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FLASH GENE

Symbol

PKD1

contributors: mct/shn/pgu - updated : 19-01-2021

HGNC name	polycystic kidney disease 1 (autosomal dominant)
HGNC id	9008

Corresponding disease

PKD	polycystic kidney disease 1
PKTS	polycystic kidney disease, infantile, severe, with tuberous sclerosis

Location

16p13.3 Physical location : 2.138.710 - 2.185.899

Synonym name

polycystin 1

polycystin-1

protein kinase C mu type

protein kinase D

transient receptor potential cation channel, subfamily P, member 1

autosomal dominant polycystic kidney disease 1 protein

polycystic kidney disease-associated protein

Synonym symbol(s)

PBP, PKD, PRKCM, nPKC-D1, nPKC-mu, PC1, Pc-1, TRPP1

EC.number

2.7.11.13

DNA

TYPE	functioning gene
SPECIAL FEATURE
text	with a duplicated portion
STRUCTURE	47.19 kb 46 Exon(s)

10 Kb 5' upstream gene genomic sequence study

regulatory sequence	Promoter
	Binding site transcription factor
text structure	transcription factor-binding sites, AP2, E2F, E-Box, EGRF, ETS, MINI, MZF1, SP1, and ZBP-89

MAPPING

cloned

linked

status

confirmed

Map

pter - D16S3024 - D16S3395 - PKD1 - D16S3124 - D16S3070 - cen

RNA

TRANSCRIPTS	type	messenger

identification	nb exons	type	bp	product
identification	nb exons	type	bp	Protein	kDa	AA	specific expression	Year	Pubmed
	46	-	14138		-	4303	-	2008	18422703
	46	-	14135		-	4302	-	2008	18422703

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		Homo sapiens
Nervous	brain				moderately		Homo sapiens

tissue

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

cells

System	Cell	Pubmed	Species	Stage	Rna symbol
Urinary	epithelial cell

cell lineage

cell lines

fluid/secretion

at STAGE

physiological period

fetal, pregnancy

cell cycle

cell cycle, checkpoint

Text

brain, kidney

PROTEIN

PHYSICAL PROPERTIES

STRUCTURE

motifs/domains	N-terminal region with an extracellular portion of >3000 amino acids, which is predicted to be a site of protein-protein or receptor-ligand interactions , 11 transmembrane spanning this extracellular region containing a number of adhesive domains
	a large extracellular segment, with (from NH2) two leucine rich repeats
	a homer-binding motif (PPxxF), which lies within its purported cytoplasmic domain
	a C-type lectin domain
	a LDL-A domain, 16 copies of a repeat
	the PKD domain with low homology to the Ig superfamily
	four type III fibronectin
	one REJ (receptor for egg jelly) domain
	one GPS domain (cleavage essential for the normal function)
	11 transmembrane domains (TM11)
	extracellular information across the plasma membrane
	a probable coiled-coil domain interacting with PKD2 and TSC2
	a cytoplasmic C-terminal tail (CTT), transmiting extracellular information across the plasma membrane, associating with beta-catenin and acting as an inhibitor of Wnt-dependent intracellular signaling (cleavage and release of CTT may be necessary components of a biological switch that acts to modulate Wnt-dependent signal transduction in renal epithelia), and can undergo proteolytic cleavage and nuclear translocation
	a conserved amino acid sequence, KVHPSST, in the C-terminus that serves as a ciliary-targeting signal , and
	interacts with numerous signaling molecules, including GNA12

conjugated

GlycoP

HOMOLOGY

interspecies	ortholog to Pkd1, Mus musculus
	ortholog to Pkd1, Rattus norvegicus
	ortholog to PKD1, Pan troglodytes

Homologene

FAMILY

polycystin family

CATEGORY

signaling , receptor membrane G , transport

SUBCELLULAR LOCALIZATION	plasma membrane,junction,desmosome
	intracellular
	intracellular,cytoplasm,organelle,Golgi
	intracellular,cytoplasm,cytoskeleton,microtubule,centrosome
	intracellular,cytoplasm,cytoskeleton,microfilament
text	localizes in cilia and has been observed in the centrosome of endothelial cells
	predicted to traverse the membrane 11 times and includes a massive extracellular amino terminal domain and a short intracellular carboxy terminal tail
	with PKD2, colocalize to cilia, where they may enable a mechano/chemosensory response triggering a rise in intracellular Ca2+

