Alteplase (Activase): Complete Drug Monograph

Pharmacokinetic Profile

Initial Half-Life

< 5 minutes (in AMI patients)

Plasma Clearance

380–570 mL/min (primarily hepatic)

Volume of Distribution

~Plasma volume

Metabolism

Hepatic (clearance via the liver)

Onset of Fibrinolysis

Minutes (fibrin-bound activation)

Fibrinogen Reduction

16–36% after 100 mg dose

Clinical Information

Drug Class

Tissue plasminogen activator (tPA); fibrinolytic

Available Forms

50 mg / 100 mg vials (Activase); 2 mg vial (Cathflo Activase)

Route

IV (Activase); intracatheter instillation (Cathflo)

Renal Adjustment

None specified in PI

Hepatic Adjustment

Caution — significant hepatic dysfunction increases bleeding risk

Pregnancy

Category C (embryocidal in rabbits)

Lactation

Excretion in human milk unknown

Schedule / Legal Status

Rx only, non-controlled

Generic Available

No (single brand: Activase / Cathflo)

Indications

Indication	Approved Population	Therapy Type	Status
Acute ischemic stroke (AIS)	Adults presenting within 3 hours of symptom onset (FDA label); intracranial haemorrhage excluded by imaging	Monotherapy with concomitant supportive care	FDA Approved
Acute myocardial infarction (AMI)	Adults — for the reduction of mortality and reduction of the incidence of heart failure	With concomitant aspirin and heparin (accelerated regimen evidence)	FDA Approved
Acute massive pulmonary embolism (PE)	Adults with acute PE obstructing flow to a lobe or multiple lung segments, or with unstable haemodynamics	Monotherapy (anticoagulation initiated near end of infusion)	FDA Approved
Restoration of central venous access device function	Adults and paediatric patients with thrombotic catheter occlusion (Cathflo Activase formulation)	Intracatheter instillation	FDA Approved

Alteplase is recombinant human tissue plasminogen activator (rt-PA), a 527-amino-acid serine protease produced by recombinant DNA technology. The complementary DNA used in its synthesis was originally obtained from a human melanoma cell line (per the FDA prescribing information). Two formulations are marketed in the United States: Activase (50 mg and 100 mg vials) for systemic intravenous fibrinolysis in stroke, MI, and pulmonary embolism, and Cathflo Activase (2 mg vial), a separately FDA-licensed product for restoration of function to occluded central venous access devices. Initial U.S. approval of Activase was 1987 (originally for AMI); the AIS indication was added in 1996. The AMI indication is limited by the FDA label, which notes that the risk of stroke may outweigh thrombolytic benefit in patients whose AMI puts them at low risk for death or heart failure.

Off-Label and Guideline-Endorsed Extended Uses

AIS within the 3 to 4.5-hour window — the FDA-approved window remains 3 hours, but the 2019 AHA/ASA acute ischemic stroke guideline recommends IV alteplase 0.9 mg/kg between 3 and 4.5 hours after symptom onset for selected eligible patients (Class of Recommendation I, Level of Evidence B-R). Use beyond 3 hours is therefore standard of care in the United States but technically off-label per the FDA label. Evidence quality: high (ECASS III; subsequent meta-analyses).

AIS with unwitnessed onset (e.g., wake-up stroke) — the 2019 AHA/ASA guideline considers IV alteplase within 4.5 hours of stroke recognition reasonable for patients with unknown time of onset when MRI shows DWI-positive / FLAIR-negative mismatch (WAKE-UP trial). Evidence quality: moderate (single pivotal RCT and supportive meta-analyses).

AIS in the 4.5 to 9-hour window with imaging selection — the most recent AHA/ASA acute ischemic stroke guideline update introduces a Class IIa recommendation for IV thrombolysis between 4.5 and 9 hours from onset (or last known well) when advanced perfusion imaging shows salvageable tissue (EXTEND trial and pooled analyses). Verify the current recommendation at the time of practice. Evidence quality: moderate.

Submassive (intermediate-risk) pulmonary embolism — use in PE with right-ventricular dysfunction but preserved systemic blood pressure is off-label and individualised; the FDA indication is restricted to “massive” PE. The PEITHO trial (which tested tenecteplase, a related fibrinolytic, not alteplase) showed reduction in haemodynamic decompensation but increased major bleeding without overall mortality benefit. Evidence quality: moderate (extrapolated from class evidence).

Catheter-directed thrombolysis for peripheral arterial occlusion or extensive deep-vein thrombosis. Evidence quality: low to moderate.

Dose

Dosing

Alteplase dosing is indication-specific and weight-based for systemic use. Reconstitute Activase only with the supplied Sterile Water for Injection USP (no preservative) to a 1 mg/mL solution; further dilution to 0.5 mg/mL with 0.9% sodium chloride or 5% dextrose is permitted. Do not mix with other medications. Reconstituted solution is stable at 2–30 °C for 8 hours.

Clinical Scenario	Starting Dose	Maintenance / Infusion	Maximum Dose	Notes
Acute ischemic stroke — within 3 h of onset (FDA label)	10% of total dose IV bolus over 1 min	Remaining 90% IV over 60 min	0.9 mg/kg, max 90 mg	Confirm no intracranial haemorrhage on imaging before initiation; pretreatment BP must be < 185/110 mm Hg No aspirin / heparin / antiplatelet for first 24 h after infusion (AIS)
Acute ischemic stroke — 3 to 4.5 h (off-label, 2019 AHA/ASA Class I)	10% of total dose IV bolus over 1 min	Remaining 90% IV over 60 min	0.9 mg/kg, max 90 mg	Same dose as 0–3 h window per AHA/ASA; benefit is time-dependent — treat as soon as eligible Off-label per FDA but recommended by guidelines in selected patients
Acute MI — accelerated regimen, > 67 kg	15 mg IV bolus	50 mg over first 30 min, then 35 mg over next 60 min	100 mg total over 90 min	Concomitant aspirin and IV heparin per pivotal evidence (GUSTO-I) Largely supplanted by primary PCI where timely PCI is available
Acute MI — accelerated regimen, ≤ 67 kg	15 mg IV bolus	0.75 mg/kg over first 30 min, then 0.50 mg/kg over next 60 min	100 mg total	Weight-banded scaling so total dose does not exceed 100 mg Concomitant aspirin and IV heparin
Acute MI — 3-hour infusion, ≥ 65 kg	6–10 mg IV bolus	50–54 mg rest of 1st hour; 20 mg in 2nd hour; 20 mg in 3rd hour	100 mg total	Older regimen retained as alternative when accelerated regimen not feasible
Acute MI — 3-hour infusion, < 65 kg	0.075 mg/kg IV bolus	0.675 mg/kg rest of 1st h; 0.25 mg/kg in 2nd h; 0.25 mg/kg in 3rd h	1.25 mg/kg over 3 h	Total dose should not exceed 100 mg in any AMI regimen — 150 mg is associated with increased intracranial haemorrhage
Acute massive pulmonary embolism	No bolus	100 mg IV over 2 hours	100 mg	Initiate parenteral anticoagulation near the end of, or immediately after, infusion when aPTT or thrombin time returns to ≤ 2× normal Risk of reembolisation from underlying DVT
Catheter occlusion — adults and children ≥ 30 kg (Cathflo)	2 mg in 2 mL instilled into occluded lumen	Dwell 30–120 min; aspirate to assess function	Up to 2 doses of 2 mg each	If function is not restored after 120 min, a second 2 mg dose may be instilled No safety / efficacy data above 2 mg per dose for this indication
Catheter occlusion — children < 30 kg (Cathflo)	110% of internal lumen volume	Not to exceed 2 mg in 2 mL	Up to 2 doses	Dose calculated to fill the catheter lumen; do not over-pressurise — vigorous suction or excessive pressure can damage the catheter

Population-Specific Considerations

Population	Adjustment	Rationale
Geriatric (> 75 years)	No formal dose adjustment	FDA PI Section 8.5 notes age > 77 years was associated with increased ICH risk in AIS exploratory analyses; functional outcome remained favourable; AHA/ASA endorses use
Renal impairment	No specified adjustment	Clearance is hepatic; severe renal disease may increase bleeding risk via uraemic platelet dysfunction (precaution, not contraindication)
Hepatic impairment	Use with caution	Significant hepatic dysfunction is listed by the FDA PI Section 5.1 as a condition that increases bleeding risk; weigh against anticipated benefit
Pediatric AIS / AMI / PE	Not established	Per FDA PI Section 8.4, safety and effectiveness for systemic indications have not been established; institutional paediatric stroke protocols may apply off-label under specialist supervision

Clinical Pearl — Reconstitution and Setup

Use only the bundled Sterile Water for Injection USP — bacteriostatic water inactivates the molecule. Slight foaming is expected; let the vial stand to allow bubbles to dissipate, do not shake. The 100 mg vial does not contain vacuum and uses the supplied transfer device; the 50 mg vial is vacuum-sealed (do not use if vacuum is absent). Do not add any other medication to the infusion line. For AIS, the 10% bolus can be drawn from a port on the primed infusion line, or the pump can be programmed to deliver the bolus volume at the start of infusion.

Critical — Activase ≠ Cathflo Activase ≠ TNKase

Three Genentech thrombolytics are commonly confused: Activase (alteplase 50 / 100 mg vials, systemic IV thrombolysis), Cathflo Activase (alteplase 2 mg vial, intracatheter only), and TNKase (tenecteplase, single IV bolus). The FDA has issued specific medication-error alerts about confusion between these products. Verify the product name, vial strength, and indication on every order.

