10. Respiratory

Question 1

What is decompression sickness?

Answer 1

Increased partial pressure at below sea level leads to diffusion of nitrogen from lungs into blood so if the diver ascends too quickly the rapid change in pressure causes bubble formation leading to tissue damage and pain.

Question 2

What is respiratory distress syndrome?

Answer 2

Loss of surfactant upsets Laplace’s law and surface tension of small alveoli isn’t kept low so there is alveolar collapse due to pressure differences in different sized alveoli. Less surface area for gas exchange and respiratory failure.

Question 3

How is respiratory distress syndrome in premature babies managed?

Answer 3

Mum is given steroid injections to stimulate surfactant generation if anticipated.

Question 4

How is carbon monoxide poisonous?

Answer 4

CO binds to haemoglobin and forms carboxyhaemoglobin so haemoglobin has less space to bind to O2 and also has greater affinity so won’t deliver O2.

Question 5

What are the results of acute and chronic carbon monoxide poisoning?

Answer 5

Acute - death.

Chronic - headaches, confusion, nausea etc.

Question 6

How is carbon monoxide treated?

Answer 6

Hyperbaric O2 therapy - O2 concentration high enough to displace CO and restore haemoglobin function.

Question 7

What is pulmonary embolism?

Answer 7

Thrombus from a site other than the lungs lodges in one of the arteries of the pulmonary tree.

Question 8

What are the effects of pulmonary embolism?

Answer 8

V/Q mismatch in the section of lung the artery supplies so pO2 of the blood leaving that section is normal but pCO2 is low as no new blood enters so has longer to equilibrate with alveolar air. The health lung is overloaded due to blood being redirected there. Too much blood means inefficient exchange of pO2 - blood has low pO2 and normal pCO2. Overall, there is type I respiratory respiratory failure.

Question 9

What is the fatal danger of a pulmonary embolism?

Answer 9

Sudden pulmonary hypertension causes mechanical shock from RV failure in the heart.

Question 10

How is hypercapnia from V/Q mismatch in pulmonary emboli corrected?

Answer 10

Increased respiratory rate.

Question 11

What are the types of respiratory failure?

Answer 11

Type I - pO2 low, pCO2 normal or low.

Type II - pO2 low, pCO2 high.

Question 12

What is type I respiratory failure caused by?

Answer 12

Diffusion defect or V/Q mismatch.

Question 13

What diffusion defects can cause type I respiratory failure?

Answer 13

Pulmonary oedema - fluid in alveoli so increased diffusion distance.
Emphysema - decreased compliance of lungs causing hyperexpansion and reduced surface area for gas exchange.
Pulmonary fibrosis - fibrous deposits between alveolus and capillary basement membrane so increased diffusion distance.

Question 14

What is type II respiratory failure caused by?

Answer 14

Decreased respiratory effort, chest wall defects, decreased compliance, extremely high airway resistance.

Question 15

What can decrease respiratory effort and hence cause type II respiratory failure?

Answer 15

Narcotics/head injuries/neurological deficits impact ability of respiratory centre. Muscular dysfunction anywhere from the brain to the NMJ (MS, Duchenne’s muscular dystrophy etc).

Question 16

What chest wall defects can cause type II respiratory failure?

Answer 16

Rigid structure means it’s harder to move and inflate the lungs. Severe scoliosis/kyphosis, severe pectum excavatum/carranatum, flail chest (multi-rib fracture), tension pneumothorax.

Question 17

What can cause decreased compliance that causes type II respiratory failure?

Answer 17

Severe pulmonary fibrosis.

Question 18

What causes increased airway resistance that leads to type II respiratory failure?

Answer 18

Severe life threatening asthma attack, acute exacerbation of late-stage COPD.

Question 19

What is asthma?

Answer 19

A reversible airway obstruction.

Question 20

What is the pathophysiology of asthma?

Answer 20

Airway remodelling: increased airway smooth muscle thickness; damaged epithelia/basement membrane from chronic inflammation from reaction to allergens. Contraction of smooth muscles, due to histamine and prostaglandin release in response to stimuli, increase airway resistance so less air is expired initially.

Question 21

What is a hypothesis that could explain why asthma is so prevalent in the Western world?

Answer 21

Hygiene hypothesis - overuse of cleaning chemicals means immune system is less trained for harmless bacteria so hyperactive.

