SlideShare a Scribd company logo

Cardioplegia

โ€ขDownload as PPTX, PDFโ€ข
โ€ข
R
Raja Lahiri

Cardioplegia

Health & Medicine
1 of 46
Cardioplegia session -Dr Raja Lahiri
Topics ๏‚— Alternative arresting agents & additives ๏‚— Crystalloid vs Blood cardioplegia ๏‚— Potential newer technology
Adenosine receptors ๏‚— Four types of adenosine receptors: A1, A2a, A2b, A3 ๏‚— Activation of adenosine A 1 receptors leads to: โ—ฆ inhibition of cyclic AMP production โ—ฆ inhibition of the slow calcium channel โ—ฆ opening of an adenosine-activated ATPsensitive potassium (K ATP ) channel ๏‚— This leads to hyperpolarization, which delays conduction through the AV node and slows the ventricular response to atrial tachycardia. ๏‚— It also causes endothelial-dependent relaxation of smooth muscle as is found inside the artery walls. ๏‚— Activation of A2A receptors produces a constellation of responses that in general can be classified as anti- inflammatory ๏‚— Pretreatment with adenosine confers a cardioprotective effect during ischemia and can inhibit the inflammatory responses initiated by ischemia and reperfusion
Minute work & Oxygen demand ๏‚— Minute work = Heart rate x Stroke volume x Pressure ๏‚— However, minute work is not the direct determinant of oxygen consumption ๏‚— The primary determinant of oxygen demand is the wall tension or stress developed in each cardiac cycle. ๏‚— The energetic cost of ejecting blood from the ventricular chamber is approximately 20 to 30% of that required for isovolumic contraction. ๏‚— An increase in afterload requires greater energy than an increase in volume ejected. ๏‚— Oxygen consumption is also increased as the heart dilates and begins ejection from a greater diastolic volume. ๏‚— Cardiac efficiency = Work/MVO2
Alternative arresting agents & Additives ๏‚— Beta Blockers: โ—ฆ As the ascending aorta is clamped, the non- exocytotic release of norepinephrine from the cardiac sympathetic nerves acts on ฮฒ-adrenergic receptors on the outer surface of the sarcolemma, causing an increase in cAMPdependent protein kinase activity, phosphorylation of the calcium release channels, and increased Ca2+ influx, resulting in increased Ca2+-dependent contractility and rapid depletion of glycogen stores. โ—ฆ Early studies suggested that long-acting beta blockers improved myocardialprotection during ischemia but unfortunately have a prolonged negative inotropic effect, which limits their clinical use.
๏‚— Beta blockers such as propranolol have been used as an adjunct to anesthesia to block ฮฒ-adrenergicโ€“ stimulating episodes associated with coronary ischemia during the course of the operative procedure. ๏‚— Ultra-short-acting cardioselective beta blockers such as landiolol and esmolol provide polarized cardiac arrest by maintaining the membrane potential at or near the resting membrane potential ๏‚— Esmolol has been used to enhance myocardial protection during intermittent arrest and has been shown to provide myocardial preservation equivalent to or better than cold crystalloid or blood cardioplegia. ๏‚— With esmolol cardioplegia, there is a slow undulating ventricular contraction that may decrease myocardial edema but does not provide a quiescent operating field
Adenocaine ๏‚— Adenosine-lidocaine (adenocaine) cardioplegia provides an exciting alternative to depolarizing cardioplegia. ๏‚— Adenosine-lidocaine cardioplegia has been shown to provide a shorter time to electromechanical arrest, greater postischemic recoveries of aortic flow, a lower coronary vascular resistance during infusion, and greater MVO2 as compared to St. Thomasโ€™ Hospital solution, while maintaining the myocardial cell membrane potential at its resting state
Agents Affecting Calcium Transport๏‚— The infusion of calcium-free cardioplegic solutions induces rapid diastolic cardiac arrest by inhibiting excitation-coupling and increases permeability of the sarcolemma. ๏‚— When a calcium-containing perfusate is then reinfused, during reperfusion, there is a rapid influx of calcium into the cell, resulting in myocardial contracture and extensive ultrastructural damage, the โ€œcalcium paradox.โ€ ๏‚— Calcium antagonist agents administered before ischemia have been proposed as a possible mechanism to reduce ischemic cellular injury. ๏‚— Calcium channel blocking agents, including verapamil, diltiazem, and nifedipine, prevent calcium-induced calcium release in myocardial cells and, as an adjunct to normothermic cardioplegia, have been shown to improve postischemic systolic function. ๏‚— Calcium blockers have no effect if they are administered before reperfusion, are temperature dependent, and have limited effect during hypothermia. ๏‚— Because high concentrations are required for cardioprotection, their prolonged membrane binding prevents rapid recovery, thus limiting their clinical usefulness.
๏‚— Magnesium: โ—ฆ Magnesium inhibits calcium entry into the cell by displacing calcium from its binding sites in the sarcolemmal membrane. โ—ฆ It has limited use as an arresting agent because high concentrations are required, cardiac arrest is delayed, and postischemic functional recovery is decreased in comparison to potassium cardioplegia. โ—ฆ The advantages of magnesium have been shown to be optimal when it is included with high-potassium cardioplegia, in which it has been demonstrated to ameliorate cytosolic, nuclear, and mitochondrial calcium accumulation; preserve high-energy phosphate moieties; and enhance postischemic functional recovery.
Avoidance of Substrate Depletion ๏‚— Metabolic substrates have been added to cardioplegic solutions to enhance anaerobic metabolism during ischemia or to provide citric acid cycle intermediaries to facilitate homeostasis during reperfusion. ๏‚— Agents used include glucose and insulin; nucleosides, such as adenosine, aspartate, and glutamate; and L-arginine to stimulate nitric oxide production. ๏‚— Although metabolic substrate enhancement has been used in various clinical situations, none has achieved universal adoption.
Blood v/s Crystalloid cardioplegia ๏‚— Crystalloid cardioplegia: โ—ฆ these solutions contain minimal amounts (0.6 mL/100 mL at a PO2 of 100 mm Hg at a temperature of 10ยฐ C) of dissolved oxygen, whereas the myocardium consumes 0.33 mL of oxygen per 100 g at 15ยฐ C. โ—ฆ Because even a short period of ischemia results in the gradual accumulation of oxygen debt, moderate to severe myocardial hypothermia is necessary to prevent the rapid degradation of energy stores โ—ฆ To overcome the oxygen deficit issue, oxygenation of crystalloid cardioplegia has been clinically used and has demonstrated a decrease in creatine kinase MB levels
Clinical steps for myocardial protection with use of crystalloid cardioplegia 1. Before the onset of surgery, the operating room temperature is cooled to 17ยฐ C to 19ยฐ C to avoid warming of the anterior surface of the heart by convection and radiation from highintensity lighting. 2. Cardiopulmonary bypass is initiated at a temperature of 28ยฐ C. 3. A myocardial electrocardiographic lead and temperature probe are placed on the anterior wall of the right ventricle because it constitutes two thirds of the anterior surface of the heart, and its rewarming during surgically induced ischemia may partially explain the occasional observation of selective right ventricular failure after the termination of bypass 4. an insulation pad is placed in the posterior pericardial sac and along the left ventricular lateral wall to protect the left phrenic nerve from thermal injury associated with regional
5. The systemic perfusate temperature is temporarily decreased to 10ยฐ C to 15ยฐ C to โ€œprecoolโ€ the heart (infusion hypothermia), and iced saline slush is placed into the pericardial sac to achieve rapid myocardial cooling 6. When a myocardial temperature of 28ยฐ C is reached, the ascending aorta is cross-clamped and cold crystalloid cardioplegia solution at a temperature of 5ยฐ C is infused into the aortic root at a pressure not exceeding 90 mm Hg @10ml/kg 7. At the termination of the initial cardioplegic infusion, the systemic temperature is elevated to 20ยฐ C, and the systemic perfusion flow rate is decreased from 2.2 to 1.5 liter/min/m2 .Increase in myocardial temperature above 20ยฐ C or if there is any electrocardiographic activity or observed ventricular motion, the solution is reinfused at a volume of 5 mL/kg. 8. Five minutes before removal of the aortic clamp, the systemic perfusate temperature is raised to 30ยฐ C, and flow is increased to 2.2 liter/min/m2. 9. After the aortic cross-clamp is removed, the perfusate temperature is raised to 38ยฐ C and the room temperature is raised to 25ยฐ C to 30ยฐ C. 10. Cardiopulmonary bypass is continued until the esophageal temperature is 37ยฐ C and the rectal temperature is in the range of 35ยฐ C to 37ยฐ C.
Disadvantage of crystalloid cardioplegia ๏‚— Extensive rewarming period, which may exceed 30 to 45 minutes. ๏‚— Slow recovery of myocardial metabolism ๏‚— Poor response to postoperative hemodynamic stress ๏‚— Gradual accumulation of oxygen debt and myocardial damage if adequate hypothermia not maintained
Blood Cardioplegia ๏‚— Advantages: โ—ฆ Optimum oxygenation (superior to oxygenated crystalloids) โ—ฆ Better removal of carbon-dioxide โ—ฆ Buffering action and reducing agent โ—ฆ Presence of colloid avoids adverse oncotic pressure gradients โ—ฆ presence of oxygen free radical scavengers โ—ฆ Preserves microvascular responses compared with crystalloid cardioplegia
Blood Cardioplegia ๏‚— Concerns: โ—ฆ the hypothermic shift to the left of the oxyhemoglobin dissociation curve, thereby reducing the release of oxygen at the tissue level โ—ฆ the experimental evidence that blood cardioplegia may not protect the myocardium at low temperatures โ—ฆ the potential of hypothermia induced sludging and red cell rouleau formation.
Warm blood cardioplegia ๏‚— In 1982 Rosenkranz and colleagues reported that warm induction with normothermic blood cardioplegia, with multidose cold blood cardioplegia maintenance of arrest, resulted in better recovery of function in canines than a similar protocol using cold blood induction ๏‚— In 1986, Teoh and colleagues provided experimental evidence that a terminal infusion of warm blood cardioplegia before removing the cross-clamp (a โ€œhot shotโ€) accelerated myocardial metabolic recovery ๏‚— This was followed by a report in 1991 by Lichtenstein and colleagues that normothermic blood cardioplegia in humans is an effective cardio-protective approach.
๏‚— Despite these encouraging reports, there are concerns that for any given patient, it is difficult to determine how long a warm heart can tolerate an ischemic insult if the infusion is interrupted or flow rates are reduced owing to an obscured surgical field or a maldistribution of the cardioplegic solution. ๏‚— Another concern is the report by Martin and colleagues that warm cardioplegia is associated with a threefold increased incidence of neurologic deficits. ๏‚— Subsequent studies have indicated however that appropriately designed protocols using intermittent antegrade warm blood cardioplegia provide clinically acceptable myocardial protection
Tepid blood cardioplegia ๏‚— Both cold blood (4 to 10ยฐC) and warm blood cardioplegic solutions (37ยฐC) have temperature- related advantages and disadvantages. ๏‚— Hayashida and colleagues were one of the first groups to study specifically the efficacy of tepid blood (29ยฐC) cardioplegia. Their study showed that tepid antegrade cardioplegia was the most effective in reducing anaerobic lactate acid release during the arrest period. ๏‚— Mallidi et al showed that warm or tepid blood cardioplegia may be associated with better early and late event-free survivals after CABG ๏‚— Although tepid blood cardioplegia may be safe and effective, the majority of studies have been single- center studies conducted in relatively small cohorts of patients. Whether tepid cardioplegia confers superior protection over other current methodologies remains to be determined.
Miniplegia ๏‚— The use of undiluted blood cardioplegia, or โ€œminiplegiaโ€ (using a minimum amount of crystalloid additives), also has been reported to be effective. ๏‚— Petrucci et al. studied the use of all blood miniplegia in a clinically relevant swine preparation and compared miniplegia with crystalloid cardioplegia. ๏‚— They concluded that the use of all blood miniplegia was effective or superior in the acutely ischemic heart. ๏‚— Rousou and colleagues showed that it is the level of hypothermia that is important in blood cardioplegia, not necessarily the hematocrit.
