Effect of the α2C-adrenoreceptor deletion322–325 variant on sympathetic activity and cardiovascular measures in healthy subjects

Kurnik, Daniel; Muszkat, Mordechai; Friedman, Eitan A.; Sofowora, Gbenga G.; Diedrich, André; Xie, Hong‐Guang; Harris, Paul A.; Choi, Leena; Wood, Alastair J.J.

doi:10.1097/hjh.0b013e328017f6e9

Cited by 16 publications

(18 citation statements)

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“…5 However, larger studies found no associations between the ADRA2C deletion and markers of elevated resting sympathetic tone, blood pressure, or heart rate. 10,22 Variable results regarding the association between the ADRA2C deletion variant and cardiac function 14,23 suggest that the functional effects of the deletion variant may be most apparent in circumstances of substantially elevated sympathetic tone (eg, after yohimbine administration or in advanced congestive heart failure), and only in subjects who are homozygous for the deletion. 10,24 Another approach to examine the functional consequences of the ADRA2C deletion is to administer an ␣ 2 -AR agonist.…”

Section: Discussionmentioning

confidence: 99%

“…10,22 Variable results regarding the association between the ADRA2C deletion variant and cardiac function 14,23 suggest that the functional effects of the deletion variant may be most apparent in circumstances of substantially elevated sympathetic tone (eg, after yohimbine administration or in advanced congestive heart failure), and only in subjects who are homozygous for the deletion. 10,24 Another approach to examine the functional consequences of the ADRA2C deletion is to administer an ␣ 2 -AR agonist. A small study in healthy white Europeans found no effects of the deletion variant on blood pressure, heart rate, and plasma norepinephrine responses to clonidine, but among the 9 subjects carrying the deletion allele, only 3 were homozygous.…”

Section: Discussionmentioning

confidence: 99%

“…The ADRA2C del322-325 variant was genotyped by DNA fragment analysis as described previously, 10 and the GNB3 C825T polymorphism (rs5443) was performed by allelic discrimination with TaqMan 5Ј-nuclease assays. 11 Further details are available in the online supplement (please see http://hyper.ahajournals.org).…”

Section: Genotypingmentioning

confidence: 99%

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Ethnic and Genetic Determinants of Cardiovascular Response to the Selective α ₂ -Adrenoceptor Agonist Dexmedetomidine

et al. 2008

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Abstract-The ␣ 2 -adrenoceptor agonist clonidine reduces blood pressure more effectively in White than Black Americans despite similar degrees of sympatholysis. Functional genetic variation in receptor signaling mechanisms, for example in the ␤3 G-protein subunit (GNB3 C825T) and in the ␣ 2C -adrenoceptor subtype (ADRA2C del322-325), may affect drug responses. We examined the hypothesis that there are ethnic differences in the responses to the highly selective ␣ 2 -agonist, dexmedetomidine, and that these genetic variants contribute to interindividual variability in drug responses. In a placebo-controlled, single-masked study, 73 healthy subjects (37 whites and 36 blacks) received 3 placebo infusions and then 3 incremental doses of dexmedetomidine (cumulative dose, 0.4 g/kg), each separated by 30 minutes. Blood pressure, heart rate, and plasma catecholamine concentrations were determined after each infusion. We measured dexmedetomidine concentrations after the last infusion and determined ADRA2C del322-325 and GNB3 C825T genotypes. Dexmedetomidine lowered blood pressure and plasma catecholamine concentrations significantly (all PϽ0.001). There was substantial interindividual variability in the reduction of systolic blood pressure (range, 1 to 34 mm Hg) and plasma norepinephrine concentrations (range, 24 to 424 pg/mL). However, there were no differences between black and white subjects in dexmedetomidine responses (PϾ0.16 for all outcomes) before or after adjustment for covariates. Neither ADRA2C del322-325 nor GNB3 C825T genotypes affected the responses to dexmedetomidine (all PϾ0.66). There is large interindividual variability in response to the selective ␣ 2 -AR agonist dexmedetomidine, and neither ethnicity nor ADRA2C and GNB3 genotypes contribute to it. Further studies to identify determinants of ␣ 2 -AR-mediated responses will be of interest. Key Words: cardiovascular physiology Ⅲ receptors, adrenergic, ␣-2 Ⅲ G-protein beta3 subunit Ⅲ dexmedetomidine Ⅲ pharmacogenetics Ⅲ ethnic groups ␣ 2 -Adrenoceptors (␣ 2 -ARs) in the central nervous system and on presynaptic sympathetic nerve terminals play a key role in the regulation of the sympathetic response and thus cardiovascular control. The systemic administration of an ␣ 2 -AR agonist causes a reduction in sympathetic tone resulting in a decrease in blood pressure and heart rate, and the ␣ 2 -AR agonist clonidine is widely used as antihypertensive medication. There is, however, substantial interindividual variability in response to ␣ 2 -AR agonists, and black hypertensive patients achieved blood pressure control with clonidine monotherapy less often than whites. 1,2 Concordant with that observation, we found that clonidine reduced blood pressure less in healthy black subjects than white subjects, despite similar decreases in norepinephrine spillover. 3 The reasons for these ethnic differences remain unclear.Functionally significant genetic variants of ␣ 2 -ARs and other proteins in their signaling pathways have been identified. The prevalence of these allelic...

