Complex Roles of Macrophages in Lipid Metabolism and Metabolic Disease: A Dissertation

Negrin, Kimberly A.

16 April 2014

The worldwide prevalence of obesity and metabolic disease is increasing at an exponential rate and current projections provide no indication of relief. This growing burden of obesity-related metabolic disorders, including type 2 diabetes mellitus (T2DM), highlights the importance of identifying how lifestyle choices, genetics and physiology play a role in metabolic disease and place obese individuals at a greater risk for obesity-related complications including insulin resistance (IR). This increased risk of IR, which is characterized by a decreased response to insulin in peripheral tissues including adipose tissue (AT) and liver, is associated with a chronic, low grade inflammatory state; however, the causative connections between obesity and inflammation remains in question. Experimental evidence suggests that adipocytes and macrophages can profoundly influence obesity-induced IR because adipocyte dysfunction leads to ectopic lipid deposition in peripheral insulin sensitive tissues, and obese AT is characterized by increased local inflammation and macrophage and other immune cell populations. Attempts to delineate the individual roles of macrophage-derived pro-inflammatory cytokines, like tumor necrosis factor alpha (TNF-α) and interleukin-1 beta (IL-1β), have demonstrated causative roles in impaired systemic insulin sensitivity, adipocyte function and hepatic glucose and lipid metabolism in obese animal models. Thus, the attenuation of macrophage-derived inflammation is an evolving area of interest to provide insight into the underlying mechanism(s) leading to obesity-induced IR. Thus, in the first chapter of this thesis, I describe experiments to refine the current paradigm of obesity-induced AT inflammation by combining gene expression profiling with computational analysis of two anatomically distinct AT depots, visceral adipose tissue (VAT) and subcutaneous adipose tissue (SAT) to address whether the inflammatory signature of AT is influenced by diet-induced obesity (DIO). Microarray and qRT-PCR analysis data revealed that DIO mouse SAT is resistant to high fat diet (HFD)-induced inflammation and macrophage infiltration, and our data support the current model of obesity-induced visceral adipose tissue macrophage (VATM) enrichment. Our data demonstrated robust increases in VAT pro-inflammatory cytokine expression, which are consistent with the significant increases in macrophage-specific gene expression and consistent with previous reports in which VAT inflammation is enhanced and attributed to classically activated (M1) macrophage infiltration. However, these data are only observed relative to the expression of invariant housekeeping gene expression. When M1-specific genes are expressed relative to macrophage-specific standards like F4/80 expression, these inflammatory makers are unchanged. These data indicate that the changes in the overall inflammatory profile of DIO mouse VAT is because of quantitative changes in adipose tissue macrophage (ATM) number and not qualitative changes in activation state. These observations are consistent with the idea that infiltrating ATMs may have roles other than the previously described role in mediating inflammation in obese adipose tissue. Hepatic IR occurs partly as a consequence of adipocyte dysfunction because the liver becomes a reservoir for AT-derived fatty acids (FAs), which leads to obesity-related non-alcoholic fatty liver disease (NAFLD). In the second part of my thesis, I used clodronate liposome-mediated macrophage depletion to define the role of macrophages in hepatic lipid metabolism regulation. We discovered that i.p. administration of clodronate liposomes depletes Kupffer cells (KCs) in ob/ob mice without affecting VATM content, whereas clodronate liposomes depletes both KCs and VATMs in DIO mice. To this end, we established that clodronate liposome-mediated KC depletion, regardless of VATM content in obese mice, abrogated hepatic steatosis by reducing hepatic de novo lipogenic gene expression. The observed reductions in hepatic inflammation in macrophage-depleted obese mice led to the hypothesis that IL-1β may be responsible for obesity-induced increased hepatic triglyceride (TG) accumulation. We determined that IL-1β treatment increases fatty acid synthase (Fas) protein expression and TG accumulation in primary mouse hepatocytes. Pharmacological inhibition of interleukin-1 (IL-1) signaling by interleukin-1 receptor antagonist (IL-1Ra) administration recapitulated these results by reducing hepatic TG accumulation and lipogenic gene expression in DIO mice. Thus, these data highlight the importance of the inflammatory cytokine IL-1β in obesity-driven hepatic steatosis and suggests that liver inflammation controls hepatic lipogenesis in obesity. To this end, the studies described herein provide new insight and appreciation to the multi-functional nature of macrophages and clinical implications for anti-inflammatory therapy in obesity and NAFLD treatment. We demonstrate the complexities of macrophage-mediated functions in insulin sensitive tissues and a role for obesity-induced inflammatory cytokine IL-1β in hepatic lipid metabolism modulation, which is reversed via IL-1Ra intervention. The use of anti-inflammatory therapy to ameliorate obesity-associated NAFLD was perhaps the most important contribution to this body of work and is full of promise for future clinical application. It is likely that the future of therapeutics will be multi-faceted and combine therapeutic approaches to enhance glucose tolerance and overall health in obese, IR and T2DM patients.

Fatty Liver

Inflammation

Insulin Resistance

Interleukin-1beta

Lipogenesis

Liposomes

Macrophages

Obesity

Dissertations, UMMS

Cellular and Molecular Physiology

Endocrinology

Current NAFLD guidelines for risk stratification in diabetic patients have poor diagnostic discrimination

Blank, Valentin, Petroff, David, Beer, Sebastian, Böhling, Albrecht, Heni, Maria, Berg, Thomas, Bausback, Yvonne, Dietrich, Arne, Tönjes, Anke, Hollenbach, Marcus, Blüher, Matthias, Keim, Volker, Wiegand, Johannes, Karlas, Thomas

14 February 2022

Patients with type 2 diabetes (T2D) are at risk for non-alcoholic fatty liver disease (NAFLD) and associated complications. This study evaluated the performance of international (EASL-EASD-EASO) and national (DGVS) guidelines for NAFLD risk stratification. Patients with T2D prospectively underwent ultrasound, liver stiffness measurement (LSM) and serum-based fibrosis markers. Guideline-based risk classification and referral rates for different screening approaches were compared and the diagnostic properties of simplified algorithms, genetic markers and a new NASH surrogate (FAST score) were evaluated. NAFLD risk was present in 184 of 204 screened patients (age 64.2 ± 10.7 years; BMI 32.6 ± 7.6 kg/m2). EASL-EASD-EASO recommended specialist referral for 60–77% depending on the fibrosis score used, only 6% were classified as low risk. The DGVS algorithm required LSM for 76%; 25% were referred for specialised care. The sensitivities of the diagnostic pathways were 47–96%. A simplified referral strategy revealed a sensitivity/specificity of 46/88% for fibrosis risk. Application of the FAST score reduced the referral rate to 35%. This study (a) underlines the high prevalence of fibrosis risk in T2D, (b) demonstrates very high referral rates for in-depth hepatological work-up, and (c) indicates that simpler referral algorithms may produce comparably good results and could facilitate NAFLD screening.

