1. Goals Understand the historical context of pulmonary emboli
Comprehend the pathophysiology and know some common risk factors
Be aware of the clinical features of PE and have a basic understanding of various diagnostic test
Gain a therapeutic approach to the treatment of PE and discuss a simplified method in the work-up of PE
Attempt to dispel a few mythsabout pulmonary emboli
1 So let us beginSo let us begin
2. Perspective A common disorder and potentially deadly
650000 cases occuring annually
Highest incidence in hospitalized patients
Autopsy reports suggest it is commonly
missed diagnosis
3. Perspective Presentation is often atypical
Signs and symptoms are frequently vague and nonspecific and rarely classic
Untreated mortality rate of 20% - 30%, plummets to 5% with timely intervention
3 PE It has a wide spectrum of patient presentation, which leads us to do suboptimal testing. This can stand in the way of a timely diagnosis
Its important, because prompt diagnosis and treatment can dramatically reduce the mortality rate and morbidity of this disease.
Unfortunately, the diagnosis is missed far more than it is made. ��I want to offer you a historical perspective of the disorderPE It has a wide spectrum of patient presentation, which leads us to do suboptimal testing. This can stand in the way of a timely diagnosis
Its important, because prompt diagnosis and treatment can dramatically reduce the mortality rate and morbidity of this disease.
Unfortunately, the diagnosis is missed far more than it is made.
4. Historical Context Pre-1930s
Heparin
4 Until the 1930s, PTE was viewed almost universally fatal, with surgery the only treatment despite an operative mortality of 100%
Enter heparin, circa 1930s, heparin was discovered and its wide spread use were so immediate and dramatically apparent that this become the mainstay of treatment for the next 70 years!
In 1977, a physician be the name of Eugene Robin published a landmark article which stimulated immense change in medicines approach to diagnosing PE.
It was robin contention the while lung scintigraphy was sensitive to the presence of clots, but also non-specific. He questioned the value of ventilation scans when the perfusion defects were small. He felt angiography was being underused, and that PE.was being OVER diagnosed.
Until the 1930s, PTE was viewed almost universally fatal, with surgery the only treatment despite an operative mortality of 100%
Enter heparin, circa 1930s, heparin was discovered and its wide spread use were so immediate and dramatically apparent that this become the mainstay of treatment for the next 70 years!
In 1977, a physician be the name of Eugene Robin published a landmark article which stimulated immense change in medicines approach to diagnosing PE.
It was robin contention the while lung scintigraphy was sensitive to the presence of clots, but also non-specific. He questioned the value of ventilation scans when the perfusion defects were small. He felt angiography was being underused, and that PE.was being OVER diagnosed.
5. Historical Context
PIOPED (Prospective Investigation of Pulmonary Embolism Diagnosis)
The Electronic Era, 2000 and Beyond
5 Jump ahead to 1990. The PIOPED investigators, stimulated by Robins article published their data on the sensitivities and specificities of V/Q scans for PE.
In summary, a random sample of 933 of 1493 patients were studied prospectively. 931 had scintography and 755 underwent angiography.
Their conclusion: clinical assessment combined with the V/Q scan can establish the diagnosis or exclusion of pulmonary embolism only for a minority of patients
Enter the electronic era, Craig Feied, MD, who has read every published article about PE written in the last 100 years and who has written the chapter in Rosens in the last two editions published this statement:
Massive PE is one of the most common causes of unexpected death, being second only to coronary artery disease as a cause of sudden unexpected natural death at any age. Most clinicians do no appreciate the extent of the problem, because the diagnosis is unsuspected until autopsy in approximately 80% of cases. Jump ahead to 1990. The PIOPED investigators, stimulated by Robins article published their data on the sensitivities and specificities of V/Q scans for PE.
In summary, a random sample of 933 of 1493 patients were studied prospectively. 931 had scintography and 755 underwent angiography.
