The Chicken Embryo in Developmental Physiology of the Cardiovascular System: A Traditional Model with New Possibilities

The following letters refer to an "In focus" article by H. Ehmke (Developmental physiology of the cardiovascular system. Am J Physiol Regulatory Integrative Comp Physiol 282: R331-R333, 2002).

	LETTER

To the Editor: In the February 2002 issue of American Journal of Physiology-Regulatory, Integrative and Comparative Physiology, Ehmke (7) focuses on unsolved issues and interesting findings in the field of developmental physiology of the cardiovascular system. Ehmke addresses the need for new useful models to study embryonic/fetal cardiovascular structure and function and rightly points out the potential of the zebrafish (Danio rerio) as an experimental model. The merits of this model organism for integrative physiology were reviewed by Briggs (4).

The chicken (Gallus gallus) is a species that deserves attention when the developmental physiology of the cardiovascular system is considered. The attractiveness of the chicken embryo as an experimental model to study angiogenesis (1), heart formation (11, 20), and the development of neurohumoral cardiac control (12, 19) has long been recognized. Recent studies have shown that the chicken embryo, like the zebrafish (9), can also be used to study developmental changes in local vascular tone and hemodynamic control. Reactivity of isolated femoral and carotid arteries of chicken embryos can be studied by means of wire myograph techniques from embryonic day 15 of the 21 days of incubation (15), and precise surgical preparation and intravital microscopy enable the measurement of mesenteric vascular diameter in the intact fetus at even earlier stages of development (22). Very recently the changes in pulmonary arterial reactivity during the transition from in ovo to ex ovo life (which takes more time than in mammalians and therefore can be studied in more detail) have been investigated in the chicken embryo (25).

Other studies have used fluorescent microspheres and cannulation procedures (branches of chorioallantoic vein) to investigate time-dependent changes in cardiac output distribution, blood pressure, and heart rate in early and late stages of incubation (2, 3, 18, 26). These studies have provided methods that give important insights in the development of cardiovascular physiological mechanisms in the chicken embryo. In addition, they demonstrate substantial comparability in basic mechanisms of fetal cardiovascular control between the chicken and mammalian species (6). The response to acute hypoxia has been extensively studied in this respect (6, 10, 17).

As Ehmke (7) mentions and argues is the case for the zebrafish (4), a good experimental model should also give the opportunity to study the developmental function of single genes or complex genetic pathways. The role of specific genes and transcription factors, like endothelial PAS protein 1, in cardiovascular development has been investigated in the chicken embryo (8). A "chicken alternative" for the endothelin (ET)-1 and ET type A receptor null mice has even been made by pharmacological in ovo inactivation of the gene product (14). Over the past few years, worldwide collaborations have made large progress in the production of a molecular map of the chicken genome and provide new molecular tools (e.g., microarray) (24). This and the large diversity in genotypes (due to natural and experimental selection) that are also phenotypically characterized (for instance, see Refs. 16, 21) will only increase the potential of the chicken embryo to be used as a model to unravel the role of specific genes in developmental physiology.

As the chicken embryo, like the zebrafish, develops outside the mother, effects of external stresses on cardiovascular development can be studied without interferences of maternal hormonal, metabolic, or hemodynamic alterations. The most common causes of prenatal stress, namely malnutrition and chronic hypoxia (as seen in placental insufficiency), can be studied independently (13, 23, 27), and pharmacological or toxic substances are easily applicable via injections of compounds into the air cell (5). These practical advantages make the chicken embryo and the adult chicken, in which cardiovascular pathology has been observed (16, 21), important animal models to study mechanisms in the intriguing new field of developmental physiology that deals with the prenatal programming of cardiovascular pathology. This tractability for experimental manipulation, its rich history in developmental biology, the short incubation time, and the new possibilities of genomic tools emphasize the importance of the chicken embryo as a model organism in developmental physiology of the cardiovascular system alongside traditional models, such as the fetal sheep, and promising new models, like the zebrafish.

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25.   Villamor, E, Ruijtenbeek K, Pulgar V, De Mey JGR, and Blanco CE. Vascular reactivity in intrapulmonary arteries of chicken embryos during transition to ex vivo life. Am J Physiol Regulatory Integrative Comp Physiol 282: R917-R927, 2002[Abstract/Free Full Text].