info:eu-repo/classification/ddc/610

ddc:610

Pediatric Percentiles for Transient Elastography Measurements

Brunnert, Lina

09 October 2023

No description available.

info:eu-repo/classification/ddc/610

ddc:610

Investigation of the relationship between genetic and environmental risk factors associated with obesity and insulin resistance in South African patients with non-alcoholic fatty liver disease(NAFLD)

Pretorius, Jakobus

12 1900

Thesis (MSCMedSc)--Stellenbosch University, 2012. / Includes bibliography / ENGLISH ABSTRACT: Non-alcoholic fatty liver disease (NAFLD) is the most prevalent chronic liver disease in the world. The disease spectrum of NAFLD extends from steatosis (types 1,2) to non-alcoholic steatohepatitis (NASH) with inflammation (types 3,4). The aims of the study were 1) to analytically validate high-throughput real time polymerase chain reaction (RT-PCR) assays for three selected single nucleotide polymorphisms (SNPs), FTO rs9939609 (intron 1 T>A), TNF-α rs1800629 (-308 G>A) and PPARγ rs1801282 (Pro12Ala, 34 C>G), and 2) to perform genotype-phenotype association studies in relation to biochemical abnormalities, disease severity and age of onset. A total of 119 patients with fatty liver identified on ultrasound, including 88 histologically confirmed NAFLD patients, and 166 control individuals were genotyped for the three selected SNPs. RT-PCR validated against direct sequencing as the gold standard was used for detection of genetic variation. All three SNPs were in Hardy Weinberg equilibrium in the study population, except for a deviation in genotype distribution detected for PPARγ rs1801282 in the NAFLD patient subgroup (p<0.001). After adjustment for age and gender, the risk-associated FTO rs9939609 A-allele was detected at a significantly higher frequency in the Caucasian compared with Coloured patients (p=0.005). The opposite was detected for the risk-associated TNF-α rs1800629 A-allele, which occurred at a significantly higher frequency in the Coloured compared with Caucasian NAFLD patients (p=0.034). The onset of fatty liver disease symptoms was on average 5 years younger in the presence of each risk-associated TNF-α rs1800629 A-allele (p=0.028). When considered in the context of an inferred genotype risk score ranging from 0-6, disease onset occurred on average 3 years earlier (p=0.008) in the presence of each risk-associated FTO A-allele, TNF-α A-allele or PPARγ C-allele. After adjustment for age, gender and race, no differences in genotype distribution or allele frequencies were observed between histologically confirmed NAFLD (types 1,2) and NASH (types 3,4) patients, while the minor allele frequency for the TNF-α rs1800629 was significantly higher in the total NAFLD (types 1-4) (p=0.047) as well as NASH subgroup (NAFLD types 3,4) (p=0.030) compared with obese patients without a histologically confirmed NAFLD diagnosis. A significant correlation was furthermore observed between the number of TNF-α rs1800629 A-alleles and increasing CRP levels (p=0.029), with a favourable reduced effect in the presence of low- to moderate alcohol intake. The average waist circumference of physically active NAFLD patients was 12% lower than in physically inactive patients (p=0.004). In view of the results presented in this study, the inclusion of the selected SNPs, and in particular the pro-inflammatory TNF-α rs1800629 polymorphism, may be considered as part of a comprehensive cardiovascular risk evaluation of NAFLD patients. Ultimately, early detection of patients with fatty liver disease symptoms and effective intervention based on the underlying disease mechanism may prevent progression from NAFLD to NASH, shown to be an independent risk factor for cardiovascular diseases. / AFRIKAANSE OPSOMMING: Nie-alkoholiese lewervervetting (NALV) is die mees algemene kroniese lewersiekte in die wêreld. Die siektespektrum van NALV strek van steatose (vervette lewer tipes 1,2) tot steatohepatitis met inflammasie (NASH tipes 3,4). Die doel van die studie was 1) om analities die hoë omset polimerase kettingreaksie (RT-PKR) metode te valideer vir die geselekteerde enkel nukleotied polimorfismes (ENPs) FTO rs9939609 (intron 1 T>A), TNF-α rs1800629 (-308 G>A) en PPARγ rs1801282 (Pro12Ala, 34 C>G), en 2) om genotipe-fenotipe assosiasie studies uit te voer ten opsigte van relevante biochemiese abnormaliteite, graad van die siekte en aanvangsouderdom. ’n Totaal van 119 pasiënte met vervette lewers is geïdentifiseer met behulp van ultraklank, insluited 88 histologies-bevestigde NALV pasiënte, en 166 kontrole individue. Hierdie pasiënte is gegenotipeer vir die 3 geselekteerde ENP’s. RT-PKR gevalideer met direkte DNA volgorde bepaling as die goue standaard, is gebruik vir opsporing van genetiese variasie. Al die ENP’s was in Hardy Weinberg ekwilibrium in die studie populasie, behalwe vir ’n afwyking in genotipe verspreiding waargeneem vir PPARγ in die NALV subgroep (p<0.001). Nadat aanpassings gemaak is vir ouderdom en geslag, is die risiko-geassosieerde FTO rs9939609 A-alleel waargeneem teen ’n betekenisvol hoër frekwensie in die Kaukasiese pasiënte in vergelyking met Kleurling pasiënte (p=0.005). Die teenoorgestelde is waargeneem vir die risiko-geassosieerde TNF-α rs1800629 A-alleel wat voorgekom het teen ’n betekenisvol hoër frekwensie in die Kleurling NALV pasiënte, in vergelyking met Kaukasiese NALV pasiënte (p=0.034). Die aanvang van NALV was gemiddeld 5 jaar vroeër in die teenwoordigheid van elke risiko-geassosieerde TNF-α rs1800629 A-alleel (p=0.028). Met inagneming van ’n genotipe risiko telling tussen 0–6, het aanvang van siekte gemiddeld 3 jaar vroeër voorgekom (p=0.008) in die teenwoordigheid van elke toenemende risiko-geassosieerde FTO A-alleel, TNF-α A-alleel en PPARγ C-alleel. Nadat aanpassings gemaak is vir ouderdom, geslag en ras, is geen verskille waargeneem in genotipe verspreiding of alleel frekwensies tussen histologies bevestigde NALV (tipes 1,2) en NASH (tipes 3,4) pasiënte nie, terwyl die minor alleel telling vir die TNF-α rs1800629 betekenisvol hoër was in die totale NALV (tipes 1–4) (p=0.047) asook die NASH subgroep (NALV tipes 3,4) (p=0.03) in vergelyking met vetsugtige pasiënte sonder ’n histologies bevestigde diagnose. ‘n Statisties beteknisvolle korrelasie is verder waargeneem tussen die aantal TNF-α rs1800629 A-allele en toenemende CRP vlakke (p=0.029), met n gunstige verlaagde effek in die teenwoordigheid van lae alcohol gebruik. Die gemiddelde middellyf-omtrek van fisies aktiewe NALV pasiënte was 12% minder as fisies onaktiewe pasiente (p=0.004). Na aanleiding van die resultate van hierdie studie behoort insluiting van geselekteerde ENP’s, en in besonder die pro-inflammatoriese TNF-α rs1800629 polimorfisme, as deel van ’n omvattende kardiovaskulere risiko evaluasie oorweeg te word. Aan die einde van die dag mag vroeë identifikasie van NALV pasiente en effektieve intervensie gebasseer op die onderliggende siekte meganisme, vordering tot NASH verhoed wat getoon is om ’n onafhanklike risiko faktor vir kardiovaskulêre siekte te wees. / Stellenbosch University. Faculty of Medicine and Health Sciences. Dept. of Pathology

