Inducible HSP70 Is Critical in Preventing the Aggregation and Enhancing the Processing of PMP22

In this study, we show that activation of the chaperone pathway in fibroblasts from PMP22 duplication-associated Charcot–Marie–Tooth disease type 1A patient with an FDA-approved small molecule increases HSP70 expression and attenuates proteasome dysfunction. Using cells from an HSP70.1/3–/– (inducible HSP70) mouse model, we demonstrate that under proteotoxic stress, this chaperone is critical in preventing the aggregation of PMP22, and this effect is aided by macroautophagy. When examined at steady-state, HSP70 appears to play a minor role in the trafficking of wild-type-PMP22, while it is crucial for preventing the buildup of the aggregation-prone Trembler-J-PMP22. HSP70 aids the processing of Trembler-J-PMP22 through the Golgi and its delivery to lysosomes via Rab7-positive vesicles. Together, these results demonstrate a key role for inducible HSP70 in aiding the processing and hindering the accumulation of misfolded PMP22, which in turn alleviates proteotoxicity within the cells.

http://asn.sagepub.com/cgi/content/abstract/7/1/1759091415569909?rss=1

Source: ASN Neuro - February 18, 2015 Category: Neuroscience Authors: Chittoor-Vinod, V. G., Lee, S., Judge, S. M., Notterpek, L. Tags: Original Article Source Type: research