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Neurologic Outcomes with Embolic Protection Devices in Patients Undergoing Transcatheter Aortic Valve Replacement: A Systematic Review and Meta-Analysis of Randomized Controlled
TrialsGennaro Giustino, MD*, Roxana Mehran, MD, FAHA*, Roland Veltkamp, MD†, Angela Del Giudice,
MD†, Michela Faggioni, MD*, Jaya Chandrasekhar, MD*, Usman Baber, MD,* and
George D. Dangas, MD, PhD, FAHA*.
*Interventional Cardiovascular Research and Clinical Trials, The Zena and Michael A. Wiener
Cardiovascular Institute, Icahn School of Medicine at Mount Sinai (New York City, New York);
†Department of Medicine, Division of Brain Sciences, Imperial College (London, UK).
Running TitleEmbolic Protection during TAVR
Word Count: 5,673
Corresponding AuthorGeorge D. Dangas MD, PhD, FACC.Mount Sinai Hospital,
One Gustave L. Levy Place, Box 1030
New York, New York 10029
Tel: 212-241-7014; Fax: 212-241-0273
E-mail: [email protected]
1
AbstractBackground: Cerebral embolism is a common complication after transcatheter aortic valve
replacement (TAVR). Randomized controlled trials (RCTs) investigating the efficacy of embolic
protection (EP) devices during TAVR were relatively underpowered. We investigated the effect of
intraprocedural EP on neurologic outcomes after TAVR.
Methods: We performed a systematic review and study-level meta-analysis of RCTs that tested the
efficacy and safety of EP during TAVR. RCTs using any type of EP and TAVR vascular access were
included. Primary imaging efficacy endpoints were total lesion volume (TLV; in mm3) and number of
new ischemic lesions. Primary clinical efficacy endpoints were any deterioration in National Institute of
Health Stroke Scale (NIHSS) and Montreal Cognitive Assessment (MoCA) score at hospital discharge.
Primary analyses were performed with the intention-to-treat approach.
Results: A total of 4 RCTs (total n=252) have been included. Use of EP was associated with lower TLV
(standardized mean difference [SMD]: -0.83; 95% confidence interval [CI]: -1.57 to -0.10; p=0.03) and
lower number of new ischemic lesions (SMD: -1.06; 95% CI: -1.77 to -0.35; p = 0.003). EP was
associated with a trend to lower risk of deterioration in NIHSS at discharge (RR: 0.55; 95% CI: 0.27 to
1.09; p=0.09) and higher MoCA score (SMD: +0.40; 95% CI: +0.04 to +0.76; p = 0.03). Risk of overt
stroke and all-cause mortality were non-significantly lower in the EP group.
Conclusions: Use of EP seems to be associated with a reduction of imaging markers of cerebral
infarction and early clinical neurologic effectiveness in patients undergoing TAVR.
Key Words: TAVR; Embolic Protection; Stroke.
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IntroductionTranscatheter aortic valve replacement (TAVR) has emerged as a standard of care to treat
degenerative aortic stenosis in patients deemed at high- or prohibitive-risk for surgical aortic valve
replacement (SAVR).1, 2 Patients undergoing TAVR are often elderly, frail and affected by multiple
comorbidities, implying a significant risk for thromboembolic cerebrovascular events.1-3 Overt stroke is
the most feared complication of TAVR being associated with a strong effect on morbidity and mortality.3,
4 Early studies suggested that TAVR is associated with an increased risk of stroke compared with
medical treatment or surgical aortic valve replacement.1, 2 Additionally, several studies demonstrated a
very high incidence of new cerebral ischemic lesions on post-procedural diffusion-weighted magnetic
resonance imaging (DW-MRI), and of high-intensity transient signals evaluated with transcranial
Doppler, respectively.5 In current TAVR practice the rate of overt stroke during or early after TAVR is
relatively low (≤ 2%);6 however the frequency and burden of micro-embolization and cerebral ischemic
injury may still have a substantial impact on mid- and long-term cognitive function.5, 7 Therefore, in order
for TAVR to expand to lower risk patients, measures to mitigate neurologic risk are warranted.
