Vascular Stiffness Clinical Trial
Official title:
A Prospective Observational Study Comparing a Non-operator Dependent Automatic PWV Analyser to Pulse Pressure, in Assessing Arterial Stiffness in Hemodialysis
Chronic kidney disease (CKD) accelerates vascular stiffening related to age. Arterial
stiffness may be evaluated measuring the carotid-femoral pulse wave velocity (PWV) or more
simply, as recommend by KDOQI, monitoring pulse pressure (PP). Both correlate to survival
and incidence of cardiovascular disease. PWV can also be estimated on the brachial artery
using a Mobil-O-Graph; a non-operator dependent automatic device. The aim was to analyse
whether, in a dialysis population, PWV obtained by Mobil-O-Graph (MogPWV) is more sensitive
for vascular aging than PP.
A cohort of 143 patients from 4 dialysis units has been followed measuring MogPWV and PP
every 3 to 6 months and compared to a control group of non-CKD patients.
Chronic hemodialysis patients should have arterial stiffness evaluated monthly using Pulse
Pressure as suggested by KDOQI guidelines [1]. This recommendation pursues a dual goal since
it outlines the importance of monitoring vascular stiffness in hemodialysis patients [2-4]
and, at the same time, emphasizes the fact that Pulse Pressure provides valuable information
on tissue perfusion characteristics [5]. Arterial stiffening in dialysis patients is the
result of aging, non-specific and End Stage Renal Disease (ESRD) related risk factors, such
as medial calcification, volume overload, uraemia-related endothelial dysfunction, increased
extracellular matrix and intimal fibroelastic thickening [6]. Arterial stiffness of the
aorta and its major branches can be evaluated by measuring Pulse Wave Velocity (PWV) - e.g.
carotid-femoral Pulse Wave Velocity ("gold standard") [7] - or, alternatively, it can be
estimated by Pulse Wave Analysis (PWA) at a peripheral site, usually the brachial artery
[8-11]. In the first case, a doppler ultrasound detector is used together with a software
tool for data analysis. The second approach requires the use of a sphygmomanometer, such as
the Mobil-O-Graph, capable of analysing the pulse wave morphology and of calculating PWV
[9-14]. The first methodology is complex, operator-dependent and not routinely applicable,
whereas the second one is potentially usable in clinical practice [9].
The increase in PWV related to the above-mentioned risk factors also accelerates with age
[7].
Both PWV and PP correlate to mortality in the dialysis population [15-17]: for each PWV
increase of 1 m/s Blacher et al. found an all-cause mortality-adjusted OR of 1.39 (95% CI,
1.19 to 1.62) [16] while for each 10 mmHg increase in PP, Tozawa et al. found an increase in
all-cause mortality relative risk of 8% [17].
Risk factors such as age, hypertension, previous history of heart diseases and diabetes
influence the evolution of Pulse Wave Velocity before dialysis initiation whereas their
impact during the course of dialysis has not yet been demonstrated [18]. In this regard, a
study published in 2013 by Utescu et al. indicated that the only risk factor significantly
associated with PWV progression was the level of an advanced glycation end-product known as
pentosidine [18]. The results of this study confirmed that specific uraemia-related risk
factors can be identified and possibly quantified.
In the above-mentioned study, the rate of PWV progression (+0.84 m/s per year) was
surprisingly high, especially when projected over time as a function of the average life
span of ESRD patients on dialysis. Another critical data point outlined in the study was the
discrepancy in the annual rate of change in carotid-femoral compared to carotid-radial Pulse
Wave Velocity, which was +0.84 m/s per year and -0.66 m/s per year, respectively. The
authors of the study postulate that this discrepancy may be due to anatomical differences
between central (elastic) and peripheral (muscular) arteries and that the latter could
deploy an adaptive response to central aortic stiffening. Although interesting, these data
raise some concerns about the promising possibility of using the brachial artery as a site
for PWV estimation, even if based on a non-operator dependent method.
Furthermore, another limitation identified in the literature currently available on
prospective longitudinal studies analysing the PWV behaviour on dialysis patients, is the
lack of a control group made up of patients with similar characteristics and co-morbidities
but without kidney failure [2,16,18].
In the light of this, we decided to test a Mobil-O-Graph, a simple device estimating PWV
(MogPWV) through a modified sphygmomanometer on the brachial artery and to analyse the
baseline and follow-up MogPWV values in a cohort of dialysis patients and in a control group
with the same risk factors but without kidney failure.
The aim of the study was answering the following 4 questions, which also reflect both the
primary and the secondary endpoints of the trial: 1. Does PWV estimated by Mobil-O-Graph on
the brachial artery, be more sensitive for vascular aging and better discriminate the
dialysis population from the control group than pulse pressure? (primary endpoint); 2. Is
MogPWV progression faster during dialysis than in the pre-dialysis setting? (secondary
endpoint); 3. Are there specific risk factors that correlate to MogPWV progression?
(secondary endpoint); 4. Does mortality correlate to MogPWV? (secondary endpoint).
;
Observational Model: Cohort, Time Perspective: Prospective
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