Leukemia, B-Cell Clinical Trial
Official title:
A Phase I Dose-escalation Study to Assess the Safety of AFM11 (CD19 x CD3 TandAb®) in Patients With Relapsed or Refractory Adult B-precursor Acute Lymphoblastic Leukemia
The purpose of the study is to determine the maximum tolerated dose (MTD) in patients with acute lymphoblastic leukemia (ALL) and to determine the safety and tolerability of increasing doses and different infusion times of AFM11 infusion in patients with adult B-precursor ALL
Acute lymphoblastic leukemia (ALL) is an aggressive type of leukemia characterized by an
overproduction of lymphoblasts or lymphocytes in the bone marrow and the peripheral blood; it
is frequently accompanied by suppression of normal hematopoiesis. It can spread to the lymph
nodes, spleen, liver, the central nervous system (CNS), and other organs (sanctuary sites).
Without treatment, ALL usually progresses quickly.
B- and T-cell lymphoblastic leukemia cells express surface antigens that parallel their
respective developmental lineages. Precursor B-cell ALL cells typically express CD10, CD19,
and CD34 on their surface, along with nuclear terminal deoxynucleotide transferase. About 20%
of adult ALL patients have a cytogenetic abnormality that is indistinguishable from the
Philadelphia chromosome (Ph1, t(9;22)), according to the National Cancer Institute (NCI).
The rationale for the use of AFM11 is based on its ability to bind to both malignant cells
via its anti-CD19 domain and to T-cells via its anti-CD3 domains. This results in the
formation of the "immunological synapse" and the subsequent T-cell activation on leading to
killing of malignant cells. AFM11 has 2 binding sites for CD19 and 2 for CD3, its molecular
weight is ~ 105kDa compared to diabodies like blinatumomab with one binding site for each
target and a much lower molecular weight ~ 55kDa. In addition, preclinical experiments have
shown that AFM11 has about a 100 fold higher affinity to CD3 compared to diabodies and is
inducing higher cytotoxicity in vitro in the presence of low effector:target cell ratios.
These differences might allow for a shortening of the infusion times and potentially higher
clinical efficacy compared to blinatumomab.
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