Skip to main content
PMC home page
Orphanet Journal of Rare Diseases logoLink to Orphanet Journal of Rare Diseases
. 2013 Oct 16;8:162. doi: 10.1186/1750-1172-8-162

The expanding spectrum of rare monogenic autoinflammatory diseases

Isabelle Touitou 1,2,3,, Caroline Galeotti 4, Linda Rossi-Semerano 4, Véronique Hentgen 5, Maryam Piram 4, Isabelle Koné-Paut 4, for the CeRéMAI, French reference center for autoinflammatory diseases
PMCID: PMC4016572  PMID: 24131530

Abstract

Monogenic autoinflammatory diseases are a group of hereditary disorders characterized by a clinical and biological inflammatory syndrome in which there is little or no evidence of autoimmunity. The discovery of the first causative gene in 1997 was rapidly followed by the identification of many others from the same group. The mutated proteins can be directly or indirectly involved in the regulation of inflammation. The available literature includes numerous reviews, which address the principle diseases, but we wanted to focus on the most recent rare syndromes. A comprehensive review is thus provided, including taxonomic, genetic, and epidemiological data, along with characteristics defining positive and differential diagnoses and treatment. We believe that this update will assist physicians in correctly naming their patient’s illness. This is an essential step for the effective and targeted management of an orphan disease.

Keywords: Autoinflammatory diseases, Histiocytosis and lymphadenopathy syndrome (H Syndrome), NLRP12 Associated Periodic Syndrome (NAPS12), Deficiency of Interleukin 1 Receptor Antagonist (DIRA), Deficiency of interleukin 36 receptor antagonist (DITRA), Pityriasis rubra pilaris (PRP), Disseminated Superficial Actinic Porokeratosis (DSAP), Autoinflammation LipoDystrophy and Dermatosis syndrome (ALDD)

Introduction

Autoinflammatory diseases arise from disorders of the innate immune system [1]. The prototype disease is familial Mediterranean fever (FMF), which belongs to the group of hereditary recurrent fevers. Periods of inflammation are predominantly triggered following unnoticed proinflammatory signals. The levels of serum markers of inflammation such as C-reactive protein are always increased during attacks, however autoantibodies remain mostly undetectable. Since the discovery in 1997 of the gene responsible for FMF [2,3], dramatic insights have been gained through establishing the central role of the inflammasomes by unraveling their components and interacting cellular partners [4-6]. Subsequent to the identification of causal mutations in monogenic autoinflammatory diseases, several sequence variants in the causative genes were found to act as susceptibility factors in the more common multifactorial diseases such as rheumatoid arthritis or multiple sclerosis [7]. More recently, monogenic autoinflammatory disorders expanded to include the so far-called inflammatory skin diseases without systemic involvement. Enhanced knowledge relating to the critical physiological mechanisms altered in these diseases fuelled the development of novel, dramatically effective targeted biological drugs such as Interleukin-1 inhibitors [8]. As autoinflammatory diseases are rare, a national referral center nominated by the French ministry of health was set-up (CeRéMAI; [http://asso.orpha.net/CEREMAI/EN/index.html]) in order to improve care for patients. This referral center created Infevers [9] [fmf.igh.cnrs.fr/infevers/], a dedicated online database for autoinflammatory mutations [9].

This review focuses on monogenic autoinflammatory diseases identified within the last five years, including epidemiological and genetic data (Table  1), an exhaustive description of the corresponding disease name and synonyms where available, OMIM and Orphacode numbers, main clinical signs and therapeutic approaches (Table  2).

Table 1.

Epidemiology and genetics of rare recently recognized monogenic autoinflammatory diseases

Year of gene discovery Disease* N patients** M/F ratio Ethnicity*** Ref Mode of inheritance Gene****   Chromosome location Most frequent mutation
2008
 H Syndrome
 Histiocytosis lymphadenopathy plus syndrome
 4
 2/2
 1 Indian case
 12
 Recessive
 SLC29A3
 Solute Carrier Family
 10q22.1
 ND
1 Pakistani case
 13
1 Morocan case
 10
 29 (Nucleoside Transporter), Member 3
1 Tunisian case
 11
2008
 NAPS12
 NLRP12 Associated Periodic Syndrome
 19
 13/6
 2 Guadeloupean families
 18
 Dominant
 NLRP12
 NLR pyrin domain containing protein 12
 19q43.42
 c.1054C>T, p.Arg352Cys
17
1 Italian family
 58
6 Eastern-European cases
 16
1 Armenian case
 16
1 Italian case
 9
1 Guadeloupean case
 9
1 Irish case
2009
 DIRA
 Deficiency of Interleukin 1 Receptor Antagonist
 17
 9/8
 1 Turkish family
 23
 Recessive
 IL1RN
 Interleukin 1
 2q13
 c.-64_1696del, p.IL1F9_IL1RNdel
1 Lebanese
 22
 receptor antagonist
family
 22
2 Dutch families
 22
 c.213_227del, p.Asp72_Ile76del
1 Dutch case
 22
1 Canadian case
 22,27
2 Puerto-Rican cases
 25
2 Brazilian cases
 24,26
2 Unknown
3 Dutch,
1 Lebanese,
1 Turkish,
1 from unknown ancestry
2011
 DITRA
 Deficiency of Interleukin
 66
 26/37
 3 Tunisian families
 30
 Recessive
 IL36RN
 Interleukin 36 receptor antagonist
 2q13
 c.80C>T, p.Leu27Pro
1 Algerian family
 9
36 Receptor Antagonist
 19 European cases
 32,35,37
 c.338C>T, p.Ser113Leu
10 Asian cases
 35
 c.28C>T, p.Arg10*
6 Tunisian cases
 30
6 German cases
 36
3 Japanese cases
 33,34
1 Spanish case
 9
1 Turkish case
 36
1 Iraqi case
 36
1 Russian case
 37
2012
 PSORS2
 Psoriasis susceptibility 2
 45
 24/21
 1 European family
 42
 Dominant 
 CARD14
 Caspase recruitment domain-containing protein 14
 17q25.3
 c.349G>A, p.Gly117Ser
1 Taiwanese family
 42
1 Tunisian family
 43
3 German cases
 36
 
