PARTICIPA

PARTICIPA

martes, 30 de junio de 2015

Prevalencia de la retinopatía diabetica en el primer nivel asistencial de Cataluña.mateo segui desde medfam

Ahora que estamos con la retinografia diabética


Prevalencia de la retinopatía diabetica en el primer nivel asistencial de Cataluña.


Según esto, la prevalencia de RD en los 108 723 pacientes (33% de la población) cribados fue del 12,3% (IC 95% 12,1-12,5%), un % bajo si comparamos con otras fuentes. En comparación con los pacientes con DM2 sin RD, aquellos con RD eran más mayores, utilizaban más insulina, eran  más hipertensos (sobre todo con hipertensión arterial sistólica), niveles de HbA1c más elevados, y su filtrado glomerular inferior a  60 ml/min/1,73 m2. La RD se incrementó con la duración de la DM2, un 6,9% en menores de 5 años llegando al 23.7% en los mayores de 15 años.




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¡Por fin entiendo los números de la evidencia! (AMF 2015) No todo es clínica

http://amf-semfyc.com/web/article_ver.php?id=1440

jueves, 25 de junio de 2015

Sesion Inhibidores tirosinquinasa y riesgo cardiovascular

Hoy hemos tenido una sesión sobre tratamiento de la LMC con inhibidores
 tirosinquinasa y riesgo cardiovascular aporto este estudio.

1. Ann Hematol. 2015 Mar;94(3):393-7. doi: 10.1007/s00277-014-2231-9. Epub 2014 Oct 12. Application of systematic coronary risk evaluation chart to identify chronic myeloid leukemia patients at risk of cardiovascular diseases during nilotinib treatment. Breccia M(1), Molica M, Zacheo I, Serrao A, Alimena G. Author information: (1)Department of Cellular Biotechnologies and Hematology, Sapienza University, Via Benevento 6, 00161, Rome, Italy, breccia@bce.uniroma1.it. Nilotinib is currently approved for the treatment of chronic myeloid leukemia (CML) in chronic (CP) and accelerated phase (AP) after failure of imatinib and in newly diagnosed patients. Atherosclerotic events were retrospectively reported in patients with baseline cardiovascular risk factors during nilotinib treatment. We estimated the risk of developing atherosclerotic events in patients treated with second or first-line nilotinib, with a median follow-up of 48 months, by retrospectively applying the SCORE chart proposed by the European Society of Cardiology (ESC) and evaluating risk factors at baseline (diabetes, obesity, smoking, and hypertension). Overall, we enrolled in the study 82 CP patients treated frontline (42 CP patients at the dose of 600 mg BID) or after failure of other tyrosine kinase inhibitors (40 CP patients treated with 400 mg BID). The SCORE chart is based on the stratification of sex (male vs female), age (from 40 to 65 years), smoker vs non-smoker, systolic pressure (from 120 to 180 mm Hg), and cholesterol (measured in mmol/l, from 150 to 300 mg/dl). For statistical purposes, we considered patients subdivided in low, moderate, high (with a score >5), and very high risk. There were 48 males and 34 females, median age 51 years (range 22-84). According to WHO classification, 42 patients were classified as normal weight (BMI <25), 26 patients were overweight (BMI 26 ≤ 30), and 14 were obese (BMI >30). Retrospective classification according to the SCORE chart revealed that 27 patients (33 %) were in the low-risk category, 30 patients (36 %) in the moderate risk category, and 24 patients (29 %) in the high risk. As regards risk factors, we revealed that 17 patients (20.7 %) had a concomitant type II controlled diabetes (without organ damage), 23 patients (28 %) were smokers, 29 patients (35 %) were receiving concomitant drugs for hypertension, and 15 patients (18 %) had concomitant dyslipidemia. Overall, the cumulative incidence of atherosclerotic events at 48 months was 8.5 % (95 % CI, 4.55-14.07): None of the low-risk patients according to the SCORE chart experienced atherosclerotic events compared to 10 % in the moderate risk category and 29 % in the high risk (p = 0.002). Atherosclerotic-free survival was 100, 89, and 69 % in the low, moderate, and high-risk population, respectively (p = 0.001). SCORE chart evaluation at disease baseline could be a valid tool to identify patients at high risk of atherosclerotic events during nilotinib treatment. PMID: 25304102 [PubMed - indexed for MEDLINE]

El Desembarco de La Flota: Manejo del Riesgo Cardiovascular en una consulta de Atención Primaria

http://eldesembarcodelaflota.blogspot.com.es/2015/06/manejo-del-riesgo-cardiovascular-en-una.html?utm_content=buffer73dfe&utm_medium=social&utm_source=twitter.com&utm_campaign=buffer&m=1

domingo, 14 de junio de 2015

JOSE MARIA TALLON DESDE MEDFAM Prevencion estatinica del ictus en mayores



Adjunto el texto completo de la reseña, que me figuro que mucha gente no podrá leer porque pide contraseña.

Personalmente estos cuasi milagros me producen mucho escepticismo. Dar medicación a gente sana no entra en mis parámetros. Como siempre, habría que ver los conflictos de interés, declarados o no, de los autores.

Un saludo.


Primary Prevention With Lipid Lowering Drugs and Long Term Risk of Vascular Events in Older People: Population Based Cohort Study

Annick Alpérovitch; Tobias Kurth; Marion Bertrand; Marie-Laure Ancelin; Catherine Helmer; Stéphanie Debette; Christophe Tzourio

BMJ 

Abstract and Introduction

Abstract

Objective To determine the association between use of lipid lowering drugs (statin or fibrate) in older people with no known history of vascular events and long term risk of coronary heart disease and stroke

Design Ongoing prospective population based cohort study recruited in 1999–2000, with five face-to-face examinations.

Setting Random sample of community dwelling population aged 65 years and over, living in three French cities (Bordeaux, Dijon, Montpellier).

Participants 7484 men and women (63%) with mean age 73.9 years and no known history of vascular events at entry. Mean follow-up was 9.1 years.

