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Anatomy, Thorax, Heart Foramen Ovale

Editor: Forshing Lui Updated: 7/24/2023 10:01:18 PM

Introduction

The foramen ovale is an opening or shunt in the heart tissue allowing blood to flow from the right atrium to the left atrium during fetal development. Blood oxygenated at the placenta is shunted away from the pulmonic circulation via this structure as the lungs are collapsed and not functioning and bathed in amniotic fluid.[1] When born, the ventilatory efforts by the neonate expand the lung resulting in an acute dramatic decrease in the intrathoracic pressure and permits a greater flux of blood to perfuse the pulmonary vessels. Higher pressure in the left atrium resulting from increased pulmonary venous flow from the lungs causes the septum primum of the interatrial septum to close the opening. Over time, the tissue will seal the foramen and become the fossa ovalis.

Inability to correctly close the foramen ovale can lead to multiple conditions, ranging from a patent foramen ovale to atrial septal defects. The clinical significance varies depending mostly on the size of the opening and shunts from early congestive heart failure in the case of a significant atrial septal defect to asymptomatic in small and relatively common patent foramen ovale. Treatment options for atrial septal defects have been implemented to reconstruct the atrial septum.

Structure and Function

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Structure and Function

The foramen ovale is an aperture in the muscular tissue between the left and right atrium that allows blood to cross the atria and bypass pulmonary circulation during fetal development. The surrounding tissue is composed of smooth muscle derived from the septum primum and septum secundum.[2] Since blood is oxygenated at the placenta and travels through the inferior vena cava to the right atrium, the fetal lungs are collapsed and bathed in amniotic fluid. They are not necessary for gas exchange during pregnancy.[1] In turn, the foramen ovale is the primary shunt to circumvent blood away from the lungs. The blood can pass through the right atrium and enter the left atrium through the foramen ovale through a pressure gradient. The collapse of the pulmonary arteries stops pulmonary circulation and increases the right atrial and ventricular pressures.[3] Downstream of the pulmonary circulation, the left atrium will not receive pulmonary venous blood and will have a lower pressure in the chamber. The higher relative pressure gradient of the right atrium will allow the blood to push against the tissue flap of the ostium primum and shuttle the blood into the left atrium. Effectually, the blood moves into the left ventricle and through the aorta to enter the systemic circulation.

Embryology

During heart development, the atria are separated from one another by the formation of an interatrial septum. The process of septation of the atria generally begins after the first four weeks of pregnancy and promotes the growth of distinct left and right atria.[2]

Initially, muscular tissue originating from where the right atrium would be situated begins to expand. This unidirectional growth of the septum primum with a mesenchymal cap towards the endocardial cushion is the first step towards septation and the creation of the left and right atria.[4] The endocardial cushion is a collection of cells located in the center of the heart, a site where the ventricles will become partitioned and from where the atrioventricular values will develop. As the interatrial septum proliferation (septum primum) reduces the orifice between the atria, the process of tissue growth promotes an ostium primum, a diminishing opening between atria located near the endocardial cushion. In unison, as the ostium primum becomes occluded from the developing muscular tissue towards the endocardial cushion, a portion of the interatrial septum superior to the ostium primum becomes porous through cell degeneration and creates a collective remnant opening between the left and right atria. Eventually, the porous slit above the ostium primum becomes a single orifice, denoted as the ostium secundum, the second opening formed in the process of developing the interatrial septum.

Since the ostium secundum allows the movement of fluid to cross the wall of the atria, additional steps are made to reduce the hole size. In turn, the heart generates another budding tissue at the apex of the heart, on the anatomical right side of the interatrial septum that moves inferiorly. As the septum secundum extends and covers the majority of the ostium secundum, a remnant piece of the ostium secundum remains, referred to as the foramen ovale. As a result of the septum primum and septum secundum developing as separate entities, the muscular tissues do not fuse. Consequently, the foramen ovale acts as a one-way valve. The septum primum lays behind the opening of the septum secundum, allowing fluid to move from the right atrium to the left atrium by a pressure gradient and limits backflow by the septum primum being forced against the septum secundum by higher left atrial pressure.