 PRP
 Pityriasis Rubra Pilaris
 17
 9/8
 4 Israeli families
 41
2012
 DSAP
 Disseminated Superficial Actinic Porokeratosis
 >45
 21/16/ND
 20 Chinese families,
 48.49
 Dominant
 MVK
 Mevalonate Kinase
 12q24
 C.604G>A
p.Gly202Arg
6 Chinese cases
2010
 ALDD (JMP, NNS, CANDLE)
 Autoinflammation, lipodystrophy, and dermatosis syndrome
 40
 26/14
 22 Japanese families
 53,57
 Recessive
 PSMB8
 Proteasome Subunit,
 6p21.32
 c.224C>T, p.Thr75Met
1 Portuguese family
 56
 Beta-Type, 8
 c.602G>T,
1 Mexican family
 56
 p.Gly201Val
3 Hispanic cases
 54
3 Spanish cases
 54
2 American cases
 54
1 Japanese case
 53
1 Israeli case
 54
1 Italian case
 9
2012
 APLAID
 Autoinflammation, Antibody deficiency, and Immune Dysregulation syndrome
 2
 1/1
 1 family of unknown origin
 14
 Dominant
 PLCG2
 Phospholipase C, gamma 2
 16q23.3
 ND
2012 NA Autoinflammatory syndrome with pyogenic bacterial infection and amylopectinosis 3 1/2 1 French family
 15 Recessive RBCK1 RANBP-Type and C3HC4-Type Zinc Finger-Containing 1 20p13 ND
1 Italian case
Open in a new tab

* Commonly used disease names as defined in Table  2 ** Genetically confirmed. *** “Family” refers to multiplex families; “Case” refers to sporadic patients **** Approved HUGO.

NA: Not assigned yet. ND: Not determined.

Table 2.

Clinical features of rare recently recognized monogenic autoinflammatory diseases

OMIM ORPHA-CODE Disease acronyme Disease extended name* Synonyms Age at onset Key symptoms Differential diagnosis Treatment
612373
 168569 254707 254712 254723
 H Syndrome
 Histiocytosis-lymphadenopathy plus syndrome
 PHID
 Pigmentary Hypertrichosis and non-autoimmune Insulin-dependent Diabetes mellitus
 FHC
 Faisalabad Histiocytosis
 SHML
 Sinus Histiocytosis with Massive Lymphadenopathy
 Infancy
 Histiocytosis
 FCAS2
 NSAID (IL-1 and TNF blockades not effective)
FCAS3
ALDD
Other causes of insulin-dependent diabetes
611762
 247868
 FCAS2
 Familial Cold Autoinflammatory Syndrome 2
 NAPS12
 NLRP12 Associated Periodic Syndrome
 NLRP12AD
 NLRP12-associated disorder
  
  
 Infancy Childhood Adulthood
 Urticaria, fever, myalgia, arthralgia
 FCAS1 FCAS3
 NSAID (IL-1 blockades not effective)
612852
 210115
 OMPP
 Osteomyelitis, sterile Multifocal, with Periostitis and Pustulosis
 DIRA
 Deficiency of Interleukin 1 Receptor Antagonist
  
  
  
  
 Neonatal
 Neutrophilic pustular dermatosis, periostitis, aseptic multifocal osteomyelitis
 PSORP Other dermatologic and infectious conditions
 IL1 blockades (NSAID not effective)
614204
 247353
 PSORP
 Pustular Psoriasis, Generalized
 DITRA
 Deficiency of Interleukin 36 Receptor Antagonist
 GPP
 Generalized Pustular Psoriasis
  
  
 Infancy, Childhood, Adulthood
 Diffuse erythematous pustular rash, fever, malaise and diffuse pain, systemic inflammation
 OMPP Other autoinflammatory diseases
 NSAID, Vitamin D3, Acitretin, TNF and IL-1 blockades
602723
 NA
 PSORS2
 Psoriasis susceptibility 2
  
  
  
  
  
  
 Variable
 Round, well circumscribed erythematous plaques covered by a thick silver scale with a predilection for elbows, knees, scalp, lumbosacral and anogenital regions
 Other papulosquamous disorders
 Corticosteroids, calcineurin inhibitor, calcipotriene, emollients, keratolytic agents, ultraviolet light, retinoids, methotrexate, cyclosporine, anti-TNF agents
173200
 2897
 PRP
 Pityriasis Rubra Pilaris
  
  
  
  
  
  
 Neonatal Early childhood
 Small keratotic follicular papules, disseminated salmon-colored scaly plaques surrounding islands of normal skin, diffuse red-orange palmoplantar keratoderma
 Phrynoderma (vitamin A deficiency), psoriasis, erythrokeratodermia, other causes of cornification
 Emollients, topical corticosteroids, tazarotene, keratolytic agents, calcineurin inhibitor, systemic retinoids, TNFα blocking agents
175900
 79152
 POROK3
 Porokeratosis 3, Disseminated Superficial Actinic Type
 DSAP
 Disseminated Superficial Actinic Porokeratosis
  
  
  
  
 Adult
 UV sensitive, Epidermal cornification, round and brownish lesions
 Neoplastic or hyperplastic squamous proliferations
 Cryotherapy, topical reagents, electrodessication, laser ablation, photodynamic therapy
256040
 2615
 ALDD
 Autoinflammation, LipoDystrophy, and Dermatosis syndrome
 JMP
 Joint contractures, muscle atrophy, Microcytic anemia, and Panniculitis-induced lipodystrophy syndrome.
 NNS
 Nakajo-Nishimura Syndrome
 CANDLE
 Chronic Atypical Neutrophilic Dermatosis with Lipodystrophy and Elevated temperature syndrome
 Neonatal
 Fever, skin rash, panniculitis, lipoatrophy
 Still’s disease, CINCA, mucopolysaccharidosis, lupus, dermatomyositis, laminopathies, Aicardi Goutieres syndrome
 NSAID, Interferon γ, JAK inhibitors?
614878
 324530
 APLAID
 Autoinflammation, antibody deficiency, and immune dysregulation syndrome
  
  
  
  
  
  
 ND
 Neutrophilic skin lesions, IBD, recurrent sino pulmonary infections
 Other immunodeficiencies, IBD, PLAID
 ND
NA 329173 NA Autoinflammatory syndrome with pyogenic bacterial infection and amylopectinosis             ND ND ND ND
Open in a new tab

*Approved OMIM; NA Not assigned yet; ND: too few patients to delineate clear criteria. Commonly used disease names are in bold text.

NSAID: nonsteroidal anti-inflammatory drugs.

CINCA: Chronic, Infantile, Neurologic, Cutaneous and Articular syndrome, IBD: inflammatory bowel disease, PLAID: PLCg2-Associated antibody Deficiency.

Rare recently recognized monogenic autoinflammatory diseases

The correct diagnosis of monogenic autoinflammatory diseases relies on the physicians’ awareness. Due to the rarity of these disorders, a very low number of cases are reported. For example, less than five patients with clear autoinflammatory features and causative mutations have been published for each of H syndrome [10-13], Autoinflammation and PLCG2-associated antibody deficiency and Immune Dysregulation syndrome (APLAID) [14], and RANBP-Type and C3HC4-Type Zinc Finger-Containing 1 (RBCK1)-related disease [15]. These three conditions are thus cited in Tables  1 and 2 only. Moreover, as mutations in these rare conditions have apparently systemic and pleiotropic effects, the patients’ clinical spectrum is heterogeneous and not yet completely delineated. Molecular analysis of the candidate genes may also fail to detect mutations. Consequently, the frequency of these diseases is unknown and too little feedback and data exist on the clinical significance and penetrance of the variants to ensure adequate genetic counseling for these patients.

