Melatonina materna e aspectos da função reprodutiva da prole adulta

Abstract

Melatonin is the marker of the dark phase of the circadian cycle. The fetus and the newborn exclusively receive melatonin from the mother. Therefore, the lack of maternal melatonin can misalign the biological clock with the light-dark (LD) cycles, leading to impairments in fetal programming. This study evaluated the role of maternal melatonin on some aspects of the hypothalamic-pituitary-gonadal (HPG) axis function in adult offspring. To do so, adult male and female rats born to pinealectomized (PINX) mothers, PINX mothers treated with melatonin during gestation and lactation (PINX-MEL), and control rats were studied in adulthood (2 months of age). In females, the estrous cycle, uterine weight, and plasma luteinizing hormone (LH) levels were analyzed. In males, testicular weight, seminal vesicle weight, epididymis weight, gonadosomatic index, and plasma LH and testosterone levels were analyzed. We observed that the proestrus frequency was lower in PINX and PINX-MEL rats compared to control rats. The estrus frequency was higher in PINX rats compared to control rats. On the other hand, the diestrus frequency was lower in the PINX group compared to the control group. The results showed irregularities in the estrous cycle in the PINX group, which were not reversed by melatonin treatment. Regarding female LH, there was no statistical difference between the groups. However, the high dispersion in plasma LH concentrations found in the offspring of PINX and PINX-MEL mothers suggested that the preovulatory LH peak may have occurred at different times of the day in these groups. As for males, we observed a reduction in LH concentrations in the offspring of PINX and PINX-MEL mothers compared to the offspring of control mothers. On the other hand, male PINX offspring showed a tendency of increased blood testosterone levels compared to control offspring. Concerning Leydig cells, PINX males exhibited larger cellular and cytoplasmic volumes than control males, indicating a potential alteration in steroidogenesis. In parallel, PINX males had a reduced number of Leydig cells compared to control males, which could be a consequence of the reduced LH values found in this group. Melatonin treatment reduced cellular and cytoplasmic volumes compared to control and PINX males. Furthermore, melatonin supplementation partially restored the number of Leydig cells. Taken together, the results suggest that maternal PINX induces alterations in the development of the hypothalamic-pituitarygonadal axis in females and males, which have repercussions on the estrous cycle and LH secretion in females, as well as testicular morphology, LH secretion, and testosterone levels in males.