49 research outputs found

    Alterações na microbiota intestinal de ratos Wistar obesos e não-obesos através da administração do extrato comercial de guaraná (Paullinia cupana)

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    O guaraná (Paullinia cupana) é uma planta nativa da América do Sul, e suas sementes tem sido utilizadas por tribos amazônicas desde antes da colonização. O extrato de guaraná é consumido popularmente nos dias de hoje, entretanto pouco se sabe sobre a relação desse extrato com a microbiota intestinal. A microbiota possui um papel central na absorção de nutrientes da dieta e na regulação do metabolismo energético, sendo modificada na obesidade. A microbiota intestinal também é afetada pelo consumo de compostos vegetais, sendo muitas vezes regulada positivamente por dietas ricas em polifenóis. Todavia, o consumo de extratos vegetais pode gerar um desfecho tóxico, assim como alterações negativas na microbiota. O efeito de extratos ricos em compostos secundários deve ser estudado individualmente. Nesse trabalho avaliamos as alterações no ecossistema intestinal causadas pelo extrato comercial de sementes do Guaraná em animais saudáveis e no contexto da obesidade.Induzimos a obesidade em animais através de uma dieta que mimetiza a dieta ocidental, caracterizada por uma maior quantidade de gordura, sal e açúcar refinado, e uma menor quantidade de fibras. Os animais também foram submetidos ao tratamento com um extrato comercial de Guaraná, cafeína ou salina. A disbiose intestinal foi medida no conteúdo cecal através da amplificação e sequenciamento da porção ribossomal 16S. Também foi medida a atividade enzimática no fígado, rins e intestino delgado, assim como a quantidade de citocinas proinflamatórias no soro. A dieta obesogênica gerou um aumento no ganho de peso e no acúmulo de gordura dos animais comparada com a dieta Chow. Tanto o Guaraná quanto a cafeína não foram capazes de reverter o ganho de peso e o acúmulo de gordura. Também observamos a diminuição da atividade da enzima CAT no rim nos animais que receberam guaraná, independente da dieta. A dieta obesogênica induziu alterações na microbiota intestinal semelhantes às da obesidade, diminuindo a proporção de Bacteroidetes sobre Firmicutes, aumentando o gênero Mucispirilum e diminuindo os gêneros Lactobacillus e Bifidobacterium. Os tratamentos com guaraná e cafeína na dieta Chow diminuíram a proporção B/F, assim como o gênero Bifidobacterium. Observamos um aumento no filo Proteobacteria nos animais do grupo controle obeso. Esse aumento foi revertido pelo tratamento com guaraná. Analisando os gráficos de clusterização e landscape, observamos uma maior distância entre a microbiota dos animais que receberam dietas diferentes do que a dos animais que receberam tratamentos diferentes. Os tratamentos com guaraná ou cafeína modificaram o ecossistema intestinal, mas sem a capacidade de diminuir o acúmulo de gordura ou o ganho de peso. A maior alteração na microbiota foi devido à dieta obesogênica e não aos tratamentos, mostrando que os efeitos anti-obesogênicos do guaraná observados em outros estudos provavelmente não são via microbiota intestinal.Guarana (Paullinia cupana) is a plant native of South America, and its seedshave been used by Amazonian tribes since before colonization. Guarana extract is consumed popularly today, however little is known about the interactions of this extract with the intestinal microbiota. The gut microbiota plays a central role in the absorption of nutrients from the diet and in the regulation of energy metabolism, being altered in obesity. The intestinal microbiota is also affected by the consumption of plant metabolites and is often regulated positively by diets rich in polyphenols. However, the consumption of plant extracts can generate a toxic outcome, as well as negative changes in the microbiota. Therefore, the effect of plant extracts should be studied individually. In this work, we evaluated the changes in the intestinal ecosystem caused by the administration of a commercial extract of Guaraná seeds in healthy animals and in the context of obesity. We induced obesity in animals through a diet that mimics the western diet, characterized by a higher amount of fat, salt and refined sugar, and a smaller amount of fiber. The animals were also treated with a commercial extract of Guarana, caffeine or saline. Intestinal dysbiosis was evaluated by cecal content, amplification and sequencing of the 16S ribosomal portion. The antioxidant enzymatic activity of the liver, kidney and small intestine was measured as well as the concentration of pro-inflammatory cytokines in the serum. The obesogenic diet increased the weight gain and fat accumulation of the animals compared to the Chow diet. Both Guarana and caffeine were unable to reverse weight gain and fat accumulation. We observed a lower activity of the Glutathione Peroxidase enzyme in the kidney and small intestine in the animals that received obesogenic diet compared to the Chow diet, regardless of the treatment. We also observed the decrease of Catalase enzyme activity in the kidney of animals that received Guarana, regardless of diet. The obesogenic diet induced changes in the intestinal microbiota similar to other works in literature, reducing the proportion of Bacteroidetes/Firmicutes (B/F), increasing the genus Mucispirilum and decreasing the genera Lactobacillus and Bifidobacterium. Guarana and caffeine treatments in the Chow diet decreased the B/F ratio, thus the Bifidobacterium genus. We observed an increase in the phylum Proteobacteria, in the animals of the Obese Control group. This increase in the phylum Proteobacteria, was reversed by the treatment with Guaraná. Analyzing the phylogenetic proximity charts and landscape, we observed a greater distance between the animals that received different diets than animals that received different treatments. Treatments with guarana or caffeine modified the intestinal ecosystem, but without the ability to decrease fat accumulation or weight gain. The major change in the microbiota was due to the obesogenic diet and not to the treatments, showing that the antiobese effects of guarana observed in other studies probably are not via intestinal microbiota