NLRP12 Associated Periodic Syndrome (NAPS12)

This disease is characterized by recurrent periods of fever, combined with various systemic manifestations such as myalgia, arthralgia, headaches and skin urticarial-like rash although some patients may display arthralgia or myalgia only [16-18]. The most severely affected patients suffer from neurosensory signs (headache, deafness) [18]. The inflammatory attacks last 5-10 days and are triggered by physical exertion or cold exposure. These attacks can be very disabling in everyday life and can have a major impact on school attendance or work. The disease appears to be more active in children and teenagers than in adults.

Treatment is not standardized and no long-term medication has proven to be effective. Patients with a mild phenotype may be treated symptomatically with non-steroidal anti-inflammatory drugs. There is currently no therapeutic option available for patients with the most severe phenotype, and long-term treatment with interleukin (IL)-1 inhibitors (Anakinra, Kineret®) failed in the two cases tested [19].

The genetic defect of this disease was identified in 2008 [18] as a mutation in the gene encoding NLR pyrin domain-containing protein 12 (NLRP12) belonging to the intracellular Nod-like receptor (NLR) family. This protein is an intracellular sensor of the innate immune system, that regulates inflammatory processes through inhibition of nuclear factor kappa B (NF-κB) [18] and IL1β [16] signaling. NLRP12 mutations are likely responsible for a loss of protein function resulting in upregulation of this pro-inflammatory pathway. However, the exact role of NLRP12 remains unknown. It may participate in the formation of an NLRP3-independent inflammasome and be crucial for the recognition of intracellular pathogens. NLRP12 could also play an important role in the homeostasis of the gut by controlling the genesis of inflammatory diseases of the gastrointestinal tract and/or colorectal cancer [20,21]. Two unambiguous mutations, c.850C > T, p.Arg284*; c.2072 + 2dupT, p.Val635Thrfs*12 [18] as well as two missense substitutions c.1054C > T, p.Arg352Cys [16] and c.882C > G, p.Asp294Glu [17] were proven pathogenic through functional studies.

Deficiency of Interleukin 1 Receptor Antagonist (DIRA)

Sterile multifocal osteomyelitis with periostitis and pustulosis (OMPP) is more commonly referred to as DIRA [22]. DIRA is an early-onset auto-inflammatory disease that presents with neutrophilic pustular dermatosis, periostitis, aseptic multifocal osteomyelitis, and high acute-phase reactants. Patients develop pustular skin rashes, gastrointestinal reflux, and multifocal osteomyelitis during the neonatal period. One patient presented with early onset intrauterine disease and intrauterine fetal demise [23]. Massive systemic inflammatory syndrome resulting in patient death has been described [22]. Other manifestations include osteopenia, interstitial pneumonia often causing hypoxemia and dyspnea or localized ground-glass opacities and areas of atelectasis at chest computed tomography, vesicular stomatitis, mouth ulcers, ribs widening, periosteal reaction, joint swelling, cervical vertebra fusion, hepatosplenomegaly, thrombosis and vasculopathy [22,24-26]. Skin biopsies show neutrophilic epidermal and dermal infiltration, concomitant superficial folliculitis, with subcorneal localization of the pustules. Differential diagnosis includes other autoinflammatory conditions especially deficiency of the Interleukin 36 receptor antagonist (DITRA), dermatologic conditions (infantile pustular psoriasis, tinea, bacterial folliculitis, scabies, eosinophilic pustular folliculitis, erythema toxicum neonatorum, transient neonatal pustular melanosis…), and infectious diseases (arthritis, osteomyelitis).

Antibiotics and conventional disease-modifying antirheumatic drugs including steroids are of limited benefit, however blocking IL-1 signaling with anakinra dramatically improved clinical symptoms within days, resolving osteolytic lesions, normalizing acute-phase reactants, and permitting appropriate growth [22,24-29]. Patients with DIRA need to remain on lifelong IL-1 inhibitory therapy. Previous attempts at stopping or weaning anakinra have resulted in disease flares.

The disease is caused by mutations of the gene encoding the protein IL1RA. This protein is a natural antagonist of the potent proinflammatory interleukins-1 cytokines and mutations result in over activity of IL-1α as well as IL-1beta is expected in case of IL-1RA deficiency Two founder deletions were reported, one Puerto Rican: c.-64_1696del, p.IL1F9_IL1RNdel [22,24,27], and one Brazilian: c.213_227del, p.Asp72_Ile76del [25].

Deficiency of IL-36 receptor antagonist (DITRA)

Interleukin-36-receptor antagonist deficiency is a hereditary auto-inflammatory disease characterized by repeated flares of generalized pustular psoriasis (GPP). The flares include sudden diffuse pustular erythematous rash associated with high fever, general malaise, systemic inflammation and sometimes 'geographic tongue’ and nail dystrophy [30]. Organ inflammation such as cholangitis can occur during the disease course. In most patients, symptoms develop during childhood though the age of onset can vary considerably. Neonatal onset has also been reported. Failure to thrive may occur. Elevated C-reactive protein serum levels and marked leukocytosis are constant during disease attacks. Differential diagnosis includes other causes of GPP, mainly DIRA [22], in cases where symptoms appear during the first weeks of life.

There is no established treatment. Topical and oral steroids, vitamin D3, acitretin and anti-TNF-α, are effective. Our group has recently successfully treated an infant with DITRA not responding to topical and oral steroids or to acitretine with anakinra [31].

IL-36 receptor antagonist (IL-36RA) is a natural antagonist of IL-36α, IL-36β and IL-36γ, three cytokines belonging to the IL-1 family. Mutations result in decreased IL-36RA antagonistic effects due to a reduction of both IL-36RA protein stability and affinity for its receptor, the consequence of which is uncontrolled inflammation [30,32-37]. The high resulting expression of IL-36R and of the three agonists in epithelial tissues like skin likely causes GPP, the main clinical feature in all DITRA patients. In a recent study, Setta-Kafetzi et al. identified IL36RN variant alleles in palmarplantar pustulosis and acrodermatitis continua of hallopeau, two forms of GPP genetically distinct from psoriasis vulgaris [35].

Among the most frequent genetic alterations are one Tunisian founder missense mutation: c.80C > T, p.Leu27Pro1; one European recurrent missense mutation: c.338C > T, p.Ser113Leu2; and one Japanese founder nonsense mutation: c.28C > T, p.Arg10*3.

