Asthma and COPD

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Asthma and COPD

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Title: Asthma and COPD

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Asthma and COPD

November 28, 2002
Cass Djurfors
Dr. M. Betzner

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Objectives

Asthma
Definition
Epidemiology
Pathophysiology
Clinical features
Diagnostic tests
Management
Disposition

4
Objectives

COPD
Definition
Epidemiology
Pathophysiology
Clinical Presentation
Diagnostic Criteria
Treatment
Chronic
Acute

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Asthma definition

Chronic inflammatory disease characterized by
reversible airflow obstruction, exacerbations and
remissions.

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NAEPP Diagnostic Criteria

Intermittent airflow obstruction indicated by a
history of nighttime cough, recurrent wheeze or
recurrent chest tightness.
Reversible airflow obstruction as documented by
pulmonary function testing, worsening symptoms in
the presence of any of several triggers, or
symptoms that occur at night.
All other possible diagnoses are excluded.
National Asthma Education and Prevention Program.
Expert panel report 2 Guidelines for the
diagnosis and management of asthma. DHHS pub
NIH 97-4051. 1997

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Epidemiology

Affects 4-6 of population in the United States
Most common chronic disease of childhood, fourth
leading cause of disability in children,
increasing in prevalence
30 of children will have persistent symptoms of
asthma into adulthood
Fatalities are real 4657 in U.S. in 1998

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Etiology

Currently believed that asthma is the result of a
combination of genetic predisposition and
environmental exposures
Common Triggers
Tobacco smoke, air pollutants, animal allergens,
dust mites, viral respiratory infections,
cockroach allergens, weather changes, molds,
outdoor allergens, gerd

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Pathophysiology

Acute and chronic inflammation and airway
hyperresponsiveness
Partially reversible airflow obstruction results
from bronchial smooth muscle constriction, airway
edema and inflammation, and mucus plugging
bronchoconstriction is superimposed in the acute
setting
Permanent changes can eventually be seen at the
microscopic levelincluding collagen deposition
and fibrosis below the basement membrane from
mast cell activity and inflammatory cell migration

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History

Symptoms
Cough, wheeze, SOB, chest tightness, sputum,
fever, poor feeding
Pattern of disease
Course, onset, duration, seasonal variation,
frequency
Aggravating factors/triggers
Usual triggers, current trigger
History of disease
previous hospitalization
previous intubation/ICU
previous ED visits
typical episode
Age at onset and method of diagnosis
Present management, meds and history of steroid
use

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History

Family History
Social History
Home environment (smoking, pets, allergens)
Identification of precipitating cause
Exacerbation profile
Usual exacerbation pattern and outcome
Past best spirometry measures
Medical history, allergies, anaphylaxis
Treatment
Medications at home and timing of last dose
Treatment before arrival

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Physical Exam

Vital signs
RR increases
HR-tachycardia from anxiety, increased work of
breathing, and hypoxia
BP-hypotension may be present in patients with
impending resp failure due to decreased venous
return and increased pleural pressures. Pulsus
paradoxus may be present

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Physical Exam

Accessory muscle use
Indrawing subcostal, intercostal,
supraclavicular
Paradoxical abdominal and chest wall movements
Nasal flaring in young children

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Physical Exam

Mental status
Prolonged expiratory phase
Lung findings
Wheeze
Silent chest

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Diagnostic Tests

Pulse Oximetry
Continuous monitoring
lt91 may be a predictor of hospital admission in
kids (Geelhoed et al, BMJ, 1988)
PEF
An approximation of FEV1
Should be measured in all but the sickest of
patients or those younger than 5 years
Compare with predicted age/size appropriate value
and with personal best

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Diagnostic Tests

CXR
Of limited utility
Useful in those with concern for complications of
asthma (pneumothorax) or those patients in whom
another diagnosis is suspected
Recommended for children with first episode of
wheeze to rule out foreign bodies, congenital
anomalies (Scarfone, Emergency Asthma, 1999)

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Diagnostic Tests

ABG
Useful as supportive evidence for the clinical
diagnosis of respiratory failure

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Asthma Severity CAEP

Mild
exertional dyspnea/cough
nocturnal symptoms.
Increased use of ß agonistfor symptom control.
Good response to ß agonist
FEV1,PEFR gt 60 predicted or best.
(FEV1 gt 2.1L PEFR gt 300L/min)

