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Cardiology Module

Comprehensive clinical resource for clinicians, residents & students — Calculators · Drug Dosing · Protocols · Indian Guidelines

CHA₂DS₂-VAScHAS-BLED HEART ScoreGRACE · TIMI Wells DVT/PEASCVD · PREVENT qSOFAeGFR · QTc InSH 2023HFAI Guidelines

🧮 Risk Stratification Calculators 10 tools

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CHA₂DS₂-VASc Score ⭐ Gold Standard

Stroke risk in Atrial Fibrillation — Anticoagulation decision

0–9AF · StrokeESC 2020

Validated stroke risk score for non-valvular AF. Score ≥2 (male) or ≥3 (female) = anticoagulation recommended. NOACs preferred over warfarin (except mechanical valves/MS).

C — CHF/LV dysfunction Recent decompensation or EF <40%

H — Hypertension BP >140/90 or on antihypertensive treatment

A — Age (years)65–74 = +1 · ≥75 = +2

D — Diabetes mellitus

S₂ — Prior stroke / TIA / thromboembolism (scores 2 points)

V — Vascular disease Prior MI, PAD, or aortic plaque

Sc — Female sex +1 point (not an independent risk factor alone)

Ref: Lip 2010 · ESC AF Guidelines 2020 · KD Tripathi 8th Ed

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HAS-BLED Score

Bleeding risk on anticoagulation in AF

0–9Bleeding RiskESC 2020

Use alongside CHA₂DS₂-VASc — NOT to withhold anticoagulation, but to identify and correct modifiable bleeding risk factors. Score ≥3 = high risk; address modifiable factors.

H — Hypertension (uncontrolled) Systolic BP >160 mmHg

A — Renal disease Dialysis, transplant, or Cr >200 µmol/L

A — Liver disease Cirrhosis or bilirubin >2× + AST/ALT >3×

S — Prior stroke history

B — Prior bleeding or predisposition Anaemia, bleeding diathesis

L — Labile INR TTR <60% (only for warfarin patients)

E — Elderly Age >65 years

D — Drugs (antiplatelets / NSAIDs)

D — Alcohol (≥8 drinks/week)

Ref: Pisters 2010 · ESC AF Guidelines 2020

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HEART Score

Chest pain risk stratification in ED — MACE prediction

0–10ACS · EDACC/AHA 2021

Identifies low-risk chest pain patients safe for early discharge. Each component scored 0–2. Validated in multiple ED populations. MACE = MI, PCI, CABG, death at 6 weeks.

H — History of chest pain

E — ECG findings

A — Age

R — Risk factors

T — Troponin (initial)

Ref: Backus 2010 · Six 2008 · ACC/AHA Chest Pain Guidelines 2021

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GRACE Score 2.0

ACS in-hospital and 6-month mortality risk

0–372ACS · MortalityESC 2020

Global Registry of Acute Coronary Events. Guides decision for in-hospital invasive strategy in NSTE-ACS. High risk (GRACE >140) → early invasive (<24h).

Age (years)

Heart rate (bpm)

Systolic BP (mmHg)

Creatinine (mg/dL)

Killip class II–IV Rales, S3, pulmonary oedema, cardiogenic shock

ST-segment deviation on ECG

Elevated cardiac enzymes Troponin or CK-MB above normal

Cardiac arrest on presentation

STEMI (vs NSTEMI/UA)

Ref: Fox 2006 · ESC NSTE-ACS Guidelines 2020 · Low ≤108 · Intermediate 109–140 · High >140

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TIMI Score (UA/NSTEMI)

14-day MACE risk in Unstable Angina / NSTEMI

0–7ACSTIMI 11B

Thrombolysis In Myocardial Infarction risk score for UA/NSTEMI. Predicts all-cause mortality, new/recurrent MI, or severe recurrent ischaemia requiring urgent revascularisation at 14 days.

Age ≥65 years

≥3 CAD risk factors Family history, HTN, hypercholesterolaemia, DM, active smoking

Aspirin use in past 7 days Suggests aspirin-refractory event

≥2 anginal events in past 24 hours

ST deviation ≥0.5 mm on ECG

Positive cardiac marker Elevated troponin or CK-MB

Prior coronary stenosis ≥50% Known CAD or prior angiogram

Ref: Antman 2000 · TIMI 11B trial · Low 0–2 · Intermediate 3–4 · High 5–7

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Wells Score — Pulmonary Embolism

Pre-test probability of Pulmonary Embolism

0–12.5PE · VTEESC PE 2019

Clinically validated score to guide PE workup. Score ≤1 (unlikely) + negative D-dimer = PE excluded without CT. Score >1 or high clinical suspicion → CTPA.