Psoriasis susceptibility (PSORS)2 and pityriasis rubra pilaris (PRP)

Psoriasis is a common and chronic immune-mediated inflammatory disease of the skin affecting approximately 2% of individuals of European descent with a strong genetic susceptibility [38]. Classic lesions consist of round, well-circumscribed erythematous plaques covered by a thick silver scale with a predilection for elbows, knees, scalp, lumbosacral and anogenital regions. Fingernail plate involvement includes pitting and distal onycholysis. Inverse psoriasis (flexural distribution), guttate psoriasis, pustular or erythrodermic psoriasis are other clinical variants. Pityriasis rubra pilaris (PRP) is a chronic skin disorder of abnormal keratinization classified by Griffiths into five types based on the age of onset and the clinical features [39]. Familial PRP belongs to the type V group (atypical juvenile) and accounts for about 5% of all cases. This chronic skin disorder usually presents at birth or appears during early childhood. It is characterized by small keratotic follicular papules forming disseminated salmon-colored scaly plaques that surround islands of normal skin, and diffuse red-orange palmoplantar keratoderma. Lesions typically progress rostral to caudal. While nails can be dystrophic, pitting of nails is not a feature of this disease. Skin biopsies can be performed if the clinical features or the responses to treatment are unusual. Histopathological analysis shows psoriasiform hyperplasia presenting as acanthosis with elongation of the rete ridges, parakeratosis and mononuclear cell infiltrate. Compared to psoriasis, the epidermal hyperplasia in PRP is more irregular, the granular layer is preserved, follicular plugging is characteristic and neutrophils in the stratum corneum are not essential. Differential diagnosis of psoriasis includes other papulosquamous disorders. PRP shows clinical features similar to phrynoderma (vitamin A deficiency), psoriasis, erythrokeratodermia and other causes of cornification.

Management of psoriasis includes patient education, topical therapy (corticosteroids, calcineurin inhibitor, calcipotriene, emollients, keratolytic agents), ultraviolet light, and systemic therapy (retinoids, methotrexate, cyclosporine and anti-TNF agents). The treatment of PRP is often disappointing. Milder cases of the disease can be treated with emollients, topical corticosteroids, tazarotene, keratolytic agents or calcineurin inhibitor whereas systemic retinoids and/or TNFα blocking agents are required in severe cases.

The prognosis of both disorders is that of most chronic diseases, with spontaneous remissions and exacerbations. Arthritis is present in about one fourth of psoriasis patients, and there is an increased risk of metabolic syndromes and cardiovascular diseases [40].

Both phenotypes have been associated to CAspase Recruitment Domain-containing protein 14 (CARD14) mutations [36,41-43]. CARD14 is an epidermal regulator of NF-κB transcription factor. Mutations in CARD14 initiate a process that includes inflammatory cell recruitment by keratinocytes and perpetuate a vicious cycle of epidermal inflammation and regeneration that cause the abnormal keratinization. More specifically, c.349G > A, p.Gly117Ser (the most prevalent mutation), and c.413A > C, p.Glu138Ala (a de novo mutation) were shown to lead to enhanced NF-κB activation and upregulation of a subset of psoriasis-associated genes in keratinocytes [43].

Disseminated Superficial Actinic Porokeratosis (DSAP)

This disease described in 1966 by Chernosky [44] represents the most common form of porokeratosis, a group of diseases characterized by epidermal cornification with epidermal cell hyperproliferation and premature apoptosis of keratinocytes. Triggers include ultraviolet light exposure and immunosuppression. Multiple small (0.5-1 cm) round and brownish lesions surrounded by a hyperkeratotic rim develop on sun-exposed areas of the skin particularly on the lower legs and forearms. Lesions usually appear in summer and improve or disappear during winter. The disease usually starts during the third or fourth decades of life, and rarely affects children. While it is usually benign, squamous cell carcinoma or Bowen’s disease may occasionally develop within the lesions.

Histopathological examination of the skin sampled from the edge of the peripheral rim characteristically shows an angulated cornoid lamella and a parakeratotic column overlying an area of epidermis with an absent or reduced granular layer [45]. Differential diagnosis includes neoplastic or hyperplastic squamous skin lesions.

Cryotherapy, topical reagents (retinoids, imiquimod, 5-fluorouracil, keratolytic), electrodessication, laser ablation or photodynamic therapy are used to destroy the abnormal keratinocyte clones [46].

The mode of inheritance is dominant however many sporadic cases of porokeratosis have been described [47]. Mutations in the MeValonate Kinase (MVK) gene were found in DSAP patients [48,49]. The MVK enzyme is involved in the biosynthesis of cholesterol and isoprenoid. It is also thought to play a role in regulating calcium-induced keratinocyte differentiation and could protect keratinocytes from apoptosis induced by type A ultraviolet radiation. All genetically confirmed patients are of Chinese origin. Fourteen different mutations have been found, among which, 10 accounted for one third of the familial cases. Mutations in this gene were initially demonstrated as responsible for recessive complete (mevalonic aciduria [50], OMIM 610377) and incomplete (hyperIgD syndrome [51,52], OMIM 260920) mevalonate kinase deficiency.

Autoinflammation, LipoDystrophy, and Dermatosis syndrome (ALDD)

ALDD is a systemic inflammatory condition starting within the first months of life, and comprising elevated fever, panniculitis with lipoatrophy, purplish and swollen eyelids, arthralgia, developmental retardation, and increased acute phase reactants [53,54]. Key symptoms include a persistent fever of >38.5°C, steroid-sensitive erythema nodosum-like (edematous and purpuric) plaques, long clubbed fingers, hyperhidrosis, myositis, hepatosplenomegaly, macroglossia, facial and limbs lipoatrophy, and developmental (height, weight and IQ) retardation. Skin biopsies show immature myeloid-lineage cells with mitoses. Some patients may have joint contracture, auricular and nasal chondritis, and calcification of the basal ganglia. Acute cardiovascular event is the leading cause of death in these patients for whom life expectancy is notably reduced. Differential diagnosis includes other autoinflammatory conditions, in particular Sweet’s syndrome, Still’s disease and Chronic, Infantile, Neurological, Cutaneous and Articular (CINCA) syndrome, storage diseases (mucopolysaccharidosis), lupus, dermatomyositis, laminopathies (progeroid syndromes), and other interferonopathies like Aicardi Goutieres syndrome, an interferon type I related disease. Biological findings include microcytic or normocytic anemia, thrombopenia (rare), mild increase in levels of amino transferase enzymes, perturbation of glucose and lipid metabolism (hyperglycemia and glucose intolerance, increased cholesterol and triglycerides), increased erythrocyte sedimentation rate and γ globulins levels, and some markers of autoimmunity (antinuclear and anti-neutrophilic cytoplasmic auto-antibodies, lupus anticoagulant, positive Coombs test).

Management of these patients is by palliative care. The need for steroids is very high even in combination with anti IL-1, anti IL-6 or anti-TNF treatments. Drugs targeting interferon γ are warranted. JAK kinase inhibitors are currently under clinical trials at the National Institute of Health, Bethesda, USA [55].