    Kratkotrajne promjene u mikrobioti usne šupljine pasa nakon žvakanja različitih vrsta autoklaviranih kostiju

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    The presence of dental calculus is one of the main issues associated with periodontitis in dogs. Mechanical removal of plaque and dental calculus can be performed through periodic oral prophylaxis conducted by veterinary dentists, and by continuous chewing of various items. Recent studies have demonstrated the effectiveness of bones as dental calculus agent removal in adult dogs. However, their effect regarding removal of oral microbiota remains unknown. The aim of the present study was to evaluate the effect of autoclaved spongy bone (SB) or compact bone (CB) supplementation on the oral microbiota of adult dogs with pre-existing dental calculus. The V4 region of the 16S rDNA gene was used for Illumina MiSeq next-generation sequencing. Transition was observed on the phyla proportion of the SB group, where the saliva sample initially presented a predominance of Bacteroidetes (51.3%) and Proteobacteria (33.0%), and changed to Proteobacteria (52.4%) and Bacteroidetes (33.9%). The gingival sulcus changed from Bacteroidetes (66.7%) and Proteobacteria (17.5%) prior to SB supplementation to Proteobacteria (76.3%) and Bacteroidetes (18.5%). No changes were observed in the proportion of saliva and gingival sulcus phyla in group CB. Moraxella sp. and Bergeyella zoohelcum increased in both saliva and gingival sulcus after SB supplementation. Saliva and gingival sulcus in the CB group showed increases in Porphyromonas species after 13 days’ supplementation. This study showed that chewing SB had a profound impact on both saliva and gingival sulcus microbiota, while CB did not cause substantial changes in the microbiota in either environment.Zubni kamenac među glavnim je uzrocima koji se povezuju s periodontitisom u pasa. Mehaničko uklanjanje plaka i zubnog kamenca može se provesti redovitom oralnom profilaksom kod veterinara stomatologa i kontinuiranim žvakanjem određenih predmeta. Najnovija istraživanja pokazuju učinkovitost kostiju pri uklanjanju zubnog kamenca u odraslih pasa. Način na koji se zubni kamenac pritom uklanja ostaje nepoznat. Cilj je ovoga rada bio istražiti učinak dodatka autoklaviranih spužvastih kostiju (SB) i čvrstih kostiju (CB) na oralnu mikrobiotu odraslih pasa sa zubnim kamencem. Za Illumina MiSeq sekvenciranje sljedeće generacije upotrijebljena je regija V4 gena 16S rDNA. Promatrana je promjena udjela pojedinih taksonomskih kategorija bakterija na razini phyla u skupini SB. U uzorcima sline inicijalno je utvrđena dominacija Bacteroidetes (51,3 %) i Proteobacteria (33,0 %) te promjene za Proteobacteria (52,4 %) i za Bacteroidetes (33,9 %). Zahvaljujući dodatku SB-a žlijeb desni promijenio je bakterijski sastav od Bacteroidetes (66,7 %) i Proteobacteria (17,5 %) na Proteobacteria (76,3 %) i Bacteroidetes (18,5 %). U skupini (CB) nisu uočene promjene u phyla kategorijama sline i žlijeba desni. Nakon dodavanja SB-a koncentracija bakterija Moraxella sp. i Bergeyella zoohelcum porasla je i u slini i u žlijebu desni. Slina i žlijeb desni u (CB) skupini pokazali su porast vrste Porphyromonas nakon 13 dana primjene. Ovo je istraživanje pokazalo da žvakanje spužvastih kosti znatno utječe na mikrobiotu i sline i žlijeba desni, dok u pasa koji su žvakali čvrste kosti bitnih promjena nije bilo

