Your search keyword '"Otaizo-Carrasquero, Francisco"' showing total 2 results

1. Therapeutic responses to Roseomonas mucosa in atopic dermatitis may involve lipid-mediated TNF-related epithelial repair.

Author

Myles, Ian A., Castillo, Carlo R., Barbian, Kent D., Kanakabandi, Kishore, Virtaneva, Kimmo, Fitzmeyer, Emily, Paneru, Monica, Otaizo-Carrasquero, Francisco, Myers, Timothy G., Markowitz, Tovah E., Moore, Ian N., Liu, Xue, Ferrer, Marc, Sakamachi, Yosuke, Garantziotis, Stavros, Swamydas, Muthulekha, Lionakis, Michail S., Anderson, Erik D., Earland, Noah J., and Ganesan, Sundar

Subjects

ATOPIC dermatitis, MUCOUS membranes, FILAGGRIN, LABORATORY mice, EPITHELIAL-mesenchymal transition, QUALITY of life, CELL culture

Abstract

A rosy outlook for Roseomonas: In a clinical trial, topical application of the healthy skin bacterium Roseomonas mucosa improved atopic dermatitis (AD) in children age 3 years or older. R. mucosa treatment was associated with improvements in disease symptoms, epithelial barrier function, the amount of Staphylococcus aureus growing on the skin, the need for topical steroids, and quality of life for children and their families. Clinical improvements and colonization of skin by R. mucosa persisted for up to 8 months after treatment cessation and were not associated with major adverse events. Cell culture analyses and studies in the MC903 mouse model of AD suggest that the therapeutic mechanism may involve lipid production by R. mucosa, cholinergic signaling, and flagellin expression leading to a TNFR2-mediated epithelial-to-mesenchymal transition. Dysbiosis of the skin microbiota is increasingly implicated as a contributor to the pathogenesis of atopic dermatitis (AD). We previously reported first-in-human safety and clinical activity results from topical application of the commensal skin bacterium Roseomonas mucosa for the treatment of AD in 10 adults and 5 children older than 9 years of age. Here, we examined the potential mechanism of action of R. mucosa treatment and its impact on children with AD less than 7 years of age, the most common age group for children with AD. In 15 children with AD, R. mucosa treatment was associated with amelioration of disease severity, improvement in epithelial barrier function, reduced Staphylococcus aureus burden on the skin, and a reduction in topical steroid requirements without severe adverse events. Our observed response rates to R. mucosa treatment were greater than those seen in historical placebo control groups in prior AD studies. Skin improvements and colonization by R. mucosa persisted for up to 8 months after cessation of treatment. Analyses of cellular scratch assays and the MC903 mouse model of AD suggested that production of sphingolipids by R. mucosa, cholinergic signaling, and flagellin expression may have contributed to therapeutic impact through induction of a TNFR2-mediated epithelial-to-mesenchymal transition. These results suggest that a randomized, placebo-controlled trial of R. mucosa treatment in individuals with AD is warranted and implicate commensals in the maintenance of the skin epithelial barrier. [ABSTRACT FROM AUTHOR]

Published

2020

2. Prolonging culture of primary human keratinocytes isolated from suction blisters with the Rho kinase inhibitor Y-27632.

Author

Anderson, Erik D., Sastalla, Inka, Earland, Noah J., Mahnaz, Minai, Moore, Ian N., Otaizo-Carrasquero, Francisco, Myers, Timothy G., Myles, Christopher A., Datta, Sandip K., and Myles, Ian A.

Subjects

KERATINOCYTES, EPIDERMIS, RHO factor, KINASE inhibitors, STAPHYLOCOCCUS aureus, CELL culture

Abstract

Keratinocytes are the most abundant cell type in the epidermis. They prevent desiccation and provide immunological and barrier defense against potential pathogens such as Staphylococcus aureus and Candida albicans. The study of this first line of immune defense may be hindered by invasive isolation methods and/or improper culture conditions to support stem cell maintenance and other potential mechanisms contributing to long-term subcultivation in vitro. Primary keratinocytes have been successfully isolated from blister roofs induced by negative pressure, which separates the epidermis from the dermis in vivo in human subjects. This method allows collection of pure epidermal cells without dermal contamination in a minimally invasive manner. However, the isolated keratinocytes differentiate and senesce when cultured in vitro beyond five passages. Here, we present evidence that the Rho kinase (ROCK) inhibitor Y-27632 can be used to effectively increase the proliferative capabilities of keratinocytes isolated using the suction blister method, similar to what has been previously reported for primary keratinocytes isolated using alternative methods. We show that the increase in passage number is directly correlated to delayed differentiation, and that cells passaged long term with the inhibitor retain their ability to stratify in organotypic raft cultures and respond to cytokine treatment; additionally, the late passage cells have a heterogeneous mix of differentiated and non-differentiated cells which may be predicted by a ratio of select differentiation markers. The described method presents a minimally invasive procedure for keratinocyte isolation and prolonged culture that allows analysis of keratinocyte function in both healthy volunteers and patients with dermatologic diseases. [ABSTRACT FROM AUTHOR]

Published

2018