Eman mohamed ahmed elnashar|Publications:Autophagy Promotes the Survival of Adipose Mesenchymal Stem/Stromal Cells and Enhances Their Therapeutic Effects in Cisplatin-Induced Liver Injury via Modulating TGF-β1/Smad and PI3K/AKT Signaling Pathways

You are in:Home/Publications/Autophagy Promotes the Survival of Adipose Mesenchymal Stem/Stromal Cells and Enhances Their Therapeutic Effects in Cisplatin-Induced Liver Injury via Modulating TGF-β1/Smad and PI3K/AKT Signaling Pathways
Prof. Eman mohamed ahmed elnashar :: Publications:

Title:	Autophagy Promotes the Survival of Adipose Mesenchymal Stem/Stromal Cells and Enhances Their Therapeutic Effects in Cisplatin-Induced Liver Injury via Modulating TGF-β1/Smad and PI3K/AKT Signaling Pathways
Authors:	Eman Mohamad El Nashar 1,2,, Mansour Abdallah Alghamdi 1,3, Wardah Abdullah Alasmari 4, Mohamed M. A. Hussein 5, Eman Hamza 6,7, Reham Ismail Taha 8, Mona M. Ahmed 9, Khulood Mohammed Al-Khater 10 and Ahmed Abdelfattah-Hassan 11,12,
Year:	2021
Keywords:	Keywords: ADSCs; cell-based therapy; rapamycin; apoptosis; liver damage; hepatoprotective pathways
Journal:	Cells
Volume:	10,
Issue:
Pages:	2475
Publisher:	MDPI
Local/International:	International
Paper Link:	https://doi.org/10.3390/cells10092475
Full paper	Eman mohamed ahmed elnashar_cells-10-02475.pdf
Supplementary materials	Not Available

Abstract:

Abstract: Autophagy is a key metabolic process where cells can recycle its proteins and organelles to regenerate its own cellular building blocks. Chemotherapy is indispensable for cancer treatment but associated with various side-effects, including organ damage. Stem cell-based therapy is a promising approach for reducing chemotherapeutic side effects, however, one of its main culprits is the poor survival of transplanted stem cells in damaged tissues. Here, we aimed to test the effects of activating autophagy in adipose-derived mesenchymal stem/stromal cells (ADSCs) on the survival of ADSCs, and their therapeutic value in cisplatin-induced liver injury model. Autophagy was activated in ADSCs by rapamycin (50 nM/L) for two hours before transplantation and were compared to non-preconditioned ADSCs. Rapamycin preconditioning resulted in activated autophagy and improved survival of ADSCs achieved by increased autophagosomes, upregulated autophagyspecific LC3-II gene, decreased protein degradation/ubiquitination by downregulated p62 gene, downregulated mTOR gene, and finally, upregulated antiapoptotic BCL-2 gene. In addition, autophagic ADSCs transplantation in the cisplatin liver injury model, liver biochemical parameters (AST, ALT and albumin), lipid peroxidation (MDA), antioxidant profile (SOD and GPX) and histopathological picture were improved, approaching near-normal conditions. These promising autophagic ADSCs effects were achieved by modulation of components in TGF-β1/Smad and PI3KAKT signaling pathways, besides reducing NF-κB gene expression (marker for inflammation), reducing TGF-β1 levels (marker for fibrosis) and increasing SDF-1 levels (liver regeneration marker) in liver. Therefore, current results highlight the importance of autophagy in augmenting the therapeutic potential of stem cell therapy in alleviating cisplatin-associated liver damage and opens the path for improved cell-based therapies, in general, and with chemotherapeutics, in particular. Keywords: ADSCs; cell-based therapy; rapamycin; apoptosis; liver damage; hepatoprotective pathways

Prof. Eman mohamed ahmed elnashar :: Publications: