Go thru` the link & let me know your feedback -esp.with respect to asthma-vis a vis GINA guidelines.
Can we give Asthmatics this vaccine?
Blog for Respiratory-Medicine-Post-Graduates of Apollo Hospitals,Chennai,India - Diplomate National Board(DNB), started in the Year 2009 October ,by PGs & the Academic Co-Ordinator of Department - Dr.R.P.Ilangho - for enabling these Young PGs to INTER_CONNECT ideally for becoming better Pulmonologists.The word~ REMAP09 ~ was coined thus:RE= RE spiratory M=M edicine A=Apollo P= P ostGraduate 09= 2009 - thus meaning "Respiratory Medicine Apollo PostGraduate 2009 batch"
Snap Your Fingers ! Slap Your face ! & Wake Up !!!
FUN is the most Sacred Word in all the religious texts put together - in Life !
Snap Your Fingers ! Slap Your Face ! & Wake Up !!!
Labels
- .ATS GUIDELINES OF TB DEFAULT AND RELAPSE (1)
- 1.WHY FASCIAL PUFFINESS OCCURS FIRST IN RENAL EDEMA (1)
- Acute (2)
- ACUTE EXACERBATION OF COPD CRITERIA (1)
- Acute exacerbation of COPS (1)
- ACUTE EXACERBATION OF ILD CRITERIA (1)
- AE COPD (1)
- Air crescent sign and Monod sign (1)
- Alveolar arterial oxygen gradient (1)
- Amphoric breathing (1)
- Anuria and oliguria definition (1)
- apical cap (1)
- Apical impulse (1)
- Assessment of respiratory muscle strength (1)
- Asthma PEF variablity (1)
- Att in hepatotoxicity (1)
- ATT weight band recent (1)
- Austin flint murmur and Graham steel murmur (1)
- BEQ (1)
- BMI (1)
- Borg dyspnoea score (1)
- breathlessness-sherwood jones (1)
- Bronchiectasis- Definition (1)
- BRONCHOPULMONARY SEGMENTS (1)
- Causes of chest pain aggrevated by cough (1)
- Causes of localised bulging of chest wall (1)
- Causes of orthopnea (1)
- Causes of palpitation (1)
- Causes of Unilateral pedal edema (1)
- Cavity (1)
- check post (1)
- Chest physiotherapy (1)
- Chronic (2)
- Classification (1)
- Clubbing (1)
- clubbing -mechanism of (1)
- Clubbing Unilateral (1)
- CLUBBING-PATHOGENESIS PDGF (1)
- cobb's angle-In Kyphoscoliosis Cobb's angle above which can be operated (1)
- Cobbs angle (1)
- Complications of Tuberculosis (1)
- Cor pulmonale (1)
- Cough reflex (2)
- Cough- aggravating factors (1)
- Cultures- significant colony count (1)
- Cyst/Bulla/Bleb (1)
- Cystic Fibrosis- Female infertility (1)
- DD of Orthopnoea (1)
- definition (1)
- DNB question bank (1)
- Drugs causing breathlessness (1)
- dysphagia - approach (1)
- Dyspnea - Causes of acute dyspnea (1)
- ECG FEATURES OF DEXTROCARDIA (1)
- Emphysema (1)
- Emphysema and chronic bronchitis definition (1)
- Empyema necessitans (1)
- Exacerbation of ILD (1)
- Factitious asthma (1)
- Fever of unknown origin (1)
- fibrinolytics in plef (1)
- FORMOTEROL (1)
- Gastro Intestinal Tract and abdominal symptoms (1)
- Gram negative cocci & gram positive bacilli (1)
- HAM (1)
- Hemothorax (1)
- Hydropneumothorax- sound of Coin test (1)
- Hyperventilation syndrome (1)
- IDSA sinusitis management (1)
- ILD CLASSIFICATION (1)
- Impalpable apical impulse (2)
- Indications for steroids in Sarcoidosis (2)
- Krogg constant (1)
- Lung areas sensitive to pain (1)
- lung cancer- age group (1)
- Lung cancers-ALK inhibitors (1)
- MARKERS OF ILD (1)
- Massive hemoptysis (1)
- Massive hemoptysis criteria (1)
- Mines in Tamil Nadu (1)
- Muscles of respiration (2)
- Name reason for Potts spine (1)
- Nephrotic syndrome (1)
- NORMAL THYMUS IN CT (1)
- NYHA (1)
- Orthopnea (1)
- Orthostatic hypotension (1)
- Pain- CRPS (1)
- Paracetamol -MOA (1)
- Pathophysiology of breath sounds (1)
- Penetration and exposure in Chest Xray (1)
