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Cardiometabolic Syndrome
Dr. Nabil Sulaiman
HOD Family and Community Medicine, Sharjah
University and University of Melbourne
&
Dr Dhafir A. Mahmood
Consultant Endocrinologist
Al- Qassimi & Al-Kuwait Hospital
Sharjah
Agenda
• History & Definition
• Clustering component of Metabolic Syndrome
• Cardiovascular disease worldwide
• Global cardiometabolic risks
• Abdominal obesity prevalence ( National &
International )
• Intra Abdominal Adiposity & associated risks
• Targeting Cardiometabolic Risk factors
• Multiple Risk Factor management
• A Critical Look at the Metabolic Syndrome
Metabolic Syndrome (History)
• 1923 - Kylin first to describe the clustering
of hypertension, hyperglycemia,
hyperuricemia
• 1936 - Himsworth first reported Insulin
insensitivity in diabetics
• 1965 - Yalow and Berson developed
insulin assay and correlated insulin levels
& glucose lowering effects in resistant and
non-resistant individuals
Metabolic Syndrome History (cont.)
• 1988 - Reaven in his Banting lecture at the
ADA meeting coined the term Syndrome X
and brought into focus the clustering of
features of Metabolic Syndrome
• Reaven now prefers the name, Insulin-
Resistance Syndrome - feels insulin
resistance is the common denominator for
Metabolic Syndrome
• Literature now extensive
Other Names Used:
• Syndrome X
• Cardiometabolic Syndrome
• Cardiovascular Dysmetabolic Syndrome
• Insulin-Resistance Syndrome
• Metabolic Syndrome
• Beer Belly Syndrome
• Reaven’s Syndrome
• etc.
Clustering of Components:
• Hypertension: BP. > 140/90
• Dyslipidemia: TG > 150 mg/ dL ( 1.7 mmol/L )
HDL- C < 35 mg/ dL (0.9 mmol/L)
• Obesity (central): BMI > 30 kg/M2
Waist girth > 94 cm (37 inch)
Waist/Hip ratio > 0.9
• Impaired Glucose Handling: IR , IGT or DM
FPG > 110 mg/dL (6.1mmol/L)
2hr.PG >200 mg/dL(11.1mmol/L)
• Microalbuninuria (WHO)
Necessary Criteria to Make Diagnosis
• WHO:
Impaired G handling + 2 other criteria.
–Also requires microalbuminuria -
Albumen/ creatinine ratio >30 mg/gm
creatinine
• IDF:
–Require central obesity plus two of the
other abnormalities
• NCEP/ATP III:
–Require three or more of the five criteria
What is cardiometabolic risk?*
• Global cardiometabolic risk represents the overall risk
of developing type 2 diabetes and/or cardiovascular
disease (including MI and stroke), which is due to a
cluster of modifiable risk factors/markers
• These include classical risk factors such as smoking,
high LDL, hypertension, elevated blood glucose and
emerging risk factors closely related to abdominal
obesity (especially intra-abdominal adiposity), such as
insulin resistance, low HDL, high triglycerides and
inflammatory markers
• Cardiometabolic risk is based on the
concept of risk continuum
* working definition
MI: myocardial infarction; LDL: low-density lipoprotein;
HDL: high-density lipoprotein
Global cardiometabolic risk*
Gelfand EV et al, 2006; Vasudevan AR et al, 2005
* working definition
Despite therapeutic advances, CV disease
remains the leading cause of death (USA)
0
100
200
300
400
500
Heart
disease and
stroke
Cancer Accidents Chronic
lower resp.
disease
Diabetes
0
5
10
15
20
25
30
35
Number
of
deaths
(thousands)
Male
Female
% of all deaths
(right axis)
No. of deaths
(left axis)
%
All
deaths
(male
+
female)
National Center for Health Statistics, 2004
Data for 2002
Substantial residual cardiovascular
risk in statin-treated patients
Placebo
Statin
Year of follow-up
%
patients
0 1 2 3 4 5 6
10
20
30
0
Risk reduction=24%
(p<0.0001)
The MRC/BHF Heart Protection Study
Heart Protection Study Collaborative Group, 2002
19.8% of statin-treated
patients had a major
cardiovascular event
by 5 years
Abdominal obesity has reached epidemic
proportions worldwide
Men (%) Women (%) Total (%)
•US1 36.9 55.1 46.0
•South Europe2 33.2 43.8 38.5
•South Korea3 21.0 42.4 32.5
•Australia4 26.8 34.1 30.5
•South Africa5 9.2 42.0 27.3
•North Europe2 22.8 25.9 24.4
Prevalence of abdominal obesity by region
1. Ford ES et al, 2003; 2 Haftenberger M et al, 2002;
3. Kim MH et al 2004; 4. Cameron AJ et al, 2003;
5. Puoane T et al, 2002
Targeting Cardiometaboilc Risk
Defining cardiometabolic Risk
• What is Abdominal Obesity ?
