| کد مقاله | کد نشریه | سال انتشار | مقاله انگلیسی | نسخه تمام متن |
|---|---|---|---|---|
| 1919157 | 1535600 | 2016 | 12 صفحه PDF | دانلود رایگان |
• Hsp22 over-expression influences mitochondrial protein expression during lifespan.
• Mitochondrial Hsp70 is one of the most affected proteins by Hsp22 expression.
• Hsp22 over-expressing flies have a better mitochondrial proteostasis.
• Cathepsin D is found both in lysosomes and mitochondria in D. melanogaster.
Hsp22 is a small mitochondrial heat shock protein (sHSP) preferentially up-regulated during aging in Drosophila melanogaster. Its developmental expression is strictly regulated and it is rapidly induced in conditions of stress. Hsp22 is one of the few sHSP to be localized inside mitochondria, and is the first sHSP to be involved in the mitochondrial unfolding protein response (UPRMT) together with Hsp60, mitochondrial Hsp70 and TRAP1. The UPRMT is a pro-longevity mechanism, and interestingly Hsp22 over-expression by-itself increases lifespan and resistance to stress. To unveil the effect of Hsp22 on the mitochondrial proteome, comparative IEF/SDS polyacrylamide 2D gels were done on mitochondria from Hsp22+ flies and controls. Among the proteins influenced by Hsp22 expression were proteins from the electron transport chain (ETC), the TCA cycle and mitochondrial Hsp70. Hsp22 co-migrates with ETC components and its over-expression is associated with an increase in mitochondrial protease activity. Interestingly, the only protease that showed significant changes upon Hsp22 over-expression in the comparative IEF/SDS-PAGE analysis was cathepsin D, which is localized in mitochondria in addition to lysosome in D. melanogaster as evidenced by cellular fractionation. Together the results are consistent with a role of Hsp22 in the UPRMT and in mitochondrial proteostasis.
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Journal: Mechanisms of Ageing and Development - Volume 155, April 2016, Pages 36–47