Abstract

This research program focuses on copper and zinc uptake by the prion protein (PrP), and the role of metal binding in PrP structure, regulation, homeostasis, and neurodegenerative diseases. Brain deposits of misfolded PrP are responsible for a remarkable class of neurodegenerative diseases termed the Transmissible Spongiform Encephalopathies (TSEs). TSEs share pathologies with prevalent, age-related, neurodegenerative illnesses including Alzheimer's and Parkinson's disease. Although originally recognized for its role in neurodegenerative disease, it is now clear that PrP is essential for sustaining neuron function. PrP takes up both copper and zinc at sites that are essential for PrP activity. Through previous funding periods, this program fully elucidated the structure and thermodynamics of the copper and zinc binding sites. Most recently, a fundamentally new Zn2+ promoted interaction was discovered in which the metal ion drives contact between PrP's N-terminal and C-terminal domains. This finding suggests that many inherited prion diseases may arise from a weakening of this newly identified structure. Also in the last funding period, new mechanisms and sites for a- cleavage were identified, fundamentally modifying concepts in PrP regulation. The proposed work will build on these findings with the following three aims. 1) New structural studies will examine how copper influences PrP tertiary contacts, how familial mutations modulate this interaction, and whether the PrP N-terminus contributes to metal ion promoted stabilization. 2) New findings in the study of neurodegeneration suggest that PrP is a primary receptor for Abeta oligomers, implicated in Alzheimer's disease. Interestingly, the Abeta binding site is proximal to the PrP segment susceptible to a-cleavage. This project will further examine how ?-cleavage is regulated and whether toxic species, such as Abeta, occlude enzymatic access to the cleavage sites. 3) Early stage cellular damage arises from unregulated transmembrane currents caused by PrP. Work from several labs suggests that these currents arise from a poorly regulated PrP N-terminal domain. This will be examined collaboratively using whole cell patch clamp electrophysiology to determine the influence of PrP structure, a-cleavage and Abeta binding. Together, these experiments will test a model in which PrP must be tightly regulated in metal ion homeostasis, and how loss of regulation might contribute to prion and Alzheimer's disease.

Public Health Relevance

Copper and zinc are essential micronutrients in the brain. This program will examine the interplay among these metal ions and proteins implicated in neurodegenerative disease, specifically the prion and Alzheimer's diseases. Concepts emerging from the planned projects on prion protein structure and regulation will identify new pathways and targets for treating neurodegeneration.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM065790-16
Application #
9512995
Study Section
Macromolecular Structure and Function A Study Section (MSFA)
Program Officer
Wehrle, Janna P
Project Start
2002-03-01
Project End
2019-06-30
Budget Start
2018-07-01
Budget End
2019-06-30
Support Year
16
Fiscal Year
2018
Total Cost
Indirect Cost

  Institution

Name
University of California Santa Cruz
Department
Chemistry
Type
Schools of Arts and Sciences
DUNS #
125084723
City
Santa Cruz
State
CA
Country
United States
Zip Code
95064

  Publications

Evans, Eric G B; Millhauser, Glenn L (2017) Copper- and Zinc-Promoted Interdomain Structure in the Prion Protein: A Mechanism for Autoinhibition of the Neurotoxic N-Terminus. Prog Mol Biol Transl Sci 150:35-56
Wu, Bei; McDonald, Alex J; Markham, Kathleen et al. (2017) The N-terminus of the prion protein is a toxic effector regulated by the C-terminus. Elife 6:
Evans, Eric G B; Pushie, M Jake; Markham, Kate A et al. (2016) Interaction between Prion Protein's Copper-Bound Octarepeat Domain and a Charged C-Terminal Pocket Suggests a Mechanism for N-Terminal Regulation. Structure 24:1057-67
Evans, Eric G B; Millhauser, Glenn L (2015) Genetic Incorporation of the Unnatural Amino Acid p-Acetyl Phenylalanine into Proteins for Site-Directed Spin Labeling. Methods Enzymol 563:503-27
Lau, Agnes; McDonald, Alex; Daude, Nathalie et al. (2015) Octarepeat region flexibility impacts prion function, endoproteolysis and disease manifestation. EMBO Mol Med 7:339-56
Zhang, Siyuan; Naab, Benjamin D; Jucov, Evgheni V et al. (2015) n-Dopants Based on Dimers of Benzimidazoline Radicals: Structures and Mechanism of Redox Reactions. Chemistry 21:10878-85
McDonald, Alex J; Dibble, Jessie P; Evans, Eric G B et al. (2014) A new paradigm for enzymatic control of ?-cleavage and ?-cleavage of the prion protein. J Biol Chem 289:803-13
McDonald, Alex J; Millhauser, Glenn L (2014) PrP overdrive: does inhibition of ?-cleavage contribute to PrP(C) toxicity and prion disease? Prion 8:
Stellato, Francesco; Minicozzi, Velia; Millhauser, Glenn L et al. (2014) Copper-zinc cross-modulation in prion protein binding. Eur Biophys J 43:631-42
Thompson, Darren A; Evans, Eric G B; Kasza, Tomas et al. (2014) Adapter reagents for protein site specific dye labeling. Biopolymers 102:273-9

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