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2a high tier > Respiratory > Flashcards

Respiratory Flashcards

1
Q

What is the pathophysiology of COPD?

A
  • Increased numbers of mucus-secreting goblet cells within the bronchial mucosa, especially in the larger bronchi
  • In advanced cases, the bronchi become overtly inflamed and pus in seen in the lumen
  • Most have emphysema and chronic bronchitis and the combination of these severely limits airflow
  • V/Q mismatch from damage and mucus plugging
  • Cigarette smoke causes mucus gland hypertrophy in larger airways, leading to an increase in neutrophils, macrophages and lymphocytes in the airways
  • These cells release inflammatory mediator, attracting inflammatory cells, inducing structural changes and breaking down connective tissue in the lung → emphysema
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2
Q

What are the risk factors of COPD?

A
  • CIGARETTE SMOKING
  • Pollutants at work (mining, building and chemical industries)
  • Outdoor air pollution
  • Inhalation of smoke from biomass fuels
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3
Q

What is the clinical presentation of COPD?

A
  • Characteristic symptoms are productive cough with white or clear sputum, wheeze and breathlessness (usually follows many years of a smoker’s cough)
  • Colds seem to settle on the chest and frequent infective exacerbations occur with purulent sputum (contains pus)
  • Symptoms worsened by cold or damp weather and atmospheric pollution
  • Systemic effects: hypertension, osteoporosis, depression, weight loss, reduced muscle mass with general weakness
  • Severe disease = breathless at rest with prolonged expiration, poor chest expansion and hyperinflated lungs (barrel chest)
  • Pursed lips on expiration (helps to prevent airway collapse)
  • Later stages are characterised by respiratory failure
  • May develop pulmonary hypertension in advanced disease
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4
Q

What are the differential diagnoses of COPD?

A
  • Asthma
  • Congestive heart failure
  • Bronchiectasis
  • Allergic fibrosing alveolitis
  • Pneumoconiosis
  • Asbestosis
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5
Q

How is COPD diagnosed?

A
  • Based on a history of breathlessness and sputum production in a chronic smoker
  • If there is no history of smoking, it’s more likely to be asthma unless there’s a family history suggesting alpha-1 antitrypsin deficiency
  • Lung function tests show progressive airflow limitation with increasing severity and breathlessness
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6
Q

How is COPD managed?

A
  • SMOKING CESSATION
  • Bronchodilators: inhaled tiotropium bromide with salbutamol
  • Corticosteroids in symptomatic patients with moderate/severe COPD  prednisolone daily
  • Oxygen therapy
  • Antimucolytic agents can reduce sputum viscosity
  • Diuretics
  • Pulmonary rehabilitation to increase exercise capacity
  • Good diet to reduce weight
  • Alpha-1 antitrypsin replacement
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7
Q

What is the pathophysiology of chronic bronchitis?

A
  • Airway narrowing and airway limitation from hypertrophy and hyperplasia of mucus secreting glands of the bronchial tree, bronchial wall inflammation and mucosal oedema
  • Infiltration of the bronchi/bronchiole walls with acute and chronic inflammatory cells
  • Epithelial layer becomes ulcerated and eventually squamous epithelium replaces the columnar cells (=squamous metaplasia) when the ulcer heals
  • Inflammation is followed by scarring and thickening of the walls, narrowing the small airways
  • Small airways are particularly affected in early disease
  • Initial inflammation is reversible so improvement in airway function can happen is smoking is stopped early (in later stages, inflammation continues even if smoking is stopped)
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8
Q

What is the classic clinical presentation of chronic bronchitis?

A
  • ‘Blue bloaters’
  • Cough with phlegm
  • Cor pulmonale
  • Respiratory failure (usually T2)
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9
Q

What is the pathophysiology of emphysema?

A
  • Dilatation and destruction of the lung tissue distal to the terminal bronchioles
  • Results in loss of elastic recoil, causing expiratory airflow limitation and air trapping
  • Premature closure of airways limits expiratory flow while the loss of alveoli decrease capacity for gas transfer
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10
Q

What is the classic clinical presentation of emphysema?

A
  • ‘Pink puffers’
  • Weight loss
  • Breathless
  • Maintained pO2
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11
Q

What is the aetiology of asthma?

