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Q14654 (IRK11_HUMAN) Reviewed, UniProtKB/Swiss-Prot
Last modified
February 19, 2014.
Version 150.
History...
Clusters with 
Names·Attributes·General annotation·Ontologies·Alt products·Sequence annotation·Sequences·References·Web links·Cross-refs·Entry info·DocumentsCustomize orderNames·Attributes·General annotation·Ontologies·Alt products·Sequence annotation·Sequences·References·Web links·Cross-refs·Entry info·DocumentsCustomize orderNames and origin
| Protein names | Recommended name: ATP-sensitive inward rectifier potassium channel 11 Alternative name(s): IKATP Inward rectifier K(+) channel Kir6.2 Potassium channel, inwardly rectifying subfamily J member 11 | ||
| Gene names |
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| Organism | Homo sapiens (Human) [Reference proteome] | ||
| Taxonomic identifier | 9606 [NCBI] | ||
| Taxonomic lineage | Eukaryota › Metazoa › Chordata › Craniata › Vertebrata › Euteleostomi › Mammalia › Eutheria › Euarchontoglires › Primates › Haplorrhini › Catarrhini › Hominidae › Homo |
Protein attributes
| Sequence length | 390 AA. |
| Sequence status | Complete. |
| Protein existence | Evidence at protein level |
General annotation (Comments)
| Function | 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. Ref.5 Ref.8 |
| Subunit structure | Interacts with ABCC8/SUR. Interacts with ABCC9/SUR2. Ref.5 Ref.8 |
| Subcellular location | |
| Post-translational modification | Phosphorylation by MAPK1 results in changes in channel gating that destabilize the closed states and reduce the ATP sensitivity. |
| Involvement in disease | Familial hyperinsulinemic hypoglycemia 2 (HHF2) [MIM:601820]: Most common cause of persistent hypoglycemia in infancy. Unless early and aggressive intervention is undertaken, brain damage from recurrent episodes of hypoglycemia may occur. Diabetes mellitus, permanent neonatal (PNDM) [MIM:606176]: A 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. Transient neonatal diabetes mellitus 3 (TNDM3) [MIM:610582]: Neonatal 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. Defects in KCNJ11 may contribute to non-insulin-dependent diabetes mellitus (NIDDM), also known as diabetes mellitus type 2. Ref.12 |
| Sequence similarities | Belongs to the inward rectifier-type potassium channel (TC 1.A.2.1) family. KCNJ11 subfamily. [View classification] |
| Sequence caution | The sequence AAH40617.1 differs from that shown. Reason: Erroneous initiation. Translation N-terminally shortened. |
Ontologies
Alternative products
| This entry describes 2 isoforms produced by alternative splicing. [Align] [Select] | ||||||
| Isoform 1 (identifier: Q14654-1) 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. | ||||||
| Isoform 2 (identifier: Q14654-2) The sequence of this isoform differs from the canonical sequence as follows: 1-87: Missing. |
Sequence annotation (Features)
| Feature key | Position(s) | Length | Description | Graphical view | Feature identifier | ||||
Molecule processing | |||||||||
|---|---|---|---|---|---|---|---|---|---|
| Chain | 1 – 390 | 390 | ATP-sensitive inward rectifier potassium channel 11 | PRO_0000154957 | |||||
Regions | |||||||||
| Topological domain | 1 – 68 | 68 | Cytoplasmic By similarity | ||||||
| Transmembrane | 69 – 93 | 25 | Helical; Name=M1; By similarity | ||||||
