Tumour‐derived leukaemia inhibitory factor is a major driver of cancer cachexia and morbidity in C26 tumour‐bearing mice

Tumour‐derived leukaemia inhibitory factor is a major driver of cancer cachexia and morbidity in C26 tumour‐bearing mice

Abstract Background Cancer cachexia is a metabolic wasting syndrome that is strongly associated with a poor prognosis. The initiating factors causing fat and muscle loss are largely unknown. Previously, we found that leukaemia inhibitory factor (LIF) secreted by C26 colon carcinoma cells was respons...

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Main Authors: Susan C. Kandarian, Rachel L. Nosacka, Andrea E. Delitto, Andrew R. Judge, Sarah M. Judge, John D. Ganey, Jesse D. Moreira, Robert W. Jackman
Format: Article
Language:English
Published: Wiley 2018-12-01
Series:Journal of Cachexia, Sarcopenia and Muscle
Subjects:
Skeletal muscle
Atrophy
Wasting
CRISPR
Tumour
Cachexia
Online Access:https://doi.org/10.1002/jcsm.12346
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spelling doaj-6a33b457614b447d98178b28dc1f45a72020-11-25T01:22:03ZengWileyJournal of Cachexia, Sarcopenia and Muscle2190-59912190-60092018-12-01961109112010.1002/jcsm.12346Tumour‐derived leukaemia inhibitory factor is a major driver of cancer cachexia and morbidity in C26 tumour‐bearing miceSusan C. Kandarian0Rachel L. Nosacka1Andrea E. Delitto2Andrew R. Judge3Sarah M. Judge4John D. Ganey5Jesse D. Moreira6Robert W. Jackman7Department of Health Sciences Boston University Boston MA 02215 USADepartment of Physical Therapy University of Florida Gainesville FL 32610 USADepartment of Oral Biology, College of Dentistry University of Florida Health Science Center Gainesville FL 32610 USADepartment of Physical Therapy University of Florida Gainesville FL 32610 USADepartment of Physical Therapy University of Florida Gainesville FL 32610 USADepartment of Health Sciences Boston University Boston MA 02215 USADepartment of Health Sciences Boston University Boston MA 02215 USADepartment of Health Sciences Boston University Boston MA 02215 USAAbstract Background Cancer cachexia is a metabolic wasting syndrome that is strongly associated with a poor prognosis. The initiating factors causing fat and muscle loss are largely unknown. Previously, we found that leukaemia inhibitory factor (LIF) secreted by C26 colon carcinoma cells was responsible for atrophy in treated myotubes. In the present study, we tested whether C26 tumour‐derived LIF is required for cancer cachexia in mice by knockout of Lif in C26 cells. Methods A C26 Lif null tumour cell line was made using CRISPR‐Cas9. Measurements of cachexia were compared in mice inoculated with C26 vs. C26Lif−/− tumour cells, and atrophy was compared in myotubes treated with medium from C26 vs. C26Lif−/− tumour cells. Levels of 25 cytokines/chemokines were compared in serum of mice bearing C26 vs. C26Lif−/− tumours and in the medium from these tumour cell lines. Results At study endpoint, C26 mice showed outward signs of sickness while mice with C26Lif−/− tumours appeared healthy. Mice with C26Lif−/− tumours showed a 55–75% amelioration of body weight loss, muscle loss, fat loss, and splenomegaly compared with mice with C26 tumours (P < 0.05). The heart was not affected by LIF levels because the loss of cardiac mass was the same in C26 and C26Lif−/− tumour‐bearing mice. LIF levels in mouse serum was entirely dependent on secretion from the tumour cells. Serum levels of interleukin‐6 and G‐CSF were increased by 79‐fold and 68‐fold, respectively, in C26 mice but only by five‐fold and two‐fold, respectively, in C26Lif−/− mice, suggesting that interleukin‐6 and G‐CSF increases are dependent on tumour‐derived LIF. Conclusions This study shows the first use of CRISPR‐Cas9 knockout of a candidate cachexia factor in tumour cells. The results provide direct evidence for LIF as a major cachexia initiating factor for the C26 tumour in vivo. Tumour‐derived LIF was also a regulator of multiple cytokines in C26 tumour cells and in C26 tumour‐bearing mice. The identification of tumour‐derived factors such as LIF that initiate the cachectic process is immediately applicable to the development of therapeutics to treat cachexia. This is a proof of principle for studies that when carried out in human cells, will make possible an understanding of the factors causing cachexia in a patient‐specific manner.https://doi.org/10.1002/jcsm.12346Skeletal muscleAtrophyWastingCRISPRTumourCachexia