  1. Allergic/ eosinophilic
  2. Non allergic/ non-eosinophilic
  3. Genetic factors
  4. Environmental factors
A

Two main categories:

  • Atopy: IgE antibodies readily produced against common exposures.
  • Increased responsiveness of airways to inhaled stimuli: histamine and methacholine

ALLERGIC/ EOSINOPHILIC:
- Allergens (e.g. fungal allergens and pets etc) and atopy

NON-ALLERGIC/ NON-EOSINOPHILIC:

  • Exercise, cold air and stress
  • Smoking and non-smoking associated
  • Obesity associated

GENETIC FACTORS:

  • No single gene, but several genes in combination with environmental factors
  • Genes controlling the production of different cytokines
  • ADAM33 is associated with hyper-responsiveness and tissue remodelling

ENVIRONMENTAL FACTORS:

  • Early childhood exposure to allergens and maternal smoking has a major influence on IgE production
  • Growing up in a ‘clean’ environment may predispose towards an IgE response to allergens
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12
Q

What is the pathophysiology of asthma? (Inflammation and muscular changes)

A

INFLAMMATION:

  • Triggers cause an inflammatory cascade in the bronchial tree
  • Mast cells, eosinophils, T lymphocytes and dendritic cells increased in bronchial wall, membranes and secretions
  • Lymphocytes produce ILs to start cascade → IgE produced

MUSCULAR:

  • Increased contraction of smooth muscle in bronchial wall
  • Remodelling causes more muscle mass in wall and increased number of goblet cells
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13
Q

What are the risk factors of asthma?

A
  • Personal history of atopy
  • Family history of asthma or atopy
  • Obesity
  • Inner-city environment
  • Premature birth, socio-economic deprivation
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14
Q

What is the clinical presentation of asthma?

General, during attack, uncontrolled attack, severe attack, life threatening attack

A
  • Intermittent dyspnoea
  • Wheeze
  • Cough (especially nocturnal)
  • Sputum
  • Symptoms worse at night
  • Episodic shortness of breath
  • Provoking factors: allergens, infection, menstrual cycle, exercise, cold air

DURING ATTACK:

  • There is reduced chest expansion
  • Prolonged expiratory time
  • Bilateral expiratory polyphonic wheezes
  • Tachypnoea

UNCONTROLLED ATTACK:

  • PEFR < 50% expected
  • Resp rate < 25/m
  • Pulse < 110bpm
  • Normal speech

SEVERE ATTACK:

  • Inability to complete sentences
  • Pulse > 110bpm
  • Resp rate > 25/m

LIFE-TREATENING ATTACK:

  • Silent chest
  • Confusion and exhaustion
  • Cyanosis (PaO2 < 8kPa)
  • Bradycardia
  • PEFR < 33%
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15
Q

What are the differential diagnoses of asthma?

A
  • Pulmonary oedema
  • COPD (may co-exist)
  • Large airway obstruction caused by a foreign body/ tumour
  • Pneumothorax
  • Bronchiectasis
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16
Q

How is asthma diagnosed?

A
  • History and evidence of obstruction (PEF/ spirometry) during episodes
  • RCP3 questions: recent nocturnal waking, usual symptoms in a day, interference with activities of daily living
  • Lung function tests (PEFR, spirometry)
  • Exercise tests
  • Trial or corticosteroids
  • Exhaled nitric oxide (measure of eosinophilic inflammation)
  • Blood and sputum tests
  • Skin prick tests to identify allergens
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17
Q

How is asthma managed?

normal, non-emergency management

A
  • Avoid triggers
BRONCHODILATORS:
→ Beta2-agonists:
- SABA last 4h e.g. salbutamol
- LABA last 12h e.g. salmeterol
→ Muscarinic agents:
- SAMA e.g. ipratropium
- LAMA e.g. tiotropium
→ Methylxanthines:
- Theophylline

ANTI-INFLAMMATORY STEROIDS (inhaled corticosteroids)

  • For all patients with regular persistent symptoms
  • E.g. prednisolone, beclomethasone, budesonide
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18
Q

What is the immediate management for a life-threatening asthma attack?

