GLOBAL MYOCARDIAL ISCHEMIA AND REPERFUSION

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GLOBAL MYOCARDIAL ISCHEMIA AND REPERFUSION

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... AGAINST MYOCARDIAL ISCHEMIA IN THE NORMAL HEART ... CHRONIC HEART FAILURE. CHRONICALLY DEPLETED OF ENERGY CHARGE ... IMPAIRED SYSTOLIC AND DIASTOLIC FUNCTION ... – PowerPoint PPT presentation

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Title: GLOBAL MYOCARDIAL ISCHEMIA AND REPERFUSION

1
GLOBAL MYOCARDIAL ISCHEMIA AND REPERFUSION

M.KUDUVALLI

2
DEFINITION

GLOBAL MYOCARDIAL ISCHEMIA REFERS TO A REDUCTION
IN OXYGEN SUPPLY TO THE WHOLE OF THE MYOCARDIUM
DUE TO AN INADEQUATE CORONARY BLOOD FLOW, DESPITE
ADEQUATE OXYGEN CONTENT OF THE PERFUSATE
TO BE DIFFERENTIATED FROM MYOCARDIAL HYPOXIA

3
PROTECTIVE MECHANISMS AGAINST MYOCARDIAL ISCHEMIA
IN THE NORMAL HEART

BLOOD IS CONTINUOUSLY MODIFIED
FOR CORRECT COMPOSTITION
FOR REMOVAL OF PARTICULATE AND GASEOUS EMBOLI
MYOCARDIAL OXYGEN SUPPLY IS KEPT IN BALANCE WITH
DEMAND
HIGH DEGREE OF AUTOREGULATION OF CORONARY BLOOD
FLOW

4
MYOCARDIAL VULNERABILITY TO ISCHEMIC DAMAGE
DURING CPB

PREOPERATIVE FUNCTIONAL CLASS
VENTRICULAR HYPERTROPHY
CORONARY ARTERY DISEASE
CYANOTIC CONG. HEART DISEASE
ISCHEMIA PRIOR TO CPB
PREOPERATIVELY IN CARDIOGENIC SHOCK
ANAESTHESIA
MANIPULATION OF THE HEART

5
VENTRICULAR HYPERTROPHY

TRANSMURAL GRADIENTS OF ENERGY SUBSTRATE
UTILIZATION MARKEDLY INCREASED
XANTHINE OXIDASE LEVELS MARKEDLY INCREASED
SUPEROXIDE DISMUTASE LEVELS MARKEDLY DECREASED
ADEQUATE REPERFUSION OF HYPERTROPHIED MYOCARDIUM
MORE DIFFICULT

6
CHRONIC HEART FAILURE

CHRONICALLY DEPLETED OF ENERGY CHARGE
ENERGY CHARGE IS THE ENERGY PRODUCING CAPACITY OF
THE PARTICULAR COMBINATION OF ADENINE NUCLEOTIDES
PRESENT IN THE MITOCHONDRIA AND CYTOPLASM OF THE
MYOCARDIAL CELL.
NORMALLY 0.85.
WOULD BE 1.0 IF ALL THE NUCLEOTIDES WERE PRESENT
ONLY AS ATP

7
EVENTS DURING CPB WHICH CAUSE ISCHEMIA

ABNORMAL PERFUSATE COMPOSITION
PERSISTENT VENTRICULAR FIBRILLATION
INADEQUATE MYOCARDIAL PERFUSION
VENTRICULAR DISTENSION
VENTRICULAR COLLAPSE
CORONARY EMBOLISM
CATECHOLAMINES
AORTIC CROSS-CLAMP
REPERFUSION

8
ABNORMALITIES IN PERFUSATE

DENATURED PLASMA PROTEINS
HIGH LEVELS OF FREE FATTY ACIDS
VASOACTIVE SUBSTANCES
CAPILLARY SLUDGING (PREDISPOSED TO BY
HEPARINIZATION BY INCREASING THE SEDIMENTATION
RATE)
GAS AND PARTICULATE MICRO-EMBOLI

