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Logo of nihpaAbout Author manuscriptsSubmit a manuscriptHHS Public Access; Author Manuscript; Accepted for publication in peer reviewed journal;
N Engl J Med. Author manuscript; available in PMC 2010 April 30.
Published in final edited form as:
PMCID: PMC2710995

A Randomized Trial of Rosuvastatin in the Prevention of Venous Thromboembolism: the JUPITER Trial



Controversies persist on whether arterial and venous thrombosis share common pathways and whether treatments of known efficacy for one disease process have consistent benefits for the other. Observational studies have yielded variable estimates of the effect of statin therapy on risk of venous thromboembolism, and randomized evidence is lacking.


Symptomatic venous thromboembolism was a pre-specified endpoint of Justification for the Use of Statins in Prevention: an Intervention Trial Evaluating Rosuvastatin (JUPITER). We randomly assigned 17,802 apparently healthy men and women with low-density lipoprotein (LDL) cholesterol levels of less than 130 mg/dL and high-sensitivity C-reactive protein levels of 2.0 mg/L or higher to rosuvastatin, 20 mg/d, or placebo. Intention-to-treat analyses followed participants for the first occurrence of pulmonary embolism or deep vein thrombosis.


During a median follow-up of 1.9 years (maximum 5.0), symptomatic venous thromboembolism occurred in 94 participants, 34 in the rosuvastatin group and 60 in the placebo group. The rates of venous thromboembolism were 0.18 and 0.32 per 100 person-years of follow-up in the rosuvastatin and placebo groups, respectively (hazard ratio for rosuvastatin 0.57; 95% confidence interval [CI], 0.37 to 0.86; P=0.007), with corresponding rates of 0.10 and 0.17 for unprovoked venous thromboembolism (hazard ratio 0.61; 95% CI, 0.35 to 1.09; P=0.089) and 0.08 and 0.16 for provoked venous thromboembolism (hazard ratio 0.52; 95% CI, 0.28 to 0.96; P=0.033). Corresponding rates of pulmonary embolism were 0.09 and 0.12 (hazard ratio 0.77; 95% CI, 0.41 to 1.45; P=0.42), whereas rates of deep vein thrombosis only were 0.09 and 0.20 (hazard ratio 0.45; 95% CI, 0.25 to 0.79; P=0.004). Consistent effects were observed in all subgroups examined. No differences were seen between treatment groups in rates of bleeding.


In this trial of apparently healthy persons, rosuvastatin significantly reduced the occurrence of symptomatic venous thromboembolism. ( number, NCT00239681.)

Venous and arterial thrombosis are strongly age-related, common, and serious events, that often co-occur1, 2, and share some risk factors3-7. Controversies persist on the extent of their shared pathways and whether treatments of demonstrated efficacy for one condition, including anticoagulants, antiplatelet therapy, thrombolytics and statins, have consistent benefits for the primary or secondary prevention of the other8-10.

Benefits of statins might accrue not only through their effects on lipid levels, but also through their influence on thrombosis and inflammation11-13. Two prospective, observational studies found substantial and significant reductions in the risk of venous thromboembolism associated with statin use, including a 50% reduced hazard among statin users in the Heart and Estrogen/progestin Replacement Study14, and a 22% reduction among statin users in Ontario, based on administrative claims data15. Four case-control studies also found reductions in the risk of venous thrombosis, ranging from a 26% to a 58% decreased risk associated with statin use16-19. However, two additional observational studies, based on computerized databases in the United Kingdom, found no association between statin use and risk of venous thrombosis20, 21. Further, reliable estimation of the potential pleiotropic effects of statins in observational studies is problematic in light of the substantial challenges arising from confounding by indication and healthy user effects22; and the need for randomized evidence has been noted23.

Justification for the Use of Statins in Prevention: an Intervention Trial Evaluating Rosuvatatin (JUPITER) tested whether treatment with rosuvastatin, 20 mg daily, as compared with placebo, would decrease the rate of first major cardiovascular events. The occurrence of venous thromboembolism was a protocol-specified secondary end point of the trial.


