TIL Therapy: Your Immune Cells,
Already Fighting Your Cancer.
Tumor-Infiltrating Lymphocytes (TIL) therapy harvests the immune cells that have naturally recognized your tumor, expands them to billions in the lab, and returns them to fight with overwhelming force. The first cell therapy FDA-approved for a solid tumor.
The 5-Step TIL Therapy Process
Unlike CAR-T which engineers cells, TIL therapy uses your body's own tumor-reactive immune cells — already selected by nature to recognize your cancer.
Tumor Resection
A piece of tumor tissue is surgically removed. Ideal sites include accessible skin metastases, lymph nodes, or liver lesions.
TIL Isolation
In a GMP laboratory, tumor-infiltrating lymphocytes are extracted from the tumor fragments and selectively expanded.
Expansion (22-33 days)
TILs are cultured with high-dose IL-2, multiplying from thousands to 50-100+ billion cells — a massive army against your cancer.
Lymphodepletion
Patient receives cyclophosphamide + fludarabine chemotherapy for 3 days to eliminate competing immune cells and make "room" for TILs.
TIL Infusion + IL-2
Expanded TILs are infused intravenously over 30 minutes, followed by up to 12 doses of IL-2 over 5 days to sustain T-cell activity.
Real Numbers from the C-145-04 Pivotal Trial
Data from the landmark study that led to FDA approval. Published in the New England Journal of Medicine (2023).
- Kochenderfer JN et al. "Lifileucel in Advanced Melanoma." NEJM 2023;389:1300-1312.
- FDA Approval Letter: Amtagvi (lifileucel) — BLA 761251, February 16, 2024.
- ClinicalTrials.gov: NCT02360579 (C-145-04 pivotal trial).
- Zacharakis N et al. "Immune recognition of somatic mutations in cervical cancer." Nat Med 2023.
Who Qualifies for TIL Therapy?
TIL therapy has strict eligibility criteria. Honest assessment saves time, money, and false hope.
Strong Candidate If
- Unresectable or metastatic melanoma
- Progressed after PD-1 inhibitor (pembrolizumab, nivolumab)
- If BRAF V600-mutated: also progressed on BRAF ± MEK inhibitors
- ECOG performance status 0-1 (fully or mostly active)
- Adequate heart, lung, liver, and kidney function
- At least one resectable tumor site for TIL harvest
- Able to tolerate lymphodepletion chemotherapy
Not Suitable If
- No resectable tumor site (TILs must come from your tumor)
- ECOG performance status 3-4 (bedridden >50% of waking hours)
- Severe cardiac disease (LVEF <45%, uncontrolled arrhythmia)
- Severe pulmonary disease (DLCO <40%)
- Active uncontrolled infection
- Active autoimmune disease requiring immunosuppression
- Pregnancy or breastfeeding
Requires Expert Review If
- Non-melanoma solid tumors (cervical, head & neck, NSCLC, breast) — currently trial-only
- Age >70 years (case-by-case based on physiologic age)
- Prior stem cell transplant
- History of severe immune-related adverse events from prior immunotherapy
- Moderate organ dysfunction (may be correctable)
- Brain metastases (must be stable/treated first)
TIL Therapy Cost by Country
Self-pay international patient pricing. Does not include travel, accommodation, or companion expenses.
| Country | Cost Range (USD) | What's Included | Notes |
|---|---|---|---|
| 🇨🇳 China | $80,000 – $120,000 Clinical research programs | TIL manufacturing, lymphodepletion, infusion, IL-2, hospital stay | Multiple centers in Beijing, Shanghai, Guangzhou |
| 🇸🇬 Singapore | $100,000 – $150,000 Private centers | Full episode of care, English-speaking teams | Established TIL programs at major cancer centers |
| 🇺🇸 USA (Amtagvi) | $375,000+ Drug list price only | Drug only; hospital, ICU, IL-2 add $100K-$200K+ | Total episode often $500K-$700K. Insurance-dependent. |
| 🇩🇪 Germany | Limited availability Trial-based only | Varies by trial protocol | Mostly academic centers, clinical trial enrollment |
| 🇹🇷 Turkey | Under development Expected 2026-2027 | TBD | Several JCI-accredited centers preparing programs |
Costs above reflect the treatment episode (manufacturing + hospital stay + medications). They do NOT include: international airfare, accommodation for companion, pre-treatment diagnostics, post-treatment follow-up scans, or management of complications. Our coordination team provides a detailed, itemized estimate after case review.
