

Pathophysiology

Pathogenesis

Genetics

In independent cohort studies, the genes which have been identified to lead to the development of Kawasaki disease include:[1]

Adapted from the AHA Scientific Statement on the diagnosis, treatment, and long term management of Kawasaki disease[1]
Gene Chromosome Location Genetic Methods Validation Populations Potential Significance
FCGR2A[2]
  • 1q23
  • European descent, Taiwanese, Koreans, Han Chinese
  • Low-affinity receptor for Fc fragment of IgG; risk allele has lower binding affinity
CASP3[3]
  • 4q34-35
  • Linkage analysis
  • Candidate gene study
  • Japanese, Taiwanese, Koreans, Chinese, Euro-Americans
HLAclass II[4]
  • 6p21.3
  • Japanese, Taiwanese, Koreans
BLK[5]
  • 8p23-22
  • Japanese, Taiwanese, Koreans
IPTKC[6]
  • 19q13.2
  • Linkage analysis
  • TDT
  • Japanese, Taiwanese, Koreans, Chinese, Euro- Americans
CD40[7]
  • 20q12-13.2
  • Japanese, Taiwanese, Koreans
Abbreviations: BLK; B-cell lymphoid kinase, CASP3;Caspase 3, FCGR; Fcγ receptor, GWAS; Genome-wide association study, HLA; human leukocyte antigen, IgG; immunoglobulin G, ITPKC; inositol 1,4,5-trisphosphate kinase-C, KD; Kawasaki disease, NFAT; nuclear factor of activated T cells, and TDT; transmission disequilibrium test.

Associated Conditions

  • Inflammation of the coronary arteries leads to the most important clinical outcomes.[8][9]
  • Kawasaki disease is defined by the systemic inflammation of the medium-sized arteries, multiple organs and tissues.
  • The systemic inflammation of the medium-sized arteries, organs and tissues can lead to the following associated conditions:
Organ and Tissue Associated conditions
Liver
Lung
Gastrointestinal tract
Meninges
Heart
Urinary tract
Pancreas
Lymph nodes

Gross Pathology

Images

Erythema of the palms, which is often accompanied by painful, brawny edema of the dorsa of the hands.[11]
Strawberry tongue and bright red, swollen lips with vertical cracking and bleeding.[12]
(A) Bilateral, non-exudative conjunctival injection with perilimbal sparing. (B) Strawberry tongue and bright red, swollen lips with vertical cracking and bleeding. (C) Erythematous rash involving perineum. (D) Erythema of the palms, which is often accompanied by painful, brawny edema of the dorsa of the hands. (E) Erythema of the soles, and swelling dorsa of the feet. (F) Desquamation of the fingers. (G) Erythema and induration at the site of a previous vaccination with Bacille Calmette-Gurin (BCG). (H) Perianal erythematous desquamation.[13]