9
VENTRICULAR FIBRILLATION

INCREASED MYOCARDIAL WALL TENSION
INCREASED MVO2
IMPAIRED SUBENDOCARDIAL BLOOD FLOW
ABOVE EFFECTS POTENTIATED BY
VENTRICULAR DISTENSION
VENTRICULAR HYPERTROPHY
CORONARY ARTERY DISEASE

10
INADEQUATE MYOCARDIAL PERFUSION

PERFUSION PRESSURE IS VARIABLE AND NONPULSATILE
CVR INCREASED DUE TO
ABNORMALITIES OF PERFUSATE COMPOSITION AND
VISCOSITY
MICROEMBOLI
ALTERED LYMPH FLOW
MYOCARDIAL OEDEMA AFTER LONG CPB
LOSS OF AUTOREGULATION

11
STRATEGIES TO IMPROVE MYOCARDIAL PERFUSION

KEEP PERFUSION GRADIENT BETWEEN 50 70 mmHg
HIGHER PERFUSION PRESSURE IN CAD, HYPERTROPHIC
VENTRICLES, AND IF VF OCCURS
?? PULSATILE FLOW

12
VENTRICULAR DISTENSION

CAUSES INCREASED MYOCARDIAL WALL TENSION AND MVO2
REDUCES SUBENDOCARDIAL PERFUSION DUE TO INCREASED
INTRACAVITY PRESSURE
POTENTIATED BY
INADEQUATE VENOUS RETURN
AORTIC INSUFFICIENCY
VF
INCREASED PV RETURN AND NONCORONARY COLLATERAL
FLOW IN THE QUIESCENT HEART
POST-REPAIR CARDIAC FAILURE

13
STRATEGIES TO PREVENT VENTRICULAR DISTENSION

OPTIMIZE VENOUS DRAINAGE
OPTIMIZE CPB FLOW RATES
VENT THE LEFT HEART
EARLY DEFIBRILLATION
EARLY CROSS CLAMPING IN AORTIC INCOMPETENCE
VASODILATORS MAY HELP SOMETIMES

14
VENTRICULAR COLLAPSE

PREDISPOSES TO ISCHEMIA IN THE PERFUSED, EMPTY,
BEATING HEART
CHANGES IN MYOCARDIAL COMPRESSIVE FORCES AND
VENTRICULAR GEOMETRY CAUSE SUBENDOCARDIAL
ISCHEMIA, ESPECIALLY IN HYPERTROPHIC,
SMALL-CHAMBERED VENTRICLES

15
CORONARY EMBOLISM

GAS OR PARTICULATE
REDUCE INCIDENCE BY
APPROPRIATE FILTERS IN THE CIRCUIT
VENTING OF VEIN GRAFTS
ADEQUATE DEAIRING OF CHAMBERS

16
INOTROPES DURING WEANING FROM CPB

ENDOGENOUS CATACHOLAMINES ALREADY HIGH AT THE END
OF CPB
PROLONGED USE OF HIGH DOSE EXOGENOUS INOTROPES
DISPROPORTIONATELY INCREASES MVO2
STRATEGY
OPTIMIZE HR, PRELOAD, AFTERLOAD PRIOR TO USE OF
INOTROPES
MECHANICAL SUPPORT IN PLACE OF VERY HIGH
INOTROPIC SUPPORT

17
AORTIC CROSS CLAMP

PROBLEMS WITH NORMOTHERMIC ISCHEMIC ARREST
PERSISTENT ELECTRICAL AND MECHANICAL ACTIVITY
DURING MUCH OF THE ISCHEMIC PERIOD DEPLETES HIGH
ENERGY PHOSPHATE AND COMPROMISES POST-REPAIR
VENTRICULAR PERFORMANCE
SAFE ISCHEMIC TIME INSUFFICIENT TO COMPLETE MOST
REPAIRS
INTERMITTENT CROSS CLAMP WITH PERIODS OF
REPERFUSION DOES LITTLE TO IMPROVE OPERATING
CONDITIONS OR PREVENT MYOCARDIAL NECROSIS.
ACTUALLY MAY BE DELETERIOUS COMPARED TO A LONGER
SINGLE PERIOD OF ISCHEMIA

