Comparative effects of human-equivalent low, moderate, and high dose oral prednisone intake on autoimmunity and glucocorticoid-related toxicity in a murine model of environmental-triggered lupus

Autoimmune diseases can be triggered by environmental toxicants such as crystalline silica dust (cSiO(2)). Here, we characterized the dose-dependent immunomodulation and toxicity of the glucocorticoid (GC) prednisone in a preclinical model that emulates onset and progression of cSiO(2)-triggered lup...

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Autores principales: Heine, Lauren K., Benninghoff, Abby D., Ross, Elizabeth A., Rajasinghe, Lichchavi D., Wagner, James G., Lewandowski, Ryan P., Richardson, Alexa L., Li, Quan-Zhen, Buchweitz, John P., Zyskowski, Justin, Tindle, Ashleigh N., Skedel, Anna E., Chargo, Nicholas J., McCabe, Laura R., Harkema, Jack R., Pestka, James J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2022
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9627297/
https://www.ncbi.nlm.nih.gov/pubmed/36341330
http://dx.doi.org/10.3389/fimmu.2022.972108
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author Heine, Lauren K.
Benninghoff, Abby D.
Ross, Elizabeth A.
Rajasinghe, Lichchavi D.
Wagner, James G.
Lewandowski, Ryan P.
Richardson, Alexa L.
Li, Quan-Zhen
Buchweitz, John P.
Zyskowski, Justin
Tindle, Ashleigh N.
Skedel, Anna E.
Chargo, Nicholas J.
McCabe, Laura R.
Harkema, Jack R.
Pestka, James J.
author_facet Heine, Lauren K.
Benninghoff, Abby D.
Ross, Elizabeth A.
Rajasinghe, Lichchavi D.
Wagner, James G.
Lewandowski, Ryan P.
Richardson, Alexa L.
Li, Quan-Zhen
Buchweitz, John P.
Zyskowski, Justin
Tindle, Ashleigh N.
Skedel, Anna E.
Chargo, Nicholas J.
McCabe, Laura R.
Harkema, Jack R.
Pestka, James J.
author_sort Heine, Lauren K.
collection PubMed
description Autoimmune diseases can be triggered by environmental toxicants such as crystalline silica dust (cSiO(2)). Here, we characterized the dose-dependent immunomodulation and toxicity of the glucocorticoid (GC) prednisone in a preclinical model that emulates onset and progression of cSiO(2)-triggered lupus. Two cohorts of 6-wk-old female NZBWF1 mice were fed either control AIN-93G diet or one of three AIN-93G diets containing prednisone at 5, 15, or 50 mg/kg diet which span human equivalent oral doses (HED) currently considered to be low (PL; 5 mg/d HED), moderate (PM; 14 mg/d HED), or high (PH; 46 mg/d HED), respectively. At 8 wk of age, mice were intranasally instilled with either saline vehicle or 1 mg cSiO(2) once weekly for 4 wk. The experimental plan was to 1) terminate one cohort of mice (n=8/group) 14 wk after the last cSiO(2) instillation for pathology and autoimmunity assessment and 2) to maintain a second cohort (n=9/group) to monitor glomerulonephritis development and survival. Mean blood concentrations of prednisone’s principal active metabolite, prednisolone, in mice fed PL, PM, and PH diets were 27, 105, 151 ng/ml, respectively, which are consistent with levels observed in human blood ≤ 12 h after single bolus treatments with equivalent prednisone doses. Results from the first cohort revealed that consumption of PM, but not PL diet, significantly reduced cSiO(2)-induced pulmonary ectopic lymphoid structure formation, nuclear-specific AAb production, inflammation/autoimmune gene expression in the lung and kidney, splenomegaly, and glomerulonephritis in the kidney. Relative to GC-associated toxicity, PM diet, but not PL diet, elicited muscle wasting, but these diets did not affect bone density or cause glucosuria. Importantly, neither PM nor PL diet improved latency of cSiO(2)-accelerated death. PH-fed mice in both cohorts displayed robust GC-associated toxicity including body weight loss, reduced muscle mass, and extensive glucosuria 7 wk after the final cSiO(2) instillation requiring their early removal from the study. Taken together, our results demonstrate that while moderate doses of prednisone can reduce important pathological endpoints of cSiO(2)-induced autoimmunity in lupus-prone mice, such as upstream ectopic lymphoid structure formation, these ameliorative effects come with unwanted GC toxicity, and, crucially, none of these three doses extended survival time.
