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A major teaching hospital of Harvard Medical School Myocardial Viability Thomas H. Hauser MD, MMSc, MPH, FACC Director of Nuclear Cardiology Beth Israel Deaconess Medical Center Instructor in Medicine Harvard Medical School Boston, MA Harvard Medical School Outline • SPECT • PET • CMR Harvard Medical School Imaging Protocol • Stress: Prone 99mTc-Sestamibi • Rest: Prone 201Tl Harvard Medical School Case 1 Stress Rest Harvard Medical School Slices Harvard Medical School Gated Slices Harvard Medical School Gated Slices: New Window Harvard Medical School QGS Results Harvard Medical School Clinical Data • 58 year-old man with diabetes, hypertension, chronic renal insufficiency, tobacco use, prior heroin abuse and liver transplantation two years ago due to hepatitides B and C. • One week prior to admission he was admitted to another hospital with community acquired pneumonia. He was discharged two days prior to admission. • He presented on the day of admission with chest pain for 12 hours. In the ER he was noted to have anterior ST elevation. Harvard Medical School Cardiac Catheterization Harvard Medical School Cardiac Catheterization Harvard Medical School Cardiac Catheterization Harvard Medical School Cardiac Catheterization Harvard Medical School Cardiac Catheterization Harvard Medical School Clinical Data • He was referred for surgical revascularization. The surgical team requested evaluation of myocardial viability given his delayed presentation and the concern for limited myocardial salvage. Harvard Medical School Stress Protocol • Dobutamine at 5 mcg/kg/min was infused for 21 minutes. • HR 64 66 • SBP 124 134 • No symptoms • No ECG changes Harvard Medical School Baseline ECG Harvard Medical School Clinical Data Should our patient be revascularized? Harvard Medical School Dysfunctional but Viable Myocardium LVEF 32% LVEF 54% Horn HR, Teichholz LE, Cohn PF, Herman MV, Gorlin R. Augmentation of left ventricular contraction pattern in coronary artery disease by an inotropic catecholamine: the epinephrine ventriculogram. Circulation 1974;49:1063-1071 Harvard Medical School Dysfunctional but Viable Myocardium • Hibernating – Chronic ischemia or repetitive stunning – Ultrastructural changes that result in • Disassembly of contractile apparatus – Recovery in weeks or months after revascularization • Stunned – Acute ischemia – No ultrastructural changes – Recovery in minutes to days after revascularization Harvard Medical School CABG in Patients with LV Dysfunction Chareonthaitawee et al, JACC 2005;46:567 Harvard Medical School Importance of Viable Myocardium J Am Coll Cardiol 2002;39:1151 Harvard Medical School Evaluation of Viability Chareonthaitawee et al, JACC 2005;46:567 Harvard Medical School Nuclear Techniques • SPECT – 201Tl – 99mTc – 123I Fatty Acids – PET Agents • PET – – 18FDG 11C Acetate Harvard Medical School SPECT • 201Tl most commonly used – Several protocols for use • Stress – redistribution • Rest – redistribution – Usually imaged 4 to 24 hours after initial injection – With or without reinjection » Usually at 4 hours – Perfusion tracer initially • Ischemia is a sign of viability – Membrane integrity tracer in the late phase • K analog – Assesses integrity of membrane and Na-K-ATPase Harvard Medical School SPECT • 99mTc also helpful – Stress – rest protocol – Perfusion tracer – Ischemia is a sign of viability – Membrane integrity tracer • Trapped by active mitochondria • PET agents act as with PET imaging Harvard Medical School 201Tl Uptake and Recovery of Function Perrone-Filardi P, Pace L, Pratarto M, et al. Dobutamine echocardiography predicts improvement of hypoperfused dysfunctional myocardium after revascularization in patients with coronary artery disease. Circulation. 1995;91:2556-2565. Harvard Medical School Comparison of 201Tl and 99mTc Udelson JE, Coleman PS, Metherall J, et al. Predicting recovery of severe regional ventricular dysfunction. Comparison of resting scintigraphy with 201Tl and 99mTc-sestamibi. Circulation. 1994;89:2552-2561. Harvard Medical School PET • All PET agents (18FDG, 11C acetate) assess cardiac energy metabolism. – 18FDG imaging assesses glucose metabolism • Ischemic myocardium generally favors glucose utilization – 11C acetate imaging assesses lipid metabolism Harvard Medical School Imaging Goal: High Quality Images Harvard Medical School Abnormal? Harvard Medical School Poor Image Quality Harvard Medical School Importance of Good Patient Preparation • In the assessment of myocardial viability, the quality and utility of the images is highly dependent on appropriate patient preparation – Inadequate patient preparation can lead to spurious results or images with no diagnostic value Harvard Medical School Myocardial Energy Metabolism • Cardiac myocytes are continuously active – Require efficient use of energy resources – Require continual repletion