26 results on '"Ahn, Sylvie A."'
Search Results
2. Potential synergistic antihyperglycemic effects of co-supplemental Amla and Olive extracts in hyperlipidemic adults with prediabetes and type 2 diabetes: results from a real-life clinical study.
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Hermans, Michel P., Ahn, Sylvie A., Rousseau, Michel F., Seidel, Laurence, Albert, Adelin, Janssens, Isabelle, Dierckxsens, Yvan, and Khan, Amjad
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- 2024
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3. Performances of a novel chemiluninescence ABEI-based NT-proBNP immunoassay.
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Adamantidou, Christina, Ahn, Sylvie, Rousseau, Michel, and Gruson, Damien
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NATRIURETIC peptides ,IMMUNOASSAY ,HEART failure ,EARLY diagnosis - Abstract
Natriuretic peptides are widely used in clinical practice as cardiac markers for early diagnosis, prognosis and for the monitoring of treatment efficiency of heart Failure (HF). According to the clinical relevance of natriuretic peptides testing, it is important to assess the performances of novel platform for testing. Our study showed the overall good performances of a new NT-proBNP ABEI-based automated immunoassay. [ABSTRACT FROM AUTHOR]
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- 2022
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4. Lipid and cardiometabolic features of T2DM patients achieving stricter LDL-C and non-HDL-C targets in accordance with ESC/EAS 2019 guidelines.
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Hermans, Michel P., Ahn, Sylvie A., and Rousseau, Michel F.
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LDL cholesterol ,LOW density lipoproteins ,TYPE 2 diabetes risk factors ,HEART metabolism disorders ,DRUG therapy for heart diseases - Abstract
New recommendations call for lowering LDL-C < 55 mg/dL and non-HDL-C < 85 mg/dL in very-high cardiovascular risk (VH-CVR) patients with type 2 diabetes (T2DM). This study assessed the proportion of VH-CVR diabetics currently meeting these primary and secondary lipid targets, and which therapies/phenotypes predict combined goals achievement. We analysed the cardiometabolic phenotype, use of lipid-modulatind drugs (LMD), pre- and post-LMD lipids levels, and CV complications among 1196 T2DM with high (n = 221; 18%) or VH-CVR (n = 975; 82%). Among the latter, the characteristics of combined lipid goal-achievers (n = 158) were compared to those of non-achievers (n = 817), with subgroup analyses of on-statin patients (n = 732) and those with established CVD taking statins (n = 362). Presence of statin-associated muscle symptoms (SAMS) was also recorded. 75% of VH-CVR patients were on statins. Both LDL-C and non-HDL-C goals were achieved by 16.2% of all VH-CVR, 19.3% of on-statin VH-CVR, and 24.3% of patients with established CVD taking statins. Achieving both targets was associated with high-intensity statins, specifically rosuvastatin, [statin + ezetimibe] combination, lower baseline LDL-C, smaller LDLs, lower TG and lipoprotein(a), and reduced metabolic syndrome frequency. SAMS reporting did not differ between achievers and non-achievers. More than 80% of patients are above targets. To bridge this gap, apart from treating more LMD-naive/refractory diabetics, one should consider for LDL-C to put most patients on high-intensity statins, more often with ezetimibe and, within statins, to switch preferably to rosuvastatin. As regards non-HDL-C, the off-target patients' phenotype suggests that intensifying lifestyle measures against metabolic syndrome should supplement current therapies. [ABSTRACT FROM AUTHOR]
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- 2021
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5. Prognostic Value of Pulmonary Transit Time by Cardiac Magnetic Resonance on Mortality and Heart Failure Hospitalization in Patients With Advanced Heart Failure and Reduced Ejection Fraction.
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Houard, Laura, Amzulescu, Mihaela S., Colin, Geoffrey, Langet, Helene, Militaru, Sebastian, Rousseau, Michel F., Ahn, Sylvie A., Vanoverschelde, Jean-Louis J., Pouleur, Anne-Catherine, and Gerber, Bernhard L.
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- 2021
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6. Crossing family histories of diabetes and cardiovascular disease leads to unexpected outcomes in diabetic offspring.
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Hermans, Michel P., Ahn, Sylvie A., and Rousseau, Michel F.
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CARDIOVASCULAR diseases - Abstract
Copyright of Journal of Diabetes is the property of Wiley-Blackwell and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)
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- 2019
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7. [HDL-C/apoA-I]: A multivessel cardiometabolic risk marker in women with T2DM.
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Hermans, Michel P., Valensi, Paul, Ahn, Sylvie A., and Rousseau, Michel F.
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Aims: Although women have higher high-density lipoprotein cholesterol (HDL-C) than have men, their HDL particles are also prone to become small, dense, and dysfunctional in case of type 2 diabetes mellitus (T2DM). To assess the vascular risk related to HDLs of different sizes/densities without direct measurement, we adjusted HDL-C to its main apolipoprotein (apoA-I) as [HDL-C/apoA-I]. This ratio estimates HDL sizes and provides indices as to their number, cholesterol load, and density.Methods: We stratified 280 Caucasian T2DM women according to [HDL-C/apoA-I] quartiles (Q) to determine how they are segregated according to cardiometabolic risk, β-cell function, glycaemic control, and vascular complications. Five parameters were derived from combined determination of HDL-C and apoA-I: HDL size, HDL number, cholesterol load per particle (pP), apoA-I pP, and HDL density.Results: An adverse cardiometabolic profile characterized QI and QII patients whose HDLs were denser and depleted in apoA-I, whereas QIII patients had HDLs with characteristics closer to those of controls. QIV patients had HDLs of supernormal size/composition and a more favourable phenotype in terms of fat distribution; insulin sensitivity (64% vs 41%), metabolic syndrome, and β-cell function (32% vs 23%); exogenous insulin (44 vs 89 U·d-1 ); and glycaemic control (glycated haemoglobin, 56 vs 61 mmol·mol-1 ), associated with lower prevalence of microvascular/macrovascular complications: all-cause microangiopathy 47% vs 61%; retinopathy 22% vs 34%; all-cause macroangiopathy 19% vs 31%; and coronary artery disease 6% vs 24% (P < .05).Conclusion: [HDL-C/apoA-I] can stratify T2DM women according to metabolic phenotype, macrovascular and coronary damage, β-cell function, microangiopathic risk, and retinopathy. This ratio is a versatile and readily available marker of cardiometabolic status and vascular complications in T2DM women. [ABSTRACT FROM AUTHOR]- Published
- 2018
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8. The mixed benefit of low lipoprotein(a) in type 2 diabetes.
