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Heat shock protein responses to aging and proteotoxicity in the olfactory bulb

Journal

JOURNAL OF NEUROCHEMISTRY
Volume 133, Issue 6, Pages 780-794

Publisher

WILEY
DOI: 10.1111/jnc.13041

Keywords

Glucose-regulated protein 78; heme oxygenase 1; heat shock protein 70; heat shock cognate 70; olfaction; proteostasis

Funding

  1. Hillman foundation
  2. C.U.R.E. Research Award from the Pennsylvania State Department of Health
  3. NIH [DK79307]
  4. NIGMS [GM067082]

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The olfactory bulb is one of the most vulnerable brain regions in age-related proteinopathies. Proteinopathic stress is mitigated by the heatshock protein (Hsp) family of chaperones. Here, we describe age-related decreases in Hsc70 in the olfactory bulb of the female rat and higher levels of Hsp70 and Hsp25 in middle and old age than at 2-4months. To model proteotoxic and oxidative stress in the olfactory bulb, primary olfactory bulb cultures were treated with the proteasome inhibitors lactacystin and MG132 or the pro-oxidant paraquat. Toxin-induced increases were observed in Hsp70, Hsp25, and Hsp32. To determine the functional consequences of the increase in Hsp70, we attenuated Hsp70 activity with two mechanistically distinct inhibitors. The Hsp70 inhibitors greatly potentiated the toxicity of sublethal lactacystin or MG132 but not of paraquat. Although ubiquitinated protein levels were unchanged with aging in vivo or with sublethal MG132 in vitro, there was a large, synergistic increase in ubiquitinated proteins when proteasome and Hsp70 functions were simultaneously inhibited. Our study suggests that olfactory bulb cells rely heavily on Hsp70 chaperones to maintain homeostasis during mild proteotoxic, but not oxidative insults, and that Hsp70 prevents the accrual of ubiquitinated proteins in these cells.

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