Hsp90 Chaperone in Disease

Publication date

2019-11-15

Authors

Rüdiger, Stefan G.D.ISNI 0000000394040769
Ferrari, LucaISNI 0000000505993192

Editors

Asea, Alexzander A. A.
Kaur, Punit

Advisors

Supervisors

Document Type

Part of book
Open Access logo

License

taverne

Abstract

The molecular chaperone Hsp90 is at the heart of protein homeostasis control. A wide range of pathologies disturbs protein homeostasis, thus placing Hsp90 at the crossroads of many diseases. Here, we evaluate the impact of recent progress in understanding the molecular mechanism of Hsp90-client interactions and their role in disease. We discuss the role of Hsp90 for hormonal imbalances, cancer and neurodegenerative disorders. For each disease class we discuss implications of complexes in which Hsp90 binds to a paradigmatic client: the transcription factor Glucocorticoid Receptor, the kinase Cdk4 and the microtubule stabilizer Tau. The mechanistic insights allow us to elaborate on possible therapeutic intervention routes. Hsp90 is a druggable chaperone. Thus, understanding Hsp90 biology at molecular resolution offers an interesting approach to tackle protein-related diseases.

Keywords

Kinases, Molecular chaperones, Neurodegeneration, Protein folding, Proteostasis, Steroid receptors, ad, Taverne, SDG 3 - Good Health and Well-being

Citation

Rüdiger, S G D & Ferrari, L 2019, Hsp90 Chaperone in Disease. in A A A Asea & P Kaur (eds), Heat Shock Protein 90 in Human Diseases and Disorders. 1 edn, Heat Shock Proteins, vol. 19, Springer, pp. 473-491. https://doi.org/10.1007/978-3-030-23158-3_21