Trial design

JUPITER was a randomized, double-blind, placebo-controlled, multicenter trial conducted at 1315 sites in 26 countries. Details of its design and findings for the primary end point are presented elsewhere24, 25. The trial protocol was designed and written by the study chair and approved by the local institutional review board at each participating center. The trial data were analyzed by the academic authors who vouch for their accuracy and completeness.

The trial was financially supported by Astra-Zeneca. The sponsor collected the trial data and monitored the study sites but played no role in the conduct of the analyses or drafting of the manuscript.

Study population

As described in detail elsewhere24, 25, the main eligibility criteria were age 50 years or older in men and 60 years or older in women, with no history of cardiovascular disease, and, at the initial screening visit, an LDL cholesterol level of less than 130 mg per deciliter (3.4 mmol per liter) and a high-sensitivity C-reactive protein level of 2.0 mg per liter or more. Exclusion criteria related to characteristics with known or possible relationships with venous thrombosis included use of lipid-lowering therapy within 6 weeks before screening, current use of post-menopausal hormone-replacement therapy, cancer within 5 years before enrollment (with the exception of basal-cell or squamous cell carcinoma of the skin), diabetes, and uncontrolled hypertension. Other requirements included a willingness to participate for the duration of the trial, provision of written informed consent, and a triglyceride level of less than 500 mg per deciliter (5.6 mmol per liter).

Randomization and follow-up

Potentially eligible subjects who remained willing and demonstrated good compliance during a 4-week, placebo run-in phase were randomly assigned in a 1:1 ratio to receive either rosuvastatin, 20 mg daily, or matching placebo. Between March 14, 2003 and December 15, 2006, the trial randomized 17,802 individuals.

Follow-up visits were scheduled to occur at 13 weeks and then 6, 12, 18, 24, 30, 36, 42, 48, 54, and 60 months after randomization. A closeout visit occurred after study termination, at which time participants were unblinded. Interviews at each follow-up visit assessed outcomes including clinically symptomatic deep vein thrombosis and pulmonary embolism. These visits also assessed initiation of concomitant medications and their indications, with a protocol-specified focus on anticoagulants because statins can potentiate the anticoagulant effect of coumadin. Personnel at each site also contacted their participants mid-way between scheduled visits to identify health changes and address any concerns regarding study participation.

End Points

The protocol specified that, upon identification of a new case of venous thromboembolism, the site investigator would complete a form indicating the source of confirmation of the event including venous ultrasonogram or venography for deep vein thrombosis, or angiogram or computed tomography scan or ventilation perfusion scan for pulmonary embolism. Consistent with the perspective on all secondary end points, cases with venous thromboembolism included all participants with a diagnosed pulmonary embolism or deep vein thrombosis. An important subgroup included those with corroborating evidence from a confirmatory diagnostic test, initiation of anticoagulation, or death likely due to pulmonary embolism (all but 3 cases). Unprovoked deep vein thrombosis or pulmonary embolism was defined as occurring in the absence of known malignancy (diagnosed either before or up to 3 months after the venous thrombosis), trauma, hospitalization, or surgery within 3 months before the event. Provoked venous thrombosis included events that occurred in patients with cancer or during or shortly after trauma, hospitalization, or surgery.

On March 30, 2008, the trial’s steering committee accepted the recommendation of the independent data monitoring board to terminate the trial based on convincing evidence of efficacy for the combined primary end point of myocardial infarction, stroke, arterial revascularization, hospitalization for unstable angina, or confirmed death from cardiovascular causes. Follow-up for the trial’s primary and secondary efficacy end points ended on that date. However, safety follow-up for the pre-specified secondary end points (These were venous thromboembolism, diabetes, study medication cessation due to an adverse event, bone fractures, any death, and non-cardiovascular death.) continued in a blinded manner for each study participant until the date he or she appeared for a formal closeout visit and discontinued study therapy. The last closeout visit occurred on August 20, 2008.