18
AORTIC CROSS CLAMP

RAPID CESSATION OF ELECTRO-MECHANICAL ACTIVITY
FOLLOWING CROSS CLAMP DESIRABLE BOTH FOR EXPOSURE
AND MYOCARDIAL PRESERVATION
DIFFERENCES IN MYOCARDIAL VULNERABILITY MAKE IT
IMPOSSIBLE TO PREDICT A SAFE PERIOD OF ISCHEMIA
EXTENT OF NECROSIS IS DIRECTLY PROPORTIONAL TO
THE DURATION OF AORTIC CROSS CLAMP

STRATEGIES FOR MINIMIZING DELETERIOUS EFFECTS OF
AORTIC CROSS CLAMP
MINIMIZE THE DURATION WITH A WELL THOUGHT OUT AND
EFFICIENTLY EXECUTED REPAIR
MANIPULATE MYOCARDIAL METABOLISM DURING THE
PERIOD OF CROSS CLAMP MYOCARDIAL PROTECTION

20
PATHOPHYSIOLOGY OF GLOBAL MYOCARDIAL ISCHEMIA
? HIGH ENERGY PHOSPHATE PRODUCTION
PERSITENT HIGH ENERGY PHOSPHATE UTILIZATION
DECREASED HIGH ENERGY PHOSPHATE AVAILABILITY
21
DECREASED HIGH ENERGY PHOSPHATE AVAILABILITY
FAILURE OF CALCIUM REGULATION
FAILURE OF CELLULAR VOLUME REGULATION
INCREASED INTRACELLULAR SODIUM
INCREASED INTRACELLULAR CALCIUM
ACTIVATION OF CALCIUM ATPASES
ACTIVATION OF CALCIUM LIPASES
MITOCHONDRIAL CALCIUM OVERLOAD
INTRACELLULAR OEDEMA
HIGH ENERGY PHOSPHATE UTILIZATION
? HIGH ENERGY PHOSPHATE PRODUCTION
22

OXIDATIVE PHOSPHORYLATION CEASES WHEN PO2 FALL
BELOW 5 10 mmHg
DURING ISCHEMIA, THE MAIN SOURCES OF HIGH ENERGY
PHOSPHATE ARE CREATINE PHOSPHATE AND ANAEROBIC
PRODUCTION OF ATP
ANAEROBIC PRODUCTION OF ATP IS SELF- LIMITED
BECAUSE OF ACCUMULATION OF METABOLITES SUCH AS
LACTATE, PYRUVATE AND PROTONS, WHICH EVENTUALLY
INHIBIT ESSENTIAL ENZYME SYSTEMS

CP AND ATP LEVELS DECLINE RAPIDLY FOLLOWING
GLOBAL ISCHEMIA BECAUSE OF PERSISTENT ENERGY
UTILIZATION FOR ELECTROMECHANICAL AND BASAL
METABOLIC ACTIVITY
THERE IS AN INITIAL RAPID REDUCTION OF ACTIVE
DEVELOPMENT OF MYOCARDIAL TENSION WITHOUT A RISE
IN RESTING TENSION
SUBSEQUENTLY, RESTING TENSION INCREASES UNTIL A
PLATEAU IS REACHED
PROLONGED ISCHEMIA RESULTS IN SEVERE MYOCARDIAL
CONTRACTURE

