The highs and lows of programmed cardiovascular disease by developmental hypoxia: studies in the chicken embryo

N. Itani; C. E. Salinas; M. Villena; K. L. Skeffington; C. Beck; E. Villamor; C. E. Blanco; D. A. Giussani

doi:10.1113/JP274111

The highs and lows of programmed cardiovascular disease by developmental hypoxia: studies in the chicken embryo

N. Itani, C. E. Salinas, M. Villena, K. L. Skeffington, C. Beck, E. Villamor, C. E. Blanco, D. A. Giussani^*

^*Corresponding author for this work

Research output: Contribution to journal › (Systematic) Review article › peer-review

Abstract

It is now established that adverse conditions during pregnancy can trigger a fetal origin of cardiovascular dysfunction and/or increase the risk of heart disease in later life. Suboptimal environmental conditions during early life that may promote the development of cardiovascular dysfunction in the offspring include alterations in fetal oxygenation and nutrition as well as fetal exposure to stress hormones, such as glucocorticoids. There has been growing interest in identifying the partial contributions of each of these stressors to programming of cardiovascular dysfunction. However, in humans and in many animal models this is difficult, as the challenges cannot be disentangled. By using the chicken embryo as an animal model, science has been able to circumvent a number of problems. In contrast to mammals, in the chicken embryo the effects on the developing cardiovascular system of changes in oxygenation, nutrition or stress hormones can be isolated and determined directly, independent of changes in the maternal or placental physiology. In this review, we summarise studies that have exploited the chicken embryo model to determine the effects on prenatal growth, cardiovascular development and pituitary-adrenal function of isolated chronic developmental hypoxia.

Original language	English
Pages (from-to)	2991-3006
Number of pages	16
Journal	Journal of Physiology
Volume	596
Issue number	15
DOIs	https://doi.org/10.1113/JP274111
Publication status	Published - 1 Aug 2018

Keywords

HIGH-ALTITUDE HYPOXIA
LOW-BIRTH-WEIGHT
INTRAUTERINE GROWTH RESTRICTION
MESENTERIC-ARTERY REACTIVITY
CHRONIC MODERATE HYPOXIA
LONG-TERM HYPOXEMIA
UTERINE BLOOD-FLOW
FETAL-GROWTH
PRENATAL HYPOXIA
ENDOTHELIAL FUNCTION

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10.1113/JP274111

Cite this

@article{cd42d817039d4ac8bcf4e4304d98c680,

title = "The highs and lows of programmed cardiovascular disease by developmental hypoxia: studies in the chicken embryo",

abstract = "It is now established that adverse conditions during pregnancy can trigger a fetal origin of cardiovascular dysfunction and/or increase the risk of heart disease in later life. Suboptimal environmental conditions during early life that may promote the development of cardiovascular dysfunction in the offspring include alterations in fetal oxygenation and nutrition as well as fetal exposure to stress hormones, such as glucocorticoids. There has been growing interest in identifying the partial contributions of each of these stressors to programming of cardiovascular dysfunction. However, in humans and in many animal models this is difficult, as the challenges cannot be disentangled. By using the chicken embryo as an animal model, science has been able to circumvent a number of problems. In contrast to mammals, in the chicken embryo the effects on the developing cardiovascular system of changes in oxygenation, nutrition or stress hormones can be isolated and determined directly, independent of changes in the maternal or placental physiology. In this review, we summarise studies that have exploited the chicken embryo model to determine the effects on prenatal growth, cardiovascular development and pituitary-adrenal function of isolated chronic developmental hypoxia.",

keywords = "HIGH-ALTITUDE HYPOXIA, LOW-BIRTH-WEIGHT, INTRAUTERINE GROWTH RESTRICTION, MESENTERIC-ARTERY REACTIVITY, CHRONIC MODERATE HYPOXIA, LONG-TERM HYPOXEMIA, UTERINE BLOOD-FLOW, FETAL-GROWTH, PRENATAL HYPOXIA, ENDOTHELIAL FUNCTION",

author = "N. Itani and Salinas, {C. E.} and M. Villena and Skeffington, {K. L.} and C. Beck and E. Villamor and Blanco, {C. E.} and Giussani, {D. A.}",

year = "2018",

month = aug,

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doi = "10.1113/JP274111",

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T1 - The highs and lows of programmed cardiovascular disease by developmental hypoxia

T2 - studies in the chicken embryo

AU - Itani, N.

AU - Salinas, C. E.

AU - Villena, M.

AU - Skeffington, K. L.

AU - Beck, C.

AU - Villamor, E.

AU - Blanco, C. E.

AU - Giussani, D. A.

PY - 2018/8/1

Y1 - 2018/8/1

N2 - It is now established that adverse conditions during pregnancy can trigger a fetal origin of cardiovascular dysfunction and/or increase the risk of heart disease in later life. Suboptimal environmental conditions during early life that may promote the development of cardiovascular dysfunction in the offspring include alterations in fetal oxygenation and nutrition as well as fetal exposure to stress hormones, such as glucocorticoids. There has been growing interest in identifying the partial contributions of each of these stressors to programming of cardiovascular dysfunction. However, in humans and in many animal models this is difficult, as the challenges cannot be disentangled. By using the chicken embryo as an animal model, science has been able to circumvent a number of problems. In contrast to mammals, in the chicken embryo the effects on the developing cardiovascular system of changes in oxygenation, nutrition or stress hormones can be isolated and determined directly, independent of changes in the maternal or placental physiology. In this review, we summarise studies that have exploited the chicken embryo model to determine the effects on prenatal growth, cardiovascular development and pituitary-adrenal function of isolated chronic developmental hypoxia.

AB - It is now established that adverse conditions during pregnancy can trigger a fetal origin of cardiovascular dysfunction and/or increase the risk of heart disease in later life. Suboptimal environmental conditions during early life that may promote the development of cardiovascular dysfunction in the offspring include alterations in fetal oxygenation and nutrition as well as fetal exposure to stress hormones, such as glucocorticoids. There has been growing interest in identifying the partial contributions of each of these stressors to programming of cardiovascular dysfunction. However, in humans and in many animal models this is difficult, as the challenges cannot be disentangled. By using the chicken embryo as an animal model, science has been able to circumvent a number of problems. In contrast to mammals, in the chicken embryo the effects on the developing cardiovascular system of changes in oxygenation, nutrition or stress hormones can be isolated and determined directly, independent of changes in the maternal or placental physiology. In this review, we summarise studies that have exploited the chicken embryo model to determine the effects on prenatal growth, cardiovascular development and pituitary-adrenal function of isolated chronic developmental hypoxia.

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KW - INTRAUTERINE GROWTH RESTRICTION

KW - MESENTERIC-ARTERY REACTIVITY

KW - CHRONIC MODERATE HYPOXIA

KW - LONG-TERM HYPOXEMIA

KW - UTERINE BLOOD-FLOW

KW - FETAL-GROWTH

KW - PRENATAL HYPOXIA

KW - ENDOTHELIAL FUNCTION

U2 - 10.1113/JP274111

DO - 10.1113/JP274111

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