A1 adenosine receptors play an essential role in protecting the embryo against hypoxia

摘要

Embryos can be exposed to environmental factors that induce hypoxia. Currently, our understanding of the effects of hypoxia on early mammalian development is modest. Potential mediators of hypoxia action include the nucleoside adenosine, which acts through A_1 adenosine receptors (A_1ARs) and mediates adverse effects of hypoxia on the neonatal brain. We hypothesized that A_1ARs may also play a role in mediating effects of hypoxia on the embryo. When pregnant dams were exposed to hypoxia (10% O_2) beginning at embryonic day (E) 7.5 or 8.5 and continued for 24-96 h, A_1AR+/+ embryos manifested growth inhibition and a disproportionate reduction in heart size, including thinner ventricular walls. Yet, when dams were exposed to hypoxia, embryos lacking A_1ARs (A_1AR-/-) had much more severe growth retardation than A_1AR+/+ or +/- embryos. When levels of hypoxia-inducible factor 1α (HIF1α) were examined, A_1AR-/- embryos had less stabilized HIF1α protein than A_1AR+/- littermates. Normal patterns of cardiac gene expression were also disturbed in A_1AR-/-embryos exposed to hypoxia. These results show that short periods of hypoxia during early embryogenesis can result in intrauter-ine growth retardation. We identify adenosine and A_1ARs as playing an essential role in protecting the embryo from hypoxia.