    Urinary bladder dysfunction in transgenic sickle cell disease mice

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    FAPESP - FUNDAÇÃO DE AMPARO À PESQUISA DO ESTADO DE SÃO PAULOCNPQ – CONSELHO NACIONAL DE DESENVOLVIMENTO CIENTÍFICO E TECNOLÓGICOBackground Urological complications associated with sickle cell disease (SCD), include nocturia, enuresis, urinary infections and urinary incontinence. However, scientific evidence to ascertain the underlying cause of the lower urinary tract symptoms in SCD is lacking. Objective Thus, the aim of this study was to evaluate urinary function, in vivo and ex vivo, in the Berkeley SCD murine model (SS). Methods Urine output was measured in metabolic cage for both wild type and SS mice (25-30 g). Bladder strips and urethra rings were dissected free and mounted in organ baths. In isolated detrusor smooth muscle (DSM), relaxant response to mirabegron and isoproterenol (1 nM-10 mu M) and contractile response to (carbachol (CCh; 1 nM-100 mu M), KCl (1 mM-300mM), CaCl2 (1 mu M-100mM), alpha,beta-methylene ATP (1, 3 and 10 mu M) and electrical field stimulation (EFS; 1-32 Hz) were measured. Phenylephrine (Phe; 10nM-100 mu M) was used to evaluate the contraction mechanism in the urethra rings. Cystometry and histomorphometry were also performed in the urinary bladder. Results SS mice present a reduced urine output and incapacity to produce typical bladder contractions and bladder emptying (ex vivo), compared to control animals. In DSM, relaxation in response to a selective beta 3-adrenergic agonist (mirabegron) and to a non-selective beta-adrenergic (isoproterenol) agonist were lower in SS mice. Additionally, carbachol, alpha,beta-methylene ATP, KCl, extracellular Ca2+ and electrical-field stimulation promoted smaller bladder contractions in SS group. Urethra contraction induced by phenylephrine was markedly reduced in SS mice. Histological analyses of SS mice bladder revealed severe structural abnormalities, such as reductions in detrusor thickness and bladder volume, and cell infiltration. Conclusions Taken together, our data demonstrate, for the first time, that SS mice display features of urinary bladder dysfunction, leading to impairment in urinary continence, which may have an important role in the pathogenesis of the enuresis and infections observed the SCD patients.Urological complications associated with sickle cell disease (SCD), include nocturia, enuresis, urinary infections and urinary incontinence. However, scientific evidence to ascertain the underlying cause of the lower urinary tract symptoms in SCD is lacking. Objective Thus, the aim of this study was to evaluate urinary function, in vivo and ex vivo, in the Berkeley SCD murine model (SS). Methods Urine output was measured in metabolic cage for both wild type and SS mice (25-30 g). Bladder strips and urethra rings were dissected free and mounted in organ baths. In isolated detrusor smooth muscle (DSM), relaxant response to mirabegron and isoproterenol (1 nM-10 mu M) and contractile response to (carbachol (CCh; 1 nM-100 mu M), KCl (1 mM-300mM), CaCl2 (1 mu M-100mM), alpha,beta-methylene ATP (1, 3 and 10 mu M) and electrical field stimulation (EFS; 1-32 Hz) were measured. Phenylephrine (Phe; 10nM-100 mu M) was used to evaluate the contraction mechanism in the urethra rings. Cystometry and histomorphometry were also performed in the urinary bladder. Results SS mice present a reduced urine output and incapacity to produce typical bladder contractions and bladder emptying (ex vivo), compared to control animals. In DSM, relaxation in response to a selective beta 3-adrenergic agonist (mirabegron) and to a non-selective beta-adrenergic (isoproterenol) agonist were lower in SS mice. Additionally, carbachol, alpha,beta-methylene ATP, KCl, extracellular Ca2+ and electrical-field stimulation promoted smaller bladder contractions in SS group. Urethra contraction induced by phenylephrine was markedly reduced in SS mice. Histological analyses of SS mice bladder revealed severe structural abnormalities, such as reductions in detrusor thickness and bladder volume, and cell infiltration. Conclusions Taken together, our data demonstrate, for the first time, that SS mice display features of urinary bladder dysfunction, leading to impairment in urinary continence, which may have an important role in the pathogenesis of the enuresis and infections observed the SCD patients108115FAPESP - FUNDAÇÃO DE AMPARO À PESQUISA DO ESTADO DE SÃO PAULOCNPQ – CONSELHO NACIONAL DE DESENVOLVIMENTO CIENTÍFICO E TECNOLÓGICOFAPESP - FUNDAÇÃO DE AMPARO À PESQUISA DO ESTADO DE SÃO PAULOCNPQ – CONSELHO NACIONAL DE DESENVOLVIMENTO CIENTÍFICO E TECNOLÓGICOFAPESP [2008/57441-0]CNPq [481761/2008-0]sem informaçãosem informaçã

