4.7 Article

Research Techniques Made Simple: Analysis of Autophagy in the Skin

Journal

JOURNAL OF INVESTIGATIVE DERMATOLOGY
Volume 141, Issue 1, Pages 5-+

Publisher

ELSEVIER SCIENCE INC
DOI: 10.1016/j.jid.2020.10.004

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Funding

  1. University of Sunderland (Sunderland, United Kingdom)
  2. Psoriasis Association
  3. NC3Rs, Forsogsdyrenes Vaern & Alternativfondet
  4. Newcastle Hospitals Healthcare Charity (Newcastle upon Tyne, United Kingdom)
  5. Cancer Research United Kingdom (London, United Kingdom)
  6. Melanoma Focus
  7. German Research Foundation (Bonn, Germany)

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Autophagy plays a crucial role in maintaining normal skin function, with dysregulation potentially leading to various skin diseases. Utilizing well-characterized biomarkers of autophagy can assist in quantifying autophagic activity experimentally and correlating it with disease progression clinically.
Autophagy is required for normal skin homeostasis and its disordered regulation is implicated in a range of cutaneous diseases. Several well-characterized biomarkers of autophagy are used experimentally to quantify autophagic activity or clinically to correlate autophagy with disease progression. This article discusses the advantages and limitations of different approaches for measuring autophagy as well as the techniques for modulating autophagy. These include analysis of endogenous LC3, a central autophagy regulatory protein, and measurement of LC3 flux using a dual-fluorescent reporter, which provides a quantitative readout of autophagy in cell culture systems in vitro and animal models in vivo. Degradation of SQSTM1/p62 during autophagy is proposed as an alternative biomarker allowing the analysis of autophagy both experimentally and clinically. However, the complex regulation of individual autophagy proteins and their involvement in multiple pathways means that several proteins must be analyzed together, preferably over a time course to accurately interpret changes in autophagic activity. Genetic modification of autophagy proteins can be used to better understand basic autophagic mechanisms contributing to health and disease, whereas small molecule inhibitors of autophagy regulatory proteins, lysosomal inhibitors, or activators of cytotoxic autophagy have been explored as potential treatments for skin disorders where autophagy is defective.

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