Lysosomal dysfunction in the brain of a mouse model with intraneuronal accumulation of carboxyl terminal fragments of the amyloid precursor protein

Kaur, Gurjinder; Pawlik, Monika; Gandy, Sam; Ehrlich, Michelle E.; Smiley, John F.; Levy, Efrat

doi:10.1038/mp.2016.189

Cited by 41 publications

(47 citation statements)

References 72 publications

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“…Genes involved in cellular aerobic respiration were not affected in the transcriptome of 12-month APPE-693Q mice but phagosomal system genes were predominantly up-regulated, possibly indicating an early compensatory mechanism to remove the excess of toxic proteins. Consistently, an age-dependent lysosomal dysfunction was recently described in the APP-E693Q mice, with a higher lysosomal count in the entorhinal cortex of the 12-month mice and autophagosomal/autolysosomal protein level increases only in 24-month old mice, leading to an inflammatory reaction and neuronal loss ( Kaur et al, 2017 ). In HCHWA-D, the lysosomal pathway was significantly down-regulated probably representing an end-stage state of the disease.…”

Section: Discussionsupporting

confidence: 63%

Brain Transcriptomic Analysis of Hereditary Cerebral Hemorrhage With Amyloidosis-Dutch Type

Moursel

Roon‐Mom

Kiełbasa

et al. 2018

Front. Aging Neurosci.

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Hereditary cerebral hemorrhage with amyloidosis-Dutch type (HCHWA-D) is an early onset hereditary form of cerebral amyloid angiopathy (CAA) caused by a point mutation resulting in an amino acid change (NP_000475.1:p.Glu693Gln) in the amyloid precursor protein (APP). Post-mortem frontal and occipital cortical brain tissue from nine patients and nine age-related controls was used for RNA sequencing to identify biological pathways affected in HCHWA-D. Although previous studies indicated that pathology is more severe in the occipital lobe in HCHWA-D compared to the frontal lobe, the current study showed similar changes in gene expression in frontal and occipital cortex and the two brain regions were pooled for further analysis. Significantly altered pathways were analyzed using gene set enrichment analysis (GSEA) on 2036 significantly differentially expressed genes. Main pathways over-represented by down-regulated genes were related to cellular aerobic respiration (including ATP synthesis and carbon metabolism) indicating a mitochondrial dysfunction. Principal up-regulated pathways were extracellular matrix (ECM)–receptor interaction and ECM proteoglycans in relation with an increase in the transforming growth factor beta (TGFβ) signaling pathway. Comparison with the publicly available dataset from pre-symptomatic APP-E693Q transgenic mice identified overlap for the ECM–receptor interaction pathway, indicating that ECM modification is an early disease specific pathomechanism.

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Section: Discussionsupporting

confidence: 63%

Brain Transcriptomic Analysis of Hereditary Cerebral Hemorrhage With Amyloidosis-Dutch Type

Moursel

Roon‐Mom

Kiełbasa

et al. 2018

Front. Aging Neurosci.

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“…and R.A.N., manuscript in preparation). APP-␤CTF has also been previously linked to lysosomal dysfunction in AD models involving overexpressed forms of FAD-mutated APP with or without additional overexpression of other mutated human AD genes (Lauritzen et al, 2012(Lauritzen et al, , 2016Yang et al, 2014;Kaur et al, 2017;Bourgeois et al, 2018), and in iPSC generated Ts21 neurons (Hung and Livesey, 2018). We discovered that luminal acidification of lysosomes is significantly impaired in DS and primarily responsible for disrupting lysosomal hydrolase activities and CTSD protein buildup.…”

Section: Discussionmentioning

confidence: 87%

“…Early neuronal accumulation of APP-␤CTF in AD mouse models is linked to neuronal hyperactivity (Goutagny et al, 2013), A␤independent LTP deficits and cognitive impairment (Simó n et al, 2009;Tamayev et al, 2011;Lauritzen et al, 2012;Mondragó n-Rodríguez et al, 2014), and cholinergic neurodegeneration (Jiang et al, 2016). Intraneuronal accumulation of APP-␤CTF is reported to be both a cause and effect of autophagy-lysosomal pathology and APP-␤CTF aggregate accumulation in 3xTg AD mice (APPswe, PS1 M146V , and Tau P301L ) (Lauritzen et al, 2012(Lauritzen et al, , 2016 and in several FAD-mutated APP overexpression models in mice (Yang et al, 2014;Kaur et al, 2017;Bourgeois et al, 2018), and in the neurons generated from induced pluripotent stem cells derived from individuals with PSEN1 as well as APP mutations (Hung and Livesey, 2018).…”

