Your search keyword '"Chambers R"' showing total 14 results

1. Nicotine effects in adolescence and adulthood on cognition and α4β2-nicotinic receptors in the neonatal ventral hippocampal lesion rat model of schizophrenia

Author

Berg, Sarah A., Sentir, Alena M., Bell, Richard L., Engleman, Eric A., and Chambers, R. Andrew

Published

2015

2. Natural reward-related learning in rats with neonatal ventral hippocampal lesions and prior cocaine exposure

Author

Andrew Chambers, R., Jones, Rachel M., Brown, Scott, and Taylor, Jane R.

Published

2005

3. More study needed for THC to be treatment option

Author

Chambers, R. Andrew

Subjects

Opioid abuse -- Prevention, Marijuana -- Laws, regulations and rules -- Usage -- Health aspects, Tetrahydrocannabinol -- Usage -- Health aspects, Addiction, Evidence (Law), Government regulation, Business, Business, regional

Abstract

The current biomedical evidence does not support the idea that legalizing marijuana is an answer to combating opioid misuse. Legalizing marijuana can be expected to produce a number of effects, [...]

Published

2019

4. On Mourning and Recovery: Integrating Stages of Grief and Change Toward a Neuroscience-Based Model of Attachment Adaptation in Addiction Treatment.

Author

Chambers, R. Andrew and Wallingford, Sue C.

Subjects

*PSYCHOLOGY of drug addiction, *ATTACHMENT behavior, *ATTACHMENT theory (Psychology), *INTERPERSONAL relations, *MENTAL illness

Abstract

Interpersonal attachment and drug addiction share many attributes across their behavioral and neurobiological domains. Understanding the overlapping brain circuitry of attachment formation and addiction illuminates a deeper understanding of the pathogenesis of trauma-related mental illnesses and comorbid substance use disorders, and the extent to which ending an addiction is complicated by being a sort of mourning process. Attention to the process of addiction recovery-as a form of grieving-in which Kubler-Ross's stages of grief and Prochaska's stages of change are ultimately describing complementary viewpoints on a general process of neural network and attachment remodeling, could lead to more effective and integrative psychotherapy and medication strategies. [ABSTRACT FROM AUTHOR]

Published

2017

5. Nicotine is more addictive, not more cognitively therapeutic in a neurodevelopmental model of schizophrenia produced by neonatal ventral hippocampal lesions.

Author

Berg, Sarah A., Sentir, Alena M., Cooley, Benjamin S., Engleman, Eric A., and Chambers, R. Andrew

Subjects

THERAPEUTIC use of nicotine, SCHIZOPHRENIA treatment, PEOPLE with schizophrenia, CAUSES of death, HIPPOCAMPUS (Brain), PHYSIOLOGICAL effects of tobacco, SELF medication

Abstract

Nicotine dependence is the leading cause of death in the United States. However, research on high rates of nicotine use in mental illness has primarily explained this co-morbidity as reflecting nicotine's therapeutic benefits, especially for cognitive symptoms, equating smoking with 'self-medication'. We used a leading neurodevelopmental model of mental illness in rats to prospectively test the alternative possibility that nicotine dependence pervades mental illness because nicotine is simply more addictive in mentally ill brains that involve developmental hippocampal dysfunction. Neonatal ventral hippocampal lesions ( NVHL) have previously been demonstrated to produce post-adolescent-onset, pharmacological, neurobiological and cognitive-deficit features of schizophrenia. Here, we show that NVHLs increase adult nicotine self-administration, potentiating acquisition-intake, total nicotine consumed and drug seeking. Behavioral sensitization to nicotine in adolescence prior to self-administration is not accentuated by NVHLs in contrast to increased nicotine self-administration and behavioral sensitization documented in adult NVHL rats, suggesting periadolescent neurodevelopmental onset of nicotine addiction vulnerability in the NVHL model. Delivering a nicotine regimen approximating the exposure used in the sensitization and self-administration experiments (i.e. as a treatment) to adult rats did not specifically reverse NVHL-induced cortical-hippocampal-dependent cognitive deficits and actually worsened cognitive efficiency after nicotine treatment stopped, generating deficits that resemble those due to NVHLs. These findings represent the first prospective evidence demonstrating a causal link between disease processes in schizophrenia and nicotine addiction. Developmental cortical-temporal limbic dysfunction in mental illness may thus amplify nicotine's reinforcing effects and addiction risk and severity, even while producing cognitive deficits that are not specifically or substantially reversible with nicotine. [ABSTRACT FROM AUTHOR]

