Treatment-resistant depression (TRD) is a common disease. It is calculated that from 60% to 70% of patients will respond to a first-line monotherapy, and that more than one third will be therapy-resistant,1 considering those patients who fail to respond to 2 different antidepressives at suitable doses and for a suitable duration to be resistant.2 Electroconvulsive therapy (ECT) has been shown to be highly effective in as a therapy for TRD as well as safe, even in geriatric patients.3 In spite of this, this, a significant number of subjects do not respond to ECT with conventional anaesthetics. We present 2 cases of TRD treated using ECT associated with ketamine.

Case 1: an 80 year-old male with a history of colon and lung adenocarcinoma, currently disease-free, with no history of psychiatric problems or known cognitive deterioration, who was admitted due to a severe depressive episode with psychotic symptoms (DSM-5 296.24 [F32.3]) evolving over 4 months without responding to 20mg/day Citalopram and 25mg/day Quetiapine; Hamilton Depression Rating Scale of 17 items4 (HDRS-17)=23. Treatment was gradually commenced with 225mg/day Venlafaxine, 45mg/day Mirtazapine, 5mg/day Olanzapine and 100mg/day Nortriptyline, without improvement. To manage anxiety 192mg Clometiazol was used to varying degrees throughout treatment. Concomitantly, 12 sessions of basic bitemporal ECT were applied (3 sessions/week) (pulse amplitude 1.0ms and 36J energy increasing to 88.3J using changes in frequency and stimulus duration), with 175mg pentothal as anaesthetic. A suboptimum electrocephalographic average convulsion time was detected (avct) (16.58s/session) and short periods of confusion and disorientation were observed post-administration. Given the persistence of depressive symptoms (HDRS-17=18) palliative treatment was initiated using 6 sessions of endovenous ketamine on alternate days (0.63mg/kg) with a notable improvement in symptoms (HDRS-17=5 following 2 sessions) which was no sustained over time (HDRS-17=19, 15 days after the end of the treatment).

Finally, after withdrawing Nortriptyline due to lack of effectiveness, 9 bilateral basic ECT sessions with ketamine as the anaesthetic were tried (0.9–1.34mg/kg), achieving a suitable avct (28.36s/session) while it was possible to reduce the energy to 75J, keeping an amplitude of 1.0ms, with good tolerability. The patient suffered the complication of a septic shock secondary to infection of the central catheter that made it necessary to suspend the ECT during 12 days. It was restarted with 8 sessions more per week of ECT-ketamine, showing a clear improvement in symptoms (HDRS-17=2). The patient is currently in remission 14 months after discharge, with maintenance ECT-ketamine (monthly) and 75mg/day Venlafaxine and 30mg/day Mirtazapine.

Case 2: a 69 year-old male without a medical-surgical or psychiatric record or known cognitive deterioration (mini mental state examination=27) who was admitted due to an episode of severe depression with psychotic symptoms (DSM-5 296.24 [F32.3]) that had evolved over 8 months. It had hardly responded to previous treatments with 100mg/day Sertraline, 30mg/day Citalopram and 225mg/day Venlafaxine combined with low doses of antipsychotic drugs. During admission 175mg/day Imipramine was tried, together with 30mg/day Mirtazapine and 15 sessions of basic bitemporal ECT (amplitude 1.0ms; energy 43J), with 200mg pentothal and avct=23s/session, with episodes of disorientation and loss of short-term memory post-administration. Given the lack of response 11 basic sessions were applied of ECT-ketamine at 1.4mg/kg (energy 38J; avct=50.9s/session) with an improvement in symptoms (HDRS=8) and no side effects.

At discharge he presented a new recurrence of the disorder (HDRS-36) following the switch from Imipramine to Venlafaxine due to a lack of supply, and after finalising the ECT-ketamine sessions. It was then decided to use treatment with 112.5mg/day Clomipramine, 100mg/day Sertraline and the commencement of 800mg/day lithium without response, so that Imipramine was restarted at 100mg/day and 17 basic sessions of ECT-ketamine at 1.28mg/kg were administered (energy 31J; avct=44.3 Imipramine/session) with a clinical improvement (HDRS=12) and good tolerability. One month after discharge he was clinically stable without complete remission, in treatment with 75mg/day Imipramine, 150mg/day Quetiapine and 15mg/day Mirtazapine, while the outpatient department decided against maintaining ECT-ketamine.

Ketamine is an anaesthetic that is an antagonist of N-methyl-d-aspartate (NMDA) receptors; it is involved in the glutamatergic route and is of growing interest in the physiopathology of depression.5 Treatment with ketamine has been shown to have a swift antidepressive response, although its use is controversial and data on this in the literature are contradictary.6–8 A study conducted with 90 subjects with TRD showed faster and more sustained improvement in depressive symptoms, increasing cognitive protection and the duration of convulsion in those patients treated with anaesthetic doses of ketamine (0.8mg/kg) and ECT.9 Nevertheless, there is a notable lack of evidence on its safety and efficacy in elderly patients, who are a group especially susceptible to TRD.

We believe that in our progress towards an increasingly personalised and technical psychiatry,10 ketamine may be a valid alternative to the use of conventional anaesthetics, giving a longer avct, which could play an important role in improving observed antidepressive efficacy. These results, together with the reported cognitive protection9—which was not evaluated in our subjects—mean that it is a desirable option for elderly patients, although more evidence is required to evaluate its effectiveness and safety in this age group.