Non-alcoholic fatty liver disease

Genetic and environmental risk factors

Pathology supported genetic testing

Theses -- Medicine

Dissertations -- Medicine

Theses -- Chemical pathology

Dissertations -- Chemical pathology

Insulin resistance and obesity

Pathology

Evaluation of high-throughput methodology for multi-gene screening in patients with Non-Alcoholic Fatty Liver Disease (NAFLD)

Fisher, Leslie Reginald

12 1900

Thesis (MScMedSc)--Stellenbosch University, 2011. / ENGLISH ABSTRACT: Non-Alcoholic Fatty Liver Disease (NAFLD) is the most prevalent chronic liver disease in Western countries and is considered the hepatic manifestation of the Metabolic Syndrome (MetS). Its heterogeneous nature ranges from hepatic steatosis through steatohepatitis to advanced fibrosis and cirrhosis where the ingestion of significant amounts of alcohol has been excluded. The disease profile of NAFLD and its necro-inflammatory subset Nonalcoholic Steatohepatitis (NASH) were described in the parent study, which provided a clinically well-characterised patient cohort for the present investigation. South African patients with NASH had significantly higher mean serum cholesterol and triglyceride levels than those with fatty liver only. The objective of this study was to implement a high-throughput real-time polymerase chain reaction (PCR) method in our laboratory to enable the assessment of cardiovascular genetic risk factors in NAFLD patients. The specific aims were to determine the clinical utility and perform analytical validation of each mutation included in the multi-gene cardiovascular disease (CVD) screening assay. The Pathology Supported Genetic Testing (PSGT) concept developed at our department provides a practical approach to personalized medicine. The CVD multi-gene screen analyses key metabolic pathways relating to atherogenic dyslipidaemia, chronic inflammation, hypercoagulation and iron dysregulation implicated in insulin resistance, which is known to be a universal factor in the pathogenesis of NAFLD. Deleterious low-penetrance mutations in the APOE (APOE2 and E4 alleles), MTHFR (677C>T and 1298A>C), F2 (20210G>A), FV (1691G>A, Leiden) and HFE (C282Y and H63D) genes were included for analysis due to their important role as genetic contributors to these biological processes. A total of 178 patients diagnosed with NAFLD and 75 controls were studied using direct DNA sequencing and a RT-PCR system for mutation detection. In addition, two patients with high ferritin levels were included as case studies. A significant association was found between HFE mutations and elevated Alanine Transaminase (ALT) levels in the NAFLD population (p = 0.04). This discovery is interpreted as the identification of a subset of patients at greater risk of developing progressive liver damage who would benefit most from genetic testing to direct more aggressive therapy at an earlier stage. The necessity of an integrative, systems-based network approach was demonstrated to more accurately distinguish between Hereditary Haemochromatosis (HH) and Insulin Resistance-associated Hepatic Iron Overload (IR-HIO) syndrome in obese patients. The PSGT approach to personalized medicine facilitates diagnosis of CVD subtypes, prevention of cumulative risk and the formulation of gene-based intervention programs tailored to the needs of the patient. These findings support the clinical utility of the CVD multi-gene test to guide chronic disease risk management in patients with NAFLD. The HFE mutation detection component of this test is of particular relevance in directing an effective treatment strategy in patients with a medical history of CVD and/or high iron stores. / AFRIKAANSE OPSOMMING: Nie-Alkoholiese Vettige Lewer Siekte (NAFLD) is die mees algemene kroniese lewer siekte in Westerse lande en word bestempel as die hepatiese manifestasie van die Metaboliese Sindroom (MetS). Die heterogene natuur van NAFLD strek van hepatiese steatose deur steatohepatietis tot gevorderde fibrose en sirrose waar grootskaalse alkohol inname uitgesluit is. Die siekte-profiel van NAFLD en sy nekro-inflammatoriese subtipe Nie-Alkoholiese Steatohepatietis (NASH) is reeds beskryf in die ouer studie, wat ‗n klinies goed-gekarakteriseerde pasiënt groep vir die huidige ondersoek daar gestel het. Suid-Afrikaanse pasiënte met NASH het beduidend hoër gemiddelde serum cholesterol en trigliseried vlakke in vergelyking met slegs vettige lewer. Die doel van hierdie studie was om ‗n hoë deurvoer rieëltyd polimerase kettingreaksie (RT-PCR) metode in ons laboratorium te implimenteer om kardiovaskulêre genetiese risiko faktore in NAFLD pasiënte te ondersoek. Die spesifieke mikpunte was om die kliniese nut en analitiese geldigheid van elke mutasie wat ingesluit is in die multi-geen kardiovaskulêre siekte (KVS) siftings toets vas te stel. Die Patologie Ondersteunde Genetiese Toetsing (PSGT) konsep wat by ons departement ontwikkel is, verskaf ‗n praktiese benadering tot persoonlike medisyne. Die KVS multi-geen toets analiseer belangrike metaboliese weë verwant aan atherogene dyslipidemie, kroniese inflammasie, oormatige bloedstolling en yster disregulering wat betrokke is by insulien weerstand wat bekend is as ‗n universele factor in the patogenese van NAFLD. Nadelige lae-penetrasie mutasies in die APOE (APOE2 en E4 allele), MTHFR (677C>T en 1298A>C) F2 (20210G>A), FV (1691G>A, Leiden) en HFE (C282Y en H63D) gene was ingesluit vir analise as gevolg van hul belangrike rol as genetiese bydraers tot die bogenoemde biologiese prosesse. ‗n Totaal van 178 pasiënte gediagnoseer met NAFLD en 75 kontroles is bestudeer deur gebruik te maak van direkte DNA volgordebepaling en ‗n RT-PCR metode vir mutasie opsporing. Twee pasiënte met verhoogde ferritien vlakke is ook as gevalle studies ingesluit. ‗n Beduidende assosiasie is gevind tussen HFE mutasies en verhoogde Alanien Transaminase (ALT) vlakke in die NAFLD studiepopulasie (p = 0.04) wat aanduidend is van ‗n subgroup van pasiënte wat die meeste baat sal vind uit genetiese toetsing om meer aggressiewe behandeling te rig op' n vroeër stadium. Die noodsaaklikheid van 'n geïntegreerde, stelsels-gebaseerde netwerk benadering is gewys om meer akkuraat te onderskei tussen Oorerflike Hemochromatose (HH) en Insulien Weerstand-geassosieerde Hepatiese Yster Oorlading (IR-HIO) sindroom in vetsugtige pasiënte. Die PSGT benadering tot persoonlike medisyne formuleer geen-gebaseerde intervensie programme aangepas tot die behoeftes van die pasiënt ek maak diagnose van KVS-subtipes en voorkoming van kumulatiewe risiko moontlik. Hierdie bevindinge ondersteun die kliniese nut van die KVS multi-geen toets om riglyne vir die risikobestuur van kroniese siektes soos NAFLD daar te stel. Die HFE mutasie opsporings komponent van hierdie toets is van besondere belang om 'n effektiewe strategie vir die behandeling van pasiënte met 'n mediese geskiedenis van KVS en/of hoë yster vlakke daar te stel.

