Mechanism of coronary microvascular responses to metabolic stimulation

doi:10.1016/S0008-6363(97)00096-5

Cardiovascular Research 1997 35(1):148-157; doi:10.1016/S0008-6363(97)00096-5
© 1997 by European Society of Cardiology

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Mechanism of coronary microvascular responses to metabolic stimulation

Richard P Embrey^a, Leonard A Brooks^b and Kevin C Dellsperger^b^,*

^aDepartment of Surgery, University of Iowa, Iowa City, IA 52242, USA
^bDepartment of Internal Medicine and the Cardiovascular Center, University of Iowa, and VA Medical Center, Iowa City, IA 52246, USA

^* Corresponding author. Tel.: +1 (319) 339-7102; fax: +1 (319) 339 7135.

Previous studies from our laboratory have shown that coronarymicrovascular dilation to increased myocardial oxygen consumption(MVO₂) is greater in vessels <100 µm. The mechanismresponsible for this response is uncertain. Objectives: We testedthe hypothesis that microvascular dilation to increased MVO₂is mediated by nitric oxide (NO). Since NO release may occurin response to increased shear, we also tested the hypothesisthat metabolic byproducts released in response to increasesin MVO₂ will stimulate opening of the ATP-sensitive potassiumchannel. Methods: Changes in epicardial coronary microvasculardiameters were measured in 9 dogs given N^G-nitro-L-arginine(LNNA; 100 µM, topically), 7 dogs given glibenclamide(10 µM, topically) and 12 control (C) dogs during increasesin metabolic demand using dobutamine (DOB, 10 µg/kg/min,i.v.) with rapid atrial pacing (PAC, 300 bpm). Diameters ofarterioles were measured using intravital microscopy coupledto stroboscopic epi-illumination. Results: During the protocol,MVO₂ increased to a similar degree in both experimental groups(LNNA and glibenclamide). Baseline hemodynamics and coronarymicrovascular diameters were similar between the two experimentalgroups and their respective control groups. In the presenceof LNNA, coronary arteriolar (<100 µm) dilation (%change from baseline) was impaired during the protocol (DOB:vehicle 18±5, LNNA 2±2 [P<0.05]; DOB+RAP: vehicle40±11, LNNA 6±2% [P<0.05]). In contrast, glibenclamidedid not impair coronary microvascular responses to increasedMVO₂ despite similar increases in MVO₂. Conclusion: This studyindicates that coronary microvascular dilation in response toincreased metabolic stimulation using dobutamine in conjunctionwith rapid pacing is mediated through a nitric-oxide-dependentmechanism and not ATP-sensitive potassium channels. These resultsmay have important implications in pathological disease stateswhere nitric oxide mechanisms are impaired, such as diabetesand hypertension.

KEYWORDS Coronary microcirculation; Dobutamine; EDRF; Arginine analogs; Glibenclamide; Potassium channel, ATP-sensitive; Nitric oxide; Endothelium; Intravital microscopy

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