Clinical signs and symptoms of DVT +3

PE is the #1 diagnosis, OR equally likely as alternative +3

Heart rate >100 bpm +1.5

Immobilisation ≥3 days OR surgery in previous 4 weeks +1.5

Previous DVT or PE +1.5

Haemoptysis +1

Active malignancy (on treatment, treated in last 6 months, or palliative) +1

Ref: Wells 2000 · ESC PE Guidelines 2019 · PE Unlikely ≤1 · Possible 2–6 · Likely >6

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ASCVD 10-Year Risk (Pooled Cohort)

10-year atherosclerotic cardiovascular disease risk — Statin indication

%Primary PreventionACC/AHA 2019

AHA/ACC Pooled Cohort Equations for primary prevention. Validated for ages 40–79 years without pre-existing CVD. Use alongside clinical judgement for South Asian/Indian patients (consider multiplying by 1.3–1.5 for Indian ethnicity).

Age (years)

Sex

Race

Total cholesterol (mg/dL)

HDL cholesterol (mg/dL)

Systolic BP (mmHg)

On BP-lowering treatment

Diabetes mellitus

Current smoker

Ref: Goff 2014 · ACC/AHA Cholesterol Guidelines 2019 · InSH 2023 for Indian adaptation

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qSOFA Score

Quick SOFA — Sepsis bedside screening in non-ICU setting

0–3SepsisSepsis-3 2016

Rapid bedside tool. ≥2 points → consider sepsis, prompt full assessment, blood cultures, lactate, fluid resuscitation. Does not replace full SOFA in ICU.

Altered mentation GCS <15, new confusion or altered behaviour

Respiratory rate ≥22/min

Systolic BP ≤100 mmHg

Ref: Singer 2016 · Seymour 2016 · Surviving Sepsis Campaign 2021

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BMI Calculator

Body Mass Index with Asian (Indian) cutoffs

kg/m²Asian CutoffsWHO 2004

Uses WHO Asian/Indian population cutoffs: Normal 18.5–22.9 · Overweight ≥23 · Obese ≥27.5 kg/m². Western cutoffs (overweight ≥25, obese ≥30) underestimate cardiometabolic risk in South Asians.

Weight (kg)

Height (cm)

Ref: WHO Expert Consultation 2004 · Misra 2009 (Indian guidelines)

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eGFR — CKD-EPI 2021

Estimated GFR for drug dose adjustment in cardiac patients

mL/min/1.73m²Dose AdjustKDIGO 2022

Race-free CKD-EPI 2021 equation. Critical for dose adjustment of: DOACs (rivaroxaban, apixaban, dabigatran), digoxin, metformin, ACE inhibitors, ARBs, spironolactone, low-molecular-weight heparin.

Serum creatinine (mg/dL)

Age (years)

Sex

💊 Key thresholds: Metformin — avoid if eGFR <30 · Dabigatran — avoid if <30 · Rivaroxaban — reduce if <50 · Digoxin — caution if <60

Ref: Inker 2021 (CKD-EPI 2021) · KDIGO CKD 2022 · KD Tripathi 8th Ed

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QTc Calculator — Bazett & Fridericia

Corrected QT interval — TdP risk assessment

msTdP RiskQTc-prolonging drugs

QTc >450ms (M) / >460ms (F) = prolonged. QTc >500ms = high Torsades de Pointes risk. Check for QTc-prolonging drugs (amiodarone, sotalol, macrolides, fluoroquinolones, antipsychotics, methadone, ondansetron) and electrolyte imbalances.

QT interval (ms)

RR interval (seconds)OR enter HR below

Heart rate (bpm) — optionalAuto-calculates RR

Sex

⚠️ QTc-prolonging drugs in cardiology: Amiodarone · Sotalol · Quinidine · Disopyramide · Ibutilide. Check full list at CredibleMeds.org

Ref: Bazett 1920 · Fridericia 1920 · AHA/ACC/HRS 2017

💊 Drug Information & Dosing 6 categories

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Anticoagulants — Warfarin & DOACs

Dosing, monitoring, reversal, renal/hepatic adjustment

WarfarinApixabanRivaroxabanDabigatran

NOACs (DOACs) are preferred over warfarin for most indications. Warfarin remains first-line for mechanical heart valves, mitral stenosis, antiphospholipid syndrome (triple positive), and where NOACs are unavailable.

