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Ductus arteriosus

The ductus arteriosus, also called the ductus Botalli, named after the Italian physiologist Leonardo Botallo, is a blood vessel in the developing fetus connecting the trunk of the pulmonary artery to the proximal descending aorta. It allows most of the blood from the right ventricle to bypass the fetus's fluid-filled non-functioning lungs. Upon closure at birth, it becomes the ligamentum arteriosum.[clarification needed]

Ductus arteriosus
The fetal circulatory system, with the ductus arteriosus visible at upper right.
Details
Precursoraortic arch 6
SystemFetal circulation
Sourcepulmonary artery
Branchesdescending aorta
Veinductus venosus
Identifiers
LatinDuctus arteriosus
MeSHD004373
TEarteriosus_by_E5.11.2.1.2.0.17 E5.11.2.1.2.0.17
FMA79871
Anatomical terminology
[edit on Wikidata]

Development and structure Edit

The ductus arteriosus is formed from the left 6th aortic arches during embryonic development[1] and attaches to the final part of the aortic arch (the isthmus of aorta) and the first part of the pulmonary artery.[2]

Disorder: Patent ductus arteriosus Edit

 
The human adult heart, showing a patent ductus arteriosus connecting the pulmonary trunk to the arch of aorta

Consequences Edit

Failure of the ductus arteriosus to close after birth results in a condition called patent ductus arteriosus, which results in the abnormal flow of blood from the aorta to the pulmonary artery: a left-to-right shunt. If left uncorrected, this usually leads to pulmonary hypertension followed by right ventricular heart failure, as well as possible cardiac arrhythmias.

Role of prostaglandins Edit

The "E" series of prostaglandins are responsible for maintaining the openness of the ductus arteriosus (by dilation of vascular smooth muscle) throughout the fetal period.[3] Prostaglandin E2 (PGE2), produced by both the placenta and the DA itself, is the most potent of the E prostaglandins, but prostaglandin E1 (PGE1) also has a role in keeping the DA open.[4] PGE1 and PGE2 keep the ductus arteriosus open via involvement of specific PGE-sensitive receptors (such as EP4 and EP2).[5] EP4 is the major receptor associated with PGE2-induced dilation of the DA and can be found across the DA in smooth muscle cells.[6] Immediately after birth, the levels of both PGE2 and the EP4 receptors reduce significantly, allowing for closure of the DA and establishment of normal postnatal circulation.[6]

Role of non-steroidal anti-inflammatory drugs Edit

Ductus arteriosus closure may be induced by administration of nonsteroidal anti-inflammatory drugs (NSAIDs), which inhibit prostaglandin production.[4] The most common NSAID used is Indomethacin, which is usually administered in the first week after birth.[4] However, in the presence of a congenital defect with impaired lung perfusion (e.g. Pulmonary stenosis and left-to-right shunt through the ductus), it may be advisable to improve oxygenation by maintaining the ductus open with prostaglandin treatment. However, such treatments are ineffective in an abnormal ductus. Persistence of the ductus may be associated with other abnormalities, and is much more common in females. By inhibiting PGE2 formation, EP4 receptor activation will decrease and normal circulation can begin. NSAIDs taken late in pregnancy can cross the placenta and lead to premature closure of the DA in the fetus.[7] In this case, exogenous PDE2 can be administered to reverse the effects of the NSAIDs and maintain the patency of the DA for the remainder of the pregnancy.[4]

Incidence Edit

A patent ductus arteriosus affects approximately 4% of infants with Down syndrome (DS). A failure to thrive is a very common sign of this condition.[8]

Maintaining patency Edit

In some types of congenital heart defect (e.g., transposition of the great arteries), prostaglandins may be administered to maintain the DA open, allowing for the continual circulation and oxygenation of blood, until surgery can be performed.[9]

Other animals Edit

Ductus arteriosus evolved with the lung in the ancestors of the lungfish as a connection between the pulmonary arteries and dorsal aorta. During embryonic development, reptiles, birds, and mammals all have either one or two paired ductus arteriosi that provide a fetal shunt of blood away from the lungs.[10]

