Title: Transcatheter Aortic and Mitral Valve‐in‐Valve Implantation Using the Edwards Sapien 3 Heart Valve
Abstract: HomeJournal of the American Heart AssociationVol. 7, No. 14Transcatheter Aortic and Mitral Valve‐in‐Valve Implantation Using the Edwards Sapien 3 Heart Valve Open AccessReview ArticlePDF/EPUBAboutView PDFView EPUBSections ToolsAdd to favoritesDownload citationsTrack citationsDownload Articles + Supplements ShareShare onFacebookTwitterLinked InMendeleyReddit Jump toSupplementary MaterialsOpen AccessReview ArticlePDF/EPUBTranscatheter Aortic and Mitral Valve‐in‐Valve Implantation Using the Edwards Sapien 3 Heart Valve Anupama Shivaraju, MD, Jonathan Michel, MBBS, Antonio H. Frangieh, MD, Ilka Ott, MD, Christian Thilo, MD, Heribert Schunkert, MD, Adnan Kastrati, MD, Martin B. Leon, MD, Danny Dvir, MD, Susheel Kodali, MD, Vinayak Bapat, MD, Mayra Guerrero, MD and Albert M. Kasel, MD Anupama ShivarajuAnupama Shivaraju Department for Cardiovascular Diseases, Deutsches Herzzentrum München, Technische Universität München, Munich, Germany Department of Cardiology, Advocate Christ Medical Center, Oak Lawn, IL Search for more papers by this author , Jonathan MichelJonathan Michel Department for Cardiovascular Diseases, Deutsches Herzzentrum München, Technische Universität München, Munich, Germany Search for more papers by this author , Antonio H. FrangiehAntonio H. Frangieh Department for Cardiovascular Diseases, Deutsches Herzzentrum München, Technische Universität München, Munich, Germany Search for more papers by this author , Ilka OttIlka Ott Department for Cardiovascular Diseases, Deutsches Herzzentrum München, Technische Universität München, Munich, Germany Search for more papers by this author , Christian ThiloChristian Thilo Department of Cardiology, Klinikum Augsburg, Herzzentrum Augsburg‐Schwaben, Augsburg, Germany Search for more papers by this author , Heribert SchunkertHeribert Schunkert Department for Cardiovascular Diseases, Deutsches Herzzentrum München, Technische Universität München, Munich, Germany Deutsches Zentrum für Herz‐ und Kreislauferkrankungen (DZHK), partner site Munich Heart Alliance, Munich, Germany Search for more papers by this author , Adnan KastratiAdnan Kastrati Department for Cardiovascular Diseases, Deutsches Herzzentrum München, Technische Universität München, Munich, Germany Deutsches Zentrum für Herz‐ und Kreislauferkrankungen (DZHK), partner site Munich Heart Alliance, Munich, Germany Search for more papers by this author , Martin B. LeonMartin B. Leon Division of Cardiology, Columbia University Medical Center, New York, NY Search for more papers by this author , Danny DvirDanny Dvir University of Washington Medical Center, Seattle, WA Search for more papers by this author , Susheel KodaliSusheel Kodali Division of Cardiology, Columbia University Medical Center, New York, NY Search for more papers by this author , Vinayak BapatVinayak Bapat Division of Cardiology, Columbia University Medical Center, New York, NY Search for more papers by this author , Mayra GuerreroMayra Guerrero Evanston Hospital/NorthShore University Health System, University of Chicago Pritzker School of Medicine, Evanston, IL Search for more papers by this author and Albert M. KaselAlbert M. Kasel Department for Cardiovascular Diseases, Deutsches Herzzentrum München, Technische Universität München, Munich, Germany Search for more papers by this author Originally published7 Jul 2018https://doi.org/10.1161/JAHA.117.007767Journal of the American Heart Association. 2018;7:e007767IntroductionValvular heart disease is a growing clinical problem with significant morbidity and mortality. Surgical valve replacement using mechanical or tissue prosthesis has remained the preferred therapy for several decades. In contrast to mechanical valves, the use of bioprosthetic valves to treat significant aortic valve stenosis (AS) or aortic valve regurgitation (AR) in the native aortic valve has continued to increase over time.1 Bioprosthetic valves are advantageous to patients as they negate the need for long‐term anticoagulation therapy; however, they have limited durability and are expected to degenerate within 5 to 20 years.2 The current standard of care for patients with a degenerated bioprosthetic valve is surgical