Hydralazine: Comprehensive Drug Monograph

Pharmacokinetic Profile

Half-Life

~3–7 h (longer in renal impairment)

Metabolism

Hepatic acetylation (NAT2 polymorphism)

Protein Binding

~87%

Bioavailability

Variable; slow acetylators have ~2× the AUC of fast acetylators

Onset / Duration

Oral: 20–30 min / 2–4 h · IV: 5–30 min / 2–6 h

Clinical Information

Drug Class

Direct arteriolar vasodilator

Available Doses

10 / 25 / 50 / 100 mg tablets · 20 mg/mL injection

Route

PO 2–4× daily; IV/IM for hypertensive emergencies

Renal Adjustment

Caution in severe impairment; reduce dose / extend interval

Hepatic Adjustment

Use with caution; reduce dose

Pregnancy

Used for severe acute HTN of pregnancy (preeclampsia/eclampsia)

Lactation

Excreted in milk; generally considered compatible

Schedule

Non-controlled (Rx only)

Generic Available

Yes (multiple generic manufacturers)

Indications

Indication	Approved Population	Therapy Type	Status
Essential hypertension — oral therapy, alone or as an adjunct	Adults; chronic management	Add-on therapy after first-line agents	FDA Approved
Severe essential hypertension when oral therapy is not feasible or BP must be lowered urgently — parenteral therapy (IV/IM)	Adults in inpatient or emergency settings	Acute/short-term parenteral use	FDA Approved

Hydralazine is one of the oldest available antihypertensives and remains a useful add-on agent in resistant hypertension and selected acute hypertensive scenarios. Per JNC 8 and current ACC/AHA hypertension guidance, it is not a first-line agent for essential hypertension because of dosing frequency, reflex tachycardia, sodium retention, and the risk of drug-induced lupus; it is added when first-line agents (thiazide, calcium channel blocker, ACEi/ARB) are insufficient or not tolerated. Its hemodynamic profile — predominantly arteriolar dilation with minimal venous effect — makes it most useful as an afterload reducer when combined with a beta-blocker (to control reflex tachycardia) and a diuretic (to control sodium and water retention). Reflex sympathetic activation also limits hydralazine monotherapy in coronary disease.

Off-Label / Guideline-Supported Uses

HFrEF — combination with isosorbide dinitrate (H-ISDN): Per the 2022 AHA/ACC/HFSA HF guideline, the fixed-dose combination of isosorbide dinitrate and hydralazine is a Class 1 recommendation in self-identified African-American patients with NYHA class III–IV HFrEF receiving optimal GDMT, based on the A-HeFT trial which showed a mortality benefit. It is also a Class 2a recommendation for patients of any race/ethnicity with current or prior symptomatic HFrEF who cannot tolerate ACEi/ARB/ARNI due to drug intolerance, hypotension, or renal insufficiency. Evidence quality: high (within the African-American HFrEF population).

Severe acute hypertension in pregnancy (preeclampsia / eclampsia / postpartum): IV hydralazine is recommended by ACOG (Practice Bulletin No. 222, incorporating Committee Opinion No. 767) as one of the first-line agents (alongside IV labetalol and oral immediate-release nifedipine) for sustained severe hypertension in pregnancy. Evidence quality: moderate.

Acute decompensated HF with severe hypertension: Sometimes used parenterally for afterload reduction when nitroprusside or nicardipine are unavailable or contraindicated. Evidence quality: low — based on hemodynamic rationale.

Dose

Dosing

Hydralazine dosing is structured by clinical scenario rather than by tablet strength. The drug has a short duration of action (approximately 2–4 hours orally), which mandates 2–4 doses per day for hypertension. For HFrEF, dosing is typically tied to the fixed-dose combination evaluated in A-HeFT.

