Gut-Selective Design of Orally Administered Izencitinib (TD-1473) Limits Systemic Exposure and Effects of Janus Kinase Inhibition in Nonclinical Species

Izencitinib (TD-1473), an oral, gut-selective pan-Janus kinase (JAK) inhibitor under investigation for treatment of inflammatory bowel diseases, was designed for optimal efficacy in the gastrointestinal tract while minimizing systemic exposures and JAK-related safety findings. The nonclinical safety...

Descripción completa

Detalles Bibliográficos
Autores principales: Hardwick, Rhiannon N, Brassil, Patrick, Badagnani, Ilaria, Perkins, Kimberly, Obedencio, Glenmar P, Kim, Andrea S, Conner, Michael W, Bourdet, David L, Harstad, Eric B
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2022
Materias:
Regulatory Science, Risk Assessment, and Decision Making
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8963331/
https://www.ncbi.nlm.nih.gov/pubmed/35134999
http://dx.doi.org/10.1093/toxsci/kfac002
_version_ 1784677967176138752
author Hardwick, Rhiannon N
Brassil, Patrick
Badagnani, Ilaria
Perkins, Kimberly
Obedencio, Glenmar P
Kim, Andrea S
Conner, Michael W
Bourdet, David L
Harstad, Eric B
author_facet Hardwick, Rhiannon N
Brassil, Patrick
Badagnani, Ilaria
Perkins, Kimberly
Obedencio, Glenmar P
Kim, Andrea S
Conner, Michael W
Bourdet, David L
Harstad, Eric B
author_sort Hardwick, Rhiannon N
collection PubMed
description Izencitinib (TD-1473), an oral, gut-selective pan-Janus kinase (JAK) inhibitor under investigation for treatment of inflammatory bowel diseases, was designed for optimal efficacy in the gastrointestinal tract while minimizing systemic exposures and JAK-related safety findings. The nonclinical safety of izencitinib was evaluated in rat and dog repeat-dose and rat and rabbit reproductive and developmental toxicity studies. Systemic exposures were compared with JAK inhibitory potency to determine effects at or above pharmacologic plasma concentrations (≥1× plasma average plasma concentration [C(ave)]:JAK 50% inhibitory concentration [IC(50)] ratio). In rats and dogs, 1000 and 30 mg/kg/day izencitinib, respectively, produced minimal systemic findings (ie, red/white cell changes) and low systemic concentrations (approximately 1× plasma C(ave):JAK IC(50) ratio) with an 8× nonclinical:clinical systemic area under the curve (AUC) margin compared with exposures at the highest clinically tested dose (300 mg, quaque die, once daily, phase 1 study in healthy volunteers). In dogs, it was possible to attain sufficient systemic exposures to result in immunosuppression characteristic of systemic JAK inhibition, but at high AUC margins (43×) compared with systemic exposures observed at the highest tested dose in humans. No adverse findings were observed in the gastrointestinal tract or systemic tissues. Izencitinib did not affect male or female fertility. Izencitinib did not affect embryonic development in rats and rabbits as commonly reported with systemic JAK inhibition, consistent with low maternal systemic concentrations (2–6× plasma C(ave):JAK IC(50) ratio, 10–33× nonclinical:clinical AUC margin) and negligible fetal exposures. In conclusion, the izencitinib gut-selective approach resulted in minimal systemic findings in nonclinical species at pharmacologic, clinically relevant systemic exposures, highlighting the impact of organ-selectivity in reducing systemic safety findings.
format Online
Article
Text
id pubmed-8963331
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher Oxford University Press
record_format MEDLINE/PubMed
spelling pubmed-89633312022-03-29 Gut-Selective Design of Orally Administered Izencitinib (TD-1473) Limits Systemic Exposure and Effects of Janus Kinase Inhibition in Nonclinical Species Hardwick, Rhiannon N Brassil, Patrick Badagnani, Ilaria Perkins, Kimberly Obedencio, Glenmar P Kim, Andrea S Conner, Michael W Bourdet, David L Harstad, Eric B Toxicol Sci Regulatory Science, Risk Assessment, and Decision Making Izencitinib (TD-1473), an oral, gut-selective pan-Janus kinase (JAK) inhibitor under investigation for treatment of inflammatory bowel diseases, was designed for optimal efficacy in the gastrointestinal tract while minimizing systemic exposures and JAK-related safety findings. The nonclinical safety of izencitinib was evaluated in rat and dog repeat-dose and rat and rabbit reproductive and developmental toxicity studies. Systemic exposures were compared with JAK inhibitory potency to determine effects at or above pharmacologic plasma concentrations (≥1× plasma average plasma concentration [C(ave)]:JAK 50% inhibitory concentration [IC(50)] ratio). In rats and dogs, 1000 and 30 mg/kg/day izencitinib, respectively, produced minimal systemic findings (ie, red/white cell changes) and low systemic concentrations (approximately 1× plasma C(ave):JAK IC(50) ratio) with an 8× nonclinical:clinical systemic area under the curve (AUC) margin compared with exposures at the highest clinically tested dose (300 mg, quaque die, once daily, phase 1 study in healthy volunteers). In dogs, it was possible to attain sufficient systemic exposures to result in immunosuppression characteristic of systemic JAK inhibition, but at high AUC margins (43×) compared with systemic exposures observed at the highest tested dose in humans. No adverse findings were observed in the gastrointestinal tract or systemic tissues. Izencitinib did not affect male or female fertility. Izencitinib did not affect embryonic development in rats and rabbits as commonly reported with systemic JAK inhibition, consistent with low maternal systemic concentrations (2–6× plasma C(ave):JAK IC(50) ratio, 10–33× nonclinical:clinical AUC margin) and negligible fetal exposures. In conclusion, the izencitinib gut-selective approach resulted in minimal systemic findings in nonclinical species at pharmacologic, clinically relevant systemic exposures, highlighting the impact of organ-selectivity in reducing systemic safety findings. Oxford University Press 2022-02-04 /pmc/articles/PMC8963331/ /pubmed/35134999 http://dx.doi.org/10.1093/toxsci/kfac002 Text en © The Author(s) 2022. Published by Oxford University Press on behalf of the Society of Toxicology. https://creativecommons.org/licenses/by-nc/4.0/This is an Open Access article distributed under the terms of the Creative Commons Attribution-NonCommercial License (https://creativecommons.org/licenses/by-nc/4.0/), which permits non-commercial re-use, distribution, and reproduction in any medium, provided the original work is properly cited. For commercial re-use, please contact journals.permissions@oup.com
spellingShingle Regulatory Science, Risk Assessment, and Decision Making
Hardwick, Rhiannon N
Brassil, Patrick
Badagnani, Ilaria
Perkins, Kimberly
Obedencio, Glenmar P
Kim, Andrea S
Conner, Michael W
Bourdet, David L
Harstad, Eric B
Gut-Selective Design of Orally Administered Izencitinib (TD-1473) Limits Systemic Exposure and Effects of Janus Kinase Inhibition in Nonclinical Species
title Gut-Selective Design of Orally Administered Izencitinib (TD-1473) Limits Systemic Exposure and Effects of Janus Kinase Inhibition in Nonclinical Species
title_full Gut-Selective Design of Orally Administered Izencitinib (TD-1473) Limits Systemic Exposure and Effects of Janus Kinase Inhibition in Nonclinical Species
title_fullStr Gut-Selective Design of Orally Administered Izencitinib (TD-1473) Limits Systemic Exposure and Effects of Janus Kinase Inhibition in Nonclinical Species
title_full_unstemmed Gut-Selective Design of Orally Administered Izencitinib (TD-1473) Limits Systemic Exposure and Effects of Janus Kinase Inhibition in Nonclinical Species
title_short Gut-Selective Design of Orally Administered Izencitinib (TD-1473) Limits Systemic Exposure and Effects of Janus Kinase Inhibition in Nonclinical Species
title_sort gut-selective design of orally administered izencitinib (td-1473) limits systemic exposure and effects of janus kinase inhibition in nonclinical species
topic Regulatory Science, Risk Assessment, and Decision Making
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8963331/
https://www.ncbi.nlm.nih.gov/pubmed/35134999
http://dx.doi.org/10.1093/toxsci/kfac002
work_keys_str_mv AT hardwickrhiannonn gutselectivedesignoforallyadministeredizencitinibtd1473limitssystemicexposureandeffectsofjanuskinaseinhibitioninnonclinicalspecies
AT brassilpatrick gutselectivedesignoforallyadministeredizencitinibtd1473limitssystemicexposureandeffectsofjanuskinaseinhibitioninnonclinicalspecies
AT badagnaniilaria gutselectivedesignoforallyadministeredizencitinibtd1473limitssystemicexposureandeffectsofjanuskinaseinhibitioninnonclinicalspecies
AT perkinskimberly gutselectivedesignoforallyadministeredizencitinibtd1473limitssystemicexposureandeffectsofjanuskinaseinhibitioninnonclinicalspecies
AT obedencioglenmarp gutselectivedesignoforallyadministeredizencitinibtd1473limitssystemicexposureandeffectsofjanuskinaseinhibitioninnonclinicalspecies
AT kimandreas gutselectivedesignoforallyadministeredizencitinibtd1473limitssystemicexposureandeffectsofjanuskinaseinhibitioninnonclinicalspecies
AT connermichaelw gutselectivedesignoforallyadministeredizencitinibtd1473limitssystemicexposureandeffectsofjanuskinaseinhibitioninnonclinicalspecies
AT bourdetdavidl gutselectivedesignoforallyadministeredizencitinibtd1473limitssystemicexposureandeffectsofjanuskinaseinhibitioninnonclinicalspecies
AT harstadericb gutselectivedesignoforallyadministeredizencitinibtd1473limitssystemicexposureandeffectsofjanuskinaseinhibitioninnonclinicalspecies

Ejemplares similares