Familial Mediterranean fever
What is familial Mediterranean fever?
Familial Mediterranean fever is an inherited autoinflammatory syndrome characterised by recurrent short episodes of high fever with skin rash and abdominal pain. Painful inflammation of joints and other body sites also occur. If untreated, amyloidosis commonly develops and may have a fatal outcome. Familial Mediterranean fever is the most common of the periodic fever syndromes.
In Type 2 familial Mediterranean fever, amyloidosis is the presenting feature with no history of typical febrile episodes.
Who gets familial Mediterranean fever and why?
Familial Mediterranean fever mainly affects specific racial groups originating from around the eastern Mediterranean Sea. These include:
- Arabs
- Armenians
- Italians (mild form)
- Jews
- Turks
In these groups, 1 in 25 to 1 in 2000 people are affected. By comparison, in west Europeans the prevalence is 2.5 per 100,000 (1 in 40,000) people. The carrier rate can be as high as 1 in 3 in some groups. Although previously believed to affect only Sephardic Jews, Ashkenazi Jews have recently been recognised to suffer a mild form of the syndrome.
Two-thirds of patients develop symptoms before the age of 5 years and 90% by 20 years of age.
Familial Mediterranean fever is usually inherited as an autosomal recessive condition, meaning both parents must carry the defective gene and there is a one in four chance of a child being affected (MIM 249100). There is a less common autosomal dominant form (MIM 134610).
Molecular biology and genetics
Familial Mediterranean fever is usually due to mutations in the Mediterranean fever (MEFV) or pyrin gene located on chromosome 16 (16p13.3). Mutations in the MEFV gene have been found in 80% of typical cases. More than 100 different disease-linked mutations have been identified. The most commonly reported mutation, M694V, is associated with severe disease and the development of secondary amyloidosis. Other common mutations are M680I and V726A. 20% of Ashkenazy Jews carry the E148Q MEFV mutation.
The MEFV gene codes for a protein called pyrin (also known as marenostrin) mainly expressed by inflammatory white cells such as neutrophils and eosinophils. The normal form of pyrin suppresses inflammation by down-regulation of pro-inflammatory cytokines (cell messenger proteins), up-regulation of anti-inflammatory cytokines and preventing the production of interleukin 1beta (IL-1β) by inflammasomes. A lack of functional pyrin releases the inflammatory cascade.
Clinical features of familial Mediterranean fever
The clinical features of familial Mediterranean fever that distinguish it from other periodic fever syndromes are:
- febrile attacks lasting for 1-3 days
- severe abdominal, chest and/or joint pain
- erysipelas-like changes on the lower legs.
Children under the age of 2 years often present with fever alone, and progress to more typical attacks by the age of 5 years.
The characteristics of the recurrent acute episodes of familial Mediterranean fever are described in the table below.
| Symptom | Features |
|---|---|
| Fever |
|
| Abdominal pain |
|
| Chest pain |
|
| Joint pain and swelling (arthralgia, arthritis) |
|
| Skin rashes |
|
| Scrotal pain (orchitis) |
|
| Spleen enlargement (splenomegaly) |
|
| Muscle pain (myalgia) |
|
| Neurologic symptoms |
|
| Amyloidosis |
|
What are the features of the skin rash?
| Erysipelas-like lesions |
|
| Henoch-Schönlein purpura |
|
| Nonspecific purpura |
|
| Polyarteritis nodosa |
|
| Angioedema |
|
| Redness of the palms |
|
| Raynaud phenomenon |
|
What triggers attacks?
The frequency of episodes is variable, ranging from weekly to every few years. Attacks may be triggered by:
- Exercise
- Infection
- Menstruation
- Stress.
Acute attacks settle spontaneously. Between episodes, health is normal.
How is familial Mediterranean fever diagnosed?
Diagnosis of familial Mediterranean fever is made on typical clinical history, requiring fever plus at least one major and one minor criterion or two minor criteria.
Major criteria
- abdominal pain
- joint pain
- chest pain
- skin eruption
In children an additional major diagnostic criterion is family history of familial Mediterranean fever, as children can present with fever alone.
Minor criteria
- high erythrocyte sedimentation rate (ESR)
- high white cell count (leukocytosis)
- high serum fibrinogen
Blood tests during an attack may show:
- Increased white blood cell count (leukocytosis), erythrocyte sedimentation rate (ESR), serum fibrinogen, C-reactive protein (CRP)
- Increase in Serum IgD in 10%
X-rays of abdomen often reveal multiple fluid levels suggesting an ‘acute abdomen’
Skin biopsy from the erysipelas-like lesion shows a heavy infiltrate of neutrophils (white blood cells). Leukocytoclastic vasculitis is seen on biopsies from Henoch-Schönlein purpura or polyarteritis nodosa-like lesions.
