Your search keyword '"Adipose Tissue physiology"' showing total 8,470 results

201. Age‐associated adipose tissue inflammation promotes monocyte chemotaxis and enhances atherosclerosis.

Author

Song, Jianrui, Farris, Diana, Ariza, Paola, Moorjani, Smriti, Varghese, Mita, Blin, Muriel, Chen, Judy, Tyrrell, Daniel, Zhang, Min, Singer, Kanakadurga, Salmon, Morgan, and Goldstein, Daniel R.

Subjects

*ADIPOSE tissues, *INFLAMMATORY mediators, *ATHEROSCLEROSIS, *ATHEROSCLEROTIC plaque, *ADIPOSE tissue physiology, *LIPID metabolism, *CAROTID artery, *CHEMOTAXIS

Abstract

Although aging enhances atherosclerosis, we do not know if this occurs via alterations in circulating immune cells, lipid metabolism, vasculature, or adipose tissue. Here, we examined whether aging exerts a direct pro‐atherogenic effect on adipose tissue in mice. After demonstrating that aging augmented the inflammatory profile of visceral but not subcutaneous adipose tissue, we transplanted visceral fat from young or aged mice onto the right carotid artery of Ldlr−/− recipients. Aged fat transplants not only increased atherosclerotic plaque size with increased macrophage numbers in the adjacent carotid artery, but also in distal vascular territories, indicating that aging of the adipose tissue enhances atherosclerosis via secreted factors. By depleting macrophages from the visceral fat, we identified that adipose tissue macrophages are major contributors of the secreted factors. To identify these inflammatory factors, we found that aged fat transplants secreted increased levels of the inflammatory mediators TNFα, CXCL2, and CCL2, which synergized to promote monocyte chemotaxis. Importantly, the combined blockade of these inflammatory mediators impeded the ability of aged fat transplants to enhance atherosclerosis. In conclusion, our study reveals that aging enhances atherosclerosis via increased inflammation of visceral fat. Our study suggests that future therapies targeting the visceral fat may reduce atherosclerosis disease burden in the expanding older population. [ABSTRACT FROM AUTHOR]

Published

2023

202. Role of gremlin-1 in the pathophysiology of the adipose tissues.

Author

Grillo, Elisabetta, Ravelli, Cosetta, Colleluori, Georgia, D'Agostino, Francesco, Domenichini, Mattia, Giordano, Antonio, and Mitola, Stefania

Subjects

*VASCULAR endothelial growth factor receptors, *WOUND healing, *BONE morphogenetic proteins, *PATHOLOGICAL physiology, *ADIPOSE tissues, *NON-alcoholic fatty liver disease, *ADIPOSE tissue physiology, *BROWN adipose tissue

Abstract

Gremlin-1 is a secreted bone morphogenetic protein (BMP) antagonist playing a pivotal role in the regulation of tissue formation and embryonic development. Since its first identification in 1997, gremlin-1 has been shown to be a multifunctional factor involved in wound healing, inflammation, cancer and tissue fibrosis. Among others, the activity of gremlin-1 is mediated by its interaction with BMPs or with membrane receptors such as the vascular endothelial growth factor receptor 2 (VEGFR2) or heparan sulfate proteoglycans (HSPGs). Growing evidence has highlighted a central role of gremlin-1 in the homeostasis of the adipose tissue (AT). Of note, gremlin-1 is involved in AT dysfunction during type 2 diabetes, obesity and non-alcoholic fatty liver disease (NAFLD) metabolic disorders. In this review we discuss recent findings on gremlin-1 involvement in AT biology, with particular attention to its role in metabolic diseases, to highlight its potential as a prognostic marker and therapeutic target. [Display omitted] • Gremlin-1 is a multifunctional secreted factor controlling development, angiogenesis and tissue fibrosis. • Gremlin-1 is an emerging adipokine controlling adipose tissue pathophysiology. • Gremlin-1 regulates adipogenesis and adipose tissue browning. • Gremlin-1 is overexpressed in obesity, diabetes and NAFLD and correlates with pathogenicity. • Gremlin-1 could become an attractive biomarker/therapeutic target for adipose tissue dysfunction. [ABSTRACT FROM AUTHOR]

Published

2023

203. Common Regulators of Lipid Metabolism and Bone Marrow Adiposity in Postmenopausal Women.

Author

Kim, Dae-Yong and Ko, Seong-Hee

Subjects

*LIPID metabolism, *BONE metabolism, *ESTROGEN receptors, *POSTMENOPAUSE, *ADIPOSE tissue physiology, *BONE marrow, *BLOOD lipids, *FATTY acid oxidation

Abstract

A variety of metabolic disorders are associated with a decrease in estradiol (E2) during natural or surgical menopause. Postmenopausal women are prone to excessive fat accumulation in skeletal muscle and adipose tissue due to the loss of E2 via abnormalities in lipid metabolism and serum lipid levels. In skeletal muscle and adipose tissue, genes related to energy metabolism and fatty acid oxidation, such as those encoding peroxisome proliferator-activated receptor-γ coactivator 1α (PGC-1α) and estrogen-related receptor alpha (ERRα), are downregulated, leading to increased fat synthesis and lipid metabolite accumulation. The same genes regulate lipid metabolism abnormalities in the bone marrow. In this review, abnormalities in lipid metabolism caused by E2 deficiency were investigated, with a focus on genes able to simultaneously regulate not only skeletal muscle and adipose tissue but also bone metabolism (e.g., genes encoding PGC-1α and ERRα). In addition, the mechanisms through which mesenchymal stem cells lead to adipocyte differentiation in the bone marrow as well as metabolic processes related to bone marrow adiposity, bone loss, and osteoporosis were evaluated, focusing on the loss of E2 and lipid metabolic alterations. The work reviewed here suggests that genes underlying lipid metabolism and bone marrow adiposity are candidate therapeutic targets for bone loss and osteoporosis in postmenopausal women. [ABSTRACT FROM AUTHOR]

Published

2023

204. Disturbance of lipid metabolism in germ-free mice transplanted with gut microbiota of DSS-induced colitis mice.

Author

Lee, Chungho, Kim, SangAh, Kim, Bobae, Holzapfel, Wilhelm H., and Hyun, Chang-Kee

Subjects

*ADIPOSE tissue physiology, *CHOLESTEROL metabolism, *SHORT-chain fatty acids, *GUT microbiome, *LIPID metabolism, *INFLAMMATORY bowel diseases, *FECAL microbiota transplantation, *ADIPONECTIN, *INSULIN receptors

Abstract

Hepatobiliary abnormality and metabolic disorders are frequently observed complications in patients with inflammatory bowel diseases (IBD). Given that microbiota dysbiosis is a common pathophysiological feature of both IBD and metabolic diseases, we examined how the IBD-induced dysbiosis affects the host metabolism and contributes to the development of associated metabolic diseases using germ-free (GF) mice transplanted with fecal microbiota of DSS-induced colitis mice. There was no significant change in inflammation or barrier integrity in the gut of GF mice that received microbiota from colitis mice compared to their counterparts that were transplanted with microbiota from non-colitis healthy mice. Interestingly, it was observed that the GF recipients of colitis-induced altered microbiota showed a significant decrease in the weight of adipose tissues including mesenteric, epididymal, subcutaneous, and brown fat without any change in body weight, which was accompanied by abnormalities in adipose tissue functions such as fat storage and adiponectin production. Transplantation of colitis-induced altered microbiota also disrupted hepatic lipid metabolism in the GF recipient mice, which was observed by increases in synthesis and accumulation of cholesterol and bile acids in hepatocytes and a decrease in plasma HDL-cholesterol. Additional observations including elevated plasma levels of insulin, decreased hepatic production of FGF21, and decreased levels of fecal short chain fatty acids (SCFAs) and hepatic expression of SCFA receptors led to a conclusion that the transplantation of the colitis-associated dysbiotic microbiota was causally associated with impairments of insulin action and FGF21-adiponectin axis, possibly due to the low SCFA-producing capacity of the colonized microbiota, leading to metabolic abnormalities including adipose tissue dysfunction and dysregulated hepatic lipid metabolism. Our findings suggest potential mechanisms that explain how colitis-associated gut dysbiosis may contribute to the development of metabolic dysfunctions, which could be applied to clinical practice to improve the efficacy of treatment of IBD patients with comorbid metabolic disorders or vice versa. [ABSTRACT FROM AUTHOR]

Published

2023

205. Whole-Body Vibration Training on Oxidative Stress Markers, Irisin Levels, and Body Composition in Women with Fibromyalgia: A Randomized Controlled Trial.

Author

dos Santos, Jousielle Márcia, Taiar, Redha, Ribeiro, Vanessa Gonçalves César, da Silva Lage, Vanessa Kelly, Scheidt Figueiredo, Pedro Henrique, Costa, Henrique Silveira, Pereira Lima, Vanessa, Sañudo, Borja, Bernardo-Filho, Mário, Sá-Caputo, Danúbia da Cunha de, Dias Peixoto, Marco Fabrício, Mendonça, Vanessa Amaral, Rapin, Amandine, and Lacerda, Ana Cristina Rodrigues

Subjects

*WHOLE-body vibration, *OXIDATIVE stress, *RANDOMIZED controlled trials, *FIBROMYALGIA, *IRISIN, *ADIPOSE tissue physiology, *BODY composition

Abstract

(1) Background: Mitochondrial dysfunction and redox imbalance seem to be involved in fibromyalgia (FM) pathogenesis. The results of our previous studies suggest that whole-body vibration training (WBVT) would improve redox status markers, increase blood irisin levels, and ameliorate the body composition of women with FM. (2) Objective: The current study aimed to investigate WBVT on oxidative stress markers, plasma irisin levels, and body composition in women with FM. (3) Methods: Forty women with FM were randomized into WBVT or untrained (UN) groups. Before and after 6 weeks of WBVT, body composition was assessed by dual-energy radiological absorptiometry (DXA), and inflammatory marker activities were measured by enzymatic assay. (4) Results: Body composition, blood irisin levels, and oxidative stress markers were similar between UN and WBVT groups before the intervention. After 6 weeks of intervention, the WBVT group presented higher irisin levels (WBVT: 316.98 ± 109.24 mg·dL³, WBVT: 477.61 ± 267.92 mg·dL³, p = 0.01) and lower TBARS levels (UN: 0.39 ± 0.02 nmol MDA/mg protein, WBVT: 0.24 ± 0.06 nmol MDA/mg protein, p = 0.001) and visceral adipose tissue mass (UN: 1.37 ± 0.49 kg, WBVT: 0.69 ± 0.54 kg, p = 0.001) compared to the UN group. (5) Conclusions: Six weeks of WBVT improves blood redox status markers, increases irisin levels, and reduces visceral adipose tissue mass, favoring less cell damage and more outstanding oxidative balance in women with FM. [ABSTRACT FROM AUTHOR]

Published

2023

206. Epiploic Adipose Tissue (EPAT) in Obese Individuals Promotes Colonic Tumorigenesis: A Novel Model for EPAT-Dependent Colorectal Cancer Progression.

Author

Iftikhar, Rida, Snarski, Patricia, King, Angelle N., Ghimire, Jenisha, Ruiz, Emmanuelle, Lau, Frank, and Savkovic, Suzana D.

Subjects

*ADIPOSE tissue physiology, *OBESITY, *COLON tumors, *BIOLOGICAL models, *CARCINOGENESIS, *ANIMAL experimentation, *RESEARCH funding, *CELL lines, *MICE

Abstract

Simple Summary: The role of epiploic adipose tissue (EPAT), understudied fat appendages attached to the colon, in obesity-facilitated colorectal cancer (CRC) is unexamined. In our novel microphysiological system, EPAT obtained from obese individuals, unlike EPAT from lean, attracts colon cancer cells' intrusion and enhances their migration and growth. Conditioned media from this model mediated gene expression in colon cancer cells that are linked to metabolic and tumorigenic remodeling. This EPAT-mediated transcriptional signature defines transcriptomes of human colon cancer. These findings highlight a tumor-promoting role of EPAT, a metabolic tissue, in the colon of obese individuals and establishes a platform for exploration of involved mechanisms and development of effective treatments. The obesity epidemic is associated with increased colorectal cancer (CRC) risk and progression, the mechanisms of which remain unclear. In obese individuals, hypertrophic epiploic adipose tissue (EPAT), attached to the colon, has unique characteristics compared to other fats. We hypothesized that this understudied fat could serve as a tumor-promoting tissue and developed a novel microphysiological system (MPS) for human EPAT-dependent colorectal cancer (CRC-MPS). In CRC-MPS, obese EPAT, unlike lean EPAT, considerably attracted colon cancer HT29-GFP cells and enhanced their growth. Conditioned media (CM) from the obese CRC-MPS significantly increased the growth and migration of HT29 and HCT116 cells (p < 0.001). In HT29 cells, CM stimulated differential gene expression (hOEC867) linked to cancer, tumor morphology, and metabolism similar to those in the colon of high-fat-diet obese mice. The hOEC867 signature represented pathways found in human colon cancer. In unsupervised clustering, hOEC867 separated transcriptomes of colon cancer samples from normal with high significance (PCA, p = 9.6 × 10−11). These genes, validated in CM-treated HT29 cells (p < 0.05), regulate the cell cycle, cancer stem cells, methylation, and metastasis, and are similarly altered in human colon cancer (TCGA). These findings highlight a tumor-promoting role of EPAT in CRC facilitated with obesity and establishes a platform to explore critical mechanisms and develop effective treatments. [ABSTRACT FROM AUTHOR]

