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Coronary Blood Flow and Myocardial Ischemia.pptx

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This document summarizes key concepts regarding coronary blood flow and myocardial ischemia from Braunwald's Heart Disease, 12th edition. It discusses how coronary blood flow is regulated and the determinants of myocardial oxygen demand. When oxygen supply and demand are disrupted by diseases affecting coronary blood flow, a vicious cycle of ischemia can result. Knowledge of coronary flow regulation, oxygen demand factors, and the relationship between ischemia and contraction is essential to understanding myocardial ischemia.

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Braunwald’s Heart Disease, 12th ed, Chapter 36 Coronary Blood Flow and Myocardial Ischemia Dirk J. Duncker, John M. Canity Jr.
“ ◦ The heart is responsible for generating the arterial pressure that is required to perfuse the systemic circulation and yet, at the same time, has its own perfusion impeded during the systolic phase of the cardiac cycle ◦ When the balance between oxygen supply and demand is acutely disrupted by diseases affecting coronary blood flow, the resulting imbalance can immediately precipitate a vicious cycle ◦ Knowledge of the regulation of coronary blood flow, determinants of myocardial oxygen consumption, and the relation between ischemia and contraction is essential Introduction
Control of Coronary Blood Flow
Control of Coronary Blood Flow ◦ Variation exists between coronary artery and venous flow between systole and diastole ◦ During systolic contraction: ◦ Tissue pressure increase  perfusion redistributed from subendocardium to epicardium  coronary arterial inflow impeded ◦ Reduced diameter of intramyocardial microcirculatory vessels  increased coronary venous outflow
Determinants of Myocardial Oxygen Consumption ◦ In contrast to most other vascular beds, myocardial oxygen extraction is near-maximal at rest, averaging 70% to 80% of arterial oxygen content. ◦ Coronary venous oxygen tension (PvO2) can only decrease from 25 mm Hg to approximately 15 mm Hg ◦ Increases in myocardial oxygen consumption are primarily met by proportional increases in coronary flow and oxygen delivery ◦ Major determinants: heart rate, systolic pressure (or myocardial wall stress), and left ventricular (LV) contractility
“
Coronary Autoregulation ◦ Regional coronary blood flow remains constant as coronary artery pressure is reduced below aortic pressure over a wide range when the determinants of myocardial oxygen consumption are kept constant ◦ Coronary flow reserve  The ability to increase flow above resting values in response to pharmacologic vasodilation
“
Coronary flow reserve… ◦ … is reduced when: ◦ diastolic time available for subendocardial perfusion is decreased (tachycardia) ◦ compressive determinants of diastolic perfusion (preload) are increased ◦ Also, by anything that increases resting flow: ◦ Increases in the hemodynamic determinants of oxygen consumption (systolic pressure, heart rate, and contractility) ◦ Reductions in arterial oxygen supply (anemia and hypoxia) ◦ Thus, circumstances can develop that precipitate subendocardial ischemia in the presence of normal coronary arteries
Transmural variations in coronary autoregulation ◦ Subendocardial flow occurs primarily in diastole and begins to decrease below a mean coronary pressure of 40 mmHg ◦ Subepicardial flow occurs throughout the cardiac cycle and is maintained until coronary pressure falls below 25 mm Hg
…continued ◦ This difference arises from increased oxygen consumption in the subendocardium, requiring a higher resting flow level, as well as the more pronounced effects of systolic contraction on subendocardial vasodilator reserve ◦ The transmural difference in the lower autoregulatory pressure limit results in vulnerability of the subendocardium to ischemia in the presence of a coronary stenosis