Section: Introductionmentioning

confidence: 99%

Lysosomal Dysfunction in Down Syndrome Is APP-Dependent and Mediated by APP-βCTF (C99)

et al. 2019

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Lysosomal failure underlies pathogenesis of numerous congenital neurodegenerative disorders and is an early and progressive feature of Alzheimer's disease (AD) pathogenesis. Here, we report that lysosomal dysfunction in Down ayndrome (trisomy 21), a neurodevelopmental disorder and form of early onset AD, requires the extra gene copy of amyloid precursor protein (APP) and is specifically mediated by the ␤ cleaved carboxy terminal fragment of APP (APP-␤CTF, C99). In primary fibroblasts from individuals with DS, lysosomal degradation of autophagic and endocytic substrates is selectively impaired, causing them to accumulate in enlarged autolysosomes/ lysosomes. Direct measurements of lysosomal pH uncovered a significant elevation (0.6 units) as a basis for slowed LC3 turnover and the inactivation of cathepsin D and other lysosomal hydrolases known to be unstable or less active when lysosomal pH is persistently elevated. Normalizing lysosome pH by delivering acidic nanoparticles to lysosomes ameliorated lysosomal deficits, whereas RNA sequencing analysis excluded a transcriptional contribution to hydrolase declines. Cortical neurons cultured from the Ts2 mouse model of DS exhibited lysosomal deficits similar to those in DS cells. Lowering APP expression with siRNA or BACE1 inhibition reversed cathepsin deficits in both fibroblasts and neurons. Deleting one Bace1 allele from adult Ts2 mice had similar rescue effects in vivo. The modest elevation of endogenous APP-␤CTF needed to disrupt lysosomal function in DS is relevant to sporadic AD where APP-␤CTF, but not APP, is also elevated. Our results extend evidence that impaired lysosomal acidification drives progressive lysosomal failure in multiple forms of AD.

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“…The initial cleavage of APP by β-secretase results in the secretion of the soluble ectodomain sAPPβ and the generation of a membrane-tethered C-terminal fragment C99 (or βCTF) that 2 of 17 is cleaved by γ-secretase to form Aβ. Increasing evidence indicates that Aβ accumulation is preceded by intraneuronal accumulation of C99, which contributes to AD pathology by affecting the endolysosomal network [2][3][4][5][6][7][8][9][10][11]. Firstly, in brain fibroblasts derived from Down's syndrome (DS) patients, a disorder in which patients develop an early form of AD likely due to a third copy of APP present on chromosome 21 [12], C99 accumulation was found to cause enlargement of Rab5-positive early endosomes [2][3][4].…”

Section: Introductionmentioning

confidence: 99%

The Transcription Factor EB Reduces the Intraneuronal Accumulation of the Beta-Secretase-Derived APP Fragment C99 in Cellular and Mouse Alzheimer’s Disease Models

Bécot

Pardossi‐Piquard

Bourgeois

et al. 2020

Cells

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: Brains that are affected by Alzheimer’s disease (AD) are characterized by the overload of extracellular amyloid β (Aβ) peptides, but recent data from cellular and animal models propose that Aβ deposition is preceded by intraneuronal accumulation of the direct precursor of Aβ, C99. These studies indicate that C99 accumulation firstly occurs within endosomal and lysosomal compartments and that it contributes to early-stage AD-related endosomal-lysosomal-autophagic defects. Our previous work also suggests that C99 accumulation itself could be a consequence of defective lysosomal-autophagic degradation. Thus, in the present study, we analyzed the influence of the overexpression of the transcription factor EB (TFEB), a master regulator of autophagy and lysosome biogenesis, on C99 accumulation occurring in both AD cellular models and in the triple-transgenic mouse model (3xTgAD). In the in vivo experiments, TFEB overexpression was induced via adeno-associated viruses (AAVs), which were injected either into the cerebral ventricles of newborn mice or administrated at later stages (3 months of age) by stereotaxic injection into the subiculum. In both cells and the 3xTgAD mouse model, exogenous TFEB strongly reduced C99 load and concomitantly increased the levels of many lysosomal and autophagic proteins, including cathepsins, key proteases involved in C99 degradation. Our data indicate that TFEB activation is a relevant strategy to prevent the accumulation of this early neurotoxic catabolite.

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Lysosomal dysfunction in the brain of a mouse model with intraneuronal accumulation of carboxyl terminal fragments of the amyloid precursor protein

Cited by 41 publications

References 72 publications

Brain Transcriptomic Analysis of Hereditary Cerebral Hemorrhage With Amyloidosis-Dutch Type

Brain Transcriptomic Analysis of Hereditary Cerebral Hemorrhage With Amyloidosis-Dutch Type

Lysosomal Dysfunction in Down Syndrome Is APP-Dependent and Mediated by APP-βCTF (C99)

The Transcription Factor EB Reduces the Intraneuronal Accumulation of the Beta-Secretase-Derived APP Fragment C99 in Cellular and Mouse Alzheimer’s Disease Models

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