Published

2023

207. Role of epicardial fat thickness for prediction of proliferative diabetic retinopathy.

Author

Abide, Sincer, Tuba, Kaygusuz, Yunus, Alkan, Mehmet, Cosgun, Umit, Dogan, Fatih, Ulas, Yilmaz, Gunes, and Sincer, Isa

Subjects

*ADIPOSE tissue physiology, *BIOMARKERS, *STATISTICS, *RESEARCH, *CONFIDENCE intervals, *PERICARDIUM, *CYTOMETRY, *ONE-way analysis of variance, *RISK assessment, *CELL proliferation, *DESCRIPTIVE statistics, *DIABETIC retinopathy, *HIGH density lipoproteins, *INFLAMMATORY mediators, *DATA analysis, *STATISTICAL correlation, *SENSITIVITY & specificity (Statistics), *ODDS ratio, *MONOCYTES, *DISEASE risk factors

Abstract

Purpose: Plenty of factors including inflammation are responsible for development of diabetic retinopathy (DR). Epicardial fat produces adipokines, cytokines and inflammatory products. Monocyte count to high density lipoprotein (HDL) ratio (MHR) has been recently suggested as an inflammatory marker. Methods: Epicardial fat thickness (EFT) and MHR were analyzed in 36 diabetics without DR (NDR), 35 diabetics with proliferative DR (PDR) and 41 diabetics with nonproliferative DR patients (nonPDR). Results: Monocyte counts, HDL, mean MHR and EFT values of NDR, nonPDR and PDR groups were significantly different. One-way analysis of variance test with post hoc Tukey test revealed that the significance of differences in MHR and EFT were dependent on the differences between NDR and PDR (p<0.001 for both) and nonPDR and PDR groups (p<0.001 and p=0.001). The differences between NDR and nonPDR (p=0.81 and p=0.06) were not significant. MHR and EFT were significantly positively correlated with PDR (r=0.453, p<0.001 and r=0.394, p<0.001) and negatively correlated with NDR (r=−0.256, p=0.006 and r= −0.380, p<0.001). Only EFT was found to be independently associated with PDR (p=0.002, 95% CI: OR: 1.643 (1.206–2.237)). An EFT value of >5.90 mm classified the presence of PDR with a sensitivity 74% and specificity of 61% (AUC = 0.750, 95% CI, 0.658–0.843), and a MHR value of >12.8 ratio classified the presence of PDR with a sensitivity of 83% and a specificity of 79% (AUC = 0.811, 95% CI, 0.728–0.893). Conclusion: We suggest that MHR and EFT were significantly increased in proliferative DR, and increased EFT may predict the presence of PDR in type 2 DM. [ABSTRACT FROM AUTHOR]

Published

2023

208. Crosstalk between Adipose Tissue and Hepatic Mitochondria in the Development of the Inflammation and Liver Injury during Ageing in High-Fat Diet Fed Rats.

Author

Cavaliere, Gina, Catapano, Angela, Trinchese, Giovanna, Cimmino, Fabiano, Menale, Ciro, Petrella, Lidia, and Mollica, Maria Pina

Subjects

*ADIPOSE tissue physiology, *ADIPOSE tissues, *HIGH-fat diet, *METABOLIZABLE energy values, *FREE fatty acids, *FATTY acid oxidation, *LIVER injuries

Abstract

Obesity is considered an epidemic disorder, due to an imbalance between energy consumption and metabolizable energy intake. This balance is increasingly disrupted during normal aging processes due to the progressive impairment of mechanisms that normally control energy homeostasis. Obesity is triggered by an excessive lipid depots but reflects systemic inflammation along with large adipocytes secreting proinflammatory adipokines, an increase of the free fatty acids levels in the bloodstream, and ectopic lipid accumulation. Hepatic fat accumulation is the most common cause of chronic liver disease, characterized by mitochondrial dysfunction with a consequent impaired fat metabolism and increased oxidative stress. Therefore, mitochondrial dysfunction is associated to hepatic lipid accumulation and related complications. In this study, we assessed the crosstalk between adipose tissue and liver, analyzing the time-course of changes in hepatic mitochondrial fatty acid oxidation capacity versus fatty acid storage, focusing on the contribution of adipose tissue inflammation to hepatic lipid accumulation, using a rodent model of high fat diet-induced obesity. Our results demonstrate that both high-fat diet-induced obesity and aging induce dysregulation of adipose tissue function and similar metabolic alterations mediated by mitochondrial function impairment and altered inflammatory profile. The high fat diet-induced obesity anticipates and exacerbates liver mitochondrial dysfunction that occurs with aging processes. [ABSTRACT FROM AUTHOR]

Published

2023

209. Hepatic Glucose Metabolism Disorder Induced by Adipose Tissue-Derived miR-548ag via DPP4 Upregulation.

Author

Chu, Xiaolong, Hou, Yanting, Zhang, Xueting, Li, Menghuan, Ma, Dingling, Tang, Yihan, Yuan, Chenggang, Sun, Chaoyue, Liang, Maodi, Liu, Jie, Wei, Qianqian, Chang, Yongsheng, Wang, Cuizhe, and Zhang, Jun

Subjects

*GLUCOSE metabolism disorders, *ABDOMINAL adipose tissue, *TYPE 2 diabetes, *GENE expression, *ADIPOSE tissue physiology, *INSULIN sensitivity, *WEIGHT loss

Abstract

The present study aimed to explore the molecular mechanism underlying the regulation of glucose metabolism by miR-548ag. For the first time, we found that miR-548ag expression was elevated in the abdominal adipose tissue and serum of subjects with obesity and type 2 diabetes mellitus (T2DM). The conditional knockout of adipose tissue Dicer notably reduced the expression and content of miR-548ag in mouse adipose tissue, serum, and liver tissue. The combined use of RNAseq, an miRNA target gene prediction software, and the dual luciferase reporter assay confirmed that miR-548ag exerts a targeted regulatory effect on DNMT3B and DPP4. miR-548ag and DPP4 expression was increased in the adipose tissue, serum, and liver tissue of diet-induced obese mice, while DNMT3B expression was decreased. It was subsequently confirmed both in vitro and in vivo that adipose tissue-derived miR-548ag impaired glucose tolerance and insulin sensitivity by inhibiting DNMT3B and upregulating DPP4. Moreover, miR-548ag inhibitors significantly improved the adverse metabolic phenotype in both obese mice and db/db mice. These results revealed that the expression of the adipose tissue-derived miR-548ag increased in obese subjects, and that this could upregulate the expression of DPP4 by targeting DNMT3B, ultimately leading to glucose metabolism disorder. Therefore, miR-548ag could be utilized as a potential target in the treatment of T2DM. [ABSTRACT FROM AUTHOR]

Published

2023

210. Association Between Different Parameters of Adipose Distribution and Transient Elastography-Assessed Hepatic Steatosis in American Adults with Diabetes, Prediabetes and Normal Glucose Tolerance.

Author

Liu, Yufang, Chai, Sanbao, and Zhang, Xiaomei

Subjects

FATTY liver, GLYCOSYLATED hemoglobin, ADIPOSE tissue physiology, PREDIABETIC state, NON-alcoholic fatty liver disease, HEPATIC fibrosis, DIABETES

Published

2023

211. Assessing welfare risks in unowned unsocialised domestic cats in Denmark based on associations with low body condition score.

Author

Nielsen, Søren Saxmose, Thuesen, Ida Sofie, Mejer, Helena, Agerholm, Jørgen Steen, Nielsen, Stine Thorsø, Jokelainen, Pikka, Thamsborg, Stig Milan, and Sandøe, Peter

Subjects

*CATS, *FELINE immunodeficiency virus, *HERNIA, *DIAPHRAGMATIC hernia, *ADIPOSE tissue physiology, *SPRING

Abstract

Background: Populations of unowned unsocialised cats are present worldwide. Generally, there is concern about their welfare. Low body condition score (BCS) is a potentially relevant indicator that is relatively easy to assess: emaciated cats are likely to have welfare problems while thin cats may be at risk of becoming emaciated. The objective of this study was to assess the association of low BSC with a selection of factors relating to the host, disease, and infection in unowned unsocialised domestic cats. We necropsied 598 euthanised unowned unsocialised cats from Denmark. We recorded each cat's age-group, sex, and neuter status, together with its pregnancy status, the season and location of trapping, as well as gross lesions at necropsy. We also tested for feline immunodeficiency virus and feline leukaemia virus, recorded presence of ectoparasites, and a subsample of the cats were also tested for endoparasites. Cats with no or sparse adipose deposits were categorised as having low BCS, and logistic regression was used to determine the factors associated with low BCS. Results: Of the cats, 11.4% had low BCS. Season, age-group and sex were associated with low BCS and confounded potential associations with other variables. Intact adult males and females in spring and early summer were at highest risk of low BCS. When these factors were taken into account, cats with biting lice had 2.8 (95% confidence interval (CI) 1.4–5.4) times higher odds of low BCS, and cats with gastro-intestinal findings (i.e., enlarged mesenteric lymph nodes, abdominal hernia, diarrhoea, obstructive foreign bodies, or diaphragmatic hernia) had 50 (95% CI 10–417) times higher odds of low BCS, than cats with no such findings. Cats with low BCS were primarily adult intact cats with tooth lesions and skin lesions, ear mite infection, and positive test result for feline immunodeficiency virus. Conclusions: The results highlight associations that can be used to define a risk profile: low BCS, notably in summer-autumn, in an unowned unsocialised cat was associated with underlying, less visible problems. Thus, low BCS can be more than a step towards being emaciated; it can also be an indicator of other underlying welfare problems. [ABSTRACT FROM AUTHOR]

Published

2023

212. Body Composition as a Comorbidity-Independent Predictor of Survival following Nephroureterectomy for Urothelial Cancer of the Upper Urinary Tract.

Author

Pickl, Christoph, Engelmann, Simon, Girtner, Florian, Gužvić, Miodrag, van Rhijn, Bas W. G., Hartmann, Valerie, Holbach, Sonja, Kälble, Sebastian, Haas, Maximilian, Rosenhammer, Bernd, Breyer, Johannes, Burger, Maximilian, and Mayr, Roman

Subjects

*SKELETAL muscle physiology, *ADIPOSE tissue physiology, *BODY composition, *NEPHRECTOMY, *URETHRA surgery, *CONFIDENCE intervals, *SARCOPENIA, *REGRESSION analysis, *URINARY organs, *TRANSITIONAL cell carcinoma, *COMPUTED tomography, *BODY mass index, *LONGITUDINAL method, *PROPORTIONAL hazards models, *OVERALL survival, SURGICAL complication risk factors, BLADDER tumors, URETER tumors

Abstract

Simple Summary: Urothelial carcinoma is a highly aggressive cancer. In addition to the further development and innovation of therapeutic strategies, research into risk and prognostic factors plays a major role. Comparatively little is known about the physical constitution of patients and its impact on the prognosis of the disease. The aim of this retrospective study was to assess specific parameters of the body composition of patients undergoing nephroureterectomy due to urothelial carcinoma of the upper urinary tract, in addition to the usual criteria with regard to commonly used ones. Computed tomography-based measurements were used to determine muscle mass and fat distribution. The cohort included 142 patients. We were able to demonstrate that loss of skeletal muscle mass is a significant comorbidity-independent risk factor. Visceral fat, on the other hand, seems to be protective. In conclusion, specific parameters of body composition can contribute to patient-specific risk stratification. Radical nephroureterectomy (NUE) is the gold standard treatment for high-risk urothelial cancer of the upper urinary tract (UTUC). Besides sarcopenia and frailty, fat distribution is moving increasingly into focus. Components of body composition were assessed in patients undergoing NUE due to UTUC. The study cohort included 142 patients. By using CT-based measurements, the skeletal muscle index (SMI), subcutaneous adipose tissue index (SATI), and visceral adipose tissue index (VATI) were measured at the height of the third lumbar vertebra. Overall survival (OS) and cancer-specific survival (CSS) were estimated using univariable und multivariable Cox regression models. The prevalence of sarcopenia in the study population (n = 142) was 37%. OS and CSS were significantly reduced in sarcopenic patients. In the multivariable cox regression analysis, including age, ACE-27, T-stage, R-stage, LVI and necrosis, sarcopenia remained a significant risk factor of OS (HR, 1.77; 95% CI 1.02–3.07; p = 0.042) and CSS (HR, 2.17; 95% CI 1.18–3.99; p = 0.012). High visceral adipose tissue seems to be protective, although not statistically significant. Sarcopenia is a comorbidity-independent risk factor in patients who underwent NUE due to UTUC. Visceral fat represents a potentially protective factor. These results suggest that specific factors of body composition can be used for better risk stratification. [ABSTRACT FROM AUTHOR]

Published

2023

213. Susceptibility of Fat Tissue to SARS-CoV-2 Infection in Female hACE2 Mouse Model.

Author

Thangavel, Hariprasad, Dhanyalayam, Dhanya, Lizardo, Kezia, Oswal, Neelam, Dolgov, Enriko, Perlin, David S., and Nagajyothi, Jyothi F.

