Prodrugs for colon-restricted delivery: Design, synthesis, and in vivo evaluation of colony stimulating factor 1 receptor (CSF1R) inhibitors

The ability to restrict low molecular weight compounds to the gastrointestinal (GI) tract may enable an enhanced therapeutic index for molecular targets known to be associated with systemic toxicity. Using a triazolopyrazine CSF1R inhibitor scaffold, a broad range of prodrugs were synthesized and ev...

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Veröffentlicht in:	PloS one 2018-09, Vol.13 (9), p.e0203567
Hauptverfasser:	George, Dawn M, Huntley, Raymond J, Cusack, Kevin, Duignan, David B, Hoemann, Michael, Loud, Jacqueline, Mario, Regina, Melim, Terry, Mullen, Kelly, Somal, Gagandeep, Wang, Lu, Edmunds, Jeremy J
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Sprache:	eng
Schlagworte:	Animals Arthritis Biocompatibility Biology and Life Sciences Chemical compounds Chemistry Colitis Colitis - chemically induced Colitis - drug therapy Colitis - immunology Colon Colon - chemistry Colony-stimulating factor Cyclodextrin Cyclodextrins Cyclodextrins - chemistry Dextran Dextran Sulfate - adverse effects Disease Disease Models, Animal Drug dosages Drug Evaluation, Preclinical Drugs Enzymes Evaluation Female Gastrointestinal system Gastrointestinal tract Gene expression HIV House mouse Human immunodeficiency virus Immunology Inflammatory bowel disease Kinases Ligands Liver Low molecular weights Macrophages Macrophages - drug effects Macrophages - metabolism Medicine and Health Sciences Metabolism Mice Models, Molecular Molecular Structure Molecular weight Monocytes Pharmacodynamics Pharmacology Physical Sciences Prodrugs Prodrugs - administration & dosage Prodrugs - chemical synthesis Prodrugs - chemistry Prodrugs - pharmacokinetics Receptors, Granulocyte-Macrophage Colony-Stimulating Factor - antagonists & inhibitors Research and Analysis Methods Signal transduction Sodium Sodium sulfate Toxicity
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creator	George, Dawn M Huntley, Raymond J Cusack, Kevin Duignan, David B Hoemann, Michael Loud, Jacqueline Mario, Regina Melim, Terry Mullen, Kelly Somal, Gagandeep Wang, Lu Edmunds, Jeremy J
description	The ability to restrict low molecular weight compounds to the gastrointestinal (GI) tract may enable an enhanced therapeutic index for molecular targets known to be associated with systemic toxicity. Using a triazolopyrazine CSF1R inhibitor scaffold, a broad range of prodrugs were synthesized and evaluated for enhanced delivery to the colon in mice. Subsequently, the preferred cyclodextrin prodrug moiety was appended to a number of CSF1R inhibitory active parent molecules, enabling GI-restricted delivery. Evaluation of a cyclodextrin prodrug in a dextran sodium sulfate (DSS)-induced mouse colitis model resulted in enhanced GI tissue levels of active parent. At a dose where no significant depletion of systemic monocytes were detected, the degree of pharmacodynamic effect-measured as reduction in macrophages in the colon-was inferior to that observed with a systemically available positive control. This suggests that a suitable therapeutic index cannot be achieved with CSF1R inhibition by using GI-restricted delivery in mice. However, these efforts provide a comprehensive frame-work in which to pursue additional gut-restricted delivery strategies for future GI targets.
doi_str_mv	10.1371/journal.pone.0203567
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subjects	Animals Arthritis Biocompatibility Biology and Life Sciences Chemical compounds Chemistry Colitis Colitis - chemically induced Colitis - drug therapy Colitis - immunology Colon Colon - chemistry Colony-stimulating factor Cyclodextrin Cyclodextrins Cyclodextrins - chemistry Dextran Dextran Sulfate - adverse effects Disease Disease Models, Animal Drug dosages Drug Evaluation, Preclinical Drugs Enzymes Evaluation Female Gastrointestinal system Gastrointestinal tract Gene expression HIV House mouse Human immunodeficiency virus Immunology Inflammatory bowel disease Kinases Ligands Liver Low molecular weights Macrophages Macrophages - drug effects Macrophages - metabolism Medicine and Health Sciences Metabolism Mice Models, Molecular Molecular Structure Molecular weight Monocytes Pharmacodynamics Pharmacology Physical Sciences Prodrugs Prodrugs - administration & dosage Prodrugs - chemical synthesis Prodrugs - chemistry Prodrugs - pharmacokinetics Receptors, Granulocyte-Macrophage Colony-Stimulating Factor - antagonists & inhibitors Research and Analysis Methods Signal transduction Sodium Sodium sulfate Toxicity
title	Prodrugs for colon-restricted delivery: Design, synthesis, and in vivo evaluation of colony stimulating factor 1 receptor (CSF1R) inhibitors
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