Additional, several studies in surgical cohorts demonstrated greater cognitive function impairment post-
SAVR compared with patients undergoing coronary artery by-pass graft surgery8, 9.
The application of EP has been explored in several small observational and few randomized
studies in TAVR but its efficacy and safety remains inconclusive. Therefore, by pooling study-level data
from randomized controlled trials (RCTs), in the present metanalysis we sought to investigate imaging
and clinical neurologic outcomes associated with intraprocedural EP in patients with severe aortic
stenosis undergoing TAVR.
MethodsStudy Design. We performed a systematic review and study-level meta-analysis of RCTs that tested
the efficacy of EP devices during TAVR according to the Preferred Reporting Items for Systematic
Reviews and Meta-Analyses (PRISMA) guidelines.10 RCTs investigating the efficacy of EP with any
device and for any TAVR vascular access were included. All non-randomized studies reporting
outcomes with EP during TAVR were excluded. We opted to include only RCTs in order to reduce the
selection and confounding bias of observational pilot studies. The two study groups were defined by the
randomized assignment to either intraprocedural EP or not. The pre-specified imaging neurologic
endpoints were total lesion volume (TLV) in mm3 assessed with DW-MRI and number of new ischemic
lesions. The pre-specified primary clinical neurologic endpoints were any clinical deterioration from
baseline in National Institute of Health Stroke Scale (NIHSS) and the Montreal Cognitive Assessment
(MoCA) score at discharge. Secondary endpoints were: percentage of patients with new cerebral
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ischemic lesions, mean number of new cerebral ischemic lesions, clinically overt stroke at follow-up, all-
cause mortality at follow-up, fluoroscopic time and acute kidney injury. Imaging endpoints were
evaluated as well according to the type of valve implanted (balloon-expandable [BE] versus self-
expandable [SE]), where available. All endpoints were estimated at the maximum time of follow-up
reported according to the intention-to-treat (ITT) principle. The study was performed according to the
PRISMA statement.10
Research strategy. MEDLINE, Scopus, the Cochrane Library, and TCTMD.org were searched for
abstracts, manuscripts, and conference reports published until December 31, 2015. There were no
language restrictions. The following key words were used for the search: “TAVR embolic protection”,
“TAVR embolic protection randomized controlled trial”, “TAVR stroke”, “TAVR Claret”, “TAVR Triguard”,
and “TAVR Embol-X”. Two investigators (GG and MF) independently reviewed the studies and reported
the results in a structured dataset. Disparities between investigators regarding the inclusion of each trial
were resolved by consensus by a third independent investigator (GD). Pre-specified data elements
were extracted from each trial and included in a structured dataset; these elements included type of EP
device, baseline characteristics, TAVR access site, type of transcatheter heart valve device implanted,
risk of bias, and outcome measures, including imaging endpoints (TLV, mean number of new ischemic
lesions, number of patients with new ischemic lesions), clinical endpoints (any worsening in NIHSS,
MoCA score, clinically overt stroke, all-cause mortality, acute kidney injury) and procedural variables
(fluoroscopic time). Additionally, device success (defined as the correct deployment and retrieval of the
device) was captured. Endpoints were collected according to both the ITT and the per-treatment (PT)
principles. Considering the potential effectiveness of EP devices on intra-procedural (acute) events, the
primary analysis included all events reported as close as possible to the date of the index TAVR
procedure in each RCT. Risk of bias in each trial for both the primary imaging (TLV) and clinical (risk for
NIHSS deterioration at discharge) endpoints was evaluated with the Cochrane’s tool as described by
Higgins et al11; the following elements potential source of bias have been evaluated: random sequence
generation (selection bias), allocation concealment (selection bias), blinding of participants and
personnel (performance bias), blinding of outcome assessment (detection bias), incomplete outcome
data (attrition bias) and selective reporting (reporting bias). For each element, a qualitative attribution of
bias was given (low risk, intermediate risk or high risk for bias) by two independent investigators (GG
and MF). Disparities between investigators regarding the risk of bias were resolved by a third
independent investigator (GD).
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Study Devices.