Advantages of Blood cardioplegia (1) provides an oxygenated environment and a method for intermittent reoxygenation of the heart during arrest (2) limits hemodilution when large volumes of cardioplegic solution are used (3) affords an excellent buffering capacity and osmotic properties (4) allows for electrolyte composition and pH that are physiologic (5) offers a number of endogenous antioxidants and free-radical scavengers (6) is less complex than other solutions to prepare.
Novel strategies for cardioprotection ๏‚— Physiologic: โ—ฆ Ischaemic preconditioning โ—ฆ Post conditioning โ—ฆ Remote ischaemic preconditioning โ—ฆ Autophagy ๏‚— Pharmacologic: โ—ฆ Adenosine โ—ฆ Acadesine โ—ฆ Sodium-Hydrogen exchanger inhibitors โ—ฆ Glucose-Insulin-Potassium (GIK)
Ischaemic preconditioning ๏‚— โ€œPrecondition with ischemiaโ€ is an endogenous adaptive phenomenon whereby the heart becomes more tolerant to a period of prolonged ischemia if first exposed to brief episodes of coronary artery occlusion. ๏‚— IPC has been demonstrated to persist as long as 1 to 2 hours after the ischemic preconditioning stimulus & becomes ineffective when the sustained ischemic insult exceeds 3 hours ๏‚— A second phase of protection appears 24 hours later and is sustained for up to 72 hours. This has been referred to as the second window of protection, late- phase preconditioning, or delayed preconditioning. ๏‚— Unlike classic IPC, which protects only against infarction, the late phase protects against both infarction and myocardial stunning.
1
Clinical relevance of IPC ๏‚— Patients experiencing angina before an MI have a better in-hospital prognosis and a reduced incidence of cardiogenic shock, fewer and less severe episodes of congestive heart failure, and smaller infarcts as assessed by cardiac enzyme release and better long term survival rates ๏‚— Patients who undergo percutaneous coronary interventions (PCI) have an enhanced tolerance to ischemia after the first balloon inflation, provided that the first balloon inflation exceeds 60 to 90 seconds ๏‚— Intermittent cross-clamping with the heart paced at 90 beats per minute to induce ischemia, followed by 2 minutes of reperfusion before a 10- minute period of global ischemia and ventricular fibrillation has shown attenuation of troponin release
Post conditioning ๏‚— First reported by Zhao et al in canine model ๏‚— Rapid intermittent interruptions of blood flow in the early phase of reperfusion, i.e., relief of ischemia in a stuttered or staccato manner. ๏‚— The reduction in infarct size appears to be comparable with that observed with IPC. ๏‚— Patients receiving brief balloon inflations/deflations in the initial minutes of reperfusion during PCI exhibited smaller ST- segment changes and lower levels of total creatine kinase release compared with patients that were not subjected to stuttering reperfusion ๏‚— Luo et al in their study on post-op patients after total correction of TOF showed that aortic reclamping for 30 seconds and declamping for 30 seconds, repeated twice, reduced perioperative troponin T and CK-MB release and decreased the need for inotropic support after surgery
Remote Ischaemic Preconditioning ๏‚— Remote ischemic preconditioning is a phenomenon whereby brief ischemia of one organ or tissue confers protection on a distant naive organ or tissue against a sustained ischemia- reperfusion injury ๏‚— Brief intermittent lower limb ischemia was associated with attenuated troponin release and a reduction in the need for postoperative inotropic support in children undergoing congenital heart surgery ๏‚— Similar findings were demonstrated in adult patients undergoing CABG where RIPC was induced by three 5-minute cycles of right forearm ischemia by inflating a blood pressure cuff on the upper arm to 200 mm Hg with an intervening 5-
Autophagy ๏‚— Autophagy is the process whereby a doublemembrane structure called the autophagosome sequesters cytoplasmic components such as ubiquitinated protein aggregates or organelles including mitochondria, peroxisomes, and endoplasmic reticulum. ๏‚— It is involved in degradation of long-lived proteins and the removal of excess or damaged organelles ๏‚— The outer autophagosomal membrane fuses with a lysosomal membrane to deliver its contents into an autophagolysosome where the cargo is degraded by lysosomal hydrolases and the resulting macromolecules recycled
๏‚— Autophagy has been reported to be upregulated in isolated cells subjected to simulated ischemia and reperfusion and rodent models of ex vivo and in vivo ischemia reperfusion injury. ๏‚— Gurusamy et al. investigated the role of autophagy during ischemia-reperfusion injury and reported that increased BAG- 1 expression in the heart correlated with the onset of protection in an in vivo model of myocardial stunning. ๏‚— Studies suggest that upregulation of autophagy promotes survival during stress such as ischemia-reperfusion ๏‚— There is also direct evidence that autophagy plays an important role in mediating ischemic and pharmacologic preconditioning. ๏‚— Autophagy may serve as an important mediator of protection of the preconditioning agent CCPA. A more detailed understanding of the role of autophagy in myocardial protection may lead to a new therapeutic approach to the management and treatment of ischemia-reperfusion injury.
Adenosine ๏‚— There is considerable experimental evidence that activation of various adenosine receptor subtypes results in cardioprotection similar to that induced by IPC. ๏‚— Preischemic administration of the nucleoside adenosine retards the rate of ischemia-induced ATP depletion, prolongs the time to onset of ischemic contracture, attenuates myocardial stunning, enhances postischemic myocardial energetics, and reduces infarct size ๏‚— Recent preclinical reports suggest that an adenosine A 2b receptor agonist confers cardioprotection when administered before the onset of ischemia (preconditioning) and at reperfusion (postconditioning) ๏‚— In clinical trials, low dose adenosine administration showed no benefit on patient outcome ๏‚— However, trials involving administration of high doses of adenosine in CABG patients showed reduction in postbypass inotropic drug utilization, improved regional wall motion, and global function measured by transthoracic echocardiography ๏‚— Its clinical use is limited because large doses are associated with marked hypotension in patients not on cardiopulmonary bypass.
Acadesine ๏‚— This agent is a member of a class of drugs referred to as adenosine regulating agents. It is a purine nucleoside analog that raises adenosine tissue levels selectively during ischemic conditions ๏‚— Early preclinical studies have indicated that acadesine treatment: โ—ฆ (1) improves left ventricular wall motion after intermittent ischemia โ—ฆ (2) attenuates frequency of ventricular arrhythmias โ—ฆ (3) attenuates myocardial stunning and preserves myocardial function after cardiac arrest and cold cardioplegia. ๏‚— Mangano et al. examined the two-year all cause mortality after perioperative MI in a follow-up of the Acadesine 1024 Trial. Although the primary outcome was negative, the findings at two years among patients experiencing post
Sodium-Hydrogen Exchange inhibitors ๏‚— The sodium-hydrogen exchangers (NHEs) are a family of membrane proteins with nine isoforms that are involved in the transport of hydrogen ions in exchange for sodium ions. ๏‚— NHE-1 is the isoform that is expressed in the heart and may play a minor role in the normal excitation-contraction coupling process; however, it has been implicated in the etiology of arrhythmias, stunning, apoptosis, necrosis associated with acute myocardial ischemia-reperfusion injury, postinfarction ventricular remodeling, and heart failure
๏‚— The driving forces for Na + /H + exchange are the relative transmembrane N + and H + gradients. ๏‚— During ischemia, cytoplasmic pH falls as low as 6.6 because of increased production of H + from anaerobic glycolysis, but upon reperfusion, NHE-1 is activated to restore intracellular pH by exchange of intracellular protons for extracellular sodium. ๏‚— The resulting accumulation of intracellular Na + is further exacerbated by diminished activity of Na + /K + ATPase as a result of ischemia and lowered ATP availability. ๏‚— The increased intracellular Na + competes for sites on the Na + /Ca ++ exchanger and can actually drive it to run in reverse, resulting in cytosolic calcium overload. ๏‚— Calcium overload has numerous adverse consequences including activation of calcium- dependent proteases and phospholipases, gap junction dysfunction, culminating in membrane rupture and cell death
๏‚— The EXPEDITION trial was initiated to address the safety and efficacy of NHE-1 inhibition by cariporide in the prevention of death or MI in patients undergoing CABG surgery. ๏‚— Although cariporide treatment was effective in reducing the incidence of nonfatal MI, its efficacy was associated with toxicity, and the overall assessment of benefits and risks associated with cariporide indicated that the imbalances in the safety profile outweighed the reduction in the observed MI rate ๏‚— The importance of the study, however, is that myocardial necrosis after CABG is higher than previously appreciated and it suggested NHE-1 inhibitors represent a new class of drugs that hold promise for reduction of myocardial infarction associated with ischemiareperfusion injury.
Glucose Insulin Potassium ๏‚— There are numerous studies that suggest glucose- insulin-potassium (GIK) infusions are effective in reducing perioperative MIs, postischemic myocardial dysfunction, and atrial fibrillation in patients undergoing heart surgery. ๏‚— The rationale for this form of treatment is based on the concept that insulin stimulates potassium reuptake through stimulation of the Na + ,K + - ATPase while it stimulates glucose uptake for glycolytic energy production. ๏‚— High glucose, insulin, and an increased glycolytic flux also increase pyruvate generation and in turn preserve the citric acid cycle. ๏‚— Additionally, glycolytic ATP protects membranes, drives uptake of Ca 2+ by the sarcoplasmic reticulum, and improves sodium homeostasis of ischemic
๏‚— Despite a strong rationale for its application in surgery, the efficacy of GIK in heart surgery remains controversial, due to mixed results with the use of GIK to treat patients with acute myocardial infarction ๏‚— Although a metaanalysis of randomized studies using GIK suggests that it may improve postoperative recovery of contractile function and reduce atrial arrhythmias, the individual studies have involved small numbers of patients and, therefore, insufficiently powered to detect efficacy. ๏‚— Until a large randomized, multicenter clinical trial has been performed, the use of GIK as a form of myocardial protection will remain controversial.
Myocardial protection during beating heart surgery ๏‚— The acceptance of OPCAB is due in part to the development and refinement of a myriad of surgical aids that allow for stabilization and local immobilization of the heart during grafting. ๏‚— Ischemia during temporary occlusion of a coronary artery during OPCAB may last from 6 to 25 minutes based on the surgeonโ€™s experience, quality and size of the vessel, and adequacy of the exposure. ๏‚— Most patients with preexisting severe coronary heart disease have experienced self-limiting episodes of ischemia during daily life and may have imparted a certain degree of tolerance to the surgically induced ischemia. ๏‚— This tolerance has been documented using ECGs, transesophageal echocardiography, and continuous SVO2 monitoring
๏‚— In order to better understand the differences between OPCAB and onpump surgery, Chowdhury et al. investigated the release pattern of various cardiac biomarkers in 50 patients undergoing cardioplegic and noncardioplegic coronary artery bypass surgery ๏‚— They observed a greater release of cardiac troponin I, high-sensitivity C-reactive protein, and heart-type fatty acid binding protein in the cardioplegic group. ๏‚— They concluded that OPCAB surgery is associated with less injury
๏‚— One approach to minimizing the risk of injury is to reduce myocardial oxygen demand. Pharmacologic beta-blockade is frequently instituted to reduce inotropy and achieve negative chronotropy using ultra-short-acting beta blockers such as esmolol and labetalol ๏‚— Another approach is to optimize the systemic mean blood pressures while reducing afterload. ๏‚— Calcium channel blockers, such as diltiazem, have been used to afford an effective reduction in blood pressure while minimizing a depression in myocardial contractility that may occur with beta blockers. ๏‚— Patients who become hypertensive during the operation may benefit from intravenous nitrates, which allows for coronary vasodilation and increased blood flow via collaterals. ๏‚— Gentle core cooling, by allowing the body temperature to drift to 35โ€“36ยฐC and deepening the level of anesthesia are concurrent measures that can also be employed.
Cardioplegia

