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Acyanotic “Taussig-Bing heart” and its surgical aspects

Case report | DOI: https://doi.org/10.31579/2834-8508/035

Acyanotic “Taussig-Bing heart” and its surgical aspects

  • Ramachandran Muthiah

President of all Nations, Morning star hospital, Enayam Thoppu, Kanyakumari District, India

*Corresponding Author: Ramachandran Muthiah, President of all Nations, Morning star hospital, Enayam Thoppu, Kanyakumari District, India.

Citation: Ramachandran Muthiah (2024), Acyanotic “Taussig-Bing heart” and its surgical aspects. Archives of Clinical and Experimental Pathology. 3(6); Doi:10.31579/2834-8508/035

Copyright: © 2024 Ramachandran Muthiah, This is an open access article distributed under the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.

Received: 21 November 2024 | Accepted: 09 December 2024 | Published: 24 December 2024

Keywords: double-outlet right ventricle, ventricular inversion, subpulmonary VSD, L-transposition, Left-sided Ebstein’s anomaly

Abstract

Aim: To report a case of acyanotic Taussig-Bing heart, anatomically consistent with L-transposition and rheumatic Left AV valve regurgitation associated with complete AV block in a male child. 

Introduction: Taussig-Bing heart is one of the conotruncal malformation, characterized by double-outlet right ventricle (DORV) and a subpulmonary VSD. Embryologically, abnormal cardiac looping and malalignment of conotruncal septum determines its complexity and great artery relationships.

Case Report: A 14-year-old acyanotic boy presented with severe left-sided AV valve regurgitation and bradycardia. ECG revealed left sided morphologic right ventricular hypertrophy (RVH) as evidenced by a loss of septal Q waves in left precordial leads suggesting ventricular inversion. X-ray chest revealed a straight upper right cardiac border due to loss of normal relationship of great vessels and cardiomegaly due to both left atrial and morphologic right ventricular enlargement suggesting a left-sided regurgitant lesion. Echocardiography revealed the ventricular inversion, primary origin of both L-transposed great arteries from the left-sided morphologic right ventricle suggesting a ‘double-outlet morphologic right ventricle’ with ‘double discordance’ and a subpulmonary VSD of Taussig-Bing type. The left-sided morphologic tricuspid valve is severely regurgitant due to rheumatic process resulting in heart failure which was improved with anti-failure measures and penicillin prophylaxis

Conclusion: The presence of left-sided regurgitation associated with bradycardia is a suspicion of ‘double discordance’ and ‘double switch’ procedure remains the mainstay of its surgical correction. Left AV valve replacement with intraventricular repair is preferred in this child since the malformation is consistent with Taussing-Bing type of DORV with L-transposition.

1.Introduction

Taussig-Bing heart” is a morphological subtype of double-outlet right ventricle (DORV) with subpulmonary VSD (ventricular septal defect) [1]. It was first described in 1949 by two outstanding physicians, Helen Brooke Taussig and Richard John Bing, who worked together at the John Hopkins Hospital in Baltimore. The original “Taussig-Bing heart” [2] may be summarized as a double-outlet right ventricle (DORV) with semilunar valves side-by-side and approximately at the same height, a bilateral conus, and a subpulmonary VSD. This original description has been broadened to include all kinds of double-outlet right ventricle with subpulmonary VSD [3],[4]. The morphological variability of “Taussig-Bing  heart” is guided by the relationship between great arteries [5] and ventricles that are associated with a bilateral conus [6],[7] and so this case had been reported.

2. Case Report

A 14-year old boy was admitted with features of heart failure in the intensive care unit. His pulse rate was 50 bpm and blood pressure 110/70 mmHg. He had a history of rheumatic fever during childhood and blood chemistry revealed a positive ASO (anti-streptolysin O) titer. Auscultation revealed a grade 4/6 pansystolic murmur over the LV apex with a shift of apical impulse to left 6th space towards mid- axillary line. ECG  revealed high-grade  AV block with features of ventricular inversion and strain pattern due to morphologic RVH as shown in Figures 1 and 2, compared to a normal right-sided  pattern as in Figure 3 with normal echocardiography  as in Figure 4 of a normal male child of similar age. X-ray chest revealed a narrow vascular pedicle with left atrial and morphologic right ventricular enlargement as shown in  Figure 5.  Transthoracic echocardiography revealed a VSD with inlet extension as in Figure 6 and a discordant relationship between atria and ventricles and a left-sided Ebstenoid morphologic tricuspid valve as shown in Figure 7 with leaflets showing the features of rheumatic etiology as in Figure 8 to 10. The leaflets are severely regurgitant as shown in Figures 13 to 16.

