Substance and claimed effects

This entry covers the class of non-statin LDL-lowering therapies used as add-ons (or, in statin intolerance, substitutes) to push LDL-C below what statin monotherapy achieves: ezetimibe (intestinal cholesterol-absorption inhibitor; NPC1L1 target), bempedoic acid (ATP-citrate lyase inhibitor; upstream of HMG-CoA reductase), PCSK9 monoclonal antibodies (evolocumab, alirocumab; subcutaneous q2–4 weeks), and inclisiran (siRNA targeting hepatic PCSK9 mRNA; subcutaneous twice yearly). The class is prescribed for atherosclerotic cardiovascular disease risk reduction in patients who remain above LDL-C goal on maximally tolerated statin, and for patients with statin intolerance. Claimed effects, in order of evidential weight: lower LDL-C (incremental 17%–60% on top of statin depending on agent), fewer major adverse cardiovascular events (myocardial infarction, stroke, coronary revascularization, cardiovascular death), and — in patients with high baseline event rates — a modest all-cause mortality signal for alirocumab. The dominant catalogue dimension is longevity via cardiovascular event prevention; effects on short-term wellness, energy, focus, sleep, mood, or appearance are negligible. The substance is prescription-only, requires a clinician decision, and the meaningful unit of analysis is the class rather than any single drug — the choice between agents turns on cost, route, LDL gap to goal, and tolerance history.

Evidence by addressing question

mechanism

The class is the natural extension of the LDL-receptor story. Hepatocyte LDL receptors clear circulating LDL particles by binding apoB-100 and pulling the particle into the cell for lysosomal degradation. The receptor can be recycled to the surface — or sent to the lysosome with its cargo and destroyed. The number of surface receptors at steady state sets clearance capacity. Each non-statin agent intervenes at a different node of this system.

Ezetimibe binds the Niemann-Pick C1-like 1 (NPC1L1) transporter on enterocytes of the small intestine, blocking absorption of dietary and biliary cholesterol. Reduced hepatic cholesterol delivery upregulates LDL-receptor expression via SREBP-2, increasing LDL clearance from the circulation. On a statin background, ezetimibe adds roughly 20%–25% further LDL-C reduction (Lloyd-Jones et al., JACC 2022).

Bempedoic acid is a prodrug activated to its CoA derivative only in hepatocytes by ACSVL1 (very long-chain acyl-CoA synthetase 1), an enzyme absent from skeletal muscle. The active metabolite inhibits ATP-citrate lyase, the enzyme one step upstream of HMG-CoA reductase in cholesterol biosynthesis. Same downstream effect as statins (reduced intracellular cholesterol, upregulated LDL receptors), but the muscle-sparing activation pattern explains the low rate of muscle adverse events observed in CLEAR Outcomes versus statin populations (Nissen et al., NEJM 2023). LDL-C reduction is ~17%–25% as monotherapy or add-on.

PCSK9 (proprotein convertase subtilisin/kexin type 9) is a hepatic secreted protein that binds the LDL receptor and routes it to lysosomal degradation rather than recycling. Blocking PCSK9 preserves surface LDL receptors and dramatically increases LDL clearance. The therapeutic target was validated by human genetics: nonsense mutations in PCSK9 in 2.6% of Black participants in the Dallas Heart Study were associated with 28% lower LDL-C and 88% lower coronary heart disease risk over 15 years (Cohen et al., NEJM 2006). Evolocumab and alirocumab are fully human monoclonal antibodies that bind extracellular PCSK9 and block the receptor interaction; LDL-C reduction is ~60% on top of statin. Inclisiran is a GalNAc-conjugated small interfering RNA that uses the asialoglycoprotein receptor for hepatocyte uptake, then engages the RISC complex to degrade PCSK9 mRNA before translation. Twice-yearly subcutaneous dosing achieves time-averaged LDL-C reduction of ~50%–52% over 18 months (Ray et al., NEJM 2020).

