UniProtKB - Q14654 (KCJ11_HUMAN)
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Protein
ATP-sensitive inward rectifier potassium channel 11
Gene
KCNJ11
Organism
Homo sapiens (Human)
Status
Functioni
This receptor is controlled by G proteins. Inward rectifier potassium channels are characterized by a greater tendency to allow potassium to flow into the cell rather than out of it. Their voltage dependence is regulated by the concentration of extracellular potassium; as external potassium is raised, the voltage range of the channel opening shifts to more positive voltages. The inward rectification is mainly due to the blockage of outward current by internal magnesium. Can be blocked by extracellular barium (By similarity). Subunit of ATP-sensitive potassium channels (KATP). Can form cardiac and smooth muscle-type KATP channels with ABCC9. KCNJ11 forms the channel pore while ABCC9 is required for activation and regulation.By similarity2 Publications
Sites
| Feature key | Position(s) | DescriptionActions | Graphical view | Length |
|---|---|---|---|---|
| Sitei | 160 | Role in the control of polyamine-mediated channel gating and in the blocking by intracellular magnesiumBy similarity | 1 |
GO - Molecular functioni
- ankyrin binding Source: BHF-UCL
- ATP-activated inward rectifier potassium channel activity Source: BHF-UCL
- ATP binding Source: BHF-UCL
- heat shock protein binding Source: Ensembl
- ion channel binding Source: BHF-UCL
- potassium ion binding Source: BHF-UCL
- protein C-terminus binding Source: Ensembl
- voltage-gated potassium channel activity Source: BHF-UCL
GO - Biological processi
- cellular response to glucose stimulus Source: Ensembl
- cellular response to nicotine Source: Ensembl
- cellular response to tumor necrosis factor Source: Ensembl
- glucose metabolic process Source: BHF-UCL
- negative regulation of insulin secretion Source: BHF-UCL
- neurological system process Source: BHF-UCL
- positive regulation of cation channel activity Source: Ensembl
- positive regulation of protein targeting to plasma membrane Source: Ensembl
- potassium ion import Source: BHF-UCL
- potassium ion transmembrane transport Source: BHF-UCL
- regulation of cardiac conduction Source: Reactome
- regulation of insulin secretion Source: BHF-UCL
- regulation of membrane potential Source: BHF-UCL
- response to ATP Source: BHF-UCL
- response to drug Source: BHF-UCL
- response to estradiol Source: Ensembl
- response to ischemia Source: Ensembl
- response to testosterone Source: Ensembl
- transmembrane transport Source: Reactome
Keywordsi
| Molecular function | Ion channel, Voltage-gated channel |
| Biological process | Ion transport, Potassium transport, Transport |
| Ligand | Potassium |
Enzyme and pathway databases
| Reactomei | R-HSA-1296025. ATP sensitive Potassium channels. R-HSA-382556. ABC-family proteins mediated transport. R-HSA-422356. Regulation of insulin secretion. R-HSA-5578775. Ion homeostasis. R-HSA-5683177. Defective ABCC8 can cause hypoglycemias and hyperglycemias. |
| SignaLinki | Q14654. |
| SIGNORi | Q14654. |
Protein family/group databases
| TCDBi | 1.A.2.1.17. inward rectifier k(+) channel (irk-c) family. |
Names & Taxonomyi
| Protein namesi | Recommended name: ATP-sensitive inward rectifier potassium channel 11Alternative name(s): IKATP Inward rectifier K(+) channel Kir6.2 Potassium channel, inwardly rectifying subfamily J member 11 |
| Gene namesi | Name:KCNJ11 |
| Organismi | Homo sapiens (Human) |
| Taxonomic identifieri | 9606 [NCBI] |
| Taxonomic lineagei | Eukaryota › Metazoa › Chordata › Craniata › Vertebrata › Euteleostomi › Mammalia › Eutheria › Euarchontoglires › Primates › Haplorrhini › Catarrhini › Hominidae › Homo |
| Proteomesi |
|
Organism-specific databases
| HGNCi | HGNC:6257. KCNJ11. |
Subcellular locationi
Topology
| Feature key | Position(s) | DescriptionActions | Graphical view | Length |
|---|---|---|---|---|
| Topological domaini | 1 – 68 | CytoplasmicBy similarityAdd BLAST | 68 | |
| Transmembranei | 69 – 93 | Helical; Name=M1By similarityAdd BLAST | 25 | |
| Topological domaini | 94 – 116 | ExtracellularBy similarityAdd BLAST | 23 | |
| Intramembranei | 117 – 128 | Helical; Pore-forming; Name=H5By similarityAdd BLAST | 12 | |
| Intramembranei | 129 – 135 | Pore-formingBy similarity | 7 | |
| Topological domaini | 136 – 144 | ExtracellularBy similarity | 9 | |
| Transmembranei | 145 – 166 | Helical; Name=M2By similarityAdd BLAST | 22 | |
| Topological domaini | 167 – 390 | CytoplasmicBy similarityAdd BLAST | 224 |
GO - Cellular componenti
- acrosomal vesicle Source: Ensembl
- ATP-sensitive potassium channel complex Source: BHF-UCL
- axolemma Source: Ensembl
- cell body fiber Source: Ensembl
- cytosol Source: Ensembl
- endoplasmic reticulum Source: Ensembl
- endosome Source: Ensembl
- integral component of plasma membrane Source: ProtInc
- intercalated disc Source: Ensembl
- mitochondrion Source: Ensembl
- myelin sheath Source: Ensembl
- neuronal cell body Source: Ensembl
- nuclear envelope Source: Ensembl
- plasma membrane Source: BHF-UCL
- T-tubule Source: BHF-UCL
- voltage-gated potassium channel complex Source: BHF-UCL
Keywords - Cellular componenti
MembranePathology & Biotechi
Involvement in diseasei
Familial hyperinsulinemic hypoglycemia 2 (HHF2)12 Publications
The disease is caused by mutations affecting the gene represented in this entry.