Question 22

What are the types of asthma?

Answer 22

Allergic, viral - disappears by 5 years, occupational asthma.

Question 23

What are the features of a history leading to an asthma diagnosis?

Answer 23

Expiratory, polyphonic wheeze; dry cough with diurnal variation (worse at night) - induced by exercise; breathlessness; chest tightness; reversed with B2 agonists.

Question 24

What are the features of examination leading to an asthma diagnosis?

Answer 24

Eczema; lethargy and uncomfortable at rest; below heigh for age and underweight; laboured breathing signs - Harrison’s sulcus (indrawing of costal cartilages), tracheal tug, subcostal recession, obvious use of accessory muscles of inspiration.

Question 25

What are the features of investigation leading to an asthma diagnosis?

Answer 25

Primary - PEFR reduces, single breath spirometry FEV1:FVC >70% but reversed with salbutamol.
Supportive (optional) - FENO high levels of NO, skin prick sensitivity to allergens, chest X ray excludes other causes.

Question 26

What is the long term treatment for asthma?

Answer 26

Lifestyle - minimise exposure to allergens, exercise, fresh air.
Pharmacological - relievers: B2 agonists salbutamol and M3 antagonists ipratropium, preventers: low dose corticosteroids to suppress local immune function.

Question 27

How is an asthma attack recognised?

Answer 27

Poor respiratory effort/loud wheeze/silent chest; panicked, agitated, sympathetic features - sweating, dry mouth, dilated pupils, nausea; altered GCS (cerebral hypoxia); O2 saturation <92% with peripheral cyanosis; pO2 low and pCO2 normal or rising.

Question 28

How is an asthma attack managed?

Answer 28

High flow 100% O2, nebulised salbutamol and ipratropium continuously, IV salbutamol, aminophylline (smooth muscle relaxation in airways), and magnesium sulphate (no smooth muscle contraction in airways).

Question 29

What is chronic obstructive pulmonary disease?

Answer 29

Progressive, worsening airway obstruction. An umbrella for chronic bronchitis and emphysema.

Question 30

What is chronic bronchitis?

Answer 30

Mucus hypersecretion and inflammation due to cigarette smoke.

Question 31

What are the features of chronic bronchitis?

Answer 31

Cough chronically productive with frequent infections. Airway remodelling to increase arterial smooth muscle.

Question 32

What is emphysema?

Answer 32

Pathological destruction of terminal bronchioles and walls between alveoli.

Question 33

What is the pathophysiology of emphysema?

Answer 33

Inflammatory response to chronic irritation from cigarette smoke causes macrophages to release elastase and other proteolytic enzymes so breaks down elastin. Redundant bullae form and collapse on expiration due to loss of supportive tissue so obstruct.

Question 34

What are the features of emphysema?

Answer 34

Fick’s law - less surface area for diffusion so impaired gas exchange. Less elastin lowers compliance so there is hyperinflation of lungs, causing barrel chest.

Question 35

What are the causes of COPD?

Answer 35

Smoking mainly, a1-antitrypsin deficiency (hereditary leading to overactivity of elastase causing emphysema), pollution, occupational.

Question 36

How do the stages of COPD present?

Answer 36

Early - productive cough, dyspnoea, tachypnea.
Middle - purse lip breathing, use of accessory muscles to inspire, barrel chesting.
Late - compensated respiratory acidosis (CO2 retention), wheeze, peripheral and central cyanosis, flapping tremor, pulmonary hypertension.

Question 37

How is COPD diagnosed?

Answer 37

History used primarily but single breath spirometry and other tests can support diagnosis.

Question 38

What single breath spirometry results support COPD diagnoses?

Answer 38

FEV1:FVC ratio affected without reversibility.
Mild 50-80%
Moderate 30-49%
Severe <30%

Question 39

What tests support diagnosis of COPD?

Answer 39

CXR excludes other differential, CT assesses bullae in emphysema, ABG checks acid/base status, a1-antitrypsin blood test in young non-smoker.

Question 40

What assesses COPD prognosis?

Answer 40

MRC dyspnoea score assesses amount of exertion that causes breathlessness:
1 - strenuous exercise
2 - hurrying or walking up hill
3 - walking at own pace
4 - 100m walking
5 - getting dressed

Question 41

What lifestyle modifications are made to manage COPD?

