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PREPRINT
www.Guidelines.co.uk
summarising clinical guidelines for primary care
cPD credits
summarising clinical guidelines for primary care
The production and printing of this Guidelines preprint has been funded by GSK UK. See inside front cover for full disclaimer. Prescribing information can be found on the outside back cover. Date of preparation: December 2018
PREPRINT
Chronic obstructive pulmonary disease in over 16s: diagnosis and management• National Institute for Health and Care Excellence •
When a clinical guideline describes a drug therapy, readers should refer to the full summary of product characteristics to confirm licensed indications and the clinical significance of a product’s contraindications, special precautions, drug interactions, adverse reactions, or overdose. While every care has been taken to ensure the accuracy of this Guidelines summary, this does not diminish the requirement to exercise clinical judgement and the publisher cannot accept liability for any errors and omissions.
The production and printing of this Guidelines preprint has been funded by GSK UK. While this preprint has been reviewed for factual accuracy, GSK UK has had no editorial input into the content.
© NICE (2018) Chronic obstructive pulmonary disease in over 16s: diagnosis and management. Available from www.nice.org.uk/guidance/NG115. All rights reserved. Subject to Notice of rights (see www.nice.org.uk/terms-and-conditions#notice-of-rights)
NICE guidance is prepared for the National Health Service in England. All guidance is subject to regular review and may be updated or withdrawn. NICE accepts no responsibility for the use of its content in this publication.
There has been no contact between the sponsors and NICE in the development of this Guidelines preprint.
The views and opinions in this preprint are not necessarily those of GSK UK, or of Guidelines, its publisher, advisers, or advertisers.
MGP Ltd owns copyright of the Guidelines brand, logo, and the design and format of this Guidelines summary preprint.
Date of preparation: December 2018
© MGP Ltd 2018
National Institute for Health and Care Excellence
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Chronic obstructive pulmonary disease in over 16s: diagnosis and management
• This Guidelines summary covers the following topics: – prognosis – further investigations – incidental findings on chest X-ray or CT scans – inhaled therapy – oral therapy – oxygen therapy – education and self-management – pulmonary hypertension and cor pulmonale – pharmacological management of COPD
• Recommendations that are new to the 2018 updated guideline are marked with (2018), amended recommendations for the 2018 updated guideline are marked with (amended 2018)
Diagnosing COPD
• The diagnosis of chronic obstructive pulmonary disease (COPD) depends on thinking of it as a cause of breathlessness or cough. The diagnosis is suspected on the basis of symptoms and signs, and is supported by spirometry
Symptoms
• Suspect a diagnosis of COPD in people over 35 who have a risk factor (generally smoking or a history of smoking) and who present with one or more of the following symptoms: – exertional breathlessness – chronic cough – regular sputum production – frequent winter ‘bronchitis’ – wheeze
• When thinking about a diagnosis of COPD, ask the person if they have: – weight loss – reduced exercise tolerance – waking at night with breathlessness
– ankle swelling – fatigue – occupational hazards – chest pain – haemoptysis (coughing up blood)
these last two symptoms are uncommon in COPD and raise the possibility of alternative diagnoses
• One of the primary symptoms of COPD is breathlessness. The Medical Research Council (MRC) dyspnoea scale (see table 1) should be used to grade the breathlessness according to the level of exertion required to elicit it
Table 1: MRC dyspnoea scaleGRADE DEGREE OF BREATHLESSNESS
RELATED TO ACTIVITIES
1 Not troubled by breathlessness except on strenuous exercise
2 Short of breath when hurrying or walking up a slight hill
3 Walks slower than contemporaries on level ground because of breathlessness, or has to stop for breath when walking at own pace
4 Stops for breath after walking about 100 metres or after a few minutes on level ground
5 Too breathless to leave the house, or breathless when dressing or undressing
Adapted from Fletcher CM, Elmes PC, Fairbairn MB et al. (1959) The significance of respiratory symptoms and the diagnosis of chronic bronchitis in a working population. British Medical Journal 2: 257–266.