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Hermans, Michel P., Ahn, Sylvie A., and Rousseau, Michel F.
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LOW density lipoproteins ,CARDIOVASCULAR diseases ,STATINS (Cardiovascular agents) ,TYPE 2 diabetes ,CARDIAC patients - Abstract
Background: Lipoprotein(a) (Lp(a)), a variant low-density lipoprotein (LDL), is a major genetic risk factor for cardiovascular disease. It is unknown whether an inverse relationship exists between Lp(a) and β-cell function (BCF), as for LDL-cholesterol (LDL-C) lowering by statins. We therefore assessedthe cardiometabolic phenotype of 340 men with type 2 diabetes mellitus (T2DM) in relation to Lp(a), focusing on BCF and hyperbolic product [BxS], which adjusts BCF to insulin sensitivity and secretion. Methods: Two groups were analyzed according to Lp(a) quartiles (Q): a (very-)low Lp(a) (Q1;n = 85) vs a normal-to-high Lp(a) group (Q2-Q4;n = 255). Results: In the overall cohort, mean Lp(a) was 52 nmol.L
-1 . Median Lp(a) was 6 nmol.L-1 (Q1) vs 38 nmol.L-1 (Q2-Q4). There were no differences between groups regarding age; education; diabetes duration; body mass index; body composition and smoking. Q1 had significantly worse glycemic control, higher systolic blood pressure, more severe metabolic syndrome, and more frequent hepatic steatosis. Insulin sensitivity was significantly lower (- 37%) in Q1, who also had lesser hyperbolic product (- 27%), and higher [BxS] loss rate (+ 15%). Q1 also had higher frequency (+31%) and severity (+20%) of atherogenic dyslipidemia. Microangiopathy and neuropathy were higher in Q1 (+ 34% and + 48%, respectively), whereas Q2-Q4 patients had increased macroangiopathy (+ 51%) and coronary artery disease (CAD; + 94%). Conclusions: Low Lp(a) appears both beneficial and unhealthy in T2DM. It is associated with unfavourable cardiometabolic phenotype, lesser BCF, poorer glycemic control, and increased microvascular damage despite being linked to markedly reduced CAD, suggesting that Lp(a)-related vascular risk) follows a J-shaped curve. [ABSTRACT FROM AUTHOR]- Published
- 2017
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9. Elevation of plasma oncostatin M in heart failure.
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Gruson, Damien, Ferracin, Benjamin, Ahn, Sylvie A, and Rousseau, Michel F
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Aim: Oncostatin M (OSM) is an inflammatory cytokine of the gp130 family. OSM could participate in adverse cardiovascular remodeling through regulation of FGF23.Materials& Methods: OSM levels were determined in 80 heart failure patients with reduced left ventricular ejection fraction (HFrEF).Results: OSM levels are significantly increased in HFrEF patients compared with healthy subjects. We have also demonstrated that, in HFrEF patients, plasma OSM levels are correlated to parathyroid hormone PTH(1-84) and 1,25(OH)2D, two other biomarkers related to bone and mineral metabolism and associated to adverse cardiovascular outcomes.Conclusion: OSM concentrations are elevated in HFrEF patients and could interplay with parathyroid hormone and vitamin D impacting cardiovascular function. Nevertheless, the prognostic value of OSM testing appears limited. [ABSTRACT FROM AUTHOR]- Published
- 2017
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10. Sflt-1 in heart failure: relation with disease severity and biomarkers.
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Gruson, Damien, Hermans, Michel P., Ferracin, Benjamin, Ahn, Sylvie A., and Rousseau, Michel F.
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HEART failure treatment ,HEART failure ,PROTEIN-tyrosine kinases ,SEVERITY of illness index ,BIOMARKERS ,PLACENTAL growth factor ,DIAGNOSIS - Abstract
Soluble fms-like tyrosine kinase-1 (sFlt-1) is an endogenous inhibitor of endothelial growth factors, such as placental growth factor (PlGF), which modulates cardiovascular (CV) remodeling. We determine sFlt-1 levels in patients with heart failure (HF) and its relationship to adverse cardiovascular (CV) events and biomarkers of cardiovascular risk. Levels of sFlt-1 and PlGF levels were also determined in healthy volunteers and patients with type 2 diabetes mellitus (T2DM). SFlt-1 and PlGF were clearly increased in HF patients in comparison to T2DM patients or healthy subjects (p < 0.01). Concentration of sFlt-1 was related to HF severity (p < 0.001) and was correlated to NT-proBNP (ρ = 0.37,p < 0.01), soluble ST2 (ρ = 0.52,p < 0.01), Galectin-3 (ρ = 0.38,p < 0.01), aldosterone (ρ = 0.25,p = 0.01) and PTH(1–84) (ρ = 0.38,p < 0.01). Furthermore, sFlt-1 levels were associated to long-term CV risk. These results suggest a potential role of sFlt-1 in HF and its potential role as biomarker of CV risk. [ABSTRACT FROM PUBLISHER]
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- 2016
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11. How to transform a metabolic syndrome score into an insulin sensitivity value?