• Can be defined by Waist Circumference;
ATP- III IDF
Male:
> 102 Cm. (> 42 Inch )
Female :
> 88 Cm. (> 35 Inch )
Male :
> 94 Cm. ( > 37 Inch )
Female :
> 80 Cm. ( > 31.5 Inch )
Fat Topography In Type 2
Diabetic Subjects
Intramuscular
Intrahepatic
Subcutaneous
Intra-
abdominal
FFA*
TNF-alpha*
Leptin*
IL-6 (CRP)*
Tissue Factor*
PAI-1*
Angiotensinogen*
Patients with abdominal obesity often present with one or more
additional cardiovascular risk factors (NCEP ATP III criteria)
Abdominal obesity is linked to multiple
cardiometabolic risk factors
National Cholesterol Education Panel/
Adult Treatment Panel III, 2002
Cardiovascular risk factor Parameters
Increased waist circumference Men ≥102 cm (40 in)
Women ≥88 cm (35 in)
Elevated LDL- Cholesterol
Elevated triglycerides
> 2.6 mmol/L (> 70 mg/d )
1.7 mmol/L (150 mg/dL)
Low HDL- Cholesterol Men <1.03 mmol/L (<40 mg/dL)
Women <1.30 mmol/L (<50 mg/dL)
Hypertension BP 130/80 mm Hg
Elevated fasting glucose 6.1 mmol/L (110 mg/dL)
HDL: high-density lipoprotein; BP: blood pressure
Targeting Cardiometaboilc Risk
Defining cardiometabolic Risk
86% At least 1 additional CM risk factor
24% 2 or more additional CM risk factors
Abdominal obesity and increased risk of
cardiovascular events
Dagenais GR et al, 2005
Adjusted
relative
risk
1 1 1
1.17 1.16 1.14
1.29 1.27
1.35
0.8
1
1.2
1.4
CVD death MI All-cause deaths
Tertile 1
Tertile 2
Tertile 3
Men Women
<95
95–103
>103
<87
87–98
>98
Waist
circumference (cm):
The HOPE study
Adjusted for BMI, age, smoking, sex, CVD disease, DM, HDL-cholesterol, total-C;
CVD: cardiovascular disease; MI: myocardial infarction; BMI: body mass index;
DM: diabetes mellitus; HDL: high-density lipoprotein cholesterol
Abdominal obesity increases the risk of
developing type 2 diabetes
<71 71–75.9 76–81 81.1–86 86.1–91 91.1–96.3 >96.3
24
20
16
12
8
4
0
Relative
risk
Waist circumference (cm)
Carey VJ et al, 1997
Abdominal obesity is linked to an
increased risk of coronary heart disease
Waist circumference has been shown to be independently
associated with increased age-adjusted risk of CHD, even after
adjusting for BMI and other cardiovascular risk factors
0.0
0.5
1.0
1.5
2.0
2.5
3.0
<69.8 69.8<74.2 74.2<79.2 79.2<86.3 86.3<139.7
1.27
2.06
2.31
2.44
p for trend = 0.007
Relative
risk
Quintiles of waist circumference (cm)
Rexrode KM et al, 1998
CHD: coronary heart disease; BMI: body mass index
Diabetes in the new millennium
Interdisciplinary problem
Diabetes
Diabetes in the new millennium
Interdisciplinary problem
OBESITY
Diabetes in the new millennium
Interdisciplinary problem
DIAB
ESITY
Targeting
Cardiometabolic Risk
Linked Metabolic Abnormalities:
• Impaired glucose handling/ insulin
resistance
• Atherogenic dyslipidemia
• Endothelial dysfunction
• Prothrombotic state
• Hemodynamic changes
• Proinflammatory state
• Excess ovarian testosterone production
• Sleep-disordered breathing
Resulting Clinical Conditions:
• Type 2 diabetes
• Essential hypertension
• Polycystic ovary syndrome (PCOS)
• Nonalcoholic fatty liver disease
• Sleep apnea
• Cardiovascular Disease (MI, PVD, Stroke)
• Cancer (Breast, Prostate, Colorectal,
Liver)
Multiple Risk Factor Management
• Obesity
• Glucose Intolerance
• Insulin Resistance
• Lipid Disorders
• Hypertension
• Goals: Minimize Risk of Type 2
Diabetes and Cardiovascular Disease
Glucose Abnormalities:
• IDF:
– FPG >100 mg/dL (5.6 mmol. L) or previously
diagnosed type 2 diabetes
• WHO:
– Presence of diabetes, IGT, IFG, insulin resistance
• ATP III:
– FBS >110 mg/dL, <126 mg/dL (6.1-7.1 mmol/L )
– (ADA: FBS >100 mg/dL [ 5.6 mmol/L ])
Hypertension:
• IDF:
– BP >130/85 or on Rx for previously
diagnosed hypertension
• WHO:
– BP >140/90
• NCEP ATP III:
– BP >130/80
Dyslipidemia:
• IDF:
– Triglycerides - >150mg/dL (1.7 mmol /L)
– HDL - <40 mg/dL (men), <50 mg/dL
(women)
• WHO:
– Triglycerides - >150 mg/dL (1.7 mmol/L)
– HDL - <35 mg/dL (men), >39 mg/dL)
women
• ATP III:
– Same as IDF
Screening/Public Health Approach
• Public Education
• Screening for at risk individuals:
– Blood Sugar/ HbA1c
– Lipids
– Blood pressure
– Tobacco use
– Body habitus
– Family history
Life-Style Modification: Is it Important?
• Exercise
– Improves CV fitness, weight control, sensitivity
to insulin, reduces incidence of diabetes
• Weight loss
– Improves lipids, insulin sensitivity, BP levels,
reduces incidence of diabetes
• Goals:
Brisk walking - 30 min./day
10% reduction in body wt.
Smoking Cessation / Avoidance:
• A risk factor for development in children and adults
• Both passive and active exposure harmful
• A major risk factor for:
– insulin resistance and metabolic syndrome
– macrovascular disease (PVD, MI, Stroke)
– microvascular complications of diabetes
– pulmonary disease, etc.
Diabetes Control - How Important?
