Chronic moderate hypoxia during in ovo development alters arterial reactivity in chickens

Ruijtenbeek, K.; Kessels, Carolina G. A.; Janssen, Ben J. A.; Bitsch, Nicole; Fazzi, Gregorio E.; Janssen, G. M. E.; Mey, Jo G. R. De; Blanco, Carlos E.

doi:10.1007/s00424-003-1170-4

Cited by 35 publications

(48 citation statements)

References 41 publications

(59 reference statements)

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“…However, data in the present study show that in vivo assessment in adult offspring from hypoxic pregnancy provides no evidence of either an increase in peripheral vascular resistance or systemic hypertension. This finding is corroborated by further evidence of no hypertension in highland residents, 40 neonatal sheep from high altitude pregnancy, 35 adult chickens subjected to hypoxia in ovo, 32 or adult rats following prenatal hypoxia. 37, 41 Despite no evidence of any changes in basal arterial blood pressure, this study revealed significant programming on the autonomic control of arterial blood pressure in adult offspring Values are mean ± SEM for baroreflex function in 4-month-old male offspring from Normoxic (N; n=8), Hypoxic (H; n=9), Hypoxic+Vitamin C (HC; n=7) and Normoxic+Vitamin C (NC; n=7) pregnancies.…”

Section: Discussionmentioning

confidence: 54%

Vitamin C Prevents Intrauterine Programming of in vivo Cardiovascular Dysfunction in the Rat

Kane

Herrera

Camm

et al. 2013

Circ J

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Background: Fetal hypoxia is common and in vitro evidence supports its role in the programming of adult cardiovascular dysfunction through the generation of oxidative stress. Whether fetal chronic hypoxia programmes alterations in cardiovascular control in vivo, and if these alterations can be prevented by antioxidant treatment, is unknown. This study investigated the effects of prenatal fetal hypoxia, with and without maternal supplementation with vitamin C, on basal and stimulated cardiovascular function in vivo in the adult offspring at 4 months of age in the rat. Methods and Results:From days 6 to 20 of pregnancy, Wistar rats were subjected to Normoxia, Hypoxia (13% O2), Hypoxia+Vitamin C (5 mg/ml in drinking water) or Normoxia+Vitamin C. At 4 months, male offspring were instrumented under urethane anaesthesia. Basal mean arterial blood pressure, heart rate and heart rate variability (HRV) were assessed, and stimulated baroreflex curves were generated with phenylephrine and sodium nitroprusside. Chronic fetal hypoxia increased the LF/HF HRV ratio and baroreflex gain, effects prevented by vitamin C administration during pregnancy. Conclusions:Chronic intrauterine hypoxia programmes cardiovascular dysfunction in vivo in adult rat offspring; effects ameliorated by maternal treatment with vitamin C. The data support a role for fetal chronic hypoxia programming cardiovascular dysfunction in the adult rat offspring in vivo through the generation of oxidative stress in utero. (Circ J 2013; 77: 2604 -2611

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Section: Discussionmentioning

confidence: 54%

Vitamin C Prevents Intrauterine Programming of in vivo Cardiovascular Dysfunction in the Rat

Kane

Herrera

Camm

et al. 2013

Circ J

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“…Hypoxia also has varying degrees of effect on the morphology and performance of the heart and systemic vasculature, ranging from no effect to profound disturbance (Asson-Batres et al, 1989;Richards et al, 1991;Burton and Palmer, 1992;Altimiras and Phu, 2000;le Noble et al, 2000;Dzialowski et al, 2002;Rouwet et al, 2002;Villamor et al, 2002;Ruijtenbeek et al, 2003;Villamor et al, 2004;Chan and Burggren, 2005;Zhang and Burggren, 2012). Corresponding with these cardiorespiratory phenotypic modifications are changes in overall metabolic rate, typically measured as oxygen consumption.…”

Section: Hypoxia Hypercapnia and Avian Critical Windowsmentioning

confidence: 99%

“…Interestingly, albumen removal also results in adult hens with modified DNA methylation and long-term alterations in the hepatic transcriptome (Willems et al, 2016). The extraction of a percentage of the egg contents reduces embryonic growth and results in a low hatching weight, but apparently without any vascular consequences (Ruijtenbeek et al, 2003).…”

Section: Fetal Programming -Beyond Mammals To Birdsmentioning

confidence: 99%

Cardio-respiratory development in bird embryos: new insights from a venerable animal model

