Using Dendrimers to Design Multivalent Therapeutic Agents
Project Number3R01GM062444-08S1
Contact PI/Project LeaderCLONINGER, MARY J
Awardee OrganizationMONTANA STATE UNIVERSITY - BOZEMAN
Description
Abstract Text
We propose to study the roles of protein-carbohydrate and carbohydrate-carbohydrate interactions in cancer
metastasis. We'll use dendrimers with clusters of carbohydrates, as well as heterogeneously-functionalized
dendrimers synthesized using techniques developed in the last funding cycle, to study binding and adhesion
processes associated with cancer metastasis. Specifically, the syntheses of N-acetyl galactosamine,
lactose, and GM3-functionalized dendrimers are described. Binding assays to determine the affinity of the
gal-NAc and lactose-functionalized dendrimers for galectin-3 and to determine the affinity of GM3-
functionalized dendrimers for carbohydrate arrays are proposed. Carbohydrate-functionalized dendrimers
that exhibit high affinity binding to their receptors will be further evaluated using cancer cell aggregation
studies.
Many reports suggest that cell surface carbohydrates serve a critical function in malignant transformation
and metastasis, and so the development of artificial carbohydrate arrays such as those described in this
proposal that can aptly mimic and interfere with cancer cell aggregation processes is critical. From the
research proposed here, our goal is to advance fundamental knowledge regarding the role of protein-
carbohydrate and carbohydrate-carbohydrateinteractions in the metastatic spread of cancer. Concurrently,
new therapeutic agents to arrest cancer cell aggregation may emerge.
Advancing the fundamental knowledge of the associations that mediate metastatic processes and
developing multivalent, nanoscale therapeutic agents to arrest cancer metastasis clearly have enormous
implications for public health.
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