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Announcements and latest updates

Welcome to the Right Decision Service (RDS) newsletter for August 2024.

  1. Contingency planning for RDS outages

Following the recent RDS outages, Tactuum and the RDS team have been reviewing the learning from these incidents. We are committed to doing all we can to ensure a positive outcome by strengthening the RDS to make it fully robust and clinically resilient for the future.

We would like to invite you to a webinar on 26th September 3-4 pm on national and local contingency planning for future RDS outages.  Tactuum and the RDS team will speak about our business continuity plans and the national contingency arrangements we are putting in place. This will also be a space to share local contingency plans, ideas and existing good practice. We would also like to gather your views on who we should send communications to in the event of future outages.

I have sent a meeting request for this date to all editors – please accept or decline to indicate attendance, and please forward on to relevant contacts. You can also contact Olivia.graham@nhs.scot directly to register your interest in participating.

 

2.National  IV fluid prescribing  calculator

This UK CA marked calculator is now live at https://righdecisions.scot.nhs.uk/ivfluids  . It has been developed by a multiprofessional steering group of leads in IV fluids management, as part of the wider Modernising Patient Pathways Programme within the Centre for Sustainable Delivery.  It aims to address a known cause of clinical error in hospital settings, and we hope it will be especially useful to the new junior doctors who started in August.

Please do spread the word about this new calculator and get in touch with any questions.

 

  1. New toolkits

The following toolkits are now live;

  1. Updated guidance on current and future Medical Device Regulations

We have updated and simplified this guidance within our standard operating procedures. We have clarified the guidance on how to determine whether an RDS tool is a medical device, and have provided an interactive powerpoint slideset to steer you through the process.

 

  1. Guide to six stages of RDS toolkit development

We have developed a guide to support editors and toolkit leads through the process of scoping, designing, delivering, quality assuring and implementing a new RDS toolkit.  We hope this will help in project planning and in building shared understanding of responsibilities throughout the full development process.  The guide emphasises that the project does not end with launch of the new toolkit. Implementation, communication and evaluation are ongoing activities throughout the lifetime of the toolkit.

 

  1. Training sessions for new editors (also serve as refresher sessions for existing editors) will take place on the following dates:
  • Thursday 5 September 1-2 pm
  • Wednesday 24 September 4-5 pm
  • Friday 27 September 12-1 pm

To book a place, please contact Olivia.graham@nhs.scot, providing your name, organisation, job role, and level of experience with RDS editing (none, a little, moderate, extensive.)

7 Evaluation projects

Dr Stephen Biggart from NHS Lothian has kindly shared with us the results of a recent survey of use of the Edinburgh Royal Infirmary of Edinburgh Anaesthesia toolkit. This shows that the majority of consultants are using it weekly or monthly, mainly to access clinical protocols, with a secondary purpose being education and training purposes. They tend to find information by navigating by specialty rather than keyword searching, and had some useful recommendations for future development, such as access to quick reference guidance.

We’d really appreciate you sharing any other local evaluations of RDS in this way – it all helps to build the evidence base for impact.

If you have any questions about the content of this newsletter, please contact his.decisionsupport@nhs.scot  If you would prefer not to receive future newsletters, please email Olivia.graham@nhs.scot and ask to be removed from the circulation list.

 

With kind regards

 

Right Decision Service team

Healthcare Improvement Scotland

Red – For medicines normally initiated and used under specialist guidance

Introduction

Description

Anaesthetic agent used with specialist supervision as a third-line analgesic to manage complex pain. It is an N-methyl-D-aspartate (NMDA) receptor inhibitor. This use is outside the UK marketing authorisation.

 

note: syringe pump and syringe driver are both relevant terms

Preparations

(Note: Will need indication for use on prescription, for example ‘for nerve pain’)

Ketamine injection

  • Used by subcutaneous injection/ infusion.
  • Specialists occasionally give ketamine IV – see below.
  • Preparations: 10mg/ml (20ml ampoule), 50mg/ml (10ml vial)

Ketamine oral solution

  • 50mg/5ml (unlicensed specials medicine)
  • (This is the preferred strength but other options are available)
  • Injection may be given orally

Ketamine is a Schedule 2 CD (Controlled Drug), therefore all prescriptions must satisfy CD prescription requirements to be valid and include details of the dose, form, strength, directions for use and total quantity (in both words and figures). It must also follow CD storage and recording regulations.

Sample prescription

 

Indications

Unlicensed

  • Neuropathic pain poorly responsive to titrated opioids and oral adjuvant analgesics (for example antidepressant and/or anticonvulsant) particularly when there is abnormal pain sensitivity - allodynia, hyperalgesia or hyperpathia.
  • Complex ischaemic limb pain or phantom limb pain.
  • Poorly controlled incident bone pain (often has a neuropathic element).
  • Complex visceral/abdominal neuropathic pain.