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K. Ruijtenbeek Dept. of Pediatrics University Hospital Maastricht 6202 AZ Maastrict, The Netherlands

J. G. R. De Mey Dept. of Pharmacology & Toxicology Cardiovascular Research Institute Maastricht 6200 MD Maastricht, The Netherlands E-mail: j.demey{at}farmaco.unimaas.nl

C. E. Blanco Dept. of Pediatrics University Hospital Maastricht 6202 AZ Maastrict, The Netherlands

	REPLY

To the Editor: I thank Ruijtenbeek et al. for their comments. They rightly make the point for the chicken embryo as a model system to study cardiovascular integrative physiology and homeostasis during development. The chicken embryo shares several features with the zebrafish, like an external development, a relatively short incubation time, and a wide availability, which substantially facilitate its investigation. Furthermore, later stages of embryological development are very similar in the chicken and mouse embryo, and many fundamental mechanisms of development (e.g., those of limb formation) have been discovered in this species. Indeed, the major textbook Principles of Development by Wolpert and colleagues (16) lists the chicken embryo, together with Xenopus laevis, Drosophila melanogaster, Caenorhabditis elegans, Arabidopsis thaliana, the mouse, and the zebrafish, as one of the canonical model systems of developmental biology.

Nevertheless, the virtues of the chicken embryo and the zebrafish as model systems of developmental physiology should not be confused. For many reasons, the zebrafish will remain the dream system for genomewide screens (2, 6, 12). Its short generation time and large progeny size, high permeability to molecules added to the water, external development, and transparency mean that zebrafish are ideally suited for large-scale random mutagenesis screens. Over the past 20 years, a huge amount of genomic information has been accumulated, and it is expected that the entire zebrafish genome will become available in the near future. Because the gene order appears to be conserved in most parts of zebrafish and human chromosomes, genetic screens in zebrafish will most likely help us to understand the function of human genes.

However, the cardiovascular system of the chicken resembles the human cardiovascular system much more closely than does that of the zebrafish. As emphasized by Ruijtenbeek et al., the basic mechanisms of cardiovascular control seem to be very similar in chicken and mammalian species (1), and cardiovascular physiology and pathology can be well studied in adult chicken. In addition, much physiological information is available for the chicken. This is also reflected by a surge of recent studies on chicken embryos published in American Journal of Physiology-Regulatory, Integrative and Comparative Physiology (1, 3-5, 7-11, 13-15). Thus the chicken appears to be particularly suited for studies investigating the long-term consequences of factors acting during embryogenesis.

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2.   Briggs, JP. The zebrafish: a new model organism for integrative physiology. Am J Physiol Regulatory Integrative Comp Physiol 282: R3-R9, 2002.

3.   Crossley, D II, and Altimiras J. Ontogeny of cholinergic and adrenergic cardiovascular regulation in the domestic chicken (Gallus gallus). Am J Physiol Regulatory Integrative Comp Physiol 279: R1091-R1098, 2000.

4.   Dragon, S, and Baumann R. Erythroid carbonic anhydrase and hsp70 expression in chick embryonic development: role of cAMP and hypoxia. Am J Physiol Regulatory Integrative Comp Physiol 280: R870-R878, 2001[Abstract/Free Full Text].

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10.   Mulder, ALM, Miedema A, De Mey JGR, Giussani DA, and Blanco CE. Sympathetic control of the cardiovascular response to acute hypoxemia in the chick embryo. Am J Physiol Regulatory Integrative Comp Physiol 282: R1156-R1163, 2002[Abstract/Free Full Text].

11.   Mulder, ALM, van Goor CA, Giussani DA, and Blanco CE. -Adrenergic contribution to the cardiovascular response to acute hypoxemia in the chick embryo. Am J Physiol Regulatory Integrative Comp Physiol 281: R2004-R2010, 2001[Abstract/Free Full Text].

12.   Patton, EE, and Zon LI. The art and design of genetic screens: zebrafish. Nat Rev Genet 2: 956-966, 2001[ISI][Medline].

13.   Ruijtenbeek, K, Kessels CGA, Villamor E, Blanco CE, and De Mey JGR Direct effects of acute hypoxia on the reactivity of peripheral arteries of the chicken embryo. Am J Physiol Regulatory Integrative Comp Physiol 283: R331-R338, 2002[Abstract/Free Full Text].

14.   Sullivan, LC, and Orgeig S. Dexamethasone and epinephrine stimulate surfactant secretion in type II cells of embryonic chickens. Am J Physiol Regulatory Integrative Comp Physiol 281: R770-R777, 2001[Abstract/Free Full Text].

15.   Villamor, E, Ruijtenbeek K, Pulgar V, De Mey JGR, and Blanco CE. Vascular reactivity in intrapulmonary arteries of chicken embryos during transition to ex ovo life. Am J Physiol Regulatory Integrative Comp Physiol 282: R917-R927, 2002.

16.   Wolpert, L, Beddington R, Jessell T, Lawrence P, Meyerowitz E, and Smith J. Principles of Development (2nd ed). Oxford: Oxford Univ. Press, 2001.

Heimo Ehmke Institut für Physiologie Universität Hamburg 20246 Hamburg, Germany E-mail: ehmke{at}uke.uni-hamburg.de