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Asthma Severity CAEP

Moderate
dyspnea at rest, cough,congested, chest
tightness,
nocturnal symptoms.
Partial relief from ß agonistand or ß agonist
neededmore often than Q4h
FEV1 PEFR 40-60 predicted or best.
(FEV1 1.6-2.1L, PEFR 200-300L/min)

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Asthma Severity CAEP

Severe
laboured respirations
agitated, diaphoretic
difficulty speaking
tachycardic,
no prehospital reliefwith ß agonist
FEV1,PEFR - unable or lt40 predicted or
best(FEV1 lt1.6L PEFR lt200L/min O2 saturation
lt90)

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Asthma Severity CAEP

Near Death
exhausted, confused,
diaphoretic, cyanotic,
silent chest, decreased resp. effort
falling heart rate
FEV1,PEFR not appropriate
O2 saturation lt90 (despite supplemental O2)

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Treatment Goals

Correct hypoxia
Reverse airflow obstruction
Treat underlying inflammatory response

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Management CAEP

Mild
O2
ß agonist (MDI chamber)MDI (Metered Dose
Inhaler) - MDI adapters available for ET
tubeChamber (valved spacer device) - use of
chamber is recommended

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Management CAEP

Moderate
O2
ß agonist (MDI chamber)
systemic corticosteroids
anticholinergics may be helpful in some cases
Frequent FEV1 /PEFR to evaluate response to
treatment

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Management CAEP

Severe
100 O2
anticipate the need for intubation
frequent/continuous ß agonistand anticholinergic
(nebulized orMDI with chamber)

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Management CAEP

Severe
Systemic corticosteroids
Cardiac monitoring
Oximetry, ABG's, CXR
Frequent reassessment
Spirometry when possible
Physician and nursingsupervision until clear
signsof improvement
UNRESPONSIVE Consider near death management

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Management CAEP

Near Death
100 O2
paralysis, intubation modified RSI technique
Intubation is a clinical decision
continuous ß agonist andanticholinergic
(nebulized orMDI ETT adaptor)UNRESPONSIVE
Rule out pneumothorax or upper airway obstruction
consider alternative drugs I.V. ß agonists,
inhalational anesthetic agents

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Management CAEP

Near Death
Systemic corticosteroids
Cardiac monitoring
Oximetry, ABG's, CXR
Frequent reassessment
Spirometry when possible
Physician and nursingsupervision until clear
signsof improvement

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Ventilatory Strategies

Cautious CO2 reduction with permissive
hypercapnea until lung function improves
Controlled mechanical hypoventilation
Bicarb as needed to keep pHgt7.2
Slow RR (6-8 breaths/min) to reduce barotrauma
and volutrauma
Low IE ratios
Low tidal volumes (6-8 mL/kg)
Frequent suctioning of mucous secretions as
required

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OXYGEN

Will not suppress respiratory drive in acute
asthma
Start high FiO2 40-100
Achieve O2Sat 92-95

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ß agonists first line therapy

titrate to response (adults and children)
e.g. inhaled salbutamol 100 µg/puff
Relaxes bronchial smooth muscle and promotes
mucociliary clearance
MDI 4-8 puffs q15-20 min X 3 is usual, increase
to 1 puff q 30-60 sec (4-20 puffs) prn
wet nebulizer 5.0 mg ( 1 ml/3ml ns) q 15-20 min.
X3 continuous if necessary
administer with oxygen
Increase dose for intubated patients

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ß agonists first line therapy

Several RCTs have shown equivalent efficacy
between MDI spacer and nebulizers in the
emergency treatment of acute asthma
Rodrigo et al, American Journal of Emergency
Medicine, 1998
Schuh et al, J Pediatr, 1999
For outpatient ß agonist use, MDIs are
equivalent to all other hand held inhaler
devices, and remain the most cost effective
delivery system.
Ram et al, BMJ, 2001

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Anticholinergics

e.g. inhaled ipratropium bromide (20 µg/puff)
Inhibits acetylcholine-mediated
bronchoconstriction and decreases mucous
production.
Not systemically absorbed
Peak effect in 60 minutes
Indicated for moderate and severe asthma in both
adults and children

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Anticholinergics

Zorc et al, Pediatrics, 1999
427 childrengt12 months were randomized in a
blinded fashion to either ipratropium (250
mcg/dose) or normal saline with each of the first
three nebulized albuterol doses.
The addition of the ipratropium to a standard ED
treatment protocol for acute asthma was
associated with reductions in duration and amount
of treatment before discharge