of energy substrates • Faced with varying levels in supply – Flexibility in substrate use Harvard Medical School Anaerobic Metabolism • Inefficient – Each glucose molecule yields two ATP • Requires glucose • Does not require oxygen • Lactate is the waste product Based on Autumn Cuellar (Bioengineering Institute, University of Auckland) Harvard Medical School Aerobic Metabolism • Efficient – Citric acid cycle produces abundant ATP • Can function with multiple substrates • Requires oxygen • Water and CO2 are the waste products Based on Autumn Cuellar (Bioengineering Institute, University of Auckland) Harvard Medical School Myocardial Energy Metabolism ketone bodies amino acids Based on Autumn Cuellar (Bioengineering Institute, University of Auckland) Harvard Medical School Myocardial Energy Metabolism ketone bodies amino acids Based on Autumn Cuellar (Bioengineering Institute, University of Auckland) Harvard Medical School Glucose Handling • Largely determined by the availability of glucose in the blood stream • Insulin is the major regulatory hormone Harvard Medical School Glucose Handling: Fasting Glucagon Harvard Medical School Glucose Handling: Fasting Glucose use Glucagon Gluconeogenesis FFA Glycogen Harvard Medical School Glucose Handling: Fed Harvard Medical School Glucose Handling: Fed Glucose use Gluconeogenesis Glycogen Fat storage Harvard Medical School Glucose Handling: Fed Glucose use Gluconeogenesis Glycogen Fat storage Harvard Medical School Glucose Handling: Diabetes (1) Harvard Medical School Glucose Handling: Diabetes (1) Glucose use Gluconeogenesis FFA Glycogen Harvard Medical School Glucose Handling: Diabetes (2) Harvard Medical School Glucose Handling: Diabetes (2) Glucose use Gluconeogenesis FFA Glycogen Harvard Medical School Glucose Handling • In normal patients, feeding causes a rise in glucose and insulin that restores glucose balance – Uptake of glucose in peripheral tissues • HEART • In type 1 diabetics, feeding causes a rise in glucose while insulin remains low/absent – Continued gluconeogenesis and glucose conservation • In type 2 diabetics, feeding causes a rise in glucose and insulin but peripheral tissues are resistant to the action of insulin – Continued gluconeogenesis and glucose conservation Harvard Medical School FDG Glucose: C6H12O6 FDG: C6H11O5 Harvard Medical School FDG Uptake and Retention glycogen Insulin glut FDG FDG – 6 – P Aerobic Metabolism Harvard Medical School Goal of Patient Preparation • Ensure that glucose is the primary substrate used for myocardial energy metabolism – Abundant Glucose – Abundant Insulin – Scarce FFA and other substrates Harvard Medical School Patient Preparation Protocols • • • • Acipimox Hyperinsulinemic/euglycemic clamp IV glucose Oral glucose Harvard Medical School Acipimox • Potent inhibitor of peripheral lypolysis – Drastically reduces FFA in blood • As FFA are the principal alternative energy source for the myocardium, glucose utilization increases – Relatively independent of insulin and glucose levels • Not FDA approved – Used in Europe Harvard Medical School Hyperinsulinemic/Euglycemic Clamp • Simultaneous infusions of insulin and glucose to increase the insulin level while keeping the glucose level from falling – High insulin – Normal glucose – Low FFA • High myocardial glucose utilization Harvard Medical School Glucose Loading • Provide a large dose of oral or IV glucose • Endogenous production of insulin – – – – Supplemented with exogenous insulin if needed Moderately high insulin Normal glucose Low FFA • High myocardial glucose utilization Harvard Medical School Glucose Loading: Diabetes • Exogenous insulin is required for appropriate patient preparation with either type 1 or type 2 diabetes – With type 1, there is little or no endogenous insulin – With type 2, there is insulin resistance, requiring higher insulin levels to ensure that insulin has an effect • Observation of a falling blood sugar after hyperglycemia is evidence of insulin action Harvard Medical School Patient Preparation Protocols • Acipimox – Easy – Effective – Not FDA approved • Hyperinsulinemic/euglycemic clamp – Difficult – Effective • IV/Oral Glucose Loading – Relatively easy – Almost always effective Harvard Medical School Insulin • Many different kinds of insulin with varying pharmacokinetics – – – – – – – Regular NPH Lispro Lente Ultralente Glargine Aspart • Pharmocokinetics also vary with the route of administration Harvard Medical School Insulin • For patient preparation for FDG imaging, use REGULAR insulin given IV – Peak action of subcutaneous regular insulin occurs ~3 hours after the dose – Peak action of IV regular insulin occurs ~15 minutes after the dose Harvard Medical School BIDMC Patient Preparation Protocol 5. If the initial BS is >250, then give IV regular insulin according to the protocol below. If oral glucose is given, recheck BS in 30 minutes and then give IV regular insulin according to the same protocol. Give IV regular insulin None BS ? 