Main outcome measures Adjusted hazard ratios of coronary heart disease and stroke in baseline lipid lowering drug users compared with non-users, calculated using multivariable Cox proportional hazard models adjusted for numerous potential confounding factors. Hazard ratios were estimated for use of any lipid lowering drug and for statin and fibrate separately.

Results Lipid lowering drug users were at decreased risk of stroke compared with non-users (hazard ratio 0.66, 95% confidence interval 0.49 to 0.90); hazard ratios for stroke were similar for statin (0.68, 0.45 to1.01) and fibrate (0.66, 0.44 to 0.98). No association was found between lipid lowering drug use and coronary heart disease (hazard ratio 1.12, 0.90 to 1.40). Analyses stratified by age, sex, body mass index, hypertension, systolic blood pressure, triglyceride concentrations, and propensity score did not show any effect modification by these variables, either for stroke or for coronary heart disease.

Conclusion In a population based cohort of older people with no history of vascular events, use of statins or fibrates was associated with a 30% decrease in the incidence of stroke.

Introduction

In high income countries, a growing proportion of vascular events occur in the oldest people. According to the French national mortality statistics for 2010, people aged 85 years and over accounted for 43% of deaths from coronary heart disease and 49% of deaths from stroke. In contrast, participants in most randomised controlled trials testing cardiovascular drugs are predominantly under the age of 70 years.[1] Therefore, the benefit of these drugs in the oldest people remains uncertain. Randomised trials support the use of hydroxymethyl glutaryl coenzyme A reductase inhibitors (statins) for reducing the incidence of major cardiovascular and cerebrovascular events in people with a history of cardiovascular disease, including those aged 65 years and over.[2–5] However, evidence of the benefit of statin treatment for primary prevention is limited, especially in older people. Regarding fibrates, the other main class of lipid lowering drugs, very few trials support their efficacy for the primary prevention of cardiovascular events.[6–9]

New guidelines about cholesterol management based on evidence from randomised controlled trials do not recommend statin treatment in people over 75 years of age without clinical atherosclerotic disease, whereas, in real life, statins are commonly prescribed to older people without clinical evidence of atherosclerosis.[10,11] Avoiding chronic use of unnecessary drugs is important in older people, who often take many drugs and are at high risk of adverse effects. Because of the limited trial based data on the effect of lipid lowering drugs for primary prevention of vascular events in older people, observational studies in this age group can be valuable. We aimed to study the association between use of lipid lowering drugs and the risk of incident cardiovascular events in a cohort study of 7484 community living people aged 65 years or over at entry with a mean follow-up of nine years.

Methods

Study Population

The Three-City study is a prospective study aiming to assess the association between vascular diseases and risk of dementia. The detailed study protocol has been previously described.[12] The Three-City cohort is composed of non-institutionalised people aged 65 years and over, randomly selected from electoral rolls of three cities in France (Bordeaux (south west), Dijon (north east), and Montpellier (south east), who agreed to participate in the study and signed an informed consent form.

Between March 1999 and March 2001, 9294 people were enrolled. A total of 1439 participants were not eligible for the study described here, as they reported a history of coronary heart disease (n=1017), stroke (n=330), or both vascular events (n=92) at baseline. Participants treated with lipid lowering drugs other than statins or fibrates (for example, bile acid sequestrants) (n=113) were also excluded. Among the 7742 remaining participants, 258 (3.3%) were lost to follow-up, leaving a study sample of 7484 participants.

Face-to-face examinations took place every two years during follow-up. Trained nurses and psychologists conducted interviews and made physical and cognitive measurements at the participant's home and at the study centre. Data collection included sociodemographic characteristics (education, occupation, and income), lifestyle (smoking, drinking, and food frequency questionnaire), assessment of disability (Instrumental Activities of Daily Living scale), global cognitive functioning (Mini Mental State examination) and depression (Centre for Epidemiologic Studies-Depression scale), and recording of height and weight.[13–15] Past history of cardiovascular disease included a history of coronary heart disease, stroke, arrhythmia, and peripheral artery disease. Blood pressure was measured twice after five minutes' rest in a seated position with an electronic device (OMRON M6; OMRON Healthcare, Kyoto, Japan). Hypertension was defined as a systolic blood pressure 140 mm Hg or above, a diastolic blood pressure 90 mm Hg or above, or the use of antihypertensive treatment. At baseline, blood was collected after overnight fasting. Lipid concentrations (total cholesterol, high density lipoprotein cholesterol, low density lipoprotein cholesterol, and triglycerides) and glycaemia were measured centrally. Diabetes was defined as use of antidiabetic drugs or a fasting blood glucose of 7 mmol/L or above.

Use of Lipid Lowering and Other Drugs

At each follow-up examination, at the participants' home, interviewers collected information on all drugs used during the preceding month. Participants were asked to show their prescriptions and drug packages. Drug names were coded according to the Anatomic Therapeutic Chemical classification of the World Health Organization.[16] Lipid lowering drugs (code C10A) included hydroxymethyl glutaryl coenzyme A reductase inhibitors (C10AA), fibrates (C10AB), and other drugs such as bile acid sequestrants or nicotinic acid derivatives (not considered in this study). Use of blood pressure lowering or antithrombotic drugs was also registered.

Ascertainment of Vascular Events During Follow-up

At each follow-up visit, participants or informants for deceased participants were systematically questioned about the occurrence of any severe medical event or hospital admission since the last contact. For those reporting a possible coronary heart disease or stroke event, all available clinical information was collected from hospital records, and interviews were conducted with the participant's physician, nursing home staff (for participants admitted to a nursing home during follow-up), or family. Expert panels reviewed all available clinical information and classified each event according to ICD-10 (international classification of diseases, 10th revision). Cardiac events included hospital admission for definite angina, definite myocardial infarction, definite cardiovascular death, coronary balloon dilatation, or coronary artery bypass. Brain imaging data were available for more than 80% of validated stroke cases (computerised tomography 82%; magnetic resonance imaging 15%) and Doppler ultrasound for 62%. When no brain imaging was available, the diagnosis was based on signs and symptoms. Stroke was confirmed if the participant had a new focal neurological deficit of sudden onset attributable to a cerebrovascular event that persisted for more than 24 hours. The panel classified stroke as ischaemic stroke, intracerebral haemorrhage, or of unspecified type.

Statistical Analysis

We described the characteristics of the cohort according to lipid lowering drug use at baseline. We compared users and non-users of lipid lowering drugs by using analysis of variance and χ2 tests adjusted for age, sex, and centre. We also compared users of statins and users of fibrates, and we assessed the associations between vascular events and classic vascular risk factors. We estimated the risk of vascular events related to lipid lowering drug use by using a Cox proportional hazards model with age as the timescale, and we calculated hazard ratios and their 95% confidence intervals with participants not taking any lipid lowering drug as the reference. Modelling included testing of the proportional hazard assumption. We estimated hazard ratios for any major fatal or non-fatal vascular event (coronary heart disease or stroke) and for each type of event separately, using successively use of any lipid lowering drug, statins, and fibrates as independent variables. If a participant had multiple cardiovascular events during follow-up, we considered only the date of the first in estimating the overall risk of vascular event. We first used a simple model adjusted for sex and study centre, with age used as the timescale (model 1). The multivariable model (model 2) was further adjusted for potential confounding factors: diabetes (yes, no), body mass index (<25, 25–29, ≥30), smoking (never, past, current), drinking alcohol (never, past, current), hypertension (yes, no), arrhythmia (yes, no), antithrombotic drugs (yes, no), triglyceride concentration (thirds), and low density lipoprotein to high density lipoprotein cholesterol ratio (thirds).

We did sensitivity analyses stratified by age (< 75, ≥75), sex, triglyceride concentration (<1.6 g/L, ≥1.6 g/L), body mass index (<27, ≥27), hypertension (yes, no), and systolic blood pressure (<145 mm Hg, ≥145 mm Hg) for coronary heart disease and stroke separately. We built a high dimensional propensity score for lipid lowering drug use with a logistic regression model including all the adjustment variables of the primary multivariable model plus other available variables (education, income, systolic blood pressure, diastolic blood pressure, use of antihypertensive drug, self reported diabetes, glycaemia ≥7 mm/L or use of antidiabetic drug, incapacities (Instrumental Activities of Daily Living and Rosow-Breslau functional health scales), cognitive functioning (Mini Mental State score), Center for Epidemiologic Studies-Depression score, APOE genotype). We used this score in different ways. We included it as an adjustment variable in the Cox model. We also calculated hazard ratios within strata defined by thirds of the propensity score distribution. Lastly, we did a matched propensity score analysis. Finally, we estimated hazard ratios in participants who did not report any change in their use of lipid lowering drug (that is, remained a user or non-user) during the first seven years of follow-up.

We did additional analyses to explore complex selection biases. We calculated hazard ratios for death in lipid lowering drug users compared with non-users (all causes of death and deaths from any vascular disease (ICD-10 codes I00-I99)). We estimated hazard ratios for stroke in participants with no previous cardiac event during follow-up, and vice versa. We also estimated the total risk of vascular event (first ever or recurrent) related to lipid lowering drugs during follow-up in the whole Three-City cohort (that is, without excluding participants reporting a history of vascular events at baseline).

We used SAS 9.1 for statistical analyses. We considered a two tailed P value below 0.05 to be statistically significant.

Results

Among the 7484 participants (mean age 73.9 years, 63% women), 2048 (27.4%) reported using lipid lowering drugs (13.5% statins and 13.8% fibrates) at baseline. Among fibrate users, 755 (73%) used fenofibrate; simvastatin (390; 38%) and pravastatin (236; 23%) were the most commonly used statins. Five participants used both categories of lipid lowering drugs. Compared with non-users, users of lipid lowering drugs were younger, were more likely to be women, and had a lower level of education, but they otherwise had a higher vascular risk profile (). Lipid lowering drug users had higher blood pressure levels and body mass index; more often had hypertension, diabetes, and cardiac rhythm disorder; and more often used antihypertensive and antithrombotic drugs. Total cholesterol, low density lipoprotein cholesterol, and triglyceride concentrations were significantly lower in users than in non-users, both for statins and fibrates. Compared with users of statins, participants taking fibrates were older, reported lower alcohol consumption, had lower diastolic blood pressure, and took less antithrombotic treatment (). Total cholesterol and triglyceride concentrations were lower in fibrate users than in statin users.

Table 1.  Baseline characteristics of users and non-users of lipid lowering therapy. Values are percentages (numbers) unless stated otherwise

Characteristic Lipid lowering therapy
No (n=5436) Yes (n=2048) P value* Statins (n=1007) Fibrates (n=1036) P value*
Mean (SD) age, years 74.1 (5.6) 73.4 (4.8) <0.001 73.1 (4.6) 73.7 (4.9) <0.001
Women 62.0 (3368) 67.4 (1380) <0.001 67.8 (683) 67.2 (696) 0.61
Education:            
   Medium or low 61.4 (3336) 66.9 (1371) <0.001 65.3 (658) 68.4 (709) 0.22
   High 38.6 (2094) 33.1 (677) 34.7 (349) 31.6 (327)
Smoking:            
   Never 62.4 (3393) 65.4 (1340) 0.17 65.4 (659) 65.6 (680) 0.99
   Past 31.3 (1700) 29.9 (613) 30.2 (304) 29.5 (306)
   Current 6.3 (341) 4.6 (95) 4.4 (44) 4.8 (50)
Alcohol consumption:            
   Never 17.5 (949) 17.4 (355) 0.008 17.1 (172) 17.7 (183) 0.07
   Past 2.8 (152) 1.7 (34) 1.1 (11) 2.2 (23)
   Current 79.7 (4322) 81.0 (1657) 81.8 (823) 80.1 (829)
Mean (SD) drinks/day 1.70 (1.6) 1.69 (1.6) 0.10 1.77 (1.7) 1.61 (1.6) 0.017
Depressive symptomatology† 12.8 (687/5367) 12.8 (261/2047) 0.58 12.3 (123/1000) 13.2 (136/1030) 0.51
No disability 91.0 (4906/5391) 94.3 (1921/2037) <0.001 95 (950/1000) 93.6 (966/1032) 0.24
Mean (SD) systolic blood pressure, mm Hg 146.2 (21.9) 147.6 (20.9) <0.001 147.6 (20.8) 147.6 (21.1) 0.24
Mean (SD) diastolic blood pressure, mm Hg 82.6 (11.3) 82.5 (10.9) 0.54 83.0 (10.9) 82.1 (10.8) 0.016
Antihypertensive treatment 41.8 (2270/5430) 54.1 (1107/2046) <0.001 54.7 (551) 53.3 (552) 0.37
Hypertension‡ 74.5 (4044/5428) 79.7 (1633/2048) <0.001 79.7 (803) 79.6 (825) 0.51
Cardiac rhythm disorder 13.1 (696/5313) 14.6 (291/1993) 0.032 15.6 (153/981) 13.7 (138) 0.13
Antithrombotic treatment 13.1 (659/5030) 18.5 (379/2048) <0.001 21.6 (217/1005) 15.5 (160/1032) <0.001
Diabetes§ 7.2 (371/5153) 11.9 (233/1958) <0.001 10.9 (105/963) 12.8 (126/984) 0.13
Mean (SD) body mass index, kg/m2 25.4 (4.0) 25.9 (4.0) <0.001 25.8 (4.0) 26.0 (4.1) 0.18
Total cholesterol, mmol/L:            
   Mean (SD) 5.97 (1.0) 5.60 (0.9) <0.001 5.68 (0.9) 5.52 (0.8) <0.001
   <5.37 26.9 (1381) 42.1 (818) <0.001 37.8 (364) 46.2 (452) <0.001
   5.37–6.18 33.8 (1736) 34.8 (677) 36.5 (351) 33.2 (325)
   ≥6.19 39.2 (2013) 23.1 (450) 25.7 (247) 20.6 (201)
High density lipoprotein cholesterol, mmol/L:            
   Mean (SD) 1.63 (0.4) 1.64 (0.4) 0.16 1.64 (0.4) 1.63 (0.4) 0.56
   <1.41 30.1 (1544) 29.8 (579) 0.04 31.1 (299) 28.3 (277) 0.86
   1.41–1.75 34.5 (1770) 35.7 (694) 33.4 (321) 38.0 (372)
   ≥1.76 35.4 (1814) 34.6 (672) 35.6 (342) 33.6 (329)
Low density lipoprotein cholesterol, mmol/L:            
   Mean (SD) 3.78 (0.9) 3.40 (0.8) <0.001 3.40 (0.9) 3.40 (0.7) 0.99
   <3.24 26.1 (1336) 45.4 (880) <0.001 46.3 (444) 44.6 (435) 0.97
   3.24–3.93 33.7 (1726) 32.1 (623) 30.6 (294) 33.5 (327)
   ≥3.94 40.1 (2053) 22.5 (436) 23.1 (222) 21.8 (213)
Triglycerides, mmol/L:            
   Geometric mean (95% CI) 1.14 (0.76 to 1.70) 1.10 (0.70 to 1.74) 0.021 1.27 (0.84–1.93) 0.96 (0.62–1.49) <0.001
   <0.94 32.1 (1646) 38.3 (745) 0.008 23.9 (230) 52.6 (514) <0.001
   0.94–1.33 35.8 (1835) 30.2 (587) 34.0 (327) 26.5 (259)
   ≥1.34 32.1 (1646) 31.5 (613) 42.1 (405) 21.0 (205)

*Pearson χ2 test and analysis of variance for comparison of categorical and continuous characteristics respectively, adjusted for sex, age, and centre. †Women scoring ≥23 and men scoring ≥17 on Centre for Epidemiologic Studies-Depression scale.
‡Blood pressure ≥140/90 mm Hg or antihypertensive treatment.
§Antidiabetic treatment or glycaemia ≥7 mmol/L.

Table 1.  Baseline characteristics of users and non-users of lipid lowering therapy. Values are percentages (numbers) unless stated otherwise

Characteristic Lipid lowering therapy
No (n=5436) Yes (n=2048) P value* Statins (n=1007) Fibrates (n=1036) P value*
Mean (SD) age, years 74.1 (5.6) 73.4 (4.8) <0.001 73.1 (4.6) 73.7 (4.9) <0.001
Women 62.0 (3368) 67.4 (1380) <0.001 67.8 (683) 67.2 (696) 0.61
Education:            
   Medium or low 61.4 (3336) 66.9 (1371) <0.001 65.3 (658) 68.4 (709) 0.22
   High 38.6 (2094) 33.1 (677) 34.7 (349) 31.6 (327)
Smoking:            
   Never 62.4 (3393) 65.4 (1340) 0.17 65.4 (659) 65.6 (680) 0.99
   Past 31.3 (1700) 29.9 (613) 30.2 (304) 29.5 (306)
   Current 6.3 (341) 4.6 (95) 4.4 (44) 4.8 (50)
Alcohol consumption:            
   Never 17.5 (949) 17.4 (355) 0.008 17.1 (172) 17.7 (183) 0.07
   Past 2.8 (152) 1.7 (34) 1.1 (11) 2.2 (23)
   Current 79.7 (4322) 81.0 (1657) 81.8 (823) 80.1 (829)
Mean (SD) drinks/day 1.70 (1.6) 1.69 (1.6) 0.10 1.77 (1.7) 1.61 (1.6) 0.017
Depressive symptomatology† 12.8 (687/5367) 12.8 (261/2047) 0.58 12.3 (123/1000) 13.2 (136/1030) 0.51
No disability 91.0 (4906/5391) 94.3 (1921/2037) <0.001 95 (950/1000) 93.6 (966/1032) 0.24
Mean (SD) systolic blood pressure, mm Hg 146.2 (21.9) 147.6 (20.9) <0.001 147.6 (20.8) 147.6 (21.1) 0.24
Mean (SD) diastolic blood pressure, mm Hg 82.6 (11.3) 82.5 (10.9) 0.54 83.0 (10.9) 82.1 (10.8) 0.016
Antihypertensive treatment 41.8 (2270/5430) 54.1 (1107/2046) <0.001 54.7 (551) 53.3 (552) 0.37
Hypertension‡ 74.5 (4044/5428) 79.7 (1633/2048) <0.001 79.7 (803) 79.6 (825) 0.51
Cardiac rhythm disorder 13.1 (696/5313) 14.6 (291/1993) 0.032 15.6 (153/981) 13.7 (138) 0.13
Antithrombotic treatment 13.1 (659/5030) 18.5 (379/2048) <0.001 21.6 (217/1005) 15.5 (160/1032) <0.001
Diabetes§ 7.2 (371/5153) 11.9 (233/1958) <0.001 10.9 (105/963) 12.8 (126/984) 0.13
Mean (SD) body mass index, kg/m2 25.4 (4.0) 25.9 (4.0) <0.001 25.8 (4.0) 26.0 (4.1) 0.18
Total cholesterol, mmol/L:            
   Mean (SD) 5.97 (1.0) 5.60 (0.9) <0.001 5.68 (0.9) 5.52 (0.8) <0.001
   <5.37 26.9 (1381) 42.1 (818) <0.001 37.8 (364) 46.2 (452) <0.001
   5.37–6.18 33.8 (1736) 34.8 (677) 36.5 (351) 33.2 (325)
   ≥6.19 39.2 (2013) 23.1 (450) 25.7 (247) 20.6 (201)
High density lipoprotein cholesterol, mmol/L:            
   Mean (SD) 1.63 (0.4) 1.64 (0.4) 0.16 1.64 (0.4) 1.63 (0.4) 0.56
   <1.41 30.1 (1544) 29.8 (579) 0.04 31.1 (299) 28.3 (277) 0.86
   1.41–1.75 34.5 (1770) 35.7 (694) 33.4 (321) 38.0 (372)
   ≥1.76 35.4 (1814) 34.6 (672) 35.6 (342) 33.6 (329)
Low density lipoprotein cholesterol, mmol/L:            
   Mean (SD) 3.78 (0.9) 3.40 (0.8) <0.001 3.40 (0.9) 3.40 (0.7) 0.99
   <3.24 26.1 (1336) 45.4 (880) <0.001 46.3 (444) 44.6 (435) 0.97
   3.24–3.93 33.7 (1726) 32.1 (623) 30.6 (294) 33.5 (327)
   ≥3.94 40.1 (2053) 22.5 (436) 23.1 (222) 21.8 (213)
Triglycerides, mmol/L:            
   Geometric mean (95% CI) 1.14 (0.76 to 1.70) 1.10 (0.70 to 1.74) 0.021 1.27 (0.84–1.93) 0.96 (0.62–1.49) <0.001
   <0.94 32.1 (1646) 38.3 (745) 0.008 23.9 (230) 52.6 (514) <0.001
   0.94–1.33 35.8 (1835) 30.2 (587) 34.0 (327) 26.5 (259)
   ≥1.34 32.1 (1646) 31.5 (613) 42.1 (405) 21.0 (205)

*Pearson χ2 test and analysis of variance for comparison of categorical and continuous characteristics respectively, adjusted for sex, age, and centre. †Women scoring ≥23 and men scoring ≥17 on Centre for Epidemiologic Studies-Depression scale.
‡Blood pressure ≥140/90 mm Hg or antihypertensive treatment.
§Antidiabetic treatment or glycaemia ≥7 mmol/L.

During a mean follow-up of 9.1 years, 732 first ever non-fatal (n=527) or fatal (n=205) cardiovascular events were diagnosed: 440 coronary events (for a total follow-up of 60 869 person years) and 292 strokes (for a total follow-up of 61 727 person years). Crude incidence rates per 100 person years were 0.72 for coronary events and 0.47 for stroke. Among stroke cases, 227 were ischaemic, 57 haemorrhagic, and eight undefined. Increased risk of stroke or coronary heart disease was associated with classic risk factors: older age, male sex, high blood pressure, diabetes, and high body mass index. Use of antihypertensive or antithrombotic drugs was associated with occurrence of coronary heart disease or stroke. For antihypertensive drugs, hazard ratios were 1.50 (95% confidence interval 1.24 to 1.82) for coronary heart disease and 1.45 (1.14 to 1.83) for stroke. The risk of coronary heart disease was increased in participants with higher total cholesterol, low density lipoprotein cholesterol, or triglycerides and lower high density lipoprotein cholesterol. We found no association between baseline blood lipid concentrations and the risk of stroke. In particular, the risk of stroke (total or ischaemic) was not increased in participants with elevated triglyceride concentrations.

We found no association between total incidence of vascular events and lipid lowering drug use, either for use of any drug (multivariate model: hazard ratio 0.91, 0.76 to 1.09) or for statins and fibrates examined separately (). However, we observed a very contrasting pattern of association according to the type of event. The risk of coronary heart disease was not lower in lipid lowering drug users (hazard ratio 1.12, 0.90 to 1.40) (). In contrast, we observed a one third decrease in the risk of stroke in lipid lowering drug users (hazard ratio 0.66, 0.49 to 0.90) compared with non-users; reduction in stroke risk was similar for the statin and fibrate groups (). Hazard ratios for ischaemic and haemorrhagic stroke in lipid lowering drug users were 0.63 (0.45 to 0.84) and 0.72 (0.37 to 1.42). All cause mortality was lower in lipid lowering drug users compared with non-users (hazard ratio 0.87, 0.77 to 0.99), but mortality from cardiovascular diseases was not significantly decreased (hazard ratio 0.92, 0.67 to1.25).

Table 2.  Association between risk of vascular events and lipid lowering drug therapy

Baseline lipid lowering drug use No of events Adjusted hazard ratios (95% CI) for vascular events*
Model 1 Model 2
Coronary heart disease or stroke
No lipid lowering drug 545 Reference Reference
Statins or fibrates 187 0.98 (0.83 to 1.16) 0.91 (0.76 to 1.09)
Statins 92 1.01 (0.81 to 1.26) 0.88 (0.69 to 1.13)
Fibrates 95 0.96 (0.77 to 1.19) 0.95 (0.75 to 1.20)
Stroke
No lipid lowering drug 234 Reference Reference
Statins or fibrates 58 0.71 (0.53 to 0.95) 0.66 (0.49 to 0.90)
Statins 29 0.74 (0.51 to 1.08) 0.68 (0.45 to 1.01)
Fibrates 29 0.70 (0.48 to 1.01) 0.66 (0.44 to 0.98)
Coronary heart disease†
No lipid lowering drug 311 Reference Reference
Statins or fibrates 129 1.18 (0.96 to 1.45) 1.12 (0.90 to 1.40)
Statins 63 1.19 (0.91 to 1.56) 1.13 (0.84 to 1.52)
Fibrates 63 1.17 (0.90 to 1.53) 1.12 (0.84 to 1.49)

*Hazard ratios estimated using Cox proportional hazard models with age as timescale. Model 1 was adjusted for sex and centre. Model 2 (multivariable model) was adjusted as for model 1 plus diabetes, body mass index, alcohol consumption, smoking, hypertension, cardiac rhythm disorder, antithrombotic therapy, triglycerides, and low density lipoprotein/high density lipoprotein ratio.
†Included hospital admission with definite angina, definite myocardial infarction, definite coronary heart disease death, coronary balloon dilatation, and coronary artery bypass.

Table 2.  Association between risk of vascular events and lipid lowering drug therapy

Baseline lipid lowering drug use No of events Adjusted hazard ratios (95% CI) for vascular events*
Model 1 Model 2
Coronary heart disease or stroke
No lipid lowering drug 545 Reference Reference
Statins or fibrates 187 0.98 (0.83 to 1.16) 0.91 (0.76 to 1.09)
Statins 92 1.01 (0.81 to 1.26) 0.88 (0.69 to 1.13)
Fibrates 95 0.96 (0.77 to 1.19) 0.95 (0.75 to 1.20)
Stroke
No lipid lowering drug 234 Reference Reference
Statins or fibrates 58 0.71 (0.53 to 0.95) 0.66 (0.49 to 0.90)
Statins 29 0.74 (0.51 to 1.08) 0.68 (0.45 to 1.01)
Fibrates 29 0.70 (0.48 to 1.01) 0.66 (0.44 to 0.98)
Coronary heart disease†
No lipid lowering drug 311 Reference Reference
Statins or fibrates 129 1.18 (0.96 to 1.45) 1.12 (0.90 to 1.40)
Statins 63 1.19 (0.91 to 1.56) 1.13 (0.84 to 1.52)
Fibrates 63 1.17 (0.90 to 1.53) 1.12 (0.84 to 1.49)

*Hazard ratios estimated using Cox proportional hazard models with age as timescale. Model 1 was adjusted for sex and centre. Model 2 (multivariable model) was adjusted as for model 1 plus diabetes, body mass index, alcohol consumption, smoking, hypertension, cardiac rhythm disorder, antithrombotic therapy, triglycerides, and low density lipoprotein/high density lipoprotein ratio.
†Included hospital admission with definite angina, definite myocardial infarction, definite coronary heart disease death, coronary balloon dilatation, and coronary artery bypass.

Table 2.  Association between risk of vascular events and lipid lowering drug therapy

Baseline lipid lowering drug use No of events Adjusted hazard ratios (95% CI) for vascular events*
Model 1 Model 2
Coronary heart disease or stroke
No lipid lowering drug 545 Reference Reference
Statins or fibrates 187 0.98 (0.83 to 1.16) 0.91 (0.76 to 1.09)
Statins 92 1.01 (0.81 to 1.26) 0.88 (0.69 to 1.13)
Fibrates 95 0.96 (0.77 to 1.19) 0.95 (0.75 to 1.20)
Stroke
No lipid lowering drug 234 Reference Reference
Statins or fibrates 58 0.71 (0.53 to 0.95) 0.66 (0.49 to 0.90)
Statins 29 0.74 (0.51 to 1.08) 0.68 (0.45 to 1.01)
Fibrates 29 0.70 (0.48 to 1.01) 0.66 (0.44 to 0.98)
Coronary heart disease†
No lipid lowering drug 311 Reference Reference
Statins or fibrates 129 1.18 (0.96 to 1.45) 1.12 (0.90 to 1.40)
Statins 63 1.19 (0.91 to 1.56) 1.13 (0.84 to 1.52)
Fibrates 63 1.17 (0.90 to 1.53) 1.12 (0.84 to 1.49)

*Hazard ratios estimated using Cox proportional hazard models with age as timescale. Model 1 was adjusted for sex and centre. Model 2 (multivariable model) was adjusted as for model 1 plus diabetes, body mass index, alcohol consumption, smoking, hypertension, cardiac rhythm disorder, antithrombotic therapy, triglycerides, and low density lipoprotein/high density lipoprotein ratio.
†Included hospital admission with definite angina, definite myocardial infarction, definite coronary heart disease death, coronary balloon dilatation, and coronary artery bypass.

Among participants who did not report any change in their use of lipid lowering drugs during the first seven years of follow-up (that is, regular users versus never users), the hazard ratio for stroke in users (any lipid lowering drug) was 0.56 (0.37 to 0.85). This analysis did not show significant association between risk of coronary heart disease and use of lipid lowering drugs (hazard ratio 1.22, 0.89 to 1.66).

Analyses stratified by age, sex, body mass index, hypertension, systolic blood pressure, and triglyceride concentrations did not show any effect modification by any of these variables ( and ). Adjustment for the propensity score did not modify hazard ratio estimates for lipid lowering drug use (1.09 (0.87 to 1.36) for coronary event and 0.65 (0.48 to 0.88) for stroke). Analysis stratified by thirds of the propensity score showed that the hazard ratios for stroke were similar in the three strata (). Lastly, risk estimates remained unchanged when treated and untreated participants were matched on propensity score ().

Supplementary Table A.  Adjusted hazard ratios of coronary heart disease event in lipid-lowering drug users by different population strata

Strata Number (%) of events Adjusted hazard ratio (95% confidence interval)
Lipid-lowering drug use No use
Age < 75 years 66 (5.2%) 163 (5.3%) 0.92 (0.68 to 1.26)
Age ≥ 75 years 63 (8.1) 148 (6.4) 1.33 (0.96 to 1.85)
Men 66 (9.9) 176 (8.5) 0.99 (0.73 to 1.35)
Women 63 (4.6) 135 (4.0) 1.24 (0.89 to 1.73)
Triglycerides < 1.6 mmol/l 78 (5.1) 218 (5.3) 1.03 (0.79 to 1.35)
Triglycerides ≥ 1.6 mmol/l 40 (9.8) 69 (7.1) 1.20 (0.79 to 1.82)
Body mass index < 27 kg/m2 78 (5.9) 217 (5.8) 1.14 (0.87 to 1.51)
Body mass index ≥ 27kg/m2 49 (6.8) 89 (5.6) 1.02 (0.69 to 1.51)
Systolic pressure < 145 mmHg 48 (5.1) 120 (4.4) 1.31 (0.91 to 1.88)
Systolic pressure ≥ 145 mmHg 79 (7.2) 190 (7.0) 0.97 (0.73 to 1.29)
No hypertension 19 (4.6) 45 (3.3) 1.82 (1.01 to 3.29)
Hypertension 110 (6.7) 266 (6.6) 1.01 (0.79 to 1.29)
Propensity score      
   Lowest third 33 (6.0) 150 (6.1) 1.06 (0.72 to 1.57)
   Middle third 37 (4.7) 98 (4.7) 0.97 (0.66 to 1.41)
   Highest third 94 (9.1) 119 (8.2) 1.04 (0.79 to 1.37)

Note
Adjusted hazard ratios were estimated using multivariate Cox proportional hazard model with age as the time scale. Subjects scoring in the first third of the propensity score distribution have the lowest probabilities of being treated with lipid – lowering drug.

Supplementary Table B.  Adjusted hazard ratios of stroke event in lipid-lowering drug users by different population strata

Strata Number (%) of events Adjusted hazard ratio (95% confidence interval)
Lipid-lowering drug use No use
Age < 75 years 21 (1.7) 93 (3.0) 0.47 (0.28 to 0.76)
Age ≥ 75 years 37 (4.8) 141 (6.1) 0.79 (0.54 to 1.16)
Men 21 (3.2) 106 (5.2) 0.58 (0.36 to 0.95)
Women 37 (2.7) 128 (3.8) 0.66 (0.45 to 0.98)
Triglycerides < 1.6 mmol/l 45 (2.9) 169 (4.1) 0.72 (0.51 to 1.02)
Triglycerides ≥ 1.6 mmol/l 7 (1.7) 46 (4.8) 0.33 (0.15 to 0.75)
Body mass index < 27 kg/m2 37 (2.8) 152 (4.0) 0.69 (0.47 to 1.02)
Body mass index ≥ 27kg/m2 21 (2.9) 80 (5.0) 0.58 (0.35 to 0.95)
Systolic pressure < 145 mmHg 24 (2.5) 88 (3.2) 0.78 (0.48 to 1.27)
Systolic pressure ≥ 145 mmHg 34 (3.1) 146 (5.4) 0.56 (0.38 to 0.83)
No hypertension 7 (1.7) 40 (2.9) 0.69 (0.30 to 1.57)
Hypertension 51 (3.1) 194 (4.8) 0.64 (0.46 to 0.89)
Propensity score      
   Lowest third 9 (2.3) 99 (4.7) 0.56 (0.28 to 1.12)
   Middle third 14 (2.1) 62 (3.4) 0.60 (0.34 to 1.08)
   Highest third 35 (3.5) 73 (4.9) 0.71 (0.46 to 1.08)

Note
Adjusted hazard ratios were estimated using multivariate Cox proportional hazard model with age as the time scale. Subjects scoring in the first third of the propensity score distribution have the lowest probabilities of being treated with lipid – lowering drug.

Supplementary Table B.  Adjusted hazard ratios of stroke event in lipid-lowering drug users by different population strata

Strata Number (%) of events Adjusted hazard ratio (95% confidence interval)
Lipid-lowering drug use No use
Age < 75 years 21 (1.7) 93 (3.0) 0.47 (0.28 to 0.76)
Age ≥ 75 years 37 (4.8) 141 (6.1) 0.79 (0.54 to 1.16)
Men 21 (3.2) 106 (5.2) 0.58 (0.36 to 0.95)
Women 37 (2.7) 128 (3.8) 0.66 (0.45 to 0.98)
Triglycerides < 1.6 mmol/l 45 (2.9) 169 (4.1) 0.72 (0.51 to 1.02)
Triglycerides ≥ 1.6 mmol/l 7 (1.7) 46 (4.8) 0.33 (0.15 to 0.75)
Body mass index < 27 kg/m2 37 (2.8) 152 (4.0) 0.69 (0.47 to 1.02)
Body mass index ≥ 27kg/m2 21 (2.9) 80 (5.0) 0.58 (0.35 to 0.95)
Systolic pressure < 145 mmHg 24 (2.5) 88 (3.2) 0.78 (0.48 to 1.27)
Systolic pressure ≥ 145 mmHg 34 (3.1) 146 (5.4) 0.56 (0.38 to 0.83)
No hypertension 7 (1.7) 40 (2.9) 0.69 (0.30 to 1.57)
Hypertension 51 (3.1) 194 (4.8) 0.64 (0.46 to 0.89)
Propensity score      
   Lowest third 9 (2.3) 99 (4.7) 0.56 (0.28 to 1.12)
   Middle third 14 (2.1) 62 (3.4) 0.60 (0.34 to 1.08)
   Highest third 35 (3.5) 73 (4.9) 0.71 (0.46 to 1.08)

Note
Adjusted hazard ratios were estimated using multivariate Cox proportional hazard model with age as the time scale. Subjects scoring in the first third of the propensity score distribution have the lowest probabilities of being treated with lipid – lowering drug.

