Immunophenotypic and Genetic Profiling Essential for Risk Stratification in Adult T-Cell ALL
This Blood review outlines the diagnosis and management of adult T-cell acute lymphoblastic leukemia, emphasizing the immunophenotypic and genetic analyses required for prognosis, risk stratification, and post-remission therapy decisions. MRD monitoring is highlighted as essential for guiding transplant decisions, with discussion of flow cytometry and molecular methods. The review also addresses novel therapies including nelarabine and gamma-secretase inhibitors for this rare disease with poor relapse outcomes.
The original study
Management of adults with T-cell lymphoblastic leukemia.
- Authors
- Marks DI, Rowntree C
- Journal
- Blood
- Type
- Journal Article, Review
- PMID
- 28115371
Original abstract
T-cell acute lymphoblastic leukemia (ALL) is a rare disease in adults with inferior survival outcomes compared with those seen in pediatric patients. Although potentially curable with ∼50% survival at 5 years, adult patients with relapsed disease have dismal outcomes with <10% of patients surviving long term. This review will discuss the diagnosis and management of adult patients with newly diagnosed T-cell ALL with an emphasis on the immunophenotypic and genetic analyses required to assign prognosis, risk stratify, and guide post-remission therapy. The evidence for the main components of complex T-cell ALL treatment regimens is described. The importance of monitoring minimal residual disease is emphasized, with a discussion of the different methods used. The results of hematopoietic cell transplantation are analyzed, and recommendations made about which patients should be considered for this intervention. The treatment of the adolescent and young adult group is delineated, and the role of using "pediatric-inspired" regimens in older adults considered. We also describe the current data and potential future options for the use of novel therapies, including nelarabine and γ-secretase inhibitors, in adult patients with T-cell ALL.