 

Cautions

  • Use low doses, carefully monitored, in cardiac failure, cerebrovascular disease, ischaemic heart disease.
  • If used for over 3 weeks and there is a need to stop treatment, discontinue ketamine gradually.
  • Consider dose reduction in severe hepatic impairment.

 

Contra-indications

  • Do not use ketamine if patient has raised intracranial pressure; uncontrolled hypertension, delirium or recent seizures; history of psychosis.

 

Drug interactions

  • Ketamine interacts with theophylline (tachycardia, seizures) and levothyroxine (monitor for hypertension, tachycardia).
  • Diazepam increases the plasma concentration of ketamine.
  • Refer to relevant British National Formulary (BNF) section for further information.

 

Side effects

  • Hallucinations, dysphoria and vivid dreams.
  • Hypertension, tachycardia, raised intracranial pressure.
  • Sedation at higher doses.
  • Erythema and pain at infusion site.
  • Urinary tract symptoms, for example frequency, urgency, urge incontinence, dysuria and haematuria. (Where there is no evidence of bacterial infection, consider discontinuing ketamine and seeking urology advice.)

 

Dose and administration

Starting ketamine

  • Ketamine is started on the recommendation of a palliative medicine consultant. This is usually done in an inpatient setting.
  • Very occasionally, a patient may need to start ketamine in the community. The route of choice is generally oral ketamine. The palliative medicine consultant will liaise closely with the GP, community nurse, and unscheduled care service.
  • 24-hour palliative medicine advice will be available.
  • Patients starting ketamine will be taking a regular opioid. Ketamine may restore the patient’s opioid sensitivity and lead to opioid toxicity.
  • The specialist may recommend changing to a short acting, regular opioid before starting ketamine, particularly if the patient has side effects from the current opioid dose.
  • Monitor closely for signs of opioid toxicity (for example sedation, confusion); reduce opioid dose by one third if the patient is drowsy and seek advice.
  • Hallucinations/dysphoria. If the patient is not drowsy this is more likely to be a ketamine side effect than due to opioids.
  • Give QThaloperidol oral 500micrograms to 1mg twice daily or SC 1mg to 2mg once daily. Midazolam SC 2mg as needed can also be used.
  • Preventing ketamine dysphoria – consider oral QThaloperidol 500micrograms to 1mg daily when starting ketamine. It can be stopped when the patient’s ketamine dose is stable.

 

Dose and administration – oral ketamine

  • Ketamine can be started using the oral route or patients may be changed from an SC infusion when pain is controlled.
  • Starting dose: 5mg to 10mg four times daily.
  • Increase dose in 5mg to 10mg increments.
  • Usual dose range: 10mg to 60mg four times daily.

 

Dose and administration – subcutaneous ketamine infusion

  • Starting dose: 50mg to 150mg/24 hours.
  • Review daily; increase dose in 50mg to 100mg increments.
  • Usual dose range: 50mg to 600mg/24 hours (higher doses are occasionally used in specialist units).

 

Administration

  • Prepare a new syringe every 24 hours.
  • Dilute ketamine with sodium chloride 0.9%.
  • Check the syringe is not cloudy and protect it from light.
  • Ketamine stability and compatibility – refer to syringe pump ketamine compatibility table.
  • Dispose of the ketamine vial in accordance with the local policy.
  • Rotate the SC infusion site daily to prevent site reactions. If these occur, increase the volume of sodium chloride 0.9% used to dilute the ketamine if possible and/or add a maximum of 1mg of dexamethasone injection to the ketamine infusion.

 

Converting from a 24-hour SC ketamine infusion to oral ketamine

  • Oral ketamine is more potent than SC ketamine (due to liver metabolism). Many patients require a dose reduction of 25 to 50% when changing to oral ketamine.
  • Prescribe the oral ketamine in divided doses - four times daily.
  • Titrate dose in 5mg to 10mg increments.
  • Some specialists stop the SC infusion when the first dose of oral ketamine is given. Others gradually reduce the infusion dose as the oral dose is increased.

 

 Dose and administration – parenteral ketamine

  • Palliative medicine consultants or anaesthetists occasionally administer SC or IV ketamine as single or ‘pulsed’ doses for severe pain or to cover painful procedures.
  • Specialists have used IV ketamine infusions to manage ischaemic limb pain.

 

Practice points

Patient monitoring

  • Patients who are at risk of hypertension, tachycardia, respiratory depression or opioid toxicity should only start ketamine in a clinical area able to monitor them 2 to 4 hourly for the first 24 hours.
  • All patients should be medically reviewed at least once daily until stable, and then weekly.
  • Once the pain is controlled, the palliative medicine specialist may recommend a gradual reduction in the dose of opioid and/or ketamine.

 

Blood pressure

  • Check blood pressure is normal or well controlled before starting ketamine. Record a baseline blood pressure.
  • Check blood pressure one hour after the first dose of oral ketamine or starting a SC infusion.
  • Check blood pressure 24 hours after the first dose of ketamine, then daily.
  • If blood pressure increases 20mmHg above baseline inform the patient’s doctor.
  • If blood pressure remains elevated 20mmHg above baseline on repeated measurement, stop the ketamine and seek advice from a palliative medicine specialist.