valve replacement; however, the morbidity and mortality for reoperation is significant because of the technical complexity of the re‐do sternotomy, and also because most of these patients are elderly with multiple comorbid conditions such as prior coronary artery bypass surgery, diabetes mellitus, and cerebrovascular disease.2Although transcatheter heart valves (THV) were initially designed to treat aortic stenosis, the design yields to its use for other indications. The first use of a THV device to treat a failing bioprosthetic heart valve in the aortic position was reported in 2007.7 Since then, valve‐in‐valve (VIV) has become a feasible alternative for treating patients who have degenerated bioprosthetic aortic valves and who are at increased risk of adverse perioperative events.2 VIV is also emerging as a treatment option for patients with failed bioprosthesis in the mitral position. Hundreds of patients with failed mitral bioprosthesis have been treated worldwide with the off‐label use of aortic transcatheter heart valves.8The procedural success rate for aortic VIV transcatheter aortic valve replacement (TAVR) was 93.1% based on the preliminary data from the Valve‐in‐Valve International Data (VIVID) registry.6 In the VIVID registry, the overall 1‐year survival was 83.2% in patients who underwent transcatheter VIV implantation for degenerated bioprosthetic aortic valves.6 The US Food and Drug Administration had approved an expanded indication for the use of the balloon‐expandable Sapien, Sapien XT valves (Edwards Lifesciences), and the self‐expanding CoreValve System (Medtronic Inc) for aortic VIV implantation. The Sapien 3 (S3) (Edwards Lifesciences) valve is the latest iteration of the US Food and Drug Administration–approved balloon‐expandable THV, and it has unique characteristics compared with previous valves. The use of S3 THV was expanded by the US Food and Drug Administration on June 5, 2017 not only for VIV implantation inside a failed bioprosthetic aortic valve, but also for a failed bioprosthetic mitral valve; this is the first approval of any THV for both aortic and mitral VIV implantation.Several new features of the S3 THV, especially its outer skirt and the ability to overexpand its stent frame,10 may have an impact for choosing the optimal size of S3 THV for aortic and mitral VIV implantation.In this article we evaluate existing methods with respect to utilization of the S3 valve in aortic and mitral VIV procedures, describe bioprosthetic valve sizing terminology (Figure 1), and discuss preprocedural sizing as well as relevant intraprocedural factors and techniques used for a successful VIV implant.Download figureDownload PowerPointFigure 1 Surgical bioprosthesis sizing terms. A schematic representation of a cross‐section through a failed bioprosthetic valve is shown. Valve size measurements may be defined in a number of ways. Manufacturer label size is variable and does not usually indicate the internal diameter of the valve. S‐ID is used to indicate the inner diameter of the valve struts/frame, including overlying fabric. T‐ID accounts for the leaflets and sutures (represented in blue) sewn within the stent frame, whereas CT‐ID also includes any accumulated pannus or calcification (represented in orange) within the degenerated bioprosthesis. CT‐ID indicates computed‐tomography inner diameter; S‐ID, stent inner diameter; T‐ID, true inner diameter.Sizing and DeploymentIn general terms, “under/oversizing” refers to the degree to which a THV is smaller/larger than the measured annulus or bioprosthesis internal diameter, respectively. A degree of oversizing is essential—particularly when implanting self‐expanding valves—to ensure THV anchoring and stability after deployment. During native valve TAVR, excessive oversizing may increase the risk of heart block requiring permanent pacemaker implantation and annulus rupture. How much oversize is required to ensure adequate fixation and at the same time avoid incomplete device expansion of balloon‐expandable THVs is unclear, and hence an oversize in the range of 2 to 3 mm is usually practiced.In this review, “under/overexpansion” refers specifically to the balloon filling volume strategy used to deploy the S3 THV, with reference to the nominal