Recommended

DHCA
DHCA DHCA
DHCA
Manu Jacob
ย 
ALPHA STAT & PH STAT.pptx
ALPHA STAT & PH STAT.pptxALPHA STAT & PH STAT.pptx
ALPHA STAT & PH STAT.pptx
ssuserb836a1
ย 
Basic principles of myocardial proctection
Basic principles of myocardial proctectionBasic principles of myocardial proctection
Basic principles of myocardial proctection
Raja Lahiri
ย 
8.myocardial protection during cpb
8.myocardial protection during cpb8.myocardial protection during cpb
8.myocardial protection during cpb
Manu Jacob
ย 
cardioplegia delivery management, perfusion safety
cardioplegia delivery management, perfusion safetycardioplegia delivery management, perfusion safety
cardioplegia delivery management, perfusion safety
Ida Simanjuntak
ย 
Deep hypothermic circulatory arrest in pediatric cardiac sur
Deep hypothermic circulatory arrest in pediatric cardiac surDeep hypothermic circulatory arrest in pediatric cardiac sur
Deep hypothermic circulatory arrest in pediatric cardiac sur
Manu Jacob
ย 
cannulation techniques during cpb
cannulation techniques during cpbcannulation techniques during cpb
cannulation techniques during cpb
Manu Jacob
ย 
Priming fluid and hemodilution
Priming fluid and hemodilutionPriming fluid and hemodilution
Priming fluid and hemodilution
Manu Jacob
ย 

Recommended

DHCA
DHCA DHCA
DHCA
Manu Jacob
ย 
ALPHA STAT & PH STAT.pptx
ALPHA STAT & PH STAT.pptxALPHA STAT & PH STAT.pptx
ALPHA STAT & PH STAT.pptx
ssuserb836a1
ย 
Basic principles of myocardial proctection
Basic principles of myocardial proctectionBasic principles of myocardial proctection
Basic principles of myocardial proctection
Raja Lahiri
ย 
8.myocardial protection during cpb
8.myocardial protection during cpb8.myocardial protection during cpb
8.myocardial protection during cpb
Manu Jacob
ย 
cardioplegia delivery management, perfusion safety
cardioplegia delivery management, perfusion safetycardioplegia delivery management, perfusion safety
cardioplegia delivery management, perfusion safety
Ida Simanjuntak
ย 
Deep hypothermic circulatory arrest in pediatric cardiac sur
Deep hypothermic circulatory arrest in pediatric cardiac surDeep hypothermic circulatory arrest in pediatric cardiac sur
Deep hypothermic circulatory arrest in pediatric cardiac sur
Manu Jacob
ย 
cannulation techniques during cpb
cannulation techniques during cpbcannulation techniques during cpb
cannulation techniques during cpb
Manu Jacob
ย 
Priming fluid and hemodilution
Priming fluid and hemodilutionPriming fluid and hemodilution
Priming fluid and hemodilution
Manu Jacob
ย 
Valvular Heart Disease & Anaesthetic Implications
Valvular Heart Disease & Anaesthetic ImplicationsValvular Heart Disease & Anaesthetic Implications
Valvular Heart Disease & Anaesthetic Implications
Dr.Daber Pareed
ย 
Transesophageal echocardiography(TEE)
Transesophageal echocardiography(TEE)Transesophageal echocardiography(TEE)
Transesophageal echocardiography(TEE)
LPS Institute of Cardiology Kanpur UP India
ย 
Transesophageal echocardiography
Transesophageal echocardiographyTransesophageal echocardiography
Transesophageal echocardiography
Amit Gulati
ย 
Pediatric cardiopulmonary bypass
Pediatric cardiopulmonary bypassPediatric cardiopulmonary bypass
Pediatric cardiopulmonary bypass
kp gourav
ย 
Anticoagulation and haemostasis during cardiopulmonary bypass
Anticoagulation and haemostasis during cardiopulmonary bypassAnticoagulation and haemostasis during cardiopulmonary bypass
Anticoagulation and haemostasis during cardiopulmonary bypass
Dhritiman Chakrabarti
ย 
ECMO - extracorporeal membrane oxygenation
ECMO - extracorporeal membrane oxygenationECMO - extracorporeal membrane oxygenation
ECMO - extracorporeal membrane oxygenation
prapulla chandra
ย 
CARDIOPULMONARY BYPASS
CARDIOPULMONARY BYPASSCARDIOPULMONARY BYPASS
CARDIOPULMONARY BYPASS
Manu Jacob
ย 
Ultrafiltration during cardiopulmonary_bypass
Ultrafiltration during cardiopulmonary_bypassUltrafiltration during cardiopulmonary_bypass
Ultrafiltration during cardiopulmonary_bypass
dr amarja nagre
ย 
principles of cardiopulmonary bypass
principles of cardiopulmonary bypassprinciples of cardiopulmonary bypass
principles of cardiopulmonary bypass
Ida Simanjuntak
ย 
WEANING FROM CPB.pptx
WEANING FROM CPB.pptxWEANING FROM CPB.pptx
WEANING FROM CPB.pptx
Manu Jacob
ย 
Cannulation and cardiopulmonary bypass.
Cannulation and cardiopulmonary bypass.Cannulation and cardiopulmonary bypass.
Cannulation and cardiopulmonary bypass.
Manu Jacob
ย 
Myocardial protection
Myocardial protectionMyocardial protection
Myocardial protection
EWOPCRE
ย 
Anesthesia Management in Aortic Regurgitation
Anesthesia Management in Aortic RegurgitationAnesthesia Management in Aortic Regurgitation
Anesthesia Management in Aortic Regurgitation
Dr. Harshil Joshi
ย 
Perioperative Arrythmias and management
Perioperative Arrythmias and managementPerioperative Arrythmias and management
Perioperative Arrythmias and management
Dr Nandini Deshpande
ย 
Anesthesia in CABG
Anesthesia in CABGAnesthesia in CABG
Anesthesia in CABG
Tenzin yoezer
ย 
Myocardial protection in cardiac surgery
Myocardial protection in cardiac surgeryMyocardial protection in cardiac surgery
Myocardial protection in cardiac surgery
drasadkhan1623
ย 
Cardioplegia.pptx
Cardioplegia.pptxCardioplegia.pptx
Cardioplegia.pptx
RajJinil
ย 
ECMO
ECMOECMO
ECMO
Dr Virbhan Balai
ย 
OPCAB
OPCABOPCAB
OPCAB
Geetanjali Verma
ย 
Pulmonary artery catheter
Pulmonary artery catheterPulmonary artery catheter
Pulmonary artery catheter
rajkumarsrihari
ย 
Myocardial protection DR NIKUNJ R SHEKHADA (MBBS ,MS GRN SURG , DNB CTS SR
Myocardial protection DR NIKUNJ R SHEKHADA (MBBS ,MS GRN SURG , DNB CTS SRMyocardial protection DR NIKUNJ R SHEKHADA (MBBS ,MS GRN SURG , DNB CTS SR
Myocardial protection DR NIKUNJ R SHEKHADA (MBBS ,MS GRN SURG , DNB CTS SR
DR NIKUNJ SHEKHADA
ย 
Myocardial Protection
Myocardial ProtectionMyocardial Protection
Myocardial Protection
Dhanesh Bhardwaj
ย 

More Related Content

What's hot

Anticoagulation and haemostasis during cardiopulmonary bypass
Anticoagulation and haemostasis during cardiopulmonary bypassAnticoagulation and haemostasis during cardiopulmonary bypass
Anticoagulation and haemostasis during cardiopulmonary bypass
Dhritiman Chakrabarti
ย 
ECMO - extracorporeal membrane oxygenation
ECMO - extracorporeal membrane oxygenationECMO - extracorporeal membrane oxygenation
ECMO - extracorporeal membrane oxygenation
prapulla chandra
ย 
Cannulation and cardiopulmonary bypass.
Cannulation and cardiopulmonary bypass.Cannulation and cardiopulmonary bypass.
Cannulation and cardiopulmonary bypass.
Manu Jacob
ย 
Myocardial protection
Myocardial protectionMyocardial protection
Myocardial protection
EWOPCRE
ย 

What's hot (20)