Microscopic Pathology

References

  1. 1.0 1.1 McCrindle, Brian W.; Rowley, Anne H.; Newburger, Jane W.; Burns, Jane C.; Bolger, Anne F.; Gewitz, Michael; Baker, Annette L.; Jackson, Mary Anne; Takahashi, Masato; Shah, Pinak B.; Kobayashi, Tohru; Wu, Mei-Hwan; Saji, Tsutomu T.; Pahl, Elfriede (2017). “Diagnosis, Treatment, and Long-Term Management of Kawasaki Disease: A Scientific Statement for Health Professionals From the American Heart Association”. Circulation. 135 (17): e927–e999. doi:10.1161/CIR.0000000000000484. ISSN 0009-7322.
  2. Khor, C. C.; Davila, S.; Shimizu, C.; Sheng, S.; Matsubara, T.; Suzuki, Y.; Newburger, J. W.; Baker, A.; Burgner, D.; Breunis, W.; Kuijpers, T.; Wright, V. J.; Levin, M.; Hibberd, M. L.; Burns, J. C. (2011). “Genome-wide linkage and association mapping identify susceptibility alleles in ABCC4 for Kawasaki disease”. Journal of Medical Genetics. 48 (7): 467–472. doi:10.1136/jmg.2010.086611. ISSN 0022-2593.
  3. Onouchi, Yoshihiro; Ozaki, Kouichi; Buns, Jane C.; Shimizu, Chisato; Hamada, Hiromichi; Honda, Takafumi; Terai, Masaru; Honda, Akihito; Takeuchi, Takashi; Shibuta, Shoichi; Suenaga, Tomohiro; Suzuki, Hiroyuki; Higashi, Kouji; Yasukawa, Kumi; Suzuki, Yoichi; Sasago, Kumiko; Kemmotsu, Yasushi; Takatsuki, Shinichi; Saji, Tsutomu; Yoshikawa, Tetsushi; Nagai, Toshiro; Hamamoto, Kunihiro; Kishi, Fumio; Ouchi, Kazunobu; Sato, Yoshitake; Newburger, Jane W.; Baker, Annette L.; Shulman, Stanford T.; Rowley, Anne H.; Yashiro, Mayumi; Nakamura, Yoshikazu; Wakui, Keiko; Fukushima, Yoshimitsu; Fujino, Akihiro; Tsunoda, Tatsuhiko; Kawasaki, Tomisaku; Hata, Akira; Nakamura, Yusuke; Tanaka, Toshihiro (2010). “Common variants in CASP3 confer susceptibility to Kawasaki disease”. Human Molecular Genetics. 19 (14): 2898–2906. doi:10.1093/hmg/ddq176. ISSN 1460-2083.
  4. Onouchi, Yoshihiro; Ozaki, Kouichi; Burns, Jane C; Shimizu, Chisato; Terai, Masaru; Hamada, Hiromichi; Honda, Takafumi; Suzuki, Hiroyuki; Suenaga, Tomohiro; Takeuchi, Takashi; Yoshikawa, Norishige; Suzuki, Yoichi; Yasukawa, Kumi; Ebata, Ryota; Higashi, Kouji; Saji, Tsutomu; Kemmotsu, Yasushi; Takatsuki, Shinichi; Ouchi, Kazunobu; Kishi, Fumio; Yoshikawa, Tetsushi; Nagai, Toshiro; Hamamoto, Kunihiro; Sato, Yoshitake; Honda, Akihito; Kobayashi, Hironobu; Sato, Junichi; Shibuta, Shoichi; Miyawaki, Masakazu; Oishi, Ko; Yamaga, Hironobu; Aoyagi, Noriyuki; Iwahashi, Seiji; Miyashita, Ritsuko; Murata, Yuji; Sasago, Kumiko; Takahashi, Atsushi; Kamatani, Naoyuki; Kubo, Michiaki; Tsunoda, Tatsuhiko; Hata, Akira; Nakamura, Yusuke; Tanaka, Toshihiro (2012). “A genome-wide association study identifies three new risk loci for Kawasaki disease”. Nature Genetics. 44 (5): 517–521. doi:10.1038/ng.2220. ISSN 1061-4036.
  5. Onouchi, Yoshihiro; Ozaki, Kouichi; Burns, Jane C; Shimizu, Chisato; Terai, Masaru; Hamada, Hiromichi; Honda, Takafumi; Suzuki, Hiroyuki; Suenaga, Tomohiro; Takeuchi, Takashi; Yoshikawa, Norishige; Suzuki, Yoichi; Yasukawa, Kumi; Ebata, Ryota; Higashi, Kouji; Saji, Tsutomu; Kemmotsu, Yasushi; Takatsuki, Shinichi; Ouchi, Kazunobu; Kishi, Fumio; Yoshikawa, Tetsushi; Nagai, Toshiro; Hamamoto, Kunihiro; Sato, Yoshitake; Honda, Akihito; Kobayashi, Hironobu; Sato, Junichi; Shibuta, Shoichi; Miyawaki, Masakazu; Oishi, Ko; Yamaga, Hironobu; Aoyagi, Noriyuki; Iwahashi, Seiji; Miyashita, Ritsuko; Murata, Yuji; Sasago, Kumiko; Takahashi, Atsushi; Kamatani, Naoyuki; Kubo, Michiaki; Tsunoda, Tatsuhiko; Hata, Akira; Nakamura, Yusuke; Tanaka, Toshihiro (2012). “A genome-wide association study identifies three new risk loci for Kawasaki disease”. Nature Genetics. 44 (5): 517–521. doi:10.1038/ng.2220. ISSN 1061-4036.
