Suprabasin-null mice retain skin barrier function and show high contact hypersensitivity to nickel upon oral nickel loading

Nakazawa, Shinsuke; Shimauchi, Takatoshi; Funakoshi, Akihiro; Aoshima, Masahiro; Phadungsaksawasdi, Pawit; Sakabe, Jun‐ichi; Asakawa, Shuichi; Hirasawa, Noriyasu; Ito, Taisuke; Tokura, Y.

doi:10.1038/s41598-020-71536-3

Cited by 11 publications

(9 citation statements)

References 42 publications

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“…The role of SBSN in immune regulation is strengthened with recent observation in Sbsn -null mice [ 36 ]. This animal model showed no aberration in skin development.…”

Section: Discussionmentioning

confidence: 83%

“…This animal model showed no aberration in skin development. However, following the low-dose nickel challenge, the mice did not develop T regulatory cells (Tregs) in the spleen, suggesting that SBSN is crucial in Treg development induced with these stimuli [ 36 ]. Other possibilities, such as induction of Treg development in general or induction of anergy in the tumour microenvironment specifically need to be evaluated in future studies.…”

Section: Discussionmentioning

confidence: 99%

“…As already mentioned, the physiological function of SBSN is currently unknown. Sbsn knockout mice do not manifest any abnormal skin phenotype [ 36 ], but shRNA-mediated SBSN knockdown abrogated the development of stratum granulosum , disrupted the formation of keratohyalin granules, and affected the morphology of some keratinocytes in the human living skin equivalent model [ 37 ]. The secretory nature of SBSN isoforms is supported by a number of reports [ 2 , 7 , 32 , 38 , 39 , 40 ], and the SBSN treatment promoted phenotypic changes in vitro [ 12 ], indicating the existence of SBSN receptor(s).…”

Section: The Function Of Sbsn In Context Of Physiology and Patholomentioning

confidence: 99%

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Suprabasin—A Review

Přibyl

Hodný

Kubíková

2021

Genes

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Among the ~22,000 human genes, very few remain that have unknown functions. One such example is suprabasin (SBSN). Originally described as a component of the cornified envelope, the function of stratified epithelia-expressed SBSN is unknown. Both the lack of knowledge about the gene role under physiological conditions and the emerging link of SBSN to various human diseases, including cancer, attract research interest. The association of SBSN expression with poor prognosis of patients suffering from oesophageal carcinoma, glioblastoma multiforme, and myelodysplastic syndromes suggests that SBSN may play a role in human tumourigenesis. Three SBSN isoforms code for the secreted proteins with putative function as signalling molecules, yet with poorly described effects. In this first review about SBSN, we summarised the current knowledge accumulated since its original description, and we discuss the potential mechanisms and roles of SBSN in both physiology and pathology.

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“…The role of SBSN in immune regulation is strengthened with recent observation in Sbsn -null mice [ 36 ]. This animal model showed no aberration in skin development.…”

Section: Discussionmentioning

confidence: 83%

Section: Discussionmentioning

confidence: 99%

Section: The Function Of Sbsn In Context Of Physiology and Patholomentioning

confidence: 99%

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Suprabasin—A Review

Přibyl

Hodný

Kubíková

2021

Genes

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“…And the SBSN −/− mice exhibit intact skin barrier function, but abnormal upper digestive tract epithelium that presents increased Ni absorption and high allergy to Ni, which is similar in intrinsic AD. 50 The implication of Sbsn's deficiency in human intrinsic AD warrants further investigation.…”

Section: Allergensmentioning

confidence: 99%

Intrinsic Atopic Dermatitis and Extrinsic Atopic Dermatitis: Similarities and Differences

Liu¹,

Song²,

Song³

2022

CCID

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In atopic dermatitis (AD), recent research advances have portrayed a complex disease profile based on different subtypes/ phenotypes and underlying molecular mechanisms/endotypes. Extrinsic and intrinsic subdivision is one of the most common types, defined in terms of total serum immune globulin E (IgE) and/or specific IgE to food and environmental allergens. Extrinsic AD is the most common type (80%), with high IgE, impaired skin barrier, as well as high incidence of comorbid atopic diseases, whereas intrinsic AD accounted for 20% of AD, with normal IgE and intact barrier function. Clinical studies have shown that extrinsic AD was a classic Th2-based inflammatory dermatitis, while the intrinsic subtype presented increased Th1/Th17/Th22 but normal Th2 cytokines. Protein sensitization, a classic Th2 response, has been clearly characterized in extrinsic AD, while metal hapten induces intrinsic AD's sensitization, which may be associated with suprabasin deficiency. In this review, we aimed to further expand our knowledge about similarities and differences between these two subtypes, which will expand our capability to further dissect pathophysiology of AD and enable us to develop personalized medicine approaches.

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“…In an RHE model, deficiency in suprabasin caused immature keratohyalin granules but did not affect the other markers of epidermal differentiation. Suprabasin-null mice showed skin barrier dysfunction as embryos but not after birth, and ultrastructural abnormalities in the stratum corneum and immature keratohyalin granules were observed ( Nakazawa et al, 2020 ). Furthermore, the amount of suprabasin was significantly decreased in atopic dermatitis patients ( Sakabe et al, 2014 ; Li et al, 2018 ).…”

Section: Fg Repeats For a Skin Barrier Formationmentioning

confidence: 99%

New Family Members of FG Repeat Proteins and Their Unexplored Roles During Phase Separation

Shinkai

Kawamura

Miyafusa

2021

Front. Cell Dev. Biol.

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The condensation and compartmentalization of biomacromolecules in the cell are driven by the process of phase separation. The main effectors of phase separation are intrinsically disordered proteins, which include proteins with a phenylalanine-glycine (FG) repeat domain. Our understanding of the biological function of FG repeat proteins during phase separation has been mainly derived from recent research on a member of the nuclear pore complex proteins, nucleoporins containing FG repeat domain (FG-NUPs). FG-NUPs form meshwork structures by inter- and intra-molecular FG domain interactions, which confine the nucleo-cytoplasmic exchange. Whereas FG-NUPs localize in the nuclear membrane, other FG repeat proteins reside in the cytoplasm and the nucleoplasm, and the biological function of the FG repeat domain of these proteins is not well described. In the present review, we list the FG repeat proteins that are known to phase separate in the cell, and review their biological functions. We extract the unraveled features of FG repeat proteins as an activator of barrier formation and homotypic cell-cell interactions. Understanding the regulatory mechanisms of FG repeat proteins will provide a potential delivery tool for therapeutic reagents.

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Suprabasin-null mice retain skin barrier function and show high contact hypersensitivity to nickel upon oral nickel loading

Cited by 11 publications

References 42 publications

Suprabasin—A Review

Suprabasin—A Review

Intrinsic Atopic Dermatitis and Extrinsic Atopic Dermatitis: Similarities and Differences

New Family Members of FG Repeat Proteins and Their Unexplored Roles During Phase Separation

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