03609nas a2200625 4500000000100000008004100001653001100042653001100053653000900064653002200073653000900095653001600104653001700120653003000137653003000167653001400197653002200211653004200233653004200275653003100317653006100348653004400409653003500453653003000488653003800518653002700556653006200583653002600645653002900671653002600700100001100726700001300737700001800750700001500768700001400783700001700797700001200814700001300826700001400839700001300853700001700866700001900883700001400902700001300916700001300929700001300942700001600955700001300971245014100984250001501125300001101140490000701151520177401158020005102932�� 2015 d�10�aFemale�10�aHumans�10�aAged�10�aFollow-Up Studies�10�aMale�10�aMiddle Aged�10�aRisk Factors�10�aPredictive Value of Tests�10�aDrug Therapy, Combination�10�aIncidence�10�aAged, 80 and over�10�aRandomized Controlled Trials as Topic�10�aCardiovascular Diseases/ epidemiology�10�aBlood Pressure/ physiology�10�aAngiotensin-Converting Enzyme Inhibitors/therapeutic use�10�aAntihypertensive Agents/therapeutic use�10�aBenzimidazoles/therapeutic use�10�aBenzoates/therapeutic use�10�aCognition Disorders/ epidemiology�10�aHeart Rate/ physiology�10�aHypertension/ complications/drug therapy/ physiopathology�10�aMultivariate Analysis�10�aRamipril/therapeutic use�10�aRetrospective Studies�1 �aTeo K.�1 �aUnger T.�1 �aSchumacher H.�1 �aSleight P.�1 �aDiener H.�1 �aO'Donnell M.�1 �aLonn E.�1 �aRedon J.�1 �aFagard R.�1 �aSliwa K.�1 �aSchmieder R.�1 �aAnderson Craig�1 �aMancia G.�1 �aBöhm M.�1 �aYusuf S.�1 �aLeong D.�1 �aCustodis F.�1 �aLaufs U.�00�aSystolic blood pressure variation and mean heart rate is associated with cognitive dysfunction in patients with high cardiovascular risk� �a2015/01/15� �a651-61�0 �v65�3 �a
Elevated systolic blood pressure (SBP) correlates to cognitive decline and incident dementia. The effects of heart rate (HR), visit to visit HR variation, and visit to visit SBP variation are less well established. Patients without preexisting cognitive dysfunction (N=24 593) were evaluated according to mean SBP, SBP visit to visit variation (coefficient of variation [standard deviation/meanx100%], CV), mean HR, and visit to visit HR variation (HR-CV) in the Ongoing Telmisartan Alone and in Combination with Ramipril Global Endpoint Trial and the Telmisartan Randomized Assessment Study in ACE Intolerant Subjects with Cardiovascular Disease. Cognitive function was assessed with mini mental state examination. Cognitive dysfunction (fall in mini mental state examination /=5 points), and cognitive deterioration (drop of >1 point per year or decline to <24 points) were assessed. SBP and HR were measured over 10.7+/-2.2 (mean+/-SD) visits. Mean SBP, mean HR, and SBP-CV were associated with cognitive decline, dysfunction, and deterioration (all P<0.01, unadjusted). After adjustment, only SBP-CV (P=0.0030) and mean HR (P=0.0008) remained predictors for cognitive dysfunction (odds ratios [95% confidence intervals], 1.32 [1.10-1.58] for 5th versus 1st quintile of SBP-CV and 1.40 [1.18-1.66] for 5th versus 1st quintile of mean HR). Similar effects were observed for cognitive decline and deterioration. SBP-CV and mean HR showed additive effects. In conclusion, SBP-CV and mean HR are independent predictors of cognitive decline and cognitive dysfunction in patients at high CV risk. CLINICAL TRIAL REGISTRATION URL: http://www.clinicaltrials.gov. Unique identifier: NCT 00153101.
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