In vitro preconditioning of equine adipose mesenchymal stem cells with prostaglandin E2, substance P and their combination changes the cellular protein secretomics and improves their immunomodulatory competence without compromising stemness

J Cabezas; D Rojas; Y Wong; F Telleria; J Manriquez; A C F Mançanares; L L Rodriguez-Alvarez; F O Castro

doi:10.1016/j.vetimm.2020.110100

In vitro preconditioning of equine adipose mesenchymal stem cells with prostaglandin E₂, substance P and their combination changes the cellular protein secretomics and improves their immunomodulatory competence without compromising stemness

Vet Immunol Immunopathol. 2020 Oct:228:110100. doi: 10.1016/j.vetimm.2020.110100. Epub 2020 Aug 20.

Authors

J Cabezas¹, D Rojas², Y Wong³, F Telleria⁴, J Manriquez⁵, A C F Mançanares⁶, L L Rodriguez-Alvarez⁷, F O Castro⁸

Affiliations

¹ Universidad de Concepción, Campus Chillan, Faculty of Veterinary Science, Department of Animal Science, Laboratorio de Biotecnología Animal, Chile. Electronic address: joecabezas@udec.cl.
² Universidad de Concepción, Campus Chillan, Faculty of Veterinary Sciences, Department of Animal Pathology, Chile. Electronic address: drojasm@udec.cl.
³ Universidad de Concepción, Campus Chillan, Faculty of Veterinary Science, Department of Animal Science, Laboratorio de Biotecnología Animal, Chile. Electronic address: ywong@udec.cl.
⁴ Universidad de Concepción, Campus Chillan, Faculty of Veterinary Science, Department of Animal Science, Laboratorio de Biotecnología Animal, Chile. Electronic address: francisca.telleria@alu.ucm.cl.
⁵ Universidad de Concepción, Campus Chillan, Faculty of Veterinary Science, Department of Animal Science, Laboratorio de Biotecnología Animal, Chile. Electronic address: jmanriquez@udec.cl.
⁶ Universidad de Concepción, Campus Chillan, Faculty of Veterinary Science, Department of Animal Science, Laboratorio de Biotecnología Animal, Chile. Electronic address: afurlanetto@udec.cl.
⁷ Universidad de Concepción, Campus Chillan, Faculty of Veterinary Science, Department of Animal Science, Laboratorio de Biotecnología Animal, Chile. Electronic address: llrodriguez@udec.cl.
⁸ Universidad de Concepción, Campus Chillan, Faculty of Veterinary Science, Department of Animal Science, Laboratorio de Biotecnología Animal, Chile. Electronic address: fidcastro@udec.cl.

PMID: 32871408
DOI: 10.1016/j.vetimm.2020.110100

Abstract

Mesenchymal stem cells (MSC) are modern tools in regenerative therapies of humans and animals owed to their immunomodulatory properties, which are activated in a pro-inflammatory environment. Different preconditioning strategies had been devised to enhance the immunomodulatory properties of MSC. In this research, we evaluated the immunological attributes of equine adipose MSC (eAMSC) before and after preconditioning in vitro with prostaglandin E₂ (PGE₂), substance P (SP), their combination and IFNγ. PGE₂/SP was the best combination to keep or enhance the mesodermal lineage differentiation of eAMSC. Alongside with this, preconditioning of eMSC with PGE₂ and SP did not affect expression of stemness MSC surface phenotype: CD90⁺, CD44⁺, MHC class I⁺, MHC class II^- and CD45^-, assessed by cytometry. Both naïve and preconditioned eAMSC expressed genes related with immune properties, such as MHC-I, PTGES, IL6, IL1A, TNFα and IL8 assessed by qPCR. Only TNFα was under expressed in treated cells, while the other markers were either overexpressed or not changed. In no cases MHC-II expression was detected. The antiproliferative effect of preconditioned eAMSC exposed to activated peripheral blood mononuclear cells (PBMC) showed that SP treatment significantly inhibited proliferation of LPS stimulated PBMC. When eAMSC were stimulated with Poly I:C, all the treatments significantly inhibited proliferation of stimulated PBMC (p < 0.05). Direct contact (coculture) between the preconditioned eAMSC and PBMC, induced a shift of significantly more (CD4/CD25/FOXP3)⁺ T-regulatory PBMC than naïve eAMSC. In the experiments of this research, we investigated the secreted proteomic profile of naïve and preconditioned eAMSC, 42 up-regulated and 40 down-regulated proteins were found in the proteomic assay. Our proteomic data revealed profound changes in the secretory pattern of MSC exposed to different treatments, compared to naïve eAMSC as well as among treatments. In overall, compared to naïve cells, the protein profile of preconditioned cells resembled the mesenchymal-epithelial transition (MET). Here we showed that the combined use of PGE₂ and SP provoked in overall the highest expression of anti-inflammatory markers as well as lead to an increased acquisition of a T-regulatory phenotype in preconditioned eAMSC without affecting their "stemness".

Keywords: Equine; Immunomodulation; Mesenchymal stem cells; Neurokinin 1; PGE(2); Preconditioning; Secretome.

MeSH terms

Animals
Biomarkers / metabolism
Cell Differentiation / immunology
Cell Proliferation
Dinoprostone / immunology*
Flow Cytometry / veterinary
Horses / immunology*
Interferon-gamma / immunology
Male
Mesenchymal Stem Cells / immunology*
Mesenchymal Stem Cells / metabolism
Mesoderm / cytology
Proteins / metabolism*
Proteome
Secretory Pathway / immunology
Substance P / immunology*

Substances

Biomarkers
Proteins
Proteome
Substance P
Interferon-gamma
Dinoprostone