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Guidelines for ketamine use in clinical psychiatry practice

Published online by Cambridge University Press:  10 May 2024

Luke A. Jelen*
Affiliation:
The Maudsley Hospital, London, UK; and Institute of Psychiatry, Psychology & Neuroscience, King's College London, UK
Rupert McShane
Affiliation:
Department of Psychiatry, Oxford University, UK; and Oxfordshire ECT and Ketamine Service, Oxford, UK
Allan H. Young
Affiliation:
Centre for Affective Disorders, Institute of Psychiatry, Psychology & Neuroscience, King's College London, UK
*
Correspondence: Luke A. Jelen. Email: [email protected]
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Abstract

In this editorial, we emphasise the efficacy and challenges of using ketamine in treatment-resistant depression. We highlight the need for comprehensive evidence-based guidelines to manage the use of both licensed and off-licence ketamine formulations and discuss recent efforts by Beaglehole et al to develop ketamine guidelines in New Zealand. We finally advocate for national registries to monitor ketamine therapy, ensuring its responsible and effective use in the management of depression.

Type
Editorial
Creative Commons
Creative Common License - CCCreative Common License - BY
This is an Open Access article, distributed under the terms of the Creative Commons Attribution licence (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted re-use, distribution and reproduction, provided the original article is properly cited.
Copyright
Copyright © The Author(s), 2024. Published by Cambridge University Press on behalf of Royal College of Psychiatrists

The efficacy of ketamine in the treatment of treatment-resistant depression (TRD) is well documented,Reference Jelen and Stone1,Reference Marcantoni, Akoumba, Wassef, Mayrand, Lai and Richard-Devantoy2 and ketamine-based therapies offer new therapeutic hope for those that do not experience beneficial outcomes from conventional antidepressants. Consequently, there has been growing interest in incorporating the use of ketamine into psychiatry in diverse settings across the globe. However, the transition of ketamine treatments from research and specialist settings to routine clinical practice poses significant challenges, including concerns over potential misuse, dissociative effects and uncertainty regarding longer-term risks.

Ketamine is a racemic mixture composed of equal amounts of (S)- and (R)-ketamine (esketamine and arketamine).Reference Jelen, Young and Stone3 Although an esketamine nasal spray has been developed and licensed for use in TRD (in combination with a conventional antidepressant) in Europe and New Zealand, neither the National Institute for Health and Care Excellence nor Pharmac (respective government agencies that evaluate cost-effectiveness of new treatments) has approved its public use. For some, the licensing of esketamine for TRD remains a controversial decision, and this has been a topic of considerable debate.Reference Horowitz and Moncrieff4,Reference Kasper, Young, Vieta, Goodwin and Meyer-Lindenberg5 In the UK, although there has been some limited National Health Service use of nasal esketamine, approved on a named-patient basis, its availability is primarily confined to select, often costly, private providers. Owing to the risks of sedation, dissociation and misuse, in certain countries intranasal esketamine is only available through a restricted distribution system under a risk evaluation and mitigation strategy that specifies standards for healthcare settings, pharmacies and healthcare professionals administering the drug.

Meanwhile, the use of racemic ketamine for depression is increasing across public and private sectors as a cost-efficient off-label approach. Intravenous (i.v.) administration of ketamine is recognised as the gold standard for off-label use, with the best supporting evidence for efficacy in TRD.Reference Marcantoni, Akoumba, Wassef, Mayrand, Lai and Richard-Devantoy2 Other modes of administering ketamine including subcutaneous, intramuscular (i.m.), oral and sublingual are being explored but require further research to validate their relative safety and efficacy and to determine the optimal dosing regime in each case. Each administration route presents distinct advantages and challenges relating to bioavailability, effect duration, practicality and patient comfort. Importantly, none of these treatment modes for racemic ketamine has received regulatory approval for on-label use for any psychiatric indication. As a result, there are no formal surveillance data on safety and effectiveness.Reference Sanacora, Frye, McDonald, Mathew, Turner and Schatzberg6 Therefore, there is a critical need to establish international expert consensus opinion, alongside comprehensive and clear guidelines to manage off-label use, including dosage recommendations for different administration routes and requisite monitoring practices.