    Neurobehavioral And Oxidative Stress Alterations Following Methylmercury And Retinyl Palmitate Co-Administration In Pregnant And Lactating Rats And Their Offspring

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    Fish consumption and ubiquitous methylmercury (MeHg) exposure represent a public health problem globally. Micronutrients presented in fish affects MeHg uptake/distribution. Vitamin A (VitA), another fish micronutrient is used in nutritional supplementation, especially during pregnancy. However, there is no information about the health effects arising from their combined exposure. The present study aimed to examine the effects of both MeHg and retinyl palmitate administered to pregnant and lactating rats. Thirty Wistar female rats were orally supplemented with MeHg (0,5 mg/Kg/day) and retinyl palmitate (7500 μg RAE1/Kg/day), either individually or in combination from the gestational day 0 to weaning. In dams, maternal behavior was scored. In neonatal and infant offspring, associative learning and neurodevelopment were evaluated. Further periadolescent male and female pups were assessed for open field, habituation and object recognition using episodic-like memory paradigm. Maternal and offspring redox parameters were evaluated. Our results showed no effects of MeHg-VitA co-administration in the quality of maternal care but showed subtle alterations in the pro-oxidant response of the hippocampus. In offspring, MeHg-VitA co-exposure affected early associative learning in neonatal pups, with no further modifications in neurodevelopment, and no locomotor or exploratory alterations in later developmental stages. Habituation was altered in a sex-dependent manner, but no overall memory disturbances were encountered

    Effects Of Methylmercury And Retinol Palmitate Co-Administration In Rats During Pregnancy And Breastfeeding: Metabolic And Redox Parameters In Dams And Their Offspring

