Recombinant Mouse Potassium voltage-gated channel subfamily KQT member 1 (Kcnq1)

1. Our data indicate that mouse embryonic stem cells are induced into islet-like cells in vitro. The gene imprinting status of Kcnq1 and Cdkn1c may be changed in differentiated cells during the induction in vitro. PMID: 28926866
2. Collectively, the authors propose that Prmt1-dependent facilitation of KCNQ-phosphatidylinositol-4,5-bisphosphate interaction underlies the positive regulation of KCNQ activity by arginine methylation, which may serve as a key target for prevention of neuronal hyperexcitability and seizures. PMID: 27466704
3. we investigated the effects of KCNQ1 A340E, a loss-of-function mutant. J343 mice bearing KCNQ1 A340E demonstrated a much higher 24-h intake of electrolytes (potassium, sodium, and chloride). KCNQ1, therefore, is suggested to play a central role in electrolyte metabolism. KCNQ1 A340E, with the loss-of-function phenotype, may dysregulate electrolyte homeostasis PMID: 27525866
4. Loss of methylation at the Kcnq1 imprinted gDMD was strongly associated with trophoblast giant cell (TGC) expansion. PMID: 26241757
5. Data show that disruption of potassium voltage-gated channel, KQT-like subfamily Q, member1 (KCNQ1) results in increased expression of cyclin-dependent kinase inhibitor 1C (Cdkn1c) only when the mutation is on the paternal allele. PMID: 26100882
6. S3 mutations in KCNQ1 cause diverse kinetic defects in I(Ks), affecting opening and closing properties, and can account for LQT1 phenotypes. PMID: 25444851
7. Characterization of the imprinted Kcnq1 domain which contains a differentially methylated region in intron 11 of Kcnq1. PMID: 25539921
8. KCNQ1, KCNE2, and SMIT1 form reciprocally regulating complexes that affect neuronal excitability. PMID: 24595108
9. low expression of KCNQ1 expression was significantly associated with poor overall survival. PMID: 23975432
10. Which participates in the allelic repression of Kcnq1. PMID: 24395636
11. H(+)-K(+)-ATPase/KCNQ1 reside in independent intracytoplasmic membrane compartments, or membrane domains, and upon activation of parietal cells, both membrane proteins are transported, possibly via Rab11-positive recycling endosomes, to apical membranes. PMID: 23154976
12. our studies reveal regulatory mechanisms within the Kcnq1 imprinted domain that operate exclusively in the heart on Kcnq1 a gene crucial for heart development and function. PMID: 23028363
13. Expression of KCNQ1 and NKCC1 protein in the stria vascularis of C57BL/6J mice decreases with age. PMID: 21426709
14. We showed the disturbance of parietal cell differentiation and mucous neck-to-zymogenic cell lineage differentiation with enhanced expression of KCNQ1 in the parietal cells. PMID: 20437101
15. Data show that in early pregnant mouse myometrium, the relative abundance of mRNA expression was KCNQ3 > KCNQ4 > KCNQ5 > KCNQ1 > KCNQ2. PMID: 20132415
16. Kcnq1 is expressed in the cell membrane of thyroid follicular cells and plays a significant role in thyroid function. plasma concentrations of T3/T4 are lower in Kcnq1 knockout mice than in their wild-type littermates PMID: 20978783
17. Repression of the paternal allele of several imprinted genes (including Kcnq1) on distal chromosome 7 is regulated by a non-coding antisense transcript, Kcnq1ot1, which is paternally expressed. PMID: 17021040
18. KCNQ1 loss-of-function mutation impairs gastric acid secretion in mice. PMID: 19306073
19. Data suggest that because the abundance and subcellular localization of KCNQ1 was unchanged in kcne3(-/-) mice, the modification of biophysical properties of KCNQ1 by KCNE3 is essential for its role in intestinal and tracheal transport. PMID: 20051516
20. Loss of Igf2 imprinting in monoclonal mouse hepatic tumor cells is not associated with abnormal methylation patterns for the H19 and Igf2 differentially methylated regions. PMID: 12475990
21. KCNQ1 and beta2-ARs associate and have a role in modulating the function of IKs channels under conditions of increased beta2-AR expression PMID: 15272004
22. Kcnq1 mutant mice are a powerful new tool for investigating the connection between acid balance, Helicobacter infection and mucin disruption in the progression to gastric cancer. PMID: 15385447
23. NF-Y transcription factor as a crucial regulator of antisense promoter-mediated bidirectional silencing and the parent of origin-specific epigenetic marks at the Kcnq1 imprinting control region PMID: 15459184
24. Based upon previous studies and the present results, it is concluded that both hKCNE4 and mKCNE4 have a drastic inhibitory impact on both hKCNQ1 and mKCNQ1 currents. PMID: 15707997
25. Kcnq1 knockout mice show histopathology comparable to that reported in human temporal bone cases of Jervell and Lange-Nielsen syndrome and provide further evidence that KCNQ1 channel dysfunction can lead to congenital deafness in this syndrome. PMID: 15891643
26. luminal KCNQ1 serves to repolarize the proximal tubule and stabilize the driving force for Na+ reabsorption PMID: 16314573
27. KCNQ1 has cell-specific roles in renal ion transport and may participate in K(+) secretion and/or absorption PMID: 16896189
28. Murine blood vessels exhibit a distinctive expression profile of KCNQ1, KCNQ4, and KCNQ5, with 'neuronal' KCNQ4 dominating PMID: 17519950
29. These results demonstrate for the first time that Kcnq1 protein is expressed in adult mouse hearts where it contributes to a beta-adrenergic-induced component of I(SS) that does not require co-assembly with Kcne1. PMID: 17597584
30. The Kcnq1 mutation in vtg-2J mice alters various physiological functions in the cardiac, gastric and adrenocortical systems. PMID: 17660684
31. We conclude that fenofibrate inhibits intestinal cAMP-stimulated Cl(-) secretion through a nongenomic mechanism that involves a selective inhibition of basolateral KCNQ1/KCNE3 channel complexes. PMID: 17916649
32. These results suggest that although it is expressed in nearly all taste bud cells, the function of KCNQ1 is not required for gross taste bud development or peripheral taste transduction pathways. PMID: 19006182
33. The mutation of KCNQ1 potassium channel did not affect the channel kinetics, whereas the surface expression increased with increasing hydrophobicity of the middle amino aicd residue. PMID: 19041715
34. The effect of APC in the regulation of gastric acid secretion requires H+/K+ ATPase activity and is at least partially due to SGK1-dependent upregulation of KCNQ1. PMID: 19255508
35. The observations indicate that KCNQ1 is a novel molecule affecting insulin sensitivity of glucose metabolism. PMID: 19369585
36. A 166 kb region near the Kcnq1 transcriptionally imprinted domain showed high recombination activity. PMID: 19439080
37. KCNQ1 channel provides K(+) to the extracellular K(+) binding site of the H(+)/K(+)-ATPase during acid secretion, and no other gastric K(+) channel can substitute for this function. PMID: 19491250

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KEGG: mmu:16535

STRING: 10090.ENSMUSP00000009689

UniGene: Mm.439769