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  1. Publikacije
  2. Heritable Influence of DBH on Adrenergic and Renal Function: Twin and Disease Studies
izvor podataka: crosbi

Heritable Influence of DBH on Adrenergic and Renal Function: Twin and Disease Studies (CROSBI ID 204322)

Prilog u časopisu | izvorni znanstveni rad | međunarodna recenzija

Pasha, Dalal N. ; Davis, Jason T. ; Rao, Fangwen ; Chen, Yuqing ; Wen, Gen ; Fung, Maple M. ; Mahata, Manjula ; Zhang, Kuixing ; Trzebinska, Danuta ; Mustapić, Maja et al. Heritable Influence of DBH on Adrenergic and Renal Function: Twin and Disease Studies // PLoS One, 8 (2013), 12; e82956, 10. doi: 10.1371/journal.pone.0082956

Podaci o odgovornosti

Pasha, Dalal N. ; Davis, Jason T. ; Rao, Fangwen ; Chen, Yuqing ; Wen, Gen ; Fung, Maple M. ; Mahata, Manjula ; Zhang, Kuixing ; Trzebinska, Danuta ; Mustapić, Maja ; Hightower, C. Makena ; Lipkowitz, Michael S. ; Ji, Ming ; Ziegler, Michael G. ; Nievergelt, Caroline M. ; O'Connor, Daniel T.

engleski

Heritable Influence of DBH on Adrenergic and Renal Function: Twin and Disease Studies

Abstract Background: Elevated sympathetic activity is associated with kidney dysfunction. Here we used twin pairs to probe heritability of GFR and its genetic covariance with other traits. Methods: We evaluated renal and adrenergic phenotypes in twins. GFR was estimated by CKD-EPI algorithm. Heritability and genetic covariance of eGFR and associated risk traits were estimated by variance- components. Meta-analysis probed reproducibility of DBH genetic effects. Effect of DBH genetic variation on renal disease was tested in the NIDDK-AASK cohort. Results: Norepinephrine secretion rose across eGFR tertiles while eGFR fell (p, 0.0001). eGFR was heritable, at h2= 67.364.7% (p = 3.0E-18), as were secretion of norepinephrine (h2= 66.565.0%, p = 3.2E-16) and dopamine (h2= 56.565.6%, p = 1.8E-13), and eGFR displayed genetic co-determination (covariance) with norepinephrine (rG=20.55760.088, p = 1.11E- 08) as well as dopamine (rG=20.22360.101, p = 2.3E-02). Since dopamine b-hydroxylase (DBH) catalyzes conversion of dopamine to norepinephrine, we studied functional variation at DBH ; DBH promoter haplotypes predicted transcriptional activity (p, 0.001), plasma DBH (p, 0.0001) and norepinephrine (p = 0.0297) secretion ; transcriptional activity was inversely (p, 0.0001) associated with basal eGFR. Meta- analysis validated DBH haplotype effects on eGFR across 3 samples. In NIDDK-AASK, we established a role for DBH promoter variation in long-term renal decline rate (GFR slope, p = 0.003). Conclusions: The heritable GFR trait shares genetic determination with catecholamines, suggesting new pathophysiologic, diagnostic and therapeutic approaches towards disorders of GFR as well as CKD. Adrenergic activity may play a role in progressive renal decline, and genetic variation at DBH may assist in profiling subjects for rational preventive treatment.

Glomerular filtration rate ; GFR ; dopamine beta-hydroxylase ; DBH ; chronic kidney disease ; CKD ; norepinephrine ; twin pair ; heritability ; genetic covariance

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Podaci o izdanju

8 (12)

2013.

e82956

10

objavljeno

1932-6203

10.1371/journal.pone.0082956

Povezanost rada

Povezane osobe
Maja Mustapić (autor/i)

Biologija, Temeljne medicinske znanosti

Poveznice
doi.org
journals.plos.org
doi.org
fulir.irb.hr
Indeksiranost
Scopus
Medline
Web of Science Core Collection, Science Citation Index Expanded (WoSCC-SCI-Exp)
Web of Science Core Collection, SCI-Exp, SSCI & A&HCI (WoSCC-SCI-Exp, SSCI, A&HCI)
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