Translation Research

Theses -- Pathology

Dissertations -- Pathology

Cardiovascular system -- Diseases

Pathology

Avaliação antropométrica e de composição corporal em mulheres sedentárias pós-menopausa com Doença Hepática Gordurosa Não Alcoólica (DHGNA) submetidas à atividade física / Anthropometric evaluation and body composition in sedentary postmenopausal women with Nonalcoholic fatty liver disease (NAFLD) submitted to physical activity

Duarte, Sebastião Mauro Bezerra

02 June 2015

A Doença hepática gordurosa não alcoólica (DHGNA) é uma das formas mais comuns de doença hepática, acometendo cerca de 20 a 30% da população adulta, sendo mais frequente em indivíduos obesos (70 a 80%). Os principais fatores de risco associados à doença são os componentes da Síndrome metabólica. Até o momento, não há um tratamento farmacológico específico para a DHGNA e modificações no estilo de vida com redução de peso e exercício físico são sempre preconizados. Existem poucos dados sobre o impacto da atividade física e uma estratégia nutricional ideal no tratamento da DHGNA. Visto a necessidade de elucidar o impacto da atividade física e a busca por uma estratégia nutricional ideal no tratamento da DHGNA, propusemos um estudo randomizado controlado avaliando os efeitos de uma dieta hipocalórica e hiperproteica e do exercício físico aeróbio associado a esta dieta nos parâmetros metabólicos e antropométricos de mulheres sedentárias pós-menopausa. Foram incluídas 40 mulheres sedentárias pós-menopausa com DHGNA, que possuíam biópsia hepática em um período igual ou menor que 2 (dois) anos. Essas pacientes foram randomizadas em 2 grupos: grupo TREINO: treinamento aeróbio associado à dieta hipocalórica e hiperproteica e grupo DIETA: somente dieta hipocalórica e hiperproteica e, acompanhadas por um período de 6 meses. Na análise intra-grupo das variáveis antropométricas nos períodos pré e pós-intervenção dietética ou exercício físico aeróbio não foram observadas diferenças significativas em ambos os grupos. Na análise intra-grupo das variáveis bioquímicas, o HDL mostrou-se estatisticamente diferente (p= 0,004) no grupo TREINO. Na análise inter-grupos das variáveis bioquímicas observamos um aumento significativo para HDL-C (p= 0,036) no grupo TREINO. Na análise intra-grupo das variáveis ergoespirométricas observamos diferença significativa para as variáveis VO2máx Relativo (p= 0,04), Tempo LA (p= 0,001), Tempo PCR (p= 0,003) e Tempo Pico (p= 0,001) no grupo TREINO. Na análise inter-grupo das variáveis ergoespirométricas a análise das variáveis VO2máx Relativo (p= 0,042), Tempo LA (p= 0,011), Tempo PCR (p= 0,002) e Tempo Pico (p= 0,007) foram estatisticamente diferentes. Nossos dados mostram uma estreita relação entre a intervenção nutricional, exercício aeróbio e a melhora da DHGNA. Apesar do tempo proposto de exercício semanal ter sido relativamente pequeno, nossos dados mostram que tanto a dieta hipocalórica e hiperproteica quanto o tratamento com exercício aeróbio duas vezes por semana associado a esta dieta podem ser eficazes para o tratamento da DHGNA em mulheres sedentárias pós-menopausa. Salientamos a importância do exercício aeróbio associado à dieta hipocalórica e hiperproteica para o aumento do HDL-C sérico e melhora da aptidão cardiorrespiratória neste grupo de mulheres. Consideramos que ambos os tratamentos podem ser recomendados de acordo com a particularidade de cada indivíduo, respeitando suas dificuldades e limitações / The Nonalcoholic fatty liver disease (NAFLD) is the most common form of liver diseases, affecting approximately 20-30% of the adult population and is more common in obese individuals (70-80%). The main risk factors associated with the disease are the components of the Metabolic syndrome. To date, there is no specific pharmacological treatment for NAFLD and changes in lifestyle with weight reduction and exercise are always recommended. Few datas exist on the impact of physical activity and optimal nutritional strategy for the treatment of NAFLD. Seen the need to elucidate the impact of physical activity and the search for an ideal nutritional strategy in the treatment of NAFLD, we proposed a randomized controlled trial evaluating the effects of a hypocaloric high-protein diet and aerobic exercise associated with this diet on metabolic and anthropometric parameters in sedentary postmenopausal women. 40 sedentary postmenopausal women with NAFLD who had liver biopsy for a period equal to or less than 2 (two) years were included. These patients were randomized into 2 groups: TRAINING group: aerobic training with hypocaloric high-protein diet and DIET group: only hypocaloric high-protein diet, and followed for a period of six months. In intra-group anthropometric variables pre and post dietary intervention or aerobic exercise analysis, no significant differences were observed in both groups. In intra-group analysis of biochemical variables, HDL was statistically different (p= 0.004) on the TRAINING group. In inter-group analysis of biochemical variables observed a significant increase in HDL-C (p= 0.036) on TRAINING group. In the analysis of intra-group ergospirometric variables significant differences were observed for the variables Relative VO2max (p= 0.04), Time at VAT (p= 0.001), Time at RCP (p= 0.003) and Time at peak (p= 0.001) in TRAINING group. In the analysis of inter-group ergospirometric variables Relative VO2máx (p= 0.042), Time at VAT (p= 0.011), Time at RCP (p= 0.002) and Time at peak (p= 0.007) were significantly different. Our data shows a close relationship between nutrition intervention, aerobic exercise and improvement of NAFLD. Although the proposed weekly exercise time was relatively small, our data show that both a low-calorie diet and protein levels as treatment with aerobic exercise twice a week associated with this diet may be effective for treating NAFLD in postmenopausal women sedentary. Stress the importance of aerobic exercise associated with low-calorie and high-protein diet for the increase in serum HDL-C and improves cardiorespiratory fitness in this group. We believe that both treatments may be recommended according to the particularity of each individual, respecting their difficulties and limitations

