ISCHEMIA

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Title: ISCHEMIA

1

ISCHEMIC HEART DISEASE/CORONARY ARTERY DISEASE

Dr.W.C.Lwabby (MMed, MD)Lecturer Int. Med. Dpt
2
Introduction

Ischemic heart disease (IHD)/CORONARY ARTERY
DISEASE(CAD)
Is a condition in which
there is an inadequate supply of blood and
oxygen to a portion of the myocardium.
Occurs when there is an imbalance between
myocardial oxygen supply and demand.
Common cause of myocardial ischemia is
atherosclerotic disease of a coronary artery,
sufficient to cause a regional reduction in
myocardial blood flow.

3
Introduction

Disease of the coronary arteries is almost always
due to
atheroma and its complications, particularly
thrombosis.
Occasionally, the coronary arteries are involved
in other disorders such as
Aortitis
Polyarteritis
Other connective tissue disorders.

4
Introduction

Patients with IHD fall into two large groups
Chronic CAD (stable angina)
Acute coronary syndromes (ACSs)
Is a term that encompasses both unstable angina
and myocardial infarction (MI).

5
Anatomy of the coronary vessels

Two main coronary arteries, branches of ascending
aorta.
Left coronary arteries
supply LA, LV and the anterior wall of the RV.
Right coronary arteries
supply RA, RV as well as the SA node.

6
Anatomy of coronary arteries
7
EPIDEMIOLOGY

gt 60 of the global burden of IHD occurs in
Developing countries.
It increases with age.
Men gt women, but CAD is the leading cause of
death in both men and women

8
RISK FACTORS OF IHD

Generally include
Hypertension
Elevated LDL /VLDL cholesterol
Reduced HDL cholesterol
Oxidant stress caused by cigarette smoking
Excess angiotensin II
Obesity
Insulin resistance
Diabetes mellitus

9
PATHOPHYSIOLOGY

The underlying pathophysiological mechanisms for
IHD begin with the process of atherosclerosis,
In ACS
Atherosclerosis can be described as a low-grade
inflammatory state of the intima of medium-sized
arteries.
It develops and progresses for decades prior to
the acute event.
This is accelerated by the risk factors, such as
Hypertension, Hyperlipidemia, smoking,
diabetes, and genetics.

10
PATHOPHYSIOLOGY..

This slow progression leads to the gradual
thickening of the intima,
which may over time narrow the lumen of the
artery to various degrees.

11
Stable angina

Angina pectoris
Is the symptom complex caused by transient
myocardial ischaemia
It constitutes a clinical syndrome rather than a
disease.
It may occur whenever there is an imbalance
between myocardial oxygen supply and demand.
Coronary atheroma is by far the most common
cause.
Coronary perfusion is impaired by fixed or stable
atheroma of the coronary arteries.

12
Clinical features

Stable angina is characterized by
Central chest pain (retro-sternal chest pain)
Discomfort
Radiating to left( right) shoulder/arm/ neck/jaw
Precipitated by exertion or other forms of stress
Promptly relieved by rest or Nitrates.
Brief duration, lasting lt10-15 min
Associated with breathlessness, diaphoresis,
nausea, anxiety

13
Clinical features

Physical examination
Is frequently unremarkable.
Should include a careful search for evidence of
Valve heart disease (particularly aortic)
Important risk factors (e.g. hypertension,
diabetes mellitus)
Left ventricular dysfunction (cardiomegaly,
gallop rhythm)
Other manifestations of arterial disease (carotid
bruits, peripheral vascular disease)
Unrelated conditions that may exacerbate angina
(anaemia, thyrotoxicosis).

14
Diagnosis

The history is the most important factor in
making the diagnosis.
Investigations
The ECG may show evidence of previous MI but is
often normal
Coronary arteriography
This provides detailed anatomical information
about the extent and nature of coronary artery
disease.

15
Treatment

Specific Treatment
Antiplatelet therapy
Aspirin -Low-dose (75 mg)
Reduces the risk of adverse events such as MI.
Clopidogrel (75 mg daily)
Is an equally effective antiplatelet agent.
Can be prescribed if aspirin causes troublesome
dyspepsia.