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    Ubiquitous low-dose methylmercury (MeHg) exposure through an increased fish consumption represents a global public health problem, especially among pregnant women. A plethora of micronutrients presented in fish affects MeHg uptake/distribution, but limited data is available. Vitamin A (VitA), another fish micronutrient is used in nutritional supplementation, especially during pregnancy. However, there is no information about the health effects arising from their combined exposure. Therefore, the present study aimed to examine the effects of both MeHg and retinyl palmitate administered on pregnant and lactating rats in metabolic and redox parameters from dams and their offspring. Thirty Wistar female rats were orally supplemented with MeHg (0,5 mg/kg/day) and retinyl palmitate (7500 µg RAE/kg/day) via gavage, either individually or in combination from the gestational day 0 to weaning. For dams (150 days old) and their offspring (31 days old), glycogen accumulation (hepatic and cardiac) and retinoid contents (plasma and liver) were analyzed. Hg deposition in liver tissue was quantified. Redox parameters (liver, kidney, and heart) were evaluated for both animals. Cytogenetic damage was analyzed with micronucleus test. Our results showed no general toxic or metabolic alterations in dams and their offspring by MeHg-VitA co-administration during pregnancy and lactation. However, increased lipoperoxidation in maternal liver and a disrupted pro-oxidant response in the heart of male pups was encountered, with apparently no particular effects in the antioxidant response in female offspring. GST activity in dam kidney was altered leading to possible redox disruption of this tissue with no alterations in offspring. Finally, the genomic damage was exacerbated in both male and female pups. In conclusion, low-dose MeHg exposure and retinyl palmitate supplementation during gestation and lactation produced a potentiated pro-oxidant effect, which was tissue-specific. Although this is a pre-clinical approach, we recommend precaution for pregnant women regarding food consumption, and we encourage more epidemiological studies to assess possible modulations effects of MeHg-VitA co-administration at safe or inadvertently used doses in humans, which may be related to specific pathologies in mothers and their children

    Guarana supplementation attenuated obesity, insulin resistance, and adipokines dysregulation induced by a standardized human Western diet via brown adipose tissue activation

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    Obesity is a metabolic disorder associated with adverse health consequences that has increased worldwide at an epidemic rate. This has encouraged many people to utilize nonprescription herbal supplements for weight loss without knowledge of their safety or efficacy. However, mounting evidence has shown that some herbal supplements used for weight loss are associated with adverse effects. Guarana seed powder is a popular nonprescription dietary herb supplement marketed for weight loss, but no study has demonstrated its efficacy or safety when administered alone. Wistar rats were fed four different diets (low‐fat diet and Western diet with or without guarana supplementation) for 18 weeks. Metabolic parameters, gut microbiota changes, and toxicity were then characterized. Guarana seed powder supplementation prevented weight gain, insulin resistance, and adipokine dysregulation induced by Western diet compared with the control diet. Guarana induced brown adipose tissue expansion, mitochondrial biogenesis, uncoupling protein‐1 overexpression, AMPK activation, and minor changes in gut microbiota. Molecular docking suggested a direct activation of AMPK by four guarana compounds tested here. We propose that brown adipose tissue activation is one of the action mechanisms involved in guarana supplementation‐ induced weight loss and that direct AMPK activation may underlie this mechanism. In summary, guarana is an attractive potential therapeutic agent to treat obesity

    Effects of Achyrocline satureioides inflorescence extracts against pathogenic intestinal bacteria : chemical characterization, in vitro tests, and in vivo evaluation