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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Ethnic and Genetic Determinants of Cardiovascular Response to the Selective α ₂ -Adrenoceptor Agonist Dexmedetomidine

et al. 2008

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“…In theory, the reduced activity of the ␣ 2C -AR, with the deletion of amino acids 322 to 325, should lead to a reduced inhibition of NE release from the presynaptic nerve terminals and ultimately result in increased adrenergic drive. However, in healthy persons, basal parameters of the sympathetic nervous system, including heart rate, heart rate variability, blood pressure, and concentrations of NE and EPI were not affected by this variant (Table 4) (Kurnik et al, 2007). Intravenous administration of the ␣ 2 -agonist dexmedetomidine to healthy subjects results in blood pressure lowering and a decrease in plasma catecholamine concentrations.…”

Section: B ␣ 2 -Adrenergic Receptor Ligandsmentioning

confidence: 99%

Pharmacogenomics of G Protein-Coupled Receptor Ligands in Cardiovascular Medicine

Rosskopf

Michel²

2008

Pharmacol Rev

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“…These mice develop clinical signs of HF such as pulmonary edema associated with severe ventricular dysfunction at 7 months of age, when the mortality rate is 50.0% 12,17 . The gene inactivation of the α 2A and α 2C adrenergic receptors leads to an increase in the release of circulating noradrenaline 18,19 . Therefore, the HF observed in this model results from sympathetic nervous system hyperactivity.…”

Section: Samplementioning

confidence: 99%

Associação de betabloqueadores e treinamento físico na insuficiência cardíaca de camundongos

Vanzelli

Medeiros

Sirvente

et al. 2010

Arq. Bras. Cardiol.

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Effect of the α2C-adrenoreceptor deletion322–325 variant on sympathetic activity and cardiovascular measures in healthy subjects

Abstract: The ADRA2C deletion polymorphism had no effect on markers of resting sympathetic activity and cardiovascular measures, and did not account for ethnic differences in blood pressure.

Cited by 16 publications

References 45 publications

Ethnic and Genetic Determinants of Cardiovascular Response to the Selective α ₂ -Adrenoceptor Agonist Dexmedetomidine

Ethnic and Genetic Determinants of Cardiovascular Response to the Selective α ₂ -Adrenoceptor Agonist Dexmedetomidine

Pharmacogenomics of G Protein-Coupled Receptor Ligands in Cardiovascular Medicine

Associação de betabloqueadores e treinamento físico na insuficiência cardíaca de camundongos

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Effect of the α2C-adrenoreceptor deletion322–325 variant on sympathetic activity and cardiovascular measures in healthy subjects

Abstract: The ADRA2C deletion polymorphism had no effect on markers of resting sympathetic activity and cardiovascular measures, and did not account for ethnic differences in blood pressure.

Cited by 16 publications

References 45 publications

Ethnic and Genetic Determinants of Cardiovascular Response to the Selective α 2 -Adrenoceptor Agonist Dexmedetomidine

Ethnic and Genetic Determinants of Cardiovascular Response to the Selective α 2 -Adrenoceptor Agonist Dexmedetomidine

Pharmacogenomics of G Protein-Coupled Receptor Ligands in Cardiovascular Medicine

Associação de betabloqueadores e treinamento físico na insuficiência cardíaca de camundongos

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Product

Resources

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Ethnic and Genetic Determinants of Cardiovascular Response to the Selective α ₂ -Adrenoceptor Agonist Dexmedetomidine

Ethnic and Genetic Determinants of Cardiovascular Response to the Selective α ₂ -Adrenoceptor Agonist Dexmedetomidine