Statistical Analysis

All analyses of venous thromboembolism were performed on an intention-to-treat basis and considered only a participant’s first diagnosed venous thromboembolism after randomization. Cox proportional hazards models were used to estimate hazard ratios and 95% confidence intervals for the comparison of event rates in the two groups. In addition to the primary focus on events that occurred by March 30, 2008, secondary analyses included the additional person-time and events that occurred until a participant’s final closeout visit and unblinding of treatment assignment. Tertiary end points included provoked and unprovoked venous thromboembolism, cases with pulmonary embolism, and cases with deep vein thrombosis only. Subgroup analyses compared rates of venous thromboembolism between treatment groups according to the presence or absence of possible or likely determinants of venous thromboembolism.

Because venous thromboembolism commonly occurs around the time of cardiovascular events, additional analyses evaluated whether the apparent effect of rosuvastatin on venous thromboembolism could be secondary to the observed benefit on cardiovascular events. Separate proportional hazards models estimated the cause-specific hazard of venous thromboembolism, and the cause-specific hazard of a primary cardiovascular event, each in analyses that censored follow-up at first occurrence of either event. A likelihood ratio test compared the relative treatment effect between the two outcomes6. As a measure of the net clinical benefit of rosuvastatin considering combined effects on venous and arterial thrombosis, we also fitted a proportional hazards model with the first occurrence of venous thromboembolism or the primary cardiovascular end point as a composite outcome, and estimated risk differences and the number needed to treat26 for absolute measures of treatment efficacy. We also repeated these analyses with a composite end point of the first occurrence of venous thromboembolism, cardiovascular disease or death from any cause.


Baseline characteristics

Among the 17,802 randomized participants in JUPITER, 32.0% were initially aged 70 years or older, 38.2% were women, and 25.2% were black or Hispanic (Table 1). In both the rosuvastatin and placebo groups, 37.6% of subjects had a body mass index of 30 kg/m2 or higher. The median waist circumference was 100 cm in men and 95 cm in women. The metabolic syndrome was present in 41.7% of participants, and 41.3% had a high-sensitivity C-reactive protein level of 5.0 mg/L or higher.

Table 1
Baseline Characteristics of the Trial Participants, According to Study Group

Occurrence of venous thromboembolism

Symptomatic pulmonary embolism or deep vein thrombosis occurred in 94 participants between randomization and March 30, 2008, a median follow-up time of 1.9 years (Table 2). The rates of venous thromboembolism were 0.18 and 0.32 events per 100 person-years of follow-up in the rosuvastatin and placebo groups, respectively (hazard ratio 0.57; 95% confidence interval [CI] 0.37-0.86; P=0.007) (Table 2). Although cumulative incidence curves did not appear to diverge until about 1 year of treatment (Figure 1), a test for interaction between treatment assignment and continuous follow-up time found no significant violation of the proportional hazards assumption (P=0.14).

Figure 1Figure 1Figure 1
Panel A. Cumulative incidence of venous thromboembolism by treatment group in JUPITER. The P-value is based on a likelihood ratio test of the effect of rosuvastatin in a proportional hazards model.
Table 2
Occurrence of Venous Thromboembolism by Study Group

Among the 94 cases, 50 were unprovoked whereas 44 occurred in the presence of cancer or recent trauma, hospitalization, or surgery. The observed hazard reductions were similar in analyses restricted to unprovoked events (hazard ratio 0.61; 95% CI: 0.35-1.09; P=0.089) or to provoked events (hazard ratio 0.52; 95% CI: 0.28-0.96; P=0.033) (Table 2 and Figure 1). Half (N=17) of the cases in the rosuvastatin group involved pulmonary embolism, compared with 37% (N=22) of the cases in the placebo group, but these percentages were not different (P=0.21).

Extension of follow-up time through the final closeout visit, when participants learned their treatment assignment, identified an additional 5 cases of venous thromboembolism, to bring the total number of cases to 35 in the rosuvastatin group and 64 in the placebo group (Table 2). Analyses of all cases as well as of components of the outcome revealed similar estimates to those obtained in the primary efficacy analysis.

Analyses that excluded the 3 cases (1 in the rosuvastatin group and 2 in the placebo group) without corroborating evidence from a confirmatory diagnostic test, initiation of anticoagulation, or death likely due to pulmonary embolism, found nearly identical results.

