Biology:Fetal membranes

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Short description: Amnion and chorion which surround and protect a developing fetus
Fetal membranes
FetalMembranes1L.jpg
Fetal membranes at end of second month with chorion shown in its two subdivisions
Details
Identifiers
Latinadnexa fetalia
Anatomical terminology

The fetal membranes are the four extraembryonic membranes, associated with the developing embryo, and fetus in humans and other mammals. They are the amnion, chorion, allantois, and yolk sac.[1] The amnion and the chorion are the chorioamniotic membranes that make up the amniotic sac which surrounds and protects the embryo.[2] The fetal membranes are four of six accessory organs developed by the conceptus that are not part of the embryo itself, the other two are the placenta, and the umbilical cord.[1]

Structure

Placenta shown with attached fetal membranes

The fetal membranes surround the developing embryo and form the fetal-maternal interface.[3] The fetal membranes are derived from the trophoblast layer (outer layer of cells) of the implanting blastocyst.[3] The trophoblast layer differentiates into amnion and the chorion, which then comprise the fetal membranes.[4] The amnion is the innermost layer and, therefore, contacts the amniotic fluid, the fetus and the umbilical cord.[5] The internal pressure of the amniotic fluid causes the amnion to be passively attached to the chorion.[4] The chorion functions to separate the amnion from the maternal decidua and uterus.[4] The placenta develops from the chorion of the embryo and the uterine tissue of the mother.

Development of the fetal membranes

Initially, the amnion is separated from the chorion by chorionic fluid.[4] The fusion of the amnion and chorion is completed in the human at the 12th week of development.[6]

Microanatomy

Fetal membranes illustrated at week 3 following gastrulation

From inside to outside, the fetal membranes consist of amnion and chorion. In addition, parts of decidua are often attached to the outside of the chorion.

Amnion

The amnion is avascular, meaning it does not contain its own blood vessels. Therefore, it must obtain necessary nutrients and oxygen from nearby chorionic and amniotic fluid, and fetal surface vessels.[7][8] The amnion is characterised by cuboidal and columnar epithelial layers.[7] The columnar cells are located in the vicinity of the placenta, whereas the cuboidal cells are found in the periphery.[7] During early pregnancy, the amnionic epithelium is sparsely covered in microvilli, which increase in number throughout pregnancy.[4] The function of this microvillous surface is associated with a densely-packed glycocalix with anionic binding sites; these are thought to be involved with intra-amnionic lipid synthesis.[4] This amnionic epithelium is connected to a basement membrane, which is then attached by filaments to a connective tissue layer.[9]

Chorion

The chorionic membrane is a fibrous tissue layer containing the fetal blood vessels.[4] Chorionic villi form on the outer surface of the chorion, which maximise surface area for contact with maternal blood.[4] The chorionic villi are involved in fetal-maternal exchange.[10]

Yolk sac

The yolk sac is a membranous sac attached to an embryo, formed by cells of the hypoblast layer of the bilaminar embryonic disc. This is alternatively called the umbilical vesicle. In humans, the yolk sac is important in early embryonic blood supply.[11]

Allantois

The human allantois is a caudal out-pouching of the yolk sac, which becomes surrounded by the mesodermal connecting stalk or body-stalk. The vasculature of the body-stalk develops into umbilical arteries that carry deoxygenated blood to the placenta.[12] It is externally continuous with the proctodeum and internally continuous with the cloaca. The embryonic allantois becomes the fetal urachus, which connects the fetal bladder (developed from cloaca) to the yolk sac. The urachus removes nitrogenous waste from the fetal bladder.[13] After birth the urachus is closed, and becomes the median umbilical ligament.

Function

The fetal membrane surrounds the fetus during the gestational period and ensures maintenance of pregnancy to delivery, protection of the fetus as well as being critical in maintaining the conditions necessary for fetal health.

Barrier function

The fetal membranes separate maternal tissue from fetal tissue at a basic mechanical level. The fetal membrane is composed of a thick cellular chorion covering a thin amnion composed of dense collagen fibrils. The amnion is in contact with the amniotic fluid and ensures structural integrity of the sac due to its mechanical strength. The underlying chorion is fused to the decidua at the maternal-fetal interface. This interaction is vital in controlling the local immune systems which in turn is vital for maintaining a semi-allogeneic fetus. At the end of gestation, a 'weak zone' develops in the fetal membrane overlying the cervix due to collage remodelling. This eventually leads to rupture of the fetal membrane and the onset of labour.[citation needed]

Signalling of fetal maturation and parturition

As pregnancy advances to term, the fetal membranes undergo weakening.[14] The amnion is vital in the synthesis of prostaglandins which reach the myometrium and create and initiate parturition. The chorion expresses chemicals that balance synthesis and metabolism of these prostaglandins to ensure that the myometrium is not activated pre-term. Prostaglandin E2 is thought to be synthesized by cells in the amnion and is essential in dilation of the cervix at the initiation of parturition.[15] Glucocorticoids have been implicated in fetal maturation, regulation of immune response and many other pregnancy associated changes.[15] As well as its function in parturition, Prostaglandin E2 is vital for fetal lung maturation. Additionally, there is an abundance of 11β-hydroxysteroid dehydrogenase 1 expressed in the foetal membranes. This enzyme converts biologically inactive cortisone into active cortisol, another chemical vital for fetal maturation and labour initiation.

Pathophysiology

Preterm births (births taking place before 37 weeks) can be the result of a number of causes such as, in utero infection, inflammation, vascular disease and uterine overdistension.[16] The risk of spontaneous preterm birth is increased by a previous preterm birth, black race, periodontal diseases and low maternal body-mass index. Key indicators of preterm birth are short cervical length and a raised cervical-vaginal fetal fibronectin concentration.

Pathophysiology of the fetal membranes, such as microfractures, senescence of cells in the fetal membrane and inflammation can lead to an increased chance of preterm premature rupture of the fetal membranes (pPROM).[17]

Microfractures of the fetal membranes

Throughout gestation the fetal membranes undergo remodeling to allow for the increase in size of the uterus. The remodeling of the fetal membranes occurs at both the level of the cells and the extracellular matrix (ECM).[15] Structural abnormalities such as areas of where collagen has degraded, known as microfractures, have been observed in the amniotic membrane layer.[18][19]

Microfractures are characterised by:

Microfractures of the fetal membranes are seen in pregnancies where pPROM has occurred.[15] It has been suggested that the presence of more fetal membrane microfractures may mean the fetal membranes may be predisposed for preterm rupture.[15]

Inflammation and senescence of the fetal membranes

Main page: Medicine:Chorioamnionitis

Inflammation of the fetal membranes is called chorioamnionitis. Balanced inflammation is an important factor in maintaining fetal membranes by regulating the remodeling. However, if the inflammatory response increases above this level it can have dangerous and potentially fatal effects for the mother and child. These elevated levels of inflammatory molecules in the fetal membrane is called ‘sterile inflammation’.[15] Sterile inflammation can be caused by both microbial infection and non-infectious factors, such as senescence of fetal membranes. Senescence is associated with the aging of actively cycling and dividing cells.[18] As the fetal membrane cells proliferate during remodelling, the telomeres (short length or non-coding DNA on the end of chromosomes that protect essential coding DNA from degradation during replication) shorten as chromosomes can not be copied end-to-end fully.[20] Once the telomeres have reached a critical length the cell can no longer divide and can hence cause telomere-dependent replicative senescence. This should occur naturally at term (37 weeks), as it is an important factor to increase the inflammatory environment in the uterus to initiate parturition. However, fetal membrane senescence can be accelerated by oxidative stress and hence, stimulate sterile inflammation to occur prior to term; consequently, causing preterm birth.[18]