The unifying mechanism: each agent ends with more LDL receptors clearing more LDL particles. The Cholesterol Treatment Trialists' meta-analyses across 26 statin trials established that vascular event rates fall by roughly 22% per 1 mmol/L (~39 mg/dL) reduction in LDL-C, irrespective of starting level (CTT Collaboration, Lancet 2010). Outcomes trials of ezetimibe and PCSK9 inhibitors have replicated this LDL-to-event slope at lower achieved LDL-C, supporting the "lower is better" framing through at least ~30 mg/dL (Sabatine et al., NEJM 2017).

evidence

Four major outcomes trials anchor the class.

IMPROVE-IT (n=18,144 post-acute coronary syndrome patients) randomized simvastatin 40 mg plus ezetimibe 10 mg versus simvastatin plus placebo. Median LDL-C: 53.7 versus 69.5 mg/dL. The 7-year Kaplan-Meier rate of the composite (CV death, nonfatal MI, unstable angina rehospitalization, coronary revascularization ≥30 days, nonfatal stroke) was 32.7% versus 34.7% (HR 0.936, 95% CI 0.89–0.99, p=0.016) — a 2 percentage-point absolute risk reduction over 7 years (Cannon et al., NEJM 2015). This was the first trial to demonstrate that adding a non-statin LDL-lowering agent improves outcomes on top of a statin and the proof of the "LDL hypothesis" beyond statin pleiotropy.

FOURIER (n=27,564 patients with established atherosclerotic cardiovascular disease and LDL-C ≥70 mg/dL on statin) randomized evolocumab 140 mg q2 weeks or 420 mg monthly versus placebo. Median LDL-C dropped from 92 to 30 mg/dL (~60% reduction). Over a median 2.2 years, the primary composite (CV death, MI, stroke, hospitalization for unstable angina, coronary revascularization) occurred in 9.8% versus 11.3% (HR 0.85, 95% CI 0.79–0.92, p<0.001) (Sabatine et al., NEJM 2017). Risk reduction accrued over time (12% in year 1, 19% beyond year 1), consistent with the slow CTT-style benefit of LDL exposure-time. No significant effect on CV death or all-cause mortality in the trial period, and a contested 2023 reanalysis of regulatory data alleged miscounting that the TIMI Study Group disputed.

ODYSSEY OUTCOMES (n=18,924 patients within 1–12 months of acute coronary syndrome, LDL-C ≥70 mg/dL on statin) randomized alirocumab 75 mg q2 weeks (titrated to 150 mg if LDL-C remained ≥50 mg/dL) versus placebo. Median follow-up 2.8 years. Primary composite (CHD death, nonfatal MI, ischemic stroke, hospitalization for unstable angina) occurred in 9.5% versus 11.1% (HR 0.85, 95% CI 0.78–0.93, p<0.001). All-cause mortality 3.5% versus 4.1% (HR 0.85, 95% CI 0.73–0.98) — the only PCSK9 outcomes trial with a mortality signal, though the trial was not formally powered for that endpoint. Absolute benefit was greater in patients with baseline LDL-C ≥100 mg/dL (Schwartz et al., NEJM 2018).

CLEAR Outcomes (n=13,970 statin-intolerant patients with or at high risk of cardiovascular disease) randomized bempedoic acid 180 mg daily versus placebo. LDL-C reduction at 6 months was 21.1 percentage points (29.2 mg/dL) greater with bempedoic acid. Over a median 40.6 months, the primary composite (CV death, nonfatal MI, nonfatal stroke, coronary revascularization) occurred in 11.7% versus 13.3% (HR 0.87, 95% CI 0.79–0.96, p=0.004) (Nissen et al., NEJM 2023). CLEAR was the first outcomes trial in a statin-intolerant population and demonstrated that the LDL-event relationship holds outside the statin context. Subgroup analyses showed a particularly strong primary-prevention effect.

Inclisiran outcomes trials are not yet reported. The pivotal phase 3 program (ORION-9 in heterozygous familial hypercholesterolemia, ORION-10 in US ASCVD patients, ORION-11 in European ASCVD/high-risk patients) demonstrated time-averaged LDL-C reductions of 49.9%–52.3% over 510 days versus placebo, with twice-yearly subcutaneous dosing after a 0/3-month loading (Ray et al., NEJM 2020). ORION-3 and ORION-8 open-label extensions confirmed durable LDL-C reduction out to 4–6 years. The cardiovascular outcomes trial VICTORION-2 PREVENT is ongoing through 2026–2027; until it reports, inclisiran's cardiovascular benefit is inferred from the LDL hypothesis and PCSK9-mAb outcomes rather than directly demonstrated.

