Genatlas sheet

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FLASH GENE

Symbol

APP

contributors: shn - updated : 05-12-2019

HGNC name	amyloid beta (A4) precursor protein
HGNC id	620

EXPRESSION

Type

ubiquitous

expressed in

(based on citations)

organ(s)

System	Organ level 1	Organ level 2	Organ level 3	Organ level 4	Level	Pubmed	Species	Stage	Rna symbol
Cardiovascular	heart				moderately
Digestive	mouth	tongue			highly
	stomach				moderately
Endocrine	pancreas				moderately
Reproductive	female system	breast	mammary gland		highly
Urinary	kidney				moderately
Visual	eye				moderately

tissue

System	Tissue	Tissue level 1	Tissue level 2	Level	Pubmed	Species	Stage	Rna symbol
Nervous	peripherous

cells

System	Cell	Pubmed	Species	Stage	Rna symbol
Nervous	neuron

cell lineage

cell lines

fluid/secretion

at STAGE

PROTEIN

PHYSICAL PROPERTIES

STRUCTURE

motifs/domains	a large extracellular N terminal domain
	a serum protease inhibitor-like motif, Kunitz type
	a single transmembrane pass
	a REXXE ferroxidase consensus motif (its ferroxidase activity of is unique among its protein family and, like ferritin, correlates with the presence of the mRNA IRE motif, which is not present in APLP1 and APLP2)
	a short cytoplasmic tail, containing a 15 AA juxtamembrane segment with a single tyrosine forming the basolateral sorting signal (see APPBP2)

conjugated

GlycoP , MetalloP

mono polymer

homomer , heteromer , dimer

isoforms

Precursor

of beta-amyloid peptide

HOMOLOGY

interspecies	ortholog to APP, pan troglodytes
	ortholog to App, Mus musculus
	ortholog to App, Rattus norvegicus

Homologene

FAMILY

APP family

CATEGORY

enzyme

SUBCELLULAR LOCALIZATION	extracellular
	plasma membrane
	intracellular
	intracellular,cytoplasm,organelle,Golgi
	intracellular,cytoplasm,organelle,endosome
text	type I integral membrane protein
	localizes to the nuclear periphery
	UBQLN1 can sequester APP in the Golgi apparatus and delay its access to the cell surface and subsequent proteolytic processing
	LRRTM3 co-localizes with both APP and BACE1 in early endosomes, where BACE1 processing of APP occurs

basic FUNCTION	undergoing proteolytic cleavages by either alpha, beta or gamma secretases in or near the transmembrane domain
	to yield several secreted derivatives, including soluble APP(4kDa) beta peptide (A beta) and a related (4 kDa) protein
	serine protease inhibitor, inhibiting gelatinase A activity
	playing a significant role in regulating cerebral thrombosis and increases can profoundly enhance cerebral hemorrhage
	modulating negatively neurogenesis through APBB1 in the CNTN2-APP signalling pathway
	primary targets of beta-amyloids is suppression of mitochondrial succinate dehydrogenase, and the vulnerability of the brain of beta-amyloids can be explained by its large dependence on mitochondrial energy production (Kaneko 1995)
	functions as a kinesin-I membrane receptor, mediating the axonal transport of beta-secretase and presenilin-1 (Kamal 2001)
	co-localizes with proteins that define the splicing factor compartment (SFC) and may play a role in pre-mRNA splicing (Muresan 2004)
	has a key role in the pathological process of Alzheimer's disease (AD) and in regulation of cholesterol and sphingomyelin metabolism (Grimm 2005)
	important role for proteolysis in determining the levels of APP and APP-associated neuropathology, supporting the hypothesis that primary defects in APP clearance can cause or contribute to late-onset form of Alzheimer disease (LOAD) pathogenesis
	APP and death receptor 6 (DR6, also known as TNFRSF21) activate a widespread caspase-dependent of a neuronal self-destruction pathway program (Nikolaev 2009)
	plays an important role in preventing iron-mediated oxidative stress through separate domains: an HO-inhibitory domain that prevents the release of Fe2+ from heme and, here, a separate ferroxidase domain
	some neurotrophic properties of APP and its fragments could be mediated by iron regulation
	capable of forming a homodimer through its extracellular domain as well as transmembrane GXXXG motifs

CELLULAR PROCESS	cell life, cell death/apoptosis
	nucleotide, RNA splicing

PHYSIOLOGICAL PROCESS

development

text

neurogenesis

PATHWAY

metabolism

lipid/lipoprotein

signaling

CENTA1-RAS-ELK1 signaling pathway acts on mitochondria to regulate dendritic spine density and synaptic plasticity in response to APP in hippocampal neurons

a component	complexing with AABP1 and histone acetyltransferase (Tip60)
	APP/APBB1/LRP1 complex is an important mediator of APP processing and affects beta-amyloid peptide production
	modulation of APP dimerization state could be one of mechanisms, which links synaptic contact and Abeta production