| Topological domain | 94 – 116 | 23 | Extracellular By similarity | ||||||
| Intramembrane | 117 – 128 | 12 | Helical; Pore-forming; Name=H5; By similarity | ||||||
| Intramembrane | 129 – 135 | 7 | Pore-forming; By similarity | ||||||
| Topological domain | 136 – 144 | 9 | Extracellular By similarity | ||||||
| Transmembrane | 145 – 166 | 22 | Helical; Name=M2; By similarity | ||||||
| Topological domain | 167 – 390 | 224 | Cytoplasmic By similarity | ||||||
| Motif | 130 – 135 | 6 | Selectivity filter By similarity | ||||||
Sites | |||||||||
| Site | 160 | 1 | Role in the control of polyamine-mediated channel gating and in the blocking by intracellular magnesium By similarity | ||||||
Amino acid modifications | |||||||||
| Modified residue | 341 | 1 | Phosphothreonine; by MAPK1 Ref.9 | ||||||
| Modified residue | 385 | 1 | Phosphoserine; by MAPK1 Ref.9 | ||||||
Natural variations | |||||||||
| Alternative sequence | 1 – 87 | 87 | Missing in isoform 2. | VSP_045270 | |||||
| Natural variant | 10 | 1 | E → K Rare polymorphism. Ref.13 | VAR_008659 | |||||
| Natural variant | 18 | 1 | A → G. Corresponds to variant rs41309072 [ dbSNP | Ensembl ]. | VAR_055978 | |||||
| Natural variant | 23 | 1 | E → K Linked to V-337. Ref.3 Ref.12 Ref.13 Ref.15 Ref.24 Ref.32 Corresponds to variant rs5219 [ dbSNP | Ensembl ]. | VAR_008660 | |||||
| Natural variant | 34 | 1 | R → H in HHF2. Ref.24 | VAR_031329 | |||||
| Natural variant | 35 | 1 | F → L in PNDM. Ref.18 | VAR_026498 | |||||
| Natural variant | 35 | 1 | F → V in PNDM. Ref.17 | VAR_026499 | |||||
| Natural variant | 40 | 1 | G → D in HHF2. Ref.34 | VAR_031330 | |||||
| Natural variant | 42 | 1 | C → R in TNDM3; increased spontaneous open probability; reduced ATP sensitivity; reduced expression at the cell surface of the functional ATP-sensitive form. Ref.28 | VAR_031331 | |||||
| Natural variant | 46 | 1 | H → Y in PNDM; one patient with mild dysmorphic features. Ref.31 Ref.35 | VAR_031332 | |||||
| Natural variant | 50 | 1 | R → P in PNDM; decreased inhibition by ATP; enhanced activation by Mg(2+); increased current; one patient with developmental delay. Ref.26 Ref.30 | VAR_026500 | |||||
| Natural variant | 50 | 1 | R → Q in PNDM; decreased inhibition by ATP; enhanced activation by Mg(2+); increased current. Ref.30 Ref.31 | VAR_031333 | |||||
| Natural variant | 52 | 1 | 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. Ref.21 Ref.23 Ref.31 | VAR_026501 | |||||
| Natural variant | 53 | 1 | G → D in PNDM; with developmental delay and epilepsy. Ref.31 | VAR_031334 | |||||
| Natural variant | 53 | 1 | G → R in TNDM3; also found in a family member with PNDM; reduction in the sensitivity to ATP when compared with wild-type. Ref.25 | VAR_026502 | |||||
| Natural variant | 53 | 1 | G → S in TNDM3; also found in a family member with PNDM; reduction in the sensitivity to ATP when compared with wild-type. Ref.25 | VAR_026503 | |||||
| Natural variant | 55 | 1 | F → L in HHF2; does neither affect channel expression nor channel response to MgADP. Ref.33 | VAR_031335 | |||||
| Natural variant | 59 | 1 | 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. Ref.21 Ref.23 Ref.31 | VAR_026504 | |||||
| Natural variant | 59 | 1 | V → M in PNDM; four patients with developmental delay and muscle weakness. Ref.17 Ref.18 Ref.21 Ref.26 Ref.31 | VAR_026505 | |||||
| Natural variant | 67 | 1 | K → N in HHF2. Ref.16 | VAR_026506 | |||||
