Trastuzumab: Complete Drug Monograph & Prescribing Guide

Pharmacokinetic Profile

Half-Life

~28 days

Metabolism

Intracellular catabolism (RES)

Protein Binding

N/A (monoclonal Ab)

Volume of Distribution

~44 mL/kg (~2.95 L central)

Clearance

0.225 L/day (linear CL)

Clinical Information

Drug Class

HER2-directed monoclonal antibody

Available Forms

150 mg lyophilised vial

Route

IV infusion only

Renal Adjustment

None required (mild-mod)

Hepatic Adjustment

Not studied

Pregnancy

Contraindicated (Boxed Warning)

Lactation

Avoid; 7-month washout

Black Box Warning

Yes — 4 warnings

Biosimilars Available

Yes (multiple approved)

Indications for Trastuzumab

Indication	Approved Population	Therapy Type	Status
HER2-overexpressing breast cancer — adjuvant	Adults; node-positive or node-negative with high-risk features (ER/PR-negative, or ≥1 high-risk feature)	Combination with AC→T, TCH, or single-agent post-anthracycline	FDA Approved
HER2-overexpressing metastatic breast cancer — first-line	Adults	Combination with paclitaxel	FDA Approved
HER2-overexpressing metastatic breast cancer — previously treated	Adults who received ≥1 prior chemo regimen for metastatic disease	Monotherapy	FDA Approved
HER2-overexpressing metastatic gastric / GEJ adenocarcinoma	Adults; previously untreated metastatic disease	Combination with cisplatin + capecitabine or 5-FU	FDA Approved

Trastuzumab fundamentally changed the treatment landscape for HER2-positive cancers following its landmark approval in 1998. It was among the first targeted biologic therapies and remains a backbone of HER2-directed treatment in both early-stage and advanced settings. Patient selection requires confirmed HER2 overexpression (IHC 3+ or IHC 2+ with FISH amplification) using an FDA-approved companion diagnostic performed by a laboratory with demonstrated proficiency.

Off-Label Uses

HER2-positive esophageal / esophagogastric junction cancer — used in combination with chemotherapy, supported by NCCN guidelines. Evidence quality: Moderate.

HER2-positive uterine serous carcinoma — in combination with carboplatin and paclitaxel, with maintenance monotherapy. Evidence quality: Moderate (based on a randomised phase II trial).

HER2-amplified, RAS/BRAF wild-type colorectal cancer — in combination with pertuzumab or other HER2-targeted agents. Evidence quality: Moderate.

Intra-CSF trastuzumab for leptomeningeal carcinomatosis — used in HER2-positive breast cancer with CNS involvement. Evidence quality: Low (case series and small prospective studies).

Dose

Dosing for Trastuzumab

Adult Dosing by Clinical Scenario

Clinical Scenario	Starting Dose (Loading)	Maintenance Dose	Maximum Dose	Notes
Early breast cancer — adjuvant, weekly schedule (with taxane phase)	4 mg/kg IV over 90 min	2 mg/kg IV over 30 min weekly during chemo (12–18 wk), then 6 mg/kg IV q3wk	52 weeks total	Weekly during paclitaxel (12 wk) or docetaxel/carboplatin (18 wk), then q3wk to complete 1 year Do not extend beyond 52 weeks (no added benefit, more toxicity)
Early breast cancer — adjuvant, q3-weekly schedule (post-anthracycline single agent)	8 mg/kg IV over 90 min	6 mg/kg IV over 30–90 min q3wk	52 weeks total	Used when given as single agent following completion of multi-modality anthracycline-based chemotherapy
Metastatic breast cancer — first-line or beyond (with or without paclitaxel)	4 mg/kg IV over 90 min	2 mg/kg IV over 30 min weekly	Until progression	Continue until disease progression or unacceptable toxicity Paclitaxel given concurrently at 175 mg/m² q3wk when used in combination
Metastatic gastric / GEJ adenocarcinoma — first-line	8 mg/kg IV over 90 min	6 mg/kg IV over 30–90 min q3wk	Until progression	Given with cisplatin 80 mg/m² + capecitabine or 5-FU; chemotherapy for 6 cycles, trastuzumab continues Steady-state exposure is lower in gastric cancer vs. breast cancer at same dose