  6. Onouchi, Yoshihiro; Gunji, Tomohiko; Burns, Jane C; Shimizu, Chisato; Newburger, Jane W; Yashiro, Mayumi; Nakamura, Yoshikazu; Yanagawa, Hiroshi; Wakui, Keiko; Fukushima, Yoshimitsu; Kishi, Fumio; Hamamoto, Kunihiro; Terai, Masaru; Sato, Yoshitake; Ouchi, Kazunobu; Saji, Tsutomu; Nariai, Akiyoshi; Kaburagi, Yoichi; Yoshikawa, Tetsushi; Suzuki, Kyoko; Tanaka, Takeo; Nagai, Toshiro; Cho, Hideo; Fujino, Akihiro; Sekine, Akihiro; Nakamichi, Reiichiro; Tsunoda, Tatsuhiko; Kawasaki, Tomisaku; Nakamura, Yusuke; Hata, Akira (2007). “ITPKC functional polymorphism associated with Kawasaki disease susceptibility and formation of coronary artery aneurysms”. Nature Genetics. 40 (1): 35–42. doi:10.1038/ng.2007.59. ISSN 1061-4036.
  7. Onouchi, Yoshihiro; Ozaki, Kouichi; Burns, Jane C; Shimizu, Chisato; Terai, Masaru; Hamada, Hiromichi; Honda, Takafumi; Suzuki, Hiroyuki; Suenaga, Tomohiro; Takeuchi, Takashi; Yoshikawa, Norishige; Suzuki, Yoichi; Yasukawa, Kumi; Ebata, Ryota; Higashi, Kouji; Saji, Tsutomu; Kemmotsu, Yasushi; Takatsuki, Shinichi; Ouchi, Kazunobu; Kishi, Fumio; Yoshikawa, Tetsushi; Nagai, Toshiro; Hamamoto, Kunihiro; Sato, Yoshitake; Honda, Akihito; Kobayashi, Hironobu; Sato, Junichi; Shibuta, Shoichi; Miyawaki, Masakazu; Oishi, Ko; Yamaga, Hironobu; Aoyagi, Noriyuki; Iwahashi, Seiji; Miyashita, Ritsuko; Murata, Yuji; Sasago, Kumiko; Takahashi, Atsushi; Kamatani, Naoyuki; Kubo, Michiaki; Tsunoda, Tatsuhiko; Hata, Akira; Nakamura, Yusuke; Tanaka, Toshihiro (2012). “A genome-wide association study identifies three new risk loci for Kawasaki disease”. Nature Genetics. 44 (5): 517–521. doi:10.1038/ng.2220. ISSN 1061-4036.
  8. McCrindle, Brian W.; Rowley, Anne H.; Newburger, Jane W.; Burns, Jane C.; Bolger, Anne F.; Gewitz, Michael; Baker, Annette L.; Jackson, Mary Anne; Takahashi, Masato; Shah, Pinak B.; Kobayashi, Tohru; Wu, Mei-Hwan; Saji, Tsutomu T.; Pahl, Elfriede (2017). “Diagnosis, Treatment, and Long-Term Management of Kawasaki Disease: A Scientific Statement for Health Professionals From the American Heart Association”. Circulation. 135 (17): e927–e999. doi:10.1161/CIR.0000000000000484. ISSN 0009-7322.
  9. Amano S, Hazama F, Hamashima Y (July 1979). “Pathology of Kawasaki disease: I. Pathology and morphogenesis of the vascular changes”. Jpn. Circ. J. 43 (7): 633–43. PMID 41111.
  10. McCrindle, Brian W.; Rowley, Anne H.; Newburger, Jane W.; Burns, Jane C.; Bolger, Anne F.; Gewitz, Michael; Baker, Annette L.; Jackson, Mary Anne; Takahashi, Masato; Shah, Pinak B.; Kobayashi, Tohru; Wu, Mei-Hwan; Saji, Tsutomu T.; Pahl, Elfriede (2017). “Diagnosis, Treatment, and Long-Term Management of Kawasaki Disease: A Scientific Statement for Health Professionals From the American Heart Association”. Circulation. 135 (17): e927–e999. doi:10.1161/CIR.0000000000000484. ISSN 0009-7322.
  11. By Kawasaki_symptoms.jpg: Dong Soo Kimderivative work: Natr (talk) – Kawasaki_symptoms.jpg, CC BY 2.0, https://commons.wikimedia.org/w/index.php?curid=12776158
  12. By Kawasaki_symptoms.jpg: Dong Soo Kimderivative work: Natr (talk) – Kawasaki_symptoms.jpg, CC BY 2.0, https://commons.wikimedia.org/w/index.php?curid=12776137
  13. By Dong Soo Kim – Kawasaki disease., CC BY-SA 4.0, https://commons.wikimedia.org/w/index.php?curid=9962875
  14. Rowley AH, Baker SC, Shulman ST, Garcia FL, Fox LM, Kos IM, Crawford SE, Russo PA, Hammadeh R, Takahashi K, Orenstein JM (February 2008). “RNA-containing cytoplasmic inclusion bodies in ciliated bronchial epithelium months to years after acute Kawasaki disease”. PLoS ONE. 3 (2): e1582. doi:10.1371/journal.pone.0001582. PMC 2216059. PMID 18270572.

