Antibody-drug Conjugates Targeted to CD79 for the Treatment of Non-Hodgkin Lymphoma

Overview

Journal Blood

Publisher Elsevier

Specialty Hematology

Date 2007 Mar 22

PMID 17374736

Citations 67

Authors

Andrew G Polson

Shang-Fan Yu

Kristi Elkins

Bing Zheng

Suzanna Clark

Gladys S Ingle

Dionysos S Slaga

Lynne Giere

Changchun Du

Christine Tan

Jo-Anne Hongo

Alvin Gogineni

Mary J Cole

Richard Vandlen

Jean-Philippe Stephan

Judy Young

Wesley Chang

Suzie J Scales

Sarajane Ross

Dan Eaton

Allen Ebens

Affiliations

Soon will be listed here.

Abstract

Targeting cytotoxic drugs to cancer cells using antibody-drug conjugates (ADCs), particularly those with stable linkers between the drug and the antibody, could be an effective cancer treatment with low toxicity. However, for stable-linker ADCs to be effective, they must be internalized and degraded, limiting potential targets to surface antigens that are trafficked to lysosomes. CD79a and CD79b comprise the hetrodimeric signaling component of the B-cell receptor, and are attractive targets for the use of ADCs because they are B-cell-specific, expressed in non-Hodgkin lymphomas (NHL), and are trafficked to a lysosomal-like compartment as part of antigen presentation. We show here that the stable-linker ADCs anti-CD79b-MCC-DM1 and anti-CD79b-MC-MMAF are capable of target-dependent killing of nonHodgkin lymphoma cell lines in vitro. Further, these 2 ADCs are equally effective as low doses in xenograft models of follicular, mantle cell, and Burkitt lymphomas, even though several of these cell lines express relatively low levels of CD79b in vivo. In addition, we demonstrate that anti-CD79b ADCs were more effective than anti-CD79a ADCs and that, as hypothesized, anti-CD79b antibodies downregulated surface B-cell receptor and were trafficked to the lysosomal-like major histocompatibility complex class II-positive compartment MIIC. These results suggest that anti-CD79b-MCC-DM1 and anti-CD79b-MC-MMAF are promising therapeutics for the treatment of NHL.

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