Missed Dose Management

Clinical Scenario	Starting Dose (Re-loading)	Maintenance Dose	Maximum Dose	Notes
Missed dose ≤1 week (weekly schedule)	Not required	2 mg/kg as soon as possible	N/A	Resume usual maintenance; next dose 7 days later
Missed dose >1 week (weekly schedule)	4 mg/kg IV over 90 min	2 mg/kg weekly thereafter	N/A	Re-load required due to long washout kinetics
Missed dose >1 week (q3wk schedule)	8 mg/kg IV over 90 min	6 mg/kg q3wk thereafter	N/A	Re-load required; resume 21-day cycle from re-load date

Clinical Pearl: Dose Modifications for Cardiomyopathy

Withhold trastuzumab for at least 4 weeks if LVEF decreases ≥16% absolute from baseline, or falls below institutional normal limits with ≥10% absolute decrease. Trastuzumab may be resumed if LVEF recovers to normal limits and the absolute decrease from baseline is ≤15% within 4–8 weeks. Permanently discontinue if LVEF decline persists >8 weeks or if dosing has been held for cardiomyopathy more than 3 times (FDA PI).

Pharmacology of Trastuzumab

Mechanism of Action

Trastuzumab is a recombinant humanised IgG1 kappa monoclonal antibody that binds with high affinity to subdomain IV of the extracellular domain of the human epidermal growth factor receptor 2 (HER2/ErbB2). HER2 is a transmembrane tyrosine kinase receptor that, when overexpressed, drives tumour cell proliferation through activation of the PI3K/AKT and RAS/MAPK signalling cascades. By binding HER2, trastuzumab blocks receptor dimerisation and downstream signalling, leading to cell cycle arrest primarily through upregulation of the cyclin-dependent kinase inhibitor p27^Kip1. Trastuzumab also mediates antibody-dependent cellular cytotoxicity (ADCC), recruiting natural killer cells and macrophages to lyse HER2-overexpressing tumour cells. This dual mechanism — signal blockade plus immune-mediated killing — accounts for its selective activity against HER2-amplified cancers while largely sparing normal tissues that express low basal levels of HER2.

ADME Profile

Parameter	Value	Clinical Implication
Absorption	IV only; 100% bioavailability; Cmax at end of infusion; steady state reached by week 12 (q3wk) or week 16–32 (weekly)	First infusion given over 90 minutes; subsequent infusions may be shortened to 30 minutes if tolerated
Distribution	Vd ~44 mL/kg (~2.95 L central compartment); does not cross the blood-brain barrier in appreciable concentrations	Limited CNS penetration explains poor activity against brain metastases; intrathecal delivery explored investigationally
Metabolism	Target-mediated disposition: HER2 binding → intracellular lysosomal degradation to peptides and amino acids; parallel non-specific IgG clearance via reticuloendothelial system. No CYP450 involvement	No hepatic enzyme-based drug interactions; clearance increases with higher tumour burden (more HER2 antigen sink)
Elimination	t½ ~28 days; total CL 0.173–0.337 L/day at steady state; renal excretion minimal; ~97% washout by 7 months	7-month washout period relevant for: (1) contraception duration after stopping, (2) timing of anthracycline use post-trastuzumab

Pharmacokinetic Variability

Trastuzumab exhibits nonlinear, dose-dependent kinetics owing to target-mediated drug disposition. Patients with higher tumour burden and more metastatic sites show increased clearance and lower serum trough concentrations. Increased body weight and reduced serum albumin are also associated with higher clearance, though these effects are modest compared with overall interpatient variability (~43% CV).

Side Effects of Trastuzumab

≥10% Very Common

Adverse Effect	Incidence	Clinical Note
Fever / chills (infusion-related)	~40% (first infusion)	Most common with first dose; drops to 21–35% on subsequent infusions; managed with paracetamol and diphenhydramine pre-medication
Headache	10–36%	More common in combination therapy; usually mild and self-limiting
Nausea	33% (monotherapy)	Higher rates when combined with AC chemotherapy (≥76%); anti-emetic regimen guided by chemotherapy backbone
Fatigue / asthenia	35–62%	Dose-related in combination regimens; counsel about activity pacing
Diarrhoea	25–45%	Increased in combination with paclitaxel; monitor hydration
Infection	20–47%	Upper respiratory tract most common; increased with chemotherapy; febrile neutropenia up to 23% with myelosuppressive chemo
Cough / dyspnoea	22–43%	Usually mild; must be distinguished from pulmonary toxicity (see Serious tier)
Rash	18–38%	Higher with paclitaxel combination; usually mild, treat symptomatically
Pain (including tumour-site pain)	47–62%	Generalised body pain; more frequent in metastatic setting
Insomnia	14–29%	Higher in combination with AC