| Natural variant | 91 | 1 | W → R in HHF2. Ref.14 | VAR_026507 | |||||
| Natural variant | 101 | 1 | A → D in HHF2. Ref.27 Ref.34 | VAR_031336 | |||||
| Natural variant | 116 | 1 | S → P in HHF2. Ref.34 | VAR_031337 | |||||
| Natural variant | 134 | 1 | G → A in HHF2. Ref.27 | VAR_031338 | |||||
| Natural variant | 136 | 1 | R → L in HHF2. Ref.27 Ref.34 | VAR_031339 | |||||
| Natural variant | 147 | 1 | L → P in HHF2. Ref.10 Ref.11 Corresponds to variant rs28936678 [ dbSNP | Ensembl ]. | VAR_001557 | |||||
| Natural variant | 148 | 1 | I → S. Ref.1 Ref.24 | VAR_031340 | |||||
| Natural variant | 164 | 1 | L → P in PNDM. Ref.31 Ref.35 | VAR_031341 | |||||
| Natural variant | 166 | 1 | C → Y in PNDM; individual also diagnosed with West syndrome. Ref.31 | VAR_031342 | |||||
| Natural variant | 170 | 1 | K → N in PNDM. Ref.26 | VAR_026508 | |||||
| Natural variant | 170 | 1 | K → R in PNDM. Ref.26 | VAR_026509 | |||||
| Natural variant | 170 | 1 | K → T in PNDM. Ref.31 | VAR_031343 | |||||
| Natural variant | 182 | 1 | I → V in TNDM3; reduction in the sensitivity to ATP when compared with wild-type. Ref.25 | VAR_026510 | |||||
| Natural variant | 195 | 1 | R → H. Corresponds to variant rs5217 [ dbSNP | Ensembl ]. | VAR_014929 | |||||
| Natural variant | 201 | 1 | 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. Ref.18 Ref.19 Ref.21 Ref.23 Ref.26 Ref.31 | VAR_026511 | |||||
| Natural variant | 201 | 1 | R → H in PNDM; ability of ATP to block mutant channels greatly reduced. Ref.17 Ref.18 Ref.21 Ref.31 Ref.35 | VAR_026512 | |||||
| Natural variant | 201 | 1 | R → L in PNDM. Ref.31 | VAR_031344 | |||||
| Natural variant | 254 | 1 | P → L in HHF2; impairs trafficking of the mutant channel. Ref.20 | VAR_026513 | |||||
| Natural variant | 259 | 1 | H → R in HHF2; impairs trafficking and abolishes channel function. Ref.29 | VAR_031345 | |||||
| Natural variant | 266 | 1 | P → L in HHF2. Ref.27 | VAR_031346 | |||||
| Natural variant | 270 | 1 | L → V. Ref.12 Ref.13 Corresponds to variant rs1800467 [ dbSNP | Ensembl ]. | VAR_008661 | |||||
| Natural variant | 296 | 1 | I → L in PNDM; with developmental delay and epilepsy. Ref.21 Ref.31 | VAR_026514 | |||||
| Natural variant | 301 | 1 | R → H in HHF2. Ref.27 Ref.34 | VAR_031347 | |||||
| Natural variant | 322 | 1 | E → K in PNDM. Ref.18 | VAR_026515 | |||||
| Natural variant | 330 | 1 | Y → C in PNDM. Ref.17 Ref.18 | VAR_026516 | |||||
| Natural variant | 330 | 1 | Y → S in PNDM. Ref.31 | VAR_031348 | |||||
| Natural variant | 333 | 1 | F → I in PNDM; alters gating characteristics, decreases sensitivity to inhibition by ATP and increases intrinsic open probability. Ref.8 Ref.17 | VAR_026517 | |||||
| Natural variant | 337 | 1 | I → V Linked to K-23. Ref.3 Ref.12 Ref.13 Ref.15 Ref.24 Ref.32 Corresponds to variant rs5215 [ dbSNP | Ensembl ]. | VAR_008662 | |||||
| Natural variant | 355 | 1 | L → P in NIDDM; Afro-Caribbean. Ref.12 | VAR_008663 | |||||
| Natural variant | 380 | 1 | P → PKP in NIDDM. | VAR_008664 | |||||
| Natural variant | 385 | 1 | S → C. Ref.12 Corresponds to variant rs41282930 [ dbSNP | Ensembl ]. | VAR_008665 | |||||
Experimental info | |||||||||
| Sequence conflict | 370 | 1 | K → E in BAG63046. Ref.2 | ||||||
Sequences
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References
| « Hide 'large scale' references | |