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Hermans, Michel P., Bouenizabila, Evariste, Ahn, Sylvie A., and Rousseau, Michel F.
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Background: The metabolic syndrome (MetS) predicts cardiovascular risk and incident type 2 diabetes mellitus. The presence of a MetS is defined by the clustering of ≥3 out of 5 cardiometabolic criteria (hyperglycemia; hypertension; enlarged waist; low high-density lipoprotein-cholesterol; and hypertriglyceridemia), each of which is connected with insulin resistance. It is not known whether the severity of MetS, ranked from the sextet of scores range [0/5 to 5/5], is linearly related to reduced insulin sensitivity (IS) and/or lesser hyperbolic product across the glycemic spectrum.Patients and Methods: A total of 839 adults (54 normoglycemic; 785 with abnormal glucose homeostasis, among whom 711 type 2 diabetes mellitus) had insulin sensitivity assessed together with their cardiometabolic phenotype.Results: There was a significant gradient according to interval-scale MetS score in insulinemia; body mass index; (visceral) fat; hepatic steatosis; and macroangiopathy. There was an inverse linear relationship between increasing MetS scores and decreased insulin sensitivity, allowing to define an insulin resistance-predicting linear equation: IS (%) = [-15.1 × MetS score] + 109.4 (R(2) = 0.221). For each MetS category, mean IS values did not significantly differ between groups of patients across the glycemic spectrum. The hyperbolic product (β-cell function × IS) and/or its loss rate were inversely related to MetS severity.Conclusion: Insulin sensitivity is linearly and inversely related to MetS severity across the 6 scores. This novel way to exploit information intrinsic to the MetS criteria provides an easy and low cost means to quantify insulin sensitivity across the glycemic spectrum. Moreover, a higher MetS score is associated with lesser residual insulin secretion, and faster B-cell function loss. Copyright © 2015 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]- Published
- 2016
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12. 1,25-Dihydroxyvitamin D to PTH(1–84) Ratios Strongly Predict Cardiovascular Death in Heart Failure.
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Gruson, Damien, Ferracin, Benjamin, Ahn, Sylvie A., Zierold, Claudia, Blocki, Frank, Hawkins, Douglas M., Bonelli, Fabrizio, and Rousseau, Michel F.
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VITAMIN D deficiency ,HYPERPARATHYROIDISM ,CARDIOVASCULAR disease related mortality ,HEART failure ,PARATHYROID hormone ,VENTRICULAR remodeling - Abstract
Objectives: Vitamin D deficiency and hyperparathyroidism are common in patients with heart failure (HF). There is a growing body of evidence supporting the role of vitamin D and parathyroid hormone (PTH) in cardiac remodeling and worsening of HF. Lack of reliable automated testing of 1,25-dihydroxyvitamin D (1,25(OH)
2 D), the biologically active metabolite of vitamin D, has limited its contribution to the prognostic assessment of HF. Here, the association of 1,25(OH)2 D and PTH(1–84) levels was evaluated for prediction of cardiovascular death in chronic HF patients. Methods: We conducted a single center prospective cohort including 170 chronic HF patients (females n = 36; males n = 134; NYHA II-IV; mean age: 67 years; etiology: ischemic n = 119, dilated cardiomyopathy n = 51; mean LVEF: 23%). The primary outcome was cardiovascular death. Results: Serum levels of 1,25(OH)2 D decreased markedly with increased HF severity. Medians were 33.3 pg/mL for NYHA-II patients, 23.4 pg/mL for NYHA-III, and 14.0 pg/mL for NYHA-IV patients (p<0.001). Most patients had levels of 25(OH)D below 30ng/mL, and stratification by NYHA functional class did not show significant differences (p = 0.249). The 1,25(OH)2 D to PTH(1–84) ratio and the (1,25(OH)2 D)2 to PTH(1–84) ratio were found to be the most significantly related to HF severity. After a median follow-up of 4.1 years, 106 out of 170 patients reached the primary endpoint. Cox proportional hazard modeling revealed 1,25(OH)2 D and the 1,25(OH)2 D to PTH(1–84) ratios to be strongly predictive of outcomes. Conclusions: 1,25(OH)2 D and its ratios to PTH(1–84) strongly and independently predict cardiovascular mortality in chronic HF. [ABSTRACT FROM AUTHOR]- Published
- 2015
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13. Baseline diabetes as a way to predict CV outcomes in a lipid-modifying trial: a meta-analysis of 330,376 patients from 47 landmark studies.
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Hermans, Michel P., Bouenizabila, Evariste, Amoussou-guenou, Daniel K., Ahn, Sylvie A., and Rousseau, Michel F.