Determinants of Coronary Vascular Resistance Conduit resistance (R1)  negligible ◦ may contribute to increasing vascular resistance at hemodynamically significant (>50%) stenosis ◦ may reduce resting flow in severely narrowed (>90%) arteries Microcirculatory resistance (R2)  dynamic ◦ distributed across a broad range of microcirculatory vessel sizes ◦ changes in response to physical forces (intraluminal pressure and shear stress) as well as the metabolic needs of the tissue Extravascular compressive resistance (R3)  varies with time throughout the cardiac cycle ◦ related to cardiac contraction and systolic pressure development within the left ventricle ◦ also affected by elevated ventricular diastolic pressure in heart failure
Effects of extravascular tissue pressure on transmural perfusion ◦ Cardiac contraction raises extravascular tissue pressure to values equal to LV pressure at the subendocardium ◦ However, this does not account for accelerated venous outflow ◦ Concept of intramyocardial pump  microcirculatory vessels are compressed, producing a capacitive discharge of blood that accelerates flow to the coronary venous system
Endothelium-dependent Modulation of Coronary Tone ◦ Arterial diameter is modulated by a wide variety of paracrine factors  many are dependent on a functional endothelium ◦ Example: ◦ Acetylcholine normally dilates arteries through an endothelium-dependent relaxing factor (NO) ◦ NO increases cyclic GMP  relaxes vascular smooth muscle  vasodilation ◦ In the absence of a functional endothelium  muscarinic vascular smooth muscle contraction  vasoconstriction
Endothelium-dependent Biochemical Pathways ◦ Nitric Oxide ◦ Produced by the enzymatic conversion of L-arginine to citrulline via type III or endothelial nitric oxide synthase (eNOS) ◦ Binds to guanylyl cyclase  increasing cGMP production  relaxation through a reduction in intracellular calcium ◦ In CAD  oxidative stress  generation of superoxide anion  inactivation of NO ◦ Endothelium- Dependent Hyperpolarizing Factor (EDHF) ◦ Hyperpolarizes vascular smooth muscle and dilates arteries by opening calcium activated potassium channels (KCa) ◦ Prostacyclin ◦ Endothelin  potent vasoconstrictor
Paracrine Vasoactive Mediators ◦ Serotonin ◦ Thromboxane A2 ◦ Adenosine diphosphate (ADP) ◦ Thrombin
Coronary Vasospasm ◦ Most frequently occurs in the setting of a coronary stenosis ◦ Results in transient functional occlusion of a coronary artery that is reversible with nitrate vasodilation ◦ Impaired endothelium- dependent is not causal, and a trigger is required (e.g., thrombus formation, sympathetic activation)
Pharmacologic Vasodilation Nitroglycerin ◦ Dilates epicardial conduit arteries and small coronary resistance arteries ◦ Transient arteriolar vasodilation is overcome by autoregulatory escape  does not increase coronary blood flow ◦ Improves the distribution of perfusion to the subendocardium when flow-mediated NO-dependent vasodilation is impaired. CCBs ◦ Induce vascular smooth muscle relaxation  coronary vasodilators ◦ Submaximally vasodilate coronary resistance vessels  sometimes precipitate subendocardial ischemia in the presence of a critical stenosis (coronary steal)
Pharmacologic Vasodilation Adenosine ◦ Dilates coronary arteries through activation of A2 receptors independent of endothelium ◦ Direct effects related to resistance vessel size and restricted primarily to vessels smaller than 100 μm  larger arteries dilate through NO- dependent mechanism Dipyridamole ◦ Inhibits reuptake of adenosine  similar mechanism of action Papaverine ◦ Inhibits phosphodiesterase and increases cyclic adenosine monophosphate (cAMP)
Structure and Function of the Coronary Microcirculation ◦ Individual coronary resistance arteries are a longitudinally distributed network ◦ Considerable spatial heterogeneity of specific resistance vessel control mechanisms ◦ This can be accomplished independently of metabolic signals by ◦ Sensing physical forces such as intraluminal flow (shear stress–mediated control); or ◦ Intraluminal pressure changes (myogenic control).