collection DOAJ
language English
format Article
sources DOAJ
author Susan C. Kandarian
Rachel L. Nosacka
Andrea E. Delitto
Andrew R. Judge
Sarah M. Judge
John D. Ganey
Jesse D. Moreira
Robert W. Jackman
spellingShingle Susan C. Kandarian
Rachel L. Nosacka
Andrea E. Delitto
Andrew R. Judge
Sarah M. Judge
John D. Ganey
Jesse D. Moreira
Robert W. Jackman
Tumour‐derived leukaemia inhibitory factor is a major driver of cancer cachexia and morbidity in C26 tumour‐bearing mice
Journal of Cachexia, Sarcopenia and Muscle
Skeletal muscle
Atrophy
Wasting
CRISPR
Tumour
Cachexia
author_facet Susan C. Kandarian
Rachel L. Nosacka
Andrea E. Delitto
Andrew R. Judge
Sarah M. Judge
John D. Ganey
Jesse D. Moreira
Robert W. Jackman
author_sort Susan C. Kandarian
title Tumour‐derived leukaemia inhibitory factor is a major driver of cancer cachexia and morbidity in C26 tumour‐bearing mice
title_short Tumour‐derived leukaemia inhibitory factor is a major driver of cancer cachexia and morbidity in C26 tumour‐bearing mice
title_full Tumour‐derived leukaemia inhibitory factor is a major driver of cancer cachexia and morbidity in C26 tumour‐bearing mice
title_fullStr Tumour‐derived leukaemia inhibitory factor is a major driver of cancer cachexia and morbidity in C26 tumour‐bearing mice
title_full_unstemmed Tumour‐derived leukaemia inhibitory factor is a major driver of cancer cachexia and morbidity in C26 tumour‐bearing mice
title_sort tumour‐derived leukaemia inhibitory factor is a major driver of cancer cachexia and morbidity in c26 tumour‐bearing mice
publisher Wiley
series Journal of Cachexia, Sarcopenia and Muscle
issn 2190-5991
2190-6009
publishDate 2018-12-01
description Abstract Background Cancer cachexia is a metabolic wasting syndrome that is strongly associated with a poor prognosis. The initiating factors causing fat and muscle loss are largely unknown. Previously, we found that leukaemia inhibitory factor (LIF) secreted by C26 colon carcinoma cells was responsible for atrophy in treated myotubes. In the present study, we tested whether C26 tumour‐derived LIF is required for cancer cachexia in mice by knockout of Lif in C26 cells. Methods A C26 Lif null tumour cell line was made using CRISPR‐Cas9. Measurements of cachexia were compared in mice inoculated with C26 vs. C26Lif−/− tumour cells, and atrophy was compared in myotubes treated with medium from C26 vs. C26Lif−/− tumour cells. Levels of 25 cytokines/chemokines were compared in serum of mice bearing C26 vs. C26Lif−/− tumours and in the medium from these tumour cell lines. Results At study endpoint, C26 mice showed outward signs of sickness while mice with C26Lif−/− tumours appeared healthy. Mice with C26Lif−/− tumours showed a 55–75% amelioration of body weight loss, muscle loss, fat loss, and splenomegaly compared with mice with C26 tumours (P < 0.05). The heart was not affected by LIF levels because the loss of cardiac mass was the same in C26 and C26Lif−/− tumour‐bearing mice. LIF levels in mouse serum was entirely dependent on secretion from the tumour cells. Serum levels of interleukin‐6 and G‐CSF were increased by 79‐fold and 68‐fold, respectively, in C26 mice but only by five‐fold and two‐fold, respectively, in C26Lif−/− mice, suggesting that interleukin‐6 and G‐CSF increases are dependent on tumour‐derived LIF. Conclusions This study shows the first use of CRISPR‐Cas9 knockout of a candidate cachexia factor in tumour cells. The results provide direct evidence for LIF as a major cachexia initiating factor for the C26 tumour in vivo. Tumour‐derived LIF was also a regulator of multiple cytokines in C26 tumour cells and in C26 tumour‐bearing mice. The identification of tumour‐derived factors such as LIF that initiate the cachectic process is immediately applicable to the development of therapeutics to treat cachexia. This is a proof of principle for studies that when carried out in human cells, will make possible an understanding of the factors causing cachexia in a patient‐specific manner.
topic Skeletal muscle
Atrophy
Wasting
CRISPR
Tumour
Cachexia
url https://doi.org/10.1002/jcsm.12346
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