140 1 units BS 141 to 160 2 units BS 161 to 180 3 units BS 181 to 200 4 units BS 201 to 220 5 units BS 221 to 240 6 units BS 241 to 260 7 units BS 261 to 280 8 units BS 281 to 300 Notify Physician BS >300 6. Check BS every 15 minutes. If BS is <140, inject FDG If BS continues to rise, give IV regular insulin according to the protocol above and continue to check BS every 15 minutes If BS is falling but remains elevated, give IV regular insulin at half the dose according to the protocol above and continue to check BS every 15 minutes If BS remains elevated after 90 minutes, contact the imaging physician 7. Have the patient eat a light meal 15 minutes after injection of FDG. 8. Continue to check BS every 30 minutes after injection of FDG to monitor for hypoglycemia. 9. Begin imaging 60-90 minutes after injection of FDG. 10. After imaging, monitor patient for 30 minutes and obtain BS. If BS >70 then the patient can be discharged. 11. Upon discharge instruct the patient to: Beware of hypoglycemia. Encourage the patient to have a meal soon after discharge. Resume all prior medications. If at any time during the protocol there is a question about how to proceed, contact the imaging physician immediately. Harvard Medical School PET: 18FDG Srinivasan G, Kitsiou AN, Bacharach SL, et al. [18F]Fluorodeoxyglucose Single Photon Emission Computed Tomography : Can It Replace PET and Thallium SPECT for the Assessment of Myocardial Viability? Circulation. 1998;97:843 - 850. Harvard Medical School PET: 18FDG Srinivasan G, Kitsiou AN, Bacharach SL, et al. [18F]Fluorodeoxyglucose Single Photon Emission Computed Tomography : Can It Replace PET and Thallium SPECT for the Assessment of Myocardial Viability? Circulation. 1998;97:843 - 850. Harvard Medical School Case 2 • 45 year-old man with a history of CAD, diabetes, CHF (LVEF 25%) who presented with repetitive ICD firing due to recurrent VT. • He was admitted to the hospital and found to have a small NSTEMI. Cardiac catheterization was performed and showed a 70% proximal LAD stenosis, a totally occluded RCA, and occluded SVGs to the LAD and PDA. Harvard Medical School Case 2 • The clinical team determined that his recurrent VT was most likely to ischemia and consulted the CT surgeons to determine his candidacy for a second CABG. The surgeons requested a myocardial viability study prior to proceeding. Harvard Medical School Case 2 Harvard Medical School Case 2 • The study was interpreted as showing nonviability of the apex and inferior wall. The remaining segments were viable. • He subsequently underwent LAD stenting and has done well since then. Harvard Medical School Case 3 A 59 year old with a history of diabetes, hypertension and dyslipidemia sees his PCP because of the new onset of dyspnea. His ECG reveals LBBB. His PCP sends him for nuclear imaging with exercise stress. During the test, he has dyspnea at a low workload. Harvard Medical School Case 3: Slices Harvard Medical School Case 3: Gated Slices Harvard Medical School Case 3: Quantitative Data Harvard Medical School Case 3 He is referred for cardiac catheterization, which reveals severe three vessel disease. The consulting cardiac surgeon asks for a determination of myocardial viability before proceeding with surgical revascularization. What can we do to further determine myocardial viability? • FDG • Delayed enhancement MR Harvard Medical School Gd Contrast Kinetics in Myocardium Circulation, Dec 1996; 94: 3318 - 3326 Harvard Medical School Delayed Contrast Enhancement: Bright is Dead Circulation, Nov 1999; 100: 1992 - 2002 Harvard Medical School Prediction of Recovery of Function N Engl J Med 2000; 343:1445-1453 Harvard Medical School Normal Myocardium Harvard Medical School Anterior/Apical Scar Harvard Medical School Ischemic CM with Viable Myocardium Harvard Medical School Case 3 The patient is sent for both FDG and delayed enhancement MR. Harvard Medical School Case 3: FDG Harvard Medical School Case 3: DE-CMR Harvard Medical School Comparison of FDG and DE-CMR Knuesel et al. Circulation. 2003;108:1095 Harvard Medical School Spatial Resolution/Scar Imaging Wagner et al. Lancet. 2003;361:374 Harvard Medical School FDG and MR for Scar/Viability FDG • Images viable myocardium • Directly assesses metabolism • Established gold standard for determining recovery of function after revascularization • • • • DE-CMR Images both scar and viable myocardium Directly assesses anatomy Becoming clinically established Improved spatial resolution compared to FDG Harvard Medical School Dobutamine CMR Mandapaka et al, J. Magn. Reson. Imaging 2006;24:499–512. Harvard Medical School Comparison of Techniques CMR SPECT with 18FDG Chareonthaitawee et al, JACC 2005;46:567 Harvard Medical School Summary • SPECT – Tl-201 – Tc-99m • PET – FDG • CMR – Late gadolinium enhancement – Dobutamine Harvard Medical School