What works and what does not work in Alzheimer’s disease? From interventions on risk factors to anti‐amyloid trials

Bullain, Szófia S.; Doody, Rachelle S.

doi:10.1111/jnc.15023

Cited by 27 publications

(25 citation statements)

References 124 publications

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“…1163 Developing disease-modifying therapies for AD presents an immense challenge, with little success despite intense work over decades. 314,[1164][1165][1166][1167] Some of the reasons why drug development for AD continues to fail include: (a) in vitro experiments poorly mimic in vivo conditions, (b) Aβ and tau exist in multiple covalent and aggregated forms of uncertain relevance to pathology and we have a poor knowledge of their structures, and (c) the limitations of animal models. 314 Amongst animal models, genetically-modified mouse lines are invaluable and widely used models for understanding genes, proteins, and biological pathways, evaluating disease progression, and assessing safety of molecules for therapeutic purposes in many diseases including neurodegenerative diseases, cancer and diabetes.…”

Section: Discussionmentioning

confidence: 99%

Amyloid Oligomers: A Joint Experimental/Computational Perspective on Alzheimer’s Disease, Parkinson’s Disease, Type II Diabetes, and Amyotrophic Lateral Sclerosis

et al. 2021

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Protein misfolding and aggregation is observed in many amyloidogenic diseases affecting either the central nervous system or a variety of peripheral tissues. Structural and dynamic characterization of all species along the pathways from monomers to fibrils is challenging by experimental and computational means because they involve intrinsically disordered proteins in most diseases. Yet understanding how amyloid species become toxic is the challenge in developing a treatment for these diseases. Here we review what computer, in vitro, in vivo and pharmacological experiments tell us about the accumulation and deposition of the oligomers of the (Aβ, tau), α-synuclein, IAPP and superoxide dismutase 1 proteins, which have been the mainstream concept underlying Alzheimer's disease (AD), Parkinson's disease (PD), type II diabetes (T2D) and amyotrophic lateral sclerosis (ALS) research, respectively for over many years.While SOD1 is a globular protein with a well-defined 3D structure, the Aβ, tau and α-synuclein proteins belong to the class of intrinsically disordered proteins (IDPs). IDPs are also known to play a critical role in many cellular functions such as signal transduction, cell growth, binding with DNA and RNA, and transcription, and are implicated in the development of cardiovascular problems and cancers 29 . The IDPs involved in neurodegenerative diseases have a few aggregation-prone regions and overall all IDPs have a low mean hydrophobicity and a high mean net charge 30 .IDPs are structurally flexible and lack stable secondary structures in aqueous solution. When isolated, they behave as polymers in a good solvent and their radii of gyration are well described by the Flory scaling law. 31 The insolubility and high self-assembly propensity of IDPs implicated in degenerative diseases have prevented high-resolution structural determination by solution nuclear magnetic resolution (NMR) and X-ray diffraction experiments. Local information at all aggregation steps can be, however, obtained by chemical shifts, residual coupling constants, and J-couplings from NMR, exchange hydrogen/deuterium (H/D) NMR, Raman spectroscopy; and secondary structure from fast Fourier infrared spectroscopy (FTIR) or circular dichroism (CD). Long-range tertiary contacts can be deduced from paramagnetic relaxation enhancement (PRE) NMR spectroscopy and single molecule Förster resonance energy transfer (sm-FRET), and short-range distance contacts can be extracted by cross linked residues determined by mass spectrometry (MS). Low-resolution 3D information of monomers and oligomers can be obtained by ion-mobility mass-spectrometry data (IM/MS) providing cross-collision sections, dynamic light scattering (DLS), pulse field gradient NMR spectroscopy and fluorescence correlation spectroscopy (FCS) providing hydrodynamics radius, small-angle X-ray scattering (SAXS) and small-angle neutron scattering (SANS), atomic force microscopy (AFM) and transmission electron microscopy (TEM) providing height features of the aggregates, as reported by some o...

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Section: Discussionmentioning

confidence: 99%

Amyloid Oligomers: A Joint Experimental/Computational Perspective on Alzheimer’s Disease, Parkinson’s Disease, Type II Diabetes, and Amyotrophic Lateral Sclerosis

et al. 2021

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“…Twenty-six of the monoclonals clearly recognize an Aß-related epitope that is located in the amino terminal ( 1 , 2 , 3 , 4 , 5 , 6 , 7 , 8 , 9 , 10 , 11 , 12 , 13 , 14 ) or central ( 7 , 15 , 16 , 17 , 18 , 19 , 20 , 21 , 22 , 23 , 24 , 25 , 26 , 27 , 28 ) third of the molecule or both ( Fig. 2 ).…”

