Antibody-drug conjugates in hematologic malignancies Journal Article


Authors: Leslie, L. A.; Younes, A.
Article Title: Antibody-drug conjugates in hematologic malignancies
Abstract: Antibody-drug conjugates (ADCs) are agents composed of a monoclonal antibody linked to cytotoxic molecules. By specifically delivering cytotoxic agents to cells expressing surface antigens of interest, ADC technology allows for the targeted use of highly toxic agents resulting in increased efficacy against malignant cells and decreased damage to normal tissue. Effector agents can be small molecules, radioisotopes, proteins, or bacterially derived toxins. Over the past several decades, ADCs have been evaluated in a variety of preclinical models of hematologic malignancies, as well as early-phase clinical trials with limited success. More recently, advancements in linkage technology, improvements in cytotoxin selection, and use of smaller conjugates containing partial rather than complete antibodies have drastically improved the potential clinical value of ADCs. In the future, ADC technology may be used to restore tumor suppressor activity, target the microenvironment, or replace nonfunctional enzymes. In this review we will discuss select ADCs in various stages of development for use in hematologic malignancies including lymphoma, multiple myeloma, and leukemia.
Keywords: treatment outcome; leukemia; antineoplastic agents; antineoplastic agent; animal; metabolism; animals; multiple myeloma; tumor markers, biological; drug design; tumor antigen; tumor marker; monoclonal antibody; immunology; antibodies, monoclonal; hematologic neoplasms; antigens, neoplasm; lymphoma; molecularly targeted therapy; antibody conjugate; immunoconjugates; molecular targeted therapy; humans; human
Journal Title: American Society of Clinical Oncology Educational Book
Volume: 33
ISSN: 1548-8756
Publisher: American Society of Clinical Oncology  
Date Published: 2013-01-01
Start Page: e108
End Page: e113
Language: English
DOI: 10.1200/EdBook_AM.2013.33.e108
PUBMED: 23714472
PROVIDER: scopus
DOI/URL:
Notes: Review -- Export Date: 25 January 2017 -- Source: Scopus
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  1. Anas Younes
    319 Younes