Spirometry
• Perform spirometry: – at diagnosis – to reconsider the diagnosis, for people who show an exceptionally good response to treatment
– to monitor disease progression (amended 2018)
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• Measure post-bronchodilator spirometry to confirm the diagnosis of COPD
• Think about alternative diagnoses or investigations for older people who have an FEV1/FVC ratio below 0.7 but do not have typical symptoms of COPD
• Think about a diagnosis of COPD in younger people who have symptoms of COPD, even when their FEV1/FVC ratio is above 0.7
• All healthcare professionals who care for people with COPD should have access to spirometry and be competent in interpreting the results
• Spirometry can be performed by any healthcare worker who has had appropriate training and has up-to-date skills
• Spirometry services should be supported by quality-control processes
• It is recommended that Global Lung Function Initiative GLI 2012 reference values are used, but it is recognised that these values are not applicable for all ethnic groups (amended 2018)
Incidental findings on chest X-rays or CT scans (2018)
• Consider primary care respiratory review and spirometry (see Spirometry, page 3) for people with emphysema or signs of chronic airways disease on a chest X-ray or CT scan
• If the person is a current smoker, their spirometry results are normal and they have no symptoms or signs of respiratory disease: – offer smoking cessation advice and treatment, and referral to specialist stop smoking services (see the NICE guideline on stop smoking interventions and services)
– warn them that they are at higher risk of lung disease
– advise them to return if they develop respiratory symptoms
– be aware that the presence of emphysema on a CT scan is an independent risk factor for lung cancer
• If the person is not a current smoker, their spirometry is normal and they have no symptoms or signs of respiratory disease: – ask them if they have a personal or family history of lung or liver disease and consider alternative diagnoses, such as alpha-1 antitrypsin deficiency
– reassure them that their emphysema or chronic airways disease is unlikely to get worse
– advise them to return if they develop respiratory symptoms
– be aware that the presence of emphysema on a CT scan is an independent risk factor for lung cancer
Further investigations
• In addition to spirometry all patients should have: – a chest radiograph to exclude other pathologies
– a full blood count to identify anaemia or polycythaemia
– body mass index (BMI) calculated
• For further information on additional investigations, please refer to our Guidelines summary online at: guidelines.co.uk/nice/copd
Reversibility testing
• For most people, routine spirometric reversibility testing is not necessary as part of the diagnostic process or to plan initial therapy with bronchodilators or corticosteroids
• Untreated COPD and asthma are frequently distinguishable on the basis of history (and examination) in people presenting for the first time. Whenever possible, use features from the history and examination (such as those listed in table 2, page 5) to differentiate COPD from asthma. For more information on diagnosing asthma, see the NICE guideline on asthma (amended 2018)
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• In addition to the features in table 2, use longitudinal observation of people (with spirometry, peak flow or symptoms) to help differentiate COPD from asthma
• When diagnostic uncertainty remains, or both COPD and asthma are present, use the following findings to help identify asthma: – a large (over 400 ml) response to bronchodilators
– a large (over 400 ml) response to 30 mg oral prednisolone daily for 2 weeks
– serial peak flow measurements showing 20% or greater diurnal or day-to-day variability
• Clinically significant COPD is not present if the FEV1 and FEV1/FVC ratio return to normal with drug therapy
• If diagnostic uncertainty remains, think about referral for more detailed investigations, including imaging and measurement of transfer factor for carbon monoxide (TLCO)
• Reconsider the diagnosis of COPD for people who report a marked improvement in symptoms in response to inhaled therapy
Assessing severity and using prognostic factors
• COPD is heterogeneous, so no single measure can adequately assess disease severity in an individual. Severity assessment is, nevertheless, important because it has implications for therapy and relates to prognosis
• Do not use a multidimensional index (such as BODE) to assess prognosis in people with stable COPD (2018)
• From diagnosis onwards, when discussing prognosis and treatment decisions with people with stable COPD, think about the following factors that are individually associated with prognosis: – FEV1