| [1] | "Reconstitution of IKATP: an inward rectifier subunit plus the sulfonylurea receptor." Inagaki N., Gonoi T., Clement J.P. IV, Namba N., Inazawa J., Gonzalez G., Aguilar-Bryan L., Seino S., Bryan J. Science 270:1166-1170(1995) [PubMed] [Europe PMC] [Abstract] Cited for: NUCLEOTIDE SEQUENCE [GENOMIC DNA], VARIANT SER-148. Tissue: Placenta. |
| [2] | "Complete sequencing and characterization of 21,243 full-length human cDNAs." Ota T., Suzuki Y., Nishikawa T., Otsuki T., Sugiyama T., Irie R., Wakamatsu A., Hayashi K., Sato H., Nagai K., Kimura K., Makita H., Sekine M., Obayashi M., Nishi T., Shibahara T., Tanaka T., Ishii S.  Sugano S.Nat. Genet. 36:40-45(2004) [PubMed] [Europe PMC] [Abstract] Cited for: NUCLEOTIDE SEQUENCE [LARGE SCALE MRNA] (ISOFORM 2). Tissue: Mammary gland. |
| [3] | "Human chromosome 11 DNA sequence and analysis including novel gene identification." Taylor T.D., Noguchi H., Totoki Y., Toyoda A., Kuroki Y., Dewar K., Lloyd C., Itoh T., Takeda T., Kim D.-W., She X., Barlow K.F., Bloom T., Bruford E., Chang J.L., Cuomo C.A., Eichler E., FitzGerald M.G. Sakaki Y.Nature 440:497-500(2006) [PubMed] [Europe PMC] [Abstract] Cited for: NUCLEOTIDE SEQUENCE [LARGE SCALE GENOMIC DNA], VARIANTS LYS-23 AND VAL-337. |
| [4] | "The status, quality, and expansion of the NIH full-length cDNA project: the Mammalian Gene Collection (MGC)." The MGC Project Team Genome Res. 14:2121-2127(2004) [PubMed] [Europe PMC] [Abstract] Cited for: NUCLEOTIDE SEQUENCE [LARGE SCALE MRNA] (ISOFORMS 1 AND 2). Tissue: Ovary and Spleen. |
| [5] | "Reconstituted human cardiac KATP channels: functional identity with the native channels from the sarcolemma of human ventricular cells." Babenko A.P., Gonzalez G., Aguilar-Bryan L., Bryan J. Circ. Res. 83:1132-1143(1998) [PubMed] [Europe PMC] [Abstract] Cited for: FUNCTION, INTERACTION WITH ABCC9. |
| [6] | "Molecular basis for Kir6.2 channel inhibition by adenine nucleotides." Ribalet B., John S.A., Weiss J.N. Biophys. J. 84:266-276(2003) [PubMed] [Europe PMC] [Abstract] Cited for: MOLECULAR BASIS OF ATP SENSITIVITY. |
| [7] | "Congenital hyperinsulinism: molecular basis of a heterogeneous disease." Meissner T., Beinbrech B., Mayatepek E. Hum. Mutat. 13:351-361(1999) [PubMed] [Europe PMC] [Abstract] Cited for: REVIEW ON VARIANTS. |
| [8] | "A mutation in the ATP-binding site of the Kir6.2 subunit of the KATP channel alters coupling with the SUR2A subunit." Tammaro P., Ashcroft F.M. J. Physiol. (Lond.) 584:743-753(2007) [PubMed] [Europe PMC] [Abstract] Cited for: FUNCTION, CHARACTERIZATION OF VARIANT PNDM ILE-333, INTERACTION WITH ABCC9. |
| [9] | "Functional modulation of the ATP-sensitive potassium channel by extracellular signal-regulated kinase-mediated phosphorylation." Lin Y.F., Chai Y. Neuroscience 152:371-380(2008) [PubMed] [Europe PMC] [Abstract] Cited for: PHOSPHORYLATION AT THR-341 AND SER-385. |
| [10] | "Homozygosity mapping, to chromosome 11p, of the gene for familial persistent hyperinsulinemic hypoglycemia of infancy." Thomas P.M., Cote G.J., Hallman D.M., Mathew P.M. Am. J. Hum. Genet. 56:416-421(1995) [PubMed] [Europe PMC] [Abstract] Cited for: VARIANT HHF2 PRO-147. |
| [11] | "Mutation of the pancreatic islet inward rectifier Kir6.2 also leads to familial persistent hyperinsulinemic hypoglycemia of infancy." Thomas P., Ye Y., Lightner E. Hum. Mol. Genet. 5:1809-1812(1996) [PubMed] [Europe PMC] [Abstract] Cited for: VARIANT HHF2 PRO-147. |