Most (N = 28) of the reported patients carried homozygous mutations in the Proteasome Subunit, Beta-Type, 8 (PSMB8) gene [53,54,56,57]. This gene encodes β5i, a catalytic subunit of the immunoproteasome, an intracellular protease complex specialized for degradation of polyubiquitinated proteins. This ubiquitin-proteasome system degrades unnecessary proteins and regulates the cell cycle, gene repair and nuclear factor NF-κB activation [53]. The mutated protein impairs the assembly of this immunoproteasome. One nonsense (c.405C > A, p.Cys135*) [54] and five missense mutations of which two are recurrent (c.224C > T, p.Thr75Met and c.602G > T, p.Gly201Val) have been reported [9]. As the prognosis is so severe, prenatal diagnosis can be discussed.

Conclusions

Hereditary recurrent fevers, as well as Majeed syndrome, Blau syndrome, and Pyogenic sterile Arthritis, Pyoderma gangrenosum and Acne (PAPA) syndrome, have been extensively reviewed since the concept of autoinflammation was created in 1999 [58]. However, very little information has been assembled regarding the phenotype, genetics and epidemiology of the more recently discovered autoinflammatory disorders. Here in this review, we aimed to offer novel diagnostic options to those patients for whom a genetic link could not be established. More than 25 autoinflammatory genes were listed during the last international conference on autoinflammation, Lausanne, 23-26 May, 2013, including at least five to six new ones in the pipeline. Both phenotype and genotype heterogeneity have been described which further hinders correct diagnosis and highlights the necessity for a gene and disease nomenclature consensus. A systematic in-depth description of the clinical features of these patients has been undertaken thanks to the Eurofever initiative [59,60]. Massively parallel sequencing approaches should help in identifying the causative gene among those already known or novel genes through whole exome or genome sequencing. Development of such innovative genetic diagnostic tools is in progress through an International network (I Touitou, personal communication).

The correct diagnosis of these diseases is essential for the relevant management of patients affected by rare autoinflammatory diseases as remarkably effective therapies have been developed recently which have the potential to avoid the risk of fatal complications such as amyloidosis, or sensorineural impairment. Rarely emphasized yet equally important is being able, even after many years as in some cases, to name the patient’s disease, which can be extremely useful from a psychological point of view.

Competing interests

The authors declare that they have no competing interests.

Authors’ contributions

IT and IKP conceived and designed the manuscript. IKP coordinated and assigned the writing of the different disease items: CG: DIRA; LR: DITRA; IKP: ALDD; VH: NALP12; MP: DSAP and PRP. IT collected the data, assembled the first draft, and polished the manuscript. All authors read the final manuscript and gave approval for the version to be published. All authors read and approved the final manuscript.

Authors’ information

All authors are members of the French reference centre for autoinflammatory diseases (CeRéMAI, [http://asso.orpha.net/CEREMAI/EN/index.html]) coordinated by IKP. IT developed infevers [http://fmf.igh.cnrs.fr/ISSAID/infevers/], an online registry devoted to autoinflammatory disease mutations.

Contributor Information

Isabelle Touitou, Email: isabelle.touitou@inserm.fr.

Caroline Galeotti, Email: caroline.galeotti@bct.aphp.fr.

Linda Rossi-Semerano, Email: linda.rossi@bct.aphp.fr.

Véronique Hentgen, Email: vhentgen@ch-versailles.fr.

Maryam Piram, Email: maryam.piram@bct.aphp.fr.

Isabelle Koné-Paut, Email: isabelle.kone-paut@bct.aphp.fr.

Acknowledgements

This work was supported by the French Ministry of Health, and the Kremlin Bicêtre, Versailles and Montpellier hospitals. We thank Angloscribe for editing the manuscript for English language.

