Toward a Computationally-Informed, Personalized Treatment for Hallucinations

Early Phase 1

Recruiting

• Conditions: Hallucinations, Auditory; Psychosis
• Interventions: Drug: Rivastigmine Transdermal System; Drug: Scopolamine; Drug: Placebo Patch

• Registration Number: NCT04366518
• Lead Sponsor: Yale University

Brief Summary

Auditory hallucinations are among the most distressing aspects of psychotic illness, and between 10 and 30% of people with hallucinations do not respond to antipsychotic medications. The authors have used computational modeling of behavior to link brain activity to development of auditory hallucinations in the hope of guiding new treatment development. The proposed studies take the first step toward individualized treatment approaches to hallucinations by attempting causal, pharmacological manipulation of relevant model parameters underlying these phenomena.

Detailed Description

Auditory verbal hallucinations (AVH) are present throughout the course of psychotic illness and are among its most distressing symptoms. The presence of hallucinations alone increases risk of suicide in patients with psychosis. While antipsychotic medications often succeed in ameliorating auditory hallucinations, 10-30% of those with hallucinations exhibit little to no response to these treatments. Understanding how the processes underlying auditory perception might go awry to produce auditory hallucinations is a critical next step in the development of new treatments that are more soundly based upon systems neuroscience and brain pathophysiology.

Perceptual systems do not rely entirely upon information coming from sensory organs like the retina and the cochlea. Rather, they blend this input with perceptual beliefs about the sensory environment in order to produce an internal model of that environment. The authors and others have proposed that hallucinations may be seen as an over-weighting of these perceptual beliefs when combined with sensory evidence during perceptual inference. In this work, the authors take advantage of a long history of sensory conditioning research to elicit hallucinatory experiences via traditional learning mechanisms: subjects are exposed to repeated pairings of visual and auditory stimuli and subsequently perceive the presence of the auditory stimulus when only the visual is present. The authors applied this Conditioned Hallucinations paradigm to four groups of subjects who varied orthogonally in having or not having hallucinations and psychosis. The authors found that conditioned hallucinations readily occur in all subjects but with markedly increased frequency in those who hallucinate compared to those who do not. The authors then employed a computational approach that formally models perception as a combination of prior knowledge and sensory input: the Hierarchical Gaussian Filter (HGF). Results indicate that the weight prior knowledge exerts during perception is significantly higher in those with hallucinations, and is related to prior-related functional activity specific brain regions like the anterior insula. This 'prior weighting' alteration may represent a novel, personalized, and computationally-informed target for the treatment of hallucinations.

Mathematically, prior weighting is the ratio of the precision of prior knowledge to the precision of incoming sensory evidence exhibited by an individual during perception. Therefore, it may be normalized by either decreasing the precision of prior knowledge or increasing the precision of incoming sensory evidence. The precision of sensory evidence appears to depend critically upon cholinergic signaling: acetylcholine increases auditory discrimination abilities and biases perceptual inference toward sensory data. Antagonism at central cholinergic receptors decreases sensory sensitivity and decreases reliance on incoming sensory evidence during perceptual inference. Consistent with this, scopolamine, a safe and reversible antagonist at the M1 cholinergic receptor used routinely for its anti-emetic effects, can both cause spontaneous hallucinations and enhance conditioned hallucinations. By contrast, increased cholinergic signaling ameliorates psychotic symptoms in schizophrenia and Alzheimer's Disease. Rivastigmine, a reversible, centrally-acting cholinesterase inhibitor, has been used study the cholinergic system and has been found to ameliorate hallucinations in some patients with schizophrenia.

The authors plan to characterize the effects of cholinergic agents on the perceptual, computational, physiological, and clinical signatures of hallucinations in healthy participants and individuals with psychosis via the following aims:

Aim 1: Characterize the effects of cholinergic antagonism on the behavioral, computational, and neural signatures of conditioned hallucinations in healthy subjects. Hypotheses: 1) Non-hallucinating healthy subjects will show increases in prior weighting and conditioned hallucinations with scopolamine vs. saline. 2) Scopolamine-related changes in prior weighting will be accompanied by increased prior-related activity in anterior insula on functional MRI (fMRI).