• For every 1% rise in Hb A1c there is an 18% rise in risk
of cardiovascular events & a 28% increase in peripheral
arterial disease
• Evidence is accumulating to show that tight blood sugar
control in both Type 1 and Type 2 diabetes reduces risk
of CVD
• Goals:
• FBS - premeal <110,
• postmeal <180.
• HbA1c <7%
Overcome Insulin Resistance/ Diabetes:
• Insulin Sensitizers:
– Biguanides - metformin
– PPAR α, γ & δ agonists – Glitazones, Gltazars
Rosiglitazon, Pioglitazon
– Can be used in combination
• Insulin Secretagogues:
– Sulfonylurea - glipizide, glyburide,
glimeparide, glibenclamide
– Meglitinides - repaglanide, netiglamide
BP Control - How Important?
• MRFIT and Framingham Heart Studies:
– Conclusively proved the increased risk of
CVD with long-term sustained hypertension
– Demonstrated a 10 year risk of cardiovascular
disease in treated patients vs non-treated
patients to be 0.40.
– 40% reduction in stroke with control of HTN
• Precedes literature on Metabolic Syndrome
• Goal: BP.<130/80
Lipid Control - How Important?
• Multiple major studies show 24 - 37%
reductions in cardiovascular disease risk with
use of statins and fibrates in the control of
hyperlipidemia.
• Goals: LDL <100 mg/dL (<3.0 mmol /l)
(high risk <70 mg/dL- <2.6 mmol/L)
TG <150 mg% (<1.7 mmol /l)
HDL >40 mg% (>1.1 mmol /l)
Medications:
• Hypertension:
– ACE inhibitors, ARBs
– Others - thiazides, calcium channel
blockers, beta blockers, alpha blockers
– Central acting Alfa agonist : Moxolidin
• Dylipidemia:
– Statins, Fibrates, Niacin
• Platelet inhibitors:
– ASA, clopidogrel
A Critical Look at the Metabolic Syndrome
Is it a Syndrome?*
• “…too much clinically important information
is missing to warrant its designations as a
syndrome.”
• Unclear pathogenesis, Insulin resistance
may not underlie all factors, & is not a
consistent finding in some definitions.
• CVD risks associated with metabolic
syndrome has not shown to be greater than
the sum of it’s individual components.
*ADA & EASD
A Critical Look at the Metabolic Syndrome
• “Until much needed research is completed,
clinicians should evaluate and treat all CVD
risk factors without regard to whether a
patient meets the criteria for diagnosis of
the ‘metabolic syndrome’.”
• The advice remains to treat individual risk
factors when present & to prescribe
therapeutic lifestyle changes & weight
management for obese patients with
multiple risk factors.
Individual metabolic abnormalities among Qatari
population according to gender (Musallam et al 08)
Men (n = 405) Women (n=412)
Variable n(%) n(%) p-Value
ATP III
Abdominal obesity 227(56.0) 308(74.8) <0.001
Hypertension 143(35.3) 156(37.9) 0.448
Diabetes 77(19.0) 107(26.0) 0.017
Hypertriglyceridemia 113(27.9) 83(20.1) 0.009
Low HDL 95(23.5) 121(29.4) 0.055
Individual metabolic abnormalities among Qatari
population according to gender
Men (n = 405) Women (n=412)
Variable n(%) n(%) p-Value
None 88(21.7) 74(18.0) –
One 103(25.4) 100(24.3) 0.033
Two 125(30.9) 111(26.9) –
Three or more 89(22.0) 127(30.8) –
No of components of ATP III
Multivariate logistic regression analysis of
factors associated with Metabolic Syndrome
according to (ATP III criteria)
Odds ratio 95% CI p-Value
Age 1.07 1.05–1.09 <0.001
Female gender 1.86 1.30–2.67 0.001
Body Mass Index 1.05 1.02–1.07 <0.001
Fam his of DM 1.66 1.12–2.44 0.011
Smoking 3.27 1.63–6.55 0.001
Prevalence of MeS in different Countries
Prevalence
(%)
Sample
Year
Country
23
542
2003
Arab Americans
21
1419
2001
Oman
36
1121
2002
Jordan
20.8
2250
2004
Saudi Arabia
17*
1998
Palestine
27.6
817
2007
Qatar
33.4*
1637
2004
Turkey
33.7
10368
?
Iran
* Crude rates Mussallam et al. Int J Food Safety and PH 2008
Prevalence of MeS in different Countries
Prevalence
(%)
Sample
Year
Country
34*
2002
2005
USA
21
1419
2005
Greece
15.3
4060
2005
South Australia
6.8
40,698
2001
S. Korea
10.2*
2776
2000
China
33.4*
1637
2004
Turkey
41*
475
2003
Chennai India
27.6
817
2001
Qatar
* Crude rates Mussallam et al. Int J Food Safety and PH 2008
Determinants and dynamics of the CVD
Epidemic in the developing Countries
Data from South Asian Immigrant studies
• Excess, early, and extensive CHD in persons of
South Asian origin
• The excess mortality has not been fully explained
by the major conventional risk factors.
• Diabetes mellitus and impaired glucose tolerance
highly prevalent. (Reddy KS, circ 1998).
• Central obesity, ↑triglycerides, ↓HDL with or
without glucose intolerance, characterize a
phenotype.
• genetic factors predispose to ↑lipoprotein(a)
levels, the central obesity/glucose
intolerance/dyslipidemia complex collectively
labeled as the “metabolic syndrome”
Determinants and dynamics of the CVD
epidemic in the developing countries
Other Possible factors
• Relationship between early life characteristics and
susceptibility to NCD in adult hood ( Barker’s
hypothesis) (Baker DJP,BMJ,1993)
– Low birth weight associated with increased CVD
– Poor infant growth and CVD relation
• Genetic–environment interactions
(Enas EA, Clin. Cardiol. 1995; 18: 131–5)
- Amplification of expression of risk to some
environmental changes esp. South Asian population)
- Thrifty gene (e.g. in South Asians)
CVD epidemic in developing &
developed countries. Are they same?