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Anticholinergics

MDI 4-8 puffs q15-20 min X 3 is usual, increase
to 1 puff q 30-60 SEC (4-20 puffs) prn
Wet nebulizer .25. - .5 mg ( 1 -2ml/3ml NS) q
15-20 min. X3 continuous if necessary
Decrease frequency in recovery phase
May be mixed with ß agonists

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Corticosteroids

All patients seen in ER for asthma should be
considered for oral or IV steroids
Associated with rapid resolution of airflow
obstruction and decreased relapse rate
Oral and IV are equally efficacious
No good evidence regarding best dose
Accepted doses are 100-200 mg of
methylprednisolone or equivalent or 500-1000mg of
hydrocortisone or equivalent, oral doses should
be in the range of 40mg of prednisone or
equivalent

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Corticosteroids at d/c

Patients discharged from the ED who require
steroid therapy should be given 30-60 mg of
prednisone orally for 7-14 days (CMAJ, Guidelines
for the emergency management of asthma in adults,
1999)
Children 1-2 mg/kg per day for a total of 5 days
Decadron has not been widely used or studied but
may be an alternative in children

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Inhaled Corticosteroids

Should be prescribed at discharge but not a
component of emergency management
CMAJ, Guidelines for the emergency management of
asthma in adults, 1999
Dose-related systemic adverse effects, especially
at doses gt0.8mg/d of fluticasone or equivalent
Lipworth, Systemic Adverse Effects of Inhaled
Corticosteroid Therapy, Arch Intern Med, 1999.

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Intubation agents

Induction Ketamine 1.5 mg/Kg I.V.
Add atropine in kids
Paralysis
Succinylcholine 1.5 mg/Kg I.V.
Roc/vec/pavulon for maintenanceof paralysis only

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Alternative Drugs

(Not usually required) May be Associated With
More ToxicityPatients unresponsive to treatment
may benefit from I.V. ß agonists or inhalational
anesthetic agents. These forms of therapy may
require consultation with respirology, ICU,
anesthesia or internal medicine.

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Alternative Drugs

Adrenaline (11000) S.C. 0.3 - 0.5 ml q 15 - 20
min prn (1 ml 11000 in 250 D5W 4 µg/ml) I.V.
Infusion 4-8 µg/minKids 0.01mL/kg of 11000
S.C.

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Alternative Drugs

Salbutamol (I.V. solution only) Load 4µg/Kg
(over 2-5 min) I.V. Infusion 0.1 - 0.2 µg/Kg/min
Methylxanthines (Aminophylline) Load 3 - 6 mg/Kg
I.V. over 30 min (1/2 if already taking)
infusion 0.2 - 1 mg/Kg/Hour (follow levels). Not
usually recommended as Bronchodilator in the
first 4 hours of treatment.

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Alternative Drugs

Magnesium
Controversial Some evidence for IV use in severe
asthma
Smooth muscle relaxant
Adults (AMA guidelines)
Severe / Near Death Asthma satslt90,
PEF/FEV1lt40
consider 2gm MgSO4 IV over 20 mins
Peds
Severe / Near Death Asthma (satslt92,PEF/FEV1lt50
of pb/predicted
consider 25mg/kg MgSO4 IV over 20 mins

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Alternative Drugs

Heliox
Mixture of helium and oxygen
Low-density gas mixture which is thought to
reduce turbulent airflow
Must be at least 60 helium which presents a
problem in hypoxic patients
Evidence is limited
Can be considered in a limited group of
nonhypoxic severe asthmatics

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Alternative Drugs

Leukotriene Modifiers
Potent bronchodilator with additive effect to
B2-agonists
Direction for the future
May have a role in acute treatment of asthma, but
that remains to be investigated

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Disposition CAEP guidelines

Pretreatment
lt 25 predicted or best(FEV1 lt 1.0 L PEFR lt 100
L/min)
Admission isusually necessary

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Disposition CAEP guidelines

Post Treatment
1. lt 40 predicted or best(FEV1 lt 1.6 L PEFR lt
200 L/min)
Admission recommended
2. 40-60 predicted or best(FEV1 lt 1.6-2.1 L
PEFR lt 200-300 L/min)
Discharge Possible
3. gt 60 predicted or best(FEV1 gt 2.1 L PEFR gt
300 L/min)
Discharge likely

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Patients at Risk for Relapse

1. Previous near death episode.2. Recent
E.D. visits.3. Frequent hospitalizations.4.
Steroid dependent or recent use.5. Sudden
attacks.6. Allergic/anaphylactic triggers.7.
Prolonged duration of recent attack.8. Poor
compliance or understanding.9. Returning to same
environmental triggers.

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Discharge instructions

MEDICATIONS
A. ß agonists
Regular use often required for 48 hours (2-4
puffs Q4h).
PRN use after 48 hours if symptoms controlled
If unable to control symptoms with ß agonists
return to E.D. or see your physician.

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Discharge instructions

B. Corticosteroids - indicated for most patients
Prednisone 30-60 mg/day for 7-14 days taper or
discontinue based on asthma control/physician
advice
Individual plans based on past treatment/recent
symptoms
Inhaled Continue at previous dose even if taking
prednisone. Initiate at 500-1000 ug/day
(Beclomethasone/Budesonide or equivalent). Higher
doses may be necessary. Consider as integral part
of long term management.

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Discharge instructions

Anti inflammatory medications (non-steroid)
To be continued on discharge.
Role in long term management to be assessed by
family physician or consultant.

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PATIENT INSTRUCTIONS

Review
1) Drug Delivery Technique (puffer, spacer
device, powder delivery)
2) Role of relievers (ß agonists) and preventers
(anti inflammatory)
Explain
Treatment failure indications for emergency
assessment or physician advice. This should be
based on signs, symptoms and medication
requirements, e.g. dose (number and frequency of
puffs) of ß agonist required for relief or
control of symptoms.

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PATIENT INSTRUCTIONS

Educate
The Lung Association, Asthma and Allergy
Information Association and the Asthma Society of
Canada has educational materials and some
communities have formal education programs.
Refer
Consider respirology, internal medicine, allergy/
immunology consultation for high risk patients.
Worsening/ persisting symptoms, modify dose and
schedule of steroid therapy. Follow up with
family MD or consultant in 1-7 days to assess
response.

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Chronic Management Considerations

Environmental control
Short-acting B2-agonists on demand
Regular inhaled glucocorticoid for all but the
mildest of asthmatics (if B2-agonist is neededgt3
times per week, other than for exercise, inhaled
glucocorticoid should be added)
If asthma is not adequately controlled by
moderate doses (500-1000mcg/d of beclomethasone
or equivalent) additional therapy should be
addedconsider long-acting B2-agonists,
leukotriene antagonists or other medications
Severe asthma may require additional treatment
with prednisone
CMAJ, Canadian Asthma Consensus Report, 1999

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COPD

ATS Definition
A disease state characterized by the presence of
airflow obstruction due to chronic bronchitis or
emphysema
Progressive
Airway hyperactivity, if present, may be
partially reversible

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COPD Definitions

Chronic Bronchitis
Presence of chronic productive cough for 3 months
in each of 2 successive years in a patient in
whom other causes of chronic cough have been
excluded
Emphysema
Abnormal permanent enlargement of the airspaces
distal to the terminal bronchioles, accompanied
by destruction of their walls and without obvious
fibrosis
Tintinalli, Emergency Medicine, 2000

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Epidemiology

Sixth leading cause of death in the world in 1990
(WHO)
Leading cause of morbidity and mortality among
smokers gt 55 yrs
Rare in those under age 40
Mengtwomen, but this is changing as more women
smoke
Mortality for patients hospitalized with a COPD
exacerbation is estimated at 5-14

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Pathophysiology

Smoking accounts for 80-90 of risk
Environmental factors have been suggested
occupational exposure, air pollution, second hand
smoke
Genetic factorsa1-antitrypsin deficiency
Earliest detectable changes in COPD evolution are
evident as small increases in peripheral airway
resistance or lung compliance

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Pathophysiology

Disease progression is slow and insidious,
spanning decades may be masked by sedentary
lifestyle of most smokers
Abstinence from smoking is most advantageous
during early course of disease
Variability in disease pattern and progression
between similar patientsmuch is still unknown

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Pathophysiology

Airflow impedance (expiratory mostly) results
primarily from increased resistance or decreased
caliber of the small bronchi and bronchioles
Airway secretions, mucosal edema, bronchospasm,
and bronchoconstriction from decreased airway
elasticity are all responsible for airflow
obstruction
Increased airway resistance reduced minute
ventilation /- increased work of breathing

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Pathophysiology

Alveolar hypoventilation hypoxemia
hypercarbia
V/Q mismatching
Pulmonary hypertension
RV hypertrophy then dilatation
Cor pulmonale

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Clinical Presentation

Chronic Stable COPD
Symptoms
Exertional dyspnea
Cough
Exam
Tachypnea
Accessory muscle use
Pursed-lip breathing
Expiratory wheeze
Coarse crackles
Reduced air entry

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Clinical Presentation

Acute exacerbation of COPD
Patients present complaining of
Worsening dyspnea
Increased sputum volume
Increased sputum purulence
Hypoxemia, tachypnea, cyanosis, agitation,
tachycardia, hypertension, acc mm use, pursed-lip
exhalation, sitting up leaning forward posture
Hypercapnea may result in confusion, tremor,
decreased LOC
Respiratory failure

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Causes of AECOPD

Superimposed respiratory infection
Cardiovascular deterioration
Smoking
Noncompliance with meds
Environmental exposures
Meds e.g. ß-blockers, benzos, narcotics
Misuse of oxygen therapy
Metabolic derangements

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DDX AECOPD

Pneumonia
IHD
CHF
Asthma
PE
Pneumothorax
Etc.

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Diagnostic Tests

Pulse Oximetry
Easy, immediate, noninvasive test that provides
information about the severity of respiratory
compromise in an acute exacerbation
ABG
Provides accurate information about pH, PaO2 and
PaCO2
Consider in most if not all patients presenting
with an acute exacerbation

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Diagnostic Tests

PFTs
FEV1 as compared to percent predicted is an
excellent measure of disease severity
As FEV1 falls below 25-30 of predicted, both
hypoxemia and hypercarbia usually occur
PEF can be used in ED to estimate FEV1, with the
understanding that PEF is effort dependent and
tends to overestimate lung function in the mid
ranges

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Diagnostic Tests

CXR
Almost always abnormal, comparisons with prior
exams should be made
Helpful in the diagnosis of complications such as
pneumothorax, pneumonia, pleural effusions,
pulmonary neoplasia

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Infectious Precipitants

Viral infections often implicated in COPD
exacerbations influenza, PAI, RSV
Atypical organisms may also be involved
Mycoplasma, Chlamydia pneumoniae, Legionella
Chronic colonization also occurs, most often with
H. flu, Strep pneumo, and Moraxellarole of these
organisms in exacerbations is controversial.

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CAP in AECOPD

COPD patients are at high risk for CAP
Symptoms of CAP are similar to those of AECOPD
sputum, fever, cough
Strep pneumo is most common, followed by H flu,
and Moraxella Catarrhalis
Legionella and Pseudomonas should always be
considered
Pneumovax and yearly influenza vaccines are
important prevention

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Antibiotics in AECOPD

Controversial and difficult to study
Currently accepted practice based on the best
evidence is that patients presenting with
infectious symptoms
Fever
Increased sputum production
Change in character of sputum
will have a better outcome with the use of
empiric antibiotic therapy

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Antibiotics in AECOPD

Increasing evidence for newer antibiotics as
first line therapy azithromycin, respiratory
fluoroquinolones, ß-lactamase inhibitors.

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Antibiotics in AECOPD

CHA recommendations
lt4 exacerbations/year
Amoxicillin 500mg po tid x 7-10d
Doxycycline 200mg po x 1d then 100mg po od x
7-10d
TMP/SMX 1 DS tablet po bid x 7-10d

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Antibiotics in AECOPD

CHA recommendations
gt or 4 exacerbations per year or failure of
first line agent or Abx last 6 weeks
Cefuroxime axetil 250-500mg bid x 7-10d
Amoxicillin-clavulanate 875mg po bid x 7-10 d
For pen allergic patients
Azithromycin 500mg x 1d then 250mg po od x 4d
Clarithromycin 250-500mg po bid x 7-10d
Levofloxacin 500mg po od x 5-10d
Moxifloxacin 400mg po od x 5-10d

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Management of stable COPD

Lifestyle modifications
Smoking cessation
Regular exercise
Weight control
Pulmonary rehabilitation
Prevention
Pneumovax
Influenza

