Chronic β1‐adrenoceptor antagonist treatment sensitizes β2‐adrenoceptors, but desensitizes M2‐muscarinic receptors in the human right atrium

Motomura, Shigeru; Deighton, N. M.; Zerkowski, H.–R.; Doetsch, N.; Michel, Martin C.; Brodde, Otto‐Erich

doi:10.1111/j.1476-5381.1990.tb12715.x

Cited by 79 publications

(38 citation statements)

References 35 publications

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“…None of the observed differences between groups before, during, and after treatment is statistically significant. adenylate cyclase activity were enhanced in right atria from patients that had been treated with 13l-selective adrenoceptor antagonists (Motomura et al, 1990). Similar findings have also been obtained in canine hearts where removal of the endogenous agonists by cardiac denervation also enhanced adenylate cyclase responsiveness (Vatner et al, 1985).…”

Section: Prostaglandin Elsupporting

confidence: 73%

Does treatment with beta‐adrenoceptor antagonists in vivo alter human adenylate cyclase responsiveness in vitro?

Michel

Klüppel

Philipp

et al. 1991

Brit J Clinical Pharma

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1. Treatment with beta‐adrenoceptor antagonists in vivo can alter adenylate cyclase responsiveness in the human heart. We have determined the effects of treatment with four different beta‐adrenoceptor antagonists in vivo on the responsiveness of lymphocyte and platelet adenylate cyclase in vitro in healthy volunteers. 2. Propranolol (non‐ selective, 4 x 40 mg day), bisoprolol (beta 1‐selective, 1 x 10 mg day), and ICI 118.551 (beta 2‐selective, 3 x 25 mg day) were tested as drugs without and pindolol (non‐selective, 2 x 5 mg day) as a drug with intrinsic sympathomimetic activity. Adenylate cyclase stimulation by GTP, prostaglandin E1 and forskolin was determined before, after a 7 day treatment period and 7 days after drug withdrawal. 3. Neither treatment with or withdrawal of any of the beta‐adrenoceptor antagonists altered adenylate cyclase responsiveness. 4. We conclude that adenylate cyclase responsiveness in circulating blood cells underlies different regulatory mechanisms than that in solid tissues such as the human heart. Our data suggest that circulating blood cells do not always reflect alterations in solid tissues.

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Section: Prostaglandin Elsupporting

confidence: 73%

Does treatment with beta‐adrenoceptor antagonists in vivo alter human adenylate cyclase responsiveness in vitro?

Michel

Klüppel

Philipp

et al. 1991

Brit J Clinical Pharma

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“…Since the most important property of carvedilol is antioxidative profile and nebivolol predominantly effects nitric oxide (NO) pathway, the common protective pathway of nebivolol and carvedilol could be the intrinsinc beta blocker properties coupled to antioxidant and NO release. Previous studies showed that patients treated with β1-selective antagonists without intrinsic sympathomimetic activity (ISA) had more adrenoceptors than control subjects [44] and that the adenylate cyclase activation by the β-adrenoceptor agonist isoprenaline is also enhanced in this situation [45]. The ISA is therefore an important criterion for the therapeutical usefulness of BBs in heart failure patients.…”

Section: Discussionmentioning

confidence: 99%

Animal study of Anthracycline-induced Cardiotoxicity and Nephrotoxicity and Evaluation of Protective Agents

Shafik¹,

Khodeir²,

Fadel³

2011

JCST

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Study background: Anticancer chemotherapy Anthracycline (ANT) antibiotics associated with cardiac and renal toxicity which represents serious complication. In this study, the protective effect of the 2 beta-blockers carvedilol and nebivolol were tested in a rat model of ANT induced cardio and renal-toxicity by repeated intraperitoneal doxorubicin (Dox) administration.Methods: Six groups of animals were used, each 8 rats divided as control group-received intraperitoneal saline every other day; control carvedilol: rats received carvedilol dose 30mg/kg/day orally; control nebivolol: rats received nebivolol 1mg/kg/day orally; doxorubicin alone: a dose of 3 mg/kg/day was administered intraperitoneal every other day; doxorubicin + carvedilol: carvedilol started at the same day with Dox; doxorubicin + nebivolol: nebivolol started at the same day with Dox. All substances were administered for 12 days. Detection & quantification of doxorubicin-induced heart and renal damage and therapeutic action of beta-blockers was done using Langendorff's technique, echo-cardiographic function examinations, serum creatinine, total proteins and histopathology.

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“…In fact, some β-1 AR blockers such as metoprolol or bisoprolol have been shown to up-regulate β-AR in the heart of patients with CHF (Gilbert et al 1996;Heilbrunn et al 1989;Sigmund et al 1996;Waagstein et al 1989). Interestingly, several studies in patients with coronary artery disease have shown that chronic treatment with β-1 AR selective blockers such as metoprolol, atenolol or bisoprolol sensitizes cardiac β-2 AR function in vitro (Hall et al 1990;Motomura et al 1990) and in vivo (Hall et al 1991). Whether this occurs also in CHF patients and whether this may contribute to the beneficial effects of β-1 AR blockers in these patients is still a matter of debate.…”

Section: Effects On β-Adrenoceptor Densitymentioning

confidence: 99%

β-adrenoceptor blocker treatment and the cardiac β-adrenoceptor-G-protein(s)-adenylyl cyclase system in chronic heart failure

Brodde

2007

Naunyn-Schmied Arch Pharmacol

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Chronic β₁‐adrenoceptor antagonist treatment sensitizes β₂‐adrenoceptors, but desensitizes M₂‐muscarinic receptors in the human right atrium

Cited by 79 publications

References 35 publications

Does treatment with beta‐adrenoceptor antagonists in vivo alter human adenylate cyclase responsiveness in vitro?

Does treatment with beta‐adrenoceptor antagonists in vivo alter human adenylate cyclase responsiveness in vitro?

Animal study of Anthracycline-induced Cardiotoxicity and Nephrotoxicity and Evaluation of Protective Agents

β-adrenoceptor blocker treatment and the cardiac β-adrenoceptor-G-protein(s)-adenylyl cyclase system in chronic heart failure

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