See also Edit

References Edit

  1. ^ Bamforth, Simon D.; Chaudhry, Bill; Bennett, Michael; Wilson, Robert; Mohun, Timothy J.; Van Mierop, Lodewyk H.S.; Henderson, Deborah J.; Anderson, Robert H. (2013-03-01). "Clarification of the identity of the mammalian fifth pharyngeal arch artery". Clinical Anatomy. 26 (2): 173–182. doi:10.1002/ca.22101. ISSN 1098-2353. PMID 22623372. S2CID 7927804.
  2. ^ Monvadi B. Srichai (2007). David P. Naidich; et al. (eds.). Computed tomography and magnetic resonance of the thorax (4th ed.). Philadelphia: Wolters Kluwer/Lippincott Williams & Wilkins. p. 100. ISBN 9780781757652.
  3. ^ Lucas, A (1978). "Prostaglandins in Patent Ductus Arteriosus". The Lancet. 312 (8096): 937–938. doi:10.1016/S0140-6736(78)91648-3. ISSN 0140-6736. PMID 81944. S2CID 54389960.
  4. ^ a b c d Olley, P.M.; Conceani F. (1981). "Prostaglandins and the Ductus Arteriosus". Annual Review of Medicine. 32 (1): 375–385. doi:10.1146/annurev.me.32.020181.002111. PMID 7013675.
  5. ^ Bouayad A, Kajino H, Waleh N, Fouron JC, Andelfinger G, Varma DR, Skoll A, Vazquez A, Gobeil F, Clyman RI, Chemtob S (2001). "Characterization of PGE2 receptors in fetal and newborn lamb ductus arteriosus". Am. J. Physiol. Heart Circ. Physiol. 280 (5): H2342–9. doi:10.1152/ajpheart.2001.280.5.H2342. PMID 11299240. S2CID 32049750.
  6. ^ a b Gruzdeva, A; Nguyena, M.; Kovarovob, M.; Koller, B (March 2012). "PGE2 through the EP4 receptor controls smooth muscle gene expression patterns in the ductus arteriosus critical for remodeling at birth". Prostaglandins and Other Lipid Mediators. 94 (3): 109–119. doi:10.1016/j.prostaglandins.2012.02.001. PMC 3312001. PMID 22342504.
  7. ^ Anonucci, R; Zaffanello, M.; Puxeddu, E.; Porcella, A.; Cuzzolin, L.; Pilloni, M.; Fanos, V. (2012). "Use of non-steroidal anti-inflammatory drugs in pregnancy:impact on the fetus and newborn". Current Drug Metabolism. 13 (4): 474–490. doi:10.2174/138920012800166607. PMID 22299823.
  8. ^ Pritchard & Korf. "Medical Genetics at a Glance". Blackwell Publishing. 2010. p63.
  9. ^ "Congenital heart defects: Prostaglandins and prostaglandin inhibitors". Healthwise. My Health Alberta.
  10. ^ Dzialowski, Edward M. (2018). "Comparative physiology of the ductus arteriosus among vertebrates". Seminars in Perinatology. 42 (4): 203–211. doi:10.1053/j.semperi.2018.05.002. ISSN 1558-075X. PMID 29937096. S2CID 49405282.

