Adult T-cell lymphoma/leukaemia refractory – Treatment – Overview of Information and Clinical Research

Adult T-cell lymphoma/leukaemia refractory is a challenging form of blood cancer that does not respond to standard treatments. For people facing this aggressive disease, understanding available therapies and new research approaches can help guide important decisions about care and quality of life.

Understanding Treatment Goals When Disease Resists Standard Therapy

When adult T-cell leukemia/lymphoma (ATLL) does not respond to initial treatment or comes back after a period of improvement, doctors describe it as relapsed or refractory disease. The term “relapsed” means the cancer has returned after a period when it could not be detected. “Refractory” describes a situation where the lymphoma keeps growing despite treatment, or any response to therapy is very brief.^[4]

Treatment goals for refractory ATLL focus on controlling symptoms, slowing disease progression, and maintaining the best possible quality of life. Because this form of the disease is particularly aggressive and difficult to treat, doctors often tailor therapy to each person’s specific situation, including their overall health, previous treatments, and personal preferences.^[7]

Unfortunately, refractory ATLL carries a serious prognosis. Studies show that people with relapsed or refractory disease typically have limited survival time, often measured in months rather than years. One systematic review found that median survival for people with relapsed or refractory ATLL ranged considerably depending on the treatment approach used, from about two to twenty months.^[6]

⚠️ Important

There is no universally accepted standard treatment for relapsed or refractory ATLL. Because the disease is rare and outcomes are generally poor, enrollment in clinical trials testing new therapies is strongly recommended whenever possible. These trials offer access to promising new drugs that may provide better outcomes than currently available options.

The rarity of ATLL, particularly outside areas where the HTLV-1 virus is common, makes conducting large clinical trials difficult. Most treatment recommendations come from smaller studies, case reports, and experience with similar types of lymphoma. Medical societies have not established firm guidelines for treating refractory disease, meaning doctors must use their best judgment based on available evidence and each patient’s circumstances.^[7]

Standard Approaches to Relapsed and Refractory Disease

When ATLL comes back or fails to respond to initial therapy, doctors typically turn to different chemotherapy combinations than those used during first-line treatment. The hope is that cancer cells resistant to one set of drugs might still respond to another combination.^[4]

Several chemotherapy regimens borrowed from the treatment of other T-cell lymphomas are commonly used. These include DHAP, a combination of dexamethasone (a steroid), cytarabine (also called ara-C), and cisplatin (a platinum-based drug). Another option is ESHAP, which includes etoposide, methylprednisolone (a steroid), cytarabine, and cisplatin. Doctors may also use GDP (gemcitabine, dexamethasone, and cisplatin) or ICE (ifosfamide, carboplatin, and etoposide).^[4]

These chemotherapy combinations work by attacking rapidly dividing cancer cells through various mechanisms. Some drugs damage the DNA inside cancer cells, preventing them from multiplying. Others interfere with the cell’s ability to copy its genetic material or complete cell division. Steroids like dexamethasone can directly kill certain lymphoma cells and also help reduce inflammation and side effects from other drugs.

Common side effects from these intensive chemotherapy regimens include severe lowering of blood cell counts, which increases infection risk and can cause fatigue and bleeding problems. People often experience nausea, vomiting, and loss of appetite. Hair loss is common. Kidney and nerve damage can occur with certain drugs, particularly cisplatin and ifosfamide. Because the immune system is already compromised in ATLL patients, infections—including serious opportunistic infections—are a major concern during treatment.^[1]

Two newer targeted drugs have shown some activity in relapsed or refractory ATLL. Pralatrexate (brand name Folotyn) is a drug that interferes with folate metabolism, which cancer cells need to grow. Belinostat (brand name Beleodaq) is a type of drug called a histone deacetylase inhibitor, which works by affecting how genes are expressed in cancer cells. Both drugs are given intravenously in specialized cancer treatment centers.^[4]

Treatment duration varies considerably based on how well the disease responds and how well the person tolerates therapy. Doctors typically assess response after several cycles of treatment using imaging scans and blood tests. If the disease continues to progress or side effects become unmanageable, treatment may be changed or stopped in favor of supportive care focused on comfort.

Promising Therapies Under Investigation in Clinical Trials

Research into new treatments for refractory ATLL is ongoing, with several innovative approaches being tested in clinical trials. These studies offer hope that more effective therapies may become available in the future.

Mogamulizumab is one of the most extensively studied newer treatments for ATLL. This drug is a type of monoclonal antibody—a laboratory-made protein designed to recognize and attach to a specific target on cancer cells. Mogamulizumab targets a protein called CCR4, which is found on the surface of most ATLL cells. When the antibody binds to CCR4, it helps the immune system recognize and destroy the cancer cells.^[6]

Mogamulizumab has been approved in Japan for relapsed ATLL based on Phase II clinical trial results. In these studies, the drug showed the ability to produce responses in some patients whose disease had not responded to chemotherapy. A systematic review examining multiple studies found that people treated with mogamulizumab had survival times ranging from about two to eighteen months, depending on the study and patient population. While these results show promise, they also highlight that the drug is not curative for most patients.^[6]

Some studies have explored using mogamulizumab as a bridge to transplant—meaning the drug is used to control the disease temporarily while preparing patients for allogeneic hematopoietic stem cell transplantation. This approach recognizes that transplant offers the best chance for long-term survival in ATLL, but patients need to achieve some disease control first to be eligible for this intensive procedure.^[6]