Their conclusion: clinical assessment combined with the V/Q scan can establish the diagnosis or exclusion of pulmonary embolism only for a minority of patients
Enter the electronic era, Craig Feied, MD, who has read every published article about PE written in the last 100 years and who has written the chapter in Rosens in the last two editions published this statement:
Massive PE is one of the most common causes of unexpected death, being second only to coronary artery disease as a cause of sudden unexpected natural death at any age. Most clinicians do no appreciate the extent of the problem, because the diagnosis is unsuspected until autopsy in approximately 80% of cases.
6. So What Do We Do ???
Confusing for Emergency Physician
Do we under diagnose/over diagnose?
Why dont we have a standardized method of work up after all these years? 6 Do we under diagnose or over diagnose?
If we over diagnose, is it such a big deal? Its just a few month of inconvenience of heparin and warfarin.
Aside from the potential morbidity of the anticoagulants,there are other problems.
The diagnoses carries a stigma which will contaminate all future medical encounters. Women may be barred from oral contraceptives, future pregnancies will be considered high risk. Elective surgery may be denied.
So, really after all these years, we are still left in the dark. We still dont have a collective conscience on a standard approach to this problem.
Before we can answer any questions we have to understand the condition and this take us to virchow.
Do we under diagnose or over diagnose?
If we over diagnose, is it such a big deal? Its just a few month of inconvenience of heparin and warfarin.
Aside from the potential morbidity of the anticoagulants,there are other problems.
The diagnoses carries a stigma which will contaminate all future medical encounters. Women may be barred from oral contraceptives, future pregnancies will be considered high risk. Elective surgery may be denied.
So, really after all these years, we are still left in the dark. We still dont have a collective conscience on a standard approach to this problem.
Before we can answer any questions we have to understand the condition and this take us to virchow.
7. Etiology Rudolph Virchow, 1858
Triad:
Hypercoagulability
Stasis to flow
Vessel injury
7 Everyone Im sure is familiar with Virchows triad. It was first described by this German pathologist.
If we think of risk factors, we should think of them as the embodiment of the triad: hypercoagulability, stasis, and vessel injury.
So, essentially, under normal conditions, microthrombi are continually formed and lysed with the venous circulatory system.
When any one of the risk states exists, potential microthrombi may escape the normal fibrinolytic system and grow and propagate.
Pulmonary Emboli occurs when fragments of thrombus break loose and are carried through the right side of the heart into the pulmonary arterial tree. Everyone Im sure is familiar with Virchows triad. It was first described by this German pathologist.
If we think of risk factors, we should think of them as the embodiment of the triad: hypercoagulability, stasis, and vessel injury.
So, essentially, under normal conditions, microthrombi are continually formed and lysed with the venous circulatory system.
When any one of the risk states exists, potential microthrombi may escape the normal fibrinolytic system and grow and propagate.
Pulmonary Emboli occurs when fragments of thrombus break loose and are carried through the right side of the heart into the pulmonary arterial tree.
8. Pathophysiology .incresed deadspace
.hyperventilation
.hypoxemia due to :
.V/Q mismatch
.pulmonary shunt
Reduced cardiac output
9. Risk Factors Hypercoagulability
Malignancy
Nonmalignant thrombophilia
Pregnancy
Postpartum status (<4wk)
Estrogen/ OCPs
Genetic mutations (Factor V Leiden, Protein C & S deficiency, Factor VIII, Prothrombin mutations, anti-thrombin III deficiency)
Venous Statis
Bedrest > 24 hr
Recent cast or external fixator
Long-distance travel or prolong automobile travel
Obesity
Vessel Injury
Recent surgery requiring endotracheal intubation
Recent trauma (especially the lower extremities and pelvis)
9 Cancers of primarily adenocarcinoma and CNS tumors most often cause thrombosis.
We need to make special mention about patients with a prior history of DVT or PE.
Studies have revealed these patients have between a 5 to 30 times increased risk of a new DVT in response to a triggering event compared to those who have not had prior episodes. Cancers of primarily adenocarcinoma and CNS tumors most often cause thrombosis.
We need to make special mention about patients with a prior history of DVT or PE.
Studies have revealed these patients have between a 5 to 30 times increased risk of a new DVT in response to a triggering event compared to those who have not had prior episodes.