Disease descriptionMost common cause of persistent hypoglycemia in infancy. Unless early and aggressive intervention is undertaken, brain damage from recurrent episodes of hypoglycemia may occur.
See also OMIM:601820| Feature key | Position(s) | DescriptionActions | Graphical view | Length |
|---|---|---|---|---|
| Natural variantiVAR_031329 | 34 | R → H in HHF2. 1 Publication | 1 | |
| Natural variantiVAR_031330 | 40 | G → D in HHF2. 1 Publication | 1 | |
| Natural variantiVAR_031335 | 55 | F → L in HHF2; does neither affect channel expression nor channel response to MgADP. 2 Publications | 1 | |
| Natural variantiVAR_026506 | 67 | K → N in HHF2. 1 Publication | 1 | |
| Natural variantiVAR_026507 | 91 | W → R in HHF2. 1 Publication | 1 | |
| Natural variantiVAR_031336 | 101 | A → D in HHF2. 2 Publications | 1 | |
| Natural variantiVAR_031337 | 116 | S → P in HHF2. 1 Publication | 1 | |
| Natural variantiVAR_031338 | 134 | G → A in HHF2. 1 Publication | 1 | |
| Natural variantiVAR_031339 | 136 | R → L in HHF2. 2 Publications | 1 | |
| Natural variantiVAR_001557 | 147 | L → P in HHF2. 2 PublicationsCorresponds to variant dbSNP:rs28936678Ensembl. | 1 | |
| Natural variantiVAR_073683 | 156 | G → R in HHF2. 1 Publication | 1 | |
| Natural variantiVAR_073685 | 204 | D → E in HHF2. 1 Publication | 1 | |
| Natural variantiVAR_026513 | 254 | P → L in HHF2; impairs trafficking of the mutant channel. 1 Publication | 1 | |
| Natural variantiVAR_031345 | 259 | H → R in HHF2; impairs trafficking and abolishes channel function. 1 Publication | 1 | |
| Natural variantiVAR_031346 | 266 | P → L in HHF2. 1 Publication | 1 | |
| Natural variantiVAR_073687 | 282 | E → K in HHF2; prevents the ER export and surface expression of the channel. 1 Publication | 1 | |
| Natural variantiVAR_031347 | 301 | R → H in HHF2. 2 Publications | 1 |
Diabetes mellitus, permanent neonatal (PNDM)12 Publications
The disease is caused by mutations affecting the gene represented in this entry.
Disease descriptionA rare form of diabetes distinct from childhood-onset autoimmune diabetes mellitus type 1. It is characterized by insulin-requiring hyperglycemia that is diagnosed within the first months of life. Permanent neonatal diabetes requires lifelong therapy.