Pharmacology

Mechanism of Action

Alteplase is a recombinant DNA-derived form of human tissue plasminogen activator — a 527-amino-acid serine protease. The complementary DNA used in its synthesis was originally obtained from a human melanoma cell line. Its activity is fibrin-enhanced: in the absence of fibrin, alteplase converts plasminogen to plasmin only minimally, but when bound to fibrin within a thrombus it catalyses local conversion of entrapped plasminogen to plasmin, initiating clot lysis. This relative fibrin specificity, compared with the older non-specific thrombolytic streptokinase, is the basis for its preferential local fibrinolytic effect. Clinically meaningful systemic fibrinogen depletion still occurs, however: a 16–36% reduction in circulating fibrinogen has been described after a 100 mg dose, and approximately 11% of patients receiving 1.25 mg/kg over 3 hours had fibrinogen fall below 100 mg/dL in a controlled trial. The downstream plasmin then degrades fibrin and other coagulation factors, restoring vessel patency.

ADME Profile

Parameter	Value	Clinical Implication
Absorption	IV administration only — no oral bioavailability (large glycoprotein); reconstituted to 1 mg/mL or further diluted to 0.5 mg/mL	Bolus and infusion can be given peripherally; do not co-infuse with other drugs in the same line
Distribution	Initial volume of distribution ≈ plasma volume; binds locally to fibrin within thrombus	Action is concentrated at the clot rather than uniformly systemic; basis for relative fibrin specificity
Metabolism	Predominantly hepatic clearance; degraded as a protein	Significant hepatic dysfunction increases bleeding risk and warrants caution
Elimination	Initial plasma half-life < 5 minutes in AMI patients (per FDA PI Section 12.3); plasma clearance 380–570 mL/min	Rapid disappearance from plasma drives bolus + short-infusion regimens; biologic effect (lysis, fibrinogen depletion, bleeding risk) outlasts measurable plasma drug

Why bleeding risk persists after the infusion

Alteplase clears from plasma in minutes, but the systemic lytic state — depleted fibrinogen, plasmin-degraded coagulation factors, and impaired haemostasis — can persist for hours to days. The FDA prescribing information notes that haemorrhage can occur one or more days after Activase administration, particularly when patients also receive heparin or aspirin. This is the rationale for delaying additional antithrombotics for 24 hours after AIS thrombolysis.

Side Effects

The FDA prescribing information identifies bleeding as the most frequent adverse reaction across all approved indications. The incidence and clinical significance differ markedly by indication and dose: intracranial haemorrhage dominates the AIS risk profile, gastrointestinal and genitourinary bleeding dominate the AMI / PE profile, and Cathflo Activase (2 mg intracatheter) has shown a very low rate of serious adverse events in registration trials. The figures below are drawn directly from FDA PI Tables 3, 4, and 5.

≥10% Very Common (AIS pivotal trials)

Adverse Effect	Incidence	Clinical Note
Total intracranial haemorrhage (AIS, in-trial follow-up)	15.4%	Placebo 6.4% (p < 0.01); pooled n = 624 from FDA PI Table 3 (NINDS rt-PA Stroke Studies 1 and 2)
All-cause 90-day mortality (AIS)	17.3%	Placebo 20.5% (p = 0.36); not increased by alteplase despite the ICH excess

No other ≥ 10% non-bleeding adverse reaction is enumerated in the FDA prescribing information for systemic alteplase.

< 10% Common Bleeding Events

Adverse Effect	Incidence	Clinical Note
Symptomatic ICH (AIS, in-trial follow-up)	8.0%	Placebo 1.3% (p < 0.01); per FDA PI Table 3
Asymptomatic ICH (AIS)	7.4%	Placebo 5.1% (p = 0.32); detected on routine repeat CT without clinical worsening
Symptomatic ICH within 36 hours (AIS)	6.4%	Placebo 0.6% (p < 0.01); the early window in which most clinically relevant ICH occurs
Bleeding requiring red-cell transfusion (AIS)	6.4%	Placebo 3.8% (p = 0.19); reflects the systemic bleeding profile in the AIS cohort
New ischemic stroke at 3 months (AIS)	5.8%	Placebo 5.4% (p = 1.00); not increased by alteplase
Gastrointestinal bleeding (AMI 3-h regimen)	5%	Per FDA PI Table 4; total dose ≤ 100 mg; n > 800
Genitourinary bleeding (AMI 3-h regimen)	4%	Per FDA PI Table 4
Ecchymosis (AMI 3-h regimen)	1%	Particularly at puncture sites; minimise venipunctures
Retroperitoneal, epistaxis, gingival bleeding (AMI 3-h regimen)	< 1% each	Per FDA PI Table 4
Intracranial haemorrhage (AMI 3-h, 100 mg)	0.4%	n = 3,272 per FDA PI Table 5
Intracranial haemorrhage (AMI accelerated, ≤ 100 mg)	0.7%	n = 10,396 per FDA PI Table 5
Intracranial haemorrhage (AMI, 150 mg)	1.3%	n = 1,779; this is the rationale that 150 mg should not be used for AMI

Serious Serious Adverse Events

Adverse Effect	Estimated Frequency	Typical Onset	Required Action
Symptomatic intracranial haemorrhage (AIS)	8.0% in AIS pivotal cohort; 6.4% within 36 h	Usually first 24–36 h	Stop infusion; urgent CT; cryoprecipitate ± antifibrinolytic (tranexamic acid or aminocaproic acid); platelet transfusion if low or on antiplatelet; neurosurgery consult
Major systemic bleeding (any indication)	Increased over baseline; specific rate varies by site (see Common Bleeding table)	During infusion or within 24 h; can occur days later if anticoagulated	Stop infusion immediately; pressure on compressible sites; cryoprecipitate; transfusion as needed
Orolingual angioedema	Reported during and up to 2 h after infusion (AIS / AMI); higher risk with concomitant ACE inhibitors	During or within 2 h of infusion	Stop infusion; airway assessment; antihistamines, IV corticosteroids, epinephrine; intubate early if airway compromised (avoid traumatic intubation — fatal haemorrhage reported)
Anaphylactoid / allergic reactions	Reported (frequency not quantified in PI)	Any time during infusion	Discontinue; standard anaphylaxis management
Cholesterol embolisation	Rare; true incidence unknown	Days after exposure	Recognise (livedo reticularis, “purple toe”, AKI, gangrenous digits, pancreatitis); supportive care; can be fatal
Pulmonary reembolisation	Reported in PE patients; lysis of underlying DVT may release further emboli	During or after infusion	Anticoagulation as soon as aPTT or thrombin time permits; supportive haemodynamic care
Cardiac complications (post-marketing, AMI)	Reported; frequency confounded by underlying AMI	During or after AMI	Recognise arrhythmia, AV block, cardiogenic shock, myocardial rupture, pericardial effusion, tamponade — manage per acute MI protocol
AIS post-marketing CNS events	Reported (frequency not quantifiable)	During or after infusion	Cerebral oedema, cerebral herniation, seizure, new ischemic stroke — manage per neurocritical care protocol; can be life-threatening

Discontinuation Infusion Termination

Infusion Length

60 min – 3 h single course

Note: alteplase is a single-course acute therapy, not a chronic medication. “Discontinuation” here refers to early termination during or before completion of the planned infusion rather than a long-term withdrawal rate.

Mandatory Reasons to Stop

Bleeding · Angioedema

Action: stop infusion immediately for serious bleeding (any site), suspected ICH, or developing orolingual angioedema. Discard remaining drug.

Reason for Discontinuation	Incidence	Context
Suspected intracranial haemorrhage	Per protocol	Sudden clinical worsening (deteriorating LOC, new headache, vomiting, BP surge) → stop infusion, urgent CT
Major extracranial bleeding	Per protocol	Stop infusion, apply pressure to compressible sites, supportive transfusion
Orolingual angioedema	Per protocol	Stop infusion immediately, secure airway, treat with antihistamines / corticosteroids / epinephrine
Pretreatment INR > 1.7 or aPTT elevated (AIS)	Per protocol	Per FDA PI Section 2.1 — discontinue if results return after initiation in patients without recent anticoagulant use

Management Pearl — Suspected Symptomatic ICH

If a patient receiving alteplase develops sudden neurological deterioration, severe headache, acute hypertension, nausea or vomiting: stop the infusion, secure the airway and IV access, and obtain an urgent non-contrast CT. While imaging is pending, send fibrinogen, platelets, PT / aPTT, and type and crossmatch. If ICH is confirmed, administer cryoprecipitate (typically 10 units; target fibrinogen ≥ 150 mg/dL), consider an antifibrinolytic (tranexamic acid 1 g IV or aminocaproic acid), correct platelets if needed, and consult neurosurgery and haematology promptly. Reversal protocols vary by institution — follow local guidance.

Int

Drug Interactions

Formal drug-interaction studies of alteplase with other cardioactive or cerebroactive drugs have not been conducted. The FDA prescribing information explicitly addresses two interaction categories: antithrombotic drugs (additive bleeding risk) and angiotensin-converting enzyme inhibitors (post-marketing reports of orolingual angioedema). Several additional clinically important interactions are based on shared bleeding mechanisms and are reflected in major reference databases (Lexicomp, Micromedex).

