Literature DB >> 25722499

Design, Synthesis and Application of Fluorine-Labeled Taxoids as 19F NMR Probes for the Metabolic Stability Assessment of Tumor-Targeted Drug Delivery Systems.

Joshua D Seitz1, Jacob G Vineberg1, Longfei Wei1, Jonathan F Khan1, Brendan Lichtenthal1, Chi-Feng Lin1, Iwao Ojima2.   

Abstract

Novel tumor-targeting drug conjugates, BLT-F2 (1) and BLT-S-F6 (2), bearing a fluorotaxoid as the warhead, a mechanism-based self-immolative disulfide linker, and biotin as the tumor-targeting module, were designed and synthesized as 19F NMR probes. Fluorine atoms and CF3 groups were strategically incorporated into the conjugates to investigate the mechanism of linker cleavage and factors that influence their plasma and metabolic stability by real-time monitoring with 19F NMR. Time-resolved 19F NMR study on probe 1 disclosed a stepwise mechanism for release of a fluorotaxoid, which might not have been detected by other analytical methods. Probe 2 was designed to bear two CF3 groups in the taxoid moiety as "3-FAB" reporters for enhanced sensitivity and a polyethylene glycol oligomer insert to improve solubility. The clean analysis of the linker stability and reactivity of drug conjugates in blood plasma or cell culture media by HPLC and 1H NMR is troublesome, due to the overlap of key signals/peaks with background arising from highly complex ingredients in biological systems. Accordingly, the use of 19F NMR would provide a practical solution to this problem. In fact, our "3-FAB" probe 2 was proven to be highly useful to investigate the stability and reactivity of the self-immolative disulfide linker system in human blood plasma by 19F NMR. It has also been revealed that the use of polysorbate 80 as excipient for the formulation of probe 2 dramatically increases the stability of the disulfide linker system. This finding further indicates that the tumor-targeting drug conjugates with polysorbate 80/EtOH/saline formulation for in vivo studies would have high stability in blood plasma, while the drug release in cancer cells proceeds smoothly.

Entities:  

Keywords:  19F NMR; Fluorine Probe; Fluorotaxoid; Self-immolative Disulfide Linker; Tumor-Targeted Drug Delivery System

Year:  2015        PMID: 25722499      PMCID: PMC4337250          DOI: 10.1016/j.jfluchem.2014.08.006

Source DB:  PubMed          Journal:  J Fluor Chem        ISSN: 0022-1139            Impact factor:   2.050


  35 in total

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3.  Biotin-containing reagents.

Authors:  M Wilchek; E A Bayer
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8.  Structure-activity relationship study of taxoids for their ability to activate murine macrophages as well as inhibit the growth of macrophage-like cells.

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Review 9.  Guided molecular missiles for tumor-targeting chemotherapy--case studies using the second-generation taxoids as warheads.

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Journal:  Acc Chem Res       Date:  2007-07-31       Impact factor: 22.384

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1.  Strategic Incorporation of Fluorine into Taxoid Anticancer Agents for Medicinal Chemistry and Chemical Biology Studies.

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Journal:  J Fluor Chem       Date:  2017-01-03       Impact factor: 2.050

2.  Design, synthesis and biological evaluation of a highly-potent and cancer cell selective folate-taxoid conjugate.

Authors:  Joshua D Seitz; Jacob G Vineberg; Evan Herlihy; Bora Park; Eduard Melief; Iwao Ojima
Journal:  Bioorg Med Chem       Date:  2015-03-06       Impact factor: 3.641

3.  Design, synthesis, and biological evaluation of theranostic vitamin-linker-taxoid conjugates.

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Review 4.  Quest for Efficacious Next-Generation Taxoid Anticancer Agents and Their Tumor-Targeted Delivery.

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Journal:  J Nat Prod       Date:  2018-02-22       Impact factor: 4.050

5.  Design, Synthesis, and Biological Evaluations of Asymmetric Bow-Tie PAMAM Dendrimer-Based Conjugates for Tumor-Targeted Drug Delivery.

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Journal:  ACS Omega       Date:  2018-04-03
  5 in total

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