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A causal study of bumetanide on a marker of excitatory-inhibitory balance in the human brain

Thomas L. Botch1, Alina Spiegel2, Catherine Ricciardi3, Caroline E. Robertson1
Dartmouth College1, Johns Hopkins University2, Massachusetts Institute of Technology3
23 Sep 2020-bioRxiv (Cold Spring Harbor Laboratory)-
TL;DR: It is shown that, contrary to expectation, acute administration of bumetanide does not alter binocular rivalry dynamics in neurotypical adult individuals, and this results raise important questions about the efficacy of acute bumeteanide administration for altering E/I balance in the human brain.
Abstract: Bumetanide has received much interest as a potential pharmacological modulator of the putative imbalance in excitatory/inhibitory (E/I) signaling that is thought to characterize autism spectrum conditions. Yet, currently, no studies of bumetanide efficacy have used an outcome measure that is modeled to depend on E/I balance in the brain. In this manuscript, we present the first causal study of the effect of bumetanide on an objective marker of E/I balance in the brain, binocular rivalry, which we have previously shown to be sensitive to pharmacological manipulation of GABA. Using a within-subjects placebo-control crossover design study, we show that, contrary to expectation, acute administration of bumetanide does not alter binocular rivalry dynamics in neurotypical adult individuals. Neither changes in response times nor response criteria can account for these results. These results raise important questions about the efficacy of acute bumetanide administration for altering E/I balance in the human brain, and highlight the importance of studies using objective markers of the underlying neural processes that drugs hope to target.

Summary (2 min read)

Jump to: [Introduction][Materials and Methods][Results][Test-retest reliability] and [Discussion]

Introduction

  • Excitatory and inhibitory (E/I) activity is balanced in neural systems at multiple spatial scales [1, 2], and this balance is thought to be critical for typical neural function [3–5].
  • In particular, studies in both humans and in animal models suggest that altered inhibitory signaling, mediated by the neurotransmitter GABA, may characterize the condition [10, 11].
  • During development, the polarity of GABAergic action transitions from excitatory to inhibitory due to a progressive reduction in intracellular chloride (Cl-) concentration in principal neurons [14, 15] -- a developmental sequence that may be disrupted in animal models of autism [16, 17].
  • Importantly, to date, direct evidence that bumetanide increases inhibition in the human brain is lacking, which complicates linking the reported symptomatic benefits to the drug’s predicted physiological effects.
  • The authors tested this hypothesis in a within-subjects drug-placebo, crossover design pharmacological study of rivalry dynamics in neurotypical adults.

Materials and Methods

  • Written consent was obtained from all participants, and all studies were approved by the Massachusetts Institute of Technology Institutional Review Board.
  • Bumetanide is an FDAapproved loop-diuretic known to antagonize sodium-potassium-chloride cotransporters, NKCC1 and NKCC2, which modulate intracellular chloride concentration.
  • For each participant and trial, the frequency of perceptual transitions as well as the duration of any perceptual event (red, green, or mixed) were calculated.
  • Binocular rivalry replay trial stimuli were identical to those used in the main rivalry experiment, and the paradigm was identical to their previously published studies [31, 33].

Results

  • The authors predicted that bumetanide, a drug known to alter intracellular Cl- concentration and, by proxy, posited to increase GABAergic inhibition, would increase perceptual suppression during rivalry.
  • The authors also assessed performance on rivalry replay control trials to establish whether any observed changes were due to non-perceptual effects on response latencies or response criteria [39, 40].
  • To test whether bumetanide affects the depth of perceptual suppression during rivalry, the authors calculated the drug effect on the proportion of suppression for each individual (Proportion of Suppression on Drug - Placebo days) using a Wilcoxon signed-rank test.
  • Drug effects are not confounded by shifts in response latency or response criteria.

Test-retest reliability

  • To examine the stability of their primary measure, perceptual suppression, the authors calculated test-retest reliability by correlating performance on drug versus placebo days across individuals in each study.
  • Bumetanide does not affect self-reported drowsiness Participants did not report significant differences in drowsiness between placebo and drug days (mean: 0.35 questionnaire points +/- 1.69 points, p = 0.367).