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DIABETES ,CARDIOVASCULAR system ,CORONARY disease ,CLINICAL trials ,LIPIDS - Abstract
Background: Diabetes is a major cardiovascular risk factor. However, its influence on the rate of occurrence of cardiovascular (CV) events during a clinical trial that included a diabetes subgroup has not yet been quantified. Aims: To establish equations relating baseline diabetes prevalence and incident CV events, based on comparator arms data of major lipid-modifying trials. Methods: Meta-analysis of primary outcomes (PO) rates of key prospective trials, for which the baseline proportion of diabetics was reported, including studies having specifically reported CV outcomes within their diabetic subgroups. Results: 47 studies, representing 330,376 patients (among whom 124,115 diabetics), were analyzed as regards the relationship between CV outcomes rates (including CHD) and the number of diabetics enrolled. Altogether, a total of 18,445 and 16,156 events occurred in the comparator and treatment arms, respectively. There were significant linear relationships between diabetes prevalence and both PO and CHD rates (%/year): y = 0.0299*x + 3.12 [PO] (p = 0.0128); and y = 0.0531*x+ 1.54 [CHD] (p = 0.0094), baseline diabetes predicting PO rates between 3.12 %/year (no diabetic included) and 6.11 %/year (all patients diabetic); and CHD rates between 1.54 %/year (no diabetic) and 6.85 %/year (all patients diabetic). The slopes of the equations did not differ according to whether they were derived from primary or secondary prevention trials. Conclusions: Absolute and relative CV risk associated with diabetes at inclusion can be readily predicted using linear equations relating diabetes prevalence to primary outcomes or CHD rates. [ABSTRACT FROM AUTHOR]
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- 2015
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14. Novel unbiased equations to calculate triglyceride-rich lipoprotein cholesterol from routine non-fasting lipids.
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Hermans, Michel P., Ahn, Sylvie A., and Rousseau, Michel F.
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EQUATIONS ,TRIGLYCERIDES ,LIPOPROTEINS ,CHOLESTEROL ,LIPIDS - Abstract
Background: Non-fasting triglyceride-rich lipoproteins cholesterol (TRL-C) contributes to cardiovascular risk, in that it includes remnant cholesterol (RC). TRL-C is computed as total C - [LDL-C + HDL-C]. Such calculation applies only if LDL-C is directly measured, or obtained from a non-Friedewald's formula, a method as yet never benchmarked against independent markers of TRL burden. Methods: The Discriminant Ratio (DR) methodology was used in 120 type 2 diabetic patients in order: (i) to compute TRL-C from non-fasting lipids, (ii) to establish the performance of TRL-C and TRL-C/apoA-I (vs. TG-based markers) to grade TRLs and atherogenic dyslipidemia (AD), and (iii) to relate TRL-C with non-fasting TG. Results: Depending on apoB
100 availability, TRL-C (mg/dL) can be derived from non-fasting lipids in two ways: (a) total cholesterol (TC) - [(0.0106 * TC - 0.0036 * TG + 0.017 * apoB100 - 0.27) * 38.6] - HDL-C, and (b) TC - [(0.0106 * TC - 0.0036 * TG + 0.017 * [0.65 * (TC - HDL-C) + 6.3] - 0.27) * 38.6] - HDL-C. Discrimination between log[TG] and TRL-C was similar (DR 0.94 and 0.84, respectively), whereas that of log[TG]/HDL-C was better than TRL-C/apoA-I (DR 1.01 vs. 0.65; p 0.0482). All Pearson's correlations between pairs reached unity, allowing formulation of two unbiased equivalence equations: (a) TRL-C = 97.8 * log[TG] - 181.9, and (b) TRL-C/apoA-I = 8.15 * (log[TG]/HDL-C) - 0.18. Conclusions: TRL-C and log[TG] are as effective and interchangeable for assessing remnant atherogenic particles. For grading TRL-AD, it is best to use log[TG]/HDL-C, inherently superior to TRL-C/apoA-I, while measuring the same underlying variable. [ABSTRACT FROM AUTHOR]- Published
- 2014
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15. Discriminant ratio and biometrical equivalence of measured vs. calculated apolipoprotein B100 in patients with T2DM.
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Hermans, Michel P., Ahn, Sylvie A., and Rousseau, Michel F.
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BIOMETRY ,APOLIPOPROTEINS ,CARDIOVASCULAR diseases ,LIPOPROTEINS ,ALGORITHMS ,CHOLESTEROL - Abstract
Background: Apolipoprotein B
100 (ApoB100 ) determination is superior to low-density lipoprotein cholesterol (LDL-C) to establish cardiovascular (CV) risk, and does not require prior fasting. ApoB100 is rarely measured alongside standard lipids, which precludes comprehensive assessment of dyslipidemia. Objectives: To evaluate two simple algorithms for apoB100 as regards their performance, equivalence and discrimination with reference apoB100 laboratory measurement. Methods: Two apoB100 -predicting equations were compared in 87 type 2 diabetes mellitus (T2DM) patients using the Discriminant ratio (DR). Equation 1: apoB100 = 0.65*non-high-density lipoprotein cholesterol + 6.3; and Equation 2: apoB100 = -33.12 + 0.675*LDL-C + 11.95*ln[triglycerides]. The underlying between-subject standard deviation (SDU ) was defined as SDU = v (SDB 2 B - SD2 W/2); the within-subject variance (Vw ) was calculated for m (2) repeat tests as (Vw) = S(xj -xi )2 /(m-1)), the within-subject SD (SDw ) being its square root; the DR being the ratio SDU /SDW . Results: All SDu , SDw and DR's values were nearly similar, and the observed differences in discriminatory power between all three determinations, i.e. measured and calculated apoB100 levels, did not reach statistical significance. Measured Pearson's product-moment correlation coefficients between all apoB100 determinations were very high, respectively at 0.94 (measured vs. equation 1); 0.92 (measured vs. equation 2); and 0.97 (equation 1 vs. equation 2), each measurement reaching unity after adjustment for attenuation. Conclusion: Both apoB100 algorithms showed biometrical equivalence, and were as effective in estimating apoB100 from routine lipids. Their use should contribute to better characterize residual cardiometabolic risk linked to the number of atherogenic particles, when direct apoB100 determination is not available. [ABSTRACT FROM AUTHOR]- Published
- 2013
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16. Sleep apnoea syndrome and 10-year cardiovascular risk in females with type 2 diabetes: relationship with insulin secretion and insulin resistance.