Drug	Indication	Standard Dose	Renal Adjustment	Reversal
Warfarin	AF, MVR, DVT/PE	Individualised — INR target 2–3 (AF/DVT) or 2.5–3.5 (MVR)	Use with caution; INR monitoring essential	Vit K, FFP, PCC (4-factor)
Apixaban	AF, DVT/PE, VTE prophylaxis	AF: 5 mg BD (2.5 mg BD if ≥2 of: age ≥80, wt ≤60 kg, Cr ≥1.5 mg/dL) DVT/PE: 10 mg BD ×7d → 5 mg BD	Use with caution if CrCl <25; avoid <15	Andexanet alfa (approved)
Rivaroxaban	AF, DVT/PE, ACS (low dose)	AF: 20 mg OD with dinner DVT/PE: 15 mg BD ×21d → 20 mg OD ACS: 2.5 mg BD (+ DAPT)	AF: reduce to 15 mg OD if CrCl 15–49	Andexanet alfa
Dabigatran	AF, DVT/PE (not ACS)	150 mg BD (AF) — or 110 mg BD if age ≥80 / + verapamil	Avoid if CrCl <30; dose reduce 30–50	Idarucizumab (specific antidote)
Edoxaban	AF, DVT/PE	60 mg OD (AF, after ≥5–10d parenteral) 30 mg OD if CrCl 15–50 or wt ≤60 kg	Reduce to 30 mg if CrCl 15–50	Andexanet alfa
Enoxaparin	Bridging, ACS, VTE prophylaxis	Therapeutic: 1 mg/kg SC BD (or 1.5 mg/kg OD) Prophylactic: 40 mg SC OD	Reduce to 1 mg/kg OD if CrCl <30; monitor anti-Xa	Protamine sulfate (partial)

⚠️ Bridging: DOACs do NOT require bridging pre-procedure in most cases. Hold based on CrCl and bleeding risk (1–2 days for low, 3–5 days for high-risk procedures). Restart 24–48h post-procedure when haemostasis achieved.

Ref: KD Tripathi 8th Ed · BNF 2024 · ESC AF 2020 · CDSCO Drug Approvals

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Antiplatelets — DAPT Regimens

Aspirin, Clopidogrel, Ticagrelor, Prasugrel — ACS & PCI protocols

AspirinClopidogrelTicagrelorPrasugrel

Drug	Dose	Duration	Key Notes
Aspirin	Loading: 300 mg stat Maintenance: 75–100 mg OD	Lifelong post-ACS/PCI	PPI co-prescription recommended. Avoid in active peptic ulcer.
Clopidogrel	Loading: 300–600 mg stat Maintenance: 75 mg OD	12 months post-ACS/drug-eluting stent; 1 month post-BMS	Prodrug — CYP2C19 polymorphism reduces efficacy (~25% South Asians). Preferred in patients taking PPIs (less interaction vs ticagrelor).
Ticagrelor	Loading: 180 mg stat Maintenance: 90 mg BD	12 months post-ACS (preferred over clopidogrel)	Direct-acting P2Y12 inhibitor. Caution: dyspnoea (common), bradycardia, avoid if prior intracranial bleed. Do NOT use with strong CYP3A4 inhibitors (ketoconazole). ESC-preferred P2Y12 in ACS.
Prasugrel	Loading: 60 mg stat Maintenance: 10 mg OD (5 mg if <60 kg or >75 yrs)	12 months post-PCI (ACS)	More potent, faster onset. Contraindicated: prior stroke/TIA, age ≥75 (relative), weight <60 kg (use 5 mg). Higher bleeding risk vs clopidogrel.

DAPT Duration Guidance (ESC/ACC 2023)

ACS (STEMI/NSTEMI) — No bleeding concern12 months DAPT → aspirin lifelong

ACS — High bleeding risk (HBR)6 months DAPT then aspirin monotherapy

Elective PCI (stable CAD) — DES6 months DAPT → aspirin lifelong

Elective PCI — BMS1 month DAPT → aspirin lifelong

AF + PCI (triple therapy)1–4 weeks triple → DAPT or OAC+single antiplatelet up to 12m

Ref: ESC ACS Guidelines 2020, 2023 · ACC/AHA 2021 · KD Tripathi · PLATO, TRITON trials

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Heart Failure Therapy — HFrEF / HFpEF

ACEI/ARB/ARNI · Beta-blockers · MRA · SGLT2 inhibitors

Sacubitril/ValsartanCarvedilolSpironolactoneDapagliflozin

The "Fantastic Four" disease-modifying therapies for HFrEF (EF ≤40%): ACEi/ARB/ARNI + Beta-blocker + MRA + SGLT2i. Target maximum tolerated doses. Start low, go slow.

