APPL, the<b><i>Drosophila</i></b>Member of the APP-Family, Exhibits Differential Trafficking and Processing in CNS Neurons

Torroja, Laura; Luo, Liqun; White, K. Andrew

doi:10.1523/jneurosci.16-15-04638.1996

Cited by 55 publications

(61 citation statements)

References 62 publications

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“…were mouse anti-Armadillo (N27A1, 1:50, Iowa Hybridoma Bank), rat anti-elav (7E8A10, 1:500, Iowa Hybridoma Bank), rabbit anti-b-gal (1:1000, Sigma), mouse anti-GFP (1:200, Sigma), rat anti-Ci (2A1, 1:3), 38 rabbit anti-Cul1 (1:250, Zymed), rabbit anti-cleaved (activated) caspase 3 (1:50, Cell Signaling Technology), rabbit anti-phospho-histone H3 (1:500, Upstate Biotechnology), rabbit anti-APPL (Ab952, 1:500), 21 and mouse anti-Myc (1:200, Roche). Secondary antibodies coupled to the appropriate fluorophore (FITC, Cy3, or Cy5; Jackson Immunoresearch Laboratories) were diluted to 1:200 in wash solution.…”

Section: Methodsmentioning

confidence: 99%

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Drosophila homolog of APP-BP1 (dAPP-BP1) interacts antagonistically with APPL during Drosophila development

Kim

et al. 2006

Cell Death Differ

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b-Amyloid precursor protein binding protein 1 (APP-BP1) was previously identified based on its binding to the carboxyl terminal of b-amyloid precursor protein. In this report, we have discovered that a mutation of dAPP-BP1 (Drosophila ortholog of APP-BP1) hinders tissue development, causes apoptosis in imaginal disc cells, and blocks the NEDD8 conjugation pathway. We show that dAPP-BP1 specifically binds the intracellular domain of APP-like protein (APPL). The dAPP-BP1 mutation partially suppresses the abnormal macrochaete phenotype of Appl d , while overexpression of dAPP-BP1 causes abnormal macrochaetes. When APPL is overexpressed, the normal bristle pattern in the fly thorax is disturbed and apoptosis is induced in wing imaginal discs. APPL overexpression phenotypes are enhanced by reducing the level of dAPP-BP1. APPL overexpression is shown to inhibit the NEDD8 conjugation pathway. APPL-induced apoptosis is rescued by overexpression of dAPP-BP1. Our data suggest that APPL and dAPP-BP1 interact antagonistically during Drosophila development.

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Section: Methodsmentioning

confidence: 99%

“…20 Different forms of Drosophila APPL protein are enriched in different areas of the brain. 21 Deletion of the Appl gene does not cause obvious defects in adult brain morphology. 20 However, loss-and gain-of-function studies have revealed a role for APPL in synapse differentiation and axonal transport.…”

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confidence: 98%

Drosophila homolog of APP-BP1 (dAPP-BP1) interacts antagonistically with APPL during Drosophila development

Kim

et al. 2006

Cell Death Differ

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“…APP is expressed at relatively high levels in the central nervous system of diverse species (6,7). Multiple APP isoforms are derived from a single gene by alternative splicing (see Ref.…”

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confidence: 99%

Amyloid Protein Precursor Stimulates Excitatory Amino Acid Transport

Masliah¹,

Raber²,

Alford³

et al. 1998

Journal of Biological Chemistry

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Excitatory neurotransmitters such as glutamate are required for the normal functioning of the central nervous system but can trigger excitotoxic neuronal injury if allowed to accumulate to abnormally high levels. Their extracellular levels are controlled primarily by transmitter uptake into astrocytes. Here, we demonstrate that the amyloid protein precursor may participate in the regulation of this important process. The amyloid protein precursor has been well conserved through evolution, and a number of studies indicate that it may function as an endogenous excitoprotectant. However, the mechanisms underlying this neuroprotective capacity remain largely unknown. At moderate levels of expression, human amyloid protein precursors increased glutamate/aspartate uptake in brains of transgenic mice, with the 751-amino acid isoform showing greater potency than the 695-amino acid isoform. Cerebral glutamate/aspartate transporter protein levels were higher in transgenic mice than in non-transgenic controls, whereas transporter mRNA levels were unchanged. Amyloid protein precursor-dependent stimulation of aspartate uptake by cultured primary astrocytes was associated with increases in protein kinase A and C activity and could be blocked by inhibitors of these kinases. The stimulation of astroglial excitatory amino acid transport by amyloid protein precursors could protect the brain against excitotoxicity and may play an important role in neurotransmission.

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“…This indicates functional conservatism between Drosophila Appl and human АРР [Luo et al, 1992]. Many researches specify the key role of Appl in formation and maintenance of synapses in Drosophila [Ashley et al, 2005;Torroja et al, 1996]. Experiments by definition of Appl localization have shown significant Appl enrichment in growing axons and synaptic www.intechopen.com structures and participation of Appl in formation and differentiations of synapses in neuromuscular junctions of larvae [Torroja et al, 1996[Torroja et al, , 1999b.…”

Section: Drosophila Models Of Alzheimer's Amyloidosismentioning

confidence: 99%

“…Many researches specify the key role of Appl in formation and maintenance of synapses in Drosophila [Ashley et al, 2005;Torroja et al, 1996]. Experiments by definition of Appl localization have shown significant Appl enrichment in growing axons and synaptic www.intechopen.com structures and participation of Appl in formation and differentiations of synapses in neuromuscular junctions of larvae [Torroja et al, 1996[Torroja et al, , 1999b. The overexpression both Appl, and human АРР caused disturbance of axon transport [Gunawardena and Goldstein, 2001;Torroja et al, 1999a].…”

Section: Drosophila Models Of Alzheimer's Amyloidosismentioning

confidence: 99%