Subjects

*SARS-CoV-2, *ADIPOSE tissue physiology, *LUNGS, *ADIPOSE tissues, *FAT cells, *COVID-19, *LABORATORY mice

Abstract

The coronavirus disease (COVID-19) is a highly contagious viral illness caused by severe acute respiratory syndrome coronavirus-2 (SARS-CoV-2). COVID-19 has had a catastrophic effect globally causing millions of deaths worldwide and causing long-lasting health complications in COVID-19 survivors. Recent studies including ours have highlighted that adipose tissue can act as a reservoir where SARS-CoV-2 can persist and cause long-term health problems. Here, we evaluated the effect of SARS-CoV-2 infection on adipose tissue physiology and the pathogenesis of fat loss in a murine COVID-19 model using humanized angiotensin-converting enzyme 2 (hACE2) mice. Since epidemiological studies reported a higher mortality rate of COVID-19 in males than in females, we examined hACE2 mice of both sexes and performed a comparative analysis. Our study revealed for the first time that: (a) viral loads in adipose tissue and the lungs differ between males and females in hACE2 mice; (b) an inverse relationship exists between the viral loads in the lungs and adipose tissue, and it differs between males and females; and (c) CoV-2 infection alters immune signaling and cell death signaling differently in SARS-CoV-2 infected male and female mice. Overall, our data suggest that adipose tissue and loss of fat cells could play important roles in determining susceptibility to CoV-2 infection in a sex-dependent manner. [ABSTRACT FROM AUTHOR]

Published

2023

214. Ceruloplasmin-Deficient Mice Show Dysregulation of Lipid Metabolism in Liver and Adipose Tissue Reduced by a Protein Replacement.

Author

Raia, Sara, Conti, Antonio, Zanardi, Alan, Ferrini, Barbara, Scotti, Giulia Maria, Gilberti, Enrica, De Palma, Giuseppe, David, Samuel, and Alessio, Massimo

Subjects

*ADIPOSE tissues, *HOMEOSTASIS, *LIPID metabolism, *ADIPOSE tissue physiology, *IRON proteins, *IRON, *LIVER, *CERULOPLASMIN

Abstract

Ceruloplasmin is a ferroxidase that plays a role in iron homeostasis; its deficiency fosters inter alia iron accumulation in the liver, which expresses the soluble form of the protein secreted into the bloodstream. Ceruloplasmin is also secreted by the adipose tissue, but its role in adipocytes has been poorly investigated. We hypothesized that ceruloplasmin might have a role in iron/lipid interplay. We investigated iron/lipid dysmetabolism in the liver and adipose tissue of the ceruloplasmin-deficient mouse (CpKO) model of aceruloplasminemia and evaluated the effectiveness of ceruloplasmin replacement. We found that CpKO mice were overweight, showing adipose tissue accumulation, liver iron deposition and steatosis. In the adipose tissue of CpKO mice, iron homeostasis was not altered. Conversely, the levels of adiponectin and leptin adipokines behaved opposite to the wild-type. Increased macrophage infiltration was observed in adipose tissue and liver of CpKO mice, indicating tissue inflammation. The treatment of CpKO mice with ceruloplasmin limited liver iron accumulation and steatosis without normalizing the expression of iron homeostasis-related proteins. In the CpKO mice, the protein replacement limited macrophage infiltration in both adipose and hepatic tissues reduced the level of serum triglycerides, and partially recovered adipokines levels in the adipose tissue. These results underline the link between iron and lipid dysmetabolism in ceruloplasmin-deficient mice, suggesting that ceruloplasmin in adipose tissue has an anti-inflammatory role rather than a role in iron homeostasis. Furthermore, these data also indicate that ceruloplasmin replacement therapy may be effective at a systemic level. [ABSTRACT FROM AUTHOR]

Published

2023

215. PPARγ Acetylation Orchestrates Adipose Plasticity and Metabolic Rhythms.

Author

He, Ying, B'nai Taub, Alana, Yu, Lexiang, Yao, Yifan, Zhang, Ruotong, Zahr, Tarik, Aaron, Nicole, LeSauter, Joseph, Fan, Lihong, Liu, Longhua, Tazebay, Ruya, Que, Jianwen, Pajvani, Utpal, Wang, Liheng, Silver, Rae, and Qiang, Li

Subjects

*ACETYLATION, *ADIPOSE tissue physiology, *LOW-calorie diet, *DEACETYLATION, *RHYTHM, *CIRCADIAN rhythms, *INSULIN sensitivity

Abstract

Systemic glucose metabolism and insulin activity oscillate in response to diurnal rhythms and nutrient availability with the necessary involvement of adipose tissue to maintain metabolic homeostasis. However, the adipose‐intrinsic regulatory mechanism remains elusive. Here, the dynamics of PPARγ acetylation in adipose tissue are shown to orchestrate metabolic oscillation in daily rhythms. Acetylation of PPARγ displays a diurnal rhythm in young healthy mice, with the peak at zeitgeber time 0 (ZT0) and the trough at ZT18. This rhythmic pattern is deranged in pathological conditions such as obesity, aging, and circadian disruption. The adipocyte‐specific acetylation‐mimetic mutation of PPARγ K293Q (aKQ) restrains adipose plasticity during calorie restriction and diet‐induced obesity, associated with proteolysis of a core circadian component BMAL1. Consistently, the rhythmicity in glucose tolerance and insulin sensitivity is altered in aKQ and the complementary PPARγ deacetylation‐mimetic K268R/K293R (2KR) mouse models. Furthermore, the PPARγ acetylation‐sensitive downstream target adipsin is revealed as a novel diurnal factor that destabilizes BMAL1 and mediates metabolic rhythms. These findings collectively signify that PPARγ acetylation is a hinge connecting adipose plasticity and metabolic rhythms, the two determinants of metabolic health. [ABSTRACT FROM AUTHOR]

Published

2023

216. Synovial Fluid Derived from Human Knee Osteoarthritis Increases the Viability of Human Adipose-Derived Stem Cells through Upregulation of FOSL1.

Author

Kitajima, Hironori, Sakamoto, Takuya, Horie, Tetsuhiro, Kuwano, Ayane, Fuku, Atsushi, Taki, Yasuhiko, Nakamura, Yuka, Tanida, Ikuhiro, Sunami, Hiroshi, Hirata, Hiroaki, Tachi, Yoshiyuki, Yamamoto, Naoki, Iida, Yasuo, Ishigaki, Yasuhito, Yamada, Sohsuke, Shimodaira, Shigetaka, Shimizu, Yusuke, Ichiseki, Toru, Kaneuji, Ayumi, and Osawa, Satoshi

Subjects

*HUMAN stem cells, *SYNOVIAL fluid, *KNEE osteoarthritis, *GENE expression profiling, *KNEE joint, *CANCER stem cells, *ADIPOSE tissue physiology

Abstract

Knee osteoarthritis (Knee OA) is an irreversible condition that causes bone deformity and degeneration of the articular cartilage that comprises the joints, resulting in chronic pain and movement disorders. The administration of cultured adipose-derived stem cells (ADSCs) into the knee joint cavity improves the clinical symptoms of Knee OA; however, the effect of synovial fluid (SF) filling the joint cavity on the injected ADSCs remains unclear. In this study, we investigated the effect of adding SF from Knee OA patients to cultured ADSCs prepared for therapeutic use in an environment that mimics the joint cavity. An increase in the viability of ADSCs was observed following the addition of SF. Gene expression profiling of SF-treated ADSCs using DNA microarrays revealed changes in several genes involved in cell survival. Of these genes, we focused on FOSL1, which is involved in the therapeutic effect of ADSCs and the survival and proliferation of cancer stem cells. We confirmed the upregulation of FOSL1 mRNA and protein expression using RT-PCR and western blot analysis, respectively. Next, we knocked down FOSL1 in ADSCs using siRNA and observed a decrease in cell viability, indicating the involvement of FOSL1 in the survival of ADSCs. Interestingly, in the knockdown cells, ADSC viability was also decreased by SF exposure. These results suggest that SF enhances cell viability by upregulating FOSL1 expression in ADSCs. For therapy using cultured ADSCs, the therapeutic effect of ADSCs may be further enhanced if an environment more conducive to the upregulation of FOSL1 expression in ADSCs can be established. [ABSTRACT FROM AUTHOR]

Published

2023

217. Monocyte Chemoattractant Protein-1-Supplemented Plasma Enhances Adiponectin and Adipogenesis-Related Gene Expression.

Author

Tsay, Tzyy-Bin, Chen, Pei-Hsuan, Li, Merton, Tang, Chia-Hua, and Chen, Lee-Wei

Subjects

*ADIPOGENESIS, *ADIPONECTIN, *GENE expression, *CD26 antigen, *PEROXISOME proliferator-activated receptors, *ADIPOSE tissues, *ADIPOSE tissue physiology, *PLATELET-rich plasma

Abstract

Increasing adipogenesis has been explored to treat metabolic diseases and atherosclerosis through the release of adiponectin. The effects and mechanism of platelet-rich plasma treatment on fat graft survival and adipogenesis have not been clarified. Here, we aimed to study the effects of monocyte chemoattractant protein-1 (MCP-1)-supplemented plasma on adipogenesis-related gene expression and adiponectin levels. Stromal vascular fractions (SVFs) purified from the inguinal adipose tissue of obese and diabetic (Leprdb/db) mice were treated with plasma from control (Lepr+/+) mice supplemented with 10 or 50 ng of MCP-1. The expression of adiponectin and interleukin-33 (IL-33) mRNA in adipose tissue was increased in Leprdb/db mice, whereas control (Lepr+/+) plasma reduced expression of IL-33 mRNA as well as peroxisome proliferator-activated receptor gamma (PPARγ), pJNK, and pNF-κB protein, and increased the expression of IL-10 mRNA in SVFs of Leprdb/db mice. MCP-1-supplemented control plasma increased the expression of adiponectin, CCAAT-enhancer-binding protein α (C/EBPα), dipeptidyl peptidase 4 (DPP4), IL-33, and PDGFα mRNA and the expression of adiponectin protein as well as PPARγ of SVFs and the expression of PPARγ mRNA in adipose tissue macrophages (ATMs). Injection of MCP-1-supplemented plasma into adipose tissue of Leprdb/db mice increased the expression of IL-33 and Col3a1 mRNA in SVFs and IL-33, FABP4, PDGFα, PPARγ and PPARγ2 of ATMs, protein expression of adiponectin and PPARγ of SVFs, and plasma adiponectin levels, as well as DPP4 activity. In conclusion, our results demonstrate that control plasma decreases adipogenesis and increases IL-10, and decreases IL-33, pJNK, and pNF-κB in adipose tissue. MCP-1-supplemented plasma enhances adipogenesis-related gene expression in SVFs and adiponectin levels, which may be mediated through an increase of IL-33 and PPARγ. Thus, our findings suggest that MCP-1-supplemented plasma represents a novel therapy to stimulate local adipogenesis and systemic adiponectin levels. [ABSTRACT FROM AUTHOR]

Published

2023

218. Is Habitual Dietary Intake of Fats Associated with Apelin Gene Expression in Visceral and Subcutaneous Adipose Tissues and Its Serum Levels in Obese Adults?

Author

Zarkesh, Maryam, Safarian, Mohammad, Asghari, Golaleh, Daneshafrooz, Afsoon, Yuzbashian, Emad, Hedayati, Mehdi, Mirmiran, Parvin, and Khalaj, Alireza

Subjects

*ADIPOSE tissues, *APELIN, *DIETARY fats, *FOOD consumption, *ADIPOSE tissue physiology, *GENE expression, *UNSATURATED fatty acids

Abstract

Introduction: Apelin could be one of the last protective defenses before developing obesity-related disorders, including insulin resistance, type 2 diabetes, and hypertension, which can be modified by dietary intake. The present study investigated the association of habitual intake of total fatty acids (TFAs), saturated-, monounsaturated-, polyunsaturated FAs, n-3, and n-6 FAs with Apelin expression in visceral adipose tissue (VAT) and subcutaneous adipose tissue (SAT). Methods: We obtained VAT and SAT from 168 participants (64 nonobese and 104 obese) who had undergone open abdominal surgery. Dietary intake information was gathered with a valid and reliable food frequency questionnaire. The mRNA expression of the Apelin gene was analyzed by realtime PCR. Results: Apelin serum levels were increased in the obese subjects compared to the nonobese group (p = 0.016). The SAT and VAT Apelin mRNA levels were significantly elevated in the obese participants compared to the nonobese ones (p < 0.05). Based on BMI status, only obese subjects indicated a positive association between SAT and VAT Apelin expression and TFA intake (p < 0.001). However, this association was observed between SAT and VAT Apelin gene expression and polyunsaturated fatty acid (PUFA) and n-3 FA intakes in both obese and nonobese groups (p < 0.05). Conclusion: High Apelin gene expression was associated with TFA intake in obese subjects in both fat tissues. However, habitual intake of PUFA and n-3 FA was associated with Apelin gene expression in obese and nonobese individuals. Our results indicate a determinative role of the quality and quantity of FA intake on adipose tissue. [ABSTRACT FROM AUTHOR]

Published

2023

219. Evaluation of supplemental fat sources and pre-farrow essential fatty acid intake on lactating sow performance and essential fatty acid composition of colostrum, milk, and adipose tissue.

