Entity Details

Primary name SCNN1B
Entity type gene
Source Source Link

Details

PrimaryID6338
RefseqGeneNG_011908
SymbolSCNN1B
Namesodium channel epithelial 1 subunit beta
Chromosome16
Location16p12.2
TaxID9606
Statuslive
SourceGenomegenomic
SourceOriginnatural
CreationDate1998-12-04
ModificationDate2021-06-13

Ontological Relatives

UniProt IDsSCNNB_HUMAN

GO terms

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GOName
GO:0002269 leukocyte activation involved in inflammatory response
GO:0002283 neutrophil activation involved in immune response
GO:0005886 plasma membrane
GO:0005887 integral component of plasma membrane
GO:0006814 sodium ion transport
GO:0007588 excretion
GO:0009897 external side of plasma membrane
GO:0010467 gene expression
GO:0014824 artery smooth muscle contraction
GO:0015280 ligand-gated sodium channel activity
GO:0016324 apical plasma membrane
GO:0030659 cytoplasmic vesicle membrane
GO:0032094 response to food
GO:0032341 aldosterone metabolic process
GO:0034101 erythrocyte homeostasis
GO:0034220 ion transmembrane transport
GO:0034706 sodium channel complex
GO:0035264 multicellular organism growth
GO:0035725 sodium ion transmembrane transport
GO:0042045 epithelial fluid transport
GO:0042493 response to drug
GO:0050699 WW domain binding
GO:0050891 multicellular organismal water homeostasis
GO:0050909 sensory perception of taste
GO:0055075 potassium ion homeostasis
GO:0055078 sodium ion homeostasis
GO:0070062 extracellular exosome
GO:0070254 mucus secretion
GO:0070944 neutrophil-mediated killing of bacterium
GO:0097274 urea homeostasis
GO:0098797 plasma membrane protein complex
GO:1904045 cellular response to aldosterone

Diseases

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Disease IDSourceNameDescription
177200 OMIMLiddle syndrome 1 (LIDLS1)A form of Liddle syndrome, an autosomal dominant disorder characterized by early onset of hypertension, hypokalemic alkalosis, and suppression of plasma renin activity and aldosterone secretion. The disease is caused by variants affecting the gene represented in this entry.
211400 OMIMBronchiectasis with or without elevated sweat chloride 1 (BESC1)A debilitating respiratory disease characterized by chronic, abnormal dilatation of the bronchi and other cystic fibrosis-like symptoms in the absence of known causes of bronchiectasis (cystic fibrosis, autoimmune diseases, ciliary dyskinesia, common variable immunodeficiency, foreign body obstruction). Clinical features include sub-normal lung function, sinopulmonary infections, chronic productive cough, excessive sputum production, and elevated sweat chloride in some cases. The disease is caused by variants affecting the gene represented in this entry.
264350 OMIMPseudohypoaldosteronism 1, autosomal recessive (PHA1B)A rare salt wasting disease resulting from target organ unresponsiveness to mineralocorticoids. PHA1B is a severe form involving multiple organ systems, and characterized by an often fulminant presentation in the neonatal period with dehydration, hyponatremia, hyperkalemia, metabolic acidosis, failure to thrive and weight loss. The disease is caused by variants affecting the gene represented in this entry. The degree of channel function impairment differentially affects the renin-aldosterone system and urinary Na/K ratios, resulting in distinct genotype-phenotype relationships in PHA1 patients. Loss-of-function mutations are associated with a severe clinical course and age-dependent hyperactivation of the renin-aldosterone system. This feature is not observed in patients with missense mutations that reduce but do not eliminate channel function. Markedly reduced channel activity results in impaired linear growth and delayed puberty (PubMed:18634878).