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Causes

Causes

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Dildar Hussain, MBBS [2]

Overview

The exact cause of Kawasaki disease has not been identified. The current etiological theories center primarily on immunological causes for the disease. Much research has been carried out to discover a definitive toxin or antigenic substance, possibly a superantigen, to be established as the specific cause of the disease. There are several hypotheses for the cause of Kawasaki disease – infectious agents which are thought to induce Kawasaki disease include parvovirus B19, meningococcal septicemia, adenovirus, bacterial toxin–mediated, superantigens, cytomegalovirus, Epstein-Barr virus, human lymphotropic virus, klebsiella pneumoniae, mycoplasma pneumoniae, mite-associated bacteria, measles, propionibacterium acnes, parainfluenza type 3 virus, rotavirus infection, rickettsia species, and tick-borne diseases.

Causes

References

  1. Pinna GS, Kafetzis DA, Tselkas OI, Skevaki CL (June 2008). “Kawasaki disease: an overview”. Curr. Opin. Infect. Dis. 21 (3): 263–70. doi:10.1097/QCO.0b013e3282fbf9cd. PMID 18448971.
  2. Yanagawa H, Nakamura Y, Yashiro M, Ojima T, Tanihara S, Oki I, Zhang T (December 1998). “Results of the nationwide epidemiologic survey of Kawasaki disease in 1995 and 1996 in Japan”. Pediatrics. 102 (6): E65. PMID 9832593.
  3. Sundel, Robert P. (2015). “Kawasaki Disease”. Rheumatic Disease Clinics of North America. 41 (1): 63–73. doi:10.1016/j.rdc.2014.09.010. ISSN 0889-857X.

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Differentiating Kawasaki disease from other Diseases

Differentiating Kawasaki disease from other Diseases

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Dildar Hussain, MBBS [2];Eiman Ghaffarpasand, M.D. [3]

Overview

Kawasaki disease must be differentiated from other diseases that cause different rash-like conditions and can be confused with Kawasaki disease. The various conditions that should be differentiated from Kawasaki disease include; infantile polyarteritis nodosa, juvenile idiopathic arthritis, leptospirosis, lyme disease, measles, mercury toxicity, pediatric rocky mountain spotted fever, toxic epidermal necrolysis, staphylococcal scalded skin syndrome, rheumatic fever, impetigoinsect bites, monkey pox, rubella, atypical measles, coxsackie virus, acne, syphilis, molluscum contagiosum, toxic erythema, rat-bite fever, parvovirus B19, cytomegalovirus, scarlet fever, Stevens-Johnson syndrome, varicella-zoster virus, chicken pox, meningococcemia, rickettsial pox, meningitis, toxic shock syndrome, roseola infantum (exanthem subitum), erythema infectiosum (fifth disease), enterovirus, dengue fever, drug – induced rash, infectious mononucleosis, pharyngoconjunctival fever, herpangina, and primary herpetic gingivostomatitis.

Differentiating Kawasaki disease from other diseases

Different rash-like conditions can be confused with Kawasaki disease and are thus included in its differential diagnosis. The various conditions that should be differentiated from Kawasaki disease include:[1][2][3][4][5][6][7]

Abbreviations: ABG= Arterial blood gas, ANA= Antinuclear antibody, ANP= Atrial natriuretic peptide, ASO= Antistreptolysin O antibody, BNP= Brain natriuretic peptide, CBC= Complete blood count, COPD= Chronic obstructive pulmonary disease, CRP= C-reactive protein, CT= Computed tomography, CXR= Chest X-ray, DVT= Deep vein thrombosis, ESR= Erythrocyte sedimentation rate, HRCT= High Resolution CT, IgE= Immunoglobulin E, LDH= Lactate dehydrogenase, PCWP= Pulmonary capillary wedge pressure, PCR= Polymerase chain reaction, PFT= Pulmonary function test.

Diseases Clinical manifestations Para-clinical findings Gold standard Additional findings
Symptoms Physical examination
Lab Findings Imaging Histopathology
Headache Fever Weight loss Arthralgia Claudication Bruit HTN Focal neurological disorder Biomarker CBC ESR Other CT scan Angiography Ultrasound/ Echocardiography Other
Kawasaki disease[8] + +/- + + +/- NT-proBNP, Meprin A, Filamin C Normochromic anemia, ↑WBC with a left shift, Thrombocytosis  Acute-phase reactants, ↓Cholesterol, ↓HDL, ↓ApolipoA Coronary artery calcifications Coronary artery aneurysms, stenosis or occlusion Coronary artery anomaly in echocardiography Electron beam CT (EBCT) Acute destruction of the media by neutrophils, with loss of elastic fibers History and physical examination Diarrhea, Vomiting
Polyarteritis nodosa[9] + + + + + + +/- +/- LAMP-2 protein autoantibodies Leukocytosis, Normochromic anemia, Thrombocytosis Cr or BUN,

