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Dive into the research topics where Sergio N. Kuriyama is active.

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Featured researches published by Sergio N. Kuriyama.


Environmental Health Perspectives | 2004

Developmental Exposure to Low-Dose PBDE-99: Effects on Male Fertility and Neurobehavior in Rat Offspring

Sergio N. Kuriyama; Chris E. Talsness; Konstanze Grote; Ibrahim Chahoud

In utero exposure to a single low dose of 2,2′,4,4′,5-pentabromodiphenyl ether (PBDE-99) disrupts neurobehavioral development and causes permanent effects on the rat male reproductive system apparent in adulthood. PBDEs, a class of flame retardants, are widely used in every sector of modern life to prevent fire. They are persistent in the environment, and increasing levels of PBDEs have been found in biota and human breast milk. In the present study we assessed the effects of developmental exposure to one of the most persistent PBDE congeners (PBDE-99) on juvenile basal motor activity levels and adult male reproductive health. Wistar rat dams were treated by gavage on gestation day 6 with a single low dose of 60 or 300 μg PBDE-99/kg body weight (bw). In offspring, basal locomotor activity was evaluated on postnatal days 36 and 71, and reproductive performance was assessed in males at adulthood. The exposure to low-dose PBDE-99 during development caused hyperactivity in the offspring at both time points and permanently impaired spermatogenesis by the means of reduced sperm and spermatid counts. The doses used in this study (60 and 300 μg/kg bw) are relevant to human exposure levels, being approximately 6 and 29 times, respectively, higher than the highest level reported in human breast adipose tissue. This is the lowest dose of PBDE reported to date to have an in vivo toxic effect in rodents and supports the premise that low-dose studies should be encouraged for hazard identification of persistent environmental pollutants.


Environmental Health Perspectives | 2007

In Utero and Lactational Exposures to Low Doses of Polybrominated Diphenyl Ether-47 Alter the Reproductive System and Thyroid Gland of Female Rat Offspring

Chris E. Talsness; Sergio N. Kuriyama; Anja Sterner-Kock; Petra Schnitker; Simone Wichert Grande; Mehdi Shakibaei; Anderson J.M. Andrade; Konstanze Grote; Ibrahim Chahoud

Background Polybrominated diphenyl ethers (PBDEs) are capable of disrupting thyroid hormone homeostasis. PBDE-47 (2,2′,4,4′-tetrabromodiphenyl ether) is one of the most abundant congeners found in human breast adipose tissue and maternal milk samples. Objectives We evaluated the effects of developmental exposure to low doses of PBDE-47 on the female reproductive system. Methods Pregnant Wistar rats were administered vehicle (peanut oil) or PBDE-47 [140 or 700 μg/kg body weight (bw)] on gestation day (GD) 6, or 5 mg 6-n-propyl-2-thiouracil (PTU)/L in the drinking water from GD7 through postnatal day (PND) 21. Results In female offspring sacrificed on PND38, there was a significant decrease in ovarian weight after exposure to PTU or 140 μg/kg PBDE-47. Alterations in folliculogenesis were apparent: we observed a decrease in tertiary follicles and serum estradiol concentrations in the offspring exposed to either PTU or 700 μg/kg PBDE-47. PTU exposure also resulted in a decrease in primordial follicles. On PND100, persistent effects on the thyroid glands included histologic and morphometric changes after exposure to either PTU or PBDE-47. No relevant changes in reproductive indices were observed after mating the exposed F1 females with nontreated males. Conclusions Administration of PBDE-47 at doses relevant to human exposure led to changes in the rat female reproductive system and thyroid gland.


Toxicology Letters | 2003

Inhibition of cyclophosphamide-induced teratogenesis by β-ionone

Maria Regina Gomes-Carneiro; Ana C.A.X. De-Oliveira; Rosangela R. De-Carvalho; I.B. Araujo; C.A.M. Souza; Sergio N. Kuriyama; Francisco José Roma Paumgartten

β-Ionone (BI) is a degraded (C 13) sesquiterpene found in plant essential oils. It has been used in the synthesis of perfume chemicals and vitamin A. Recently, it was reported that BI is a rather potent in vitro inhibitor of CYP2B1-catalysed reactions in rat liver microsomes. The present study was performed to investigate whether inhibition of CYP2B1 reactions by BI could lead to an attenuation of cyclophosphamide (CP)-induced embryotoxicity in the rat. In a preliminary experiment, a dose-dependent prolongation of pentobarbital sleeping time in male and female Wistar rats suggested that BI inhibits CYP2B1 in vivo as well. In a second experiment, rats were treated by gavage with BI (0, 250, 500, 750 or 1000 mg/kg body wt) 45 min prior to a subcutaneous injection of either CP (7.5 mg/kg body wt) or its vehicle (saline) on day 11 of pregnancy. BI alone, at the highest dose tested, caused a high proportion of resorptions. Lower doses of BI, however, clearly attenuated CP-induced embryolethality and teratogenicity. These results seem to support the view that, as far as rats are concerned, CYP2B1 plays an important role in the conversion of CP into its embryolethal and teratogenic metabolites.


