What is Bevacizumab? Bevacizumab (brand name Avastin) is a targeted therapy drug that starves tumors by blocking the formation of new blood vessels. It works by inhibiting VEGF (vascular endothelial growth factor), a protein that tumors use to grow their own blood supply. Unlike traditional chemotherapy that directly kills cancer cells, bevacizumab is almost always given WITH chemotherapy to make the chemotherapy more effective. It's used for colorectal, lung, kidney, brain, cervical, and ovarian cancers.
Drug Class
Anti-Angiogenic
How Bevacizumab Works
Bevacizumab represents a fundamentally different approach to cancer treatment - instead of attacking cancer cells directly, it attacks their blood supply:
The Angiogenesis Process
- Normal blood vessels: Healthy tissues have stable blood vessels that rarely grow new branches
- Tumor growth problem: Once a tumor grows beyond 1-2 mm, it needs its own blood supply to get oxygen and nutrients
- VEGF production: Tumors produce large amounts of VEGF (vascular endothelial growth factor), a signal protein that tells the body "grow blood vessels here!"
- Angiogenesis: VEGF triggers rapid growth of new, abnormal blood vessels into the tumor (this process is called angiogenesis)
- Tumor expansion: With their own blood supply, tumors can grow larger and spread (metastasize)
How Bevacizumab Stops This
Bevacizumab Mechanism:
- VEGF neutralization: Bevacizumab is a monoclonal antibody that binds to VEGF-A in the bloodstream, preventing it from attaching to VEGF receptors on blood vessel cells
- Blocks new vessel formation: Without VEGF signaling, new blood vessels don't form
- Normalizes existing vessels: Tumor blood vessels are typically chaotic and leaky. Bevacizumab helps "normalize" them - making them more like normal blood vessels
- Enhances chemotherapy delivery: Normalized blood vessels may allow better delivery of chemotherapy to the tumor
- Tumor starvation: Without adequate blood supply, tumor growth slows or stops
Why Bevacizumab is Used WITH Chemotherapy
Bevacizumab is rarely used alone because:
- Synergistic effect: It makes chemotherapy work better by improving drug delivery to tumors
- Single-agent activity is limited: Bevacizumab alone rarely shrinks tumors significantly
- Best results in combination: Clinical trials show the biggest benefit when combined with chemotherapy
- Maintenance role: After initial chemotherapy + bevacizumab, some patients continue bevacizumab alone as "maintenance therapy"
What is Bevacizumab Used For?
FDA-Approved Uses
Colorectal Cancer
- First-line metastatic: Combined with FOLFOX or FOLFIRI chemotherapy
- Second-line metastatic: Combined with fluoropyrimidine-based chemotherapy
- Maintenance therapy: Continue bevacizumab after stopping chemotherapy to maintain disease control
Non-Small Cell Lung Cancer (NSCLC)
- First-line metastatic: Combined with carboplatin/paclitaxel for non-squamous NSCLC
- Important restriction: NOT for squamous cell lung cancer (increased bleeding risk)
Glioblastoma (Brain Cancer)
- Recurrent disease: As single agent or with lomustine chemotherapy
- Unique benefit: Reduces brain swelling (cerebral edema), may reduce steroid requirements
- Note: Improves progression-free survival but NOT overall survival
Renal Cell Carcinoma (Kidney Cancer)
- Metastatic disease: Combined with interferon-alfa (less common now; newer targeted therapies preferred)
Cervical Cancer
- Persistent, recurrent, or metastatic: Combined with paclitaxel/cisplatin or paclitaxel/topotecan
Ovarian, Fallopian Tube, or Primary Peritoneal Cancer
- Platinum-sensitive recurrent disease: Combined with carboplatin/paclitaxel or carboplatin/gemcitabine, then continued as maintenance
- Platinum-resistant recurrent disease: Combined with paclitaxel, pegylated liposomal doxorubicin, or topotecan
Hepatocellular Carcinoma (Liver Cancer)
- Combination with atezolizumab: First-line treatment for unresectable/metastatic HCC
- Landmark regimen: Atezolizumab + bevacizumab now standard first-line (replaced sorafenib)
Common Off-Label Uses
- Gastric/gastroesophageal cancer
- Pancreatic cancer (limited benefit)
- Breast cancer (was FDA-approved but approval withdrawn due to lack of overall survival benefit; still used off-label in some cases)
How is Bevacizumab Given?
Standard Dosing by Indication
Colorectal Cancer
- Dose: 5 mg/kg IV every 2 weeks OR 7.5 mg/kg IV every 3 weeks
- With: FOLFOX, FOLFIRI, or other fluoropyrimidine-based regimens
- Maintenance: Can continue bevacizumab 5 mg/kg Q2W after stopping chemotherapy
Lung Cancer (Non-Squamous NSCLC)
- Dose: 15 mg/kg IV every 3 weeks
- With: Carboplatin/paclitaxel typically
- Duration: Up to 6 cycles of chemotherapy, then may continue bevacizumab alone as maintenance
Glioblastoma
- Dose: 10 mg/kg IV every 2 weeks
- Can be used: As single agent or with lomustine
- Continue: Until disease progression or unacceptable toxicity
Ovarian Cancer
- Platinum-sensitive: 15 mg/kg IV every 3 weeks with chemotherapy, then continue as maintenance for up to 22 cycles total
- Platinum-resistant: 10 mg/kg IV every 2 weeks OR 15 mg/kg IV every 3 weeks
Cervical Cancer
- Dose: 15 mg/kg IV every 3 weeks with paclitaxel/cisplatin or paclitaxel/topotecan
Hepatocellular Carcinoma
- Dose: 15 mg/kg IV every 3 weeks
- With: Atezolizumab 1200 mg IV every 3 weeks
- Continue: Until disease progression or unacceptable toxicity
Infusion Details
Administration Guidelines:
- First infusion: Over 90 minutes with close monitoring
- Second infusion: If first dose tolerated well, give over 60 minutes
- Subsequent infusions: If 60-minute infusion tolerated, can give over 30 minutes
- Do NOT give as IV push or bolus
- Timing with chemotherapy: Give bevacizumab AFTER chemotherapy in the same visit
- No dose reductions: Unlike chemotherapy, bevacizumab dose is typically not reduced. If toxicity occurs, hold or discontinue
Side Effects and Management
BLACK BOX WARNINGS - Potentially Fatal Side Effects:
- Gastrointestinal perforation: Hole in the intestines (2-3% risk, can be fatal)
- Surgery/wound healing complications: Impaired healing, dehiscence (wound opening)
- Severe or fatal hemorrhage: Bleeding including pulmonary hemorrhage, GI bleeding, CNS bleeding
Most Common Side Effects
1. Hypertension (High Blood Pressure) - VERY COMMON
Incidence and Management:
- Incidence: 25-40% develop new or worsening hypertension; 5-15% severe
- Mechanism: VEGF normally helps keep blood vessels dilated; blocking it causes vasoconstriction
- Monitoring: Check blood pressure before EVERY infusion. Home monitoring recommended
- Target: Keep BP <140/90 mmHg (or <130/80 if diabetic/kidney disease)
- Treatment:
- Usually managed with standard BP medications (ACE inhibitors, calcium channel blockers, diuretics)
- May need multiple medications
- Hold bevacizumab if BP >150/100 despite medications
- Discontinue if hypertensive crisis or hypertensive encephalopathy
- Home monitoring: Check BP twice weekly at home, keep a log
2. Proteinuria (Protein in Urine)
- Incidence: 20-40% develop some proteinuria; 3-8% severe (nephrotic syndrome)
- Monitoring: Urine dipstick before each infusion
- If ≥2+ on dipstick: Get 24-hour urine collection to measure protein
- Hold bevacizumab if: Protein ≥2 grams per 24 hours
- Discontinue if: Nephrotic syndrome develops (protein >3.5 g/day + edema)
- Usually reversible: Proteinuria improves after stopping bevacizumab
3. Bleeding and Hemorrhage
Ranges from Minor to Life-Threatening:
- Minor bleeding (common 20-40%): Nosebleeds, bleeding gums, easy bruising
- Serious bleeding (1-5%): GI bleeding, pulmonary hemorrhage (coughing blood), CNS bleeding
- Highest risk groups:
- Squamous cell lung cancer (why it's contraindicated)
- Brain metastases
- Recent hemoptysis (coughing blood)
- On anticoagulation
