ACE inhibitor potentiation of bradykinin‐induced venoconstriction

Hecker, Markus; Blaukat, Andree; Bara, Agnieszka T.; Müller‐Esterl, Werner; Busse, Rudi

doi:10.1038/sj.bjp.0701281

Cited by 57 publications

(50 citation statements)

References 31 publications

(43 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…This interpretation is in agreement with binding studies in which it was also found that there were no alterations in B 2 receptor affinity in the presence of ACE inhibitors. 15,18 In only 1 model of transfected Chinese hamster ovary cells expressing the human B 2 receptor and ACE genes was an increase in the density and affinity of BK binding reported in the presence of enalaprilat. 14 This effect was dependent on the presence of ACE, and it occurred only when enalaprilat was applied in concentrations substantially higher than those needed for the inhibition of the enzymatic activity of ACE, 14 a condition that was not investigated in the present study.…”

Section: Discussionmentioning

confidence: 99%

“…In the rat heart, the influence of kininase inhibitors on local kinin concentrations has been established in tracer transit studies that demonstrated a marked increase in kinin concentrations during ACE inhibition specifically in an extravascular distribution compartment. 6 Additional observations have been made suggesting that some of the kinin potentiation properties of ACE inhibitors might be related to mechanisms independent of the inhibition of kinin degradation; for example, (1) ACE inhibitors act as kinin mimetics under conditions in which kinin breakdown should be negligible, 10 (2) ACE inhibitors can enhance the effects of degradation-resistant BK analogs, [11][12][13][14] (3) ACE inhibitors show structure-related differences in their kinin potentiation activities, 15 and (4) ACE inhibitors can provoke a kinin-mediated response even when B 2 receptors have been desensitized through kinin pretreatment. 11,13 The last phenomenon is addressed further here as "receptor resensitization."…”

mentioning

confidence: 99%

“…In addition to inhibition of BK breakdown, ACE inhibitors could act directly on B 2 receptors or their signal transduction by increasing receptor affinity, preventing receptor internalization, or enhancing second-messenger activation. 14,15 However, none of these mechanisms have ever been demonstrated in a physiological model that can reveal the classic consequences of kinin potentiation, namely a leftward shift in the BK dose-response curve.…”

mentioning

confidence: 99%

See 2 more Smart Citations

Potentiation of the Vascular Response to Kinins by Inhibition of Myocardial Kininases

et al. 2000

View full text Add to dashboard Cite

Abstract-Inhibitors of angiotensin I-converting enzyme (ACE) are very efficacious in the potentiation of the actions of bradykinin (BK) and are able to provoke a B 2 receptor-mediated vasodilation even after desensitization of this receptor. Because this activity cannot be easily explained only by an inhibition of kinin degradation, direct interactions of ACE inhibitors with the B 2 receptor or its signal transduction have been hypothesized. To clarify the significance of degradation-independent potentiation, we studied the vasodilatory effects of BK and 2 degradation-resistant B 2 receptor agonists in the isolated rat heart, a model in which ACE and aminopeptidase P (APP) contribute equally to the degradation of BK. Coronary vasodilation to BK and to a peptidic (B6014) and a nonpeptidic (FR190997) degradation-resistant B 2 agonist was assessed in the presence or absence of the ACE inhibitor ramiprilat, the APP inhibitor mercaptoethanol, or both. Ramiprilat or mercaptoethanol induced leftward shifts in the BK dose-response curve (EC 50 ϭ3.4 nmol/L) by a factor of 4.6 or 4.9, respectively. Combined inhibition of ACE and APP reduced the EC 50 of BK to 0.18 nmol/L (ie, by a factor of 19) but potentiated the activity of B6014 (EC 50 ϭ1.9 nmol/L) only weakly without altering that of FR190997 (EC 50 ϭ0.34 nmol/L). Desensitization of B 2 receptors was induced by the administration of BK (0.2 mol/L) or FR190997 (0.1 mol/L) for 30 minutes; the vascular reactivity to ramiprilat or increasing doses of BK was tested thereafter. After desensitization with BK, but not FR190997, an additional application of ramiprilat provoked a B 2 receptor-mediated vasodilation. High BK concentrations were still effective at the desensitized receptor. The process of desensitization was not altered by ramiprilat. These results show that in this model, all potentiating actions of ACE inhibitors on kinin-induced vasodilation are exclusively related to the reduction in BK breakdown and are equivalently provoked by APP inhibition. The desensitization of B 2 receptors is overcome by increasing BK concentrations, either directly or through the inhibition of ACE. These observations do not suggest any direct interactions of ACE inhibitors with the B 2 receptor or its signal transduction but point to a very high activity of BK degradation in the vicinity of the B 2 receptor in combination with a stimulation-dependent reduction in receptor affinity. (Hypertension. 2000;35:32-37.)Key Words: bradykinin Ⅲ angiotensin-converting enzyme Ⅲ receptor, bradykinin Ⅲ rats Ⅲ heart I nhibitors of angiotensin I-converting enzyme (ACE) have been proved to be clinically effective against diseases such as hypertension, congestive heart failure, and myocardial infarction. Through their main mechanism of action (ie, inhibition of the peptidase ACE), ACE inhibitors not only prevent the activation of angiotensin I but also eliminate a degradation pathway for the vasodilatory peptide bradykinin (BK) and thus increase the availability and effectiveness of kinins. The results...