10. Clinical Presentation The Classic Triad: (Hemoptysis, Dyspnea, Pleuritic Pain)
Not very common!
Occurs in less than 20% of patients with documented PE
Three Clinical Presentations
Pulmonary Infarction
Submassive Embolism
Massive Embolism : sys pressure< 90 or fall in BP>40 10 All the above symptoms are a manifestation of cardiopulmonary stress caused by the clot in the lung.
These produce symptoms perceived by the patient and the signs observed by you!
There are three common clinical presentations that you should be aware of:
1. Patients with pulmonary infarction may have pleuritic chest pain and can be hard to distinguish between that patient with infection pneumonitis
2. Submassive embolism are the hardest of all. By definition, they have an angiographically defined blockage of flow to an area served by less than two lobar arteries.
These patients have acute or unexplained dyspnea with exertion or at rest. So, they can be easily confused with infection, asthma, CHF and the like.
3. Finally, Massive PE, or a clot which obstructs two lobar arteries, so-called Saddle Embolus. These patients have acute cor pulmonaly often with syncope. You might think there having an MI or look septic!
All the above symptoms are a manifestation of cardiopulmonary stress caused by the clot in the lung.
These produce symptoms perceived by the patient and the signs observed by you!
There are three common clinical presentations that you should be aware of:
1. Patients with pulmonary infarction may have pleuritic chest pain and can be hard to distinguish between that patient with infection pneumonitis
2. Submassive embolism are the hardest of all. By definition, they have an angiographically defined blockage of flow to an area served by less than two lobar arteries.
These patients have acute or unexplained dyspnea with exertion or at rest. So, they can be easily confused with infection, asthma, CHF and the like.
3. Finally, Massive PE, or a clot which obstructs two lobar arteries, so-called Saddle Embolus. These patients have acute cor pulmonaly often with syncope. You might think there having an MI or look septic!
11. Mythology of PE
Myth
Patients with pulmonary embolism are short of breath and have chest pain!
Reality:
You can forget about making the diagnosis on clinical grounds, but waitdont plan on completely ruling it out either!
11 While its true the most common symptom is shortness of breath, even patients with circulatory collapse may have no dyspnea, tachypnea, or pleuritic pain!
In fact, A normal paO2 > 80 is more prevalent in patients with pulmonary infarction syndrome.
As a simple rule, if you have a patient in your department and you dont have a good reason to explain there dyspnea, its a good idea to consider PE!
While its true the most common symptom is shortness of breath, even patients with circulatory collapse may have no dyspnea, tachypnea, or pleuritic pain!
In fact, A normal paO2 > 80 is more prevalent in patients with pulmonary infarction syndrome.
As a simple rule, if you have a patient in your department and you dont have a good reason to explain there dyspnea, its a good idea to consider PE!
12. Clinical Features Symptoms in Patients with Angio Proven PTE
Symptom Percent
Dyspnea 84
Chest Pain, pleuritic 74
Anxiety 59
Cough 53
Hemoptysis 30
Sweating 27
Chest Pain, nonpleuritic 14
Syncope 13 12 These are the common symptoms that are associated with PE
As we mentioned in the previous slide, dyspnea and chest pain are not always present.
The explanation is that with a small V/Q mismatch, the adaptive physiology of the pulmonary vasculature and bronchi produce intermittent shortness of breath. Because of this, we are easily distracted and looking for a cardiogenic cause of the dyspnea.
What about pleuritic chest pain, still not a home run!
In fact, up to 25% of patients ultimately diagnosed with a PE, never had any chest pain!
This is what makes the diagnosis so difficult! These are the common symptoms that are associated with PE
As we mentioned in the previous slide, dyspnea and chest pain are not always present.
The explanation is that with a small V/Q mismatch, the adaptive physiology of the pulmonary vasculature and bronchi produce intermittent shortness of breath. Because of this, we are easily distracted and looking for a cardiogenic cause of the dyspnea.
What about pleuritic chest pain, still not a home run!
In fact, up to 25% of patients ultimately diagnosed with a PE, never had any chest pain!
This is what makes the diagnosis so difficult!