- Call doctor immediately for: Any significant bleeding, coughing blood, black tarry stools, severe headache
4. Gastrointestinal Perforation - MEDICAL EMERGENCY
Rare but Potentially Fatal (2-3% overall risk):
- What it is: Hole in the stomach or intestines → abdominal infection (peritonitis)
- Risk factors: Prior abdominal surgery, diverticulitis, inflammatory bowel disease, bowel obstruction, intra-abdominal tumor
- Timing: Can occur any time but median ~6 months into treatment
- Symptoms:
- Severe abdominal pain (new or worsening)
- Nausea and vomiting
- Fever
- Constipation or inability to pass gas
- Treatment: Emergency surgery, discontinue bevacizumab permanently
- Action: Severe abdominal pain while on bevacizumab = GO TO ER
5. Wound Healing Complications
VEGF is Essential for Normal Wound Healing:
- Problem: Bevacizumab impairs wound healing, increasing risk of wound dehiscence (opening), infections, fistulas
- Critical timing rules:
- Before surgery: Stop bevacizumab at least 4 weeks (preferably 6-8 weeks) before elective surgery
- After surgery: Do not resume bevacizumab until surgical incision fully healed (typically 4+ weeks)
- For minor procedures: Discuss with oncologist and surgeon
- If wound dehiscence occurs: Discontinue bevacizumab permanently
6. Arterial Thromboembolic Events (Blood Clots in Arteries)
- Incidence: 2-5% (stroke, heart attack, angina)
- Higher risk if: Age >65, prior history of arterial clots, diabetes, smoking
- Symptoms to report immediately: Chest pain, sudden weakness/numbness, speech problems, vision changes
- Discontinue permanently if arterial thromboembolism occurs
7. Reversible Posterior Leukoencephalopathy Syndrome (RPLS)
- Incidence: Rare (<1%)
- What it is: Brain swelling syndrome causing neurologic symptoms
- Symptoms: Severe headache, seizures, confusion, vision changes, altered consciousness
- Diagnosis: MRI shows characteristic changes
- Treatment: Discontinue bevacizumab, control BP, supportive care
- Usually reversible if recognized early
Common but Less Serious Side Effects
- Fatigue (40-60%): Can be significant
- Headache (20-30%): Usually mild-moderate
- Diarrhea (20-40%): Often from concurrent chemotherapy
- Nausea (20-30%): Usually mild
- Loss of appetite (30-40%)
- Stomatitis (mouth sores) (15-30%)
- Skin changes (10-20%): Dry skin, rash
- Hand-foot syndrome (10-15%): More common when combined with capecitabine
- Changes in voice (hoarseness) (5-10%)
Special Considerations
- Bone marrow suppression: Bevacizumab alone does NOT cause low blood counts, but chemotherapy given with it does
- No hair loss: Bevacizumab does not cause hair loss (but concurrent chemotherapy may)
- Ovarian failure: May accelerate ovarian failure in premenopausal women (especially with chemotherapy)
- Congestive heart failure: Rare; increased risk if prior anthracycline exposure
Monitoring During Treatment
Before EVERY Infusion
| Test/Check |
Purpose |
Action if Abnormal |
| Blood pressure |
Detect hypertension |
Hold if >150/100; start/adjust BP meds |
| Urine protein (dipstick) |
Detect proteinuria |
If ≥2+, get 24-hour urine; hold if ≥2g/24h |
| Recent surgeries/procedures |
Wound healing assessment |
Ensure 4+ weeks from surgery, wound healed |
| New symptoms |
Detect complications early |
Address bleeding, pain, neurologic changes |
Periodic Monitoring
- CBC: Before each cycle (for concurrent chemotherapy)
- Comprehensive metabolic panel: Periodically (kidney function)
- Home BP monitoring: Twice weekly recommended
- Imaging: Per standard schedule for cancer type (usually every 2-3 months)
How Well Does Bevacizumab Work?