INTERACTION

DNA

RNA

small molecule	metal binding,
	copper Cu2+ (reducing)

protein	gamma secretase putatively (PSEN1 and PSEN2) to cleavage of APP in Abeta 42 with deposition in brain (fibrillar myeloid plaques to cause neurodegeneration)
	APBB1, via its C-ter region (LRP2 interacts with APP and APBB1 in neurons
	sortilin-related receptor, L(DLR class) A repeats-containing (SORL1)
	APP and APLP bind to heme oxygenase (HO) and inhibit HO activity
	amyloid beta (A4) precursor protein-binding, family B, member 1 (Fe65)
	forms a multimeric complex with the nuclear adaptor protein Fe65 and the histone acetyltransferase Tip60
	amyloid beta (A4) precursor protein-binding, family A, member 1 (APBA1)
	amyloid beta (A4) precursor protein-binding, family A, member 2 (ABPA2)
	amyloid beta (A4) precursor protein-binding, family A, member 3 (APBA3)
	amyloid beta (A4) precursor protein-binding, family B, member 2 (APBB2)
	amyloid beta (A4) precursor protein-binding, family B, member 3 (APBB3)
	acetylcholinesterase (AChE)
	protein interacting with APP tail 1 (PAT1)
	heparan sulfate proteoglycan 2 (HSPG2)
	Human bleomycin hydrolase (hBH)
	Disruption of the disabled-1 gene (Dab1)
	fibulin 1 (FBLN1)
	Calreticulin (CALR)
	glyceraldehyde-3-phosphate dehydrogenase (GAPDH)
	growth factor receptor-bound protein 2 (GRB2)
	SHC (Src homology 2 domain containing) transforming protein 1 (SHC1)
	gelsolin (GSN)
	intracellular amyloid beta-peptide (A beta) binding protein (ERAB)
	kinesin-I
	kininogen 1 (KING1)
	low density lipoprotein (LDL) receptor-related protein 1B (LRP1B)
	Jun NH2-terminal kinase (JNK) interacting protein 1 (JIP1)
	59-kDa APP-binding protein, called APP-BP1
	nicastrin (NCSTN)
	Notch inhibitors Numb and Numb-like in mouse brain
	alpha 1-antichymotrypsin (ACT)
	synuclein, alpha (non A4 component of amyloid precursor) (SNCA)
	spondin 1, extracellular matrix protein (SPON1)
	Transforming growth factor-beta (TGF-beta)
	TM2 domain containing 1 (TM2D1)
	mitogen-activated protein kinase 8 interacting protein 1 (MAPK8IP1 aslo known as JIP-1)
	presenilin 1 (PS1) and presenilin 2 (PS2)
	human serine protease HtrA2/Omi
	death receptor 6 (DR6)
	alpha7 nicotinic acetylcholine receptor (alpha7nAChR)
	cell death mediator p75(NTR)
	microtubule-associated protein tau (MAPT)
	have major interactions with ferroportin to facilitate iron export from certain cells including neurons
	NSG1 profoundly affects the processing of APP production
	GAS1 negatively regulated APP intracellular trafficking
	GULP1-APP interaction is mediated by the NPTY motif of APP and the GULP1 PTB (phosphotyrosine-binding) domain (
	CDH2 expression facilitates cis-dimerization of APP (
	interaction between APP and neuroligin-1 (NLGN1), increasing the formation of APP oligomers, and suggesting that this interaction could triggers the targeting of APP oligomer to the postsynaptic regions of excitatory synapses
	mechanistic link between APOE-regulated cholesterol homeostasis and APP degradation
	HAP1 regulates APP subcellular trafficking to the non-amyloidogenic pathway and may negatively regulate APP production in neurons
	APP-activated NFATC3 proteins were associated with astrocytic BACE1 gene expression via direct interaction with the BACE1 promoter region
	UBQLN1 inhibits the maturation of APP by sequestering it in the early secretory pathway, primarily within the Golgi apparatus
	APP endocytic trafficking to lysosomes for degradation is a major APP clearance pathway that is differentially regulated by APOE isoforms
	APBB1 might have signalling properties together with APP and LRP1
	APOE influences soluble APP metabolism not through direct binding to soluble APP in solution but through its actions with other interacting receptors/transporters and cell surfaces
	is able to affect the downstream effects of protease inhibition in neural cells including enhancement of CTSB activity, with these changes in CTSB significantly and inversely related to the levels of ubiquitinated protein
	interacts with MAP1LC3B via OPTN/optineurin and is degraded by an autophagic process mediated by the PRKAA1 pathway
	APP-stimulated neuronal differentiation of neural stem/progenitor cells (NSPCs) is mediated by NEUROG2
	APP enhances SCN8A sodium channel cell surface expression through a Go-coupled JNK pathway
	WASF1 interacts and colocalizes with APP in the Golgi apparatus
	APP,is a novel interaction partner of PIKFYVE (furthermore, it has been shown that APP modulates PIKFYVE function and PI(3,5)P2 dynamics)
	SEPTIN8 modulates likely bta-amyloidogenic processing of APP through a mechanism affecting the intracellular sorting and accumulation of BACE1
	EGR1 promotes APP synthesis via transcriptional activation of BACE1, suggesting that EGR1 plays role in activation of BACE1 and acceleration of APP synthesis in Alzheimer disease brain
	GKN1 directly interacted with APP C-terminal fragments, C83 and C99
	novel role for SORL1 as a physiological and pathological EPHA4 modulator, which attenuates synaptotoxic EPHA4 activation and cognitive impairment associated with APP-induced neurodegeneration in Alzheimer disease
	GNB5 and VPS35 showed direct interactions with the APP gene, a hallmark genetic risk factor for Alzheimer disease

