Review

Severely frail elderly patients do not need lipid-lowering drugs

Laurie Herzig Mallery, MD, FRCPC, MSM, Paige Moorhouse, MD, MPH, FRCPC, MSM, Pam McLean Veysey, BSc (Pharm), Michael Allen, MD, MSc and Isobel Fleming, BScPharm, ACPR
Cleveland Clinic Journal of Medicine February 2017, 84 (2) 131-142; DOI: https://doi.org/10.3949/ccjm.84a.15114

Article Figures & Data

Tables

  • TABLE 1

    Studies of lipid-lowering therapy discussed in this paper

    StudyDesignPopulationMean follow-up
    PROSPER13Randomized controlled trial
    Pravastatin 40 mg vs placebo    		N = 5,804, mean age 75
    Primary and secondary prevention
    Mini-Mental State score ≥ 24 of 30    		3.2 years
    JUPITER28,29Randomized controlled trial
    Rosuvastatin 20 mg vs placebo    		N = 5,695 (elderly subgroup)
    Median age 74
    Primary prevention    		1.9 years (stopped prematurely)
    CTT32Meta-analysisNot applicableaVariable
    Afilalo et al31Meta-analysisN = 19,569
    Age range 65–82
    Secondary prevention    		4.9 years
    SPARCL27,30Randomized controlled trial
    Atorvastatin 80 mg vs placebo    		N = 2,249 (subgroup age ≥ 65)
    Mean age of subgroup 72.4
    Secondary prevention    		4.9 years
    GISSI-HF25Randomized controlled trial
    Rosuvastatin 10 mg vs placebo    		N = 4,574, mean age 68
    Heart failure, NYHA class II to IV    		3.9 years (median)
    CORONA26Randomized controlled trial
    Rosuvastatin 10 mg vs placebo    		N = 5,011, mean age 73
    Heart failure, NYHA class II to IV    		2.7 years

    • a The CTT meta-analysis presents the effects of statins on major vascular events per annum, per 1.0 mmol/L reduction in LDL-C according to 5-year risk at baseline. The analysis in patients > 70 years old includes a total of 2,952 events in the statin group and 3,385 events in the control group (or a total of 6,337 events.

    • CORONA = Controlled Rosuvastatin Multinational Trial in Heart Failure; CTT = Cholesterol Treatment Trialists; GISSI-HF= Gruppo Italiano per lo Studio della Sopravvivenza nell’Insufficienza Cardiaca Heart Failure; JUPITER = Justification for the Use of Statins in Prevention; NYHA = New York Heart Association; PROSPER = Prospective Study of Pravastatin in the Elderly at Risk; SPARCL = Stroke Prevention by Aggressive Reduction in Cholesterol Levels

  • TABLE 2

    Coronary heart disease outcomes

    Trial and outcomeEvent rate P valueAbsolute risk reductionRelative risk reductionNumber needed to treat (95% CI)
    PlaceboStatin
    Primary prevention studies
    PROSPER13
    Coronary heart disease death and nonfatal myocardial infarction    		8.8%7.9%.4010.9%9%NSa
    JUPITER28,29
    yocardial infarction    		1.1%0.6%.0460.5%45%211 (106–32,924)
    Secondary prevention studies
    PROSPER13
    Coronary heart disease death and nonfatal myocardial infarction (includes definite and suspect events)    		16.8%12.7%.0044.1%24%25 (15–77)
    Afilalo et al meta-analysis31
    Nonfatal myocardial infarction    		NANANANA26%b38 (16–118)b
    Combined primary and secondary prevention studies
    PROSPER13
    Nonfatal myocardial infarction (excluding silent and unrecognized events)    		4.3%3.4%.0990.9%20%NSa

    • a Not statistically significant (P > .05) and numbers needed to treat (NNT) not calculated on these results. NNT calculated on raw numbers if not provided in publication. See Table 1 for duration of treatment required for NNT.

    • b Afilalo et al provided relative risk reductions and NNTs in their publication. Absolute risk reductions not calculated on meta-analytic outcomes.

    • CI = confidence interval; NA = not available; NS = not statistically significant

  • TABLE 3

    Stroke outcomes

    Trial and outcomeEvent rate P valueAbsolute risk reductionRelative risk reductionaNumber needed to treat (95% CI)
    PlaceboStatin
    Primary prevention studies
    PROSPER13
    Fatal or nonfatal stroke
    Transient ischemic attack    		3.7%3.8%.8820.1% increase3% increaseNSb
    2.3%1.9%.4220.4%18%NS
    JUPITER28,29
    Stroke (percent based on raw number of events)    		1.4%0.8%.0230.6%45%161 (86–1,192)
    Secondary prevention studies
    PROSPER13
    Fatal and nonfatal stroke
    Transient ischemic attack    		5.5%5.7%.8380.2% increase3% increaseNS
    5.1%3.6%.0651.5%29%NS
    Afilalo meta-analysis31
    Stroke (disabling and nondisabling)    		NANANANA25%58c (27–177)
    SPARCL27
    Fatal or nonfatal stroke
    Nonfatal stroke    		13.1%11.2%.031.9%15%52 (26–1,303)
    11.8%10.4%.111.4%12%NS
    SPARCL subgroup ≥ 6530
    Fatal or nonfatal stroke    		16.2%14.7%.331.5%10%NS
    SPARCL subgroup < 6530
    Fatal or nonfatal stroke    		10.5%7.9%.0222.6%24%39 (21–354)

    • a Numbers for relative risk reduction are rounded to the nearest whole number

    • b Not statistically significant (P >.05) and numbers needed to treat not calculated on these results. Number needed to treat (NNT) calculated on raw numbers if not provided in publication. See Table 1 for duration of treatment required for NNT. CI = confidence interval

    • c Afilalo et al provided relative risk reductions and NNT. Absolute risk reductions not calculated on meta-analytic outcomes.

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