Colorectal Cancer - Most Robust Evidence
First-Line Metastatic Colorectal Cancer:
- E3200 Trial: IFL + bevacizumab vs. IFL alone
- Median survival: 20.3 vs. 15.6 months (nearly 5-month improvement)
- Progression-free survival: 10.6 vs. 6.2 months
- Response rate: 45% vs. 35%
- With modern regimens (FOLFOX/FOLFIRI): Median survival now 24-30 months with bevacizumab
- Impact: Bevacizumab became standard first-line therapy for metastatic colorectal cancer
Lung Cancer (Non-Squamous NSCLC)
E4599 Trial:
- Carboplatin/paclitaxel + bevacizumab vs. chemo alone:
- Median survival: 12.3 vs. 10.3 months
- 1-year survival: 51% vs. 44%
- Note: Excluded squamous cell due to bleeding risk
Ovarian Cancer
- GOG-218 (newly diagnosed): Improved PFS (14.1 vs. 10.3 months) but not overall survival
- AURELIA (platinum-resistant): PFS 6.7 vs. 3.4 months; quality of life benefits
Glioblastoma
- Recurrent disease: Response rate 25-30% as single agent
- PFS benefit: Median PFS ~4 months (vs. 1.5 months historical)
- No overall survival benefit demonstrated in randomized trials
- Clinical benefit: Reduces cerebral edema, may allow steroid reduction, improves symptoms
Hepatocellular Carcinoma
IMbrave150 Trial - NEW Standard of Care:
- Atezolizumab + bevacizumab vs. sorafenib:
- Median survival: 19.2 vs. 13.4 months
- 1-year survival: 67% vs. 55%
- PFS: 6.8 vs. 4.3 months
- Impact: Replaced sorafenib as first-line standard
Important Limitation
Bevacizumab typically improves progression-free survival consistently but overall survival benefit is more variable and often modest (2-5 months). Quality of life and symptom control can also be important benefits.
How Long is Treatment?
Duration Varies by Cancer Type
- Colorectal cancer:
- Often continued until disease progression
- Some patients continue for years if tolerating and responding
- Can use as maintenance after stopping chemotherapy
- Lung cancer:
- Usually 4-6 cycles with chemotherapy
- Then continue bevacizumab alone as maintenance
- Continue until progression
- Ovarian cancer:
- Usually up to 22 cycles total (about 15 months)
- Includes treatment phase + maintenance phase
- Glioblastoma:
- Continue until progression (median 4-6 months)
- HCC:
- Continue with atezolizumab until progression or toxicity
Drug Interactions and Precautions
Important Interactions
- Sunitinib (Sutent): Combination causes microangiopathic hemolytic anemia. DO NOT use together
- Anticoagulants/antiplatelets: Increased bleeding risk. Use with caution; monitor closely
- Chemotherapy: Bevacizumab may increase toxicity of concurrent chemotherapy (especially capecitabine - hand-foot syndrome)
- Immunotherapy: Can be safely combined (atezolizumab + bevacizumab is standard for HCC)
Contraindications and Cautions
DO NOT use bevacizumab if:
- Recent hemoptysis (>2.5 mL blood)
- Serious/untreated infection
- Recent surgery (<28 days) or planned surgery (<28 days)
- Uncontrolled hypertension
- Recent GI perforation or fistula
- Active GI bleeding
- Pregnancy: Category C - can cause fetal harm. Effective contraception required during treatment and for 6 months after last dose
- Breastfeeding: Do not breastfeed during treatment and for 6 months after last dose
- Elderly: Increased risk of arterial thromboembolic events
- Renal impairment: Use with caution; may worsen kidney function
Cost and Insurance Coverage
Medication Cost
- Bevacizumab (Avastin): $3,000-6,000 per dose depending on dose and body weight
- Biosimilars: Mvasi, Zirabev (slightly less expensive, ~15-30% discount)
- Per month cost: $6,000-12,000+ depending on dosing schedule
- Annual cost: $100,000-150,000+ for continuous treatment
Insurance Coverage
- Coverage: Generally covered for FDA-approved indications
- Prior authorization: Usually required
- Patient responsibility: Can be substantial; many patients need financial assistance
Financial Assistance
- Genentech Access Solutions: 1-888-249-4918 (copay assistance and patient assistance programs)
- Biosimilar manufacturer programs: Available for Mvasi and Zirabev
- CancerCare Co-Payment Assistance: 1-866-552-6729
- Patient Advocate Foundation: 1-800-532-5274
Biosimilars
Biosimilar Options Available:
- Mvasi (bevacizumab-awwb): FDA-approved 2017
- Zirabev (bevacizumab-bvzr): FDA-approved 2019
- What are biosimilars? Highly similar to Avastin with no clinically meaningful differences in safety or effectiveness
- Benefits: Lower cost (though still expensive); same clinical outcomes
- Interchangeability: Can be substituted for Avastin; insurance often prefers biosimilars
Frequently Asked Questions
Q: How is bevacizumab different from chemotherapy?