• Urban populations have higher levels of CVD risk
factors related to diet and physical activity
(overweight, hypertension, dyslipidaemia and diabetes)
• Tobacco consumption is more widely prevalent in rural
population
• The social gradient will reverse as the epidemics
mature.
• The poor will become progressively vulnerable to the
ravages of these diseases and will have little access
to the expensive and technology-curative care.
• The scarce societal resources to the treatment of
these disorders dangerously depletes the resources
available for the ‘unfinished agenda’ of infectious and
nutritional disorders that almost exclusively afflict
the poor
Burden of CVD in Pakistan
Coronary heart disease
Mortality statistics
• Specific mortality data ideal for making
comparisons with other countries are not
available
• Inadequate and inappropriate death certification,
and multiple concurrent causes of death
Central obesity: a driving force for
cardiovascular disease & diabetes
“Balzac” by Rodin
Front
Back
Developing A New Definition of
the Metabolic Syndrome: IDF
Objectives
Needs:
• To identify individuals at high risk of developing
cardiovascular disease (and diabetes)
• To be useful for clinicians
• To be useful for international comparisons
The new IDF definition focusses on abdominal obesity
rather than insulin resistance
International Diabetes Federation
(IDF) Consensus Definition 2005
Why people physically inactive?
• Lack of awareness regarding the of physical
activity for health fitness and prevention of
diseases
• Social values and traditions regarding
physical exercise (women, restriction).
• Non-availability public places suitable for
physical activity (walking and cycling path,
gymnasium).
• Modernization of life that reduce physical
activity (sedentary life, TV, Computers, tel,
cars).
Insulin Resistance: Associated
Conditions
Prevalence of the Metabolic Syndrome
Among US Adults NHANES 1988-1994
Prevalence
(%)
0
5
10
15
20
25
30
35
40
45
20-29 30-39 40-49 50-59 60-69 > 70
Men
Women
Age (years)
Ford E et al. JAMA. 2002(287):356.
1999-2002 Prevalence by IDF vs. NCEP Definitions (Ford ES,
Diabetes Care 2005; 28: 2745-9) (unadjusted, age 20+)
NCEP : 33.7% in men and 35.4% in women
IDF: 39.9% in men and 38.1% in women
Prevention of CVD
• There is an urgent need to establish
appropriate research studies, increase
awareness of the CVD burden, and develop
preventive strategies.
• Prevention and treatment strategies that have
been proven to be effective in developed
countries should be adapted for developing
countries.
• Prevention is the best option as an approach
to reduce CVD burden.
• Do we know enough to prevent this CVD
Epidemic in the first place.
The new IDF definition focusses on
abdominal obesity rather than insulin
resistance
International Diabetes Federation
(IDF) Consensus Definition 2005
International Diabetes Federation (IDF)
Consensus Definition 2005
Central Obesity
Waist circumference – ethnicity specific*
– for Europids: Male > 94 cm
Female > 80 cm
plus any two of the following:
Raised triglycerides > 150 mg/dL (1.7 mmol/L)
or specific treatment for this lipid abnormality
Reduced HDL cholesterol < 40 mg/dL (1.03 mmol/L) in males
< 50 mg/dL (1.29 mmol/L) in females
or specific treatment for this lipid abnormality
Raised blood pressure Systolic : > 130 mmHg or
Diastolic: > 85 mmHg or
Treatment of previously diagnosed hypertension
Raised fasting plasma
glucose
Fasting plasma glucose > 100 mg/dL (5.6 mmol/L) or
Previously diagnosed type 2 diabetes
If above 5.6 mmol/L or 100 mg/dL, OGTT is strongly
recommended but is not necessary to define presence of the
syndrome.
Treatment of Metabolic Syndrome: 2005
Aspirin
Diet,
Exercise,
Lifestyle
change
Stop
smoking
CB1 Receptor
Blocker
Oral hypoglycaemics
Antihypertensives
Statins &
Fibrates
Insulin
ACEI &/or A2 receptor
blockers
Primary management for the Metabolic Syndrome
is healthy lifestyle promotion. This includes:
• moderate calorie restriction (to achieve a 5-10%
loss of body weight in the first year)
• moderate increases in physical activity
• change dietary composition to reduce saturated
fat and total intake, increase fibre and, if
appropriate, reduce salt intake.
Recommendations for treatment
• Appropriate & aggressive therapy is essential
for reducing patient risk of cardiovascular
disease
• Lifestyle measures should be the first action
• Pharmacotherapy should have beneficial effects
on
– Glucose intolerance/diabetes
– Obesity
– Hypertension
– Dyslipidaemia
• Ideally, treatment should address all of the
components of the syndrome and not the
individual components
Management of the Metabolic Syndrome
Summary: new IDF definition for the
Metabolic Syndrome
The new IDF definition addresses both clinical
and research needs:
•
provides a simple entry point for primary care
physicians to diagnose the Metabolic Syndrome
•
providing an accessible, diagnostic tool
suitable for worldwide use, taking into account
ethnic differences
•
establishing a comprehensive ‘platinum
standard’ list of additional criteria that should
be included in epidemiological studies and
other research into the Metabolic Syndrome
Lifestyle modification
• Diet
• Exercise
• Weight loss
• Smoking
cessation
If a 1% reduction in HbA1c
is achieved, you could
expect a reduction in risk
of:
• 21% for any diabetes-
related endpoint
• 37% for microvascular
complications
• 14% for myocardial
infarction
However, compliance is poor and most patients will require
oral pharmacotherapy within a few years of diagnosis
Stratton IM et al. BMJ 2000; 321: 405–412.