Major Heparin / LMWH (therapeutic dosing)

MechanismAdditive antithrombotic effect on top of the systemic lytic state

EffectIncreased bleeding risk, including intracranial

ManagementIn AIS, do not give heparin or aspirin within the first 24 h after alteplase. In AMI / PE, concomitant heparin is part of the regimen — adjust per protocol and monitor closely

FDA PI 5.1, 7

Major Direct oral anticoagulants (DOACs) and warfarin

MechanismActive anticoagulation compounding the lytic state

EffectSignificantly increased bleeding risk

ManagementFor AIS, alteplase is contraindicated by FDA label if INR > 1.7 (warfarin) or if aPTT is elevated; for DOACs, AHA/ASA suggests typically avoiding within ~48 h of last dose (longer in renal impairment) unless reversed

FDA PI 2.1; AHA/ASA 2019

Major Antiplatelet agents (aspirin, P2Y12 inhibitors, GP IIb/IIIa inhibitors)

MechanismAdditive haemostatic impairment

EffectIncreased bleeding risk, including intracranial

ManagementIn AIS, defer all antiplatelet drugs (including aspirin) for 24 h after alteplase. In AMI, aspirin and IV heparin are co-administered per the accelerated regimen evidence

FDA PI 5.1, 7

Moderate ACE inhibitors

MechanismBradykinin accumulation (post-marketing reports of orolingual angioedema with concomitant use)

EffectHigher reported incidence of orolingual angioedema, especially in AIS

ManagementMonitor airway during and for ≥ 2 h after infusion; have antihistamines, corticosteroids, and epinephrine available at the bedside

FDA PI 5.2, 7

Moderate NSAIDs and SSRIs / SNRIs

MechanismPlatelet dysfunction (NSAIDs) or impaired platelet serotonin uptake (SSRIs / SNRIs)

EffectMarginal additional bleeding risk

ManagementRecognise as a risk factor; not a contraindication; avoid additional NSAIDs in the 24 h after alteplase

Lexicomp / Micromedex

Minor Nitroglycerin (during AMI)

MechanismHypothesised increased hepatic blood flow leading to faster alteplase clearance (mechanism debated)

EffectPossible reduction in fibrinolytic effect; clinical significance uncertain

ManagementUse nitroglycerin only when clinically indicated; not a contraindication

Lexicomp

Coagulation tests during therapy

The FDA prescribing information cautions that coagulation tests and measures of fibrinolytic activity may be unreliable during alteplase therapy because circulating drug remains active in vitro and can degrade fibrinogen in blood samples after collection. Specific precautions (rapid sample handling and inhibitor addition) are required for accurate post-treatment fibrinogen measurement.

Mon

Monitoring

Alteplase requires intensive bedside monitoring during and after infusion. The dominant priorities are early detection of bleeding (especially intracranial), tight blood-pressure control, and airway assessment for angioedema. AHA/ASA stroke guidelines specify a structured neurological- and BP-monitoring schedule for the first 24 hours after AIS thrombolysis, summarised below.

Blood Pressure (AIS) Every 15 min × 2 h, then q 30 min × 6 h, then q 60 min × 16 h
Routine Goal < 180/105 mm Hg for the first 24 h after AIS thrombolysis (AHA/ASA). Treat with IV labetalol, nicardipine, or clevidipine per institutional protocol. Pretreatment BP must be < 185/110 mm Hg before the bolus.
Neurological Exam Same schedule as BP for first 24 h
Routine NIHSS or focused neurological check; any acute deterioration mandates immediate stop of infusion and urgent CT to exclude ICH.
Bleeding Surveillance Continuous during infusion; clinical monitoring ≥ 24 h
Routine Inspect arterial puncture sites, mucous membranes, urine, and stool. Avoid IM injections, urinary catheters, NG tubes, and central venous access during the first 24 h unless essential.
Airway / Angioedema During and for ≥ 2 h after infusion
Routine Inspect tongue and oropharynx, especially in patients on ACE inhibitors. Have antihistamines, corticosteroids, and epinephrine available.
Cardiac Rhythm (AMI) Continuous telemetry
Routine Watch for reperfusion arrhythmias, AV block, hypotension; recognise mechanical complications (rupture, tamponade) early.
Repeat CT (AIS) At 24 h or sooner if deterioration
Routine Required before initiating antiplatelet or anticoagulant therapy; sooner if any neurological worsening, severe headache, or BP surge.
Coagulation Panel Baseline; repeat with bleeding
Trigger-based Pretreatment INR (must be ≤ 1.7 for AIS per FDA PI), aPTT, platelets, fibrinogen, type and screen. In AIS without recent anticoagulant use, treatment can begin before results return; discontinue if INR > 1.7 or aPTT elevated.
Glucose At presentation in AIS
Trigger-based Hypoglycaemia (typically < 50 mg/dL) and severe hyperglycaemia can mimic stroke; the AHA/ASA guideline recommends correcting glucose abnormalities before treatment but does not categorically exclude eligible patients once glucose is corrected.
Catheter Function (Cathflo) At 30 min and 120 min after instillation
Routine Aspirate gently to test patency. If unsuccessful at 120 min, a second 2 mg dose may be instilled.

