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Literature DB >> 34617884

NHE6 depletion corrects ApoE4-mediated synaptic impairments and reduces amyloid plaque load.

Theresa Pohlkamp^1,2, Xunde Xian^1,2,3, Connie H Wong^1,2, Murat S Durakoglugil^1,2, Gordon Chandler Werthmann^1,2, Takaomi C Saido⁴, Bret M Evers², Charles L White⁵, Jade Connor^1,2, Robert E Hammer⁶, Joachim Herz^1,2,7,8.

Abstract

Apolipoprotein E4 (ApoE4) is the most important and prevalent risk factor for late-onset Alzheimer's disease (AD). The isoelectric point of ApoE4 matches the pH of the early endosome (EE), causing its delayed dissociation from ApoE receptors and hence impaired endolysosomal trafficking, disruption of synaptic homeostasis, and reduced amyloid clearance. We have shown that enhancing endosomal acidification by inhibiting the EE-specific sodium-hydrogen exchanger 6 (NHE6) restores vesicular trafficking and normalizes synaptic homeostasis. Remarkably and unexpectedly, loss of NHE6 (encoded by the gene Slc9a6) in mice effectively suppressed amyloid deposition even in the absence of ApoE4, suggesting that accelerated acidification of EEs caused by the absence of NHE6 occludes the effect of ApoE on amyloid plaque formation. NHE6 suppression or inhibition may thus be a universal, ApoE-independent approach to prevent amyloid buildup in the brain. These findings suggest a novel therapeutic approach for the prevention of AD by which partial NHE6 inhibition reverses the ApoE4-induced endolysosomal trafficking defect and reduces plaque load.

Entities: Chemical

Keywords: Alzheimer's; ApoE; NHE6; endosome; mouse; neurodegeneration; neuroscience; trafficking

Mesh：

Substances：

Year: 2021 PMID： 34617884 PMCID： PMC8547963 DOI： 10.7554/eLife.72034

Source DB: PubMed Journal: Elife ISSN： 2050-084X Impact factor: 8.713

108 in total

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Journal: Nat Neurosci Date: 2019-01-07 Impact factor: 24.884

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Authors: Samuel F Yanuck
Journal: Front Psychiatry Date: 2019-10-03 Impact factor: 4.157

NHE6 depletion corrects ApoE4-mediated synaptic impairments and reduces amyloid plaque load.

1. Structure of the LDL receptor extracellular domain at endosomal pH.

2. Recognition of double-stranded RNA by human toll-like receptor 3 and downstream receptor signaling requires multimerization and an acidic pH.

3. Hematoxylin and eosin staining of tissue and cell sections.

4. Loss of TREM2 function increases amyloid seeding but reduces plaque-associated ApoE.

5. Genetic variation within endolysosomal system is associated with late-onset Alzheimer's disease.

6. Endocytic pathway abnormalities precede amyloid beta deposition in sporadic Alzheimer's disease and Down syndrome: differential effects of APOE genotype and presenilin mutations.

7. Acid-dependent ligand dissociation and recycling of LDL receptor mediated by growth factor homology region.

8. Microglial Phagocytosis of Neurons: Diminishing Neuronal Loss in Traumatic, Infectious, Inflammatory, and Autoimmune CNS Disorders.

9. Intracellular processing of endocytosed triglyceride-rich lipoproteins comprises both recycling and degradation.

10. Reversal of ApoE4-induced recycling block as a novel prevention approach for Alzheimer's disease.

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2. Loss of endosomal exchanger NHE6 leads to pathological changes in tau in human neurons.