– smoking status – breathlessness (MRC scale) – chronic hypoxia and/or cor pulmonale – low BMI – severity and frequency of exacerbations – hospital admissions – symptom burden (for example, COPD Assessment Test [CAT] score)
– exercise capacity (for example, 6-minute walk test)
– TLCO – whether the person meets the criteria for long-term oxygen therapy and/or home non-invasive ventilation
– multimorbidity (see the NICE guideline on multimorbidity)
– frailty (amended 2018)
Assessing and classifying the severity of airflow obstruction
• Assess the severity of airflow obstruction according to the reduction in FEV1 as shown on table 3, page 6
• For people with mild airflow obstruction, only diagnose COPD if they have one or more of the symptoms (described in Symptoms, page 3)
Table 2: Clinical features differentiating COPD and asthmaCOPD ASTHMA
Smoker or ex-smoker Nearly all Possibly
Symptoms under age 35 Rare Often
Chronic productive cough Common Uncommon
Breathlessness Persistent and progressive Variable
Night-time waking with breathlessness and/or wheeze Uncommon Common
Significant diurnal or day-to-day variability of symptoms Uncommon Common
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Table 4: Reasons for referral include
REASON PURPOSE
There is diagnostic uncertainty Confirm diagnosis and optimise therapy
Suspected severe COPD Confirm diagnosis and optimise therapy
The person with COPD requests a second opinion
Confirm diagnosis and optimise therapy
Onset of cor pulmonale Confirm diagnosis and optimise therapy
Assessment for oxygen therapy Optimise therapy and measure blood gases
Assessment for long-term nebuliser therapy
Optimise therapy and exclude inappropriate prescriptions
Assessment for oral corticosteroid therapy Justify need for continued treatment or supervise withdrawal
Bullous lung disease Identify candidates for lung volume reduction procedures
A rapid decline in FEV1 Encourage early intervention
Assessment for pulmonary rehabilitation Identify candidates for pulmonary rehabilitation
Assessment for a lung volume reduction procedure
Identify candidates for surgical or bronchoscopic lung volume reduction
Assessment for lung transplantation Identify candidates for surgery
Dysfunctional breathing Confirm diagnosis, optimise pharmacotherapy and access other therapists
Onset of symptoms under 40 years or a family history of alpha-1 antitrypsin deficiency
Identify alpha-1 antitrypsin deficiency, consider therapy and screen family
Symptoms disproportionate to lung function deficit
Look for other explanations including cardiac impairment, pulmonary hypertension, depression and hyperventilation
Frequent infections Exclude bronchiectasis
Haemoptysis Exclude carcinoma of the bronchus
Table 3: Gradation of severity of airflow obstruction
NICE GUIDELINE CG12 (2004)
ATS/ERS 20041
GOLD 20082 NICE GUIDELINE CG101 (2010)
Post-bronchodilator FEV1/FVC
FEV1 % predicted
Severity of airflow obstruction
– – Post-bronchodilator
Post-bronchodilator
Post-bronchodilator
<0.7 ≥80% – Mild Stage 1–Mild Stage 1–Mild<0.7 50–79% Mild Moderate Stage 2–
ModerateStage 2–Moderate
<0.7 30–49% Moderate Severe Stage 3–Severe Stage 3–Severe<0.7 <30% Severe Very severe Stage 4–Very
severe*Stage 4–Very severe*
* Or FEV1 below 50% with respiratory failure.1 Celli BR, MacNee W, Agusti A et al. (2004) Standards for the diagnosis and treatment of patients with COPD: a summary of the ATS/ERS position paper. European Respiratory Journal 23 (6): 932–946.2 Global Initiative for Chronic Obstructive Lung Disease (GOLD; 2008) Global strategy for the diagnosis, management and prevention of COPD.
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Figure 1: Non-pharmacological management and use of inhaled therapies
COPD=chronic obstructive pulmonary disease; SABA=short-acting beta2 agonists; SAMA=short-acting muscarinic antagonists, LABA=long-acting beta2 agonists, LAMA=long-acting muscarinic antagonists, ICS=inhaled corticosteroids; FEV1=forced expiratory volume in the fi rst second.*Asthmatic features/features suggesting steroid responsiveness in this context include any previous secure diagnosis of asthma or atopy, a higher blood eosinophil count, substantial variation in FEV1 over time (at least 400 ml) or substantial diurnal variation in peak expiratory fl ow (at least 20%).
This is a summary of the recommendations on non-pharmacological management of chronic obstructive pulmonary disease and use of inhaled therapies in people over 16. The guideline also covers diagnosis and other areas of management (see www.nice.org.uk/guidance/NG115)
Asthmatic features/features suggesting steroid responsiveness*
Consider LABA + ICS
Person still breathless or has exacerbations despite further treatment?
