Aberrant CARD14 function might cause defective barrier formation

Murase, Yuya; Takeichi, Takuya; Akiyama, Masashi

doi:10.1016/j.jaci.2018.11.044

Cited by 7 publications

(6 citation statements)

References 5 publications

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“…The present CARD14 variant, p.Asp176His, is known as a gain‐of‐function variant that causes increased NF‐κB activation 4 . We previously reported a case of PRP who showed cutaneous features of CAPE, eczematous lesions and moderately elevated serum IgE and TARC, which suggested defective barrier function 3 . In addition, Peled et al 5 .…”

Section: Figurementioning

confidence: 96%

“…Genomic DNA from the patient's peripheral blood leukocytes was used for Sanger sequencing analysis as described previously 1 . She had a previously reported heterozygous missense variant in CARD14 , c.526G>C (p.Asp176His) 1,3 . None of the 10 loss‐of‐function FLG mutations reported in the Japanese population was found in the genomic DNA of the patient.…”

Section: Figurementioning

confidence: 99%

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A patient with CARD14‐associated papulosquamous eruptions showing atopic dermatitis‐like features

Takeichi

Terawaki²,

Kubota³

et al. 2020

Acad Dermatol Venereol

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Section: Figurementioning

confidence: 96%

Section: Figurementioning

confidence: 99%

A patient with CARD14‐associated papulosquamous eruptions showing atopic dermatitis‐like features

Takeichi

Terawaki²,

Kubota³

et al. 2020

Acad Dermatol Venereol

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“…173 Eczematous lesions and both high IgE and thymusand activation-regulated chemokine were also found in 2 unrelated patients with the missense CARD14 mutation D176H in addition to their respective T H 17-associated diagnoses (pityriasis rubra pilaris and CARD14-associated papulosquamous eruption). 174,175 A sixth patient with the CARD14 missense Q223H had severe AD, multiple food allergies, and enteropathy in the context of an immune dysregulation, polyendocrinopathy, enteropathy, X-linked-like disease. 176 Although the underlying mechanisms are largely unknown, these studies illustrate the clinical heterogeneity of CARD14 mutations and expands the spectrum of CARD14-related inflammatory diseases to include T H 2related manifestations.…”

Section: Caspase Activation and Recruitment Domain 14 Card14 In Aller...mentioning

confidence: 99%

“…As discussed earlier, several CARD14 missense mutations (D176H, Q223H, I593T, and N737H) have been found in patients with AD or eczematous lesions. [173][174][175][176] Although the functional impacts of the D176H and Q223H mutations on CARD14 signaling are unclear, 5,179 the I593T and N737H mutations are DN mutations that attenuate keratinocyte NF-kB signaling. However, CARD14-deficient mice do not develop spontaneous AD, 165,180 suggesting that at least some low-level-but not absent-CARD14 signaling is required to promote AD.…”

Section: Card14 In Admentioning

confidence: 99%

The role of the CBM complex in allergic inflammation and disease

DeVore

Hershey²

2022

Journal of Allergy and Clinical Immunology

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“…Autoinflammatory keratinization disease (AiKD) is an umbrella term recently introduced to describe inflammatory keratinization diseases caused by mutations in single genes associated with autoinflammatory diseases (6,7). AiKDs are genetically heterogeneous, and their different subtypes show various clinical features, complications, and prognoses (8)(9)(10)(11). We propose that KLICK syndrome associated with the POMP mutation be categorized as an AiKD.…”

Section: Introductionmentioning

confidence: 99%

KLICK Syndrome Linked to a POMP Mutation Has Features Suggestive of an Autoinflammatory Keratinization Disease

Takeichi

Akiyama

2020

Front. Immunol.

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Keratosis linearis with ichthyosis congenita and sclerosing keratoderma (KLICK) syndrome is a rare autosomal recessive skin disorder characterized by palmoplantar keratoderma, linear hyperkeratotic plaques, ichthyosiform scaling, circular constrictions around the fingers, and numerous papules distributed linearly in the arm folds and on the wrists. Histologically, the affected skin shows hypertrophy and hyperplasia of the spinous, granular, and horny epidermal layers with mild infiltration of inflammatory cells in the upper dermis. There are 14 patients with KLICK syndrome described in the literature, and they all carry the same nucleotide deletion. Proteasome maturation protein (POMP), encoded by POMP, is an ubiquitously expressed protein that functions as a chaperone for proteasome maturation. KLICK syndrome is caused by a reduction in POMP levels that leads to proteasome insufficiency in differentiating keratinocytes. It is noteworthy that POMP is also known to be the causative gene for proteasome-associated autoinflammatory syndrome-2 (PRAAS2). It is considered that the disrupted proteasome assembly caused by the POMP mutation might lead to both skin inflammation and then hyperkeratosis in KLICK syndrome. Inflammation caused by the hyperactivation of innate immunity occasionally leads to inflammatory diseases of the skin, recently denoted as autoinflammatory keratinization diseases (AiKDs). We propose that KLICK syndrome caused by the specific 1-bp nucleotide deletion mutation in the regulatory region of POMP might be in a spectrum of proteasome-associated phenotypes.

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Aberrant CARD14 function might cause defective barrier formation

Cited by 7 publications

References 5 publications

A patient with CARD14‐associated papulosquamous eruptions showing atopic dermatitis‐like features

A patient with CARD14‐associated papulosquamous eruptions showing atopic dermatitis‐like features

The role of the CBM complex in allergic inflammation and disease

KLICK Syndrome Linked to a POMP Mutation Has Features Suggestive of an Autoinflammatory Keratinization Disease

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