Author

Holen, Julia P, Woodworth, Jason C, Tokach, Mike D, Goodband, Robert D, DeRouchey, Joel M, and Gebhardt, Jordan T

Subjects

*ESSENTIAL fatty acids, *ADIPOSE tissues, *ADIPOSE tissue physiology, *ANIMAL litters, *FAT, *COLOSTRUM, *SOY oil, *DIETARY fats

Abstract

A total of 91 sows (Line 241, DNA Genetics) were used to evaluate the effects of supplemental fat sources and essential fatty acid intake on sow farrowing performance, litter growth performance, and essential fatty acid composition of colostrum, milk, and adipose tissue. At approximatelyday 107 of gestation, sows were blocked by body weight and parity, then allotted to 1 of 5 experimental treatments as part of a 2 × 2 + 1 factorial arrangement. Experimental diets were corn-soybean meal-based with a control diet that contained no added fat or diets with 3% added fat as either beef tallow or soybean oil, with consumption of the added fat diets starting on day 107 or 112 of gestation and fed until weaning. Thus, sows were provided low essential fatty acids (EFA; as linoleic and α-linolenic acid) without supplemental fat or with beef tallow or high EFA with soybean oil. Sows were provided approximately 2.8 kg/d of their assigned lactation diet pre-farrow and then provided ad libitum access after parturition. Sows consuming diets with beef tallow had greater lactation ADFI (fat source, P  = 0.030), but lower daily linoleic acid (LA) and α-linolenic acid (ALA) intake than sows that consumed diets with soybean oil (fat source, P  < 0.001). Supplemental fat sources providing either low or high EFA did not influence litter growth performance (fat source, P  > 0.05). Sows fed diets with beef tallow did not influence the LA composition of colostrum; however, lactation diets with high EFA provided by soybean oil on day 107 of gestation increased colostrum LA concentration compared to providing diets on day 112 of gestation (fat source × time, P  = 0.084; time, P  < 0.001). Additionally, regardless of pre-farrow timing, ALA concentration of colostrum increased when sows consumed diets with soybean oil compared to beef tallow (fat source, P  < 0.001). Both LA and ALA concentrations of milk at weaning were greater for sows that consumed diets with soybean oil compared to beef tallow (fat source, P  < 0.001). Furthermore, concentrations of LA and ALA within adipose tissue were greater at weaning when sows consumed diets with high EFA compared to low EFA (fat source, P  < 0.05). These responses suggest that providing dietary fat sources with high concentrations of EFA can increase backfat, colostrum, and milk LA and ALA. However, in this experiment, changes in colostrum and milk composition did not influence litter growth performance. [ABSTRACT FROM AUTHOR]

Published

2023

220. Serpentine Enhances Insulin Regulation of Blood Glucose through Insulin Receptor Signaling Pathway.

Author

Wang, Yinghao, Liu, Guanfu, Liu, Xutao, Chen, Minhua, Zeng, Yuping, Li, Yuyan, Wu, Xiaoyun, Wang, Xuanjun, and Sheng, Jun

Subjects

*BLOOD sugar, *INSULIN receptors, *SERPENTINE, *ANIMAL models of diabetes, *CELLULAR signal transduction, *CELL receptors, *ADIPOSE tissue physiology

Abstract

Insulin sensitizers targeting insulin receptors (IR) are a potential drug for the treatment of diabetes. Serpentine is an alkaloid component in the root of Catharanthus roseus (L.) G. Don. Serpentine screened by surface plasmon resonance (SPR) technology has the ability to target IR. The objective of this study was to investigate whether serpentine could modulate the role of insulin in regulating blood glucose through insulin receptors in cells and in animal models of diabetes. SPR technology was used to detect the affinity of different concentrations of serpentine with insulin receptors. The Western blotting method was used to detect the expression levels of key proteins of the insulin signaling pathway in C2C12 cells and 3T3-L1 cells as well as in muscle and subcutaneous adipose tissue of diabetic mice after serpentine and insulin treatment. Diabetic mice were divided into four groups and simultaneously injected with insulin or serpentine, and the blood glucose concentration and serum levels of insulin, glucagon, and C-peptide were measured 150 min later. mRNA levels of genes related to lipid metabolism and glucose metabolism in liver, muscle, and subcutaneous adipose tissue were detected by RT-PCR. Serpentine was able to bind to the extracellular domain of IR with an affinity of 2.883 × 10−6 M. Serpentine combined with insulin significantly enhanced the ability of insulin to activate the insulin signaling pathway and significantly enhanced the glucose uptake capacity of C2C12 cells. Serpentine enhanced the ability of low-dose insulin (1 nM) and normal-dose insulin (100 nM) to activate the insulin signaling pathway. Serpentine also independently activated AMPK phosphorylation, thus stimulating glucose uptake by C2C12 cells. In high-fat-diet/streptozotocin (HFD/STZ)-induced diabetic mice, serpentine significantly prolonged the hypoglycemic time of insulin, significantly reduced the use of exogenous insulin, and inhibited endogenous insulin secretion. In addition, serpentine alone significantly increased the expression of GSK-3β mRNA in muscle tissue, thus enhancing glucose uptake, and at the same time, serpentine significantly increased glucagon secretion and liver gluconeogenesis. Serpentine enhances the ability of insulin to regulate blood glucose through the insulin receptor, and can also regulate blood glucose alone, but it has a negative regulation mechanism and cannot produce a hypoglycemic effect. Therefore, serpentine may be useful as an insulin sensitizer to assist insulin to lower blood glucose. [ABSTRACT FROM AUTHOR]

Published

2023

221. Current Understanding on the Role of Lipids in Macrophages and Associated Diseases.

Author

Florance, Ida and Ramasubbu, Seenivasan

Subjects

*PERITONEAL macrophages, *CELL physiology, *LIPIDS, *DISEASE complications, *LIPID metabolism, *MEMBRANE lipids, *MACROPHAGES, *ADIPOSE tissue physiology

Abstract

Lipid metabolism is the major intracellular mechanism driving a variety of cellular functions such as energy storage, hormone regulation and cell division. Lipids, being a primary component of the cell membrane, play a pivotal role in the survival of macrophages. Lipids are crucial for a variety of macrophage functions including phagocytosis, energy balance and ageing. However, functions of lipids in macrophages vary based on the site the macrophages are residing at. Lipid-loaded macrophages have recently been emerging as a hallmark for several diseases. This review discusses the significance of lipids in adipose tissue macrophages, tumor-associated macrophages, microglia and peritoneal macrophages. Accumulation of macrophages with impaired lipid metabolism is often characteristically observed in several metabolic disorders. Stress signals differentially regulate lipid metabolism. While conditions such as hypoxia result in accumulation of lipids in macrophages, stress signals such as nutrient deprivation initiate lipolysis and clearance of lipids. Understanding the biology of lipid accumulation in macrophages requires the development of potentially active modulators of lipid metabolism. [ABSTRACT FROM AUTHOR]

Published

2023

222. Salicylate Sodium Suppresses Monocyte Chemoattractant Protein-1 Production by Directly Inhibiting Phosphodiesterase 3B in TNF-α-Stimulated Adipocytes.

Author

Zhang, Xiaoyu, Gao, Yuan, Liu, Zhuangzhuang, Li, Wenjing, Kang, Yuan, Li, Ximeng, Xu, Zhenlu, Peng, Cheng, and Qi, Yun

Subjects

*SODIUM salicylate, *FAT cells, *ADIPOSE tissues, *ADIPOSE tissue physiology, *AMP-activated protein kinases, *THERAPEUTICS

Abstract

As a worldwide health issue, obesity is associated with the infiltration of monocytes/macrophages into the adipose tissue causing unresolved inflammation. Monocyte chemoattractant protein-1 (MCP-1) exerts a crucial effect on obesity-related monocytes/macrophages infiltration. Clinically, aspirin and salsalate are beneficial for the treatment of metabolic diseases in which adipose tissue inflammation plays an essential role. Herein, we investigated the effect and precise mechanism of their active metabolite salicylate on TNF-α-elevated MCP-1 in adipocytes. The results indicated that salicylate sodium (SAS) could lower the level of MCP-1 in TNF-α-stimulated adipocytes, which resulted from a previously unrecognized target phosphodiesterase (PDE), 3B (PDE3B), rather than its known targets IKKβ and AMPK. The SAS directly bound to the PDE3B to inactivate it, thus elevating the intracellular cAMP level and activating PKA. Subsequently, the expression of MKP-1 was increased, which led to the decrease in p-EKR and p-p38. Both PDE3B silencing and the pharmacological inhibition of cAMP/PKA compromised the suppressive effect of SAS on MCP-1. In addition to PDE3B, the PDE3A and PDE4B activity was also inhibited by SAS. Our findings identify a previously unrecognized pathway through which SAS is capable of attenuating the inflammation of adipocytes. [ABSTRACT FROM AUTHOR]

Published

2023

223. Asprosin Exerts Pro-Inflammatory Effects in THP-1 Macrophages Mediated via the Toll-like Receptor 4 (TLR4) Pathway.

Author

Shabir, Kiran, Gharanei, Seley, Orton, Sophie, Patel, Vanlata, Chauhan, Parbata, Karteris, Emmanouil, Randeva, Harpal S., Brown, James E., and Kyrou, Ioannis

Subjects

*ADIPOSE tissue physiology, *TOLL-like receptors, *HOMEOSTASIS, *CAFFEIC acid, *TYPE 2 diabetes, *ADIPOSE tissues, *MACROPHAGES, *CELLULAR signal transduction

Abstract

Adipose tissue is a dynamic endocrine organ, secreting a plethora of adipokines which play a key role in regulating metabolic homeostasis and other physiological processes. An altered adipokine secretion profile from adipose tissue depots has been associated with obesity and related cardio-metabolic diseases. Asprosin is a recently described adipokine that is released in response to fasting and can elicit orexigenic and glucogenic effects. Circulating asprosin levels are elevated in a number of cardio-metabolic diseases, including obesity and type 2 diabetes. In vitro studies have reported pro-inflammatory effects of asprosin in a variety of tissues. The present study aimed to further elucidate the role of asprosin in inflammation by exploring its potential effect(s) in THP-1 macrophages. THP-1 monocytes were differentiated to macrophages by 48 h treatment with dihydroxyvitamin D3. Macrophages were treated with 100 nM recombinant human asprosin, 100 ng/mL lipopolysaccharide (LPS), and 10 μM caffeic acid phenethyl ester (CAPE; an inhibitor of NFκB activation) or 1 µM TAK-242 (a Toll-like receptor 4, TLR4, inhibitor). The expression and secretion of pertinent pro-inflammatory mediators were measured by qPCR, Western blot, ELISA and Bioplex. Asprosin stimulation significantly upregulated the expression and secretion of the pro-inflammatory cytokines: tumour necrosis factor α (TNFα), interleukin-1β (IL-1β), IL-8 and IL-12 in vitro. This pro-inflammatory response in THP-1 macrophages was partly attenuated by the treatments with CAPE and was significantly inhibited by TAK-242 treatment. Asprosin-induced inflammation is significantly counteracted by TLR4 inhibition in THP-1 macrophages, suggesting that asprosin exerts its pro-inflammatory effects, at least in part, via the TLR4 signalling pathway. [ABSTRACT FROM AUTHOR]

Published

2023

224. The role of the novel adipokines vaspin and omentin in chronic inflammatory diseases.

Author

Radzik-Zając, Joanna, Wytrychowski, Krzysztof, Wiśniewski, Andrzej, and Barg, Wojciech

Subjects

WHITE adipose tissue, ADIPOKINES, ADIPOSE tissue physiology, FAT cells, CHRONIC diseases, ADIPOSE tissues, INSULIN sensitivity

Abstract

Copyright of Pediatric Endocrinology, Diabetes & Metabolism is the property of Termedia Publishing House and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2023

225. Partitioning of Persistent Organic Pollutants between Adipose Tissue and Serum in Human Studies.

Author

Moriceau, Meg-Anne, Cano-Sancho, German, Kim, MinJi, Coumoul, Xavier, Emond, Claude, Arrebola, Juan-Pedro, Antignac, Jean-Philippe, Audouze, Karine, and Rousselle, Christophe

Subjects

PERSISTENT pollutants, ADIPOSE tissue physiology, BLOOD lipids, HUMAN experimentation, BODY mass index, ADIPOSE tissues, EPIDEMIOLOGICAL models

Abstract

Blood is the most widely used matrix for biomonitoring of persistent organic pollutants (POPs). It is assumed that POPs are homogenously distributed within body lipids at steady state; however, the variability underlying the partitioning of POPs between fat compartments is poorly understood. Hence, the objective of this study was to review the state of the science about the relationships of POPs between adipose tissue and serum in humans. We conducted a narrative literature review of human observational studies reporting concentrations of POPs in paired samples of adipose tissue with other lipid-based compartments (e.g., serum lipids). The searches were conducted in SCOPUS and PUBMED. A meta-regression was performed to identify factors responsible for variability. All included studies reported high variability in the partition coefficients of POPs, mainly between adipose tissue and serum. The number of halogen atoms was the physicochemical variable most strongly and positively associated with the partition ratios, whereas body mass index was the main biological factor positively and significantly associated. To conclude, although this study provides a better understanding of partitioning of POPs to refine physiologically based pharmacokinetic and epidemiological models, further research is still needed to determine other key factors involved in the partitioning of POPs. [ABSTRACT FROM AUTHOR]