Subgroup analyses

None of the baseline characteristics considered significantly modified the relationship of rosuvastatin with the hazard of venous thromboembolism (each P-value for interaction > 0.10) (Figure 2). Subgroups with the highest rates of venous thromboembolism in the placebo group included those participants aged 70 years or older, those with a body mass index of 30 kg/m2 or above, and those with a waist circumference at or above the gender-specific median (≥95 cm in women or ≥100 cm in men). Similar estimated reductions in the hazard of venous thromboembolism were observed in each of these higher risk subgroups, although confidence intervals were wide and effects not individually significant for some comparisons. The rate of venous thromboembolism was also elevated in the placebo group in follow-up time beyond 2 years after randomization, perhaps reflecting the interim development of comorbid conditions that can trigger venous thromboembolism.

Figure 2
Effects of rosuvastatin on the occurrence of venous thromboembolism according to baseline characteristics. The relative hazards for rosuvastatin as compared with placebo are shown, with the size of each black square proportionate to the number of participants ...

Venous thromboembolism and cardiovascular events

Additional analyses sought to identify the independent and possibly incremental effects of rosuvastatin on venous thromboembolism, beyond the benefits previously described for arterial thrombosis25. From randomization until March 30, 2008, 173 participants in the rosuvastatin group either had a venous thromboembolism or a primary cardiovascular end point (32 had venous thromboembolism first), and 305 participants in the placebo group had a venous thromboembolism or a primary cardiovascular event (56 had venous thromboembolism first) (Table 3). Few participants had both venous thromboembolism and the primary cardiovascular end point: 6 had venous thromboembolism after a primary cardiovascular event, and 3 had a primary cardiovascular event after venous thromboembolism. The estimated relative hazard of venous thromboembolism as a first event was not different from the estimated relative hazard of 0.56 associated with rosuvastatin for prevention of a primary cardiovascular event (P=0.99). Consideration of the first occurrence of either venous thromboembolism or the primary cardiovascular end point found that rates of this composite end point were 0.93 and 1.66 per 100 person-years of follow-up in the rosuvastatin and placebo groups, respectively (hazard ratio for rosuvastatin, 0.56; 95% CI: 0.47-0.68; P<0.001).

Table 3
Occurrence of Venous Thromboembolism, Cardiovascular Disease and Death by Study Group

Net benefits of statin treatment

If venous thromboembolism is combined with the primary cardiovascular end point to consider the first occurrence of either end point, the difference in rates between the placebo and rosuvastatin groups is 0.73 events per 100 person-years (Table 3). This is 24% larger than the rate difference of 0.59 observed for the primary cardiovascular end point alone25. The estimated number needed to treat for 4 years to prevent either one venous thromboembolism or one primary cardiovascular end point is 26, and projected to a 5-year treatment period this number is 21. These are reduced from the estimated numbers needed to treat for 4 and 5 years of 31 and 25, respectively, based only on the primary cardiovascular end point25.

Among the 94 participants who developed venous thromboembolism, 21 died by March 30, 2008 (14 in the placebo group). Altogether, 320 participants in the rosuvastatin group had a first cardiovascular event, venous thromboembolism or died, whereas 483 participants in the placebo group had one of these outcomes (hazard ratio 0.66; 95% CI, 0.57 to 0.76, P<0.001). With consideration of this composite end point, the number of patients needed to treat to prevent one event was estimated to be 23 for 4 years and projected to be 18 for 5 years.

Adverse Events

Rates of monitored adverse events and other reported adverse events of interest by treatment group were previously reported25. In particular, bleeding was reported as an adverse event in 258 participants assigned to rosuvastatin versus 275 participants assigned to placebo, P=0.45.


In this large, randomized trial of initially healthy men and women, 20 mg of rosuvastatin daily was associated with a substantial and statistically significant reduction in the occurrence of venous thromboembolism. The observed effect was comparable in relative magnitude and independent of the benefit seen previously for arterial events. The apparent benefit was also comparable in magnitude for provoked and unprovoked venous thromboembolism, and was of somewhat larger magnitude for the end point of deep vein thrombosis only. Consistent effects were seen across subgroups, with a notable benefit observed in the high risk subgroups of older participants and those with elevated waist circumference.

