Severe gestational diabetes mellitus in lean dams is associated with low IL-1α levels and affects the growth of the juvenile mouse offspring
We investigated how maternal gestational diabetes (GDM) impacts the metabolic status of offspring. GDM was induced in CD1 mice consuming a fast-food diet (FFD) by repeated low-dose streptozotocin injections before mating. Offspring of normoglycemic standard chow or the FFD consuming dams served as c...
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Published in | Scientific reports Vol. 13; no. 1; pp. 1700 - 14 |
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Main Authors | , , , , , , , , , , |
Format | Journal Article |
Language | English |
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London
Nature Publishing Group UK
30.01.2023
Nature Publishing Group Nature Portfolio |
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Online Access | Get full text |
ISSN | 2045-2322 2045-2322 |
DOI | 10.1038/s41598-023-28903-7 |
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Abstract | We investigated how maternal gestational diabetes (GDM) impacts the metabolic status of offspring. GDM was induced in CD1 mice consuming a fast-food diet (FFD) by repeated low-dose streptozotocin injections before mating. Offspring of normoglycemic standard chow or the FFD consuming dams served as controls. In 4-week-old offspring weaned to standard chow, plasma concentrations of extracellular DNA, inflammatory markers, and parameters of the cardiometabolic status (glycemia, liver lipid content; body, organ, and fat weight) were determined. Two-factor analysis of variance indicated that the male offspring of GDM dams manifest postnatal growth retardation and lower relative kidney weight. Regardless of sex, GDM offspring manifest the lowest IL-1α levels, and other inflammatory markers showed mild and inconsistent alterations. Offspring of dams consuming the FFD displayed higher liver triacylglycerols content. The three groups of offspring showed no significant differences in glycemia and extracellular DNA. Partial least squares-discriminant analysis indicated that male GDM offspring present lower kidney, body, and brown adipose tissue weights; lower IL-1α levels, and higher concentrations of GM-CSF and IL-10 compared with their FFD counterparts. The model failed to select discriminative variables in females. In conclusion, in mice, maternal GDM in the absence of obesity adversely affects the early growth of juvenile male offspring. |
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AbstractList | We investigated how maternal gestational diabetes (GDM) impacts the metabolic status of offspring. GDM was induced in CD1 mice consuming a fast-food diet (FFD) by repeated low-dose streptozotocin injections before mating. Offspring of normoglycemic standard chow or the FFD consuming dams served as controls. In 4-week-old offspring weaned to standard chow, plasma concentrations of extracellular DNA, inflammatory markers, and parameters of the cardiometabolic status (glycemia, liver lipid content; body, organ, and fat weight) were determined. Two-factor analysis of variance indicated that the male offspring of GDM dams manifest postnatal growth retardation and lower relative kidney weight. Regardless of sex, GDM offspring manifest the lowest IL-1α levels, and other inflammatory markers showed mild and inconsistent alterations. Offspring of dams consuming the FFD displayed higher liver triacylglycerols content. The three groups of offspring showed no significant differences in glycemia and extracellular DNA. Partial least squares-discriminant analysis indicated that male GDM offspring present lower kidney, body, and brown adipose tissue weights; lower IL-1α levels, and higher concentrations of GM-CSF and IL-10 compared with their FFD counterparts. The model failed to select discriminative variables in females. In conclusion, in mice, maternal GDM in the absence of obesity adversely affects the early growth of juvenile male offspring. We investigated how maternal gestational diabetes (GDM) impacts the metabolic status of offspring. GDM was induced in CD1 mice consuming a fast-food diet (FFD) by repeated low-dose streptozotocin injections before mating. Offspring of normoglycemic standard chow or the FFD consuming dams served as controls. In 4-week-old offspring weaned to standard chow, plasma concentrations of extracellular DNA, inflammatory markers, and parameters of the cardiometabolic status (glycemia, liver lipid content; body, organ, and fat weight) were determined. Two-factor analysis of variance indicated that the male offspring of GDM dams manifest postnatal growth retardation and lower relative kidney weight. Regardless of sex, GDM offspring manifest the lowest IL-1α levels, and other inflammatory markers showed mild and inconsistent alterations. Offspring of dams consuming the FFD displayed higher liver triacylglycerols content. The three groups of offspring showed no significant differences in glycemia and extracellular DNA. Partial least squares-discriminant analysis indicated that male GDM offspring present lower kidney, body, and brown adipose tissue weights; lower IL-1α levels, and higher concentrations of GM-CSF and IL-10 compared with their FFD counterparts. The model failed to select discriminative variables in females. In conclusion, in mice, maternal GDM in the absence of obesity adversely affects the early growth of juvenile male offspring.We investigated how maternal gestational diabetes (GDM) impacts the metabolic status of offspring. GDM was induced in CD1 mice consuming a fast-food diet (FFD) by repeated low-dose streptozotocin injections before mating. Offspring of normoglycemic standard chow or the FFD consuming dams served as controls. In 4-week-old offspring weaned to standard chow, plasma concentrations of extracellular DNA, inflammatory markers, and parameters of the cardiometabolic status (glycemia, liver lipid content; body, organ, and fat weight) were determined. Two-factor analysis of variance indicated that the male offspring of GDM dams manifest postnatal