Requirement of zinc transporter ZIP10 for epidermal development: Implication of the ZIP10–p63 axis in epithelial homeostasis

Bin, Bum-Ho; Bhin, Jinhyuk; Takaishi, Mikiro; Toyoshima, Koh-éi; Kawamata, Saeko; Ito, Kana; Hara, Takafumi; Watanabe, Takashi; Irié, Tarou; Takagishi, Teruhisa; Lee, Su-Hyon; Jung, Haeng-Sun; Rho, Sangchul; Seo, Juyeon; Choi, Dongkyu; Hwang, Dae Hee; Koseki, Haruhiko; Ohara, Osamu; Sano, Shigetoshi; Tsuji, Takashi; Mishima, Kenji; Fukada, Toshiyuki

doi:10.1073/pnas.1710726114

Cited by 44 publications

(41 citation statements)

References 55 publications

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“…Treatment of human epidermal keratinocytes with scrambled control or siRNA targeting SLC39A6 (encoding ZIP6), which is similar to SLC39A10 in its structure and function, did not affect epidermal differentiation in the reconstituted human skin model (Fig. a), similar to results observed for Zip6 knockout mice . However, KD of ZIP10 by SLC39A10 siRNA treatment in keratinocytes severely disturbed epidermal formation (Fig.…”

Section: Resultssupporting

confidence: 74%

“…As HATs normally function as coactivators for TFs, we wondered whether the TFs that are affected by ZIP10 may be functionally and physically associated with HATs. Previously, a set of TFs related to the upregulation of genes in a ZIP10‐dependent manner was analysed . To examine whether these TFs were more associated with HATs than ZIP10‐independent TFs (Table S1; see Supporting Information), we calculated the ratio of the ZIP10‐dependent or ‐independent TFs interacting with HATs.…”

Section: Resultsmentioning

confidence: 99%

“…It is well established that zinc is important for genomic stability, and zinc deficiency causes epigenetic alterations . ZIP10 is a crucial zinc transporter for epidermal development and also remains a major epidermal ZIP transporter in adult skin, based on analyses of conditional knockout mice . Therefore, it is reasonable to hypothesize that an alteration of ZIP10‐mediated cytosolic zinc homeostasis could disturb the expression of genes involved in epidermal differentiation of adult skin by changing the activity of epigenetic enzymes.…”

Section: Discussionmentioning

confidence: 99%

“…Recent advances have shown that several ZIP proteins, particularly ZIP4, ZIP7, ZIP10 and ZIP13, play an important role in murine and human skin . Among them, ZIP10 is a crucial zinc transporter in murine epidermal development that supplies zinc to support the increased activity of elevated p63 levels starting at embryonic day 14, when epidermal progenitor cells proliferate vigorously to form stratified mature epidermis . Therefore, the regulated expression of p63 and ZIP10 has been suggested to be essential during epidermal morphogenesis, highlighting the importance of zinc uptake during embryonic development of the skin epidermis.…”

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confidence: 99%

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The epithelial zinc transporter ZIP 10 epigenetically regulates human epidermal homeostasis by modulating histone acetyltransferase activity

et al. 2018

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Background The skin is the first organ that manifests changes in response to zinc deficiency. However, the molecular mechanism underlying how zinc is involved in skin homeostasis, especially its epigenetic regulation, is largely unknown. Objectives In this study we demonstrate the importance of zinc levels and the zinc transporter ZIP10 in the epigenetic maintenance of human epidermal homeostasis. Methods Adult human skin, including skin appendages, were stained with anti-ZIP10 antibody. Histone acetyltransferase (HAT) activity was assessed after treating human keratinocytes with ZIP10 small interfering (si)RNAs or the zinc chelator TPEN. ZIP10-or HAT-regulated genes were analysed based on limma bioinformatics analysis for keratinocytes treated with ZIP10 siRNAs or a HAT inhibitor, or using a public database for transcription factors. A reconstituted human skin model was used to validate the role of ZIP10 in epidermal differentiation and the functional association between ZIP10 and HAT. Results ZIP10 is predominantly expressed in the interfollicular epidermis, epidermal appendages and hair follicles. ZIP10 depletion resulted in epidermal malformations in a reconstituted human skin model via downregulation of the activity of the epigenetic enzyme HAT. This decreased HAT activity, resulting from either ZIP10 depletion or treatment with the zinc chelator TPEN, was readily restored by zinc supplementation. Through bioinformatics analysis for gene sets regulated by knockdown of SLC39A10 (encoding ZIP10) and HAT inhibition, we demonstrated that ZIP10 and HATs were closely linked with the regulation of genes related to epidermal homeostasis, particularly filaggrin and metallothionein. Conclusions Our study suggests that ZIP10-mediated zinc distribution is crucial for epidermal homeostasis via HATs. Therefore, zinc-dependent epigenetic regulation could provide alternatives to maintaining healthy skin or alleviating disorders with skin barrier defects.