Valvular Heart Disease & Anaesthetic Implications
Valvular Heart Disease & Anaesthetic ImplicationsValvular Heart Disease & Anaesthetic Implications
Valvular Heart Disease & Anaesthetic Implications
ย 
Transesophageal echocardiography(TEE)
Transesophageal echocardiography(TEE)Transesophageal echocardiography(TEE)
Transesophageal echocardiography(TEE)
ย 
Transesophageal echocardiography
Transesophageal echocardiographyTransesophageal echocardiography
Transesophageal echocardiography
ย 
Pediatric cardiopulmonary bypass
Pediatric cardiopulmonary bypassPediatric cardiopulmonary bypass
Pediatric cardiopulmonary bypass
ย 
Anticoagulation and haemostasis during cardiopulmonary bypass
Anticoagulation and haemostasis during cardiopulmonary bypassAnticoagulation and haemostasis during cardiopulmonary bypass
Anticoagulation and haemostasis during cardiopulmonary bypass
ย 
ECMO - extracorporeal membrane oxygenation
ECMO - extracorporeal membrane oxygenationECMO - extracorporeal membrane oxygenation
ECMO - extracorporeal membrane oxygenation
ย 
CARDIOPULMONARY BYPASS
CARDIOPULMONARY BYPASSCARDIOPULMONARY BYPASS
CARDIOPULMONARY BYPASS
ย 
Ultrafiltration during cardiopulmonary_bypass
Ultrafiltration during cardiopulmonary_bypassUltrafiltration during cardiopulmonary_bypass
Ultrafiltration during cardiopulmonary_bypass
ย 
principles of cardiopulmonary bypass
principles of cardiopulmonary bypassprinciples of cardiopulmonary bypass
principles of cardiopulmonary bypass
ย 
WEANING FROM CPB.pptx
WEANING FROM CPB.pptxWEANING FROM CPB.pptx
WEANING FROM CPB.pptx
ย 
Cannulation and cardiopulmonary bypass.
Cannulation and cardiopulmonary bypass.Cannulation and cardiopulmonary bypass.
Cannulation and cardiopulmonary bypass.
ย 
Myocardial protection
Myocardial protectionMyocardial protection
Myocardial protection
ย 
Anesthesia Management in Aortic Regurgitation
Anesthesia Management in Aortic RegurgitationAnesthesia Management in Aortic Regurgitation
Anesthesia Management in Aortic Regurgitation
ย 
Perioperative Arrythmias and management
Perioperative Arrythmias and managementPerioperative Arrythmias and management
Perioperative Arrythmias and management
ย 
Anesthesia in CABG
Anesthesia in CABGAnesthesia in CABG
Anesthesia in CABG
ย 
Myocardial protection in cardiac surgery
Myocardial protection in cardiac surgeryMyocardial protection in cardiac surgery
Myocardial protection in cardiac surgery
ย 
Cardioplegia.pptx
Cardioplegia.pptxCardioplegia.pptx
Cardioplegia.pptx
ย 
ECMO
ECMOECMO
ECMO
ย 
OPCAB
OPCABOPCAB
OPCAB
ย 
Pulmonary artery catheter
Pulmonary artery catheterPulmonary artery catheter
Pulmonary artery catheter
ย 

Similar to Cardioplegia

Vasodilators & the Treatment of Angina Pectoris.ppt
Vasodilators & the Treatment of Angina Pectoris.pptVasodilators & the Treatment of Angina Pectoris.ppt
Vasodilators & the Treatment of Angina Pectoris.ppt
NorhanKhaled15
ย 
adenosine for casualty and icu patients ppt
adenosine for casualty and icu patients pptadenosine for casualty and icu patients ppt
adenosine for casualty and icu patients ppt
dinesh kumar
ย 
Preparation for separation 2010 final
Preparation for separation 2010 finalPreparation for separation 2010 final
Preparation for separation 2010 final
Abeer Nakera
ย 
Anaesthesia for off pump coronary artery bypass grafting
Anaesthesia for off pump coronary artery bypass graftingAnaesthesia for off pump coronary artery bypass grafting
Anaesthesia for off pump coronary artery bypass grafting
Manisha Sagar
ย 
Evaluation of antianginal drugs
Evaluation of antianginal drugsEvaluation of antianginal drugs
Evaluation of antianginal drugs
Nitin Shinde
ย 
Inotropes and vasopressors in cardiogenic shock
Inotropes and vasopressors in cardiogenic shockInotropes and vasopressors in cardiogenic shock
Inotropes and vasopressors in cardiogenic shock
Anwar Yusr
ย 
Pharmacology angina
Pharmacology anginaPharmacology angina
Pharmacology angina
MBBS IMS MSU
ย 
Pathophysiological approach of Angina Pectoris
Pathophysiological approach of Angina PectorisPathophysiological approach of Angina Pectoris
Pathophysiological approach of Angina Pectoris
Sreenivasa Reddy Thalla
ย 

Similar to Cardioplegia (20)

Myocardial protection DR NIKUNJ R SHEKHADA (MBBS ,MS GRN SURG , DNB CTS SR
Myocardial protection DR NIKUNJ R SHEKHADA (MBBS ,MS GRN SURG , DNB CTS SRMyocardial protection DR NIKUNJ R SHEKHADA (MBBS ,MS GRN SURG , DNB CTS SR
Myocardial protection DR NIKUNJ R SHEKHADA (MBBS ,MS GRN SURG , DNB CTS SR
ย 
Myocardial Protection
Myocardial ProtectionMyocardial Protection
Myocardial Protection
ย 
Antianginal drugs.pptx
Antianginal drugs.pptxAntianginal drugs.pptx
Antianginal drugs.pptx
ย 
5. ISCHEMIC HEART DISEASES (IHD).pptx
5. ISCHEMIC HEART DISEASES (IHD).pptx5. ISCHEMIC HEART DISEASES (IHD).pptx
5. ISCHEMIC HEART DISEASES (IHD).pptx
ย 
Htk costodial clinical effect edited nice
Htk costodial clinical effect edited nice Htk costodial clinical effect edited nice
Htk costodial clinical effect edited nice
ย 
Vasodilators & the Treatment of Angina Pectoris.ppt
Vasodilators & the Treatment of Angina Pectoris.pptVasodilators & the Treatment of Angina Pectoris.ppt
Vasodilators & the Treatment of Angina Pectoris.ppt
ย 
adenosine for casualty and icu patients ppt
adenosine for casualty and icu patients pptadenosine for casualty and icu patients ppt
adenosine for casualty and icu patients ppt
ย 
Preparation for separation 2010 final
Preparation for separation 2010 finalPreparation for separation 2010 final
Preparation for separation 2010 final
ย 
Integrated myocardial protection
Integrated myocardial protectionIntegrated myocardial protection
Integrated myocardial protection
ย 
Anaesthesia for off pump coronary artery bypass grafting
Anaesthesia for off pump coronary artery bypass graftingAnaesthesia for off pump coronary artery bypass grafting
Anaesthesia for off pump coronary artery bypass grafting
ย 
Inotropes and vasopressors in cardiogenic shock
Inotropes and vasopressors in cardiogenic shockInotropes and vasopressors in cardiogenic shock
Inotropes and vasopressors in cardiogenic shock
ย 
Evaluation of antianginal drugs
Evaluation of antianginal drugsEvaluation of antianginal drugs
Evaluation of antianginal drugs
ย 
PH1.28 Describe the mechanisms of action, types, doses, side effects, indicat...
PH1.28 Describe the mechanisms of action, types, doses, side effects, indicat...PH1.28 Describe the mechanisms of action, types, doses, side effects, indicat...
PH1.28 Describe the mechanisms of action, types, doses, side effects, indicat...
ย 
Inotropes and vasopressors in cardiogenic shock
Inotropes and vasopressors in cardiogenic shockInotropes and vasopressors in cardiogenic shock
Inotropes and vasopressors in cardiogenic shock
ย 
Hypothermia, DHCA, RCP, ACP,Oxygen consumption,Cooling, Rewarming.
Hypothermia, DHCA, RCP, ACP,Oxygen consumption,Cooling, Rewarming.Hypothermia, DHCA, RCP, ACP,Oxygen consumption,Cooling, Rewarming.
Hypothermia, DHCA, RCP, ACP,Oxygen consumption,Cooling, Rewarming.
ย 
Angina pectoris
Angina pectorisAngina pectoris
Angina pectoris
ย 
Pharmacology angina
Pharmacology anginaPharmacology angina
Pharmacology angina
ย 
MI-2013.ppt
MI-2013.pptMI-2013.ppt
MI-2013.ppt
ย 
Pathophysiological approach of Angina Pectoris
Pathophysiological approach of Angina PectorisPathophysiological approach of Angina Pectoris
Pathophysiological approach of Angina Pectoris
ย 
Clinical Implications of Ischemic Pre and Postconditioning
Clinical Implications of Ischemic Pre and PostconditioningClinical Implications of Ischemic Pre and Postconditioning
Clinical Implications of Ischemic Pre and Postconditioning
ย 

More from Raja Lahiri

More from Raja Lahiri (12)

Coronary angiography
Coronary angiographyCoronary angiography
Coronary angiography
ย 
Pr after tof
Pr after tofPr after tof
Pr after tof
ย 
Lvad
LvadLvad
Lvad
ย 
Dabigatran2
Dabigatran2Dabigatran2
Dabigatran2
ย 
Pft dr s kundu sskm
Pft dr s kundu sskmPft dr s kundu sskm
Pft dr s kundu sskm
ย 
Vsd surgery
Vsd surgeryVsd surgery
Vsd surgery
ย 
Tolvaptan cme slide
Tolvaptan cme slideTolvaptan cme slide
Tolvaptan cme slide
ย 
Ross preocedure
Ross preocedureRoss preocedure
Ross preocedure
ย 
vsd
vsdvsd
vsd
ย 
Pa banding new
Pa banding newPa banding new
Pa banding new
ย 
Heart transplant
Heart transplantHeart transplant
Heart transplant
ย 
Aortic aneurysm
Aortic aneurysmAortic aneurysm
Aortic aneurysm
ย 