Venous thromboembolism is common, difficult to diagnose, costly to treat, and has frequent consequences including venous insufficiency and chronic thromboembolic pulmonary hypertension, so preventive strategies with acceptable costs and side effects are needed. With 94 observed cases, the frequency of venous thromboembolism among the participants in JUPITER was comparable to that of fatal or nonfatal stroke (97 cases) and fatal or nonfatal myocardial infarction (99 cases). This is consistent with population-based estimates that the incidence of venous thromboembolism is similar to that of stroke in Rochester County, Minnesota28 and that of myocardial infarction in the Brest district of France29.

In JUPITER, we observed little evidence of increased rates of venous thromboembolism among participants in the placebo group with higher levels of LDL cholesterol or triglycerides, or among those with lower levels of HDL cholesterol. This is consistent with two prospective cohort studies that found no associations of levels of HDL, LDL, total cholesterol or triglycerides with risk of venous thromboembolism5, 30, 31, but contrasts with the observation of an increased risk of recurrent venous thromboembolism associated with lower levels of HDL cholesterol32. Also consistent with the JUPITER data is the lack of association of non-statin lipid-lowering drugs with the occurrence of venous thromboembolism seen in prior studies15, 17, 18. Participants in JUPITER with a baseline level of high-sensitivity C-reactive protein at or above 5 mg/L had a somewhat elevated rate of venous thromboembolism. However, prospective observational studies indicate that high-sensitivity C-reactive protein has limited ability to predict future venous thromboembolism after control for body mass index33, 34. Statins have several other mechanisms of action that could limit venous thromboembolism. Statins inhibit isoprenylation of signaling proteins, with several potential antithrombotic consequences such as reduced tissue factor expression and thrombin generation, attenuated fibrinogen cleavage, and activation of factors V and VII11,12,34. Statins also augment the activity of the transcription factor Kruppel-like factor-2 (KLF-2), promoting thrombomodulin and reducing PAI-1 expression in human endothelial cells35.

Limitations of our study include its restriction to initially healthy participants, limited long-term follow-up, and the need to elaborate the potential mechanisms of action of statins on the occurrence of venous thromboembolism. Main strengths of our study include its prospective, double-blind treatment assignment and end point ascertainment, and its pre-specification of venous thromboembolism as a trial end point. Our study also does not allow for evaluation of the relationship of dose of statin with risk of venous thromboembolism. Some observational evidence suggests a possibly greater benefit with higher doses16, but confounding and small study size were limitations. While JUPITER focused on symptomatic venous thromboembolism, asymptomatic venous thromboembolism is common and consequential36, thus the magnitude of the absolute risk may have been underestimated. Overall, validation of our results, and further elucidation of the potential mechanisms, will be important to confirm our findings. In particular, randomized evidence on statin use in high risk individuals, such as those with a prior venous thrombosis, is needed.

In conclusion, in this randomized trial of apparently healthy men and women, rosuvastatin was associated with a significant reduction in the risk of venous thromboembolism. This risk reduction appears to be an independent benefit of statin use, beyond the reduction in risk of arterial thrombosis. Widening the treatment target to a consideration of venous thromboembolism and death in addition to arterial thrombosis increases the estimated benefits associated with statin use.


Supported by Astra-Zeneca and grant AG031061 from the US National Institute on Aging


The JUPITER trial was investigator-initiated and supported by Astra-Zeneca, US.