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Cardiometabolic Syndrome-Nabil Sulaiman(1).ppt

  • 1. Cardiometabolic Syndrome Dr. Nabil Sulaiman HOD Family and Community Medicine, Sharjah University and University of Melbourne & Dr Dhafir A. Mahmood Consultant Endocrinologist Al- Qassimi & Al-Kuwait Hospital Sharjah
  • 2. Agenda • History & Definition • Clustering component of Metabolic Syndrome • Cardiovascular disease worldwide • Global cardiometabolic risks • Abdominal obesity prevalence ( National & International ) • Intra Abdominal Adiposity & associated risks • Targeting Cardiometabolic Risk factors • Multiple Risk Factor management • A Critical Look at the Metabolic Syndrome
  • 3. Metabolic Syndrome (History) • 1923 - Kylin first to describe the clustering of hypertension, hyperglycemia, hyperuricemia • 1936 - Himsworth first reported Insulin insensitivity in diabetics • 1965 - Yalow and Berson developed insulin assay and correlated insulin levels & glucose lowering effects in resistant and non-resistant individuals
  • 4. Metabolic Syndrome History (cont.) • 1988 - Reaven in his Banting lecture at the ADA meeting coined the term Syndrome X and brought into focus the clustering of features of Metabolic Syndrome • Reaven now prefers the name, Insulin- Resistance Syndrome - feels insulin resistance is the common denominator for Metabolic Syndrome • Literature now extensive
  • 5. Other Names Used: • Syndrome X • Cardiometabolic Syndrome • Cardiovascular Dysmetabolic Syndrome • Insulin-Resistance Syndrome • Metabolic Syndrome • Beer Belly Syndrome • Reaven’s Syndrome • etc.
  • 6. Clustering of Components: • Hypertension: BP. > 140/90 • Dyslipidemia: TG > 150 mg/ dL ( 1.7 mmol/L ) HDL- C < 35 mg/ dL (0.9 mmol/L) • Obesity (central): BMI > 30 kg/M2 Waist girth > 94 cm (37 inch) Waist/Hip ratio > 0.9 • Impaired Glucose Handling: IR , IGT or DM FPG > 110 mg/dL (6.1mmol/L) 2hr.PG >200 mg/dL(11.1mmol/L) • Microalbuninuria (WHO)
  • 7. Necessary Criteria to Make Diagnosis • WHO: Impaired G handling + 2 other criteria. –Also requires microalbuminuria - Albumen/ creatinine ratio >30 mg/gm creatinine • IDF: –Require central obesity plus two of the other abnormalities • NCEP/ATP III: –Require three or more of the five criteria
  • 8. What is cardiometabolic risk?* • Global cardiometabolic risk represents the overall risk of developing type 2 diabetes and/or cardiovascular disease (including MI and stroke), which is due to a cluster of modifiable risk factors/markers • These include classical risk factors such as smoking, high LDL, hypertension, elevated blood glucose and emerging risk factors closely related to abdominal obesity (especially intra-abdominal adiposity), such as insulin resistance, low HDL, high triglycerides and inflammatory markers • Cardiometabolic risk is based on the concept of risk continuum * working definition MI: myocardial infarction; LDL: low-density lipoprotein; HDL: high-density lipoprotein
  • 9. Global cardiometabolic risk* Gelfand EV et al, 2006; Vasudevan AR et al, 2005 * working definition
  • 10. Despite therapeutic advances, CV disease remains the leading cause of death (USA) 0 100 200 300 400 500 Heart disease and stroke Cancer Accidents Chronic lower resp. disease Diabetes 0 5 10 15 20 25 30 35 Number of deaths (thousands) Male Female % of all deaths (right axis) No. of deaths (left axis) % All deaths (male + female) National Center for Health Statistics, 2004 Data for 2002
  • 11. Substantial residual cardiovascular risk in statin-treated patients Placebo Statin Year of follow-up % patients 0 1 2 3 4 5 6 10 20 30 0 Risk reduction=24% (p<0.0001) The MRC/BHF Heart Protection Study Heart Protection Study Collaborative Group, 2002 19.8% of statin-treated patients had a major cardiovascular event by 5 years
  • 12. Abdominal obesity has reached epidemic proportions worldwide Men (%) Women (%) Total (%) •US1 36.9 55.1 46.0 •South Europe2 33.2 43.8 38.5 •South Korea3 21.0 42.4 32.5 •Australia4 26.8 34.1 30.5 •South Africa5 9.2 42.0 27.3 •North Europe2 22.8 25.9 24.4 Prevalence of abdominal obesity by region 1. Ford ES et al, 2003; 2 Haftenberger M et al, 2002; 3. Kim MH et al 2004; 4. Cameron AJ et al, 2003; 5. Puoane T et al, 2002
  • 13. Targeting Cardiometaboilc Risk Defining cardiometabolic Risk • What is Abdominal Obesity ? • Can be defined by Waist Circumference; ATP- III IDF Male: > 102 Cm. (> 42 Inch ) Female : > 88 Cm. (> 35 Inch ) Male : > 94 Cm. ( > 37 Inch ) Female : > 80 Cm. ( > 31.5 Inch )