Clinical trials of mogamulizumab have been conducted primarily in Japan and other Asian countries where ATLL is more common, but some studies have included patients from North America and Europe. Side effects from mogamulizumab can include infusion reactions (symptoms like fever, chills, or rash during drug administration), skin rashes, and increased risk of infections. A particular concern is that the drug can make a complication of stem cell transplant called graft-versus-host disease more severe, which requires careful monitoring.^[8]

Another promising avenue of research involves drugs that target specific genetic abnormalities found in ATLL cells. Scientists have discovered that ATLL cells often carry mutations in genes involved in cell survival and growth. One recent case report described two patients with refractory ATLL who achieved complete remission using venetoclax, a drug that inhibits a protein called BCL-2.^[9]

BCL-2 is an anti-apoptotic protein, meaning it prevents cells from dying when they should. Cancer cells often have too much BCL-2, which allows them to survive when normal cells would die. Venetoclax blocks BCL-2, essentially removing the cancer cell’s protection against death. In the reported cases, genetic testing of the patients’ ATLL cells revealed mutations affecting anti-apoptotic pathways, suggesting these cells were particularly dependent on BCL-2 for survival. Both patients experienced dramatic reductions in their viral load and achieved complete remission.^[9]

This finding is particularly exciting because it demonstrates the potential value of using next-generation sequencing—detailed genetic testing—to identify specific mutations in each patient’s cancer. This personalized approach could help doctors select targeted therapies most likely to work for an individual patient. However, these were only two patients, and much more research is needed to understand how widely venetoclax might help people with refractory ATLL.

Scientists are also investigating other molecular targets found in ATLL cells. Research has identified mutations in genes like PLCG1, PRKCB, CARD11, STAT3, VAV1, NOTCH1, IRF4, and TP53 in ATLL cells. Each of these mutations potentially represents a target for new drugs. For example, drugs that block NOTCH signaling or inhibit specific enzymes in cancer cell growth pathways are being studied in early-phase trials.^[5]

Immunotherapy approaches beyond monoclonal antibodies are also under investigation. Researchers are exploring whether treatments that enhance the body’s own immune response against ATLL cells might be effective. This includes studying checkpoint inhibitors—drugs that remove the “brakes” on the immune system—and cellular therapies where a patient’s own immune cells are modified to better recognize and attack cancer cells.

Combination strategies are another active area of research. Scientists are testing whether combining mogamulizumab with chemotherapy or other targeted agents produces better results than either approach alone. Some trials are also examining whether adding antiviral therapy (zidovudine and interferon-alpha) to other treatments might help, based on evidence that this combination can be effective in some ATLL subtypes.^[10]

⚠️ Important

Clinical trials typically have specific eligibility requirements. Factors like previous treatments received, current health status, organ function, and disease characteristics all affect whether someone qualifies for a particular trial. People interested in clinical trials should discuss options with their oncologist, who can help identify trials that might be appropriate and assist with the enrollment process.

The Role of Stem Cell Transplantation

For people with relapsed or refractory ATLL who achieve some response to salvage chemotherapy or newer agents, allogeneic hematopoietic stem cell transplantation (alloHCT) offers the best chance for long-term survival. This procedure involves using high-dose chemotherapy or radiation to destroy the patient’s diseased bone marrow and immune system, then replacing it with healthy stem cells from a donor.^[7]

The goal of alloHCT in ATLL is not just to replace the bone marrow, but to harness the donor’s immune system to attack any remaining cancer cells—an effect called graft-versus-lymphoma. This immune effect is particularly important in ATLL because the disease is so resistant to chemotherapy alone.

Studies examining outcomes after alloHCT for relapsed or refractory ATLL have shown mixed results. Survival times ranging from about four to six months have been reported in various studies, though some patients do achieve long-term remission. The procedure carries significant risks, including serious infections due to immune suppression, graft-versus-host disease (where the donor immune cells attack the patient’s normal tissues), and organ damage from the conditioning regimen.^[6]

Not everyone is a candidate for alloHCT. Patients need to be in relatively good overall health despite their cancer, have adequate organ function, and have an available donor with matching tissue types. Age is also a consideration, though older patients may be considered for reduced-intensity conditioning regimens that use lower doses of chemotherapy before transplant.

The decision to pursue transplant requires careful discussion between the patient, their family, and the medical team. The potential for cure or long-term survival must be weighed against the substantial risks and the significant impact on quality of life during and after the procedure.

Most common treatment methods

Combination chemotherapy regimens
- DHAP (dexamethasone, cytarabine, and cisplatin) used to treat relapsed disease
- ESHAP (etoposide, methylprednisolone, cytarabine, and cisplatin) for salvage therapy
- GDP (gemcitabine, dexamethasone, and cisplatin) as an alternative regimen
- ICE (ifosfamide, carboplatin, and etoposide) for treatment after relapse
Targeted therapy drugs
- Pralatrexate (Folotyn), a drug that interferes with folate metabolism
- Belinostat (Beleodaq), a histone deacetylase inhibitor affecting gene expression
- Venetoclax, a BCL-2 inhibitor blocking anti-apoptotic pathways (under investigation)
Monoclonal antibody therapy
- Mogamulizumab, targeting the CCR4 protein on ATLL cells
- Approved in Japan for relapsed disease based on Phase II trials
- Can be used as bridge therapy before stem cell transplantation
Allogeneic stem cell transplantation
- High-dose therapy followed by donor stem cell infusion
- Offers graft-versus-lymphoma effect from donor immune cells
- Best option for potential long-term survival in responding patients
- Reduced-intensity conditioning available for some older patients

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