Literature DB >> 23236171

Heterobivalent ligands target cell-surface receptor combinations in vivo.

Liping Xu1, Jatinder S Josan, Josef Vagner, Michael R Caplan, Victor J Hruby, Eugene A Mash, Ronald M Lynch, David L Morse, Robert J Gillies.   

Abstract

A challenge in tumor targeting is to deliver payloads to cancers while sparing normal tissues. A limited number of antibodies appear to meet this challenge as therapeutics themselves or as drug-antibody conjugates. However, antibodies suffer from their large size, which can lead to unfavorable pharmacokinetics for some therapeutic payloads, and that they are targeted against only a single epitope, which can reduce their selectivity and specificity. Here, we propose an alternative targeting approach based on patterns of cell surface proteins to rationally develop small, synthetic heteromultivalent ligands (htMVLs) that target multiple receptors simultaneously. To gain insight into the multivalent ligand strategy in vivo, we have generated synthetic htMVLs that contain melanocortin (MSH) and cholecystokinin (CCK) pharmacophores that are connected via a fluorescent labeled, rationally designed synthetic linker. These ligands were tested in an experimental animal model containing tumors that expressed only one (control) or both (target) MSH and CCK receptors. After systemic injection of the htMVL in tumor-bearing mice, label was highly retained in tumors that expressed both, compared with one, target receptors. Selectivity was quantified by using ex vivo measurement of Europium-labeled htMVL, which had up to 12-fold higher specificity for dual compared with single receptor expressing cells. This proof-of-principle study provides in vivo evidence that small, rationally designed bivalent htMVLs can be used to selectively target cells that express both, compared with single complimentary cell surface targets. These data open the possibility that specific combinations of targets on tumors can be identified and selectively targeted using htMVLs.

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Year:  2012        PMID: 23236171      PMCID: PMC3535626          DOI: 10.1073/pnas.1211762109

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  35 in total

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3.  Novel targeting strategy based on multimeric ligands for drug delivery and molecular imaging: homooligomers of alpha-MSH.

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  31 in total

1.  Multivalent activation of GLP-1 and sulfonylurea receptors modulates β-cell second-messenger signaling and insulin secretion.

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2.  Multivalent Peptoid Conjugates Which Overcome Enzalutamide Resistance in Prostate Cancer Cells.

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Review 3.  Bench-top to clinical therapies: A review of melanocortin ligands from 1954 to 2016.

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Review 4.  Peptides and peptidomimetics as immunomodulators.

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5.  Tumor Targeting and Pharmacokinetics of a Near-Infrared Fluorescent-Labeled δ-Opioid Receptor Antagonist Agent, Dmt-Tic-Cy5.

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Review 6.  Nanoparticle ligand presentation for targeting solid tumors.

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7.  Hetero-bivalent GLP-1/glibenclamide for targeting pancreatic β-cells.

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8.  An in Vitro and in Vivo Investigation of Bivalent Ligands That Display Preferential Binding and Functional Activity for Different Melanocortin Receptor Homodimers.

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9.  Development and in vivo quantitative magnetic resonance imaging of polymer micelles targeted to the melanocortin 1 receptor.

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Review 10.  Homo- and Heterodimerization of Proteins in Cell Signaling: Inhibition and Drug Design.

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Journal:  Adv Protein Chem Struct Biol       Date:  2017-10-06       Impact factor: 3.507

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