Investigations for myalgia (muscle pain) reveal normal muscle enzymes, electromyography (EMG) and muscle biopsy.
Amyloidosis most commonly presents as protein in the urine (proteinuria) without red cells (haematuria) or raised blood pressure (hypertension).
Gene sequencing can be performed by specialised laboratories as targeted mutation analysis (looking for the commonest mutations) or sequence analysis of select exons (looking at exon 10 and possibly others).
Once the gene mutations have been identified in the patient, the carrier status of parents, screening of other first degree blood relatives even if asymptomatic, and prenatal diagnosis can be determined. Identification of asymptomatic but genetically affected individuals means treatment can be commenced to prevent the development of amyloidosis.
Treatment of familial Mediterranean fever
Colchicine, taken orally each day for life, is the drug of choice for familial Mediterranean fever to:
- reduce the frequency of attacks,
- reduce the severity of attacks
- prevent secondary systemic amyloidosis.
Colchicine is potentially toxic so it is very important not to take an excessive dose.
The starting dose of colchicine for adults is 1mg/day. The usual dose required long term is 1.2 mg/day, ranging from 0.9-2mg/day.
The starting dose of colchicine for children depends on age:
- <5 years of age 0.5 mg/day
- 5-10 years of age 1 mg/day
- >10 years of age 1.5 mg/day
The dose of colchicine is increased stepwise up to a maximum dose of 2.5 mg/day. The dose is usually determined by the frequency and severity of attacks. Colchicine results in a marked improvement in symptoms for 90-95% of patients, and 75% have virtually complete remission. It is not known how it works.
Other treatment
Acute attacks are treated with non-steroidal anti-inflammatory drugs (NSAID) and pain relief.
Prolonged fever with muscle pain responds to systemic corticosteroids.
The most common reason for failure to respond to colchicine is poor compliance due to gastrointestinal upset. However 5-10% do not respond to colchicine and this may be due to ABCB1 gene polymorphisms affecting colchicine uptake by mononuclear cells. Thalidomide and biologic agents, such as daily subcutaneous anakinra (an interleukin-1 receptor antagonist), may then be considered to prevent attacks and the development of amyloidosis. To reduce the severity of an attack, single dose methylprednisolone or anakinra at the start of episodes have been reported to relieve symptoms.
Related information
References:
- Braun-Falco M, Ruzicka T. Skin manifestations in autoinflammatory syndromes. J Dtsch Dermatol Ges 2010 (Dec). doi: 10.1111/j.1610-0387.2010.07580.x
- De Sanctis S, Nozzi M, Del Torto M, Scardapane A, Gaspari S, de Michele G, Breda L, Chiarelli F. Autoinflammatory syndromes: diagnosis and management. Italian Journal of Pediatrics 2010; 36: 57. http://www.ijponline.net/content/36/1/57
- Grateau G, Duruöz MT. Autoinflammatory conditions: when to suspect? How to treat? Best Practice & Research Clinical Rheumatology 2010; 24: 401–411.
- Kanazawa N, Furukawa F. Autoinflammatory syndromes with a dermatological perspective. Journal of Dermatology 2007; 34: 601– 618.
- Montealegre Sanchez GA, Hashkes PJ. Neurological manifestations of the Mendelian-inherited autoinflammatory syndromes. Dev Med Child Neurol 2009; 51: 420-428.
- Toro JR, Aksentijevich I, Hull K, Dean J, Kastner DL. Tumor necrosis factor receptor–associated periodic syndrome. A novel syndrome with cutaneous manifestations. Arch Dermatol. 2000;136:1487-1494.
- Website: Familial Mediterranean fever. GeneReviews. NCBI Bookshelf. Pagon RA, Bird TD, Dolan CR, et al., editors. GeneReviews [Internet]. Seattle (WA): University of Washington, Seattle; 1993-. Bookshelf ID: NBK1227 PMID: 20301405 http://www.ncbi.nlm.nih.gov/books/NBK1227/
On DermNet NZ:
Other websites:
- Hereditary Periodic Fever Syndromes – Medscape Reference
- Familial Mediterranean Fever – The Merck Manual for Healthcare Professionals
- Familial Mediterranean fever – MedlinePlus
- Familial Mediterranean fever; FMF: MIM ID #249100 – OMIM
- Familial Mediterranean fever, autosomal dominant: MIM ID #134610 – OMIM
- Periodic Fever Syndrome – Cleveland Clinic
Books:
See the DermNet NZ bookstore