We thank dr. Katsouras for his response to our long-term EXPLORE manuscript (1). We agree that in the ST-segment elevation (STEMI) population the presence of collaterals to the concurrent chronic total occlusion (CTO) is of prognostic relevance. We previously reported in 413 consecutive STEMI patients with a CTO that the presence of well-developed collaterals to the CTO compared to poorly developed collaterals was associated with improved outcome. We also assessed the influence of the collateral origin on survival, as collaterals coming distally from the culprit lesion are (partially) blocked during the acute phase of STEMI. In 16% of the patients the collaterals originated directly or distal from the culprit lesion and these patients had a lower survival compared to the patients in whom the collaterals were not blocked during STEMI (2).

In the EXPLORE trial patients with well-developed collaterals to the CTO had a significantly better left ventricular (LV) function at 4 months follow-up. Nonetheless, we did not find a significant treatment effect of CTO-PCI on global LV function nor on clinical outcome in patients with poorly developed nor with well-developed collaterals (3). On a regional level we found that the recovery of segmental wall thickening of the dysfunctional CTO myocardium was better in patients with well-developed collaterals. However, no significant interaction of collateral quality on the effect of CTO PCI was found (4). In EXPLORE there were 34 patients (11%) with no visible collaterals or collaterals originating from the IRA occluded during STEMI. These patients had a significantly lower LVEF (38% versus 45%, p=0.001) and a higher LVEDV (226ml versus 213ml, p=0.37) at 4 months follow-up. Long-term MACE rates were also numerically higher in this group (20% versus 12%, Log-rank p=0.21). Mortality rates were not different between both groups (9.4% versus 9.3%, Log-rank p=0.40). We did not find an effect of CTO-PCI on LV function nor on clinical outcome in the patients with collaterals blocked during STEMI nor in patients with present collaterals.

Therefore, data regarding the value of the collateral circulation are conflicting and their exact role remains controversial. Further CTO research should focus more on the collateral circulation to determine whether collaterals should be of influence on treatment strategies or whether they are just unmodifiable markers of prognosis in these complex patients.

References:
1. Elias J, van Dongen IM, Ramunddal T, et al. Long-term impact of chronic total occlusion recanalisation in patients with ST-elevation myocardial infarction. Heart 2018 doi: 10.1136/heartjnl-2017-312698
2. Elias J, Hoebers LPC, van Dongen IM, et al. Impact of Collateral Circulation on Survival in ST-Segment Elevation Myocardial Infarction Patients Undergoing Primary Percutaneous Coronary Intervention With a Concomitant Chronic Total Occlusion. JACC Cardiovasc Interv 2017;10(9):906-14. doi: 10.1016/j.jcin.2017.01.026
3. Van Dongen IM, Elias J, Van Houwelingen KG, et al. P5156Impact of collateral filling on LVF and survival in STEMI patients with a concomitant CTO. An explorative subanalysis of the EXPLORE trial. European Heart Journal 2017;38(suppl_1):ehx493.P5156-ehx493.P56. doi: 10.1093/eurheartj/ehx493.P5156
4. Elias J, van Dongen IM, Hoebers LP, et al. Improved recovery of regional left ventricular function after PCI of chronic total occlusion in STEMI patients: a cardiovascular magnetic resonance study of the randomized controlled EXPLORE trial. J Cardiovasc Magn Reson 2017;19(1):53. doi: 10.1186/s12968-017-0369-z

I read with interest the bright review of stable coronary syndromes (1). In the formation of the fetal muscular part

of the interventricular septum (IVS), the expanding ventricles grow and their medial walls approach and fuse, forming

the septum. The inside corner between the septum and the right anterior ventricular wall exhibits the deep pits being

called interventricular sinuses (ISs). The IS passes through the right IVS formed from the medial wall of the expanding

fetal right ventricle (RV). The opening of the interventricular vessel (IV) (kuuselian vessel) is located in the IS between

the medial walls of the expanding fetal RV and fetal left ventricle (LV). The IV is not a canal or channel or blood

vessel, but a slit between the fibres of the muscle to the outer layer of the left central muscular part of the IVS and runs

at an angle of about 90 degrees through sphincter and the left IVS into the LV. The IV exhibits 2 to 3 oval 2x5 mm

openings in the left central muscular part of the IVS surrounded by the interventricular sphincter (ISP). The ISP and the

IV are feasible to be patent by relaxing and widening of the helical heart at the right atrial filling phase at the end of the

fetal diastole. The left to right communication do not result as the earliest left ventricular activation close the ISP. The

sinoatrial node initially activates the right atrium (RA), followed by activation of the left atrium (LA). An abnormal

fourth heart sound is common in hypertrophy of systemic hypertension and in ischemic heart disease, because the atrial

´booster pump´ is needed to assist the relatively stiff ischaemic ventricle. The fourth heart sound disappears when

coordinated atrial contraction ceases, as in atrial fibrillation (2). Hypoxia may be the physiological factor to recruit the

fetal IV and augment the flow of venous blood from right to left (3). The LV may develop negative pressure and

sucking effect at the early diastole of the normal heart (4).

