Abstract

Two mechanisms defend against self-poisoning: taste neophobia and conditioned taste aversion (CTA). Taste neophobia limits the ingestion of an unknown, potentially poisonous food. If the new food proves harmless then neophobia habituates. However, if aversive postingestive consequences occur then a CTA develops and the food is avoided on later encounters. CTAs can be learned after only one taste-illness pairing, even when many hours separate the component events and even if the individual is unconscious after ingestion. Such properties ensure that we are protected from a wide range of naturally occurring poisons. However, in certain clinical populations (e.g., patients receiving chemotherapy or radiotherapy - which, unfortunately, also have extremely aversive gastrointestinal consequences) these same properties can, mistakenly, cause genuinely harmless foods to become disgusting and unpalatable. Work in our laboratory has helped establish that a brainstem nucleus, the medial parabrachial nucleus (mPBN), is the single most important nucleus for CTA acquisition; CTAs do not develop in rats with mPBN lesions. Furthermore, we have also discovered that forebrain structures (i.e., the basolateral [BLA] and medial [MeA] amygdala, gustatory insular cortex [GC] and gustatory thalamus [GT]) are essential for the normal occurrence of taste neophobia. Taste novelty regulates the rate of CTA acquisition: novel tastes readily acquire CTAs whereas familiar and safe tastes are CTA resistant. Our work suggests that the forebrain taste neophobia structures modulate the mPBN associative mechanism that governs CTA formation. A comprehensive understanding of CTA learning requires knowledge about this interaction, which represents our first short-term goal. This goal will be achieved by using a crossed- disconnection lesion strategy to determine the nature of the interaction between the four forebrain structures during taste neophobia (Aim 1) and which of these structures functionally interact with the PBN to modulate CTA acquisition (Aim 2). We recently discovered that intra-PBN infusions of anisomycin (a protein-synthesis inhibitor) induce a CTA to the preceding taste. Building on this finding, our second short-term goal seeks to understand how the PBN mediates CTA learning.
In Aim 3, we will determine the neurochemical mechanisms of illness-based CTA by antagonizing serotonergic and dopaminergic activity in the PBN.
Aim 4 will investigate whether the PBN is involved in CTAs induced by other forms of stimulation (including internal pain and a commonly abused opioid drug that is also used in the clinic to manage pain) to determine the boundary conditions of the PBN CTA mechanism. The results of the proposed studies will provide significant progress towards our long-term goal of understanding the neurochemistry and neurocircuitry of CTA learning, which will provide a foundation for the development of clinical interventions to mitigate the unwanted CTAs that develop consequent to essential medical therapies.

Public Health Relevance

Conditioned taste aversions (CTAs), which normally serve as a defense mechanism to protect us against the repeated ingestion of poisonous food, can threaten our health and well-being in certain clinical situations (e.g., chemotherapy or radiotherapy for cancer, or palliative medicine for chronic pain management) by causing genuinely harmless foods to taste disgusting and unpalatable. Understanding the neurochemistry and neurocircuitry of CTA not only promises new insights into the integration of taste and visceral functions but may also provide a foundation for the development of treatments and interventions to mitigate the unwanted and debilitating side effects of essential medical therapies.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Deafness and Other Communication Disorders (NIDCD)
Type
Research Project (R01)
Project #
5R01DC006456-12
Application #
9702780
Study Section
Neurobiology of Motivated Behavior Study Section (NMB)
Program Officer
Sullivan, Susan L
Project Start
2004-04-01
Project End
2021-05-31
Budget Start
2019-06-01
Budget End
2020-05-31
Support Year
12
Fiscal Year
2019
Total Cost
Indirect Cost

  Institution

Name
University of Illinois at Chicago
Department
Psychology
Type
Schools of Arts and Sciences
DUNS #
098987217
City
Chicago
State
IL
Country
United States
Zip Code
60612

  Publications

Arthurs, Joe; Lin, Jian-You; Reilly, Steve (2018) Inhibiting gustatory thalamus or medial amygdala has opposing effects on taste neophobia. Neurobiol Learn Mem 156:24-32
Arthurs, Joe; Lin, Jian-You; Ocampo, Roberto et al. (2017) Lactose malabsorption and taste aversion learning. Physiol Behav 180:39-44
Lin, Jian-You; Arthurs, Joe; Reilly, Steve (2017) Conditioned taste aversions: From poisons to pain to drugs of abuse. Psychon Bull Rev 24:335-351
Lin, Jian-You; Arthurs, Joe; Reilly, Steve (2017) Anesthesia-inducing drugs also induce conditioned taste aversions. Physiol Behav 177:247-251
Lin, Jian-You; Arthurs, Joe; Reilly, Steve (2015) Gustatory insular cortex, aversive taste memory and taste neophobia. Neurobiol Learn Mem 119:77-84
Lin, Jian-You; Arthurs, Joe; Reilly, Steve (2014) Conditioned taste aversion, drugs of abuse and palatability. Neurosci Biobehav Rev 45:28-45
Arthurs, Joe; Reilly, Steve (2013) Role of the gustatory thalamus in taste learning. Behav Brain Res 250:9-17
Lin, Jian-You; Arthurs, Joe; Reilly, Steve (2013) Reduced palatability in pain-induced conditioned taste aversions. Physiol Behav 119:79-85
Lin, Jian-You; Arthurs, Joe; Amodeo, Leslie Renee et al. (2012) Reduced palatability in drug-induced taste aversion: I. Variations in the initial value of the conditioned stimulus. Behav Neurosci 126:423-32
Lin, Jian-You; Amodeo, Leslie Renee; Arthurs, Joe et al. (2012) Anisomycin infusions in the parabrachial nucleus and taste neophobia. Neurobiol Learn Mem 98:348-53

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