24
ENERGY UTILIZATION IS CLOSELY LINKED TO MOVEMENT
OF CALCIUM IONS
TRANSPORT OF CALCIUM INTO THE MYOCYTE (CONSUMES
LITTLE ENERGY)
RISE IN INTRACELLULAR CALCIUM TRIGGERS A SERIES
OF REGULATORY REACTIONS RESULTING IN MYOCARDIAL
CONTRACTION AND ENERGY UTILIZATION
ENERGY DEPENDENT TRANSPORT OF CALCIUM TO OUTSIDE
THE CELL FOR MYOCARDIAL RELAXATION
25
INCREASED PRODUCTION AND ACCUMULATION OF H IONS
AND FREE FATTY ACIDS
LOW PRODUCTION OF ATP DUE TO ANAEROBIC METABOLISM
INCREASED CYTOSOLIC CONCENTRATION OF IONIZED
CALCIUM
RELEASE OF INTRACELLULAR LIPOPROTEIN LIPASE
FORMATION OF RIGOR BONDS BETWEEN CONTRACTILE
PROTEINS WITH PERSISTENT ENERGY UTILIZATION
LOSS OF CELL INTEGRITY AND FUNCTION
26
DAMAGE FROM GLOBAL MYOCARDIAL ISCHEMIA

INVOLVES
MYOCYTES
VASCULAR ENDOTHELIUM
SPECIALIZED CONDUCTION CELLS

27
(MYOCARDIAL STUNNING)
(MYOCARDIAL NECROSIS)
28
MYOCARDIAL STUNNING

DEFINED AS REVERSIBLE DEPRESSION OF SYSTOLIC AND
DIASTOLIC MYOCARDIAL FUNCTION, WITHOUT MYOCARDIAL
NECROSIS, THAT ACCOMPANIES, AND FOR A TIME
FOLLOWS, MYOCARDIAL ISCHEMIA
STUNNED MYOCARDIUM HAS BEEN SHOWN TO HAVE A HIGH,
NOT LOW, OXYGEN CONSUMPTION

29
HYPOTHETICAL CAUSES OF MYOCARDIAL STUNNING

ISCHEMIA INDUCED INFLUX OF CALCIUM INTO THE
MYOCARDIAL CELLS
RELEASE OF OXYGEN-DERIVED FREE RADICALS,
PRESUMABLY BY ACTIVATED NEUTROPHILS IN THE FIRST
FEW MINUTES OF REPERFUSION
PROLONGED POST-ISCHEMIC DEPLETION OF MYOCARDIAL
CELL ENERGY CHARGE
POST-ISCHEMIC IMPAIRMENT OF CORONARY BLOOD FLOW
OR CORONARY RESERVE
APOPTOSIS (PROGRAMMED CELL DEATH)

30
MYOCARDIAL NECROSIS

END STAGE OF A COMPLEX PROCESS
INITIATED BY THE ONSET OF GLOBAL MYOCARDIAL
ISCHEMIA
MAINTAINED BY CONTINUING ISCHEMIA
AGGRAVATED BY REPERFUSION
COMMONER WHEN ISCHEMIC PERIOD IS EXCESSIVE
HOWEVER, EXCESSIVE IS DIFFICULT TO DEFINE

INITIAL MICROSCOPIC CHANGES
GROSS MICROSCOPY
CELLULAR SWELLING
ULTRASTRUCTURAL CHANGES
LOSS OF GLYCOGEN GRANULES
INTRACELLULAR AND ORGANELLE SWELLING
LATE MICROSCOPIC CHANGES
GROSS MICROSCOPY
FURTHER CELLULAR SWELLING
DISRUPTION OF REGULAR MYOFIBRILLAR PATTERN
CONTRACTURE BANDS
ULTRASTRUCTURAL CHANGES
CELLULAR AUTOLYSIS
STRUCTURAL DEGENERATION OF INTRACELLULAR
ORGANELLES

