Doxorubicin-Induced Cardiotoxicity in Collaborative Cross (CC) Mice Recapitulates Individual Cardiotoxicity in Humans

Doxorubicin-Induced Cardiotoxicity in Collaborative Cross (CC) Mice Recapitulates Individual Cardiotoxicity in Humans

Anthracyclines cause progressive cardiotoxicity whose ultimate severity is individual to the patient. Genetic determinants contributing to this variation are difficult to study using current mouse models. Our objective was to determine whether a spectrum of anthracycline induced cardiac disease can...

Full description

Bibliographic Details
Main Authors: Caroline J. Zeiss, Daniel M. Gatti, Olga Toro-Salazar, Crystal Davis, Cathleen M. Lutz, Francis Spinale, Timothy Stearns, Milena B. Furtado, Gary A. Churchill
Format: Article
Language:English
Published: Oxford University Press 2019-08-01
Series:G3: Genes, Genomes, Genetics
Subjects:
Anthracyclines
cardiotoxicity
biomarkers
fibrosis
mouse
Online Access:http://g3journal.org/lookup/doi/10.1534/g3.119.400232
id doaj-fabbdfebe0ba4b8d96fa418a6dcfb938
record_format Article
spelling doaj-fabbdfebe0ba4b8d96fa418a6dcfb9382021-07-02T04:34:52ZengOxford University PressG3: Genes, Genomes, Genetics2160-18362019-08-01982637264610.1534/g3.119.40023224Doxorubicin-Induced Cardiotoxicity in Collaborative Cross (CC) Mice Recapitulates Individual Cardiotoxicity in HumansCaroline J. ZeissDaniel M. GattiOlga Toro-SalazarCrystal DavisCathleen M. LutzFrancis SpinaleTimothy StearnsMilena B. FurtadoGary A. ChurchillAnthracyclines cause progressive cardiotoxicity whose ultimate severity is individual to the patient. Genetic determinants contributing to this variation are difficult to study using current mouse models. Our objective was to determine whether a spectrum of anthracycline induced cardiac disease can be elicited across 10 Collaborative Cross mouse strains given the same dose of doxorubicin. Mice from ten distinct strains were given 5 mg/kg of doxorubicin intravenously once weekly for 5 weeks (total 25 mg/kg). Mice were killed at acute or chronic timepoints. Body weight was assessed weekly, followed by terminal complete blood count, pathology and a panel of biomarkers. Linear models were fit to assess effects of treatment, sex, and sex-by-treatment interactions for each timepoint. Impaired growth and cardiac pathology occurred across all strains. Severity of these varied by strain and sex, with greater severity in males. Cardiac troponin I and myosin light chain 3 demonstrated strain- and sex-specific elevations in the acute phase with subsequent decline despite ongoing progression of cardiac disease. Acute phase cardiac troponin I levels predicted the ultimate severity of cardiac pathology poorly, whereas myosin light chain 3 levels predicted the extent of chronic cardiac injury in males. Strain- and sex-dependent renal toxicity was evident. Regenerative anemia manifested during the acute period. We confirm that variable susceptibility to doxorubicin-induced cardiotoxicity observed in humans can be modeled in a panel of CC strains. In addition, we identified a potential predictive biomarker in males. CC strains provide reproducible models to explore mechanisms contributing to individual susceptibility in humans.http://g3journal.org/lookup/doi/10.1534/g3.119.400232Anthracyclinescardiotoxicitybiomarkersfibrosismouse
collection DOAJ
language English
format Article
sources DOAJ
author Caroline J. Zeiss
Daniel M. Gatti
Olga Toro-Salazar
Crystal Davis
Cathleen M. Lutz
Francis Spinale
Timothy Stearns
Milena B. Furtado
Gary A. Churchill
spellingShingle Caroline J. Zeiss
Daniel M. Gatti
Olga Toro-Salazar
Crystal Davis
Cathleen M. Lutz
Francis Spinale
Timothy Stearns
Milena B. Furtado
Gary A. Churchill
Doxorubicin-Induced Cardiotoxicity in Collaborative Cross (CC) Mice Recapitulates Individual Cardiotoxicity in Humans
G3: Genes, Genomes, Genetics
Anthracyclines
cardiotoxicity
biomarkers
fibrosis
mouse
author_facet Caroline J. Zeiss
Daniel M. Gatti
Olga Toro-Salazar
Crystal Davis
Cathleen M. Lutz