Contraindications & Cautions

Absolute Contraindications — Acute Ischemic Stroke (FDA PI Section 4.1)

Current intracranial haemorrhage
Subarachnoid haemorrhage
Active internal bleeding
Recent (within 3 months) intracranial or intraspinal surgery, or serious head trauma
Intracranial conditions that may increase the risk of bleeding — e.g., some neoplasms, arteriovenous malformations, aneurysms
Bleeding diathesis
Current severe uncontrolled hypertension — generally interpreted clinically as BP that cannot be lowered to < 185/110 mm Hg with antihypertensives prior to thrombolysis

Absolute Contraindications — Acute MI or Pulmonary Embolism (FDA PI Section 4.2)

Active internal bleeding
History of recent stroke
Recent (within 3 months) intracranial or intraspinal surgery, or serious head trauma
Intracranial conditions that may increase the risk of bleeding
Bleeding diathesis
Current severe uncontrolled hypertension

Absolute Contraindication — Cathflo Activase

Known hypersensitivity to alteplase or any formulation excipient

Relative Contraindications (Specialist Input Recommended)

The FDA PI Section 5.1 lists conditions in which the bleeding risks of Activase therapy for all approved indications are increased and should be weighed against the anticipated benefits. These include:

Recent major surgery or procedure — coronary artery bypass graft, obstetric delivery, organ biopsy, previous puncture of non-compressible vessels
Cerebrovascular disease
Recent intracranial haemorrhage
Recent gastrointestinal or genitourinary bleeding
Recent trauma
Hypertension — systolic BP above 175 mm Hg or diastolic BP above 110 mm Hg per the FDA PI; the AHA/ASA threshold for AIS is < 185/110 mm Hg before bolus
High likelihood of left heart thrombus — e.g., mitral stenosis with atrial fibrillation
Acute pericarditis
Subacute bacterial endocarditis
Hemostatic defects, including those secondary to severe hepatic or renal disease
Significant hepatic dysfunction
Pregnancy
Diabetic haemorrhagic retinopathy or other haemorrhagic ophthalmic conditions
Septic thrombophlebitis or occluded AV cannula at a seriously infected site
Advanced age — increased ICH risk in AIS analyses (especially > 77 years), but functional benefit retained per AHA/ASA
Patients currently receiving anticoagulants (e.g., warfarin)
Any other condition in which bleeding constitutes a significant hazard or would be particularly difficult to manage because of its location

Use with Caution

Concomitant ACE inhibitor — higher reported risk of orolingual angioedema; monitor airway during and after infusion.
Pulmonary embolism with extensive proximal DVT — risk of reembolisation as the lytic state dissolves the source clot.
Pediatric systemic use (AIS, AMI, PE) — safety and effectiveness not established per FDA PI Section 8.4; institutional paediatric stroke protocols may apply off-label under specialist supervision.
Pregnancy — animal data show embryocidal effects; no adequate human data. Use only when clearly indicated and the benefit outweighs the unknown risk.
Lactation — excretion in human milk unknown per FDA PI Section 8.3; risk-benefit decision based on the acuity of the indication.

FDA Warnings & Precautions (Section 5) Bleeding Risk and Orolingual Angioedema

Activase increases the risk of bleeding (intracranial, retroperitoneal, gastrointestinal, genitourinary, respiratory, or external — especially at puncture sites). Avoid intramuscular injections and minimise venipunctures. If serious bleeding occurs, terminate the infusion immediately. There is no FDA boxed warning on the Activase label, but the bleeding caution is the central theme of the prescribing information.

Orolingual angioedema has been reported during and up to 2 hours after Activase infusion, particularly in patients also receiving angiotensin-converting enzyme inhibitors. Monitor patients during and for several hours after infusion. If angioedema develops, discontinue Activase and treat with antihistamines, IV corticosteroids, and epinephrine; secure the airway early. Cholesterol embolism has rarely been reported with thrombolytics. Reembolisation from underlying deep vein thrombosis should be considered when treating PE.

Patient Counselling

Purpose of Therapy

Alteplase is an emergency, single-dose therapy. Most patients (or surrogate decision-makers) receive it under acute, time-pressured conditions for stroke, heart attack, or major pulmonary embolism. Counselling typically occurs in two phases: a brief consent conversation before the infusion (when feasible) covering the trade-off between potential benefit and bleeding risk, and a more thorough post-infusion conversation about ongoing observation, recovery, and follow-up. For Cathflo Activase used to clear an occluded venous catheter, counselling focuses on the procedural nature of the dose and what to expect.

