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ARDS

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Title: ARDS

1
ARDS

DR. T. MOHAN KUMAR, MD, AB, DPPR, FCCP
CHIEF SENIOR CONSULTANT,
DEPARTMENT OF PULMONOLOGY CRITICAL CARE,
SRI RAMAKRISHNA HOSPITAL,
COIMBATORE

2
DIAGNOSTIC CRITERIA

ARDS
Acute
PaO2/Fio2lt200 mmHg
Bilateral interstitial
or alveolar infiltrates
Pcwp lt15-18 mmHg

ALI
Acute
lt300 mm Hg
Same
same

3
Clinical diagnosis

Rapid
Within 12 to 48 hr of the predisposing event
Awake patients become anxious,agitated
dyspnoeic
Dyspnoea on exertion proceeding to severe when
hypoxemia intervenes
Stiffening of lung leads to increase work of
breathing,small tidal volumes,rapid respiratory
rate
Initially respiratory alkalosis
Respiratory failure

4
Clinical disorders associated with ARDS

Direct lung injury
Aspiration of gastric contents
Pulmonary contusion
Toxic gas inhalation
Near drowning
Diffuse pulmonary infection

Indirect lung injury
Severe sepsis
Major trauma
Hypertransfusion
Acute pancreatitis
Drug overdose
Reperfusion injury
Post cardiac bypass/lung transplants

5
Clinical disorders associated with ARDS

FREQUENT CAUSES
SEPSIS
BACTEREMIA WITHOUT SEPSIS SYNDROME
4
SEVERE SEPSIS/SEPSIS SYNDROME
35-45
MAJOR TRAUMA
MULTIPLE BONE FRACTURES
5-10
PULMONARY CONTUSION
17-22
HYPERTRANSFUSION
5-36
ASPIRATION OF GASTRIC CONTENTS
22-36

6
CLINICAL MANIFESTATIONS

ARDS occurs in the setting of acute severe
illness
Clinical manifestations may vary
Sepsis and trauma most important
Multiple organ failure
Atelectasis and fluid filled lungs
Hypoxemia/dyspnoea
Fever /leukocytosis

7
Laboratory studies

To date no lab findings pathognomonic of ARDS
X-ray chest shows bilateral infiltrates
consistent with pulmonary edema, may be mild or
dense, interstitial or alveolar, patchy or
confluent
ABG shows hypoxemia with respiratory alkalosis.
In late stages hypoxemia, acidosis, hypercarbia
may be seen.

Leukocytosis/Leukopenia/anemia are common
Renal function abnormalities/or liver function
Von willebrands factor or complement in serum
may be high
Acute phase reactants like ceruloplasmin or
cytokine (TNF,IL-1,IL-6,IL-8) may be high.

9
BRONCHOALVEOLAR LAVAGE

Inflammatory mediators like cytokines, reactive
oxygen species, leukotrienes activated
complement fragments are found in the fluid
Cellular analysis shows more than 60 of
neutrophils.
As ARDS resolves neutrophils are replaced with
alveolar macrophages.
Another interesting finding is the presence of a
marker of pulmonary fibrosis called procollagen
peptide III (PCPIII) and this correlates with
mortality.
Presence of more eosinophils suggest eosinophilic
pneumonia, high lymphocyte counts may be seen in
hypersensitivity pneumonitis, sarcoidosis, BOOP,
or other acute forms of interstitial lung disease.

10
Differential diagnosis

Infectious causes
Bacteria - Gm neg pos , mycobacteriae,
mycoplasma, rickettsia, chlamydia
Viruses- CMV, RSV, hanta virus, adeno virus,
influenza virus
Fungi- H.capsulatum, C.immitis
parasites- pneumocytis carinii, toxoplasma gondii

11
Differential Diagnosis

Non infectious causes
CCF
Drugs toxins (paraquat, aspirin, heroin,
narcotics, toxic gas, tricyclic anti depressants,
acute radiation pneumonitis)
Idiopathic (esinophilic pneumonia, Acute
interstitial pneumonitis, BOOP, sarcoidosis,
rapidly involving idiopathic pulmonary fibrosis)
Immunologic (acute lupus pneumonitis, Good
Pastures syndrome, hypersensitivity pneumonitis)
Metabolic (alveolar proteinosis)
Miscellaneous (fat embolism, neuro/high altitude
pulmonary oedema)
Neoplastic (leukemic infiltration, lymphoma)

12
Therapy -goals

Treatment of the underlying precipitating event
Cardio-respiratory support
Specific therapies targeted at the lung injury
Supportive therapies

13
Respiratory Support
14
Spontaneously Breathing Patient

In the early stages of ARDS the hypoxia may be
corrected by 40 to 60 inspired oxygen with CPAP
Peak inspiratory flow rates of gt 70ltrs / min
require a tight-fitting face mask with a large
reservoir bag or a high flow generator
If the patient is well oxygenated on lt 60
inspired oxygen and apparently stable without CO2
retention and apparently stable, then ward
monitoring may be feasible but close observation(
15 to 30 Min), continuous oximetry, and regular
blood gases are required

Contd..
15
Indications for mechanical ventilation

Inadequate Oxygenation(PaO2 lt 8k Pa on FiO2 gt
0.6)
Rising or elevated PaCO2(gt 6k Pa)
Clinical signs of incipient respiratory failure

16
Mechanical Ventilation
The Aims are to increase PaO2 while minimizing
the risk of further lung injury (Oxygen toxicity,
Barotrauma). This is the realm of the IRCU
Physician seek specialist advice early to
prevent complications. The general principles are
the following
Contd..
17

Start with FiO2 1.0, tidal volume 6 to 10 ml
per Kg, PEEP lt 5 cm H2O and inspiratory flow
rates 60 L / min. Subsequent adjustments are
done to try to achieve arterial oxygen sats. of gt
90 with FiO2 lt 0.6 and peak airway pressures lt
40 to 45 cm H20
Controlled Mandatory Ventilation (CMV) with
sedation and neuromuscular blockade (to try to
suppress the respiratory drive and reduce
respiratory muscle oxygen requirement.)