Answer 41

Stop smoking (KEY), moderate exercise if MRC allows it, manage other co-morbidities.

Question 42

What are the pharmacological interventions that are used to manage COPD?

Answer 42

B2 agonists, e.g. salbutamol, for bronchodilation but also causes systemic effects like tachycardia.
M3 antagonists, e.g. ipratropium, for bronchodilation but side effects like dry mouth and nausea.
Aminophylline for bronchodilation from inhibits phosphodiesterase so more cAMP and PKA so MLCK phosphorylated. Also increases respiratory drive and power.
Oral corticosteroids to reduce inflammation to improve chronic bronchitis.
Mucolytics thin the mucus so easier airway clearance.

Question 43

What are some non-pharmacological interventions used in COPD management?

Answer 43

Pulmonary rehab - breaks cycle of breathlessness.
Long term O2 therapy - need 16 hours a day, no smoking around it due to flamability.
Pneumonectomy - remove damaged lung lobe so FEV1 increased and V/Q mismatch is corrected but less surface area for gas exchange.

Question 44

What are the investigation performed in acute exacerbations of COPD?

Answer 44

Pulse oximetry, ABG, sputum culture, CRP, U&Es, FBC, CXR.

Question 45

What is the management of acute exacerbations of COPD?

Answer 45

Titrated O2 therapy to get O2 sats above 88%.
Salbutamol, atrovent, aminophylline.
High dose steroids if non-infectious.
Non-invasive ventilation if conscious.

Question 46

What are upper respiratory tract infections?

Answer 46

Acute inflammation of the middle airways, nothing sinister in most cases and usually viral.

Question 47

What is the presentation of URTIs?

Answer 47

Dyspnoea, productive cough, fever, malaise. Associated with sinusitis and otitis media due to connections to nasal cavity.

Question 48

What is the CXR of URTIs?

Answer 48

Clear as only middle airways affected.

Question 49

What is pneumonia?

Answer 49

A lower respiratory tract infection with inflammation of the lung alveoli. It impairs gas exchange and causes type I respiratory failure if unchecked.

Question 50

How is pneumonia classified?

Answer 50

Place of acquiring - community or hospital.
Presentation - acute or chronic.
Organism - bacterial, viral, or fungal.
Pathology - lobar, broncho, or interstitial.

Question 51

What are the symptoms of pneumonia?

Answer 51

Productive cough, fever, malaise, rigors, pleuritic chest pain, nausea and vomiting.

Question 52

What are the signs of pneumonia?

Answer 52

Pyrexia, tachycardia, tachypnea, cyanosis, dullness to percussion, bronchial breathing, pulmonary crackles.

Question 53

What are the investigations for pneumonia?

Answer 53

Bloods - FBC, CRP, U&Es, lactate, culture.
Erect CXR (shows consolidation in affected lobe), sputum culture.

Question 54

How is the management plan for pneumonia decided?

Answer 54

Using CURB-65 score: confusion, urea >7mmol/L, respiratory rate >30/min, BP <90/60, age >65 years.
If score over 1 - severe and needs hospital admission.
If score 1 or 0 - moderate pneumonia so care in the community.

Question 55

How are hospital admitted pneumonia patients treated?

Answer 55

Co-amoxiclav and clarithromycin given. B2 agonists/M2 antagonists particularly in asthmatics. High flow O2.

Question 56

How are community cared for pneumonia patients treated?

Answer 56

Amoxicillin as probably streptococcus pneumoniae.

Question 57

What are the sequelae of pneumonia?

Answer 57

Resolution with minimal scarring so normal lung function. Lung abscess formation that ruptures and cause empyema. Bronchiectasis (permanent dilation of bronchioles). Septicaemia or meningitis. Death from type I respiratory failure.

Question 58

What are the atypical causes of pneumonia with their treatment?

Answer 58

Gram negative bacteria: legionella, chlamydia.

Treat with macrolides (clarithromycin) or tetracyclines (doxycycline).

Question 59

What are the viral causes of pneumonia?

Answer 59

Adenovirus, respiratory synctial virus, influenza.

Question 60

What is the presentation of viral pneumonia?

Answer 60

Severe, haemorrhage into lung parenchyma, patchy diffuse ground glass appearance on CXR.

Question 61

How is hospital acquired pneumonia treated?