A
  • Oxygen therapy to maintain O2 sat (94-98%)
  • Nebulised 5mg salbutamol (+ ipratropium if life threatening) – repeat/ IV infusion
  • Prednisolone (± IV hydrocortisone)
  • Take ABG and repeat within 2 hours if severe or if deteriorating
  • CXR if fails to respond to treatment
  • Check PEFR within 15-30m / regularly
  • Oximetry to ensure SaO2>92%
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19
Q

What is the aetiology of mesothelioma?

A

Asbestos exposure

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20
Q

What is the pathophysiology of mesothelioma?

A
  • High grade malignancy of the pleura that spreads around pleural surfaces
  • Can also start in the pericardial space, peritoneal space and paratesticular space
  • Tumour begins as nodules in the pleura which extend as a confluent sheet to surround the lung and extend into fissures
  • The chest wall if often invaded with infiltration of intercostal nerves, giving severe intractable pain
  • Lymphatics may be invaded, giving hilar node metastases
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21
Q

What is the main risk factor for mesothelioma?

A

Asbestos exposure

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22
Q

What is the clinical presentation of mesothelioma?

A
  • Chest pain
  • Dyspnoea
  • Weight loss
  • Finger clubbing
  • Recurrent pleural effusions
  • Breathlessness
  • Signs of metastases: lymphadenopathy, hepatomegaly, bone pain/tenderness, abdominal pain/obstruction
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23
Q

How is mesothelioma diagnosed?

A
  • CXR and CT: unilateral pleural effusion, pleural thickening
  • Blood/straw coloured pleural fluid
  • Pleural biopsy
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24
Q

How is mesothelioma managed?

A
  • Surgery for extremely localised mesothelioma
  • Generally resistant to surgery, chemotherapy and radiotherapy
  • Average time from diagnosis to death is 8m
  • Refer all mesothelioma deaths to HM coroner
  • Poor prognosis
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25
Q

What is the pathophysiology of a small cell lung carcinoma?

A
  • Often arises from endocrine cells in a central bronchus

- Secretes polypeptide hormones and have early development of widespread metastases

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26
Q

What is the pathophysiology of a squamous cell carcinoma (type of non-small cell lung carcinoma)?

A
  • Tumours are usually central in location and frequently cavitate with central necrosis
  • Arise from epithelial cells and are associated with keratin production
  • Cause obstructive lesions of bronchus with post-obstructive infection
  • Local spread common and metastases relatively late
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27
Q

What is the pathophysiology of an adenocarcinoma (type of non-small cell lung carcinoma)?

A
  • May be central or peripheral
  • Usually single lesions but they can arise in a multifocal pattern, sometimes bilaterally
  • Originate from mucus-secreting glandular cells
  • Most common type in non-smokers
  • Often cause peripheral lesions on CXR/ CT
  • Metastases common to pleura, lymph nodes, brain, bones and adrenal glands
    Carcinoid tumours:
  • Characteristic neuroendocrine secreting cells and relatively low rates of invasion and growth
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28
Q

What is the pathophysiology of lymphomas (type of non-small cell lung carcinoma)?

A
  • Involve the lung primarily but are usually a component of disseminated disease
  • Main lung lymphoma is a B cell lymphoma
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29
Q

What is the pathophysiology of benign non-small cell lung tumours (hamartomas)?

A
  • Irregular proliferations of benign/normal tissues not normally found in this pattern within the lung
  • Most common one in the lung is chondroid hamartoma
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30
Q

What are the risk factors for lung cancers?

general, occupational, environmental, host factors

A
  • Cigarette smoking (including passive smoking)
  • OCCUPATIONAL: asbestos, coal (and products of coal combustion), chromium, arsenic, nickel, petroleum products, iron oxide
  • ENVIRONMENTAL: radon exposure, ionising radiation
  • HOST FACTORS: pre-existing lung disease such as pulmonary fibrosis, HIV infection, genetic factors
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31
Q

What is the clinical presentation of lung cancers? (local and metastatic disease)

A

LOCAL DISEASE:

  • Cough
  • Breathlessness
  • Haemoptysis
  • Chest pain
  • Wheeze
  • Recurrent infections e.g. pneumonia
  • Clubbing

METASTATIC DISEASE:

  • Bone pain
  • Headache
  • Seizures
  • Neurological deficit
  • Hepatic pain
  • Abdominal pain
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32
Q

How are lung cancers diagnosed?