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Management of stable COPD

Oxygen
Started after room air ABGs document PaO2lt55 or
56-59 in the face of cor pulmonale
Bronchodilators
ß-agonists
Ipratropium bromide
Long acting ß-agonists
/- Theophylline

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Management of stable COPD

Steroids
20-30 are steroid responders
Inhaled or oral

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Management AECOPD

Goals of therapy
Relieve bronchoconstriction
Improve oxygenation
Approach to treatment
Multi-modal
Be cognizant of previous disease pattern

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Management AECOPD

Oxygen
All patients in respiratory distress should
receive supplemental oxygen
Target O2satgt90
Be aware that patients known to be CO2-retainers
may require controlled oxygen therapy
Hypercarbia is likely secondary to the Haldane
effect a shift of the hemoglobin-CO2 binding
curve, as well as due to increased CO2 production
and changes in physiologic dead space

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Management AECOPD

ß2-agonists
COPD patients will have some reversibility to
their airflow obstruction that can effectively be
relieved by inhaled short acting ß2-agonist
therapy
Long acting ß2-agonist therapy should be reserved
for chronic management only
No evidence that one specific agent has any
greater efficacy than any other
Little evidence regarding timing of
administration (q60 min vs. q20 min etc.)

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Management AECOPD

Anticholinergics
Preferentially dilate larger central airways
compared to ß2-agonists which dilate peripheral
airways
Slower onset of action than ß2-agonists
Thought to inhibit vagal stimulation of the
bronchithereby promoting smooth muscle
relaxation
Atropine and glycopyrrolate have been used
Most common agent is ipratropium bromide q4-6h by
neb or MDI

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Management AECOPD

Theophylline
Controversial
Narrow therapeutic window
Significant side effects dysrhythmias, seizures
Limited evidence for efficacy

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Management AECOPD

Corticosteroids
Conflicting results in the literature
In acute exacerbation, there is likely a role for
systemic steroids, but not for inhaled
Steroid response is likely a continuum rather
than an all or none phenomenon

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Management AECOPD

Magnesium
Studied mostly in asthma
One study showed benefit in COPD, used as 1-2g IV
over 20 min
Heliox
No large-scale studies
Probably should only be considered as a last
alternative

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Mechanical Ventilation the controversies

Widespread fear among healthcare workers that
patients will become ventilator dependent
Evidence suggests that most patients in fact will
be extubated around day 10 but that 1-5 year
mortality rate following an episode of
respiratory failure is very high
Likely a decision that should be addressed by the
patient, family, primary health care provider
PRIOR to the actual event

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Mechanical Ventilation

Decision to begin assisted ventilation is a
clinical one
Noninvasive ventilation (BiPAP)
BiPAP works by providing nasal, bilevel positive
airway pressure. This overcomes the intrinsic
PEEP of most COPD patients, and significantly
reduces work of breathing, thereby improving gas
exchange
Response is usually seen within the first hour
Should be considered first line before
endotracheal intubation unless patient has
impaired mental status or cardiovascular
instability

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Mechanical Ventilation

Kramer et al
Selection criteria for NPPV (any two)
Moderate to severe dyspnea with use of accessory
muscles and paradoxical abdominal motion
Moderate to severe acidosis (pH 7.3-7.35) and
hypercapnia (PaCO2 45-60)
Respiratory frequency gt 25 breaths/min

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Mechanical Ventilation

Kramer et al
Exclusion Criteria for NPPV (any one)
Respiratory arrest
Cardiovascular instability (hypotension,
dysrhythmias, AMI)
Somnolence, impaired mental status, uncooperative
patient
High risk of aspiration
Viscous or copious secretions
Recent facial or gastroesophageal surgery
Craniofacial trauma with fixed nasopharyngeal
abnormalities
Extreme obesity

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Mechanical Ventilation

Indications for invasive mechanical ventilation
in AECOPD (Pierson, Respiratory Care, 2002)
Severe dyspnea with accessory muscle use and
paradoxical abdominal motion
RRgt35
Life-threatening hypoxemia (PaO2lt40)
Severe acidosis (pH lt 7.25) and hypercapnea
(PaCO2 gt 60)
Respiratory arrest
Somnolence or impaired mental status
Cardiovascular complications
Other complications (sepsis, pneumonia, PE)
Failure of NPPV

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Disposition