Post-translational Processing and Turnover Kinetics of Presynaptically Targeted Amyloid Precursor Superfamily Proteins in the Central Nervous System

Lyckman, Alvin W.; Confaloni, Annamaria; Wang, Shuai; Sisodia, Sangram S.; Moya, Kenneth L.

doi:10.1074/jbc.273.18.11100

Cited by 69 publications

(55 citation statements)

References 52 publications

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“…Hematoxyline counterstaining revealed the linearly distributed granules to be intraaxonal, indicating presence and transport of -sAPP in the axon. The normal presence of -sAPP in the axon is supported by several previous studies [22][23][24][25][26] and the axonally transported APP can be processed in the axolemma or the axon [28,29]. Newly synthesised APP is believed to be delivered to the synaptic terminal by fast anterograde axonal transport and then transported to the dendrites by a transcytotic mechanism [23].…”

Section: Discussionsupporting

confidence: 53%

β‐secretase‐cleaved amyloid precursor protein in Alzheimer brain: a morphologic study

Sennvik

Bogdanović

Volkmann

et al. 2004

J Cellular Molecular Medi

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Alzheimer's disease (AD) is characterised by the presence of intracellular neurofibrillary tangles (NFTs), neurofibrillary threads, extracellular amyloid plaques and accumulation of amyloid in cerebral blood vessels. The major component of the amyloid is a 39-43 amino acids peptide calledamyloid (A ). A derives from the amyloid precursor protein (APP), which is a widely expressed transmembrane protein [1]. Although the function of APP is not known, it has been proposed to have a role in regulation of neurite extension, synapse formation, neuronal development and neuroprotection [2][3][4].A is produced from APP via proteolytic cleavage by proteases called -and -secretase. Abstract-amyloid (A ) is the main constituent of senile plaques seen in Alzheimer's disease. A is derived from the amyloid precursor protein (APP) via proteolytic cleavage by proteases -and -secretase. In this study, we examined content and localization of -secretase-cleaved APP ( -sAPP) in brain tissue sections from the frontal, temporal and occipital lobe. Strong granular -sAPP staining was found throughout the gray matter of all three areas, while white matter staining was considerably weaker. -sAPP was found to be localized in astrocytes and in axons. We found the -sAPP immunostaining to be stronger and more extensive in gray matter in Alzheimer disease (AD) cases than controls. The axonal -sAPP staining was patchy and unevenly distributed for the AD cases, indicating impaired axonal transport. -sAPP was also found surrounding senile plaques and cerebral blood vessels. The results presented here show altered -sAPP staining in the AD brain, suggestive of abnormal processing and transport of APP.

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Section: Discussionsupporting

confidence: 53%

β‐secretase‐cleaved amyloid precursor protein in Alzheimer brain: a morphologic study

Sennvik

Bogdanović

Volkmann

et al. 2004

J Cellular Molecular Medi

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“…We have shown that the 2z tag does not alter the proteolytic processing of APP but stabilizes its C-terminal fragments and enhances their detection (23). This method has enabled the detection of a novel ⑀-cleavage site of APP at the C-terminal end of the transmembrane domain, between Leu 49 and Val 50 (23). Thus, the 2z tag was fused to the C termini of APLP-1 and APLP-2-763, and these constructs, which we termed APLP-1-2z and APLP-2-2z, respectively, were overexpressed in SH-SY5Y cells.…”

Section: Detection Of the C-terminal Fragments Of App695 Aplp-1 Andmentioning

confidence: 99%

“…An additional cleavage within the APP ectodomain at position Ϫ12 (relative to A␤), which was termed ␦-cleavage, has only been observed in hippocampal neurons so far (22). Recently, we and others have identified a presenilindependent cleavage at the C-terminal end of the APP transmembrane domain between Leu 49 and Val 50 , which we termed ⑀-cleavage (23)(24)(25)(26), that is homologous to the S3 cleavage of Notch (27,28). The exact mechanism of the two presenilin-dependent ␥-and ⑀-cleavages within the transmembrane domain of APP remains unclear.…”

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confidence: 99%

The Proteolytic Processing of the Amyloid Precursor Protein Gene Family Members APLP-1 and APLP-2 Involves α-, β-, γ-, and ϵ-Like Cleavages