Supplementary Table C.  Matched propensity score analysis: risk of vascular events in lipid-lowering drug users compared to non users

Baseline lipid-lowering drug (LLD) use Number of events Hazard ratios (95% confidence interval) for vascular events
Coronary heart disease or stroke
No lipid-lowering drug 206 Reference
Statins or fibrates 185 0.95 [0.75–1.22]
Stroke
No lipid-lowering drug 89 Reference
Statins or fibrates 57 0.68 [0.44–1.05]
Coronary heart disease
No lipid-lowering drug 117 Reference
Statins or fibrates 128 1.17 [0.86–1.58]

Note
Each participant treated with lipid-lowering drug was matched on propensity score with an untreated participant (2,026 individuals in each treatment group). Due to reduced sample size, hazard ratio confidence intervals are larger than those estimated in the whole study population (n=7,484).

Secondary analyses including participants with a history of a vascular event before entering in the Three-City study also showed a lower risk of total (first ever or recurrent) incident strokes in lipid lowering drug users (statins: hazard ratio 0.70 (0.51 to 0.96); fibrates: 0.66 (0.46 to 0.94)). In the same group, hazard ratios for coronary heart disease were 1.45 (1.17 to 1.79) for statins and 1.17 (0.92 to 1.49) for fibrates. The hazard ratio for stroke did not change when participants with a previous cardiac event during follow-up were excluded from the analysis (hazard ratio of stroke in lipid lowering drug users 0.56 (0.41 to 0.77).

Discussion

In a community dwelling population of older people with no known history of vascular events, we found that use of lipid lowering drugs at baseline was associated with a decreased risk of stroke during a mean follow-up of nine years, whereas no protective effect was found for coronary heart disease. This pattern was similar for statin and fibrate use.

Comparison With Previous Studies

Previous observational studies have shown that a person's lipid profile is a major risk modifying factor for coronary heart disease, whereas the association between lipid concentrations and stroke is weaker.[17] Several studies have, however, reported an association between elevated lipid concentrations, particularly triglycerides, and an increased incidence of ischaemic stroke.[18,19] For intracerebral haemorrhage, an association with low lipid concentrations (both low density lipoprotein cholesterol and triglycerides) has been described.[20–22] Data from the Cardiovascular Health Study have suggested that among people for whom lipid lowering treatment was recommended, those using a statin had a fourfold lower risk of silent cerebral infarcts compared with non-users.[23] However, no observational study has ever described a significant association between use of lipid lowering drugs and decreased risk of stroke.

Clinical trials in different populations of patients have extensively evaluated the effects of statins on the incidence of major cardiovascular events. Meta-analyses consistently showed that, compared with placebo, statin treatment reduced the incidence of cardiovascular events by about 20%; the risk reduction was higher for coronary events than for ischaemic stroke.[5] Overall, statin treatment had no significant effect on the incidence of haemorrhagic stroke in individual trials, except in a study in which a high dose of atorvastatin was associated with an increased risk of cerebral haemorrhage in patients with a past history of stroke or transient ischaemic attack.[24] Randomised controlled trials have shown that use of fibrates for secondary prevention of cardiovascular events produced an average 10% reduction in the incidence of total events, but no consistent effect on the risk of stroke was found.[10] Some primary prevention trials were conducted in patients at high risk, especially in those with type 2 diabetes.[7,25] In the ACCORD (Action to Control Cardiovascular Risk in Diabetes) study, simvastatin monotherapy was compared with a combination of simvastatin plus fenofibrate in patients with type 2 diabetes. The combination of statin and fibrate did not reduce the risk of vascular events, compared with simvastatin alone.[26] In a large meta-analysis focusing on the relation of incident stroke to lipid lowering drug (statins or fibrates) and non-drug (such as diet) interventions, statin treatment was the only intervention that decreased the risk of total stroke.[27] A recent meta-analysis of individual data from 27 randomised trials concluded that lowering low density lipoprotein cholesterol with statins resulted in a significant reduction in coronary heart disease and stroke. Interestingly, the effect of lowering low density lipoprotein cholesterol was similar in participants with the lowest risk of vascular events and in the highest risk groups.[28] In these meta-analyses, as in most trials, the mean age of participants was around 60–65 years. PROSPER (Prospective Study of Pravastatin in the Elderly at Risk) was the only trial that focused specifically on people aged 70 to 82 years with a history of risk factors for cardiovascular disease. This trial showed that pravastatin reduced the incidence of major coronary events but not of ischaemic stroke.[29]

Meaning of Results and Potential for Bias

Our results are at variance with those of randomised controlled trials, as we found that only the risk of stroke was decreased in users of lipid lowering drugs, whereas no decrease was observed for risk of coronary heart disease. Could our results be explained by biases? Confounding by indication is a major bias in observational epidemiological studies of drug effects. In real world conditions, the indication for treatment is related to the risk profile of the patient. In this study, such a bias was observed for use of antihypertensive and antithrombotic drugs, as both were associated with an increased risk of stroke. Users of lipid lowering drugs were at higher vascular risk than non-users, and an indication bias would have resulted in an increased risk of stroke, as we observed for other drugs prescribed for reducing the vascular risk (antihypertensive and antithrombotic). Furthermore, use of propensity scores to better take into account all the characteristics associated with use of lipid lowering drugs, including antihypertensive and antithrombotic drug intake, did not modify the estimated association of lipid lowering drug use with the vascular risk. As use of lipid lowering drugs was associated with a 13% decrease in all cause mortality, a mortality bias cannot be excluded, but it is unlikely that it could completely explain our results. Stroke and coronary heart disease share most vascular factors, including intake of vascular drugs, and it is therefore implausible that confounding by indication, mortality bias, or any other systematic bias would have resulted in an isolated lowering of the risk of stroke. We also explored the possibility that excluding participants with a history of vascular events at baseline could result in an over-estimation of risk reduction. Participants with a past history of vascular events were at higher risk of an incident v