| [12] | "Sequence variations in the human Kir6.2 gene, a subunit of the beta-cell ATP-sensitive K-channel: no association with NIDDM in white Caucasian subjects or evidence of abnormal function when expressed in vitro." Sakura H., Wat N., Horton V., Millns H., Turner R.C., Ashcroft F.M. Diabetologia 39:1233-1236(1996) [PubMed] [Europe PMC] [Abstract] Cited for: VARIANTS NIDDM PRO-355 AND LYS-PRO-380 INS, VARIANTS LYS-23; VAL-270; VAL-337 AND CYS-385. |
| [13] | "Sequence variants in the pancreatic islet beta-cell inwardly rectifying K+ channel Kir6.2 (Bir) gene: identification and lack of role in Caucasian patients with NIDDM." Inoue H., Ferrer J., Warren-Perry M., Zhang Y., Millns H., Turner R.C., Elbein S.C., Hampe C.L., Suarez B.K., Inagaki N., Seino S., Permutt M.A. Diabetes 46:502-507(1997) [PubMed] [Europe PMC] [Abstract] Cited for: VARIANTS LYS-10; LYS-23; VAL-270 AND VAL-337. |
| [14] | "Molecular biology of adenosine triphosphate-sensitive potassium channels." Aguilar-Bryan L., Bryan J. Endocr. Rev. 20:101-135(1999) [PubMed] [Europe PMC] [Abstract] Cited for: VARIANT HHF2 ARG-91. |
| [15] | "Patterns of single-nucleotide polymorphisms in candidate genes for blood-pressure homeostasis." Halushka M.K., Fan J.-B., Bentley K., Hsie L., Shen N., Weder A., Cooper R., Lipshutz R., Chakravarti A. Nat. Genet. 22:239-247(1999) [PubMed] [Europe PMC] [Abstract] Cited for: VARIANTS LYS-23 AND VAL-337. |
| [16] | "Acute insulin response tests for the differential diagnosis of congenital hyperinsulinism." Huopio H., Jaeaeskelaeinen J., Komulainen J., Miettinen R., Kaerkkaeinen P., Laakso M., Tapanainen P., Voutilainen R., Otonkoski T. J. Clin. Endocrinol. Metab. 87:4502-4507(2002) [PubMed] [Europe PMC] [Abstract] Cited for: VARIANT HHF2 ASN-67. |
| [17] | "Permanent neonatal diabetes due to mutations in KCNJ11 encoding Kir6.2: patient characteristics and initial response to sulfonylurea therapy." Sagen J.V., Raeder H., Hathout E., Shehadeh N., Gudmundsson K., Baevre H., Abuelo D., Phornphutkul C., Molnes J., Bell G.I., Gloyn A.L., Hattersley A.T., Molven A., Soevik O., Njoelstad P.R. Diabetes 53:2713-2718(2004) [PubMed] [Europe PMC] [Abstract] Cited for: VARIANTS PNDM VAL-35; MET-59; HIS-201; CYS-330 AND ILE-333. |
| [18] | "Kir6.2 mutations are a common cause of permanent neonatal diabetes in a large cohort of French patients." Vaxillaire M., Populaire C., Busiah K., Cave H., Gloyn A.L., Hattersley A.T., Czernichow P., Froguel P., Polak M. Diabetes 53:2719-2722(2004) [PubMed] [Europe PMC] [Abstract] Cited for: VARIANTS PNDM LEU-35; MET-59; CYS-201; HIS-201; LYS-322 AND CYS-330. |
| [19] | "Permanent neonatal diabetes due to paternal germline mosaicism for an activating mutation of the KCNJ11 gene encoding the Kir6.2 subunit of the beta-cell potassium adenosine triphosphate channel." Gloyn A.L., Cummings E.A., Edghill E.L., Harries L.W., Scott R., Costa T., Temple I.K., Hattersley A.T., Ellard S. J. Clin. Endocrinol. Metab. 89:3932-3935(2004) [PubMed] [Europe PMC] [Abstract] Cited for: VARIANT PNDM CYS-201. |
| [20] | "Hyperinsulinism of infancy: novel ABCC8 and KCNJ11 mutations and evidence for additional locus heterogeneity." Tornovsky S., Crane A., Cosgrove K.E., Hussain K., Lavie J., Heyman M., Nesher Y., Kuchinski N., Ben-Shushan E., Shatz O., Nahari E., Potikha T., Zangen D., Tenenbaum-Rakover Y., de Vries L., Argente J., Gracia R., Landau H. Glaser B.J. Clin. Endocrinol. Metab. 89:6224-6234(2004) [PubMed] [Europe PMC] [Abstract] Cited for: VARIANT HHF2 LEU-254, CHARACTERIZATION OF VARIANT HHF2 LEU-254. |