The following EP devices have been used in the included RCTs:
The Claret Montage system is composed of two polyurethane mesh filters with 140-mm pores
mounted on a nitinol frame, and delivered through transradial access. This is a selective EP device,
with 1 filter deployed in the brachiocephalic trunk and one filter in the left common carotid artery. This
device allows for capture and retrieval of embolic material.
The Triguard embolic deflection device is a nitinol-based, temporary, non-selective filter delivered
through transfemoral access and positioned in the aortic arch in order to cover the ostia of the
innominate artery, the left common carotid and the left subclavian while maintaining blood flow to the
cerebral vessels through 130 mm pores while deflecting larger emboli to the descending aorta.
The EMBOL-X device is a filtration system composed of a self-expanding nitinol-based frame
covered by a semi permeable polyester mesh with 120-mm pore diameter. It is delivered through the
radial or brachial artery and positioned within the ascending aorta where it captures embolic material
while allowing blood flow. This device allows for capture and retrieval of embolic material.
Statistical Analysis. We estimated risk ratios (RRs) and standardized mean differences (SMD) with
95% confidence intervals (CIs) for all available categorical and continuous variables, respectively.
Given the possible heterogeneity in outcomes ascertainment across trials, we opted to use SMD as this
is a more conservative summary statistic that expresses the size of the intervention effect in each study
relative to the variability observed in that study. During data extraction, continuous variables reported
as median with low- and high-end of the range were converted to mean and standard deviations
according to the method of Hozo et al.12 If ranges were not directly reported, these were extracted by
visual estimation of the plots. Primary analytic method was the more conservative random effect model
according to DerSimonian and Laird. The primary and secondary analytic approaches (for the imaging
and neurologic endpoints) were according the ITT and PT principles, respectively. Publication bias for
the primary imaging and clinical endpoints was estimated via visual inspection of the Funnel Plot.
Heterogeneity among trials for each outcome was estimated with Chi2 test and quantified with I2
statistics (with I2 > 75% indicating substantial heterogeneity).13 If a trial did not report one of the pre-
specified primary and efficacy endpoint, this was excluded from that specific analysis. Analysis for the
imaging neurologic endpoints was stratified by type of valve (BE and SE TAVR devices) with
subsequent formal interaction test. Analyses were conducted with Cochrane’s Review Manager
(RevMan) version 5.3.
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ResultsSystematic Review.
The research flow diagram according to the PRISMA guidelines is illustrated in Supplementary
Figure 1. Out of more than 200 screened article, 4 RCTs (N = 252) that met the inclusion criteria were
found (Table 1).
The CLaret Embolic Protection ANd TAVI - Trial (CLEAN-TAVI; NCT01833052)14 was a double-
blind randomized controlled trial that assigned 100 patients to either EP (n = 50) with the Claret
MontageTM dual-filter or to no EP (n = 50). Patients were all treated with femoral access and a SE
device. All patients underwent DW-MRI at baseline, day 2, day 7 and day 30 (not available for data
extraction) after TAVR. All patients underwent serial assessment with NIHSS at 2 days, 7 days and 30
days. DW-MRI endpoints at 7 days were included in this analysis. The drop-out rate for DW-MRI
assessment at 7 days was 13% (87 / 100). NIHSS results at 2 days were included. The drop-out rate
for NIHSS assessment was not reported. Device success was achieved in 96% of patients (48 / 50).
The A Prospective, Randomized Evaluation of the TriGuard™ HDH Embolic Deflection Device
During TAVI (DEFLECT-III; NCT02070731) study15 was a single-blind randomized controlled trial in
which 85 patients were randomized to either EP (n = 46) with the deflector TriGuard HDH or no EP (n =
39). Ninety-six percent of patients underwent TAVR through a transfemoral approach and 4% through a
transapical approach. A BE valve was implanted in 63% of patients and a SE in 31%. DW-MRI was
performed in all patients at day 4 ± 2 and day 30 ± 7 after TAVR. All patients underwent serial
neurologic assessment with NIHSS, MoCA and computerized Cogstate Research Test. DW-MRI
endpoints at 4 days were included. Drop-out rate for DW-MRI assessment at 4 days was 30% (33/46 in
the EP group and 26/39 in the no EP group). NIHSS and MoCA assessment at discharge were
included. Drop-out rate for NIHSS and MoCA assessment at discharge was 6% (5/85). Device success
was achieved in 88.9% of patients (40 / 45).