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Dose	Notes
Essential hypertension — initial titration (oral)	10 mg PO four times daily × 2–4 days	25 mg PO four times daily × 1 week, then 50 mg PO four times daily	200 mg/day usual ceiling; up to 300 mg/day in resistant cases per the FDA label	Take with food at consistent times each day Pair with beta-blocker (controls reflex tachycardia) and a diuretic (controls fluid retention)
Hypertensive emergency / urgency in adults (parenteral, non-pregnant)	10 mg slow IV; max initial dose 20 mg per StatPearls; FDA injection label cites 20–40 mg IV/IM	Repeat every 4–6 hours as needed	Per FDA injection label, certain patients (especially with marked renal damage) require lower doses	BP often falls within minutes; maximal effect at 10–80 min Avoid in suspected aortic dissection (reflex tachycardia worsens shear stress)
Severe acute hypertension in pregnancy (per ACOG)	5–10 mg IV or IM	5–10 mg IV every 20 minutes if BP remains ≥160/110 mmHg	Cumulative 20 mg per ACOG protocol; switch agent if not controlled	Higher and more frequent dosing is associated with maternal hypotension, headaches, and abnormal fetal tracings Continuous fetal monitoring during administration
HFrEF — adjunctive (with isosorbide dinitrate, per A-HeFT / fixed-dose BiDil)	Hydralazine 37.5 mg + ISDN 20 mg PO three times daily	Titrate to hydralazine 75 mg + ISDN 40 mg PO three times daily	Hydralazine 225 mg/day + ISDN 120 mg/day (at the maintenance dose taken three times daily)	BiDil fixed-dose product approved at the maintenance dose; same totals achievable with separate generic tablets Continue background ARNI/ACEi/ARB plus beta-blocker plus MRA plus SGLT2i unless contraindicated
HFrEF — patient intolerant to ACEi/ARB/ARNI (Class 2a, any race)	Hydralazine 25–50 mg + ISDN 20 mg PO three times daily	Hydralazine 75 mg + ISDN 40 mg PO three times daily as tolerated	Hydralazine 225 mg/day + ISDN 120 mg/day	Lower individual-component doses are reasonable when titrating outside the fixed-dose combination A nitrate-free interval is typical to limit nitrate tolerance
Missed dose (oral)	Take as soon as remembered if close to the scheduled time	—	—	If almost time for the next scheduled dose, skip the missed one and resume normal schedule Never double up

Population-Specific Adjustments

Population	Starting Dose	Maintenance Dose	Maximum Dose	Notes
Slow acetylator phenotype (NAT2)	Use lower starting doses	Lower than usual maintenance	Lower ceiling; higher DILE risk	Slow acetylators have approximately twice the AUC of fast acetylators after a single oral dose, with higher steady-state plasma concentrations and a markedly higher risk of drug-induced lupus
Severe renal impairment (CrCl <10 mL/min)	Reduce starting dose or extend interval (e.g., q12–q24 h)	Individualize	Use the lowest effective dose	Reduced clearance and risk of accumulation; titrate slowly and monitor for hypotension
Hepatic impairment	Reduce dose	Individualize	Use the lowest effective dose	Hepatic acetylation is the primary metabolic pathway; impaired clearance increases exposure
Older adults (≥65 y)	Start at the low end of the range	Titrate slowly	As tolerated	Higher risk of orthostatic hypotension and falls; check standing BP
Pediatric oral (off-label, supported by clinical experience)	0.75 mg/kg/day PO divided every 6–12 h	Titrate as needed up to 7.5 mg/kg/day	7.5 mg/kg/day or 200 mg/day (whichever is less)	Per Mayo Clinic patient information and pediatric references; FDA label states safety/efficacy not established in controlled pediatric trials
Pediatric parenteral (hypertensive crisis)	0.1–0.2 mg/kg/dose IV/IM every 4–6 hours PRN	May increase to 1.7–3.5 mg/kg/day in 4–6 divided doses (FDA injection label)	20 mg per dose; 3.5 mg/kg/day	Clinical practice ranges per Medscape and major pediatric formularies; FDA label dose for severe acute hypertension is 1.7–3.5 mg/kg/day

Clinical Pearl — The Three-Drug Pattern

Chronic oral hydralazine for hypertension is rarely prescribed alone. Two predictable physiologic responses — reflex sympathetic activation (tachycardia, palpitations, anginal triggers) and renal sodium retention (edema, blunted antihypertensive effect) — are the reason. Pairing hydralazine with a beta-blocker (or non-dihydropyridine CCB) and a diuretic neutralizes both, and is the regimen that historically delivered sustained BP control. If a patient on hydralazine monotherapy is failing to respond, the answer is usually adding the missing partner drug rather than escalating the hydralazine dose.