1–10% Common

Adverse Effect	Incidence	Clinical Note
Arthralgia / myalgia	6–8% (adjuvant)	More common in combination with taxanes
Peripheral oedema	5–10%	Differentiate from fluid retention due to cardiac dysfunction
Hypertension	4%	Monitor blood pressure at each cycle
Ejection fraction decrease (asymptomatic)	3.5–8.6%	Requires serial LVEF monitoring; see cardiac monitoring protocol
Nail disorders	2%	Higher frequency with taxane combination (up to 11.5%)
Constipation / dyspepsia	2%	Usually mild; manage symptomatically
Paresthesia	2–9%	Differentiate from taxane-related neuropathy

Serious Serious Adverse Effects (Regardless of Frequency)

Adverse Effect	Estimated Frequency	Typical Onset	Required Action
Cardiomyopathy / CHF (NYHA III–IV)	0.4–4% (adjuvant); 4–19% (metastatic with AC)	Weeks to months; highest risk during concurrent anthracycline	Withhold or permanently discontinue based on LVEF decline criteria; cardiology consultation; initiate heart failure treatment
Severe infusion reactions (anaphylaxis, angioedema, bronchospasm)	<1% (severe); fatal events reported post-marketing	During or within 24 hours of infusion; variable onset	Stop infusion immediately; administer epinephrine, corticosteroids, bronchodilators as indicated; permanently discontinue for severe reactions
Pulmonary toxicity (interstitial pneumonitis, ARDS, pulmonary fibrosis)	0.2–0.7%	Variable; may be acute (infusion-related) or subacute	Permanently discontinue; initiate corticosteroids; pulmonology consultation; rule out infection
Embryo-fetal toxicity (oligohydramnios)	Reported in post-marketing; frequency not quantified	Any trimester	Verify pregnancy status before treatment; effective contraception during and for 7 months after last dose
Febrile neutropenia	5% (gastric); up to 23% with myelosuppressive chemotherapy	During chemotherapy phase	G-CSF support; antimicrobial therapy; hold chemotherapy as indicated
Nephrotic syndrome / glomerulopathy	Rare (post-marketing)	4–18 months	Discontinue trastuzumab; nephrology referral; renal biopsy may be indicated
Tumour lysis syndrome	Very rare (post-marketing)	First cycles; risk highest with bulky disease	Monitor uric acid, phosphate, potassium, calcium; aggressive hydration; rasburicase if indicated

Discontinuation Discontinuation Rates

Adjuvant Breast Cancer (NSABP B31)

15% cardiac-related d/c

Primary reason: Clinical myocardial dysfunction or significant LVEF decline at 8.7 years median follow-up

Adjuvant (HERA, 1-year arm)

2.6% cardiac-related d/c

Primary reason: Cardiac toxicity at 12.6 months median follow-up

Reason for Discontinuation	Incidence	Context
Cardiac dysfunction / LVEF decline	2.6–15%	Highest in AC→TH regimen (NSABP B31); lower in non-anthracycline regimens (TCH ~2.9%)
Severe infusion reactions	<1%	Most patients successfully re-treated with premedication; rare permanent d/c
Pulmonary toxicity	<1%	Interstitial pneumonitis, ARDS
Infection (metastatic gastric)	~2%	In combination with cisplatin/fluoropyrimidine (ToGA)

Cardiotoxicity Management

Trastuzumab-related cardiomyopathy is generally reversible with early detection and treatment. In the NSABP B31 long-term follow-up, approximately 24% of patients who developed CHF recovered to a normal LVEF (≥50%) with ongoing medical management. The risk is substantially lower when trastuzumab is combined with non-anthracycline regimens (TCH: CHF rate 0.4% vs. AC→TH: 2%). Consider TCH over AC→TH for patients with borderline cardiac function or additional cardiovascular risk factors.

Int

Drug Interactions with Trastuzumab

Trastuzumab does not undergo hepatic metabolism via cytochrome P450 enzymes, and no formal drug interaction studies have identified clinically significant pharmacokinetic interactions with chemotherapy agents used in combination. Interaction concerns are primarily pharmacodynamic, centred on additive cardiotoxicity with other cardiotoxic agents.

