Research Output
Keratins regulate β‐cell mitochondrial morphology, motility, and homeostasis
  Loss of the epithelial intermediate filament protein keratin 8 (K8) in murine β cells leads to irregular insulin vesicles and decreased insulin levels. Because mitochondria are central in glucose-stimulated insulin secretion, the relationship between keratins and β-cell mitochondrial function and morphology was investigated. β cells in murine K8-knockout (K8−/−) islets of Langerhans have increased numbers of mitochondria, which are rounder and have diffuse cristae, as seen by electron microscopy. The mitochondrial network in primary cultured K8−/− β cells is more fragmented compared with K8+/+ mitochondria, correlating with decreased levels of mitofusin 2 and the mitofusin 2- and keratin-binding protein trichoplein. K8−/− β-cell mitochondria have decreased levels of total and mitochondrial cytochrome c, which correlates with a reduction in electron transport complexes I and IV. This provokes loss of mitochondrial membrane potential and reduction of ATP and insulin amount, as seen in K8−/− β cells. Mitochondria in K8 wild-type β cells and MIN6 insulinoma cells overexpressing K8 and 18 are more stationary compared with mitochondria in keratin-deficient cells. In conclusion, keratins, likely through trichoplein-mitofusin interactions, regulate both structural and dynamic functions of β-cell mitochondria, which could have implications for downstream insulin secretion.

  • Type:

    Article

  • Date:

    19 September 2017

  • Publication Status:

    Published

  • Publisher

    Wiley

  • DOI:

    10.1096/fj.201700095r

  • Cross Ref:

    10.1096/fj.201700095r

  • ISSN:

    0892-6638

  • Funders:

    Historic Funder (pre-Worktribe)

Citation

Silvander, J. S. G., Kvarnström, S. M., Kumari‐Ilieva, A., Shrestha, A., Alam, C. M., & Toivola, D. M. (2017). Keratins regulate β‐cell mitochondrial morphology, motility, and homeostasis. FASEB Journal, 31(10), 4578-4587. https://doi.org/10.1096/fj.201700095r

Authors

Keywords

TEM, insulin secretion, islets, K8-null mice, fusion

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