Guideline alignment is broad. The 2018 AHA/ACC/multisociety cholesterol guideline endorses ezetimibe and then PCSK9 inhibitors as sequential add-ons in very-high-risk ASCVD when LDL-C remains ≥70 mg/dL on maximally tolerated statin (Grundy et al., Circulation 2019). The 2019 ESC/EAS guidelines moved more aggressively, recommending LDL-C <55 mg/dL with ≥50% reduction from baseline as the target in very-high-risk patients (Mach et al., Eur Heart J 2020). The 2022 ACC Expert Consensus Decision Pathway operationalizes the choice: ezetimibe first if the LDL-C gap is <25%, PCSK9 inhibitor first if >25%, with bempedoic acid as a further add-on or as a primary option in statin intolerance (Lloyd-Jones et al., JACC 2022).

protocol

Each agent has a fixed-dose protocol; there is no titration to LDL except in alirocumab.

• Ezetimibe — 10 mg once daily, any time, with or without food. Available as monotherapy or co-formulated with simvastatin, atorvastatin, or rosuvastatin. Generic (Zetia equivalents) is <$100/year retail with coupons.
• Bempedoic acid — 180 mg once daily oral. Also co-formulated with ezetimibe (Nexlizet/Nustendi). Wholesale price ~$470/month (~$5,640/year list) in the US as of 2024; manufacturer copay programs reduce out-of-pocket to as low as $10/month for commercially insured patients.
• Evolocumab — 140 mg subcutaneous every 2 weeks or 420 mg monthly, self-injected with pre-filled pen. List price was $14,000/year at 2015 launch; cut 60% to ~$5,850/year in 2018; further reduced in patient-direct programs to ~$239/month (~$2,870/year) by 2025.
• Alirocumab — 75 mg subcutaneous every 2 weeks, titrated to 150 mg if LDL-C remains above goal. Listed at ~$5,850/year after the 2018 price cut.
• Inclisiran — 284 mg subcutaneous injection administered by a healthcare provider at month 0, month 3, then every 6 months. US list price ~$3,250 per dose: ~$9,750 in year 1 (three doses), ~$6,500 in subsequent years (two doses). Marketed as a "buy-and-bill" medical-benefit injection rather than a pharmacy-benefit drug.

Goal: in very-high-risk ASCVD, LDL-C <55 mg/dL (ESC/EAS) or <70 mg/dL (AHA/ACC threshold to escalate); in extremely high-risk or recurrent-event patients, <40 mg/dL is increasingly considered (Mach et al., Eur Heart J 2020). Reassessment is via fasting lipid panel 4–12 weeks after initiation or dose change, then every 3–12 months.

contraindications

None of the non-statin agents has been studied in pregnancy; class labelling discourages use during pregnancy and breastfeeding. Bempedoic acid raises serum uric acid by ~0.8 mg/dL on average and increases gout risk modestly (3.1% vs 2.1% in CLEAR Outcomes) — a relative contraindication in patients with frequent gout flares (Nissen et al., NEJM 2023). Tendon rupture has been reported with bempedoic acid (low absolute rate). Ezetimibe is hepatically metabolized — caution in active hepatic disease. PCSK9 monoclonal antibodies and inclisiran have favorable safety profiles in trials; injection-site reactions (2.6%–4.7% with inclisiran versus <1% placebo) are the most common nuisance. No signal for neurocognitive dysfunction, new-onset diabetes, or cataracts in the PCSK9 trials despite achieved LDL-C levels as low as 20 mg/dL.

misconceptions

Three patterns recur in clinical practice.