From Submission to Infusion: 6-10 Weeks
TIL therapy requires more time than CAR-T due to the surgical harvest and extended manufacturing. Plan for 2-3 weeks in-country.
Medical Records Review & Center Matching
Submit pathology reports, imaging, treatment history. Our oncology team conducts peer review and matches you to appropriate TIL centers within 48 hours.
Travel & Surgical Tumor Resection
Travel to destination country. Surgical procedure (often outpatient or 1-night stay) to obtain tumor tissue. Tissue shipped to GMP manufacturing lab.
TIL Manufacturing & Expansion
TILs are isolated and expanded in IL-2 over 22-33 days. Patient may return home or stay near the treatment center. Quality control testing throughout.
Admission & Lymphodepletion
Patient admitted to hospital. Receives cyclophosphamide + fludarabine for 3 days to deplete native lymphocytes and create "space" for TILs.
TIL Infusion Day
50-100+ billion expanded TILs infused intravenously over ~30 minutes. One-time infusion. Patient monitored closely for initial reactions.
IL-2 Support & Recovery
Up to 12 doses of high-dose IL-2 over 5 days to sustain T-cell activity. Requires ICU-capable monitoring due to capillary leak risk. Discharge when stable.
Follow-Up & Response Assessment
First response scan at 4-8 weeks post-infusion. Ongoing monitoring every 2-3 months for first 2 years. Return home with local oncologist follow-up plan.
Side Effects: What to Expect
TIL therapy is intensive. Side effects come from two sources: lymphodepletion chemotherapy and high-dose IL-2. Most are manageable in experienced centers.
Cytokine Release (from IL-2)
Fever, chills, fatigue, nausea — very common during IL-2 administration. Usually resolves within 24-48 hours of stopping IL-2.
ManageableCapillary Leak Syndrome
IL-2 can cause fluid to leak from blood vessels, leading to hypotension, edema, weight gain. Requires ICU monitoring and IV fluid management.
Requires ICUProlonged Cytopenias
From lymphodepletion chemotherapy. Low white cells, red cells, platelets for 1-3 weeks. Infection risk managed with prophylactic antibiotics/antifungals.
ExpectedPulmonary Effects
Shortness of breath, pulmonary edema (from IL-2). Monitored with daily chest exams and oxygen saturation. Resolves with IL-2 discontinuation.
MonitoredNeurotoxicity
Confusion, somnolence, dizziness — much less common than with CAR-T. Usually mild and reversible. ICANS is rare with TIL.
UncommonCardiac Effects
Tachycardia, transient arrhythmias possible with IL-2. Continuous cardiac monitoring during IL-2 phase. Contraindicated in severe cardiac disease.
MonitoredTIL therapy should only be performed at experienced centers with ICU capability and staff trained in IL-2 toxicity management. Mortality in the C-145-04 trial was <1%, but serious adverse events occurred in ~54% of patients. Patient selection and center experience are critical to safety.
TIL vs Other Cellular Therapies
How does TIL compare to CAR-T, NK, and Gamma Delta? Each has distinct strengths and ideal use cases.
| Dimension | 🔬 TIL | 🧬 CAR-T | 🛡️ NK Cell | ⚔️ Gamma Delta |
|---|---|---|---|---|
| Best For | Melanoma, Cervical, Solid tumors | Blood cancers (ALL, DLBCL, MM) | Blood + adjuvant solid | Solid tumors (broad) |
| FDA Approval | Yes (Feb 2024, melanoma) | Yes (6 products) | No | No |
| Response Rate | 36% ORR (melanoma) | 70-90% (B-ALL) | 35-50% | 40-60% DCR |
| Cost (China) | $80K-$120K | $50K-$80K | $30K-$50K | $30K-$60K |
| Timeline | 6-10 weeks | 4-8 weeks | 2-4 weeks | 3-5 weeks |
| Source | Tumor tissue (autologous) | Blood (autologous) | Off-the-shelf OK | Off-the-shelf OK |
| Side Effects | IL-2 toxicity, cytopenias | CRS, ICANS | Mild | Very mild |
| Hospital Stay | 2-3 weeks | 1-2 weeks | Outpatient/short | Outpatient |
Frequently Asked Questions About TIL Therapy
Honest answers based on published clinical data and our coordination experience.
