词条 | Hypoblast |
释义 |
| Name = Hypoblast | Latin = hypoblastus | Image = File:Human Embryo Day9.png | Caption = Human Embryo in day 9. Hypoblast (brown) is beneath the epiblast (pink) | Image2 = | Caption2 = "D" points to the hypoblast. | System = | CarnegieStage = | Days = 8 | Precursor = inner cell mass | GivesRiseTo = endoderm }} The hypoblast is a tissue type that forms from the inner cell mass.[1] It lies beneath the epiblast and consists of small cuboidal cells.[2] Extraembryonic endoderm (including Yolk sac) is derived from hypoblast cells. The absence of hypoblast results in multiple primitive streaks in chicken embryos.[3] The formation of the primitive streak, through which gastrulation occurs, is induced by Koller's sickle.[4] StructureIn miceIn mouse embryo, the visceral endoderm develop from the primitive endoderm of the blastocyst during the implantation stage covering the epiblast cells and elongates to become an egg cylinder. A distinct morphological domain has been identified by Martin and colleagues, at the distal tip of the mouse egg cylinder, thus this domain was called distal visceral domain (DVE).[5] The DVE cells will move unilaterally to the future anterior until reaching the embryonic/ extra embryonic boundary and at this point, the DVE cells are also named as anterior visceral endoderm (AVE).[6] This migration has been proved to be essential for establishing anteroposterior axis. Besides the AVE, another cell population appears to be separated at the posterior edge of the embryonic egg cylinder, referred to as posterior visceral endoderm (PVE). However, the function of this cell population was not as well studied as AVE. FunctionAlthough the hypoblast does not contribute to the embryo, it has great influences on the orientation of the embryonic axis. For example, the AVE in hypoblast plays an important role in positioning the primitive streak at the midland of the amniote embryos. In chick, people had observed that removal of the hypoblast caused multiple, ectopic primitive streaks formation.[7] Similarly, in mice embryo, the AVE expresses secreted molecules, including two antagonists of nodal signaling, Cerberus-like (Cerl) and a TGFβ superfamily molecule, Lefty1. It was shown that Cerberus−/−;Lefty1−/− compound mutants mice developed a primitive streak ectopically in the embryo.[8] There is also finding suggested that the hypoblast also inhibit primitive streak formation by depositing extracellular matrix components to inhibit epithelial-mesenchymal transition (EMT).[9] Besides the role of positioning the site of gastrulation, AVE also showed other function including continued protection against caudalization of the early nervous system.[10] Also primitive endoderm derived yolk sac has major function in guaranteeing the proper organogenesis of the fetus and efficient exchange of nutrients, gases and wastes. HistoryIn mammals, the existence of primitive endoderm had been observed as early as the end of the 19th century as first recognized by Duval and Sobotta.[11][12] However, it took long time before people realized that the primitive endoderm will be replaced by definitive endoderm which will further develop into the gut tube. The first convincing experiment was conducted by Bellairs in chick embryo with the careful observation under electron and light microscopy. In his experiment, Bellairs demonstrated that there is a transitory endoderm cell layer in the chick embryo at its ventral surface before the formation of primitive streak. This layer of cell was replaced by definitive endoderm migration from the primitive streak through ingression and de-epithelialization.[13][14][15][16] Later on, more insights on primitive endoderm and definitive endoderm origin and formation have been provided in different species including rat and mouse, rhesus monkey, baboon et al.