Targeted Therapy: Complete Treatment Guide

Written by: Dr. Michael Chen, MD, PhD | Reviewed by: Dr. Sarah Johnson, MD | Last updated: January 25, 2026

Quick Facts About Targeted Therapy

  • Targets specific proteins, genes, or pathways in cancer cells
  • Requires biomarker/molecular testing before starting
  • Generally more precise with fewer side effects than chemotherapy
  • Available as oral pills or intravenous infusions
  • Resistance typically develops after 9-18 months

What is Targeted Therapy?

Targeted therapy is a type of cancer treatment that uses drugs designed to target specific proteins, genes, or molecular pathways that contribute to cancer growth and survival. Unlike chemotherapy, which affects all rapidly dividing cells, targeted therapies are designed to attack cancer cells more precisely while causing less damage to normal cells.

This approach represents the foundation of precision medicine - matching specific treatments to the unique molecular characteristics of each patient's cancer. Targeted therapy has revolutionized treatment for many cancer types, particularly lung cancer, breast cancer, melanoma, and chronic myeloid leukemia.

Key Points

  • Works only if your cancer has specific molecular targets (biomarkers)
  • Requires molecular/genetic testing of tumor tissue or blood
  • Often combined with chemotherapy, immunotherapy, or other treatments
  • Generally causes different side effects than chemotherapy
  • Drug resistance is common - median response duration 9-18 months
  • Next-generation drugs available when resistance develops

How Targeted Therapy Works

Targeted therapies interfere with specific molecules involved in cancer growth, progression, and spread:

Mechanisms of Action

  • Signal blocking: Prevents growth signals from reaching cancer cells
  • Receptor inhibition: Blocks receptors on cancer cell surface (EGFR, HER2, ALK)
  • Angiogenesis inhibition: Prevents new blood vessel formation that feeds tumors (VEGF inhibitors)
  • Cell cycle disruption: Stops cancer cells from dividing (CDK4/6 inhibitors)
  • DNA repair blocking: Prevents cancer cells from repairing damaged DNA (PARP inhibitors)
  • Protein degradation: Destroys specific proteins cancer cells need (proteasome inhibitors)

The key difference from chemotherapy: targeted therapies exploit specific vulnerabilities in cancer cells that normal cells don't have, leading to more selective cancer cell killing.

Precision Medicine Approach

Your oncologist will order molecular testing (genomic profiling, next-generation sequencing, or specific biomarker tests) to identify whether your cancer has targetable mutations or alterations. Not all cancers have targetable changes, and different cancer types have different common targets.

Types of Targeted Therapy

Small Molecule Inhibitors

Small drugs that can enter cells and interfere with specific proteins inside the cell.

  • Usually taken as oral pills
  • Examples: Tyrosine kinase inhibitors (TKIs)
  • Daily administration at home
  • Convenient but requires adherence

Monoclonal Antibodies

Large protein molecules that bind to specific targets on the cancer cell surface.

  • Given intravenously (IV infusion)
  • End in "-mab" (trastuzumab, bevacizumab)
  • Require clinic visits
  • Usually every 2-3 weeks

Antibody-Drug Conjugates

Monoclonal antibodies linked to chemotherapy drugs, delivering chemo directly to cancer cells.

  • Combines targeting with cytotoxic payload
  • IV administration
  • T-DM1 (Kadcyla) for HER2+ breast cancer

Combination Approaches

Often combined with other treatments for synergistic effects.

  • Targeted + chemotherapy
  • Targeted + immunotherapy
  • Dual targeted therapy
  • Sequential targeted agents

Major Drug Categories

Tyrosine Kinase Inhibitors (TKIs)

The largest class of targeted therapies, blocking enzymes that promote cell growth:

  • EGFR inhibitors: Erlotinib, gefitinib, osimertinib (lung cancer)
  • ALK inhibitors: Crizotinib, alectinib, lorlatinib (ALK+ lung cancer)
  • ROS1 inhibitors: Crizotinib, entrectinib (ROS1+ lung cancer)
  • BRAF inhibitors: Vemurafenib, dabrafenib (BRAF-mutant melanoma)
  • HER2 inhibitors: Lapatinib, neratinib (HER2+ breast cancer)
  • VEGF inhibitors: Sunitinib, pazopanib, cabozantinib (kidney cancer)
  • BCR-ABL inhibitors: Imatinib, dasatinib, nilotinib (CML)
  • FLT3 inhibitors: Midostaurin, gilteritinib (FLT3+ AML)
  • JAK inhibitors: Ruxolitinib (myelofibrosis)

mTOR Inhibitors

Block the mTOR protein involved in cell growth:

  • Everolimus (breast cancer, kidney cancer, neuroendocrine tumors)
  • Temsirolimus (kidney cancer)

CDK4/6 Inhibitors

Prevent cancer cells from dividing:

  • Palbociclib (Ibrance)
  • Ribociclib (Kisqali)
  • Abemaciclib (Verzenio)
  • Used for hormone receptor-positive breast cancer

PARP Inhibitors

Block DNA repair in cancer cells with BRCA mutations:

  • Olaparib (Lynparza) - ovarian, breast, pancreatic, prostate cancer
  • Rucaparib (Rubraca) - ovarian cancer
  • Niraparib (Zejula) - ovarian cancer
  • Talazoparib (Talzenna) - breast cancer

Proteasome Inhibitors

Prevent breakdown of proteins in cancer cells:

  • Bortezomib (Velcade) - multiple myeloma
  • Carfilzomib (Kyprolis) - multiple myeloma
  • Ixazomib (Ninlaro) - multiple myeloma

Biomarker Testing

Before starting targeted therapy, your cancer must be tested to determine if it has the specific molecular targets. This is called biomarker testing, molecular profiling, or genomic testing.

Types of Testing

  • Single gene tests: Test for one specific mutation (e.g., EGFR mutation test)
  • Multi-gene panels: Test for multiple genes simultaneously
  • Next-generation sequencing (NGS): Comprehensive genomic profiling of hundreds of genes
  • Immunohistochemistry (IHC): Tests for protein expression (e.g., HER2, PD-L1)
  • FISH testing: Fluorescence test for gene amplification or rearrangement
  • Liquid biopsy: Blood test for circulating tumor DNA (ctDNA)

When Testing is Done

At Diagnosis

Comprehensive molecular testing on tumor biopsy or surgical specimen

At Progression

Repeat testing if cancer grows on targeted therapy to identify resistance mechanisms

Serial Monitoring

Liquid biopsies to monitor response and detect emerging resistance

Important Testing Notes

  • Results typically take 1-3 weeks
  • Not all cancers have targetable mutations (about 30-40% of lung cancers, 60-70% don't)
  • Insurance usually covers testing for advanced cancers
  • Request comprehensive NGS panel rather than single gene tests when possible
  • Keep a copy of your molecular testing results

How Targeted Therapy is Given

Oral Medications (Pills)

Many targeted therapies are oral medications taken at home:

  • Advantages: Convenient, no clinic visits for drug administration, flexibility
  • Challenges: Requires adherence, managing side effects at home, cost (often expensive copays)
  • Timing: Some must be taken on empty stomach, others with food - follow instructions carefully
  • Storage: Most require room temperature storage away from heat/moisture

Oral Medication Adherence Tips

  • Set daily alarms as reminders
  • Use pill organizers
  • Keep medication with you when traveling
  • Never double up if you miss a dose - contact your team
  • Don't stop without consulting your oncologist
  • Keep medication in original bottles with labels

Intravenous (IV) Infusions

Monoclonal antibodies and some other targeted drugs are given IV:

  • Frequency: Usually every 2-3 weeks
  • Duration: 30 minutes to several hours
  • Location: Infusion center or clinic
  • Monitoring: Vital signs checked, observation for infusion reactions

Treatment Duration

  • Continuous treatment: Most targeted therapies are given continuously until progression or intolerable side effects
  • No defined end date: Unlike chemotherapy cycles, treatment continues as long as it's working
  • Dose modifications: Doses may be reduced or temporarily held for side effects
  • Treatment breaks: Some patients take scheduled breaks or intermittent dosing