  • 14. Fat Topography In Type 2 Diabetic Subjects Intramuscular Intrahepatic Subcutaneous Intra- abdominal FFA* TNF-alpha* Leptin* IL-6 (CRP)* Tissue Factor* PAI-1* Angiotensinogen*
  • 15. Patients with abdominal obesity often present with one or more additional cardiovascular risk factors (NCEP ATP III criteria) Abdominal obesity is linked to multiple cardiometabolic risk factors National Cholesterol Education Panel/ Adult Treatment Panel III, 2002 Cardiovascular risk factor Parameters Increased waist circumference Men ≥102 cm (40 in) Women ≥88 cm (35 in) Elevated LDL- Cholesterol Elevated triglycerides > 2.6 mmol/L (> 70 mg/d ) 1.7 mmol/L (150 mg/dL) Low HDL- Cholesterol Men <1.03 mmol/L (<40 mg/dL) Women <1.30 mmol/L (<50 mg/dL) Hypertension BP 130/80 mm Hg Elevated fasting glucose 6.1 mmol/L (110 mg/dL) HDL: high-density lipoprotein; BP: blood pressure
  • 16. Targeting Cardiometaboilc Risk Defining cardiometabolic Risk 86% At least 1 additional CM risk factor 24% 2 or more additional CM risk factors
  • 17. Abdominal obesity and increased risk of cardiovascular events Dagenais GR et al, 2005 Adjusted relative risk 1 1 1 1.17 1.16 1.14 1.29 1.27 1.35 0.8 1 1.2 1.4 CVD death MI All-cause deaths Tertile 1 Tertile 2 Tertile 3 Men Women <95 95–103 >103 <87 87–98 >98 Waist circumference (cm): The HOPE study Adjusted for BMI, age, smoking, sex, CVD disease, DM, HDL-cholesterol, total-C; CVD: cardiovascular disease; MI: myocardial infarction; BMI: body mass index; DM: diabetes mellitus; HDL: high-density lipoprotein cholesterol
  • 18. Abdominal obesity increases the risk of developing type 2 diabetes <71 71–75.9 76–81 81.1–86 86.1–91 91.1–96.3 >96.3 24 20 16 12 8 4 0 Relative risk Waist circumference (cm) Carey VJ et al, 1997
  • 19. Abdominal obesity is linked to an increased risk of coronary heart disease Waist circumference has been shown to be independently associated with increased age-adjusted risk of CHD, even after adjusting for BMI and other cardiovascular risk factors 0.0 0.5 1.0 1.5 2.0 2.5 3.0 <69.8 69.8<74.2 74.2<79.2 79.2<86.3 86.3<139.7 1.27 2.06 2.31 2.44 p for trend = 0.007 Relative risk Quintiles of waist circumference (cm) Rexrode KM et al, 1998 CHD: coronary heart disease; BMI: body mass index
  • 20. Diabetes in the new millennium Interdisciplinary problem Diabetes
  • 21. Diabetes in the new millennium Interdisciplinary problem OBESITY
  • 22. Diabetes in the new millennium Interdisciplinary problem DIAB ESITY
  • 24. Linked Metabolic Abnormalities: • Impaired glucose handling/ insulin resistance • Atherogenic dyslipidemia • Endothelial dysfunction • Prothrombotic state • Hemodynamic changes • Proinflammatory state • Excess ovarian testosterone production • Sleep-disordered breathing
  • 25. Resulting Clinical Conditions: • Type 2 diabetes • Essential hypertension • Polycystic ovary syndrome (PCOS) • Nonalcoholic fatty liver disease • Sleep apnea • Cardiovascular Disease (MI, PVD, Stroke) • Cancer (Breast, Prostate, Colorectal, Liver)
  • 26. Multiple Risk Factor Management • Obesity • Glucose Intolerance • Insulin Resistance • Lipid Disorders • Hypertension • Goals: Minimize Risk of Type 2 Diabetes and Cardiovascular Disease
  • 27. Glucose Abnormalities: • IDF: – FPG >100 mg/dL (5.6 mmol. L) or previously diagnosed type 2 diabetes • WHO: – Presence of diabetes, IGT, IFG, insulin resistance • ATP III: – FBS >110 mg/dL, <126 mg/dL (6.1-7.1 mmol/L ) – (ADA: FBS >100 mg/dL [ 5.6 mmol/L ])
  • 28. Hypertension: • IDF: – BP >130/85 or on Rx for previously diagnosed hypertension • WHO: – BP >140/90 • NCEP ATP III: – BP >130/80
  • 29. Dyslipidemia: • IDF: – Triglycerides - >150mg/dL (1.7 mmol /L) – HDL - <40 mg/dL (men), <50 mg/dL (women) • WHO: – Triglycerides - >150 mg/dL (1.7 mmol/L) – HDL - <35 mg/dL (men), >39 mg/dL) women • ATP III: – Same as IDF
  • 30. Screening/Public Health Approach • Public Education • Screening for at risk individuals: – Blood Sugar/ HbA1c – Lipids – Blood pressure – Tobacco use – Body habitus – Family history
  • 31. Life-Style Modification: Is it Important? • Exercise – Improves CV fitness, weight control, sensitivity to insulin, reduces incidence of diabetes • Weight loss – Improves lipids, insulin sensitivity, BP levels, reduces incidence of diabetes • Goals: Brisk walking - 30 min./day 10% reduction in body wt.
  • 32. Smoking Cessation / Avoidance: • A risk factor for development in children and adults • Both passive and active exposure harmful • A major risk factor for: – insulin resistance and metabolic syndrome – macrovascular disease (PVD, MI, Stroke) – microvascular complications of diabetes – pulmonary disease, etc.