Discussion

  • The authors have shown that acute administration of bumetanide does not alter binocular rivalry dynamics in neurotypical adult individuals.
  • Indeed, the effects the authors observed (lower perceptual suppression) here trended in the opposite direction as predicted from previous studies of the impact of GABA modulators on rivalry dynamics [31, 32].
  • Previous studies examining the longitudinal effects of bumetanide in individuals with autism have often demonstrated success in modulating social processing.
  • It is thought that bumetanide may affect neural processing by modulating E/I balance in the brain.
  • By this measure (and excluding self-citations to the and last authors of their current paper), their references contained 3.8% woman/ woman(last), 3.8% man/woman, 22.6% woman/man, 69.8% man/man, and 0% unknow n categorization.

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RUNNING HEAD: BUMETANIDE EFFECTS ON BINOCULAR RIVALRY
1
A causal study of bumetanide on a marker of excitatory-inhibitory balance in the
human brain
Thomas L. Botch
1
, Alina Spiegel
2
, Catherine Ricciardi
3
, Caroline E. Robertson
1+
1
Department of Psychological and Brain Sciences, Dartmouth College, Hanover, NH
03755, USA
2
School of Medicine, Johns Hopkins University, Baltimore, MD, 21205
3
Clinical Research Center, Massachusetts Institute of Technology, Cambridge, MA
02139, USA
+
Corresponding author: Dr. Caroline Robertson, caroline.e.robertson@dartmouth.edu
(which was not certified by peer review) is the author/funder. All rights reserved. No reuse allowed without permission.
The copyright holder for this preprintthis version posted September 23, 2020. ; https://doi.org/10.1101/2020.09.22.304279doi: bioRxiv preprint
BUMETANIDE EFFECTS ON BINOCULAR RIVALRY
2
Abstract
Bumetanide has received much interest as a potential pharmacological modulator of the
putative imbalance in excitatory/inhibitory (E/I) signaling that is thought to characterize
autism spectrum conditions. Yet, currently, no studies of bumetanide efficacy have used
an outcome measure that is modeled to depend on E/I balance in the brain. In this
manuscript, we present the first causal study of the effect of bumetanide on an objective
marker of E/I balance in the brain, binocular rivalry, which we have previously shown to
be sensitive to pharmacological manipulation of GABA. Using a within-subjects placebo-
control crossover design study, we show that, contrary to expectation, acute
administration of bumetanide does not alter binocular rivalry dynamics in neurotypical
adult individuals. Neither changes in response times nor response criteria can account
for these results. These results raise important questions about the efficacy of acute
bumetanide administration for altering E/I balance in the human brain, and highlight the
importance of studies using objective markers of the underlying neural processes that
drugs hope to target.
(which was not certified by peer review) is the author/funder. All rights reserved. No reuse allowed without permission.
The copyright holder for this preprintthis version posted September 23, 2020. ; https://doi.org/10.1101/2020.09.22.304279doi: bioRxiv preprint
BUMETANIDE EFFECTS ON BINOCULAR RIVALRY
3
Introduction
Excitatory and inhibitory (E/I) activity is balanced in neural systems at multiple spatial
scales [1, 2], and this balance is thought to be critical for typical neural function [35].
Multiple lines of evidence implicate disrupted E/I balance in the neurobiology of Autism
Spectrum Conditions (ASC; autism henceforth) [612]. In particular, studies in both
humans and in animal models suggest that altered inhibitory signaling, mediated by the
neurotransmitter GABA, may characterize the condition [10, 11]. Despite the
accumulating evidence, the intricacies of autism neurobiology are poorly understood,
hindering efforts to develop treatment strategies for the condition.
One prominent developmental account of autism proposes a disruption of an important
neurobiological milestone, known as the GABA-switch, as a potential explanation for
disturbed inhibitory action in the autistic brain [13]. During development, the polarity of
GABAergic action transitions from excitatory (depolarizing) to inhibitory (hyperpolarizing)
due to a progressive reduction in intracellular chloride (Cl-) concentration in principal
neurons [14, 15] -- a developmental sequence that may be disrupted in animal models of
autism [16, 17]. In light of these accounts, it has been posited that augmenting GABAergic
action might provide a promising therapeutic for some symptoms associated with autism
[13, 18].