Common Targeted Therapy Drugs

Drug (Brand Name) Target Cancer Types Route
Imatinib (Gleevec) BCR-ABL Chronic myeloid leukemia (CML), GIST Oral
Erlotinib (Tarceva) EGFR EGFR-mutant lung cancer Oral
Osimertinib (Tagrisso) EGFR (including T790M) EGFR-mutant lung cancer Oral
Crizotinib (Xalkori) ALK, ROS1 ALK+ or ROS1+ lung cancer Oral
Alectinib (Alecensa) ALK ALK+ lung cancer Oral
Vemurafenib (Zelboraf) BRAF V600E BRAF-mutant melanoma Oral
Dabrafenib (Tafinlar) BRAF V600 BRAF-mutant melanoma, lung cancer Oral
Trastuzumab (Herceptin) HER2 HER2+ breast, gastric cancer IV
Pertuzumab (Perjeta) HER2 HER2+ breast cancer IV
Bevacizumab (Avastin) VEGF Colorectal, lung, kidney, ovarian cancer IV
Palbociclib (Ibrance) CDK4/6 HR+ breast cancer Oral
Olaparib (Lynparza) PARP BRCA-mutant breast, ovarian, pancreatic, prostate Oral
Sunitinib (Sutent) Multi-kinase (VEGF, PDGF) Kidney cancer, GIST Oral
Cetuximab (Erbitux) EGFR Colorectal, head & neck cancer (KRAS wild-type) IV
Entrectinib (Rozlytrek) NTRK, ROS1, ALK NTRK fusion-positive solid tumors Oral

Note: This is not a complete list. Many other targeted therapies are available and new drugs are constantly being approved.

Side Effects Management

When to Call Your Doctor

  • Severe diarrhea (more than 6 stools/day)
  • Severe rash or blistering
  • High blood pressure (above 150/100)
  • Chest pain or difficulty breathing
  • Severe abdominal pain
  • Signs of liver problems (yellowing of skin/eyes, dark urine)
  • Uncontrolled bleeding
  • Severe headache or vision changes

Targeted therapies generally cause different side effects than chemotherapy. Side effects vary significantly depending on the specific drug and target. Most patients do NOT experience hair loss or severe nausea.

Common Side Effects by Drug Class

Diarrhea

Very Common

Especially with EGFR inhibitors, multi-kinase inhibitors. Managed with loperamide, diet modification, hydration.

Prevention: Avoid dairy, fiber, spicy foods initially

Skin Rash

Very Common

Acne-like rash with EGFR inhibitors. Actually correlates with treatment effectiveness.

Management: Gentle cleansers, moisturizers, topical antibiotics, oral antibiotics if severe

Hypertension

Common

Especially with VEGF inhibitors (bevacizumab, sunitinib). Requires blood pressure monitoring.

Management: Blood pressure medications, regular monitoring

Hand-Foot Syndrome

Common

Redness, pain, blistering of palms and soles with multi-kinase inhibitors.

Prevention: Moisturize hands/feet, avoid friction, cool compresses

Fatigue

Common

Less severe than chemotherapy-related fatigue but still significant for some patients.

Management: Energy conservation, light exercise, adequate sleep

Liver Toxicity

Serious

Elevated liver enzymes common, requires regular blood test monitoring.

Monitoring: Liver function tests every 2-4 weeks initially

Cardiac Effects

Serious

Decreased heart function with HER2 inhibitors (trastuzumab). QT prolongation with some TKIs.

Monitoring: Baseline and periodic echocardiograms, EKGs

Bleeding Risk

Serious

Increased with VEGF inhibitors. Avoid surgery for 4-6 weeks.

Precautions: Report any unusual bleeding, avoid blood thinners without approval

Thyroid Problems

Common

Hypothyroidism with multi-kinase inhibitors (sunitinib, sorafenib).

Monitoring: Regular thyroid function tests, thyroid replacement if needed

Vision Changes

Uncommon

Blurred vision, floaters with some TKIs (MEK inhibitors).

Action: Report changes immediately, eye exams

Mouth Sores

Common

Especially with mTOR inhibitors (everolimus).

Management: Gentle oral care, magic mouthwash, avoid irritants

Nausea

Common

Generally milder than chemotherapy-induced nausea.

Management: Take with food (if allowed), anti-nausea medications

Managing Side Effects

  • Don't suffer silently: Report all side effects - many are manageable with dose adjustments or supportive medications
  • Dose modifications: Temporary dose reductions or treatment breaks can help manage side effects
  • Supportive care: Dermatology, cardiology, gastroenterology consultations may be helpful
  • Keep taking medication: Don't stop without consulting your oncologist, even if you feel fine

Drug Resistance

One of the major challenges with targeted therapy is the development of resistance - when cancer cells develop ways to evade the drug's effects.