13. Clinical Features Signs with Angiographically Proven PE
Sign Percent
Tachypnea > 20/min 92
Rales 58
Accentuated S2 53
Tachycardia >100/min 44
Fever > 37.8 43
Diaphoresis 36
S3 or S4 gallop 34
Thrombophebitis 32
Lower extremity edema 24
13 Lets look a t a couple of these:
Tachycardia!
Myth #2 We are all taught this is a key component of the diagnosis. Right?
In fact, actually not having tachycardia is more commonly seen in patients who are found to have a PE!
What about fever? ��If a patient has a fever, it must not be a PE, right?
Not true.
Although not common, Among patients with PE and no other source of fever, fever was present in one study in 43 of 311 patients (14%).
Lets look a t a couple of these:
Tachycardia!
Myth #2 We are all taught this is a key component of the diagnosis. Right?
In fact, actually not having tachycardia is more commonly seen in patients who are found to have a PE!
What about fever?
14. Who do we work up?� - Pretest Probability Definition: The probability of the target disorder (PE) before a diagnostic test result is known.
Used to decide how to proceed with diagnostic testing and final disposition
14 For example
This could represent the likelihood that a specific patient , say a middle-aged man, with a specific past history, say hypertension and tobacco smoking who presents with a specific symptom complex: Chest pain, Dsypnea, or Diaphoresis has a specific diagnosis.
Final Statement:
Because PE can present with or with any of the classic signs and symptoms and even the risk factors which contribute to PE are varied in frequency, we are left with a intuition at best!
For example
This could represent the likelihood that a specific patient , say a middle-aged man, with a specific past history, say hypertension and tobacco smoking who presents with a specific symptom complex: Chest pain, Dsypnea, or Diaphoresis has a specific diagnosis.
Final Statement:
Because PE can present with or with any of the classic signs and symptoms and even the risk factors which contribute to PE are varied in frequency, we are left with a intuition at best!
15. Wells Scoring
16. Prognostic factors Dysfunction of right ventricle
Rise of brain natriuretic peptide>90pg/ml
Or N-terminal pro-BNP
Simultaneous DVT
Thrombus in right ventricle
Rise of troponin
Hyponatremia
17. Diagnostic Test Imaging Studies
CXR
V/Q Scans
Spiral Chest CT
Pulmonary Angiography
Echocardiograpy
Laboratory Analysis
CBC, ESR, Hgb/Hct,
D-Dimer
ABGs
Ancillary Testing
EKG
Pulse Oximetry 17 As you can see there are a variety of test that we use to arrive at a diagnosis.
Some better than others!
So, lets talk about these individually. As you can see there are a variety of test that we use to arrive at a diagnosis.
Some better than others!
So, lets talk about these individually.
18. Diagnostic Testing� - CXRs
Chest X-Ray Myth:
You have to do a chest x-ray so you can find Hamptons hump or a Westermark sign.
Reality:
Most chest x-rays in patients with PE are nonspecific and insensitive
18 Granted that most are abnormal, but certainly not diagnostic.
It is true that in the original PIOPED study it was recommended but the main value is to exclude diagnoses the mimic PE and to aid in the interpretation of the V/Q scanGranted that most are abnormal, but certainly not diagnostic.
It is true that in the original PIOPED study it was recommended but the main value is to exclude diagnoses the mimic PE and to aid in the interpretation of the V/Q scan
19. Diagnostic Testing � - CXRs
Chest radiograph findings in patient with pulmonary embolism
Result Percent
Cardiomegaly 27%
Normal study 24%
Atelectasis 23%
Elevated Hemidiaphragm 20%
Pulmonary Artery Enlargement 19%
Pleural Effusion 18%
Parenchymal Pulmonary Infiltrate 17% 19 Cardiomegaly was the most frequent finding in those with PE of In-patients
Out-patients, it seemed to be atelectasis in the above study.
Cardiomegaly was the most frequent finding in those with PE of In-patients
Out-patients, it seemed to be atelectasis in the above study.
20. Chest X-ray Eponyms of PE Westermark's sign
A dilation of the pulmonary vessels proximal to the embolism along with collapse of distal vessels, sometimes with a sharp cutoff.