To date, the major evidence-based guidelines for treating depressive disorders have either not mentioned7 or only briefly touched on ketamine, with no formal recommendation for its use in depressionReference Cleare, Pariante, Young, Anderson, Christmas and Cowen8,Reference Bauer, Pfennig, Severus, Whybrow, Angst and Möller9 aside from that limited to specialist academic treatment centres.Reference Kennedy, Lam, McIntyre, Tourjman, Bhat and Blier10 However, a key consensus paper from an international group of mood disorders experts provides a helpful synthesis with respect to the efficacy, safety and tolerability of ketamine and esketamine in TRD.Reference McIntyre, Rosenblat, Nemeroff, Sanacora, Murrough and Berk11 This review of the evidence supports the rapid-onset efficacy (within 1–2 days) of esketamine and ketamine in TRD, which is best established for intranasal esketamine and i.v. ketamine routes. Conversely, there is rather limited evidence supporting the efficacy of oral, subcutaneous or i.m. ketamine in TRD. Intranasal esketamine has proven effective, safe and tolerable for up to 1 year in TRD, although the long-term effects of i.v. ketamine remain insufficiently studied.Reference Wajs, Aluisio, Holder, Daly, Lane and Lim12 Both ketamine and esketamine give rise to safety concerns encompassing psychiatric (dissociation, psychotomimetic and increased suicidality), neurological/cognitive, genitourinary and hemodynamic effects that require monitoring. The Ketamine Side Effect Tool was been developed as one approach to systematically monitor and report ketamine-related side-effects.Reference Short, Dong, Gálvez, Vulovic, Martin and Bayes13 Considering safety concerns, the consensus view is that these compounds should be administered in environments with multidisciplinary personnel, including experts in mood disorder assessment. To aid clinicians and healthcare providers, a detailed discussion of the risks and practical recommendations for the use of oral, sublingual and nasal ketamine has been recently outlined.Reference Swainson, Klassen, Brennan, Chokka, Katzman and Tanguay14

We welcome the efforts by Beaglehole et alReference Beaglehole, Glue, Clarke and Porter15 to establish ketamine guidelines for use by adult specialist mental health services in New Zealand. A particularly novel aspect is that they seek to address the need for long-term treatment in a way that is scalable in a public health service. The primary identification of TRD patients for potential ketamine treatment provides a reasonable pathway for identifying those in need of intervention. The authors highlight a paradox in the clinical adoption of off-label ketamine for treating depression: clinicians’ hesitance to use it is perpetuated by a lack of first-hand experience. The underpinning published research, on its own, appears to have been insufficiently persuasive to overcome this hesitancy and risk aversion. To address this, the authors propose an approach beginning with i.m. administration to gauge patient response, followed by an oral regimen. It is reasonable to use parenteral administration as a test of responsiveness and then follow this with something more pragmatic, but, as described, the current evidence base is for i.v. not i.m.; i.m. may give a variable response that depends more on administration technique. Another challenge the authors highlight is establishing the requisite experience level for psychiatrists to prescribe ketamine. It is recommended that psychiatrists observe at least three i.m. administrations to become acquainted with the dissociative effects experienced by patients. The guidelines suggest a maximum treatment duration of 12 weeks. This duration is a balance between practicality – allowing sufficient time to evaluate clinical responses and reinforce benefits – and caution, as the authors were reluctant to endorse long-term treatment. However, this approach could introduce complications, especially as ketamine-responders may, like responders to esketamine nasal spray, be at a high risk of relapse following cessation of regular dosing. Finally, we agree with the authors about the necessity of diligent monitoring in ketamine therapy clinics, with particular emphasis on assessing mood and cognitive function, which are crucial indicators of a patient's response to ketamine treatment. However, although the guidelines promote oral administration as a strategy to enhance treatment accessibility, this approach potentially increases the risks associated with overuse and potential misuse. Therefore, it underscores the need for more stringent oversight across any healthcare facilities offering ketamine therapies.