Toxicology | 2002

Maternal protein-and-energy restriction reduces the developmental toxicity of cyclophosphamide and hydroxyurea in rats

Ibrahim Chahoud; Sergio N. Kuriyama; Francisco José Roma Paumgartten

In this study, we examined the relationship between maternal weight gain deficits induced by protein-and-energy restriction (PER) and pregnancy outcome. We also evaluated whether PER would potentiate the developmental toxicity of cyclophosphamide (CP) and hydroxyurea (HU). Two independent experiments--employing two different methods of inducing protein-and-energy malnourishment-were performed. In the first experiment, well-nourished (fed ad libitum, normal diet, 22% of protein, 11.9 kJ/g) and food restricted (fed approximately half of ad libitum food intake, i.e. 12 g/day) rats received CP (0, 5 and 7.5 mg/kg sc) on pregnancy day 11. In the second experiment, well-nourished (normal diet, 24% of protein, 12.4 kJ/g) and malnourished (protein-and-energy deficient diet, 8% of protein, 6.2 kJ/g) rats received HU (0, 300 and 500 mg/kg ip) on pregnancy day 11. PER alone caused pronounced reductions of pregnancy weight gain and low fetal body weight, but induce no embryolethality and, except for a few sternum anomalies, no malformation. PER attenuated embryolethal and teratogenic effects of CP. PER reduced teratogenicity but did not alter effects of HU on embryolethality and fetal body weight. Therefore severe maternal weight gain deficits are not necessarily associated to embryolethality and terata and PER attenuates the teratogenic effects of CP and HU.


Toxicology Letters | 2003

Absence of tumor promoting activity of Euphorbia milii latex on the mouse back skin.

I.F Delgado; Rosangela R. De-Carvalho; Ana C.A.X. De-Oliveira; Sergio N. Kuriyama; E.C Oliveira-Filho; C.A.M. Souza; Francisco José Roma Paumgartten

Euphorbia milii (Euphorbiaceae) is a decorative plant used in gardens and living fences. In China, it has also been employed in herbal remedies for hepatitis and abdominal edema. Since E. milii latex--lyophilized or in natura--proved to be a potent plant molluscicide, its toxicity to non-target organisms has been comprehensively studied. Concerns on a possible tumor promoting activity have discouraged its use as a locally-available alternative molluscicide in schistosomiasis control programs. Two in vitro assays (inhibition of metabolic cooperation in V79 cells and Epstein-Barr virus induction in Raji cells) had suggested that E. milii latex contained tumor-promoting substances. This study was undertaken to verify whether the latex acts as a tumor promoter in vivo as well. A single dose of the initiating agent DMBA (400 nmol) was applied on the back skin of male and female DBA/2 mice. Testing for tumor promoting activity began 10 days after initiation. Tetradecanoyl phorbol acetate (TPA) (5 nmol, positive control), lyophilized latex (20, 60 and 200 microg per mouse) or acetone (vehicle control) were applied on mouse back skin twice a week for 20 weeks. In TPA-treated mice, papillomas were firstly noted during the 11th week, and by the 17th week all animals exhibited skin tumors. No tumors developed in mice treated with the solvent alone and in those exposed to latex. Findings from the present study therefore indicated that E. milii crude latex does not act as a tumor promoting agent on the mouse back skin assay.


Reproductive Toxicology | 2016

Thyroid hormone disruption and cognitive impairment in rats exposed to PBDE during postnatal development.

Andressa S. de-Miranda; Sergio N. Kuriyama; Camille S. da-Silva; Monicke S.C. do-Nascimento; Thiago E. Parente; Francisco José Roma Paumgartten

Polybrominated diphenyl ether flame-retardants (PBDEs) are thyroid-disrupting environmental chemicals. We investigated the effects of postnatal exposure to DE-71 (a mixture of tetra- and penta-brominated congeners), n-propylthiouracil (PTU) and thyroxine (T4) replacement on open-field (OF) and radial maze (RAM) tests. Wistar rats (5 males/5 females per litter, 32 litters) were treated orally (PND 5-22) with PTU (4mg/kg bw/d), DE-71 (30mg/kg bw/d), with and without co-administration of T4 (15μg/kg bw/d, sc). PTU depressed T4 serum levels and body weight gain and enlarged thyroid gland. Although decreasing T4 levels, DE-71 did not change thyroid and body weights. PTU-treated rats showed hyperactivity (PND 42 and 70), and working and reference memory learning deficits (RAM, PND 100). Although not altering motor activity and working memory, DE-71 caused a reference memory deficit (females only). T4 co-administration averted hypothyroxinemia and long-term cognitive deficits caused by PTU and DE-71.


