Strategies and Tools for Modulating Pathologic Protein Self-Assembly in Proteinopathies

Editors

Gal Bitan

Department of Neurology, David Geffen School of Medicine, University of California, Los Angeles

Sandra Macedo-Ribeiro

Institute of Molecular and Cellular Biology, University of Porto

Maria Rosário Almeida

Institute of Biomedical Sciences Abel Salazar, University of Porto

Impact

Retraction

23 September 2021

Retraction: Different Amyloid-β Self-Assemblies Have Distinct Effects on Intracellular Tau Aggregation

Frontiers Editorial Office

1,943 views

0 citations

Review

11 December 2020

Modulation of the Mechanisms Driving Transthyretin Amyloidosis

Filipa Bezerra

, 1 more and

Maria Rosário Almeida

11,393 views

33 citations

Review

27 November 2020

MIRRAGGE – Minimum Information Required for Reproducible AGGregation Experiments

Pedro M. Martins

, 19 more and

Sandra Macedo-Ribeiro

7,099 views

25 citations

Review

04 August 2020

Targeting Amyloidogenic Processing of APP in Alzheimer’s Disease

Jing Zhao

, 3 more and

Chunyu Wang

20,466 views

119 citations

ASC specks released from activated microglia cross-seed Aβ aggregation. The NLRP3 inflammasome is activated in microglia in response to a variety of stimuli, including Aβ fibrils. This activation leads to the release of specks formed from ASC, an adaptor protein that is involved in the inflammasome pathway. ASC specks cross-seed Aβ peptide, resulting in the formation of further Aβ aggregates in the brain and may create a cycle of inflammasome activation and amyloid formation.

Review

26 November 2020

Modulation of β-Amyloid Fibril Formation in Alzheimer’s Disease by Microglia and Infection

Madeleine R. Brown

, 1 more and

Eric W. Hewitt

19,347 views

52 citations

Mini Review

09 June 2020

Therapeutic Approaches Targeting Protein Aggregation in Amyotrophic Lateral Sclerosis

Ravinder Malik

and

Martina Wiedau

9,724 views

36 citations

Review

19 May 2020

Substrate–Enzyme Interactions in Intramembrane Proteolysis: γ-Secretase as the Prototype

Xinyue Liu

, 5 more and

Chunyu Wang

4,195 views

6 citations

Review

19 March 2020

CNS-Derived Blood Exosomes as a Promising Source of Biomarkers: Opportunities and Challenges

Simon Hornung

, 1 more and

Gal Bitan

Isolation of CNS-derived exosomes from blood. (A) The protocol of the Zhang group relies on anti-L1CAM antibody-coupled epoxy beads, which are incubated directly with diluted plasma to bind neuronal exosomes. The following washing steps in 0.1% BSA remove unbound, non-neuronal exosomes in the sample. (B) The method described by Goetzl et al. The protocol uses first an exosome precipitation step by ExoQuick followed by capturing specifically neuronal exosomes with biotinylated anti-L1CAM antibodies and a streptavidin-conjugated resin. Subsequent washing steps remove non-neuronal exosomes as well as the antibody and resin to yield neuronal exosomes.

Eukaryotic cells release different types of extracellular vesicles (EVs) including exosomes, ectosomes, and microvesicles. Exosomes are nanovesicles, 30–200 nm in diameter, that carry cell- and cell-state-specific cargo of proteins, lipids, and nucleic acids, including mRNA and miRNA. Recent studies have shown that central nervous system (CNS)-derived exosomes may carry amyloidogenic proteins and facilitate their cell-to-cell transfer, thus playing a critical role in the progression of neurodegenerative diseases, such as tauopathies and synucleinopathies. CNS-derived exosomes also have been shown to cross the blood-brain-barrier into the bloodstream and therefore have drawn substantial attention as a source of biomarkers for various neurodegenerative diseases as they can be isolated via a minimally invasive blood draw and report on the biochemical status of the CNS. However, although isolating specific brain-cell-derived exosomes from the blood is theoretically simple and the approach has great promise, practical details are of crucial importance and may compromise the reproducibility and utility of this approach, especially when different laboratories use different protocols. In this review we discuss the role of exosomes in neurodegenerative diseases, the usefulness of CNS-derived blood exosomes as a source of biomarkers for these diseases, and practical challenges associated with the methodology of CNS-derived blood exosomes and subsequent biomarker analysis.