A
  • TNM classification
  • CXR: appear as round shadow, edge has a fluffy spiked appearance, hilar enlargement, consolidation, lung collapse, pleural effusion
  • CT for staging
  • Bronchoscopy to give histology and assess operability
  • Cytology for sputum and pleural fluid
  • Bloods: low FBC
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33
Q

How are small cell lung cancers managed?

A
  • Limited disease is treated with combined chemo and radiotherapy
  • Extensive disease treated with chemotherapy
  • Palliation to relieve symptoms; radiotherapy used for bronchial obstruction, haemoptysis, bone pain and cerebral metastases
  • Superior vena cava stent + radiotherapy + dexamethasone for superior vena cava obstruction
  • Endobronchial therapy used to treat symptoms of airway narrowing (tracheal stenting, cryotherapy, brachytherapy)
  • Pleural drainage for symptomatic relief
  • Drugs: analgesia, steroids, antiemetics, codeine, bronchodilators, antidepressants
34
Q

How are non-small cell lung cancers managed?

A
  • Surgical excision for peripheral tumours with no metastatic spread
  • Curative radiotherapy if respiratory reserve is poor
  • Chemo ± radiotherapy for more advanced disease
35
Q

What is the pathophysiology of a pulmonary embolism?

A
  • Circulatory stasis, endothelial injury and hypercoagulable state
  • Arise from venous thrombosis in the pelvis or legs, clots break up and pass through the IVC → right side of heart → pulmonary circulation
  • Becomes lodged in the small capillaries supplying the alveoli, causing a PE
  • After a PE, lung tissue is ventilated but not perfused, resulting in intrapulmonary dead space and impaired gas exchange
  • After a while, the non-perfused lung no longer produced surfactant, resulting in alveolar collapse, exaggerating hypoxaemia
36
Q

What are the risk factors of a pulmonary embolism?

A
  • Change in blood flow: immobility (paralysis/ post op), obesity, pregnancy
  • Change in blood vessel: smoking, hypertension
  • Change in blood constituents: dehydration, malignancy, high oestrogen (e.g. combined oral contraceptive pill), nephrotic syndrome, polycythaemia, inherited
  • Recent surgery (esp. abdo/pelvic or hip/knee replacement)
  • Leg fracture
  • Aged >60y
37
Q

What is the clinical presentation of a pulmonary embolism?

A
  • Depends on the number, size and distribution of emboli (small ones may be asymptomatic, large ones are often fatal)
  • Sudden onset unexplained dyspnoea is the most common symptoms (may be only symptom)
  • Pleuritic chest pain and haemoptysis when infarction has occurred
  • Dizziness
  • Past history/ family history of thromboembolism
  • Pyrexia
  • Cyanosis
  • Tachypnoea
  • Tachycardiac
  • Hypotension
  • Raised jugular venous pressure
  • Pleural rub (audible sign on stethoscope)
  • Pleural effusion
38
Q

What are the differential diagnoses of a pulmonary embolism?

A
  • Asthma
  • COPD
  • MI
  • Pneumonia
  • Heart failure
39
Q

How is a pulmonary embolism diagnosed?

A

CT pulmonary angiography:
- Gold standard test

CXR:

  • Often normal
  • Decreased vascular markings
  • Blunting of costophrenic angle
  • Wedge-shaped areas of infarction
  • Pulmonary oligaemia in massive embolism

ECG:

  • May be normal
  • May show sinus tachycardia
  • Right atrial dilation with tall peaked P waves in lead II
  • Right BBB
  • Right ventricular strain (inverted T wave in V1 to V4)

Blood gasses:

  • May be normal
  • Arterial hypoxaemia with significant PE

Plasma D-dimer:

  • Elevated
  • Not specific to PE therefore not diagnostic

USS:
- Look at legs and pelvis for clots

40
Q

How is a pulmonary embolism managed?

standard, non-massive PE

A
  • High flow oxygen (60-100%)
  • Anticoagulants (low molecular weight heparin)
  • IV fluids and inotropic agents in severe cases (improves pumping of right heart)
  • Thrombolysis for massive PE to improve pulmonary perfusion
  • Surgical embolectomy
  • Vena cava filter in patients who still develop emboli after anticoagulation
41
Q

How are pulmonary emboli prevented?