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    Three Achyrocline satureioides (AS) inflorescences extracts were characterized: (i) a freeze-dried extract prepared fromthe aqueous extractive solution and (ii) a freeze-dried and (iii) a spray-dried extract prepared from hydroethanol extractive solution (80% ethanol).The chemical profile, antioxidant potential, and antimicrobial activity against intestinal pathogenic bacteria of AS extracts were evaluated. In vitro antioxidant activity was determined by the total reactive antioxidant potential (TRAP) assay. In vivo analysis and characterization of intestinal microbiota were performed in male Wistar rats (saline versus treated animals with AS dried extracts) by high-throughput sequencing analysis: metabarcoding. Antimicrobial activity was tested in vitro by the disc diffusion tests. Moisture content of the extracts ranged from 10 to 15% and 5.7 to 17mg kg−1 of fluorine. AS exhibited antioxidant activity, especially in its freeze-dried form which also exhibited a wide spectrum of antimicrobial activity against intestinal pathogenic bacteria greater than those observed by the antibiotic, amoxicillin, when tested against Bacillus cereus and Staphylococcus aureus. Antioxidant and antimicrobial activities of AS extracts seemed to be positively correlated with the present amount of flavonoids. These findings suggest a potential use of AS as a coadjuvant agent for treating bacterial-induced intestinal diseases with high rates of antibiotic resistance

    Intranasal HSP70 administration protects against dopaminergic denervation and modulates neuroinflammatory response in the 6-OHDA rat model

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    HSP70 is one of the main molecular chaperones involved in the cellular stress response. Besides its chaperone action, HSP70 also modulates the immune response. Increased susceptibility to toxic insults in intra- and extracellular environments has been associated with insufficient amounts of inducible HSP70 in adult neurons. On the other hand, exogenous HSP70 administration has demonstrated neuroprotective effects in experimental models of age-related disorders. In this regard, this study investigated the effects of exogenous HSP70 in an animal model of dopaminergic denervation of the nigrostriatal axis. After unilateral intrastriatal injection with 6-hydroxydopamine (6-OHDA), the animals received purified recombinant HSP70 through intranasal administration (2 μg/rat/day) for 15 days. Our results indicate a neuroprotective effect of intranasal HSP70 against dopaminergic denervation induced by 6-OHDA. Exogenous HSP70 improved motor impairment and reduced the loss of dopaminergic neurons caused by 6-OHDA. Moreover, HSP70 modulated neuroinflammatory response in the substantia nigra, an important event in Parkinson’s disease pathogenesis. Specifically, HSP70 treatment reduced microglial activation and astrogliosis induced by 6-OHDA, as well as IL-1β mRNA expression in this region. Also, recombinant HSP70 increased the protein content of HSP70 in the substantia nigra of rats that received 6-OHDA. These data suggest the neuroprotection of HSP70 against dopaminergic neurons damage after cellular stress. Finally, our results indicate that HSP70 neuroprotective action against 6-OHDA toxicity is related to inflammatory response modulation

    Effects of Achyrocline satureioides

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    Three Achyrocline satureioides (AS) inflorescences extracts were characterized: (i) a freeze-dried extract prepared from the aqueous extractive solution and (ii) a freeze-dried and (iii) a spray-dried extract prepared from hydroethanol extractive solution (80% ethanol). The chemical profile, antioxidant potential, and antimicrobial activity against intestinal pathogenic bacteria of AS extracts were evaluated. In vitro antioxidant activity was determined by the total reactive antioxidant potential (TRAP) assay. In vivo analysis and characterization of intestinal microbiota were performed in male Wistar rats (saline versus treated animals with AS dried extracts) by high-throughput sequencing analysis: metabarcoding. Antimicrobial activity was tested in vitro by the disc diffusion tests. Moisture content of the extracts ranged from 10 to 15% and 5.7 to 17 mg kg−1 of fluorine. AS exhibited antioxidant activity, especially in its freeze-dried form which also exhibited a wide spectrum of antimicrobial activity against intestinal pathogenic bacteria greater than those observed by the antibiotic, amoxicillin, when tested against Bacillus cereus and Staphylococcus aureus. Antioxidant and antimicrobial activities of AS extracts seemed to be positively correlated with the present amount of flavonoids. These findings suggest a potential use of AS as a coadjuvant agent for treating bacterial-induced intestinal diseases with high rates of antibiotic resistance
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