The child was treated with anti-failure medications such as diuretics, angiotensin-converting enzyme inhibitors (enalapril) with penicillin prophylaxis and the regurgitant lesion became decreased as shown in Figures 17 and 18 and M-mode mRV  study showing the marked improvement in ejection fraction from 36% to 46% as shown in Figures 21 and 22. 

Since the great arteries are primarily originating from morphologic RV as in Figure 23 and it is L-transposed with side-by-side relationship as in Figure 24 with a subpulmonary VSD, it is consistent with Taussig-Bing anomaly of L-transposition, a Kawashima intraventricular repair was advised if further deterioration of mRV function occurs on periodic follow-up with a continuation of medical treatment along with lifelong penicillin prophylaxis. Palliative procedures are not indicated in this child since there is no aortic arch obstruction and outflow tract lesions as shown in Figure 25 and 26.

(Figure 1- ECG showing complete AV block with narrow  QRS (QRS duration < 120>

Figure 2. ECG showing the QS complexes in inferior leads (L11,III, aVF) and a QS pattern in right-sided chest leads, compared to a normal ECG of right-sided leads  in the same age of a male child as in Figure 3.

Figure 3. ECG showing RS complexes in the right sided leads of a normal 14-year old boy.

Figure 4. X-ray chest (postero-anterior) view showing the narrow vascular pedicle since great arteries are not border forming, appears straight due to loss of normal relationship between  arterial trunks as ascending aorta is typically not visualized on the right side, convexities from descending aortic knob and pulmonary trunk are absent  on the left side due to posteriorly positioned pulmonary artery suggesting L-transposition. The cardiomegaly is due to aneurysmal Left atrial (LA) enlargement and a dilated morphologic right ventricle (mRV). The visceral situs is normal.

Figure 5. Apical view showing the normal atrioventricular relationships, AV valves (mitral and tricuspid) attachments and the shape of ventricles in a normal 14-year old boy

Figure 6. Apical view showing the VSD (ventricular septal defect) with inlet extension

Figure 7. Apical view showing the ‘Ebstenoid malformation” of left-sided morphologic tricuspid valve (mTV) , The mTV is identified by a long and elongated posterior leaflet which is short in mitral valve as in Figure 5 of a normal 14-year old boy and a discordant AV connection.

Figure 8. Subcostal view-long sweep –showing the thick, calcified morphologic tricuspid valve (mTV) with commissural fusion due to rheumatic etiology.

Figure 9. Subcostal view-showing the calcification and thickening which is more prominent at leaflet tips due to rheumatic involvement, the normal tricuspid annulus (30 mm) and a dilated morphologic right ventricle (mRV) (65 mm)

Figure 10. Subcostal view showing the marked rheumatic involvement of posterior leaflet of the morphologic tricuspid valve (mRV)

Figure 11. Subcostal view showing the normally attached rheumatic morphologic tricuspid valve and the pulmonary valve.

Figure 12. Subcostal view- long sweep showing the subpulmonary conus

Figure 13.  Apical view showing the severe tricuspid regurgitation (TR)

Figure 14. Apical view showing the tricuspid regurgitation jet, originating from the posterior tricuspid leaflet (PTL) swirling around the interatrial septum.

Figure 15. Apical view showing the tricuspid regurgitation jet, originating from the septal tricuspid leaflet (STL) swirling around the lateral wall of left atrium.