basic FUNCTION	may be functioning through a signaling pathway necessary for normal tubulogenesis and involved in adhesive protein-protein and protein-carbohydrate interactions
	involved in regulating ion transport required for the structural integrity of blood vessels
	maintaining cell adhesion, protein sorting and cell polarity (features disrupted in cystic epithelium)
	involved in chondrocyte development and in renal epithelium development
	mediating mechanosensation in the primary cilium of kidney cells
	acting as a regulator of G1 checkpoint, which controls entry into the S phase and prevents the replication of damaged DNA
	playing a role in preventing immortalized proliferation of renal tubular epithelial cells through the induction of TP53 and activation of MAPK8
	modulating renal tubular fluid and electrolyte transport
	having a central role in regulating morphogenic protein signaling at cell-matrix interfaces in non-confluent cells
	role in modulating cell proliferation through calcium oscillations in kidney cells
	regulates induction of cell death by wild-type PTRH2 following loss of cell attachment to the extracellular matrix
	one of the signaling molecules through which integrin-mediated cell attachment controls PTRH2 activity and anoikis
	acting as an upstream activating kinase that regulates the function of PTRH2 in anoikis by phosphorylating the Ser5 and Ser87 residues
	may play a role in regulating the stability of a pool of the beta-catenin protein
	tumor suppressive function that may be at least partially dependent upon the ability of the free CTT to inhibit beta-catenin-dependent Wnt signaling
	critical in both epithelium and chondrocyte development (
	regulates tubular morphology in both developing and adult kidney (
	can inhibit the mTOR pathway and regulate cell size
	phosphorylates SSH1 in response to RhoA activation and blocks it in the cytoplasm, consequently blocking the formation of free actin-filament barbed ends
	inhibits Ca2+ release, perhaps opposing the effect of PKD2, which facilitates Ca2+ release through the IP3R
	plays a novel role in the regulation of ITPR1 to modulate intracellular Ca2+ signaling
	may mediate the function of PRKX in kidney development
	involved in cell/cell/matrix interaction and the regulation of several signalling pathways linked to cell proliferation
	can both activate and coactivate multiple STATs, and STAT activation requires the membrane-anchored PC1 tail, whereas STAT coactivation requires the cleaved, soluble PKD1 tail
	plays an essential role in stereocilia structure and maintenance but not directly in mechanoelectrical transduction channel function or planar cell polarity (
	acts as a negative regulator of STAT3
	MTOR-mediated inhibition of PKD1 expression drives renal cyst formation in tuberous sclerosis complex
	PKD1, PKD2 form an ion channel complex that may mediate ciliary sensory processes and regulate endoplasmic reticulum (ER) Ca2+ release
	role for PKD1, PKD2 in sensing and responding to cellular O2 levels
	PKD1 is required to couple mechanical deflection of cilia to MTOR in tubular cells

CELLULAR PROCESS

cell communication

PHYSIOLOGICAL PROCESS

cardiovascular

text

ion

PATHWAY

metabolism

signaling

a component

heterodimerizing with PKD2, 3 PKD2 and 1 PKD1 (disruption of the complex PKD1/PKD2 is involved in the pathogenesis of cyst formation through a mechanosensor action in renal primary cilia for fluid flow)

INTERACTION

DNA

RNA

small molecule

protein	PKD2
	RGS7
	talin, vinculin, p130Cas, FAK, alpha-actinin, paxillin, pp60c-src, E-cadherin, beta- and gamma-catenin
	collagens type I, II and IV
	Cytokeratins K8 and K18, Vimentin, and desmin (
	extracellular matrix, ECM (
	Protein kinase-X (
	ITPR1 (
	interaction between the PKD1 polyproline motif and the NPHP1 SH3 domain
	STAT3 (
	binds a multimeric protein complex consisting of several GTPases (ARF4, RAB6, RAB11) and the GTPase-activating protein (GAP), ArfGAP with SH3 domain, ankyrin repeat and PH domain 1 (ASAP1) in the Golgi, which facilitates vesicle budding and Golgi exocytosis
	its cytoplasmic tail associates with the transcription factors TPX2 and STAT6
	PKD1, PKD2 are both required to amplify inositol-trisphosphate-induced Ca2+ release
	reciprocal functional link between PKD1 and PKD2 which is critically dependent on their interaction
	PKD1 function on JAK2 and ERK signaling pathways might be regulated by calpains in response to the changes in intracellular calcium concentration
	PKD1 interacts with BBS1, BBS4, BBS5 and BBS8, four of the seven components of the BBSome
	BBS3 and BBS1 regulate the ciliary trafficking of PKD1
	interaction of polycystin-1 (PKD1) and GNA12 is important for development of kidney cysts in autosomal dominant polycystic kidney disease (ADPKD)
	CDH1/CTNNB1 signaling pathway is regulated by PKD1 and GNA12 via ADAM10
	GNAT1, NPHP3, and PKD1 bind with high affinity to UNC119, whereas a peptide derived from a non-ciliary localizing protein (SRC) has low affinity
	PKD1 enhances the stability of CDH2 on cell membrane and promotes synapse morphogenesis and synaptic plasticity in an activity-dependent manner
	WWTR1 constitutes a key mechanistic link through which PKD1 mediates its physiological functions
	dual role for MYC, as a major contributor in PKD1-induced cystogenesis and in a feed-forward regulatory PKD1-MYC loop mechanism that may also prevail in human ADPKD