Recently uploaded

Call Girls Bangalore - 450+ Call Girl Cash Payment ๐Ÿ’ฏCall Us ๐Ÿ” 6378878445 ๐Ÿ” ๐Ÿ’ƒ ...
Call Girls Bangalore - 450+ Call Girl Cash Payment ๐Ÿ’ฏCall Us ๐Ÿ” 6378878445 ๐Ÿ” ๐Ÿ’ƒ ...Call Girls Bangalore - 450+ Call Girl Cash Payment ๐Ÿ’ฏCall Us ๐Ÿ” 6378878445 ๐Ÿ” ๐Ÿ’ƒ ...
Call Girls Bangalore - 450+ Call Girl Cash Payment ๐Ÿ’ฏCall Us ๐Ÿ” 6378878445 ๐Ÿ” ๐Ÿ’ƒ ...
gragneelam30
ย 
Kolkata Call Girls Naktala ๐Ÿ’ฏCall Us ๐Ÿ” 8005736733 ๐Ÿ” ๐Ÿ’ƒ Top Class Call Girl Se...
Kolkata Call Girls Naktala ๐Ÿ’ฏCall Us ๐Ÿ” 8005736733 ๐Ÿ” ๐Ÿ’ƒ Top Class Call Girl Se...Kolkata Call Girls Naktala ๐Ÿ’ฏCall Us ๐Ÿ” 8005736733 ๐Ÿ” ๐Ÿ’ƒ Top Class Call Girl Se...
Kolkata Call Girls Naktala ๐Ÿ’ฏCall Us ๐Ÿ” 8005736733 ๐Ÿ” ๐Ÿ’ƒ Top Class Call Girl Se...
Namrata Singh
ย 
๐Ÿ’šChandigarh Call Girls Service ๐Ÿ’ฏPiya ๐Ÿ“ฒ๐Ÿ”8868886958๐Ÿ”Call Girls In Chandigarh No...
๐Ÿ’šChandigarh Call Girls Service ๐Ÿ’ฏPiya ๐Ÿ“ฒ๐Ÿ”8868886958๐Ÿ”Call Girls In Chandigarh No...๐Ÿ’šChandigarh Call Girls Service ๐Ÿ’ฏPiya ๐Ÿ“ฒ๐Ÿ”8868886958๐Ÿ”Call Girls In Chandigarh No...
๐Ÿ’šChandigarh Call Girls Service ๐Ÿ’ฏPiya ๐Ÿ“ฒ๐Ÿ”8868886958๐Ÿ”Call Girls In Chandigarh No...
Sheetaleventcompany
ย 
โค๏ธChandigarh Escorts Serviceโ˜Ž๏ธ9814379184โ˜Ž๏ธ Call Girl service in Chandigarhโ˜Ž๏ธ ...
โค๏ธChandigarh Escorts Serviceโ˜Ž๏ธ9814379184โ˜Ž๏ธ Call Girl service in Chandigarhโ˜Ž๏ธ ...โค๏ธChandigarh Escorts Serviceโ˜Ž๏ธ9814379184โ˜Ž๏ธ Call Girl service in Chandigarhโ˜Ž๏ธ ...
โค๏ธChandigarh Escorts Serviceโ˜Ž๏ธ9814379184โ˜Ž๏ธ Call Girl service in Chandigarhโ˜Ž๏ธ ...
Sheetaleventcompany
ย 
Jaipur Call Girl Service ๐Ÿ“ž9xx000xx09๐Ÿ“žJust Call Divya๐Ÿ“ฒ Call Girl In Jaipur No๐Ÿ’ฐ...
Jaipur Call Girl Service ๐Ÿ“ž9xx000xx09๐Ÿ“žJust Call Divya๐Ÿ“ฒ Call Girl In Jaipur No๐Ÿ’ฐ...Jaipur Call Girl Service ๐Ÿ“ž9xx000xx09๐Ÿ“žJust Call Divya๐Ÿ“ฒ Call Girl In Jaipur No๐Ÿ’ฐ...
Jaipur Call Girl Service ๐Ÿ“ž9xx000xx09๐Ÿ“žJust Call Divya๐Ÿ“ฒ Call Girl In Jaipur No๐Ÿ’ฐ...
Sheetaleventcompany
ย 
Race Course Road } Book Call Girls in Bangalore | Whatsapp No 6378878445 VIP ...
Race Course Road } Book Call Girls in Bangalore | Whatsapp No 6378878445 VIP ...Race Course Road } Book Call Girls in Bangalore | Whatsapp No 6378878445 VIP ...
Race Course Road } Book Call Girls in Bangalore | Whatsapp No 6378878445 VIP ...
dishamehta3332
ย 
Call 8250092165 Patna Call Girls โ‚น4.5k Cash Payment With Room Delivery
Call 8250092165 Patna Call Girls โ‚น4.5k Cash Payment With Room DeliveryCall 8250092165 Patna Call Girls โ‚น4.5k Cash Payment With Room Delivery
Call 8250092165 Patna Call Girls โ‚น4.5k Cash Payment With Room Delivery
Jyoti singh
ย 
Call Girls Shahdol Just Call 8250077686 Top Class Call Girl Service Available
Call Girls Shahdol Just Call 8250077686 Top Class Call Girl Service AvailableCall Girls Shahdol Just Call 8250077686 Top Class Call Girl Service Available
Call Girls Shahdol Just Call 8250077686 Top Class Call Girl Service Available
Dipal Arora
ย 
Whitefield { Call Girl in Bangalore โ‚น7.5k Pick Up & Drop With Cash Payment 63...
Whitefield { Call Girl in Bangalore โ‚น7.5k Pick Up & Drop With Cash Payment 63...Whitefield { Call Girl in Bangalore โ‚น7.5k Pick Up & Drop With Cash Payment 63...
Whitefield { Call Girl in Bangalore โ‚น7.5k Pick Up & Drop With Cash Payment 63...
dishamehta3332
ย 
โค๏ธCall Girl Service In Chandigarhโ˜Ž๏ธ9814379184โ˜Ž๏ธ Call Girl in Chandigarhโ˜Ž๏ธ Cha...
โค๏ธCall Girl Service In Chandigarhโ˜Ž๏ธ9814379184โ˜Ž๏ธ Call Girl in Chandigarhโ˜Ž๏ธ Cha...โค๏ธCall Girl Service In Chandigarhโ˜Ž๏ธ9814379184โ˜Ž๏ธ Call Girl in Chandigarhโ˜Ž๏ธ Cha...
โค๏ธCall Girl Service In Chandigarhโ˜Ž๏ธ9814379184โ˜Ž๏ธ Call Girl in Chandigarhโ˜Ž๏ธ Cha...
Sheetaleventcompany
ย 
๐Ÿ’šCall Girls In Amritsar ๐Ÿ’ฏAnvi ๐Ÿ“ฒ๐Ÿ”8725944379๐Ÿ”Amritsar Call Girl No๐Ÿ’ฐAdvance Cash...
๐Ÿ’šCall Girls In Amritsar ๐Ÿ’ฏAnvi ๐Ÿ“ฒ๐Ÿ”8725944379๐Ÿ”Amritsar Call Girl No๐Ÿ’ฐAdvance Cash...๐Ÿ’šCall Girls In Amritsar ๐Ÿ’ฏAnvi ๐Ÿ“ฒ๐Ÿ”8725944379๐Ÿ”Amritsar Call Girl No๐Ÿ’ฐAdvance Cash...
๐Ÿ’šCall Girls In Amritsar ๐Ÿ’ฏAnvi ๐Ÿ“ฒ๐Ÿ”8725944379๐Ÿ”Amritsar Call Girl No๐Ÿ’ฐAdvance Cash...
Sheetaleventcompany
ย 
Gastric Cancer: ะกlinical Implementation of Artificial Intelligence, Synergeti...
Gastric Cancer: ะกlinical Implementation of Artificial Intelligence, Synergeti...Gastric Cancer: ะกlinical Implementation of Artificial Intelligence, Synergeti...
Gastric Cancer: ะกlinical Implementation of Artificial Intelligence, Synergeti...
Oleg Kshivets
ย 
Jual Obat Aborsi Di Dubai UAE Wa 0838-4800-7379 Obat Penggugur Kandungan Cytotec
Jual Obat Aborsi Di Dubai UAE Wa 0838-4800-7379 Obat Penggugur Kandungan CytotecJual Obat Aborsi Di Dubai UAE Wa 0838-4800-7379 Obat Penggugur Kandungan Cytotec
Jual Obat Aborsi Di Dubai UAE Wa 0838-4800-7379 Obat Penggugur Kandungan Cytotec
jualobat34
ย 

Recently uploaded (20)