Published

2023

226. Macrophages in Tumor‐Associated Adipose Microenvironment Accelerate Tumor Progression.

Author

Li, Bei, Liu, Siqing, Yang, Qian, Li, Zhiyu, Li, Juanjuan, Wu, Juan, Sun, Shengrong, Xu, Zhiliang, Sun, Si, and Wu, Qi

Subjects

CANCER invasiveness, MACROPHAGES, TUMOR microenvironment, TUMOR growth, FAT cells, EXOSOMES, ANIMAL models in research, ADIPOSE tissue physiology

Abstract

Adipose‐tissue macrophages (ATMs), a complex ensemble of diverse macrophage subtypes, are prevalent in the tumor‐adipose microenvironment (TAME) and facilitate tumor growth. However, the mechanisms in which the tumor‐adipocyte crosstalk may enable the properties and plasticity of macrophages remain unclear. The single‐cell RNA‐sequence profiling reveals that a subset of macrophages expressed CD163, CCL2, and CCL5 in TAME, exhibiting an immunosuppressive subtype. It is demonstrated that CD163+ macrophages aggregate to surround adipocytes in breast cancer tissues. The expressions of CCL2 and CCL5 are also elevated in TAME and enable the recruitment and polarize macrophages. Mechanically, the level of exosomal miRNA‐155 increased in the coculture of tumor cells and adipocytes, and then it promoted the generation and release of CCL2 and CCL5 from adipocytes by targeting the SOCS6/STAT3 pathway. Inhibition of exosomal miRNA‐155 in tumor cells reduced the CCL2 and CCL5 levels in tumor‐adipocytes coculture and further retarded tumor growth. Finally, the deletion of macrophages partially inhibited adipocyte‐induced tumor proliferation. Likewise, inhibiting chemokines and their receptors or suppressing the phosphorylation of STAT3 decreased tumor burden in preclinical models. These results demonstrate that the niche factors in TAME, such as exosomal miRNA‐155, regulate the function and polarity of macrophages to facilitate tumor progression. [ABSTRACT FROM AUTHOR]

Published

2023

227. Dietary Isoleucine and Valine: Effects on Lipid Metabolism and Ureagenesis in Pigs Fed with Protein Restricted Diets.

Author

Goodarzi, Parniyan, Habibi, Mohammad, Gorton, Matthew William, Walsh, Katherine, Tarkesh, Firoozeh, Fuhrig, Mallory, and Pezeshki, Adel

Subjects

LIPID metabolism, FATTY acid synthases, DIETARY proteins, ISOLEUCINE, LIPOLYSIS, VALINE, ADIPOSE tissue physiology

Abstract

A mixture of valine (Val) and isoleucine (Ile) not only decreases the negative impact of very low protein (VLP) diets on the growth of pigs, but also influences the nitrogen (N) balance and lipid metabolism; however, the underlying pathways are not well understood. This study aimed to investigate the effect of dietary Val and Ile on lipogenesis, lipolysis, and ureagenesis under protein restriction. After one week of acclimation, forty three-week-old pigs were randomly assigned to following dietary treatments (n = 8/group) for 5 weeks: positive control (PC): normal protein diet; negative control (NC): VLP diet; HV: NC supplemented with Val; HI: NC supplemented with Ile; and HVI: NC supplemented with both Val and Ile. HVI partially improved the body weight and completely recovered the feed intake (FI) of pigs fed with NC. HVI increased thermal radiation and improved the glucose clearance. HVI had a lower blood triglyceride than PC and blood urea N than NC. NC and HV promoted lipogenesis by increasing the transcript of fatty acid synthase (FAS) in the liver and lipoprotein lipase (LPL) in adipose tissue but reducing hormone-sensitive lipase (HSL) in the liver. HVI reduced the increased rate of lipogenesis induced by the NC group through normalizing the mRNA abundance of hepatic FAS, sterol regulatory element binding transcription factor 1, and HSL and LPL in adipose tissue. NC, HV, HI, and HVI reduced the ureagenesis by decreasing the protein abundance of carbamoyl phosphate synthetase I, ornithine transcarboxylase, and arginosuccinate lyase in the liver. Overall, HVI improved the growth, FI, and glucose clearance, and decreased the rate of lipogenesis induced by VLP diets. [ABSTRACT FROM AUTHOR]

Published

2023

228. Obesity-Induced Brain Neuroinflammatory and Mitochondrial Changes.

Author

Schmitt, Luisa O. and Gaspar, Joana M.

Subjects

METABOLIC disorders, HIGH-fat diet, PATHOLOGICAL physiology, INFLAMMATION, MITOCHONDRIA, ENERGY consumption, ADIPOSE tissue physiology

Abstract

Obesity is defined as abnormal and excessive fat accumulation, and it is a risk factor for developing metabolic and neurodegenerative diseases and cognitive deficits. Obesity is caused by an imbalance in energy homeostasis resulting from increased caloric intake associated with a sedentary lifestyle. However, the entire physiopathology linking obesity with neurodegeneration and cognitive decline has not yet been elucidated. During the progression of obesity, adipose tissue undergoes immune, metabolic, and functional changes that induce chronic low-grade inflammation. It has been proposed that inflammatory processes may participate in both the peripheral disorders and brain disorders associated with obesity, including the development of cognitive deficits. In addition, mitochondrial dysfunction is related to inflammation and oxidative stress, causing cellular oxidative damage. Preclinical and clinical studies of obesity and metabolic disorders have demonstrated mitochondrial brain dysfunction. Since neuronal cells have a high energy demand and mitochondria play an important role in maintaining a constant energy supply, impairments in mitochondrial activity lead to neuronal damage and dysfunction and, consequently, to neurotoxicity. In this review, we highlight the effect of obesity and high-fat diet consumption on brain neuroinflammation and mitochondrial changes as a link between metabolic dysfunction and cognitive decline. [ABSTRACT FROM AUTHOR]

Published

2023

229. Exosomal IL-8 derived from Lung Cancer and Colon Cancer cells induced adipocyte atrophy via NF-κB signaling pathway.

Author

Xiong, Hairong, Ye, Jiaxin, Xie, Kairu, Hu, Wenjun, Xu, Ning, and Yang, Hongmei

Subjects

*COLON cancer, *CANCER cells, *FAT cells, *LUNG cancer, *ADIPOSE tissues, *ADIPOSE tissue physiology, *EXOSOMES

Abstract

Background: Cytokines secreted in the tumor microenvironment function in cancer cachexia (CC), a common clinicopathological syndrome associated with adipocyte wasting and skeletal muscle atrophy. Extracellular vesicles (EVs) secreted by cancer cells actively engage in inter-tissue communication; EVs and enclosed cytokines are largely undefined in CC adipocytes wasting. Methods: EVs derived from Lewis lung carcinoma (LLC) and colorectal cancer C26 cells were extracted and characterized. Conditioned medium and EVs from cancer cells were applied to 3 T3-L1 adipocytes. Recombinant IL-8, IL-8 neutralizing antibody, CXCR2 and NF-κB inhibitor were examined in functional assays. Lipolysis of adipocytes was monitored by Western blots, Oil red O staining and glycerol assays. Furthermore, LLC and C26 cell lines were established as cachexia model to explore the relevance of IL-8 and NF-κB signaling in CC adipose wasting. Adipose tissues were collected for histology analyses. Results: LLC and C26 cell-derived EVs induced lipolysis of 3 T3-L1 adipocytes. Specially, Dil-labeled EVs were effectively taken up by 3 T3-L1 adipocytes, which were motivated by the delivered IL-8 to elicit the NF-κB pathway. In comparison, special IL-8 neutralizing antibody relieved that lipolysis of 3 T3-L1 adipocytes induced by EVs together with conditioned medium of LLC and C26 cells, respectively. Consistently, both CXCR2 and NF-κB inhibitors would lessen the phenotype of lipolysis in 3 T3-L1 adipocytes. In the in vivo settings, both LLC and C26-tumor bearing mice had higher serum IL-8 levels as compared to the control groups. Two typical lipolysis markers, PGC1α and UCP1, were also up-regulated in the adipose tissues of LLC and C26-tumor mice groups, respectively. Conclusions: EVs secreted by LLC and C26 tumor cells would induce adipocyte wasting via extracellular IL-8-mediated NF-κB signaling. Our study pointed out the physiological and therapeutic values of exosomal IL-8 in CC lipolysis. [ABSTRACT FROM AUTHOR]

Published

2022

230. The continuum of disrupted metabolic tempo, mitochondrial substrate congestion, and metabolic gridlock toward the development of non-communicable diseases.

Author

Tippairote, Torsak, Bjørklund, Geir, and Yaovapak, Augchara

Subjects

*NON-communicable diseases, *BLOOD lipids, *BURDEN of care, *DIET therapy, *MITOCHONDRIA, *ADIPOSE tissue physiology

Abstract

Non-communicable diseases (NCD) are the slow-motion disasters with imminent global health care burden. The current dietary management for NCD is dominated by the calorie balance model. Apart from the quantitative balance of calorie, healthy bioenergetics requires temporal eating and fasting rhythms, and the subsequent switching for different metabolic fuels. We herein term these three bioenergetic attributes, i.e., caloric balance, diurnal eating-fasting rhythm, and metabolic flexibility, as the metabolic tempo. These three attributes are intertwined with each other; alteration of one attribute affects one or more other attributes. Lifestyle-induced disrupted metabolic tempo presents a high flux of mixed carbon substrates to mitochondria, with the resulting congestion and indecisiveness of metabolic switches. Such indecisiveness impairs metabolic flexibility, promotes anabolism, and accumulates the energy storage pools. The triggers from hypoxic inducible factor expression could further promote the metabolic gridlock and adipocyte maladaptation. The maladaptive adipocytes lead to ectopic fat deposition, increased circulating lipid levels, insulin resistance, and chronic systemic inflammation. These continuum set stages for clinical NCDs. We propose that the restoration of all tempo attributes through the combined diet-, time-, and calorie-restricted interventions could be the preferred strategy for NCD management. [ABSTRACT FROM AUTHOR]

Published

2022

231. Skipping breakfast regimen induces an increase in body weight and a decrease in muscle weight with a shifted circadian rhythm in peripheral tissues of mice.

Author

Kiriyama, Kohei, Yamamoto, Mizuki, Kim, Daeun, Sun, Shumin, Yamamoto, Hirotaka, and Oda, Hiroaki

Subjects

SKELETAL muscle physiology, LIPID metabolism, OBESITY risk factors, ADIPOSE tissue physiology, METABOLIC syndrome risk factors, LIVER physiology, FOOD habits, BODY weight, ANIMAL experimentation, CIRCADIAN rhythms, SARCOPENIA, GENE expression, DESCRIPTIVE statistics, BREAKFASTS, MICE

Abstract

Meal timing is a key factor in synchronising the circadian clock in peripheral tissues. Circadian disorders are associated with the metabolic syndrome. Previously, we demonstrated that a skipping breakfast regimen (SBR) with a high-fat diet increased body weight gain in rats. In this study, we investigated whether SBR with a normal diet led to abnormal lipid metabolism and muscle metabolism in mice. Male C57BL/6 mice were fed during zeitgeber time (ZT) 12–24 in the control group and ZT 16–24 in the SBR group for 2 weeks. SBR mice showed increased body weight gain and perirenal adipose tissue weight. The plantar muscle weight was decreased in the SBR group compared with that in the control group. Furthermore, SBR delayed the circadian oscillations in clock gene expression in peripheral tissues, such as the liver, adipose tissue and muscle, as well as the oscillations in the expression of lipid metabolism-related genes in the liver and adipose tissue. These results suggest that skipping breakfast over a long period of time is associated with a risk of obesity, the metabolic syndrome and muscle loss, such as sarcopenia. [ABSTRACT FROM AUTHOR]

Published

2022

232. 高强度间歇运动肥胖大鼠鸢尾素、瘦素、脂联素和内脏脂肪的变化.

