Download except subgroup TG > 200 mg/dL and HDL-C

Survey
yes no Was this document useful for you?
   Thank you for your participation!

* Your assessment is very important for improving the workof artificial intelligence, which forms the content of this project

page
1
page
2
page
3
page
4
page
5
page
6
page
7
page
8
page
9
page
10
page
11
page
12
page
13
page
14
page
15
page
16
page
17
page
18
page
19
page
20
page
21
page
22
page
23
page
24
Document related concepts

Neuropharmacology wikipedia , lookup

Polysubstance dependence wikipedia , lookup

Adherence (medicine) wikipedia , lookup

Prescription costs wikipedia , lookup

Pharmacogenomics wikipedia , lookup

Bad Pharma wikipedia , lookup

Theralizumab wikipedia , lookup

Bilastine wikipedia , lookup

Transcript 
An Update on Niacin
Ernst J. Schaefer, MD
Distinguished University Professor, Tufts University
School of Medicine, Director, Lipid Metabolism
Laboratory & Cardiovascular Research Clinic, Boston, MA
February 25th, 2013
Ernst J. Schaefer, MD
Consulting: Merck and Company, Inc.
Grant Support: Abbott Laboratories and DuPont
Honoraria: Arisaph Pharmaceuticals
Stocks, Stock Options, other ownership interest:
Boston Heart Laboratory
An Update on
Niacin
Ernst J. Schaefer, MD
Distinguished University Professor
Director, Lipid Metabolism Laboratory,
Human Nutrition Research Center on
Aging at Tufts University &Tufts University
School of Medicine, Boston, MA USA
Washington DC, February 25th, 2013
Rudolph Altschul (1901-1963): Niacin
Arch Biochem 1955;54:558-9.
Niacin