OfferLAMA + LABA + ICS
No asthmatic features/features suggesting steroid responsiveness*
Offer LABA + LAMA
For ALL inhaled therapies:
Train people in correct inhaler technique, and review medication and assess inhaler
technique and adherence regularly
Inhaled therapies
Offer SABA or SAMA to use if needed
Person still breathless or has exacerbations despite treatment?
� Start inhaled therapies only if: —all the above interventions have been offered (if appropriate), and — inhaled therapies are needed to relieve breathlessness or exercise limitation
Fundamentals of COPD care� Offer treatment and support to stop smoking� Offer pneumococcal and infl uenza vaccinations� Offer pulmonary rehabilitation if indicated� Co-develop a personalised self-management plan� Optimise treatment for comorbidities
These treatments and plans should be revisited at every review
Confi rmed diagnosis of COPD
Explore further treatment options if needed (see full guideline at: www.nice.org.uk/guidance/NG115)
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Referral for specialist advice
• When clinically indicated, refer people for specialist advice. Referral may be appropriate at all stages of the disease and not solely in the most severely disabled people (see table 4, page 6)
Managing stable COPD
• See Figure 1, page 7 for a visual summary covering non-pharmacological management and use of inhaled therapies (2018)
• For guidance on the management of multimorbidity, see the NICE guideline on multimorbidity (2018)
Inhaled therapy
Short-acting beta2 agonists (SABA) and short-acting muscarinic antagonists (SAMA)
• Use short-acting bronchodilators, as necessary, as the initial empirical treatment to relieve breathlessness and exercise limitation
Inhaled corticosteroids (ICS)
• Do not use oral corticosteroid reversibility tests to identify which people should be prescribed inhaled corticosteroids, because they do not predict response to inhaled corticosteroid therapy
• Be aware of, and be prepared to discuss with the person, the risk of side-effects (including pneumonia) in people who take inhaled corticosteroids for COPD* (amended 2018)
Inhaled combination therapy
• Inhaled combination therapy refers to combinations of long-acting muscarinic antagonists (LAMA), long-acting beta2 agonists (LABA) and inhaled corticosteroids (ICS)
• Do not assess the effectiveness of bronchodilator therapy using lung function alone. Include a variety of other measures such as improvement in symptoms, activities of daily living, exercise capacity, and rapidity of symptom relief
• Offer LAMA+LABA† to people who: – have spirometrically confirmed COPD and – do not have asthmatic features/features suggesting steroid responsiveness and
– remain breathless or have exacerbations despite:
having used or been offered treatment for tobacco dependence if they smoke andoptimised non-pharmacological management and relevant vaccinations andusing a short-acting bronchodilator (2018)
• Consider LABA+ICS for people who: – have spirometrically confirmed COPD and – have asthmatic features/features suggesting steroid responsiveness and
– remain breathless or have exacerbations despite:
having used or been offered treatment for tobacco dependence if they smoke andoptimised non-pharmacological management and relevant vaccinations andusing a short-acting bronchodilator (2018)
• For people using long-acting bronchodilators outside of the recommendations above, and before this guideline was published (December 2018), explain to them that they can continue with their current treatment until both they and their NHS healthcare professional agree it is appropriate to change (2018)
• Offer LAMA+LABA+ICS† to people with COPD with asthmatic features/features suggesting steroid responsiveness who remain breathless or have exacerbations despite taking LABA+ICS (amended 2018)
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– continue to have one or more of the following, particularly if they have significant daily sputum production:
frequent (typically four or more per year) exacerbations with sputum production prolonged exacerbations with sputum productionexacerbations resulting in hospitalisation‡
• Before offering prophylactic antibiotics, ensure that the person has had: – sputum culture and sensitivity (including tuberculosis culture), to identify other possible causes of persistent or recurrent infection that may need specific treatment (for example, antibiotic-resistant organisms, atypical mycobacteria or Pseudomonas aeruginosa)
– training in airway clearance techniques to optimise sputum clearance)
– a CT scan of the thorax to rule out bronchiectasis and other lung pathologies
• Before starting azithromycin, ensure the person has had: – an electrocardiogram (ECG) to rule out prolonged QT interval and
– baseline liver function tests