 

 Pulse

  • Record a baseline pulse rate.
  • Check pulse one hour after the first dose of ketamine or starting SC infusion.
  • Check pulse 24 hours after the first dose of ketamine, then daily.
  • If pulse rate increases 20bpm above baseline or rises above 100bpm, inform the patient’s doctor.
  • If there is no other cause of tachycardia, seek advice from a palliative medicine specialist.

 

Respiratory rate

  • Record a baseline respiratory rate.
  • The palliative medicine specialist will advise on frequency of monitoring.
  • If respiratory rate decreases to 10 breaths/minute inform medical staff. Seek advice from a palliative medicine specialist.
  • Naloxone (in small titrated doses) is only required for reversal of life-threatening respiratory depression due to opioid analgesics, indicated by:
    • a low respiratory rate, fewer than 8 respirations/minute
    • oxygen saturation below 85%, patient cyanosed.
  • Naloxone should not be given in large bolus doses as it can precipitate an acute opioid withdrawal reaction. Refer to Naloxone guideline.

 

Dysphoria, hallucinations, vivid dreams

Assess patient daily until ketamine dose is stable; then stop any regular QThaloperidol or midazolam.

 

Patient and carer advice points

  • There can be a delay of several days in obtaining further supplies of ketamine. Advise patients to ensure new supplies are requested in adequate time.
  • The taste of ketamine can be unpleasantly bitter. Patients can suck or chew on something sweeter after taking. Other flavours can also be requested.

 

References

Prommer EE. Ketamine for pain: An update of uses in Palliative Care. Journal of Palliative Medicine 2012;15(4):474-483.

Quibell R, Prommer EE, Mihalyo M. Ketamine. Journal of Pain & Symptom Management 2011;41(3):640-649.

Twycross R and Wilcock A. Palliative Care Formulary (Fourth Edition). Palliativedrugs.com Ltd, Nottingham, 2011.

Hanks G et al. The Oxford Textbook of Palliative Medicine (Fourth edition). Oxford Univeristy Press, 2010.

Fallon M, Welsh J. The role of ketamine in pain control. European Journal of Palliative Care 1996; 3:143-146.

Mercadante S. Ketamine in cancer pain: an update. Palliative Medicine 1996; 10: 225-230.

Edmonds P. The role of ketamine in the management of chronic pain. CME Bulletin Palliative Medicine 1998; 1:3-5.

Grant I, Nimmo W, Clements J. Pharmacokinetics and analgesic effects of IM and oral ketamine. British Journal of Anaesthesia 1981; 53:805-809.

Enarson M, Hays H, Woodroffe M. Clinical experience with oral ketamine. Journal Pain & Symptom Management 1999; 5: 384-386.

Bell RF. Low-dose subcutaneous ketamine infusion and morphine tolerance. Pain 1999; 83: 101-103.

Fitzgibbon E, Hall P, Schroder C et al. Low Dose Ketamine as an Analgesic Adjuvant in Difficult Pain Syndromes: A Strategy for Conversion from Parenteral to Oral Ketamine. Journal Pain & Symptom Management 2002; 23(2): 165-170.

Beitez-Rosario M, Feria M, Salinas-Martin A. A retrospective comparison of the dose ratio between subcutaneous and oral ketamine. Journal Pain & Symptom Management 2003; 25: 400-402.

Kannan T, Saxena A, Bhatnagar, Barry A. Oral ketamine as an adjuvant to oral morphine for neuropathic pain in cancer patients. Journal Pain & Symptom Management 2002; 23: 6065.

Bell R, Eccleston C, Kalso E. Ketamine as an adjuvant to opioids for cancer pain (Cochrane Review). In: The Cochrane Library. Issue 3, 2004. Oxford: Update Software.

Hocking G, Cousins M. Ketamine in chronic pain management: an evidence-based review. AnaesthAnalg. 2003; 97: 1730-9.

Visser E, Schug S. The role of ketamine in pain management. Biomedicine and Pharmacotherapy 2006; 60: 341-348.

Webster L, Walker M. Safety and efficacy of prolonged outpatient ketamine infusions for neuropathic pain. American Journal of Therapeutics 2006; 13: 300-5.

 

Stability references

Watson D, Lin M, Morton A et al. Compatibility and stability of dexamethasone sodium phosphate and ketamine hydrochloride subcutaneous infusions in polypropylene syringes. Journal Pain & Symptom Management 2005; 30: 80-86.

Twycross R and Wilcock A. Palliative Care Formulary (Fourth Edition). Palliativedrugs.com Ltd, Nottingham, 2011.

Dickman A, Schneider J and Varga J. The Syringe Driver (Third Edition). Oxford University Press 2011.