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Acta Cardiologica Sinica 2015-Mar

The Effects of Niacin on Inflammation in Patients with Non-ST Elevated Acute Coronary Syndrome.

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Entra registrati
Il collegamento viene salvato negli appunti
Emir Karacaglar
Ilyas Atar
Cihan Altin
Begum Yetis
Abdulkadir Cakmak
Nilufer Bayraktar
Ali Coner
Bulent Ozin
Haldun Muderrisoglu

Parole chiave

Astratto

BACKGROUND

In this study, we aimed to evaluate the effects of niacin on high sensitivity C reactive protein (hs-CRP) and cholesterol levels in non-ST elevated acute coronary syndrome (NSTE-ACS) patients.

METHODS

In this prospective, open label study, 48 NSTE-ACS were randomized to niacin or control group. Patients continued their optimal medical therapy in the control group. In the niacin group patients were assigned to receive extended-release niacin 500 mg/day. Patients were contacted 1 month later to assess compliance and side effects. Blood samples for hs-CRP were obtained upon admittance to the coronary care unit, in the third day and in the first month of the treatment. Fasting blood samples for cholesterol levels were obtained before and 30 days after the treatment. The primary end point of the study was to evaluate changes in hs-CRP, cholesterol levels, short-term cardiovascular events, and the safety of niacin in NSTE-ACS.

RESULTS

Baseline demographic, clinical and laboratory characteristics were similar between the two groups. Logarithmic transformation of baseline and 3(rd) day hs-CRP levels were similar between the groups; but 1 month later, logarithmic transformation of hs-CRP level was significantly lower in the niacin group (0.43 ± 0.39 to 0.83 ± 0.91, p = 0.04). HDL-C level was significantly increased in the niacin group during follow-up. Drug related side effects were seen in 7 patients in the niacin group but no patients discontinued niacin.

CONCLUSIONS

Our findings demonstrate that lower dose extended release niacin can be used safely and decreases hs-CRP and lipid parameters successfully in NSTE-ACS patients.

BACKGROUND

Acute coronary syndrome; hs-CRP; Inflammation; Niacin.

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