Assessment and Primary Prevention of CAD. Tuan D. Nguyen, M.D. Non-Invasive Cardiology Seton Heart Institute

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Transcription:

Assessment and Primary Prevention of CAD Tuan D. Nguyen, M.D. Non-Invasive Cardiology Seton Heart Institute

Objectives Identify risk factors for CV disease Identify populations that likely benefit from cholesterol lowering medications and assess treatment goals Select appropriate therapies for lipid lowering Identify additional risk stratification tools Power slide

BMI <25 HbA1c < 6.5-7% <130/80 PLANT-based Low sugar, salt Low saturated fat 40, 3-4x/week Weight training 1-800-QUIT-NOW

2018 ACC/AHA Guideline 21+ yo Screen CV risk factors, check lipids (LDL) Clinical CVD (Secondary Prevention) LDL 190+ (+FH) Age 40-75, LDL 70-189 High intensity statin (<75 y.o.) High intensity statin Non-DM (PRIMARY PREVENTION) DM-1/2 10-yr Risk calculation Mod-high intensity Statin *LDL >160 mg/dl *hs-crp > 2 mg/l, High Lp(a), Apo B > 130 mg/dl *ABI < 0.9 *+FHx (M<65, F <55) *Southern Asian ancestry *Comorbidities (Metabolic sx, CKD, HIV, Rheumatologic d/o, premature menopause **CAC >100 or 75 th %tile 7.5-20%: Shared decision-making; Mod intensity statin (IIb) >20%: High intensity statin (I) 5-7.5%: Shared decision-making; *Consider add l testing

Other populations No formal recommendations: ESRD (maintenance HD) Non-Ischemic CHF (NYHA II-IV) Primary prevention patients age > 75 (no clinical ASCVD)

Lipid management Focus on heart-healthy habits across lifecourse Shared decision-making process

Lipid management Secondary causes of elevated LDL Diet: Saturated or trans fats Drugs: Thiazide diuretics, BBl, cyclosporine, Amiodarone, Gluco- and androgenic steroids, protease inhibitors Diseases: Nephrotic syndrome, Biliary obstruction, hypothyroidism, obesity, pregnancy

Lipid management Continued focus on use of HMG Co-A reductase inhibitors( aka statins) High intensity: Lowers LDL 50%+ Rosuvastatin (Crestor) 20-40 mg Atorvastatin (Lipitor) 40-80 mg Moderate intensity statin: Lowers LDL 30-50% Simvastatin 20-40 mg Pravastatin 40-80 mg

Caveats If unable to tolerate high intensity Examples Previous statin intolerance Severe comorbidities: Severe hepatic or renal impairment Asian population Unexplained LFTS > 3x ULN Concomitant use of drugs (Cyt P450) effecting statin metabolism >75 y.o. Default to moderate intensity or lowest tolerable dose

Non-statin medications Lower is better: CTT data Ezetimibe [Zetia] Additional 20% reduction in LDL (-16 mg dl) *Within 30 days of ACS Modest benefit in CV event reduction (MI, CVA) No change in 10 yr all-cause mortality Used in combination with statins (unclear utility as mono-therapy) PCSK-9 Monoclonal Abs *IMPROVE-IT

PCSK-9 Inhibitors Monoclonal Abs against PCSK-9 protein Alirocumab [Praluent] or Evolocumab [Repatha]: SC injection No dose adjustment in mild-moderate renal/hepatic impairment Adverse reactions: Local injection site reaction No muscle or hepatic toxicity (ie: myalgias) Clinical benefit PCSK-9 inhibitor + statin: Additional 60% reduction in LDL vs. statin alone Statistically significant reduction in MI and CVA Mortality benefit suggested by meta-analysis

Non-statin medications Complete statin intolerance Combination Rx in patients with inadequate response High risk (secondary prevention): If LDL >70 mg/dl +FH: If LDL >100 Not clinically beneficial ^Niacin: No CV event risk reduction Trend toward MSK/GI events, infection, ischemic CVA, bleeding *Fibrates: No mortality benefit ^AIM-HIGH, HPS-2-THRIVE *VA-HIT, Helsinki Heart, FIELD, ACCORD-Lipid

Beyond LDL Hypertriglyceridemia Secondary target in CV risk prevention Treat secondary causes DM/metabolic syndrome EtOH abuse CKD/ESRD/nephrotic syndrome Hypothyroid Meds (similar to LDL medication culprits) Primary prevention 500+ mg/dl è Treat to prevent Pancreatitis before use of LDL lowering medication (Ic) *>150-199: O-3 Fish oil *Secondary prevention >150-199 è O-3 Fish oil (Pure EPA; Vascepa) Reduction of MACE *REDUCE-IT

Beyond LDL Low HDL: M <40 mg/dl, F < 50 mg/dl Strongly determined by genetics *No clinical benefit to raising HDL with existing pharmacotherapies Cholesteryl ester transfer protein (CETP) inhibitors Niacin *Heartwire (Medscape), 7/2014