Figure 16. Subcostal view showing the severe tricuspid regurgitation originating from the posterior tricuspid leaflet (PTL) swirling around the interatrial septum

Figure 17. Apical view view showing the decreasing in regurgitant jet due to aggressive medical treatment

Figure 18. Subcostal view showing the marked decrease in regurgitant jet due to aggressive medical treatment

Figure 19. Subcostal view showing the “ sail-like” deformity of posteriot leaflet of morphplogiv tricuspid valve.

Figure 20. Subcostal view showing the normal attachments of morphologic tricuspid (mTV) and mitral valves (mMV) to the annulus

Figure 21. M-mode mRV study showing the severe dysfunction of morphologic right ventricle (mRV). EF – 36 %.

Figure 22. M-mode mRV study showing the improvement in RV function following aggressive medical measures- EF 46%

Figure 23. Subcostal view-short sweep showing the primary origin of great vessels from the morphological right ventricle (mRV) and it is side-by-side (L-transposition)

Figure 24.  Basal short axis view showing the great arteries seen as circles

Figure 25. Showing the dilated pulmonary trunk in Taussig-Bing heart and there is no obstructive lesions.

Figure 26. Suprasternal view showing the normal aortic arch

3.Discussion

Review of literature

Taussig-Bing suspected a totally different malformation at autopsy in a five and a half year old girl who had cyanosis since birth and died during angiocardiography  after a third intravenous injection of contrast material, the diodrast, the child sat bolt upright and the heart stopped. The malformation consists of a transposed aorta, a large pulmonary artery which arises primarily from the right ventricle and partially overrides the ventricular septum, a high ventricular septal defect, and right ventricular hypertrophy. Maurice Lev was one of the first to call this anomaly as “Taussig-Bing syndrome”[8].

This anomaly was initially described in 1949 by Taussig and Bing as transposition of the great arteries. The important difference between Taussig-Bing anomaly and transposition of the great arteries were described by Richard Van Praagh in his editorial review and stressed that the absence of pulmonary-mitral continuity is the characteristic feature of this anomaly. Taussig and Bing emphasized that the overriding of pulmonary artery was an integral part of this malformation. This anomaly was eventually named as “Taussig-Bing heart” in 1950 by Lev and associates [9] and subsequently introduced the spectrum of Taussig-Bing hearts depending on the degree of pulmonary artery overriding (right-sided, intermediate, and left sided) [10].

DORV is a heterogeneous groups of conusarteriosus malformations and its anatomy was first described by Mery in 1703 [11] and the term”double-outlet ventricle” was introduced by Braun, et al [12] in 1952 and thereafter, Witham described “double-outlet right ventricle” as a ‘partial transposition complex’ in 1957 [13]. In 1983, Birmingham first described the “Double-outlet right ventricle (DORV)” as both great arteries (pulmonary and aorta) arise primarily from the morphologic right ventricle. In 1962, Neufeld defined it as “both great arteries and arterial trunks are exclusively arise from the morphologic right ventricle, neither semilunar  valves is in fibrous continuity with atrioventricular valves[14].  Lev and Anderson, et al[15] defined DORV as “all of one great artery or more of the other artery must arise from the right ventricle” or “an anomaly in which two cusps and part of third of both the semilunar valvesarise from the right ventricle“. These great arteries may override the ventricular septum by > 50% ( > 50% of each of the great vessels arise from the morphologic right ventricle, which is known as “50% rule”), 90% or both arteries arise fully from the right ventricle (200%) [16].In 1972, Lev, et al [17] used the relationship of VSD to the great arteries to categorize its subtypes.  Van Praag proposed a classification system to describe the primary malformations of the outflow tract as type 1 DORV, with additional malformations of the AV canal, AV valves, ventricles, venous and arterial connections as type II and with defects in cardiac lateralization as type III. Taussig-Bing heart is a form of type II DORV (ie, DORV of Taussig-Bing type) and all cases of juxta-pulmonary VSD with double subarterial conus (bilateral infundibulum) due to malalignment of infundibular septum as a fundamental requisite to define these hearts, collectively termed as “ Taussig-Bing complex”.

Thus, defining the Taussig-Bing heart has been the subject of some controversy as whether it is indeed a double-outlet right ventricle or whether the pulmonary artery trunk “overrides” the left ventricle and most authors of surgical reviews described it as “double-outlet right ventricle,  sub pulmonary VSD, and subarterial  conus or coni”.