21
Myogenic Response ◦ The ability of vascular smooth muscle to oppose changes in coronary arterial diameter ◦ ↓Distending pressure  relaxation, vice versa ◦ Depends on vascular smooth muscle calcium entry, perhaps through stretch- activated L- type Ca2+ channels Flow-Mediated Vasodilation ◦ Regulate their diameter in response to changes in local shear stress ◦ Endothelium dependent, mediated by NO
Physiologic Assessment of Coronary Artery Stenoses
Stenosis Pressure-Flow Relation ◦ The total pressure drop across a stenosis is governed by three hydrodynamic factors: ◦ Viscous losses; ◦ Separation losses; and ◦ Turbulence ◦ The most important determinant  minimum lesional crosssectional area within the stenosis
25 ◦ No significant pressure drop across a stenosis (ΔP) until stenosis severity exceeds 50% ◦ As stenosis severity exceeds 50%, the pressure flow relation becomes curvilinear ◦ Because of coronary autoregulation, resting flow remains constant as stenosis severity increases
Flow- and Pressure- Derived Indices of Coronary Reserve ◦ The development of invasive approaches to assess distal coronary pressure and flow using transducers placed on coronary guidewires have led to indices of coronary stenosis severity based on coronary flow reserve and resting and vasodilated distal coronary pressure ◦ Leading to more complete understanding of the role of epicardial coronary stenoses versus the coronary microcirculation in limiting myocardial perfusion
Absolute Flow Reserve ◦ The ratio of maximally vasodilated flow to the corresponding resting flow value in a specific region of the heart ◦ Altered by factors that affect maximal coronary flow and the corresponding resting flow value Relative Flow Reserve ◦ Relative differences in regional perfusion (per gram of tissue) assessed during maximal pharmacologic vasodilation ◦ Fairly insensitive to variations in mean arterial pressure, heart rate, and preload Perfusion/Flow-based Indices
Fractional Flow Reserve ◦ Based on the principle that the distal coronary pressure measured during vasodilation is directly proportional to maximum vasodilated perfusion ◦ An indirect index  driving pressure for microcirculatory flow distal to the stenosis relative to the coronary driving pressure available in the absence of a stenosis Instantaneous Wave-free Ratio ◦ The ratio of distal coronary pressure to aortic pressure averaged throughout mid-diastole (i.e., the “wave- free period”) ◦ Free of the compressive effects of systole and phasic coronary flow and the stenosis diastolic pressure gradient are maximal Pressure-based Indices
Pathophysiologic States Affecting Microcirculatory Coronary Flow Reserve Left Ventricular Hypertrophy ◦ Resting flow per gram of myocardium remains constant, increase in the absolute level of resting flow ◦ Pathologic hypertrophy does not result in appreciable vascular proliferation ◦ The increase in LV mass in the absence of vascular proliferation reduces the maximum perfusion per gram of myocardium
Pathophysiologic States Affecting Microcirculatory Coronary Flow Reserve Microvascular Dysfunction ◦ Flow per gram of myocardium will be normal at rest and reduced during pharmacologic vasodilation ◦ Absolute flow remains normal at rest in microvascular disease, and the absolute vasodilated flow is reduced
31 Endothelial Dysfunction and Coronary Flow Reserve • NO inactivation associated with risk factors for CAD  abnormal control of local resistance vessel through impaired endothelium-dependent vasodilation • Reversed with L-arginine
Coronary Collateral Circulation
Arteriogenesis and Angiogenesis ◦ Proliferation of coronary collaterals occurs in response to repetitive stress-induced ischemia and the development of transient interarterial pressure gradients  arteriogenesis ◦ In contrast to de novo vessel growth  angiogenesis  sprouting of smaller, capillary-like structures from preexisting blood vessels ◦ Progressive enlargement of collaterals happen through a process dependent on physical forces and growth factors  VEGF, mediated by NOS ◦ Thus, patients with impaired NO-mediated vasodilation may have a limited ability to develop coronary collaterals
Regulation of Collateral Resistance ◦ Collateral blood flow is governed by a series resistance arising from interarterial collateral anastomoses  major determinant of perfusion ◦ Collaterals constrict when NO synthesis is blocked, which aggravates myocardial ischemia  overcome by nitroglycerin
Metabolic And Functional Consequences of Ischemia
Irreversible Injury and Myocyte Death ◦ Irreversible myocardial injury begins after 20 minutes of coronary occlusion in the absence of significant collaterals ◦ Starts in the subendocardium and progresses as a wavefront over time, to the subepicardial layers.