filling volume. For example, overexpansion of the 23‐mm S3 THV, with an extra 2 mL of filling volume, results in a prosthesis diameter of ≈24 mm—mainly at the in‐ and outflow part of the valve frame—while preserving normal valve function.10 This under/overexpansion capability of the S3 means that the size of the implanted THV can be more precisely tailored to the dimensions of the bioprosthesis during VIV procedures, thus avoiding excessive oversizing. As a general principle during VIV procedures, we recommend implanting the smallest size S3 device that can be adequately deployed and anchored to achieve a minimum of 1 mm oversizing (Figure 2), within the constraints of the bioprosthesis and notwithstanding other anatomical considerations.Download figureDownload PowerPointFigure 2 Algorithm for determining the choice of S3 THV size. This simplified flow chart can be used during VIV TAVR to facilitate selection of the S3 THV size, and guide when balloon sizing may be appropriate. A minimum of 1 mm oversizing is required in order to ensure adequate anchoring of the S3 THV within the bioprosthesis. Use of the smallest possible THV reduces the risk of excessive flaring of the outflow portion of the stent frame. N.B. In small bioprosthetic valves (label size ≤21), the risk of patient–prosthesis mismatch is high after VIV TAVR. High‐pressure balloon postdilatation with bioprosthetic valve fracture may enable implantation of a larger size THV with improved transvalvular gradient. CT‐ID indicates computed‐tomography inner diameter; S3, Sapien 3; THV, transcatheter heart valve; T‐ID, true inner diameter; VIV TAVR, valve‐in‐valve transcatheter aortic valve replacement.ForeshorteningUnlike preceding iterations of balloon‐expandable THV, S3 foreshortening during deployment occurs almost exclusively from the inflow side of the device. This technical feature has implications when choosing the deployment height of the valve, particularly as deliberate under‐ or overexpansion will result in a lesser or greater degree of foreshortening, respectively.Appropriate Valve ExpansionAppropriate S3 expansion is important to achieve an optimal hemodynamic outcome. An inadequately expanded THV may be at risk of elevated transvalvular gradient because of inadequate leaflet expansion and mobility, also potentially increasing the risk of accelerated leaflet degeneration.1Measure of VIV SuccessThe requirements for a successful VIV implantation are as follows: secure anchoring of the THV within the failed bioprosthesis, a good seal around the valve to eliminate intervalvular leak, patent coronary arteries (in aortic VIV) and left ventricular outflow tract (in mitral VIV), a low gradient across the newly implanted THV, and lack of central regurgitation. Selection of the appropriate size THV and preprocedural identification of potential complications are key to a successful VIV procedure.Identification and Sizing of the Failed Bioprosthetic ValveAn important component of performing the VIV procedure starts with an in‐depth understanding of the failed bioprosthetic valve, which includes the following: the type of valve used (stented, stentless, sutureless, transcatheter valve), its structural elements, the technical details of the primary valve surgery (intra‐annular versus supra‐annular), and the cause of bioprosthetic valve failure (wear and tear, calcification, endocarditis, thrombosis, leaflet dysfunction, and pannus formation).1 Selection of the THV size for the aortic and mitral VIV implantation depends on many factors listed above.Failed Bioprosthetic Valve Inner DiameterThe type of bioprosthesis and manufacturer‐defined label size could be obtained from the operative report. When this information is not available, the type of implant may be identified by fluoroscopy, chest radiograph, and/or cardiac multidetector computed tomography (MDCT).5 The sizing and labeling of the surgical bioprosthetic valves are not standardized and vary widely based on the different manufacturers. The minimum internal diameter of the surgical bioprosthetic valve may vary markedly from the given labeled valve size1 (Figure 1); label size alone is therefore not suitable as a guide to THV size selection.The “true” inner diameter (T‐ID) of the surgical bioprosthesis