“Niacin is the only available
agent that significantly
increases HDL-C
concentrations”1.
“Among lipid-lowering
agents, niacin is the most
effective “HDL-raising drug”
and effectively modifies all
of the lipoprotein
abnormalities associated
with atherogenic
dyslipidemia”2.
1Genest
J, Frohlich J, Fodor G, McPherson R. CMAJ 2003;168(9):921-4, 2Expert Panel on
Detection, Evaluation, and Treatment of High Blood Cholesterol in Adults, NIH 2002.
Niacin
Niacin – Mechanisms of Action
 Niacin is an effective TG lowering agent,
especially in those with elevated TG levels
 Decreases FFA flux, decreases TG production
in the liver, and also enhances the clearance of
TRL apoB-48 and apoB-100.
 Increases ABCA1 and ABCG1 gene
expression in cell and animal studies, and
increases very large protective alpha-1 HDL in
animal and human studies.
 Increase adiponectin gene expression and
plasma levels.
Human Apolipoprotein (Apo) Metabolism
Synthetic
Sites
FFA
LPL, HL,
LCAT
Chylomicron
ApoB-48
other Apos
Lipids
4
Chylomicron
Remnant
ApoB-48, ApoE
Lipids
Catabolic
Sites
5 hours, +48%
Liver
6
1
8
Kidney
Intestine
HDL
ApoA-I
other Apos
Lipids
12 mg/kg/d
3
Liver
+24%
Scavenger
Cells
9
2
VLDL
ApoB-100
other Apos
Lipids
12 mg//kg/d
LPL, HL, 5
LCAT
4 hours
FFA
LDL
ApoB-100
Lipids
3.5 days
Peripheral
Cells
7
, +46%
Cohn JS et al J Clin Invest 1990: 85:804, Lamon-Fava S et al ATVB 2008; 28:1672-8.
Niaspan: Combined Data from Pivotal Placebo-Controlled Studies
30
HDL-C
20
Change from Baseline
10
0
-10
16%
21%
24%
10%
-3%
-5%
-8%
-12%
-14%
-20
-13%
-17%
-21%
-30
-16%
LDL-C
-25% Lp(a)
-32%
-40
-50
500 mg
1000 mg
1500 mg
2000 mg
TG
* p<0.01
Niacin and Cardiovascular Protection:
Secondary Prevention Studies
Study
Coronary Drug
Project (CDP)1,-4
Treatment(s)
Duration
(years)
Results
5
Non-fatal MI  27%
Stroke/TIA  24%
Nicotinic acid vs placebo
15
Stockholm
Ischemic Heart
Disease Study
(IHD)5
Nicotinic acid + clofibrate
HDL
Atherosclerosis
Treatment Study
(HATS)6
Nicotinic acid + simvastatin ±
antioxidants vitamins vs
placebo
5
3
Total mortality  11%
Total mortality  26%
CHD mortality  36%
CHD mortality, non-fatal MI or
revascularization procedure –
 60%-90%
1. CDP Research Group. JAMA. 1975;231:360 (n=1119 in the niacin group) , 2. Canner PL et all J Am Coll Cardiol.
1986;8:1245, 3. Canner PL et al Am J Cardiol 2005;95:254-257, 4.Canner PL et al Am J Cardiol 2006;97:477-479.,
5. Carlson LA, Rosenhamer G. Acta Med Scand. 1988;223:405 , 6. Brown BG et al. New Engl J Med. 2001;345:1583
(n=160 total, 80 got niacin plus simvastatin with or without antioxidants).
Coronary Drug Project:
Effect of Niacin in Post-MI Patients
Cumulative Rate of Nonfatal MI in
Post-MI Patients Treated With Niacin or Placebo
Cumulative Event Rate (%)
15
Recurrent
nonfatal MI
Placebo
Niacin
10
27%
5
(P < 0.004)
0
12
34
36
48
60
Months of Follow-up
Patients receiving niacin (n=1119) vs patients receiving placebo (n=2789). Total mortality
was similar between the 2 groups at 5 years.
The Coronary Drug Project Research Group. JAMA. 1975;231:360-381.
ApoA-I-Containing HDL Subpopulation Profiles of a Control
and a CHD Patient (b) – Lack of Large HDL in CHD
pre
 pre
[nm]
17.0
9.51
8.16
7.10
4.66
Asztalos et al. Arterioscler Thromb Vasc Biol. 2003;23:847-852;
2004; 24:2181-2187, 2005; 25:2185-2191, HATS Trial, Framingham
Offspring Study, and the Veterans Affairs HDL Intervention Trial
Differences in HDL Particles in Male CHD Cases vs
Controls in the Framingham Offspring Study
Apo A-I Concentration
Controls (n=1277)
17 mg/dl
% Difference
Cases (n=169)
- 39%*
(16% of total)
40 mg/dl
- 9%
(37% of total)
38 mg/dl
+ 29%*
(36% of total)
12 mg/dl
+ 16%*
(11% of total)
“For each 1 mg/dl apoA-I increase in alpha 1 HDL - 26% reduction in CHD risk
Asztalos BF et al. Arterioscler Thromb Vasc Biol 2004; 24:2181-2187.
Effects of Simvastatin/Niacin on HDL Particles in CHD
Cases in HATS (n=123)
Apo A-I Concentration
Difference
9 mg/dl
%
+ 115%*
30 mg/dl
+ 27%
45 mg/dl
- 17%*
15 mg/dl
- 39%*
“The increase in apoA-I in large alpha 1 HDL was significantly related (p<0.01) to
lack of progression or regression of coronary artery stenosis.”
Asztalos BF, Batista M, Horvath KV, Cox CE, Dallal GE, Morse JS, Brown GB, Schaefer EJ. Arterioscler
Thromb Vasc Biol 2003;23:847-852.
AIM HIGH -1
(Atherothrombosis Intervention in Metabolic
Syndrome with Low HDL/ Hi TG and Impact on Global Health Outcomes)
> 3414 vascular disease patients on simvastatin or
simvastatin/ezetimibe received niacin (1718) or placebo (1696).
> The trial was stopped after a mean follow-up period of 3 years
owing to a lack of efficacy. At 2 years vs. baseline, niacin
therapy had significantly:
- increased HDL-C by 20% from 35 mg/dL to 42 mg/dl
- lowered TG levels by 26% from 164 mg/dL to 122 mg/dL
- lowered LDL-C by 16% from 74 mg/dL to 62 mg/dl.
> However the primary end point occurred in 282 patients in the
niacin group (16.4%) and in 274 patients in the placebo group
(16.2%) (hazard ratio, 1.02, P=0.79 by the log-rank test).
AIM HIGH -2
(Atherothrombosis Intervention in Metabolic
Syndrome with Low HDL/ Hi TG and Impact on Global Health Outcomes)
 Each placebo capsule contained 50 mg of niacin, so
subjects on placebo received up to 200 mg/day of
niacin.
 In order to control for LDL-C levels, 22% of subjects in
