Stroke Clinical Trial
Official title:
Prognostic Value of the Circadian Pattern of Ambulatory Blood Pressure for Multiple Risk Assessment
The HYGIA study was designed to investigate prospectively
1. the prognostic value of ambulatory blood pressure (BP) monitoring among subjects
primarily evaluated at primary care settings
2. the impact of changes in ambulatory BP during follow-up in cardiovascular,
cerebrovascular, metabolic, and renal risk in hypertensive patients
3. the influence of circadian time of treatment in cardiovascular, cerebrovascular,
metabolic, and renal risk in hypertensive patients
4. the prevalence of an altered BP profile as a function of antihypertensive treatment,
circadian time of treatment, age, and presence of diabetes, among other factors.
Ambulatory blood pressure (BP) measurements (ABPM) correlate more closely with target organ
damage and cardiovascular events than clinical cuff measurements. ABPM reveals the
significant circadian variation in BP, which in most individuals presents a morning increase,
small post-prandial decline, and more extensive lowering during nocturnal rest. However,
under certain pathophysiological conditions, the nocturnal BP decline may be reduced
(non-dipper pattern) or even reversed (riser pattern). This is clinically relevant since the
non-dipper and riser circadian BP patterns constitute a risk factor for left ventricular
hypertrophy, albuminuria, cerebrovascular disease, congestive heart failure, vascular
dementia, and myocardial infarction. Hence, there is growing interest in how to best tailor
and individualize the treatment of hypertension according to the specific circadian BP
pattern of each patient.
The reduction of the normal 10-20% sleep-time BP decline that is characteristic of the
non-dipper and riser patterns is indeed associated with elevated risk of target organ damage,
particularly to the heart (left ventricular hypertrophy, congestive heart failure, and
myocardial infarction), brain (stroke), and kidney (albuminuria and progression to end-stage
renal failure). These results suggest that cardiovascular risk could be influenced not by BP
elevation alone, but also by the magnitude of the circadian BP variability. However, the
potential dimension of an altered BP profile is still under debate, as there is current
discrepancy on the actual prevalence of a non-dipper BP profile among groups of interest,
mainly the elderly, patients with diabetes and patients with resistant hypertension.
Moreover, several independent prospective studies have suggested that nighttime BP may be a
better predictor of cardiovascular risk than daytime BP. Common to all previous trials is
that prognostic significance of ABPM has relied on a single baseline profile from each
participant, without accounting for possible changes in the BP pattern, mainly associated to
antihypertensive therapy and aging during follow-up. Moreover, the potential benefit, i.e.,
reduction in cardiovascular risk, associated with the normalization of the circadian BP
variability (e.g., conversion from non-dipper to dipper pattern) from appropriately
envisioned treatment strategy is still a matter of debate.
The HYGIA study was designed to investigate, first, the comparative prognostic value of
several BP parameters (including, among many others, BP variability, the diurnal/nocturnal
ratio, diurnal and nocturnal means, hyperbaric index, slope of morning rise, etc) in the
prediction of vascular, metabolic, and renal morbidity and mortality; second, whether
potential changes in the circadian BP pattern after treatment with hypertension medications
may be associated to changes in the risk of cardiovascular events, stroke, diabetes, and/or
chronic kidney disease; and third, in keeping with the second major objective above, to
further assess the potential changes in efficacy, safety profile, and/or capability of
hypertension medications, used either alone or in combination, to modulate the circadian BP
pattern and to reduce vascular, metabolic, and renal risks as a function of the circadian
time of administration.
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