Vol. 123, No. 1 (Supplement) 2018
Supplement abstract

Role of the microenvironment in the imbalance between Th1/Th17 and Th2 cytokines of Mesenchymal stem Cells derived from psoriatic skin

Monia Orciani
Università Politecnica delle Marche, Dipartimento di Scienze cliniche e moleoclari- Istologia, Ancona, Italia
Giulia Sorgentoni
Università Politecnica delle Marche, Dipartimento di Scienze cliniche e moleoclari- Istologia, Ancona, Italia
Elisa Molinelli
Università Politecnica delle Marche, Dipartimento di Scienze cliniche e moleoclari- Dermatologia, Ancona, Italia
Miriam Caffarini
Università Politecnica delle Marche, Dipartimento di Scienze cliniche e moleoclari- Istologia, Ancona, Italia
Anna Maria Offidani
Università Politecnica delle Marche, Dipartimento di Scienze cliniche e moleoclari- Dermatologia, Ancona, Italia
Roberto Di Primio
Università Politecnica delle Marche, Dipartimento di Scienze cliniche e moleoclari- Istologia, Ancona, Italia

Published 2018-12-30

Keywords

  • Mesenchymal stem cells (MSCs),
  • psoriasis,
  • inflammation

How to Cite

Orciani, M., Sorgentoni, G., Molinelli, E., Caffarini, M., Offidani, A. M., & Di Primio, R. (2018). Role of the microenvironment in the imbalance between Th1/Th17 and Th2 cytokines of Mesenchymal stem Cells derived from psoriatic skin. Italian Journal of Anatomy and Embryology, 123(1), 162. https://doi.org/10.13128/ijae-11476

Abstract

Psoriasis is an inflammatory and immuno-mediated disease [1] characterized by the over- expression of several Th1-Th17 cytokines, which are able to maintain a low-grade inflamma- tory status. The expression and secretion of Th1, Th2 and Th17 cytokines has been extensive- ly evaluated in differentiated skin cells of psoriatic patients, while little is known about their production by MSCs in psoriatic skin. Indeed, it is known that the psoriatic microenvironment influences the MSCs phenotypic profile [2]. This works aims to evaluate the immunobiology of psoriatic MSCs (PsO-MSCs) and the potential paracrine effect that can be exerted by Healthy MSCs (H-MSCs) on PsO-MSCs.

To assess these questions, MSCs were isolated from skin of psoriatic and healthy subjects. Subsequently, indirect co-culture of H-MSCs with PsO-MSCs was performed; effects on prolif- eration and expression of cytokines linked to Th1/Th17 and Th2 pathways were assayed before and after co-culture.

The results show that before co-culture, proliferation of PsO-MSCs was significantly higher than H-MSCs (p<0.05) and the levels of secreted cytokines confirmed the imbalance of Th1/17 versus Th2 axis.

After co-culture of H-MSCs with PsO-MSCs, healthy MSCs seem to exert a “positive” influ- ence on PsO-MSCs driving the inflammatory phenotypic profile of PsO-MSCs towards a physi- ological pattern. The proliferation rate decreased, towards values nearer to those observed in H-MSCs and the secretion of the cytokines that mostly identified the inflammatory microenvi- ronment that characterized psoriasis, such as IL6, IL12, IL13, IL17A, TNFα, and GCSF, is sig- nificantly lower in co-cultured PsO-MSCs than in individually cultured PSO-MSCs (p at least <0.05).

In conclusions, our preliminary results seem to provide an intriguing molecular explanation for the ever increasing evidence of therapeutic efficacy of allogeneic MSCs infusion in psoriatic patients.

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