Pharmacology

Mechanism of Action

Hydralazine produces direct relaxation of arteriolar smooth muscle, with little to no venous effect. The exact molecular mechanism remains incompletely characterized, but proposed actions include inhibition of inositol trisphosphate (IP3)-induced calcium release from the smooth muscle sarcoplasmic reticulum, interference with myosin light-chain phosphorylation, and contributions from prostaglandin- and nitric oxide-mediated pathways. The net hemodynamic effect is a fall in systemic vascular resistance and afterload.

The arteriolar selectivity has two clinically important consequences. First, hydralazine reduces afterload without preload reduction, which makes it complementary to nitrates (preload reducers) — the rationale behind the H-ISDN combination in HFrEF. Second, the abrupt drop in systemic resistance triggers a baroreceptor-mediated reflex sympathetic response with tachycardia, increased contractility, and renin–angiotensin–aldosterone activation. These compensatory responses can blunt the antihypertensive effect, precipitate angina in patients with coronary disease, and drive sodium and water retention. The standard countermeasures are concurrent therapy with a beta-blocker and a diuretic.

ADME Profile

Parameter	Value	Clinical Implication
Absorption	Rapidly absorbed orally; oral Tmax ~1 hour; bioavailability is highly variable and acetylator-dependent — slow acetylators have approximately twice the AUC of fast acetylators	Wide interpatient variability in exposure; titrate to clinical response rather than dose alone
Distribution	Wide tissue distribution; protein binding ~87%; crosses placenta and is excreted in breast milk	Extensive distribution; pregnancy and lactation considerations apply but the drug is widely used in obstetric care
Metabolism	Hepatic acetylation by N-acetyltransferase 2 (NAT2), with bimodal slow vs fast acetylator phenotypes; additional oxidation and conjugation	NAT2 polymorphism drives both response and toxicity: slow acetylators have higher exposure and substantially greater risk of drug-induced lupus
Elimination	Half-life approximately 3–7 hours (longer in renal impairment); <10% of an oral dose recovered in urine as parent drug; the remainder excreted as metabolites in urine and feces	Short half-life mandates 2–4× daily dosing; renal impairment prolongs duration and amplifies hypotension risk

Side Effects

Most adverse reactions to hydralazine fall into two categories: (1) the predictable consequences of vasodilation and reflex sympathetic activation (headache, palpitations, tachycardia, flushing, hypotension, fluid retention), and (2) immune-mediated reactions from chronic exposure (drug-induced lupus, peripheral neuritis, rare blood dyscrasias, and rare ANCA-associated vasculitis). The FDA prescribing information explicitly notes that systematic frequency data have not been collected for most reactions, so the categorization below combines PI listings with published clinical observations.

≥10% Very Common

Adverse Effect	Incidence	Clinical Note
Headache	Very common precise rate not characterized in PI	Vasodilatory; usually most pronounced early in therapy and improves with continued use; treat with simple analgesia
Palpitations / reflex tachycardia	Very common	Predictable physiologic response; mitigated by concurrent beta-blocker
Anorexia, nausea, vomiting, diarrhea	Very common	Generally mild; taking with food may reduce GI symptoms

1–10% Common

Adverse Effect	Incidence	Clinical Note
Drug-induced lupus erythematosus (DILE)	~5–10% cumulative; dose- and duration-dependent	Higher in slow acetylators, women, prolonged therapy (>6 months), and doses >200 mg/day; rates as high as 10–20% have been reported with cumulative exposure ≥400 mg/day. Most common features are arthralgia, fever, malaise, rash, and serositis. Most cases reverse after discontinuation.
Hypotension / dizziness	Common	Often orthostatic; counsel on slow positional changes; reduce diuretic dose if volume-depleted
Flushing, lacrimation, conjunctivitis, nasal congestion	Common	Mucosal vasodilation; usually self-limited and well-tolerated
Sodium and water retention / peripheral edema	Common	Counter-regulatory response to vasodilation; routinely managed by concomitant diuretic
Peripheral neuritis (paresthesia, numbness)	Uncommon to common	Antipyridoxine effect described in the FDA PI; pyridoxine (vitamin B6) supplementation usually reverses symptoms

