Diabetes and lipid lowering: where are we?

doi:10.1136/bmj.332.7550.1103

BMJ 2006;332:1103-1104 (13 May), doi:10.1136/bmj.332.7550.1103

Editorial

Diabetes and lipid lowering: where are we?

We're now sure that statins cut cardiovascular risks in type2 diabetes

Premature morbidity and mortality is substantially due to cardiovasculardisease, with tobacco use, hypertension, and abnormal lipidsbeing the main modifiable causal factors. Glycaemia is directlyrelated to cardiovascular risk,¹ and in people with diabetesthe risk of cardiovascular disease approaches that in non-diabeticpeople with previous myocardial infarction.^{2 3}

Because most people with type 2 diabetes have an absolute riskof cardiovascular disease of 20% or more over 10 years, guidelinessuggest active intervention to reduce risk factors in patientswith diabetes, including statin therapy to reduce the serumconcentration of low density lipoprotein cholesterol (LDL-C)to < 2 mmol/l.³ In this week's BMJ Costa and colleagues reporta meta-analysis of trials of lipid lowering drug therapy forprimary and secondary coronary heart disease prevention in patientswith and without diabetes.⁴

Review by the National Institute for Health and Clinical Excellence(NICE) of the role of statins in preventing cardiovascular diseasehas endorsed the routine use of statins in people with an absoluterisk of ³ 20% over 10 years as effective and cost effective(especially with the use of generic statins).⁵ Recent largerandomised trials of treatment with statins, such as the heartprotection study,⁶ have extended the evidence base over a widerange of populations. A prospective meta-analysis of more than90 000 patients in cholesterol lowering trials showed that fora 1 mmol/l reduction in serum low density lipoprotein (LDL)cholesterol there is a 21% (95% confidence interval 0.77% to0.81%) reduction in cardiovascular events and similarly in strokeof 21% (0.73% to 0.85%).⁷ These associations are largely independentof baseline cholesterol and demographic factors, while the largerthe reduction in LDL cholesterol, the greater the risk reduction.

Although previous trials did not include large numbers of patientswith diabetes, the many thousands of patients in the heart protectionstudy (HPS)⁶ and the collaborative atorvastatin diabetes study(CARDS) trials⁸ have now provided further evidence that loweringLDL cholesterol is beneficial for people with diabetes. Thedata from the heart protection study show little heterogeneityin the reduction in cardiovascular risk in the presence or absenceof diabetes. But do people with diabetes respond to lipid loweringtherapy better, equally, or less well than those with normalglucose handling?

In their meta-analysis (p 1115), Costa and colleagues identified581 relevant studies up to April 2004.⁴ Of these, 12 were randomisedplacebo controlled trials (six primary prevention, eight secondaryprevention) which fulfilled the criteria of having > 500patients per group treated for three years in whom cardiovascularoutcome data for diabetes and nondiabetes subgroups could beidentified separately. What did the meta-analysis find? In bothprimary and secondary prevention of major coronary events therewere highly significant and similar relative risk reductionsof 21% (diabetes) and 23% (non-diabetes), in the presence ofsimilar lipid changes. In the analyses of secondary preventionthe absolute risk was three times higher than in those for primaryprevention.

Are there any difficulties with this study? This meta-analysislooked at lipid lowering drugs in general and not just statins(the agents of first choice to achieve target LDL cholesterolconcentrations). Two studies used the fibrate gemfibrozil, whichis less well tolerated and has more potential side effects thanother agents,³ but their omission would not materially affectthe overall results. Some data came from unplanned analysesof subgroups of participants with diabetes. Unfortunately, theanalyses of secondary prevention excluded data from the heartprotection study because there was no separate information forgroups with diabetes. Data were insufficient to examine individualdrugs or doses. Finally, no data from the CARDS study were includedbecause this study was a randomised trial between placebo andthe standard active drug in type 2 diabetes without a concurrentnon-diabetes group.⁸

Where are we now, and what does this meta-analysis add to ourknowledge? Statins are clearly a highly effective treatmentfor primary and secondary prevention of cardiovascular disease,yielding similar relative risk reductions in patients with andwithout diabetes. Absolute risk is higher in patients needingsecondary prevention and in patients with diabetes.