Hamptons Hump
A triangular or rounded pleural-based infiltrate with the apex toward the hilum, usually located adjacent to the hilum. 20
21. Radiographic Eponyms � - Hamptons Hump, Westermarks Sign 21 Here we see the dilated vessels and oligemia of westermarks sign
And below Hamptons HumpHere we see the dilated vessels and oligemia of westermarks sign
And below Hamptons Hump
22. Diagnostic Testing � EKGs EKG
Most Common Findings:
Tachycardia or nonspecific ST/T-wave changes
Acute cor pulmonale or right strain patterns
Tall peaked P-waves in lead II (P pulmonale)
Right axis deviation
RBBB
S1-Q3-T3 (occurs in only 20% of PE patients)
22 A brief mention about the classic S1-Q3-T3, its appearance on the EKG may suggest PE, but study after study has shown it has no predictive value what so ever!
But you got to know it because question writers for the boards love it!A brief mention about the classic S1-Q3-T3, its appearance on the EKG may suggest PE, but study after study has shown it has no predictive value what so ever!
But you got to know it because question writers for the boards love it!
23. Diagnostic Testing � - Pulse Oximetry
The Pulse Oximetry Myth:
You must do a pulse oximetry reading, since patients with pulmonary embolism are hypoxemic!
Reality:
Most patients with a PE have a normal pulse oximetry, and most patients with an abnormal pulse oximetry will not have a PE. 23 Actually, it is opposite of what you might think!Actually, it is opposite of what you might think!
24. Diagnostic Testing � - ABGs
The ABG/ A-a Gradient myth:
You must do an arterial blood gas and calculate the alveolar-arterial gradient. Normal A-a gradient virtually rules out PE.
Reality:
The A-a gradient is a better measure of gas exchange than the pO2, but it is nonspecific and insensitive in ruling out PE. 24 As with most dogma, we are taken back by what we thought was truth.
About 15% of patients with proven pulmonary embolism have a pO2 of 85mmHg or higher!
In one study, researches drew from there data various combinations of the PaO2 of 80mm Hg or more, the PaCO2 of 35mmHg or higher, and the A-a gradient of 20 mmHg or less.
They found that PE could not be excluded in more than 30% of patients with no prior cardiopulmonary disease.
Moreover, PE could not be excluded in more than 14% of patients with prior cardiopulmonary disease.
Conclusion, Blood gas levels are poor discriminate value to permit the exclusion of PE.
As with most dogma, we are taken back by what we thought was truth.
About 15% of patients with proven pulmonary embolism have a pO2 of 85mmHg or higher!
In one study, researches drew from there data various combinations of the PaO2 of 80mm Hg or more, the PaCO2 of 35mmHg or higher, and the A-a gradient of 20 mmHg or less.
They found that PE could not be excluded in more than 30% of patients with no prior cardiopulmonary disease.
Moreover, PE could not be excluded in more than 14% of patients with prior cardiopulmonary disease.
Conclusion, Blood gas levels are poor discriminate value to permit the exclusion of PE.
25. Diagnostic Testing Echocardiography
Consider in every patient with a documented pulmonary embolism
EKG maybe helpful in demonstrating right heart strain
Early fibrinolysis can reduce mortality 50%!
25 Diagnosing of early right ventricular strain is important because it is a strong predictor of subsequent death
Important to recommend echocardiogram with your admitting internist if a pattern of right heart strain is suggested by EKG.
Studies have documented that lives are saved with early fibrinolysis is considered in these patients.
Diagnosing of early right ventricular strain is important because it is a strong predictor of subsequent death
Important to recommend echocardiogram with your admitting internist if a pattern of right heart strain is suggested by EKG.
Studies have documented that lives are saved with early fibrinolysis is considered in these patients.