is one of the most important pieces of information needed for selecting the size of the THV for the aortic or mitral VIV procedure.4 It is important to note that most bioprosthetic valves have a “stent” inner diameter, which consists of the frame/skeleton of the valve, including the overlying fabric, and the T‐ID, which takes into account the leaflets sewn within the valve frame13 (Figure 1). The term “neo‐annulus” has been used to describe the narrowest physical plane—determined in vitro by balloon inflation—of a surgical bioprosthesis, and it is this benchtop dimension that determines the T‐ID. In most bioprosthesis types, this minimum diameter is located at the level of the sewing ring.14 Another crucial point to remember is that when we factor in the additional space taken up by degenerated leaflets and accumulated material in the failed bioprosthesis including pannus formation, the actual internal diameter of that valve is likely to be even less than the T‐ID. In addition to providing information regarding the degree and distribution of calcific degeneration, accumulated material at the level of the sewing ring within a bioprosthesis can be assessed using contrast‐enhanced MDCT. We propose using the definition “CT” inner diameter (CT‐ID) to describe this minimum internal diameter in degenerated in vivo bioprosthetic valves (Figure 1). Use of the CT‐ID may indicate that a smaller S3 valve is preferable in order to achieve an optimal VIV result (Figures 3 and 4).Download figureDownload PowerPointFigure 3 Central regurgitation after extensive oversizing of a 26‐mm S3 THV within a St. Jude Epic 27‐mm bioprosthesis in the mitral position. Although the T‐ID of the 27‐mm St. Jude Epic is 22.5 mm, a mean preoperative CT‐ID of 18.2 mm was measured in this degenerated bioprosthesis (Panel A1). The VIV app recommends use of a 26‐mm S3 THV; however, deployment resulted in underexpansion of the device within the bioprosthesis and extensive flaring of the outflow portion of the frame (Panels B1 to B4), associated with central regurgitation (Panels C1 and C2). CT‐ID indicates computed‐tomography inner diameter; S3, Sapien 3; THV, transcatheter heart valve; T‐ID, true inner diameter; VIV, valve‐in‐valve.Download figureDownload PowerPointFigure 4 Mitral VIV. S3 valve choice based on CT‐ID, balloon‐sizing, and tug‐test. Case of S3 26‐mm valve inside an Epic 31 mm (St. Jude Medical) with a T‐ID of 26.5 mm. The VIV Mitral App recommends implanting a S3 29‐mm valve. Based on the CT‐ID of 18.7 mm and balloon‐sizing and tug‐test with a 25‐mm balloon, the decision was to deploy a 26‐mm S3 valve with nominal filling volume. A1. Epic 31‐mm (St. Jude Medical) valve: CT‐ID was measured at 18.7 mm. A2. Aorto‐mitral angle: 138 degrees. B1. Coplanar view of the mitral valve. B2. Balloon‐sizing and tug‐test with a 25‐mm Edwards balloon. B3. S3 26‐mm positioning towards left ventricle because of expected underdeployment. B4. S3 26‐mm implantation result with a flared frame on the ventricular side. B5. Left ventricular angiography to assess for MV regurgitation. B6. S3 26‐mm “round” deployment. CT‐ID indicates computed‐tomography inner diameter; MV, mitral valve; S3, Sapien 3; T‐ID, true inner diameter; VIV, valve‐in‐valve.In order to facilitate suitable valve sizing, Bapat et al have developed a mobile app “ViV Aortic” and “ViV Mitral” in collaboration with the technology company UBQO.15 This app provides data that guide proper identification of all available surgical and transcatheter valves and rings, as well an in vitro estimate of the valve T‐ID, and sizing recommendation for the S3 THV.3 Although the ViV App (version 2.0) is invaluable, there are a few limitations of this App when using the Edwards S3 valve for VIV. The ViV App sizing recommendation may in some cases exceed the optimal THV size for a selected bioprosthesis. For example, the 21‐mm Perimount valve (Edwards Lifesciences) has a 19‐mm T‐ID, and the App recommends selecting a 23‐mm Sapien XT or S3 THV (Edwards Lifesciences).3 This may lead to inadequate expansion of the 23‐mm valve within the bioprosthesis frame, leading to prosthesis–patient mismatch with possible higher transvalvular gradients and inadequate function of the valve leaflets, and hence a 20‐mm Sapien 3 could