See also OMIM:606176| Feature key | Position(s) | DescriptionActions | Graphical view | Length |
|---|---|---|---|---|
| Natural variantiVAR_026498 | 35 | F → L in PNDM. 1 Publication | 1 | |
| Natural variantiVAR_026499 | 35 | F → V in PNDM. 1 Publication | 1 | |
| Natural variantiVAR_031332 | 46 | H → Y in PNDM; one patient with mild dysmorphic features. 2 Publications | 1 | |
| Natural variantiVAR_026500 | 50 | R → P in PNDM; decreased inhibition by ATP; enhanced activation by Mg(2+); increased current; one patient with developmental delay. 2 Publications | 1 | |
| Natural variantiVAR_031333 | 50 | R → Q in PNDM; decreased inhibition by ATP; enhanced activation by Mg(2+); increased current. 2 Publications | 1 | |
| Natural variantiVAR_026501 | 52 | Q → R in PNDM; with developmental delay and epilepsy; produces larger current and more change in ATP sensitivity than mutation associated with mild disease C-201. 3 Publications | 1 | |
| Natural variantiVAR_031334 | 53 | G → D in PNDM; with developmental delay and epilepsy. 1 Publication | 1 | |
| Natural variantiVAR_026502 | 53 | G → R in TNDM3; also found in a family member with PNDM; reduction in the sensitivity to ATP when compared with wild-type. 1 Publication | 1 | |
| Natural variantiVAR_026503 | 53 | G → S in TNDM3; also found in a family member with PNDM; reduction in the sensitivity to ATP when compared with wild-type. 1 Publication | 1 | |
| Natural variantiVAR_026504 | 59 | V → G in PNDM; with developmental delay and epilepsy; with neurologic features; produces larger current and more change in ATP sensitivity than mutation associated with mild disease C-201; decreases ATP sensitivity indirectly by favoring the open conformation of the channel. 3 Publications | 1 | |
| Natural variantiVAR_026505 | 59 | V → M in PNDM; four patients with developmental delay and muscle weakness. 5 Publications | 1 | |
| Natural variantiVAR_073681 | 60 | F → Y in PNDM; present on the same allele as L-64; increases the intrinsic channel open probability. 1 Publication | 1 | |
| Natural variantiVAR_073682 | 64 | V → L in PNDM; present on the same allele as Y-60; enhances the ability of MgATP to stimulate channel activity. 1 Publication | 1 | |
| Natural variantiVAR_031341 | 164 | L → P in PNDM. 2 Publications | 1 | |
| Natural variantiVAR_031342 | 166 | C → Y in PNDM; individual also diagnosed with West syndrome. 1 Publication | 1 | |
| Natural variantiVAR_073684 | 167 | I → L in PNDM; has severely impaired sensitivity to ATP and markedly increases open channel probability. 1 Publication | 1 | |
| Natural variantiVAR_026508 | 170 | K → N in PNDM. 1 Publication | 1 | |
| Natural variantiVAR_026509 | 170 | K → R in PNDM. 1 Publication | 1 | |
| Natural variantiVAR_031343 | 170 | K → T in PNDM. 1 Publication | 1 | |
| Natural variantiVAR_026511 | 201 | R → C in PNDM; two individuals with developmental delay; produces smaller current and less change in ATP sensitivity than mutations associated with severe disease R-52 and G-59. 6 Publications | 1 | |
| Natural variantiVAR_026512 | 201 | R → H in PNDM; ability of ATP to block mutant channels greatly reduced. 5 Publications | 1 | |
| Natural variantiVAR_031344 | 201 | R → L in PNDM. 1 Publication | 1 | |
| Natural variantiVAR_026514 | 296 | I → L in PNDM; with developmental delay and epilepsy. 2 Publications | 1 | |
| Natural variantiVAR_026515 | 322 | E → K in PNDM. 1 Publication | 1 | |
| Natural variantiVAR_026516 | 330 | Y → C in PNDM. 2 Publications | 1 | |
| Natural variantiVAR_031348 | 330 | Y → S in PNDM. 1 Publication | 1 | |
| Natural variantiVAR_026517 | 333 | F → I in PNDM; alters gating characteristics, decreases sensitivity to inhibition by ATP and increases intrinsic open probability. 2 Publications | 1 |
Transient neonatal diabetes mellitus 3 (TNDM3)2 Publications
The disease is caused by mutations affecting the gene represented in this entry.
Disease descriptionNeonatal diabetes mellitus, defined as insulin-requiring hyperglycemia within the first month of life, is a rare entity. In about half of the neonates, diabetes is transient and resolves at a median age of 3 months, whereas the rest have a permanent form of diabetes. In a significant number of patients with transient neonatal diabetes mellitus, diabetes type 2 appears later in life. The onset and severity of TNDM3 is variable with childhood-onset diabetes, gestational diabetes or adult-onset diabetes described.
See also OMIM:610582| Feature key | Position(s) | DescriptionActions | Graphical view | Length |
|---|---|---|---|---|
| Natural variantiVAR_031331 | 42 | C → R in TNDM3; increased spontaneous open probability; reduced ATP sensitivity; reduced expression at the cell surface of the functional ATP-sensitive form. 1 Publication | 1 | |
| Natural variantiVAR_026502 | 53 | G → R in TNDM3; also found in a family member with PNDM; reduction in the sensitivity to ATP when compared with wild-type. 1 Publication | 1 | |
| Natural variantiVAR_026503 | 53 | G → S in TNDM3; also found in a family member with PNDM; reduction in the sensitivity to ATP when compared with wild-type. 1 Publication | 1 | |
| Natural variantiVAR_026510 | 182 | I → V in TNDM3; reduction in the sensitivity to ATP when compared with wild-type. 1 Publication | 1 |
Defects in KCNJ11 may contribute to non-insulin-dependent diabetes mellitus (NIDDM), also known as diabetes mellitus type 2.