Brazilian Journal of Medical and Biological Research | 2000

Effects of pregnancy and protein-energy malnutrition on monooxygenase O-dealkylation activity in rat liver microsomes

Sergio N. Kuriyama; Ana C.A.X. De-Oliveira; Antonio Augusto Fidalgo-Neto; Francisco José Roma Paumgartten

Xenobiotic metabolism is influenced by a variety of physiological and environmental factors including pregnancy and nutritional status of the individual. Pregnancy has generally been reported to cause a depression of hepatic monooxygenase activities. Low-protein diets and protein-energy malnutrition have also been associated with a reduced activity of monooxygenases in nonpregnant animals. We investigated the combined effects of pregnancy and protein-energy malnutrition on liver monooxygenase O-dealkylation activity. On pregnancy day 0 rats were assigned at random to a group fed ad libitum (well-nourished, WN) or to a malnourished group (MN) which received half of the WN food intake (12 g/day). WN and MN rats were killed on days 0 (nonpregnant), 11 or 20 of pregnancy and ethoxy- (EROD), methoxy- (MROD) and penthoxy- (PROD) resorufin O-dealkylation activities were measured in liver microsomes. Only minor changes in enzyme activities were observed on pregnancy day 11, but a clear-cut reduction of monooxygenase activities (pmol resorufin min-1 mg protein-1) was noted near term (day 0 vs 20, means +/- SD, Student t-test, P<0.05) in WN (EROD: 78.9 +/- 15.1 vs 54.6 +/- 10.2; MROD: 67.8 +/- 10.0 vs 40.9 +/- 7.2; PROD: 6.6 +/- 0. 9 vs 4.3 +/- 0.8) and in MN (EROD: 89.2 +/- 23.9 vs 46.9 +/- 15.0; MROD: 66.8 +/- 13.8 vs 27.9 +/- 4.4; PROD: 6.3 +/- 1.0 vs 4.1 +/- 0. 6) dams. On pregnancy day 20 MROD was lower in MN than in WN dams. Malnutrition did not increase the pregnancy-induced reduction of EROD and PROD activities. Thus, the present results suggest that the activities of liver monooxygenases are reduced in near-term pregnancy and that protein-energy malnutrition does not alter EROD or PROD in pregnant rats.


Ensaios e Ciência: Ciências Biológicas, Agrárias e da Saúde | 2013

PERFIL CRONOBIOLÓGICO DOS PROFISSIONAIS DE ENFERMAGEM OFFSHORE

Victor Marcos Figueiredo; Sergio N. Kuriyama; Rafael Tubino; Antonio Augusto Fidalgo-Neto

De modo geral um metodo analitico deve, idealmente, ser exato para fornecer valor real, ser preciso para fornecer, com menor numero de ensaios, este valor real, ser seletivo para que a exatidao nao se desvie com interferentes potencias, ser sensivel ou capaz de determinar as menores concentracoes possiveis e responder de forma proporcional linear. A validacao tem por intuito assegurar que o metodo analitico que sera utilizado posteriormente para quantificacao de determinado principio ativo. Como principio ativo de referencia, sera utilizada a Fluoxetina Cloridrato e o antidepressivo mais utilizado no mundo, comercialmente conhecido como Prozac. Assim, este estudo tem o objetivo de validar uma metodologia para quantificar este composto tendo como ferramenta a espectrofotometria baseada na interacao entre energia eletromagnetica e materia.


Organohalogen compounds | 2003

Ultrastructural changes in the ovaries of adult offspring following a single maternal exposure to low dose 2,2', 4, 4', 5-pentabromodiphenyl ether

Chris E. Talsness; Mehdi Shakibaei; Sergio N. Kuriyama; Cristina de Souza; Ibrahim Chahoud


Toxicology Letters | 2003

653 EROD, UDPGT activity and thyroid hormone level after in utero exposure to a low dose of 2,2′,4,4′,5-penta-BDE (PBDE 99) in rat offspring

Ibrahim Chahoud; Sergio N. Kuriyama; A.A. Fidalgo-Neto; W. Wittfoht

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C.A.M. Souza

Oswaldo Cruz Foundation

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