Trial PaperDepressive DisordersAnxiety DisordersChronic PainPalliative & End-of-Life DistressLSD

LSD in the supportive care of the terminally ill cancer patient

This open-label case study (1985, n=4) describes the experience of administrating LSD (100-400μg, multiple sessions) in supportive circumstances but without much knowledge of set & setting and effective therapeutic interventions.

Authors

  • Albert Kurland

Published

Journal of Psychoactive Drugs
individual Study

Abstract

From the conclusion: In the search for new techniques that might enhance the efficacy of psychotherapy, particularly in those patients whose motivational powers have been weakened or lost, a compound such as LSD may hold considerable promise. This is reinforced by the fact that the experiences in this study indicate that trained personnel can implement the psychedelic procedure with relatively high safety and replicate its major objective, the peak experience, to a degree that makes the phenomenon difficult to sweep under the experimental rug. At the same time, it underscores the need for controlled studies, an objective that may be very difficult to achieve in view of the unique nature of the drug experience and its therapeutic objective.

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Research Summary of 'LSD in the supportive care of the terminally ill cancer patient'

Editorial

βBlossom's Take

This paper sits in the Spring Grove line of end-of-life LSD work, but from a later and more provisional angle. Its value is in showing how the programme tried to generalise beyond a single dramatic case report, while still making plain that the apparent benefit depended on preparation, support, and careful patient selection.

Introduction

Supportive care for terminal cancer patients often fails to address psychological suffering alongside physical symptoms, and persistent pain plus heavy use of narcotics can restrict awareness and impede psychotherapeutic efforts. Earlier anecdotal and small observational reports suggested that lysergic acid diethylamide (LSD) can alter perception, reduce pain and sometimes produce profound meaningful or mystical experiences that might relieve despair and facilitate communication between dying patients and their families. Prior work cited by the author includes chemotherapeutic use of LSD as an analgesic and literary and clinical accounts that framed mystical states as potentially helpful at the end of life. Kurland and colleagues initiated an experimental programme to evaluate LSD administered within a structured psychotherapeutic framework they term psychedelic peak psychotherapy. The intervention sought to maintain patient awareness while easing depression, anxiety and pain, and to encourage a peak or “psychedelic” experience that could reduce isolation and enhance interpersonal connection. The programme grew from a single unplanned clinical treatment of a staff member and the authors set out to describe their methods, clinical vignettes and impressions of safety and therapeutic effect in terminal cancer patients.

Methods

The intervention programme enrolled terminal cancer patients referred for significant pain, depression, tension, anxiety or psychological isolation and required an estimated life expectancy of at least three months to allow assessment of the duration of effects. Cardiovascular disease and central nervous system complications were exclusion criteria. At referral a psychiatrist discussed benefits, risks and the noncurative intent of the treatment with patient and family. Treatment consisted of three phases. Preparatory psychotherapy typically lasted two to three weeks and involved six to 12 hours of interviews and psychometric testing; sessions focused on current relationships, awareness of diagnosis/prognosis, intrapsychic conflicts and making life meaningful rather than deep excavation of long‑standing conflict. One week before dosing, tranquilizers were stopped while maintenance medications continued. The LSD session occupied a day with a male–female therapist dyad present; patients reclined wearing eyeshades and headphones and listened to a preselected music programme intended to structure imagery. Dosing was individualised: initial oral doses typically began at 200–300 micrograms and could be escalated (authors report up to about 600 micrograms) if anxiety or clinging-to-reality persisted. Non‑verbal support, brief intermittent verbal contact and family visits during re‑entry were part of the session protocol. Integration psychotherapy began the day after dosing and continued for several days to a week, including a written or verbal account of the session; further sessions were offered only if peak experience had not been attained or symptoms later recurred. The extracted text presents these procedural details and several case vignettes. It does not specify a formal sample size for the whole programme, randomisation, control conditions or quantitative analysis methods; outcomes are reported qualitatively in clinical descriptions and selected psychometric data for individual patients (for example, an MMPI retest for one patient).