A: Bevacizumab is a targeted therapy, NOT traditional chemotherapy. Chemotherapy directly kills rapidly dividing cells (including cancer cells and some normal cells like hair follicles). Bevacizumab is a monoclonal antibody that specifically blocks VEGF, starving tumors by preventing blood vessel formation. Because it targets a specific protein rather than all dividing cells, it has a different side effect profile - no hair loss, no bone marrow suppression, but unique issues like hypertension, proteinuria, and bleeding risk. It's almost always used WITH chemotherapy, not instead of it.
Q: Why is my blood pressure suddenly high?
A: Hypertension is one of the most common side effects of bevacizumab, occurring in 25-40% of patients. VEGF normally helps blood vessels stay dilated (relaxed). When bevacizumab blocks VEGF, blood vessels constrict, raising blood pressure. This is actually somewhat expected and manageable. Your oncologist will monitor your BP before every infusion and may prescribe BP medications. Monitor your BP at home twice weekly and report values >140/90. The good news: BP usually returns to normal or near-normal after stopping bevacizumab.
Q: I'm scheduled for dental work. Should I tell my dentist I'm on bevacizumab?
A: YES, always tell your dentist and any doctor performing procedures that you're on bevacizumab. For minor dental work (cleaning, fillings), usually okay to proceed with caution. For extractions or oral surgery, there's increased risk of bleeding and poor wound healing. Your dentist and oncologist should coordinate timing - ideally schedule dental work between infusions when drug levels are lower, or consider holding bevacizumab for 4+ weeks before major dental surgery. The wound healing concern is real but manageable with proper planning.
Q: Can I have surgery while on bevacizumab?
A: Elective surgery requires careful timing. Stop bevacizumab at least 4 weeks (preferably 6-8 weeks) before surgery. The drug impairs wound healing because VEGF is essential for healing. After surgery, wait until the incision is completely healed (typically 4+ weeks, but surgeon's assessment is critical) before restarting. For emergency surgery, understand there's increased risk of wound complications. Always coordinate between your surgeon and oncologist. Minor procedures (port access, skin biopsies) are generally okay with shorter intervals.
Q: I have protein in my urine. Is this serious?
A: Proteinuria (protein in urine) is common with bevacizumab (20-40%). Most cases are mild and not concerning. Your team monitors with urine dipstick before each infusion. If you have 2+ or more on dipstick, they'll do a 24-hour urine collection to measure exact protein amount. Bevacizumab is held if protein ≥2 grams/24 hours and discontinued if nephrotic syndrome develops (protein >3.5 g/day with swelling). The good news: proteinuria usually improves or resolves after stopping bevacizumab. Kidney damage from bevacizumab is typically reversible.
Q: What's the difference between Avastin and the biosimilars (Mvasi, Zirabev)?
A: Biosimilars (Mvasi and Zirabev) are highly similar to brand-name Avastin with no clinically meaningful differences in safety, purity, or effectiveness. Think of them like generic versions, though technically they're "biosimilars" not "generics" because they're made from living cells (more complex than chemical drugs). They work the same way, have the same side effects, and same clinical outcomes. Main difference: cost is somewhat lower (though still very expensive). Insurance companies often prefer biosimilars. All three are FDA-approved and medically appropriate.
Q: I'm getting nosebleeds. Should I stop bevacizumab?