Anthropometry

Antropometria

Body composition

Composição corporal

Diet high-fat

Dieta hiperlípidica

Exercício físico

Nonalcoholic fatty liver disease

Physical activity

Efeito da Síndrome dos Ovários Policísticos em múltiplos marcadores ultrassonográficos e laboratoriais de risco metabólico e doença cardiovascular em mulheres obesas sem outras condições de saúde que interferem com critérios de elegibilidade de contraceptivo oral combinado / Effect of polycystic ovary syndrome on multiple ultrasonographic and laboratorial markers of metabolic and cardiovascular disease risk in obese women without any other health condition that interferes with combined oral contraceptive elegibility criteria: a case-control study

Zueff, Lucimara Facio Nobre

04 October 2011

OBJETIVO: Avaliamos se a presença da síndrome dos ovários policísticos (SOP) altera múltiplos marcadores ultrassonográficos e laboratoriais de risco metabólico e doença cardiovascular em mulheres obesas sem outras condições que interferem com o critério de elegibilidade do contraceptivo oral combinado (COC). MÉTODOS: Estudo caso-controle avaliando 90 mulheres obesas ( 30,0 Kg/m² e < 40 Kg/m²), com idade entre 18 e 40 anos, sem outras condições de saúde que interferem com os critérios de elegibilidade de COC: 45 com SOP e 45 controles, pareadas por idade. Índice de massa corporal; circunferência da cintura e do quadril; pressão arterial sanguínea; insulina e glicemia de jejum; quantitative insulin sensitivity check index (QUICKI); HDL, LDL e colesterol total; triglicérides; testosterona; globulina carreadora de hormônios sexuais (SHBG); índice de androgênio livre (FAI); índice de rigidez da carótida e espessura íntimamédia (EIM); dilatação mediada por fluxo da artéria braquial (DMF) e doença hepática gordurosa não alcoólica (DHGNA) foram avaliados. RESULTADOS: Em mulheres obesas com SOP, observamos uma maior freqüência de DHGNA quando comparada a obesas sem SOP (73,4% vs. 46,6%, p<0,01). Embora não significativo, observamos uma tendência a aumento da insulina (10,06±6,66 UI/mL vs. 7,45±5,88 UI/mL, p=0,05), diminuição do QUICKI (0,36±0,06 vs. 0,39±0,07, p=0,05) e diminuição da DMF (7,00±3,87% vs. 8,41±3,79%, p=0,08). Nenhuma outra diferença significativa foi observada. CONCLUSÕES: DHGNA é freqüente em mulheres obesas sem outras condições que interferem com o critério de elegibilidade do COC, especialmente naquelas com SOP. Isto deveria ser considerado na escolha da melhor opção contraceptiva. / OBJECTIVE: To evaluate whether the presence of polycystic ovary syndrome (PCOS) alters multiple ultrasonographic and laboratorial markers of metabolic and cardiovascular disease risk in obese women without any other health condition that interferes with combined oral contraceptive (COC) eligibility criteria. METHOD: A case-control study evaluating 90 obese women ( 30.0kg/m² and <40kg/m²) aged between 18 and 40 years without any other health condition that interferes with COC eligibility criteria: 45 with PCOS and 45 age-matched controls. Body mass index; waist and hip circumference; arterial blood pressure; fasting insulin and glucose; quantitative insulin sensitivity check index (QUICKI); HDL, LDL and total cholesterol; triglycerides; testosterone; sex hormone-binding globulin (SHBG), free androgen index (FAI); carotid stiffness index and intima media thickness; flow-mediated dilatation of brachial artery; and nonalcoholic fatty liver disease (NAFLD) were assessed. Results: In PCOS women, we observed a higher frequency of NAFLD (73.4% vs. 46.6%, p<0.01) and higher FAI (10.43% vs. 6.84%, p<0.01). We also observe a trend of increased insulin (10.06±6.66IU/mL vs. 7.45±5.88IU/mL, p=0.05), decreased QUICKI (0.36±0.06 vs. 0.39±0.07, p = 0.05), and decreased FMD (7.00±3.87% vs. 8.41±3.79%, p=0.08). No other significant difference was observed. Conclusions: NAFLD is frequent in obese women without any other health condition that interferes with COC eligibility criteria, especially in those with PCOS. This should be considered when choosing the best contraceptive option.

cardiovascular disease

doença cardiovascular

endotélio

endothelium

nonalcoholic fatty liver disease

obesidade

obesity

Polycystic ovary syndrome

Análise metabolômica e histomorfométrica do fígado de ratas adultas em modelo experimental da síndrome dos ovários policísticos induzida por exposição neonatal a esteroides sexuais / Metabolomic and histomorphometric analysis of the liver of rat models of polycystic ovary syndrome induced by neonatal exposure to sex steroids.