2016

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-The avian embryo is a time-honored animal model for understanding vertebrate development. A key area of extensive study using bird embryos centers on developmental phenotypic plasticity of the cardio-respiratory system and how its normal development can be affected by abiotic factors such as temperature and oxygen availability. Through the investigation of the plasticity of development, we gain a better understanding of both the regulation of the developmental process and the embryo's capacity for self-repair. Additionally, experiments with abiotic and biotic stressors during development have helped delineate not just critical windows for avian cardio-respiratory development, but the general characteristics (e.g., timing and dose-dependence) of critical windows in all developing vertebrates. Avian embryos are useful in exploring fetal programming, in which early developmental experiences have implications (usually negative) later in life. The ability to experimentally manipulate the avian embryo without the interference of maternal behavior or physiology makes it particularly useful in future studies of fetal programming. The bird embryo is also a key participant in studies of transgenerational epigenetics, whether by egg provisioning or effects on the germline that are transmitted to the F1 generation (or beyond). Finally, the avian embryo is heavily exploited in toxicology, in which both toxicological testing of potential consumer products as well as the consequences of exposure to anthropogenic pollutants are routinely carried out in the avian embryo. The avian embryo thus proves useful on numerous experimental fronts as an animal model that is concurrently both of adequate complexity and sufficient simplicity for probing vertebrate cardio-respiratory development.

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“…Hypoxia alters the endothelial properties of fetal pulmonary (23), fetal carotid (16,17), cerebral (24), and femoral arteries (10,25,26). The effect of chronic hypoxia on fetal tissue eNOS gene expression is variable among different cell types.…”

Section: Articlesmentioning

confidence: 99%

“…*P < 0.05; **P < 0.01, maternal hypoxia (black bars) as compared with control (white bars). sequence of the human and bovine eNOS gene (30)(31)(32), the changes in blood flow occurring during fetal hypoxemia may alter arterial shear stress (26), which in turn can modulate the expression and activity of eNOS (33). One of the well-studied signaling pathways activated during endothelial response to shear stress is the cascade consisting of G-protein → phospholipase C/Ca 2+ → protein kinase C → c-fos/c-jun → activator protein 1 site-dependent transcription; this pathway is operative in the elevation of eNOS expression by shear stress.…”

Section: Articlesmentioning

confidence: 99%

Intermittent maternal hypoxia has an influence on regional expression of endothelial nitric oxide synthase in fetal arteries of rabbits

Chen¹,

Wang

Chen

et al. 2013

Pediatr Res

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Background: Maternal hypoxia induces sustained fetal adaptations associated with changes in gene expression. We hypothesized that intermittent maternal hypoxia has an influence on regional expression of endothelial nitric oxide synthase (eNOS) in fetal arteries of New Zealand White rabbits. Methods: Timed-pregnant New Zealand White rabbits (term = 30 ± 1 d) were randomly assigned to a normoxic control group (n = 5) or a hypoxia group (12% O 2 , n = 5) during days 10-29 of pregnancy. At the end of pregnancy (29 d gestation), blood samples were collected from mothers and fetuses. Carotid and femoral arteries of fetuses were extracted for eNOS mRNA and protein concentration and analysis of total NOS activities. results: Our data demonstrate that chronic intermittent maternal hypoxia significantly increased eNOS mRNA and protein concentrations and total NOS activities in carotid artery segments but decreased eNOS mRNA and protein concentrations and total NOS activities in femoral artery segments in the same fetuses. Vascular endothelial cells, but not smooth muscle cells, of fetal rabbits exhibited positive immunostaining for the eNOS protein. conclusion: These observations suggest that chronic hypoxia can regulate regional expression of eNOS as an adaptive response to hypoxic stress in fetal arteries.

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Chronic moderate hypoxia during in ovo development alters arterial reactivity in chickens

Cited by 35 publications

References 41 publications

Vitamin C Prevents Intrauterine Programming of in vivo Cardiovascular Dysfunction in the Rat

Vitamin C Prevents Intrauterine Programming of in vivo Cardiovascular Dysfunction in the Rat

Cardio-respiratory development in bird embryos: new insights from a venerable animal model

Intermittent maternal hypoxia has an influence on regional expression of endothelial nitric oxide synthase in fetal arteries of rabbits

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