| [21] | "Activating mutations in the gene encoding the ATP-sensitive potassium-channel subunit Kir6.2 and permanent neonatal diabetes." Gloyn A.L., Pearson E.R., Antcliff J.F., Proks P., Bruining G.J., Slingerland A.S., Howard N., Srinivasan S., Silva J.M.C.L., Molnes J., Edghill E.L., Frayling T.M., Temple I.K., Mackay D., Shield J.P.H., Sumnik Z., van Rhijn A., Wales J.K.H. Hattersley A.T.N. Engl. J. Med. 350:1838-1849(2004) [PubMed] [Europe PMC] [Abstract] Cited for: VARIANTS PNDM ARG-52; GLY-59; MET-59; HIS-201; CYS-201 AND LEU-296, CHARACTERIZATION OF VARIANT PNDM HIS-201. |
| [22] | Erratum Gloyn A.L., Pearson E.R., Antcliff J.F., Proks P., Bruining G.J., Slingerland A.S., Howard N., Srinivasan S., Silva J.M.C.L., Molnes J., Edghill E.L., Frayling T.M., Temple I.K., Mackay D., Shield J.P.H., Sumnik Z., van Rhijn A., Wales J.K.H. Hattersley A.T.N. Engl. J. Med. 351:1470-1470(2004) |
| [23] | "Molecular basis of Kir6.2 mutations associated with neonatal diabetes or neonatal diabetes plus neurological features." Proks P., Antcliff J.F., Lippiat J., Gloyn A.L., Hattersley A.T., Ashcroft F.M. Proc. Natl. Acad. Sci. U.S.A. 101:17539-17544(2004) [PubMed] [Europe PMC] [Abstract] Cited for: CHARACTERIZATION OF VARIANTS PNDM ARG-52; GLY-59 AND CYS-201. |
| [24] | "Genotypes of the pancreatic beta-cell K-ATP channel and clinical phenotypes of Japanese patients with persistent hyperinsulinaemic hypoglycaemia of infancy." Ohkubo K., Nagashima M., Naito Y., Taguchi T., Suita S., Okamoto N., Fujinaga H., Tsumura K., Kikuchi K., Ono J. Clin. Endocrinol. (Oxf.) 62:458-465(2005) [PubMed] [Europe PMC] [Abstract] Cited for: VARIANT HHF2 HIS-34, VARIANTS LYS-23; SER-148 AND VAL-337. |
| [25] | "Relapsing diabetes can result from moderately activating mutations in KCNJ11." Gloyn A.L., Reimann F., Girard C., Edghill E.L., Proks P., Pearson E.R., Temple I.K., Mackay D.J.G., Shield J.P.H., Freedenberg D., Noyes K., Ellard S., Ashcroft F.M., Gribble F.M., Hattersley A.T. Hum. Mol. Genet. 14:925-934(2005) [PubMed] [Europe PMC] [Abstract] Cited for: VARIANTS TNDM3 SER-53; ARG-53 AND VAL-182, CHARACTERIZATION OF VARIANTS TNDM3 SER-53; ARG-53 AND VAL-182. |
| [26] | "KCNJ11 activating mutations in Italian patients with permanent neonatal diabetes." The early onset diabetes study group of the Italian society of pediatric endocrinology and diabetes Massa O., Iafusco D., D'Amato E., Gloyn A.L., Hattersley A.T., Pasquino B., Tonini G., Dammacco F., Zanette G., Meschi F., Porzio O., Bottazzo G., Crino A., Lorini R., Cerutti F., Vanelli M., Barbetti F. Hum. Mutat. 25:22-27(2005) [PubMed] [Europe PMC] [Abstract] Cited for: VARIANTS PNDM PRO-50; MET-59; ARG-170; ASN-170 AND CYS-201. |
| [27] | "Genotype-phenotype correlations in children with congenital hyperinsulinism due to recessive mutations of the adenosine triphosphate-sensitive potassium channel genes." Henwood M.J., Kelly A., MacMullen C., Bhatia P., Ganguly A., Thornton P.S., Stanley C.A. J. Clin. Endocrinol. Metab. 90:789-794(2005) [PubMed] [Europe PMC] [Abstract] Cited for: VARIANTS HHF2 ASP-101; ALA-134; LEU-136; LEU-266 AND HIS-301. |