During the period of this project, Dr Glynn reports receiving research grant support from Astra-Zeneca and Bristol Myers Squibb. Dr Fonseca reports having received research grants, lecture fees, and consulting fees from Astra-Zeneca, Pfizer, Schering-Plough, Sanofi-Aventis, and Merck. Dr Genest reports having received lecture fees from Astra-Zeneca, Schering Plough, Merck Schering Plough, Pfizer, Novartis, and Sanofi-Aventis; and consulting fees from Astra-Zeneca, Merck, Merck Frosst, Schering-Plough, Pfizer, Novartis, Resverlogix, and Sanofi-Aventis. Dr Gotto reports having received consulting fees from Dupont, Novartis, Aegerion, Arisaph, KOWA, Merck, Merck Schering Plough, Pfizer, Genentech, Martek, and Reliant, having served as an expert witness, and as having received publication royalties. Dr Kastelein reports receiving research grant support from Astra-Zeneca, Pfizer, Roche, Novartis, Merck, Merck Schering Plough, ISIS, Genzyme, and Sanofi-Aventis; lecture fees from Astra-Zeneca, Glaxo Smith Kline, Pfizer, Novartis, Merck-Schering Plough, Roche, ISIS, and Boehringer-Ingelhiem; and consulting fees from Astra-Zeneca, Abbott, Pfizer, ISIS, Genzyme, Roche, Novartis, Merck, Merck Schering Plough, and Sanofi-Aventis. Dr Koenig reports receiving research grant support from Anthera, Dade-Behring and Glaxo-Smith-Kline; lecture fees from Astra-Zeneca, Pfizer, Novartis, Glaxo-Smith-Kline, DiaDexus, Roche, and Boehringer-Ingelheim; and consulting fees from Glaxo-Smith Kline, Medlogix, Anthera, and Roche. Dr Libby reports receiving lecture fees from Pfizer and lecture or consulting fees from Astra-Zeneca, Bristol Myers Squibb, Glaxo Smith Kline, Merck, Pfizer, Sanofi-Aventis, VIA Pharmaceutical, Interleukin Genetics, Kowa Research Institute, Novartis, and Merck Schering Plough. Dr Lorenzatti reports receiving research grant support, lecture fees, and consulting fees from Astra-Zeneca, Takeda, and Novartis. Dr Nordestgaard reports receiving lecture fees from Astra-Zeneca, Abbott, Sanofi-Aventis, Pfizer, Boehringer Ingelheim and Merck; and consulting fees from Astra-Zeneca and BG Medicine. Dr Shepherd reports receiving lecture fees from Astra-Zeneca, Pfizer, and Merck; and consulting fees from Astra-Zeneca, Merck, Roche, Glaxo SmithKline, Pfizer, Nicox, and Oxford Biosciences. Dr Ridker reports having received investigator-initiated research grant support from Astra-Zeneca, Novartis, Roche, and Sanofi-Aventis, as well as non-financial research support from Amgen; consulting fees and/or lecture fees from Astra-Zeneca, Novartis, Merck, Merck-Schering Plough, Sanofi-Aventis, ISIS, Seimens, and Vascular Biogenics; and is listed as a co-inventor on patents held by the Brigham and Women’s Hospital that relate to the use of inflammatory biomarkers in cardiovascular disease. These patents have been licensed to several entities, including Astra-Zeneca and Seimens. Dr. Willerson, Ms Danielson, and Ms MacFadyen report no conflicts.