show abstract

Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

mentioning

confidence: 99%

See 1 more Smart Citation

Potentiation of the Vascular Response to Kinins by Inhibition of Myocardial Kininases

et al. 2000

View full text Add to dashboard Cite

show abstract

“…110 For this reason ACEis have diverse effects independent of their BP-lowering effect (Figure 2). Indeed, different ACEis like moexiprilate, ramipirilate, captopril, enalpril and quinaprilate amplified the effects of bradykinin in vessels that lacked measurable ACE activity 154 and also enhanced the effect of an ACE-resistant B 2 -kinin receptor agonist. These findings demonstrate that ACEis selectively potentiate the B 2 -receptor-mediated vascular effects of bradykinin independently of their ACE-inhibiting properties, and this might be related to differences in molecular structure.…”

Section: Looking Beyond Ace Inhibitionmentioning

confidence: 99%

“…These findings demonstrate that ACEis selectively potentiate the B 2 -receptor-mediated vascular effects of bradykinin independently of their ACE-inhibiting properties, and this might be related to differences in molecular structure. 154,155 ACEis also induce cross-talk between the transmembrane protein ACE and the B 2 -kinin receptor, probably by formation of a heterodimer. This protects high-affinity receptors, blocks receptor desensitization and decreases internalization, thereby potentiating BK beyond blocking its hydrolysis.…”

Section: Looking Beyond Ace Inhibitionmentioning

confidence: 99%

Reinventing the ACE inhibitors: some old and new implications of ACE inhibition

2009

View full text Add to dashboard Cite

Since their inception, angiotensin-converting enzyme (ACE) inhibitors have been used as first-line therapy for the treatment of cardiovascular and renal diseases. They restore the balance between the vasoconstrictive salt-retentive and hypertrophy-causing peptide angiotensin II (Ang II) and bradykinin, a vasodilatory and natriuretic peptide. As ACE is a promiscuous enzyme, ACE inhibitors alter the metabolism of a number of other vasoactive substances. ACE inhibitors decrease systemic vascular resistance without increasing heart rate and promote natriuresis. They have been proven effective in the treatment of hypertension, and reduce mortality in congestive heart failure and left ventricular dysfunction after myocardial infarction. They inhibit ischemic events and stabilize plaques. Furthermore, they delay the progression of diabetic nephropathy and neuropathy and act as antioxidants. Ongoing studies have elucidated protective roles for them in both memory-related disorders and cancer. INTRODUCTIONIn recent years, stressful and fiercely competitive lifestyles and food habits have compounded the problems of hypertension. Long-standing and stressful, progressively rising hypertension can lead to many disorders, including myocardial infarction (MI), cerebrovascular events, congestive heart failure, peripheral arterial insufficiency, premature mortality 1 and renal dysfunction leading to glomerulosclerosis and kidney artery aneurysm. 2 A number of therapies are available, but angiotensin-converting enzyme (ACE) inhibitors have been the preferred first-line therapy for hypertension, congestive heart failure, left ventricular (LV) systolic dysfunction and MI. 3,4 ACE inhibitors (ACEis) have been in use for the past two decades, and the interest in them is still growing. Recently, the discovery of domain-selective ACEis and new members of the renin-angiotensin system (RAS) (that is, angiotensin-converting enzyme 2) have again fueled the interest of researchers. Some new studies have expanded the already impressive clinical profile of ACEis. This review traces some already known and new facets of ACE inhibition and introduces new advances in the designing of a new generation of ACEis.

show abstract