Adapting proteostasis to ameliorate aggregation-associated amyloid diseases

Kelly, Jeffery W.

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Introduction
The central dogma of molecular biology
Protein folding
Competition - folding, misfolding, aggregation
The proteostasis network
Gain of function disease
Loss of function disease
The transthyretin (TTR) amyloidoses
The mechanism of protein aggregation
Transthyretin (TTR)
The mechanism by which TTR aggregates
Ligand binding can stabilize tetramers
A key human genetics observation
TTR tetramer dissociation is rate-limiting
Interallelic trans–suppression improves pathology
Native state kinetic stabilization
Tafamidis designed with X-ray crystallography
Clinical trials
NIS-LL neurological exam
mBMI: modified body mass index
Tafamidis therapy approved in EU for TTR-FAP
Liver transplant: the only approach until 2011
Portuguese experience with tafamidis
Kinetic stabilizers extend lifespan in TTR
Pfizer cardiomyopathy trial completed
Repurposing diflunisal
Pharmacologic support for the amyloid hypothesis
Eye and CNS pathology emerging in patients
PIB-PET transthyretin cerebral amyloid angiopathy
The tafamidis development timeline
Part 1: Conclusions
Improving protein misfolding/aggregation diseases
Sub-cellular proteostasis network regulation
Protein folding vs. degradation in the ER
The unfolded protein response (UPR)
Arm-selective UPR transcriptional programs
The ER proteostasis network pathways
ATF6 activation reduces secretion of TTR mutant
Screening strategy for discovering UPR activators
ERSE-FLuc reporter small molecule activation
Transcriptional program drives structure-activity
ATF6 activation reduces secretion of mutant TTR
Part 2: Conclusions
Acknowledgments

Topics Covered

Protein folding, misfolding, aggregation
The proteostasis network and its regulation
Gain and loss of function diseases
The transthyretin (TTR) amyloidosis
Kinetic stabilizers & clinical trial results
Tafamidis & Diflunisal: evidence for the amyloid hypothesis
Improving protein misfolding/aggregation diseases
The unfolded protein response (UPR) and its arm-selective activators
ATF6 activation & reduction of TTR mutant
Clinical trials in amyloidosis with cardiac involvement

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Protein Folding, Aggregation and Design

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Neurology

Talk Citation

Kelly, J.W. (2018, December 31). Adapting proteostasis to ameliorate aggregation-associated amyloid diseases [Video file]. In The Biomedical & Life Sciences Collection, Henry Stewart Talks. Retrieved November 4, 2025, from https://doi.org/10.69645/ROLG5239.
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Publication History

Published on December 31, 2018

Financial Disclosures

Dr. Jeffery W. Kelly has not informed HSTalks of any commercial/financial relationship that it is appropriate to disclose.

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Adapting proteostasis to ameliorate aggregation-associated amyloid diseases

Dr. Jeffery W. Kelly – The Scripps Research Institute, USA

Published on December 31, 2018 49 min

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Transcript

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0:00

Hello, I'm Jeff Kelly from the Scripps Research Institute and it's a privilege today to give a Henry Stewart talk. Focused on adapting the biology and/or chemistry of protein homeostasis to ameliorate diseases where protein aggregation causes degenerative phenotypes.

0:19

Even the most experienced scientists sometimes catch themselves thinking about translation as affording folded functional proteins.

0:30

But in fact, translation affords an unordered ensemble of conformers that generally speaking, have to fold in order to function, and while protein folding can be spontaneous. For the vast majority of human proteins, protein folding is assisted in some cases catalyzed by the protein homeostasis network. This is because of the reasons listed at the bottom of the slide in part. That is, there are chemical processes like peptidyl-prolyl amide bond isomerization and disulfide bond formation that are simply too slow to support life, and those processes must be catalyzed by enzymes.

1:14

Moreover, there's always a kinetic competition between protein folding, protein misfolding, and concentration dependent protein aggregation. And it's important that the biological components of the protein homeostasis network regulate these competitive processes such that sufficient function is maintained in the cell and in the extracellular space.

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Adapting proteostasis to ameliorate aggregation-associated amyloid diseases

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Adapting proteostasis to ameliorate aggregation-associated amyloid diseases