26. Ancillary Test WBC
Poor sensitivity and nonspecific
Can be as high as 20,000 in some patients
Hgb/Hct
PTE does not alter count but if extreme, consider polycythemia, a known risk factor
ESR
Dont get one, terrible test in regard to any predictive value
26
27. D-dimer Test Fibrin split product
Circulating half-life of 4-6 hours
Quantitative test have 80-85% sensitivity, and 93-100% negative predictive value
False Positives:
Pregnant Patients Post-partum < 1 week
Malignancy Surgery within 1 week
Advanced age > 80 years Sepsis
Hemmorrhage CVA
AMI Collagen Vascular Diseases
Hepatic Impairment
27 Well, what is it?
Basically, the assay is enzyme-linked monoclonal antibody test used to identify the protein, D-Dimer.
D-Dimer itself is a unique degradation product that is produced by a plasmin mediated breakdown of cross-linked fibrin
Good test with respect to its negative predictive value.
The drawbacks are some of the false positives that we commonly see in the ER.
Well, what is it?
Basically, the assay is enzyme-linked monoclonal antibody test used to identify the protein, D-Dimer.
D-Dimer itself is a unique degradation product that is produced by a plasmin mediated breakdown of cross-linked fibrin
Good test with respect to its negative predictive value.
The drawbacks are some of the false positives that we commonly see in the ER.
28. Diagnostic Testing D-dimer
Qualitative
Bed side RBC agglutination test
SimpliRED D-dimer
Quantitative
Enzyme linked immunosorbent asssay Dimertest
Positive assay is > 500ng/ml
VIDAS D-dimer, 2nd generation ELISA test
28 Two types,
Qualitative RBC agglutination assay, low sensitivity and specificity and not good enough to comfortably rule out PE.
Quantitative, which measure the accurately the amount using a spectrophotometer.
Our lab uses the 2nd generation VIDAS d-dimer with a negative predictive value of 99.3%!
Two types,
Qualitative RBC agglutination assay, low sensitivity and specificity and not good enough to comfortably rule out PE.
Quantitative, which measure the accurately the amount using a spectrophotometer.
Our lab uses the 2nd generation VIDAS d-dimer with a negative predictive value of 99.3%!
29. Ventilation/Perfusion Scan� - V/Q Scan A common modality to image the lung and its use still stems from the PIOPED study.
Relatively noninvasive and sadly most often nondiagnostic
In many centers remains the initial test of choice
Preferred test in pregnant patients
50mrad vs 800mrad (with spiral CT) 29
31. V/Q Scan Technique
Interpretation
Normal
Low probability/nondiagnostic (most common)
High Probability
Simplified approached to the interpretation of results:
High probability ? Treat for PE
Normal Scan ? If low pre-test, your done
Everything else ? Purse another study (CT, Angio)
31 Essentially, a patient is injected with a radioisotope that travels through the pulmonary microcirculation and are detected by a gamma camera over the patient
A normal Perfusion study will have evenly distributed blood flow.
Then a patient inhales a radioactive gas and it is viewed as it washes over the bronchopulmonary tree.
A mismatch, areas of blocked perfusion and normal ventilation is interpreted by the radiologist and given reading as normal (never), high probability, or non-diagnostic/low-probability
The reason the low probability or non diagnostic scan category is so suspect is because in the PIOPED study this group had terrible inter-reader reliability. So, just beware.
Essentially, a patient is injected with a radioisotope that travels through the pulmonary microcirculation and are detected by a gamma camera over the patient
A normal Perfusion study will have evenly distributed blood flow.
Then a patient inhales a radioactive gas and it is viewed as it washes over the bronchopulmonary tree.
A mismatch, areas of blocked perfusion and normal ventilation is interpreted by the radiologist and given reading as normal (never), high probability, or non-diagnostic/low-probability
The reason the low probability or non diagnostic scan category is so suspect is because in the PIOPED study this group had terrible inter-reader reliability. So, just beware.
32. Spiral (Helical) Chest CT Advantages
Noninvasive and Rapid
Alternative Diagnosis
Disadvantages
Costly ($600 - 900/scan)
Risk to patients with borderline renal function
Hard to detect subsegmental pulmonary emboli
32 The entire lung can be scanned while the patient holds there breath.
Advantages:
CT most useful benefit is in providing evidence for an alternative diagnosis or excluding it entirely.