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spelling pubmed-96272972022-11-03 Comparative effects of human-equivalent low, moderate, and high dose oral prednisone intake on autoimmunity and glucocorticoid-related toxicity in a murine model of environmental-triggered lupus Heine, Lauren K. Benninghoff, Abby D. Ross, Elizabeth A. Rajasinghe, Lichchavi D. Wagner, James G. Lewandowski, Ryan P. Richardson, Alexa L. Li, Quan-Zhen Buchweitz, John P. Zyskowski, Justin Tindle, Ashleigh N. Skedel, Anna E. Chargo, Nicholas J. McCabe, Laura R. Harkema, Jack R. Pestka, James J. Front Immunol Immunology Autoimmune diseases can be triggered by environmental toxicants such as crystalline silica dust (cSiO(2)). Here, we characterized the dose-dependent immunomodulation and toxicity of the glucocorticoid (GC) prednisone in a preclinical model that emulates onset and progression of cSiO(2)-triggered lupus. Two cohorts of 6-wk-old female NZBWF1 mice were fed either control AIN-93G diet or one of three AIN-93G diets containing prednisone at 5, 15, or 50 mg/kg diet which span human equivalent oral doses (HED) currently considered to be low (PL; 5 mg/d HED), moderate (PM; 14 mg/d HED), or high (PH; 46 mg/d HED), respectively. At 8 wk of age, mice were intranasally instilled with either saline vehicle or 1 mg cSiO(2) once weekly for 4 wk. The experimental plan was to 1) terminate one cohort of mice (n=8/group) 14 wk after the last cSiO(2) instillation for pathology and autoimmunity assessment and 2) to maintain a second cohort (n=9/group) to monitor glomerulonephritis development and survival. Mean blood concentrations of prednisone’s principal active metabolite, prednisolone, in mice fed PL, PM, and PH diets were 27, 105, 151 ng/ml, respectively, which are consistent with levels observed in human blood ≤ 12 h after single bolus treatments with equivalent prednisone doses. Results from the first cohort revealed that consumption of PM, but not PL diet, significantly reduced cSiO(2)-induced pulmonary ectopic lymphoid structure formation, nuclear-specific AAb production, inflammation/autoimmune gene expression in the lung and kidney, splenomegaly, and glomerulonephritis in the kidney. Relative to GC-associated toxicity, PM diet, but not PL diet, elicited muscle wasting, but these diets did not affect bone density or cause glucosuria. Importantly, neither PM nor PL diet improved latency of cSiO(2)-accelerated death. PH-fed mice in both cohorts displayed robust GC-associated toxicity including body weight loss, reduced muscle mass, and extensive glucosuria 7 wk after the final cSiO(2) instillation requiring their early removal from the study. Taken together, our results demonstrate that while moderate doses of prednisone can reduce important pathological endpoints of cSiO(2)-induced autoimmunity in lupus-prone mice, such as upstream ectopic lymphoid structure formation, these ameliorative effects come with unwanted GC toxicity, and, crucially, none of these three doses extended survival time. Frontiers Media S.A. 2022-10-19 /pmc/articles/PMC9627297/ /pubmed/36341330 http://dx.doi.org/10.3389/fimmu.2022.972108 Text en Copyright © 2022 Heine, Benninghoff, Ross, Rajasinghe, Wagner, Lewandowski, Richardson, Li, Buchweitz, Zyskowski, Tindle, Skedel, Chargo, McCabe, Harkema and Pestka https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Immunology
Heine, Lauren K.
Benninghoff, Abby D.
Ross, Elizabeth A.
Rajasinghe, Lichchavi D.
Wagner, James G.
Lewandowski, Ryan P.
Richardson, Alexa L.
Li, Quan-Zhen
Buchweitz, John P.
Zyskowski, Justin
Tindle, Ashleigh N.
Skedel, Anna E.
Chargo, Nicholas J.
McCabe, Laura R.
Harkema, Jack R.
Pestka, James J.
Comparative effects of human-equivalent low, moderate, and high dose oral prednisone intake on autoimmunity and glucocorticoid-related toxicity in a murine model of environmental-triggered lupus
title Comparative effects of human-equivalent low, moderate, and high dose oral prednisone intake on autoimmunity and glucocorticoid-related toxicity in a murine model of environmental-triggered lupus
title_full Comparative effects of human-equivalent low, moderate, and high dose oral prednisone intake on autoimmunity and glucocorticoid-related toxicity in a murine model of environmental-triggered lupus
title_fullStr Comparative effects of human-equivalent low, moderate, and high dose oral prednisone intake on autoimmunity and glucocorticoid-related toxicity in a murine model of environmental-triggered lupus
title_full_unstemmed Comparative effects of human-equivalent low, moderate, and high dose oral prednisone intake on autoimmunity and glucocorticoid-related toxicity in a murine model of environmental-triggered lupus
title_short Comparative effects of human-equivalent low, moderate, and high dose oral prednisone intake on autoimmunity and glucocorticoid-related toxicity in a murine model of environmental-triggered lupus
title_sort comparative effects of human-equivalent low, moderate, and high dose oral prednisone intake on autoimmunity and glucocorticoid-related toxicity in a murine model of environmental-triggered lupus
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9627297/
https://www.ncbi.nlm.nih.gov/pubmed/36341330
http://dx.doi.org/10.3389/fimmu.2022.972108
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