Before the Infusion (where time permits)

Explain in plain language that the medicine works by dissolving the clot blocking a brain artery, heart artery, or major lung vessel. Earlier treatment increases the chance of a good outcome. The most important risk is bleeding — including bleeding into the brain, which in stroke trials occurred symptomatically in around 8 of every 100 patients treated, and which can be fatal in some cases. Despite this risk, the trial evidence shows that more patients return to independent living than would without the medicine. Allergic reactions, including swelling of the tongue and lips, are uncommon but possible, especially in patients on certain blood-pressure medicines.

Bleeding — What to Watch For

Tell patient For at least 24 hours and up to several days after the infusion, you are at higher risk of bleeding. You will be observed in hospital. Avoid blowing your nose forcefully, brushing teeth too vigorously, or shaving with a razor while admitted. Tell staff if you notice unusual bruising, blood in urine or stool, coughing up blood, vomit that looks like coffee grounds, or new headache.

Call prescriber After discharge: any unexpected bleeding, dark or tarry stools, blood in vomit or urine, coughing up blood, severe headache, sudden weakness, or speech change — call emergency services immediately.

Stroke Symptoms After Discharge

Tell patient Recognise stroke warning signs using the FAST acronym: Face drooping, Arm weakness, Speech difficulty, Time to call emergency services. Stroke can recur. Take prescribed prevention therapy (typically antiplatelet therapy, blood-pressure medicine, and a statin) as directed once the team confirms it is safe to start.

Call prescriber Any new neurological symptom — call emergency services immediately. Do not wait to see if it resolves.

Lip / Tongue Swelling (Angioedema)

Tell patient A small number of patients develop swelling of the lips or tongue during or shortly after the infusion. The team will watch closely. If you notice tongue thickening, lip swelling, or trouble speaking, tell staff immediately. This usually resolves with treatment but can rarely affect breathing.

Call prescriber After discharge: any new tongue, lip, or facial swelling, especially with difficulty breathing — call emergency services. Mention you recently received alteplase and (if applicable) take an ACE inhibitor.

After Heart Attack or PE Treatment

Tell patient For heart attack: you will continue on aspirin and other heart medicines, and the team will discuss longer-term prevention (statins, beta-blockers, ACE inhibitors, dual antiplatelets, lifestyle changes). For pulmonary embolism: you will continue on an anticoagulant for at least three months (often longer), and follow-up imaging may be arranged.

Call prescriber Worsening chest pain, severe shortness of breath, leg swelling or pain, or fainting after discharge — seek emergency assessment.

Catheter Clearance with Cathflo

Tell patient The medicine is being put into your central line, not into your bloodstream. It works locally to dissolve the clot blocking the catheter. The dwell takes about 30 minutes to 2 hours, and a second dose may be given if the line is still blocked. Bleeding from the catheter site or systemic bleeding is uncommon at this dose.

Call prescriber Bleeding from the line site, fever or chills (possible infection), or any new shortness of breath after the procedure.

Follow-up and Recovery

Tell patient Stroke and heart attack recovery often involve rehabilitation (physical therapy, occupational therapy, speech therapy). Address vascular risk factors: blood pressure, cholesterol, diabetes, smoking, weight, and physical activity. Take the prescribed medicines exactly as directed, even if you feel well.

Call prescriber Any new neurological, cardiac, or respiratory symptom; medication side effects; or questions about the medicines you are now taking.

Ref

Sources

Regulatory (PI / SmPC)

Activase® (alteplase) US Prescribing Information. Genentech, Inc. Revised February 2015. accessdata.fda.gov Primary FDA label for systemic Activase; source for indications, dosing, contraindications, and adverse-reaction tables (Tables 3, 4, 5) and pharmacokinetic values cited throughout this monograph.
Cathflo® Activase® (alteplase) US Prescribing Information. Genentech, Inc. accessdata.fda.gov Separate FDA label for the 2 mg intracatheter formulation, including the paediatric weight-based instillation rule.