Call Girls Bangalore - 450+ Call Girl Cash Payment ๐Ÿ’ฏCall Us ๐Ÿ” 6378878445 ๐Ÿ” ๐Ÿ’ƒ ...
Call Girls Bangalore - 450+ Call Girl Cash Payment ๐Ÿ’ฏCall Us ๐Ÿ” 6378878445 ๐Ÿ” ๐Ÿ’ƒ ...Call Girls Bangalore - 450+ Call Girl Cash Payment ๐Ÿ’ฏCall Us ๐Ÿ” 6378878445 ๐Ÿ” ๐Ÿ’ƒ ...
Call Girls Bangalore - 450+ Call Girl Cash Payment ๐Ÿ’ฏCall Us ๐Ÿ” 6378878445 ๐Ÿ” ๐Ÿ’ƒ ...
ย 
Kolkata Call Girls Naktala ๐Ÿ’ฏCall Us ๐Ÿ” 8005736733 ๐Ÿ” ๐Ÿ’ƒ Top Class Call Girl Se...
Kolkata Call Girls Naktala ๐Ÿ’ฏCall Us ๐Ÿ” 8005736733 ๐Ÿ” ๐Ÿ’ƒ Top Class Call Girl Se...Kolkata Call Girls Naktala ๐Ÿ’ฏCall Us ๐Ÿ” 8005736733 ๐Ÿ” ๐Ÿ’ƒ Top Class Call Girl Se...
Kolkata Call Girls Naktala ๐Ÿ’ฏCall Us ๐Ÿ” 8005736733 ๐Ÿ” ๐Ÿ’ƒ Top Class Call Girl Se...
ย 
Shazia Iqbal 2024 - Bioorganic Chemistry.pdf
Shazia Iqbal 2024 - Bioorganic Chemistry.pdfShazia Iqbal 2024 - Bioorganic Chemistry.pdf
Shazia Iqbal 2024 - Bioorganic Chemistry.pdf
ย 
ANATOMY AND PHYSIOLOGY OF RESPIRATORY SYSTEM.pptx
ANATOMY AND PHYSIOLOGY OF RESPIRATORY SYSTEM.pptxANATOMY AND PHYSIOLOGY OF RESPIRATORY SYSTEM.pptx
ANATOMY AND PHYSIOLOGY OF RESPIRATORY SYSTEM.pptx
ย 
๐Ÿ’šChandigarh Call Girls Service ๐Ÿ’ฏPiya ๐Ÿ“ฒ๐Ÿ”8868886958๐Ÿ”Call Girls In Chandigarh No...
๐Ÿ’šChandigarh Call Girls Service ๐Ÿ’ฏPiya ๐Ÿ“ฒ๐Ÿ”8868886958๐Ÿ”Call Girls In Chandigarh No...๐Ÿ’šChandigarh Call Girls Service ๐Ÿ’ฏPiya ๐Ÿ“ฒ๐Ÿ”8868886958๐Ÿ”Call Girls In Chandigarh No...
๐Ÿ’šChandigarh Call Girls Service ๐Ÿ’ฏPiya ๐Ÿ“ฒ๐Ÿ”8868886958๐Ÿ”Call Girls In Chandigarh No...
ย 
โค๏ธChandigarh Escorts Serviceโ˜Ž๏ธ9814379184โ˜Ž๏ธ Call Girl service in Chandigarhโ˜Ž๏ธ ...
โค๏ธChandigarh Escorts Serviceโ˜Ž๏ธ9814379184โ˜Ž๏ธ Call Girl service in Chandigarhโ˜Ž๏ธ ...โค๏ธChandigarh Escorts Serviceโ˜Ž๏ธ9814379184โ˜Ž๏ธ Call Girl service in Chandigarhโ˜Ž๏ธ ...
โค๏ธChandigarh Escorts Serviceโ˜Ž๏ธ9814379184โ˜Ž๏ธ Call Girl service in Chandigarhโ˜Ž๏ธ ...
ย 
Ahmedabad Call Girls Book Now 9630942363 Top Class Ahmedabad Escort Service A...
Ahmedabad Call Girls Book Now 9630942363 Top Class Ahmedabad Escort Service A...Ahmedabad Call Girls Book Now 9630942363 Top Class Ahmedabad Escort Service A...
Ahmedabad Call Girls Book Now 9630942363 Top Class Ahmedabad Escort Service A...
ย 
Jaipur Call Girl Service ๐Ÿ“ž9xx000xx09๐Ÿ“žJust Call Divya๐Ÿ“ฒ Call Girl In Jaipur No๐Ÿ’ฐ...
Jaipur Call Girl Service ๐Ÿ“ž9xx000xx09๐Ÿ“žJust Call Divya๐Ÿ“ฒ Call Girl In Jaipur No๐Ÿ’ฐ...Jaipur Call Girl Service ๐Ÿ“ž9xx000xx09๐Ÿ“žJust Call Divya๐Ÿ“ฒ Call Girl In Jaipur No๐Ÿ’ฐ...
Jaipur Call Girl Service ๐Ÿ“ž9xx000xx09๐Ÿ“žJust Call Divya๐Ÿ“ฒ Call Girl In Jaipur No๐Ÿ’ฐ...
ย 
Race Course Road } Book Call Girls in Bangalore | Whatsapp No 6378878445 VIP ...
Race Course Road } Book Call Girls in Bangalore | Whatsapp No 6378878445 VIP ...Race Course Road } Book Call Girls in Bangalore | Whatsapp No 6378878445 VIP ...
Race Course Road } Book Call Girls in Bangalore | Whatsapp No 6378878445 VIP ...
ย 
Call 8250092165 Patna Call Girls โ‚น4.5k Cash Payment With Room Delivery
Call 8250092165 Patna Call Girls โ‚น4.5k Cash Payment With Room DeliveryCall 8250092165 Patna Call Girls โ‚น4.5k Cash Payment With Room Delivery
Call 8250092165 Patna Call Girls โ‚น4.5k Cash Payment With Room Delivery
ย 
VIP Hyderabad Call Girls KPHB 7877925207 โ‚น5000 To 25K With AC Room ๐Ÿ’š๐Ÿ˜‹
VIP Hyderabad Call Girls KPHB 7877925207 โ‚น5000 To 25K With AC Room ๐Ÿ’š๐Ÿ˜‹VIP Hyderabad Call Girls KPHB 7877925207 โ‚น5000 To 25K With AC Room ๐Ÿ’š๐Ÿ˜‹
VIP Hyderabad Call Girls KPHB 7877925207 โ‚น5000 To 25K With AC Room ๐Ÿ’š๐Ÿ˜‹
ย 
Call Girls Shahdol Just Call 8250077686 Top Class Call Girl Service Available
Call Girls Shahdol Just Call 8250077686 Top Class Call Girl Service AvailableCall Girls Shahdol Just Call 8250077686 Top Class Call Girl Service Available
Call Girls Shahdol Just Call 8250077686 Top Class Call Girl Service Available
ย 
Whitefield { Call Girl in Bangalore โ‚น7.5k Pick Up & Drop With Cash Payment 63...
Whitefield { Call Girl in Bangalore โ‚น7.5k Pick Up & Drop With Cash Payment 63...Whitefield { Call Girl in Bangalore โ‚น7.5k Pick Up & Drop With Cash Payment 63...
Whitefield { Call Girl in Bangalore โ‚น7.5k Pick Up & Drop With Cash Payment 63...
ย 
Intramuscular & Intravenous Injection.pptx
Intramuscular & Intravenous Injection.pptxIntramuscular & Intravenous Injection.pptx
Intramuscular & Intravenous Injection.pptx
ย 
โค๏ธCall Girl Service In Chandigarhโ˜Ž๏ธ9814379184โ˜Ž๏ธ Call Girl in Chandigarhโ˜Ž๏ธ Cha...
โค๏ธCall Girl Service In Chandigarhโ˜Ž๏ธ9814379184โ˜Ž๏ธ Call Girl in Chandigarhโ˜Ž๏ธ Cha...โค๏ธCall Girl Service In Chandigarhโ˜Ž๏ธ9814379184โ˜Ž๏ธ Call Girl in Chandigarhโ˜Ž๏ธ Cha...
โค๏ธCall Girl Service In Chandigarhโ˜Ž๏ธ9814379184โ˜Ž๏ธ Call Girl in Chandigarhโ˜Ž๏ธ Cha...
ย 
๐Ÿ’šCall Girls In Amritsar ๐Ÿ’ฏAnvi ๐Ÿ“ฒ๐Ÿ”8725944379๐Ÿ”Amritsar Call Girl No๐Ÿ’ฐAdvance Cash...
๐Ÿ’šCall Girls In Amritsar ๐Ÿ’ฏAnvi ๐Ÿ“ฒ๐Ÿ”8725944379๐Ÿ”Amritsar Call Girl No๐Ÿ’ฐAdvance Cash...๐Ÿ’šCall Girls In Amritsar ๐Ÿ’ฏAnvi ๐Ÿ“ฒ๐Ÿ”8725944379๐Ÿ”Amritsar Call Girl No๐Ÿ’ฐAdvance Cash...
๐Ÿ’šCall Girls In Amritsar ๐Ÿ’ฏAnvi ๐Ÿ“ฒ๐Ÿ”8725944379๐Ÿ”Amritsar Call Girl No๐Ÿ’ฐAdvance Cash...
ย 
Genuine Call Girls Hyderabad 9630942363 Book High Profile Call Girl in Hydera...
Genuine Call Girls Hyderabad 9630942363 Book High Profile Call Girl in Hydera...Genuine Call Girls Hyderabad 9630942363 Book High Profile Call Girl in Hydera...
Genuine Call Girls Hyderabad 9630942363 Book High Profile Call Girl in Hydera...
ย 
ANATOMY AND PHYSIOLOGY OF REPRODUCTIVE SYSTEM.pptx
ANATOMY AND PHYSIOLOGY OF REPRODUCTIVE SYSTEM.pptxANATOMY AND PHYSIOLOGY OF REPRODUCTIVE SYSTEM.pptx
ANATOMY AND PHYSIOLOGY OF REPRODUCTIVE SYSTEM.pptx
ย 
Gastric Cancer: ะกlinical Implementation of Artificial Intelligence, Synergeti...
Gastric Cancer: ะกlinical Implementation of Artificial Intelligence, Synergeti...Gastric Cancer: ะกlinical Implementation of Artificial Intelligence, Synergeti...
Gastric Cancer: ะกlinical Implementation of Artificial Intelligence, Synergeti...
ย 
Jual Obat Aborsi Di Dubai UAE Wa 0838-4800-7379 Obat Penggugur Kandungan Cytotec
Jual Obat Aborsi Di Dubai UAE Wa 0838-4800-7379 Obat Penggugur Kandungan CytotecJual Obat Aborsi Di Dubai UAE Wa 0838-4800-7379 Obat Penggugur Kandungan Cytotec
Jual Obat Aborsi Di Dubai UAE Wa 0838-4800-7379 Obat Penggugur Kandungan Cytotec
ย 