- Perception of Dyspnoea (1)
- Pleuroscopy guidelines (1)
- PND causes (1)
- Pneumatocele (1)
- pneumonia phases of (1)
- Positional variation in chest pain (1)
- Puddle sign (1)
- Pulmonary embolism (1)
- Pulsations in different areas- causes (1)
- Pulsus paradoxus (1)
- Pulsus paradoxus - Measuremen (2)
- RADS-Definition and Criteria (1)
- Respiratory system clinical examination (1)
- S3 (1)
- S4 HEART SOUNDS (1)
- Serum cortisol (1)
- Sherwood jones classification (1)
- Shivering (1)
- Silhouette sign (1)
- Six minute walk test (1)
- Skodaic resonance (1)
- Sleep study and polysomnography (1)
- Spinoscapular distance (1)
- Split pleura sign (1)
- Subacute (2)
- Subpulmonic effusion (1)
- Swellin (1)
- Terminal respiratory unit (1)
- Test (1)
- Tidal percussion (1)
- Tongue in HIV (1)
- Upper respiratory tract (1)
- Velcro crackles (1)
- Vesicular breath sounds - Physiology (1)
- weight loss (1)
Labels
.ATS GUIDELINES OF TB DEFAULT AND RELAPSE
(1)
1.WHY FASCIAL PUFFINESS OCCURS FIRST IN RENAL EDEMA
(1)
Acute
(2)
ACUTE EXACERBATION OF COPD CRITERIA
(1)
Acute exacerbation of COPS
(1)
ACUTE EXACERBATION OF ILD CRITERIA
(1)
AE COPD
(1)
Air crescent sign and Monod sign
(1)
Alveolar arterial oxygen gradient
(1)
Amphoric breathing
(1)
Anuria and oliguria definition
(1)
apical cap
(1)
Apical impulse
(1)
Assessment of respiratory muscle strength
(1)
Asthma PEF variablity
(1)
Att in hepatotoxicity
(1)
ATT weight band recent
(1)
Austin flint murmur and Graham steel murmur
(1)
BEQ
(1)
BMI
(1)
Borg dyspnoea score
(1)
breathlessness-sherwood jones
(1)
Bronchiectasis- Definition
(1)
BRONCHOPULMONARY SEGMENTS
(1)
Causes of chest pain aggrevated by cough
(1)
Causes of localised bulging of chest wall
(1)
Causes of orthopnea
(1)
Causes of palpitation
(1)
Causes of Unilateral pedal edema
(1)
Cavity
(1)
check post
(1)
Chest physiotherapy
(1)
Chronic
(2)
Classification
(1)
Clubbing
(1)
clubbing -mechanism of
(1)
Clubbing Unilateral
(1)
CLUBBING-PATHOGENESIS PDGF
(1)
cobb's angle-In Kyphoscoliosis Cobb's angle above which can be operated
(1)
Cobbs angle
(1)
Complications of Tuberculosis
(1)
Cor pulmonale
(1)
Cough reflex
(2)
Cough- aggravating factors
(1)
Cultures- significant colony count
(1)
Cyst/Bulla/Bleb
(1)
Cystic Fibrosis- Female infertility
(1)
DD of Orthopnoea
(1)
definition
(1)
DNB question bank
(1)
Drugs causing breathlessness
(1)
dysphagia - approach
(1)
Dyspnea - Causes of acute dyspnea
(1)
ECG FEATURES OF DEXTROCARDIA
(1)
Emphysema
(1)
Emphysema and chronic bronchitis definition
(1)
Empyema necessitans
(1)
Exacerbation of ILD
(1)
Factitious asthma
(1)
Fever of unknown origin
(1)
fibrinolytics in plef
(1)
FORMOTEROL
(1)
Gastro Intestinal Tract and abdominal symptoms
(1)
Gram negative cocci & gram positive bacilli
(1)
HAM
(1)
Hemothorax
(1)
Hydropneumothorax- sound of Coin test
(1)
Hyperventilation syndrome
(1)
IDSA sinusitis management
(1)
ILD CLASSIFICATION
(1)
Impalpable apical impulse
(2)
Indications for steroids in Sarcoidosis
(2)
Krogg constant
(1)
Lung areas sensitive to pain
(1)
lung cancer- age group
(1)
Lung cancers-ALK inhibitors
(1)
MARKERS OF ILD
(1)
Massive hemoptysis
(1)
Massive hemoptysis criteria
(1)
Mines in Tamil Nadu
(1)
Muscles of respiration
(2)
Name reason for Potts spine
(1)
Nephrotic syndrome
(1)
NORMAL THYMUS IN CT
(1)
NYHA
(1)
Orthopnea
(1)
Orthostatic hypotension
(1)
Pain- CRPS
(1)
Paracetamol -MOA
(1)
Pathophysiology of breath sounds
(1)
Penetration and exposure in Chest Xray
(1)
Perception of Dyspnoea
(1)
Pleuroscopy guidelines
(1)
PND causes
(1)
Pneumatocele
(1)