Anti-anginal drug treatment
Five groups of drug are used to relieve or
prevent the symptoms of angina
Nitrates
ß-blockers
Calcium antagonists
Potassium channel activators
an If channel antagonist.

Nitrates
Act directly on vascular smooth muscle to produce
venous and arteriolar dilatation.
Their beneficial effects are due to
Reduction in myocardial oxygen demand (lower
preload and afterload)
Increase in myocardial oxygen supply (coronary
vasodilatation).
Sublingual glyceryl trinitrate (GTN)
Administered from
a metered-dose aerosol (400 µg per spray) or
as a tablet (300 or 500 µg), will relieve an
attack of angina in 23 minutes.
Side-effects include headache, hypotension,
syncope.
Other nitrates (isosorbide dinitrate , isosorbide
mononitrate )

Beta-blockers
These lower myocardial oxygen demand by
reducing heart rate, BP and myocardial
contractility
They may provoke bronchospasm in patients with
asthma.
Non- cardioselective ß-blockers may aggravate
coronary vasospasm by
blocking the coronary artery ß2adrenoceptors.
so a once-daily cardioselective preparation is
used (e.g. metoprolol 50200 mg daily, bisoprolol
515 mg daily).

Calcium channel antagonists
They lower myocardial oxygen demand by
reducing BP and myocardial contractility.
Dihydropyridine calcium antagonists, (nifedipine
and nicardipine), often cause a reflex
tachycardia.
This may be counterproductive and it is best to
use them in combination with a ß-blocker.
Verapamil and diltiazem
Are suitable for patients who are not receiving
a ß-blocker (e.g. those with airways obstruction)
because
Slow SA node firing
Inhibit conduction through the AV node
Tend to cause a bradycardia.

Invasive treatment
Percutaneous coronary intervention (PCI)
Is performed by passing a fine guidewire across a
coronary stenosis under radiographic control.
using it to position a balloon, which is then
inflated to dilate the stenosis.
Coronary artery bypass grafting
The internal mammary arteries
radial arteries or
reversed segments of the patients own saphenous
vein can be used to bypass coronary artery
stenoses

21
Acute coronary syndrome (ACS)

Is a term that encompasses both
Unstable angina(UA)
Myocardial infarction (MI) -(NSTEMI, and STEMI).
It is characterized by
New-onset or rapidly worsening angina (crescendo
angina) or,
Angina on minimal exertion or,
Angina at rest in the absence of myocardial
damage.

22
Introduction..

An ACS may present as a new phenomenon or against
a background of chronic stable angina.
The culprit lesion is usually a complex ulcerated
or fissured atheromatous plaque with
Adherent platelet-rich thrombus
Local coronary artery spasm.
This is a dynamic process whereby the degree of
obstruction may either
Increase, leading to complete vessel occlusion,
or
Regress due to the effects of platelet
disaggregation and endogenous fibrinolysis.

23
Myocardial infarction

Myocardial infarction (MI) occurs when
Symptoms occur at rest.
There is evidence of myocardial necrosis, as
demonstrated by an elevation in cardiac
biomarkers (troponin or CK-MB isoenzyme).
STEMI occurs when
Coronary blood flow decreases abruptly after a
total thrombotic occlusion of a coronary artery,
previously affected by atherosclerosis.
A coronary artery thrombus develops rapidly at a
site of vascular injury resulting into STEMI.
The injury is produced or facilitated by factors
such as cigarette smoking, hypertension, and
lipid accumulation.

24
Myocardial infarction..

The diagnosis of NSTEMI, is established if a
patient with the clinical features of UA
develops
Evidence of myocardial necrosis, as reflected in
elevated cardiac biomarkers (CKMB / Troponin).
NSTEMI is caused by
a reduction in oxygen supply and/or
an increase in myocardial oxygen demand
superimposed on a lesion that causes partial
coronary arterial obstruction, usually an
atherothrombotic coronary plaque.