Author

林家煜, 黄惠斌, 梁 波, and 陈丽君

Subjects

*HIGH-intensity interval training, *ADIPOSE tissues, *HDL cholesterol, *LDL cholesterol, *WHITE adipose tissue, *LEPTIN, *ADIPOSE tissue physiology, *LIPID metabolism

Abstract

BACKGROUND: Exercise induces the secretion of muscle factors, such as irisin, which regulates the browning process of white adipose tissue and may contribute to the treatment of obesity. Exercise-mediated browning effects are related to exercise intensity and high-intensity intermittent exercise is superior to moderate-intensity continuous training in inducing adipose tissue browning. OBJECTIVE: To observe the effects of different exercise interventions on irisin, leptin, adiponectin and visceral fat in obese rats. METHODS: Fifty male SPF Sprague-Dawley rats were divided into normal control group (n=10) and obese model group (n=40). Changes in body mass were recorded for 10 weeks. Thirty rats with higher body mass were selected from the successful modeling rats and randomly divided into three groups (n=10 per group): obese quiet control group, obese moderate-intensity continuous exercise group and obese high-intensity intermittent exercise group. The two exercise groups were subjected to moderate-intensity continuous exercise or high-intensity intermittent exercise. The body mass, visceral fat, blood glucose, blood lipids, blood irisin, leptin and adiponectin levels in the obese rats were measured after different exercise interventions. RESULTS AND CONCLUSION: (1) The body mass of the rats in the obese model group increased significantly compared with that of the normal control group (P < 0.01). The final body mass of the high-intensity intermittent exercise group was significantly lower than that of the moderate-intensity continuous exercise group (P < 0.01). (2) The Lee’s index of the obese quiet control group was significantly higher than that of the normal control group (P < 0.01) and the Lee’s index of the high-intensity intermittent exercise group was significantly lower than that of the obese quiet control group (P < 0.01). However, there was no significant difference between the high-intensity intermittent exercise group and the normal control group (P > 0.05). (3) The fat content of the obese quiet control group was significantly higher than that of the normal control group, moderate-intensity continuous exercise group and high-intensity intermittent exercise group (all P < 0.01). (4) The results of serological analysis showed that fasting blood glucose in the obese quiet control group was significantly higher than that in the normal control group (P < 0.01). During high-fat feeding, the blood glucose level was significantly lower in the moderate-intensity continuous exercise group and high-intensity intermittent exercise group than the obese quiet control group (both P < 0.01). (5) Triglyceride, cholesterol and lowdensity lipoprotein levels in the obese quiet control group were significantly higher than those in the normal control group (all P < 0.01). Compared with the obese quiet control group, the moderate-intensity continuous exercise significantly decreased the levels of triglycerides, cholesterol, low-density lipoprotein cholesterol, and high-density lipoprotein cholesterol (all P < 0.01), while the high-intensity intermittent exercise significantly downregulated the levels of triglycerides and high-density lipoprotein cholesterol (P < 0.05). (6) Serum irisin and adiponectin levels were significantly decreased and leptin level was significantly increased in the obese quiet control group (all P < 0.01), while serum irisin and leptin levels were significantly increased in the moderate-intensity continuous exercise group and high-intensity intermittent exercise group (all P < 0.01). (7) Triglycerides, leptin, and final body mass were positively correlated with total fat mass (r=0.959, 0.842, 0.923, all P < 0.01), and irisin and adiponectin levels were negatively correlated with total fat mass (r=-0.720, -0.669, both P < 0.01). (8) To conclude, high-fat diet could increase body mass and visceral fat, decrease serum irisin and adiponectin levels, and increase leptin level in rats. Exercise training could reduce visceral fat, improve blood glucose and lipid metabolism, regulate leptin and adiponectin levels, and increase serum irisin level in obese rats. Moreover, the high-intensity intermittent exercise has a better effect on fat loss in obese rats. [ABSTRACT FROM AUTHOR]

Published

2022

233. Vaccarin improves insulin sensitivity and glucose uptake in diet-induced obese mice via activation of GPR120-PI3K/AKT/GLUT4 pathway.

Author

Jia, Xiong and Liu, Weishuai

Subjects

*INSULIN sensitivity, *INSULIN, *WHITE adipose tissue, *GLUCOSE, *BLOOD circulation, *TYPE 2 diabetes, *ADIPOSE tissue physiology

Abstract

Insulin resistance is a risk factor for type 2 diabetes and is often associated with obesity. Vaccarin, a flavonoid found in vaccaria seeds, is commonly used in traditional Chinese medicine for activating blood circulation. Here, we showed that vaccarin ameliorates high-fat diet-induced obesity and insulin resistance in mice by reducing fat accumulation and improving insulin sensitivity in white adipose tissue. Further hyperinsulinemic-euglycemic clamp test revealed enhanced glucose uptake in vaccarin-treated WAT and skeletal muscle, consistent with activated insulin signaling pathway in these tissues. Mechanistically, vaccarin activates adipose tissue GPR120 and subsequently activating the PI3K/AKT/GLUT4 signaling pathway in 3T3-L1 cells. Together, these results reveal an undiscovered function of vaccarin in preventing obesity-related insulin resistance and advocates that vaccarin holds promise for further development as an innovative agent for the prevention of metabolic disorders. • Vaccarin ameliorates high-fat diet-induced obesity and insulin resistance in mice. • Hyperinsulinemic-euglycemic clamp test revealed enhanced glucose uptake in vaccarin-treated WAT and skeletal muscle. • Mechanistically, vaccarin activates adipose tissue GPR120 and subsequently activating the PI3K/AKT/GLUT4 signaling pathway in 3T3-L1 cells. [ABSTRACT FROM AUTHOR]

Published

2022

234. Supplementing Diets with Agriophyllum squarrosum Reduced Blood Lipids, Enhanced Immunity and Anti-Inflammatory Capacities, and Mediated Lipid Metabolism in Tan Lambs.

Author

Jiao, Dan, Liang, Yanping, Zhou, Shanshan, Wu, Xiukun, Degen, Abraham Allan, Hickford, Jonathan, Zhou, Huitong, Cong, Haitao, Shi, Xinxin, Ma, Xiaofei, and Yang, Guo

Subjects

*BLOOD lipids, *DIETARY supplements, *LIPID metabolism, *LAMBS, *HDL cholesterol, *FAT cells, *ADIPOSE tissue physiology

Abstract

Simple Summary: Agriophyllum squarrosum (sand rice) is an annual psammophyte that has been used in traditional Chinese medicine for many years. Its medicinal properties have been studied in mice and human, but the nutritional value and metabolic function of the above-ground parts as a ruminant feed ingredient have not been reported. Here, we find that supplementing lamb diets with A. squarrosum reduced blood lipids, enhanced immunity and anti-inflammatory capacities, and mediated lipid metabolism in adipose tissue and adipocytes of Tan lambs. These findings have provided strong evidence that A. squarrosum has the potential to be used as a beneficial dietary supplement for ruminants. Agriophyllum squarrosum (sand rice), a widespread desert plant, possesses anti-hyperglycemic and anti-inflammatory properties, and has been used in traditional Chinese medicine for many years. However, its effects on ruminants are unknown. To fill this gap, we examined the effects of A. squarrosum on the immune and anti-inflammatory responses of lambs. A total of 23, 6-month-old Tan ewe-lambs (27.6 ± 0.47 kg) were divided into four groups and offered a basic diet (C—control), or a diet that contained 10%, 20%, or 30% A. squarrosum, on a dry matter basis, for 128 days. Serum concentrations of total cholesterol were lower (p = 0.004) in the 30% supplemented lambs than controls, while concentrations of high-density lipoprotein cholesterol were lower (p = 0.006) in the 10% and 20%, but not in 30% supplemented lambs than controls. Serum-cortisol concentrations were lower (p = 0.012) in the 30% supplemented lambs and free fatty acid concentrations were higher in the 10% and 20% supplemented lambs than in control lambs (p < 0.001). Supplementation with A. squarrosum decreased (p < 0.05) the area of adipocytes in subcutaneous adipose tissue, but there was no difference between the 20% and 30% diets. Conversely, the area in visceral adipose tissue (VAT) increased (p < 0.05), especially for the 10% and 20% supplemented diets. Supplementation with A. squarrosum also enriched immune and anti-inflammatory related and lipid and glucose-metabolic pathways and associated differentially expressed gene expressions in adipose tissue. A total of 10 differential triacylglycerol, 34 differential phosphatidylcholines and seven differential phosphatidylethanolamines decreased in the diet with 30% supplementation, when compared to the other diets. Finally, adipocyte-differentiation genes, and immune and inflammatory response-related gene expression levels decreased in lamb adipocytes cultured with an aqueous A. squarrosum extract. In conclusion, supplementing lamb diets with A. squarrosum reduced blood lipids, enhanced immunity and anti-inflammatory capacities, and mediated lipid metabolism in adipose tissue and adipocytes of Tan lambs. A level of approximately 10% is recommended, but further research is required to determine the precise optimal level. [ABSTRACT FROM AUTHOR]

Published

2022

235. Ketogenic Diet Increases Serum and White Adipose Tissue SIRT1 Expression in Mice.

Author

Tozzi, Rossella, Campolo, Federica, Baldini, Enke, Venneri, Mary Anna, Lubrano, Carla, Ulisse, Salvatore, Gnessi, Lucio, and Mariani, Stefania

Subjects

*ADIPOSE tissues, *WHITE adipose tissue, *SIRTUINS, *KETOGENIC diet, *ADIPOSE tissue physiology, *HOMEOSTASIS, *LABORATORY mice

Abstract

Overnutrition and its sequelae have become a global concern due to the increasing incidence of obesity and insulin resistance. A ketogenic diet (KD) is widely used as a dietary treatment for metabolic disorders. Sirtuin1 (SIRT1), a metabolic sensor which regulates fat homeostasis, is modulated by dietary interventions. However, the influence of nutritional ketosis on SIRT1 is still debated. We examined the effect of KD on adipose tissue, liver, and serum levels of SIRT1 in mice. Adult C57BL/6J male mice were randomly assigned to two isocaloric dietary groups and fed with either high-fat KD or normal chow (NC) for 4 weeks. Serum SIRT1, beta-hydroxybutyrate (βHB), glucose, and triglyceride levels, as well as SIRT1 expression in visceral (VAT), subcutaneous (SAT), and brown (BAT) adipose tissues, and in the liver, were measured. KD-fed mice showed an increase in serum βHB in parallel with serum SIRT1 (r = 0.732, p = 0.0156), and increased SIRT1 protein expression in SAT and VAT. SIRT1 levels remained unchanged in BAT and in the liver, which developed steatosis. Normal glycemia and triglycerides were observed. Under a KD, serum and white fat phenotypes show higher SIRT1, suggesting that one of the molecular mechanisms underlying a KD's potential benefits on metabolic health involves a synergistic interaction with SIRT1. [ABSTRACT FROM AUTHOR]

Published

2022

236. Role of Adiponectin in Cardiovascular Diseases Related to Glucose and Lipid Metabolism Disorders.

Author

Han, Wen, Yang, Shuxian, Xiao, Haiyan, Wang, Min, Ye, Jingxue, Cao, Li, and Sun, Guibo

Subjects

*LIPID metabolism disorders, *GLUCOSE metabolism disorders, *CARDIOVASCULAR diseases, *CARDIAC hypertrophy, *CELL physiology, *ADIPOSE tissue physiology

Abstract

Lifestyle changes have led to increased incidence of cardiovascular disease (CVD); therefore, potential targets against CVD should be explored to mitigate its risks. Adiponectin (APN), an adipokine secreted by adipose tissue, has numerous beneficial effects against CVD related to glucose and lipid metabolism disorders, including regulation of glucose and lipid metabolism, increasing insulin sensitivity, reduction of oxidative stress and inflammation, protection of myocardial cells, and improvement in endothelial cell function. These effects demonstrate the anti-atherosclerotic and antihypertensive properties of APN, which could aid in improving myocardial hypertrophy, and reducing myocardial ischemia/reperfusion (MI/R) injury and myocardial infarction. APN can also be used for diagnosing and predicting heart failure. This review summarizes and discusses the role of APN in the treatment of CVD related to glucose and lipid metabolism disorders, and explores future APN research directions and clinical application prospects. Future studies should elucidate the signaling pathway network of APN cardiovascular protective effects, which will facilitate clinical trials targeting APN for CVD treatment in a clinical setting. [ABSTRACT FROM AUTHOR]

Published

2022

237. Elucidating type 2 diabetes mellitus risk factor by promoting lipid metabolism with gymnemagenin: An in vitro and in silico approach.

Author

DasNand1y, Anusree, Patil, Vishal S., Hegde, Harsha V., Harish, Darasaguppe R., and Roy, Subarna

Subjects

TYPE 2 diabetes, LIPID metabolism, ADIPOKINES, ADIPOSE tissue physiology, LIPOLYSIS, FAT cells, GENE expression, MOLECULAR dynamics, CARRIER proteins

Abstract

Introduction: Adipose tissue functions as a key endocrine organ which releases multiple bioactive substances and regulate obesity-linked complications. Dysregulation of adipocyte differentiation, triglyceride metabolism, adipokines production and lipid transport contributes to impaired lipid metabolism resulting in obesity, insulin resistance and type 2 diabetes. Gymnema sylvestre plant is frequently used in Ayurveda for treatment of diabetes and obesity. Gymnemagenin is a major bioactive compound of Gymnema sylvestre. The present study was undertaken to elucidate the role of gymnemagenin in lipid metabolism by in vitro and computational approaches. Methods: A panel of twelve genes viz., Fasn, Lipe, Lpl, Pparg, Plin2, Cidea, Scd1, Adipoq, Lep, Ccl2, Fabp4, and Slc2a4, essential in lipid metabolism were selected and gene expression pattern and triglyceride content were checked in adipocytes (3T3L1 cells) with/without treatment of gymnemagenin by Real time PCR and colorimetric estimation, respectively. Mode of action of gymnemagenin on Pparg and Fabp4 was accomplished by computational studies. Gene set enrichment and network pharmacology were performed by STRING and Cytoscape. Molecular docking was performed by AutoDock vina by POAP pipeline. Molecular dynamics, MM-PBSA were done by Gromacs tool. Results: In vitro study showed that gymnemagenin improved triglyceride metabolism by up regulating the expression of lipase genes viz., Lipe and Lpl which hydrolyse triglyceride. Gymnemagenin also up regulated the expression of anti-inflammatory gene Adipoq. Importantly, gymnemagenin treatment up regulated the expression of Pparg gene and the downstream target genes (Plin2, Cidea, and Scd1) which are associated with adipogenesis. However, gymnemagenin has no effect on expression of Fabp4, codes for a lipid transport protein. In silico study revealed that gymnemagenin targeted 12 genes were modulating 6 molecular pathways involved in diabetes and obesity. Molecular docking and dynamics revealed that gymnemagenin stably bind to active site residue of Pparg and failed to bind to Fabp4 active site compared to its standard molecules throughout 100 ns MD production run. Gymnemagenin scored binding free energy of −177.94 and −25.406 kJ/mol with Pparg and Fabp4, respectively. Conclusion: Gymnemagenin improved lipid metabolism by increasing triglyceride hydrolysis (lipolysis), up regulating the crucial gene of adipogenesis and increasing the expression of anti-inflammatory adipokine proving its therapeutic importance as anti-obesity and anti-diabetic phytocompound. [ABSTRACT FROM AUTHOR]

Published

2022

238. Field‐based adipose tissue quantification in sea turtles using bioelectrical impedance spectroscopy validated with CT scans and deep learning.