Serious Serious — Regardless of Frequency

Adverse Effect	Estimated Frequency	Typical Onset	Required Action
Hydralazine-induced lupus syndrome with glomerulonephritis	Rare subset of DILE	Months to years; usually with prolonged or high-dose therapy	Discontinue hydralazine; rheumatology and nephrology consultation; long-term steroid therapy may be required per FDA PI
Angina or myocardial infarction (in coronary artery disease)	Uncommon overall; higher with monotherapy in CAD	Hours to days	Discontinue; standard ACS workup and management; avoid hydralazine monotherapy in known CAD
ANCA-positive vasculitis	Rare	Months to years	Discontinue; rheumatology referral; immunosuppression often required
Blood dyscrasias (hemolytic anemia, leukopenia, thrombocytopenia, agranulocytosis)	Rare	Weeks to months	Discontinue; CBC and reticulocyte count; hematology referral; usually reversible after withdrawal
Severe hypotension (especially parenteral; in volume-depleted or renally impaired patients)	Uncommon	Minutes (parenteral) to hours (oral)	Position supine; IV fluids; per FDA PI, vasopressors should be avoided if possible — if required, use with caution to avoid worsening tachyarrhythmia
Hypersensitivity reactions (rash, urticaria, anaphylaxis)	Rare	Any time	Discontinue permanently; standard hypersensitivity management; document allergy

Discontinuation Drug Discontinuation Considerations

Adults

Variable

Top reasons: headache, palpitations, GI upset, dose-related lupus-like symptoms, fluid retention not controlled by diuretic. Pooled discontinuation rates are not reported in a standardized way in the FDA PI.

Pediatric

Limited data

Use is largely off-label and based on clinical experience; tolerability follows the adult pattern.

Reason for Discontinuation	Incidence	Context
Drug-induced lupus / positive ANA with symptoms	Uncommon	Resolves in most patients within weeks of stopping; corticosteroids occasionally required
Headache and palpitations	Common reason	Often dose-related and may improve with concurrent beta-blocker
Worsening angina or new ischemic symptoms	Uncommon	Reflex tachycardia in CAD; switch to a non-stimulating antihypertensive class
Refractory fluid retention	Uncommon	Usually resolves with diuretic optimization rather than drug discontinuation

Management Focus — Recognizing Drug-Induced Lupus

Hydralazine-induced lupus presents most often as arthralgia or polyarthritis, low-grade fever, malaise, and a positive ANA, frequently with anti-histone antibodies; however, hydralazine is also an unusually common cause of drug-induced ANCA-associated vasculitis (often anti-MPO). Renal and CNS involvement, classic of idiopathic SLE, are less common. Risk factors include cumulative dose >200 mg/day, duration >6 months, female sex, and slow acetylator phenotype. Stop hydralazine, document the reaction in the chart, and avoid rechallenge. Serologies usually normalize over weeks to months; corticosteroids are reserved for severe organ involvement.

Int

Drug Interactions

Most clinically important hydralazine interactions are pharmacodynamic — additive hypotension with other vasodilators, or antagonism by sodium-retaining agents. Hydralazine is not a major substrate of CYP enzymes; clearance is dominated by hepatic acetylation, so CYP-based interactions are not a typical concern.

Major MAO inhibitors (phenelzine, tranylcypromine, selegiline, linezolid, isocarboxazid)

MechanismPharmacodynamic — potential exaggerated hypotensive response or unpredictable BP effects

EffectVariable; the FDA label specifies caution rather than absolute contraindication

ManagementPer FDA PI, “MAO inhibitors should be used with caution in patients receiving hydralazine”; close BP monitoring; consider an alternative antihypertensive when feasible

FDA PI

Major Diazoxide

MechanismPharmacodynamic synergy of two arteriolar vasodilators

EffectMarked, potentially severe hypotension

ManagementAvoid concurrent use; if both required, hospital monitoring

Lexicomp

Moderate Other antihypertensives (ACEi, ARB, CCB, beta-blockers, diuretics, alpha-blockers)

MechanismAdditive lowering of systemic BP

EffectIncreased symptomatic hypotension during titration; clinically intentional in most regimens

ManagementMost combinations are intended (especially beta-blocker + diuretic); stagger dose changes; check standing BP

Clinical experience

Moderate Nitrates (isosorbide dinitrate, isosorbide mononitrate, nitroglycerin)

MechanismAdditive vasodilation; clinically synergistic — hydralazine appears to attenuate nitrate tolerance

EffectAdditive hypotension; in HFrEF, intentional combination provides mortality benefit (A-HeFT)

ManagementIntentional combination in HFrEF (BiDil); monitor BP closely; counsel patients on orthostatic precautions

