Inhibin βE (INHBE) is a possible insulin resistance-associated hepatokine identified by comprehensive gene expression analysis in human liver biopsy samples

The liver plays a major role in whole-body energy homeostasis by releasing secretory factors, termed hepatokines. To identify novel target genes associated with insulin resistance, we performed a comprehensive analysis of gene expression profiles using a DNA chip method in liver biopsy samples from...

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Published inPloS one Vol. 13; no. 3; p. e0194798
Main Authors Sugiyama, Masakazu, Kikuchi, Akihiro, Misu, Hirofumi, Igawa, Hirobumi, Ashihara, Motooki, Kushima, Youichi, Honda, Kiyofumi, Suzuki, Yoshiyuki, Kawabe, Yoshiki, Kaneko, Shuichi, Takamura, Toshinari
Format Journal Article
LanguageEnglish
Published United States Public Library of Science 29.03.2018
Public Library of Science (PLoS)
Subjects
Biology
Biology and life sciences
Biopsy
Body fat
Body mass
Body mass index
Body size
Body weight
Body weight gain
Deoxyribonucleic acid
Diabetes
Diabetes mellitus
Diabetes mellitus (non-insulin dependent)
DNA
Endocrinology
Energy balance
Gene expression
Glucose
Growth factors
Growth hormones
Homeostasis
Hormone replacement therapy
Human subjects
Inhibin
Insulin
Insulin resistance
Ketones
Liver
Medicine and Health Sciences
Metabolism
Mice
Musculoskeletal system
Mutation
Obesity
Pharmaceuticals
Research and Analysis Methods
Respiratory quotient
Rodents
siRNA
Target recognition
University graduates
United States > US
Japan
Online AccessGet full text
ISSN1932-6203
1932-6203
DOI10.1371/journal.pone.0194798