See also

References

  1. 1.0 1.1 Saladin, Kenneth S. (2011). Human anatomy (3rd ed.). New York: McGraw-Hill. pp. 91–94. ISBN 9780071222075. 
  2. "15.7E: Extraembryonic Membranes and the Physiology of the Placenta" (in en). 20 July 2016. https://bio.libretexts.org/Bookshelves/Introductory_and_General_Biology/Book%3A_Biology_(Kimball)/15%3A_The_Anatomy_and_Physiology_of_Animals/15.07%3A_Sexual_Reproduction/15.7E%3A_Extraembryonic_Membranes_and_the_Physiology_of_the_Placenta. 
  3. 3.0 3.1 Essential reproduction (Eighth ed.). Hoboken, NJ. 2018-01-12. ISBN 9781119246473. OCLC 1008770296. 
  4. 4.0 4.1 4.2 4.3 4.4 4.5 4.6 4.7 Benirschke, Kurt; Kaufmann, Peter; Baergen, Rebecca (2006). Pathology of the human placenta (5th ed.). New York: Springer. ISBN 0387267387. OCLC 86076129. 
  5. "The foetal membranes. A review of the anatomy of normal amnion and chorion and some aspects of their function". Postgraduate Medical Journal 38 (438): 193–201. April 1962. doi:10.1136/pgmj.38.438.193. PMID 13871927. 
  6. "Terminology". The Human Placenta. Palgrave Macmillan UK. 1970. pp. 20–26. doi:10.1007/978-1-349-02807-8_2. ISBN 9781349028092. 
  7. 7.0 7.1 7.2 Baergen, Rebecca N (2005). Manual of Benirschke and Kaufmann's Pathology of the human placenta. Benirschke, Kurt.. New York: Springer. ISBN 0387220895. OCLC 64222323. 
  8. Wang, Yuping; Zhao, Shuang (2010). "Placental Blood Circulation" (in en). Morgan & Claypool Life Sciences. https://www.ncbi.nlm.nih.gov/books/NBK53254/. 
  9. "The microscopic anatomy of the fetal membranes with particular reference to the detailed structure of the amnion". American Journal of Obstetrics and Gynecology 75 (3): 536–47; discussion 548–50. March 1958. doi:10.1016/0002-9378(58)90610-0. PMID 13508744. 
  10. Rebecca N. Baergen. (2011). Manual of Pathology of the Human Placenta.. Springer Science+Business Media, LLC. ISBN 978-1283087018. OCLC 823129086. 
  11. Lutfey, Karen; Freese, Jeremy (2005). "Toward Some Fundamentals of Fundamental Causality: Socioeconomic Status and Health in the Routine Clinic Visit for Diabetes". American Journal of Sociology 110 (5): 1326–1372. doi:10.1086/428914. ISSN 0002-9602. https://www.jstor.org/stable/10.1086/428914. 
  12. Moore, Keith; Persaud, T.V.N.; Torchia, Mark G. (2016). The Developing Human: Clinically Oriented Embryology (10th ed.). Philadelphia: Elsevier. p. 58. ISBN 978-0-323-31338-4. 
  13. First AID for the USMLE Step 1 2008
  14. Sun, Kang, ed (2017-03-28). "Function and failure of the fetal membrane: Modelling the mechanics of the chorion and amnion". PLOS ONE 12 (3): e0171588. doi:10.1371/journal.pone.0171588. PMID 28350838. Bibcode2017PLoSO..1271588V. 
  15. 15.0 15.1 15.2 15.3 15.4 15.5 15.6 15.7 15.8 15.9 "Role of fetal membranes in signaling of fetal maturation and parturition". The International Journal of Developmental Biology 54 (2–3): 545–53. 2010. doi:10.1387/ijdb.082771lm. PMID 19924634. 
  16. "Epidemiology and causes of preterm birth" (in English). Lancet 371 (9606): 75–84. January 2008. doi:10.1016/S0140-6736(08)60074-4. PMID 18177778. 
  17. "Fetal membrane architecture, aging and inflammation in pregnancy and parturition". Placenta. TR: Proceedings of PREBIC meeting 2018 79: 40–45. April 2019. doi:10.1016/j.placenta.2018.11.003. PMID 30454905. 
  18. 18.0 18.1 18.2 "Programmed Fetal Membrane Senescence and Exosome-Mediated Signaling: A Mechanism Associated With Timing of Human Parturition". Frontiers in Endocrinology 8: 196. 2017-08-17. doi:10.3389/fendo.2017.00196. PMID 28861041. 
  19. "Preterm prelabor rupture of the membranes: A disease of the fetal membranes". Seminars in Perinatology. Current Preterm Birth Prevention Strategies 41 (7): 409–419. November 2017. doi:10.1053/j.semperi.2017.07.012. PMID 28807394. 
  20. "Cell-Free Fetal DNA, Telomeres, and the Spontaneous Onset of Parturition" (in en-US). Reproductive Sciences 22 (10): 1186–201. October 2015. doi:10.1177/1933719115592714. PMID 26134037.