Focusing the amyloid cascade hypothesis on N-truncated Abeta peptides as drug targets against Alzheimer’s disease

Bayer, Thomas A.; Wirths, Oliver

doi:10.1007/s00401-014-1287-x

Cited by 134 publications

(143 citation statements)

References 111 publications

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“…Besides full-length Aß peptides, a variety of different N-truncated Ab peptides have been identified within the cored and diffuse amyloid plaques in the AD brain starting with amino residue Ala-2, pyroglutamylated Glu-3, Phe-4, Arg-5, His-6, Asp-7, Ser-8, Gly-9, Tyr-10, and pyroglutamylated Glu-11 (Antonios et al, 2013;Bayer and Wirths, 2014;Lemere et al, 1996;Saido et al, 1995).…”

Section: Introductionmentioning

confidence: 99%

Oleuropein aglycone protects against pyroglutamylated-3 amyloid-ß toxicity: biochemical, epigenetic and functional correlates

Luccarini

Grossi

Rigacci

et al. 2015

Neurobiology of Aging

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a b s t r a c tAmyloid-ß (Aß) fragments, oligomeric Aß aggregates, and pyroglutamylated-Aß peptides, as well as epigenetic mechanisms and autophagy dysfunction all appear to contribute in various ways to Alzheimer's disease progression. We previously showed that dietary supplementation of oleuropein aglycone, a natural phenol abundant in the extra virgin olive oil, can be protective by reducing Aß42 deposits in the brain of young and middle-aged TgCRND8 mice. Here, we extended our study to aged TgCRND8 mice showing increased pE3-Aß in the brain deposits. We report that oleuropein aglycone is active against glutaminylcyclase-catalyzed pE3-Aß generation reducing enzyme expression and interferes both with Aß42 and pE3-Aß aggregation. Moreover, the phenol astonishingly activates neuronal autophagy even in mice at advanced stage of pathology, where it increases histone 3 and 4 acetylation, which matches both a decrease of histone deacetylase 2 expression and a significant improvement of synaptic function. The occurrence of these functional, epigenetic, and histopathologic beneficial effects even at a late stage of the pathology suggests that the phenol could be beneficial at the therapeutic, in addition to the prevention, level.

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Section: Introductionmentioning

confidence: 99%

Oleuropein aglycone protects against pyroglutamylated-3 amyloid-ß toxicity: biochemical, epigenetic and functional correlates

Luccarini

Grossi

Rigacci

et al. 2015

Neurobiology of Aging

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“…Indeed, a series of studies on human CSF has identified numerous APP N-terminal fragments (29) and N-terminally extended A␤ species that may have (patho)physiological functions (44,45). Evidence also exists for the N-terminal truncation of the A␤ peptide at every one of its first 11 amino acids, although again, the biological relevance of the majority of these species remains uncertain (46). At least one N-terminally truncated species of A␤ (A␤5-X) has been shown to increase in the CSF of patients treated with a BACE1 inhibitor, suggesting that it is liberated in a BACE1-independent manner and that the protease responsible for its liberation acts in direct competition with BACE1 (47).…”

Section: Mystery Proteasesmentioning

confidence: 99%

A Greek Tragedy: The Growing Complexity of Alzheimer Amyloid Precursor Protein Proteolysis