Etiopathogenesis

The Taussig-Bing anomaly is relatively rare and it accounted for approximately 8% of cases in Sridaromont series [18]. In these cases, the pulmonary stenosis does not occur, the pulmonary trunk is markedly dilated as in Figure 25 and there is a high VSD immediately subjacent to the pulmonary valve (sub pulmonary) and the pulmonary valve is not in continuity with AV (atrioventricular) valve because of interposed sub pulmonary conal free wall musculature as in Figure 12. The anatomic feature of Taussig-Bing malformation appears to result from marked and symmetrical development of both conal free walls. The semilunar valves have been protruded anteriorly to about the same extent by the underlying conal musculature and remain side-by-side, so that both great arteries arise above the anterior (right) ventricle and the failure of complete absorption of the conus or coni result in fibrous discontinuity with atrioventricular valves.

During the development of the heart, the outflow tracts initially connects exclusively with the primitive right ventricle and undergo extensive remodeling to divide into aorta and pulmonary artery with connection to left and right ventricles respectively. Goor and Edwards {19} stated that double-outlet right ventricle appears to represent a primitive embryologic condition as failure to achieve conotruncal inversion and leftward shift of conus results in persistence of this condition with complete origin of both great arteries from the morphologic right ventricle. The primitive cardiac tube anchored at one end by the sinus venosus and at the other end by truncus arteriosus. The chambers of the heart develop by ballooning from the primary heart tube  as atrial appendage ballooning in parallel to the atrial component of the tube and the apical component of the ventricle balloons in series from the inlet and outlet parts of the ventricular loop. The ‘looping’ of the straight heart tube during the 3rd week of gestation is one of the key embryologic process leading to anatomic alignment of chambers of the heart and it normally ‘loops’ to the right (D-loop) resulting in normal morphological position of right ventricle  to the right side. The abnormal cardiac looping to the left side (L-loop) brings the morphologic right ventricle to the left and the ventricles are reversed (ventricular inversion), the atrioventricular valves ‘follow’ the ventricles and the two great arteries are transposed or exit from the ‘wrong’ ventricle, but the systemic venous blood flows from the morphologic left ventricle to the pulmonary artery and the systemic arterial blood flows from the morphologic right ventricle to the aorta and so the circulation is corrected. Thus, during embryologic development, left-handed looping of the heart tube results in AV (atrioventricular) discordance and the aorto-pulmonary septum fails to rotate 180⁰ , resulting in ventriculoarterial discordance. This heart defect is called as ‘corrected transposition’ by Baron Rokitansky in 1875 and described as ‘Rokitansky’s malformation’ [20] in 1957  or L-transposition (Levo-transposition) or ‘ventricular inversion’ and subsequently designated as ‘congenitally corrected transposition’(ccTGV) by Schiebler since the correction was a gift of God, rather than the gift of the surgeon [21]. Abnormalities of the morphologic tricuspid valve (left AV valve) was seen in 90% of L-transposition  in autopsy series and significant Ebstein-like malformation of left AV valve, ie, the septal leaflet is displaced inferiorly towards the cardiac apex [22] as in Figure 7, 17 mm apical to the right-sided mitral valve (normally the distance between the tricuspid and mitral annulus is < 8>Figure 19 which is rarely seen in left-sided Ebstein’s malformation. The unusual disposition of the conduction tissue that predisposes to spontaneous AV block [25] as in Figure 1, occurs in 1/10thofinfants born with this anomaly [26],[27] with an incidence of 2%/year [28], as 45% will have developed third-degree AV block on 20-year follow up [29] and it reaches a prevalence of 10 to 15% by adolescence and 30% in adulthood [30]. In older patients, fibrotic invasion of proximal and distal bundle branches was involved in its pathogenesis.