  • 33. Diabetes Control - How Important? • For every 1% rise in Hb A1c there is an 18% rise in risk of cardiovascular events & a 28% increase in peripheral arterial disease • Evidence is accumulating to show that tight blood sugar control in both Type 1 and Type 2 diabetes reduces risk of CVD • Goals: • FBS - premeal <110, • postmeal <180. • HbA1c <7%
  • 34. Overcome Insulin Resistance/ Diabetes: • Insulin Sensitizers: – Biguanides - metformin – PPAR α, γ & δ agonists – Glitazones, Gltazars Rosiglitazon, Pioglitazon – Can be used in combination • Insulin Secretagogues: – Sulfonylurea - glipizide, glyburide, glimeparide, glibenclamide – Meglitinides - repaglanide, netiglamide
  • 35. BP Control - How Important? • MRFIT and Framingham Heart Studies: – Conclusively proved the increased risk of CVD with long-term sustained hypertension – Demonstrated a 10 year risk of cardiovascular disease in treated patients vs non-treated patients to be 0.40. – 40% reduction in stroke with control of HTN • Precedes literature on Metabolic Syndrome • Goal: BP.<130/80
  • 36. Lipid Control - How Important? • Multiple major studies show 24 - 37% reductions in cardiovascular disease risk with use of statins and fibrates in the control of hyperlipidemia. • Goals: LDL <100 mg/dL (<3.0 mmol /l) (high risk <70 mg/dL- <2.6 mmol/L) TG <150 mg% (<1.7 mmol /l) HDL >40 mg% (>1.1 mmol /l)
  • 37. Medications: • Hypertension: – ACE inhibitors, ARBs – Others - thiazides, calcium channel blockers, beta blockers, alpha blockers – Central acting Alfa agonist : Moxolidin • Dylipidemia: – Statins, Fibrates, Niacin • Platelet inhibitors: – ASA, clopidogrel
  • 38. A Critical Look at the Metabolic Syndrome Is it a Syndrome?* • “…too much clinically important information is missing to warrant its designations as a syndrome.” • Unclear pathogenesis, Insulin resistance may not underlie all factors, & is not a consistent finding in some definitions. • CVD risks associated with metabolic syndrome has not shown to be greater than the sum of it’s individual components. *ADA & EASD
  • 39. A Critical Look at the Metabolic Syndrome • “Until much needed research is completed, clinicians should evaluate and treat all CVD risk factors without regard to whether a patient meets the criteria for diagnosis of the ‘metabolic syndrome’.” • The advice remains to treat individual risk factors when present & to prescribe therapeutic lifestyle changes & weight management for obese patients with multiple risk factors.
  • 40. Individual metabolic abnormalities among Qatari population according to gender (Musallam et al 08) Men (n = 405) Women (n=412) Variable n(%) n(%) p-Value ATP III Abdominal obesity 227(56.0) 308(74.8) <0.001 Hypertension 143(35.3) 156(37.9) 0.448 Diabetes 77(19.0) 107(26.0) 0.017 Hypertriglyceridemia 113(27.9) 83(20.1) 0.009 Low HDL 95(23.5) 121(29.4) 0.055
  • 41. Individual metabolic abnormalities among Qatari population according to gender Men (n = 405) Women (n=412) Variable n(%) n(%) p-Value None 88(21.7) 74(18.0) – One 103(25.4) 100(24.3) 0.033 Two 125(30.9) 111(26.9) – Three or more 89(22.0) 127(30.8) – No of components of ATP III
  • 42. Multivariate logistic regression analysis of factors associated with Metabolic Syndrome according to (ATP III criteria) Odds ratio 95% CI p-Value Age 1.07 1.05–1.09 <0.001 Female gender 1.86 1.30–2.67 0.001 Body Mass Index 1.05 1.02–1.07 <0.001 Fam his of DM 1.66 1.12–2.44 0.011 Smoking 3.27 1.63–6.55 0.001
  • 43. Prevalence of MeS in different Countries Prevalence (%) Sample Year Country 23 542 2003 Arab Americans 21 1419 2001 Oman 36 1121 2002 Jordan 20.8 2250 2004 Saudi Arabia 17* 1998 Palestine 27.6 817 2007 Qatar 33.4* 1637 2004 Turkey 33.7 10368 ? Iran * Crude rates Mussallam et al. Int J Food Safety and PH 2008
  • 44. Prevalence of MeS in different Countries Prevalence (%) Sample Year Country 34* 2002 2005 USA 21 1419 2005 Greece 15.3 4060 2005 South Australia 6.8 40,698 2001 S. Korea 10.2* 2776 2000 China 33.4* 1637 2004 Turkey 41* 475 2003 Chennai India 27.6 817 2001 Qatar * Crude rates Mussallam et al. Int J Food Safety and PH 2008
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  • 49. Determinants and dynamics of the CVD Epidemic in the developing Countries Data from South Asian Immigrant studies • Excess, early, and extensive CHD in persons of South Asian origin • The excess mortality has not been fully explained by the major conventional risk factors. • Diabetes mellitus and impaired glucose tolerance highly prevalent. (Reddy KS, circ 1998). • Central obesity, ↑triglycerides, ↓HDL with or without glucose intolerance, characterize a phenotype. • genetic factors predispose to ↑lipoprotein(a) levels, the central obesity/glucose intolerance/dyslipidemia complex collectively labeled as the “metabolic syndrome”
  • 50. Determinants and dynamics of the CVD epidemic in the developing countries Other Possible factors • Relationship between early life characteristics and susceptibility to NCD in adult hood ( Barker’s hypothesis) (Baker DJP,BMJ,1993) – Low birth weight associated with increased CVD – Poor infant growth and CVD relation • Genetic–environment interactions (Enas EA, Clin. Cardiol. 1995; 18: 131–5) - Amplification of expression of risk to some environmental changes esp. South Asian population) - Thrifty gene (e.g. in South Asians)
