Impact of metabolic syndrome on fractional flow reserve

P. Türker Bayir; S. Duyuler; Ü. Güray; B. Kalayci; S. Kalayci; S. Cerşit; M. Gençaslan

this issue

previous article in this issue

next article in this issue

Document Details :

Title: Impact of metabolic syndrome on fractional flow reserve
Author(s): P. Türker Bayir , S. Duyuler , Ü. Güray , B. Kalayci , S. Kalayci , S. Cerşit , M. Gençaslan
Journal: Acta Cardiologica
Volume: 68 Issue: 6 Date: 2013
Pages: 569-574
DOI: 10.2143/AC.68.6.8000003

Abstract :
Objective: Fractional flow reserve (FFR) assessment is widely used to determine significance of intermediate coronary lesions. Previously, components of the metabolic syndrome (MS) which may affect FFR validity were not tested cumulatively. In this study, we investigate the possible effect of MS on FFR assessment.
Methods and results: We retrospectively evaluated 178 consecutive patients who had undergone FFR assessment. Thirty-two patients were excluded. All of the coronary lesions were in the left anterior descending artery. They were evaluated with quantitative coronary angiography (QCA). In 105 patients the MS was present and 41 patients were without the MS. According to the severity of the coronary lesions in QCA, patients were divided into three groups: 40-50%, 51-60% and 61-70% lesions. FFR measurements were compared in each group with respect to MS presence. Coronary artery lesions were accepted as haemodynamically significant if FFR ≤ 0.80. Age of the population, lesion length, lesion diameter and adenosine dosage performed during FFR assessment were not different between patients with MS or without MS. When the lesions were divided into three categories according to the severity of the luminal narrowing expressed in stenosis percentages as 40-50, 51-60, and more than 61%, the observed FFR values decreased with advancing lesion category (P = 0.04). However, observed FFR values did not differ between the patients with MS and without MS in each category (P = 0.88). After exclusion of the diabetic patients, FFR values still did not differ between the patients with MS and without MS in each category (P = 0.78).
Conclusions: Presence of the metabolic syndrome has no significant effect on FFR assessment. This study provides additional data for the reliability of FFR in patients with MS.