The tricuspid valve tends to remain competent during the first decade of life, but progressively become incompetent during the 2nd to 5th decade in 20 to 50% of patients and it has been implicated as a cause of ventricular dysfunction due to volume overload. Since the morphologic right ventricle is in the systemic position, it is unable to generate the necessary  forces to sustain the increasing work demand , such as exercise , similar to normal systemic left ventricle [31] due to the loss of special twisting motion during systole and early diastole [32] as it lacks the helical myocyte arrangement seen in left ventricle. The RV muscle mass  increase significantly since it is subjected to systemic pressure, leading to right ventricular hypertrophy (RVH0 as in ECG shown in Figure 1.

The VSD is neither membranous nor conal septal defect and it is due to its malalignment of well developed distal conal free walls, the parietal and septal bands may separate or dissociate widely in Taussig-Bing malformation. In L-TGA, the VSDs occur in 60-80% of cases, usually perimembranous, located below the pulmonary valve, extends posteriorly and inferiorly towards the crux of the heart and opening into the inlet of the morphologic left ventricle as in Figure 6. Endocardial cushions in the outflow tract are responsible for the formation of semilunar valves and the development of conal septum (the portion of ventricular septum between the distal ventricular outflow tracts). During conus malrotation, changes in position of anterior portion of the muscular interventricular septum and differential conus absorption leads to malposition of great artery relations. In S.L.L. type of ccTGV [33] (S-situs solitus of the viscera and atriaI, L-loop ventricle, L-transposition of great arteries), deviation in the normal development of interventricular septum as the ventral limb of the left interventricular sulcus on the primary heart tube gives rise to a left-sided crista supraventricularis, which, determines, in part,the right ventricular morphology of the left-sided ventricle. The dorsal limb spirals towards the atrioventricular canal, giving rise to a malpositioned  interventricular septum, and displaces the embryologic right ventricle to the left. The course of outlet septum establishes the alignment of VSD with great arteries. If the outflow tract is straight and parallel to the trabecular septum, the VSD becomes subpulmonary and the extreme leftward rotation of the aorta resulting the great arteries nearly in a side-by-side relationship, with the aorta to the left.

The molecular and biological forces that dictate the abnormal cardiac looping in humans are not clear. Cytogenetic analysis identified the discrete chromosomal lesions in the morphogenesis of the heart and appears to be associated with subtypes of DORV. Type 1 DORV is associated with chromosome 22q11 deletion, the type II with trisomy 13 or 18.  The transcription factors such as Nkx 2.5, Gate 4 and Tbx 20 are postulated to influence the right ventricular development via IsI 1, Mef2c and Hand 2 pathways and Pitr 2, Fgf8,Fgf 10 are essential for the development of great arteries [34]. Type 1 DORV might reflect the abnormalities of neural crest cells  necessary for the normal outflow tract development and the TGFβ superfamily genes (activin type IIB receptor, noggin, TGFβ2 ), Sox4[35], NF1,RAR genes, Endothelin converting enzyme genes (ECE-1, ECE-2) and Pax 3 genes play a role.Mutations of Gate 4 gene has a potential for the development of type II DORV. Genes determining the body plans such as Pitx 2, CFC1, Cx43 (left-right axis determination), Hox 1.5 (rostral-caudal specification) and  jefty 1, inversin (abnormalities of situs and looping) for type 111 DORV and mutations in several other genes had been implicated in few cases of human DORV pertinent to animal models[36],[37]. Recently, it is noted that there is a relationship between primary ciliary dyskinesis (PCD) and ccTGV [38]. The association between cilia and cardiogenesis was made in a baby chick and Willaredt et al [39] found a link between Sonic hedgehog signaling at the primary cilium and the role of bone morphogenic protein in the cardiogenesis of endocardial cushions.

Animal studies also implicate diverse teratogens , the commonly used drugs (ephedrine, theophylline, sodium valproate, retinoic acid/vitamin A, tedral (combination of theophylline, ephedtine, phenobarbitone), other agents including bis-diamine, bromodeoxyuridine), copper citrate, environmental factors such as hair dye, air pollutants [40] and maternal diabetes are enhancing the susceptibility of DORV phenotypes.