Section: Resultsmentioning

confidence: 99%

“…Monoclonal antibodies against Aß are a leading class of therapeutic for AD. Many of these antibodies have been evaluated in clinical trials, but so far none have demonstrated consistent therapeutic activity in slowing the progression of AD and none have been approved by the FDA (reviewed in (4,5)). Conformation-dependent monoclonal antibodies against Aβ are also an invaluable tool for research in the role of amyloids in Alzheimer's disease because they recognize epitopes that are differentially displayed on distinct structural polymorphs or folded states of the peptide, providing insight into the role of polymorphisms in the pathogenic spectrum of the disease (6).…”

Section: Introductionmentioning

confidence: 99%

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An “epitomic” analysis of the specificity of conformation-dependent, anti-Aß amyloid monoclonal antibodies

Reyes-Ruiz

Nakajima

Baghallab

et al. 2021

Journal of Biological Chemistry

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Antibodies against Aß amyloid are indispensable research tools and potential therapeutics for Alzheimer’s disease. They display several unusual properties, such as specificity for aggregated forms of the peptide, the ability to distinguish polymorphic aggregate structures, and the ability to recognize generic aggregation-related epitopes formed by unrelated amyloid sequences. Understanding the mechanisms underlying these unusual properties and the structures of their corresponding epitopes is crucial for the understanding why antibodies display different therapeutic activities and for the development of more effective therapeutic agents. Here we employed a novel “epitomic” approach to map the fine structure of the epitopes of 28 monoclonal antibodies against amyloid-beta using immunoselection of random sequences from a phage display library, deep sequencing, and pattern analysis to define the critical sequence elements recognized by the antibodies. Although most of the antibodies map to major linear epitopes in the amino terminal 1 to 14 residues of Aß, the antibodies display differences in the target sequence residues that are critical for binding and in their individual preferences for nontarget residues, indicating that the antibodies bind to alternative conformations of the sequence by different mechanisms. Epitomic analysis also identifies discontinuous, nonoverlapping sequence Aß segments that may constitute the conformational epitopes that underlie the aggregation specificity of antibodies. Aggregation-specific antibodies recognize sequences that display a significantly higher predicted propensity for forming amyloid than antibodies that recognize the monomer, indicating that the ability of random sequences to aggregate into amyloid is a critical element of their binding mechanism.

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Section: Introductionmentioning

confidence: 99%

Epitomic analysis of the specificity of conformation-dependent, anti-Aß amyloid monoclonal antibodies

Reyes-Ruiz

Nakajima

Baghallab

et al. 2020

Preprint

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Antibodies against Aß amyloid are indispensable research tools and potential therapeutics for Alzheimer’s Disease, but display unusual properties, such as specificity for aggregated forms of the peptide, ability to distinguish several polymorphic aggregate structures and ability to recognize generic aggregation-related epitopes formed by unrelated amyloid sequences. Understanding the mechanisms underlying these unusual properties of anti-amyloid antibodies and the structures of their corresponding epitopes is crucial for the understanding why they display different therapeutic activities and for the development of more effective therapeutic agents. Here we employed a novel “epitomic” approach (1) to map the fine structure of the epitopes of 28 monoclonal antibodies against amyloid-beta using immunoselection of random sequences from a phage display, deep sequencing and pattern analysis to define the critical sequence elements recognized by the antibodies. Although most of the antibodies map to linear epitopes in the amino terminal 1-14 residues of Aß, the antibodies display differences in the target sequence residues that are critical for binding and in their individual preferences for non-target residues, indicating that the antibodies bind to alternative conformations of the sequence by different mechanisms. Epitomic analysis identifies more non-overlapping sequence Aß segments than peptide array approaches that may constitute the conformational epitopes that underly the aggregation specificity of antibodies. Aggregation specific antibodies also recognize sequences that display a significantly higher predicted propensity for forming amyloid than antibodies that recognize Aß monomer, indicating that the ability of the random sequences to aggregate into amyloid structures is a critical element of their binding mechanism.

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What works and what does not work in Alzheimer’s disease? From interventions on risk factors to anti‐amyloid trials

Cited by 27 publications

References 124 publications

Amyloid Oligomers: A Joint Experimental/Computational Perspective on Alzheimer’s Disease, Parkinson’s Disease, Type II Diabetes, and Amyotrophic Lateral Sclerosis

Amyloid Oligomers: A Joint Experimental/Computational Perspective on Alzheimer’s Disease, Parkinson’s Disease, Type II Diabetes, and Amyotrophic Lateral Sclerosis

An “epitomic” analysis of the specificity of conformation-dependent, anti-Aß amyloid monoclonal antibodies

Epitomic analysis of the specificity of conformation-dependent, anti-Aß amyloid monoclonal antibodies

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