Published

2014

6. Adult hippocampal neurogenesis in the pathogenesis of addiction and dual diagnosis disorders

Author

Chambers, R. Andrew

Subjects

*ADDICTIONS, *DEVELOPMENTAL neurobiology, *HIPPOCAMPUS (Brain), *DUAL diagnosis, *NEURAL physiology, *NEUROPLASTICITY, *PHARMACEUTICAL research, *PATHOLOGICAL physiology, *THERAPEUTICS

Abstract

Abstract: Background: As knowledge deepens about how new neurons are born, differentiate, and wire into the adult mammalian brain, growing evidence depicts hippocampal neurogenesis as a special form of neuroplasticity that may be impaired across psychiatric disorders. This review provides an integrated-evidence based framework describing a neurogenic basis for addictions and addiction vulnerability in mental illness. Methods: Basic studies conducted over the last decade examining the effects of addictive drugs on adult neurogenesis and the impact of neurogenic activity on addictive behavior were compiled and integrated with relevant neurocomputational and human studies. Results: While suppression of hippocampal neurogenic proliferation appears to be a universal property of addictive drugs, the pathophysiology of addictions involves neuroadaptative processes within frontal–cortical–striatal motivation circuits that the neurogenic hippocampus regulates via direct projections. States of suppressed neurogenic activity may simultaneously underlie psychiatric and cognitive symptoms, but also confer or signify hippocampal dysfunction that heightens addiction vulnerability in mental illness as a basis for dual diagnosis disorders. Conclusions: Research on pharmacological, behavioral and experiential strategies that enhance adaptive regulation of hippocampal neurogenesis holds potential in advancing preventative and integrative treatment strategies for addictions and dual diagnosis disorders. [Copyright &y& Elsevier]

Published

2013

7. Accentuated behavioral sensitization to nicotine in the neonatal ventral hippocampal lesion model of schizophrenia

Author

Berg, Sarah A. and Chambers, R. Andrew

Subjects

*NICOTINE, *SCHIZOPHRENIA, *HIPPOCAMPUS (Brain), *PRECANCEROUS conditions

Abstract

Abstract: The prevalence of smoking in schizophrenia patients far exceeds that in the general population. Increased vulnerability to nicotine and other drug addictions in schizophrenia may reflect the impact of developmental limbic abnormalities on cortical–striatal mediation of behavioral changes associated with drug use. Rats with neonatal ventral hippocampal lesions (NVHLs), a neurodevelopmental model of schizophrenia, have previously been shown to exhibit altered patterns of behavioral sensitization to both cocaine and ethanol. This study explored nicotine sensitization in NVHLs by testing locomotor activity of NVHL vs. SHAM-operated controls over 3 weeks in response to nicotine (0.5mg/kg) or saline injections (s.c.) followed by a nicotine challenge delivered to all rats 2 weeks later. At the beginning of the initial injection series, post-injection locomotor activation was indistinguishable among all treatment groups. However, nicotine but not saline injections produced a progressive sensitization effect that was greater in NVHLs compared to SHAMs. In the challenge session, rats with previous nicotine history showed enhanced locomotor activation to nicotine when compared to drug naïve rats, with NVHL-nicotine rats showing the greatest degree of activity overall. These results demonstrate that NVHLs exhibit altered short- and long-term sensitization profiles to nicotine, similar to altered long-term sensitization profiles produced by cocaine and ethanol. Collectively, these findings suggest the neurodevelopmental underpinnings of schizophrenia produce enhanced behavioral sensitization to addictive drugs as an involuntary and progressive neurobehavioral process, independent of the acute psychoactive properties uniquely attributed to nicotine, cocaine, or alcohol. [Copyright &y& Elsevier]

Published

2008

8. A scale-free systems theory of motivation and addiction

Author

Chambers, R. Andrew, Bickel, Warren K., and Potenza, Marc N.

Subjects

*NEUROTRANSMITTERS, *NEURAL transmission, *MOTIVATION (Psychology), *COGNITIVE dissonance

Abstract

Abstract: Scale-free organizations, characterized by uneven distributions of linkages between nodal elements, describe the structure and function of many life-based complex systems developing under evolutionary pressures. We explore motivated behavior as a scale-free map toward a comprehensive translational theory of addiction. Motivational and behavioral repertoires are reframed as link and nodal element sets, respectively, comprising a scale-free structure. These sets are generated by semi-independent information-processing streams within cortical–striatal circuits that cooperatively provide decision-making and sequential processing functions necessary for traversing maps of motivational links connecting behavioral nodes. Dopamine modulation of cortical–striatal plasticity serves a central-hierarchical mechanism for survival-adaptive sculpting and development of motivational–behavioral repertoires by guiding a scale-free design. Drug-induced dopamine activity promotes drug taking as a highly connected behavioral hub at the expense of natural-adaptive motivational links and behavioral nodes. Conceptualizing addiction as pathological alteration of scale-free motivational–behavioral repertoires unifies neurobiological, neurocomputational and behavioral research while addressing addiction vulnerability in adolescence and psychiatric illness. This model may inform integrative research in defining more effective prevention and treatment strategies for addiction. [Copyright &y& Elsevier]