Anzai, Alvaro

11 August 2015

A síndrome dos ovários policísticos (SOP) é um distúrbio endócrino complexo, associado a resistência insulínica, hiperinsulinemia, obesidade, acúmulo de gordura visceral e dislipidemia. Essas alterações podem levar a aumento de risco de doenças como \"diabetes mellitus\", doenças cardiovasculares, esteatose hepática ou até mesmo esteato-hepatite. Em ratas, o excesso de androgênios ou estrogênios no período neonatal induz a alterações metabólicas e reprodutivas similares às observadas na SOP em humanos. O objetivo deste estudo é analisar os efeitos da exposição neonatal à testosterona e ao estrogênio no fígado de ratas adultas. Para isso foram utilizadas 30 ratas, divididas em três grupos de 10 animais cada. Foi administrada por via subcutânea, entre 1 e 3 dias de vida, uma única dose dos seguintes compostos: 0,1 mL de óleo de oliva (veículo) - grupo Controle (n=10); propionato de testosterona (1,25 mg/0,1mL de veículo) - grupo Testosterona (n=10); benzoato de estradiol (0,5 mg/0,1mL de veículo) - grupo Estradiol (n=10), de acordo com o grupo a que pertenciam. Após cerca de 90 dias, os animais foram sacrificados, sendo retirados fragmentos do fígado que foram preparados para análise da metabolômica e da histomorfologia. Histologicamente, o fígado dos animais do grupo testosterona apresentaram maior infiltração gordurosa e infiltrado inflamatório; e do grupo estradiol apresentou hepatócitos binucleados, além do aumento do volume nuclear. Houve, no grupo testosterona modificações no perfil metabolômico ligadas a maior resistência à insulia e maior risco para diabete. O grupo exposto ao estrogênio apresentou alterações relacionadas ao metabolismo e síntese de lipídeos. Nossos resultados sugerem que os riscos metabólicos associados à SOP podem ter origem e mecanismos diferentes / Polycystic ovary syndrome (PCOS) is a complex endocrine disorder associated with insulin resistance, hyperinsulinemia, central obesity, accumulation of visceral fat and dyslipidemia. Those changes can lead to increased risk of diseases such as diabetes mellitus, cardiovascular disease, nonalcoholic fat liver disease or even nonalcoholic steatohepatitis. In rats, the excess of androgens or estrogens in the neonatal period leads to metabolic and reproductive alterations similar to those observed in SOP in humans. The objective of this study is to analyze the effects of exposure to neonatal testosterone and estrogen in the liver of adult rats. For this we used 30 female rats, sorted into three groups of 10 animals each. It was administered subcutaneously between 1 and 3 days of age a single dose of the following compounds: 0.1 mL olive oil (vehicle) - Control Group (n = 10); testosterone propionate (1.25 mg / 0.1 mL vehicle) - Testosterone (n = 10); estradiol benzoate (0.5 mg / 0.1 mL vehicle) - Estradiol group (n = 10). After 90 days, the animals were sacrificed, and the liver removed fragments were prepared for analysis of metabolomics and histomorphometry. Histologically, the testosterone group displayed greater fat deposition and higher degree of inflammatory infiltration. The estradiol group had binucleate hepatocytes and increased nuclear volume. Testosterone group showed changes in the metabolomic profile linked to increased insulin resistance and increased risk for diabetes mellitus. The group exposed to estrogen showed changes related to metabolism and synthesis of lipids. Our results indicate that the metabolic risks associated with PCOS may have origin and different mechanisms

Animal models

Fatty liver

Fígado gorduroso

Hepatopatia gordurosa não alcoólica

Histomorfometria

Metabolômica

Metabolomics

Modelos animais

Non alcoholic fat liver disease

Síndrome do ovário policístico

Papel da alça ECA2/Ang 1-7/Mas na prevenção da doença hepática gordurosa não alcoólica por meio do treinamento físico aeróbio / Role of the ACE2/Ang 1-7/Mas in the prevention of non-alcoholic fatty liver disease through aerobic physical training