Cardioplegia

  • 2. Topics ๏‚— Alternative arresting agents & additives ๏‚— Crystalloid vs Blood cardioplegia ๏‚— Potential newer technology
  • 3.
  • 4.
  • 5. Adenosine receptors ๏‚— Four types of adenosine receptors: A1, A2a, A2b, A3 ๏‚— Activation of adenosine A 1 receptors leads to: โ—ฆ inhibition of cyclic AMP production โ—ฆ inhibition of the slow calcium channel โ—ฆ opening of an adenosine-activated ATPsensitive potassium (K ATP ) channel ๏‚— This leads to hyperpolarization, which delays conduction through the AV node and slows the ventricular response to atrial tachycardia. ๏‚— It also causes endothelial-dependent relaxation of smooth muscle as is found inside the artery walls. ๏‚— Activation of A2A receptors produces a constellation of responses that in general can be classified as anti- inflammatory ๏‚— Pretreatment with adenosine confers a cardioprotective effect during ischemia and can inhibit the inflammatory responses initiated by ischemia and reperfusion
  • 6.
  • 7. Minute work & Oxygen demand ๏‚— Minute work = Heart rate x Stroke volume x Pressure ๏‚— However, minute work is not the direct determinant of oxygen consumption ๏‚— The primary determinant of oxygen demand is the wall tension or stress developed in each cardiac cycle. ๏‚— The energetic cost of ejecting blood from the ventricular chamber is approximately 20 to 30% of that required for isovolumic contraction. ๏‚— An increase in afterload requires greater energy than an increase in volume ejected. ๏‚— Oxygen consumption is also increased as the heart dilates and begins ejection from a greater diastolic volume. ๏‚— Cardiac efficiency = Work/MVO2
  • 8. Alternative arresting agents & Additives ๏‚— Beta Blockers: โ—ฆ As the ascending aorta is clamped, the non- exocytotic release of norepinephrine from the cardiac sympathetic nerves acts on ฮฒ-adrenergic receptors on the outer surface of the sarcolemma, causing an increase in cAMPdependent protein kinase activity, phosphorylation of the calcium release channels, and increased Ca2+ influx, resulting in increased Ca2+-dependent contractility and rapid depletion of glycogen stores. โ—ฆ Early studies suggested that long-acting beta blockers improved myocardialprotection during ischemia but unfortunately have a prolonged negative inotropic effect, which limits their clinical use.
  • 9. ๏‚— Beta blockers such as propranolol have been used as an adjunct to anesthesia to block ฮฒ-adrenergicโ€“ stimulating episodes associated with coronary ischemia during the course of the operative procedure. ๏‚— Ultra-short-acting cardioselective beta blockers such as landiolol and esmolol provide polarized cardiac arrest by maintaining the membrane potential at or near the resting membrane potential ๏‚— Esmolol has been used to enhance myocardial protection during intermittent arrest and has been shown to provide myocardial preservation equivalent to or better than cold crystalloid or blood cardioplegia. ๏‚— With esmolol cardioplegia, there is a slow undulating ventricular contraction that may decrease myocardial edema but does not provide a quiescent operating field
  • 10. Adenocaine ๏‚— Adenosine-lidocaine (adenocaine) cardioplegia provides an exciting alternative to depolarizing cardioplegia. ๏‚— Adenosine-lidocaine cardioplegia has been shown to provide a shorter time to electromechanical arrest, greater postischemic recoveries of aortic flow, a lower coronary vascular resistance during infusion, and greater MVO2 as compared to St. Thomasโ€™ Hospital solution, while maintaining the myocardial cell membrane potential at its resting state
  • 11. Agents Affecting Calcium Transport๏‚— The infusion of calcium-free cardioplegic solutions induces rapid diastolic cardiac arrest by inhibiting excitation-coupling and increases permeability of the sarcolemma. ๏‚— When a calcium-containing perfusate is then reinfused, during reperfusion, there is a rapid influx of calcium into the cell, resulting in myocardial contracture and extensive ultrastructural damage, the โ€œcalcium paradox.โ€ ๏‚— Calcium antagonist agents administered before ischemia have been proposed as a possible mechanism to reduce ischemic cellular injury. ๏‚— Calcium channel blocking agents, including verapamil, diltiazem, and nifedipine, prevent calcium-induced calcium release in myocardial cells and, as an adjunct to normothermic cardioplegia, have been shown to improve postischemic systolic function. ๏‚— Calcium blockers have no effect if they are administered before reperfusion, are temperature dependent, and have limited effect during hypothermia. ๏‚— Because high concentrations are required for cardioprotection, their prolonged membrane binding prevents rapid recovery, thus limiting their clinical usefulness.
  • 12. ๏‚— Magnesium: โ—ฆ Magnesium inhibits calcium entry into the cell by displacing calcium from its binding sites in the sarcolemmal membrane. โ—ฆ It has limited use as an arresting agent because high concentrations are required, cardiac arrest is delayed, and postischemic functional recovery is decreased in comparison to potassium cardioplegia. โ—ฆ The advantages of magnesium have been shown to be optimal when it is included with high-potassium cardioplegia, in which it has been demonstrated to ameliorate cytosolic, nuclear, and mitochondrial calcium accumulation; preserve high-energy phosphate moieties; and enhance postischemic functional recovery.
  • 13. Avoidance of Substrate Depletion ๏‚— Metabolic substrates have been added to cardioplegic solutions to enhance anaerobic metabolism during ischemia or to provide citric acid cycle intermediaries to facilitate homeostasis during reperfusion. ๏‚— Agents used include glucose and insulin; nucleosides, such as adenosine, aspartate, and glutamate; and L-arginine to stimulate nitric oxide production. ๏‚— Although metabolic substrate enhancement has been used in various clinical situations, none has achieved universal adoption.
  • 14. Blood v/s Crystalloid cardioplegia ๏‚— Crystalloid cardioplegia: โ—ฆ these solutions contain minimal amounts (0.6 mL/100 mL at a PO2 of 100 mm Hg at a temperature of 10ยฐ C) of dissolved oxygen, whereas the myocardium consumes 0.33 mL of oxygen per 100 g at 15ยฐ C. โ—ฆ Because even a short period of ischemia results in the gradual accumulation of oxygen debt, moderate to severe myocardial hypothermia is necessary to prevent the rapid degradation of energy stores โ—ฆ To overcome the oxygen deficit issue, oxygenation of crystalloid cardioplegia has been clinically used and has demonstrated a decrease in creatine kinase MB levels
  • 15. Clinical steps for myocardial protection with use of crystalloid cardioplegia 1. Before the onset of surgery, the operating room temperature is cooled to 17ยฐ C to 19ยฐ C to avoid warming of the anterior surface of the heart by convection and radiation from highintensity lighting. 2. Cardiopulmonary bypass is initiated at a temperature of 28ยฐ C. 3. A myocardial electrocardiographic lead and temperature probe are placed on the anterior wall of the right ventricle because it constitutes two thirds of the anterior surface of the heart, and its rewarming during surgically induced ischemia may partially explain the occasional observation of selective right ventricular failure after the termination of bypass 4. an insulation pad is placed in the posterior pericardial sac and along the left ventricular lateral wall to protect the left phrenic nerve from thermal injury associated with regional
  • 16. 5. The systemic perfusate temperature is temporarily decreased to 10ยฐ C to 15ยฐ C to โ€œprecoolโ€ the heart (infusion hypothermia), and iced saline slush is placed into the pericardial sac to achieve rapid myocardial cooling 6. When a myocardial temperature of 28ยฐ C is reached, the ascending aorta is cross-clamped and cold crystalloid cardioplegia solution at a temperature of 5ยฐ C is infused into the aortic root at a pressure not exceeding 90 mm Hg @10ml/kg 7. At the termination of the initial cardioplegic infusion, the systemic temperature is elevated to 20ยฐ C, and the systemic perfusion flow rate is decreased from 2.2 to 1.5 liter/min/m2 .Increase in myocardial temperature above 20ยฐ C or if there is any electrocardiographic activity or observed ventricular motion, the solution is reinfused at a volume of 5 mL/kg. 8. Five minutes before removal of the aortic clamp, the systemic perfusate temperature is raised to 30ยฐ C, and flow is increased to 2.2 liter/min/m2. 9. After the aortic cross-clamp is removed, the perfusate temperature is raised to 38ยฐ C and the room temperature is raised to 25ยฐ C to 30ยฐ C. 10. Cardiopulmonary bypass is continued until the esophageal temperature is 37ยฐ C and the rectal temperature is in the range of 35ยฐ C to 37ยฐ C.
  • 17. Disadvantage of crystalloid cardioplegia ๏‚— Extensive rewarming period, which may exceed 30 to 45 minutes. ๏‚— Slow recovery of myocardial metabolism ๏‚— Poor response to postoperative hemodynamic stress ๏‚— Gradual accumulation of oxygen debt and myocardial damage if adequate hypothermia not maintained
  • 18. Blood Cardioplegia ๏‚— Advantages: โ—ฆ Optimum oxygenation (superior to oxygenated crystalloids) โ—ฆ Better removal of carbon-dioxide โ—ฆ Buffering action and reducing agent โ—ฆ Presence of colloid avoids adverse oncotic pressure gradients โ—ฆ presence of oxygen free radical scavengers โ—ฆ Preserves microvascular responses compared with crystalloid cardioplegia
  • 19. Blood Cardioplegia ๏‚— Concerns: โ—ฆ the hypothermic shift to the left of the oxyhemoglobin dissociation curve, thereby reducing the release of oxygen at the tissue level โ—ฆ the experimental evidence that blood cardioplegia may not protect the myocardium at low temperatures โ—ฆ the potential of hypothermia induced sludging and red cell rouleau formation.
  • 20. Warm blood cardioplegia ๏‚— In 1982 Rosenkranz and colleagues reported that warm induction with normothermic blood cardioplegia, with multidose cold blood cardioplegia maintenance of arrest, resulted in better recovery of function in canines than a similar protocol using cold blood induction ๏‚— In 1986, Teoh and colleagues provided experimental evidence that a terminal infusion of warm blood cardioplegia before removing the cross-clamp (a โ€œhot shotโ€) accelerated myocardial metabolic recovery ๏‚— This was followed by a report in 1991 by Lichtenstein and colleagues that normothermic blood cardioplegia in humans is an effective cardio-protective approach.
  • 21. ๏‚— Despite these encouraging reports, there are concerns that for any given patient, it is difficult to determine how long a warm heart can tolerate an ischemic insult if the infusion is interrupted or flow rates are reduced owing to an obscured surgical field or a maldistribution of the cardioplegic solution. ๏‚— Another concern is the report by Martin and colleagues that warm cardioplegia is associated with a threefold increased incidence of neurologic deficits. ๏‚— Subsequent studies have indicated however that appropriately designed protocols using intermittent antegrade warm blood cardioplegia provide clinically acceptable myocardial protection
  • 22. Tepid blood cardioplegia ๏‚— Both cold blood (4 to 10ยฐC) and warm blood cardioplegic solutions (37ยฐC) have temperature- related advantages and disadvantages. ๏‚— Hayashida and colleagues were one of the first groups to study specifically the efficacy of tepid blood (29ยฐC) cardioplegia. Their study showed that tepid antegrade cardioplegia was the most effective in reducing anaerobic lactate acid release during the arrest period. ๏‚— Mallidi et al showed that warm or tepid blood cardioplegia may be associated with better early and late event-free survivals after CABG ๏‚— Although tepid blood cardioplegia may be safe and effective, the majority of studies have been single- center studies conducted in relatively small cohorts of patients. Whether tepid cardioplegia confers superior protection over other current methodologies remains to be determined.
  • 23. Miniplegia ๏‚— The use of undiluted blood cardioplegia, or โ€œminiplegiaโ€ (using a minimum amount of crystalloid additives), also has been reported to be effective. ๏‚— Petrucci et al. studied the use of all blood miniplegia in a clinically relevant swine preparation and compared miniplegia with crystalloid cardioplegia. ๏‚— They concluded that the use of all blood miniplegia was effective or superior in the acutely ischemic heart. ๏‚— Rousou and colleagues showed that it is the level of hypothermia that is important in blood cardioplegia, not necessarily the hematocrit.
  • 24. Advantages of Blood cardioplegia (1) provides an oxygenated environment and a method for intermittent reoxygenation of the heart during arrest (2) limits hemodilution when large volumes of cardioplegic solution are used (3) affords an excellent buffering capacity and osmotic properties (4) allows for electrolyte composition and pH that are physiologic (5) offers a number of endogenous antioxidants and free-radical scavengers (6) is less complex than other solutions to prepare.