be a better option with just 1‐mm oversizing. In this situation, our preferred approach is to use high‐pressure postdilatation after 20‐mm S3 valve deployment to optimize expansion and stretching of the bioprosthetic frame and sewing ring16 or consider implanting a supra‐annular THV; however, if there is adequate space in the aortic root, then “cracking the ring” with high‐pressure postdilatation technique (described below) can enable implantation of a 23‐mm S3 THV (Figure 5).Download figureDownload PowerPointFigure 5 Examples of using high‐pressure postdilatation to optimize THV deployment in small bioprosthetic valves. Contrast and brightness are adjusted to minimize blooming artifact. A. Edwards S3 20‐mm THV inside a Perimount 21 valve (true inner diameter 19 mm). A1. Stent inner diameter of the Perimount sewing ring measured on the baseline CT—18.1×18.9 mm. A2. Twenty‐mm S3 angiographic appearance after deployment. Note the waist appearance at the level of the sewing ring. A3. Angiographic appearance of the 20‐mm S3 after postdilatation with a 20‐mm True Dilatation balloon (Bard) to 16 atmospheres showing improved device expansion within the bioprosthesis. A4. Stent inner diameter of the Perimount sewing ring on CT after high‐pressure postdilatation showing increased dimensions of 18.9×20.1 mm. A residual transvalvular mean gradient of 12 mm Hg was observed on echocardiography. B. Edwards S3 23‐mm THV inside a Perimount 21 valve (true inner diameter 19 mm). B1. Stent inner diameter of the Perimount sewing ring measured on the baseline CT—18.4×20.2 mm. B2. Twenty‐three‐mm S3 angiographic appearance after deployment. Note the mild waist appearance at the level of the sewing ring. B3. Angiographic appearance of the 23‐mm S3 after postdilatation with a 22‐mm Atlas Gold balloon (Bard) to 20 atmospheres showing improved device expansion within the bioprosthesis. B4. Stent inner diameter of the Perimount sewing ring on CT after high‐pressure postdilatation showing increased dimensions of 20.2×20.1 mm. A residual transvalvular mean gradient of 18 mm Hg was observed on echocardiography. CT indicates computed tomography; S3, Sapien 3; THV, transcatheter heart valve.Balloon‐Sizing and Tug‐TestBalloon sizing is not routinely recommended in VIV procedures, as there is an increased risk of embolization or creating aortic insufficiency,1 which can result in acute hemodynamic instability. However, in addition to selecting the size of the THV based on the T‐ID of the initially implanted bioprosthetic valve, balloon sizing can provide additional information and better understanding in selected cases such as when the CT‐ID suggests a smaller size S3 may be suitable, borderline valve sizes, stentless bioprostheses, or valves with a high risk of coronary artery obstruction. In these situations, balloon sizing can be performed along with a tug‐test (Figures 4 and 6). The tug‐test involves applying negative tension to the fully inflated balloon within the bioprosthetic valve to help assess how well the balloon is anchored in the valve. This information can be used to guide the selection of the appropriate THV size and to assess the solidity of any material that may be accumulated within the bioprosthesis.Download figureDownload PowerPointFigure 6 Balloon‐sizing, tug‐test, and S3 overdeployment. Case of S3 23‐mm valve inside a Mitroflow 27‐mm valve with a T‐ID of 23 mm. The VIV Aortic App recommends implanting a S3 26‐mm valve in this circumstance. Planned overdeployment of a S3 23‐mm (+2 mL in deployment‐balloon) THV after balloon‐sizing and tug‐test with a 23‐mm balloon. A. Coplanar View. B. Balloon sizing and the tug‐test show that the coronary arteries are not obstructed, and the balloon is fixed in the bioprosthetic surgical valve. C. Placement of the S3 23‐mm middle marker is at the bottom of the suture ring of the bioprosthetic surgical valve (“low position”). D. Implantation result shows no aortic insufficiency with a peak‐to‐peak gradient of 5 mm Hg across this valve. S3 indicates Sapien 3; THV, transcatheter heart valve; T‐ID, true inner diameter; VIV, valve‐in‐valve.Balloon sizing can be useful when the pre‐existing valve is supra‐annular with external leaflets, such as the Mitroflow (Sorin) and Trifecta (Abbott), and