Maturity-onset diabetes of the young 13 (MODY13)1 Publication
The disease is caused by mutations affecting the gene represented in this entry.
Disease descriptionA form of diabetes that is characterized by an autosomal dominant mode of inheritance, onset in childhood or early adulthood (usually before 25 years of age), a primary defect in insulin secretion and frequent insulin-independence at the beginning of the disease.
See also OMIM:616329| Feature key | Position(s) | DescriptionActions | Graphical view | Length |
|---|---|---|---|---|
| Natural variantiVAR_073686 | 227 | E → K in MODY13. 1 Publication | 1 |
Keywords - Diseasei
Diabetes mellitus, Disease mutationOrganism-specific databases
| DisGeNETi | 3767. |
| MalaCardsi | KCNJ11. |
| MIMi | 601820. phenotype. 606176. phenotype. 610582. phenotype. 616329. phenotype. |
| Orphaneti | 276580. Autosomal dominant hyperinsulinism due to Kir6.2 deficiency. 79644. Autosomal recessive hyperinsulinism due to Kir6.2 deficiency. 79134. DEND syndrome. 276603. Diazoxide-resistant focal hyperinsulinism due to Kir6.2 deficiency. 99989. Intermediate DEND syndrome. 552. MODY. 99885. Permanent neonatal diabetes mellitus. 99886. Transient neonatal diabetes mellitus. |
| PharmGKBi | PA217. |
Chemistry databases
| ChEMBLi | CHEMBL1886. |
| DrugBanki | DB01119. Diazoxide. DB00222. Glimepiride. DB01016. Glyburide. DB00308. Ibutilide. DB00922. Levosimendan. DB01154. Thiamylal. DB00839. Tolazamide. DB00661. Verapamil. DB01392. Yohimbine. |
Polymorphism and mutation databases
| BioMutai | KCNJ11. |
| DMDMi | 76803775. |
PTM / Processingi
Molecule processing
| Feature key | Position(s) | DescriptionActions | Graphical view | Length |
|---|---|---|---|---|
| ChainiPRO_0000154957 | 1 – 390 | ATP-sensitive inward rectifier potassium channel 11Add BLAST | 390 |
Amino acid modifications
| Feature key | Position(s) | DescriptionActions | Graphical view | Length |
|---|---|---|---|---|
| Modified residuei | 341 | Phosphothreonine; by MAPK11 Publication | 1 | |
| Modified residuei | 385 | Phosphoserine; by MAPK11 Publication | 1 |
Post-translational modificationi
Phosphorylation by MAPK1 results in changes in channel gating that destabilize the closed states and reduce the ATP sensitivity.1 Publication
Keywords - PTMi
PhosphoproteinProteomic databases
| PaxDbi | Q14654. |
| PeptideAtlasi | Q14654. |
| PRIDEi | Q14654. |
PTM databases
| iPTMneti | Q14654. |
| PhosphoSitePlusi | Q14654. |
Expressioni
Gene expression databases
| Bgeei | ENSG00000187486. |
| CleanExi | HS_KCNJ11. |
| ExpressionAtlasi | Q14654. baseline and differential. |
| Genevisiblei | Q14654. HS. |
Organism-specific databases
| HPAi | HPA048891. |
Interactioni
Subunit structurei
Interacts with ABCC8/SUR. Interacts with ABCC9/SUR2.2 Publications
GO - Molecular functioni
- ankyrin binding Source: BHF-UCL
- heat shock protein binding Source: Ensembl
- ion channel binding Source: BHF-UCL
- protein C-terminus binding Source: Ensembl
Protein-protein interaction databases
| BioGridi | 109969. 12 interactors. |
| DIPi | DIP-58643N. |
| IntActi | Q14654. 4 interactors. |
| STRINGi | 9606.ENSP00000345708. |
Chemistry databases
| BindingDBi | Q14654. |
Family & Domainsi
Motif
| Feature key | Position(s) | DescriptionActions | Graphical view | Length |
|---|---|---|---|---|
| Motifi | 130 – 135 | Selectivity filterBy similarity | 6 |
Sequence similaritiesi
Belongs to the inward rectifier-type potassium channel (TC 1.A.2.1) family. KCNJ11 subfamily. [View classification]Curated
Keywords - Domaini
Transmembrane, Transmembrane helixPhylogenomic databases
| eggNOGi | KOG3827. Eukaryota. ENOG410XQ62. LUCA. |
| HOGENOMi | HOG000237325. |
| HOVERGENi | HBG006178. |
| InParanoidi | Q14654. |
| KOi | K05004. |
| OrthoDBi | EOG091G08HC. |
| PhylomeDBi | Q14654. |
| TreeFami | TF313676. |
Family and domain databases
| Gene3Di | 2.60.40.1400. 1 hit. |
| InterProi | View protein in InterPro IPR014756. Ig_E-set. IPR016449. K_chnl_inward-rec_Kir. IPR003279. K_chnl_inward-rec_Kir6.2. IPR013518. K_chnl_inward-rec_Kir_cyto. |
| PANTHERi | PTHR11767. PTHR11767. 1 hit. PTHR11767:SF83. PTHR11767:SF83. 1 hit. |
| Pfami | View protein in Pfam PF01007. IRK. 1 hit. |
| PIRSFi | PIRSF005465. GIRK_kir. 1 hit. |
| PRINTSi | PR01332. KIR62CHANNEL. PR01320. KIRCHANNEL. |
| SUPFAMi | SSF81296. SSF81296. 1 hit. |
Sequences (2)i
Sequence statusi: Complete.