ALT or AST, Proteinuria

Focal regions of infarction or hemorrhage Multiple microaneurysms, Hemorrhage due to focal rupture, Occlusion Aneurysms and renal arteriovenous fistula in color Doppler sonography Necrotizing inflammatory lesions Angiography Sudden weight loss, Abdominal pain
Hepatitis B virus-associated polyarteritis nodosa[10] +/- +/- + + +/- +/- + HBsAg Leukocytosis, Normochromic anemia, Thrombocytosis ALT or AST Focal regions of infarction or hemorrhage Microaneurysms in mesenteric artery Aneurysms and renal arteriovenous fistula in color Doppler sonography Necrotizing inflammatory lesions Angiography Peripheral neuropathy, Livedo reticularis
Infectious disease Parvovirus B19 infection[11] + + + + +/- B19 DNA, ↓Reticulocyte count Anemia anti–parvovirus B19 IgM Hydrops in fetal ultrasonography B19 DNA Purpuric rash, Erythema multiforme
Scarlet fever[12] + + +/- + Antistreptolysin-O (ASO) titers Leukocytosis CRP Thickened pulmonary markings if pneumonia Sparse neutrophilic perivascular infiltrate History and physical examination Sand-paper rashes, Sore throat
Toxic shock syndrome[13] + + + + +/- Procalcitonin Leukocytosis with left shift Myoglobinuria, Sterile pyuria Acute respiratory distress syndrome Necrolysis of keratinocytes in epidermis, Perivascular lymphocytic infiltrate Clinical criteria Peeling or rashes, Organ dysfunction
Mononucleosis[14] + + + + EBV DNA Atypical lymphocyte Heterophile antibodies CNS involvement Splenomegaly Encephalitis in MRI Lymphoproliferative response in oropharynx, Lymphocytic infiltration in spleen Heterophile antibody test Splenomegaly, Palatal petechiae
Leptospirosis[15] + + + + +/- IL-6, IL-8 and IL-10 Anemia Cr or BUN,

ALT or AST, Proteinuria

 Diffuse alveolar hemorrhage Toxin-mediated break down of endothelial cell membranes of capillaries Culture and the microscopic agglutination test Red eyes, Skin rash
Lyme Disease[16] +/- + +/- + +/- CXCL9 (MIG), CXCL10 (IP-10) and CCL19 (MIP3B) Leukopenia, Thrombocytopenia Microscopic hematuria, Proteinuria, ↑ALT or AST Punctate lesions in periventricular white matter in brain SPECT Acrodermatitis chronica atrophicans Serologic tests Erythema migrans
Measles[17] +/- + +/- + Measles IgM Leukopenia, Lymphocytosis, Thrombocytopenia ALT or AST Pneumonia CXR Spongiosis and vesiculation in the epidermis with scattered dyskeratotic keratinocytes PCR Generalized rash, Cough, Coryza, or Conjunctivitis
Rocky Mountain Spotted Fever[18] + + + + R rickettsii serology Thrombocytopenia, Anemia  ALT or AST, Hyponatremia Infarction, edema, and meningeal enhancement Myocardial or conduction abnormalities in echocardiography Immunofluorescent or immunoperoxidase staining of R rickettsii Clinical criteria and tick exposure Rash on the palms and soles
Staphylococcal Scalded Skin Syndrome[19] + + + + +/- +/- Anti exfoliatin and anti alpha-toxin antibodies Leukocytosis with left shift Blood culture Pneumonia Intraepidermal blister, dense superficial perivascular lymphohistiocytic infiltrate  Blood culture and clinical findings Widespread skin erythema, fluid-filled blisters
Toxic Epidermal Necrolysis[20] + + +/- MicroRNA-124 Normochromic normocytic anemia, Eosinophilia Fluid loss and electrolyte abnormalities Tracheobronchial inflammation Necrotic keratinocytes with full-thickness epithelial necrosis Histopathology and clinical findings Erythematous macular rash with purpuric centers
Systemic disease Antiphospholipid Syndrome[21] + + +/- Antiphospholipid antibodies Thrombocytopenia, Hemolytic anemia Lupus anticoagulant (LA) Stroke,

Pulmonary embolism, Budd-Chiari syndrome

Thrombus in major vessels Valve thickening, vegetations, or insufficiency in echocardiography Noninflammatory bland thrombosis without perivascular inflammation Hx of thrombosis and antiphospholipid antibodies Miscarriage, Pulmonary hypertension
Juvenile Idiopathic Arthritis[22] + +/- Rheumatoid factor (RF), S100A12 Lymphocytosis, Thrombocytopenia Myeloid-related proteins 8/14 (MRP8/14) Synovial hypertrophy, Joint effusions Cerebral vasculitis Inflamed synovium Bone scanning Vascular congestion, RBC extravasation, Venular lumen occlusion Conventional radiography Evanescent rash, Dactylitis 