Cardioprotection from Local and Remote Conditioning ◦ Brief reversible ischemia preceding a prolonged coronary occlusion reduced infarct size, a phenomenon termed acute preconditioning ◦ Myocardial postconditioning  the ability to engage cardiac protection by producing intermittent ischemia or administering pharmacologic agonists at reperfusion ◦ Remote conditioning is particularly attractive because it can be easily implemented using a blood pressure cuff and has been shown to experimentally reduce infarct size ◦ Nevertheless, large randomized clinical trials of postconditioning and remote conditioning have failed to translate these into measurable impacts on clinical end points or infarct size
38
Reversible Ischemia and Perfusion- Contraction Matching ◦ Reductions in subendocardial flow are closely related to reductions in regional contractile function of the heart
Functional Consequences of Reversible Ischemia ◦ Late consequences of ischemia have been documented after normal myocardial perfusion is reestablished ◦ In the most chronic state, they result in hibernating myocardium  characterized by chronic contractile dysfunction and regional cellular mechanisms that downregulate contractile and metabolic function of the heart so as to protect it from irreversible injury
Stunned Myocardium ◦ Myocardial function normalizes rapidly after single episodes of ischemia lasting less than 2 minutes ◦ Regional myocardial function remains depressed for up to 6 hours after resolution of ischemia following a 15- minute occlusion  myocardial stunning ◦ Function remains depressed while resting  dissociation of the usual close relation between subendocardial flow and function
Chronic Hibernating Myocardium ◦ Viable dysfunctional myocardium  any myocardial region in which contractile function improves after coronary revascularization ◦ Chronically stunned  When resting flow relative to a remote region is normal in dysfunctional myocardium distal to a stenosis ◦ Hibernating myocardium  When relative resting flow is reduced in the absence of symptoms or signs of ischemia
Cellular Responses in Hibernating Myocardium Apoptosis, Myocyte Loss, and Myofibrillar Loss ◦ Approximately 30% regional myocytes undergo apoptosis Cell Survival and Antiapoptotic Program in Response to Repetitive Ischemia ◦ Upregulation of antiapoptotic proteins in patients without HF Metabolism and Energetics in Hibernating Myocardium ◦ Once adapted, the metabolic and contractile response of hibernating myocardium appears to be dissociated from external determinants of workload Inhomogeneity in Sympathetic Innervation, Beta- Adrenergic Responses, and Sudden Death ◦ The contractile response of hibernating myocardium is blunted  regional downregulation in beta- adrenergic adenylyl cyclase coupling 43
44 Conclusion and Future Directions • The major factors determining myocardial perfusion and oxygen delivery have been incorporated into the current management of angina and have withstood the test of time • Important gaps remain in basic knowledge and in the translation of this knowledge to clinical care • Our understanding of the physiologic and cellular mechanisms responsible for microvascular dysfunction is limited • Continued bench-to-bedside translational investigation in these and other areas is needed
Thank You

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Coronary Blood Flow and Myocardial Ischemia.pptx

  • 1. Braunwald’s Heart Disease, 12th ed, Chapter 36 Coronary Blood Flow and Myocardial Ischemia Dirk J. Duncker, John M. Canity Jr.
  • 2. “ ◦ The heart is responsible for generating the arterial pressure that is required to perfuse the systemic circulation and yet, at the same time, has its own perfusion impeded during the systolic phase of the cardiac cycle ◦ When the balance between oxygen supply and demand is acutely disrupted by diseases affecting coronary blood flow, the resulting imbalance can immediately precipitate a vicious cycle ◦ Knowledge of the regulation of coronary blood flow, determinants of myocardial oxygen consumption, and the relation between ischemia and contraction is essential Introduction
  • 4. Control of Coronary Blood Flow ◦ Variation exists between coronary artery and venous flow between systole and diastole ◦ During systolic contraction: ◦ Tissue pressure increase  perfusion redistributed from subendocardium to epicardium  coronary arterial inflow impeded ◦ Reduced diameter of intramyocardial microcirculatory vessels  increased coronary venous outflow
  • 5. Determinants of Myocardial Oxygen Consumption ◦ In contrast to most other vascular beds, myocardial oxygen extraction is near-maximal at rest, averaging 70% to 80% of arterial oxygen content. ◦ Coronary venous oxygen tension (PvO2) can only decrease from 25 mm Hg to approximately 15 mm Hg ◦ Increases in myocardial oxygen consumption are primarily met by proportional increases in coronary flow and oxygen delivery ◦ Major determinants: heart rate, systolic pressure (or myocardial wall stress), and left ventricular (LV) contractility
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  • 7. Coronary Autoregulation ◦ Regional coronary blood flow remains constant as coronary artery pressure is reduced below aortic pressure over a wide range when the determinants of myocardial oxygen consumption are kept constant ◦ Coronary flow reserve  The ability to increase flow above resting values in response to pharmacologic vasodilation