Author

Kophamel, Sara, Ward, Leigh C., Konovalov, Dmitry A., Mendez, Diana, Ariel, Ellen, Cassidy, Nathan, Bell, Ian, Balastegui Martínez, María T., and Munns, Suzanne L.

Subjects

*BIOELECTRIC impedance, *SEA turtles, *BODY composition, *IMPEDANCE spectroscopy, *ADIPOSE tissue physiology, *DEEP learning, *COMPUTED tomography

Abstract

Loss of adipose tissue in vertebrate wildlife species is indicative of decreased nutritional and health status and is linked to environmental stress and diseases. Body condition indices (BCI) are commonly used in ecological studies to estimate adipose tissue mass across wildlife populations. However, these indices have poor predictive power, which poses the need for quantitative methods for improved population assessments. Here, we calibrate bioelectrical impedance spectroscopy (BIS) as an alternative approach for assessing the nutritional status of vertebrate wildlife in ecological studies. BIS is a portable technology that can estimate body composition from measurements of body impedance and is widely used in humans. BIS is a predictive technique that requires calibration using a reference body composition method. Using sea turtles as model organisms, we propose a calibration protocol using computed tomography (CT) scans, with the prediction equation being: adipose tissue mass (kg) = body mass − (−0.03 [intercept] − 0.29 * length2/resistance at 50 kHz + 1.07 * body mass − 0.11 * time after capture). CT imaging allows for the quantification of body fat. However, processing the images manually is prohibitive due to the extensive time requirement. Using a form of artificial intelligence (AI), we trained a computer model to identify and quantify nonadipose tissue from the CT images, and adipose tissue was determined by the difference in body mass. This process enabled estimating adipose tissue mass from bioelectrical impedance measurements. The predictive performance of the model was built on 2/3 samples and tested against 1/3 samples. Prediction of adipose tissue percentage had greater accuracy when including impedance parameters (mean bias = 0.11%–0.61%) as predictor variables, compared with using body mass alone (mean bias = 6.35%). Our standardized BIS protocol improves on conventional body composition assessment methods (e.g., BCI) by quantifying adipose tissue mass. The protocol can be applied to other species for the validation of BIS and to provide robust information on the nutritional and health status of wildlife, which, in turn, can be used to inform conservation decisions at the management level. [ABSTRACT FROM AUTHOR]

Published

2022

239. An organoid model derived from human adipose stem/progenitor cells to study adipose tissue physiology.

Author

Mandl, Markus, Viertler, Hans P., Hatzmann, Florian M., Brucker, Camille, Großmann, Sonja, Waldegger, Petra, Rauchenwald, Tina, Mattesich, Monika, Zwierzina, Marit, Pierer, Gerhard, and Zwerschke, Werner

Subjects

*ADIPOSE tissue physiology, *PROGENITOR cells, *FAT cells, *WHITE adipose tissue, *FATTY acid-binding proteins

Abstract

We established a functional adipose organoid model system for human adipose stem/progenitor cells (ASCs) isolated from white adipose tissue (WAT). ASCs were forced to self-aggregate by a hanging-drop technique. Afterwards, spheroids were transferred into agar-coated cell culture dishes to avoid plastic-adherence and dis-aggregation. Adipocyte differentiation was induced by an adipogenic hormone cocktail. Morphometric analysis revealed a significant increase in organoid size in the course of adipogenesis until d 18. Whole mount staining of organoids using specific lipophilic dyes showed large multi- and unilocular fat deposits in differentiated cells indicating highly efficient differentiation of ASCs into mature adipocytes. Moreover, we found a strong induction of the expression of key adipogenesis and adipocyte markers (CCAAT/enhancer-binding protein (C/EBP) β, peroxisome proliferator-activated receptor (PPAR) γ, fatty acid-binding protein 4 (FABP4), adiponectin) during adipose organoid formation. Secreted adiponectin was detected in the cell culture supernatant, underscoring the physiological relevance of mature adipocytes in the organoid model. Moreover, colony formation assays of collagenase-digested organoids revealed the maintenance of a significant fraction of ASCs within newly formed organoids. In conclusion, we provide a reliable and highly efficient WAT organoid model, which enables accurate analysis of cellular and molecular markers of adipogenic differentiation and adipocyte physiology. [ABSTRACT FROM AUTHOR]

Published

2022

240. Connecting epicardial adipose tissue and heart failure with preserved ejection fraction: mechanisms, management and modern perspectives.

Author

van Woerden, Gijs, van Veldhuisen, Dirk J., Westenbrink, B. Daan, de Boer, Rudolf A., Rienstra, Michiel, and Gorter, Thomas M.

Subjects

*ADIPOSE tissues, *ADIPOSE tissue physiology, *HEART failure, *VENTRICULAR ejection fraction, *BODY mass index

Abstract

Obesity is very common in patients with heart failure with preserved ejection fraction (HFpEF) and it has been suggested that obesity plays an important role in the pathophysiology of this disease. While body mass index defines the presence of obesity, this measure provides limited information on visceral adiposity, which is probably more relevant in the pathophysiology of HFpEF. Epicardial adipose tissue is the visceral fat situated directly adjacent to the heart and recent data demonstrate that accumulation of epicardial adipose tissue is associated with the onset, symptomatology and outcome of HFpEF. However, the mechanisms by which epicardial adipose tissue may be involved in HFpEF remain unclear. It is also questioned whether epicardial adipose tissue may be a specific target for therapy for this disease. In the present review, we describe the physiology of epicardial adipose tissue and the pathophysiological transformation of epicardial adipose tissue in response to chronic inflammatory diseases, and we postulate conceptual mechanisms on how epicardial adipose tissue may be involved in HFpEF pathophysiology. Lastly, we outline potential treatment strategies, knowledge gaps and directions for further research. [ABSTRACT FROM AUTHOR]

Published

2022

241. A modest change in housing temperature alters whole body energy expenditure and adipocyte thermogenic capacity in mice.

Author

Sadler, Daniel G., Treas, Lillie, Sikes, James D., and Porter, Craig

Subjects

*WHITE adipose tissue, *BROWN adipose tissue, *BODY temperature, *FAT cells, *ADIPOSE tissues, *ADIPOSE tissue physiology, *LABORATORY mice, *SEXUAL dimorphism

Abstract

Typical vivarium temperatures (20-26°C) induce facultative thermogenesis in mice, a process attributable in part to uncoupling protein-1 (UCP1). The impact of modest changes in housing temperature on whole body and adipose tissue energetics in mice remains unclear. Here, we determined the effects of transitioning mice from 24°C to 30° C on total energy expenditure and adipose tissue protein signatures. C57BL/6J mice were housed at 24°C for 2 wk and then either remained at 2°C (n = 16/group, 8M/8F) or were transitioned to 30°C (n = 16/group, 8M/8F) for 4 wk. Total energy expenditure and its components were determined by indirect calorimetry. Interscapular brown adipose tissue (iBAT) and inguinal white adipose tissue (iWAT) proteins were quantified by Western blot and quantitative proteomics. Transitioning from 24°C to 30°C reduced total energy expenditure in both male (-25%) and female (-16%) mice, which was attributable to lower basal energy expenditure in males (-36%) and females (-40%). Total iBAT UCP1 protein content was 50% lower at 30°C compared with 24°C, whereas iWAT UCP1 protein content was similar between conditions. iBAT UCP1 protein content remained 20-fold greater than iWAT at 30°C. In iBAT and iWAT, 183 and 41 proteins were differentially expressed between 24°C and 30°C, respectively. iWAT proteins (257) differentially expressed between sexes at 30°C were not differentially expressed at 24°C. Thus, 30°C housing lowers total energy expenditure of mice when compared with an ambient temperature (24°C) that falls within the National Research Council's guidelines for housing laboratory mice. Lower iBAT UCP1 content accompanied chronic housing at 30°C. Furthermore, housing temperature influences sexual dimorphism in the iWAT proteome. These data have implications regarding the optimization of preclinical models of human disease. [ABSTRACT FROM AUTHOR]

Published

2022

242. Heat stress exposure changed liver lipid metabolism and abdominal fat deposition in broilers.

Author

Lan, Ruixia, Wang, Yuchen, Wei, Linlin, Wu, Fan, and Yin, Fuquan

Subjects

*LIPID metabolism, *PHYSIOLOGICAL effects of heat, *FATTY acid synthases, *ABDOMINAL adipose tissue, *ADIPOSE tissue physiology, *LIVER, *HEAT shock proteins, *GENE expression

Abstract

To evaluate the effects of heat stress on lipid metabolism in the liver and abdominal adipose deposition in broilers, totally, 120 female 21-day old broilers were selected and randomly allocated to 2 groups with 6 replication and 10 broilers per each replication. Broilers in the control group (CON) were reared at 24 °C, and broilers in the heat stress group (HS) were reared at 34 °C. Heat stress exposure increased (P < 0.05) rectal temperature, relative weight of abdominal adipose and liver, serum triacylglycerol (TG) and total cholesterol (TC) level, liver TG, TC, and very low-density lipoprotein (VLDL) content. Hepatic mRNA expression level of fatty acid synthase (FAS), acetyl-coenzyme A carboxylase (ACC), and abdominal adipose mRNA expression level of ACC and CCAAT/enhancer-binding protein-α (C/EBPα) were up-regulated (P < 0.05) when compared with the CON group. Heat stress exposure increased serum and hepatic TC and TG content, up-regulated the mRNA expression of FAS and ACC in liver, and promoted preadipocytes differentiation by increasing C/EBPα mRNA expression in abdominal adipose. Therefore, heat stress exposure increased abdominal adipose deposition, which related to increase in hepatic de novo lipogenesis, and promoted preadipocytes differentiation in abdominal adipose. Heat stress increased abdominal adipose deposition Heat stress increased hepatic de novo lipogenesis Heat stress promoted preadipocytes differentiation in abdominal adipose [ABSTRACT FROM AUTHOR]

Published

2022

243. Exogenous butyrate regulates lipid metabolism through GPR41-ERK-AMPK pathway in rabbits.

Author

Zhang, Bin, Liu, Hongli, Liu, Mengqi, Yue, Zhengkai, Liu, Lei, and Fuchang, Li

Subjects

*LIPID metabolism, *FATTY acid-binding proteins, *CARNITINE palmitoyltransferase, *FATTY acid synthases, *LIPOLYSIS, *ADIPOSE tissue physiology, *BUTYRATES

Abstract

Diets containing higher levels of fat can lead to obesity, which is potentially harmful to health. Endogenous butyric acid is produced by intestinal microbial fermentation and participates in lipid metabolism. However, there is less butyric acid produced in the body, butyric acid has a shorter half-life in the blood. We used intraperitoneal injection of sodium butyrate to study the mechanism of butyrate involved in body lipid metabolism. Triglycerides in adipose tissue and liver were significantly reduced by butyrate. The content of triglyceride in plasma in butyrate group was also significantly decreased. In adipose tissue, butyrate up-regulated gene expression of hormone-sensitive lipase (HSL), carnitine palmitoyl transferase (CPT)1 and CPT2, and increased protein expression of G protein-coupled receptor (GPR)41, phosphorylated extracellular-signal-regulated kinase (P-ERK), adenosine 5'-monophosphate (AMP)-activated protein kinase (AMPK) and P-AMPK. Gene expression of lipoprotein lipase (LPL), differentiation-dependent factor 1 (ADD1) and fatty acid synthase (FAS) was down-regulated. In liver, butyrate up-regulated protein expression of GPR41, ERK, P-ERK, P-AMPK. Gene expression of ADD1 and FAS was down-regulated. In muscle tissue, butyrate significantly up-regulated the expression of gene LPL, fatty acid transport protein (FATP) and fatty acid-binding protein (FABP) and protein GPR41, GPR43. Thus, butyrate is involved in body lipid metabolism mainly through the GPR41-mediated ERK-AMPK pathway. Inhibits lipid synthesis in adipose tissue and the liver and promotes lipolysis, avoiding obesity caused by diets with higher fat content. Butyrate affects lipid metabolism in the body by affecting lipid synthesis/decomposition in adipose tissue and liver. Butyrate mainly through GPR41-mediated ERK-AMPK pathway, inhibit lipid synthesis, promote lipid decomposition, and avoid a large amount of fat accumulation induced by higher-fat diet. [ABSTRACT FROM AUTHOR]

Published

2022

244. Self-reported dietary omega-3 polyunsaturated fatty acids are associated with adipose tissue markers and glucose metabolism in apparently healthy subjects.

