Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
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Gene/Protein
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Target Concepts:
Gene/Protein
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Query: UNIPROT:P01185 (
vasopressin
)
23,126
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
PYRIN- and CARD-containing proteins belong to a recently identified protein family involved in the regulation of apoptosis and inflammatory processes. Variations in the gene products of the family members PYPAF1 and NOD2/CARD15 have been associated with several autoinflammatory diseases. We could identify the mouse orthologs of PYPAF1,
PYPAF5
, NOD1, NOD2 and the rat ortholog of
PYPAF5
. Intriguingly, we found that
PYPAF5
has been reported previously not only as regulator of NF-kappaB and caspase-1, but also as angiotensin II and
vasopressin
receptor. In particular, based on a comprehensive sequence analysis, we propose a structural model for this hormone receptor that is different from the model suggested previously.
...
PMID:Identification of mammalian orthologs associates PYPAF5 with distinct functional roles. 1263 74
The angiotensin-
vasopressin
receptor (AVR) responds with equivalent affinities to angiotensin II (ANG II) and
vasopressin
and is coupled to adenylate cyclase and hence a V2-type
vasopressin
receptor. AVR maps to the Nalp6 locus and overlaps with the larger Nalp6/
PYPAF5
reported to be a T cell/granulocyte-specific, cytoplasmic-specific proapoptotic protein, thus questioning the existence of AVR. Here we confirm, through different experimental modalities, that AVR is distinct from Nalp6/
PYPAF5
based on different mRNA and protein sizes, subcellular localization, and tissue-specific expression patterns. Binding studies of
PYPAF5
-specific Cos1 transfectants detect high-affinity binding to
vasopressin
but not ANG II, thus assigning
PYPAF5
as a non-AVR (NAVR). Signaling array analysis reveals that AVP stimulation of AVR- and NAVR-specific Cos1 transfectants results in diametrical activation as well as coactivation of signaling pathways known to mediate renal sodium and water balance. Likewise, ANG II stimulation of Cos1-AVR transfectants reveals a signaling profile distinct from that of AVP-stimulated Cos1-AVR transfectants. Analysis of genomic organization of the AVR/NAVR locus shows an overlapping gene arrangement with alternative promoter usage resulting in different NH(2) termini for NAVR and AVR. In addition to core promoter elements, androgen and estrogen response elements are detected. Promoter analysis of NAVR/AVR 5'-regulatory region detects transcriptional upregulation by testosterone and synergistic upregulation by testosterone and estrogen, thus suggesting that AVR and/or NAVR contribute to sex-specific V2-type
vasopressin
-mediated effects. Altogether, confirmation of AVR and identification of NAVR as
vasopressin
receptors are concordant with emerging
vasopressin
functions not attributable to V1a, V1b, or V2 receptors and add molecular bases for the multifunctional complexity of
vasopressin
-mediated functions and regulation.
...
PMID:Overlapping genes in Nalp6/PYPAF5 locus encode two V2-type vasopressin isoreceptors: angiotensin-vasopressin receptor (AVR) and non-AVR. 1841 81
Coronary artery disease, heart failure, fatal arrhythmias, stroke, and renal disease are the most common causes of mortality for humans, and essential hypertension remains a major risk factor. Elucidation of susceptibility loci for essential hypertension has been difficult because of its complex, multifactorial nature involving genetic, environmental, and sex- and age-dependent nature. We investigated whether the 11p15.5 region syntenic to rat chromosome 1 region containing multiple blood pressure quantitative trait loci (QTL) detected in Dahl rat intercrosses harbors polymorphisms that contribute to susceptibility/resistance to essential hypertension in a Sardinian population. Initial testing performed using microsatellite markers spanning 18 Mb of 11p15.5 detected a strong association between D11S1318 (at 2.1 Mb, P = 0.004) and D11S1346 (at 10.6 Mb, P = 0.00000004), suggesting that loci in close proximity to these markers may contribute to susceptibility in our Sardinian cohort.
NLR family, pyrin domain containing 6
/angiotensin-
vasopressin
receptor (
NLRP6
/AVR), and adrenomedullin (ADM) are in close proximity to D11S1318 and D11S1346, respectively; thus we tested single nucleotide polymorphisms (SNPs) within
NLRP6
/AVR and ADM for their association with hypertension in our Sardinian cohort. Upon sex stratification, we detected one
NLRP6
/AVR SNP associated with decreased susceptibility to hypertension in males (rs7948797G, P = 0.029; OR = 0.73 [0.57-0.94]). For ADM, sex-specific analysis showed a significant association between rs4444073C, with increased susceptibility to essential hypertension only in the male population (P = 0.006; OR = 1.44 [1.13-1.84]). Our results revealed an association between
NLRP6
/AVR and ADM loci with male essential hypertension, suggesting the existence of sex-specific
NLRP6
/AVR and ADM variants affecting male susceptibility to essential hypertension.
...
PMID:Sex-specific effects of NLRP6/AVR and ADM loci on susceptibility to essential hypertension in a Sardinian population. 2414 25