This entry describes 2 isoformsi produced by alternative splicing. AlignAdd to basket
Isoform 1 (identifier: Q14654-1) [UniParc]FASTAAdd to basket
This isoform has been chosen as the 'canonical' sequence. All positional information in this entry refers to it. This is also the sequence that appears in the downloadable versions of the entry.
10 20 30 40 50
MLSRKGIIPE EYVLTRLAED PAEPRYRARQ RRARFVSKKG NCNVAHKNIR
60 70 80 90 100
EQGRFLQDVF TTLVDLKWPH TLLIFTMSFL CSWLLFAMAW WLIAFAHGDL
110 120 130 140 150
APSEGTAEPC VTSIHSFSSA FLFSIEVQVT IGFGGRMVTE ECPLAILILI
160 170 180 190 200
VQNIVGLMIN AIMLGCIFMK TAQAHRRAET LIFSKHAVIA LRHGRLCFML
210 220 230 240 250
RVGDLRKSMI ISATIHMQVV RKTTSPEGEV VPLHQVDIPM ENGVGGNSIF
260 270 280 290 300
LVAPLIIYHV IDANSPLYDL APSDLHHHQD LEIIVILEGV VETTGITTQA
310 320 330 340 350
RTSYLADEIL WGQRFVPIVA EEDGRYSVDY SKFGNTIKVP TPLCTARQLD
360 370 380 390
EDHSLLEALT LASARGPLRK RSVPMAKAKP KFSISPDSLS
Sequence cautioni
The sequence AAH40617 differs from that shown. Reason: Erroneous initiation. Translation N-terminally shortened.Curated
Experimental Info
| Feature key | Position(s) | DescriptionActions | Graphical view | Length |
|---|---|---|---|---|
| Sequence conflicti | 370 | K → E in BAG63046 (PubMed:14702039).Curated | 1 |
Natural variant
| Feature key | Position(s) | DescriptionActions | Graphical view | Length |
|---|---|---|---|---|
| Natural variantiVAR_008659 | 10 | E → K Rare polymorphism. 1 Publication | 1 | |
| Natural variantiVAR_055978 | 18 | A → G. Corresponds to variant dbSNP:rs41309072Ensembl. | 1 | |
| Natural variantiVAR_008660 | 23 | E → K Linked to V-337. 6 PublicationsCorresponds to variant dbSNP:rs5219Ensembl. | 1 | |
| Natural variantiVAR_031329 | 34 | R → H in HHF2. 1 Publication | 1 | |
| Natural variantiVAR_026498 | 35 | F → L in PNDM. 1 Publication | 1 | |
| Natural variantiVAR_026499 | 35 | F → V in PNDM. 1 Publication | 1 | |
| Natural variantiVAR_031330 | 40 | G → D in HHF2. 1 Publication | 1 | |
| Natural variantiVAR_031331 | 42 | C → R in TNDM3; increased spontaneous open probability; reduced ATP sensitivity; reduced expression at the cell surface of the functional ATP-sensitive form. 1 Publication | 1 | |
| Natural variantiVAR_031332 | 46 | H → Y in PNDM; one patient with mild dysmorphic features. 2 Publications | 1 | |
| Natural variantiVAR_026500 | 50 | R → P in PNDM; decreased inhibition by ATP; enhanced activation by Mg(2+); increased current; one patient with developmental delay. 2 Publications | 1 | |
| Natural variantiVAR_031333 | 50 | R → Q in PNDM; decreased inhibition by ATP; enhanced activation by Mg(2+); increased current. 2 Publications | 1 | |
| Natural variantiVAR_026501 | 52 | Q → R in PNDM; with developmental delay and epilepsy; produces larger current and more change in ATP sensitivity than mutation associated with mild disease C-201. 3 Publications | 1 | |
| Natural variantiVAR_031334 | 53 | G → D in PNDM; with developmental delay and epilepsy. 1 Publication | 1 | |
| Natural variantiVAR_026502 | 53 | G → R in TNDM3; also found in a family member with PNDM; reduction in the sensitivity to ATP when compared with wild-type. 1 Publication | 1 | |
| Natural variantiVAR_026503 | 53 | G → S in TNDM3; also found in a family member with PNDM; reduction in the sensitivity to ATP when compared with wild-type. 1 Publication | 1 | |
| Natural variantiVAR_031335 | 55 | F → L in HHF2; does neither affect channel expression nor channel response to MgADP. 2 Publications | 1 | |
| Natural variantiVAR_026504 | 59 | V → G in PNDM; with developmental delay and epilepsy; with neurologic features; produces larger current and more change in ATP sensitivity than mutation associated with mild disease C-201; decreases ATP sensitivity indirectly by favoring the open conformation of the channel. 3 Publications | 1 | |