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  • 9. Coronary flow reserve… ◦ … is reduced when: ◦ diastolic time available for subendocardial perfusion is decreased (tachycardia) ◦ compressive determinants of diastolic perfusion (preload) are increased ◦ Also, by anything that increases resting flow: ◦ Increases in the hemodynamic determinants of oxygen consumption (systolic pressure, heart rate, and contractility) ◦ Reductions in arterial oxygen supply (anemia and hypoxia) ◦ Thus, circumstances can develop that precipitate subendocardial ischemia in the presence of normal coronary arteries
  • 10. Transmural variations in coronary autoregulation ◦ Subendocardial flow occurs primarily in diastole and begins to decrease below a mean coronary pressure of 40 mmHg ◦ Subepicardial flow occurs throughout the cardiac cycle and is maintained until coronary pressure falls below 25 mm Hg
  • 11. …continued ◦ This difference arises from increased oxygen consumption in the subendocardium, requiring a higher resting flow level, as well as the more pronounced effects of systolic contraction on subendocardial vasodilator reserve ◦ The transmural difference in the lower autoregulatory pressure limit results in vulnerability of the subendocardium to ischemia in the presence of a coronary stenosis
  • 12. Determinants of Coronary Vascular Resistance Conduit resistance (R1)  negligible ◦ may contribute to increasing vascular resistance at hemodynamically significant (>50%) stenosis ◦ may reduce resting flow in severely narrowed (>90%) arteries Microcirculatory resistance (R2)  dynamic ◦ distributed across a broad range of microcirculatory vessel sizes ◦ changes in response to physical forces (intraluminal pressure and shear stress) as well as the metabolic needs of the tissue Extravascular compressive resistance (R3)  varies with time throughout the cardiac cycle ◦ related to cardiac contraction and systolic pressure development within the left ventricle ◦ also affected by elevated ventricular diastolic pressure in heart failure
  • 13. Effects of extravascular tissue pressure on transmural perfusion ◦ Cardiac contraction raises extravascular tissue pressure to values equal to LV pressure at the subendocardium ◦ However, this does not account for accelerated venous outflow ◦ Concept of intramyocardial pump  microcirculatory vessels are compressed, producing a capacitive discharge of blood that accelerates flow to the coronary venous system
  • 14. Endothelium-dependent Modulation of Coronary Tone ◦ Arterial diameter is modulated by a wide variety of paracrine factors  many are dependent on a functional endothelium ◦ Example: ◦ Acetylcholine normally dilates arteries through an endothelium-dependent relaxing factor (NO) ◦ NO increases cyclic GMP  relaxes vascular smooth muscle  vasodilation ◦ In the absence of a functional endothelium  muscarinic vascular smooth muscle contraction  vasoconstriction
  • 15. Endothelium-dependent Biochemical Pathways ◦ Nitric Oxide ◦ Produced by the enzymatic conversion of L-arginine to citrulline via type III or endothelial nitric oxide synthase (eNOS) ◦ Binds to guanylyl cyclase  increasing cGMP production  relaxation through a reduction in intracellular calcium ◦ In CAD  oxidative stress  generation of superoxide anion  inactivation of NO ◦ Endothelium- Dependent Hyperpolarizing Factor (EDHF) ◦ Hyperpolarizes vascular smooth muscle and dilates arteries by opening calcium activated potassium channels (KCa) ◦ Prostacyclin ◦ Endothelin  potent vasoconstrictor
  • 16. Paracrine Vasoactive Mediators ◦ Serotonin ◦ Thromboxane A2 ◦ Adenosine diphosphate (ADP) ◦ Thrombin
  • 17. Coronary Vasospasm ◦ Most frequently occurs in the setting of a coronary stenosis ◦ Results in transient functional occlusion of a coronary artery that is reversible with nitrate vasodilation ◦ Impaired endothelium- dependent is not causal, and a trigger is required (e.g., thrombus formation, sympathetic activation)
  • 18. Pharmacologic Vasodilation Nitroglycerin ◦ Dilates epicardial conduit arteries and small coronary resistance arteries ◦ Transient arteriolar vasodilation is overcome by autoregulatory escape  does not increase coronary blood flow ◦ Improves the distribution of perfusion to the subendocardium when flow-mediated NO-dependent vasodilation is impaired. CCBs ◦ Induce vascular smooth muscle relaxation  coronary vasodilators ◦ Submaximally vasodilate coronary resistance vessels  sometimes precipitate subendocardial ischemia in the presence of a critical stenosis (coronary steal)
  • 19. Pharmacologic Vasodilation Adenosine ◦ Dilates coronary arteries through activation of A2 receptors independent of endothelium ◦ Direct effects related to resistance vessel size and restricted primarily to vessels smaller than 100 μm  larger arteries dilate through NO- dependent mechanism Dipyridamole ◦ Inhibits reuptake of adenosine  similar mechanism of action Papaverine ◦ Inhibits phosphodiesterase and increases cyclic adenosine monophosphate (cAMP)
  • 20. Structure and Function of the Coronary Microcirculation ◦ Individual coronary resistance arteries are a longitudinally distributed network ◦ Considerable spatial heterogeneity of specific resistance vessel control mechanisms ◦ This can be accomplished independently of metabolic signals by ◦ Sensing physical forces such as intraluminal flow (shear stress–mediated control); or ◦ Intraluminal pressure changes (myogenic control).