"Statin intolerance" is mostly the nocebo effect. SAMSON, a blinded n-of-1 crossover trial in 60 patients who had stopped statins for muscle symptoms, found symptom-intensity scores of 16.3 on atorvastatin, 15.4 on placebo, and 8.0 on no pill (p<0.001 versus pill) — meaning ~90% of the symptomatic burden was attributable to the act of taking a pill rather than to the statin itself (Howard et al., JACC 2021). Half of SAMSON participants successfully restarted statins after being shown their data. The clinical implication: before jumping to bempedoic acid or a PCSK9 inhibitor for "statin intolerance," re-challenge with a different statin (rosuvastatin or pravastatin), lower dose, or every-other-day dosing is the evidence-based first step. The 2022 ACC pathway makes this explicit.

"PCSK9 inhibitors are too new and too expensive to use." Both halves of this have shifted. Evolocumab was first approved in 2015; outcomes data are 8+ years old and safety follow-up extends past 5 years. Price-wise, list prices for evolocumab and alirocumab were cut 60% in 2018–2019 and further patient-assistance and direct-purchase programs have reduced effective costs in the US to $2,500–$5,000/year. The ICER cost-effectiveness threshold (<$150,000/QALY) is now met at current pricing for very-high-risk secondary prevention.

"Ezetimibe is too weak to matter." Effect size is modest in isolation (~20%–25% additional LDL-C), but on the CTT slope (~22% RR reduction per 1 mmol/L), 20 mg/dL of incremental LDL-C reduction translates to ~10% RR reduction in major vascular events — exactly the IMPROVE-IT result. The 2 percentage-point absolute risk reduction over 7 years in a high-risk population is meaningful even if the relative hazard ratio looks small.

alternatives

Within the non-statin LDL-lowering space, the four classes are mostly complementary rather than competitive. The 2022 ACC pathway orders them by gap-to-goal: ezetimibe first if <25% additional reduction needed, PCSK9 mAb first if >25% needed, bempedoic acid as further add-on or first-line in statin intolerance, inclisiran as a PCSK9-mAb substitute when adherence to self-injection is poor or as switch therapy (Lloyd-Jones et al., JACC 2022).

Outside this class: niacin failed to reduce events when added to statin in AIM-HIGH and HPS2-THRIVE despite raising HDL and lowering LDL — abandoned for LDL-lowering use. Bile acid sequestrants (cholestyramine, colesevelam) lower LDL ~15% but are GI-tolerability-limited; clinical use is now niche. Fibrates primarily address triglycerides and have minimal LDL effect; not part of this entry. Lp(a)-lowering antisense and siRNA agents (pelacarsen, olpasiran, lepodisiran) are in phase 3 outcomes trials but not yet approved as of 2026; these target lipoprotein(a), not LDL, and belong to a separate entry on Lp(a). Investigational oral PCSK9 inhibitors (e.g., enlicitide) are in development; not yet approved.

failure-modes

The dominant failure mode is undertreatment. Registry data (e.g., GOULD, DA VINCI) show that >70% of very-high-risk ASCVD patients in the US and Europe are not at the LDL-C target despite statin therapy, and add-on non-statin use is below 10%–15%. Common upstream causes: clinicians not escalating beyond statin, patients not knowing their LDL-C number, insurance prior-authorization friction for PCSK9 inhibitors, and the false belief that "on statin" equals "treated."

A specific failure mode for PCSK9 mAbs is adherence — q2-week self-injection has real-world persistence rates around 60%–70% at 1 year. Inclisiran's twice-yearly clinic injection model exists partly to address this, though it shifts the cost into the medical benefit and creates a different administrative bottleneck.

Statin abandonment is its own failure mode: a patient who had real or perceived statin intolerance, stopped, was not re-challenged, and was not switched to bempedoic acid or PCSK9 monotherapy — and is therefore on no LDL-lowering therapy at all. CLEAR Outcomes proves that bempedoic acid is a defensible monotherapy for this population.

practicalities

Cost and access are the dominant practical concerns, and they vary across agents by orders of magnitude. Ezetimibe is generic, cheap, and universally covered. Bempedoic acid has manufacturer copay programs that can reduce commercial-insurance out-of-pocket to ~$10–$25/month. PCSK9 monoclonal antibodies require self-injection comfort and either pharmacy-benefit coverage with prior authorization or use of the manufacturer's patient-direct programs. Inclisiran is administered in a clinical setting under the medical benefit (Part B in Medicare), shifting administrative complexity from pharmacy to provider but eliminating the patient-injection step entirely. Geographic and insurance variation is large; what's free for one patient is unobtainable for another.