Echocardiographic features

Transthoracic echocardiography is the first line modality to assess the specific relations of the different segments of the heart and to determine the presence of any associated malformations. The anatomical designation is first assigned by demonstrating atrial position, ventricular and arterial loopings. The morphology of right ventricle is determined by the presence of coarse trabeculations, moderator band and the level of tricuspid valve, which is inferior (apical)to mitral valve, also give a clue to ventricular inversion as shown in Figure 7. The morphology of tricuspid valve is characterized by a long, elongated posterior leaflet and a short septal or anterior leaflet. . in comparison to mitral valve in which the posterior leaflet is short and the anterior leaflet is long and elongated as in Figure 5. The morphologic TV (tricuspid valve) is a systemic AV valve and its septal leaflet is abnormally displaced inferiorly.This systemic AV valve (mTV) is anatomically abnormal, that predicts the occurrence of regurgitationand transthoracic echocardiography is the technique of choice to evaluate the etiology of TR (tricuspid regurgitation) and in most cases, it is so called “functional” (secondary TR (tricuspid regurgitation) due to dilatation of annulus (diastolic diameter > 40 mm or 21 mm/m2) as a consequence of RV dilation secondary to pulmonary hypertension. In 15 to 20% of cases, the injury to tricuspid valve can be organic and generally of rheumatic in origin. The morphologic TV (mTV) is thickened calcified as in Figure 7 , more prominent at leaflet tips as in Figure 9 with commissural fusion as in Figure 8, the posterior tricuspid leaflet is predominantly affected as in Figure 10 and it is severely regurgitant as shown in Figures  13 to 16, the annulus diameter is 30 mm (< 40>Figure  9.

The anatomic objective such as “double discordance”, ie, discordant connection at both atrioventricular and ventriculo-arterial junctions can be defined by echocardiography. The discordance between the atrium and ventricle as left atrium is connected to the morphologic Right ventricle (mRV) and the right atrium is connected to the morphologic left ventricle (mLV) was shown in Figure 7 .

The origin of great arteries in relation to the septum and its spatial relationships are best visualized in subcostal coronal views. Figure 23 shows the origin of both great arteries primarily from the morphologic RV (mRV), it is parallel to each other (normally cross each other) and the pulmonary trunk is identified by its bifurcation into right and left branches. The great arteries appear as double circles in basal short axis view as in Figure 24 with posterior ‘sausage’ caused by the main pulmonary artery segment, transected tangentially and an anterior circle which is the aorta, positioned leftward, anterior and superior to the pulmonary artery [41] suggesting  L-transposition. The subcostal coronal view also help to determine the lack of fibrous continuity  between the posterior semilunar valve (pulmonary) and the anterior tricuspid leaflet as in Figures  9 and 10 and suggesting double-outlet right ventricle with a subpulmonary VSD (Taussig-Bing type).  In about 50% of cases of Taussig-Bing anomaly, the congenital malformation of the aorta including coarctation, isthmic hypoplasia, interruption, patent ductus arteriosus and subaortic conus may occur [42],[43]. The aorta is identified by its brachiocephalic branches, but the aortic arch appears normal in this patient as shown in Figure 26.

Management

Systemic AV valve regurgitation is a potential risk factor for the development of dysfunction of the morphologic RV and early heart failure [44] and those patients without such complications (ie, in the absence of hemodynamic lesions) appear to function well into late adulthood in ccTGV [45],[46]. Medical management with diuretics, afterload reduction with angiotensin converting enzyme inhibitors such as captopril and digoxin (inotropic) is adapted for the failing systemic right ventricle [47], depending on the severity of associated malformations [48]. The role of angiotensin receptor blocker with  losartan was evaluated and found to have no improvement in exercise capacity and no reduction in neurohormonal levels in patients with systemic right ventricle [49]. Beta blockers did not improve outcome in a randomized trial included pediatric patients with systemic RV dysfunction [50] and must be used cautiously in ccTGV patients as they may precipitate AV block, but an improvement in systemic ventricular function occurred after carvedilol (a vasodilatory beta blocker) administrationin a 80-year old woman with ccTGV [51], Aggressive medical treatment with afterload reduction is indicated for patients with ventricular enlargement and early symptom. The benefits of prophylactic use of vasodilators is unproven to delay or prevent systemic ventricular dysfunction. 