References

1. Ford T J, Corcoran D, Berry C: Stable coronary syndromes: pathophysiology, diagnostic advances and

therapeutic need. Heart 2017 Oct 13. pii:heartjnl-2017-311446. doi10.1136/heartjnl-311446. [epub ahead of print]

Review.

2. Kuusela P J: The Heart exhibits right to left Communication between the fibres of the muscular part of the

Interventricular Septum. Folia Morphol. Vol. 73, No 1, pp. 42-50 (2014). DOI: 10.5603/FM.2014.0006

3. Aronow W S, Papageorge`s N P, Uyeyama R R, Cassidy J: Maximal treadmill stress test correlates with postexercise

phonocardiogram in normal subjects. Circulation 1971; 43: 884-888. Https://doi.org/10.1161/01.CIR.44.3.397

4. Udelson J E, Bacharach S L, Cannon R O, Bonow R O:Minimum left ventricular pressure during beta-adrenergic

stimulation in human subjects. Evidence for elastic recoil and diastolic “suction” in the normal heart. Circulation 1990;

82: 1174-1182. Https://doi.org /10.1161/01.CIR82.4.1174

We read with interest the excellent and timely article on increasingly detected cases of isolated tricuspid valve regurgitation (1) . The authors rightly note that there is an emerging population of adult patients without left-sided heart disease, pulmonary hypertension or congenital abnormalities who develop symptomatic isolated tricuspid regurgitation. While this is true, we believe that a proportion of these cases of isolated tricuspid regurgitation may well be congenital in origin.
The spectrum of congenital abnormalities of tricuspid valve abnormalities is large (2), and while Ebstein anomaly and tricuspid valve anomalies associated with atrioventricular septal defects and pulmonary atresia are the most commonly discussed, there is a group of patients with tricuspid valve dysplasia or congenitally abnormal tricuspid valves that are under-recognized. Said et al (3) and Dearani et al (4) from the authors’ institution have previously discussed the wide spectrum of congenital tricuspid valve anomalies. The importance of recognizing this group of cases as a separate entity is twofold. One that tricuspid valve dysplasia from failure of delamination of the tricuspid valve, like Ebstein anomaly can be associated with cardiomyopathy and arrhythmia and other congenital anomalies can be missed if focus if just on the valve. Secondly, surgical approach for tricuspid valve surgery, as authors suggest, should focus on the mechanisms of tricuspid regurgitation, which are unique to each given patient. For example, the surgical management of a cleft tricuspid valve (another well-known congenital entity) would be different from a case of tricuspid valve dysplasia when the mechanism of tricuspid regurgitation is a tethered anterior leaflet of tricuspid valve, which is failure of delamination issue.
We recognize this manuscript as an excellent resource for isolated tricuspid valve regurgitation; we would nonetheless underscore that congenital tricuspid valve disease (other than Ebstein anomaly) may be more common than anticipated, and may masquerade as primary idiopathic tricuspid regurgitation. We believe (likely as do the authors) that evaluation of all presumed isolated tricuspid valve disease deserves assessment by cardiologists expert in such distinction and classification.

1. Fender EA, Zack CJ, Nishimura RA. Isolated tricuspid regurgitation: outcomes and therapeutic interventions. Heart 2017.
2. Becker AE, Becker MJ, Edwards JE. Pathologic spectrum of dysplasia of the tricuspid valve. Features in common with Ebstein's malformation. Arch Pathol 1971;91:167-78.
3. Said SM, Burkhart HM, Dearani JA. Surgical management of congenital (non-Ebstein) tricuspid valve regurgitation. Semin Thorac Cardiovasc Surg Pediatr Card Surg Annu 2012;15:46-60.
4. Dearani JA, Danielson GK. Congenital Heart Surgery Nomenclature and Database Project: Ebstein's anomaly and tricuspid valve disease. Ann Thorac Surg 2000;69:S106-17.