Disadvantages:
The clinical significance for subsegmental PE are not well
known, but may be a marker for a larger PE
Given that the majority of V/Q studies are non-diagnostic, I prefer the CT as the initial test of choice in place of V/Q scan.
The entire lung can be scanned while the patient holds there breath.
Advantages:
CT most useful benefit is in providing evidence for an alternative diagnosis or excluding it entirely.
Disadvantages:
The clinical significance for subsegmental PE are not well
known, but may be a marker for a larger PE
Given that the majority of V/Q studies are non-diagnostic, I prefer the CT as the initial test of choice in place of V/Q scan.
37. Pulmonary Angiography
Gold Standard
Performed in an Interventional Cath Lab
Positive result is a cutoff of flow or intraluminal filling defect
Court of Last Resort 37 Right now there is no better test on the horizon of the immediate present to virtually rule out or in PE.
Right now there is no better test on the horizon of the immediate present to virtually rule out or in PE.
39. Treatment:
Goals:
Prevent death from a current embolic event
Reduce the likelihood of recurrent embolic events
Minimize the long-term morbidity of the event
39 I thought this cartoon kind of summarizes how patients sometimes feel about the medical jargon we throw about and the puzzled look are there face when we try to explain this condition and how to treat it.
So what are our goals???I thought this cartoon kind of summarizes how patients sometimes feel about the medical jargon we throw about and the puzzled look are there face when we try to explain this condition and how to treat it.
So what are our goals???
40. Treatment Anticoagulants
Heparin
Provides immediate thrombin inhibition, which prevents thrombus extension
Does not dissolve existing clot
Will not work in patients with antithrombin III def.
In this case use hirudins
Few absolute contraindications
40 Heparin is the most frequently used drug in the treatment of PE.
Because heparin works by activating antithrombin III, this genetic mutation makes heparin ineffective.
Heparin is the most frequently used drug in the treatment of PE.
Because heparin works by activating antithrombin III, this genetic mutation makes heparin ineffective.
41. Treatment Anticoagulants
Heparin
Available as Unfractionated or LMW Heparin
FDA approved dosing:
Unfractionated: 80 units/kg bolus, 18 units/kg/hr
LMWH: 1 mg/kg Q 12 or 1.5mg/kg Q D
LMWH (Lovenox) prefered in pregnant patients
41 FDA approved dose for Unfractionated heparin is 80units/kg IV bolus, then 18 units/kg/hr infusion to maintain the INR at 2.5-3
Lovenox is dosed at 1mg/kg every 12 hours or 1.5 mg/kg per day.
LMWH in pregnancy only preferred for convenience sake.
FDA approved dose for Unfractionated heparin is 80units/kg IV bolus, then 18 units/kg/hr infusion to maintain the INR at 2.5-3
Lovenox is dosed at 1mg/kg every 12 hours or 1.5 mg/kg per day.
LMWH in pregnancy only preferred for convenience sake.
42. Treatment Anticoagulants
Warfarin (Coumadin)
Interferes with the action of Vit-K dependent factors: II, VII, IX, and X, as well as protein C & S
Causes temporary hypercoagulable state in first 5 days of treatment
Important a patient is anticoagulated with heparin before initiating warfarin therapy
Target INR is 2.5 3.0
42 This is because the anticoagulants protein C and S have short half-lives compared with the procoagulant vitamin K-dependent proteins.
So, this gives rise to the clinical importance that heparin must be continued for at least five days after beginning Coumadin
The incidence of progressive thrombosis and embolization is 40% when starting warfarin directly, compared to only 8% when beginning after a patient has been anticoagulated with heparin.
Treatment is usually for 6 months, but may continue lifelongThis is because the anticoagulants protein C and S have short half-lives compared with the procoagulant vitamin K-dependent proteins.
So, this gives rise to the clinical importance that heparin must be continued for at least five days after beginning Coumadin
The incidence of progressive thrombosis and embolization is 40% when starting warfarin directly, compared to only 8% when beginning after a patient has been anticoagulated with heparin.