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Hermans, Michel P., Ahn, Sylvie A., Mahadeb, Yovan P., and Rousseau, Michel F.
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Background Obstructive sleep apnoea syndrome (OSAS) is a risk factor for type 2 diabetes mellitus (T2DM) and promotes cardiovascular events, especially in men. The prevalence of sleep apnoea and its association with microvascular and macrovascular diseases and glycaemic control are poorly documented in T2DM women. Methods A total of 305 T2DM women were sleep apnoea diagnosed through (hetero)anamnesis, Epworth's score, oximetry and polysomnography. Sleep apnoea[+] ( n = 25) were compared with sleep apnoea[−] ( n = 280) regarding cardiovascular risk factors, glucose homeostasis, micro/macrovascular complications and the United Kingdom Prospective Diabetes Study (UKPDS) 10-year risk. Results Mean (1 SD) age was 66 (12) years, diabetes duration 15 (9) years, sleep apnoea prevalence 8.2% and metabolic syndrome 86%. There were no differences in age, diabetes duration, education, smoking and blood pressure between groups. Sleep apnoea[+] had significantly higher values of body mass index, waist, relative/absolute fat, conicity, visceral fat (all p < 0.0001) and lower skeletal muscle ( p = 0.0008). The sleep apnoea[+] group was more insulin resistant [homeostasis model assessment (HOMA S): 37 (20)% versus 59 (44)%; p < 0.0001] and had lesser residual insulin secretion (HOMA B × S: 20 (12)% versus 30 (19)%; p = 0.0006), increased hyperbolic product loss ( p = 0.0442) and poorer glycaemic control (HbA
1c 69 (12) versus 62 (13) mmol mol−1 ; p = 0.0099). All atherogenic dyslipidaemia components and inflammatory markers were worsened in sleep apnoea[+]. Women with sleep apnoea had higher UKPDS risk of CAD: 18 (11)% versus 12 (10)% ( p = 0.0136). Prevalent micro/macrovascular complications were not different between groups. Conclusions Sleep apnoea, a frequent comorbidity of T2DM women, is associated with central fat, atherogenic dyslipidaemia, inflammation, worsening β-cell function, poorer glycaemic control and coronary artery disease risk. Sleep apnoea may increase residual vascular risk for microvascular and macrovascular events in T2DM women. Copyright © 2013 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]- Published
- 2013
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17. eNOS [Glu298Asp] polymorphism, erectile function and ocular pressure in type 2 diabetes.
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Hermans, Michel P., Ahn, Sylvie A., and Rousseau, Michel F.
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GENETIC polymorphisms ,TYPE 2 diabetes ,NITRIC oxide ,VASODILATORS ,CARDIOVASCULAR diseases ,SYNTHASES ,PHENOTYPES ,METABOLIC syndrome - Abstract
Eur J Clin Invest 2012; 42 (7): 729-737 Abstract Background Imbalance in nitric oxide (NO), an atheroprotective vasodilator, is associated with endothelial dysfunction, cardiovascular diseases (CVD) and diabetic complications. Various endothelial NO synthase (eNOS) polymorphisms may affect NO bioavailability, thereby promoting adverse cardiovascular milieu. Materials and methods To analyze glucose homeostasis, cardiometabolic phenotype, and micro- and macroangiopathies associated with eNOS G894T gene polymorphism in type 2 diabetes (T2DM). 210 T2DM outpatients (mean age (1SD) 70 (12); diabetes duration 19 (9) years; males:females 64:36%; metabolic syndrome 87%) had insulin sensitivity and b-cell function modelled with HOMA, alongside routine laboratory and endothelin measurements. Results GG, GT and TT genotypes represented 48% ( n = 100), 39% ( n = 83) and 13% ( n = 27). Overall microangiopathy (retinopathy, neuropathy and/or nephropathy) was present in 74%, and overall macroangiopathy (CAD, PAD and/or TIA/stroke) in 45%. The TT genotype did not translate into a more severe vascular phenotype, as TT patients carrying the proposed risk genotype did not suffer a higher rate of micro- and macrovascular complications. On the other hand, erectile dysfunction, present in 60% of males ( n = 135), was much more prevalent in TT males: 57% [GG & GT] vs. 93% in TT (p 0.0088). Ocular hypertension/glaucoma frequency (18% of the whole group) was also markedly different, albeit in opposing directions, between eNOS G894T gene polymorphism subgroups: 21% [GG & GT] vs. 0% prevalence (TT; p 0.0057). Conclusions eNOS G894T gene polymorphism in homozygous TT carriers translates into opposing effects on erectile function (detrimental) and ocular hypertension/glaucoma (protective) in T2DM, without affecting glucose homeostasis determinants or the presence of micro- and macrovascular complications. [ABSTRACT FROM AUTHOR]
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- 2012
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18. The atherogenic dyslipidemia ratio [log(TG)/HDL-C] is associated with residual vascular risk, beta-cell function loss and microangiopathy in type 2 diabetes females.
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Hermans, Michel P., Ahn, Sylvie A., and Rousseau, Michel F.
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DYSLIPIDEMIA ,PANCREATIC beta cells ,DIABETES ,TRIGLYCERIDES ,HOMEOSTASIS - Abstract
Background: Atherogenic dyslipidemia (AD), defined as low HDL-C plus elevated triglycerides (TG), comorbid to T2DM, increases cardiometabolic risk for CAD even when LDL-C is at target. In T2DM males, AD was shown to correlate with β-cell function loss, yet it is not established whether this applies across gender. Aim: To establish the prevalence and severity of AD in T2DM females, and to determine how it relates to cardiometabolic phenotype, glucose homeostasis, micro- and macrovascular complications, and 10-year absolute CV risk (UKPDS Risk Engine). Methods: 340 T2DM females were ranked according to quintiles (Q) of the continuous variable log(TG)/HDL-C, with AD prevalence defined as HDL-C <50 mg.dL-1 plus TG ≥150 mg.dL
-1 , and β-cell function assessed with HOMA. Results: AD prevalence was 35%; mean HDL-C and TG were 52 (15) and 160 (105) mg.dL-1 . AD was significantly related to central fat, metabolic syndrome, sedentarity and skeletal sarcopenia, as well as to hsCRP, fibrinogen, uric acid, cystatin-C, Big ET-1, and 10-year UKPDS CV risk. AD correlated stepwise with lower β-cell function and hyperbolic product, and with accelerated loss of residual insulin secretion, higher HbA1c and prevalent microangiopathy. Conclusions: log(TG)/HDL-C is a simple means to grade AD and residual macrovascular risk in T2DM females. This ratio associates with major non-LDL cardiometabolic variables and ranks predicted CAD risk. In addition, log(TG)/ HDL-C identifies worsening glucose homeostasis, poorer glycemic control, and prevalent microangiopathy. [ABSTRACT FROM AUTHOR]- Published
- 2012
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19. Non-HDL-cholesterol as valid surrogate to apolipoprotein B100 measurement in diabetes: Discriminant Ratio and unbiased equivalence.
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Hermans, Michel P., Sacks, Frank M., Ahn, Sylvie A., and Rousseau, Michel F.
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APOLIPOPROTEINS ,HYPERTRIGLYCERIDEMIA ,CHOLESTEROL ,ISOPENTENOIDS ,LIPOPROTEINS - Abstract
Background: Apolipoprotein B
100 (apoB) is a superior indicator of CV risk than total or LDL-C. Non-HDL-C represents a simple surrogate for apoB in hypertriglyceridemic and/or T2DM patients. ApoB and non-HDL-C show high correlation, although the degree of mutual concordance remains debated in CV risk evaluation. Objectives: We used the Discriminant Ratio (DR) methodology to compare the performance of non-HDL-C with that of apoB to rank diabetic patients according to dyslipidemia and to establish the underlying relationship between these variables taking measurement noise and intra-/intersubject variation into account, and to derive an unbiased equivalence equation. Methods: Fasting total C, HDL-C, apoB and triglycerides were measured in 45 diabetic patients. The DR of the underlying between-subject standard deviation (SD) to the within-subject SD was calculated from duplicates. Correlation coefficients between pairs were adjusted to include an estimate of the underlying correlation. Results: Mean values [day 1 (1SD)] were 143 (36) mg/dl (non-HDL-C) and 98 (24) mg/dl (apoB). The DR's of both parameters were similar (1.76 and 1.83) (p = 0.83). Pearson's product-moment correlation coefficient between tests was very high (0.94), reaching unity (1.00) after attenuation adjustment. The unbiased equation of equivalence relating apoB to non-HDL-C had a slope of 0.65 and an intercept of 6.3 mg/dl. Conclusions: The discrimination power of non-HDL-C is similar to that of apoB to rank diabetic patients according to atherogenic cholesterol and lipoprotein burden. Since true correlation between variables reached unity, non- HDL-C may provide not only a metabolic surrogate but also a candidate biometrical equivalent to apoB, as non- HDL-C calculation is readily available. [ABSTRACT FROM AUTHOR]- Published
- 2011
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20. log(TG)/HDL-C is related to both residual cardiometabolic risk and β-cell function loss in type 2 diabetes males.
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Hermans, Michel P., Ahn, Sylvie A., and Rousseau, Michel F.
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TYPE 2 diabetes ,HYPOGLYCEMIC agents ,INSULIN ,HOMEOSTASIS ,GLUCOSE - Abstract
Background: T2DM is associated with atherogenic dyslipidemia (AD), defined as decreased HDL-C plus raised triglycerides (TG). AD confers increased risk for CAD, even when LDL-C is at target. AD is rarely assessed due to lack of screening methods consensus. Aim: To establish the prevalence and severity of AD from log(TG)/HDL-C in T2DM males, and to determine how it relates to cardiometabolic phenotype, glucose homeostasis, micro- and macrovascular complications, and 10-year UKPDS CV risk. Methods: 585 T2DM males divided according to quintiles (Q) of log(TG)/HDL-C. AD prevalence defined as HDL-C <40 mg.dL-1 plus TG ≥150 mg.dL
-1 . β-cell function assessed with HOMA. Results: Mean HDL-C and TG were 44 (13) and 204 (155) mg.dL-1 . AD prevalence was 35%. AD correlated with lower b-cell function, with accelerated loss of insulin secretion, and with poorer HbA1c levels. AD was related to a high prevalence of CAD, and also to 10-year absolute CAD risk. Conclusions: log(TG)/HDL-C is a simple means to estimate AD and the residual CV risk it confers in T2DM. AD closely associates with major cardiometabolic and glucose homeostasis determinants and poorer metabolic control. The ratio also relates to macroangiopathy prevalence and ranks future CAD risk, and is well-suited to capture non- LDL-related macrovascular residual risk and major glycemic determinants. [ABSTRACT FROM AUTHOR]- Published
- 2010
- Full Text
- View/download PDF
21. Raised natriuretic peptides, Big-endothelin-1 and improved beta-cell function in type 2 diabetic males with hyperuricaemia.
- Author
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Hermans, Michel P., Ahn, Sylvie A., and Rousseau, Michel F.
- Abstract
Urate, a naturally-occurring antioxidant, is a marker/factor for cardiovascular disease. Hyperuricaemia is associated with IR, MetS and endothelial dysfunction. We characterised the associations between neurohormones, uricaemia, and glucose homeostasis in type 2 diabetes mellitus (T2DM) males. Cross-sectional; 705 T2DM males divided into two groups: uric acid < 7.0 mg/dl (normouricaemic; n=476) versus uric acid ≥ 7.0 mg/dl (hyperuricaemic; n=229). HOMA beta-cell function (B), insulin sensitivity (S), hyperbolic product (B×S), and (B×S) loss rate were determined alongside neurohormones (Nt-proANP, BNP, Big ET-1 and UII). Mean age and diabetes duration were not different between groups. Hyperuricaemics had more macroangiopathy, total/central adiposity, IR, hypertension, dyslipidemia and MetS prevalence. Nt-proANP and BNP levels were more than twice as high in hyperuricaemics, whereas Big ET-1 and UII were higher by 46% and 14%, respectively. HOMA (B×S) was higher in hyperuricaemics: 31 (16)% vs. 26 (18)% (p=0.0004). B×S loss rate was faster in normouricaemics: 1.36 (0.54)% vs. 1.20 (0.43)%/year-1 (p<0.0001 ). The proportion with HbA1C < 7.0% was 39% (normouricaemics) vs. 49% (hyperuricaemics; p=0.0091). In T2DM males, hyperuricaemia is associated with raised neurohormones together with better beta-cell indices. Urate's dual properties may translate into beneficial (glucose homeostasis) and detrimental (raised neurohormones) effects. [ABSTRACT FROM PUBLISHER]
- Published
- 2009
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22. Accuracy of N-terminal-pro-atrial natriuretic peptide in patients admitted to emergency department.
- Author
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Gruson, Damien, Rousseau, Michel F., Ahn, Sylvie, Van Linden, François, Thys, Frédéric, Ketelslegers, Jean‐Marie, and Verschuren, Franck
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ATRIAL natriuretic peptides ,CONGESTIVE heart failure ,IMMUNOASSAY ,NEUROPEPTIDES ,HOSPITAL emergency services - Abstract
Objective. B-type natriuretic peptide (BNP) and N-terminal-pro-BNP (Nt-proBNP) are commonly used for the triage of patients in the emergency department (ED) with dyspnoea and/or chest pain. The aim of our study was to determine the accuracy of N-terminal-pro-ANP (Nt-proANP) in such patients. Material and methods. Nt-proANP was measured by home-made radioimmunoassay in 137 ED patients admitted with cardiovascular and/or pulmonary disorders. BNP and Nt-pro-BNP were determined with automated assays. Final diagnosis was confirmed at discharge or after follow-up. Results. Nt-proANP levels were significantly influenced by the diagnostic subgroups (ANOVA: p<0.001) and were [geometric mean (range)]: 19727 ng/L (5260-45200) in congestive heart failure (CHF, n = 31), 6575 ng/L (1350-36000) in coronary artery disease (CAD, n = 19) , 5324 ng/L (1710-13150) in pulmonary embolism (PE, n = 20), 5035 ng/L (1510-16600) in pulmonary diseases (PD, n = 24) and 3001 ng/L (750-11860) in patients without cardiopulmonary diseases (n = 43). Pairwise comparisons demonstrated that CHF patients had Nt-pro-ANP values higher than all other groups (p<0.05) and that patients without cardiopulmonary diseases had the lowest values (p<0.05). For diagnosis of CHF, the area under the ROC curve of Nt-proANP was 0.94 (95 % CI: 0.89-0.98) and was equivalent to Nt-proBNP (0.91; p = 0.284) and BNP (0.93; p = 0.572). Conclusions. The diagnostic accuracy of Nt-proANP was equivalent to BNP and Nt-proBNP in the present cohort of patients admitted to ED with dyspnoea and/or chest pain. [ABSTRACT FROM AUTHOR]
- Published
- 2008
- Full Text
- View/download PDF
23. Increased plasma myostatin in heart failure.
- Author
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Gruson, Damien, Ahn, Sylvie A., Ketelslegers, Jean-Marie, and Rousseau, Michel F.
- Subjects
TRANSFORMING growth factors-beta ,CONGESTIVE heart failure ,CARDIAC hypertrophy ,BIOMARKERS ,HEART cells ,CELL growth ,IMMUNOASSAY ,ATRIAL natriuretic peptides - Abstract
Aims Myostatin (Mstn), a member of the transforming growth factors (TGF)-β family that regulate skeletal muscle growth, has been identified as a regulator of cardiomyocyte growth. The aim of our study was to measure Mstn plasma concentrations in patients with congestive heart failure (CHF) and to evaluate their relationship with other neurohormones released in CHF. Methods and results concentrations of Mstn were measured using a competitive immunoassay, in 76 CHF patients who were receiving optimal treatment and 60 healthy controls. Circulating levels of other neurohormones N-terminal pro-atrial natriuretic peptide (NT-proANP), B-type natriuretic peptide (BNP), N-terminal pro-B-type natriuretic peptide (NT-proBNP), and Big ET-1 were also measured. Plasma Mstn was higher in CHF patients than in controls (63.0 vs. 43.0 ng/mL; P < 0.001). In CHF, Mstn levels correlated positively with NT-proANP (r = 0.25; P = 0.03), BNP (r = 0.33; P < 0.01), NT-proBNP (r = 0.32; P < 0.01), and Big ET-1 (r = 0.26; P = 0.02). No significant correlations were observed with age and creatinine. Conclusion Our results demonstrate that plasma concentrations of Mstn are significantly increased in CHF patients and that Mstn correlates with biomarkers related to HF severity. Our study confirms the activation of Mstn in patients with heart failure. [ABSTRACT FROM AUTHOR]
- Published
- 2011
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- View/download PDF
24. Can viability assessment by DE-MRI predict survival in patients with multivessel disease and low ejection fraction? Influence of treatment strategies.