When the fetus is born, the act of lung expansion during the initial respiration closes the ductus arteriosus and reduces the resistance along the pulmonary arteries. Increased flux of blood through the pulmonic circulation decreases pressure in the right atrium and increases the pressure in the left atrium. A net left-to-right force in the atria causes the septum primum to obstruct the opening of the foramen ovale. Over time, the foramen ovale tissues fuse to become the fossa ovalis, a closed remnant of the foramen ovale.[5][6]

Blood Supply and Lymphatics

The interatrial septum receives vascular perfusion from the branches of the coronary arteries. Both the left and right coronary arteries, as well as the posterior descending artery, contribute to the network of blood that nourishes the tissues of the atrial septum. Since the exact blood supply of the heart varies between individuals, the assumption is that the right and left coronary arteries contribute blood for the interatrial tissue to varying degrees among people. 

Blood gets drained from the heart by cardiac veins that meet at the coronary sinus on the posterior end of the heart and funnel into the right atrium.

Nerves

Regarding the conduction pathway of cardiac action potentials, neurons that originate from the sinoatrial node pass through and along the interatrial septum to the atrioventricular node. Bachmann’s bundle allows signal transduction between the right and left atrium while multiple neuronal pathways connect the sinoatrial node, located at the top of the right atrium, to the atrioventricular node near the base of the interatrial septum.[7]

Muscles

The foramen ovale is a structure derived from muscular tissue. During embryogenesis of the heart, the septum secundum pulls the right horn of the sinus venosus into the right atrium and allows expansion of the right atrium. The right horn of the sinus venosus generates the smooth muscle of the right atrium and also contributes to the smooth muscle of the septum secundum on the wall where the foramen ovale is situated. Whereas in the left atrium, the pulmonary veins produce the smooth muscle in the chamber, which aids in the development of the atrial septum.[2]

Physiologic Variants

The size of the foramen ovale can vary between individuals. Generally, the foramen ovale is ovular and has been shown to occupy 33% of the whole developing atrial septum. Investigation shows that fetuses between 17.5 and 37 weeks in gestation with variances in the size of the foramen ovale have a risk of congenital defects. Those with lower ratios of foramen ovale size to atrial septum have associated left heart obstructive diseases, like coarctation of the aorta. On the other side, those with larger ratios have associated right heart obstructive issues, like Ebstein anomaly, pulmonic valve, or tricuspid valve abnormalities.[8][9]

Surgical Considerations

Since the foramen ovale is a structure integral during the development of the fetus, the foramen ovale should self-resolve and is generally not t a consideration for surgery during pregnancy. In the extreme circumstances where surgery is recommended to prevent additional complications associated with a congenital defect, surgery to repair the atrial septum by connecting each part may be viable.

Patent foramen ovale (PFO) currently does not have a conclusive treatment method and is still in discussion to date.[10] Most patients with an incidental finding of an asymptomatic PFO do not require any treatment. In patients with a cryptogenic stroke, especially younger patients with no other vascular risk factors, treatment will be necessary, yet the treatment method is still controversial at this present moment. Medical therapies include most commonly antiplatelets with aspirin or clopidogrel. Percutaneous closure is gaining popularity with increasing success and less invasiveness resulting in much less frequent performance of open surgical closure. Most younger patients who presented with a cryptogenic stroke and larger PFO, especially when associated with an atrial septal aneurysm will be candidates for catheter closure of the PFO.[8][11]

Clinical Significance

Enlarged Ostium Secundum - If the ostium secundum is significantly large, the septum secundum may not be able to cover the ostium secundum completely. This morphological variant will allow a persistent opening between the right and left atrium. This abnormality is the most common form of an atrial septal defect.[2]

Unsealed Ostium Primum - If the septum primum does not completely connect with the dorsal and ventral endocardial cushions and cover the ostium primum, holes in the ostium primum will persist. This variant will allow fluid to pass between left and right atria, which results in a different etiology of another atrial septal defect called ostium primum or endocardial cushion defect.

Patent Foramen Ovale (PFO) - This is the commonest congenital defect. In certain instances, the septum primum and the septum secundum may not fuse during infantile development, causing a persistent foramen ovale. Most of the time, this opening between atria is asymptomatic as the higher left atrial pressure will push the septum primum up against the septum secundum, reproducing the effects of the heart as if a fossa ovalis were present. However, a patent foramen ovale can lead to right-to-left shunting if the right atrial pressure becomes higher than the left atria, such as during the Valsalva maneuver, which may cause a stroke via a paradoxical embolus.[12][10] While most patent foramen ovale is asymptomatic and non-life-threatening, the prevalence of this remnant opening occurs in around 25% of individuals upon autopsy.[10] If the PFO is larger or when it is associated with an atrial septal aneurysm, the risk of paradoxical embolism and subsequent stroke will be considerably higher.[13] PFO also correlates with an increased prevalence of migraines. PFO is diagnosable with echocardiography, especially with agitated saline contrast. A transthoracic echocardiogram (TTE) can detect a right to left shunt with bubble contrast. A transesophageal echocardiogram (TEE) can also visualize the anatomy better including detection o the important associated atrial septal aneurysm. Transcranial doppler with bubble contrast is more sensitive than TEE in detecting a right to left shunt, yet it does not provide any clue on the site of the shunt.

Individuals who have an atrial septal defect arising from an unclosed ostium primum have increased incidences of Down syndrome.[14] Upon physical examination, an atrial septal defect will present with a fixed wide splitting of the S2 sound as a result of prolonging the pulmonary valve circulation from increased right-sided pressure.[15]

Other Issues

While the foramen ovale does not serve a functional purpose in a healthy postpartum human, the anatomical structure plays an integral role in circulating blood during embryological development. The use of the opening between the atria allows the passage of oxygenated blood to enter the left atrium from the right atrium and to bypass the lungs, which have not fully matured during fetal development. Abnormalities in the development and closure of the foramen ovale can lead to blood flow irregularities. Such conditions can lead to a patent foramen ovale or other congenital atrial septal defects. However, in specific congenital developmental abnormalities, a right to left shunt is vital for a neonate to survive after birth. Specifically, total anomalous pulmonary venous return and tricuspid atresia are notable for neonates to have a shunt similar to that of a foramen ovale.

Media


(Click Image to Enlarge)
<p>Patent Foramen Ovale

Patent Foramen Ovale. Most adult patients with patent foramen ovale are asymptomatic. In some adults, patent foramen ovale may result in an interatrial, right-to-left shunting of deoxygenated blood and the potential for shunting venous thromboembolism to the arterial circulation. 


Contributed by O Chaigasame, MD

References


[1]

Morton SU, Brodsky D. Fetal Physiology and the Transition to Extrauterine Life. Clinics in perinatology. 2016 Sep:43(3):395-407. doi: 10.1016/j.clp.2016.04.001. Epub 2016 Jun 11     [PubMed PMID: 27524443]


[2]

Jensen B, Wang T, Moorman AFM. Evolution and Development of the Atrial Septum. Anatomical record (Hoboken, N.J. : 2007). 2019 Jan:302(1):32-48. doi: 10.1002/ar.23914. Epub 2018 Oct 18     [PubMed PMID: 30338646]


[3]

Naqvi N, McCarthy KP, Ho SY. Anatomy of the atrial septum and interatrial communications. Journal of thoracic disease. 2018 Sep:10(Suppl 24):S2837-S2847. doi: 10.21037/jtd.2018.02.18. Epub     [PubMed PMID: 30305943]


[4]

Elliott GC, Gurtu R, McCollum C, Newman WG, Wang T. Foramen ovale closure is a process of endothelial-to-mesenchymal transition leading to fibrosis. PloS one. 2014:9(9):e107175. doi: 10.1371/journal.pone.0107175. Epub 2014 Sep 12     [PubMed PMID: 25215881]

Level 3 (low-level) evidence

[5]

Oduah MTA, Sharma P, Brown KN. Anatomy, Thorax, Heart Fossa Ovalis. StatPearls. 2023 Jan:():     [PubMed PMID: 30860703]