cell & other

REGULATION

induced by

cellular uptake and degradation by LRP1

inhibited by	entactin
	Zn2+ in Alzheimer disease tissue

Phosphorylated by

by NTRK1 and regulates NGF/NTRK1 signaling

Other	cleaved at the cell surface and released as a soluble APP
	PS1 that regulates the gamma-secretase proteolysis of the amyloid precursor protein (APP)
	prolyl isomerase Pin1 regulates amyloid precursor protein processing and amyloid-beta production
	JIP1b can directly modulate APP metabolism by interacting with the APP cytoplasmic domain

ASSOCIATED DISORDERS

corresponding disease(s)

AD1 , HCHWAD

related resource

Alzheimer Disease Mutation Database

Other morbid association(s)

Type	Protein expression	Protein Function
constitutional	--over
in cerebral hemorrhage due to congophilic amyloid angiopathy (CAA) with periventricular and subcortical white matter lesions at young age
constitutional	--low
in autism with duplicated UBE3A
constitutional		loss of function
inhibition of APP ferroxidase activity may contribute to neuronal iron accumulation in Alzheimer cortex, and elevated brain iron is a complication of aging
constitutional	--other
in FRA X fibroblasts, a dual dysregulation of APP and ADAM10 leads to the production of an excess of soluble APPalpha and to synaptic and behavioral deficits

Susceptibility

to schizophrenia

to Alzheimer disease

Variant & Polymorphism other	mutation APP692
	APP-promoter mutations that significantly increase APP expression levels are associated with AD
	association between rs463946 (-3102 G/C) and AD
	mutation (A673T) in the APP gene that protects against Alzheimer disease and cognitive decline in the elderly without Alzheimer disease

Candidate gene

Marker

Therapy target

System	Type	Disorder	Pubmed
neurology	neurodegenerative	alzheimer
postmenopausal estrogen (17beta-estradiol) replacement therapy may prevent or delay the onset of AD

ANIMAL & CELL MODELS

	transgenic mouse models expressing human Alzheimer's A beta peptide exhibit brain regions severely affected in Alzheimer's disease resulting in extensive neuronal degeneration (LaFerla 1995)
	double mutant (tau/APP) mice exhibited neurofibrillary tangle pathology substantially enhanced in the limbic system and olfactory cortex (Lewis 2001)
	co-expression of both mutant transgenes presenilin 1 and APP results in acceleration of amyloid accumulation and associative learning deficits (Dineley 2002)
	expression of human Abeta42 peptide in the Drosophila brain led to the formation of diffused amyloid deposits, age-dependent learning defects, and extensive neurodegeneration and Abeta40 caused only age-dependent learning defects (Iijima 2004)
	FVB/N mice overexpressing human APP695 develop a central nervous system disorder and die prematurely, precluding development of Abeta peptide amyloid plaques whereas 129S6 mice are resistant to the lethal effects of APP overexpression (Krezowski 2004)
	gene expression analysis revealed that the genes related to mitochondrial energy metabolism and apoptosis were up-regulated in 2-month-old Tg2576 mouse AD model and that the same genes were up-regulated at 5 and 18 months of age suggesting that mitochondrial energy metabolism is impaired by the expression of mutant APP and/or Abeta, and that the up-regulation of mitochondrial genes is a compensatory response (Reddy 2004)
	estrogen-deficient APP23 mice exhibited greatly reduced brain estrogen, early-onset and increased beta amyloid peptide (Abeta) deposition and increased Abeta production (Yue 2005)
	memory deficits in middle-aged Tg2576 mice are caused by the extracellular accumulation of a 56-kDa soluble amyloid-beta assembly suggesting that Abeta*56 impairs memory independently of plaques or neuronal loss, and may contribute to cognitive deficits associated with Alzheimer's disease (Lesné 2006)
	Lack of NO synthase 2 in the amyloid precursor protein Swedish mutant mouse increased insoluble beta-amyloid peptide levels, neuronal degeneration, caspase-3 activation, and tau cleavage (Colton 2006)
	Alzheimer disease mice deficient in Ccr2 accumulated Abeta earlier and died prematurely. Ccr2 deficiency accelerates early disease progression and markedly impairs microglial accumulation (El Khoury 2007)