Abstract
Chronic lymphocytic leukemia (CLL) is a disease in which a single B-cell clone proliferates relentlessly in peripheral lymphoid organs, bone marrow, and blood. DNA sequencing experiments have shown that about 30% of CLL patients have stereotyped antigen-specific B-cell receptors (BCRs) with a high level of sequence homology in the variable domains of the heavy and light chains. These include many of the most aggressive cases that haveIGHV-unmutated BCRs whose sequences have not diverged significantly from the germ line. This suggests a personalized therapy strategy in which a toxin or immune effector function is delivered selectively to the pathogenic B-cells but not to healthy B-cells. To execute this strategy, serum-stable, drug-like compounds able to target the antigen-binding sites of most or all patients in a stereotyped subset are required. We demonstrate here the feasibility of this approach with the discovery of selective, high affinity ligands for CLL BCRs of the aggressive, stereotyped subset 7P that cross-react with the BCRs of several CLL patients in subset 7p, but not with BCRs from patients outside this subset.
Highlights
Chronic lymphocytic leukemia (CLL)2 is the most common type of adult blood cancer leukemia with ϳ15,000 new cases reported every year in the United States [1]
We report the discovery of selective, high affinity synthetic ligands for the B-cell receptor (BCR) of a patient from stereotyped subset 7P [10], which represents an aggressive, unmutated group of U-CLLs
Combinatorial Library Screening Provides Non-peptidic Ligands for an Unmutated, Stereotyped CLL BCR—We set as our target BCRs that belong to stereotype 7P, an example of U-CLL BCRs
Summary
Chronic lymphocytic leukemia (CLL) is the most common type of adult blood cancer leukemia with ϳ15,000 new cases reported every year in the United States [1]. Drug targets would be identified that allow selective suppression or killing of the malignant CLL cells without interfering with the normal function of the humoral immune system [5]. One such target is the antigen-specific B-cell receptor (BCR) itself. We demonstrated recently that high affinity, non-peptidic, and serum-stable ligands for a CLL BCR can be discovered via combinatorial library screening [9] These studies support the feasibility of targeting CLL BCR for the development of highly selective drugs
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