Interventional therapy

In patients with widened QRS complex (QRS duration > 120-140 ms, sometimes >200ms) due to bundle branch blocks, the electromechanical dyssynchrony create insufficiency in ventricular ejection and restoration of electrical synchrony with transvenous permanent para-Hisian pacing (cardiac resynchronization therapy) reduces the QRS duration and improves the hemodynamics of the failing systemic right ventricle [52],[53], but is technically challenging [54]

Complete heart block is also a common cause of death [55]. Early pacemaker placement is recommended in the setting of complete heart block if there is RV dysfunction, symptoms of bradycardia or heart failure and urgently done if it occursduring or after the surgical intervention when the bradycardia is intolerable. It can be technically challenging pertaining to the complex heart anatomy [56] such as modification in position of ventricular septum that induces a septal shift and failure of tricuspid valve coaptation [57] leading to worsening of systemic ventricular function and AV valve regurgitation.

Surgical therapy

The evolution of surgical repair for the Taussig-Bing anomaly has progressed from atrial baffle procedures to arterial switch with VSD closure and intraventricular repair. The need for surgical interventions vary according to the associated defects and several options are available as

  1. physiologic or conventional repair- which emphasizes the correcting of associated defects without addressing the discordant connections and leaves the morphologic RV to propel the systemic circulation. The tricuspid valve and morphologic RV function is the Achilles heel of the physiology of ccTGV [58],[59]. Timely performed systemic AV valve replacement may preserve ventricular function, improves long-term outcome [60] and should be done  prior to significant RV dIlation in symptomatic patients and a preoperative ejection fraction of ≥ 40%. Systemic AV valve repair have had disappointing intermediate and late results [61].
  2. Anatomical repair- In physiological correction, the morphological RV will likely to fail over long-term, there is an increasing trend towards anatomical correction by “switch procedures” introduced in 1987 by Ilbawi and colleagues with an aim to utilize the morphologic LV as a systemic pumping chamber and the mitral valve as the systemic valve [62]. The goal of anatomic correction is the rerouting of the pulmonary venous return to mLV(morphologic LV) and aorta, the systemic venous return to mRV(morphologic RV) and pulmonary artery that achieving a normal anatomical pattern of circulation., ie, morphologic LV to aorta and morphologic RV to pulmonary artery.

It represents a group of procedures in which AV discordance is corrected by an inflow, baffling procedure at atrial level, called as atrial or venous switch (Mustard or Senning) and the ventriculo--arterial discordance is corrected by either an outflow procedure at arterialor ventricular level, called as arterial or ventricular switch or by translocation of the aortic root (Jatane procedure) and collectively termed as “ double-switch”. The choice of procedures depending on the underlying anatomy of LVOT/or morphology of VSD [63]. A modification of atrial switch procedures to a hemi-Mustard technique can be performed to overcome the high early morbidity and mortality in more complex  ccTGV patients to decrease the surgical challenge [64].

The indication for anatomic repair for those with a “balanced” systemic and pulmonary blood flow without clinically significant cyanosis is still unclear. Current indication for ‘double switch’ operation include patients who have developed symptoms attributed to tricuspid regurgitation or RV dysfunction or both [65]. The anatomic repair is currently the first choice for most surgeons in treating ccTGV [66], only meant for patients with a favourable anatomy [67]and it remains the best choice for TGA type of DORV [68]. Early prophylactic pulmonary banding [69] as a bridge to ‘double switch surgery’ related to LV retraining in selected asymptomatic young infants with isolated ccTGA is a challenging practice to expand anatomic repair in those patients who suffer from persistent late LV failure due to LV retraining.