Drug	Starting Dose	Target Dose	Key Monitoring
Ramipril (ACEi)	1.25–2.5 mg OD/BD	5–10 mg OD	BP, K⁺, creatinine (check 1–2 wk after initiation). Avoid if K⁺ >5.5, eGFR <30, bilateral RAS.
Enalapril (ACEi)	2.5 mg BD	10–20 mg BD	As above. Switch to sacubitril/valsartan when haemodynamically stable.
Sacubitril/Valsartan (ARNI)	24/26 mg BD (after 36h wash-out from ACEi)	97/103 mg BD	Preferred over ACEi if tolerated. Contraindicated with ACEi (36h wash-out required to avoid angioedema). Monitor BP, K⁺, eGFR.
Carvedilol (Beta-blocker)	3.125 mg BD	25 mg BD (50 mg BD if >85 kg)	Initiate when euvolaemic. HR, BP. Avoid in reactive airways disease — use bisoprolol instead.
Bisoprolol (Beta-blocker)	1.25 mg OD	10 mg OD	More cardioselective. Safe in mild-moderate COPD/asthma. Titrate every 2 weeks.
Spironolactone (MRA)	12.5–25 mg OD	25–50 mg OD	Monitor K⁺ and creatinine (↑ risk hyperkalaemia with ACEi). Avoid if K⁺ >5.0 or eGFR <30. Gynaecomastia in males — switch to eplerenone.
Eplerenone (MRA)	25 mg OD	50 mg OD	No gynaecomastia. Post-MI HFrEF (EPHESUS trial). Same K⁺/renal monitoring.
Dapagliflozin (SGLT2i)	10 mg OD	10 mg OD (fixed)	HFrEF AND HFpEF benefit (DAPA-HF, DELIVER). Beneficial regardless of diabetes status. Caution: recurrent UTI, DKA risk. Hold peri-operatively (3 days prior).
Empagliflozin (SGLT2i)	10 mg OD	10 mg OD (fixed)	Also HFrEF + HFpEF (EMPEROR-Reduced/Preserved). As above.
Furosemide (loop diuretic)	20–40 mg OD	Symptom-guided	NOT disease-modifying. Use for decongestion only. Monitor electrolytes (K⁺, Na⁺, Mg²⁺). Worsens renal function in dehydration.
Ivabradine	5 mg BD	7.5 mg BD	Add if HR ≥75 despite max beta-blocker + sinus rhythm. Do not use in AF.
Digoxin	0.125–0.25 mg OD	Serum level 0.5–0.9 ng/mL	Reduce dose if eGFR <60. Drug interactions (amiodarone, verapamil ↑ levels). Narrow TI — check levels if toxicity suspected.

📋 HFpEF (EF >50%): SGLT2i (dapagliflozin/empagliflozin) are now recommended. Evidence also supports spironolactone (modest benefit). ACEi/ARBs and beta-blockers — no mortality benefit proven in HFpEF but used for comorbidities.

Ref: ESC HF Guidelines 2021 · HFAI (Heart Failure Association of India) 2022 · DAPA-HF · EMPEROR · PARADIGM-HF · KD Tripathi

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Antihypertensives — InSH 2023 Guidelines

Drug selection, doses, and special populations — Indian context

ACEi/ARBCCBThiazideInSH 2023

Indian Society of Hypertension 2023 recommends: single-pill combination (SPC) preferred from initiation for stage 2 HTN. Target <130/80 mmHg for most patients. CCBs are particularly effective in South Asians (lower renin activity).

Drug Class	First-line Agents	Usual Dose	Preferred In	Avoid In
ACE Inhibitors	Ramipril, Enalapril, Perindopril	Ramipril: 2.5–10 mg OD Perindopril: 4–8 mg OD	CKD, DM with proteinuria, HFrEF, post-MI	Pregnancy, bilateral RAS, K⁺>5.5, Angioedema hx
ARBs	Losartan, Telmisartan, Olmesartan, Candesartan	Telmisartan: 40–80 mg OD Losartan: 50–100 mg OD	As ACEi — use if ACEi-intolerant (cough)	Pregnancy. Never combine with ACEi.
CCB (dihydropyridine)	Amlodipine, Cilnidipine	Amlodipine: 2.5–10 mg OD Cilnidipine: 5–10 mg OD (N+L channel — less oedema)	Elderly, isolated systolic HTN, Angina, South Asian patients	Severe aortic stenosis
CCB (non-DHP)	Diltiazem, Verapamil	Diltiazem SR: 120–360 mg OD	Angina + HTN, Supraventricular arrhythmia	HFrEF, AV block, WPW
Thiazide / Thiazide-like	Chlorthalidone, Indapamide (preferred over HCTZ)	Chlorthalidone: 12.5–25 mg OD Indapamide: 1.5 mg SR OD	Elderly, isolated systolic HTN, Salt-sensitive HTN (common in Indians)	Gout (caution), Hyponatraemia
Beta-blockers	Metoprolol, Bisoprolol, Nebivolol	Bisoprolol: 2.5–10 mg OD Metoprolol XL: 25–200 mg OD	Post-MI, HFrEF, AF rate control, Young HTN with tachycardia, Pregnancy (labetalol/methyldopa preferred)	Asthma, High-degree AV block. NOT first-line monotherapy for uncomplicated HTN
MRA / Potassium-sparing	Spironolactone, Eplerenone	Spironolactone: 25–50 mg OD	Resistant HTN (4th agent), HF, Primary hyperaldosteronism	K⁺>5.0, eGFR <30
Alpha-1 blocker	Prazosin, Doxazosin	Doxazosin: 1–8 mg OD	BPH + HTN, Resistant HTN (add-on)	Orthostatic hypotension risk — 1st dose at night
Central acting	Methyldopa, Clonidine	Methyldopa: 250–500 mg BD–TDS	Methyldopa: Pregnancy (drug of choice)	Clonidine — rebound hypertension on withdrawal

