LBODP003 Effects Of 4-weeks’ Treatment With Intraperitoneal Colchicine On Metabolic And Inflammatory Outcomes In Mice Fed A High-fat Diet

Health-deteriorating effects of obesity include chronic inflammation and insulin resistance (IR). A recent pilot human trial reported reduced IR in colchicine-treated vs. placebo-treated adults with obesity. Thus, we examined anti-inflammatory and metabolic effects of two commonly employed dosing re...

Descripción completa

Detalles Bibliográficos
Autores principales: Arner, Brooke E, Levine, Jordan A, Miller, Emily K, Patel, Tushar P, Jain, Arad, Gupta, Suryaa, Roberson, Robin B, Demidowich, Andrew P, Yanovski, Jack A
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2022
Materias:
Adipose Tissue, Appetite, & Obesity
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9624528/
http://dx.doi.org/10.1210/jendso/bvac150.003
_version_ 1784822252127125504
author Arner, Brooke E
Levine, Jordan A
Miller, Emily K
Patel, Tushar P
Jain, Arad
Gupta, Suryaa
Roberson, Robin B
Demidowich, Andrew P
Yanovski, Jack A
author_facet Arner, Brooke E
Levine, Jordan A
Miller, Emily K
Patel, Tushar P
Jain, Arad
Gupta, Suryaa
Roberson, Robin B
Demidowich, Andrew P
Yanovski, Jack A
author_sort Arner, Brooke E
collection PubMed
description Health-deteriorating effects of obesity include chronic inflammation and insulin resistance (IR). A recent pilot human trial reported reduced IR in colchicine-treated vs. placebo-treated adults with obesity. Thus, we examined anti-inflammatory and metabolic effects of two commonly employed dosing regimens of colchicine, 0.2 mg/kg and 0. 02mg/kg, in a high-fat diet (HFD; 45%) mouse obesity model. We placed male C57BL/6J mice on HFD from ages 8 through 16 weeks. At age 12 weeks, mice were randomized to: high-dose colchicine (CHD 0.2 mg/kg, n=28), low dose colchicine (CLD, 0. 02mg/kg, n=26) or vehicle (V, n=26), injected intraperitoneally (IP) for 4 weeks. Serum CRP was measured by ELISA. Dual-energy X-ray absorptiometry (DXA) scans and fasting IP glucose tolerance (GTT) and insulin-tolerance (ITT) tests were performed at baseline and following treatment. Hepatic tissue was processed for immunoblotting to determine expression of NLRP3 and caspase-1. Changes in pre- vs. post-treatment serum CRP were significantly different in the CHD group (Mean±SD: -0.57±3.1µg/mL) vs. V (+3.64±2.9µg/mL; p<0. 001) and CLD (+0.72±2.3µg/mL) compared to V (p=0. 03). Changes in CRP for CHD compared to CLD did not differ significantly (p=0.47). DXA-measured body composition changes pre-vs. post-treatment for fat mass were significantly reduced for CHD (-0.26±2. 0g) vs. V (+1.24±2.1g; p=0. 04) and CHD vs. CLD (+1.52±2.2g; p=0. 01). Lean body mass changes were not significant between treatments (p=0.69). GTT glucose concentrations were not significantly different between treatments across timepoints (Group x time interaction: p=0.24) and GTT areas under curves (AUC) were not significantly different between treatments (p=0.96). Analysis of ITT glucose measures revealed a significant group x time interaction (p=0. 03) and group effect for CHD vs. V (p=0. 009) as well as significant differences in ITT AUCs (p=0. 03) such that insulin tolerance was significantly worse for CHD: CHD AUC 19803±2662, CLD 18487±3703, V 17436±3138mg/dLx120min. Hepatic NLRP3 fold-change protein expression of treatment groups compared to V was not significant for CHD (p=0.75) or CLD (p=0.21). However, hepatic caspase-1 protein expression fold-change was significantly lower in the CHD (p=0. 008), but not the CLD group (p=0.19). We conclude that 4-weeks of IP colchicine at 0.2mg/kg (CHD) significantly suppressed serum CRP and hepatic caspase-1 protein expression compared to V, indicating CHD reduced inflammation, whereas 0. 02mg/kg colchicine (CLD) did not. However, our data suggest that 4 weeks of the CHD dose may potentially worsen whole-body insulin resistance, even though it induced a reduction in fat mass, suggesting a possible toxicity from chronic high-dose colchicine treatment. Further studies are warranted to elucidate metabolic effects of colchicine administration in murine diet-induced obesity models. Presentation: No date and time listed