A: Minor nosebleeds are very common with bevacizumab (happens in 20-40%). Usually they're not dangerous and don't require stopping treatment. Management: use saline nasal spray or gel to keep nasal passages moist, humidifier at night, avoid nose-picking. However, tell your doctor about any bleeding. STOP treatment and call immediately if: coughing up blood (hemoptysis), severe/uncontrollable nosebleeds, blood in stool (black/tarry stools or bright red blood), severe bruising, or any significant bleeding. The distinction between minor expected bleeding and serious hemorrhage is important.
Q: Does bevacizumab cure cancer?
A: For metastatic cancer, bevacizumab does not cure but helps control the disease and extend life. It slows tumor growth by cutting off blood supply and makes chemotherapy work better. In colorectal cancer, adding bevacizumab extends median survival by 2-5 months (from ~20 to ~24-25 months on average). Some patients respond very well and live much longer. Benefits vary by cancer type. In glioblastoma, it improves progression-free survival and symptoms but hasn't shown overall survival benefit. The goal is disease control, prolonging life, and maintaining quality of life.
Q: I have severe abdominal pain. What should I do?
A: Severe abdominal pain while on bevacizumab is a RED FLAG for possible GI perforation (hole in intestines), which is a medical emergency. GO TO THE EMERGENCY ROOM immediately. Don't wait. GI perforation occurs in 2-3% of patients and can be fatal if not treated urgently. Other warning signs: fever, nausea/vomiting, inability to pass gas or stool. Even if it turns out to be something else (constipation, gas, unrelated issue), severe abdominal pain needs immediate evaluation. Better safe than sorry with this particular side effect.
Q: Will bevacizumab cause hair loss?
A: No, bevacizumab itself does NOT cause hair loss. It's a targeted therapy that doesn't affect hair follicles. However, bevacizumab is almost always given WITH chemotherapy, and many chemotherapy drugs DO cause hair loss (like docetaxel, paclitaxel, doxorubicin, irinotecan). So if you're experiencing hair loss, it's from the chemotherapy component of your treatment, not the bevacizumab. When bevacizumab is used alone (like maintenance therapy after stopping chemo), you won't lose hair from it.
Living with Bevacizumab Treatment
Home Blood Pressure Monitoring
- Get a home BP cuff: Automatic upper-arm cuff recommended (more accurate than wrist)
- Check twice weekly: Same time of day, sitting quietly for 5 minutes first
- Keep a log: Bring to appointments
- Call if BP >150/100 or symptoms (severe headache, vision changes, chest pain)
Preventing Complications
- Avoid NSAIDs if possible: Increased bleeding risk; use acetaminophen instead
- Good dental hygiene: Soft toothbrush, gentle flossing, regular dental checkups
- Moisturize nasal passages: Saline spray for nosebleed prevention
- Watch for signs of infection: Notify doctor of fever, persistent cough
- Communicate about upcoming procedures/surgeries: Plan timing carefully
When to Call Your Doctor
Contact your oncology team or go to ER immediately for:
- Severe abdominal pain
- Coughing up blood
- Blood in stool (black/tarry or bright red)
- Severe headache, confusion, vision changes, seizures
- Chest pain or sudden shortness of breath
- Sudden weakness, numbness, speech problems (stroke symptoms)
- Uncontrolled bleeding from any source
- Signs of wound dehiscence (surgical wound opening)
Support Resources
- Genentech (manufacturer): 1-888-249-4918
- American Cancer Society: 1-800-227-2345
- CancerCare: 800-813-4673
- Disease-specific organizations: Based on your cancer type
Medical Disclaimer: This information is for educational purposes only and is not a substitute for professional medical advice, diagnosis, or treatment. Bevacizumab has serious risks including potentially fatal complications (GI perforation, severe bleeding, arterial blood clots). Every patient's situation is unique. Always consult your oncologist and healthcare team about your specific condition, treatment plan, and any questions or concerns you have. If you have a medical emergency, call 911 or go to the nearest emergency room immediately.
Sources: This guide is based on FDA prescribing information for Avastin and biosimilars, National Comprehensive Cancer Network (NCCN) guidelines, landmark clinical trials (E2100, E4599, GOG-218, AURELIA, IMbrave150), peer-reviewed medical literature on anti-angiogenic therapy, and clinical practice guidelines from major cancer centers. Content reviewed for medical accuracy and updated to reflect current standards of care as of 2025.