FDA PI / A-HeFT

Moderate PDE-5 inhibitors (sildenafil, tadalafil, vardenafil)

MechanismAdditive vasodilation; concern is greater when patient is also on nitrates

EffectIncreased hypotension risk

ManagementUse caution; PDE-5 inhibitors are absolutely contraindicated with concurrent nitrates, including the H-ISDN combination

Lexicomp

Moderate NSAIDs (ibuprofen, naproxen, indomethacin)

MechanismNSAIDs reduce prostaglandin-mediated vasodilation and promote sodium retention

EffectReduced antihypertensive effect of hydralazine

ManagementLimit chronic NSAID exposure when possible; monitor BP if combination is unavoidable

Lexicomp / Medscape

Moderate Sympathomimetics (pseudoephedrine, phenylephrine, amphetamines, epinephrine)

MechanismVasoconstriction antagonizes vasodilator effect; may also induce angina in CAD

EffectReduced BP control; risk of anginal pain

ManagementCounsel patients to avoid OTC decongestants; monitor BP if unavoidable

Medscape / Lexicomp

Minor Beta-blockers (metoprolol, propranolol)

MechanismHydralazine may modestly increase the bioavailability of some beta-blockers (immediate-release propranolol, metoprolol); pharmacodynamically, beta-blockers blunt hydralazine-induced reflex tachycardia

EffectGenerally beneficial — combination is therapeutically intended

ManagementNo specific dose change required; monitor heart rate and BP

PK literature / clinical practice

Minor Alcohol

MechanismAdditive vasodilation

EffectIncreased orthostatic hypotension

ManagementCounsel on moderation; advise sitting before standing; avoid heavy intake

Clinical experience

Mon

Monitoring

Monitoring on hydralazine has two distinct rhythms: a short-term focus on hemodynamic tolerance during dose titration, and a long-term surveillance program for drug-induced autoimmune phenomena.

Blood Pressure & Heart Rate Each visit during titration; periodically thereafter
Routine Check seated and standing BP. Watch for reflex tachycardia >90 bpm at rest, which often signals the need for a beta-blocker. For parenteral dosing, monitor BP frequently until stable.
CBC & Antinuclear Antibody (ANA) Baseline; periodically during prolonged therapy
Routine FDA PI specifies ANA and CBC determinations before therapy and periodically during prolonged use, even in asymptomatic patients. Repeat with new arthralgia, fever, chest pain, malaise, or other unexplained symptoms. A rising ANA without symptoms does not always require discontinuation, but warrants closer follow-up.
Renal Function (creatinine, urinalysis) Baseline; with routine HF/HTN labs
Routine Surveillance for hydralazine-associated glomerulonephritis (rare DILE complication) and for confirming safe dosing in declining renal function. New proteinuria or active urinary sediment merits prompt evaluation.
Symptoms of DILE Each visit; structured screen at 6, 12 months and annually
Routine Ask specifically about new joint pain or stiffness, low-grade fever, unusual fatigue, rashes, pleuritic chest pain, and serositis-type symptoms. Classic onset is after several months of therapy on doses ≥200 mg/day.
Volume Status / Edema Each visit
Routine Reflex sodium and water retention can blunt antihypertensive effect; check daily weights in HF patients and adjust diuretic before adding more antihypertensive load.
Peripheral Sensory Symptoms As needed
Trigger-based Numbness, tingling, or paresthesia suggest pyridoxine deficiency. Trial of vitamin B6 supplementation usually relieves symptoms; persistent neuritis warrants further workup.
ECG / Cardiac Symptoms As needed
Trigger-based Re-evaluate if new chest pain, worsening angina, or pronounced tachycardia. Caution in patients with known coronary disease or recent MI; reflex sympathetic activation can precipitate ischemia.
Fetal Heart Rate (during obstetric use) Continuous during parenteral dosing
Trigger-based Maternal hypotension after IV hydralazine has been associated with abnormal fetal tracings; intravenous fluid pre-loading and slow administration reduce this risk.

Contraindications & Cautions

FDA Class-Wide Regulatory Warning Drug-Induced Lupus Erythematosus and Coronary Stimulation

The FDA prescribing information for hydralazine carries explicit warnings on two issues clinicians must internalize. First, hydralazine may produce a clinical syndrome resembling systemic lupus erythematosus, including glomerulonephritis; symptoms typically regress on discontinuation but residua may persist for years and long-term steroid therapy may be required. Second, myocardial stimulation produced by hydralazine can precipitate anginal attacks and ECG changes of myocardial ischemia; the drug has been associated with myocardial infarction and should be used with caution in patients with suspected coronary artery disease.