Major Anthracyclines (doxorubicin, epirubicin)

MechanismAdditive cardiotoxicity; trastuzumab impairs HER2-mediated cardiac repair, while anthracyclines cause direct oxidative myocyte damage

Effect4–6-fold increase in symptomatic cardiac dysfunction (CHF up to 28% with concurrent AC vs. 7% with AC alone)

ManagementNever give concurrently; use sequential dosing (anthracycline first, then trastuzumab). Avoid anthracyclines for ≥7 months after stopping trastuzumab. Monitor LVEF closely.

FDA PI · NSABP B31

Major Belimumab

MechanismAdditive immunosuppression

EffectIncreased risk of severe neutropenia and infection

ManagementAvoid co-administration

Lexicomp

Moderate Myelosuppressive Chemotherapy (general)

MechanismTrastuzumab exacerbates chemotherapy-induced neutropenia

EffectIncreased incidence of Grade 3–4 neutropenia and febrile neutropenia (e.g., 32% vs. 22% for NCI-CTC Grade 3/4 neutropenia in metastatic breast cancer trials)

ManagementMonitor CBCs closely; G-CSF support per institutional guidelines; no dose adjustment of trastuzumab needed

FDA PI

Moderate Live Vaccines

MechanismImmunosuppression from concurrent chemotherapy may lead to inadequate immune response or risk of vaccine-induced infection

EffectPotential for disseminated vaccine infection or reduced vaccine efficacy

ManagementAvoid live vaccines during treatment and until immune recovery; inactivated vaccines are preferred

General oncology guidelines

Minor Paclitaxel / Docetaxel / Carboplatin

MechanismNo pharmacokinetic interaction identified in formal studies

EffectNo alteration in plasma concentrations of either agent

ManagementStandard combination; no dose modification required for PK reasons

FDA PI

Minor Cisplatin / Capecitabine / 5-FU

MechanismNo pharmacokinetic interaction identified (ToGA substudy)

EffectNo alteration of cisplatin, capecitabine, or metabolite concentrations

ManagementStandard gastric cancer combination; no dose modification

FDA PI · ToGA

Mon

Monitoring for Trastuzumab

LVEF (echo or MUGA) Baseline, then every 3 months during treatment, and every 6 months for ≥2 years after completion
Routine The most critical monitoring parameter. Withhold for ≥16% absolute decrease from baseline, or LVEF below institutional limits with ≥10% absolute decrease. Repeat LVEF at 4-week intervals during holds.
HER2 Status Before treatment initiation
Routine Confirm HER2 overexpression (IHC 3+ or IHC 2+/FISH-amplified) via FDA-approved companion diagnostic. IHC 2+ alone requires FISH or CISH confirmation.
Pregnancy Status Before treatment initiation
Routine Verify pregnancy status in females of reproductive potential prior to first dose. Counsel regarding contraception during and for 7 months after treatment.
Vital Signs (during infusion) Every infusion; especially first infusion
Routine Monitor for infusion reactions: fever, chills, dyspnoea, hypotension. First infusion given over 90 minutes with 60-minute post-infusion observation.
CBC with Differential Per chemotherapy schedule
Routine Trastuzumab exacerbates chemotherapy-induced neutropenia. Monitor for febrile neutropenia, especially with anthracycline-based regimens.
Signs of Heart Failure Each cycle & as symptoms arise
Trigger-based Assess for dyspnoea on exertion, orthopnoea, peripheral oedema, weight gain, or new-onset cough. Obtain urgent LVEF and cardiology review if symptomatic CHF suspected.
Respiratory Symptoms Each cycle & as symptoms arise
Trigger-based Promptly investigate new cough, dyspnoea, or hypoxia to rule out interstitial pneumonitis or ARDS. CT chest and pulmonology consultation if suspected.
Renal Function If proteinuria develops
Trigger-based Rare cases of nephrotic syndrome reported (onset 4–18 months). Monitor urinalysis if clinically indicated; nephrology referral for significant proteinuria.

Contraindications & Cautions for Trastuzumab

Absolute Contraindications

Pregnancy — Boxed warning for embryo-fetal toxicity. Oligohydramnios, pulmonary hypoplasia, skeletal abnormalities, and neonatal death have been reported.
Prior severe hypersensitivity reaction to trastuzumab — including anaphylaxis or angioedema. No safe re-challenge protocol established.

Relative Contraindications (Specialist Input Recommended)

Pre-existing cardiac dysfunction (LVEF <50%) — patients with baseline impaired cardiac function were excluded from pivotal trials. If trastuzumab is considered essential, joint oncology-cardiology decision required with intensified monitoring.
Prior cumulative anthracycline exposure exceeding recommended limits — increased risk of irreversible cardiomyopathy when followed by trastuzumab.
Symptomatic intrinsic lung disease — patients with extensive pulmonary tumour involvement and dyspnoea at rest appear to have more severe pulmonary toxicity.
Concurrent anthracycline therapy — synergistic cardiotoxicity precludes simultaneous administration in current standard-of-care protocols.