The Intraprocedural Intraaortic Embolic Protection with the EmbolX Device in Patients
Undergoing Transaortic Transcatheter Aortic Valve Implantation (TAo-EmbolX; NCT01735513) trial16
randomized 30 patients to either EP (n = 14) with Embol-X or no EP (n = 16). All patients underwent
TAVR through transaortic approach and all patients received a BE valve. DW-MRI was performed at
baseline (pre-TAVR) and within a week after TAVR. No specific serial neurologic assessment was
performed. Drop-out rate for DW-MRI assessment was 0% (0/30). Device success was of 100%
(14/14).
The MRI Investigation in TAVI with Claret (MISTRAL-C; NTR4236) study17 was a multicenter,
double-blind randomized trial that randomly assigned 65 patients to TAVR with (n = 32) or without (n =
33) EP with the Sentinel Cerebral Protection System. All patients underwent DW-MRI at baseline (pre-
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TAVR) and 5 days after TAVR. All patients underwent serial neurocognitive assessment with NIHSS,
MoCA, mini-mental status examination and Center for Epidemiological Studies-Depression scale by
trained neurologist blinded to allocation at baseline and 5 days after TAVR. Both DW-MRI and clinical
neurologic evaluation at 5 days were included. The drop-out rates for DW-MRI and neurologic clinical
assessment were 43% (28 / 65) and 26% (17 / 63), respectively. Device success was achieved in 94%
of patients (30 / 32).
Neurologic Imaging Endpoint.TLV was reported in all 4 RCTs, number of new ischemic lesions in 3 RCTs and number of
patients with new ischemic lesions in 3 RCTs. At ITT analysis, use of EP during TAVR was associated
with lower TLV (Figure 1A; SMD: -0.83; 95% CI: -1.57 to -0.10; I2=84%; p = 0.03), lower mean number
of new ischemic lesions (Figure 1B; SMD: -1.06; 95% CI: -1.77 to -0.35; I2=74%; p = 0.003) and a trend
to lower number of patients with new ischemic lesions (Figure 1C; 72.4% vs. 82.5%; RR: 0.87; 95% CI:
0.73 to 1.04; I2=0%; p = 0.12). There was no evidence of publication bias for TLV and mean number of
new ischemic lesions endpoints at visual inspection of the Funnel plot (Supplementary Figure 2).
TLV and percentage of patients with new ischemic lesions according to valve types were
reported in 2 RCTs. The effect of EP during TAVR was consistent between BE and SE devices with
non-significant interaction test for both TLV (Figure 2A; pinteraction = 0.99) and risk of new ischemic lesions
(Figure 2B; pinteraction = 0.25), and absence of within-subgroup heterogeneity for both endpoints (I2=0%
for TLV in SE and BE subgroups; I2=0% for new ischemic lesions in SE and BE subgroups).
The direction of the effect estimates for the neurologic imaging endpoint were consistent at the
PT analysis, with an accentuation of the magnitude of the benefit for all three outcome metrics
(Supplementary Figure 3).
Neurologic Clinical Endpoint.NIHSS evaluation and MoCA score at discharge were reported in 3 and 2 RCTs, respectively.
Patients who were randomized to intraprocedural EP had a trend to lower risk of worsening in NIHSS at
discharge (8.3% vs. 16.8%; Figure 3A; RR: 0.55; 95% CI: 0.27 to 1.09; I2=0%; p = 0.09. Patients
randomized to EP had higher MoCA score at discharge (SMD: +0.40; 95% CI: +0.04 to +0.76; I2=0%; p
= 0.03). There was no evidence of publication bias for the risk of NIHSS deterioration and MoCA at
discharge at visual inspection of the Funnel plot (Supplementary Figure 2).
