Modified activity-based anorexia paradigm dampens chronic food restriction-induced hyperadiponectinemia in adolescent female mice

Modified activity-based anorexia paradigm dampens chronic food restriction-induced hyperadiponectinemia in adolescent female mice

Anorexia nervosa (AN) is a chronic, life-threatening disease with mental and physical components that include excessive weight loss, persistent food restriction, and altered body image. It is sometimes accompanied by hyperactivity, day-night reversal, and amenorrhea. No medications have been approve...

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Veröffentlicht in:PloS one 2023-07, Vol.18 (7), p.e0289020-e0289020
Hauptverfasser: Kuriyama, Toru, Murata, Yusuke, Ohtani, Reika, Yahara, Rei, Nakashima, Soichiro, Mori, Masayoshi, Ohe, Kenji, Mine, Kazunori, Enjoji, Munechika
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Adiponectin
Adipose tissue
Adipose tissues
Amenorrhea
Analysis
Anorexia
Anorexia nervosa
Appetite
Biology and Life Sciences
Biomarkers
Body fat
Body image
Body mass index
Body weight
Body weight loss
Care and treatment
Chronic illnesses
Diagnosis
Eating disorders
Estrus cycle
Females
Food
Food availability
Food intake
Health aspects
Hyperactivity
Laboratory animals
Medicine and Health Sciences
Mice
Morphology
Mortality
Psychological aspects
Research and Analysis Methods
Teenage girls
Teenagers
Vagina
Weight control
Weight loss
Weight loss maintenance
Weight reduction
Wheel running
Youth
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container_volume 18
creator Kuriyama, Toru
Murata, Yusuke
Ohtani, Reika
Yahara, Rei
Nakashima, Soichiro
Mori, Masayoshi
Ohe, Kenji
Mine, Kazunori
Enjoji, Munechika
description Anorexia nervosa (AN) is a chronic, life-threatening disease with mental and physical components that include excessive weight loss, persistent food restriction, and altered body image. It is sometimes accompanied by hyperactivity, day-night reversal, and amenorrhea. No medications have been approved specific to the treatment of AN, partially due to its unclear etiopathogenesis. Because adiponectin is an appetite-regulating cytokine released by adipose tissue, we hypothesized that it could be useful as a specific biomarker that reflects the disease state of AN, so we developed a modified AN mouse model to test this hypothesis. Twenty-eight 3-week-old female C57BL/6J mice were randomly assigned to the following groups: 1) no intervention; 2) running wheel access; 3) food restriction (FR); and 4) activity-based anorexia (ABA) that included running wheel access plus FR. After a 10-day cage adaptation period, the mice of the FR and ABA groups were given 40% of their baseline food intake until 30% weight reduction (acute FR), then the body weight was maintained for 2.5 weeks (chronic FR). Running wheel activity and the incidence of the estrous cycle were assessed. Spontaneous food restriction and the plasma adiponectin level were evaluated at the end of the acute and chronic FR phases. An increase in running wheel activity was found in the light phase, and amenorrhea was found solely in the ABA group, which indicates that this is a good model of AN. This group showed a slight decrease in spontaneous food intake accompanied with an attenuated level of normally induced plasma adiponectin at the end of the chronic FR phase. These results indicate that the plasma adiponectin level may be a useful candidate biomarker for the status or stage of AN.
doi_str_mv 10.1371/journal.pone.0289020
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subjects Adiponectin
Adipose tissue
Adipose tissues
Amenorrhea
Analysis
Anorexia
Anorexia nervosa
Appetite
Biology and Life Sciences
Biomarkers
Body fat
Body image
Body mass index
Body weight
Body weight loss
Care and treatment
Chronic illnesses
Diagnosis
Eating disorders
Estrus cycle
Females
Food
Food availability
Food intake
Health aspects
Hyperactivity
Laboratory animals
Medicine and Health Sciences
Mice
Morphology
Mortality
Psychological aspects
Research and Analysis Methods
Teenage girls
Teenagers
Vagina
Weight control
Weight loss
Weight loss maintenance
Weight reduction
Wheel running
Youth
title Modified activity-based anorexia paradigm dampens chronic food restriction-induced hyperadiponectinemia in adolescent female mice
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