Complete blood counts and antinuclear antibody titer determinations should be obtained before initiating prolonged therapy and periodically during treatment, even in asymptomatic patients.

Absolute Contraindications

Hypersensitivity to hydralazine
Coronary artery disease — listed as a contraindication in the FDA parenteral (IV) label; the oral label warns against monotherapy in CAD because of reflex tachycardia
Mitral valvular rheumatic heart disease — listed as a contraindication in the FDA parenteral label; afterload reduction can worsen hemodynamics in mitral stenosis

Relative Contraindications (Specialist Input Recommended)

Suspected aortic dissection — reflex tachycardia and increased shear stress are detrimental; agents such as labetalol or esmolol (with nitroprusside if needed) are preferred
Severe renal impairment (CrCl <10 mL/min) — reduced clearance and increased exposure; reduce dose or extend interval
Pre-existing autoimmune disease (especially SLE) — risk of flare; use only if alternatives are unavailable and with rheumatology input
Slow acetylator phenotype with prior reactions or family history of DILE — markedly elevated risk of drug-induced lupus
Increased intracranial pressure (parenteral use) — abrupt BP lowering may worsen cerebral perfusion per the FDA injection label

Use with Caution

Older adults — higher risk of orthostatic hypotension and falls; titrate slowly; check standing BP at each visit
Pulmonary hypertension — reflex tachycardia and unpredictable hemodynamic effects; use only with specialist input
Concurrent NSAID use — sodium retention may blunt antihypertensive effect; reassess if BP control is inadequate
Patients with anginal symptoms — co-administration of a beta-blocker is essential to control reflex tachycardia
Pregnancy — although IV hydralazine is widely used for severe acute hypertension in pregnancy, animal studies showed teratogenicity (cleft palate, craniofacial malformations) at exposures many times the maximum daily human dose; chronic oral use during pregnancy should be carefully weighed against alternatives such as labetalol or extended-release nifedipine
Lactation — hydralazine is excreted in breast milk; clinical experience supports use during breastfeeding when needed, but observe the infant for unusual sedation, feeding difficulty, or hypotension

Pregnancy & Lactation Detail

Hydralazine has a long history of use in obstetric care. ACOG includes IV hydralazine among first-line agents (with IV labetalol and oral immediate-release nifedipine) for severe acute hypertension in pregnancy and the postpartum period, with a recommended cumulative IV ceiling of 20 mg before switching agents. Animal teratogenicity has been observed at high doses, but extensive clinical experience in obstetric care does not demonstrate adverse fetal effects with therapeutic short-term use. Hydralazine is excreted in breast milk in small amounts and is generally considered compatible with breastfeeding; the infant should still be observed for unusual sedation, feeding difficulty, or hypotension.

Patient Counselling

Purpose of Therapy

Frame hydralazine as a blood pressure-lowering medicine that works by relaxing the arteries and reducing the workload on the heart. For patients with heart failure, the combination with a long-acting nitrate (isosorbide dinitrate) has additional benefits for symptoms and survival, especially in patients of African-American background or in those who cannot tolerate the standard heart failure medicines (ACE inhibitors, ARBs, or ARNI). The drug controls blood pressure rather than curing the underlying condition; benefits accrue with consistent daily use.

How to Take

Hydralazine is taken by mouth two to four times each day, depending on the prescribed dose. Take it at the same times every day, and try to take it with meals or a snack to reduce nausea. Patients should not change or stop their dose without instruction from the prescriber, as abrupt withdrawal can cause rebound rises in blood pressure. Most early side effects (headache, palpitations, mild dizziness) settle as the body adjusts.

Headache, Palpitations, and Lightheadedness

Tell patient Most common in the first weeks. Stand up slowly, especially first thing in the morning. Stay well-hydrated unless on a fluid restriction. Episodes typically settle as the body adjusts.

Call prescriber If headache is severe and not relieved by simple analgesia, if you actually faint or fall, or if a racing heartbeat is constant or comes with chest pain.