For patients with Taussig-Bing type of DORV, the ‘arterial switch’ operation still appears to be the procedure of choice and can be performed in the neonatal period[70] and also in patients with all types of great artery anatomy without ventriculotomy. The arterial switch for Taussig-Bing heart was first reported byin 1981 [71]. The issue of great artery anatomy was first addressed by Yacoub and Radley- Smith [72] and many surgeons have thought that the side-by-side great arteries are most suitable for intraventricular repair (Kawashima repair) [73],[74], which is also applicable to unusual coronary artery anatomy or a pulmonary valve that is not considered adequate to function as a systemic valve. The antero-posterior great arteries are most suitable for arterial switch with a closure of VSD.. The distance between the tricuspid and pulmonary valve for an intraventricular tunnel [75] is more important than the great artery relations and in side-by-side great arteries, the conduit can pass posteriorly and allow unimpeded flow to the pulmonary valve, ie, by tunneling the left ventricular flow posterior to the pulmonary valve. The operative mortality for arterial switch is13%, 3% for intraventricular repair and late mortality for both series is 5 to 6%.

  1. Single -ventricle palliation -  such as ‘Fontain circulation’(redirection of systemic (deoxygenated) blood into the pulmonary artery without traversing a ventricle) should be considered in more complex and unfavourable anatomy  due to small RV, chordae straddling and remote VSD, however, it may affects the organs outside the heart leading to cirrhosis, protein loosing enteropathy and  plastic bronchitis [76]

Outcome.

In patients without tricuspid valve regurgitation, the survival rate at 20 years is > 90% and it is < 50> 40%, the patients do reasonably well. In addition,  a number of reports of ccTGA in adults come to medical attention for either cardiac or non cardiac reasons in 6th to 8th decade, indeed, the right ventricle can function as a systemic ventricle for many tears [77].

Case Analysis

The 14-year old boy was presented with features of “double discordance” (Figure 7) with primary origin of L-transposed great arteries from the left-sided morphologic right ventricle (Figure 23) and a pulmonary-tricuspid discontinuity with well developed pulmonary conus (Figure) and a malaligned subpulmonary VSD (Figure 8), suggesting a “Taussig-Bing heart”  with L-transposition. The visceral situs was normal (Figure 4)  and there Is a marked RV dilatation (Figure 9) with severe tricuspid regurgitation (Figures 13 to 16) due to rheumatic etiology (Figures  8 to 12) and so it is designated as “Rheumatic Taussig-Bing heart”. 

The septal malalignment in situ solitus alters the cardiac hemodynamics and conduction pathways, leading to increased risk of complications. The atrial and ventricular septa are malaligned  and the AV node cannot penetrate the ventricular mass, indeed, a secondary node penetrates the anterior septum, predisposing to high grade atrioventricular block [78] (Figure 1) with a tolerable heart rate (50 bpm) due to congenital etiology. The septal malalignment in situs solitus also leads to a high prevalence of Ebstein-like anomalies and 50% of ccTGV patients had abnormal tricuspid valve , compared to normal in situs inversus group. The  left-sided Ebstenoid-like malformation of mTV as in Figure 7  (apical four chamber view) is due to septal malalignment, mimicking as apical displacement of septal tricuspid leaflet which is normally attached to annulus as in Figure 20 shown in subcostal views with a subpulmonary VSD (Figure 10) as the result of this septal  malalignment.

On aggressive medical management with antifailure measures and penicillin prophylaxis, the severe tricuspid regurgitation decreases as shown in Figures 17 and 18. It is a primary tricuspid regurgitation due to rheumatic involvement of mTV and the tricuspid annulus is not dilated (< 40>Figure 9 which is an usual feature of secondary TR due to pulmonary hypertension. The mRV  function improves from the severe dysfunction (Figure 21- EF 36%) to a moderate degree (Figure 22- EF 46%).

The boy remains acyanotic with an improvement in hemodynamic status, the medical measures are continued with lifelong penicillin prophylaxis and advised periodic echocardiographic evaluation to assess the ventricular function. Since the left-sided morphologic RV is a systemic pumping chamber, it is hypertrophied (Figure 1) and may deteriorate in function on long-term follow-up. Since the both ventricles are adequate without any outflow tract obstructions (Figures 25, 26 ) and the great arteries are in side-by-side, the Kawashima intraventricular repair is the preferred surgical option with tricuspid valve replacement  in this child. The pacemaker implantation is necessary when the heart rate becomes intolerable especially during surgical procedures.

4. Conclusion

Taussig-Bing heart is one of the variants of double-outlet right ventricle (DORV) and it  constitues < 10>

References

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