[17][18][19][20][21] References1. ^UNSW Embryology- Glossary H {{webarchive|url=https://web.archive.org/web/20070818020419/http://embryology.med.unsw.edu.au/Notes/Index/H.htm |date=2007-08-18 }} 2. ^Moore, K. L., and Persaud, T. V. N. (2003). The Developing Human: Clinically Oriented Embryology. 7th Ed. Philadelphia: Elsevier. {{ISBN|0-7216-9412-8}}. 3. ^{{cite journal |doi= 10.1016/S1534-5807(02)00321-0 |vauthors=Perea-Gomez A, Vella FD, Shawlot W, Oulad-Abdelghani M, Chazaud C, Meno C, Pfister V, Chen L, Robertson E, Hamada H, Behringer RR, Ang SL |title= Nodal antagonists in the anterior visceral endoderm prevent the formation of multiple primitive streaks |journal= Dev Cell |volume= 3 |pages= 745–56. |year= 2002 |pmid=12431380| issue=5}} 4. ^Gilbert SF. Developmental Biology. 10th edition. Sunderland (MA): Sinauer Associates; 2014. Early Development in Birds. Print 5. ^Rosenquist T. A., Martin G. R. (1995). Visceral endoderm-1 (VE-1): an antigen marker that distinguishes anterior from posterior embryonic visceral endoderm in the early post-implantation mouse embryo. Mech. Dev. 49, 117–121 6. ^Thomas P., Beddington R. (1996). Anterior primitive endoderm may be responsible for patterning the anterior neural plate in the mouse embryo. Curr. Biol. 6, 1487–1496. 7. ^Bertocchini F., Stern C. D. (2002). The hypoblast of the chick embryo positions the primitive streak by antagonizing nodal signaling. Dev. Cell 3, 735–744. 8. ^Perea-Gomez A., Vella F. D., Shawlot W., Oulad-Abdelghani M., Chazaud C., Meno C., Pfister V., Chen L., Robertson E., Hamada H., et al. (2002).Nodal antagonists in the anterior visceral endoderm prevent the formation of multiple primitive streaks. 9. ^Egea J., Erlacher C., Montanez E., Burtscher I., Yamagishi S., Hess M., Hampel F., Sanchez R., Rodriguez-Manzaneque M. T., Bosl M. R., et al. (2008). Genetic ablation of FLRT3 reveals a novel morphogenetic function for the anterior visceral endoderm in suppressing mesoderm differentiation.Genes Dev. 22, 3349–3362. 10. ^Wilson S. W., Houart C. (2004). Early steps in the development of the forebrain. Dev. Cell 6, 167–181. 11. ^Duval M. (1891). The rodent placenta. Third part. The placenta of the mouse and of the rat. J. Anat. Physiol. Normales et Pathol. de l’Homme et des Animaux 27, 24-73; 344-395; 515-612. 12. ^Sobotta J. (1911). Die Entwicklung des Eies der Maus vom ersten Auftreten des Mesoderms an bis zur Ausbildung der Embryonalanlage und dem Auftreten der Allantois. I. Teil: Die Keimblase. Archiv. fur mikroskopische Anatomie 78, 271–352. 13. ^Bellairs R. (1953a). Studies on the development of the foregut in the chick blastoderm. 1. The presumptive foregut area. J. Embryol. Exp. Morph. 1, 115–124. 14. ^Bellairs R. (1953b). Studies on the development of the foregut in the chick blastoderm. 2. The morphogenetic movements. J. Embryol. Exp. Morph. 1, 369–385. 15. ^Bellairs R. (1964). Biological aspects of the yolk of the hen’s egg. Adv. Morphog. 4, 217–272. 16. ^Bellairs R. (1986). The primitive streak. Anat. Embryol. 17. ^Enders A. C., Given R. L., Schlafke S. (1978). Differentiation and migration of endoderm in the rat and mouse at implantation. Anat. Rec. 190, 65–77. 18. ^Enders A. C., Schlafke S., Hendrickx A. G. (1986). Differentiation of the embryonic disc, amnion, and yolk sac in the rhesus monkey. Am. J. Anat. 177, 161–185. 19. ^Enders A. C., Lantz K. C., Schlafke S. (1990). Differentiation of the inner cell mass of the baboon blastocyst. Anat. Rec. 226, 237–248. 20. ^Gardner R. L. (1982). Investigation of cell lineage and differentiation in the extraembryonic endoderm of the mouse embryo. J. Embryol. Exp. Morphol. 68, 175–198. 21. ^Gardner R. L. (1984). An in situ cell marker for clonal analysis of development of the extraembryonic endoderm in the mouse. J. Embryol. Exp. Morphol. 80, 251–288. External links
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