stakes

For very-high-risk secondary-prevention patients (history of MI, stroke, multi-vessel CAD, peripheral artery disease), staying at LDL-C ~90–100 mg/dL on statin alone — instead of pushing to ~50 — translates to a measurable absolute increase in 5-year MACE incidence. The FOURIER-ODYSSEY absolute risk reductions of ~1.5 percentage points over 2–3 years compound over a decade. The harder consequence to make legible: recurrent ACS, second strokes, and revascularization procedures are the lived form of the missing 15% relative risk reduction.

payoff

For the population that uses this class correctly — very-high-risk ASCVD with LDL above goal on statin — the projected payoff is fewer MIs, fewer strokes, fewer revascularizations, fewer hospitalizations across the next decade. The mechanism is slow plaque stabilization and modest regression (HOPE-3, GLAGOV, HUYGENS imaging data on evolocumab show measurable atheroma reduction at very low LDL-C). The effect is invisible day-to-day — there is no felt difference at LDL 50 versus LDL 100. The win is statistical and prospective: a smaller population of future cardiovascular events.

history

The field moved from "statins are the only proven LDL-lowering therapy that reduces events" (the position after the 2000–2010 ENHANCE controversy with ezetimibe-simvastatin in familial hypercholesterolemia) to "any agent that lowers LDL by an LDL-receptor mechanism reduces events proportionally to LDL change" (the position after IMPROVE-IT 2015 and FOURIER/ODYSSEY OUTCOMES 2017–2018). Bempedoic acid (CLEAR Outcomes 2023) extended this to the statin-intolerant population. Inclisiran is the field's first siRNA therapeutic for a chronic-disease indication and the operational template for twice-yearly dosing of chronic biologics.

out-of-scope

Lp(a)-specific therapeutics, oral PCSK9 inhibitors in development, and CETP inhibitors (obicetrapib) are adjacent but warrant their own entries. Familial hypercholesterolemia genetic testing, apoB measurement as a more accurate atherogenic-particle proxy, and coronary CT angiography for risk stratification are companion topics.

The credibility range

The optimist case. The LDL hypothesis is one of the best-supported causal claims in modern medicine. Mendelian randomization across genes affecting LDL-C (PCSK9, HMG-CoA reductase, NPC1L1, LDL receptor, APOB) converges on the same exposure-response relationship that pharmacologic trials produce: each 1 mmol/L lower lifetime LDL-C is associated with ~50%+ lower CHD risk, and each 1 mmol/L lower trial-achieved LDL-C is associated with ~22% RR reduction over 3–5 years (CTT Collaboration, Lancet 2010). The four outcomes trials (IMPROVE-IT, FOURIER, ODYSSEY OUTCOMES, CLEAR Outcomes) are positive, mechanistically diverse (intestinal absorption, ATP-citrate lyase, two PCSK9 targets), and convergent. Inclisiran lacks an outcomes trial but produces the same LDL-C reduction as PCSK9 mAbs through the same target; the inferential bridge is strong. Safety data through 5–8 years across hundreds of thousands of patient-years show no major class signal. The optimist case is that any high-risk patient above goal on statin should be on a non-statin add-on, and the only question is which agent.

The skeptic case. Absolute risk reductions in the trials are modest: 2 percentage points over 7 years for IMPROVE-IT, 1.5 percentage points over 2 years for FOURIER, 1.6 percentage points over 2.8 years for ODYSSEY OUTCOMES, 1.6 percentage points over 3.4 years for CLEAR Outcomes. Numbers-needed-to-treat sit in the 50–80 range over trial durations. Cost-effectiveness for PCSK9 mAbs and inclisiran depends sensitively on price and on real-world LDL-C reduction matching trial-achieved values; current list prices remain expensive without negotiated pricing. FOURIER showed no significant CV mortality benefit and a contested 2023 reanalysis alleged underreported deaths (TIMI disputes the reanalysis). Inclisiran's cardiovascular outcomes remain unproven — it is being prescribed on LDL-C reduction and the PCSK9 outcomes-trial precedent, not on its own outcomes data. ENHANCE and earlier ezetimibe-imaging trials disappointed for surrogate endpoints, though IMPROVE-IT vindicated the agent on hard outcomes.