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  • 22. Myogenic Response ◦ The ability of vascular smooth muscle to oppose changes in coronary arterial diameter ◦ ↓Distending pressure  relaxation, vice versa ◦ Depends on vascular smooth muscle calcium entry, perhaps through stretch- activated L- type Ca2+ channels Flow-Mediated Vasodilation ◦ Regulate their diameter in response to changes in local shear stress ◦ Endothelium dependent, mediated by NO
  • 24. Stenosis Pressure-Flow Relation ◦ The total pressure drop across a stenosis is governed by three hydrodynamic factors: ◦ Viscous losses; ◦ Separation losses; and ◦ Turbulence ◦ The most important determinant  minimum lesional crosssectional area within the stenosis
  • 25. 25 ◦ No significant pressure drop across a stenosis (ΔP) until stenosis severity exceeds 50% ◦ As stenosis severity exceeds 50%, the pressure flow relation becomes curvilinear ◦ Because of coronary autoregulation, resting flow remains constant as stenosis severity increases
  • 26. Flow- and Pressure- Derived Indices of Coronary Reserve ◦ The development of invasive approaches to assess distal coronary pressure and flow using transducers placed on coronary guidewires have led to indices of coronary stenosis severity based on coronary flow reserve and resting and vasodilated distal coronary pressure ◦ Leading to more complete understanding of the role of epicardial coronary stenoses versus the coronary microcirculation in limiting myocardial perfusion
  • 27. Absolute Flow Reserve ◦ The ratio of maximally vasodilated flow to the corresponding resting flow value in a specific region of the heart ◦ Altered by factors that affect maximal coronary flow and the corresponding resting flow value Relative Flow Reserve ◦ Relative differences in regional perfusion (per gram of tissue) assessed during maximal pharmacologic vasodilation ◦ Fairly insensitive to variations in mean arterial pressure, heart rate, and preload Perfusion/Flow-based Indices
  • 28. Fractional Flow Reserve ◦ Based on the principle that the distal coronary pressure measured during vasodilation is directly proportional to maximum vasodilated perfusion ◦ An indirect index  driving pressure for microcirculatory flow distal to the stenosis relative to the coronary driving pressure available in the absence of a stenosis Instantaneous Wave-free Ratio ◦ The ratio of distal coronary pressure to aortic pressure averaged throughout mid-diastole (i.e., the “wave- free period”) ◦ Free of the compressive effects of systole and phasic coronary flow and the stenosis diastolic pressure gradient are maximal Pressure-based Indices
  • 29. Pathophysiologic States Affecting Microcirculatory Coronary Flow Reserve Left Ventricular Hypertrophy ◦ Resting flow per gram of myocardium remains constant, increase in the absolute level of resting flow ◦ Pathologic hypertrophy does not result in appreciable vascular proliferation ◦ The increase in LV mass in the absence of vascular proliferation reduces the maximum perfusion per gram of myocardium
  • 30. Pathophysiologic States Affecting Microcirculatory Coronary Flow Reserve Microvascular Dysfunction ◦ Flow per gram of myocardium will be normal at rest and reduced during pharmacologic vasodilation ◦ Absolute flow remains normal at rest in microvascular disease, and the absolute vasodilated flow is reduced
  • 31. 31 Endothelial Dysfunction and Coronary Flow Reserve • NO inactivation associated with risk factors for CAD  abnormal control of local resistance vessel through impaired endothelium-dependent vasodilation • Reversed with L-arginine
  • 33. Arteriogenesis and Angiogenesis ◦ Proliferation of coronary collaterals occurs in response to repetitive stress-induced ischemia and the development of transient interarterial pressure gradients  arteriogenesis ◦ In contrast to de novo vessel growth  angiogenesis  sprouting of smaller, capillary-like structures from preexisting blood vessels ◦ Progressive enlargement of collaterals happen through a process dependent on physical forces and growth factors  VEGF, mediated by NOS ◦ Thus, patients with impaired NO-mediated vasodilation may have a limited ability to develop coronary collaterals