Lima, Vanessa Cristina Fortunato

06 December 2017

A doença hepática gordurosa não alcoólica (DHGNA) consiste na alteração morfofisiológica do fígado decorrente do acúmulo de lipídios nos hepatócitos. O desenvolvimento de DHGNA pode estar associado à obesidade e o diabetes tipo 2, e um dos possíveis mecanismos mediadores é a hiperatividade da alça ECA/Ang II/AT1 do sistema renina angiotensina (SRA). Por outro lado, evidências mais recentes mostraram que a ativação da alça ECA2/Ang 1-7/Mas do SRA age na direção oposta, podendo atenuar as manifestações clínicas das doenças metabólicas. O treinamento físico aeróbio (TFA) tem sido amplamente recomendado para a prevenção e o tratamento de doenças metabólicas, inclusive da DHGNA, e parte das respostas benéficas podem estar associadas com a melhora do metabolismo oxidativo. Assim, o objetivo desse estudo foi investigar se a prevenção da DHGNA por meio do TFA é mediada pela melhora do metabolismo hepático associada à ativação da alça do SRA ECA2/ Ang1-7/ Mas. Para isso, camundongos C57BL/6 foram separados em grupos (n=10/grupo) sedentários (SED) alimentados com dieta normocalórica (NO) ou de cafeteria (CAF) (SED-NO e SED-CAF, respectivamente) e submetidos ao TFA alimentados com dieta NO ou CAF (TF-NO e TF-CAF, respectivamente). O grupo SED-CAF apresentou maior ganho de peso corporal, conteúdo de lipídios e de IL-6 no fígado, e o TFA previniu esses aumentos no grupo TF-CAF. Não houve diferença na concentração sérica das enzimas ALT e AST, na expressão de genes relacionados com o metabolismo lipídico e na expressão das proteínas AMPK, PGC1- , SIRT-1, ACC e receptor Mas no fígado. Os grupos TF-NO e TF-CAF apresentaram maior atividade da ECA2 no soro comparados ao SED-NO e SED-CAF, porém a atividade da ECA2 e o conteúdo do peptídio Ang1-7 não foram diferentes entre os grupos. O TF-NO apresentou menor atividade da enzima ECA no fígado comparado ao grupo TF-CAF. Coletivamente, os dados obtidos permitem afirmar que o TFA preveniu a DHGNA evidenciado pelo menor conteúdo de lipídios e citocina pró-inflamatória IL-6, no entanto, essa resposta foi independente de mudanças na expressão de genes e de proteínas reguladoras do metabolismo hepático associada à alça do SRA ECA2/ Ang1-7/ Mas / Non-alcoholic fatty liver disease (NAFLD) consists in the morphophysiological alteration of the liver due to the accumulation of lipids in the hepatocytes. The development of NAFLD may be associated with obesity and type 2 diabetes, and one of the possible mediating mechanisms is the hyperactivity of the ACE/Ang II/AT1 axis of the renin angiotensin system (RAS). On the other hand, evidence have shown that the activation of the ACE2/Ang 1-7/Mas have opposite effect, being able to attenuate clinical manifestations of the metabolic diseases. Aerobic physical training (APT) has been widely recommended for the prevention and treatment of metabolic diseases, including NAFLD, and some of the beneficial responses may be associated with improved oxidative metabolism. Thus, the aim of this study was to investigate whether the prevention of NAFLD by APT is mediated by the improvement of the metabolism associated with the activation of the RAS ACE2/Ang1-7/Mas axis. For this, C57BL/6 mice were separated into sedentary groups (SED) fed normocaloric (NO) or cafeteria (CAF) diet (SED-NO and SED-CAF, respectively) and trained with APT fed NO or CAF diet (TF-NO and TF-CAF, respectively). The SED-CAF group presented higher body weight gain, lipid and IL-6 content in the liver, and APT prevented these increases in the TF-CAF group. No differences were observed in the concentration of ALT and AST enzymes, in the expression of genes related to lipid metabolism and in the expression of AMPK, PGC1- , SIRT-1, ACC and receptor Mas in the liver. TF-NO and TF-CAF groups had higher serum ACE2 activity compared to SED-NO and SED-CAF, however ACE2 activity and Ang1-7 content were not different among groups. TF-NO showed lower ACE activity in the liver compared to the TF-CAF group. Collectively, the results showed that APT prevented NAFLD evidenced by the lower lipid content and pro-inflammatory cytokine IL-6, however, this response is independent of changes in gene expression and in hepatic metabolism regulatory proteins expression associated with the SRA ACE2/Ang1-7/Mas axis

Aerobic physical training

Angiotensin 1-7

Angiotensina 1-7

Cafeteria diet

Dieta de cafeteria

Non-alcoholic fatty liver disease

Treinamento físico aeróbio

Modelo experimental para indução de esteatose hepática e esteatohepatite: estudo em ratos / Experimental model for induction of steatosis and steatohepatitis - study in rats