Bumetanide, a loop diuretic, has proven hopeful in rectifying GABA polarity in valproic
acid and Fragile X animal models of autism [16, 19]. Bumetanide is thought to increase
the hyperpolarizing potential of GABA by blocking NKCC1 receptors, which are
(which was not certified by peer review) is the author/funder. All rights reserved. No reuse allowed without permission.
The copyright holder for this preprintthis version posted September 23, 2020. ; https://doi.org/10.1101/2020.09.22.304279doi: bioRxiv preprint
BUMETANIDE EFFECTS ON BINOCULAR RIVALRY
4
responsible for Cl- entrance into the cell [20]. Further, some studies of bumetanide in
humans, specifically children with autism, have shown evidence for attenuation of social
symptom severity and improvement of emotion recognition [2123], although, notably,
these benefits are not universally observed [24]. Importantly, to date, direct evidence that
bumetanide increases inhibition in the human brain is lacking, which complicates linking
the reported symptomatic benefits to the drug’s predicted physiological effects.
Therefore, we sought to test the effects of bumetanide on a robust behavioral index of E/I
balance, binocular rivalry. Rivalry is a simple visual phenomenon that is modeled to rely
on the on the balance of inhibition and excitation in visual cortex [2530]. Prior
pharmacological studies in humans reveal a causal link between rivalry dynamics and
GABAergic inhibition using both GABA
A
and GABA
B
modulators [31, 32], as well as a
dependence of rivalry dynamics on tonic levels of GABA in visual cortex [11, 32]. Given
these links between rivalry dynamics and E/I balance in visual cortex, as well as recent
evidence showing altered rivalry dynamics in adult individuals with autism [11, 3335],
rivalry has been suggested as a noninvasive perceptual marker of E/I signaling in visual
cortex, and its putative disturbance in psychiatric conditions, including autism.
Here, we asked whether acute bumetanide administration would alter rivalry dynamics.
We hypothesized that bumetanide would increase the degree to which individuals
predominantly perceive one image fully suppressed from awareness (“perceptual
suppression”), which computational and empirical data suggest is gated by GABAergic
(which was not certified by peer review) is the author/funder. All rights reserved. No reuse allowed without permission.
The copyright holder for this preprintthis version posted September 23, 2020. ; https://doi.org/10.1101/2020.09.22.304279doi: bioRxiv preprint
BUMETANIDE EFFECTS ON BINOCULAR RIVALRY
5
inhibition [31, 36, 37]. We tested this hypothesis in a within-subjects drug-placebo, cross-
over design pharmacological study of rivalry dynamics in neurotypical adults.
Materials and Methods
Participants. 21 healthy adults (N = 15 female; mean age 22.5 +/- 3.68 SD years)
participated in the study. Written consent was obtained from all participants, and all
studies were approved by the Massachusetts Institute of Technology Institutional Review
Board. All participants had normal or corrected-to-normal vision, were neither pregnant
nor nursing, and were free from: (1) any known history of psychiatric or neurological
conditions; (2) any other diagnosed medical conditions, including a history of heart failure;
(3) any psychiatric medications; and (4) any known drug allergies (including bumetanide).
All studies took place at the MIT Clinical Research Center, under the constant observation
of a research nurse/nurse practitioner (C.R.) and nursing team.
Study drugs: bumetanide (loop-diuretic). Participants participated in a study investigating
the effects of bumetanide (1 mg) on binocular rivalry dynamics. Bumetanide is an FDA-
approved loop-diuretic known to antagonize sodium-potassium-chloride cotransporters,
NKCC1 and NKCC2, which modulate intracellular chloride concentration. At low
concentrations, bumetanide has a high affinity to block NKCC1, thereby reducing
intracellular chloride concentration and, by proxy, altering GABAergic action potentials
[14, 20]. Bumetanide dosage was chosen to fall within the standard prescribed range.
Experimental design: placebo-controlled crossover design. Each participant took part in
a 3-day study, comprised of: a health assessment/practice session (Day 1) and 2
(which was not certified by peer review) is the author/funder. All rights reserved. No reuse allowed without permission.
The copyright holder for this preprintthis version posted September 23, 2020. ; https://doi.org/10.1101/2020.09.22.304279doi: bioRxiv preprint
Citations
More filters
Journal Article
Reduced perceptual exclusivity during object and grating rivalry in autism.

[...]