Why Resistance Develops

  • Secondary mutations: Cancer develops new mutations that bypass the drug (e.g., T790M mutation after first-generation EGFR inhibitors)
  • Alternative pathways: Cancer activates different growth pathways
  • Target amplification: Cancer produces more of the target protein
  • Histologic transformation: Cancer changes cell type (e.g., adenocarcinoma to small cell)

Timeline

Median duration of response varies by drug and cancer type:

  • EGFR inhibitors (lung): 9-18 months
  • ALK inhibitors (lung): 10-34 months (varies by generation)
  • Imatinib (CML): Many years with proper response
  • BRAF inhibitors (melanoma): 6-12 months (longer with combination therapy)
  • HER2 inhibitors (breast): Variable, often longer with combination therapy

Overcoming Resistance

Next-Generation Drugs

Newer drugs designed to overcome specific resistance mechanisms

  • Osimertinib for T790M resistance
  • Lorlatinib for ALK resistance mutations
  • Multiple generations available for many targets

Combination Therapy

Using multiple drugs together to block resistance pathways

  • BRAF + MEK inhibitors
  • Targeted therapy + immunotherapy
  • Dual HER2 blockade

Rebiopsy

Testing tumor tissue at progression to identify resistance mechanisms

  • Tissue biopsy or liquid biopsy
  • Guides next treatment selection
  • May reveal new targetable alterations

Switch Strategies

Changing to different treatment approaches

  • Chemotherapy
  • Immunotherapy
  • Clinical trials
  • Different targeted agent

Importance of Repeat Testing

When cancer progresses on targeted therapy, repeat molecular testing (tissue or liquid biopsy) is crucial. This can identify the specific resistance mechanism and guide selection of the next treatment. New actionable mutations may also emerge.

Monitoring & Follow-up

Regular Monitoring Schedule

Before Starting

  • Baseline imaging (CT, PET, MRI)
  • Blood tests (CBC, liver/kidney function)
  • EKG and echocardiogram (for certain drugs)
  • Thyroid function tests
  • Blood pressure baseline

During Treatment - First Month

  • Blood tests every 2 weeks
  • Blood pressure checks weekly (for VEGF inhibitors)
  • Symptom assessment
  • Side effect monitoring

Ongoing - Every 2-3 Months

  • Imaging scans to assess response
  • Blood tests monthly or as needed
  • Clinical examination
  • Cardiac monitoring (if applicable)

Response Assessment

How doctors determine if treatment is working:

  • CT/PET scans: Measure tumor size, look for new lesions
  • Tumor markers: Blood tests for specific cancer markers (CEA, CA 19-9, etc.)
  • Liquid biopsy: Circulating tumor DNA levels
  • Clinical improvement: Symptom relief, improved function
  • Physical examination: Palpable masses, lymph nodes

Laboratory Monitoring

Test Frequency Purpose
Liver function tests (AST, ALT, bilirubin) Every 2-4 weeks initially, then monthly Detect hepatotoxicity
Complete blood count (CBC) Monthly or as needed Monitor for cytopenias
Thyroid function (TSH) Every 2-3 months Detect hypothyroidism
Kidney function (creatinine) Monthly Monitor renal function
EKG Baseline and as needed Monitor for QT prolongation
Echocardiogram Every 3-4 months (HER2 inhibitors) Monitor heart function

Cost Considerations

Targeted therapies are among the most expensive cancer treatments, with significant financial implications for patients.

Cost Range

  • Monthly cost: $10,000 - $15,000+ without insurance
  • Annual cost: $120,000 - $180,000+
  • Patient copays: Can range from $0 to $10,000+ per month depending on insurance
  • Specialty pharmacy: Most oral targeted therapies require specialty pharmacy

Financial Assistance Options

Manufacturer Programs

Most drug companies offer copay assistance and patient assistance programs

  • Copay cards (commercial insurance)
  • Free drug programs (uninsured)
  • Foundation assistance

Insurance Coverage

Work with your insurance and care team

  • Prior authorization required
  • Appeal denials
  • Request medical exception
  • Consider Medicare Part D

Independent Foundations

Nonprofit organizations providing financial assistance

  • Patient Advocate Foundation
  • HealthWell Foundation
  • Chronic Disease Fund
  • Cancer organizations

Hospital Programs

Resources through your treatment center

  • Financial counselors
  • Social workers
  • Charity care programs
  • Payment plans

Important Financial Planning

  • Discuss costs BEFORE starting treatment
  • Understand your insurance coverage (deductible, out-of-pocket max)
  • Apply for assistance programs early - don't wait until bills accumulate
  • Ask about generic alternatives (available for some older drugs like imatinib)
  • Consider clinical trials - drugs are provided free
  • Keep detailed records of all expenses for tax purposes

Frequently Asked Questions

How is targeted therapy different from chemotherapy?