Neurologic clinical endpoint estimates were consistent at the PT analysis (Supplementary
Figure 4). Clinically overt stroke was reported in 3 RCTs. EP was associated with a non-significant
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lower risk of stroke at 30-day of follow-up (Figure 3B; 2.2% vs. 4.5%; RR: 0.56; 95% CI: 0.11 to 2.82;
I2=0%; p = 0.49) at the ITT analysis.
Procedural Outcomes and Safety.Use of EP was associated with increased fluoroscopic time (Supplementary Figure 5A; SMD:
0.28; 95% CI: -0.02 to 0.58; I2=0%; p = 0.06). There were no differences in acute kidney injury (2.1%
vs. 5.6%; Supplementary Figure 5B; RR: 0.54; 95% CI: 0.05 to 6.11; I2=42%; p = 0.62). No evidence of
other major intraprocedural complications became evident in the systematic review of all RCTs.
Finally, EP was associated with non-significantly lower risk of all-cause mortality at 30 days of
follow-up (Figure 4; 1.4% vs. 5.1%; RR: 0.32; 95% CI: 0.08 – 1.34; I2=0%; p = 0.12).
DiscussionThe present metanalysis investigated the efficacy and safety of EP use during TAVR. The main
findings of the present study are: (i) EP is associated with significantly lower TLV and number of new
ischemic lesions after TAVR as assessed with DW-MRI; results were consistent at PT analysis, with an
accentuation of the magnitude of the benefit on all three neuroimaging endpoints (ii) EP resulted in
higher MoCA score and a trend to lower risk of any worsening in NIHSS at discharge; results were
consistent at PT analysis (iii) EP was associated with a non-significant reduction in stroke and all-cause
mortality; and (iv) use of EP was safe with no evidence of increased adverse events alongside a trend
to increased fluoroscopic time.
TAVR has become a standard of care for patients with severe aortic stenosis deemed at high or
prohibitive risk for surgery.1, 2 However, several concerns regarding its neurological safety rose early
after its introduction into clinical practice.18, 19 The incidence of clinically apparent neurological events
after TAVR is variable due to clinical endpoint definitions, ascertainment bias and underdiagnosis due
to lack of standardized, routine imaging and neurocognitive assessment.3, 20 Early after TAVR, cerebral
embolization is strongly related to technical and procedural factors such as retrograde crossing of the
degenerated stenotic aortic valve during diagnostic catheterization, catheter manipulation in an aortic
arch with severe atherosclerosis, preparatory balloon aortic valvuloplasty prior to bioprosthesis
implantation, eventual device malpositioning / dislodgment / embolization and need for valvular balloon
post-dilation in case of significant residual paravalvular leak. Histopathological studies revealed that
emboli composition is heterogeneous, with thrombotic material and tissue-derived debris identified in
74% and 63% of patients with embolization, respectively.20 As ischemic brain injury related to TAVR
spans a spectrum ranging between clinically overt strokes to seemingly silent ischemic lesions
identified with brain imaging studies and neurocognitive assessment, its evaluation is challenging.3, 5, 19
8
Previous studies suggest that new cerebral parenchymal ischemic lesions are common, usually
multiple,and distributed to both cerebral hemispheres.5 Clinically covert ischemic brain injury can result
in both acute and chronic cognitive and functional impairment which may have a substantial effect on
morbidity and mortality.21 Hence, intraprocedural strategies to mitigate cerebral embolization risk and
development of permanent neurologic deficit are essential in order to expand TAVR indication to lower
risk populations. Additionally, prior studies in surgical cohorts indicated higher risk of neurocognitive
deterioration in patients undergoing SAVR compared with age-matched patients undergoing coronary
artery by-pass graft surgery.9
EP devices have been introduced in TAVR practice. RCTs investigating the efficacy and safety
of EP during TAVR have been small and relatively underpowered for imaging and neurocognitive
endpoints.15 Additionally, TAVR studies with serial imaging follow-up are challenging due to technical
and logistic limitations in this elderly and sick patient population, with drop-out rate as high as 40% at
30 days.15, 17 Within this context, the present study-level metanalysis with enhanced statistical power
aimed to better define the role of EP during TAVR. EP was associated with significantly reduced TLV
and number of ischemic lesions compared with no EP, alongside higher MoCA score and a trend to
lower risk of NIHSS worsening at discharge. TLV is currently considered the most informative brain
imaging measure with excellent intra- and interrater concordance for DWI and fluid-attenuated inversion
recovery MRI and is one of the strongest predictors of supra-tentorial stroke outcomes.22, 23 The MoCA
and NIHSS are validated metric of neurocognitive function and neurologic dysfunction, respectively,
with excellent interrater reliability and a strong predictor of long-term outcomes after cerebrovascular
events.24-26 Additionally, we observed an accentuation of the benefits of EP on the neuroimaging
endpoint at the PT analysis. Possibly, this is consistent with the fact that when device success is
achieved intraprocedural EP is indeed effective in preventing cerebral embolization.