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Abstract The liver plays a major role in whole-body energy homeostasis by releasing secretory factors, termed hepatokines. To identify novel target genes associated with insulin resistance, we performed a comprehensive analysis of gene expression profiles using a DNA chip method in liver biopsy samples from humans with varying degrees of insulin resistance. Inhibin βE (INHBE) was identified as a novel putative hepatokine with hepatic gene expression that positively correlated with insulin resistance and body mass index in humans. Quantitative real time-PCR analysis also showed an increase in INHBE gene expression in independent liver samples from insulin-resistant human subjects. Additionally, Inhbe gene expression increased in the livers of db/db mice, a rodent model of type 2 diabetes. To preliminarily screen the role of Inhbe in vivo in whole-body energy metabolic status, hepatic mRNA was knocked down with siRNA for Inhbe (siINHBE) in db/db mice. Treatment with siINHBE suppressed body weight gain during the two-week experimental period, which was attributable to diminished fat rather than lean mass. Additionally, treatment with siINHBE decreased the respiratory quotient and increased plasma total ketone bodies compared with treatment with non-targeting siRNA, both of which suggest enhanced whole-body fat utilization. Our study suggests that INHBE functions as a possible hepatokine to alter the whole-body metabolic status under obese insulin-resistant conditions.
AbstractList The liver plays a major role in whole-body energy homeostasis by releasing secretory factors, termed hepatokines. To identify novel target genes associated with insulin resistance, we performed a comprehensive analysis of gene expression profiles using a DNA chip method in liver biopsy samples from humans with varying degrees of insulin resistance. Inhibin βE (INHBE) was identified as a novel putative hepatokine with hepatic gene expression that positively correlated with insulin resistance and body mass index in humans. Quantitative real time-PCR analysis also showed an increase in INHBE gene expression in independent liver samples from insulin-resistant human subjects. Additionally, Inhbe gene expression increased in the livers of db/db mice, a rodent model of type 2 diabetes. To preliminarily screen the role of Inhbe in vivo in whole-body energy metabolic status, hepatic mRNA was knocked down with siRNA for Inhbe (siINHBE) in db/db mice. Treatment with siINHBE suppressed body weight gain during the two-week experimental period, which was attributable to diminished fat rather than lean mass. Additionally, treatment with siINHBE decreased the respiratory quotient and increased plasma total ketone bodies compared with treatment with non-targeting siRNA, both of which suggest enhanced whole-body fat utilization. Our study suggests that INHBE functions as a possible hepatokine to alter the whole-body metabolic status under obese insulin-resistant conditions.
The liver plays a major role in whole-body energy homeostasis by releasing secretory factors, termed hepatokines. To identify novel target genes associated with insulin resistance, we performed a comprehensive analysis of gene expression profiles using a DNA chip method in liver biopsy samples from humans with varying degrees of insulin resistance. Inhibin βE ( INHBE ) was identified as a novel putative hepatokine with hepatic gene expression that positively correlated with insulin resistance and body mass index in humans. Quantitative real time-PCR analysis also showed an increase in INHBE gene expression in independent liver samples from insulin-resistant human subjects. Additionally, Inhbe gene expression increased in the livers of db/db mice, a rodent model of type 2 diabetes. To preliminarily screen the role of Inhbe in vivo in whole-body energy metabolic status, hepatic mRNA was knocked down with siRNA for Inhbe (siINHBE) in db/db mice. Treatment with siINHBE suppressed body weight gain during the two-week experimental period, which was attributable to diminished fat rather than lean mass. Additionally, treatment with siINHBE decreased the respiratory quotient and increased plasma total ketone bodies compared with treatment with non-targeting siRNA, both of which suggest enhanced whole-body fat utilization. Our study suggests that INHBE functions as a possible hepatokine to alter the whole-body metabolic status under obese insulin-resistant conditions.
The liver plays a major role in whole-body energy homeostasis by releasing secretory factors, termed hepatokines. To identify novel target genes associated with insulin resistance, we performed a comprehensive analysis of gene expression profiles using a DNA chip method in liver biopsy samples from humans with varying degrees of insulin resistance. Inhibin βE (INHBE) was identified as a novel putative hepatokine with hepatic gene expression that positively correlated with insulin resistance and body mass index in humans. Quantitative real time-PCR analysis also showed an increase in INHBE gene expression in independent liver samples from insulin-resistant human subjects. Additionally, Inhbe gene expression increased in the livers of db/db mice, a rodent model of type 2 diabetes. To preliminarily screen the role of Inhbe in vivo in whole-body energy metabolic status, hepatic mRNA was knocked down with siRNA for Inhbe (siINHBE) in db/db mice. Treatment with siINHBE suppressed body weight gain during the two-week experimental period, which was attributable to diminished fat rather than lean mass. Additionally, treatment with siINHBE decreased the respiratory quotient and increased plasma total ketone bodies compared with treatment with non-targeting siRNA, both of which suggest enhanced whole-body fat utilization. Our study suggests that INHBE functions as a possible hepatokine to alter the whole-body metabolic status under obese insulin-resistant conditions.The liver plays a major role in whole-body energy homeostasis by releasing secretory factors, termed hepatokines. To identify novel target genes associated with insulin resistance, we performed a comprehensive analysis of gene expression profiles using a DNA chip method in liver biopsy samples from humans with varying degrees of insulin resistance. Inhibin βE (INHBE) was identified as a novel putative hepatokine with hepatic gene expression that positively correlated with insulin resistance and body mass index in humans. Quantitative real time-PCR analysis also showed an increase in INHBE gene expression in independent liver samples from insulin-resistant human subjects. Additionally, Inhbe gene expression increased in the livers of db/db mice, a rodent model of type 2 diabetes. To preliminarily screen the role of Inhbe in vivo in whole-body energy metabolic status, hepatic mRNA was knocked down with siRNA for Inhbe (siINHBE) in db/db mice. Treatment with siINHBE suppressed body weight gain during the two-week experimental period, which was attributable to diminished fat rather than lean mass. Additionally, treatment with siINHBE decreased the respiratory quotient and increased plasma total ketone bodies compared with treatment with non-targeting siRNA, both of which suggest enhanced whole-body fat utilization. Our study suggests that INHBE functions as a possible hepatokine to alter the whole-body metabolic status under obese insulin-resistant conditions.
Author Misu, Hirofumi
Ashihara, Motooki
Suzuki, Yoshiyuki
Honda, Kiyofumi
Kawabe, Yoshiki
Kushima, Youichi
Sugiyama, Masakazu
Kikuchi, Akihiro
Takamura, Toshinari
Kaneko, Shuichi
Igawa, Hirobumi
AuthorAffiliation 3 Department of System Biology, Kanazawa University Graduate School of Medical Sciences, Kanazawa, Ishikawa, Japan
1 Research Division, Chugai Pharmaceutical Co., Ltd., Gotemba, Shizuoka, Japan
4 PRESTO, Japan Science and Technology Agency, Kawaguchi, Saitama, Japan
2 Department of Endocrinology and Metabolism, Kanazawa University Graduate School of Medical Sciences, Kanazawa, Ishikawa, Japan
INRA, FRANCE
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BackLink https://www.ncbi.nlm.nih.gov/pubmed/29596463$$D View this record in MEDLINE/PubMed
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Competing Interests: TT has received a grant support from Chugai Pharmaceutical Co, Ltd. Co-authors MS, MA, Y. Kushima, KH, YS, and Y. Kawabe are employed by Chugai Pharmaceutical Co, Ltd. There are no competing interests to declare for any of the other authors. These affiliations do not alter the authors' adherence to PLOS ONE policies on sharing data and materials.
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Snippet The liver plays a major role in whole-body energy homeostasis by releasing secretory factors, termed hepatokines. To identify novel target genes associated...
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StartPage e0194798
SubjectTerms Biology
Biology and life sciences
Biopsy
Body fat
Body mass
Body mass index
Body size
Body weight
Body weight gain
Deoxyribonucleic acid
Diabetes
Diabetes mellitus
Diabetes mellitus (non-insulin dependent)
DNA
Endocrinology
Energy balance
Gene expression
Glucose
Growth factors
Growth hormones
Homeostasis
Hormone replacement therapy
Human subjects
Inhibin
Insulin
Insulin resistance
Ketones
Liver
Medicine and Health Sciences
Metabolism
Mice
Musculoskeletal system
Mutation
Obesity
Pharmaceuticals
Research and Analysis Methods
Respiratory quotient
Rodents
siRNA
Target recognition
University graduates
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Title Inhibin βE (INHBE) is a possible insulin resistance-associated hepatokine identified by comprehensive gene expression analysis in human liver biopsy samples
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https://www.proquest.com/docview/2020481611
https://pubmed.ncbi.nlm.nih.gov/PMC5875797
https://doaj.org/article/3ed405419b0e48a2948fd11b5f597d6c
http://dx.doi.org/10.1371/journal.pone.0194798
Volume 13
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