Author's call. The LDL hypothesis is settled; the only live questions are pricing, sequencing, and how aggressively to push goals in lower-risk populations. For the entry's target reader (a high-risk patient on statin who has heard of these drugs but doesn't know whether to ask about them), the answer is unambiguous: yes, ask, particularly if your LDL-C remains above 70 mg/dL after maximally tolerated statin. The class deserves a high evidence rating (5) and a high longevity rating (4) — substantial but not population-bending in the way base statins are, because the incremental benefit on top of statin is smaller in absolute terms. controversy is low (1) — the field disagrees on tactical questions (which agent first, exact LDL targets in lower-risk groups) but not on the core position.

Stakeholder and incentive map

• Manufacturers: Amgen (evolocumab), Sanofi/Regeneron (alirocumab), Novartis (inclisiran, after acquiring Medicines Co.), Esperion (bempedoic acid), Merck (originator of ezetimibe; now generic). Outcomes-trial-driven launches and high initial pricing followed by 60% price cuts after slow uptake.
• Professional bodies: AHA, ACC, ESC, EAS, National Lipid Association — all aligned on the "lower is better" framing and on sequential add-on therapy. The 2022 ACC pathway and 2019 ESC/EAS guidelines are the operational documents.
• Payers: Initial PCSK9 prior-authorization rejection rates exceeded 70% in 2015–2017; rates fell as prices fell. Inclisiran's medical-benefit billing creates a different payer dynamic.
• Cost-effectiveness analysts: ICER — drove the public conversation about PCSK9 cost-effectiveness and the subsequent price cuts.
• Skeptic camp: A small "statin-skeptic" / LDL-skeptic group disputes the LDL-causal hypothesis entirely, citing the FOURIER mortality reanalysis and pleiotropy arguments. This camp is not in the cardiology mainstream.

Population variability

The effect of LDL-C reduction on cardiovascular events scales with baseline absolute risk, not with baseline LDL-C. Patients with established ASCVD, diabetes with multiple risk factors, familial hypercholesterolemia, or recent ACS see the largest absolute benefit; primary prevention with low absolute risk sees small absolute benefit even with substantial LDL-C lowering. The 2018 AHA/ACC guideline operationalizes this with the <70 mg/dL threshold for very-high-risk ASCVD and a more permissive approach for moderate-risk groups (Grundy et al., Circulation 2019).

Variability by population:

• Familial hypercholesterolemia (heterozygous and homozygous) — PCSK9 mAbs and inclisiran are particularly effective; evolocumab is approved for HoFH from age 10.
• Statin-intolerant patients — CLEAR Outcomes establishes bempedoic acid; PCSK9 mAb monotherapy is supported by GAUSS-3, ALTERNATIVES.
• Diabetes — CLEAR Outcomes prespecified-subgroup analysis showed consistent benefit; PCSK9 outcomes trials similarly consistent.
• Older adults (≥75) — ODYSSEY OUTCOMES subgroup analysis showed preserved benefit; safety profile maintained.
• Women — historically under-represented in lipid trials; recent registries and subgroup analyses confirm similar relative benefit, though baseline event rates differ.
• Trial populations have under-represented Black and South Asian patients, who carry differential CV risk; effect-size extrapolation is plausible but not proven within those groups.

Knowledge gaps

The most consequential open question is inclisiran's cardiovascular outcomes — VICTORION-2 PREVENT reports in 2026–2027. A positive result will lock in the twice-yearly siRNA model as a peer of mAbs; a null result would reframe inclisiran as an LDL-lowering tool whose CV benefit is inferred rather than demonstrated. Long-term safety beyond 8 years at very low LDL-C (<30 mg/dL) is incompletely characterized — current data are reassuring but the follow-up is shorter than for statins. The LDL-C threshold below which additional reduction stops adding benefit, if such a threshold exists, has not been identified in trials so far. Effect-size in primary prevention with non-statin add-on is not directly trial-tested (FOURIER and ODYSSEY OUTCOMES enrolled established ASCVD); CLEAR Outcomes provided some primary-prevention data via its mixed population, but a dedicated trial is absent. Comparative-effectiveness between PCSK9 mAb and inclisiran on hard endpoints will not be available before the late 2020s.