growth retardation and lower relative kidney weight. Regardless of sex, GDM offspring manifest the lowest IL-1α levels, and other inflammatory markers showed mild and inconsistent alterations. Offspring of dams consuming the FFD displayed higher liver triacylglycerols content. The three groups of offspring showed no significant differences in glycemia and extracellular DNA. Partial least squares-discriminant analysis indicated that male GDM offspring present lower kidney, body, and brown adipose tissue weights; lower IL-1α levels, and higher concentrations of GM-CSF and IL-10 compared with their FFD counterparts. The model failed to select discriminative variables in females. In conclusion, in mice, maternal GDM in the absence of obesity adversely affects the early growth of juvenile male offspring. Abstract We investigated how maternal gestational diabetes (GDM) impacts the metabolic status of offspring. GDM was induced in CD1 mice consuming a fast-food diet (FFD) by repeated low-dose streptozotocin injections before mating. Offspring of normoglycemic standard chow or the FFD consuming dams served as controls. In 4-week-old offspring weaned to standard chow, plasma concentrations of extracellular DNA, inflammatory markers, and parameters of the cardiometabolic status (glycemia, liver lipid content; body, organ, and fat weight) were determined. Two-factor analysis of variance indicated that the male offspring of GDM dams manifest postnatal growth retardation and lower relative kidney weight. Regardless of sex, GDM offspring manifest the lowest IL-1α levels, and other inflammatory markers showed mild and inconsistent alterations. Offspring of dams consuming the FFD displayed higher liver triacylglycerols content. The three groups of offspring showed no significant differences in glycemia and extracellular DNA. Partial least squares-discriminant analysis indicated that male GDM offspring present lower kidney, body, and brown adipose tissue weights; lower IL-1α levels, and higher concentrations of GM-CSF and IL-10 compared with their FFD counterparts. The model failed to select discriminative variables in females. In conclusion, in mice, maternal GDM in the absence of obesity adversely affects the early growth of juvenile male offspring. |
ArticleNumber | 1700 |
Author | Uličná, Oľga Šebeková, Katarína Mihalovičová, Lucia Rausová, Zuzana Gurecká, Radana Janko, Jakub Pastorek, Michal Kunšteková, Veronika Celec, Peter Miláček, Dávid Konečná, Barbora |
Author_xml | – sequence: 1 givenname: Lucia surname: Mihalovičová fullname: Mihalovičová, Lucia organization: Institute of Molecular Biomedicine, Faculty of Medicine, Comenius University – sequence: 2 givenname: Veronika surname: Kunšteková fullname: Kunšteková, Veronika organization: Institute of Molecular Biomedicine, Faculty of Medicine, Comenius University, Department of Biology, Faculty of Medicine, Slovak Medical University – sequence: 3 givenname: Dávid surname: Miláček fullname: Miláček, Dávid organization: Institute of Molecular Biomedicine, Faculty of Medicine, Comenius University – sequence: 4 givenname: Jakub surname: Janko fullname: Janko, Jakub organization: Institute of Molecular Biomedicine, Faculty of Medicine, Comenius University – sequence: 5 givenname: Michal surname: Pastorek fullname: Pastorek, Michal organization: Institute of Molecular Biomedicine, Faculty of Medicine, Comenius University – sequence: 6 givenname: Barbora surname: Konečná fullname: Konečná, Barbora organization: Institute of Molecular Biomedicine, Faculty of Medicine, Comenius University – sequence: 7 givenname: Radana surname: Gurecká fullname: Gurecká, Radana organization: Institute of Molecular Biomedicine, Faculty of Medicine, Comenius University, Institute of Medical Physics, Biophysics, Informatics and Telemedicine, Faculty of Medicine, Comenius University – sequence: 8 givenname: Zuzana surname: Rausová fullname: Rausová, Zuzana organization: Pharmacobiochemical Laboratory of 3rd Department of Internal Medicine, Faculty of Medicine, Comenius University – sequence: 9 givenname: Oľga surname: Uličná fullname: Uličná, Oľga organization: Pharmacobiochemical Laboratory of 3rd Department of Internal Medicine, Faculty of Medicine, Comenius University – sequence: 10 givenname: Peter surname: Celec fullname: Celec, Peter organization: Institute of Molecular Biomedicine, Faculty of Medicine, Comenius University, Institute of Pathophysiology, Faculty of Medicine, Comenius University, Department of Molecular Biology, Faculty of Natural Sciences, Comenius University – sequence: 11 givenname: Katarína surname: Šebeková fullname: Šebeková, Katarína email: kata.sebekova@gmail.com organization: Institute of Molecular Biomedicine, Faculty of Medicine, Comenius University |
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Snippet | We investigated how maternal gestational diabetes (GDM) impacts the metabolic status of offspring. GDM was induced in CD1 mice consuming a fast-food diet (FFD)... Abstract We investigated how maternal gestational diabetes (GDM) impacts the metabolic status of offspring. GDM was induced in CD1 mice consuming a fast-food... |
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SubjectTerms | 631/136 631/337 631/443 692/4017 692/53 Adipose tissue Adipose tissue (brown) Animals Blood glucose Deoxyribonucleic acid Diabetes mellitus Diabetes, Gestational - metabolism Diet Discriminant analysis DNA Factor analysis Fast food Female Gestational diabetes Granulocyte-macrophage colony-stimulating factor Growth rate Humanities and Social Sciences Humans Inflammation Interleukin 10 Kidneys Liver Liver - metabolism Male Mice multidisciplinary Nutrient deficiency Obesity - complications Offspring Pregnancy Prenatal Exposure Delayed Effects - metabolism Science Science (multidisciplinary) Streptozocin Variance analysis |
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Title | Severe gestational diabetes mellitus in lean dams is associated with low IL-1α levels and affects the growth of the juvenile mouse offspring |
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