format Online
Article
Text
id pubmed-9624528
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher Oxford University Press
record_format MEDLINE/PubMed
spelling pubmed-96245282022-11-14 LBODP003 Effects Of 4-weeks’ Treatment With Intraperitoneal Colchicine On Metabolic And Inflammatory Outcomes In Mice Fed A High-fat Diet Arner, Brooke E Levine, Jordan A Miller, Emily K Patel, Tushar P Jain, Arad Gupta, Suryaa Roberson, Robin B Demidowich, Andrew P Yanovski, Jack A J Endocr Soc Adipose Tissue, Appetite, & Obesity Health-deteriorating effects of obesity include chronic inflammation and insulin resistance (IR). A recent pilot human trial reported reduced IR in colchicine-treated vs. placebo-treated adults with obesity. Thus, we examined anti-inflammatory and metabolic effects of two commonly employed dosing regimens of colchicine, 0.2 mg/kg and 0. 02mg/kg, in a high-fat diet (HFD; 45%) mouse obesity model. We placed male C57BL/6J mice on HFD from ages 8 through 16 weeks. At age 12 weeks, mice were randomized to: high-dose colchicine (CHD 0.2 mg/kg, n=28), low dose colchicine (CLD, 0. 02mg/kg, n=26) or vehicle (V, n=26), injected intraperitoneally (IP) for 4 weeks. Serum CRP was measured by ELISA. Dual-energy X-ray absorptiometry (DXA) scans and fasting IP glucose tolerance (GTT) and insulin-tolerance (ITT) tests were performed at baseline and following treatment. Hepatic tissue was processed for immunoblotting to determine expression of NLRP3 and caspase-1. Changes in pre- vs. post-treatment serum CRP were significantly different in the CHD group (Mean±SD: -0.57±3.1µg/mL) vs. V (+3.64±2.9µg/mL; p<0. 001) and CLD (+0.72±2.3µg/mL) compared to V (p=0. 03). Changes in CRP for CHD compared to CLD did not differ significantly (p=0.47). DXA-measured body composition changes pre-vs. post-treatment for fat mass were significantly reduced for CHD (-0.26±2. 0g) vs. V (+1.24±2.1g; p=0. 04) and CHD vs. CLD (+1.52±2.2g; p=0. 01). Lean body mass changes were not significant between treatments (p=0.69). GTT glucose concentrations were not significantly different between treatments across timepoints (Group x time interaction: p=0.24) and GTT areas under curves (AUC) were not significantly different between treatments (p=0.96). Analysis of ITT glucose measures revealed a significant group x time interaction (p=0. 03) and group effect for CHD vs. V (p=0. 009) as well as significant differences in ITT AUCs (p=0. 03) such that insulin tolerance was significantly worse for CHD: CHD AUC 19803±2662, CLD 18487±3703, V 17436±3138mg/dLx120min. Hepatic NLRP3 fold-change protein expression of treatment groups compared to V was not significant for CHD (p=0.75) or CLD (p=0.21). However, hepatic caspase-1 protein expression fold-change was significantly lower in the CHD (p=0. 008), but not the CLD group (p=0.19). We conclude that 4-weeks of IP colchicine at 0.2mg/kg (CHD) significantly suppressed serum CRP and hepatic caspase-1 protein expression compared to V, indicating CHD reduced inflammation, whereas 0. 