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FLASH GENE

Symbol

NIPA1

contributors: npt/mct/shn - updated : 21-10-2013

HGNC name	non-imprinted in Prader-Willi/Angelman syndrome 1
HGNC id	17043

FLASH GENE DNA RNA EXPRESSION PROTEIN DISORDER ANIMAL & CELL MODELS

Corresponding disease	SPG6 spastic paraplegia 6
Location	15q11.2      Physical location : 23.043.280 - 23.086.843
Synonym name	spastic paraplegia 6 (autosomal dominant)
	magnesium transporter NIPA1
	non-imprinted in Prader-Willi/Angelman syndrome 1
	non-imprinted in Prader-Willi/Angelman syndrome region protein 1
	spastic paraplegia 6 protein
Synonym symbol(s)	FSP3, MGC35570, MGC102724, SPG6

DNA

TYPE	functioning gene
SPECIAL FEATURE	arranged in tandem
text	located in tandem with NIPA2 on chromosome 15q
STRUCTURE	43.16 kb     5 Exon(s)

MAPPING

cloned

Y

linked

N

status

provisional

Map	cen - D15S1035 - NIPA1 - D15S646 - D15S817 - qter

regionally located

located between BP1 and BP2 in the WPS/AS critical region

RNA

TRANSCRIPTS	type	messenger

identification nb exons type bp product Protein kDa AA specific expression Year Pubmed NM_001142275 5 - 6386 NP_001135747 27.3 254 - - NM_144599 5 splicing 6565 NP_653200 34.6 329 - -

EXPRESSION

Type

widely

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       lowly Homo sapiens Adult Digestive liver       moderately Homo sapiens Adult Endocrine pancreas       moderately Homo sapiens Adult Nervous brain       highly Homo sapiens Adult   brain forebrain cerebral lobe temporal lobe highly Homo sapiens Adult   brain forebrain cerebral lobe frontal lobe highly Homo sapiens Adult   brain forebrain cerebral lobe occipital lobe highly Homo sapiens Adult   brain hindbrain medulla oblongata   highly Homo sapiens Adult   brain forebrain cerebral cortex   highly Homo sapiens Adult   brain hindbrain cerebellum   highly Homo sapiens Adult   brain basal nuclei putamen   highly Homo sapiens Adult   spinal cord       moderately Homo sapiens Adult Reproductive female system placenta     moderately Homo sapiens Adult Respiratory lung       moderately Homo sapiens Adult Urinary kidney       moderately Homo sapiens Adult

tissue

System Tissue Tissue level 1 Tissue level 2 Level Pubmed Species Stage Rna symbol Muscular striatum skeletal   moderately Homo sapiens Adult

cell lineage

cell lines

fluid/secretion

at STAGE

physiological period

fetal

Text	expressed in fetal heart

PROTEIN

PHYSICAL PROPERTIES

STRUCTURE

motifs/domains	two polyadenylation signals
	nine predicted transmembrane domains

HOMOLOGY

interspecies	ortholog to Nipa1, Mus musculus
	ortholog to Nipa1, Rattus norvegicus
	ortholog to nipa1, Danio rerio
	ortholog to NIPA1, Pan troglodytes

Homologene

FAMILY

NIPA family

CATEGORY

receptor

SUBCELLULAR LOCALIZATION	intracellular
	intracellular,cytoplasm,organelle,membrane
	intracellular,cytoplasm,organelle,endoplasmic reticulum
	intracellular,cytoplasm,organelle,endosome
text	accumulation at the peripheral membrane in response to changes in magnesium
	localize to the endosomal membrane traffic compartment, suggesting that the long axons of the corticospinal tract may be especially vulnerable to endosomal dysfunction (Tsang 2009)

basic FUNCTION	playing a role in nervous system development and maintenance
	mediating Mg2+ transport and regulated by magnesium, indicating that it may play a role in control of cellular magnesium homeostasis
	inhibitor of BMP signalling in neuronal and non-neuronal cells (Tsang 2009)
	important role of NIPA1 in ALS pathogenesis and as a modulator of disease progression

CELLULAR PROCESS

PHYSIOLOGICAL PROCESS

PATHWAY

metabolism

signaling

a component

INTERACTION

DNA

RNA

small molecule

protein

interacts with the type II BMP receptor (BMPR2) and promotes its degradation through endocytosis and lysosomal degradation

cell & other

REGULATION

ASSOCIATED DISORDERS

corresponding disease(s)

SPG6

Other morbid association(s)

Type Gene Modification Chromosome rearrangement Protein expression Protein Function constitutional   deletion     in congenital heart disease constitutional       loss of function mutations or NIPA1 polyalanine expansions may result in defects in synapse and axon development

Susceptibility

Variant & Polymorphism

Candidate gene

Marker

Therapy target

ANIMAL & CELL MODELS

transgenic rats expressing a human NIPA1/SPG6 mutation in neurons show marked early onset behavioral and electrophysiologic abnormalities, accumulation of tubulovesicular organelles with endosomal features that start at axonal and dendritic terminals, followed by multifocal vacuolar degeneration in both the central nervous system and peripheral nerves