The effect of EP on neurologic imaging endpoints appeared to be uniform between SE and BE
valve types which differ significantly in term of design and implantation technique. While this analysis
could have been underpowered to detect statistically significant interactions, our results are consistent
with previous reports that failed to detect significant differences in stroke incidence and transcranial
Doppler-detected embolizations.18, 27
There was no evidence of safety concerns with intraprocedural EP, EP use was associated with
an overall device success of 97% and longer fluoroscopic time. The small, yet possibly clinically
relevant EP failure rate has to be interpreted carefully. Cardiac computed tomography (CT) scan has
become a standard of care in many TAVR centers as it allows the characterization of the ascending
aorta, aortic valve anatomy and calcifications, aortic root size and height of the coronary ostia from the
aortic annular plane.28, 29 Additionally, cardiac computed tomography (CT) angiography can be used to
9
assess peripheral vascular access sites, coronary and great epicardial vessels anatomy.29 Therefore
CTCA may play a pivotal role in screening patients suitable for EP and / or select the optimal type of EP
device according to the underlying anatomy.
We failed to detect a significant reduction in clinically overt stroke and all-cause mortality.
However both endpoints were numerically lower in the EP group. The present total sample size may be
insufficient to detect significant differences in overt stroke due to the rarity of this event. Larger RCTs
designed to detect differences in hard clinical endpoints and long-term neurocognitive assessment are
therefore warranted to provide conclusive evidence regarding the efficacy of EP during TAVR. For this
purpose, several larger RCTs investigating outcomes with EP are currently ongoing (NCT02214277;
NCT02536196). As a substantial amount of emboli during TAVR are of thrombotic origin
complementary antithrombotic strategies to EP are warranted. Recent studies demonstrated that both
alternative anticoagulation agents30 and anticoagulation regimens31 are safe in terms of neurologic
complications and possibly associated with a lower risk of bleeding compared with conventional
antithrombotic strategies. Conversely the role of antiplatelet agents in reducing the risk of intra- and
periprocedural cerebrovascular events has been poorly investigated. The role of antiplatelet agents to
prevent periprocedural thrombotic complications during TAVR may merit further investigation.
LimitationsThe present study has several limitations: (i) the present findings are subject to the inherent
limitations of the included RCTs due to study design, follow-up, imaging and neurocognitive
assessment drop-out and endpoint ascertainment; additionally, statistical heterogeneity was substantial
for some neuroimaging endpoints underscoring differences across trials; (ii) most of the valves
implanted in the included RCTs were SE or BE first-generation TAVR devices; as new-generation
TAVR devices seem to be associated with improved efficacy and safety compared with older
generations,32, 33 the magnitude of the benefit of EP may be attenuated with newer devices; (iii) due to
the relatively small sample size and low event rates the present study remains underpowered to detect
differences in hard clinical endpoints such as stroke and all-cause mortality; (iv) as longer term (≥ 1
year) follow-up was not available we cannot investigate the effect of intraprocedural EP on long-term
functional status.
ConclusionsNeuroprotection with EP devices during TAVR was associated with improved early imaging and
clinical neurologic outcomes. The neurologic benefits of EP appear to be consistent among valve types.
While the differences in overt stroke were not significant, use of intraoperative EP was associated with
10
a numeric stroke reduction which may become significant in larger RCTs powered for hard endpoints.