Beyond LDL Low HDL è*lifestyle Rx! Diet Olive oil (polyphenols higher in EVOO) Coconut oil (2T daily; incorporated in diet) Red/purple vegetables (anthocyanins and anti-oxidants in eggplant, red cabbage, blueberries/blackberries) Fatty fish (Omega-3 fa with 4x/wk consumption: Salmon, herring, sardines, mackerel) Lower carbohydrate diet ( Ketogenic particularly in pre-existing DM, Obese, and Metabolic syndrome) AVOID artificial trans-fats ( partially hydrogenated ) Exercise (particularly high intensity exercise) Quit tobacco (potential benefit of simply switching to vapor cigarettes) Weight loss (via several methods of wt loss) *Heartwire (Medscape), 7/2014

Follow-up Recheck FLP 4-12 weeks following initiation Routine q3-12 month reassessment Follow-up visits Assess effectiveness of treatment Assess compliance/adherence Reinforcement tool Up-titration if necessary Assess/address other secondary causes/lifestyle changes Assess side effects

Follow-up Check LFT s at baseline No routine check thereafter (unless signs of hepatic dysfunction) CK not routinely checked (unless muscle symptoms)

Statin safety MAIN concern: Drug-drug interactions NOT metabolized by Cyt P450 Pravastatin Pitavastatin [Livalo] Simva, Atorva, Lova-statin: CYP 3A4 Avoid with: Try to avoid / LOW dose with Diltiazem, Verapamil (non-dhp) HIV PI -azole (antifungals) -mycin (Macrolide Abx) Gemfibrozil Grapefruit juice Simvastatin Max dose 10 mg: Non-DHP CCB (Diltiazem, Verapamil) Max dose 20 mg: Amiodarone, Ranolazine

Statin safety Safety in pregnancy Category X: Recommend discontinuation prior to conception Not recommended during breast-feeding Myopathy* Myalgias reported: 5-29%% Myositis 0.5% Rhabdomyolysis <0.1% Highest risk: Renal dysfunction, hypothyroidism, liver dysfunction, concomitant meds Measurement of CK (if muscle symptoms) Hepatic dysfunction 0.5% - 3% Dose dependent, and usually within first 4 months Hepatic failure: Incidence no different from general population 2012 FDA labeling: Baseline LFTs, with repeat monitoring only if clinically indicated (not routine) If ALT > 3ULN, decrease dose or change statin DM Accelerates development of DM in pre-diabetics Assess risk: benefit (although overall benefit of vascular event reduction likely outweighs risk) Cognition Data not definitive Higher rates of concern with lipophilic statins (atorva, simva) compared to hydrophilic (prava, rosuva) CA No data to support an increased risk *Pravastatin and fluvastatin less intrinsic muscle toxicity Pravastatin: Diminished DM risk Source: Uptodate

Statin safety -Statins associated with LOW risk of adverse effects Serious muscle injury <0.1% Myalgias 5-29% 10% will discontinue Incidence of muscle symptoms in statin v. placebo-treated: <1% >50% pts also had sx w/ placebo* Serious hepatotoxicity <0.001 Newly dx d DM 0.2%/year Potential increase in hemorrhagic CVA NO causal relationship: Cancer Cognitive dysfxn Cataracts, peripheral neuropathy, ED benefit of reducing CV risk with statin therapy far outweighs any safety concerns. AHA Scientific Statement, 12/2018, Arteriosclerosis, Thrombosis, and Vascular Biology * GAUSS-3 trial

CV Risk stratification Asymptomatic adult screening exams For CAD (CHD risk stratification) Resting 12-lead ECG Calcium artery score CT ( Heart Healthy CT) ABI study (2 nd line) Hs-CRP (2 nd line) For AAA Abdominal aortic U/S *Stress testing (ETT, stress-echo, stress-nuclear) NOT recommended screening tool in asymptomatic adults

Coronary artery calcium CT ( Heart Healthy CT) M > 40 or F > 45 yo 1 Framingham risk (HTN, HLD, *FHx) 5-20% CV event risk by calculator Cash pay study Widely available/accessible *Family hx not included in risk calculators

Management of CV disease: Yes or No? Treatment/Test 1. Diet, exercise 2. Lipid mgmt. 3. HTN mgmt. 4. DM mgmt. 5. Tobacco cess 6. Carotid doppler 7. AAA screen 8. PAD screen (ABI) 9. Calcium score 10. Lp(a), hs-crp, apo-b 11. Stress testing 12. Aspirin Primary Prevention ABSOLUTELY YES YES* YES YES ABSOLUTELY YES NO YES (>65 y.o.^) YES (risk strat) YES (risk strat) YES (risk strat) NO?? Secondary Prevention ABSOLUTELY YES ABSOLUTELY YES* YES; ACEi, +/- BBl YES# ABSOLUTELY YES Symptom-driven YES / symptom-driven Symptom-driven NO NO Symptom-driven YES; Rivaroxaban *Ezetimibe, PCSK-9, O-3 fish oil (TG) ^Males >65yo + smoked 100+ cigarettes Males or females >65yo with a +FHx of AAA # SGLT-2-I, GLP-1R-A

Summary Modifiable CV risk factors and heart healthy habits Assess early, often, and encourage/treat aggressively throughout life Identify the 4 patient groups that would benefit from lipid management Still focus on statins as workhorse medication in lipid Rx Ezetimibe, PCSK-9 inhibitors, O-3 fish oil Consider additional CV risk stratification tools in more ambiguous clinical scenarios (ie: CAC CT) Lipid management and CV risk management (similar to all therapeutic decisions) is never an absolutism è shared decision-making process