Answer 61

Co-amoxiclav as normally staph. aureus, tazocin if no improvement.

Question 62

What is aspiration pneumonia?

Answer 62

Contents of the GI tract end up in the lungs due to compromise to epiglottis/larynx as protective mechanisms.

Question 63

What is the normal cause and treatment for aspiration pneumonia?

Answer 63

Viridans streptococci and other anaerobes. Co-amoxiclav as first line.

Question 64

What are the causes of immunosuppressive pneumonia?

Answer 64

PCP, TB, other mcyobacteria, aspergillus, cytomegalovirus.

Question 65

How do splenectomies affect risk of pneumonia?

Answer 65

Patient at increased risk of colonisation by strep. pneumonia, H.influenzae etc. so have immunosuppressive pneumonia but with normal pathogens.

Question 66

What is tuberculosis?

Answer 66

Bacterial infection of the lungs by mycobacterium tuberculosis, or M. bovis, or other mycobacteria.

Question 67

What are the features of mycobacterium tuberculosis that make it a good invader?

Answer 67

Mycolic acid coating gives it structural rigidity and makes it hard for antibiotics to penetrate. Non-motile and obligate aerobe so colonises upper lobes normally. Transmitted via respiratory droplets but not very infectious so need chronic exposure.

Question 68

What is the pathogenesis of tuberculosis?

Answer 68

Initially phagocytosed by alveolar macrophages but not destroyed due to mycolic acid coat. So drains to lymph nodes to form Ghon focus with local inflammation and local lymph node involvement.

Question 69

What is latent TB?

Answer 69

The Ghon focus is contained and usually self heals but bacteria stay present in small numbers so can activate.

Question 70

What are the risk factors for activation of latent TB?

Answer 70

Immunocompromised, diabetes, kidney disease, etc.

Question 71

What is active TB?

Answer 71

Bacteria multiply and this manifests as symptoms of the disease.
Primary - direct progression from initial Ghon focus (5%)
Secondary (<5 years) and reactivation (>5 years) - re-emergence of bacteria despite initial containment of Ghon focus (95%).

Question 72

How do INF gamma blood tests and sputum culture results differ in latent and active TB?

Answer 72

INF gamma blood - positive in latent and in active.

Sputum cultue - negative in latent, positive in active.

Question 73

What are the features of TB granulomas?

Answer 73

Immune granuloma made of lymphocytes, Langhan’s giant cells, epitheloids. Central caseous necrosis.

Question 74

What is the presentation of TB?

Answer 74

Risk factors from history: migrant to UK, low socio-economic status, HIV, close contact with relatives with TB.
Symptoms: fever and night sweats, anorexia and resultant cachexia, fatigue/malaise, productive cough, dyspnoea.
Signs: occasional pulmonary creackles, signs of cavitation/fibrosis (dull percussion), effusion signs (stony dulness in percussion).

Question 75

What are the investigations of TB?

Answer 75

CXR where apices of lung have patchy consolidation with central cavitation.
Sputum analysis with ZN stain to look for acid fast bacteria.
Sputum cultures takes 1-3 weeks.
Check exposure to TB: Mantoux test intradermal infection that forms lump if encountered TB, interferon gamma releasing array detects antigen specific INF gamma.

Question 76

How is TB treated?

Answer 76

RIPE:
Rifampicin for four-six months, interferes with TB RNA synthesis, but hepatotoxic and turns body secretions orange.
Isoniazid for four-six months, breaks down mycolic acid shell so rifampicin can access TB, but hepatotoxic and peripheral neuropathy.
Pyranzinamide for two months, inhibits trans-translation by binding ribosomes, but hepatotoxic.
Ethambutol for two months, obstructs cell wall formation, but visual disturbances.

Question 77

What is atypical TB?

Answer 77

Not normal pulmonary TB that is susceptible to RIPE protocol, it’s resistant (MDR to rifampicin and isoniazid, XDR to all fluoroquinolones and some of protocol), or miliary TB (diffuse through body from bacteraemia), extrapulmonary TB (from miliary TB or unique infection).

Question 78

How is TB prevented?

Answer 78

Notifiable disease. BCG is 70-80% effective in preventing severe childhood TB, little evidence for preventing adult TB so only high risk. Barrier medicine - negative pressure isolation and limit number of different staff dealing with patient.