InSH 2023 — Preferred Single-Pill Combinations (SPCs)

Step 1 (low–moderate risk)ACEi/ARB + CCB or ACEi/ARB + Thiazide

Step 2ACEi/ARB + CCB + Thiazide (triple SPC)

Step 3 (resistant)+ Spironolactone 25–50 mg OD

BP Target (general)<130/80 mmHg; <140/90 if elderly/frail

Ref: InSH Guidelines 2023 · ESC HTN 2018/2023 update · JNC 8 · KD Tripathi 8th Ed

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Statins & Lipid-Lowering Therapy

Intensity classification, LDL targets, monitoring, interactions

RosuvastatinAtorvastatinEzetimibeACC/AHA 2019

Intensity	Agent + Dose	LDL ↓	Indication
High intensity	Atorvastatin 40–80 mg OD Rosuvastatin 20–40 mg OD	>50%	ASCVD ≥20%, known CVD (post-MI, stroke, PAD), very high-risk primary prevention
Moderate intensity	Atorvastatin 10–20 mg OD Rosuvastatin 5–10 mg OD Simvastatin 20–40 mg OD	30–50%	ASCVD 7.5–20%, DM age 40–75, LDL ≥4.9 mmol/L
Low intensity	Simvastatin 10 mg OD Pravastatin 10–20 mg OD	<30%	Statin intolerance, elderly (>75 years) — use lower doses
Ezetimibe (add-on)	10 mg OD	+18–25% on top of statin	Add if LDL target not met on maximally tolerated statin. IMPROVE-IT trial.

LDL-C Targets (ACC/AHA 2019 · ESC 2019)

Very high risk (known ASCVD, DM + organ damage)<1.4 mmol/L (<55 mg/dL)

High risk (ASCVD 10yr 10–20%, DM no complications)<1.8 mmol/L (<70 mg/dL)

Moderate risk (ASCVD 5–10%)<2.6 mmol/L (<100 mg/dL)

⚠️ Myopathy risk: Simvastatin 80 mg — avoid. Simvastatin + amlodipine — max 20 mg. Rosuvastatin 40 mg — monitor in Asian patients (lower doses effective). CK if myalgia >10× ULN — stop statin. Statin + fibrate: avoid gemfibrozil (prefer fenofibrate if needed).

Ref: ACC/AHA Cholesterol 2019 · ESC/EAS 2019 · IMPROVE-IT · KD Tripathi · CDSCO

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QTc-Prolonging Drugs in Cardiology

High-risk drug combinations, monitoring, and management

TdP RiskAmiodaroneSotalol

Drug	Class	QTc Risk	Management
Amiodarone	Class III antiarrhythmic	HIGH — QTc prolongation common but TdP paradoxically low	Baseline ECG, monitor QTc. Thyroid, LFTs, pulmonary function annually.
Sotalol	Class III antiarrhythmic	HIGH — dose-dependent TdP risk. Avoid if QTc >500ms	Initiate in hospital with cardiac monitoring. Dose reduce in renal impairment. Correct K⁺/Mg²⁺.
Quinidine	Class IA	HIGH — TdP risk	Largely replaced by safer agents. Monitor QTc closely.
Azithromycin	Macrolide antibiotic	MODERATE — especially with other QTc-prolonging drugs	Avoid with amiodarone/sotalol. Use with caution in HF, bradycardia. Clarithromycin: higher risk.
Moxifloxacin	Fluoroquinolone	HIGH — among fluoroquinolones	Avoid in prolonged QTc, with antiarrhythmics. Ciprofloxacin: lower risk.
Haloperidol/Antipsychotics	Dopamine antagonist	MODERATE–HIGH	IV haloperidol: HIGH risk — use oral route. Monitor ECG in ICU patients.
Ondansetron	5-HT3 antagonist	MODERATE — 32 mg IV dose highest risk (now restricted)	Max IV dose 16 mg in adults. Avoid with other QTc-prolonging agents.
Methadone	Opioid analgesic	HIGH — dose-dependent, unpredictable	Baseline ECG, monitor QTc. Avoid with CYP3A4 inhibitors (antifungals, macrolides).

🚨 High-risk combinations: Amiodarone + Azithromycin · Sotalol + Moxifloxacin · Any two QTc-prolonging drugs + hypokalaemia + bradycardia. Always correct K⁺ >4.0 mmol/L and Mg²⁺ >0.8 mmol/L in at-risk patients.

Ref: CredibleMeds.org · AHA/ACC/HRS 2017 · KD Tripathi · Arizona CERT QTDrugs Database

📋 Guideline-Based Protocols 4 protocols

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Hypertension Management Protocol

Stepwise approach — InSH 2023 · Indian clinical practice

InSH 2023India

Confirm Diagnosis: ≥2 readings on ≥2 occasions. BP ≥140/90 = HTN. Use HBPM or ABPM to exclude white coat HTN. Classify: Stage 1 (140–159/90–99) vs Stage 2 (≥160/100).

