Developmental Exposure of Mice to Dioxin Promotes Transgenerational Testicular Inflammation and an Increased Risk of Preterm Birth in Unexposed Mating Partners

Exposure to Tetrachlorodibenzo-p-dioxin (TCDD) in male rats promotes, decreased sperm concentration, alterations in motility and in sperm transit time. We evaluated the effect transgenerational of in utero exposure to low doses TCDD in the sperm quality. Pregnant rats (F0) were exposed to 0.1; 0.5 and 1.0μg of TCDD, on gestational day 15, coincides with the end of most organogenesis in the fetus. Adult male offspring (F1, F2 and F3 generation) were investigated for fertility after artificial insemination in utero. After collection of the uterus and ovaries, the numbers of corpora lutea and implants were determined. TCDD provoked alterations in sperm morphology and diminution in serum testosterone levels and sperm transit time in the cauda epididymis. The fertility significantly decreased in all the generations, at least at one dose. In conclusion, TCDD exposure decreases rat sperm quality and fertility in adult male offspring and this effects persist into the next generation.

Section: Discussionsupporting

confidence: 92%

Section: Discussionsupporting

confidence: 91%

Sperm quality and fertility in rats after prenatal exposure to low doses of TCDD: A three-generation study

Sanabria

Cucielo

Guerra

et al. 2016

“…In another transgenerational study performed by another research group, exposure of pregnant mice to 10 [H9262]g/kg TCDD by gavage on gestation day 15.5 resulted in decrease in fertility and bias to preterm birth [83]: about 50% of F1–F3 males were sterile, 33–38% that were able to impregnate their mating female showed spontaneous delivery prior to E19.0. In all three generations of treated male mice there were signs of testicular inflammation and increased apoptosis of germ cells.…”

Section: Transgenerational Effects In Animal Experimentsmentioning

confidence: 99%

Spermatogenesis disruption by dioxins: Epigenetic reprograming and windows of susceptibility

Pilsner

Parker

Sergeyev

et al. 2017

Dioxins are a group of highly persistent chemicals that are generated as by-products of industrial and natural processes. Reduction in sperm counts is among the most sensitive endpoints of dioxin toxicity. The exact mechanism by which dioxins reduce sperm counts is not known. Recent data implicate the role of epididymal factors rather than disruption of spermatogenesis. Studies reviewed here demonstrate that dioxins induce the transfer of environmental conditions to the next generation via male germline following exposures during the window of epigenetic reprogramming of primordial germ cells. Increased incidence of birth defects in offspring of male veterans exposed to dioxin containing, Agent Orange, suggest that dioxins may induce epigenomic changes in male germ cells of adults during spermatogenesis. This is supported by recent animal data that show that environmental conditions can cause epigenetic dysregulation in sperm in the context of specific windows of epigenetic reprogramming during spermatogenesis.

“…At 10-12 weeks, F2 females were mated to control males of similar age and monitored as above. Note: As previously described, like their siblings, F1 and F2 males exhibit subfertility [11, 157]. Perhaps as a consequence of reduced fertility in directly exposed animals, to date, mating of non-sibling F1 male and female mice or non-sibling F2 male and female mice has not resulted in offspring [103]; thus, toxicant exposed mice are necessarily mated to control partners.…”

Section: Methodsmentioning

confidence: 99%

Exposure to the environmental endocrine disruptor TCDD and human reproductive dysfunction: Translating lessons from murine models

Bruner‐Tran

Gnecco

Ding

et al. 2017

Self Cite

Humans and other animals are exposed to a wide array of man-made toxicants, many of which act as endocrine disruptors that exhibit differential effects across the lifespan. In humans, while the impact of adult exposure is known for some compounds, the potential consequences of developmental exposure to endocrine disrupting chemicals (EDCs) is more difficult to ascertain. Animal studies have revealed that exposure to EDCs prior to puberty can lead to adult reproductive disease and dysfunction. Specifically, in adult female mice with an early life exposure to 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD), we demonstrated a transgenerational occurrence of several reproductive diseases that have been linked to endometriosis in women. Herein, we review the evidence for TCDD-associated development of adult reproductive disease as well as known epigenetic alterations associated with TCDD and/or endometriosis. We will also introduce new “Organ-on-Chip” models which, combined with our established murine model, are expected to further enhance our ability to examine alterations in gene-environment interactions that lead to heritable disease.