All patients with type 2 diabetes should be considered for,and the vast majority should receive, statin treatment if theirserum concentration of LDL cholesterol is $≥$ 2 mmol/l. The situationis much less clear for treatment with fibrates. Fibrates willprobably remain mainly second line agents after the LDL targetis achieved, and—despite the finding of only moderatebenefits in the fenofibrate intervention and event loweringin diabetes (FIELD) study⁹—fenofibrate is the agent ofchoice rather than gemfibrozil.

The study by Costa and colleagues does not contribute to therelative lack of information about patients with type 1 diabetes,because few such patients have been included in the many statintrials (apart from moderate numbers in the heart protectionstudy), but responses among such patients would probably besimilar. People with type 1 diabetes have substantial macrovascularrisk, related to age and duration of diabetes. Statin therapyis indicated for those aged 40 and over, and also for adultsunder 40 who have microvascular complications, hypertension,sustained poor glycaemic control, metabolic syndrome, or anadverse family history.³ Statins should be avoided, however,among women from the planning of conception to the end of breastfeeding.

In statins we now have highly effective treatments to preventcardiovascular disease in people with diabetes, and as clinicianswe need to ensure that this treatment is widely used along withother effective strategies. Nevertheless, even with statin therapy,70% of cardiovascular events still occur.

John P D Reckless, consultant endocrinologist

Royal United Hospital, Bath BA1 3NG
(mpsjpdr{at}bath.ac.uk)

Competing interests: JPDR was a centre investigator in the heartprotection study and the collaborative atorvastatin diabetesstudy.

Research p 1115

References

DECODE Study Group, on behalf of the European Diabetes Epidemiology Group. Glucose tolerance and cardiovascular mortality: comparison of fasting and 2-hour diagnostic criteria. Arch Intern Med 2001;161: 397-405[Abstract/Free Full Text]
Haffner SM, Lehto S, Ronnemaa T, Pyorala K, Laako M. Mortality from coronary heart disease in subjects with type 2 diabetes and in non-diabetic subjects with and without prior myocardial infarction. N Engl J Med 1998; 339: 229-34.[Abstract/Free Full Text]
Joint British Societies' guidelines on prevention of cardiovascular disease in clinical practice. Heart 2005;91(suppl V): 1-52.[Abstract/Free Full Text]
Costa J, Borges M, David C, Carneiro AV. Efficacy of lipid lowering drug treatment for diabetic and non-diabetic patients: meta-analysis of randomised controlled trials. BMJ 2006;332: 1115-8.[Abstract/Free Full Text]
National Institute of Health and Clinical Excellence. Cardiovascular diseases—statins. (NICE HTA 094.) Jan 2006. www.nice.org.uk/page.aspx?o=63311 (accessed 18 Apr 2006).
Heart Protection Study Collaborative Group. MRC/BHF heart protection study of cholesterol lowering with simvastatin in 20,536 high-risk individuals: a randomised, placebo-controlled trial. Lancet 2002; 360: 7-22.[CrossRef][ISI][Medline]
Cholesterol Treatment Trialists' Collaboration. Efficacy and safety of cholesterol-lowering treatment: prospective meta-analysis of data from 90,056 participants in 14 randomised trials of statins. Lancet 2005; 366: 1267-78.[CrossRef][ISI][Medline]
Colhoun HM, Betteridge DJ, Durrington PN, Hitman GA, Neil NA, Livingstone SJ, et al. Primary prevention of cardiovascular disease with atorvastatin in type 2 diabetes in the Collaborative Atorvastatin Diabetes Study (CARDS): multicentre, randomised placebo-controlled trial. Lancet 2004;364: 685-96.[CrossRef][ISI][Medline]
FIELD Study Investigators. Effects of long-term fenofibrate therapy on cardiovascular events in 9795 people with type 2 diabetes mellitus (the FIELD study): randomised controlled trial. Lancet 2005;366: 1849-61.[CrossRef][ISI][Medline]

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Efficacy of lipid lowering drug treatment for diabetic and non-diabetic patients: meta-analysis of randomised controlled trials: João Costa, Margarida Borges, Cláudio David, and António Vaz Carneiro
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