[6]

Cole-Jeffrey CT, Terada R, Neth MR, Wessels A, Kasahara H. Progressive anatomical closure of foramen ovale in normal neonatal mouse hearts. Anatomical record (Hoboken, N.J. : 2007). 2012 May:295(5):764-8. doi: 10.1002/ar.22432. Epub 2012 Feb 21     [PubMed PMID: 22354769]

Level 3 (low-level) evidence

[7]

Anderson RH, Yanni J, Boyett MR, Chandler NJ, Dobrzynski H. The anatomy of the cardiac conduction system. Clinical anatomy (New York, N.Y.). 2009 Jan:22(1):99-113. doi: 10.1002/ca.20700. Epub     [PubMed PMID: 18773472]


[8]

Abdelghani M, El-Shedoudy SAO, Nassif M, Bouma BJ, de Winter RJ. Management of Patients with Patent Foramen Ovale and Cryptogenic Stroke: An Update. Cardiology. 2019:143(1):62-72. doi: 10.1159/000501028. Epub 2019 Jul 15     [PubMed PMID: 31307049]


[9]

Feit LR, Copel JA, Kleinman CS. Foramen ovale size in the normal and abnormal human fetal heart: an indicator of transatrial flow physiology. Ultrasound in obstetrics & gynecology : the official journal of the International Society of Ultrasound in Obstetrics and Gynecology. 1991 Sep 1:1(5):313-9     [PubMed PMID: 12797035]


[10]

Ning M, Lo EH, Ning PC, Xu SY, McMullin D, Demirjian Z, Inglessis I, Dec GW, Palacios I, Buonanno FS. The brain's heart - therapeutic opportunities for patent foramen ovale (PFO) and neurovascular disease. Pharmacology & therapeutics. 2013 Aug:139(2):111-23. doi: 10.1016/j.pharmthera.2013.03.007. Epub 2013 Mar 23     [PubMed PMID: 23528225]


[11]

Alkhouli M, Sievert H, Holmes DR. Patent foramen ovale closure for secondary stroke prevention. European heart journal. 2019 Jul 21:40(28):2339-2350. doi: 10.1093/eurheartj/ehz157. Epub     [PubMed PMID: 30957864]


[12]

Anyfantakis D, Karona P, Kastanaki P, Kourakos A, Kastanakis M. Multiorgan paradoxical embolism in an elderly female with a patent foramen ovale: a case report. Medicine and pharmacy reports. 2019 Jan:92(1):83-86. doi: 10.15386/cjmed-1031. Epub 2019 Jan 15     [PubMed PMID: 30957092]

Level 3 (low-level) evidence

[13]

Sadrameli SS, Gadhia RR, Kabir R, Volpi JJ. Patent Foramen Ovale in Cryptogenic Stroke and Migraine with Aura: Does Size Matter? Cureus. 2018 Aug 27:10(8):e3213. doi: 10.7759/cureus.3213. Epub 2018 Aug 27     [PubMed PMID: 30405989]


[14]

Corona-Rivera JR, Nieto-García R, Gutiérrez-Chávez AS, Bobadilla-Morales L, Rios-Flores IM, Corona-Rivera A, Fabián-Morales GE, Zavala-Cortés I, Lugo-Iglesias C, Peña-Padilla C. Maternal risk factors for congenital heart defects in infants with Down syndrome from Western Mexico. American journal of medical genetics. Part A. 2019 Sep:179(9):1857-1865. doi: 10.1002/ajmg.a.61300. Epub 2019 Jul 19     [PubMed PMID: 31321895]


[15]

Matsumoto T, Tamiya E, Kanoh T, Takabe T, Kuremoto KI, Kamiyama T, Yamamoto S, Daida H. Atrial Septal Defect of the Ostium Secundum Type in A 101-Year-Old Patient. International heart journal. 2019 Mar 20:60(2):489-491. doi: 10.1536/ihj.18-354. Epub 2019 Feb 22     [PubMed PMID: 30799379]