cell & other

REGULATION

Other	cleavage is modulated by PKD2 expression
	regilated by PKD2 (its expression is required for the movement of PKD1 to the plasma and ciliary membranes)

ASSOCIATED DISORDERS

corresponding disease(s)

PKTS , PKD

related resource

Polycystickidneyresearchfoundation

Other morbid association(s)

Type	Gene Modification	Protein expression
constitutional	somatic mutation
in PKD2 cysts (modification of disease severity)
constitutional		--low
in renal cysts
constitutional		--low
in aortic dissection

Susceptibility

Variant & Polymorphism

Candidate gene

Marker

Therapy target

PRKX can restore normal function to PKD1-deficient kidneys (

pyrimethamine or similar drugs may be an attractive therapy for human ADPKD

System	Type	Disorder	Pubmed
cancer	urinary
Treatment with pyrimethamine decreases cell proliferation in human ADPKD cells and blocks renal cyst formation in an adult and a neonatal PKD mouse model
cancer	urinary
a specific STAT3 inhibitor, S3I-201, reduces cyst formation and growth in a neonatal PKD mouse model

ANIMAL & CELL MODELS

	disruption of the PKD1 gene in mice leads to cystic kidneys and embryonic or perinatal death (
	Pkd1(del34) -/- and Pkd1(L) -/- mice have cysts but no cardiac abnormalities, although vascular fragility was reported in the latter (
	Pkd1(del17-21betageo) +/- adult mice develop renal and hepatic cysts, Pkd1(del17-21betageo) -/- embryos die at embryonic days 13.5-14.5 from a primary cardiovascular defect that includes double outflow right ventricle, disorganized myocardium, and abnormal atrio-ventricular septation, and skeletal development is also severely compromised (
	mice that overexpress polycystin-1 develop renal cysts (
	targeted mouse mutant with a homozygous null mutation in Pkd1 develop aggressive and severe renal and pancreatic cystic disease but also polyhydramnios, hydrops fetalis, spina bifida occulta and osteochondrodysplasia (
	targeted mouse mutant with a heterozygoous null mutation in Pkd1 develop adult-onset pancreatic disease (
	mouse with a homozygous targeted deletion of exons 2-6 of Pkd1 develop hydrops, cardiac conotruncal defects and renal cystogenesis (
	Pkd1(+/-), Pkd2 (+/-) and Pkd1(+/-) : Pkd2 (+/-) mice, the renal cystic lesion was mild and variable with no adverse effect on survival at 1 year (
	mouse model with a hypomorphic Pkd1 allele, Pkd1(nl), are viable, showing bilaterally enlarged polycystic, kidneys dilatations of pancreatic and liver bile ducts, and cardiovascular abnormalities (
	inactivation of Pkd1 in mice before postnatal day 13 results in severely cystic kidneys within 3 weeks, whereas inactivation at day 14 and later results in cysts only after 5 months (
	transgenic mice from a Pkd1-BAC modified by introducing a silent tag develop tubular and glomerular cysts leading to renal insufficiency, renal fibrosis and calcium deposits in papilla reminiscent of nephrolithiasis hepatic fibrosis and approximately 15% intrahepatic cysts of the bile ducts affecting females preferentially and a significant proportion of mice developed cardiac anomalies with severe left-ventricular hypertrophy, marked aortic arch distention and/or valvular stenosis and calcification (
	mouse models of PC-1, a knock-in (KI) mutant line and a hair cell-specific inducible Cre-mediated knock-out line exhibit normal mechanoelectrical transduction channel function at neonatal ages despite hearing loss and ultrastructural abnormalities of sterecilia that remain properly polarized at adult ages (
	treatment with pioglitazone improved survival of Pkd1(-/-) embryos and ameliorated the cardiac defects and the degree of renal cystogenesis (