  • 25.
  • 26.
  • 27. Novel strategies for cardioprotection ๏‚— Physiologic: โ—ฆ Ischaemic preconditioning โ—ฆ Post conditioning โ—ฆ Remote ischaemic preconditioning โ—ฆ Autophagy ๏‚— Pharmacologic: โ—ฆ Adenosine โ—ฆ Acadesine โ—ฆ Sodium-Hydrogen exchanger inhibitors โ—ฆ Glucose-Insulin-Potassium (GIK)
  • 28. Ischaemic preconditioning ๏‚— โ€œPrecondition with ischemiaโ€ is an endogenous adaptive phenomenon whereby the heart becomes more tolerant to a period of prolonged ischemia if first exposed to brief episodes of coronary artery occlusion. ๏‚— IPC has been demonstrated to persist as long as 1 to 2 hours after the ischemic preconditioning stimulus & becomes ineffective when the sustained ischemic insult exceeds 3 hours ๏‚— A second phase of protection appears 24 hours later and is sustained for up to 72 hours. This has been referred to as the second window of protection, late- phase preconditioning, or delayed preconditioning. ๏‚— Unlike classic IPC, which protects only against infarction, the late phase protects against both infarction and myocardial stunning.
  • 29. 1
  • 30. Clinical relevance of IPC ๏‚— Patients experiencing angina before an MI have a better in-hospital prognosis and a reduced incidence of cardiogenic shock, fewer and less severe episodes of congestive heart failure, and smaller infarcts as assessed by cardiac enzyme release and better long term survival rates ๏‚— Patients who undergo percutaneous coronary interventions (PCI) have an enhanced tolerance to ischemia after the first balloon inflation, provided that the first balloon inflation exceeds 60 to 90 seconds ๏‚— Intermittent cross-clamping with the heart paced at 90 beats per minute to induce ischemia, followed by 2 minutes of reperfusion before a 10- minute period of global ischemia and ventricular fibrillation has shown attenuation of troponin release
  • 31. Post conditioning ๏‚— First reported by Zhao et al in canine model ๏‚— Rapid intermittent interruptions of blood flow in the early phase of reperfusion, i.e., relief of ischemia in a stuttered or staccato manner. ๏‚— The reduction in infarct size appears to be comparable with that observed with IPC. ๏‚— Patients receiving brief balloon inflations/deflations in the initial minutes of reperfusion during PCI exhibited smaller ST- segment changes and lower levels of total creatine kinase release compared with patients that were not subjected to stuttering reperfusion ๏‚— Luo et al in their study on post-op patients after total correction of TOF showed that aortic reclamping for 30 seconds and declamping for 30 seconds, repeated twice, reduced perioperative troponin T and CK-MB release and decreased the need for inotropic support after surgery
  • 32. Remote Ischaemic Preconditioning ๏‚— Remote ischemic preconditioning is a phenomenon whereby brief ischemia of one organ or tissue confers protection on a distant naive organ or tissue against a sustained ischemia- reperfusion injury ๏‚— Brief intermittent lower limb ischemia was associated with attenuated troponin release and a reduction in the need for postoperative inotropic support in children undergoing congenital heart surgery ๏‚— Similar findings were demonstrated in adult patients undergoing CABG where RIPC was induced by three 5-minute cycles of right forearm ischemia by inflating a blood pressure cuff on the upper arm to 200 mm Hg with an intervening 5-
  • 33. Autophagy ๏‚— Autophagy is the process whereby a doublemembrane structure called the autophagosome sequesters cytoplasmic components such as ubiquitinated protein aggregates or organelles including mitochondria, peroxisomes, and endoplasmic reticulum. ๏‚— It is involved in degradation of long-lived proteins and the removal of excess or damaged organelles ๏‚— The outer autophagosomal membrane fuses with a lysosomal membrane to deliver its contents into an autophagolysosome where the cargo is degraded by lysosomal hydrolases and the resulting macromolecules recycled
  • 34.
  • 35. ๏‚— Autophagy has been reported to be upregulated in isolated cells subjected to simulated ischemia and reperfusion and rodent models of ex vivo and in vivo ischemia reperfusion injury. ๏‚— Gurusamy et al. investigated the role of autophagy during ischemia-reperfusion injury and reported that increased BAG- 1 expression in the heart correlated with the onset of protection in an in vivo model of myocardial stunning. ๏‚— Studies suggest that upregulation of autophagy promotes survival during stress such as ischemia-reperfusion ๏‚— There is also direct evidence that autophagy plays an important role in mediating ischemic and pharmacologic preconditioning. ๏‚— Autophagy may serve as an important mediator of protection of the preconditioning agent CCPA. A more detailed understanding of the role of autophagy in myocardial protection may lead to a new therapeutic approach to the management and treatment of ischemia-reperfusion injury.
  • 36. Adenosine ๏‚— There is considerable experimental evidence that activation of various adenosine receptor subtypes results in cardioprotection similar to that induced by IPC. ๏‚— Preischemic administration of the nucleoside adenosine retards the rate of ischemia-induced ATP depletion, prolongs the time to onset of ischemic contracture, attenuates myocardial stunning, enhances postischemic myocardial energetics, and reduces infarct size ๏‚— Recent preclinical reports suggest that an adenosine A 2b receptor agonist confers cardioprotection when administered before the onset of ischemia (preconditioning) and at reperfusion (postconditioning) ๏‚— In clinical trials, low dose adenosine administration showed no benefit on patient outcome ๏‚— However, trials involving administration of high doses of adenosine in CABG patients showed reduction in postbypass inotropic drug utilization, improved regional wall motion, and global function measured by transthoracic echocardiography ๏‚— Its clinical use is limited because large doses are associated with marked hypotension in patients not on cardiopulmonary bypass.
  • 37. Acadesine ๏‚— This agent is a member of a class of drugs referred to as adenosine regulating agents. It is a purine nucleoside analog that raises adenosine tissue levels selectively during ischemic conditions ๏‚— Early preclinical studies have indicated that acadesine treatment: โ—ฆ (1) improves left ventricular wall motion after intermittent ischemia โ—ฆ (2) attenuates frequency of ventricular arrhythmias โ—ฆ (3) attenuates myocardial stunning and preserves myocardial function after cardiac arrest and cold cardioplegia. ๏‚— Mangano et al. examined the two-year all cause mortality after perioperative MI in a follow-up of the Acadesine 1024 Trial. Although the primary outcome was negative, the findings at two years among patients experiencing post
  • 38. Sodium-Hydrogen Exchange inhibitors ๏‚— The sodium-hydrogen exchangers (NHEs) are a family of membrane proteins with nine isoforms that are involved in the transport of hydrogen ions in exchange for sodium ions. ๏‚— NHE-1 is the isoform that is expressed in the heart and may play a minor role in the normal excitation-contraction coupling process; however, it has been implicated in the etiology of arrhythmias, stunning, apoptosis, necrosis associated with acute myocardial ischemia-reperfusion injury, postinfarction ventricular remodeling, and heart failure
  • 39. ๏‚— The driving forces for Na + /H + exchange are the relative transmembrane N + and H + gradients. ๏‚— During ischemia, cytoplasmic pH falls as low as 6.6 because of increased production of H + from anaerobic glycolysis, but upon reperfusion, NHE-1 is activated to restore intracellular pH by exchange of intracellular protons for extracellular sodium. ๏‚— The resulting accumulation of intracellular Na + is further exacerbated by diminished activity of Na + /K + ATPase as a result of ischemia and lowered ATP availability. ๏‚— The increased intracellular Na + competes for sites on the Na + /Ca ++ exchanger and can actually drive it to run in reverse, resulting in cytosolic calcium overload. ๏‚— Calcium overload has numerous adverse consequences including activation of calcium- dependent proteases and phospholipases, gap junction dysfunction, culminating in membrane rupture and cell death
  • 40. ๏‚— The EXPEDITION trial was initiated to address the safety and efficacy of NHE-1 inhibition by cariporide in the prevention of death or MI in patients undergoing CABG surgery. ๏‚— Although cariporide treatment was effective in reducing the incidence of nonfatal MI, its efficacy was associated with toxicity, and the overall assessment of benefits and risks associated with cariporide indicated that the imbalances in the safety profile outweighed the reduction in the observed MI rate ๏‚— The importance of the study, however, is that myocardial necrosis after CABG is higher than previously appreciated and it suggested NHE-1 inhibitors represent a new class of drugs that hold promise for reduction of myocardial infarction associated with ischemiareperfusion injury.
  • 41. Glucose Insulin Potassium ๏‚— There are numerous studies that suggest glucose- insulin-potassium (GIK) infusions are effective in reducing perioperative MIs, postischemic myocardial dysfunction, and atrial fibrillation in patients undergoing heart surgery. ๏‚— The rationale for this form of treatment is based on the concept that insulin stimulates potassium reuptake through stimulation of the Na + ,K + - ATPase while it stimulates glucose uptake for glycolytic energy production. ๏‚— High glucose, insulin, and an increased glycolytic flux also increase pyruvate generation and in turn preserve the citric acid cycle. ๏‚— Additionally, glycolytic ATP protects membranes, drives uptake of Ca 2+ by the sarcoplasmic reticulum, and improves sodium homeostasis of ischemic
  • 42. ๏‚— Despite a strong rationale for its application in surgery, the efficacy of GIK in heart surgery remains controversial, due to mixed results with the use of GIK to treat patients with acute myocardial infarction ๏‚— Although a metaanalysis of randomized studies using GIK suggests that it may improve postoperative recovery of contractile function and reduce atrial arrhythmias, the individual studies have involved small numbers of patients and, therefore, insufficiently powered to detect efficacy. ๏‚— Until a large randomized, multicenter clinical trial has been performed, the use of GIK as a form of myocardial protection will remain controversial.
  • 43. Myocardial protection during beating heart surgery ๏‚— The acceptance of OPCAB is due in part to the development and refinement of a myriad of surgical aids that allow for stabilization and local immobilization of the heart during grafting. ๏‚— Ischemia during temporary occlusion of a coronary artery during OPCAB may last from 6 to 25 minutes based on the surgeonโ€™s experience, quality and size of the vessel, and adequacy of the exposure. ๏‚— Most patients with preexisting severe coronary heart disease have experienced self-limiting episodes of ischemia during daily life and may have imparted a certain degree of tolerance to the surgically induced ischemia. ๏‚— This tolerance has been documented using ECGs, transesophageal echocardiography, and continuous SVO2 monitoring
  • 44. ๏‚— In order to better understand the differences between OPCAB and onpump surgery, Chowdhury et al. investigated the release pattern of various cardiac biomarkers in 50 patients undergoing cardioplegic and noncardioplegic coronary artery bypass surgery ๏‚— They observed a greater release of cardiac troponin I, high-sensitivity C-reactive protein, and heart-type fatty acid binding protein in the cardioplegic group. ๏‚— They concluded that OPCAB surgery is associated with less injury
  • 45. ๏‚— One approach to minimizing the risk of injury is to reduce myocardial oxygen demand. Pharmacologic beta-blockade is frequently instituted to reduce inotropy and achieve negative chronotropy using ultra-short-acting beta blockers such as esmolol and labetalol ๏‚— Another approach is to optimize the systemic mean blood pressures while reducing afterload. ๏‚— Calcium channel blockers, such as diltiazem, have been used to afford an effective reduction in blood pressure while minimizing a depression in myocardial contractility that may occur with beta blockers. ๏‚— Patients who become hypertensive during the operation may benefit from intravenous nitrates, which allows for coronary vasodilation and increased blood flow via collaterals. ๏‚— Gentle core cooling, by allowing the body temperature to drift to 35โ€“36ยฐC and deepening the level of anesthesia are concurrent measures that can also be employed.