Published

2007

9. Animal Modeling and Neurocircuitry of Dual Diagnosis.

Author

Chambers, R. Andrew

Subjects

*NEURAL circuitry, *DUAL diagnosis, *MENTAL illness, *SCHIZOPHRENIA, *ANIMAL models in research, *NUCLEUS accumbens

Abstract

Dual diagnosis is a problem of tremendous depth and scope, spanning many classes of mental disorders and addictive drugs. Animal models of psychiatric disorders studied in addiction paradigms suggest a unitary nature of mental illness and addiction vulnerability both on the neurocircuit and clinical-behavioral levels. These models provide platforms for exploring the interactive roles of biological, environmental and developmental factors on neurocircuits commonly involved in psychiatric and addiction diseases. While suggestive of the artifice of segregated research, training, and clinical cultures between psychiatric and addiction fields, this research may lead to more parsimonious, integrative and preventative treatments for dual diagnosis. [ABSTRACT FROM AUTHOR]

Published

2007

10. Natural reward-related learning in rats with neonatal ventral hippocampal lesions and prior cocaine exposure.

Author

Chambers, R. Andrew, Jones, Rachel M., Brown, Scott, and Taylor, Jane R.

Subjects

*COCAINE, *HIPPOCAMPUS (Brain), *LABORATORY rats, *SCHIZOPHRENIA, *DUAL diagnosis

Abstract

Discusses a research on natural reward-related learning in rats with neonatal ventral hippocampal lesions and prior cocaine exposure. Dissolution of concaine hydrochloride; Assessment of reward-conditioned learning; Information on lesion verification.

Published

2005

11. Polysubstance addiction vulnerability in mental illness: Concurrent alcohol and nicotine self-administration in the neurodevelopmental hippocampal lesion rat model of schizophrenia.

Author

Sentir, Alena M., Bell, Richard L., Engleman, Eric A., and Chambers, R. Andrew

Subjects

NICOTINE, MENTAL illness, PEOPLE with mental illness, ALCOHOL, ALCOHOL drinking, COMPLICATIONS of alcoholism, BIOLOGICAL models, ANIMAL behavior, HIPPOCAMPUS (Brain), SUBSTANCE abuse, ALCOHOLISM, SCHIZOPHRENIA, SELF medication, RATS, RESEARCH funding, ETHANOL, ANIMALS, DISEASE complications

Abstract

Multiple addictions frequently occur in patients with mental illness. However, basic research on the brain-based linkages between these comorbidities is extremely limited. Toward characterizing the first animal modeling of polysubstance use and addiction vulnerability in schizophrenia, adolescent rats with neonatal ventral hippocampal lesions (NVHLs) and controls had 19 weekdays of 1 hour/day free access to alcohol/sucrose solutions (fading from 10% sucrose to 10% alcohol/2% sucrose on day 10) during postnatal days (PD 35-60). Starting in adulthood (PD 63), rats acquired lever pressing for concurrent oral alcohol (10% with 2% sucrose) and iv nicotine (0.015 mg/kg/injection) across 15 sessions. Subsequently, 10 operant extinction sessions and 3 reinstatement sessions examined drug seeking upon withholding of nicotine, then both nicotine and alcohol, then reintroduction. Adolescent alcohol consumption did not differ between NVHLs and controls. However, in adulthood, NVHLs showed increased lever pressing at alcohol and nicotine levers that progressed more strongly at the nicotine lever, even as most pressing by both groups was at the alcohol lever. In extinction, both groups showed expected declines in effort as drugs were withheld, but NVHLs persisted with greater pressing at both alcohol and nicotine levers. In reinstatement, alcohol reaccess increased pressing, with NVHLs showing greater nicotine lever activity overall. Developmental temporal-limbic abnormalities that produce mental illness can thus generate adult polydrug addiction vulnerability as a mechanism independent from putative cross-sensitization effects between addictive drugs. Further preclinical modeling of third-order (and higher) addiction-mental illness comorbidities may advance our understanding and treatment of these complex, yet common brain illnesses. [ABSTRACT FROM AUTHOR]

