Journal
INTERNATIONAL JOURNAL OF MOLECULAR SCIENCES
Volume 23, Issue 7, Pages -Publisher
MDPI
DOI: 10.3390/ijms23073892
Keywords
retina; calpain; cell death; biomarker
Funding
- European Union (transMed) [H2020-MSCA-765441]
- Charlotte and Tistou Kerstan Foundation
- German Research Council (DFG) [PA1751/10-1]
- University of Tuebingen
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In this study, the researchers successfully detected the activity of calpain in the retina using a specific substrate. They found that calpain-2 activity may occur in the late stage of photoreceptor cell death, and the substrate used was not toxic to photoreceptor cells. These findings support the development of calpain activity detection as a novel in vivo biomarker for RD, which can be combined with non-invasive imaging techniques.
Calpains are a family of calcium-activated proteases involved in numerous disorders. Notably, previous studies have shown that calpain activity was substantially increased in various models for inherited retinal degeneration (RD). In the present study, we tested the capacity of the calpain-specific substrate t-BOC-Leu-Met-CMAC to detect calpain activity in living retina, in organotypic retinal explant cultures derived from wild-type mice, as well as from rd1 and Rho(P23H/+) RD-mutant mice. Test conditions were refined until the calpain substrate readily detected large numbers of cells in the photoreceptor layer of RD retina but not in wild-type retina. At the same time, the calpain substrate was not obviously toxic to photoreceptor cells. Comparison of calpain activity with immunostaining for activated calpain-2 furthermore suggested that individual calpain isoforms may be active in distinct temporal stages of photoreceptor cell death. Notably, calpain-2 activity may be a relatively short-lived event, occurring only towards the end of the cell-death process. Finally, our results support the development of calpain activity detection as a novel in vivo biomarker for RD suitable for combination with non-invasive imaging techniques.
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