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      Proteasomes in corneal epithelial cells and cultured autologous oral mucosal epithelial cell sheet (CAOMECS) graft used for the ocular surface regeneration

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          Abstract

          Purpose:

          This study focuses on characterizing proteasomes in corneal epithelial cells (CEC) and in cultured autologous oral mucosal epithelial cell sheets (CAOMECS) used to regenerate the ocular surface.

          Methods:

          Limbal stem cell deficiency (LSCD) was surgically induced in rabbit corneas. CAOMECS was engineered and grafted onto corneas with LSCD to regenerate the ocular surface.

          Results:

          LSCD caused an increase in inflammatory cells in the ocular surface, an increase in the formation of immunoproteasomes (IPR), and a decrease in the formation of constitutive proteasome (CPR). Specifically, LSCD-diseased CEC (D-CEC) showed a decrease in the CPR chymotrypsin-like, trypsin-like and caspase-like activities, while healthy CEC (H-CEC) and CAOMECS showed higher activities. Quantitative analysis of IPR inducible subunit (B5i, B2i, and B1i) were performed and compared to CPR subunit (B5, B2, and B1) levels. Results showed that ratios B5i/B5, B2i/B2 and B1i/B1 were higher in D-CEC, indicating that D-CEC had approximately a two-fold increase in the amount of IPR compared to CAOMECS and HCEC. Histological analysis demonstrated that CAOMECS-grafted corneas had a re-epithelialized surface, positive staining for CPR subunits, and weak staining for IPR subunits. In addition, digital quantitative measurement of fluorescent intensity showed that the CPR B5 subunit was significantly more expressed in CAOMECS-grafted corneas compared to non-grafted corneas with LSCD.

          Conclusion:

          CAOMECS grafting successfully replaced the D-CEC with oral mucosal epithelial cells with higher levels of CPR. The increase in constitutive proteasome expression is possibly responsible for the recovery and improvement in CAOMECS-grafted corneas.

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          Author and article information

          Journal
          101156063
          32850
          Ocul Surf
          Ocul Surf
          The ocular surface
          1542-0124
          1937-5913
          11 January 2019
          18 May 2017
          October 2017
          31 January 2019
          : 15
          : 4
          : 749-758
          Affiliations
          Los Angeles Biomedical Research Institute (LA BioMed) at Harbor-UCLA Medical Center, Torrance, CA 90502, USA
          Author notes
          [1]

          Dr. Yutaka Niihara is the CEO and President of Emmaus Life Science Inc., the sponsor of this research. The other authors have no commercial or proprietary interest in any concept or product described in this article.

          [* ]Corresponding author. Department of Medicine, LA BioMed at Harbor UCLA Medical Center, 1124 W. Carson Street, Torrance, CA 90502, USA, fgorce@ 123456labiomed.org (F. Bardag-Gorce).
          Article
          PMC6354778 PMC6354778 6354778 nihpa1005815
          10.1016/j.jtos.2017.05.010
          6354778
          28528957
          123b9e1a-eadf-41ac-8ff4-3b0662d028b6
          History
          Categories
          Article

          Corneal epithelial cells (CEC),Cultured autologous oral mucosal epithelial,cell sheets (CAOMECS),Limbal stem cell deficiency,Proteasome

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