References

  1. Kastner DL, Aksentijevich I, Goldbach-Mansky R. Autoinflammatory disease reloaded: a clinical perspective. Cell. 2010;8:784–790. doi: 10.1016/j.cell.2010.03.002. [DOI] [PMC free article] [PubMed] [Google Scholar]
  2. Consortium TFF. A candidate gene for familial Mediterranean fever. Nat Genet. 1997;8:25–31. doi: 10.1038/ng0997-25. [DOI] [PubMed] [Google Scholar]
  3. TheInternationalFMFConsortium. Ancient missense mutations in a new member of the RoRet gene family are likely to cause familial Mediterranean fever. Cell. 1997;8:797–807. doi: 10.1016/s0092-8674(00)80539-5. [DOI] [PubMed] [Google Scholar]
  4. Conforti-Andreoni C, Ricciardi-Castagnoli P, Mortellaro A. The inflammasomes in health and disease: from genetics to molecular mechanisms of autoinflammation and beyond. Cell Mol Immunol. 2011;8:135–145. doi: 10.1038/cmi.2010.81. [DOI] [PMC free article] [PubMed] [Google Scholar]
  5. Schroder K, Tschopp J. The inflammasomes. Cell. 2010;8:821–832. doi: 10.1016/j.cell.2010.01.040. [DOI] [PubMed] [Google Scholar]
  6. Jeru I, Amselem S. Inflammasome and interleukin 1. Rev Med Interne. 2011;8(4):218–224. doi: 10.1016/j.revmed.2010.02.013. doi:10.1016/j.revmed.2010.02.013. Epub 2010 Jun 11. French. [DOI] [PubMed] [Google Scholar]
  7. Touitou I. Inheritance of autoinflammatory diseases: shifting paradigms and nomenclature. J Med Genet. 2013;8:349–359. doi: 10.1136/jmedgenet-2013-101577. [DOI] [PubMed] [Google Scholar]
  8. Ter Haar N, Lachmann H, Ozen S, Woo P, Uziel Y, Modesto C, Kone-Paut I, Cantarini L, Insalaco A, Neven B. et al. Treatment of autoinflammatory diseases: results from the Eurofever Registry and a literature review. Ann Rheum Dis. 2013;8(5):678–685. doi: 10.1136/annrheumdis-2011-201268. doi:10.1136/annrheumdis-2011-201268. Epub 2012 Jun 29. [DOI] [PubMed] [Google Scholar]
  9. Milhavet F, Cuisset L, Hoffman HM, Slim R, El-Shanti H, Aksentijevich I, Lesage S, Waterham H, Wise C, Sarrauste Dementhiere C. et al. The infevers autoinflammatory mutation online registry: update with new genes and functions. Hum Mutat. 2008;8:803–808. doi: 10.1002/humu.20720. [DOI] [PubMed] [Google Scholar]
  10. De Jesus J, Imane Z, Senee V, Romero S, Guillausseau PJ, Balafrej A, Julier C. SLC29A3 mutation in a patient with syndromic diabetes with features of pigmented hypertrichotic dermatosis with insulin-dependent diabetes, H syndrome and Faisalabad histiocytosis. Diabetes Metab. 2013;8:281–285. doi: 10.1016/j.diabet.2013.03.007. [DOI] [PubMed] [Google Scholar]
  11. Melki I, Lambot K, Jonard L, Couloigner V, Quartier P, Neven B, Bader-Meunier B. Mutation in the SLC29A3 gene: a new cause of a monogenic, autoinflammatory condition. Pediatrics. 2013;8:e1308–e1313. doi: 10.1542/peds.2012-2255. [DOI] [PubMed] [Google Scholar]
  12. Mohanan S, Chandrashekar L, Semple RK, Thappa DM, Rajesh NG, Negi VS, Gulati R. H syndrome with a novel homozygous R134C mutation in SLC29A3 gene. Int J Dermatol. 2013;8:820–823. doi: 10.1111/j.1365-4632.2012.05838.x. [DOI] [PubMed] [Google Scholar]
  13. Senniappan S, Hughes M, Shah P, Shah V, Kaski JP, Brogan P, Hussain K. Pigmentary hypertrichosis and non-autoimmune insulin-dependent diabetes mellitus (PHID) syndrome is associated with severe chronic inflammation and cardiomyopathy, and represents a new monogenic autoinflammatory syndrome. J Pediatr Endocrinol Metab. 2013;8:6. doi: 10.1515/jpem-2013-0062. [DOI] [PubMed] [Google Scholar]
  14. Zhou Q, Lee GS, Brady J, Datta S, Katan M, Sheikh A, Martins MS, Bunney TD, Santich BH, Moir S. et al. A Hypermorphic Missense Mutation in PLCG2, Encoding Phospholipase Cgamma2, Causes a Dominantly Inherited Autoinflammatory Disease with Immunodeficiency. Am J Hum Genet. 2012;8:713–720. doi: 10.1016/j.ajhg.2012.08.006. [DOI] [PMC free article] [PubMed] [Google Scholar]
  15. Boisson B, Laplantine E, Prando C, Giliani S, Israelsson E, Xu Z, Abhyankar A, Israel L, Trevejo-Nunez G, Bogunovic D. et al. Immunodeficiency, autoinflammation and amylopectinosis in humans with inherited HOIL-1 and LUBAC deficiency. Nat Immunol. 2012;8:1178–1186. doi: 10.1038/ni.2457. [DOI] [PMC free article] [PubMed] [Google Scholar]
  16. Jeru I, Le Borgne G, Cochet E, Hayrapetyan H, Duquesnoy P, Grateau G, Morali A, Sarkisian T, Amselem S. Identification and functional consequences of a recurrent NLRP12 missense mutation in periodic fever syndromes. Arthritis Rheum. 2012;8:1459–1464. doi: 10.1002/art.30241. [DOI] [PubMed] [Google Scholar]
  17. Borghini S, Tassi S, Chiesa S, Caroli F, Carta S, Caorsi R, Fiore M, Delfino L, Lasiglie D, Ferraris C. et al. Clinical presentation and pathogenesis of cold-induced autoinflammatory disease in a family with recurrence of an NLRP12 mutation. Arthritis Rheum. 2011;8:830–839. doi: 10.1002/art.30170. [DOI] [PMC free article] [PubMed] [Google Scholar]
  18. Jeru I, Duquesnoy P, Fernandes-Alnemri T, Cochet E, Yu JW, Lackmy-Port-Lis M, Grimprel E, Landman-Parker J, Hentgen V, Marlin S. et al. Mutations in NALP12 cause hereditary periodic fever syndromes. Proc Natl Acad Sci U S A. 2008;8:1614–1619. doi: 10.1073/pnas.0708616105. [DOI] [PMC free article] [PubMed] [Google Scholar]
  19. Jeru I, Hentgen V, Normand S, Duquesnoy P, Cochet E, Delwail A, Grateau G, Marlin S, Amselem S, Lecron JC. Role of interleukin-1beta in NLRP12-associated autoinflammatory disorders and resistance to anti-interleukin-1 therapy. Arthritis Rheum. 2011;8:2142–2148. doi: 10.1002/art.30378. [DOI] [PubMed] [Google Scholar]
  20. Allen IC, Wilson JE, Schneider M, Lich JD, Roberts RA, Arthur JC, Woodford RM, Davis BK, Uronis JM, Herfarth HH. et al. NLRP12 suppresses colon inflammation and tumorigenesis through the negative regulation of noncanonical NF-kappaB signaling. Immunity. 2012;8:742–754. doi: 10.1016/j.immuni.2012.03.012. [DOI] [PMC free article] [PubMed] [Google Scholar]
