Plakophilin-3-Deficient Mice Develop Hair Coat Abnormalities and Are Prone to Cutaneous Inflammation

Sklyarova, Tatyana; Bonné, Stefan; D'hooge, Petra; Denecker, Geertrui; Goossens, Steven; Rycke, Riet De; Borgonie, Gaëtan; Bösl, Michael R.; Roy, Frans van; Hengel, Jolanda van

doi:10.1038/sj.jid.5701189

Cited by 72 publications

(82 citation statements)

References 42 publications

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“…Recently a new syndrome featuring severe dermatitis, multiple allergies, and metabolic wasting (SAM syndrome) caused by homozygous mutations in DSG1 supports the hypothesis that impaired epidermal barrier function may also contribute to the development of infl ammatory skin diseases (Samuelov et al, 2013). Data from mice defi cient in plakophilin-3 (PKP3), a member of the Armadillo-repeat family, and a component of desmosomes also strongly supports this hypothesis (Sklyarova et al, 2008). In the basal layer of PKP3-null epidermis, densities of desmosomes, and AJs were remarkably altered.…”

Section: Desmosomes and Keratin Network In Skin Inflammationsupporting

confidence: 48%

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Junctions and Inflammation in the Skin

Kobielak

Boddupally

2014

Cell Communication & Adhesion

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The skin forms a life-sustaining barrier between the organism and physical environment. The physical barrier of skin is mainly localized in the stratum corneum (SC); however, nucleated epidermis also contributes to the barrier through tight, gap, and adherens junctions (AJs), as well as through desmosomes and cytoskeletal elements. Many infl ammatory diseases, such as atopic dermatitis (AD) and psoriasis, are associated with barrier dysfunction. It is becoming increasingly clear that the skin barrier function is not only affected by infl ammatory signals but that defects in structural components of the barrier may be the initiating event for infl ammatory diseases. This view is supported by fi ndings that mutations in fi laggrin, a key structural epidermal barrier protein, cause the infl ammatory skin disease AD, and that a loss of AJ components, namely epidermal p120 catenin or α -catenin results in skin infl ammation.

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Section: Desmosomes and Keratin Network In Skin Inflammationsupporting

confidence: 48%

“…In the basal layer of PKP3-null epidermis, densities of desmosomes, and AJs were remarkably altered. PKP3-null mice were prone to dermatitis providing in vivo evidence that PKP3 plays a critical role in limiting infl ammatory responses in the skin (Sklyarova et al, 2008).…”

Section: Desmosomes and Keratin Network In Skin Inflammationmentioning

confidence: 99%

Junctions and Inflammation in the Skin

Kobielak

Boddupally

2014

Cell Communication & Adhesion

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“…However, PKP2 KO mice died around day 11.5 of embryonic development because of heart defects, indicating that at least one PKP is required for stable intercellular adhesion (Grossmann et al 2004). In contrast, PKP3 2/2 mice were viable but developed hair abnormalities and increased inflammation of the skin, manifest in mice kept in a nonpathogen-free environment (Sklyarova et al 2008). We have recently shown that PKP1 is essential for epidermal integrity in vivo.…”

Section: Evidence From Mouse Models and Human Diseasesmentioning

confidence: 96%

Desmosomes and Intermediate Filaments: Their Consequences for Tissue Mechanics

Hatzfeld

Keil

Magin

2017

Cold Spring Harb Perspect Biol

116

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Adherens junctions (AJs) and desmosomes connect the actin and keratin filament networks of adjacent cells into a mechanical unit. Whereas AJs function in mechanosensing and in transducing mechanical forces between the plasma membrane and the actomyosin cytoskeleton, desmosomes and intermediate filaments (IFs) provide mechanical stability required to maintain tissue architecture and integrity when the tissues are exposed to mechanical stress. Desmosomes are essential for stable intercellular cohesion, whereas keratins determine cell mechanics but are not involved in generating tension. Here, we summarize the current knowledge of the role of IFs and desmosomes in tissue mechanics and discuss whether the desmosome-keratin scaffold might be actively involved in mechanosensing and in the conversion of chemical signals into mechanical strength.

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“…Although no human pathologies are associated with mutations in PKP3, conditional ablation of PKP3 in mouse epidermis resulted in defective hair follicle morphogenesis, increased keratinocyte proliferation, and desmoplakin mislocalization. These mice are also more susceptible to dermatitis (skin inflammation) and secondary alopecia (hair loss) (Sklyarova et al 2008).…”

Section: Plakophilinsmentioning

confidence: 99%