| Natural variantiVAR_026505 | 59 | V → M in PNDM; four patients with developmental delay and muscle weakness. 5 Publications | 1 | |
| Natural variantiVAR_073681 | 60 | F → Y in PNDM; present on the same allele as L-64; increases the intrinsic channel open probability. 1 Publication | 1 | |
| Natural variantiVAR_073682 | 64 | V → L in PNDM; present on the same allele as Y-60; enhances the ability of MgATP to stimulate channel activity. 1 Publication | 1 | |
| Natural variantiVAR_026506 | 67 | K → N in HHF2. 1 Publication | 1 | |
| Natural variantiVAR_026507 | 91 | W → R in HHF2. 1 Publication | 1 | |
| Natural variantiVAR_031336 | 101 | A → D in HHF2. 2 Publications | 1 | |
| Natural variantiVAR_031337 | 116 | S → P in HHF2. 1 Publication | 1 | |
| Natural variantiVAR_031338 | 134 | G → A in HHF2. 1 Publication | 1 | |
| Natural variantiVAR_031339 | 136 | R → L in HHF2. 2 Publications | 1 | |
| Natural variantiVAR_001557 | 147 | L → P in HHF2. 2 PublicationsCorresponds to variant dbSNP:rs28936678Ensembl. | 1 | |
| Natural variantiVAR_031340 | 148 | I → S2 Publications | 1 | |
| Natural variantiVAR_073683 | 156 | G → R in HHF2. 1 Publication | 1 | |
| Natural variantiVAR_031341 | 164 | L → P in PNDM. 2 Publications | 1 | |
| Natural variantiVAR_031342 | 166 | C → Y in PNDM; individual also diagnosed with West syndrome. 1 Publication | 1 | |
| Natural variantiVAR_073684 | 167 | I → L in PNDM; has severely impaired sensitivity to ATP and markedly increases open channel probability. 1 Publication | 1 | |
| Natural variantiVAR_026508 | 170 | K → N in PNDM. 1 Publication | 1 | |
| Natural variantiVAR_026509 | 170 | K → R in PNDM. 1 Publication | 1 | |
| Natural variantiVAR_031343 | 170 | K → T in PNDM. 1 Publication | 1 | |
| Natural variantiVAR_026510 | 182 | I → V in TNDM3; reduction in the sensitivity to ATP when compared with wild-type. 1 Publication | 1 | |
| Natural variantiVAR_014929 | 195 | R → H. Corresponds to variant dbSNP:rs5217Ensembl. | 1 | |
| Natural variantiVAR_026511 | 201 | R → C in PNDM; two individuals with developmental delay; produces smaller current and less change in ATP sensitivity than mutations associated with severe disease R-52 and G-59. 6 Publications | 1 | |
| Natural variantiVAR_026512 | 201 | R → H in PNDM; ability of ATP to block mutant channels greatly reduced. 5 Publications | 1 | |
| Natural variantiVAR_031344 | 201 | R → L in PNDM. 1 Publication | 1 | |
| Natural variantiVAR_073685 | 204 | D → E in HHF2. 1 Publication | 1 | |
| Natural variantiVAR_073686 | 227 | E → K in MODY13. 1 Publication | 1 | |
| Natural variantiVAR_026513 | 254 | P → L in HHF2; impairs trafficking of the mutant channel. 1 Publication | 1 | |
| Natural variantiVAR_031345 | 259 | H → R in HHF2; impairs trafficking and abolishes channel function. 1 Publication | 1 | |
| Natural variantiVAR_031346 | 266 | P → L in HHF2. 1 Publication | 1 | |
| Natural variantiVAR_008661 | 270 | L → V2 PublicationsCorresponds to variant dbSNP:rs1800467Ensembl. | 1 | |
| Natural variantiVAR_073687 | 282 | E → K in HHF2; prevents the ER export and surface expression of the channel. 1 Publication | 1 | |
| Natural variantiVAR_026514 | 296 | I → L in PNDM; with developmental delay and epilepsy. 2 Publications | 1 | |
| Natural variantiVAR_031347 | 301 | R → H in HHF2. 2 Publications | 1 | |
| Natural variantiVAR_026515 | 322 | E → K in PNDM. 1 Publication | 1 | |
| Natural variantiVAR_026516 | 330 | Y → C in PNDM. 2 Publications | 1 | |
| Natural variantiVAR_031348 | 330 | Y → S in PNDM. 1 Publication | 1 | |