A

Prevention:

  • Vitamin K antagonist e.g. warfarin
  • Early mobilisation
  • TED stockings
42
Q

How is a massive PE managed?

A
  • Oxygen if hypoxic
  • Morphine with anti-emetic if patient is in pain or very distressed
  • Consider immediate thrombolysis if critically ill
  • Rapid colloid infusion if systolic BP <90mmHg
  • Warfarin if systolic BP >90mmHg
43
Q

What is the aetiology of TB?

A

Caused by 4 main mycobacterial species:

  • Mycobacterium tuberculosis (most common)
  • Mycobacterium bovis (from unpasteurised milk)
  • Mycobacterium africanum
  • Mycobacterium microti
44
Q

What is the pathophysiology of primary TB?

full detail of process

A
  • First infection with a mycobacteria
  • Alveolar macrophages ingest the inhaled bacteria
  • Bacteria proliferate inside macrophages, causing the release of neutrophil chemo-attractants and cytokines
  • This results in a cellular immune response and a delayed hypersensitivity-type reaction, causing tissue necrosis and granuloma formation
  • Initial granuloma = Primary Ghon Focus (found in upper region of lung in sub-pleural region)
  • Primary lesion can also occur in the GI tract
  • The caveated areas heal completely and may become calcified
  • Some of the calcified nodes contain bacteria which can lie dormant for many years
  • If the bacteria can’t be contained, there is dissemination of the primary infection → miliary TB (it spreads to other organs)
45
Q

What is the pathophysiology of latent TB?

A

Immune system contains the infection and the patient develops cell-mediated immunity memory of the bacteria

46
Q

What is the pathophysiology of reactivation TB?

A

When there’s a depression of host immunity causing latent TB to reactivate

47
Q

What are the risk factors for TB?

A
  • Origination from a high-incidence country e.g. sub-Saharan Africa
  • HIV +immunosuppression
  • Immunosuppressant therapy (chemo or MAB)
  • Diabetes mellitus
  • IVDU
  • Ageing
  • Malnutrition
  • Homeless i.e. poverty
  • Prisons
  • Smoking
  • Alcohol
48
Q

What are the systemic clinical features of TB?

A
  • Weight loss and night sweats = most predictive
  • Low grade fever
  • Anorexia
  • Malaise
49
Q

What are the pulmonary clinical features of TB?

A
  • Can be asymptomatic
  • Productive cough with occasional haemoptysis
  • Cough for >3w
  • Can be pleuritic pain if pleural involvement
  • Chest pain
  • Breathlessness
  • Can be hoarse voice if laryngeal involvement
  • Associated with consolidation, pleural effusion and pulmonary collapse
50
Q

What are the extra-pulmonary clinical features of TB?

lymph nodes, bone, abdominal, GU, CNS

A

LYMPH NODES: swelling ± discharge

BONE: joint pain/ swelling, Potts disease (spinal cord/ vertebral TB)

ABDOMINAL: ascites, abdo lymph nodes, ileal malabsorption

GU: epididymitis, frequency, dysuria, haematuria

CNS: bacilli in CSF, meningeal inflammation (produces thick exudate leading to cranial nerve strangulation and raised ICP), low grade meningitis, random cranial palsies and symptoms of raised ICP

51
Q

How is TB diagnosed?

non-miliary

A
  • CXR: patchy/nodular shadows in upper zones with loss of volume and fibrosis; consolidation; may be normal in miliary TB
  • Sputum: stain for bacteria (e.g. red with Ziehl-Neelsen)
  • Bronchoscopy if no sputum available
  • Culture and histology
  • Nucleic acid amplification (useful for differentiating between tuberculosis and non-tuberculosis mycobacterium)
  • Lumbar puncture and CSF examination for miliary TB
52
Q

How is miliary TB diagnosed?