  • 34. Regulation of Collateral Resistance ◦ Collateral blood flow is governed by a series resistance arising from interarterial collateral anastomoses  major determinant of perfusion ◦ Collaterals constrict when NO synthesis is blocked, which aggravates myocardial ischemia  overcome by nitroglycerin
  • 36. Irreversible Injury and Myocyte Death ◦ Irreversible myocardial injury begins after 20 minutes of coronary occlusion in the absence of significant collaterals ◦ Starts in the subendocardium and progresses as a wavefront over time, to the subepicardial layers.
  • 37. Cardioprotection from Local and Remote Conditioning ◦ Brief reversible ischemia preceding a prolonged coronary occlusion reduced infarct size, a phenomenon termed acute preconditioning ◦ Myocardial postconditioning  the ability to engage cardiac protection by producing intermittent ischemia or administering pharmacologic agonists at reperfusion ◦ Remote conditioning is particularly attractive because it can be easily implemented using a blood pressure cuff and has been shown to experimentally reduce infarct size ◦ Nevertheless, large randomized clinical trials of postconditioning and remote conditioning have failed to translate these into measurable impacts on clinical end points or infarct size
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  • 39. Reversible Ischemia and Perfusion- Contraction Matching ◦ Reductions in subendocardial flow are closely related to reductions in regional contractile function of the heart
  • 40. Functional Consequences of Reversible Ischemia ◦ Late consequences of ischemia have been documented after normal myocardial perfusion is reestablished ◦ In the most chronic state, they result in hibernating myocardium  characterized by chronic contractile dysfunction and regional cellular mechanisms that downregulate contractile and metabolic function of the heart so as to protect it from irreversible injury
  • 41. Stunned Myocardium ◦ Myocardial function normalizes rapidly after single episodes of ischemia lasting less than 2 minutes ◦ Regional myocardial function remains depressed for up to 6 hours after resolution of ischemia following a 15- minute occlusion  myocardial stunning ◦ Function remains depressed while resting  dissociation of the usual close relation between subendocardial flow and function
  • 42. Chronic Hibernating Myocardium ◦ Viable dysfunctional myocardium  any myocardial region in which contractile function improves after coronary revascularization ◦ Chronically stunned  When resting flow relative to a remote region is normal in dysfunctional myocardium distal to a stenosis ◦ Hibernating myocardium  When relative resting flow is reduced in the absence of symptoms or signs of ischemia
  • 43. Cellular Responses in Hibernating Myocardium Apoptosis, Myocyte Loss, and Myofibrillar Loss ◦ Approximately 30% regional myocytes undergo apoptosis Cell Survival and Antiapoptotic Program in Response to Repetitive Ischemia ◦ Upregulation of antiapoptotic proteins in patients without HF Metabolism and Energetics in Hibernating Myocardium ◦ Once adapted, the metabolic and contractile response of hibernating myocardium appears to be dissociated from external determinants of workload Inhomogeneity in Sympathetic Innervation, Beta- Adrenergic Responses, and Sudden Death ◦ The contractile response of hibernating myocardium is blunted  regional downregulation in beta- adrenergic adenylyl cyclase coupling 43
  • 44. 44 Conclusion and Future Directions • The major factors determining myocardial perfusion and oxygen delivery have been incorporated into the current management of angina and have withstood the test of time • Important gaps remain in basic knowledge and in the translation of this knowledge to clinical care • Our understanding of the physiologic and cellular mechanisms responsible for microvascular dysfunction is limited • Continued bench-to-bedside translational investigation in these and other areas is needed