Jan Freyberg1, Caroline E. Robertson2, Simon Baron-Cohen1
University of Cambridge1, Harvard University2
01 Jan 2015-Journal of Visualization
TL;DR: The authors found that participants with ASC experienced a slower rate of binocular rivalry, driven by longer transitional states between dominant percepts, and these exaggerated transitional states were present at both low and high levels of stimulus complexity (gratings and objects).
Abstract: The dynamics of binocular rivalry may be a behavioral footprint of excitatory and inhibitory neural transmission in visual cortex. Given the presence of atypical visual features in Autism Spectrum Conditions (ASC), and the growing evidence in support of the idea of an imbalance in excitatory/inhibitory neural transmission in animal and genetic models of ASC, we hypothesized that binocular rivalry might prove a simple behavioral marker of such a transmission imbalance in the autistic brain. In support of this hypothesis, we previously reported a slower rate of rivalry in ASC, driven by longer transitional states between dominant percepts. We tested whether atypical dynamics of binocular rivalry in ASC are specific to certain stimulus features. 53 participants (26 with ASC, matched for age, sex, and IQ) participated in a binocular rivalry experiment in which the dynamics of rivalry were measured at two levels of stimulus complexity, low (grayscale gratings) and high (colored objects). Individuals with ASC experienced a slower rate of binocular rivalry, driven by longer transitional states between dominant percepts. These exaggerated transitional states were present at both low and high levels of stimulus complexity (gratings and objects), suggesting that atypical binocular dynamics in autism are robust with respect to stimulus choice. Interactions between stimulus properties and rivalry dynamics in autism indicate that achromatic grating stimuli produce stronger group differences. These results confirm the finding of atypical dynamics of binocular rivalry in ASC. These dynamics were present for stimuli of both low and high levels of visual complexity, suggesting a pervasive imbalance in competitive interactions throughout the visual system of individuals with ASC.

5 citations

References
More filters
Journal ArticleDOI
Role of mutual inhibition in binocular rivalry

[...]

Jeffrey Scott Seely1, Carson C. Chow1
National Institutes of Health1
20 Jul 2011-Journal of Neurophysiology
TL;DR: Here, it is shown how various biophysically plausible modifications to mutual inhibition models can resolve the problem of not complying with Levelt's fourth proposition, which states that percepts alternate faster as the stimulus contrasts to both eyes are increased simultaneously.
Abstract: Binocular rivalry is a phenomenon that occurs when a different image is presented to each eye. The observer generally perceives just one image at a time, with perceptual switches occurring every few seconds. A natural assumption is that this perceptual mutual exclusivity is achieved via mutual inhibition between populations of neurons that encode for either percept. Theoretical models that incorporate mutual inhibition have been largely successful at capturing experimental features of rivalry, including Levelt's propositions, which characterize perceptual dominance durations as a function of image contrasts. However, basic mutual inhibition models do not fully comply with Levelt's fourth proposition, which states that percepts alternate faster as the stimulus contrasts to both eyes are increased simultaneously. This theory-experiment discrepancy has been taken as evidence against the role of mutual inhibition for binocular rivalry. Here, we show how various biophysically plausible modifications to mutual inhibition models can resolve this problem.

108 citations

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Global motion perception deficits in autism are reflected as early as primary visual cortex

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Caroline E. Robertson1, Caroline E. Robertson2, Cibu Thomas2, Dwight J. Kravitz2, Gregory L. Wallace2, Simon Baron-Cohen1, Alex Martin2, Chris I. Baker2 
University of Cambridge1, National Institutes of Health2
01 Sep 2014-Brain
TL;DR: The findings suggest that reduced global motion perception in autism is driven by an atypical response early in visual processing and may reflect a fundamental perturbation in neural circuitry.
Abstract: Individuals with autism are often characterized as 'seeing the trees, but not the forest'-attuned to individual details in the visual world at the expense of the global percept they compose. Here, we tested the extent to which global processing deficits in autism reflect impairments in (i) primary visual processing; or (ii) decision-formation, using an archetypal example of global perception, coherent motion perception. In an event-related functional MRI experiment, 43 intelligence quotient and age-matched male participants (21 with autism, age range 15-27 years) performed a series of coherent motion perception judgements in which the amount of local motion signals available to be integrated into a global percept was varied by controlling stimulus viewing duration (0.2 or 0.6 s) and the proportion of dots moving in the correct direction (coherence: 4%, 15%, 30%, 50%, or 75%). Both typical participants and those with autism evidenced the same basic pattern of accuracy in judging the direction of motion, with performance decreasing with reduced coherence and shorter viewing durations. Critically, these effects were exaggerated in autism: despite equal performance at the long duration, performance was more strongly reduced by shortening viewing duration in autism (P 0.574). These findings suggest that reduced global motion perception in autism is driven by an atypical response early in visual processing and may reflect a fundamental perturbation in neural circuitry.