Joint Pain, Fever, or Rash After Months of Use

Tell patient This medicine can occasionally cause a lupus-like reaction with joint pain, low-grade fever, rash, or unusual tiredness. It is uncommon but important to recognize. Symptoms usually appear after several months of treatment.

Call prescriber If new joint pain, persistent fever, unusual rash, breathing pain, or swelling develops. The team can run blood tests and decide whether to stop the medicine.

Numbness or Tingling in Hands or Feet

Tell patient Some patients on long-term hydralazine notice tingling or pins-and-needles sensations. This is often related to vitamin B6 deficiency caused by the drug and is usually corrected with a B6 (pyridoxine) supplement.

Call prescriber If numbness or tingling persists, gets worse, or affects daily activities. The team may add a vitamin B6 supplement or reassess the dose.

Fluid Retention and Weight Gain

Tell patient Hydralazine can cause the body to hold on to extra salt and water, sometimes leading to swollen ankles or weight gain. A water pill (diuretic) is often prescribed alongside to manage this.

Call prescriber If you gain more than 1–2 kg in a few days, your shoes feel tight, or your breathing worsens with normal activity.

Chest Pain or Worsening Angina

Tell patient If you have heart-related chest pain (angina), let your team know — this medicine can sometimes make angina worse. It is usually combined with a heart-rate-controlling medicine (a beta-blocker) to prevent this.

Call prescriber For new chest pain, pain that lasts more than a few minutes, or if your usual angina pattern changes. Call emergency services for severe or sudden chest pain.

Over-the-Counter Medicines

Tell patient Avoid over-the-counter cold and flu medicines containing pseudoephedrine or phenylephrine — these can raise blood pressure and counteract hydralazine. Ibuprofen, naproxen, and similar painkillers can also reduce its effectiveness when used regularly. Always check with the pharmacist before starting any new OTC medication.

Call prescriber If you need a regular pain medicine for arthritis or back pain, the team can suggest an alternative such as paracetamol that does not interfere.

Missed Dose

Tell patient Take the missed dose as soon as you remember. If it is almost time for the next dose, skip the missed one and continue your usual schedule. Never take two doses at the same time to make up.

Call prescriber If multiple doses are missed in a row, before any planned hospital stay, or before any procedure where you will be unable to take oral medications.

Storage & Travel

Tell patient Store tablets at room temperature in the original container, away from heat and moisture. When travelling, carry a written list of all medicines and a few extra days’ supply.

Call prescriber If running short before a refill is possible, or if travelling for an extended period.

Ref

Sources

Regulatory (PI / SmPC)

U.S. Food and Drug Administration. Apresoline (hydralazine hydrochloride) tablets — prescribing information. accessdata.fda.gov/drugsatfda_docs/label/1996/008303s068lbl.pdf FDA-approved oral hydralazine label including indication, dosing, adverse reaction listings, and the warnings on lupus-like syndrome and coronary stimulation.
U.S. Food and Drug Administration. Hydralazine hydrochloride injection — prescribing information. accessdata.fda.gov/drugsatfda_docs/label/2013/040136s005lbl.pdf FDA-approved parenteral label specifying the contraindications (CAD, mitral valvular rheumatic heart disease) and the dosing for severe acute hypertension.
U.S. Food and Drug Administration. BiDil (isosorbide dinitrate / hydralazine hydrochloride) — prescribing information. NDA 020727 (approval 2005). accessdata.fda.gov — NDA 020727 FDA approval record for the fixed-dose H-ISDN combination, with maintenance dosing of 37.5 mg/20 mg three times daily titrated up to 75 mg/40 mg three times daily.

