Francisco J. Muñoz scite author profile

Brain acetylcholinesterase (AChE) forms stable complexes with amyloid-␤ peptide (A␤) during its assembly into filaments, in agreement with its colocalization with the A␤ deposits of Alzheimer's brain. The association of the enzyme with nascent A␤ aggregates occurs as early as after 30 min of incubation. Analysis of the catalytic activity of the AChE incorporated into these complexes shows an anomalous behavior reminiscent of the AChE associated with senile plaques, which includes a resistance to low pH, high substrate concentrations, and lower sensitivity to AChE inhibitors. Furthermore, the toxicity of the AChE-amyloid complexes is higher than that of the A␤ aggregates alone. Thus, in addition to its possible role as a heterogeneous nucleator during amyloid formation, AChE, by forming such stable complexes, may increase the neurotoxicity of A␤ fibrils and thus may determine the selective neuronal loss observed in Alzheimer's brain.

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Functions and dysfunctions of nitric oxide in brain

Picón-Pagès

Garcia-Buendia

Muñoz

2019

Biochimica et Biophysica Acta (BBA) - Molecular Basis of Diseas

249

170

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Francisco J. Muñoz

The physiology and pathophysiology of nitric oxide in the brain

The role of oxidative stress in the toxicity induced by amyloid β-peptide in Alzheimer’s disease

Clinical Outcome of Patients With Upper-Extremity Deep Vein Thrombosis

Stable Complexes Involving Acetylcholinesterase and Amyloid-β Peptide Change the Biochemical Properties of the Enzyme and Increase the Neurotoxicity of Alzheimer’s Fibrils

Functions and dysfunctions of nitric oxide in brain

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