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Section: Resultssupporting

confidence: 74%

Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

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The epithelial zinc transporter ZIP 10 epigenetically regulates human epidermal homeostasis by modulating histone acetyltransferase activity

et al. 2018

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“…Among them, ΔNp63α 1 is the main isoform in proliferating keratinocytes 2 and thought to be obligatory for proper development of epithelial structures. 6 Although much is known about the genes regulated by p63 in keratinocytes and the epidermis, [9][10][11] how p63 is regulated is less clear. 2,5 Furthermore, ΔNp63 prevents Notch signaling, which inhibits p21 expression, thereby retarding epidermal differentiation.…”

Section: Introductionmentioning

confidence: 99%

FIH‐1 engages novel binding partners to positively influence epithelial proliferation via p63

et al. 2019

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Whereas much is known about the genes regulated by ΔNp63α in keratinocytes, how ΔNp63α is regulated is less clear. During studies with the hydroxylase, factor inhibiting hypoxia‐inducible factor 1 (FIH‐1), we observed increases in epidermal ΔNp63α expression along with proliferative capacity in a conditional FIH‐1 transgenic mouse. Conversely, loss of FIH‐1 in vivo and in vitro attenuated ΔNp63α expression. To elucidate the FIH‐1/p63 relationship, BioID proteomics assays identified FIH‐1 binding partners that had the potential to regulate p63 expression. FIH‐1 interacts with two previously unknown partners, Plectin1 and signal transducer and activator of transcription 1 (STAT1) leading to the regulation of ΔNp63α expression. Two known interactors of FIH‐1, apoptosis‐stimulating of P53 protein 2 (ASPP2) and histone deacetylase 1 (HDAC1), were also identified. Knockdown of ASPP2 upregulated ΔNp63α and reversed the decrease in ΔNp63α by FIH‐1 depletion. Additionally, FIH‐1 regulates growth arrest and DNA damage‐45 alpha (GADD45α), a negative regulator of ΔNp63α by interacting with HDAC1. GADD45α knockdown rescued reduction in ΔNp63α by FIH‐1 depletion. Collectively, our data reveal that FIH‐1 positively regulates ΔNp63α in keratinocytes via variety of signaling partners: (a) Plectin1/STAT1, (b) ASPP2, and (c) HDAC1/GADD45α signaling pathways.

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ZIP transporters‐regulated Zn²⁺ homeostasis: A novel determinant of human diseases

Liu,

Li,

2024

Journal Cellular Physiology

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As an essential trace element for organisms, zinc participates in various physiological processes, such as RNA transcription, DNA replication, cell proliferation, and cell differentiation. The destruction of zinc homeostasis is associated with various diseases. Zinc homeostasis is controlled by the cooperative action of zinc transporter proteins that are responsible for the influx and efflux of zinc. Zinc transporter proteins are mainly categorized into two families: Zrt/Irt‐like protein (SLC39A/ZIP) family and zinc transporter (SLC30A/ZNT) family. ZIP transporters contain 14 members, namely ZIP1‐14, which can be further divided into four subfamilies. Currently, ZIP transporters‐regulated zinc homeostasis is one of the research hotspots. Cumulative evidence suggests that ZIP transporters‐regulated zinc homeostasis may cause physiological dysfunction and contribute to the onset and progression of diverse diseases, such as cancers, neurological diseases, and cardiovascular diseases. In this review, we initially discuss the structure and distribution of ZIP transporters. Furthermore, we comprehensively review the latest research progress of ZIP transporters‐regulated zinc homeostasis in diseases, providing a new perspective into new therapeutic targets for treating related diseases.

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Requirement of zinc transporter ZIP10 for epidermal development: Implication of the ZIP10–p63 axis in epithelial homeostasis

Cited by 44 publications

References 55 publications

The epithelial zinc transporter ZIP 10 epigenetically regulates human epidermal homeostasis by modulating histone acetyltransferase activity

The epithelial zinc transporter ZIP 10 epigenetically regulates human epidermal homeostasis by modulating histone acetyltransferase activity

FIH‐1 engages novel binding partners to positively influence epithelial proliferation via p63

ZIP transporters‐regulated Zn²⁺ homeostasis: A novel determinant of human diseases

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Requirement of zinc transporter ZIP10 for epidermal development: Implication of the ZIP10–p63 axis in epithelial homeostasis

Cited by 44 publications

References 55 publications

The epithelial zinc transporter ZIP 10 epigenetically regulates human epidermal homeostasis by modulating histone acetyltransferase activity

The epithelial zinc transporter ZIP 10 epigenetically regulates human epidermal homeostasis by modulating histone acetyltransferase activity

FIH‐1 engages novel binding partners to positively influence epithelial proliferation via p63

ZIP transporters‐regulated Zn2+ homeostasis: A novel determinant of human diseases

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ZIP transporters‐regulated Zn²⁺ homeostasis: A novel determinant of human diseases