2001
DOI: 10.1161/01.hyp.37.6.1473
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Normal Blood Pressure and Renal Function in Mice Lacking the Bradykinin B 2 Receptor

Abstract: Abstract-Telemetric blood pressure determinations, heart rate measurements, and pressure-natriuresis-diuresis experiments were used to characterize cardiovascular and renal function in bradykinin B 2 receptor knockout mice fed mouse chow containing 0.25% NaCl or mouse chow containing 4% NaCl. In B 2 receptor knockout mice fed usual mouse chow, the mean arterial blood pressure leveled between 108Ϯ1 and 110Ϯ3 mm Hg, and the heart rate leveled between 520Ϯ26 and 525Ϯ29 bpm, values that were not different from tho… Show more

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Cited by 58 publications
(34 citation statements)
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References 36 publications
(46 reference statements)
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“…Indeed, the only obvious cardiac abnormality that we found in B 2 Ϫ/Ϫ mice is a lower heart rate compared with that of WT mice after both saline and dipyridamole infusion. This bradycardia contrasts with previous studies in B 2 Ϫ/Ϫ mice showing either normal 8,9,18 or increased heart rate values. 3-5,19 -21 The bradycardia presently observed is, however, consistent with the suppression of the classical effects of centrally or peripherally administered bradykinin, ie, tachycardia 22,23 and stimulation of the sympathetic system, 24 -26 which are most likely related to an enhancement of norepinephrine release via a presynaptic B 2 receptor-dependent mechanism.…”
Section: Discussioncontrasting
confidence: 99%
See 1 more Smart Citation
“…Indeed, the only obvious cardiac abnormality that we found in B 2 Ϫ/Ϫ mice is a lower heart rate compared with that of WT mice after both saline and dipyridamole infusion. This bradycardia contrasts with previous studies in B 2 Ϫ/Ϫ mice showing either normal 8,9,18 or increased heart rate values. 3-5,19 -21 The bradycardia presently observed is, however, consistent with the suppression of the classical effects of centrally or peripherally administered bradykinin, ie, tachycardia 22,23 and stimulation of the sympathetic system, 24 -26 which are most likely related to an enhancement of norepinephrine release via a presynaptic B 2 receptor-dependent mechanism.…”
Section: Discussioncontrasting
confidence: 99%
“…Thus, the lack of B 2 receptor has been reported to induce either permanent [3][4][5] or transient hypertension, 6 to induce no hypertension unless the mice are fed a high-salt diet, 7,8 or to never induce hypertension, even on high salt intake. 9 These discrepancies may be explained in part by differences in the genetic background of B 2 Ϫ/Ϫ mice, which was 129Sv, 129SvEvTac, or C57BL/6. More problematic, they could also result from the fact that control mice were not littermates but mice issued from separate strains chosen to match the genetic background of B 2 Ϫ/Ϫ mice.…”
mentioning
confidence: 99%
“…Basic parameters, including body, heart, and kidney weights, as well as blood pressure, plasma glucose, food intake, urine volume, and daily excretion of albumin, were determined for each animal ( Table 1). Comparison of the singly mutant B2 receptor knockout males with their wild-type littermates showed that the receptor knockout animals do not differ significantly from wild type in any of these parameters, which is in general agreement with a previous report (11) for the same null mutation. Heterozygous males for the dominant Akita mutation (Akita diabetic) have severe diabetes at 6 months of age with 38.8 Ϯ 1.9 mmol͞liter (698 Ϯ 34 mg͞dl) plasma glucose.…”
Section: Resultssupporting
confidence: 91%
“…Together, these findings suggested that a high‐salt diet enhanced NHE3 expression but did not elevate BP because of suppressed aldosterone and decreased intestinal ENaC expression. Although the tail‐cuff method that we used to measure BP in this study might not be able to detect slight differences, this lack of BP elevation under salt loading alone is consistent with the results of previous studies that used radiotelemetry to measure BP after a high‐salt diet and reported no increase in BP 26, 39. Although NHE3 expression in the distal colon was significantly lower in IEC‐MR‐KO than control mice, intestinal sodium absorption was similar in the 2 genotypes.…”
Section: Discussionsupporting
confidence: 89%