• When prescribing azithromycin, advise people about the small risk of hearing loss and tinnitus, and tell them to contact a healthcare professional if this occurs
• Review prophylactic azithromycin after the first 3 months, and then at least every 6 months
• Only continue treatment if the continued benefits outweigh the risks. Be aware that there are no long-term studies on the use of prophylactic antibiotics in people with COPD
• For people who are taking prophylactic azithromycin and are still at risk of exacerbations, provide a non-macrolide antibiotic to keep at home as part of their exacerbation action plan
• Base the choice of drugs and inhalers on: – how much they improve symptoms – the person’s preferences and ability to use the inhalers
– the drugs’ potential to reduce exacerbations – their side-effects – their cost
• Minimise the number of inhalers and the number of different types of inhaler used by each person as far as possible (2018)
• When prescribing long-acting drugs, ensure people receive inhalers they have been trained to use (for example, by specifying the brand and inhaler in prescriptions) (2018)
Spacers and nebulisers
• For further information, please refer to our Guidelines summary online at: guidelines.co.uk/nice/copd
Oral therapy
• Please refer to our Guidelines summary online at: guidelines.co.uk/nice/copd for recommendations on oral: – corticosteroids – theophylline – mucolytic therapy – anti-oxidant therapy – anti-tussive therapy
Oral prophylactic antibiotic therapy (2018)
• Before starting prophylactic antibiotic therapy in a person with COPD, think about whether respiratory specialist input is needed
• Consider azithromycin (usually 250 mg three times a week) for people with COPD if they: – do not smoke and – have optimised non-pharmacological management and inhaled therapies, relevant vaccinations and (if appropriate) have been referred for pulmonary rehabilitation and
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• Base the decision on whether long-term oxygen therapy is suitable on the results of the structured risk assessment (2018)
• Do not offer long-term oxygen therapy to people who continue to smoke despite being offered smoking cessation advice and treatment, and referral to specialist stop smoking services (2018)
• Advise people who are having long-term oxygen therapy that they should breathe supplemental oxygen for a minimum of 15 hours per day (2018)
• Do not offer long-term oxygen therapy to treat isolated nocturnal hypoxaemia caused by COPD (2018)
Short-burst oxygen therapy
• Do not offer short-burst oxygen therapy to manage breathlessness in people with COPD who have mild or no hypoxaemia at rest (2018)
Managing pulmonary hypertension and cor pulmonale
Treating pulmonary hypertension (2018)
• Do not offer the following treatments solely to manage pulmonary hypertension caused by COPD, except as part of a randomised controlled trial: – bosentan – losartan – nifedipine – nitric oxide – pentoxifylline – phosphodiesterase-5 inhibitors – statins
Treating cor pulmonale (2018)
• Ensure that people with cor pulmonale caused by COPD are offered optimal COPD treatment, including advice and interventions to help them stop smoking. For people who
• Be aware that it is not necessary to stop prophylactic azithromycin during an acute exacerbation of COPD
Oral phosphodiesterase-4 inhibitors (2018)
• For guidance on treating severe COPD with roflumilast, see NICE’s technology appraisal guidance on roflumilast for treating chronic obstructive pulmonary disease
Oxygen
• Please refer to our Guidelines summary online at: guidelines.co.uk/nice/copd for recommendations on: – long-term oxygen therapy – ambulatory oxygen therapy – short-burst oxygen therapy
Long-term oxygen therapy
• Consider long-term oxygen therapy§ for people with COPD who do not smoke and who: – have a partial pressure of oxygen in arterial blood (PaO2) below 7.3 kPa when stable or
– have a PaO2 above 7.3 and below 8 kPa when stable, if they also have one or more of the following:
secondary polycythaemiaperipheral oedemapulmonary hypertension (2018)
• Conduct and document a structured risk assessment for people being assessed for long-term oxygen therapy who meet the criteria above. As part of the risk assessment, cover the risks for both the person with COPD and the people who live with them, including: – the risks of falls from tripping over the equipment
– the risks of burns and fires, and the increased risk of these for people who live in homes where someone smokes (including e-cigarettes)
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need treatment for hypoxia, see the section on long-term oxygen therapy, page 8
• Oedema associated with cor pulmonale can usually be controlled symptomatically with diuretic therapy
• Do not use the following to treat cor pulmonale caused by COPD: – alpha-blockers – angiotensin-converting enzyme inhibitors – calcium channel blockers – digoxin (unless there is atrial fibrillation)
