Short and long-term effects of bisphenol S (BPS) exposure during pregnancy and lactation on plasma lipids, hormones, and behavior in rats.

Bisphenol S (BPS) has replaced bisphenol A (BPA), a known non-persistent endocrine disrupting chemical, in several products. Considering that little is known regarding BPS effects, especially during critical windows of ontogenetic development, and that BPA, which is quite similar to BPS, is know to be transferred to the offspring via the placenta and milk, in the present study we investigated the behavioral, biochemical and endocrine profiles of Wistar rats born from dams that were BPS-exposed [groups: BPS10 (10 µg/kg/day), BPS50 (50 µg/kg/day)] during pregnancy and lactation. Due to the non-monotonic dose-response effect of bisphenol, the data of both BPS groups were directly compared with those of the controls, not to each other. Males and females were analyzed separately. At weaning, male BPS50 offspring had hypotriglyceridemia and hyperthyroxinemia, whereas BPS50 females showed higher 25(OH)D levels. At adulthood, BPS offspring of both sexes had lower food intake. BPS males showed lower visceral adiposity. BPS50 females had smaller fat droplets in brown adipocytes. BPS males showed higher anxiety and higher locomotor activity, while BPS10 females showed lower exploration. During a food challenge test at adulthood, BPS males consumed more high-fat diet at 30 min. BPS10 females initially (at 30 min) consumed more high-fat diet but, after 12 h, less of this diet was consumed. BPS50 males had hypertriglyceridemia and lower plasma T3, while BPS females showed lower plasma T4. BPS10 females had lower progesterone, whereas BPS50 females had higher plasma 25(OH)D. Maternal BPS exposure has adverse effects on the triacylglycerol, hormones levels and behavior of the progeny. Furthermore, the increased preference for the fat-enriched diet suggests an increased risk for obesity and its health consequences in the long term.

The phytoecdysteroid ß-ecdysone is genotoxic in Rodent Bone Marrow Micronuclei and Allium cepa L. Assays.

ETHNAOPHARMACOLOGIAL RELEVANCE: In South America, the ß-ecdysone ecdysteroid has been found in species of the genus Pfaffia Mart. Due to the similar morphology of its roots to the Panax ginseng C. A. Mey. (Korean ginseng), some species of this genus has been known as Brazilian ginseng and have been used as tonic and aphrodisiac, as well as for the treatment of diabetes and rheumatism. AIM OF THE STUDY: Here we report a cytogenotoxic evaluation of ß-ecdysone (a natural ecdysteroid found in plants) in Rodent Bone Marrow Micronuclei and Allium cepa Assays. MATERIALS AND METHODS: Three ß-ecdysone (pure) concentrations (based in human therapeutic dosage) were used in the Micronucleus Assay. The animals were treated during two consecutive days. Micronucleated cells were counted in 2000 polychromatic erythrocytes per animal. For A. cepa L. Assay, one ß-ecdysone concentration was analyzed. The onions bulbs were exposed for 24h. RESULTS: The Micronucleus Assay showed genotoxic effects for all treatments, expressed by an increase of micronucleated cells. In A. cepa L. Assay, cell abnormalities associated to the malfunction/non-formation of mitotic spindle (aneugenic effect) and chromosomal bridges (clastogenic effect) were observed. CONCLUSIONS: The results indicate a cytogenotoxic activity of ß-ecdysone. Therefore, the popular use of Pfaffia and others species containing ß-ecdysone should be considered with caution.

Efficacy of Morus nigra L. on reproduction in female Wistar rats.

Morus nigra L. is a plant employed as a substitute for the conventional hormonal replacement therapy. This work analyzes the estrogenic effect of M. nigra on the reproductive system and embryonic development of Wistar rats. Female rats were orally treated with M. nigra hydroalcoholic extract (MnHE) at the dose levels of 25, 50, 75, 350 and 700 mg/kg of body weight over 15 days, and continued through mating until the 14th day of gestation. Vaginal smears were performed daily and the body weight of the females was recorded at 5 days intervals. On day 15 of gestation, the females were killed and their kidneys, liver, spleen and ovaries were removed and weighed. The number of implants, resorptions, and live and dead fetuses were evaluated. Histological sections of ovaries, measurement of the height of the uterine epithelium and vaginal smears were performed to assess the estrogenic activity. The results showed that the administration of MnHE did not significantly alter the analyzed variables. Therefore, considering the experimental model used in this study, the data obtained indicate that M. nigra did not exhibit any estrogenic activity nor did exert a toxic effect on the female reproductive system and on the embryonic development of rats.

Avaliação do potencial interceptivo da ipriflavona em ratas wist / Evaluation of the potential of interceptive ipriflavone in wistar rats

A ipriflavona possui efeito inibitório sobre o citocromo p450 e sobre a proliferação do DNA, interferindo na síntese de hormônios estereoidianos, e consequente interferência no transporte e desenvolvimento pré-implantacional e na implantação do blastocisto. Consumidos em altas doses pode acarretar abortamentos e malformações. Para verificar a embriotoxicidade da ipriflavona durante as fases de transporte tubário e implantação do blastocisto de ratas, ratas Wistar prenhes foram tratadas duas vezes ao dia com 1mL de suspensão aquosa de ipriflavona, nas doses de 0 (C), 300 (T1), 1500 (T2) e 3000 (T3) mg/kg/dose, durante os oito primeiros dias de prenhez com eutanásia no 14o dia. Indícios de toxicidade foram avaliados por análises hematimétricas, bioquímicas e comportamentais. Foram contados fetos vivos, mortos e reabsorvidos (inicial e tardiamente). Os animais não apresentaram sinais clínicos de toxicidade. Índice de implantação e perdas pré-embrionária sofreram interferência do uso da ipriflavona. Dados apontam para um efeito estrogênico da ipriflavona, observados na interferência da implantação do blastocisto de ratas Wistar.

Ipriflavone has inhibitory effect on the cytochrome p450 and the proliferation of DNA, interfering with hormone synthesis estereoidianos, and consequent interference with the transport and preimplantation development and implantation of the blastocyst. Consumed in high doses can cause miscarriages and malformations. To verify the embryotoxicity of ipriflavone during the phases of tubal transport and implantation of the blastocyst in rats, Wistar rats were treated twice daily with 1 mL of aqueous suspension of ipriflavone at doses of 0 (C), 300 (T1), 1500 (T2) and 3000 (T3) mg / kg / dose during the first eight days of pregnancy with euthanasia on day 14. Signs of toxicity were characterized by hematological, biochemical and behavioral. Live fetuses were counted, dead and resorbed (early and late). The animals showed no clinical signs of toxicity. Index pre-implantation embryo and losses suffered interference from the use of ipriflavone. Data point to an estrogenic effect of ipriflavone, due to interference in blastocyst implantation in Wistar rats.