  21. Zaki MH, Vogel P, Malireddi RK, Body-Malapel M, Anand PK, Bertin J, Green DR, Lamkanfi M, Kanneganti TD. The NOD-like receptor NLRP12 attenuates colon inflammation and tumorigenesis. Cancer Cell. 2011;8:649–660. doi: 10.1016/j.ccr.2011.10.022. [DOI] [PMC free article] [PubMed] [Google Scholar]
  22. Aksentijevich I, Masters SL, Ferguson PJ, Dancey P, Frenkel J, Van Royen-Kerkhoff A, Laxer R, Tedgard U, Cowen EW, Pham TH. et al. An autoinflammatory disease with deficiency of the interleukin-1-receptor antagonist. N Engl J Med. 2009;8:2426–2437. doi: 10.1056/NEJMoa0807865. [DOI] [PMC free article] [PubMed] [Google Scholar]
  23. Altiok E, Aksoy F, Perk Y, Taylan F, Kim PW, Ilikkan B, Asal GT, Goldbach-Mansky R, Sanal O. A novel mutation in the interleukin-1 receptor antagonist associated with intrauterine disease onset. Clin Immunol. 2012;8:77–81. doi: 10.1016/j.clim.2012.08.003. [DOI] [PMC free article] [PubMed] [Google Scholar]
  24. Reddy S, Jia S, Geoffrey R, Lorier R, Suchi M, Broeckel U, Hessner MJ, Verbsky J. An autoinflammatory disease due to homozygous deletion of the IL1RN locus. N Engl J Med. 2009;8:2438–2444. doi: 10.1056/NEJMoa0809568. [DOI] [PMC free article] [PubMed] [Google Scholar]
  25. Jesus AA, Osman M, Silva CA, Kim PW, Pham TH, Gadina M, Yang B, Bertola DR, Carneiro-Sampaio M, Ferguson PJ. et al. A novel mutation of IL1RN in the deficiency of interleukin-1 receptor antagonist syndrome: description of two unrelated cases from Brazil. Arthritis Rheum. 2011;8:4007–4017. doi: 10.1002/art.30588. [DOI] [PMC free article] [PubMed] [Google Scholar]
  26. Stenerson M, Dufendach K, Aksentijevich I, Brady J, Austin J, Reed AM. The first reported case of compound heterozygous IL1RN mutations causing deficiency of the interleukin-1 receptor antagonist. Arthritis Rheum. 2011;8:4018–4022. doi: 10.1002/art.30565. [DOI] [PubMed] [Google Scholar]
  27. Minkis K, Aksentijevich I, Goldbach-Mansky R, Magro C, Scott R, Davis JG, Sardana N, Herzog R. Interleukin 1 receptor antagonist deficiency presenting as infantile pustulosis mimicking infantile pustular psoriasis. Arch Dermatol. 2012;8:747–752. doi: 10.1001/archdermatol.2011.3208. [DOI] [PMC free article] [PubMed] [Google Scholar]
  28. Schnellbacher C, Ciocca G, Menendez R, Aksentijevich I, Goldbach-Mansky R, Duarte AM, Rivas-Chacon R. Deficiency of Interleukin-1 Receptor Antagonist Responsive to Anakinra. Pediatr Dermatol. 2012. doi:10.1111/j.1525-1470.2012.01725.x. [Epub ahead of print] [DOI] [PMC free article] [PubMed]
  29. Brau-Javier CN, Gonzales-Chavez J, Toro JR. Chronic cutaneous pustulosis due to a 175-kb deletion on chromosome 2q13: excellent response to anakinra. Arch Dermatol. 2012;8:301–304. doi: 10.1001/archdermatol.2011.2857. [DOI] [PMC free article] [PubMed] [Google Scholar]
  30. Marrakchi S, Guigue P, Renshaw BR, Puel A, Pei XY, Fraitag S, Zribi J, Bal E, Cluzeau C, Chrabieh M. et al. Interleukin-36-receptor antagonist deficiency and generalized pustular psoriasis. N Engl J Med. 2011;8:620–628. doi: 10.1056/NEJMoa1013068. [DOI] [PubMed] [Google Scholar]
  31. Rossi-Semerano L, Piram M, Chiaverini C, De Ricaud D, Smahi A, Kone-Paut I. First Clinical Description of an Infant With Interleukin-36-Receptor Antagonist Deficiency Successfully Treated With Anakinra. Pediatrics. 2013;8(4):e1043–e1047. doi: 10.1542/peds.2012-3935. Epub 2013 Sep 9. [DOI] [PubMed] [Google Scholar]
  32. Onoufriadis A, Simpson MA, Pink AE, Di Meglio P, Smith CH, Pullabhatla V, Knight J, Spain SL, Nestle FO, Burden AD. et al. Mutations in IL36RN/IL1F5 are associated with the severe episodic inflammatory skin disease known as generalized pustular psoriasis. Am J Hum Genet. 2011;8:432–437. doi: 10.1016/j.ajhg.2011.07.022. [DOI] [PMC free article] [PubMed] [Google Scholar]
  33. Sugiura K, Takeichi T, Kono M, Ogawa Y, Shimoyama Y, Muro Y, Akiyama M. A novel IL36RN/IL1F5 homozygous nonsense mutation, p.Arg10X, in a Japanese patient with adult-onset generalized pustular psoriasis. Br J Dermatol. 2012;8:699–701. doi: 10.1111/j.1365-2133.2012.10953.x. [DOI] [PubMed] [Google Scholar]
  34. Farooq M, Nakai H, Fujimoto A, Fujikawa H, Matsuyama A, Kariya N, Aizawa A, Fujiwara H, Ito M, Shimomura Y. Mutation Analysis of the IL36RN Gene in 14 Japanese Patients with Generalized Pustular Psoriasis. Hum Mutat. 2013;8:176–183. doi: 10.1002/humu.22203. [DOI] [PubMed] [Google Scholar]
  35. Setta-Kaffetzi N, Navarini AA, Patel VM, Pullabhatla V, Pink AE, Choon SE, Allen MA, Burden AD, Griffiths CE, Seyger MM. et al. Rare Pathogenic Variants in IL36RN Underlie a Spectrum of Psoriasis-Associated Pustular Phenotypes. J Invest Dermatol. 2013;8(5):1366–1369. doi: 10.1038/jid.2012.490. doi:10.1038/jid.2012.490. Epub 2013 Jan 10. [DOI] [PubMed] [Google Scholar]
  36. Korber A, Mossner R, Renner R, Sticht H, Wilsmann-Theis D, Schulz P, Sticherling M, Traupe H, Huffmeier U. Mutations in IL36RN in Patients with Generalized Pustular Psoriasis. J Invest Dermatol. 2013. doi:10.1038/jid.2013.214. [Epub ahead of print] [DOI] [PubMed]
  37. Navarini AA, Valeyrie-Allanore L, Setta-Kaffetzi N, Barker JN, Capon F, Creamer D, Roujeau JC, Sekula P, Simpson MA, Trembath RC. et al. Rare Variations in IL36RN in Severe Adverse Drug Reactions Manifesting as Acute Generalized Exanthematous Pustulosis. J Invest Dermatol. 2013;8:1904–1907. doi: 10.1038/jid.2013.44. [DOI] [PubMed] [Google Scholar]
  38. Fung MA, Barr KL. Current knowledge in inflammatory dermatopathology. Dermatol Clin. 2012;8:667–684. doi: 10.1016/j.det.2012.06.004. [DOI] [PubMed] [Google Scholar]
  39. Griffiths WA. Pityriasis rubra pilaris: the problem of its classification. J Am Acad Dermatol. 1992;8:140–142. doi: 10.1016/s0190-9622(08)80543-9. [DOI] [PubMed] [Google Scholar]
  40. Tsoi LC, Spain SL, Knight J, Ellinghaus E, Stuart PE, Capon F, Ding J, Li Y, Tejasvi T, Gudjonsson JE. et al. Identification of fifteen new psoriasis susceptibility loci highlights the role of innate immunity. Nat Genet. 2012;8:1341–1348. doi: 10.1038/ng.2467. [DOI] [PMC free article] [PubMed] [Google Scholar]
