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Amyloid-beta Degradation Pathways

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Amyloid-beta Degradation Pathways

Overview

The enzymatic degradation of amyloid-beta (Aβ) peptides represents a critical clearance pathway in the brain. Multiple proteolytic systems have evolved to degrade Aβ, with neprilysin (NEP) and insulin-degrading enzyme (IDE) being the two most important Aβ-degrading peptidases [@miners2011]. Dysfunction of these clearance pathways contributes to Aβ accumulation in Alzheimer's disease (AD), making them attractive therapeutic targets [@nalivaeva2012].

Major Aβ-Degrading Enzymes

Overview of Proteolytic Systems

graph TD A["Abeta Peptides<br/>Abeta40, Abeta42"] --> B["Proteolytic<br/>Enzymes"] B --> C["Neprilysin<br/>NEP"] B --> D["IDE"] B --> E["MMPs<br/>MMP-2, MMP-9"] B --> F["Cathepsins<br/>B, D, L"] B --> G["Other<br/>Plasmin, ECE"] C --> H["SOLUBLE<br/>Abeta Clearance"] D --> H E --> H F --> H G --> H

| Enzyme | Location | Substrate Specificity | Efficiency |
|--------|----------|----------------------|------------|
| Neprilysin | Neurons, Endothelium | Abeta40 > Abeta42 | Highest |
| IDE | Neurons, Glia | Abeta42 > Abeta40 | High |
| MMP-2/9 | Astrocytes, Microglia | Abeta40, Abeta42 | Moderate |
| Cathepsin B | Lysosomes | Abeta40 | Moderate |
| Cathepsin D | Lysosomes | Abeta42 | High |

Neprilysin (NEP)

Structure and Function

Neprilysin (CD10, EC 3.4.24.11) is a zinc-dependent metalloprotease [@saido1998]:

  • Type II transmembrane glycoprotein
  • Extracellular catalytic domain
  • Broad substrate specificity beyond Aβ

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