02mg/kg colchicine (CLD) did not. However, our data suggest that 4 weeks of the CHD dose may potentially worsen whole-body insulin resistance, even though it induced a reduction in fat mass, suggesting a possible toxicity from chronic high-dose colchicine treatment. Further studies are warranted to elucidate metabolic effects of colchicine administration in murine diet-induced obesity models. Presentation: No date and time listed Oxford University Press 2022-11-01 /pmc/articles/PMC9624528/ http://dx.doi.org/10.1210/jendso/bvac150.003 Text en © The Author(s) 2022. Published by Oxford University Press on behalf of the Endocrine Society. https://creativecommons.org/licenses/by-nc-nd/4.0/This is an Open Access article distributed under the terms of the Creative Commons Attribution-NonCommercial-NoDerivs licence (https://creativecommons.org/licenses/by-nc-nd/4.0/), which permits non-commercial reproduction and distribution of the work, in any medium, provided the original work is not altered or transformed in any way, and that the work is properly cited. For commercial re-use, please contact journals.permissions@oup.com
spellingShingle Adipose Tissue, Appetite, & Obesity
Arner, Brooke E
Levine, Jordan A
Miller, Emily K
Patel, Tushar P
Jain, Arad
Gupta, Suryaa
Roberson, Robin B
Demidowich, Andrew P
Yanovski, Jack A
LBODP003 Effects Of 4-weeks’ Treatment With Intraperitoneal Colchicine On Metabolic And Inflammatory Outcomes In Mice Fed A High-fat Diet
title LBODP003 Effects Of 4-weeks’ Treatment With Intraperitoneal Colchicine On Metabolic And Inflammatory Outcomes In Mice Fed A High-fat Diet
title_full LBODP003 Effects Of 4-weeks’ Treatment With Intraperitoneal Colchicine On Metabolic And Inflammatory Outcomes In Mice Fed A High-fat Diet
title_fullStr LBODP003 Effects Of 4-weeks’ Treatment With Intraperitoneal Colchicine On Metabolic And Inflammatory Outcomes In Mice Fed A High-fat Diet
title_full_unstemmed LBODP003 Effects Of 4-weeks’ Treatment With Intraperitoneal Colchicine On Metabolic And Inflammatory Outcomes In Mice Fed A High-fat Diet
title_short LBODP003 Effects Of 4-weeks’ Treatment With Intraperitoneal Colchicine On Metabolic And Inflammatory Outcomes In Mice Fed A High-fat Diet
title_sort lbodp003 effects of 4-weeks’ treatment with intraperitoneal colchicine on metabolic and inflammatory outcomes in mice fed a high-fat diet
topic Adipose Tissue, Appetite, & Obesity
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9624528/
http://dx.doi.org/10.1210/jendso/bvac150.003
work_keys_str_mv AT arnerbrookee lbodp003effectsof4weekstreatmentwithintraperitonealcolchicineonmetabolicandinflammatoryoutcomesinmicefedahighfatdiet
AT levinejordana lbodp003effectsof4weekstreatmentwithintraperitonealcolchicineonmetabolicandinflammatoryoutcomesinmicefedahighfatdiet
AT milleremilyk lbodp003effectsof4weekstreatmentwithintraperitonealcolchicineonmetabolicandinflammatoryoutcomesinmicefedahighfatdiet
AT pateltusharp lbodp003effectsof4weekstreatmentwithintraperitonealcolchicineonmetabolicandinflammatoryoutcomesinmicefedahighfatdiet
AT jainarad lbodp003effectsof4weekstreatmentwithintraperitonealcolchicineonmetabolicandinflammatoryoutcomesinmicefedahighfatdiet
AT guptasuryaa lbodp003effectsof4weekstreatmentwithintraperitonealcolchicineonmetabolicandinflammatoryoutcomesinmicefedahighfatdiet
AT robersonrobinb lbodp003effectsof4weekstreatmentwithintraperitonealcolchicineonmetabolicandinflammatoryoutcomesinmicefedahighfatdiet
AT demidowichandrewp lbodp003effectsof4weekstreatmentwithintraperitonealcolchicineonmetabolicandinflammatoryoutcomesinmicefedahighfatdiet
AT yanovskijacka lbodp003effectsof4weekstreatmentwithintraperitonealcolchicineonmetabolicandinflammatoryoutcomesinmicefedahighfatdiet

Ejemplares similares