An Example of Neuro-Glial Commitment and Differentiation of Muse Stem Cells Obtained from Patients with IQSEC2-Related Neural Disorder: A Possible New Cell-Based Disease Model

Author:

Al Sammarraie Sura Hilal Ahmed1ORCID,Aprile Domenico1ORCID,Meloni Ilaria2,Alessio Nicola1ORCID,Mari Francesca2ORCID,Manata Marianna2,Lo Rizzo Caterina2,Di Bernardo Giovanni13ORCID,Peluso Gianfranco4,Renieri Alessandra2ORCID,Galderisi Umberto135ORCID

Affiliation:

1. Department of Experimental Medicine, Luigi Vanvitelli Campania University, 80138 Naples, Italy

2. Department of Medical Biotechnology, University of Siena, 53100 Siena, Italy

3. Sbarro Institute for Cancer Research and Molecular Medicine, Center for Biotechnology, Temple University, Philadelphia, PA 19122, USA

4. UniCamillus, 00131 Rome, Italy

5. Genome and Stem Cell Center (GENKÖK), Erciyes University, 38280 Kayseri, Turkey

Abstract

Although adult stem cells may be useful for studying tissue-specific diseases, they cannot be used as a general model for investigating human illnesses given their limited differentiation potential. Multilineage-differentiating stress-enduring (Muse) stem cells, a SSEA3(+) cell population isolated from mesenchymal stromal cells, fat, and skin fibroblasts, may be able to overcome that restriction. The Muse cells present in fibroblast cultures obtained from biopsies of patients’ skin may be differentiated into cells of interest for analyzing diseases. We isolated Muse stem cells from patients with an intellectual disability (ID) and mutations in the IQSEC2 gene (i.e., BRAG1 gene) and induced in vitro neuroglial differentiation to study cell commitment and the differentiation of neural lineages. The neuroglial differentiation of Muse cells revealed that IQSEC2 mutations may alter the self-renewal and lineage specification of stem cells. We observed a decrease in the percentage of SOX2 (+) neural stem cells and neural progenitors (i.e., SOX2+ and NESTIN+) in cultures obtained from Muse cells with the mutated IQSEC2 gene. The alteration in the number of stem cells and progenitors produced a bias toward the astrocytes’ differentiation. Our research demonstrates that Muse stem cells may represent a new cell-based disease model.

Funder

Regione Campania Progetto POR

Publisher

MDPI AG

Subject

General Medicine

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