25
UNSTABLE ANGINA(UA)

Is caused by
dynamic (partial) obstruction of a coronary
artery due to plaque rupture with superimposed
coronary thrombosis and spasm.
Occurs even at rest or with minimal exertion
More severe and lasts longer than stable angina,
may be as long as 30 minutes
May not disappear with rest or use of angina
medication
May lead to complete occlusion of vessel causing
MI.

26
Clinical features of ACS

Chest Pain
Is the cardinal symptom of an ACS.
Occurs in the same sites as angina but is usually
more severe and lasts longer
it is often described as a tightness, heaviness
or constriction in the chest.
In acute MI
the pain can be excruciating
Breathlessness, vomiting and collapse
Are common features.
Most patients are breathless and in some, this is
the only symptom.

27
Clinical features of AClinical features of
ACSCS cont

Vomiting and sinus bradycardia
are often due to vagal stimulation and are
particularly common in patients with inferior MI.
Nausea and vomiting may also be caused or
aggravated by opiates given for pain relief.
Syncope
If syncope occurs, it is usually due to an
arrhythmia or profound hypotension.

28

Clinical features of ACS

Painless or silent MI
Indeed, MI may pass unrecognized.
Is particularly common in older patients or those
with diabetes mellitus.
Sudden death
From ventricular fibrillation or asystole
May occur immediately and often within the first
hour.
The development of cardiac failure reflects the
extent of myocardial ischaemia.
Cardiac failure is the major cause of death in
those who survive the first few hours.

Physical Exam (in large area of myocardial
ischemia)
Diaphoresis
Pale
Cool skin
Sinus tachycardia
Hypotension
a third and/or fourth heart sound basilar rales

30
Diagnosis

The assessment of ACS depends heavily on
Analysis of the character of the chest pain and
its associated features.
Evaluation of the ECG.
Serial measurements of biochemical markers of
cardiac damage.

31
Investigations

Electrocardiography(ECG)
Is central to confirming the diagnosis.
The earliest ECG change is usually ST-segment
elevation.
With proximal occlusion of a major coronary
artery
ST-segment elevation (or new bundle branch block)
is seen initially
later diminution in the size of the R wave
In Transmural (full-thickness) infarction
There is development of a Q wave.
Subsequently, the T wave becomes inverted because
of a change in ventricular repolarisation.

32

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34

Electrocardiography(ECG).
In NST segement elevation there is
Partial occlusion of a major vessel
Complete occlusion of a minor vessel
This causing unstable angina or partial-thickness
(subendocardial) MI.
This is usually associated with ST-segment
depression and T-wave changes.
In the presence of infarction
this may be accompanied by some loss of R waves
in the absence of Q waves.

Plasma cardiac biomarkers
These biochemical markers are
Creatine kinase (CK), a more sensitive and
cardio-specific isoform of this enzyme is
-CK-MB.
Troponins T and I -the cardio-specific proteins.
In unstable angina (UA)
There is no detectable rise in cardiac biomarkers
or enzymes.
The initial diagnosis is made from the clinical
history and ECG only.
In contrast MI
causes a rise in the plasma cardiac biomarkers or
enzymes, that are normally concentrated within
cardiac cells.
The change in plasma concentrations of these
markers confirms the diagnosis of MI.

CK
Starts to rise at 46 hours
Peaks at about 12 hours and falls to normal
within 4872 hours.
Is also present in skeletal muscle
a modest rise in CK (but not CK-MB) may
sometimes be due to
An intramuscular injection
Vigorous physical exercise
The most sensitive markers of myocardial cell
damage are the troponins T and I
These are released within 46 hours and remain
elevated for up to 2 weeks.

Chest X-ray
This may demonstrate pulmonary oedema that is not
evident on clinical examination.
The heart size is often normal, but there may be
cardiomegaly due to pre-existing myocardial
damage.
Echocardiography
Is useful for assessing ventricular function and
for detecting important complications, such as
Mural thrombus
Cardiac rupture
Ventricular septal defect
Mitral regurgitation and
Pericardial effusion.