Aim 2: Determine the effect of cholinergic potentiation on the behavioral, computational, and neural signatures of conditioned hallucinations in subjects with psychosis and hallucinations. Hypotheses: 1) Subjects with hallucinations and high prior weighting will show decreases in prior weighting and conditioned hallucinations with rivastigmine patch vs placebo patch. 2) Rivastigmine-related changes in prior weighting will be accompanied by lower prior-related functional activity in anterior insula. 3) Subjects with hallucinations and lower prior weighting will show none of these physostigmine-related changes.

In proposing these aims, the authors apply a formalized, theoretical understanding of perceptual processing to probe the interplay between perceptual, computational, circuit-level, and neurotransmitter-level dysfunction seen in hallucinations. This approach also has the potential for an immediate clinical impact: it is the first attempt to leverage the powerful tools of computational psychiatry to identify distinct patient subgroups likely to respond to emerging cholinergically-mediated treatments for hallucinations.

Study Timeline

• Study First Submitted: 2020-03-24
• Study First Submitted QC: 2020-04-24
• Study First Posted: 2020-04-29
• Study Start: 2021-07-15
• Status Verified: 2024-07
• Last Update Submitted: 2024-07-23
• Last Update Posted: 2024-07-25
• Primary Completion: 2032-08
• Study Completion: 2032-08

Recruitment & Eligibility

• Status: RECRUITING
• Sex: All
• Target Recruitment: 35

Inclusion Criteria

• Age 18-65
• English speaking
• Right handedness
• Diagnosed with schizophrenia schizoaffective, schizophreniform, schizotypal, or brief psychotic disorder
• History of auditory verbal hallucinations occurring at least weekly

Exclusion Criteria

• Current substance dependence or active use as determined by drug test.
• Any neurological, medical or developmental problem that is known to impair cognition significantly
• Contraindications for MR scanning including metallic implants of any kind, pacemakers and history of accidents with metal, claustrophobia
• History of seizures
• History of violence
• History of suicide
• Pregnancy (determined by urine pregnancy test)
• Concurrent participation in any other intervention study
• History of urinary retention
• History of delirium
• Current use of any cholinergic or anticholinergic medication
• History of asthma, diabetes, and cardiovascular disease
• Evidence of cardiovascular disease on EKG
• Individuals who have been on dopamine-2 antagonists for less than 6 months (to limit risk of EPS)

Study & Design

• Study Type: INTERVENTIONAL
• Study Design: CROSSOVER

Arm && Interventions

Group	Intervention	Description
Aim 2: Those with psychosis/hallucinations	Rivastigmine Transdermal System	Participants who have a psychosis spectrum diagnosis and frequent auditory hallucinations will be given Rivastigmine capsule versus placebo capsule.
Aim 1: Healthy Controls	Placebo Patch	Healthy controls will be given scopolamine patches versus placebo patch.
Aim 2: Those with psychosis/hallucinations	Placebo Patch	Participants who have a psychosis spectrum diagnosis and frequent auditory hallucinations will be given Rivastigmine capsule versus placebo capsule.
Aim 1: Healthy Controls	Scopolamine	Healthy controls will be given scopolamine patches versus placebo patch.

Primary Outcome Measures

Name	Time	Method
Number of conditioned hallucinations exhibited during saline vs placebo administration	During fMRI scans / task completion which will take approximately 90 minutes	Participants will perform the Conditioned Hallucinations task while in the scanner; the authors hypothesize that number of conditioned hallucinations exhibited during the task will be higher under placebo than physostigmine, but only in those who have high prior weighting on baseline assessment.

Secondary Outcome Measures

Name	Time	Method
Prior-Weighting Parameter of the Hierarchical Gaussian Filter	During fMRI scans / task completion which will take approximately 90 minutes	Behavioral responses will be used to fit a parameter of the Hierarchical Gaussian Filter model corresponding to the ratio of precision of priors to precision of incoming sensory evidence.
Functional correlation with model belief trajectories	During fMRI scans / task completion which will take approximately 90 minutes	Behavioral responses will be used to fit belief trajectories across the course of the experiment, and whole-brain analyses will measure correlation of brain activity with these computed trajectories.

Trial Locations

Locations (1)

Connecticut Mental Health Center; 🇺🇸 New Haven, Connecticut, United States