32
ENDOTHELIAL CELL DAMAGE

ENDOTHELIAL CELL SWELLING DEVELOPS DURING
ISCHEMIA AND BECOMES MORE PROMINENT DURING
REPERFUSION
AFFECTS THE SECRETION OF EDRF AS WELL AS
ENDOTHELINS (CONSTRICTORS)
CONTRIBUTE TO THE WHOLE BODY INFLAMMATORY
RESPONSE TO CPB
CAN CAUSE INCREASE IN CVR, AND OBSTRUCTION TO
CAPILLARY PERFUSION DURING REPERFUSION THE NO
REFLOW PHENOMENON

33
SPECIALIZED CONDUCTION CELL DAMAGE

BECOME NON-FUNCTIONAL EARLY IN THE COURSE OF
GLOBAL MYOCARDIAL ISCHEMIA
RECOVERY TAKES LONGER THAN RECOVERY OF MYOCYTES

34
ALL THE PATHOLOGICAL CHANGES DESCRIBED OCCUR
PREFERENTIALLY IN THE SUBENDOCARDIAL LAYERS OF
THE MYOCARDIUM, WITH THE SUBEPICARDIAL LAYERS
BEING LEAST AFFECTED
35
CAN GLOBAL MYOCARDIAL ISCHEMIA BE BENEFICIAL?

THE CONCEPT OF ISCHEMIC PRECONDITIONING AND ITS
POTENTIAL APPLICATION IN CARDIAC SURGERY

DEFINED AS THE CONCEPT OF ENDOGENOUS ADAPTATION
TO SUBLETHAL GLOBAL ISCHEMIA RESULTING IN
PROTECTION AGAINST A LONGER LETHAL ISCHAEMIC
EPISODE
HAS BEEN DEMONSTRATED EXPERIMENTALLY IN ANIMAL
HEARTS, AND ALSO IN CLINICAL CIRCUMSTANCES IN
HUMANS IN A FEW STUDIES

37
POSSIBLE MECHANISMS OF PRECONDITIONING

INITIALLY THOUGHT TO BE DUE MANIFESTATION OF
INCREASED COLLATERAL FLOW
PRESENT RESEARCH HYPOYHETISES THE EFFECTS TO BE
MEDIATED BY ADENOSINE AND A SIGNAL TRANSDUCTION
PATHWAY INVOLVING G-PROTEINS, A PHOSPHOLIPASE AND
PROTEIN KINASE C (PKC)
ANOTHER HYPOTHESIS INVOLVED ATP-DEPENDANT K
CHANNELS

SHOWN TO HAVE MAXIMUM BENEFIT WHEN THE ISCHEMIC
PERIOD IS A SINGLE EPISODE OF 3 - 5 MINS, ABOUT 3
- 5 MINS PRIOR TO THE PROLONGED ISCHEMIC PERIOD
THE BENEFITS WEAR OFF BEYOND ABOUT 2 HOURS OF
PROLONGED ISCHEMIA
BENEFITS SEEN MAXIMALLY WITH LIMITING INFARCT
SIZE AND ARRHYTHIAS AFTER THE ISCHEMIC PERIOD
HAS NOT BEEN SHOWN TO HAVE SIGNIFICANT BENEFITS
IN DECREASING MYOCARDIAL STUNNING RELATED LOW
CARDIAC OUTPUT

39
REPERFUSION AFTER GLOBAL MYOCARDIAL ISCHEMIA

POST ISCHEMIA, THE MYOCARDIUM IS COMPOSED OF A
HETEROGENOUS POPULATION OF CELLS
IRREVERSIBLE DAMAGED
MINIMALLY DAMAGED
STUNNED MYOCARDIAL CELLS

POOR MYOCARDIAL PROTECTION BEFORE AND DURING
CROSS CLAMP
LARGE MASS OF IRREVERSIBLY DAMAGED CELLS LEADING
USUALLY TO PATIENT DEATH
OPTIMAL PROTECTION
VIABLE MYOCARDIUM AND SURVIVAL WITH MINIMUM
INTERVENTIONS
SUBOPTIMAL PROTECTION
POPULATION OF STUNNED CELLS WHOSE FATE DEPENDS ON
REPERFUSION MANAGEMENT

