V. A. Da-Silva scite author profile

Postnatal depression is a significant problem affecting 10-15% of mothers in many countries and has been the subject of an increasing number of publications. Prenatal depression has been studied less. The aims of the present investigation were: 1) to obtain information on the prevalence of prenatal and postnatal depression in low income Brazilian women by using an instrument already employed in several countries, i.e., the Edinburgh Postnatal Depression Scale (EPDS); 2) to evaluate the risk factors involved in prenatal and postnatal depression in Brazil. The study groups included 33 pregnant women interviewed at home during the second and third trimesters of pregnancy, and once a month during the first six months after delivery. Questions on life events and the mother's relationship with the baby were posed during each visit. Depressed pregnant women received less support from their partners than non-depressed pregnant women (36.4 vs 72.2%, P<0.05; Fisher exact test). Black women predominated among pre-and postnatally depressed subjects. Postnatal depression was associated with lower parity (0.4 ± 0.5 vs 1.1 ± 1.0, P<0.05; Student ttest). Thus, the period of pregnancy may be susceptible to socioenvironmental factors that induce depression, such as the lack of affective support from the partner. The prevalence rate of 12% observed for depression in the third month postpartum is comparable to that of studies from other countries.

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Postnatal development of rats exposed to fluoxetine or venlafaxine during the third week of pregnancy

Da-Silva

Altenburg

Malheiros

et al. 1999

Braz J Med Biol Res

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The aim of the present study was to compare the toxic effects of fluoxetine (F) (8 and 16 mg/kg) and venlafaxine (V) (40 and 80 mg/kg) administered during the third week of pregnancy on early development of rats. Both antidepressants were administered by gavage on pregnancy days 15 to 20 to groups of 10 to 12 animals each. Duration of gestation, food and water consumption, number of live pups and birth weight were recorded. Litters were culled to six pups at birth (day 1) and followed for growth until weaning (day 25). On day 60, a male and a female from each litter were injected with the 5-HT 1 agonist, 5-methoxy-N,N-dimethyltryptamine (6 mg/kg, ip) and the serotonergic syndrome was graded. Fluoxetine but not venlafaxine reduced the duration of pregnancy when compared to the control (C) group (F = 21.1 days and C = 21.6 days, mean, P<0.02; maximum = 22 days and minimum = 21 days in both groups). The highest doses of both fluoxetine, 16 mg/kg (F16), and venlafaxine, 80 mg/kg (V80), reduced the food intake of pregnant rats, resulting in different rates of body weight gain during treatment (from pregnancy day 15 to day 20): F16 = 29.0 g, V80 = 28.7 g vs C = 39.5 g (median). Birth weight was influenced by treatment and sex (P<0.05; two-way ANOVA). Both doses of fluoxetine or venlafaxine reduced the body weight of litters; however, the body weight of litters from treated dams was equal to the weight of control litters by the time of weaning. At weaning there was no significant difference in weight between sexes. There was no difference among groups in number of live pups at birth, stillbirths, mortality during the lactation period or in the manifestation of serotonergic syndrome in adult rats. The occurrence of low birth weight among pups born to dams which did not show reduced food ingestion or reduction of body weight gain during treatment with lower doses of fluoxetine or venlafaxine suggests that these drugs may have a deleterious effect on prenatal development when administered during pregnancy. In addition, fluoxetine slightly but significantly affected the duration of pregnancy (about half a day), an effect not observed in the venlafaxine-treated groups.

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Can calories from ethanol contribute to body weight preservation by malnourished rats?

Aguiar

Da-Silva

Boaventura

2004

Braz J Med Biol Res

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Our objective was to compare the use of calories from ethanol by wellnourished and malnourished rats in terms of body weight. Female Wistar rats weighing 170-180 g at the beginning of the study were used. The animals were divided into two groups (N = 12 each): group W received water ad libitum and group E an ethanol solution ad libitum as the only source of liquid throughout the experiment. The concentration of ethanol was increased weekly from 0 to 5, 10, 20 and 40% (v/v). In the well-nourished phase (A), all rats received food ad libitum (AW and AE). Ethanol treatment (AE) was then interrupted and water was offered to both groups. After 2 weeks both AW and AE rats were submitted to food restriction (50% of group AW food consumption), thus initiating the malnutrition phase (M). Liquid was offered as described before to the same W (MW) and E (ME) groups. The weight gain during the 1-week treatment of AE rats was similar to that of AW animals only when AE rats received the 5% (v/v) ethanol solution (9.16 vs 10.47 g). Weight loss was observed after exposure to 10% ethanol (P < 0.05) in spite of maintenance of caloric intake. Malnourished rats presented weight loss, which was attenuated by ethanol intake up to the 20% (v/v) solution and was related to an increased caloric offer. This effect was not observed with the 40% ethanol solution (-9.98 g). These data suggest that calories from ethanol were used to maintain body weight up to the concentration of 10% (v/v) (well-nourished) and 20% (v/v) (malnourished) and that ethanol has a toxic profile which depends on nutritional status.

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The role of forced swim test on neutrophil leukocytosis observed during inflammation induced by LPS in rodents

Altenburg

Ventura

Da-Silva

et al. 2002

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Behavioral toxicity of increasing doses of ethanol in malnourished rats

Aguiar

Boaventura

Malheiros

et al. 2006

Nutritional Neuroscience

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In order to verify the toxicity of ethanol in malnourished rats, the following procedure was applied to two groups of rats (n = 12 each): group W: drinking water ad libitum and group E: drinking only an ethanol solution in a gradual dosage (0, 5, 10, 20 and 40% v/v). In the well-nourished phase, all rats received food ad libitum (AW and AE). Ethanol treatment (AE) was interrupted for two weeks. Rats from both AW and AE groups were submitted to food restriction (50% of AW consumption)--malnourished phase (M)--and liquid was offered as described before. Signs of ethanol intoxication were recorded daily. Ethanol withdrawal symptoms and the open-field test were performed 24 h after the well-nourished and malnourished phases. Rats were sacrificed for macroscopic evaluation of liver, spleen, thymus and biochemical analyses of the blood (hematocrit, hemoglobin, proteins and albumin). Malnourished rats showed more signs of ethanol intoxication and withdrawal. In the open-field test, malnourished rats ambulated more and made more rearing up. This effect of malnutrition was not observed during ethanol withdrawal. Consumption of ethanol decreased the levels of hemoglobin, hematocrit and total proteins. Data suggested that toxic profile of ethanol was dependent on nutritional status.

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V. A. Da-Silva

Prenatal and postnatal depression among low income Brazilian women

Postnatal development of rats exposed to fluoxetine or venlafaxine during the third week of pregnancy

Can calories from ethanol contribute to body weight preservation by malnourished rats?

The role of forced swim test on neutrophil leukocytosis observed during inflammation induced by LPS in rodents

Behavioral toxicity of increasing doses of ethanol in malnourished rats

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