  41. Ammar M, Bouchlaka-Souissi C, Zaraa I, Helms C, Doss N, Bouazizi F, Dhaoui R, Ossman AB. Ammar-el Gaied AB, Mokni M: Family-based association study in Tunisian familial psoriasis. Int J Dermatol. 2012;8:1329–1334. doi: 10.1111/j.1365-4632.2012.05523.x. [DOI] [PubMed] [Google Scholar]
  42. Fuchs-Telem D, Sarig O, Van Steensel MA, Isakov O, Israeli S, Nousbeck J, Richard K, Winnepenninckx V, Vernooij M, Shomron N. et al. Familial pityriasis rubra pilaris is caused by mutations in CARD14. Am J Hum Genet. 2012;8:163–170. doi: 10.1016/j.ajhg.2012.05.010. [DOI] [PMC free article] [PubMed] [Google Scholar]
  43. Jordan CT, Cao L, Roberson ED, Pierson KC, Yang CF, Joyce CE, Ryan C, Duan S, Helms CA, Liu Y. et al. PSORS2 is due to mutations in CARD14. Am J Hum Genet. 2012;8:784–795. doi: 10.1016/j.ajhg.2012.03.012. [DOI] [PMC free article] [PubMed] [Google Scholar]
  44. Chernosky ME. Porokeratosis: report of twelve patients with multiple superficial lesions. South Med J. 1966;8:289–294. doi: 10.1097/00007611-196603000-00011. [DOI] [PubMed] [Google Scholar]
  45. Rouhani P, Fischer M, Meehan S, Pomeranz MK. Disseminated superficial actinic porokeratosis. Dermatol Online J. 2012;8:24. [PubMed] [Google Scholar]
  46. Skupsky H, Skupsky J, Goldenberg G. Disseminated superficial actinic porokeratosis: a treatment review. J Dermatolog Treat. 2012;8:52–56. doi: 10.3109/09546634.2010.495381. [DOI] [PubMed] [Google Scholar]
  47. Kaur S, Thami GP, Mohan H, Kanwar AJ. Co-existence of variants of porokeratosis: a case report and a review of the literature. J Dermatol. 2002;8:305–309. doi: 10.1111/j.1346-8138.2002.tb00268.x. [DOI] [PubMed] [Google Scholar]
  48. Zhou Y, Liu J, Fu X, Yu Y, Shi B, Yu G, Shi Z, Wu W, Pan F, Tian H. et al. Identification of three novel frameshift mutations of the MVK gene in four Chinese families with disseminated superficial actinic porokeratosis. Br J Dermatol. 2013;8:193–195. doi: 10.1111/bjd.12224. [DOI] [PubMed] [Google Scholar]
  49. Zhang SQ, Jiang T, Li M, Zhang X, Ren YQ, Wei SC, Sun LD, Cheng H, Li Y, Yin XY. et al. Exome sequencing identifies MVK mutations in disseminated superficial actinic porokeratosis. Nat Genet. 2012;8:1156–1160. doi: 10.1038/ng.2409. [DOI] [PubMed] [Google Scholar]
  50. Schafer BL, Bishop RW, Kratunis VJ, Kalinowski SS, Mosley ST, Gibson KM, Tanaka RD. Molecular cloning of human mevalonate kinase and identification of a missense mutation in the genetic disease mevalonic aciduria. J Biol Chem. 1992;8:13229–13238. [PubMed] [Google Scholar]
  51. Drenth JP, Cuisset L, Grateau G, Vasseur C, van de Velde-Visser SD, De Jong JG, Beckmann JS, van der Meer JW, Delpech M. Mutations in the gene encoding mevalonate kinase cause hyper-IgD and periodic fever syndrome. International Hyper-IgD Study Group. Nat Genet. 1999;8:178–181. doi: 10.1038/9696. [DOI] [PubMed] [Google Scholar]
  52. Houten SM, Kuis W, Duran M, De Koning TJ, Van Royen-Kerkhof A, Romeijn GJ, Frenkel J, Dorland L, De Barse MM, Huijbers WA. et al. Mutations in MVK, encoding mevalonate kinase, cause hyperimmunoglobulinaemia D and periodic fever syndrome. Nat Genet. 1999;8:175–177. doi: 10.1038/9691. [DOI] [PubMed] [Google Scholar]
  53. Arima K, Kinoshita A, Mishima H, Kanazawa N, Kaneko T, Mizushima T, Ichinose K, Nakamura H, Tsujino A, Kawakami A. et al. Proteasome assembly defect due to a proteasome subunit beta type 8 (PSMB8) mutation causes the autoinflammatory disorder, Nakajo-Nishimura syndrome. Proc Natl Acad Sci U S A. 2011;8:14914–14919. doi: 10.1073/pnas.1106015108. [DOI] [PMC free article] [PubMed] [Google Scholar]
  54. Liu Y, Ramot Y, Torrelo A, Paller AS, Si N, Babay S, Kim PW, Sheikh A, Lee CC, Chen Y. et al. Mutations in proteasome subunit beta type 8 cause chronic atypical neutrophilic dermatosis with lipodystrophy and elevated temperature with evidence of genetic and phenotypic heterogeneity. Arthritis Rheum. 2012;8:895–907. doi: 10.1002/art.33368. [DOI] [PMC free article] [PubMed] [Google Scholar]
  55. Compassionate Use Treatment Protocol I4V-MC-JAGA. Treatment of Autoinflammatory Syndromes Expected to Benefit from JAK Inhibition. http://clinicalstudies.info.nih.gov/cgi/wais/bold032001.pl?A_12-AR-8001.html@CANDLE@@@@.
  56. Agarwal AK, Xing C, DeMartino GN, Mizrachi D, Hernandez MD, Sousa AB, Martinez DeVillarreal L, DosSantos HG, Garg A. PSMB8 encoding the beta5i proteasome subunit is mutated in joint contractures, muscle atrophy, microcytic anemia, and panniculitis-induced lipodystrophy syndrome. Am J Hum Genet. 2010;8:866–872. doi: 10.1016/j.ajhg.2010.10.031. [DOI] [PMC free article] [PubMed] [Google Scholar]
  57. Kanazawa N. Nakajo-Nishimura syndrome: an autoinflammatory disorder showing pernio-like rashes and progressive partial lipodystrophy. Allergol Int. 2012;8:197–206. doi: 10.2332/allergolint.11-RAI-0416. [DOI] [PubMed] [Google Scholar]
  58. McDermott MF, Aksentijevich I, Galon J, McDermott EM, Ogunkolade BW, Centola M, Mansfield E, Gadina M, Karenko L, Pettersson T. et al. Germline mutations in the extracellular domains of the 55 kDa TNF receptor, TNFR1, define a family of dominantly inherited autoinflammatory syndromes. Cell. 1999;8:133–144. doi: 10.1016/s0092-8674(00)80721-7. [DOI] [PubMed] [Google Scholar]
  59. Toplak N, Frenkel J, Ozen S, Lachmann HJ, Woo P, Kone-Paut I, De Benedetti F, Neven B, Hofer M, Dolezalova P. et al. An international registry on autoinflammatory diseases: the Eurofever experience. Ann Rheum Dis. 2012;8:1177–1182. doi: 10.1136/annrheumdis-2011-200549. [DOI] [PubMed] [Google Scholar]
  60. Ozen S, Frenkel J, Ruperto N, Gattorno M. The Eurofever Project: towards better care for autoinflammatory diseases. Eur J Pediatr. 2011;8:445–452. doi: 10.1007/s00431-011-1411-z. [DOI] [PubMed] [Google Scholar]

Articles from Orphanet Journal of Rare Diseases are provided here courtesy of BMC

RESOURCES