Key Clinical Trials

The National Institute of Neurological Disorders and Stroke rt-PA Stroke Study Group. Tissue plasminogen activator for acute ischemic stroke. N Engl J Med. 1995;333(24):1581-1587. doi.org/10.1056/NEJM199512143332401 Pivotal NINDS trial that established alteplase efficacy in AIS within 3 hours; source of the 3-month outcome data summarised in FDA PI Table 7.
Hacke W, Kaste M, Bluhmki E, et al; ECASS Investigators. Thrombolysis with alteplase 3 to 4.5 hours after acute ischemic stroke. N Engl J Med. 2008;359(13):1317-1329. doi.org/10.1056/NEJMoa0804656 ECASS III — pivotal evidence supporting the 3 to 4.5-hour extended treatment window adopted by AHA/ASA guidelines.
The GUSTO Investigators. An international randomized trial comparing four thrombolytic strategies for acute myocardial infarction. N Engl J Med. 1993;329(10):673-682. doi.org/10.1056/NEJM199309023291001 GUSTO-I — pivotal accelerated-infusion AMI trial (n = 41,021) referenced in FDA PI Table 8.
Thomalla G, Simonsen CZ, Boutitie F, et al; WAKE-UP Investigators. MRI-guided thrombolysis for stroke with unknown time of onset. N Engl J Med. 2018;379(7):611-622. doi.org/10.1056/NEJMoa1804355 Imaging-selection trial supporting the wake-up / unwitnessed-onset stroke recommendation.
Ma H, Campbell BCV, Parsons MW, et al; EXTEND Investigators. Thrombolysis guided by perfusion imaging up to 9 hours after onset of stroke. N Engl J Med. 2019;380(19):1795-1803. doi.org/10.1056/NEJMoa1813046 EXTEND — extended-window evidence underpinning the 4.5–9 h Class IIa recommendation in subsequent AHA/ASA guideline updates.
Meyer G, Vicaut E, Danays T, et al; PEITHO Investigators. Fibrinolysis for patients with intermediate-risk pulmonary embolism. N Engl J Med. 2014;370(15):1402-1411. doi.org/10.1056/NEJMoa1302097 PEITHO tested tenecteplase, not alteplase, but is the most-cited contemporary evidence on fibrinolysis for intermediate-risk PE — informs the off-label submassive PE discussion only as class-level evidence.
Blaney M, Shen V, Kerner JA, et al; CAPS Investigators. Alteplase for the treatment of central venous catheter occlusion in children: results of a prospective, open-label, single-arm study (Cathflo Activase Pediatric Study). J Vasc Interv Radiol. 2006;17(11 Pt 1):1745-1751. pubmed.ncbi.nlm.nih.gov/17142704 Paediatric Cathflo Activase efficacy and safety dataset supporting the < 30 kg dosing rule.

Guidelines

Powers WJ, Rabinstein AA, Ackerson T, et al; American Heart Association Stroke Council. Guidelines for the early management of patients with acute ischemic stroke: 2019 update to the 2018 guidelines for the early management of acute ischemic stroke. Stroke. 2019;50(12):e344-e418. doi.org/10.1161/STR.0000000000000211 2019 AHA/ASA AIS guideline update — basis for the 3 to 4.5-hour Class I recommendation, the wake-up stroke recommendation, and post-thrombolysis BP targets cited in the monitoring section.
American Heart Association / American Stroke Association. Most recent guideline for the early management of patients with acute ischemic stroke (published 2025/2026). Stroke. ahajournals.org/journal/str Most recent AHA/ASA AIS guideline introducing the 4.5–9 h Class IIa extended-window recommendation and equivalence statement for tenecteplase 0.25 mg/kg vs alteplase 0.9 mg/kg. Confirm the published citation (authors, journal, year, DOI) at time of publication.
O’Gara PT, Kushner FG, Ascheim DD, et al; American College of Cardiology Foundation / American Heart Association Task Force. 2013 ACCF/AHA guideline for the management of ST-elevation myocardial infarction. J Am Coll Cardiol. 2013;61(4):e78-e140. doi.org/10.1016/j.jacc.2012.11.019 ACC/AHA STEMI guideline — context for fibrinolytic therapy when timely PCI is not available.
Konstantinides SV, Meyer G, Becattini C, et al; The Task Force for the diagnosis and management of acute pulmonary embolism of the European Society of Cardiology. 2019 ESC Guidelines for the diagnosis and management of acute pulmonary embolism. Eur Heart J. 2020;41(4):543-603. doi.org/10.1093/eurheartj/ehz405 ESC PE guideline — defines high-risk (massive) and intermediate-risk PE and the role of systemic thrombolysis.

Mechanistic / Basic Science

Pennica D, Holmes WE, Kohr WJ, et al. Cloning and expression of human tissue-type plasminogen activator cDNA in E. coli. Nature. 1983;301(5897):214-221. doi.org/10.1038/301214a0 Original cloning paper that enabled recombinant production of human t-PA — historical foundation for the molecule.

Pharmacokinetics / Special Populations

Activase® (alteplase) US Prescribing Information, Section 12.3 (Pharmacokinetics). Genentech, Inc. accessdata.fda.gov Primary source for the initial half-life (< 5 minutes), plasma clearance (380–570 mL/min), volume of distribution (~ plasma volume), and hepatic clearance described in this monograph.
Alteplase. Drugs and Lactation Database (LactMed®). National Library of Medicine, Bethesda (MD). ncbi.nlm.nih.gov/books/NBK500827 Lactation safety summary — confirms human milk excretion data are not available; informs the cautions in this monograph.

Activase / Cathflo Activase (Alteplase)