Loss of endophilin-B1 exacerbates Alzheimer’s disease pathology | Zendy

David B. Wang | Zendy; Yoshito Kinoshita | Zendy; C. Kinoshita | Zendy; Takuma Uo | Zendy; Bryce L. Sopher | Zendy; Eiron Cudaback | Zendy; C. Dirk Keene | Zendy; Tina Bilousova | Zendy; Karen H. Gylys | Zendy; Amanda Case | Zendy; Suman Jayadev | Zendy; HongGang Wang | Zendy; Gwenn A. Garden | Zendy; Richard S. Morrison | Zendy

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Loss of endophilin-B1 exacerbates Alzheimer’s disease pathology

Author(s) -

David B. Wang,

Yoshito Kinoshita,

C. Kinoshita,

Takuma Uo,

Bryce L. Sopher,

Eiron Cudaback,

C. Dirk Keene,

Tina Bilousova,

Karen H. Gylys,

Amanda Case,

Suman Jayadev,

HongGang Wang,

Gwenn A. Garden,

Richard S. Morrison

Publication year - 2015

Publication title -

brain

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 5.142

H-Index - 336

eISSN - 1460-2156

pISSN - 0006-8950

DOI - 10.1093/brain/awv128

Subject(s) - neuroprotection , gene isoform , astrogliosis , neuroscience , autophagy , presenilin , alzheimer's disease , neurodegeneration , amyloid precursor protein , chemistry , microbiology and biotechnology , biology , disease , apoptosis , medicine , pathology , central nervous system , biochemistry , gene

Endophilin-B1, also known as Bax-interacting factor 1 (Bif-1, and encoded by SH3GLB1), is a multifunctional protein involved in apoptosis, autophagy and mitochondrial function. We recently described a unique neuroprotective role for neuron-specific alternatively spliced isoforms of endophilin-B1. To examine whether endophilin-B1-mediated neuroprotection could be a novel therapeutic target for Alzheimer's disease we used a double mutant amyloid precursor protein and presenilin 1 (APPswe/PSEN1dE9) mouse model of Alzheimer's disease and observed that expression of neuron-specific endophilin-B1 isoforms declined with disease progression. To determine if this reduction in endophilin-B1 has a functional role in Alzheimer's disease pathogenesis, we crossed endophilin-B1(-/-) mice with APPswe/PSEN1dE9 mice. Deletion of endophilin-B1 accelerated disease onset and progression in 6-month-old APPswe/PSEN1dE9/endophilin-B1(-/-) mice, which showed more plaques, astrogliosis, synaptic degeneration, cognitive impairment and mortality than APPswe/PSEN1dE9 mice. In mouse primary cortical neuron cultures, overexpression of neuron-specific endophilin-B1 isoforms protected against amyloid-β-induced apoptosis and mitochondrial dysfunction. Additionally, protein and mRNA levels of neuron-specific endophilin-B1 isoforms were also selectively decreased in the cerebral cortex and in the synaptic compartment of patients with Alzheimer's disease. Flow sorting of synaptosomes from patients with Alzheimer's disease demonstrated a negative correlation between amyloid-β and endophilin-B1 levels. The importance of endophilin-B1 in neuronal function was further underscored by the development of synaptic degeneration and cognitive and motor impairment in endophilin-B1(-/-) mice by 12 months. Our findings suggest that endophilin-B1 is a key mediator of a feed-forward mechanism of Alzheimer's disease pathogenesis where amyloid-β reduces neuron-specific endophilin-B1, which in turn enhances amyloid-β accumulation and neuronal vulnerability to stress.

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