  • 51. CVD epidemic in developing & developed countries. Are they same? • Urban populations have higher levels of CVD risk factors related to diet and physical activity (overweight, hypertension, dyslipidaemia and diabetes) • Tobacco consumption is more widely prevalent in rural population • The social gradient will reverse as the epidemics mature. • The poor will become progressively vulnerable to the ravages of these diseases and will have little access to the expensive and technology-curative care. • The scarce societal resources to the treatment of these disorders dangerously depletes the resources available for the ‘unfinished agenda’ of infectious and nutritional disorders that almost exclusively afflict the poor
  • 52. Burden of CVD in Pakistan Coronary heart disease Mortality statistics • Specific mortality data ideal for making comparisons with other countries are not available • Inadequate and inappropriate death certification, and multiple concurrent causes of death
  • 53. Central obesity: a driving force for cardiovascular disease & diabetes “Balzac” by Rodin Front Back
  • 54. Developing A New Definition of the Metabolic Syndrome: IDF Objectives Needs: • To identify individuals at high risk of developing cardiovascular disease (and diabetes) • To be useful for clinicians • To be useful for international comparisons
  • 55. The new IDF definition focusses on abdominal obesity rather than insulin resistance International Diabetes Federation (IDF) Consensus Definition 2005
  • 56. Why people physically inactive? • Lack of awareness regarding the of physical activity for health fitness and prevention of diseases • Social values and traditions regarding physical exercise (women, restriction). • Non-availability public places suitable for physical activity (walking and cycling path, gymnasium). • Modernization of life that reduce physical activity (sedentary life, TV, Computers, tel, cars).
  • 58. Prevalence of the Metabolic Syndrome Among US Adults NHANES 1988-1994 Prevalence (%) 0 5 10 15 20 25 30 35 40 45 20-29 30-39 40-49 50-59 60-69 > 70 Men Women Age (years) Ford E et al. JAMA. 2002(287):356. 1999-2002 Prevalence by IDF vs. NCEP Definitions (Ford ES, Diabetes Care 2005; 28: 2745-9) (unadjusted, age 20+) NCEP : 33.7% in men and 35.4% in women IDF: 39.9% in men and 38.1% in women
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  • 60. Prevention of CVD • There is an urgent need to establish appropriate research studies, increase awareness of the CVD burden, and develop preventive strategies. • Prevention and treatment strategies that have been proven to be effective in developed countries should be adapted for developing countries. • Prevention is the best option as an approach to reduce CVD burden. • Do we know enough to prevent this CVD Epidemic in the first place.
  • 61. The new IDF definition focusses on abdominal obesity rather than insulin resistance International Diabetes Federation (IDF) Consensus Definition 2005
  • 62. International Diabetes Federation (IDF) Consensus Definition 2005 Central Obesity Waist circumference – ethnicity specific* – for Europids: Male > 94 cm Female > 80 cm plus any two of the following: Raised triglycerides > 150 mg/dL (1.7 mmol/L) or specific treatment for this lipid abnormality Reduced HDL cholesterol < 40 mg/dL (1.03 mmol/L) in males < 50 mg/dL (1.29 mmol/L) in females or specific treatment for this lipid abnormality Raised blood pressure Systolic : > 130 mmHg or Diastolic: > 85 mmHg or Treatment of previously diagnosed hypertension Raised fasting plasma glucose Fasting plasma glucose > 100 mg/dL (5.6 mmol/L) or Previously diagnosed type 2 diabetes If above 5.6 mmol/L or 100 mg/dL, OGTT is strongly recommended but is not necessary to define presence of the syndrome.
  • 63. Treatment of Metabolic Syndrome: 2005 Aspirin Diet, Exercise, Lifestyle change Stop smoking CB1 Receptor Blocker Oral hypoglycaemics Antihypertensives Statins & Fibrates Insulin ACEI &/or A2 receptor blockers
  • 64. Primary management for the Metabolic Syndrome is healthy lifestyle promotion. This includes: • moderate calorie restriction (to achieve a 5-10% loss of body weight in the first year) • moderate increases in physical activity • change dietary composition to reduce saturated fat and total intake, increase fibre and, if appropriate, reduce salt intake. Recommendations for treatment
  • 65. • Appropriate & aggressive therapy is essential for reducing patient risk of cardiovascular disease • Lifestyle measures should be the first action • Pharmacotherapy should have beneficial effects on – Glucose intolerance/diabetes – Obesity – Hypertension – Dyslipidaemia • Ideally, treatment should address all of the components of the syndrome and not the individual components Management of the Metabolic Syndrome
  • 66. Summary: new IDF definition for the Metabolic Syndrome The new IDF definition addresses both clinical and research needs: • provides a simple entry point for primary care physicians to diagnose the Metabolic Syndrome • providing an accessible, diagnostic tool suitable for worldwide use, taking into account ethnic differences • establishing a comprehensive ‘platinum standard’ list of additional criteria that should be included in epidemiological studies and other research into the Metabolic Syndrome
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  • 68. Lifestyle modification • Diet • Exercise • Weight loss • Smoking cessation If a 1% reduction in HbA1c is achieved, you could expect a reduction in risk of: • 21% for any diabetes- related endpoint • 37% for microvascular complications • 14% for myocardial infarction However, compliance is poor and most patients will require oral pharmacotherapy within a few years of diagnosis Stratton IM et al. BMJ 2000; 321: 405–412.