Lung surgery and lung volume reduction procedures
• For further information, please refer to our Guidelines summary online at: guidelines.co.uk/nice/copd
Multidisciplinary management
• COPD care should be delivered by a multidisciplinary team
Education
• There are significant differences in the response of people with COPD and asthma to education programmes. Programmes designed for asthma should not be used in COPD
• At diagnosis and at each review appointment, offer people with COPD and their family members or carers (as appropriate): – written information about their condition – opportunities for discussion with a healthcare professional who has experience in caring for people with COPD (2018)
• Ensure the information provided is: – available on an ongoing basis – relevant to the stage of the person’s condition – tailored to the person’s needs (2018)
• At minimum, the information should cover: – an explanation of COPD and its symptoms
– advice on quitting smoking (if relevant) and how this will help with the person’s COPD
– advice on avoiding passive smoke exposure – managing breathlessness – physical activity and pulmonary rehabilitation – medicines, including inhaler technique and the importance of adherence
– vaccinations – identifying and managing exacerbations – details of local and national organisations and online resources that can provide more information and support
– how COPD will affect other long-term conditions that are common in people with COPD (for example, hypertension, heart disease, anxiety, depression and musculoskeletal problems) (2018)
• Advise people with COPD that the following factors increase their risk of exacerbations: – continued smoking or relapse for ex-smokers – exposure to passive smoke – viral or bacterial infection – indoor and outdoor air pollution – lack of physical activity – seasonal variation (winter and spring) (2018)
Self-management (2018)
• Develop an individualised self-management plan in collaboration with each person with COPD and their family members or carers (as appropriate), and: – include education on all relevant points from Education, see page 11
– review the plan at future appointments
• Develop an individualised exacerbation action plan in collaboration with each person with COPD who is at risk of exacerbations
• Offer people a short course of oral corticosteroids and a short course of oral antibiotics to keep at home as part of their exacerbation action plan if: – they have had an exacerbation within the last year, and remain at risk of exacerbations
– they understand and are confident about when and how to take these medicines, and the associated benefits and harms
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Table 6: Factors to consider when deciding where to treat the person with COPD
FACTOR TREAT AT HOME TREAT IN HOSPITAL
Able to cope at home Yes No
Breathlessness Mild Severe
General condition Good Poor/deteriorating
Level of activity Good Poor/confined to bed
Cyanosis No Yes
Worsening peripheral oedema No Yes
Level of consciousness Normal Impaired
Already receiving long-term oxygen therapy
No Yes
Social circumstances Good Living alone/not coping
Acute confusion No Yes
Rapid rate of onset No Yes
Significant comorbidity (particularly cardiac disease and insulin-dependent diabetes)
No Yes
SaO2 <90% No Yes
Changes on chest radiograph No Present
Arterial pH level ≥7.35 <7.35
Arterial PaO2 ≥7 kPa <7 kPa
Table 5: Summary of follow up of people with COPD in primary careMILD/MODERATE/SEVERE (STAGES 1 TO 3)
VERY SEVERE (STAGE 4)
Frequency At least annual At least twice per year
Clinical assessment
• Smoking status and motivation to quit• Adequacy of symptom control:
– breathlessness – exercise tolerance – estimated exacerbation frequency
• Need for pulmonary rehabilitation • Presence of complications• Effects of each drug treatment• Inhaler technique• Need for referral to specialist and
therapy services
• Smoking status and motivation to quit• Adequacy of symptom control:
– breathlessness – exercise tolerance – estimated exacerbation frequency
• Presence of cor pulmonale• Need for long-term oxygen therapy• Person with COPD’s nutritional state• Presence of depression• Effects of each drug treatment• Inhaler technique• Need for social services and
occupational therapy input• Need for referral to specialist and
therapy services• Need for pulmonary rehabilitation
Measurements to make
• FEV1 and FVC• Calculate BMI• MRC dyspnoea score
• FEV1 and FVC• Calculate BMI• MRC dyspnoea score• SaO2
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– they know to tell their healthcare professional when they have used the medicines, and to ask for replacements
• For guidance on the choice of antibiotics, see the NICE guideline on antimicrobial prescribing for acute exacerbations of COPD