- Author
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Gerber, Bernhard L., Ahn, Sylvie, de Waroux, Jean-Benoit le Polain, Pouleur, Anne-Catherine, Pasquet, Agnès, Vanoverschelde, Jean-Louis, and Rousseau, Michel
- Subjects
VASCULAR diseases - Abstract
An abstract of the paper "Can Viability Assessment by DE-MRI Predict Survival in Patients With Multivessel Disease and Low Ejection Fraction? Influence of Treatment Strategies," by Bernhard L. Gerber and colleagues is presented.
- Published
- 2011
- Full Text
- View/download PDF
25. Marked Differences in Stroke Prevalence in a Coronary Type 2 Diabetes Population Followed in Cardiac vs. Diabetes Clinics.
- Author
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Hermans, Michel P., Ahn, Sylvie, and Rousseau, Michel
- Subjects
CEREBROVASCULAR disease ,PEOPLE with diabetes ,DIABETES complications ,TYPE 2 diabetes ,CORONARY disease ,SMOKING ,ASPIRIN - Abstract
Coronary artery disease (CAD) is a major cardiovascular (CV) complication in type 2 diabetes (T2DM) populations with metabolic syndrome (MS) phenotype, while T2DM is increasingly recognized as a major co-morbidity in CAD patients. It is not established whether those overlapping populations share a similar macrovascular phenotype. We therefore compared the clinical and biochemical characteristics of patients with both T2DM and CAD followed either in the cardiac or diabetes out/inpatient clinics. From a cohort of 385 patients with T2DM and CAD, we analyzed 314 patients followed in the cardiology clinic (CC) and compared this group to 71 patients followed in the diabetes clinic (DC) from the same university hospital. Data are expressed as means (1SD) or proportions (%). Age, sex, family CV history, blood pressure, smoking exposure and aspirin use were similar in both groups, as were BMI, abdominal circumference and MS (ATP III definition) prevalence. MS severity was lesser in CC, 38% of whom scored at the lowest (3/5) category vs. 18% in DC (p<0.05). The CC group was less often treated with statins/fibrates (44/13 vs. 63/40%), glitazones (2 vs. 10%) and insulin (20 vs. 60%), and more often with beta-blockers (74 vs. 61%) as compared to the DC group (all p<0.05). HbA1c and serum creatinine were higher in DC (8.0 vs. 7.4% and 1.38 vs. 1.12 mg/dL respectively; p<0.05). LDL-C was lower in DC (102 vs. 116 mg/dL), while triglycerides were higher (211 vs. 174 mg/dL; p<0.05). BNP [27 (45) vs. 16 (15)] and Big-ET-1 [9.3 (4.8) vs. 7.7 (2.9)] were higher in CC than in DC (p<0.05). Peripheral artery disease was more prevalent in DC as compared to CC (28 vs. 17%; p<0.05), as a result of a markedly higher stroke prevalence recorded in DC (24 vs. 8% in CC; p<0.001). Our results indicate that patients with both CAD and T2DM followed in the diabetes clinic have a markedly higher stroke prevalence than those followed in the cardiology clinic, despite similar conventional risk factors such as BMI, blood pressure, smoking exposure and family CV history. This unexpected and unreported divergence warrants further investigations regarding established and putative stroke determinants in these seemingly overlapping populations. [ABSTRACT FROM AUTHOR]
- Published
- 2007
26. Association Between Stroke Prevalence and Vasoactive Peptides but not with Adiponectin in Men with Type 2 Diabetes.
- Author
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Hermans, Michel P., Ahn, Sylvie, and Rousseau, Michel
- Subjects
CEREBROVASCULAR disease ,PEPTIDES ,PEOPLE with diabetes ,DIABETES complications ,TYPE 2 diabetes ,CORONARY disease - Abstract
Adiponectin plasma levels are inversely correlated with insulin resistance and central fat, as well as with development of peripheral and coronary artery disease (CAD) and acute vascular complications. Transient ischemic attacks (TIA) and ischemic strokes are frequently observed in type 2 diabetes mellitus but the relationship between TIA, stroke and adiponectin levels are yet poorly documented in this condition. We analyzed 156 type 2 diabetes male patients (>90% white caucasians; age [mean (1SD)]: 64 (11) years) in whom overall TIA/stroke prevalence was 13% (TIA/stroke+; n=21; TIA/stroke-;' n=135). Mean age was 67 (10) in TIA/stroke+ vs. 63 (12) years in TIA/stroke- (NS). Each group was compared with respect to clinico-biochemical phenotype, plasma adiponectin levels, fat mass and vasoactive Nt-pro-atrial and brain natriuretic peptides (Nt-proANP and Nt-proBNP). Data are listed in the Table and expressed as means (1SD) or proportions. Our results clearly demonstrate that TIA/stroke prevalence is associated not only with systolic blood pressure (BP) and homocysteine levels, but also with elevated vasoactive peptides Nt-proANP and Nt-proBNP. On the other hand, the higher fat mass observed in patients with TIA/stroke was associated with paradoxically higher plasma adiponectin, suggesting a lack (or loss) of association between adiponectin, fat mass and stroke prevalence in white caucasian males with type 2 diabetes mellitus. [ABSTRACT FROM AUTHOR]
- Published
- 2007
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