Eggert

Paliga

Soba

et al. 2004

Journal of Biological Chemistry

199

189

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Amyloid precursor protein (APP) processing is of major interest in Alzheimer's disease research, since sequential cleavages by ␤-and ␥-secretase lead to the formation of the 4-kDa amyloid A␤ protein peptide that accumulates in Alzheimer's disease brain. The processing of APP involves proteolytic conversion by different secretases leading to ␣-, ␤-, ␥-, ␦-, and ⑀-cleavages. Since modulation of these cleavages represents a rational therapeutic approach to control amyloid formation, its interference with the processing of the members of the APP gene family is of considerable importance. By using C-terminally tagged constructs of APLP-1 and APLP-2 and the untagged proteins, we have characterized their proteolytic C-terminal fragments produced in stably transfected SH-SY5Y cells. Pharmacological manipulation with specific protease inhibitors revealed that both homologues are processed by ␣-and ␥-secretase-like cleavages, and that their intracellular domains can be released by cleavage at ⑀-sites. APLP-2 processing appears to be the most elaborate and to involve alternative cleavage sites. We show that APLP-1 is the only member of the APP gene family for which processing can be influenced by N-glycosylation. Additionally, we were able to detect p3-like fragments of APLP-1 and p3-like and A␤-like fragments of APLP-2 in the media of stably transfected SH-SY5Y cells.

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“…APP operates in a cell autonomous fashion to mediate axonal pruning in the adult after changes in sensory input, similar to its cell autonomous role in sensory neuron and retinal axon pruning (8,29). Previous work demonstrates that APP is expressed both pre-and postsynaptically (13)(14)(15)(16)(17)(18) and is present in growth cones (30,31). Furthermore, the E1 portion of the APP protein plays a role in cell adhesion (27).…”

Section: Discussionmentioning

confidence: 99%

Physiological role for amyloid precursor protein in adult experience-dependent plasticity

Marik

Olsen

Tessier‐Lavigne

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

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Changes in neural circuits after experience-dependent plasticity are brought about by the formation of new circuits via axonal growth and pruning. Here, using a combination of electrophysiology, adeno-associated virus-delivered fluorescent proteins, analysis of mutant mice, and two-photon microscopy, we follow long-range horizontally projecting axons in primary somatosensory cortex before and after selective whisker plucking. Whisker plucking induces axonal growth and pruning of horizontal projecting axons from neurons located in the surrounding intact whisker representations. We report that amyloid precursor protein is crucial for axonal pruning and contributes in a cell autonomous way.axon pruning | long-range axons | amyloid precursor protein | somatosensory cortex | experience-dependent plasticity A lterations in sensory experience lead to substantial modifications in cortical circuits. This plasticity is mediated, in part, through changes in the strength of synaptic transmission, but can also involve massive anatomical changes that include the sprouting of new axon collaterals, pruning of existing collaterals (1-3), and turnover of synapses along stable axons. After sensory loss, the cortical topography of the sensory map is permanently altered within the lesion projection zone (LPZ), the area of the cortex that receives input from the deafferented part of the periphery (4). Initially, the LPZ is silenced, but it subsequently recovers sensory input by the sprouting of afferents originating from nondeprived regions of the sensory periphery. This culminates in the reorganization of the cortical topographic map (4, 5). We have previously demonstrated that this reorganization of the cortical map is mediated through anatomical changes in horizontally projecting axons of layer II/III neurons within and around the LPZ (1-3). Electrophysiological changes occur along the same temporal scale (4, 5).Axonal changes associated with adult cortical plasticity are seen for both excitatory neurons, which send enriched projections into the LPZ, and inhibitory neurons located within the LPZ, which send reciprocal connections outside the LPZ (1-3). Previously, we demonstrated that axonal pruning after sensory deprivation (e.g., selective whisker plucking) requires death receptor 6 (DR6) (6). DR6 interacts with the E2 domain of amyloid precursor protein (APP) (7,8), and together, these proteins initiate an apoptotic cascade that mediates axon pruning in the absence of cell body death during development (8-10). It remains to be determined whether DR6-mediated pruning of axons after sensory deprivation in the adult may also involve APP.APP is best known for its role in Alzheimer's disease, where proteolytic cleavage of APP by beta-and gamma-secretases liberates Aβ (11), which impairs synaptic plasticity (12) and is thought to induce neuronal cell death. However, the physiological roles for APP are slowly coming into focus. Under normal conditions, APP is present on both sides of the synapse (13-18). APP −/− mice show performance ...

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Post-translational Processing and Turnover Kinetics of Presynaptically Targeted Amyloid Precursor Superfamily Proteins in the Central Nervous System

Cited by 69 publications

References 52 publications

β‐secretase‐cleaved amyloid precursor protein in Alzheimer brain: a morphologic study

β‐secretase‐cleaved amyloid precursor protein in Alzheimer brain: a morphologic study

The Proteolytic Processing of the Amyloid Precursor Protein Gene Family Members APLP-1 and APLP-2 Involves α-, β-, γ-, and ϵ-Like Cleavages

Physiological role for amyloid precursor protein in adult experience-dependent plasticity

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