Complete suppression of Htt fibrilization and disaggregation of Htt fibrils by a trimeric chaperone complex |
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| Authors: | Annika Scior Alexander Buntru Kristin Arnsburg Anne Ast Manuel Iburg Katrin Juenemann Maria Lucia Pigazzini Barbara Mlody Dmytro Puchkov Josef Priller Erich E Wanker Alessandro Prigione Janine Kirstein |
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| Affiliation: | 1. Leibniz‐Institute for Molecular Pharmacology (FMP) im Forschungsverbund Berlin, Berlin, Germany;2. Max Delbrueck Center for Molecular Medicine, Berlin, Germany;3. Charité – Universit?tsmedizin and NeuroCure Cluster of Excellence, Berlin, Germany;4. Department of Neuropsychiatry and Laboratory of Molecular Psychiatry, Charite Universit?tsmedizin Berlin, Berlin, Germany |
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| Abstract: | ![]()
Huntington's disease (HD) is a neurodegenerative disorder caused by an expanded CAG trinucleotide repeat in the huntingtin gene (HTT). Molecular chaperones have been implicated in suppressing or delaying the aggregation of mutant Htt. Using in vitro and in vivo assays, we have identified a trimeric chaperone complex (Hsc70, Hsp110, and J‐protein) that completely suppresses fibrilization of HttExon1Q48. The composition of this chaperone complex is variable as recruitment of different chaperone family members forms distinct functional complexes. The trimeric chaperone complex is also able to resolubilize Htt fibrils. We confirmed the biological significance of these findings in HD patient‐derived neural cells and on an organismal level in Caenorhabditis elegans. Among the proteins in this chaperone complex, the J‐protein is the concentration‐limiting factor. The single overexpression of DNAJB1 in HEK293T cells is sufficient to profoundly reduce HttExon1Q97 aggregation and represents a target of future therapeutic avenues for HD. |
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| Keywords: | disaggregation HttpolyQ molecular chaperones NPCs suppression |
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