the placebo group and 10% in the niacin group were
on ezetimibe 10 mg/day.
 LDL-C and HDL-C were 68 and 38 mg/dl on trial in the
control group and 63 (-7%) and 42 (+9%) mg/dl in the
treatment group on trial.
 The study was powered to see a 25% risk reduction in
the primary endpoint.
Boden W et al N Engl J Med.2011;365:2255-67.
AIM HIGH – Why Did the Study Fail? All of the
Below May Have Contributed.
 The study was underpowered.
 The study was stopped too early.
 The placebo group got low dose niacin which may have had an
effect, and also had beneficial changes relative to baseline.
 Twice as many patients in the placebo group received ezetimibe
as compared to the treatment group.
 Mean LDL-C at 63 mg/dL was only 7% lower in the treatment
group than in the placebo group. Raising HDL-C when LDL-C is <
70 mg/dL may not be effective in CHD risk reduction.
 Mean HDL-C at 42 mg/dL was only 9% higher in the treatment
group than in the placebo group.
AIM HIGH – Subgroup Analysis
 Post-hoc subgroup analysis of AIM-HIGH
 CHD subjects with TG > 200 mg/dL and HDL-C <
32 mg/dL
 This group had the highest risk of recurrent CHD
events in the placebo group (statin alone or statin
plus ezetimibe)
 Moreover in this subgroup those who received
niacin had a relative risk of 0.63 (p=0.017) versus
placebo group.
Guyton J et al AHA November 7th, 2012
Fibrates
Fibrates – Subgroup Analysis
 In ACCORD Lipid – overall event rate was 11.3%
in the simvastatin monotherapy group and 10.5%
in the simvastatin/ fenofibrate group (p=0.32).
 In the subgroup with TG > 200 mg/dL and HDLC < 35 mg/dL event rate was 17.3% (+53%) in the
simvastatin monotherapy group and 12.4% (-28%)
in the simvastatin/ fenofibrate group (p=0.03).
 Similar observations in BIP and FIELD
Ginsberg HN et al New Engl J Med 2010;362:1563-9
HPS2-THRIVE: Heart Protection Study 2: Treatment of
HDL to Reduce the Incidence of Vascular Events
 Presented by Prof. Jane Armitage, Oxford, PI, ESC/ 9/2012
 25,673 high-risk patients with occlusive arterial disease from
China, Scandinavia and UK randomized into study
 Randomized blinded comparison: ER niacin/ laropiprant
(ERN/LRPT) 2g daily versus placebo
 Primary end point: Major vascular events after median
follow-up of 4 years
 Pre-specified safety analyses: Median follow-up of 3.4 years
(to January 2012)
 Background LDL-lowering therapy with: Simvastatin 40mg
(+/- ezetimibe 10mg) daily
HPS2-THRIVE
Lipid levels by Region: Effect of 8 Weeks
ERN/LRPT during Pre-randomization Run-in
LDL-C (mg/dL)
n
Baseline Change % Change
China
10932
59
-12.4
Europe
14741
68
-14.0
All
25673
64
-13.2
-20%*
HDL-C (mg/dL)
China
Europe
10932
14741
41.2
46.2
+5.8
+7.8
All
25673
44.3
+7.0
+17%*
HPS2-THRIVE
Summary HPS2-THRIVE
• Largest ever randomized trial of effects of ER niacin on safety and CV events
in diverse high-risk patients – no significant benefit reported in press 2012.
• Among those tolerating ERN/LRPT for 8 weeks, 76% remained compliant
with active treatment after 3 years vs 85% on placebo
• ERN/LRPT increases risk of myopathy among patients on statin therapy,
particularly in the Chinese
• No clear adverse effects of ERN/LRPT on liver, but known niacin side-effects
on skin & GI confirmed
• Effects of 4 years of ERN/LRPT on vascular events in HPS2-THRIVE - full data
to be presented at ACC 3/9/13
Potential Adverse Effects of Laropiprant
 The effects of niacin on lipids are independent of GPR109A, but not the
flushing effects, which are due to cyclooxygenase (COX)-1 mediated
production of prostaglandin (PG) D2, followed by the COX-2 mediated
production of PGE2 (1).
 PGD2 acts by binding to the prostanoid receptors DP1 and DP2. Laropiprant
decreases the flushing induced by niacin by inhibiting the DP1 receptor.
 DP1 depletion in mice leads to increased atherosclerosis, thrombosis,
aneurysm formation, and hypertensive response to angiotensinogen II (2).
 Niacin inhibits atherosclerosis in mice via GPR109A by inducing ABCG1
dependent macrophage cholesterol efflux, and by inhibiting MIP-1 dependent
macrophage recruitment (1).
 Laropiprant, like COX-2 inhibitors, may cause increased CVD risk. Low dose
aspirin might be a far better alternative to lower flushing (2).
(1) Lukasova M et al J Clin Invest 2010;121:1163-73.
(2) Song WL et al. J Clin Invest 2012;122:1459-68.
Niacin Score Card
 Coronary Drug Project +
 Stockholm Ischemic Heart Disease
Study +
 HATS, Other Angiographic Studies +
 AIM HIGH – except subgroup TG > 200
mg/dL and HDL-C < 32 mg/dL -37% RR
 HPS2-THRIVE – subgroup analysis?
 More data from Dr. Armitage at ACC
3/9/13 Late Breaking Trials
Niacin
Thank you for your attention
Related documents
Quantification of Niacin and Folate Contents in Peanuts
Quantification of Niacin and Folate Contents in Peanuts
Modifying Coronary Artery Atherosclerosis : Dr Thomas Challenger
Modifying Coronary Artery Atherosclerosis : Dr Thomas Challenger
Niacinamide - Douglas Laboratories
Niacinamide - Douglas Laboratories
Niacin - Get Heart Healthy Today
Niacin - Get Heart Healthy Today
Cover
Cover
Document
Document
niacin niacinamide - DavisPlus
niacin niacinamide - DavisPlus
Therapy with riboflavin VITAMIN B
Therapy with riboflavin VITAMIN B
Table 1 Cholesterol Med Chart
Table 1 Cholesterol Med Chart
Public Health Quiz - Basic
Public Health Quiz - Basic