Silva, Eliana Pinheiro da

29 October 2012

Introdução: A Doença Hepática Gordurosa Não Alcoólica (DHGNA) tem sido considerada atualmente a forma mais comum de doença hepática no mundo ocidental, relacionada principalmente ao aumento da prevalência da obesidade.A DHGNA abrange um largo espectro de doença, desde casos de esteatose simples (EH) até esteato-hepatite não alcoólica (EHNA) e fibrose, podendo evoluir para cirrose e carcinoma hepatocelular (CHC). Embora se conheçam os fatores predisponentes para o desenvolvimento de EHNA, sua patogênese, assim como tratamento eficaz, permanecem pouco conhecidos.Os lípides, principalmente gorduras neutras, fosfolipídios e colesterol, são componentes fundamentais das células, assim como as proteínas e os hidratos de carbono. Embora aumentos marcantes de proteínas e hidratos de carbono não produzam quaisquer alterações macroscópicas no fígado, um acúmulo de gordura é prontamente reconhecido pela coloração amarelada e pelo aumento de volume do órgão. Várias dietas tem sido usadas em animais de laboratórios, principalmente camundongos e ratos no sentido de induzir esteatose, esteatohepatite e fibrose hepática, embora nenhuma delas consiga reproduzir na totalidade os componentes essenciais da doença humana. Não encontramos em nenhum trabalho da literatura a utilização da dieta deficiente em colina e hiperlipídica (DCH), por nós utilizada. Objetivo: O objetivo deste estudo foi avaliar o efeito de uma dieta deficiente em colina e hiperlipídica (DCH) para desenvolver esteatose hepática, esteatohepatite e fibrose hepática no rato. Métodos: A doença hepática foi induzida em ratos Sprague-Dawley machos pesando de 300 a 350 gramas, hospedados em gaiolas padrão e recebendo água à vontade. Foi usado dieta deficiente em colina e hiperlipídica (DCH). Os animais foram distribuídos por meio de tabela sequencial randomizada em dois grupos. No grupo 1 dez ratos receberam a dieta por 4 meses e no grupo 2 dez ratos receberam a dieta durante 8 meses. Após o tempo estipulado das dietas os animais foram anestesiados e sacrificados. Os fígados dos animais foram retirados, pesados e enviados para estudo histopatológico de acordo com os critérios estabelecidos por Kleiner. Os animais foram pesados no início do experimento e por ocasião do sacrifício. Resultados: o peso dos animais do grupo 1 (DCH - 4 meses) no início do experimento variou de 305 a 350 gramas com média de 329,9 gramas e no fim do experimento de 529 a 615 gramas com média de 579,2 gramas. O percentual de ganho de peso dos animais variou de 60 a 86,93% com média de 75,72%. O peso dos animais do grupo 2 (DCH - 8 meses) no início do experimento variou de 320 a 353 gramas com média de 339,4 gramas e no fim do experimento variou de 661,5 a 783 gramas com média de 705,6 gramas. O percentual do ganho de peso dos animais variou de 95,58 a 123,71% com média de 107,78%. O peso do fígado dos animais do grupo 1 no fim do experimento variou de 24,5 a 29,5 gramas. O percentual do peso do fígado em relação ao peso dos animais do grupo 1 variou de 4,16 a 5,54% com média de 4,75%. O peso do fígado dos animais do grupo 2 no fim do experimento variou de 31 gramas a 39 gramas com média de 33,8 gramas. O percentual do peso do fígado em relação ao peso dos animais do grupo 2 variou de 4,63% a 5,07%, com média de 4,78%. A análise histopatológica dos animais do grupo 1 demonstrou intensa balonização e esteatose microgoticular com inflamação lobular; o estadiamento de fibrose foi discreto nestes animais. O estudo histopatológico dos animais do grupo 2 revelou intensa esteatose microgoticular e balonização com inflamação lobular; alguns animais apresentaram esteatose macrogoticular. Os animais deste grupo 2 apresentaram fibrose com grande variação individual. Os animais de ambos os grupos experimentais desenvolveram esteatohepatite, pois apresentaram o índice de atividade da doença hepática gordurosa não alcoólica (NAS)>=5. A análise comparativa demonstrou não haver diferença estatística no valor do NAS entre os dois grupos experimentais. Em relação ao estadiamento da fibrose na esteatohepatite não alcoólica, os animais do grupo 2 apresentaram uma tendência de escores mais elevados do que os animais do grupo 1. No entanto não houve diferença estatística entre os grupos devido a grande variação individual (p=0,2755). Conclusões: A dieta DCH administrada durante 4 e 8 meses induziu nos ratos aumento considerável de peso corpóreo e do peso do fígado. Os animais do grupo 1 apresentaram intensa balonização, esteatose microgoticular e inflamação lobular com discreta fibrose hepática. Os animais do grupo 2 apresentaram intensa balonização, esteatose macro e microgoticular, inflamação lobular e maior grau de fibrose hepática, bem estabelecida com formação de colágeno e expansão fibrosa nos espaços vasculares. A dieta deficiente em colina e hiperlipídica (DCH) induziu no rato esteatose hepática e esteatohepatite com fibrose, servindo de modelo experimental para proporcionar melhor entendimento para procedimentos terapêuticos futuros desta importante patologia do fígado. / Introduction: Nonalcoholic Fatty Liver Disease (NAFLD) has currently been regarded as the most common form of liver disease in the western world, mainly related to the increased prevalence of obesity. NAFLD covers a broad spectrum of diseases, since cases of simple steatosis (HS) to steatohepatitis (EHNA) and fibrosis, and may evolve to cirrhosis and hepatocellular carcinoma (CHC). Although the predisposing factors for the development of EHNA are well established, there is little knowledge on its pathogenesis as well as the effective treatment options. Lipids, especially phospholipids, neutral fats and cholesterol, are fundamental cell components, as well as proteins and carbohydrates. Although striking increases of proteins and carbohydrates do not produce liver macroscopic changes, fat build up can be rapidly recognized by the yellow coloring and increased organ volume. Many diets have been used in laboratory animals, mainly rats although none of them can fully reproduce the fundamental components of the human disease. We could not find in the literature any study on the use of choline-deficient and hiperlipidic diet (CHD), used in the present study. Goal: The objective of this study was to evaluate the effect of a cholinedeficient and hiperlipidic diet (CHD) on the development of steatosis, steatohepatitis and hepatic fibrosis in rats. Methods: The liver disease was induced in male Sprague-Dawley rats, weighing from 300 to 350 grams, hosted in standard cages and receiving water ad libitum and fed with a choline-deficient and hiperlipidic diet (CHD). The experimental animals were distributed by means of a random sequential table in two groups. In Group 1 ten rats received the diet for four months and in Group 2 ten rats received the same diet for eight months. After these predetermined feeding time periods the animals were anesthetized and sacrificed. The animal livers were then removed, weighed and sent to histopathological study according to the criteria established by Kleiner. All the animals were weighed at the beginning of the experiment and by the time of the sacrifice. Results: The weight of Group 1 animals (4 months CHD) at the beginning of the experiment varied from 305 to 350 grams with an average of 329.9 grams and at the end of the experiment from 529 to 615 grams averaging 579.2 grams. The percentage of weight gain in animals of this group ranged from 60% to 86.93% with an average of 75.72%. The weight of Group 2 animals (8 months CHD) at the start of the experiment varied from 320 to 353 grams with an average of 339.4 grams and at the end of the experiment from the 661.5 to 783 g with an average of 705.6 grams. The percentage of weight gain in animals of this group varied from 95.58% to 123.71%, averaging 107.78%. The liver weight of Group 1 animals at the end of the experiment varied from 24.5 to 29.5 grams. The percentage of liver weight in relation to the animals\' weight, in Group 1, ranged from 4.16% to 5.54%, with an average of 4.75%. The liver weight of Group 2 animals at the end of the experiment varied from 31gramas to 39 grams, with an average of 33.8 gram. The percentage of liver weight in relation to the animals\' weight, in Group 2, ranged from 4.63% to 5.07%, with an average of 4.78%. Liver histopathological analysis in Group 1 animals showed marked ballooning degeneration and microgoticular steatosis with lobular inflammation; fibrosis staging was discreet in these animals. Liver histopathological study in animals of Group 2 showed an intense microgoticular steatosis and ballooning with lobular inflammation; some animals of this group presented macrogoticular steatosis. The amount of hepatic fibrosis in animals of this group was extremely variable. Animals of both experimental groups developed steatohepatitis, as they presented the activity index of nonalcoholic fatty liver disease (NAS) >= 5. Statistical analysis did not show a significant difference between the NAS values of the two experimental groups. Fibrosis staging analysis in non-alcoholic steatohepatitis showed a trend toward higher scores in animals of Group 2 as compared to Group 1 animals. However there was no statistical difference between the groups due to a large individual variation (p = 0.2755). Conclusions: CHD diet administered for four and eight months induced considerable increases in the rats\' body weight and liver weight. Animals in Group 1 showed intense liver ballooning, steatosis and lobular inflammation with discrete microgoticular fibrosis. Animals in Group 2 presented intense ballooning, steatosis macro and microgoticular, lobular inflammation and a higher degree of well-established hepatic fibrosis, with collagen formation with fibrotic expansion in vascular spaces. Choline-deficient and hiperlipidic diet (CHD) in the rat induced hepatic steatosis and steatohepatitis with fibrosis, representing an experimental model, which can provide a better knowledge for future therapeutic procedures of this important liver pathology.

Carcinoma hepatocelular

Esteato hepatite

Fatty liver

Fibrose hepática

Fígado gorduroso

Hepatic fibrosis

Hepatocellular carcinoma

Ratos Sprague-Dawley

Sprague - Dawley rats

Steato hepatitis