| [28] | "The C42R mutation in the Kir6.2 (KCNJ11) gene as a cause of transient neonatal diabetes, childhood diabetes, or later-onset, apparently type 2 diabetes mellitus." Yorifuji T., Nagashima K., Kurokawa K., Kawai M., Oishi M., Akazawa Y., Hosokawa M., Yamada Y., Inagaki N., Nakahata T. J. Clin. Endocrinol. Metab. 90:3174-3178(2005) [PubMed] [Europe PMC] [Abstract] Cited for: VARIANT TNDM3 ARG-42, CHARACTERIZATION OF VARIANT TNDM3 ARG-42. |
| [29] | "Severe congenital hyperinsulinism caused by a mutation in the Kir6.2 subunit of the adenosine triphosphate-sensitive potassium channel impairing trafficking and function." Marthinet E., Bloc A., Oka Y., Tanizawa Y., Wehrle-Haller B., Bancila V., Dubuis J.-M., Philippe J., Schwitzgebel V.M. J. Clin. Endocrinol. Metab. 90:5401-5406(2005) [PubMed] [Europe PMC] [Abstract] Cited for: VARIANT HHF2 ARG-259, CHARACTERIZATION OF VARIANT HHF2 ARG-259. |
| [30] | "Mutations at the same residue (R50) of Kir6.2 (KCNJ11) that cause neonatal diabetes produce different functional effects." Shimomura K., Girard C.A.J., Proks P., Nazim J., Lippiat J.D., Cerutti F., Lorini R., Ellard S., Hattersely A.T., Barbetti F., Ashcroft F.M. Diabetes 55:1705-1712(2006) [PubMed] [Europe PMC] [Abstract] Cited for: VARIANTS PNDM GLN-50 AND PRO-50, CHARACTERIZATION OF VARIANTS PNDM GLN-50 AND PRO-50. |
| [31] | "Mutations in KCNJ11, which encodes Kir6.2, are a common cause of diabetes diagnosed in the first 6 months of life, with the phenotype determined by genotype." Flanagan S.E., Edghill E.L., Gloyn A.L., Ellard S., Hattersley A.T. Diabetologia 49:1190-1197(2006) [PubMed] [Europe PMC] [Abstract] Cited for: VARIANTS PNDM TYR-46; GLN-50; ARG-52; ASP-53; GLY-59; MET-59; PRO-164; TYR-166; THR-170; CYS-201; HIS-201; LEU-201; LEU-296 AND SER-330. |
| [32] | "Mutation spectra of ABCC8 gene in Spanish patients with Hyperinsulinism of Infancy (HI)." Fernandez-Marmiesse A., Salas A., Vega A., Fernandez-Lorenzo J.R., Barreiro J., Carracedo A. Hum. Mutat. 27:214-214(2006) [PubMed] [Europe PMC] [Abstract] Cited for: VARIANTS LYS-23 AND VAL-337. |
| [33] | "A novel KCNJ11 mutation associated with congenital hyperinsulinism reduces the intrinsic open probability of beta-cell ATP-sensitive potassium channels." Lin Y.-W., MacMullen C., Ganguly A., Stanley C.A., Shyng S.-L. J. Biol. Chem. 281:3006-3012(2006) [PubMed] [Europe PMC] [Abstract] Cited for: VARIANT HHF2 LEU-55, CHARACTERIZATION OF VARIANT HHF2 LEU-55. |
| [34] | "Molecular and immunohistochemical analyses of the focal form of congenital hyperinsulinism." Suchi M., MacMullen C.M., Thornton P.S., Adzick N.S., Ganguly A., Ruchelli E.D., Stanley C.A. Mod. Pathol. 19:122-129(2006) [PubMed] [Europe PMC] [Abstract] Cited for: VARIANTS HHF2 ASP-40; ASP-101; PRO-116; LEU-136 AND HIS-301. |
| [35] | "Prevalence of permanent neonatal diabetes in Slovakia and successful replacement of insulin with sulfonylurea therapy in KCNJ11 and ABCC8 mutation carriers." Stanik J., Gasperikova D., Paskova M., Barak L., Javorkova J., Jancova E., Ciljakova M., Hlava P., Michalek J., Flanagan S.E., Pearson E., Hattersley A.T., Ellard S., Klimes I. J. Clin. Endocrinol. Metab. 92:1276-1282(2007) [PubMed] [Europe PMC] [Abstract] Cited for: VARIANTS PNDM TYR-46; PRO-164 AND HIS-201. |
| + | Additional computationally mapped references. |
Web resources
Cross-references
Sequence databases | |
|---|---|
| EMBL GenBank DDBJ | 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. |