1. Prandoni P, Bilora F, Marchiori A, Bernardi E, Petrobelli F, Lensing AWA, Prins MH, Girolami A. An association between atherosclerosis and venous thrombosis. N Engl J Med. 2003;348:1435–1441. [PubMed]
2. Sørensen HT, Horvath-Puho E, Pedersen L, Baron JA, Prandoni P. Venous thromboembolism and subsequent hospitalization due to acute arterial cardiovascular events: a 20-year cohort study. Lancet. 2007;370:1773–1779. [PubMed]
3. Goldhaber SZ, Grodstein F, Stampfer MJ, Manson JE, Colditz GA, Speizer FE, Willett WC, Hennekens CH. A prospective study of risk factors for pulmonary embolism in women. JAMA. 1997;277:642–645. [PubMed]
4. Hansson P-O, Eriksson H, Welin L, Svårdsudd K, Wilhelmsen L. Smoking and abdominal obesity. Risk factors for venous thromboembolism among middle-aged men: the study of men born in 1913. Arch Intern Med. 1999;159:1886–1890. [PubMed]
5. Tsai AW, Cushman M, Rosamond W, Heckbert SR, Polak JF, Folsom AR. Cardiovascular risk factors and venous thromboembolism incidence. Arch Intern Med. 2002;162:1182–1189. [PubMed]
6. Glynn RJ, Rosner B. Comparison of risk factors for the competing risks of coronary heart disease, stroke, and venous thromboembolism. Am J Epidemiol. 2005;162:975–982. [PubMed]
7. Ageno W, Beccattini C, Brighton T, Selby R, Kamphuisen PW. Cardiovascular risk factors and venous thromboembolism: a meta-analysis. Circulation. 2008;117:93–102. [PubMed]
8. Lowe GDO. Arterial disease and venous thrombosis: are they related, and if so, what should we do about it? J Thromb Haemost. 2006;4:1882–1885. [PubMed]
9. Agnelli G, Becattini C. Venous thromboembolism and atherosclerosis: common denominators or different diseases? J Thromb Haemost. 2006;4:1886–1890. [PubMed]
10. Glynn RJ, Ridker PM, Goldhaber SZ, Buring JE. Effect of low-dose aspirin on the occurrence of venous thromboembolism: a randomized trial. Ann Intern Med. 2007;147:525–533. [PubMed]
11. Undas A, Brummel-Ziedins KE, Mann KG. Statins and blood coagulation. Arterioscler Thromb Vasc Biol. 2005;25:287–294. [PubMed]
12. Kaba NK, Francis CW, Moss AJ, Zareba W, Oakes D, Knox KL, Fernández ID, Rainwater DL. Effects of lipids and lipid-lowering therapy on hemostatic factors in patients with myocardial infarction. J Thromb Haemost. 2004;2:718–725. [PubMed]
13. Albert MA, Danielson E, Rifai N, Ridker PM. Effect of statin therapy on C-reactive protein levels: the pravastatin inflammation/CRP evaluation (PRINCE): a randomized trial and cohort study. JAMA. 2001;286:64–70. [PubMed]
14. Grady D, Wenger NK, Herrington D, Khan S, Furberg C, Hunninghake D, Vittinghoff E, Hulley S. Postmenopausal hormone therapy increases risk for venous thromboembolic disease. Ann Intern Med. 2000;132:689–696. [PubMed]
15. Ray JG, Mamdani M, Tsuyuki RT, Anderson DR, Yeo EL, Laupacis A. Use of statins and the subsequent development of deep vein thrombosis. Arch Intern Med. 2001;161:1405–1410. [PubMed]
16. Doggen CJM, Lemaitre RN, Smith NL, Heckbert SR, Psaty BM. HMG CoA reductase inhibitors and the risk of venous thrombosis among postmenopausal women. J Thromb Haemost. 2004;2:700–701. [PubMed]
17. Lacut K, Oger E, Le Gal G, Couturaud F, Louis S, Leroyer C, Mottier D. Statins but not fibrates are associated with a reduced risk of venous thromboembolism: a hospital-based case-control study. Fundam Clin Pharmacol. 2004;18:477–482. [PubMed]
18. Ramcharan AS, van Stralen KJ, Snoep JD, Mantel-Teeuwisse AK, Rosendaal FR, Doggen CJM. HMG-CoA-reductase inhibitors, other lipid lowering medication, antiplatelet therapy, and the risk of venous thrombosis. J Thromb Haemost. 2009 epub ahead of print. [PubMed]
19. Sørensen HT, Horvath-Puho E, Søgaard KK, Christensen S, Johnsen SP, Thomsen RW, Prandoni P, Baron JA. Arterial cardovascular events, statins, low dose aspirin and subsequent risk of venous thromboembolism: a population-based case-control study. J Thromb Haemost. 2009 epub ahead of print. [PubMed]