38
Treatment

Immediate treatment
Analgesia
Is essential, not only to relieve distress but
also to lower adrenergic drive and there by
reduce
vascular resistance,
BP
Infarct size and
Susceptibility to ventricular arrhythmias.
Intravenous opiates ( morphine sulphate 510 mg
or diamorphine 2.55 mg)
OXYGEN THERAPY

Antithrombotic therapy
Antiplatelet therapy
Aspirin
Oral administration of 75325 mg aspirin daily
improves survival, with a 25 relative risk
reduction in mortality.
The first tablet (300 mg) should be given orally
within the first 12 hours.
Clopidogrel
In combination with aspirin
The early (within 12 hours) use of Clopidogrel
(600 mg, followed by 150 mg daily for 1 week and
75 mg daily thereafter)
This confers a further reduction in ischaemic
events.

Anticoagulants
Reduces the risk of thromboembolic complications
Prevents re-infarction in the absence of
reperfusion therapy or after successful
thrombolysis.
Can be achieved using
Unfractionated heparin
Fractioned (low-molecularweight) heparin

Anti-anginal therapy
Nitrates
Sublingual glyceryl trinitrate (300500 µg)
Is a valuable first-aid measure in UA or
threatened infarction
I/V nitrates (glyceryl trinitrate 0.61.2 mg/hr
or isosorbide dinitrate 12 mg/hr)
are useful for the treatment of LV failure and
the relief of recurrent or persistent ischaemic
pain.

ß-blockers
I/V ß-blockers (e.g. atenolol 510 mg or
metoprolol 515 mg given over 5 mins)
Relieve pain
Reduce arrhythmias
Improve short-term mortality in patients who
present within 12 hours of the onset of symptoms.
They should be avoided if there is
HF (pulmonary oedema)
Hypotension (systolic BP lt 105 mmHg)
Bradycardia (heart rate lt 65/min).

Calcium channel antagonist
A dihydropyridine calcium channel antagonist
(e.g. nifedipine or amlodipine)
This can be added to the ß-blocker if there is
persistent chest discomfort but may cause
tachycardia if used alone.
verapamil and diltiazem
Because of their rate-limiting action, these are
the calcium channel antagonists of choice if a
ß-blocker is contraindicated

Fibrinolysis
Fibrinolytic therapy should ideally be initiated
within 30 min of presentation.
The principal goal prompt restoration of full
coronary arterial patency.
The approved fibrinolytics
Tissue plasminogen activator (tPA),
streptokinase, tenecteplase (TNK), and reteplase
(rPA)
Promote the conversion of plasminogen to plasmin,
which subsequently lyses fibrin thrombi.

Interventional Cardiology
Percutaneous coronary intervetion (PCI)
Is a procedure that's used to open a blocked or
narrowed coronary arteries.
Improve blood flow to heart, relieve chest pain,
and possibly prevent a heart attack.
Sometimes a small mesh tube (stent) is placed in
the artery to keep it open after the procedure.
Antiplatelet admin. post stent
Aspirin for life
Clopidogrel for at least 6wks for metal stent

Coronary artery by pass grafting (CABG)
To improve blood flow to the myocardial tissue
that are at risk for
Ischemia
Infarction as a result of the occluded artery.
Arteries or veins from elsewhere in the patient's
body are grafted to the coronary arteries to
bypass atherosclerotic narrowings
This improves the blood supply to the coronary
circulation supplying the myocardium.

47
Long-term Treatment

Risk factor modification eg. cessation of
smoking
Lipid lowering drugs ( e.g. statins,fibrates)
ACE inhibitors are recommended for long-term
plaque stabilization.
Antiplatelet therapy,
Now recommended to be the combination of
aspirin and clopidogrel for at least 912 months,
then continue with aspirin to prevent rupture of
plaque.

48
References

Brian R,Walker N,Stuart H. Davdsons Principle
and Practice of Medicine 22nd Edition.CORONARY
ARTERY DISEASE,Pg 583-600.
KASPER F,HAUSER LONGO. HARRISONS PRINCIPLES OF
INTERNAL MEDICINE 19th Edition. Ischemic Heart
Disease pg 1998-2004.

THANK YOU

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