| Natural variantiVAR_026517 | 333 | F → I in PNDM; alters gating characteristics, decreases sensitivity to inhibition by ATP and increases intrinsic open probability. 2 Publications | 1 | |
| Natural variantiVAR_008662 | 337 | I → V Linked to K-23. 6 PublicationsCorresponds to variant dbSNP:rs5215Ensembl. | 1 | |
| Natural variantiVAR_008663 | 355 | L → P in NIDDM; Afro-Caribbean. 1 Publication | 1 | |
| Natural variantiVAR_008664 | 380 | P → PKP in NIDDM. | 1 | |
| Natural variantiVAR_008665 | 385 | S → C1 PublicationCorresponds to variant dbSNP:rs41282930Ensembl. | 1 |
Alternative sequence
| Feature key | Position(s) | DescriptionActions | Graphical view | Length |
|---|---|---|---|---|
| Alternative sequenceiVSP_045270 | 1 – 87 | Missing in isoform 2. 2 PublicationsAdd BLAST | 87 |
Sequence databases
| Select the link destinations: EMBLi GenBanki DDBJi Links Updated | D50582 Genomic DNA. Translation: BAA09131.1. AK301550 mRNA. Translation: BAG63046.1. AC124798 Genomic DNA. No translation available. BC064497 mRNA. Translation: AAH64497.1. BC040617 mRNA. Translation: AAH40617.1. Different initiation. BC112358 mRNA. Translation: AAI12359.1. |
| CCDSi | CCDS31436.1. [Q14654-1] CCDS53606.1. [Q14654-2] |
| PIRi | A57616. |
| RefSeqi | NP_001159762.1. NM_001166290.1. |
| UniGenei | Hs.248141. |
Genome annotation databases
| Ensembli | ENST00000339994; ENSP00000345708; ENSG00000187486. ENST00000528731; ENSP00000434755; ENSG00000187486. |
| GeneIDi | 3767. |
| KEGGi | hsa:3767. |
| UCSCi | uc001mna.4. human. [Q14654-1] |
Keywords - Coding sequence diversityi
Alternative splicing, PolymorphismCross-referencesi
Sequence databases
| Select the link destinations: EMBLi GenBanki DDBJi Links Updated | D50582 Genomic DNA. Translation: BAA09131.1. AK301550 mRNA. Translation: BAG63046.1. AC124798 Genomic DNA. No translation available. BC064497 mRNA. Translation: AAH64497.1. BC040617 mRNA. Translation: AAH40617.1. Different initiation. BC112358 mRNA. Translation: AAI12359.1. |
| CCDSi | CCDS31436.1. [Q14654-1] CCDS53606.1. [Q14654-2] |
| PIRi | A57616. |
| RefSeqi | NP_001159762.1. NM_001166290.1. |
| UniGenei | Hs.248141. |
3D structure databases
| ProteinModelPortali | Q14654. |
| ModBasei | Search... |
| MobiDBi | Search... |
Protein-protein interaction databases
| BioGridi | 109969. 12 interactors. |
| DIPi | DIP-58643N. |
| IntActi | Q14654. 4 interactors. |
| STRINGi | 9606.ENSP00000345708. |
Chemistry databases
| BindingDBi | Q14654. |
| ChEMBLi | CHEMBL1886. |
| DrugBanki | DB01119. Diazoxide. DB00222. Glimepiride. DB01016. Glyburide. DB00308. Ibutilide. DB00922. Levosimendan. DB01154. Thiamylal. DB00839. Tolazamide. DB00661. Verapamil. DB01392. Yohimbine. |
Protein family/group databases
| TCDBi | 1.A.2.1.17. inward rectifier k(+) channel (irk-c) family. |
PTM databases
| iPTMneti | Q14654. |
| PhosphoSitePlusi | Q14654. |
Polymorphism and mutation databases
| BioMutai | KCNJ11. |
| DMDMi | 76803775. |
Proteomic databases
| PaxDbi | Q14654. |
| PeptideAtlasi | Q14654. |
| PRIDEi | Q14654. |
Protocols and materials databases
| Structural Biology Knowledgebase | Search... |
Genome annotation databases
| Ensembli | ENST00000339994; ENSP00000345708; ENSG00000187486. ENST00000528731; ENSP00000434755; ENSG00000187486. |
| GeneIDi | 3767. |
| KEGGi | hsa:3767. |
| UCSCi | uc001mna.4. human. [Q14654-1] |
Organism-specific databases
| CTDi | 3767. |
| DisGeNETi | 3767. |
| GeneCardsi | KCNJ11. |
| GeneReviewsi | KCNJ11. |
| H-InvDBi | HIX0035982. |
| HGNCi | HGNC:6257. KCNJ11. |
| HPAi | HPA048891. |
| MalaCardsi | KCNJ11. |
| MIMi | 600937. gene. 601820. phenotype. 606176. phenotype. 610582. phenotype. 616329. phenotype. |
| neXtProti | NX_Q14654. |