TIL (Tumor-Infiltrating Lymphocyte) therapy is a type of adoptive cell transfer immunotherapy. It uses the patient's own immune cells that have already recognized and infiltrated their tumor. A piece of tumor is surgically removed, TILs are isolated and expanded in the lab with interleukin-2 (IL-2) over 3-5 weeks to reach billions of cells, then reinfused after lymphodepleting chemotherapy. This approach leverages the natural anti-tumor immunity already present in the tumor microenvironment.
Yes. On February 16, 2024, the FDA approved lifileucel (brand name Amtagvi, developed by Iovance Biotherapeutics) for adult patients with unresectable or metastatic melanoma previously treated with a PD-1 blocking antibody, and if BRAF V600 mutation positive, a BRAF inhibitor with or without a MEK inhibitor. This was the first FDA-approved TIL therapy and the first cell therapy approved for any solid tumor.
In the C-145-04 pivotal trial published in NEJM (2023), lifileucel achieved an objective response rate (ORR) of 36% in 153 patients with advanced melanoma who had progressed on prior immunotherapy and targeted therapy. Complete response (CR) was observed in 11% of patients. Among responders, the duration of response was durable, with 85% of responses lasting 6 months or longer, and many exceeding 2 years.
In the USA, the list price for lifileucel (Amtagvi) is approximately $375,000, not including hospital fees, lymphodepletion chemotherapy, IL-2 administration, and ICU monitoring, which can bring the total episode of care to $500,000+. In China, TIL therapy is available through clinical research programs at $80,000-$120,000. In Singapore, costs range from $100,000-$150,000. These prices reflect self-pay international patient pricing.
Ideal candidates have unresectable or metastatic melanoma that has progressed after PD-1 inhibitor therapy (and BRAF/MEK inhibitors if BRAF V600-mutated). Patients must have ECOG performance status 0-1, adequate organ function (heart, lungs, liver, kidneys), and a resectable tumor site for TIL harvest. Active uncontrolled infection, severe autoimmune disease, or need for chronic immunosuppression are contraindications.
TIL therapy has two distinct phases of side effects: (1) Lymphodepletion chemotherapy (typically cyclophosphamide + fludarabine) causes prolonged cytopenias, infection risk, and fatigue for 1-2 weeks. (2) High-dose IL-2 support (up to 12 doses) can cause capillary leak syndrome with hypotension, edema, and requires ICU-capable monitoring. Other common effects include fever, chills, nausea, and transient liver enzyme elevation. Most side effects are manageable in experienced centers.
The full TIL therapy timeline is typically 6-10 weeks: Week 1 — surgical tumor resection and tissue shipping; Weeks 2-6 — TIL isolation and expansion in the GMP lab (22-33 days); Week 6-7 — patient admission, lymphodepleting chemotherapy (2-3 days); Week 7 — TIL infusion day; Weeks 7-8 — IL-2 support (up to 12 doses over 5 days) and recovery monitoring. Total hospital stay is typically 2-3 weeks.
While FDA approval is currently limited to melanoma, TIL therapy is being actively investigated in clinical trials for cervical cancer (with promising Phase 2 data showing 44% ORR in PD-1 refractory patients), head and neck cancers, non-small cell lung cancer, breast cancer, and gastrointestinal cancers. Iovance is running the C-145-06 trial in cervical cancer. Access to TIL for non-melanoma indications is currently through clinical trials in China, Singapore, and select US academic centers.
Is TIL Therapy Right for Your Case?
Submit your medical records. Our oncology team will review your pathology, prior treatments, and performance status — and respond within 48 hours with an honest assessment of your TIL eligibility.
Free Case Review — 48 Hour Response
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