References

  1. Hartman-Adams H, Banvard C, Juckett G (2014). “Impetigo: diagnosis and treatment”. Am Fam Physician. 90 (4): 229–35. PMID 25250996.
  2. Mehta N, Chen KK, Kroumpouzos G (2016). “Skin disease in pregnancy: The approach of the obstetric medicine physician”. Clin Dermatol. 34 (3): 320–6. doi:10.1016/j.clindermatol.2016.02.003. PMID 27265069.
  3. Moore, Zack S; Seward, Jane F; Lane, J Michael (2006). “Smallpox”. The Lancet. 367 (9508): 425–435. doi:10.1016/S0140-6736(06)68143-9. ISSN 0140-6736.
  4. Ibrahim F, Khan T, Pujalte GG (2015). “Bacterial Skin Infections”. Prim Care. 42 (4): 485–99. doi:10.1016/j.pop.2015.08.001. PMID 26612370.
  5. Ramoni S, Boneschi V, Cusini M (2016). “Syphilis as “the great imitator”: a case of impetiginoid syphiloderm”. Int J Dermatol. 55 (3): e162–3. doi:10.1111/ijd.13072. PMID 26566601.
  6. Kimura U, Yokoyama K, Hiruma M, Kano R, Takamori K, Suga Y (2015). “Tinea faciei caused by Trichophyton mentagrophytes (molecular type Arthroderma benhamiae ) mimics impetigo : a case report and literature review of cases in Japan”. Med Mycol J. 56 (1): E1–5. doi:10.3314/mmj.56.E1. PMID 25855021.
  7. CEDEF (2012). “[Item 87–Mucocutaneous bacterial infections]”. Ann Dermatol Venereol. 139 (11 Suppl): A32–9. doi:10.1016/j.annder.2012.01.002. PMID 23176858.
  8. Takahashi K, Oharaseki T, Yokouchi Y (2011). “Pathogenesis of Kawasaki disease”. Clin Exp Immunol. 164 Suppl 1: 20–2. doi:10.1111/j.1365-2249.2011.04361.x. PMC 3095860. PMID 21447126.
  9. Howard T, Ahmad K, Swanson JA, Misra S (2014). “Polyarteritis nodosa”. Tech Vasc Interv Radiol. 17 (4): 247–51. doi:10.1053/j.tvir.2014.11.005. PMC 4363102. PMID 25770638.
  10. Sharma A, Sharma K (September 2013). “Hepatotropic viral infection associated systemic vasculitides-hepatitis B virus associated polyarteritis nodosa and hepatitis C virus associated cryoglobulinemic vasculitis”. J Clin Exp Hepatol. 3 (3): 204–12. doi:10.1016/j.jceh.2013.06.001. PMC 4216827. PMID 25755502.
  11. Heegaard ED, Brown KE (2002). “Human parvovirus B19”. Clin Microbiol Rev. 15 (3): 485–505. PMC 118081. PMID 12097253.
  12. Basetti S, Hodgson J, Rawson TM, Majeed A (2017). “Scarlet fever: a guide for general practitioners”. London J Prim Care (Abingdon). 9 (5): 77–79. doi:10.1080/17571472.2017.1365677. PMC 5649319. PMID 29081840.
  13. Vostral SL (2011). “Rely and Toxic Shock Syndrome: a technological health crisis”. Yale J Biol Med. 84 (4): 447–59. PMC 3238331. PMID 22180682.
  14. Balfour HH, Dunmire SK, Hogquist KA (2015). “Infectious mononucleosis”. Clin Transl Immunology. 4 (2): e33. doi:10.1038/cti.2015.1. PMC 4346501. PMID 25774295.
  15. Levett PN (April 2001). “Leptospirosis”. Clin. Microbiol. Rev. 14 (2): 296–326. doi:10.1128/CMR.14.2.296-326.2001. PMC 88975. PMID 11292640.
  16. Biesiada G, Czepiel J, Leśniak MR, Garlicki A, Mach T (2012). “Lyme disease: review”. Arch Med Sci. 8 (6): 978–82. doi:10.5114/aoms.2012.30948. PMC 3542482. PMID 23319969.
  17. White SJ, Boldt KL, Holditch SJ, Poland GA, Jacobson RM (2012). “Measles, mumps, and rubella”. Clin Obstet Gynecol. 55 (2): 550–9. doi:10.1097/GRF.0b013e31824df256. PMC 3334858. PMID 22510638.
  18. Walker DH (1989). “Rocky Mountain spotted fever: a disease in need of microbiological concern”. Clin Microbiol Rev. 2 (3): 227–40. PMC 358117. PMID 2504480.
  19. Mishra AK, Yadav P, Mishra A (2016). “A Systemic Review on Staphylococcal Scalded Skin Syndrome (SSSS): A Rare and Critical Disease of Neonates”. Open Microbiol J. 10: 150–9. doi:10.2174/1874285801610010150. PMC 5012080. PMID 27651848.
  20. Hoetzenecker W, Mehra T, Saulite I, Glatz M, Schmid-Grendelmeier P, Guenova E; et al. (2016). “Toxic epidermal necrolysis”. F1000Res. 5. doi:10.12688/f1000research.7574.1. PMC 4879934. PMID 27239294.
  21. Chaturvedi S, McCrae KR (2015). “The antiphospholipid syndrome: still an enigma”. Hematology Am Soc Hematol Educ Program. 2015: 53–60. doi:10.1182/asheducation-2015.1.53. PMC 4877624. PMID 26637701.
  22. Espinosa M, Gottlieb BS (July 2012). “Juvenile idiopathic arthritis”. Pediatr Rev. 33 (7): 303–13. doi:10.1542/pir.33-7-303. PMID 22753788.

