Interleukin-2 fusion protein: an investigational therapy for interleukin-2 receptor expressing malignancies

Authors

Jean Nichols, Seragen Inc, USA
Foss Francine, Boston University, USA
Kuzel Timothy, Info Northwestern University, USA
LeMaistre Charles Fred, Sarah Cannon, USA
Platanias Leonidas, Northwestern University, USA
Ratain Mark, The University of Chicago, USA
Rook Alain, Info Penn Medicine, USA
Mansoor Saleh, Aga Khan UniversityFollow
Schwartz Gary, Info Dartmouth-Hitchcock Medical Center,USA

Document Type

Article

Department

Haematology and Oncology, East Africa

Abstract

DAB3s91L-2 is an interleukin-2 receptor (IL-2R) specific fusion protein with a molecular weight of 58 kD containing the enzymatic and translocation domains of diphtheria toxin (DT) and human IL-2. This fusion protein is able to direct the cytocidal action of the DT enzymatic region only to cells which bear the IL-2R. The human IL-2R exists in three forms: low, intermediate and high affinity. The high-affinity form is believed to be the biologically relevant form on mature, activated T-lymphocytes, B-lymphocytes and monocytes. DAB3sgIL-2 is able to bind selectively to the high-affinity IL-2R in a concentration-dependent manner, and once bound is internalised via receptor-mediated endocytosis. Upon acidification of the formed vesicle, the enzymatic portion of the fusion protein is believed to pass into the cytosol where it ultimately inhibits protein synthesis by inactivation of elongation factor-2, resulting in cell death. The constitutive expression of the IL-2R on certain leukaemic and lymphomatous cells of T and B cell origin has been reported to occur in patients with chronic lymphocytic ieukaemia, cutaneous T cell lymphoma (CTCL), Hodgkin's disease and non-Hodgkin's lymphomas (NHLs). A multicentre DAB3s91L-2 dose-escalation study of patients with IL-2R expressing lymphomas has been conducted. A 10-fold range of doses were evaluated on a five-daily dose schedule. Patients received up to six courses, with an additional two courses permitted for patients with partial responses that appeared to be still improving after six courses. Most adverse experiences were transient and mild. Preliminary assessment of response indicated five complete responses (CR, duration ongoing at 20, 11, 7, 5 and 4 months) and seven partial responses (PR, duration 3-20 months) in the 35 patients with CTCL. One CR (duration > 20 months) in a patient with NHL (Lennett's lymphoma) and two PR (duration 9 and 2 months) in 17 patients with B-cell NHL have been observed. Based on the mode of action of DAB3s9IL-2, its safety profile, and the patient responses associated with the phase I/II clinical trials, a phase III programme in CTCL patients has been initiated and plans for additional trials in NHL patients are targeted for 1996. © 1997 Elsevier Science Ltd. All rights reserved. Key words: clinical trial, CTCL, DAB3s9IL-2, fusion protein, IL-2, IL-2R, lymphoma.

Comments

This work was published before the author joined Aga Khan University.

Publication (Name of Journal)

European Journal of Cancer

DOI

https://doi.org/10.1016/S0959-8049(96)00327-9

Recommended Citation

Nichols, J., Francine, F., Timothy, K., Fred, L. C., Leonidas, P., Mark, R., Alain, R., Saleh, M., Gary, S. (1997). Interleukin-2 fusion protein: an investigational therapy for interleukin-2 receptor expressing malignancies. European Journal of Cancer, 33(1), 34-36.
Available at: https://ecommons.aku.edu/eastafrica_fhs_mc_haematol_oncol/119