Andrew

Kellett

Wang

et al. 2016

Journal of Biological Chemistry

150

122

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Proteolysis of the amyloid precursor protein (APP) liberates various fragments including the proposed initiator of Alzheimer disease-associated dysfunctions, amyloid-␤. However, recent evidence suggests that the accepted view of APP proteolysis by the canonical ␣-, ␤-, and ␥-secretases is simplistic, with the discovery of a number of novel APP secretases (including ␦-and -secretases, alternative ␤-secretases) and additional metabolites, some of which may also cause synaptic dysfunction. Furthermore, various proteins have been identified that interact with APP and modulate its cleavage by the secretases. Here, we give an overview of the increasingly complex picture of APP proteolysis.Currently over 46 million people worldwide are living with dementia (see the Alzheimer's Disease International website) with Alzheimer disease (AD) 3 representing the most common form of dementia. In AD, the amyloid cascade hypothesis posits that amyloid-␤ (A␤), produced through the sequential proteolytic cleavage of the amyloid precursor protein (APP) by the ␤-and ␥-secretases, is a key molecule in initiating and propagating disease pathology including neurofibrillary tangle formation, neuronal cell loss, aberrant synaptic activity, and brain atrophy that lead to the clinically recognized symptoms of dementia (1). However, identification of the A␤ peptide 25 years ago has not yet led to the advent of a viable therapeutic strategy that can slow or halt the progression of AD. Recent studies have revealed new complexities in the proteolytic processing of APP, including the identification of novel secretases which generate APP metabolites that accumulate in the brains of AD patients and may contribute to the synaptic dysfunction observed in the disease. In addition, numerous proteins are being identified that interact with APP, modulating its proteolysis and A␤ production. These new APP secretases and metabolites, along with the APP interactors, may present novel therapeutic targets that are independent of direct modulation of the canonical secretases and that will need to be considered when evaluating the results from current A␤-directed therapies. In this Minireview, we summarize the recent developments in APP proteolysis focusing on the novel secretases, APP interactors, and APP metabolites that are impacting on our understanding of both APP biology and the neurodegenerative disease process. The Canonical ␣-, ␤-, and ␥-Secretases and APP FragmentsThe generally accepted model of APP proteolysis is that APP is processed by one of two distinct proteolytic pathways (Fig. 1A). In the amyloidogenic pathway, ␤-secretase, the ␤-site APP-cleaving enzyme 1 (BACE1), cleaves APP within the ectodomain and liberates a soluble proteolytic fragment, termed soluble APP␤ (sAPP␤), primarily in the endosomal system from the transmembrane APP holoprotein (2). The remaining C-terminal membrane-bound APP fragment, CTF␤, is subsequently cleaved by the presenilin (PS)-containing ␥-secretase multisubunit complex to liberate the A␤ peptide and the APP intrace...

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“…Nevertheless, according to the amyloid cascade hypothesis first proposed in the 1990s, [6] the imbalance between production and clearance of the A peptides is the origin of the accumulation of peptides that further leads to the aggregation of the soluble monomeric peptide into fibrils and amorphous aggregates detected in the senile plaque. [3][4][5][6][7][8][9] The amyloid cascade is an early event and plays a causal role in AD (Scheme 1). The complete aggregation pathway from the monomeric peptide to the fibrils contains several steps including oligomers, protofibrils, and fi-etiology of the disease.…”

Section: Alzheimer's Disease (Ad)mentioning

confidence: 99%

“…[9,[24][25][26] The reason for such heterogeneity is unclear. In seminal reports by Masters and co-workers, [27,28] the quantity of A 4-n was found to be predominant in the amyloid deposits of AD patients.…”

Section: N-terminally Truncated Peptidesmentioning

confidence: 99%

Cu^II Binding to Various Forms of Amyloid‐β Peptides: Are They Friends or Foes?

2017

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Abstract:In the present microreview, we describe Cu II binding to several forms of amyloid-peptides, the peptides involved in Alzheimer's disease. It has indeed been shown that in addition to the "full-length" peptide that originates from the precursor protein after cleavage at the 1-position, several other shorter peptides do exist in large proportion and might be involved in the disease as well. Cu II binding to amyloid-peptides is one of the key interactions that impact both the aggregating properties of the amyloid peptides and the production of reactive oxygen species (ROS), two events that are linked to the

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Focusing the amyloid cascade hypothesis on N-truncated Abeta peptides as drug targets against Alzheimer’s disease

Cited by 134 publications

References 111 publications

Oleuropein aglycone protects against pyroglutamylated-3 amyloid-ß toxicity: biochemical, epigenetic and functional correlates

Oleuropein aglycone protects against pyroglutamylated-3 amyloid-ß toxicity: biochemical, epigenetic and functional correlates

A Greek Tragedy: The Growing Complexity of Alzheimer Amyloid Precursor Protein Proteolysis

Cu^II Binding to Various Forms of Amyloid‐β Peptides: Are They Friends or Foes?

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Focusing the amyloid cascade hypothesis on N-truncated Abeta peptides as drug targets against Alzheimer’s disease

Cited by 134 publications

References 111 publications

Oleuropein aglycone protects against pyroglutamylated-3 amyloid-ß toxicity: biochemical, epigenetic and functional correlates

Oleuropein aglycone protects against pyroglutamylated-3 amyloid-ß toxicity: biochemical, epigenetic and functional correlates

A Greek Tragedy: The Growing Complexity of Alzheimer Amyloid Precursor Protein Proteolysis

CuII Binding to Various Forms of Amyloid‐β Peptides: Are They Friends or Foes?

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Cu^II Binding to Various Forms of Amyloid‐β Peptides: Are They Friends or Foes?