CVD Risk Assessment: Estimate 10-year ASCVD risk. Assess for target organ damage (LVH, CKD, retinopathy, stroke), DM, dyslipidaemia. Fasting lipids, fasting glucose/HbA1c, urine ACR, eGFR, ECG baseline.

Lifestyle Modification (all patients): DASH diet (reduce Na⁺ <5g/day), weight reduction (BMI <23 kg/m²), physical activity (150 min/week moderate), smoking cessation, alcohol reduction (<1 unit/day women, <2 men), stress management.

Pharmacotherapy Initiation (InSH 2023):
• Stage 1 + low risk: Lifestyle 3–6 months, then drug if target not achieved
• Stage 1 + high risk / Stage 2: Start drug therapy immediately alongside lifestyle
• Preferred first-line SPC: ACEi/ARB + CCB (Amlodipine) — most evidence in Indians
• Step 2: Add Chlorthalidone/Indapamide (thiazide-like)
• Step 3 (resistant): Add Spironolactone 25–50 mg OD after ruling out secondary causes

Special Populations:
• Pregnancy: Methyldopa, Labetalol, Nifedipine (avoid ACEi/ARB, diuretics in 1st trimester)
• CKD: ACEi/ARB first-line (reduce proteinuria); target <130/80
• DM: ACEi/ARB preferred; target <130/80
• Elderly (≥65): Start low; target <140/80 (SBP); beware orthostasis

Follow-up: Review in 4 weeks initially (or 1 week if stage 2/high risk). Once at target: every 3–6 months. Annual bloods: K⁺, creatinine, fasting glucose, urine ACR.

🚨 Hypertensive Emergency (BP >180/120 + end-organ damage): IV labetalol 20 mg bolus then infusion, or IV nicardipine, or IV sodium nitroprusside. Target: reduce MAP by ≤25% in first hour, then gradual. Admit HDU/ICU.

Ref: InSH Guidelines 2023 · ESC/ESH HTN 2018 · JNC 8 · WHO HEARTS Technical Package

💔

Heart Failure (HFrEF) Management Protocol

EF ≤40% — ESC 2021 & HFAI stepwise protocol

ESC HF 2021HFAI 2022

Diagnosis: Symptoms (dyspnoea, orthopnoea, oedema) + Signs + Evidence of structural/functional cardiac abnormality. Echo (EF ≤40%) is key. BNP >35 pg/mL or NT-proBNP >125 pg/mL supports diagnosis.

Identify & Treat Precipitants: ACS, AF (rate control), hypertensive emergency, infection, anaemia, non-adherence to diet/drugs, NSAID/steroid use, thyroid disease, alcohol.

Initiate "Fantastic Four" (ESC 2021 — Class I, Level A):
① ACEi/ARB → switch to ARNI (sacubitril/valsartan) when stable
② Beta-blocker (bisoprolol/carvedilol/metoprolol XL) — start only when euvolaemic
③ MRA (spironolactone/eplerenone) — start after ACEi + beta-blocker
④ SGLT2i (dapagliflozin 10 mg OD or empagliflozin 10 mg OD) — add regardless of DM status
Start all four at low doses; up-titrate every 2 weeks targeting maximum tolerated doses.

Diuretics for Congestion: Furosemide — use minimum effective dose to maintain euvolaemia. Combination with thiazide (metolazone) in diuretic resistance. Daily weight monitoring (alert if +2 kg in 2 days).

Device Therapy (when appropriate):
• ICD: EF ≤35% + NYHA II–III despite ≥3 months GDMT + life expectancy >1 year
• CRT: EF ≤35% + LBBB + QRS ≥150 ms + sinus rhythm (NYHA II–IV)
• Ivabradine: Add if HR ≥75 in sinus rhythm despite max beta-blocker

Monitoring: BP, HR, weight daily at home. Renal function, K⁺, eGFR: at initiation of each drug, 1–2 weeks after each dose change, then 3–6 monthly. NT-proBNP trend for treatment response.

ℹ️ HFAI (India) note: Access to ARNI and SGLT2i is improving in India. If unavailable, ACEi + beta-blocker + MRA remain Class I and should be maximally up-titrated. Generic sacubitril/valsartan now available in India (2023).

Ref: ESC HF Guidelines 2021 · HFAI Consensus 2022 · PARADIGM-HF · DAPA-HF · EMPEROR · EMPHASIS-HF

🚨

Acute Coronary Syndrome (ACS) Protocol

STEMI · NSTEMI · Unstable Angina — Initial management

EmergencyESC ACS 2020

Immediate Assessment (0–10 min): 12-lead ECG within 10 minutes. IV access × 2. O₂ only if SpO₂ <90%. Continuous cardiac monitoring. Troponin (high-sensitivity), CBC, RFT, LFT, coagulation, lipid profile. CXR.

