Aortic Stenosis Clinical Trial
Official title:
Prospective Study Focused on idEntification of cliNical, Biological and Imagistic Parameters in rapId-proGression Subgroup Patients With Moderate Aortic Stenosis
The investigators aim to identify all clinical, biological, echo and imagistic parameters that predispose to increased progression rates in a prospective observational trial which will include ONLY patients with moderate AS, with the complete cardiological investigational tools provided in 2012. Once those parameters are found, medical and interventional treatment could be implemented to decrease the mortality rates.
1. Why this study? 1.1. Significance and difficulty of the problem being addressed. Aortic
stenosis is the most encountered valvular disease According to the 2007 ESC guidelines
(1), moderate aortic stenosis (AS) is defined as valve area 1.0-1.5 cm² (0.6 cm²/m² to
0.9 cm²/m² body surface area (BSA)) or mean aortic gradient of 30-50 mmHg in the
presence of normal flow conditions. We already know how to treat patients with severe
AS, symptomatic or not. On the contrary, in patients with moderate AS there is not a
clear agreement on what to do to reduce the excess mortality (detailed below). Why do
these patients die and what can we do to reduce mortality rates? 1.2. Originality of
the proposed solution and the appropriateness of the objectives. There are already some
progression factors in all spectrum of AS that have been highlighted (discussed below)
and which could influence mortality in this patient subgroup, but none of the studies
address exclusively to moderate AS. The majority of these studies have major
limitations, are not prospective, and even if some are, the parameters followed do not
cover the complete cardiological investigational tools (no 3D left ventricular (LV)
ejection fraction (EF), no strain, no magnetic resonance imaging (MRI), etc.). As in
any major disease, lots of studies that include moderate AS are contradictory on the
same matter (see progression of AS). We aim to identify all clinical, biological, echo
and imagistic parameters that predispose to increased progression rates in a
prospective randomized trial which will include ONLY patients with moderate AS, with
the investigational tools provided in 2012. Once those parameters are found, medical
and interventional treatment could be implemented to decrease the mortality rates.
But first, some data about survival and death in moderate AS. I would like to start by
paraphrasing one of the most passionate researchers in the field of aortic stenosis, C.
Otto (2): "even mild disease is important" (referring of course at the outcomes of
patients with mild AS). Similarly, people with moderate AS/ aortic sclerosis, not even
mentioning moderate to severe AS (3) have an increased death rate in comparison to
age-matched healthy population. The same author reported in 1999 the results of a
prospective study (4) with a follow-up (FU) at 5 years and she observed a cardiac death
rate of 6.1% in general population (normal aortic valves), 10.1% in patients with
aortic sclerosis and 19.6% in patients with AS. In 2004 Rosenhek et al. (5) found a
cardiac death rate of 8.7% in a population with mean age of 67 years, with moderate AS
at the initial examination. Even though the largest study (6) evaluating medical
treatment in moderate AS reported a cardiac death rate of 6.0% (similar to general
population), we consider this study not eloquent because there was a super-selected
population enrolled (investigators ruled out the most important progression factors of
AS: exclusion criteria included history of coronary artery disease (CAD), stroke and
diabetes mellitus (DM)).
2. Trials involving patients with moderate AS. In this presentation we will not review or
discuss outcomes of severe AS, but ONLY outcomes of patients with MODERATE AS.
The first step in our research was the identification of all studies involving moderate
AS. We observed that there are few studies that included ONLY patients with moderate
AS. At the opposite, the large majority of studies included moderate AS among all
spectrum of AS patients (sclerosis, mild, moderate, severe- alone or combined). That is
why we categorized all previous studies regarding moderate AS by the baseline inclusion
criteria. We found 4 major groups of enrolled patients that we reviewed and discussed
below: patients with mild to moderate AS (Table 1) (5-10), patients with moderate AS
(Table 2)(11-12), patients with mild, moderate and severe AS (Table 3)(13-20) and
patients with moderate to severe AS (Table 4)(21-27).