pneumonia phases of
(1)
Positional variation in chest pain
(1)
Puddle sign
(1)
Pulmonary embolism
(1)
Pulsations in different areas- causes
(1)
Pulsus paradoxus
(1)
Pulsus paradoxus - Measuremen
(2)
RADS-Definition and Criteria
(1)
Respiratory system clinical examination
(1)
S3
(1)
S4 HEART SOUNDS
(1)
Serum cortisol
(1)
Sherwood jones classification
(1)
Shivering
(1)
Silhouette sign
(1)
Six minute walk test
(1)
Skodaic resonance
(1)
Sleep study and polysomnography
(1)
Spinoscapular distance
(1)
Split pleura sign
(1)
Subacute
(2)
Subpulmonic effusion
(1)
Swellin
(1)
Terminal respiratory unit
(1)
Test
(1)
Tidal percussion
(1)
Tongue in HIV
(1)
Upper respiratory tract
(1)
Velcro crackles
(1)
Vesicular breath sounds - Physiology
(1)
weight loss
(1)
Search This Blog
Pages
Wednesday, March 31, 2010
Sunday, March 14, 2010
PULMONARY EMBOLISM
Pulmonary embolism presents with a wide clinical
spectrum, from asymptomatic disease to life
threatening massive PE that causes hypotension and
cardiogenic shock. Several studies have been published,
since the seminal trial that tested anticoagulation
against no therapy12. There is hardly any published data
on PE from India.
The clinical presentation and the investigations
including electrocardiography, chest radiography, and
analysis of arterial blood gases cannot be relied on to
confirm or rule out PE because of lack of adequate
specificity13. The presence of one or more risk factors
may lower the threshold for diagnostic evaluation. This
did not help in the present series as none of the patients
had any obvious risk factor. D-dimer testing has been
reported to have a sensitivity ranging from almost 80-
100 percent. However, in the present series due to the
unavailability of the test at all times, it could be
performed only in six patients and was found to be
positive.
Since the origin of the thrombus is mostly from deep
veins of the legs, compression ultrasound of lower limb
veins is a useful investigation in the diagnosis of PE. It
is, however, reported to be positive only in 10-20% of
patients without leg symptoms or signs who undergo
evaluation and in approximately 50% of patients with
proven PE13. Thus, PE cannot be ruled out on the basis
of negative results on ultrasound. Compression
ultrasound has its value in situations where there is a
high clinical probability of PE and the patient has no
past history of VTE13. In our study, eight patients had
symptoms and signs of DVT, whereas 16 had an
ultrasonographic evidence of DVT. Thus, compression
ultrasound is a useful investigation in patients with
symptomatic PE. Perfusion scan has been used for
almost three decades for the diagnosis of PE and is a
valuable tool when the results are definitive. But
approximately 30-70% of scans are non-diagnostic and
the clinician is left in a diagnostic dilemma of
uncertainty14. Further, it is insensitive in patients with
pre-existing lung diseases, especially the chronic
obstructive lung disease15.
The use of spiral CTPA is a major advancement in the
diagnosis of PE. The sensitivity and specificity for
detection of pulmonary embolus by CTPA at the main,
lobar and segmental levels are greater than 90% with
accuracy decreasing when isolated subsegmental
vessels are involved14. Also, spiral CTPA has a greater
interobserver agreement. With the third-generation
scanners which provide 1-mm resolution in a single
breath hold, the spiral CTPA is now the preferred
Figure 3. Spiral computed tomographic pulmonary angiography
showing isolated subsegmental thrombus.