Title of E-letter: Intra coronary imaging to detect mal apposition: Are We Seeing Too Much!
Authors Name: Dr Yasir Parviz
Institution: Columbia University Medical Center
Intracoronary Imaging Heart 2017; 0: heartjnl-2015-307888v1
Link to the original paper: http://hwmaint.heart.bmj.com/cgi/content/full/heartjnl-2015-307888v1
Main Text:

We would like to congratulate Giavarini A et al on this comprehensive, educational article on intracoronary imaging. [1] Various modalities can be used to understand the mechanism of stent failure, and there is an ongoing debate on detection of stent mal-apposition, and whether this has any clinical impact. Acute stent mal-apposition on its own is not associated with adverse clinical events unless associated with under expansion or having inflow- outflow issues. Acute mal-apposition and its associated clinical events are possibly reduced due to negative remodelling.[2] The clinically events are non-significant may be due to the fact that newer generation of stents and stronger antiplatelets are performing very well. There is limited literature evidence to support that acute mal-apposition is associated with stent thrombosis. [3] Late acquired malaposition in combination with other contributing factors can be associated with stent failure. Most of the available literature looking into the mechanism of stent failure is from IVUS studies and newer technology, OCT due to superior resolution has the ability to detect a higher percentage of mal appositions.[4] There is on-going research on to the clinical significance of these findings.
We are presenting a summary of some evidence in detection of malapposition by IVUS /OCT and its clinical impact.

1)Im et al. Circ Cardiovasc Interv 2014;7:88-96.
 356(n),62%(OCT), no impact.
2)Kubo et al. JACCCardiovasc Imaging 2013;6:1095-104.
 100(n), 14%(IVUS), 39%(OCT), no impact
3)Kawamori et al. EHJ Cardiovasc Imaging 2013;14:865-75.
 40(n), 65%(OCT), no impact
4)Bezerra et al. JACC Cardiovasc Interv 2013;6:228-36
 26(n), 42% (IVUS), 96%(OCT), no impact
5)Ali ZA et al Lancet. 2016 Nov 26;388(10060):2618-2628.
 304(n), 39% (IVUS), 41% OCT, no impact
6)Prati et al JACC Cardiovascular Imaging November 2015 2015;8:1297.
 832(n), 50%(OCT), no impact
7)Prati F et al Am Heart J. 2015 Feb;169(2):249-56.
 63(n), 52%(OCT), no impact
8)Hong et al, Circulation. 2006;113:414-9.
 557(n), 12 %(IVUS),no impact
9)Steinberg et al J Am Coll Cardiol Intv 3:486-494.
 1580(n), 7-10%(IVUS), no impact
10)Soeda et al Circulation. 2015 Sep 15;132(11):1020-9.
 786(n), 39%(OCT), no impact
11)Kimura M Am J Cardiol. 2006;98:436-442.
 168(n) 77% (IVUS), no impact

References.
1.Giavarini A, Kilic ID, Redondo Dieguez A, Longo G, Vandormael I, Pareek N, Kanyal R, De Silva R and Di Mario C. Intracoronary Imaging. Heart. 2017.
2. Guo N, Maehara A, Mintz GS, He Y, Xu K, Wu X, Lansky AJ, Witzenbichler B, Guagliumi G, Brodie B, Kellett MA, Jr., Dressler O, Parise H, Mehran R and Stone GW. Incidence, mechanisms, predictors, and clinical impact of acute and late stent malapposition after primary intervention in patients with acute myocardial infarction: an intravascular ultrasound substudy of the Harmonizing Outcomes with Revascularization and Stents in Acute Myocardial Infarction (HORIZONS-AMI) trial. Circulation. 2010;122:1077-84.
3. Alfonso F, Suarez A, Angiolillo DJ, Sabate M, Escaned J, Moreno R, Hernandez R, Banuelos C and Macaya C. Findings of intravascular ultrasound during acute stent thrombosis. Heart. 2004;90:1455-9.
4. Ali ZA, Maehara A, Genereux P, Shlofmitz RA, Fabbiocchi F, Nazif TM, Guagliumi G, Meraj PM, Alfonso F, Samady H, Akasaka T, Carlson EB, Leesar MA, Matsumura M, Ozan MO, Mintz GS, Ben-Yehuda O, Stone GW and Investigators IIOP. Optical coherence tomography compared with intravascular ultrasound and with angiography to guide coronary stent implantation (ILUMIEN III: OPTIMIZE PCI): a randomised controlled trial. Lancet. 2016;388:2618-2628.