Scope and what the brief named. The brief named ezetimibe, bempedoic acid, PCSK9 inhibitors, and inclisiran, plus their effects on LDL, cardiovascular events, tolerability, and access. All four agents are covered end-to-end in mechanism, evidence, protocol, contraindications, practicalities, and misconceptions. Inclisiran's cardiovascular outcomes data are pending (VICTORION-2 PREVENT, reading out 2026–2027) — the article notes this honestly rather than implying outcomes parity with the PCSK9 monoclonals.

Action verb. Chose decide over do because these are prescription-only with multiple branching paths the reader can't operationalize alone — the right move is asking the cardiologist the right questions, not picking a drug. do would have undersold the clinician-required nature.

Cadence. Chose daily because the dominant pattern across the class once initiated is daily oral therapy (ezetimibe, bempedoic acid) plus chronic medication that doesn't fit the other tokens (PCSK9 mAb q2 weeks, inclisiran twice yearly). as-needed and course both mis-signal episodic use. The cadence token is imperfect — this is really "ongoing chronic medication" — but daily matches the lifelong-medication framing called out in the meta spec.

Longevity score (4 vs 5). Considered 5 given the LDL-event slope and the four positive outcomes trials. Settled on 4 because the absolute risk reductions on top of statin are modest (1.5–2 percentage points over 2–7 years), and the population-bending base effect of LDL lowering belongs to the statin entry, not this one. This is incremental therapy on top of a foundation.

Cost burden score (3). The range spans from generic ezetimibe (~$70/year, score 1) to inclisiran ($6,500–9,750/year list, score 4). A single number can't capture that. Chose 3 with a justification that names the range honestly. A reader who lands on ezetimibe sees the lower bound; a reader who lands on inclisiran without insurance sees the upper.

Evidence score (5) despite inclisiran outcomes gap. The class as a whole has four positive outcomes trials, Mendelian-randomization target validation, and triple-society guideline endorsement. Inclisiran's outcomes-trial gap is a real qualifier but doesn't move the class-level evidence score off 5 — the LDL-event slope is the most robust quantitative relationship in cardiovascular medicine.

Audience scoping. Left unscoped despite the population being largely 40+ with cardiovascular disease. Familial hypercholesterolemia and young secondary-prevention cases pull the under-40 slice in. Restrictive scoping would have shrunk reach to no real benefit.

Excluded explicitly. Niacin (failed AIM-HIGH, HPS2-THRIVE — abandoned for LDL use); bile acid sequestrants (GI tolerability, niche); fibrates (triglyceride-focused, not LDL); red yeast rice / monacolin K (essentially low-dose lovastatin, not "beyond" statins); CETP inhibitors (obicetrapib still in trials).

Future-link candidates. statins (the foundation), apob-testing, lipoprotein-a (with its own emerging drug class), familial-hypercholesterolemia, coronary-calcium-score. None known to exist yet — left out of related so the renderer doesn't break, but flagged in the article's out-of-scope section and here for backlog.

Separate-entry candidates. Lp(a)-lowering therapeutics (pelacarsen, olpasiran, lepodisiran) deserve their own entry once outcomes trials report. Oral PCSK9 inhibitors (enlicitide and successors) likely a separate near-term entry. Statin intolerance and statin re-challenge protocols are big enough to warrant their own entry rather than living in this article's misconceptions section.

FOURIER mortality controversy. Mentioned the 2023 reanalysis briefly in research (TIMI Group rebutted) but kept it out of the reader-facing article — the dispute is technical and doesn't change the headline reading of the trial.

SAMSON inclusion in misconceptions. Considered putting the statin-intolerance reframe in alternatives or failure-modes instead. Chose misconceptions because the dominant pattern is the patient's mental model ("I can't take statins") not a clinical-pathway gap. The friend-test reading lands cleaner there.