Question 79

What are the risk factors of lung cancer?

Answer 79

Smoking, asbestos (mesothelioma), radon, genetics/familial factors, occupational carcinogens.

Question 80

How is lung cancer staged?

Answer 80

TNM staging.
T1/2, N0, M0 = stage I.
T3/4, N0, M0 = stage II,
Any T, N1 or N2, M0 = stage III.
Any T, any N, M1 = stage IV.

Question 81

What are the T stages of lung cancer?

Answer 81

T1a <2cm
T1b 2-3cm
T2a 3-5cm
T2b 5-7cm
T3 >7cm
T4 any

Question 82

What are the N stages of lung cancer?

Answer 82

N1 = ipsilateral hilar lymph node
N2 = ipsilateral mediastinal lymph node
N3 = contralateral lymph node (hilar or mediastinal)

Question 83

What are the symptoms of lung cancer?

Answer 83

Direct: none, cough/haemoptysis, dyspnoea, wheezing, chest pain, recurrent chest infections.
Local metastatic: bloated face, dyspnoea, dysphagia, hoarse voice, Horner’s syndrome.
Systemic metastatic: pathological bone fracture, headaches, double vision, thirst and constipation, seizures.

Question 84

What are the signs of lung cancer?

Answer 84

Elevated non-pulsatile JVP, clubbing, no signs (commonest).

Paraneoplastic syndromes: Cushing’s if small cell, SIADH.

Question 85

What are the investigations of lung cancer?

Answer 85

Erect CXR, staging CT with or without contrast, PET scan, MRI, ultrasounds scan, biopsy to check malignancy, tumour screening for molecular markers - e.g. EGFR mutations.

Question 86

How is the management strategy of lung cancer decided?

Answer 86

MDT to deal with it. Based on performance status grade: 0=fully active, 1=restricted by intensive work, 2=up and about >50% of time, 3=limited self care ambulatory <50% of time, 4=bed/chair bound, 5=dead. 0-2 have surgery, 3+ get palliative care.

Question 87

What are the treatment options for lung cancer?

Answer 87

Surgery - for non-small cell, only 25% are operable.
Radiotherapy - radical is curative option, palliative for symptom control.
Chemotherapy - potentially curative in small cell, palliative in non-small cell.
Palliative - >2 WHO grade, analgesia, patient support, low dose radiotherapy/chemotherapy.

Question 88

What are the features of addiction?

Answer 88

Continued used despite knowledge of negative consequences, craving during abstinence, failure to stop, denial.

Question 89

What is the physiology of nicotine addiction?

Answer 89

NAChR stimulated to cause dopamine release so feel satisfied. Increased use leads to upregulation of receptors so more nicotine is needed for the same hit, so craving increases. Drop in nicotine leads to cravings and withdrawal.

Question 90

How should nicotine addiction be managed?

Answer 90

Quitting:
- ask do you smoke, advice them to stop, act refer to NHS stop smoking services
- nicotine replacement therapy (twice as likely to quit)
- varenicline - partial NAChR agonist
Harm reduction:
- cutting down
- E-cigarettes

Question 91

What is interstitial lung disease?

Answer 91

An umbrella term for the disease processes that affect the parenchyma between the alveoli.

Question 92

What are the types of interstitial lung disease?

Answer 92

Idiopathic pulmonary fibrosis, asbestosis, drug induced, connective tissue disorders, extrinsic allergic alveolitits, sarcoidosis.

Question 93

What are the features and treatment of idiopathic pulmonary fibrosis?

Answer 93

Cause unknown, in >80 year olds, treat with pirfenidine (bad side effects).

Question 94

What are the features of asbestosis?

Answer 94

From asbestos exposure, formation of asbestos plaques and thickening of interstitium and can lead to mesothelioma, rounded atelectasis, and bronchogenic lung cancer.

Question 95

What are the drugs that lead to drug induced interstitial lung disease?

Answer 95

Exposure for over 10 years to cause it: methotrexate, bleomycin, amiodarone, nitrofurantoin amongst others.

Question 96

What are the connective tissue disorders that can cause interstitial lung disease?

Answer 96

Lupus, scleroderma, rheumatoid arthritis, polymyositis, Sjogren’s syndrome.

Question 97

What are the type of extrinsic allergic alveolitis?