| PIR | A57616. |
| RefSeq | NP_001159762.1. NM_001166290.1. |
| UniGene | Hs.248141. |
3D structure databases | |
| ProteinModelPortal | Q14654. |
| SMR | Q14654. Positions 32-356. |
| ModBase | Search... |
| MobiDB | Search... |
Protein-protein interaction databases | |
| DIP | DIP-58643N. |
| IntAct | Q14654. 1 interaction. |
| STRING | 9606.ENSP00000345708. |
Chemistry | |
| BindingDB | Q14654. |
| ChEMBL | CHEMBL2095198. |
| DrugBank | DB01119. Diazoxide. DB01016. Glibenclamide. DB00222. Glimepiride. DB00308. Ibutilide. DB00922. Levosimendan. DB01252. Mitiglinide. DB00731. Nateglinide. DB00912. Repaglinide. DB00661. Verapamil. |
| GuidetoPHARMACOLOGY | 442. |
PTM databases | |
| PhosphoSite | Q14654. |
Polymorphism databases | |
| DMDM | 76803775. |
Proteomic databases | |
| PaxDb | Q14654. |
| PRIDE | Q14654. |
Protocols and materials databases | |
| StructuralBiologyKnowledgebase | Search... |
Genome annotation databases | |
| Ensembl | ENST00000339994; ENSP00000345708; ENSG00000187486. ENST00000528731; ENSP00000434755; ENSG00000187486. |
| GeneID | 3767. |
| KEGG | hsa:3767. |
| UCSC | uc001mnb.4. human. |
Organism-specific databases | |
| CTD | 3767. |
| GeneCards | GC11M017406. |
| H-InvDB | HIX0035982. |
| HGNC | HGNC:6257. KCNJ11. |
| HPA | HPA048891. |
| MIM | 600937. gene. 601820. phenotype. 606176. phenotype. 610582. phenotype. |
| neXtProt | NX_Q14654. |
| Orphanet | 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. 552. MODY syndrome. 99885. Permanent neonatal diabetes mellitus. 99886. Transient neonatal diabetes mellitus. |
| PharmGKB | PA217. |
| GenAtlas | Search... |
Phylogenomic databases | |
| eggNOG | NOG72812. |
| HOGENOM | HOG000237325. |
| HOVERGEN | HBG006178. |
| InParanoid | Q14654. |
| KO | K05004. |
| OrthoDB | EOG7XPZ5K. |
| TreeFam | TF313676. |
Enzyme and pathway databases | |
| Reactome | REACT_111217. Metabolism. REACT_13685. Neuronal System. |
| SignaLink | Q14654. |
Gene expression databases | |
| ArrayExpress | Q14654. |
| Bgee | Q14654. |
| CleanEx | HS_KCNJ11. |
| Genevestigator | Q14654. |
Family and domain databases | |
| Gene3D | 2.60.40.1400. 1 hit. |
| 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. [Graphical view] |
| PANTHER | PTHR11767. PTHR11767. 1 hit. |
| Pfam | PF01007. IRK. 1 hit. [Graphical view] |
| PIRSF | PIRSF005465. GIRK_kir. 1 hit. |
| PRINTS | PR01332. KIR62CHANNEL. PR01320. KIRCHANNEL. |
| SUPFAM | SSF81296. SSF81296. 1 hit. |
| ProtoNet | Search... |
Other | |
| ChiTaRS | KCNJ11. human. |
| GeneWiki | Kir6.2. |
| GenomeRNAi | 3767. |
| NextBio | 14771. |
| PRO | Q14654. |
| SOURCE | Search... |
Entry information
| Entry name | IRK11_HUMAN | ||||||||
| Accession | Primary (citable) accession number: Q14654 Secondary accession number(s): B4DWI4 Q8IW96 | ||||||||
| Entry history |
| ||||||||
| Entry status | 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. | ||||||||
Relevant documents
| SIMILARITY comments Index of protein domains and families |
| MIM cross-references Online Mendelian Inheritance in Man (MIM) cross-references in UniProtKB/Swiss-Prot |
| Human polymorphisms and disease mutations Index of human polymorphisms and disease mutations |
| Human entries with polymorphisms or disease mutations List of human entries with polymorphisms or disease mutations |
| Human chromosome 11 Human chromosome 11: entries, gene names and cross-references to MIM |