there is a short distance to the coronary ostia, thereby increasing the risk of coronary artery obstruction.2 Furthermore, balloon sizing may be useful to assess for height of the prosthetic valve neo‐annulus and to assess for unanticipated expansion of a stentless bioprosthesis, a technical issue that can lead to THV embolization.17Prosthesis–Patient MismatchProsthesis–patient mismatch (PPM) is the phenomenon when the implanted prosthetic valve has a lower effective orifice area (EOA) than a normal human valve.18 Calculations based on patients’ body surface area, direct measurements of the aortic root during surgery, and echocardiographic parameters such as transvalvular gradient and EOA are calculated to assess PPM. In general, an echocardiographically derived prosthetic EOA, indexed to body surface area (indexed EOA), of ≤0.60 cm2/m2 is considered severe, of 0.60 to 0.85 cm2/m2 is moderate, and ≥0.85 cm2/m2 is considered nonsignificant.19 Based on the surgical literature, severe PPM following aortic valve replacement is associated with worse clinical outcomes, less reduction in left ventricular mass, and lower long‐term survival.22 Likewise, severe PPM following surgical mitral valve replacement is also associated with lower long‐term survival.24Aortic VIV procedures are associated with a higher rate of PPM than native valve TAVR,6 particularly in surgical valves with a manufacturer size of ≤21 mm.25 Results from the VIVID registry revealed an elevated postprocedural mean aortic transvalvular gradient of ≥20 mm Hg in 28% of patients.When considering a VIV procedure, it is important to determine whether a high gradient across a surgical valve is because of degeneration of the valve or simply as a result of postoperative PPM.26 A VIV procedure will not correct a stable elevated transvalvular gradient caused by surgical PPM unless an adjunctive technique—such as bioprosthetic ring fracture—can be used.Treatment of small bioprosthetic valves (label size ≤21 mm) remains a challenging problem during aortic VIV procedures because of the risk of high postprocedural transvalvular gradient with new, or persistent, PPM.6 As a result, a preprocedural evaluation of the EOA may be particularly important to determine appropriate clinical management and THV implantation strategy; however, in selected cases the benefit of acute gradient reduction and hemodynamic improvement in highly symptomatic patients at prohibitive risk of re‐do surgery may, nevertheless, outweigh the risk of PPM that can occur after a VIV procedure. More recently, deliberate bioprosthetic sewing ring fracture (discussed below) using high‐pressure balloon dilatation (“cracking‐the‐ring”) has emerged as a promising adjunct for aortic VIV in a small bioprosthesis in order to facilitate implantation of a larger THV size and effectively reduce postprocedural gradients.27Balloon‐Inflatable Versus Self‐Expanding THVs in VIV ProceduresRegistry and in vitro data suggest that supra‐annular THVs are associated with lower gradients after aortic VIV procedures; however, technical factors, such as future access to the coronary vessels, concerns about THV recoil associated with self‐expanding devices, or use of deliberate bioprosthetic ring fracture, may prompt selection of a balloon‐expandable intra‐annular THV.11 While randomized comparisons of the transvalvular gradient after S3 versus supra‐annular THV implantation in surgical bioprostheses have not been performed, accurate sizing, positioning, and deployment of the S3 is clearly essential in order to achieve a good functional outcome with low transvalvular gradients.It should be noted that because of anatomical constraints, balloon‐expandable valves are currently mandated in mitral VIV procedures.Anticipating Complications During VIV ProceduresThe risk of potential complications can often be determined by rigorous evaluation of preprocedural investigations. The MDCT data, in particular, provide valuable information when assessing the risk of severe intraprocedural complications.During aortic VIV procedures, coronary artery occlusion may occur because of impingement of displaced surgical leaflets and/or bulky degenerative material on the coronary ostia, especially in stentless valves and valves with leaflet