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Epidemiology and Demographics

Epidemiology and Demographics

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Dildar Hussain, MBBS [2], Sabawoon Mirwais, M.B.B.S, M.D.[3]

Overview

Kawasaki disease (Kawasaki syndrome or KS) occurs worldwide, with the highest incidence in Japan, and it most often affects boys and younger children. KS may have a winter-spring seasonality, and community-wide outbreaks have been reported occasionally. In the continental United States, population-based and hospitalization studies have estimated an incidence of KS ranging from 9 to 19 per 100,000 children younger than 5 years of age. Approximately, 4248 hospitalizations for Kawasaki disease, of which 3277 (77%) were for children under 5 years of age, were estimated among children younger than 18 years of age in the United States in the year 2000.

Epidemiology and Demographics

Incidence

  • The incidence of Kawasaki disease is approximately 175 per 100,000 individuals in Japan.[1]
  • In the continental United States, population-based and hospitalization studies estimate an incidence ranging from 9 to 19 per 100,000 children under 5 years of age.[2]
  • The occurrence incidence of Kawasaki disease in the US is between 17.5 and 20.8 per 100,000 children < 5 years.[3]
  • Below is the list of the countries with the corresponding incidence rates of Kawasaki disease:
    • Japan: 243.1 and 264.8 per 100,000 in children younger than 5 years in 2011 and 2012, respectively.
    • South Korea: 134.4 cases per 100,000 for children under 5 years of age.[4]
    • Ireland: 15.2 per 100,000 children younger than 5 years.[5]
    • Finland:11.4 per 100,000 children younger than 5 years.[6]
    • Norway: 5.4 per 100,000 children younger than 5 years.
    • Sweden: 7.4 per 100,000 children younger than 5 years.

    Prevalence

    • In 1999, the prevalence of Kawasaki disease was estimated to be in range of 5000 to 6000 in Japan.[7]

    Age

    • Kawasaki disease commonly affects individuals younger than 5 years of age.[7]
    • 80% of patients with Kawasaki disease are younger than 5 years of age

    Race

    • Kawasaki disease usually affects individuals of the Asian race.[7]
    • Pacific Islanders are also more commonly affected.

    Gender

    • Males are more commonly affected by Kawasaki disease than females.[7]

    References

    1. Kawasaki T (March 1967). “[Acute febrile mucocutaneous syndrome with lymphoid involvement with specific desquamation of the fingers and toes in children]”. Arerugi (in Japanese). 16 (3): 178–222. PMID 6062087.
    2. https://www.cdc.gov/kawasaki/about.html
    3. Uehara R, Belay ED (2012). “Epidemiology of Kawasaki disease in Asia, Europe, and the United States”. J Epidemiol. 22 (2): 79–85. doi:10.2188/jea.je20110131. PMC 3798585. PMID 22307434.
    4. Kim GB, Park S, Eun LY, Han JW, Lee SY, Yoon KL, Yu JJ, Choi JW, Lee KY (May 2017). “Epidemiology and Clinical Features of Kawasaki Disease in South Korea, 2012-2014”. Pediatr. Infect. Dis. J. 36 (5): 482–485. doi:10.1097/INF.0000000000001474. PMID 27997519.
    5. Lynch M, Holman RC, Mulligan A, Belay ED, Schonberger LB (November 2003). “Kawasaki syndrome hospitalizations in Ireland, 1996 through 2000”. Pediatr. Infect. Dis. J. 22 (11): 959–63. doi:10.1097/01.inf.0000095194.83814.ee. PMID 14614367.
    6. Salo E, Griffiths EP, Farstad T, Schiller B, Nakamura Y, Yashiro M, Uehara R, Best BM, Burns JC (December 2012). “Incidence of Kawasaki disease in northern European countries”. Pediatr Int. 54 (6): 770–2. doi:10.1111/j.1442-200X.2012.03692.x. PMC 3467350. PMID 22726311.
    7. 7.0 7.1 7.2 7.3 Yanagawa H, Nakamura Y, Ojima T, Yashiro M, Tanihara S, Oki I (January 1999). “Changes in epidemic patterns of Kawasaki disease in Japan”. Pediatr. Infect. Dis. J. 18 (1): 64–6. PMID 9951983.

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    Risk Factors

    Risk Factors

    Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Dildar Hussain, MBBS [2]

    Overview

    Common risk factors in the development of Kawasaki disease are a combination of non-modifiable and modifiable risk factors, that include environmental, genetic, and viral factors.

    Risk Factors

    Common risk factors in the development of Kawasaki disease are a combination of non-modifiable and modifiable risk factors, that include environmental, genetic, and viral factors.[1][2]

    References

    1. Sánchez-Manubens, Judith; Bou, Rosa; Anton, Jordi (2014). “Diagnosis and classification of Kawasaki disease”. Journal of Autoimmunity. 48-49: 113–117. doi:10.1016/j.jaut.2014.01.010. ISSN 0896-8411.
    2. McCrindle, Brian W.; Rowley, Anne H.; Newburger, Jane W.; Burns, Jane C.; Bolger, Anne F.; Gewitz, Michael; Baker, Annette L.; Jackson, Mary Anne; Takahashi, Masato; Shah, Pinak B.; Kobayashi, Tohru; Wu, Mei-Hwan; Saji, Tsutomu T.; Pahl, Elfriede (2017). “Diagnosis, Treatment, and Long-Term Management of Kawasaki Disease: A Scientific Statement for Health Professionals From the American Heart Association”. Circulation. 135 (17): e927–e999. doi:10.1161/CIR.0000000000000484. ISSN 0009-7322.

