Melanoma cells repress Desmoglein 1 in keratinocytes to promote tumor cell migration

Burks, Hope E.; Pokorny, Jenny L.; Koetsier, Jennifer L.; Roth-Carter, Quinn R.; Arnette, Christopher R.; Gerami, Pedram; Seykora, John T.; Johnson, Jodi L.; Ren, Ziyou; Green, Kathleen J.

doi:10.1083/jcb.202212031

Cited by 7 publications

References 49 publications

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Dangerous liaisons: Loss of keratinocyte control over melanocytes in melanomagenesis

Green,

Pokorny,

Jarrell

2024

BioEssays

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Melanomas arise from transformed melanocytes, positioned at the dermal‐epidermal junction in the basal layer of the epidermis. Melanocytes are completely surrounded by keratinocyte neighbors, with which they communicate through direct contact and paracrine signaling to maintain normal growth control and homeostasis. UV radiation from sunlight reshapes this communication network to drive a protective tanning response. However, repeated rounds of sun exposure result in accumulation of mutations in melanocytes that have been considered as primary drivers of melanoma initiation and progression. It is now clear that mutations in melanocytes are not sufficient to drive tumor formation—the tumor environment plays a critical role. This review focuses on changes in melanocyte‐keratinocyte communication that contribute to melanoma initiation and progression, with a particular focus on recent mechanistic insights that lay a foundation for developing new ways to intercept melanoma development.

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Dangerous liaisons: Loss of keratinocyte control over melanocytes in melanomagenesis

Green,

Pokorny,

Jarrell

2024

BioEssays

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Effect of Ritanserin and Duloxetine on the Gene Expression of Primary Aniridia and Healthy Human Limbal Stromal Cells, In Vitro

Li,

Szentmáry,

Fries

et al. 2024

Ophthalmol Ther

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Introduction In congenital aniridia caused by mutations in paired box 6 (PAX6), PAX6 influences the migration and differentiation of limbal epithelial cells (LECs), thereby playing a pivotal role in aniridia-associated keratopathy. The antidepressants ritanserin and duloxetine affect PAX6 expression in LECs. Limbal stromal cells, which support limbal epithelial stem cells, are crucial in the limbal stem cell niche. This study explores how ritanserin and duloxetine influence gene expression in primary human limbal stromal cells from subjects with congenital aniridia and from healthy subjects, in vitro. Methods Primary human limbal stromal cells from corneas affected by aniridia (AN-LSCs) ( n = 8) and from healthy corneas (LSCs) ( n = 8) were isolated and cultured in either low-glucose serum-free (LGSF) or normal-glucose serum-containing (NGSC) media. Cells were treated with 4 µM ritanserin or duloxetine for 24 h. Quantitative PCR (qPCR) and western blot were used to assess the expression of PAX6, FOSL2, TGF-β1, ACTA2A1, LUM, COL1A1, COL5A1, DSG1, FABP5 and ADH7. Results In AN-LSCs with LGSF-medium, ritanserin increased PAX6 messenger RNA (mRNA) ( p = 0.007) and decreased TGF-β1 and FOSL2 mRNA levels ( P = 0.005, P = 0.038). In addition, TGF-β1 protein levels decreased with both treatments ( P = 0.02, P = 0.007), and FABP5 protein level increased, using ritanserin ( P = 0.019). In LSCs with LGSF-medium, ACTA2A1 mRNA levels decreased using ritanserin and duloxetine ( P = 0.028; P = 0.031), while FABP5 mRNA levels increased with ritanserin treatment ( P = 0.003). Also, duloxetine use reduced α-SMA protein ( P = 0.013) and increased FABP5 protein levels ( P = 0.029). In LSCs with NGSC-medium, ritanserin elevated LUM, FABP5 and ADH7 mRNA and protein levels ( P = 0.025, P = 0.003, P = 0.047, P = 0.024, P = 0.013, P = 0.039). Conclusions The results of our study confirmed that the antipsychotropic drugs ritanserin and duloxetine alter PAX6 and TGF-β1 gene expression in AN-LSCs cultured in LGSF-medium. These drugs were found to have an impact on retinoic acid signaling pathways and keratocyte characteristic markers both in LSCs and AN-LSCs, using different culture media. Supplementary Information The on...

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Crosstalk in Skin: Loss of Desmoglein 1 in Keratinocytes Inhibits BRAFV600E-induced Cellular Senescence in Human Melanocytes

Tong,

Burks,

Ren

et al. 2024

Journal of Investigative Dermatology

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Melanoma cells repress Desmoglein 1 in keratinocytes to promote tumor cell migration

Cited by 7 publications

References 49 publications

Dangerous liaisons: Loss of keratinocyte control over melanocytes in melanomagenesis

Dangerous liaisons: Loss of keratinocyte control over melanocytes in melanomagenesis

Effect of Ritanserin and Duloxetine on the Gene Expression of Primary Aniridia and Healthy Human Limbal Stromal Cells, In Vitro

Crosstalk in Skin: Loss of Desmoglein 1 in Keratinocytes Inhibits BRAFV600E-induced Cellular Senescence in Human Melanocytes

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