Figure 4. Computed tomography showing peripheral wedgeshaped
infarct on right side.
respectively (Table).
Massive PE was diagnosed in 10 patients and submassive
PE in five patients, respectively; while nine
patients had minor PE. Of the 15 patients, 14 were
thrombolysed. One patient had only sub-massive PE
without hypoxemia and was, therefore, not
thrombolysed. All the patients received low molecular
weight haparin (LMWH) followed by oral
anticoagulants. Of the 24 patients, 20 (83.4%) recovered
and were discharged from the hospital. Four patients
died, three due to refractory shock and respiratory
failure and one after a massive upper gastrointestinal
114
imaging modality16. In our study, perfusion scans were
performed in 14 patients and CTPA contributed to
diagnosis in 21 patients. Perfusion scans were of high
probability in 11 patients and non-contributory in the
remaining three patients; CTPA confirmed the diagnosis
in these three patients.
Echocardiography is not used routinely in the
diagnosis of PE, but it is a useful tool in identifying high
risk patients such as those with right ventricular
dysfunction, patent foramen ovale, free floating
thrombus and persistent pulmonary hypertension17. All
our patients underwent echocardiography, and right
ventricular dysfunction was identified in 62.5 percent.
Although there is little doubt about the role of
anticoagulation in PE, thrombolysis is a debatable
indication18,19. There is no conclusive evidence till date to
show that thrombolysis reduces mortality in massive
PE, except a small study which consisted only of eight
patients20. Thrombolysis in sub-massive PE is also a
controversial indication. In a large randomised trial in
patients with PE, Konstantinides et al11 randomised 256
patients to receive both thrombolysis and anticoagulation
or anticoagulation alone. There was no
survival benefit but patients receiving anticoagulation
alone required escalation of treatment in form of
secondary thrombolysis, vasopressor requirement and
mechanical ventilation to prevent clinical deterioration.
We had thrombolysed 14 out of the 24 patients (83.4%),
10 with massive PE and four with sub-massive PE. Of
these 14 patients, four died, three from cardiogenic
shock and one from massive upper gastrointestinal
bleed. All the patients received LMWH followed by oral
warfarin. Monitoring of anticoagulation is important
but is not available widely in India. Finger-prick
techniques for monitoring INR are being increasingly
used in the west11 but again are not available in India.
In conclusion, PE is an under recognised and
underdiagnosed clinical problem in India. A high index
of suspicion is necessary to consider the diagnosis, and
the increasing availability of radiographic and nuclear
imaging techniques are likely to improve its diagnosis
in India. Early recognition and aggressive and
appropriate therapy improves outcome in this
potentially fatal condition.
ACKNOWLEDGEMENTS
Authors thank Dr Balamugesh, Dr Shiva, Dr Pralay,
Dr Mahendran, and Dr Shriraam for their constructive
criticism.
spectrum, from asymptomatic disease to life
threatening massive PE that causes hypotension and
cardiogenic shock. Several studies have been published,
since the seminal trial that tested anticoagulation
against no therapy12. There is hardly any published data
on PE from India.
The clinical presentation and the investigations
including electrocardiography, chest radiography, and
analysis of arterial blood gases cannot be relied on to
confirm or rule out PE because of lack of adequate
specificity13. The presence of one or more risk factors
may lower the threshold for diagnostic evaluation. This
did not help in the present series as none of the patients
had any obvious risk factor. D-dimer testing has been
reported to have a sensitivity ranging from almost 80-
100 percent. However, in the present series due to the
unavailability of the test at all times, it could be
performed only in six patients and was found to be
positive.
Since the origin of the thrombus is mostly from deep
veins of the legs, compression ultrasound of lower limb
veins is a useful investigation in the diagnosis of PE. It
is, however, reported to be positive only in 10-20% of
patients without leg symptoms or signs who undergo
evaluation and in approximately 50% of patients with
proven PE13. Thus, PE cannot be ruled out on the basis
of negative results on ultrasound. Compression
ultrasound has its value in situations where there is a
high clinical probability of PE and the patient has no
past history of VTE13. In our study, eight patients had
symptoms and signs of DVT, whereas 16 had an
ultrasonographic evidence of DVT. Thus, compression
ultrasound is a useful investigation in patients with
symptomatic PE. Perfusion scan has been used for
almost three decades for the diagnosis of PE and is a
valuable tool when the results are definitive. But
approximately 30-70% of scans are non-diagnostic and
the clinician is left in a diagnostic dilemma of
uncertainty14. Further, it is insensitive in patients with
pre-existing lung diseases, especially the chronic
obstructive lung disease15.