attachment outside the frame, such as the Mitroflow (Sorin Group) and the Trifecta (Abbott) valves. In this regard, MDCT enables accurate assessment of the height of the coronary ostia in relation to the surgical bioprosthesis and the width of the aortic sinus. Low coronary height (<12 mm) and/or small sinus of Valsalva diameter (<30 mm) will increase the risk for coronary artery obstruction during native valve TAVR,33 and aortic VIV procedures are associated with a higher risk.29 Unfavorable anatomy identified on MDCT may prompt avoidance of a VIV procedure altogether; it may also direct the implanter to use balloon sizing, or use a risk‐minimization strategy, such as less aggressive valve oversizing and deeper valve implantation, to avoid coronary artery occlusion. A recently described first‐in‐humans procedure involving intentional laceration of the bioprosthetic leaflet scallop before valve implantation (BASILICA) may enable a successful aortic VIV procedure despite a high risk of coronary occlusion (unpublished data—TCT 2017).Mitral VIV poses a unique set of challenges to the operator. Closing pressure is higher across bioprosthetic valves in the mitral position when compared with those in the aortic position; this is because of exposure to left ventricular systolic, rather than aortic diastolic, pressure. For this reason, secure anchoring of a VIV THV may be more important in the mitral position than the aortic. The principles of MDCT‐based valve sizing also apply to mitral VIV.Mitral VIV also carries with it a risk of left ventricular outflow tract (LVOT) obstruction because of displacement of the bioprosthetic leaflets and coverage of the open part of the THV frame. Mitral VIV‐induced LVOT obstruction with hemodynamic compromise is a serious complication with limited treatment options and can be fatal; therefore, it should be avoided whenever possible. Bioprostheses with bovine pericardial leaflets are at particular risk of creating a LVOT obstruction because the leaflets are positioned higher up the stent frame, thus resulting in greater THV frame coverage in the LVOT. Assessing the LVOT tract anatomical morphology with MDCT can be helpful to identify patients at high risk of this complication.34 Prominent septal hypertrophy and a narrow aorto‐mitral angle increase the risk of subsequent LVOT obstruction. The aorto‐mitral‐annular angle—defined as the angle formed at the intersection of lines running through the intercommissural diameter of the mitral annulus and the center of the aortic annulus—is readily determined from preprocedural MDCT images. Acute angles <115 degrees may increase the risk of LVOT obstruction after deployment of a balloon‐expandable valve35 (Figure 4). Preprocedural virtual valve implantation, performed using commercially available 3‐dimensional reconstruction software, and calculation of the neo‐LVOT area can assist preemptive identification of this complication (Figure 7). Preliminary studies suggest that a neo‐LVOT area of 250 mm2 or larger is associated with a low risk of LVOT obstruction.36Download figureDownload PowerPointFigure 7 Mitral annular area and neo‐LVOT area measurements. A, Cardiac computed tomography–based measurement of the mitral internal annular area using 3Mensio Structural Heart Mitral Workflow version 8.1 (Pie Medical Imaging, Maastricht, the Netherlands). B, Short‐axis view of the mitral bioprosthesis with a 23‐mm virtual valve in place (pink circle). C, Measurement of the LVOT tract area in systole in short‐axis (white circle) view using 3Mensio Structural Heart Mitral Workflow version 8.1 (Pie Medical Imaging, Maastricht, the Netherlands). D, Measurement of the remaining LVOT area in short axis (white circle) after placement of the virtual transcatheter heart valve (pink). The remaining space in the LVOT after placement of the virtual valve is the neo‐LVOT. A neo‐LVOT area of 250 mm2 or larger is associated with a low risk of LVOT obstruction. LVOT indicates left ventricular outflow tract.Our S3 THV Sizing Recommendation for VIV ImplantationWhen using the S3 THV for VIV, we recommend a minimum oversizing of 1 mm in relation to the T‐ID. However, when the measured CT‐ID suggests that a smaller size THV could be selected, we would recommend balloon sizing and