To address safety concerns and monitor the effectiveness of ketamine treatments, we believe it is crucial to establish mandatory national registers encompassing all individuals receiving these treatments, whether licensed or unlicensed. Such registries would address risk mitigation, facilitate pharmacovigilance and enable tracking of patient outcomes across diagnoses, routes and doses. In every state of the USA and in the Australian states of Queensland, Victoria and South Australia, Prescription Drug Monitoring Program mandate that prescriptions of controlled substances to be taken at home are logged centrally and that prescribers check before prescribing. This should be extended to ketamine, including in-clinic administration. The growing use of oral ketamine, which increases potential risks of overuse and diversion, emphasises the need for closer surveillance. Indeed, the recent legalisation of telehealth consultations and postal supply of ketamine in the USA during COVID increased access but raised concerns regarding patient safety, given the lack of rigorous monitoring. Significant efforts are being made towards reformulating oral ketamine to manage its misuse potential,Reference Glue, Loo, Fam, Lane, Young and Surman16 and ketamine formulations will be entering phase 3 trials. Therefore, guidelines need to focus on regulating the use of compounded oral or sublingual liquids, lozenges or capsules. Finally, owing to the limited long-term real-world dosing data for ketamine, a national registry would also allow for tracking of outcomes across different routes and doses, which could help to optimise treatment. Therefore, these registers are vital for ensuring optimal cost-effectiveness, patient safety and treatment efficacy. Voluntary registries, such as those used to improve service delivery of electroconvulsive therapy,Reference Martin, Gálvez, Lauf, Dong, Baily and Cardoner17 offer an alternative to mandatory national registries. These registries could be expanded to include treatments such as ketamine and esketamine, providing a framework for data collection and a shared clinical registry, informing how care is being delivered.

As we work to broaden the availability of ketamine treatments to those with TRD, any framework that promotes its use in a manner that is safe, effective and equitable is a step in the right direction. Refining our guidelines and vigilant monitoring will be imperative as we further our understanding of both the benefits and the limitations associated with ketamine therapy.

Author contributions

L.A.J.: writing – original draft; R.M.: writing – review and editing; A.H.Y.: writing – review and editing.

Funding

L.A.J. is supported by a Medical Research Council Clinical Research Training Fellowship (MR/T028084/1).

Declaration of interest

R.M. has received remuneration for advisory board and education work and conference attendance from Janssen. A.H.Y. is Deputy Editor of BJPsych Open; has provided paid lectures and served on advisory boards for the following companies with drugs used in affective and related disorders: Flow Neuroscience, Novartis, Roche, Janssen, Takeda, Noema Pharma, Compass, AstraZeneca, Boehringer Ingelheim, Eli Lilly, LivaNova, Lundbeck, Sunovion, Servier, Allegan, Bionomics, Sumitomo Dainippon Pharma, Sage and Neurocentrx; Principal Investigator on the Restore-Life VNS registry study funded by LivaNova; Principal Investigator on ESKETINTRD3004: ‘An open-label, long-term, safety and efficacy study of intranasal esketamine in treatment-resistant depression’, ‘The effects of psilocybin on cognitive function in healthy participants’, ‘The safety and efficacy of psilocybin in participants with treatment-resistant depression (P-TRD)’, ‘A double-blind, randomized, parallel-group study with quetiapine extended release as comparator to evaluate the efficacy and safety of seltorexant 20 mg as adjunctive therapy to antidepressants in adult and elderly patients with major depressive disorder with insomnia symptoms who have responded inadequately to antidepressant therapy’ (Janssen), ‘An open-label, long-term, safety and efficacy study of aticaprant as adjunctive therapy in adult and elderly participants with major depressive disorder (MDD)’ (Janssen), ‘A randomized, double-blind, multicentre, parallel-group, placebo-controlled study to evaluate the efficacy, safety, and tolerability of aticaprant 10 mg as adjunctive therapy in adult participants with major depressive disorder (MDD) with moderate-to-severe anhedonia and inadequate response to current antidepressant therapy’ and ‘A study of disease characteristics and real-life standard of care effectiveness in patients with major depressive disorder (MDD) with anhedonia and inadequate response to current antidepressant therapy including an SSRI or SNR’ (Janssen); UK Chief Investigator for Compass, COMP006 and COMP007 studies; and UK Chief Investigator for Novartis MDD study MIJ821A12201. Grant funding (past and present): NIMH (USA), CIHR (Canada), NARSAD (USA), Stanley Medical Research Institute (USA), MRC (UK), Wellcome Trust (UK), Royal College of Physicians (UK), BMA (UK), UBC-VGH Foundation (Canada), WEDC (Canada), CCS Depression Research Fund (Canada), MSFHR (Canada), NIHR (UK), Janssen (UK) and EU Horizon 2020. No shareholdings in pharmaceutical companies.

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