STEMI — Reperfusion (Door-to-Balloon <90 min / Door-to-Needle <30 min):
• Primary PCI preferred if available within 120 min
• Fibrinolysis if PCI not possible within 120 min: Tenecteplase (weight-based IV bolus), Streptokinase 1.5 MU over 60 min (if tenecteplase unavailable)
• Anticoagulation during PCI: Heparin (UFH) 70–100 U/kg IV bolus

NSTEMI/UA — Anti-ischaemic & Antiplatelet:
• Aspirin 300 mg loading immediately
• P2Y12 inhibitor: Ticagrelor 180 mg (preferred) OR Clopidogrel 300–600 mg
• Anticoagulation: Fondaparinux 2.5 mg SC OD (preferred for NSTEMI/UA) OR Enoxaparin 1 mg/kg BD
• Beta-blocker (oral) within 24h if no contraindication
• High-intensity statin immediately (Atorvastatin 40–80 mg)

Invasive Strategy (NSTE-ACS):
• Immediate (<2h): Haemodynamic instability, refractory ischaemia, life-threatening arrhythmia
• Early (<24h): GRACE >140, significant troponin rise, new ST changes
• Selective invasive (<72h): GRACE 109–140, recurrent symptoms, LVEF <40%
• Conservative: GRACE <109, no recurrence, LVEF >40%

Secondary Prevention (post-ACS — initiate before discharge):
• DAPT: Aspirin 75 mg + Ticagrelor 90 mg BD (or Clopidogrel 75 mg) × 12 months
• ACEi/ARB: Ramipril (start low, titrate up)
• Beta-blocker: Continue for ≥1 year; lifelong if EF reduced
• High-intensity statin: Atorvastatin 40–80 mg
• Aldosterone antagonist if EF <40% + DM or HF symptoms

🚨 Morphine use in ACS: Evidence suggests potential harm (CRUSADE registry). Use with caution — may delay oral antiplatelet absorption. Prefer IV nitrates for pain relief if BP permits.

Ref: ESC STEMI 2017 · ESC NSTE-ACS 2020 · ACC/AHA 2022 · KD Tripathi · Cardiological Society of India

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Anticoagulation — Special Populations

Renal impairment · Pregnancy · Elderly · Obesity

RenalPregnancyESC 2020

Population	Preferred Agent	Dose Adjustment	Avoid
CKD Stage 3a (eGFR 45–59)	Apixaban or Rivaroxaban	Standard dose; monitor closely	Dabigatran (renally cleared 80%)
CKD Stage 3b–4 (eGFR 15–44)	Apixaban 2.5 mg BD (if criteria met) or Warfarin	Reduce dose; anti-Xa monitoring for LMWH	Dabigatran (avoid <30); Rivaroxaban (reduce to 15 mg in AF if 15–49)
ESRD / Dialysis (eGFR <15)	Warfarin (INR 2–3) or Apixaban 5 mg BD (limited data)	Frequent INR monitoring if warfarin	All DOACs — limited evidence; avoid if possible
Pregnancy (AF/VTE)	LMWH (Enoxaparin) throughout pregnancy	1 mg/kg BD; anti-Xa monitoring target 0.6–1.0 U/mL (peak, 4h post-dose); increase dose in 3rd trimester as weight increases	Warfarin (1st trimester — embryopathy; 3rd trimester — neonatal haemorrhage); All DOACs (teratogenic, contraindicated)
Postpartum	LMWH or warfarin (warfarin safe in breastfeeding)	Resume 4–6h post-SVD, 6–12h post-CS if haemostasis achieved	DOACs — limited data in breastfeeding; avoid
Elderly (>75 years)	Apixaban (best safety profile in elderly — ARISTOTLE)	Check 2-of-3 criteria for dose reduction: age ≥80, wt ≤60 kg, Cr ≥1.5 mg/dL → 2.5 mg BD	Dabigatran 150 mg BD — high GI bleed risk in elderly; use 110 mg BD
Obesity (BMI >40 or >120 kg)	Warfarin or LMWH (weight-based)	Peak anti-Xa monitoring for LMWH; max capped dose or twice-daily regimen. DOACs: limited pharmacokinetic data in extreme obesity	Fixed low-dose LMWH (prophylaxis underdosing common in obesity)
Mechanical Heart Valve	Warfarin ONLY	INR 2.5–3.5 (mitral position or tilting disc); INR 2–3 (bileaflet aortic with no risk factors)	All DOACs (RE-ALIGN trial — excess valve thrombosis and bleeding with dabigatran)

⚠️ Anticoagulation in active cancer: LMWH traditionally preferred. Apixaban and rivaroxaban now recommended by ESC/ISTH in most cancers except high GI/GU bleed risk cancers (gastric, GI tumours) where LMWH remains preferred.