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    Screening

    Screening

    Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Dildar Hussain, MBBS [2]

    Overview

    There is insufficient evidence to recommend routine screening for Kawasaki disease.

    Screening

    There is insufficient evidence to recommend routine screening for Kawasaki disease.

    References

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    Natural History, Complications and Prognosis

    Natural History, Complications and Prognosis

    Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Dildar Hussain, MBBS [2]

    Overview

    If left untreated, the symptoms will eventually relent, but coronary artery aneurysms will not improve, resulting in a significant risk of death or disability due to myocardial infarction. If treated in a timely fashion, this risk can be mostly avoided and the course of illness cut short. Patients with Kawasaki disease may progress to develop long term cardiovascular illness such as coronary artery disease, and pre-mature atherosclerosis. Common complications of Kawasaki disease include vasculitis and coronary artery aneurysms. Prognosis is generally excellent and the mortality rate of patients with Kawasaki disease is approximately 2%.

    Natural History, Complications, and Prognosis

    Natural History

    Complications

    Organ and Tissue Associated Conditions
    Liver
    Lung
    Gastrointestinal tract
    Meninges
    Heart
    Urinary tract
    Pancreas
    Lymph nodes

    Prognosis

    • With early treatment, rapid recovery from the acute symptoms can be expected and the risk of coronary artery aneurysms greatly reduced.
    • Untreated, the acute symptoms of Kawasaki disease are self-limited, but the risk of coronary artery involvement is much greater.
    • Patients who have had Kawasaki disease should have an echocardiogram initially every few weeks, and then every 1 – 2 years to screen for the progression of cardiac involvement.
    • Overall, about 2% of the patients die from complications of coronary vasculitis.
    • It is also not uncommon that a relapse of symptoms may occur soon after initial treatment with IVIG.
      • This usually requires re-hospitalization and retreatment. Treatment with IVIG can cause allergic and non-allergic acute reactions, aseptic meningitis, fluid overload and rarely other serious reactions.
      • Aspirin may increase the risk of bleeding from other causes and may be associated with Reye’s syndrome.
      • Overall, life-threatening complications resulting from therapy for Kawasaki disease are exceedingly rare, especially compared with the risk of non-treatment.

    References

    1. Kato H (September 2014). “[Natural history of Kawasaki disease vasculitis]”. Nippon Rinsho (in Japanese). 72 (9): 1530–5. PMID 25518398.
    2. Belay E, Maddox R, Holman R, Curns A, Ballah K, Schonberger L (2006). “Kawasaki syndrome and risk factors for coronary artery abnormalities: United States, 1994-2003”. Pediatr Infect Dis J. 25 (3): 245–9. PMID 16511388.
    3. McCrindle, Brian W.; Rowley, Anne H.; Newburger, Jane W.; Burns, Jane C.; Bolger, Anne F.; Gewitz, Michael; Baker, Annette L.; Jackson, Mary Anne; Takahashi, Masato; Shah, Pinak B.; Kobayashi, Tohru; Wu, Mei-Hwan; Saji, Tsutomu T.; Pahl, Elfriede (2017). “Diagnosis, Treatment, and Long-Term Management of Kawasaki Disease: A Scientific Statement for Health Professionals From the American Heart Association”. Circulation. 135 (17): e927–e999. doi:10.1161/CIR.0000000000000484. ISSN 0009-7322.
    4. Amano S, Hazama F, Hamashima Y (July 1979). “Pathology of Kawasaki disease: I. Pathology and morphogenesis of the vascular changes”. Jpn. Circ. J. 43 (7): 633–43. PMID 41111.

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    Diagnosis

    Diagnosis

    Diagnostic criteria | History and Symptoms | Physical Examination | Laboratory Findings | Electrocardiogram | X-Ray Findings | Echocardiography and Ultrasound | CT-Scan Findings | MRI Findings | Other Imaging Findings | Other Diagnostic Studies

    Treatment

    Treatment

    Medical Therapy | Surgery | Primary Prevention | Cost-Effectiveness of Therapy | Future or Investigational Therapies

    Case Studies

    Case Studies

    Case #1

    External links

    Template:Diseases of the musculoskeletal system and connective tissue


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    de:Kawasaki-Syndrom it:Sindrome di Kawasaki he:מחלת קווסקי nl:Ziekte van Kawasaki th:โรคคาวาซากิ

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