The use of spiral CTPA is a major advancement in the
diagnosis of PE. The sensitivity and specificity for
detection of pulmonary embolus by CTPA at the main,
lobar and segmental levels are greater than 90% with
accuracy decreasing when isolated subsegmental
vessels are involved14. Also, spiral CTPA has a greater
interobserver agreement. With the third-generation
scanners which provide 1-mm resolution in a single
breath hold, the spiral CTPA is now the preferred
Figure 3. Spiral computed tomographic pulmonary angiography
showing isolated subsegmental thrombus.
Figure 4. Computed tomography showing peripheral wedgeshaped
infarct on right side.
respectively (Table).
Massive PE was diagnosed in 10 patients and submassive
PE in five patients, respectively; while nine
patients had minor PE. Of the 15 patients, 14 were
thrombolysed. One patient had only sub-massive PE
without hypoxemia and was, therefore, not
thrombolysed. All the patients received low molecular
weight haparin (LMWH) followed by oral
anticoagulants. Of the 24 patients, 20 (83.4%) recovered
and were discharged from the hospital. Four patients
died, three due to refractory shock and respiratory
failure and one after a massive upper gastrointestinal
114
imaging modality16. In our study, perfusion scans were
performed in 14 patients and CTPA contributed to
diagnosis in 21 patients. Perfusion scans were of high
probability in 11 patients and non-contributory in the
remaining three patients; CTPA confirmed the diagnosis
in these three patients.
Echocardiography is not used routinely in the
diagnosis of PE, but it is a useful tool in identifying high
risk patients such as those with right ventricular
dysfunction, patent foramen ovale, free floating
thrombus and persistent pulmonary hypertension17. All
our patients underwent echocardiography, and right
ventricular dysfunction was identified in 62.5 percent.
Although there is little doubt about the role of
anticoagulation in PE, thrombolysis is a debatable
indication18,19. There is no conclusive evidence till date to
show that thrombolysis reduces mortality in massive
PE, except a small study which consisted only of eight
patients20. Thrombolysis in sub-massive PE is also a
controversial indication. In a large randomised trial in
patients with PE, Konstantinides et al11 randomised 256
patients to receive both thrombolysis and anticoagulation
or anticoagulation alone. There was no
survival benefit but patients receiving anticoagulation
alone required escalation of treatment in form of
secondary thrombolysis, vasopressor requirement and
mechanical ventilation to prevent clinical deterioration.
We had thrombolysed 14 out of the 24 patients (83.4%),
10 with massive PE and four with sub-massive PE. Of
these 14 patients, four died, three from cardiogenic
shock and one from massive upper gastrointestinal
bleed. All the patients received LMWH followed by oral
warfarin. Monitoring of anticoagulation is important
but is not available widely in India. Finger-prick
techniques for monitoring INR are being increasingly
used in the west11 but again are not available in India.
In conclusion, PE is an under recognised and
underdiagnosed clinical problem in India. A high index
of suspicion is necessary to consider the diagnosis, and
the increasing availability of radiographic and nuclear
imaging techniques are likely to improve its diagnosis
in India. Early recognition and aggressive and
appropriate therapy improves outcome in this
potentially fatal condition.
ACKNOWLEDGEMENTS
Authors thank Dr Balamugesh, Dr Shiva, Dr Pralay,
Dr Mahendran, and Dr Shriraam for their constructive
criticism.
Saturday, March 13, 2010
To Do Wish List
Bimal & Supraja:
All matters discussed on 13th.
a) Clinical presentation headers for complaints & sections eg: H/o presenting illness- what to ask etc.
b) Fix class schedules
To ALL:
a)Update your thesis b) make sms & Email alerts for all Blog posts & schedule-class-alerts(Plz.get Bimal`s help on this)
All matters discussed on 13th.
a) Clinical presentation headers for complaints & sections eg: H/o presenting illness- what to ask etc.
b) Fix class schedules
To ALL:
a)Update your thesis b) make sms & Email alerts for all Blog posts & schedule-class-alerts(Plz.get Bimal`s help on this)
Thursday, March 4, 2010
Subscribe to:
Posts (Atom)