• At all review appointments, discuss corticosteroid and antibiotic use with people who keep these medicines at home, to check that they still understand how to use them. For people who have used three or more courses of oral corticosteroids and/or oral antibiotics in the last year, investigate the possible reasons for this
• See full guideline for more guidance on oral corticosteroids
• Encourage people with COPD to respond promptly to exacerbation symptoms by following their action plan, which may include: – adjusting their short-acting bronchodilator therapy to treat their symptoms
– taking a short course of oral corticosteroids if their increased breathlessness interferes with activities of daily living
– adding oral antibiotics if their sputum changes colour and increases in volume or thickness beyond their normal day-to-day variation
– telling their healthcare professional
• Ask people with COPD if they experience breathlessness they find frightening. If they do, consider including a cognitive behavioural component in their self-management plan to help them manage anxiety and cope with breathlessness
• For people at risk of hospitalisation, explain to them and their family members or carers (as appropriate) what to expect if this happens (including non-invasive ventilation and discussions on future
treatment preferences, ceilings of care and resuscitation)
Telehealth monitoring (2018)
• Do not offer routine telehealth monitoring of physiological status as part of management for stable COPD
Follow-up of people with COPD
• See table 5, page 12, and guidelines.co.uk/nice/copd for further information
Managing exacerbations of COPD
Definition of an exacerbation
• A sustained acute-onset worsening of the person’s symptoms from their usual stable state, which goes beyond their normal day-to-day variations. Commonly reported symptoms are worsening breathlessness, cough, increased sputum production and change in sputum colour. The change in these symptoms often necessitates a change in medication
Assessing the need for hospital treatment
• Use the factors in table 6 (see page 12)to assess whether people with COPD need hospital treatment
Investigating an exacerbation
• The diagnosis of an exacerbation is made clinically and does not depend on the results of investigations. However, investigations may sometimes be useful in ensuring appropriate treatment is given. Different investigation strategies are needed for people in hospital (who will tend to have more severe exacerbations) and people in the community
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Primary care
• For people who have their exacerbation managed in primary care: – sending sputum samples for culture is not recommended in routine practice
– pulse oximetry is of value if there are clinical features of a severe exacerbation
Terms used in this guideline
Asthmatic features/features suggesting steroid responsiveness
• This includes any previous, secure diagnosis of asthma or of atopy, a higher blood eosinophil count, substantial variation in FEV1 over time (at least 400 ml) or substantial diurnal variation in peak expiratory flow (at least 20%)
Mild or no hypoxaemia
• People who are not taking long-term oxygen therapy and who have a mean PaO2 greater than 7.3 kPa
* The Medicines and Healthcare products Regulatory Agency (MHRA) has published advice on the risk of psychological and behavioural side-effects associated with inhaled corticosteroids (2010).
† The MHRA has published advice on the risk for people with certain cardiac conditions when taking tiotropium delivered via Respimat or HandiHaler (2015).
‡ At the time of publication (December 2018), azithromycin did not have a UK marketing authorisation for this indication. The prescriber should follow relevant professional guidance, taking full responsibility for the decision. Informed consent should be obtained and documented. See the General Medical Council’s Prescribing guidance: prescribing unlicensed medicines for further information.
§ The MHRA has published an alert on the risk of death and severe harm from failure to obtain and continue flow from oxygen cylinders (2018).
© NICE 2018. Chronic obstructive pulmonary disease in over 16s: diagnosis and management. Available from: www.nice.org.uk/NG115. All rights reserved. Subject to Notice of rights (see www.nice.org.uk/terms-and-conditions#notice-of-rights)
NICE guidance is prepared for the National Health Service in England. All NICE guidance is subject to regular review and may be updated or withdrawn. NICE accepts no responsibility for the use of its content in this product/publication
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A once daily LAMA/LABA for symptomatic patients with COPD1
START WITH
ANORO
Reference: 1. Anoro SmPC
Adverse events should be reported. Reporting forms and information can be found at www.mhra.gov.uk/yellowcard or search for MHRA Yellowcard in the Google Play or Apple App store.