External links Edit

  • Circulatory changes at birth at berkeley.edu

ductus, arteriosus, ductus, arteriosus, also, called, ductus, botalli, named, after, italian, physiologist, leonardo, botallo, blood, vessel, developing, fetus, connecting, trunk, pulmonary, artery, proximal, descending, aorta, allows, most, blood, from, right. The ductus arteriosus also called the ductus Botalli named after the Italian physiologist Leonardo Botallo is a blood vessel in the developing fetus connecting the trunk of the pulmonary artery to the proximal descending aorta It allows most of the blood from the right ventricle to bypass the fetus s fluid filled non functioning lungs Upon closure at birth it becomes the ligamentum arteriosum clarification needed Ductus arteriosusThe fetal circulatory system with the ductus arteriosus visible at upper right DetailsPrecursoraortic arch 6SystemFetal circulationSourcepulmonary arteryBranchesdescending aortaVeinductus venosusIdentifiersLatinDuctus arteriosusMeSHD004373TEarteriosus by E5 11 2 1 2 0 17 E5 11 2 1 2 0 17FMA79871Anatomical terminology edit on Wikidata Contents 1 Development and structure 2 Disorder Patent ductus arteriosus 2 1 Consequences 2 2 Role of prostaglandins 2 3 Role of non steroidal anti inflammatory drugs 2 4 Incidence 2 5 Maintaining patency 3 Other animals 4 See also 5 References 6 External linksDevelopment and structure EditThe ductus arteriosus is formed from the left 6th aortic arches during embryonic development 1 and attaches to the final part of the aortic arch the isthmus of aorta and the first part of the pulmonary artery 2 Disorder Patent ductus arteriosus EditMain article Patent ductus arteriosus nbsp The human adult heart showing a patent ductus arteriosus connecting the pulmonary trunk to the arch of aortaConsequences Edit Failure of the ductus arteriosus to close after birth results in a condition called patent ductus arteriosus which results in the abnormal flow of blood from the aorta to the pulmonary artery a left to right shunt If left uncorrected this usually leads to pulmonary hypertension followed by right ventricular heart failure as well as possible cardiac arrhythmias Role of prostaglandins Edit The E series of prostaglandins are responsible for maintaining the openness of the ductus arteriosus by dilation of vascular smooth muscle throughout the fetal period 3 Prostaglandin E2 PGE2 produced by both the placenta and the DA itself is the most potent of the E prostaglandins but prostaglandin E1 PGE1 also has a role in keeping the DA open 4 PGE1 and PGE2 keep the ductus arteriosus open via involvement of specific PGE sensitive receptors such as EP4 and EP2 5 EP4 is the major receptor associated with PGE2 induced dilation of the DA and can be found across the DA in smooth muscle cells 6 Immediately after birth the levels of both PGE2 and the EP4 receptors reduce significantly allowing for closure of the DA and establishment of normal postnatal circulation 6 Role of non steroidal anti inflammatory drugs Edit Ductus arteriosus closure may be induced by administration of nonsteroidal anti inflammatory drugs NSAIDs which inhibit prostaglandin production 4 The most common NSAID used is Indomethacin which is usually administered in the first week after birth 4 However in the presence of a congenital defect with impaired lung perfusion e g Pulmonary stenosis and left to right shunt through the ductus it may be advisable to improve oxygenation by maintaining the ductus open with prostaglandin treatment However such treatments are ineffective in an abnormal ductus Persistence of the ductus may be associated with other abnormalities and is much more common in females By inhibiting PGE2 formation EP4 receptor activation will decrease and normal circulation can begin NSAIDs taken late in pregnancy can cross the placenta and lead to premature closure of the DA in the fetus 7 In this case exogenous PDE2 can be administered to reverse the effects of the NSAIDs and maintain the patency of the DA for the remainder of the pregnancy 4 Incidence Edit A patent ductus arteriosus affects approximately 4 of infants with Down syndrome DS A failure to thrive is a very common sign of this condition 8 Maintaining patency Edit In some types of congenital heart defect e g transposition of the great arteries prostaglandins may be administered to maintain the DA open allowing for the continual circulation and oxygenation of blood until surgery can be performed 9 Other animals EditDuctus arteriosus evolved with the lung in the ancestors of the lungfish as a connection between the pulmonary arteries and dorsal aorta During embryonic development reptiles birds and mammals all have either one or two paired ductus arteriosi that provide a fetal shunt of blood away from the lungs 10 See also EditThis article uses anatomical terminology References Edit Bamforth Simon D Chaudhry Bill Bennett Michael Wilson Robert Mohun Timothy J Van Mierop Lodewyk H S Henderson Deborah J Anderson Robert H 2013 03 01 Clarification of the identity of the mammalian fifth pharyngeal arch artery Clinical Anatomy 26 2 173 182 doi 10 1002 ca 22101 ISSN 1098 2353 PMID 22623372 S2CID 7927804 Monvadi B Srichai 2007 David P Naidich et al eds Computed tomography and magnetic resonance of the thorax 4th ed Philadelphia Wolters Kluwer Lippincott Williams amp Wilkins p 100 ISBN 9780781757652 Lucas A 1978 Prostaglandins in Patent Ductus Arteriosus The Lancet 312 8096 937 938 doi 10 1016 S0140 6736 78 91648 3 ISSN 0140 6736 PMID 81944 S2CID 54389960 a b c d Olley P M Conceani F 1981 Prostaglandins and the Ductus Arteriosus Annual Review of Medicine 32 1 375 385 doi 10 1146 annurev me 32 020181 002111 PMID 7013675 Bouayad A Kajino H Waleh N Fouron JC Andelfinger G Varma DR Skoll A Vazquez A Gobeil F Clyman RI Chemtob S 2001 Characterization of PGE2 receptors in fetal and newborn lamb ductus arteriosus Am J Physiol Heart Circ Physiol 280 5 H2342 9 doi 10 1152 ajpheart 2001 280 5 H2342 PMID 11299240 S2CID 32049750 a b Gruzdeva A Nguyena M Kovarovob M Koller B March 2012 PGE2 through the EP4 receptor controls smooth muscle gene expression patterns in the ductus arteriosus critical for remodeling at birth Prostaglandins and Other Lipid Mediators 94 3 109 119 doi 10 1016 j prostaglandins 2012 02 001 PMC 3312001 PMID 22342504 Anonucci R Zaffanello M Puxeddu E Porcella A Cuzzolin L Pilloni M Fanos V 2012 Use of non steroidal anti inflammatory drugs in pregnancy impact on the fetus and newborn Current Drug Metabolism 13 4 474 490 doi 10 2174 138920012800166607 PMID 22299823 Pritchard amp Korf Medical Genetics at a Glance Blackwell Publishing 2010 p63 Congenital heart defects Prostaglandins and prostaglandin inhibitors Healthwise My Health Alberta Dzialowski Edward M 2018 Comparative physiology of the ductus arteriosus among vertebrates Seminars in Perinatology 42 4 203 211 doi 10 1053 j semperi 2018 05 002 ISSN 1558 075X PMID 29937096 S2CID 49405282 External links EditCirculatory changes at birth at berkeley edu Retrieved from https en wikipedia org w index php title Ductus arteriosus amp oldid 1136414883, wikipedia, wiki, book, books, library,

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