| Orphaneti | 276580. Autosomal dominant hyperinsulinism due to Kir6.2 deficiency. 79644. Autosomal recessive hyperinsulinism due to Kir6.2 deficiency. 79134. DEND syndrome. 276603. Diazoxide-resistant focal hyperinsulinism due to Kir6.2 deficiency. 99989. Intermediate DEND syndrome. 552. MODY. 99885. Permanent neonatal diabetes mellitus. 99886. Transient neonatal diabetes mellitus. |
| PharmGKBi | PA217. |
| GenAtlasi | Search... |
Phylogenomic databases
| eggNOGi | KOG3827. Eukaryota. ENOG410XQ62. LUCA. |
| HOGENOMi | HOG000237325. |
| HOVERGENi | HBG006178. |
| InParanoidi | Q14654. |
| KOi | K05004. |
| OrthoDBi | EOG091G08HC. |
| PhylomeDBi | Q14654. |
| TreeFami | TF313676. |
Enzyme and pathway databases
| Reactomei | R-HSA-1296025. ATP sensitive Potassium channels. R-HSA-382556. ABC-family proteins mediated transport. R-HSA-422356. Regulation of insulin secretion. R-HSA-5578775. Ion homeostasis. R-HSA-5683177. Defective ABCC8 can cause hypoglycemias and hyperglycemias. |
| SignaLinki | Q14654. |
| SIGNORi | Q14654. |
Miscellaneous databases
| GeneWikii | Kir6.2. |
| GenomeRNAii | 3767. |
| PROi | PR:Q14654. |
| SOURCEi | Search... |
Gene expression databases
| Bgeei | ENSG00000187486. |
| CleanExi | HS_KCNJ11. |
| ExpressionAtlasi | Q14654. baseline and differential. |
| Genevisiblei | Q14654. HS. |
Family and domain databases
| Gene3Di | 2.60.40.1400. 1 hit. |
| InterProi | View protein in InterPro IPR014756. Ig_E-set. IPR016449. K_chnl_inward-rec_Kir. IPR003279. K_chnl_inward-rec_Kir6.2. IPR013518. K_chnl_inward-rec_Kir_cyto. |
| PANTHERi | PTHR11767. PTHR11767. 1 hit. PTHR11767:SF83. PTHR11767:SF83. 1 hit. |
| Pfami | View protein in Pfam PF01007. IRK. 1 hit. |
| PIRSFi | PIRSF005465. GIRK_kir. 1 hit. |
| PRINTSi | PR01332. KIR62CHANNEL. PR01320. KIRCHANNEL. |
| SUPFAMi | SSF81296. SSF81296. 1 hit. |
| ProtoNeti | Search... |
Entry informationi
| Entry namei | KCJ11_HUMAN | |
| Accessioni | Q14654Primary (citable) accession number: Q14654 Secondary accession number(s): B4DWI4 Q8IW96 | |
| Entry historyi | Integrated into UniProtKB/Swiss-Prot: | November 1, 1997 |
| Last sequence update: | September 27, 2005 | |
| Last modified: | June 7, 2017 | |
| This is version 185 of the entry and version 2 of the sequence. See complete history. | ||
| Entry statusi | Reviewed (UniProtKB/Swiss-Prot) | |
| Annotation program | Chordata Protein Annotation Program | |
| Disclaimer | Any medical or genetic information present in this entry is provided for research, educational and informational purposes only. It is not in any way intended to be used as a substitute for professional medical advice, diagnosis, treatment or care. | |
Miscellaneousi
Keywords - Technical termi
Complete proteome, Reference proteomeDocuments
- Human chromosome 11
Human chromosome 11: entries, gene names and cross-references to MIM - Human entries with polymorphisms or disease mutations
List of human entries with polymorphisms or disease mutations - Human polymorphisms and disease mutations
Index of human polymorphisms and disease mutations - MIM cross-references
Online Mendelian Inheritance in Man (MIM) cross-references in UniProtKB/Swiss-Prot - SIMILARITY comments
Index of protein domains and families
Similar proteinsi
Links to similar proteins from the UniProt Reference Clusters (UniRef) at 100%, 90% and 50% sequence identity:| 100% | UniRef100 combines identical sequences and sub-fragments with 11 or more residues from any organism into one UniRef entry. |
| 90% | UniRef90 is built by clustering UniRef100 sequences that have at least 90% sequence identity to, and 80% overlap with, the longest sequence (a.k.a seed sequence). |
| 50% | UniRef50 is built by clustering UniRef90 seed sequences that have at least 50% sequence identity to, and 80% overlap with, the longest sequence in the cluster. |