Treatment is usually for 6 months, but may continue lifelong
43. Treatment Fibrinolytic Therapy (Alteplase)
Indications:
Documented PE with:
Persistent hypotension
Syncope with persistent hemodynamic compromise
Significant hypoxemia
+/- patient with acute right heart strain
Approved alteplase regimen is 100mg as a continuous IV infusion.
43 For critically ill patients, a very rapid infusion of 100mg over 10 minutes is preferred.
Alternative is Retavase, you can give it as two IV doses of 10 units, each over two minutes. For critically ill patients, a very rapid infusion of 100mg over 10 minutes is preferred.
Alternative is Retavase, you can give it as two IV doses of 10 units, each over two minutes.
44. Contraindication to fibrinolytic therapy Absolute:
History of hemorrhagic stroke
Active intracranial neoplasm
Recent <2 month intracranial surgery
Active or recent internal bleeding in prior 6 month
Relative:
Bleeding diathesis
Uncontrolled severe hypertension> 200/110
Nonhemorrhagic stroke
Surgery whithin previous 10 days
Thrombocytopenia< 100000
45. Treatment Embolectomy
Prefininolytic therapy this was only therapy for massive PE
Carries a 40% operative mortality
Alternative is Transvenous Catheter Embolectomy 45 This is a procedure where a suction tip catheter is placed in contact with the thrombus under fluoroscopy and sucked out while catheter is withdrawnThis is a procedure where a suction tip catheter is placed in contact with the thrombus under fluoroscopy and sucked out while catheter is withdrawn
46. A Simplified Algorithm Pre-test probability
D-dimer (VIDAS-DD)
CT angiography 46 The simplest algorithm says you can safely rule out PE in a low pre-test patient with a negative D-dimer
I believe our institution and my personal practice is similar to the Mayo Clinic Group who uses a combination of pre-test probability, D-dimers, and CT angio, and limited V/Q to arrive at a disposition.
The simplest algorithm says you can safely rule out PE in a low pre-test patient with a negative D-dimer
I believe our institution and my personal practice is similar to the Mayo Clinic Group who uses a combination of pre-test probability, D-dimers, and CT angio, and limited V/Q to arrive at a disposition.
47. Special Circumstances Morbid Obesity
Pregnancy
V/Q has considerable less radiation
50mrad vs. 800 mrad
Almost all will have positive D-Dimer
Heparin safe in pregnancy
Witnessed Cardiac Arrest
Standard ACLS, if known PE, the lytics.
47 These patients are difficult if not impossible to image. D-dimer may be useful if < 500 and you can support an alternative diagnosis. These patients are difficult if not impossible to image. D-dimer may be useful if < 500 and you can support an alternative diagnosis.
48. Conclusion� Summary Points
Pulmonary Emboli remain a potentially deadly and common event which may present in various ways
Don't be fooled if your patient lacks the classic signs and symptoms!
Consider PE in any patient with an unexplainable cause of dyspnea, pleuritic chest pain, or findings of tachycardia, tachpnea, or hypoxemia
2nd Generation Qualitative D-Dimers have NPV of 93-99%
Heparin remains the mainstay of therapy with the initiation of Warfarin to follow
Simplified Algorithm: ( Pretest probability, D-Dimer, +/- CT angio), then disposition)
48
49. The End! 49
50. 1. Which of the following is not a part of virchows triad?
Hypercoagulability
Stasis to flow
Vessel injury
History of previous DVT
50
51. Which of the following is the propper treatment of fat emboli?
Platelets
High dose steroids
Heparin
cryoprecipitate
51
52. The Classic Triad of patients presenting to the ED with PE includes all of the following except:
Hemoptysis
Dyspnea
+ Homans sign
Pleuritic Pain
52
53. What is the most common symptom in a patient with Angio Proven PTE?
Dyspnea
Chest Pain, pleuritic
Anxiety
Cough 53
54. What is the most common ecg finding in patients with PE?
Right axis deviation
RBBB
S1-Q3-T3
Tall peaked T-waves in lead II (P pulmonale)
Sinus tachycardia
54
55. Answers D
B
C
A
E 55