Ref: ESC AF 2020 · ESC VTE Guidelines 2019 · BTS/RCOG Pregnancy VTE · ISTH Guidance Cancer-associated VTE · KD Tripathi

🔬 Drug Interactions & Therapeutic Drug Monitoring

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Key Drug Interactions — Cardiac Patients

High-risk combinations in clinical practice

InteractionsCYP450

Drug 1	Drug 2	Interaction	Management
Warfarin	Amiodarone	Amiodarone inhibits CYP2C9 → ↑ warfarin levels → ↑ bleeding risk (may persist 6+ months after amiodarone stopped)	Reduce warfarin dose by 30–50% proactively. Increase INR monitoring frequency to weekly initially.
Warfarin	Fluconazole / Antifungals	Strong CYP2C9 inhibition → marked ↑ INR	Avoid if possible; if essential, reduce warfarin dose 25–50% and monitor INR every 2–3 days.
Statin (Simvastatin/Lovastatin)	Amlodipine, Diltiazem, Verapamil	CYP3A4 inhibition → ↑ statin levels → myopathy/rhabdomyolysis risk	Simvastatin max 20 mg with amlodipine. Switch to rosuvastatin or pravastatin (not CYP3A4 metabolised).
Digoxin	Amiodarone, Verapamil, Spironolactone, Clarithromycin	↑ Digoxin levels (P-glycoprotein inhibition and/or reduced renal clearance) → toxicity	Halve digoxin dose when starting amiodarone/verapamil. Monitor digoxin levels and ECG (AV block, arrhythmias).
ACEi / ARB	Spironolactone / MRA	↑ Hyperkalaemia risk — especially in CKD, DM, high K⁺ diet	Avoid if K⁺ >5.0 or eGFR <30. Monitor K⁺ and creatinine at 1–2 weeks and 1 month after initiation.
Ticagrelor	Strong CYP3A4 inhibitors (Ketoconazole, Ritonavir, Clarithromycin)	↑ Ticagrelor plasma levels → ↑ bleeding risk	Contraindicated. Use clopidogrel instead if these drugs are essential.
Beta-blocker	Verapamil / Diltiazem (IV)	Synergistic AV nodal blockade → severe bradycardia, complete heart block, asystole	Never give IV verapamil/diltiazem to patient on beta-blocker without careful monitoring. Oral combination is relatively safer but requires ECG monitoring.
Metformin	IV Contrast (iodinated)	↑ Risk of contrast-induced nephropathy + lactic acidosis	Hold metformin 48h before IV contrast if eGFR <60. Resume only after renal function confirmed stable 48h post-procedure.

Ref: KD Tripathi 8th Ed · BNF 2024 · Stockley's Drug Interactions · CDSCO · CredibleMeds.org

🧪

Therapeutic Drug Monitoring (TDM) — Cardiac Drugs

Target levels, timing, and interpretation

DigoxinAmiodaroneWarfarin

Drug	Target Level / INR	Sampling Time	Notes on Interpretation
Digoxin	0.5–0.9 ng/mL (HF/AF rate control) <1.2 ng/mL to avoid toxicity	Trough: ≥6h post-dose (≥12h preferred)	Levels >2 ng/mL = toxicity likely. Hypokalaemia, hypomagnesaemia, hypothyroidism potentiate toxicity even at "normal" levels. Adjust dose in renal impairment.
Warfarin (INR)	2.0–3.0 (most AF/VTE) 2.5–3.5 (mechanical MV, some tilting disc valves)	Any time after stable dosing; trough preferred	INR <2 = subtherapeutic (thrombosis risk). INR >5 = high bleed risk (hold dose, consider Vit K). Labile INR: check adherence, dietary Vit K, drug interactions.
Amiodarone (thyroid/LFT monitoring)	Not routinely measured; Metabolite DEA therapeutic range approximately 0.5–2.0 mg/L if assay available	Not routine — assess for toxicity	Monitor TFTs, LFTs, PFTs, CXR annually (pulmonary toxicity). Corneal microdeposits, photosensitivity — counsel patients. Half-life 40–55 days.
Enoxaparin (anti-Xa)	Therapeutic: peak 0.6–1.0 U/mL (BD dosing) Prophylactic: peak 0.2–0.4 U/mL	4h post SC dose (peak)	Indicated in: renal impairment (eGFR <30), obesity, pregnancy, extremes of weight. Anti-Xa not needed for standard dosing in normal renal function.
Unfractionated Heparin (UFH)	APTT ratio 1.5–2.5× control (60–100 seconds typically)	6h after initiation; 6h after each dose change	Highly variable response. Use weight-based nomogram. Platelet count every 2–3 days — monitor for HIT (fall >50% from baseline).

Ref: KD Tripathi 8th Ed · BNF 2024 · BCSH Guidelines · WHO Essential Medicines TDM guidance