Use with Caution

Elderly patients (≥65 years) — increased risk of cardiac dysfunction compared with younger patients in both adjuvant and metastatic settings.
Patients with cardiovascular risk factors (prior radiation to chest, hypertension, diabetes, obesity) — may increase baseline cardiac risk.
Patients with bulky metastatic disease — rare cases of tumour lysis syndrome reported; ensure adequate hydration.
Breastfeeding — manufacturer recommends discontinuing breastfeeding during treatment and for 7 months after the last dose due to insufficient safety data.

FDA Boxed Warning Cardiomyopathy

Trastuzumab can result in subclinical and clinical cardiac failure, including CHF and decreased LVEF. The incidence and severity are highest when administered concurrently with anthracycline-containing chemotherapy. A 4–6-fold increase in symptomatic myocardial dysfunction has been observed. Evaluate cardiac function prior to and during treatment. Discontinue for cardiomyopathy.

FDA Boxed Warning Infusion Reactions & Pulmonary Toxicity

Serious and fatal infusion reactions and pulmonary toxicity have been reported. Symptoms usually occur during or within 24 hours of administration. Interrupt infusion for dyspnoea or clinically significant hypotension. Monitor until symptoms completely resolve. Discontinue for anaphylaxis, angioedema, interstitial pneumonitis, or ARDS.

FDA Boxed Warning Embryo-Fetal Toxicity

Exposure during pregnancy can result in oligohydramnios and oligohydramnios sequence, including pulmonary hypoplasia, skeletal abnormalities, and neonatal death. Verify pregnancy status before initiation. Advise effective contraception during treatment and for 7 months after the last dose.

Patient Counselling for Trastuzumab

Purpose of Therapy

Trastuzumab targets a specific protein (HER2) that is overproduced by the cancer cells. By blocking this protein, trastuzumab slows tumour growth and helps the immune system recognise and destroy cancer cells. It is used alongside or after chemotherapy, and in early breast cancer, treatment typically lasts one year. For advanced cancer, treatment continues as long as it is working and tolerable.

How to Receive Treatment

Trastuzumab is given as an intravenous infusion in a clinical setting. The first infusion takes approximately 90 minutes, and if well tolerated, subsequent infusions may be shortened to 30 minutes. Patients will need regular heart function monitoring (echocardiograms or MUGA scans) throughout treatment and for two years after completion. Blood tests will also be performed regularly.

Infusion Reactions

Tell patient Fever, chills, and flu-like symptoms are common during or shortly after the first infusion and tend to be milder with subsequent doses. Pre-medication with paracetamol and antihistamines may help. Patients will be monitored during and after each infusion.

Call prescriber If experiencing severe difficulty breathing, throat tightness, facial swelling, chest pain, or severe dizziness during or after the infusion — these may indicate a serious reaction requiring emergency intervention.

Heart Function

Tell patient Trastuzumab can affect heart function. Regular heart scans are essential. Any new or worsening shortness of breath, persistent cough, ankle swelling, or sudden weight gain should be reported promptly. Heart effects are often reversible if caught early.

Call prescriber If experiencing worsening breathlessness at rest or with minimal exertion, waking up at night gasping for air, or rapid unexplained weight gain (>2 kg in a week).

Pregnancy & Contraception

Tell patient Trastuzumab can cause serious harm to an unborn baby. Effective contraception is required during treatment and for 7 months after the last dose, because the drug remains in the body for many months after stopping.

Call prescriber Immediately if pregnancy is suspected or confirmed at any time during treatment or within 7 months of the last dose.

Breathing Problems

Tell patient Rare but serious lung complications can occur. A new persistent cough, worsening breathlessness, or fever with respiratory symptoms should be reported, as these may require chest imaging and a change in treatment.

Call prescriber For any sudden onset of difficulty breathing, especially if accompanied by fever or chest tightness.

Infection Risk

Tell patient When given with chemotherapy, trastuzumab can increase the risk of infections by lowering white blood cell counts. Practice good hand hygiene and avoid close contact with people who are unwell.

Call prescriber If temperature rises above 38°C (100.4°F), or for signs of infection such as persistent sore throat, painful urination, or unusual fatigue.