Published

2020

12. Alcohol seeking and consumption in the NVHL neurodevelopmental rat model of schizophrenia

Author

Berg, S.A., Czachowski, C.L., and Chambers, R. Andrew

Subjects

*SCHIZOPHRENIA, *MENTAL illness, *SUBSTANCE abuse, *DUAL diagnosis, *ALCOHOLISM, *LABORATORY rats

Abstract

Abstract: Alcohol abuse in schizophrenia exceeds rates in the general population and worsens illness outcomes. Neonatal ventral hippocampal lesion (NVHL) rats model multiple schizophrenia dimensions including addiction vulnerability. This study compared NVHL vs. SHAM-controls in operant alcohol seeking and consumption. NVHLs enhanced consumption of combined ethanol/sucrose solution but neither ethanol or sucrose only solutions, consistent with increased vulnerability specific to carbohydrate-laden alcohol beverages typically consumed in early stages of human alcoholism. [Copyright &y& Elsevier]

Published

2011

13. Ethanol sensitization in a neurodevelopmental lesion model of Schizophrenia in rats

Author

Conroy, Susan K., Rodd, Zachary, and Chambers, R. Andrew

Subjects

*ALCOHOL, *NEURODEVELOPMENTAL treatment, *SCHIZOPHRENIA, *RATS

Abstract

Abstract: Substance use disorder comorbidity in schizophrenia may reflect dysfunctional cortical-striatal-limbic circuitry commonly involved in the addiction process and the pathogenesis of schizophrenia. Rats with neonatal ventral hippocampal lesions (NVHL) demonstrate post-adolescent onset of schizophrenia-like symptoms and increased addiction vulnerability in paradigms using cocaine in adulthood. Here, we investigated response profiles of young adult NVHL vs. SHAM rats to ethanol, an addictive drug with many psychopharmacological effects divergent from those of cocaine, in a locomotor sensitization paradigm. Over 15 days of daily injections of saline, low (0.15 g/kg) or high (1.0 g/kg) doses of ethanol, NVHL rats showed stimulatory effects at the low dose compared to saline and high-dose conditions, while SHAM rats showed expected patterns of dose-dependent suppression of locomotor activity. In a challenge session 2 weeks later in which a moderate dose (0.25 g/kg) of ethanol was given to all subjects, NVHL rats with history of prior ethanol exposure showed greater locomotor activity consistent with installment of alcohol-induced sensitization not present in SHAMs. These findings provide further evidence of enhanced short- and long-term responsivity to abused drugs in a neurodevelopmental model of schizophrenia, and may reflect potentiation of common mechanisms of addiction shared between pharmacologically diverse addictive drugs. [Copyright &y& Elsevier]

Published

2007

14. The adverse childhood experiences questionnaire: Two decades of research on childhood trauma as a primary cause of adult mental illness, addiction, and medical diseases.

Author

Zarse, Emily M., Neff, Mallory R., Yoder, Rachel, Hulvershorn, Leslie, Chambers, Joanna E., Chambers, R. Andrew, and Schumacher, Udo

Subjects

*ADVERSE childhood experiences, *ETIOLOGY of mental illnesses, *MENTAL health services, *PRENATAL drug exposure, *HEALTH care reform, *ADDICTIONS

Abstract

Objective. In 1998, Felitti and colleagues published the first study of the Adverse Childhood Experiences-Questionnaire (ACE-Q), a 10-item scale used to correlate childhood maltreatment and adverse rearing contexts with adult health outcomes. This paper qualitatively reviews nearly two decades of research utilizing the ACE-Q, highlighting its contribution to our understanding of the causal roots of common, interlinked comorbidities of the brain and body. Methods. An OVID/PubMed search was conducted for English language articles published before 2016, containing the phrase "Adverse Childhood Experiences" in which the ACE-Q was utilized. Source review included a manual search of bibliographies, resulting in 134 articles, including 44 based on the original ACE-Q study population. Results. ACE-Q research has demonstrated that exposures to adverse childhood experiences converge dose-dependently to potently increase the risk for a wide array of causally interlinked mental illnesses, addictions, and multi-organ medical diseases. The intergenerational transmission of this disease burden via disrupted parenting and insecure rearing contexts is apparent throughout this literature. However, the ACE-Q does not tease out genetic or fetal drug exposure components of this transmission. Conclusions. Adverse childhood experiences and rearing may generate a public health burden that could rival or exceed all other root causes. Translating this information to health-care reform will require strengthening brain-behavioral health as core public and preventative health-care missions. Greater integration of mental health and addiction services for parents should be accompanied by more research into brain mechanisms impacted by different forms and interactions between adverse childhood experiences. [ABSTRACT FROM AUTHOR]

Published

2019