Even though all essential data regarding moderate AS can be easily read in the tables
(patient characteristics, progression of moderate AS, outcomes, survival, limitations
and conclusions) and even though progression factors are summed-up below, of great
importance are the results of some echo studies recently published on which I would
like to briefly discuss. Monin et al. enrolled 107 patients with baseline peak velocity
(PV) of 3.5 to 4.4 m/s (26), he concluded that female sex, PV and brain natriuretic
peptide (BNP) at baseline were correlated with AS progression and developed a score to
best stratify outcomes in these patients (see Table 4 for limitations). Marechaux et
al. (27) included 135 patients with at least moderate AS (53% had severe AS), with
normal stress test at baseline. Increased progression was present in those with resting
mean gradient (MG) >35 mmHg and exercise-induced increase in MG >20 mmHg (see Table 4
for limitations). Two studies tried to clarify the role of strain in AS. One of the
studies showed that strain gradually decreased as severity of AS increases and that
global longitudinal strain (GLS) might be useful to assess subtle changes in LV
function in patients with mild, moderate and severe AS (17). In the second study, Ng et
al. (19) found that longitudinal, radial and circumferential strain and strain rate
(SR) deteriorate with aortic valve disease progression. Important limitations of both
studies are found in Table 3.
3. Progression of AS. There is a wide variability in AS progression. Progression rates
(for the PV) begin from 0.15±0.01 m/s/y in population without cardiovascular risk
factors (6) and increase to 0.34±0.42 m/s/y in patients with CAD, reaching 0.45±0.38
m/s/y in patients with cardiovascular events (5).
High progressors are those that have at least one abnormal parameter of the followings:
echocardiography parameters: baseline PV (3, 12, 5, 10, 16, 20, 26), baseline peak
gradient (24), mean gradient (3), rate of increase in PV (3, 20), moderate to severe
aortic valve calcification on echo (5, 12), LV hypertrophy (27), resting MG >35 mmHg
(27), exercise-induced increase in MG >20 mmHg (27), E velocity (16), bicuspid aortic
valve (16); clinical predictors: CAD (5, 21), age (>80 years-8, 12, 18, 20, >64
years-21, >65years-27), diabetes (14, 27), metabolic syndrome (MS) (24), dialysis (28,
29), increased BMI (7), functional status (3), history of smoking (7, 30), systolic
blood pressure (SBP) (18, 30), male gender (24, 30), female gender (26); and biological
parameters: parathyroid hormone (PTH) level (18), BNP at baseline (26), high
lipoprotein (a) (Lp(a)) and low density lipoprotein (LDL) cholesterol levels (30).
No influence on AS progression were treatment with simvastatin and ezetimibe (6),
elprenone (25) or rosuvastatin (9) and statins (14).
Slower progression was observed after osteoporosis (11) and bisphosphonate treatment
(15), but studies were either too small, retrospective (11, 15) or biased (11).
Geographical differences are evident in two papers which show that Korean patients
progress slower than western population (12, 16).
Data regarding the role of C-reactive protein in AS progression are controversial (10,
13).
We did not discuss the old studies or small series of patients with AS, some in the era
of cardiac catheterizations (31-36), some in the early echo decades (37-41). Their
capability to address this subject was limited by a retrospective design in most cases,
potential selection bias, limited clinical, functional, or exercise data, the
availability of only two data points per patient, lack of factors that predict the rate
of hemodynamic progression and clinical outcome.
4. Incidence of AS. Degenerative aortic valve disease evolves slowly from aortic sclerosis
to aortic stenosis. Aortic sclerosis and stenosis are found in about 29% and 2-9%
respectively in adults older than 65 years (4). In 5,201 subjects > 65 years, aortic
valve sclerosis was present in 26% and AS in 2% of the entire study cohort; in subjects
>75 years of age, sclerosis was present in 37% and stenosis in 2.6% (30). The
prevalence of critical AS was 2.9% in the group 75 to 86 years of age in another study
(42). In an observational study (43) which enrolled 953 subjects (aged 25-74 years),
the overall prevalence of degenerative aortic valve disease (defined as the presence of
valvular sclerosis, calcification, or thickening on echocardiographical examination)
was 28%. The prevalence of degenerative aortic valve disease by age groups was the
following: 7% (35-44 years), 19% (45-54), 30% (55-64), 38% (65-74) and 64% (75-84).
There were no significant differences between men and women.
Clinical factors associated with AS are similar to those associated with CAD (3, 44). Even
though several small non-randomized studies (45, 46-49) suggested a beneficial effect of
statins, three prospective randomized studies did not find any effect of lipid-lowering
therapy on the progression of aortic-valve stenosis.(6, 10, 50).
;
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