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Zinc-Chelating Small Molecules Preferentially Accumulate and Function within Pancreatic β Cells.

Citation
Horton, T. M., et al. “Zinc-Chelating Small Molecules Preferentially Accumulate And Function Within Pancreatic Β Cells.”. Cell Chemical Biology, pp. 213-222.e6.
Center Stanford University
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Author Timothy M Horton, Paul A Allegretti, Sooyeon Lee, Hannah P Moeller, Mark Smith, Justin P Annes
Keywords chelation, diabetes, islet, targeted compound delivery, targeting, tissue selectivity, zinc, β cell, β-cell regeneration, β-cell-replication
Abstract

Diabetes is a hyperglycemic condition characterized by pancreatic β-cell dysfunction and depletion. Whereas methods for monitoring β-cell function in vivo exist, methods to deliver therapeutics to β cells are lacking. We leveraged the rare ability of β cells to concentrate zinc to preferentially trap zinc-binding molecules within β cells, resulting in β-cell-targeted compound delivery. We determined that zinc-rich β cells and islets preferentially accumulated TSQ (6-methoxy-8-p-toluenesulfonamido-quinoline) in a zinc-dependent manner compared with exocrine pancreas. Next, we asked whether appending a zinc-chelating moiety onto a β-cell replication-inducing compound was sufficient to confer preferential β-cell accumulation and activity. Indeed, the hybrid compound preferentially accumulated within rodent and human islets in a zinc-dependent manner and increased the selectivity of replication-promoting activity toward β cells. These data resolve the fundamental question of whether intracellular accumulation of zinc-chelating compounds is influenced by zinc content. Furthermore, application of this principle yielded a proof-of-concept method for β-cell-targeted drug delivery and bioactivity.

Year of Publication
2019
Journal
Cell chemical biology
Volume
26
Issue
2
Number of Pages
213-222.e6
Date Published
12/2019
ISSN Number
2451-9448
DOI
10.1016/j.chembiol.2018.10.019
Alternate Journal
Cell Chem Biol
PMID
30527998
PMCID
PMC6386607
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