41
ABNORMALITIES ENCOUNTERED DURING REPERFUSION
ELECTRICAL HETEROGENOUS ACTIVITY INCREASED
AUTOMATICITY
STRUCTURAL MYOCARDIAL OEDEMA PLATELET
DEPOSITION VASCULAR INJURY VASCULAR COMPRESSION
BIOCHEMICAL ACIDOSIS DECREASED OXYGEN
UTILIZATION DECREASED H-E-P PRODUCTION INCREASED
CATACHOLAMINES INCREASED CELLULAR
CALCIUM INCREASED FREE RADICALS
MECHANICAL IMPAIRED SYSTOLIC AND DIASTOLIC
FUNCTION
42

THE RESPONSE OF MYOCARDIAL CELLS TO UNCONTROLLED
REPERFUSION DEPENDS IN LARGE PART ON THE
TIME-RELATED POINT ALONG THE PATHWAY TO CELL
DEATH THAT HAS BEEN REACHED DURING THE PERIOD OF
ISCHEMIA
THE CRITICAL POINT AT WHICH THE EXPLOSIVE
CELLULAR RESPONSE TO UNCONTROLLED PERFUSION IS
SEEN CANNOT BE DEFINED

43
MYOCARDIAL RESPONSE TO REPERFUSION

MYOCARDIAL STUNNING
REPERFUSION ARRHYTHMIAS
VENTRICULAR TACHYCARDIA
VENTRICULAR FIBRILLATION
STONE HEART
HARD AND FIBRILLATING HEART
MAY INVOLVE ONLY SOME REGIONS OF THE HEART,
TYPICALLY THE BASILAR PORTION OF THE LEFT
VENTRICLE AND THE SUBENDOCARDIUM
INDICATES USUALLY THAT THE HEART HAS REACHED THE
POINT OF NO-RETURN, THOUGH NOT NECESSARILY SO.

44
ENDOTHELIAL CELL DAMAGE DUE TO REPERFUSION

MINIMAL AFTER ISCHEMIA, ALMOST EXCLUSIVELY
POTENTIATED BY REPERFUSION
SWELLING OF ENDOTHELIAL CELLS, AGGREGATION OF
NEUTROPHILS AND PLATELET PLUGS CAUSE
MICROVASCULAR OBSTRUCTION
ADDITIONALLY, MYOCARDIAL OEDEMA CAN ALSO COMPRESS
THE MICROVASCULATURE LEADING TO INHOMOGENEOUS
REPERFUSION, OR SOMETIMES, THE NO-REFLOW
PHENOMENON

45
MOLECULAR BASIS OF REPERFUSION RESPONSE

INFLUX OF CALCIUM INTO MYOCYTES, ESPECIALLY
ACCUMULATION IN MITOCHONDRIA
RELEASE OF COMPLEMENT FRAGMENTS SUCH AS C5a FROM
ISCHEMIC MYOCARDIUM
CHEMOTACTIC FOR NEUTROPHILS, WHICH
PLUG MYOCARDIAL CAPILLARIES
RELEASE LARGE AMOUNT OF OXYGEN DERIVED FREE
RADICALS
RELEASE ARACHIDONIC ACID METABOLITES WHICH CAUSE
ENDOTHELIAL INJURY, PLATELET AGGREGATION AND
VASOCONSTRICTION

46
MECHANISM OF OXYGEN DERIVED FREE RADICAL
PRODUCTION ON REPERFUSION
47
CONTROLLED REPERFUSION

MINIMIZES THE PERSISTENCE OF MYOCARDIAL STUNNING
INTO THE POST-CPB PERIOD
PROVIDES FOR OPTIMAL RECOVERY OF FUNCTION OF
REVERSIBLY DAMAGED MYOCARDIUM
RESUSCITATES MYOCYTES THAT WOULD OTHERWISE HAVE
UNDERGONE NECROSIS