PEEP improves PaO2 in most patients and allows
reduction of FiO2. Increase by 2 to 5 cm H2O
increments every 20 min watching for hemodynamic
deterioration (due to impaired venous return and
decreased cardiac out put). Optimal PEEP is
usually 10 to 15 cm H2O
Inverse Ratio Ventilation may decrease peek
inflation pressures and thus Barotrauma.
Inspiratory time Expiratory time ratio (IE
ratio) of between 11 and 41 may be tried.

Contd..
19

The ventilatory rate required to clear CO2 and
normalize pH is commonly high (20 to 25 breaths /
min). However this may result in unacceptable
airway pressures.
Another strategy is permissive hypercapnoea
which as the name suggests is controlled
hypoventilation. PaCO2 up to 13 kPa is generally
well tolerated acidosis (pH lt 7.25) may be
treated with intravenous bicarbonate

Changing the patients position (lateral decubitus
or prone instead of supine) can improve
oxygenation by improving perfusion of aerated
portion of lung. Consider this in patients with
non uniform or predominantly posterior and lower
lobe infiltrates
Inhaled nitric oxide (18 ppm) reduces pulmonary
artery pressures, intra pulmonary shunting and
improves oxygenation while not affecting mean
arterial pressure or cardiac output. However
studies showing an effect on mortality are
awaited.
Newer methods such as high frequency jet
ventilation, extra corporeal gas exchange (CO2
removal - Oxygenation) and intravascular
oxygenation devices (IVOX) may be of use but are
currently not widely available.

21
Cardiovascular Support
22

Invasive monitoring is mandatory(Arterial line,
PA catheter (Swan-Ganz) to measure cardiac
outputs and if available, continuous mixed venous
oxygen saturation)
In order to minimize pulmonary oedema, aim to
keep PCWP low (8 to 10 mm Hg) and support the
circulation with inotropes if necessary
The role of colloids and albumin is relatively
minor the increased capillary permeability
allows these molecules to equilibrate with the
alveolar fluid with little increase in net plasma
oncotic pressure

Contd..
23

Renal failure is common and may require
haemofiltration to achieve a negative fluid
balance and normalize blood chemistry.
Oxygen consumption (VO2) in patients with ARDS
appears to be delivery dependent. The current
trend is to aim for target levels of oxygen
delivery (DO2 Cardiac Index(HbXSao2X1.34)X10)
as guided by tissue perfusion (clinically and
serum lactate, pHi from a gastric tonometer). DO2
may be increased by blood transfusion, inotropes
and vasodilators including prostacyclin).

Selection of appropriate inotropes and
vasodilators can only be made by repeated
measurements of haemodynamic parameters and
calculating DO2 and VO2 while evaluating the
effects of the various agents
Nutritional support must be chosen to try to
avoid fluid overload. Lipid metabolism produces
marginally less CO2 than dextrose metabolism and
thus favourably affects the respiratory quotient
but there is controversy as to whether lipid can
exacerbate lung injury

25
Treatment of Sepsis
26

Fever, Neutrophil leukocytosis and raised
inflammatory markers (CRP) are common in
patients with ARDS and do not always imply
sepsis. However sepsis is common precipitant of
ARDS
A trial of empirical antibiotics guided by
possible pathogens should be given early. Eg
Cefotaxime. This may be modified in light of the
results of appropriate cultures. Avoid
nephrotoxic antibiotics.
Enteral feeding seems to carry a lower risk of
sepsis than parenteral feeding and helps maintain
the integrity of the gut mucosa. Ileus is common
in multi-organ failure, so entral feeding may not
be possible.

27
Minimizing lung injury and treating the cause
28

Look for a precipitant
In general prevention (example of aspiration of
gastric acid) is more effective than trying to
treat ARDS. However there are no effective
measures for prophylaxis in patients at risk ( Eg
from Trauma)
Steroids there is no benefit from treatment
early in the disease. Treatment later (gt 7
to 14 days from onset) especially in patients
with peripheral blood eosinophilia or eosinophils
in bronchoalveolar lavage, improves prognosis

Give 2 to 4 mg / Kg prednisolone or equivalent
the duration depends on the clinical response( 1
to 3 weeks)
Other therapies such as inhaled nitric oxide ,
exogenous surfactant, antioxidants
(acetylcysteine), ketoconazole, NSAIDs,
Pentoxifylline and anticytokine antibodies are
still under investigation

30
Causes of Sudden deterioration in ARDS
Respiratory Cardiovascular
Pneumothorax Arrhythmia
Bronchial plugging Cardiac tamponade
Displaced ET tube Myocardial infarction
Pleural effusion (Haemothorax) GI bleed(Stress Ulcer)
Aspiration(Eg NG feed) Septicaemia
31
Completed trials