Targeted therapy attacks specific molecular targets in cancer cells, while chemotherapy affects all rapidly dividing cells. Targeted therapy generally causes fewer systemic side effects (less nausea, hair loss) but has its own unique side effects. It requires molecular testing to identify appropriate targets.

Will targeted therapy cure my cancer?

In most cases, targeted therapy controls cancer rather than curing it. Some exceptions include chronic myeloid leukemia (CML) with BCR-ABL inhibitors, where many patients achieve long-term remission. For most solid tumors, resistance eventually develops and cancer progresses, but targeted therapy can provide significant periods of disease control.

What happens if my cancer doesn't have targetable mutations?

Not all cancers have actionable targets. If comprehensive molecular testing doesn't reveal targetable alterations, other treatment options include chemotherapy, immunotherapy (if appropriate), clinical trials, or combination approaches. Your oncologist will develop an alternative treatment plan.

Why do I need to keep taking it if my cancer is responding?

Targeted therapy requires continuous treatment to maintain response. If you stop, cancer cells that aren't actively dividing (dormant cells) or resistant clones will likely start growing again. The medication keeps suppressing cancer growth. Unlike chemotherapy cycles that have a defined end, targeted therapy is typically continued indefinitely as long as it's working.

Can I take breaks from targeted therapy?

Generally, continuous treatment is recommended. However, some patients may take treatment breaks for specific reasons (major surgery, severe side effects, patient preference). Discuss with your oncologist - some drugs and situations may allow breaks, but there's risk of progression. Intermittent dosing schedules are being studied for some drugs.

What if I miss a dose?

Don't double up. Follow specific instructions for your medication - some allow taking a missed dose if it's been less than a certain number of hours, others recommend skipping and taking the next dose as scheduled. Call your oncology team for guidance. Never stop taking medication on your own.

Can I drink alcohol while on targeted therapy?

Depends on the specific drug. Many targeted therapies are metabolized by the liver, and alcohol can increase liver stress. Some drugs have specific warnings about alcohol. Discuss with your oncologist - moderate use may be acceptable for some drugs, while others require complete avoidance.

How will I know when the drug stops working?

Regular imaging scans (usually every 2-3 months) monitor tumor response. Signs of progression include growing tumors, new lesions, rising tumor markers, or worsening symptoms. When progression is detected, your oncologist will discuss repeat testing to identify resistance mechanisms and next treatment options.

Are there any drug interactions I should worry about?

Yes, many targeted therapies have significant drug interactions, especially with medications metabolized by the same liver enzymes (CYP450 system). Always inform all your doctors about your cancer treatment. Be cautious with: antibiotics, antifungals, seizure medications, heart medications, grapefruit juice, and herbal supplements (especially St. John's Wort). Check with your oncology pharmacist before starting any new medications or supplements.

Can I travel while on oral targeted therapy?

Yes, with planning. Bring extra medication, keep it in carry-on luggage in original bottles, bring a copy of your prescription, and research medical facilities at your destination. Consider travel insurance. Ensure you have enough medication plus extra in case of travel delays. Some medications require specific storage conditions.

What about side effects that develop after months of treatment?

Some side effects appear or worsen with prolonged treatment (cumulative toxicity). Examples include hypothyroidism with multi-kinase inhibitors or cardiac dysfunction with HER2 inhibitors. This is why ongoing monitoring is important. Report new symptoms even if you've been on treatment for a long time. Dose adjustments may be needed.

Is targeted therapy covered by insurance?

Most insurance plans cover targeted therapy when medically necessary and biomarker testing confirms the target. However, prior authorization is usually required, and appeals may be necessary. Out-of-pocket costs can be substantial. Work with your treatment center's financial counselors and apply for assistance programs early in treatment.

Related Resources

Molecular Testing

Understanding genomic profiling and biomarker tests

Testing Guide

Immunotherapy

Another precision medicine approach

Learn More

Clinical Trials

Access to newer targeted therapies

Find Trials

Drug Database

Detailed information on specific targeted drugs

Search Drugs

Managing Side Effects

Comprehensive guides for targeted therapy side effects

Side Effects Hub

Financial Assistance

Resources for medication costs and copay assistance

Get Help

Medical Disclaimer: This information is educational only. Treatment decisions should be made with your oncology team based on your specific cancer type, molecular profile, and individual circumstances. Not all targeted therapies are appropriate for all cancers.