48
CONTROLLED REPERFUSION CONSISTS OF THE FOLLOWING

MAINTINING ELECTROMECHANICAL QUIESCENCE DURING
THE FIRST 3 5 MINS. OF REPERFUSION
PERMITS MORE RAPID REPLETION OF MYOCARDIAL ENERGY
CHARGE
MINIMIZES REGIONAL HETEROGENECITY OF FLOW
MINIMIZES MYOCARDIAL ENERGY EXPENDITURE TILL
RECOVERY HAS BEEN ESTABLISHED
MINIMIZES INTRACELLULAR ACCUMULATION OF CALCIUM
LARGE BUFFERING CAPACITY OF REPERFUSATE TO COMBAT
ACCUMULATED ACIDOSIS

MINIMIZING DAMAGE BY OXYGEN-DERIVED FREE RADICALS
MAINTAINING LOW CALCIUM IN THE INITIAL PERFUSATE
TO PREVENT INTRACELLULAR ACCUMULATION OF CALCIUM
SUBTRATE ENHANCEMENT OF THE REPERFUSATE FOR
REPLETION OF ENERGY CHARGE
MAINTAINING LOW PERFUSION PRESSURES AROUND 30
40 mmHg DURING THE FIRST COUPLE OF MINUTES OF
REPERFUSION TO MINIMIZE ENDOTHELIAL CELL DAMAGE
AND SWELLING

50
SUGGESTED STRATEGIES FOR CONTROLLED REPERFUSION

USING BLOOD AS THE REPERFUSATE INSTEAD OF
CRYSTALLOID
RBCs CONTAIN ABUNDANT FREE RADICAL SCAVENGERS
BUFFERING CAPACITY OF BLOOD PROTEINS
SUBSTRATE ENHANCEMENT s/a GLUTAMATE OR
L-ASPARTATE
BUFFERING AGENTS SUCH AS HYDROXYMETHYAL
AMINOMETHANE AND HISTIDINE
LOW CALCIUM CONTENT

ENOUGH POTASSIUM CONTENT TO MAINTAIN
ELECTROMECHANICAL QUIESCENCE, USUALLY 10 20
mEq/L
OPTIMUM PERFUSION PRESSURE OF THE REPERFUSATE
MAINTAINING TEMPERATURE OF REPERFUSATE BETWEEN 35
37 DEG. CENT.
CONTINUING CONTROLLED REPERFUSION TILL THE HEART
IS BEATING FORCEFULLY, PREFERABLY IN SINUS RHYTHM

RECENT RESEARCH SHOWS THAT SODIUM INFLUX INTO THE
CELL ON REPERFUSION AND THE RESULTANT CELLULAR
OEDEMA CONTRIBUTES SIGNIFICANTLY TO CELL INJURY
AND DEATH
ISCHEMIC PRECONDITONING HAS BEEN SHOWN TO REDUCE
REPERFUSION INJURY BY COMPLEX MECHANISMS, BUT
PRINICIPALLY BY PROTECTION OF MITOCHONDRIA.
THIS IMPROVES ATP PRODUCTION AND ENHANCES THE
FUNCTION OF ATP DEPENDENT Na/K EXCHANGE PUMPS

53
CONCLUSION

ADEQUATE INSIGHT OF PATHOPHYSIOLOGY OF GLOBAL
MYOCARDIAL ISCHEMIA AND REPERFUSION IS ESSENTIAL
FOR APPROPRIATE MYOCARDIAL MANAGEMENT DURING AND
AFTER CPB
SEVERAL DEFICIENCIES IN AVAILABLE INFORMATION,
PRESENTLY THE SUBJECT OF RESEARCH
PRESENT DAY STRATEGIES OF MYOCARDIAL PROTECTION
WOULD PROBABLY BE BETTER DESCRIBED AS MYOCARDIAL
DAMAGE LIMITATION !

54
Thank you!

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