Ref

Sources

Regulatory (PI / SmPC)

Herceptin (trastuzumab) for injection. Full Prescribing Information. Genentech, Inc. Revised June 2024. FDA Label Primary source for all dosing, boxed warnings, adverse reactions, pharmacokinetics, and drug interaction data in this monograph.
FDA Approval Letter. Herceptin (trastuzumab). September 25, 1998. FDA Approval Historical regulatory milestone as one of the first targeted cancer therapies approved by the FDA.

Key Clinical Trials

Romond EH, Perez EA, Bryant J, et al. Trastuzumab plus adjuvant chemotherapy for operable HER2-positive breast cancer. N Engl J Med. 2005;353(16):1673-1684. doi:10.1056/NEJMoa052122 Joint NSABP B31/NCCTG N9831 analysis establishing adjuvant trastuzumab as standard of care, demonstrating DFS hazard ratio of 0.48.
Piccart-Gebhart MJ, Procter M, Leyland-Jones B, et al. Trastuzumab after adjuvant chemotherapy in HER2-positive breast cancer (HERA). N Engl J Med. 2005;353(16):1659-1672. doi:10.1056/NEJMoa052306 HERA trial demonstrating benefit of 1-year adjuvant trastuzumab over observation, and that 2 years offered no additional benefit over 1 year.
Slamon DJ, Leyland-Jones B, Shak S, et al. Use of chemotherapy plus a monoclonal antibody against HER2 for metastatic breast cancer that overexpresses HER2. N Engl J Med. 2001;344(11):783-792. doi:10.1056/NEJM200103153441101 Pivotal H0648g trial in metastatic breast cancer showing improved TTP and OS with trastuzumab plus chemotherapy versus chemotherapy alone.
Slamon D, Eiermann W, Robert N, et al. Adjuvant trastuzumab in HER2-positive breast cancer (BCIRG 006). N Engl J Med. 2011;365(14):1273-1283. doi:10.1056/NEJMoa0910383 BCIRG 006 trial comparing AC-TH vs. TCH, establishing TCH as an effective lower-cardiotoxicity alternative.
Bang YJ, Van Cutsem E, Feyereislova A, et al. Trastuzumab in combination with chemotherapy versus chemotherapy alone for treatment of HER2-positive advanced gastric or gastro-oesophageal junction cancer (ToGA). Lancet. 2010;376(9742):687-697. doi:10.1016/S0140-6736(10)61121-X Landmark trial extending trastuzumab indications to HER2-positive gastric cancer, showing median OS of 13.8 vs. 11.1 months.

Guidelines

National Comprehensive Cancer Network (NCCN). Clinical Practice Guidelines in Oncology: Breast Cancer. Version 4.2024. NCCN Current NCCN guidelines for HER2-positive breast cancer management, incorporating adjuvant and metastatic trastuzumab regimens.
National Comprehensive Cancer Network (NCCN). Clinical Practice Guidelines in Oncology: Gastric Cancer. Version 2.2024. NCCN NCCN recommendations for HER2-directed therapy in gastric and GEJ adenocarcinoma.

Mechanistic / Basic Science

Hudis CA. Trastuzumab — mechanism of action and use in clinical practice. N Engl J Med. 2007;357(1):39-51. doi:10.1056/NEJMra043186 Comprehensive review of trastuzumab’s mechanism of action, including ADCC, receptor downregulation, and anti-angiogenic effects.
Greenblatt K, Khaddour K. Trastuzumab. In: StatPearls [Internet]. Treasure Island (FL): StatPearls Publishing; Updated June 22, 2024. StatPearls Current comprehensive review of trastuzumab pharmacology, indications, adverse effects, and monitoring requirements.

Pharmacokinetics / Special Populations

Bruno R, Washington CB, Lu JF, et al. Population pharmacokinetics of trastuzumab in patients with HER2+ metastatic breast cancer. Cancer Chemother Pharmacol. 2005;56(4):361-369. doi:10.1007/s00280-005-1026-z Population PK model establishing t½ of 28.5 days, CL of 0.225 L/day, and influence of tumour burden on clearance.
Leveque D, Gigou L, Bergerat JP. Clinical pharmacology of trastuzumab. Curr Clin Pharmacol. 2008;3(1):51-55. doi:10.2174/157488408783329931 Review of trastuzumab pharmacokinetics characterising low clearance, low Vd (~4 L), and long half-life comparable to endogenous IgG.

Herceptin (Trastuzumab)