A

TUBERCULIN SKIN TEST (Mantoux)

  • TB antigen is injected intradermally
  • Cell-mediated response at 48-72h is recorded as a type 4 hypersensitivity reaction should be stimulated
  • Positive results indicated immunity and therefore contact with TB
  • Immunosuppressed or miliary TB won’t react (false negative)
  • Will react with BCG vaccine (false positive)

INTERFERON GAMMA RELEASE ASSAYS (IGRAs)

  • Use antigens specific to M. tuberculosis to distinguish between BCG vaccine or environmental bacteria
  • Demonstrates exposure to M. tuberculosis but not active infection
53
Q

How is TB treated?

A

Patients with fully sensitive TB require 6m of treatment (12m if CNS TB):

  • RIFAMPICIN for 6m (bactericidal, blocks protein synthesis, effective throughout treatment)
  • ISONIAZID for 6m (bactericidal for rapidly growing bacilli)
  • PYRAZINAMIDE for first 2m (bactericidal initially, but less effective later on)
  • ETHAMBUTOL for first 2m (bacteriostatic, blocks cell wall synthesis)
54
Q

How is TB prevented?

A
  • Active case finding to reduce infectivity
  • Detection and treatment of TB via community nursing team using Mantoux and IGRAs
  • Vaccination: neonatal BCG
55
Q

What is the aetiology of community-acquired pneumonia?

A
  • Most common cause is Streptococcus pneumoniae

- Atypical causes include Haemophilus influenzae and Mycoplasma pneumoniae

56
Q

What is the aetiology of hospital-acquired pneumonia?

A
  • Aerobic G-ve bacilli

- Pseudomonas aeruginosa, Escherichia coli, Klebsiella pneumoniae

57
Q

What is the pathophysiology of pneumonia?

A
  • Spread by respiratory droplets
  • Bacteria translocate to the normally sterile distal airway where they overwhelm resident host defence
  • Alveolar macrophages change roles coordinate the response instead of fulfilling their normal roles
  • E.g. they cause stimulation of neutrophils to fill alveolar space and produce inflammatory exudate (→ pneumonia)
  • Thus is normally resolved when inflammatory cells are removed by apoptosis
  • Severe disease occurs if there is excessive inflammation, lung injury of failure to resolve without lung damage
58
Q

What are the risk factors of pneumonia?

A
  • Under 16 and over 65
  • Comorbidities: HIV infection, diabetes mellitus, cystic fibrosis, COPD, bronchiectasis
  • Smoking
  • Excess alcohol
  • IVDU
  • Immunosuppressant therapy
59
Q

What is the clinical presentation of pneumonia?

A
  • Pneumonia is likely if there are no upper respiratory tract symptoms, but there’s fever, night sweats, raised resp. rate and productive cough
  • Symptoms vary depending on infecting agent
  • Fever ± raised resp rate, heart rate and low BP
  • Rigors
  • Malaise
  • Anorexia
  • Dyspnoea and breathlessness
  • Signs of consolidation and auscultation
  • Dry of productive cough (dry is non-productive in atypical causes)
  • Purulent sputum
  • Pleuritic chest pain
  • Cyanosis
  • Confusion (might be only sign in elderly patients)
60
Q

What are the differential diagnoses of pneumonia?

A
  • TB

- Lung cancer

61
Q

How is pneumonia diagnosed?

diagnosis + severity indicator

A
  • CXR: air bronchogram (black branch) in consolidated area (multi-lobar suggests S.pneumoniae, S.aureus and Legionella spp., upper lobe cavity = klebsiella
  • Blood tests: FBC (look for raised WCC as a marker of severity)
  • Biochemistry: U&E, electrolytes, LFTs, renal function for severity
  • Microbiological tests: sputum culture and antibiotic sensitivities ± gram stain, blood culture, serology for viruses and atypical organisms

CURB-65 to assess severity: one point each for confusion, urea>7mmol/L, respiratory rate> 30/min, BP < 90mmHg systolic and/or 60mmHg diastolic, age > 65

Implications of CURB-65:

  • 0-1 = mild, only admit if social circumstance or single worrying feature
  • 2 = moderate, admit to hospital
  • 3-5 = severe, admit and monitor closely
  • 4-5 = consider admission to ICU
62
Q

How is pneumonia managed?

