Macrophage cell morphology‐imprinted substrates can modulate mesenchymal stem cell behaviors and macrophage M1/M2 polarization for wound healing applications

Author:

Majidi Mohammad1,Pakzad Saeedreza2,Salimi Maryam3,Azadbakht Abdolnaser45,Hajighasemlou Saieh6,Amoupour Moein7,Nokhbedehghan Zeinab7,Bonakdar Shahin8ORCID,Sineh Sepehr Koushan9,Pal Singh Chauhan Narendra10,Gholipourmalekabadi Mazaher711ORCID

Affiliation:

1. Department of Tissue Engineering & Regenerative Medicine, Faculty of Advanced Technologies in Medicine Iran University of Medical Sciences Tehran Iran

2. Food and Drug Laboratory Research Center, Food and Drug Administration Iran Ministry of Health and Medical Education Tehran Iran

3. Hematopoietic Stem Cell Research Center Shahid Beheshti University of Medical Sciences Tehran Iran

4. Department of Biomedical Engineering Central Tehran Branch, Islamic Azad University Tehran Iran

5. Stem Cell Research Center, Tissue Engineering and Regenerative Medicine Institute, Central Tehran Branch Islamic Azad University Tehran Iran

6. Food and Drug Administration Iran Ministry of Health and Medical Education Tehran Iran

7. Department of Medical Biotechnology, Faculty of Allied Medicine Iran University of Medical Sciences Tehran Iran

8. National Cell Bank Pasteur Institute of Iran Tehran Iran

9. Laboratory Sciences Research Center Golestan University of Medical Sciences Gorgan Iran

10. Department of Chemistry, Faculty of Science Bhupal Nobles' University Udaipur Rajasthan India

11. Cellular and Molecular Research Centre Iran University of Medical Sciences Tehran Iran

Abstract

AbstractMesenchymal stem cells and macrophages (MQ) are two very important cells involved in the normal wound healing process. It is well understood that topological cues and mechanical factors can lead to different responses in stem cells and MQ by influencing their shape, cytoskeleton proliferation, migration, and differentiation, which play an essential role in the success or failure of biomaterial implantation and more importantly wound healing. On the other hand, the polarization of MQ from proinflammatory (M1) to prohealing (M2) phenotypes has a critical role in the acceleration of wound healing. In this study, the morphology of different MQ subtypes (M0, M1, and M2) was imprinted on a silicon surface (polydimethylsiloxane [PDMS]) to prepare a nano‐topography cell‐imprinted substrate with the ability to induce anti‐inflammatory effects on the mouse adipose‐derived stem cells (ADSCs) and RAW264.7 monocyte cell line (MO). The gene expression profiles and flow cytometry of MQ revealed that the cell shape microstructure promoted the MQ phenotypes according to the specific shape of each pattern. The ELISA results were in agreement with the gene expression profiles. The ADSCs on the patterned PDMS exhibited remarkably different shapes from no‐patterned PDMS. The MOs grown on M2 morphological patterns showed a significant increase in expression and section of anti‐inflammatory cytokine compared with M0 and M1 patterns. The ADSCs homing in niches heavily deformed the cytoskeletal, which is probably why the gene expression and phenotype unexpectedly changed. In conclusion, wound dressings with M2 cell morphology‐induced surfaces are suggested as excellent anti‐inflammatory and antiscarring dressings.

Publisher

Wiley

Subject

Applied Microbiology and Biotechnology,Bioengineering,Biotechnology

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