Author

Reyes-Barrera, Juan, Medina-Urrutia, Aida X., Osorio-Alonso, Horacio, Jorge-Galarza, Esteban, Olvera-Mayorga, Gabriela, Sánchez-Ortiz, Néstor A., Arellano-Buendía, Abraham S., Márquez-García, José E., Santibáñez-Escobar, Felipe, Pérez-Rodríguez, Elizabeth, Torres-Tamayo, Margarita, Granados-Portillo, Omar, Torre-Villalvazo, Ivan, and Juárez-Rojas, Juan G.

Subjects

*UNSATURATED fatty acids, *OMEGA-3 fatty acids, *GLUCOSE metabolism, *ADIPOSE tissues, *PLASMINOGEN activator inhibitors, *ADIPOSE tissue physiology, *BODY mass index

Abstract

Plasminogen activator inhibitor 1 (PAI-1) and resistin are associated with dysfunctional adipose tissue (AT)-related metabolic complications. The role of dietary eicosapentaenoic (EPA) and docosahexaenoic (DHA) fatty acids in this relationship is unknown. To investigate the association of EPA and DHA with PAI-1 and resistin, as well as the role of this association on the glucose metabolism of apparently healthy subjects. Thirty-six healthy individuals were included. Validated food frequency questionnaires were used to analyse dietary habits. Inflammatory and glucose metabolism markers were quantified. Subcutaneous AT samples were obtained, and adipocyte number, area, and macrophage content were assessed. In 36 subjects aged 56 ± 8 years and with a body mass index of 26 ± 4 kg/m2, logEPA, and logDHA showed significant association with logresistin and a marginal association with PAI-1. Adipocyte number, area, and lognumber of macrophages per adipocyte significantly correlated with PAI-1 but not with logresistin. Although logEPA and logDHA were independently associated with loginsulin, loginsulin resistance, and C-Peptide, the addition of logresistin, but not of PAI-1, into the multivariable model, abolished the associations. EPA and DHA could modulate glucose metabolism across AT functional states. Our data indicate that this association is independent of other metabolic risk factors. [ABSTRACT FROM AUTHOR]

Published

2022

245. Nutrition Education to Reduce Metabolic Dysfunction for Spinal Cord Injury: A Module-Based Nutrition Education Guide for Healthcare Providers and Consumers.

Author

Sneij, Alicia, Farkas, Gary J., Carino Mason, Marisa Renee, and Gater, David R.

Subjects

*MEDICAL personnel, *METABOLIC disorders, *NUTRITION education, *SPINAL cord injuries, *CONSUMERS, *ADIPOSE tissue physiology, *NUTRITION

Abstract

Spinal cord injury (SCI) results in a high prevalence of neurogenic obesity and metabolic dysfunction. The increased risk for neurogenic obesity and metabolic dysfunction is mainly due to the loss of energy balance because of significantly reduced energy expenditure following SCI. Consequently, excessive energy intake (positive energy balance) leads to adipose tissue accumulation at a rapid rate, resulting in neurogenic obesity, systemic inflammation, and metabolic dysfunction. The purpose of this article is to review the existing literature on nutrition, dietary intake, and nutrition education in persons with SCI as it relates to metabolic dysfunction. The review will highlight the poor dietary intakes of persons with SCI according to authoritative guidelines and the need for nutrition education for health care professionals and consumers. Nutrition education topics are presented in a module-based format with supporting literature. The authors emphasize the role of a diet consisting of low-energy, nutrient-dense, anti-inflammatory foods consistent with the Dietary Guidelines for Americans' MyPlate to effectively achieve energy balance and reduce the risk for neurogenic obesity and metabolic dysfunction in individuals with SCI. [ABSTRACT FROM AUTHOR]

Published

2022

246. ATL I, Acts as a SIRT6 Activator to Alleviate Hepatic Steatosis in Mice via Suppression of NLRP3 Inflammasome Formation.

Author

Kong, Danli, Mai, Zhenhua, Chen, Yongze, Luo, Ling, Liu, Hao, Zhao, Le, Huang, Ruixian, Wang, Shuang, Chen, Rong, Zhou, Hao, Chen, Hao, Zhang, Jingjing, Yu, Haibing, and Ding, Yuanlin

Subjects

*FATTY liver, *NLRP3 protein, *INFLAMMASOMES, *TUMOR necrosis factors, *PEROXISOME proliferator-activated receptors, *ADIPOSE tissue physiology, *SIRTUINS

Abstract

Accumulating evidence has highlighted that sirtuin-6 (SIRT6) plays an important role in hepatic gluconeogenesis and lipogenesis. We aim to investigate the underlying mechanisms and pharmacological interventions of SIRT6 on hepatic steatosis treatment. Herein, our results showed that atractylenolide I (ATL I) activated the deacetylase activity of SIRT6 to promote peroxisome proliferator-activated receptor alpha (PPARα) transcription and translation, while suppressing nuclear factor NF-kappa-B (NFκB)-induced NACHT, LRR, and PYD domains containing protein 3 (NLRP3) inflammasome formation. Together, these decreased the infiltration of F4/80 and CD11B positive macrophages, accompanied by decreased mRNA expression and serum levels of tumor necrosis factor alpha (TNF-α), interleukin-6 (IL6), and interleukin-1 beta (IL1β). Additionally, these changes decreased sterol regulatory element-binding protein-1c (SREBP-1c) expression, while restoring carnitine O-palmitoyltransferase 1a (Cpt1a) expression, to decrease the size of adipocytes and adipose deposition, which, in turn, reversed high-fat diet (HFD)-induced liver weight and body weight accumulation in C57 mice. SIRT6 knockout or hepatic SIRT6 knockout in C57 mice largely abolished the effect of ATL I on ameliorating hepatic steatosis. Taken together, our results suggest that ATL I acts as a promising compound that activates SIRT6/PPARα signaling and attenuates the NLRP3 inflammasome to ameliorate hepatic inflammation and steatosis. [ABSTRACT FROM AUTHOR]

Published

2022

247. Mangiferin Ameliorates Obesity-Associated Inflammation and Autophagy in High-Fat-Diet-Fed Mice: In Silico and In Vivo Approaches.

Author

Noh, Ji-Won, Lee, Han-Young, and Lee, Byung-Cheol

Subjects

*AUTOPHAGY, *MANGIFERIN, *KUPFFER cells, *METABOLIC disorders, *ADIPOSE tissue physiology, *LIPID metabolism, *WEIGHT loss, *FIBROBLAST growth factors

Abstract

Obesity-induced insulin resistance is the fundamental cause of metabolic syndrome. Accordingly, we evaluated the effect of mangiferin (MGF) on obesity and glucose metabolism focusing on inflammatory response and autophagy. First, an in silico study was conducted to analyze the mechanism of MGF in insulin resistance. Second, an in vivo experiment was conducted by administering MGF to C57BL/6 mice with high-fat-diet (HFD)-induced metabolic disorders. The in silico analysis revealed that MGF showed a high binding affinity with macrophage-related inflammatory cytokines and autophagy proteins. In the in vivo study, mice were divided into three groups: normal chow, HFD, and HFD + MGF 150 mg/kg. MGF administration to obese mice significantly improved the body weight, insulin-sensitive organs weights, glucose and lipid metabolism, fat accumulation in the liver, and adipocyte size compared to HFD alone. MGF significantly reduced the macrophages in adipose tissue and Kupffer cells, inhibited the gene expression ratio of tumor necrosis factor-α and F4/80 in adipose tissue, reduced the necrosis factor kappa B gene, and elevated autophagy-related gene 7 and fibroblast growth factor 21 gene expressions in the liver. Thus, MGF exerted a therapeutic effect on metabolic diseases by improving glucose and lipid metabolism through inhibition of the macrophage-mediated inflammatory responses and activation of autophagy. [ABSTRACT FROM AUTHOR]

Published

2022

248. Increased Number of Mucosal-Associated Invariant T Cells Is Associated with the Inhibition of Nonalcoholic Fatty Liver Disease in High Fat Diet–Fed Mice.

Author

Kishi, Haruka, Usui, Isao, Jojima, Teruo, Fujisaka, Shiho, Wakamatsu, Sho, Mizunuma-Inoue, Yuiko, Niitani, Takafumi, Sakurai, Shintaro, Iijima, Toshie, Tomaru, Takuya, Tobe, Kazuyuki, and Aso, Yoshimasa

Subjects

*NON-alcoholic fatty liver disease, *LIVER cells, *LIPID metabolism, *ADIPOSE tissues, *T cells, *MICE, *ADIPOSE tissue physiology

Abstract

Nonalcoholic fatty liver disease (NAFLD) is an emerging worldwide health concern. The disease may involve immune cells including T cells, but little is known about the role(s) of the innate-like T cells in the liver. Furthermore, the most abundant innate-like T cells in the human liver are mucosal-associated invariant T (MAIT) cells, but the involvement of MAIT cells in NAFLD remains largely unexplored because of their paucity in mice. In this study, we used a novel mouse line, Vα19, in which the number of MAIT cells is equivalent to or greater than that in humans. Compared with the control mice, Vα19 mice fed a high-fat diet (HFD) exhibited a reduction in lipid accumulation, NAFLD activity score, and transcripts relevant to lipogenesis. In addition, serum triglyceride and non-esterified fatty acids were lower in Vα19 mice fed normal chow or HFD. In contrast, the Vα19 mice showed little or no change in glucose tolerance, insulin sensitivity, inflammation in adipose tissues, or intestinal permeability compared with the controls, irrespective of diet. These results suggest that the presence of MAIT cells is associated with reduced lipogenesis and lipid accumulation in the liver; however, further studies are needed to clarify the role of MAIT cells in hepatic lipid metabolism. [ABSTRACT FROM AUTHOR]

Published

2022

249. The Role of Adipokines in Inflammatory Mechanisms of Obesity.

Author

Kirichenko, Tatiana V., Markina, Yuliya V., Bogatyreva, Anastasia I., Tolstik, Taisiya V., Varaeva, Yurgita R., and Starodubova, Antonina V.

Subjects

*ADIPOKINES, *REGULATION of blood pressure, *ADIPOSE tissue physiology, *INSULIN sensitivity, *OBESITY, *CELL communication, *CELL physiology

Abstract

Adipokines are currently widely studied cellular signaling proteins produced by adipose tissue and involved in various processes, including inflammation; energy and appetite modulation; lipid and glucose metabolism; insulin sensitivity; endothelial cell functioning; angiogenesis; the regulation of blood pressure; and hemostasis. The current review attempted to highlight the key functions of adipokines in the inflammatory mechanisms of obesity, its complications, and its associated diseases. An extensive search for materials on the role of adipokines in the pathogenesis of obesity was conducted online using the PubMed and Scopus databases until October 2022. [ABSTRACT FROM AUTHOR]

Published

2022

250. Identification of Differentially Expressed miRNAs in Porcine Adipose Tissues and Evaluation of Their Effects on Feed Efficiency.

Author

Liao, Mingxing, Ren, Zhuqing, and Miao, Yuanxin

Subjects

*MICRORNA, *SWINE nutrition, *ADIPOSE tissue physiology, *LIPID metabolism, *GENE expression, *ENERGY metabolism, *ADIPOSE tissues

Abstract

Feed efficiency (FE) is a very important trait affecting the economic benefits of pig breeding enterprises. Adipose tissue can modulate a variety of processes such as feed intake, energy metabolism and systemic physiological processes. However, the mechanism by which microRNAs (miRNAs) in adipose tissues regulate FE remains largely unknown. Therefore, this study aimed to screen potential miRNAs related to FE through miRNA sequencing. The miRNA profiles in porcine adipose tissues were obtained and 14 miRNAs were identified differentially expressed in adipose tissues of pigs with extreme differences in FE, of which 9 were down-regulated and 5 were up-regulated. GO and KEGG analyses indicated that these miRNAs were significantly related to lipid metabolism and these miRNAs modulated FE by regulating lipid metabolism. Subsequently, quantitative reverse transcription–polymerase chain reaction (qRT-PCR) of five randomly selected DEMs was used to verify the reliability of miRNA-seq data. Furthermore, 39 differentially expressed target genes of these DEMs were obtained, and DEMs–target mRNA interaction networks were constructed. In addition, the most significantly down-regulated miRNAs, ssc-miR-122-5p and ssc-miR-192, might be the key miRNAs for FE. Our results reveal the mechanism by which adipose miRNAs regulate feed efficiency in pigs. This study provides a theoretical basis for the further study of swine feed efficiency improvement. [ABSTRACT FROM AUTHOR]

Published

2022