These results are hypothesis-generating and further prospective, adequately powered RCTs are
needed to establish the role of EP during TAVR.
Funding SourceNo external funding was available for this study.
DisclosuresDrs. Giustino, Faggioni, Chandrasekhar and Baber have no conflicts of interest to disclose. Drs.
Mehran and Dangas have received consultant and speaker honoraria (modest level) from Bristol-Myers
Squibb, Sanofi-Aventis, Eli Lilly, Daiichi Sankyo, Abbott Vascular, AstraZeneca, Boston Scientific, and
Johnson & Johnson. Dr. Veltkamp has received research support, consultant and speaker honoraria
from Bayer, Boehringer, BMS, Pfizer, Daiichi Sankyo, Medtronic, Morphosys, St. Jude medical,
Apoplex Medical technologies and Sanofi.
11
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Figure LegendFigure 1. Neurologic Imaging Endpoints. Total lesion volume in mm3 (1A), mean number of new
ischemic lesions (1B) and patients with new ischemic lesions (1C). Results are reported as
standardized mean differences (with 95% confidence intervals [CI]) for continuous variables and risk
ratio (with 95% confidence intervals [CI]) for categorical variables.
Figure 2. Primary neurologic imaging endpoints per type of valve implanted. Total lesion volume
in mm3 (2A) and number of new lesions (2B).
Figure 3. Neurologic Clinical Endpoints. Any worsening in National Institutes of Health Stroke Scale
(NIHSS) at discharge (3A) and MoCA score at discharge (3B); clinically overt strokes at 30 days (3C).
Figure 4. All-cause Mortality. Risk of 30-day all-cause mortality.
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Table 1. Characteristics of the included randomized controlled trials.
Trial Year
Device type
EP arm (n)
No EP arm (n)
Mean
age
Male
(%)
STS score
(%)
TAVR access
site
Type of THV
devicePrimaryendpoint
Type ofimaging
test
Timing of
imaging
Neurological
assessment
CLEAN-TAVI14
2014
Claret MontageTM dual-filter
50 50 80 43% 5.4%Femoral100% SE 100%
Number of ischemic brain lesions at 2 days vs baseline in protected territories
DW-MRI 3THigh-resolution T1-weighted anatomical image. Diffusion-weighted imaging (DWI) for ischemic lesions
Baseline andday 2-7-30 after TAVR
Serial assessment with NIHSS
DEFLECT-III15
2015
TriGuard HDH 46 39 82 45% 6.9%
Femoral96%transapical 4%
BE 63%SE 31%Other 6%
MACCE (all-cause mortality, all stroke,life-threatening bleeding, AKIstage 2 or 3, and major vascular complications)
DW-MRI
Baseline andDay 4±2 and 30 ±7 after TAVR
Serial assessment with NIHSS, mRS, MoCAcomputerized Cogstate Research Test
EMBOL-X16 2015
Claret Embol-X
14 16 82 40% 10.3% Transaortic 100%
BE 100%
Number and size of new ischemic cerebral lesion within 7 days after TAVR
DW-MRI 1.5T transversal fluid-attenuated inversion recover and transversal diffusion-weighted
Baseline andwithin a week after TAVR
Clinical observation
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images of the whole brain
MISTRAL-C17
2015
Claret Sentinel 32 33 82 52% - NA BE 74%
SE 26%
New brain ischemic lesions 5 days after TAVR
DW-MRI 3T
Baseline andday 5
Serial assessment with CES-D, MMSE, MOCA
AKI=Acute Kidney Injury; BE=Balloon-Expandable; CES-D= Center for Epidemiological Studies-Depression; DW-MRI= Diffusion Weighted Magnetic Resonance Imaging; EP=Embolic Protection; MACCE= Major Adverse Cardiac and Cerebrovascular Event; MoCA= Montreal Cognitive Assessment; NA=Not Available; NIHSS= National Institute of Health Stroke Scale; nRS= modified Rankin Scale; SE= Self-Expandable; TAVR=Transcatheter Aortic Valve Replacement; THV=Transcatheter Heart Valve.
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