Answer 97

Acute - farmer’s lung, from thermophilic actinomyocytes in hay, inspiratory crackles.
Chronic - pigeon fancier’s lung, from chronic immune response to antigens from pigeons so granulomas form with inspiratory crackles.

Question 98

How is sarcoidosis treated?

Answer 98

High dose steroids to dampen immune system.

Question 99

What are the patient features of interstitial lung disease?

Answer 99

Older, smokers, previous exposure to respiratory toxins, non-productive cough, dyspnoea, canosis, tachycardia, tachypnea, reduced SaO2, velcro crackles, clubbing, signs of cor pulmonale, ABG low O2 and low or high (late stage) pCO2, restrictive spirometry.

Question 100

What is pleural effusion?

Answer 100

Collection of some types of fluid between the layers of the pleura.

Question 101

What is the pathogenesis of pleural effusion?

Answer 101

Increased production - hydrostatic pressure increase (hypertension), permability increase (sepsis), oncotic pressure decrease (cirrhosis).
Decreased clearance - lymphatic blockage (tumour), increased venous pressure (right sided heart failure).

Question 102

What is the difference between transudate and exudate in terms of causes of pleural effusion?

Answer 102

Exudate has high serum protein and high serum LDH and is caused by infection, malignancy, pancreatitis, sepsis etc.
Transudate has low serum protein, and low serum LDG and is caused by anything that affects Starling’s forces - left sided heart failure, cirrhosis, kwashiorkor, atelectasis, hypertension.

Question 103

What are the symptoms and signs of pleural effusion?

Answer 103

Breathlessness, pleuritic chest pain, stony dullness to percussion, coarse crackles, dry cough, paroxsymal nocturnal dyspnoea.

Question 104

What are the less common types of pleural effusion?

Answer 104

Haemothorax - blood.
Empyema - acidosis from infection, systemically unwell.
Chylothorax - lymphatic fluid.

Question 105

How is pleural effusion treated?

Answer 105

Thoracentesis to acquire fluid and test appearance to determine route cause.
Drain fluid, chemical pleurodesis to unite pleura together, surgery rarely.

Question 106

What is a pneumothorax?

Answer 106

Air within the pleural space.

Question 107

What are the types and causes of pneumothoraces?

Answer 107

Primary - in healthy patients, lanky and smokers.
Secondary - unferlying respiratory pathology.
Iatrogenic - central line etc.

Question 108

What is the presentation of pneumothoraces?

Answer 108

Pleuritic chest pain and dyspnoea. Reduced air entry on one side and hyperresonance in affected area of lung.

Question 109

How is a pneumothorax investigated?

Answer 109

Erect CXR - blackout where air is. If >2cm - large, if <2cm - small.

Question 110

How are pneumothaces treated?

Answer 110

Small - leave it if no SOB.
Large or any size with SOB - simple needle aspiration, chest drain, chemical pleurodesis (last resort if surgery contraindicative), surgical pleurectomy.

Question 111

What are the consequences of a pneumothorax?

Answer 111

Discharge whenever stable with a primary pneumothorax or after 24hrs of stable observations.
Can’t fly until CXR shows complete resolution after 6+ weeks.
Diving avoided unless bilateral pleurectomy.

Question 112

What is a tension pneumothorax?

Answer 112

Huge pneumothorax that is large enough to cause mediastinal deviation and compress great vessels, leading to circulatory compromise.

Question 113

What are the signs of tension pneumothorax?

Answer 113

Almost absent chest movement, hyper resonance, tracheal deviation away from affected side, hypoxia signs, early signs of mechanical shock.

Question 114

What is the treatment of tension pneumothoraces?

Answer 114

Emergency needle decompression, O2, chest drain, cardiothoracic surgical referral.

Question 115

What is chest wall disease?

Answer 115

Any disease that distorts the shape of the thoracic cage and/or impact respiratory function.

Question 116

What are the types of chest wall disease?

Answer 116

Congenital - pectus deformity, scoliosis, kyphosis, muscular dystrophy etc.
Acquired - trauma, iatrogenic, ankylosing spondylosis.

Question 117

What is the presentation of chest wall disease?

Answer 117

Decreased ability to clear secretions through the coughing reflex so recurrent infections. Sleep discorded breathing - paroxysmal nocturnal dyspnoea. If severe, hypoventilation so type II respiratory failure.