Key Clinical Trials

Taylor AL, Ziesche S, Yancy C, et al; African-American Heart Failure Trial Investigators. Combination of isosorbide dinitrate and hydralazine in blacks with heart failure. N Engl J Med. 2004;351(20):2049–2057. doi.org/10.1056/NEJMoa042934 A-HeFT — pivotal trial showing a mortality and hospitalization benefit of fixed-dose H-ISDN added to standard therapy in self-identified African-American patients with HFrEF.
Cohn JN, Archibald DG, Ziesche S, et al. Effect of vasodilator therapy on mortality in chronic congestive heart failure: results of a Veterans Administration Cooperative Study. N Engl J Med. 1986;314(24):1547–1552. doi.org/10.1056/NEJM198606123142404 V-HeFT I — first trial demonstrating a survival benefit of H-ISDN over placebo in chronic heart failure.
Cohn JN, Johnson G, Ziesche S, et al. A comparison of enalapril with hydralazine-isosorbide dinitrate in the treatment of chronic congestive heart failure. N Engl J Med. 1991;325(5):303–310. doi.org/10.1056/NEJM199108013250502 V-HeFT II — found enalapril superior to H-ISDN in overall survival but with similar mortality in self-identified Black participants, foundation for the racial subgroup hypothesis.
Carson P, Ziesche S, Johnson G, Cohn JN; Vasodilator-Heart Failure Trial Study Group. Racial differences in response to therapy for heart failure: analysis of the vasodilator-heart failure trials. J Card Fail. 1999;5(3):178–187. doi.org/10.1016/S1071-9164(99)90001-5 Post-hoc V-HeFT analysis identifying differential H-ISDN response in self-identified Black patients — the rationale that prompted A-HeFT.

Guidelines

Heidenreich PA, Bozkurt B, Aguilar D, et al. 2022 AHA/ACC/HFSA Guideline for the Management of Heart Failure. Circulation. 2022;145(18):e895–e1032. doi.org/10.1161/CIR.0000000000001063 Class 1 recommendation for fixed-dose H-ISDN in self-identified African-American patients with NYHA III–IV HFrEF on optimal GDMT; Class 2a recommendation in any race intolerant to ACEi/ARB/ARNI.
Whelton PK, Carey RM, Aronow WS, et al. 2017 ACC/AHA/AAPA/ABC/ACPM/AGS/APhA/ASH/ASPC/NMA/PCNA Guideline for the Prevention, Detection, Evaluation, and Management of High Blood Pressure in Adults. Hypertension. 2018;71(6):e13–e115. doi.org/10.1161/HYP.0000000000000065 U.S. hypertension guideline framework that places hydralazine as a secondary agent for resistant hypertension.
American College of Obstetricians and Gynecologists. ACOG Practice Bulletin No. 222: Gestational Hypertension and Preeclampsia. Obstet Gynecol. 2020;135(6):e237–e260. doi.org/10.1097/AOG.0000000000003891 Practice Bulletin that incorporates ACOG Committee Opinion No. 767, designating IV hydralazine, IV labetalol, and oral immediate-release nifedipine as first-line for severe acute hypertension in pregnancy and the postpartum period (with a 20 mg cumulative IV hydralazine ceiling).

Mechanistic / Basic Science

Cole RT, Kalogeropoulos AP, Georgiopoulou VV, et al. Hydralazine and isosorbide dinitrate in heart failure: historical perspective, mechanisms, and future directions. Circulation. 2011;123(21):2414–2422. doi.org/10.1161/CIRCULATIONAHA.110.012781 Comprehensive mechanistic review covering arteriolar vasodilation, nitric oxide modulation, attenuation of nitrate tolerance, and racial differences in response.
Solhjoo M, Goyal A, Chauhan K. Drug-induced lupus erythematosus. StatPearls. Updated 2023. ncbi.nlm.nih.gov/books/NBK441889 Authoritative review of drug-induced lupus syndromes including hydralazine, with risk-factor profiles (slow acetylator, female sex, dose >200 mg/day, duration >6 months) and management.

Pharmacokinetics / Special Populations

Herman LL, Bashir K. Hydralazine. StatPearls. Updated 2023. ncbi.nlm.nih.gov/books/NBK470296 Up-to-date overview of hydralazine pharmacology, dosing, monitoring, and toxicity with emphasis on acetylator phenotype variability.
Ludden TM, McNay JL, Shepherd AM, Lin MS. Clinical pharmacokinetics of hydralazine. Clin Pharmacokinet. 1982;7(3):185–205. doi.org/10.2165/00003088-198207030-00001 Detailed PK review covering bioavailability, acetylator phenotype effect on exposure, half-life, first-pass metabolism, and dosing implications.
Reece PA, Cozamanis I, Zacest R. Pharmacokinetics of hydralazine and its acid-labile hydrazone metabolites in relation to acetylator phenotype. J Pharmacokinet Biopharm. 1980;8(3):261–272. doi.org/10.1007/BF01059448 Foundational study showing that slow acetylators have approximately twice the AUC of fast acetylators after oral hydralazine — the empirical basis for acetylator-aware dosing.