Francis Spinale
Timothy Stearns
Milena B. Furtado
Gary A. Churchill
author_sort Caroline J. Zeiss
title Doxorubicin-Induced Cardiotoxicity in Collaborative Cross (CC) Mice Recapitulates Individual Cardiotoxicity in Humans
title_short Doxorubicin-Induced Cardiotoxicity in Collaborative Cross (CC) Mice Recapitulates Individual Cardiotoxicity in Humans
title_full Doxorubicin-Induced Cardiotoxicity in Collaborative Cross (CC) Mice Recapitulates Individual Cardiotoxicity in Humans
title_fullStr Doxorubicin-Induced Cardiotoxicity in Collaborative Cross (CC) Mice Recapitulates Individual Cardiotoxicity in Humans
title_full_unstemmed Doxorubicin-Induced Cardiotoxicity in Collaborative Cross (CC) Mice Recapitulates Individual Cardiotoxicity in Humans
title_sort doxorubicin-induced cardiotoxicity in collaborative cross (cc) mice recapitulates individual cardiotoxicity in humans
publisher Oxford University Press
series G3: Genes, Genomes, Genetics
issn 2160-1836
publishDate 2019-08-01
description Anthracyclines cause progressive cardiotoxicity whose ultimate severity is individual to the patient. Genetic determinants contributing to this variation are difficult to study using current mouse models. Our objective was to determine whether a spectrum of anthracycline induced cardiac disease can be elicited across 10 Collaborative Cross mouse strains given the same dose of doxorubicin. Mice from ten distinct strains were given 5 mg/kg of doxorubicin intravenously once weekly for 5 weeks (total 25 mg/kg). Mice were killed at acute or chronic timepoints. Body weight was assessed weekly, followed by terminal complete blood count, pathology and a panel of biomarkers. Linear models were fit to assess effects of treatment, sex, and sex-by-treatment interactions for each timepoint. Impaired growth and cardiac pathology occurred across all strains. Severity of these varied by strain and sex, with greater severity in males. Cardiac troponin I and myosin light chain 3 demonstrated strain- and sex-specific elevations in the acute phase with subsequent decline despite ongoing progression of cardiac disease. Acute phase cardiac troponin I levels predicted the ultimate severity of cardiac pathology poorly, whereas myosin light chain 3 levels predicted the extent of chronic cardiac injury in males. Strain- and sex-dependent renal toxicity was evident. Regenerative anemia manifested during the acute period. We confirm that variable susceptibility to doxorubicin-induced cardiotoxicity observed in humans can be modeled in a panel of CC strains. In addition, we identified a potential predictive biomarker in males. CC strains provide reproducible models to explore mechanisms contributing to individual susceptibility in humans.
topic Anthracyclines
cardiotoxicity
biomarkers
fibrosis
mouse
url http://g3journal.org/lookup/doi/10.1534/g3.119.400232
work_keys_str_mv AT carolinejzeiss doxorubicininducedcardiotoxicityincollaborativecrossccmicerecapitulatesindividualcardiotoxicityinhumans
AT danielmgatti doxorubicininducedcardiotoxicityincollaborativecrossccmicerecapitulatesindividualcardiotoxicityinhumans
AT olgatorosalazar doxorubicininducedcardiotoxicityincollaborativecrossccmicerecapitulatesindividualcardiotoxicityinhumans
AT crystaldavis doxorubicininducedcardiotoxicityincollaborativecrossccmicerecapitulatesindividualcardiotoxicityinhumans
AT cathleenmlutz doxorubicininducedcardiotoxicityincollaborativecrossccmicerecapitulatesindividualcardiotoxicityinhumans
AT francisspinale doxorubicininducedcardiotoxicityincollaborativecrossccmicerecapitulatesindividualcardiotoxicityinhumans
AT timothystearns doxorubicininducedcardiotoxicityincollaborativecrossccmicerecapitulatesindividualcardiotoxicityinhumans
AT milenabfurtado doxorubicininducedcardiotoxicityincollaborativecrossccmicerecapitulatesindividualcardiotoxicityinhumans
AT garyachurchill doxorubicininducedcardiotoxicityincollaborativecrossccmicerecapitulatesindividualcardiotoxicityinhumans
_version_ 1721339862808788992

Similar Items