26,758 views

183 citations

IAPP on physiological and pathological contexts and (poly)phenols-mediated protection. (A) In healthy conditions, IAPP is co-secreted with insulin to regulate glucose metabolism and homeostasis in a post-meal condition. Several functions are attributed to IAPP: slowing down gastric emptying, thereby reducing food intake and body weight; reducing glucose output from liver and glucagon secretion; and stimulating the renin-angiotensin system, vasodilation, and blood glucose uptake. (B) In disease conditions, IAPP pathological species deposit in the pancreas and in brain microvasculature where they induce the injury of small vessels and reach the brain parenchyma. In the brain environment, IAPP forms heterogeneous deposits with Aβ molecules increasing neurotoxicity. Proteostasis imbalance caused by Aβ/IAPP and tau may promote a set of molecular changes that culminate in glucose homeostasis dysregulation, cell death, and neurodegeneration. The molecular pathways of β-cell dysfunction are depicted: autophagy dysregulation; ER stress; UPP overload; membrane instability; and mitochondrial damage. (C) Protection mediated by (poly)phenols is associated with the stabilization of IAPP monomers, the remodeling of amyloids, protofibrils, and toxic oligomers to non-fibrillogenic “off-pathway” oligomers and monomers. Aβ, Amyloid beta; ER, Endoplasmic Reticulum; IAPP, Islet Amyloid Polypeptide; Ub, Ubiquitin; UPP, Ubiquitin Proteasome Pathway.

Mini Review

20 March 2020

Islet Amyloid Polypeptide: A Partner in Crime With Aβ in the Pathology of Alzheimer's Disease

Ana F. Raimundo

, 2 more and

Regina Menezes

18,874 views

60 citations

Perspective

11 March 2020

Protein Aggregation and Dysfunction of Autophagy-Lysosomal Pathway: A Vicious Cycle in Lysosomal Storage Diseases

Antonio Monaco

and

Alessandro Fraldi

10,665 views

73 citations

Schematic representation of the possible mechanism of fibril formation by Aβ peptide and its fragments. (A) Monomers; (B) ring-like oligomers; and (C) single fibril. R is a recombinant sample and S is synthetic.

Perspective

31 January 2020

Oligomers Are Promising Targets for Drug Development in the Treatment of Proteinopathies

Oxana V. Galzitskaya

3,960 views

16 citations

Untangling the conformational heterogeneity and molecular interactions of monomeric intrinsically disordered proteins (IDPs) through single-molecule fluorescence (SMF) approaches. Single-molecule Förster resonance energy transfer (smFRET) histogram discriminating between distinct conformational ensembles of double-label protein (donor–acceptor): monomeric free protein in solution and bound states with extended (low ETeff) or compacted conformations (high ETeff). Fluorescence correlation spectroscopy (FCS) autocorrelation curve reporting on changes in the diffusion time of single-label protein free in solution (blue curve) and upon interaction with aggregation inducers or binding partners (gray curve). The binding results into a shift of the autocorrelation curve to the right (longer translational diffusion times).

Review

10 January 2020

Untangling the Conformational Polymorphism of Disordered Proteins Associated With Neurodegeneration at the Single-Molecule Level

Melissa Birol

and

Ana M. Melo

5,153 views

13 citations

Review

05 December 2019

Targeting Alpha-Synuclein as a Therapy for Parkinson’s Disease

Carroll Rutherford Fields

, 1 more and

Richard Wade-Martins

Parkinson’s disease (PD) is one of the most common neurodegenerative disorders with a global burden of approximately 6.1 million patients. Alpha-synuclein has been linked to both the sporadic and familial forms of the disease. Moreover, alpha-synuclein is present in Lewy-bodies, the neuropathological hallmark of PD, and the protein and its aggregation have been widely linked to neurotoxic pathways that ultimately lead to neurodegeneration. Such pathways include autophagy/lysosomal dysregulation, synaptic dysfunction, mitochondrial disruption, and endoplasmic reticulum (ER) and oxidative stress. Alpha-synuclein has not only been shown to alter cellular pathways but also to spread between cells, causing aggregation in host cells. Therapeutic approaches will need to address several, if not all, of these angles of alpha-synuclein toxicity. Here we review the current advances in therapeutic efforts for PD that aim to produce a disease-modifying therapy by targeting the spread, production, aggregation, and degradation of alpha-synuclein. These include: receptor blocking strategies whereby putative alpha-synuclein receptors could be blocked inhibiting alpha-synuclein spread, an alpha-synuclein reduction which will decrease the amount alpha-synuclein available for aggregation and pathway disruption, the use of small molecules in order to target alpha-synuclein aggregation, immunotherapy and the increase of alpha-synuclein degradation by increasing autophagy/lysosomal flux. The research discussed here may lead to a disease-modifying therapy that tackles disease onset and progression in the future.

59,752 views

264 citations