Results

The paper presents a series of clinical vignettes illustrating a range of responses. The extracted text does not clearly report the total number of patients treated in the programme; four individual cases are described in detail. Patient 1 was a 43‑year‑old female staff member with metastatic breast cancer who underwent three weeks of preparation and received 100 micrograms of LSD in the session described. She reported a profound peak experience with intense imagery, a strong sense that love was the core of life, renewed closeness with family and a radiant affect afterwards. Objective psychometric testing (MMPI) one and two weeks before and after the session showed a significant reduction on the depression scale and lessening of pathological signs. She died about five weeks after the session from progressive disease. Patient 2 was a 58‑year‑old woman with long‑standing metastatic breast cancer and spinal involvement. She received multiple LSD treatments (reported as four sessions over about two years). Initial doses (reported at 300 micrograms for the first session) produced only partial peak reactions but were followed by marked improvements in mood, motivation and interpersonal closeness. After the first session she engaged intensively in physiotherapy and progressed from paralysis to walking with aids over months. Subsequent sessions produced intense mystical‑type experiences, transient relief of pain and periods of marked interpersonal reconciliation; she participated in her daughter’s wedding and later requested further sessions when pain recurred. She died shortly after an attempted hypophysectomy when haemorrhage prevented completion of the operation. Patient 3, a 43‑year‑old woman with metastatic pancreatic cancer and severe pain, had a limited initial response to a 250 microgram session but, after an intensified preparatory period, received a second 400 microgram session that produced several psychedelic peak reactions, improved mood and better tolerance of pain; she was discharged home and spent her remaining weeks with family, dying about a month later. Patient 4, a 56‑year‑old woman with advanced uterine cancer and marked physical debility, showed little therapeutic engagement. She received two 100 microgram oral doses one hour apart but suffered severe diarrhoea and pain during the session that prevented immersion in the experience; the session was halted with intramuscular chlorpromazine. Some subsequent relaxation and increased non‑verbal communication with therapists and family were noted, but the patient died 22 days later. Across the clinical material the authors report a spectrum of outcomes: approximately one third of patients reportedly attained maximal, peak‑type responses with relief of fear, depression and isolation; another third derived some benefit without dramatic change; and the remaining third were nonreactors. Adverse physiological effects noted in the programme included transient headaches, tremor, nausea, palpitations and breathing difficulties, but the authors state there was no evidence that LSD aggravated cancer symptoms or materially worsened medical status. No deaths were attributed to LSD in the extracted text.

Discussion

Kurland discusses several unresolved questions about mechanisms, emphasising that the psychedelic state’s psychological diversity suggests that nondrug contextual factors (personality, preparation, set and setting) do not fully account for the experiences and therapeutic outcomes. The authors raise the open question of whether observed benefits are attributable to LSD’s pharmacology alone, the psychotherapeutic context, or an interaction of both, and note that prior investigators who moved from purely chemotherapeutic use to more psychologically informed approaches reported improved emotional outcomes. A central point in the authors’ interpretation is that attainment and stabilisation of a psychedelic peak experience appears critical to clinical benefit; they report that roughly one third of patients achieved such peaks and experienced marked reductions in fear of death, depression and social isolation. The discussion also considers a possible analgesic component to LSD that may be partly independent of emotional change, citing earlier reports that suggested longer‑lasting analgesia compared with some narcotics. The authors propose psychological mechanisms including enhanced internal locus of control, catharsis/abreaction, rapid access to depth material and reshaping of values as contributors to improved coping. Limitations are acknowledged: mechanisms remain unclear, responses vary widely between individuals, and it is not understood why some patients peak while others do not. The authors emphasise the need for controlled studies to identify predictors of response and to compare psychedelic‑assisted psychotherapy with counselling or non‑drug psychotherapeutic approaches, but they observe that the distinctive and ineffable nature of the drug experience poses methodological challenges for such trials. Safety observations are cautiously optimistic: when delivered by trained personnel in this setting, LSD was described as medically tolerable even in gravely ill patients, yet further systematic evaluation was deemed necessary.

Conclusion

The authors conclude that LSD administered within a structured, psychotherapeutically informed programme may hold promise as an adjunct to supportive care for terminal cancer patients, particularly for those with diminished motivation or intense psychological suffering. They state that trained teams can implement the procedure with a reasonable safety profile and replicate the intended peak experience in a proportion of patients, but they stress the imperative for controlled research despite practical difficulties in studying such an unusual therapeutic objective.

Study Details

Related Clinical Trial

Completed

Spring Grove / Maryland Psychiatric Research Center LSD-Assisted Psychotherapy Program for Terminal Cancer (Pahnke, Grof, Richards, Kurland ~1965–1972)

Uncontrolled open pilot clinical series of LSD- and DPT-assisted psychotherapy for terminal cancer patients conducted at Spring Grove State Hospital and the Maryland Psychiatric Research Center, Baltimore MD (~1965–1972; key investigators: Walter Pahnke, Stanislav Grof, William Richards, Albert Kurland). Total n~60 terminal cancer patients by July 1972 (P1 reports n=31 in earlier series; P2/P5 overlap with later cohort). Participants: referred for significant pain, depression, tension, anxiety or psychological isolation; estimated life expectancy ≥3 months. Sessions: single supervised psychedelic session (LSD 200–500 mcg IM, modal 300 mcg; or DPT 60–105 mg parenterally for shorter effect), with male-female therapist dyad, eyeshades, headphones, classical music, family involvement at termination. Preparatory psychotherapy ~6–12 h; integration psychotherapy beginning day after session. Outcome: Pahnke-Richards 7-domain observer rating (depression, isolation, fear of death, pain, etc. −6 to +6) by therapists, nurses, physicians, family; narcotic scale for analgesic use. Repeated sessions permitted if peak experience not achieved or symptoms recurred. No control arm; no registration (pre-registration era). Multiple publications report overlapping cohorts: Pahnke WN (1972, book chapter); Grof S et al. (Int Pharmacopsychiatry 1973, PMID 4140164); Kurland AA (J Psychoactive Drugs 1985, PMID 2418186).

Started
Type
interventional
Randomized
No
Registry ID
SPRING-GROVE-1965-1972-LSD-DPT-TERMINAL-CANCER-PROGRAM

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