A
  • Maintain O2 sats between 94-98% (unless COPD then lower)
  • First dose of antibiotics within 4h of presentation in hospital
  • Narrow spectrum antibiotics if mild → amoxicillin
  • IV antibiotics if severe → co-amoxiclav or clarithromycin
  • Analgesia e.g. paracetamol or NSAID for pleuritic pain

Special cases:

  • Severe legionella spp. Pneumonia → fluoroquinolone ± clarithromycin
  • Necrotising pneumonia → IV linezoid, IV clindamycin, IV rifampicin
  • Pseudomonas aeruginosa → IV ceftazidime with gentamicin
63
Q

How is pneumonia prevented?

A
  • Polysaccharide pneumococcal vaccine
  • Influenza vaccine to those >65y, immuno-compromised or with co-morbidities
  • Smoking cessation
64
Q

What is the aetiology of pharyngitis/ tonsillitis?

A
  • Most common viral cause are adenoviruses
  • Can also be rhinovirus, EBV and acute HIV infection
  • Bacterial causes include Lancefield Group A Beta-haemolytic streptococci e.g. strep pyogenes
65
Q

What is the clinical presentation of pharyngitis/ tonsillitis?

A
  • Sore throat
  • Fever
  • Inflamed, swollen tonsils with exudate
  • Tender anterior cervical lymph nodes
  • Reddened oropharynx and soft palette
66
Q

How is pharyngitis/ tonsillitis diagnosed?

A

Clinical diagnosis

67
Q

How is pharyngitis/ tonsillitis managed?

A
  • Self-limiting disease
  • Symptomatic treatment
  • No antibiotics required
  • Persistent and severe tonsillitis should be treated with phenoxymethylpenicillin or cefaclor
68
Q

What is the aetiology of sinusitis?

A

Bacterial: streptococcus pneumoniae, haemophilus influenzae

69
Q

What is the clinical presentation of sinusitis?

A
  • Frontal headache
  • Purulent rhinorrhoea (nasal cavity filled with a significant amount of mucus fluid)
  • Bacterial sinusutis presents with unilateral pain and purulent discharge ± fever for >10d
70
Q

How is sinusitis diagnosed?

A

Clinical diagnosis

71
Q

How is sinusitis managed?

A
  • Nasal decongestants e.g. xylometazoline

- Broad spectrum antibiotics e.g. co-amoxiclav

72
Q

What is the aetiology of acute epiglottis?

A
  • Disease in adults is most severe due to Haemophilus influenzae
  • Hib vaccine has made this rare
73
Q

What is the clinical presentation of acute epiglottis?

A
  • High fever
  • Severe airflow obstruction
  • Meningitis
  • Septic arthritis
  • Osteomyelitis
74
Q

How is acute epiglottis diagnosed?

A

Clinical diagnosis

75
Q

How is acute epiglottis managed?

A
  • Requires urgent endotracheal intubation

- IV antibiotics e.g. ceftazidime

76
Q

What is the aetiology of whooping cough?

A

Caused by Bordetella pertussis (G-ve coccobacillus)

77
Q

What is the pathophysiology of whooping cough?

A

Spreads by droplet infection

78
Q

What is the clinical presentation of whooping cough? (general, catarrhal and paroxysmal phases)

A
  • Chronic cough and one clinical feature indicated pertussis
  • Characteristic whoop and history of contact with an infected individual

CATARRHAL PHASE (1-2w):

  • Patient highly infectious
  • Malaise
  • Anorexia
  • Rhinorrhoea
  • Conjunctivitis

PAROXYSMAL PHASE (1-6w):

  • Coughing spasms
  • Classic inspiratory whoop in younger individuals
  • Spasms usually end by vomiting
  • Cough for >14d
  • May be associated with complications like pneumonia, encephalopathy and sub-conjunctival haemorrhage
79
Q

How is whooping cough diagnosed?

A
  • Chronic cough and history of contact/ microbiological diagnosis
  • PCR tests
  • Culture of a nasopharyngeal swab is needed for definitive diagnosis
80
Q

How is whooping cough managed?

A
  • Antimicrobials (macrolides e.g. clarithromycin) to eliminate carriage of bacteria
  • Antibiotics have little role to play in the paroxysmal stage
  • Vaccination against acellular pertussis as part of the dTap vaccine

2a high tier (10 decks)

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