Adverse events should also be reported to GlaxoSmithKline on 0800 221 441
(umeclidinium/vilanterol)
Anoro Ellipta (umeclidinium bromide/vilanterol [as trifenatate]) Prescribing information(Please consult the full Summary of Product Characteristics (SmPC) before prescribing)
Anoro Ellipta 55/22mcg (umeclidinium bromide /vilanterol [as trifenatate]) inhalation powder. Each single inhalation provides a delivered dose (the dose leaving the mouthpiece) of 55 micrograms umeclidinium (equivalent to 65 micrograms of umeclidinium bromide) and 22 micrograms of vilanterol (as trifenatate). Indications: Anoro is indicated as a maintenance bronchodilator treatment to relieve symptoms in adult patients with chronic obstructive pulmonary disease (COPD). Dosage and administration: Inhalation only. One inhalation once daily of Anoro. Contraindications: Hypersensitivity to the active substances or to any of the excipients (lactose monohydrate and magnesium stearate). Precautions: Anoro should not be used in patients with asthma. Treatment with Anoro should be discontinued in the event of paradoxical bronchospasm and alternative therapy initiated if necessary. Cardiovascular effects may be seen after the administration of muscarinic receptor antagonists and sympathomimetics therefore Anoro should be used with caution in patients with severe cardiovascular disease. Anoro should be used with caution in patients with urinary retention, narrow angle glaucoma, convulsive disorders, thyrotoxicosis, hypokalaemia, hyperglycaemia and severe hepatic impairment. No dosage adjustment is required in renal or mild to moderate hepatic impairment. Acute symptoms: Anoro is not indicated for acute episodes of bronchospasm. Warn patients to seek medical advice if short-acting inhaled bronchodilator use increases, a re-evaluation of the patient
and of the COPD treatment regimen should be undertaken. Interactions with other medicinal products: Avoid β-blockers. Caution is advised when co-administering with strong CYP3A4 inhibitors (e.g. ketoconazole, clarithromycin, itraconazole, ritonavir, telithromycin). Anoro should not be used in conjunction with other long-acting β2-adrenergic agonists ormedicinal products containing long-acting muscarinic antagonists. Caution is advised with concomitant use with methylxanthine derivatives, steroids or non-potassium-sparing diuretics as it may potentiate possible hypokalaemic effect of β2-adrenergic agonists. Fertility, pregnancy, and breast-feeding: No available data. Balance risks against benefits. Side effects: Common (≥1/100 to <1/10): urinary tract infection, sinusitis, nasopharyngitis, pharyngitis, upper respiratory tract infection, headache, cough, oropharyngeal pain, constipation and dry mouth. Other important side effects include: Uncommon (≥1/1,000 to <1/100) atrial fibrillation, supraventricular tachycardia, rhythm idioventricular, tachycardia, supraventricular extrasystoles, palpitations, and hypersensitivity reactions including rash. Rare (≥1/10,000 to <1/1,000) anaphylaxis, angioedema, and urticaria. Glaucoma, vision blurred, intraocular pressure increased and paradoxical bronchospasm. See SmPC for other adverse reactions. Legal category: POM. Presentation and Basic NHS cost: Anoro Ellipta. 1 inhaler x 30 doses. Anoro Ellipta 55/22mcg - £32.50. Marketing authorisation (MA) no. 55/22mcg 1x30 doses [EU/1/14/898/002]; MA holder: Glaxo Group Ltd, 980 Great West Road, Brentford, Middlesex TW8 9GS, UK. Last date of revision: July 2018. UK/UCV/0095/15(2)b. Anoro and Ellipta are registered trademarks of the GlaxoSmithKline group of companies. All rights reserved. Anoro was developed in collaboration with Innoviva Inc.
Read the clinical data at www.anoro.co.uk© 2018 GlaxoSmithKline Group of Companies.
Zinc code: UK/UCV/0029/18 I Date of preparation: December 2018
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