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Improving emotional face perception in autism with diuretic bumetanide: A proof-of-concept behavioral and functional brain imaging pilot study:

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Nouchine Hadjikhani1, Nicole R. Zürcher1, Ophélie Rogier1, Torsten Ruest1, Loyse Hippolyte1, Yehezkel Ben-Ari2, Eric Lemonnier 
École Polytechnique Fédérale de Lausanne1, INMED2
01 Feb 2015-Autism
TL;DR: Results from an open-label trial pilot study in which bumetanide treatment improves emotion recognition and enhances the activation of brain regions involved in social and emotional perception during the perception of emotional faces show the usefulness of bumetAnide as a promising treatment to improve social interactions in autism.
Abstract: Clinical observations have shown that GABA-acting benzodiazepines exert paradoxical excitatory effects in autism, suggesting elevated intracellular chloride (Cl-)i and excitatory action of GABA. In a previous double-blind randomized study, we have shown that the diuretic NKCC1 chloride importer antagonist bumetanide, that decreases (Cl-)i and reinforces GABAergic inhibition, reduces the severity of autism symptoms. Here, we report results from an open-label trial pilot study in which we used functional magnetic resonance imaging and neuropsychological testing to determine the effects of 10 months bumetanide treatment in adolescents and young adults with autism. We show that bumetanide treatment improves emotion recognition and enhances the activation of brain regions involved in social and emotional perception during the perception of emotional faces. The improvement of emotion processing by bumetanide reinforces the usefulness of bumetanide as a promising treatment to improve social interactions in autism.

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Extracellular proteolysis in structural and functional plasticity of mossy fiber synapses in hippocampus.

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Grzegorz Wiera1, Jerzy W. Mozrzymas1
Wrocław Medical University1
04 Nov 2015-Frontiers in Cellular Neuroscience
TL;DR: The role of extracellular proteolysis in various aspects of synaptic plasticity in hippocampal mossy fiber synapses is reviewed, and a growing body of evidence demonstrates that among perisynaptic proteases, tissue plasminogen activator (tPA)/plasmin system, β-site amyloid precursor protein-cleaving enzyme 1 (BACE1) and metalloproteinases play a crucial role in shaping plastic changes in this projection.
Abstract: Brain is continuously altered in response to experience and environmental changes. One of the underlying mechanisms is synaptic plasticity, which is manifested by modification of synapse structure and function. It is becoming clear that regulated extracellular proteolysis plays a pivotal role in the structural and functional remodeling of synapses during brain development, learning and memory formation. Clearly, plasticity mechanisms may substantially differ between projections. Mossy fiber synapses onto CA3 pyramidal cells display several unique functional features, including pronounced short-term facilitation, a presynaptically expressed long-term potentiation (LTP) that is independent of NMDAR activation, and NMDA-dependent metaplasticity. Moreover, structural plasticity at mossy fiber synapses ranges from the reorganization of projection topology after hippocampus-dependent learning, through intrinsically different dynamic properties of synaptic boutons to pre- and postsynaptic structural changes accompanying LTP induction. Although concomitant functional and structural plasticity in this pathway strongly suggests a role of extracellular proteolysis, its impact only starts to be investigated in this projection. In the present report, we review the role of extracellular proteolysis in various aspects of synaptic plasticity in hippocampal mossy fiber synapses. A growing body of evidence demonstrates that among perisynaptic proteases, tissue plasminogen activator (tPA)/plasmin system, β-site amyloid precursor protein-cleaving enzyme 1 (BACE1) and metalloproteinases play a crucial role in shaping plastic changes in this projection. We discuss recent advances and emerging hypotheses on the roles of proteases in mechanisms underlying mossy fiber target specific synaptic plasticity and memory formation.

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