20. Yang CC, Jick SS, Jick H. Statins and the risk of idiopathic venous thromboembolism. Br J Clin Pharmacol. 2002;53:101–105. [PMC free article] [PubMed]
21. Smeeth L, Douglas I, Hall AJ, Hubbard R, Evans S. Effect of statins on a wide range of health outcomes: a cohort study validated by comparison with randomized trials. Br J Clin Pharmacol. 2008;67:99–109. [PMC free article] [PubMed]
22. Glynn RJ, Schneeweiss S, Wang PS, Levin R, Avorn J. Selective prescribing led to overestimation of the benefits of lipid-lowering drugs. J Clin Epidemiol. 2006;59:819–828. [PubMed]
23. Ray JG. Do we care if statins prevent venous thromboembolism? J Thromb Haemost. 2004;2:695–696. [PubMed]
24. Ridker PM, Fonseca FAH, Genest J, et al. Baseline characteristics of participants in the JUPITER trial, a randomized placebo-controlled primary prevention trial of statin therapy among individuals with low low-density lipoprotein cholesterol and elevated high-sensitivity C-reactive protein. Am J Cardiol. 2007;100:1659–1664. [PubMed]
25. Ridker PM, Danielson E, Fonseca FAH, et al. Rosuvastatin to prevent vascular events in men and women with elevated C-reactive protein. N Engl J Med. 2008;359:2195–2207. [PubMed]
26. Altman DG, Andersen PK. Calculating the number needed to treat for trials where the outcome is time to an event. BMJ. 1999;319:1492–1495. [PMC free article] [PubMed]
27. Grundy SM, Cleeman JI, Daniels SR, et al. Diagnosis and management of the metabolic syndrome: an American Heart Association/National Heart, Lung, and Blood Institute scientific statement: executive summary. Circulation. 2005;112:2735–2752. Errata, Circulation 2005; 112(17):e297,e298. [PubMed]
28. Silverstein MD, Heit JA, Mohr DN, Petterson TM, O’Fallon WM, Melton LJ., 3rd Trends in the incidence of deep-vein thrombosis and pulmonary embolism: a 25-year population-based study. Arch Intern Med. 1998;158:583–593. [PubMed]
29. Oger E. Incidence of venous thromboembolism: a community-based study in Western France. EPI-GETBP Study Group. Groupe d’Etude de la Thrombose de Bretagne Occidentale. Thromb Haemost. 2000;83:657–660. [PubMed]
30. Everett BM, Glynn RJ, Buring JE, Ridker PM. Lipid biomarkers, hormone therapy, and risk of venous thromboembolism in women. J Thromb Haemost. 2009 epub ahead of print. [PMC free article] [PubMed]
31. Chamberlain AM, Folsom AR, Heckbert SR, Rosamond WD, Cushman M. High-density lipoprotein cholesterol and venous thromboembolism in the Longitudinal Investigation of Thromboembolism Etiology (LITE) Blood. 2008;112:2675–2680. [PubMed]
32. Eichinger S, Pecheniuk NM, Hron G, Deguchi H, Schemper M, Kyrle PA, Griffin JH. High-density lipoprotein and the risk of recurrent venous thromboembolism. Circulation. 2007;115:1609–1614. [PubMed]
33. Ridker PM, Cushman M, Stampfer MJ, Tracy RP, Hennekens CH. Inflammation, aspirin, and the risk of cardiovascular disease in apparently healthy men. N Engl J Med. 1997;336:973–979. [PubMed]
34. Tsai AW, Cushman M, Rosamond WD, Heckbert SR, Tracy RP, Aleksic N, Folsom AR. Coagulation factors, inflammation markers, and venous thromboembolism: the Longitudinal Investigation of Thromboembolism Etiology (LITE) Am J Med. 2002;113:636–642. [PubMed]
35. Sen-Banerjee S, Mir S, Lin Z, Hamik A, Atkins GB, Das H, Banerjee P, Kumar A, Jain MK. Kruppel-like factor 2 as a novel mediator of statin effects in endothelial cells. Circulation. 2005;112:720–726. [PubMed]
36. Vaitkus PT, Leizorovicz A, Cohen AT, Turpie AGG, Olsson C-G, Goldhaber SZ. Mortality rates and risk factors for asymptomatic deep vein thrombosis in medical patients. Thromb Haemost. 2005;93:76–79. [PubMed]