Maternal Separation in the Rat : The Short- and Long-term effects of Early-life Experience on Neuropeptides, Monoamines and Voluntary Ethanol Consumption

Oreland, Sadia

January 2009

Early-life experience has profound effects on the individual’s neurobiology and behaviour later in life. The rodent animal experimental model maternal separation (MS) was used to study this more in detail. The MS model involves short and prolonged postnatal separations simulating an emotionally safe and stressful environment, respectively. The aims of the thesis were to examine the impact of individual MS on ethanol consumption and on brain dopamine and serotonin systems in adult male rats. Furthermore, the influence of separation conditions on the short- and long-term consequences of MS on several neurotransmitter systems was examined. Rat pups were assigned to either litter-wise MS for 15 or 360 minutes (MS15l or MS360l) or individual MS for 15 or 360 minutes (MS15i or MS360i). Control rats were subjected to conventional animal facility rearing (AFR). Ethanol intake was assessed in a two-bottle free-choice paradigm. Neuropeptides were analyzed with radioimmunoassay, monoamines and metabolites with electrochemical detection and gene expression with qPCR. Using the MSi paradigm, minor effects on voluntary ethanol consumption were observed. However, the monoaminergic responses elicited by ethanol were dependent on the early-life environment. Furthermore, short- and long-term consequences of MS on serotonin, opioid, oxytocin and vasopressin systems were studied. Multiple neurobiological measurements in one and the same rat offered a unique possibility to examine the effects of duration (MS15 versus MS360) and condition (l versus i) of MS. Time-, region-, sex- and transmitter-specific effects were observed. More pronounced differences were seen in serotonin measures and oxytocin in young rats. In adults these differences in basal levels were normalized. Opioid peptides differed in stress-related brain areas in young rats and in limbic areas in adults. Rats subjected to the MS15l environment that relates to natural conditions generally exhibited a different neurobiological profile than other groups. AFR rats, i.e. conventional control rats, were more similar to the putative most stressful condition MS360. Taken together, the networks examined in the present thesis are important for the establishment of normal social behaviour and derangements in these systems may result in neurobiological changes leading to the susceptibility for psychopathological conditions later in life.

Early-life stress

Handling

Serotonin

Dopamine

Oxytocin

Vasopressin

Enkephalin

Dynorphin

Two-bottle free choice

Maternal deprivation

Pharmaceutical pharmacology

Farmaceutisk farmakologi

Endogenous opioids and voluntary ethanol drinking : consequences of postnatal environmental influences in rats /

Gustafsson, Lisa,

January 2007

Diss. (sammanfattning) Uppsala : Uppsala universitet, 2007. / Härtill 5 uppsatser.

Childhood loss and indicators of adult mental health report submitted in partial fulfillment ... for the degree of Master of Science, Psychiatric/Mental Health Nursing ... /

Eggleston, Katherine Jane.

January 1999

Thesis (M.S.)--University of Michigan, 1999. / eContent provider-neutral record in process. Description based on print version record. Includes bibliographical references.

The social network and its importance for the mental health of children in single-parent families a comparison between a clinical group and a control group.

Samuelsson, Margareta.

January 1995

Thesis (Ph. D.)--Lund University, 1995. / Summary in Swedish. Errata sheet inserted. Includes bibliographical references.

Childhood loss and indicators of adult mental health report submitted in partial fulfillment ... for the degree of Master of Science, Psychiatric/Mental Health Nursing ... /

Eggleston, Katherine Jane.

January 1999

Thesis (M.S.)--University of Michigan, 1999. / eContent provider-neutral record in process. Description based on print version record. Includes bibliographical references.

The social network and its importance for the mental health of children in single-parent families a comparison between a clinical group and a control group.

Samuelsson, Margareta.

January 1995

Thesis (Ph. D.)--Lund University, 1995. / Summary in Swedish. Errata sheet inserted. Includes bibliographical references.

Consequências da privação materna para o comportamento tipo-ansioso: participação do eixo hipotálamo-pituitária-adrenal e do sistema de neurotransmissão GABAaérgico / Effects of maternal deprivation for the anxious-like behavior: involvement of the hypothalamic-pituitary-adrenal system and neurotransmission GABAaérgico

Faturi, Claudia de Brito [UNIFESP]

29 July 2009

Made available in DSpace on 2015-07-22T20:49:47Z (GMT). No. of bitstreams: 0 Previous issue date: 2009-07-29. Added 1 bitstream(s) on 2015-08-11T03:26:28Z : No. of bitstreams: 1 Publico-345.pdf: 1277830 bytes, checksum: 6d2949e2d33e045cfec88a295d473e41 (MD5) / Associação Fundo de Incentivo à Psicofarmacologia (AFIP) / Coordenação de Aperfeiçoamento de Pessoal de Nível Superior (CAPES) / Fundação de Amparo à Pesquisa do Estado de São Paulo (FAPESP) / Alguns estudos pré-clínicos têm demostrado que eventos adversos na infância e adolescência representam um fator de vulnerabilidade para o surgimento de transtornos psiquiátricos na idade adulta, e que a redução da resiliência à eventos estressantes deve desempenhar um papel importante neste fenômeno. As manipulações em animais de laboratório, como a privação materna (PM) por 24 h durante o período de hiporresposividade ao estresse (PHRE), podem ser um instrumento útil para a compreensão de como os eventos no período precoce do desenvolvimento resultam em alterações comportamentais e da atividade do eixo Hipotálamo-Pituitária-Adrenal (HPA) na idade adulta. Alguns autores têm observado que a PM, quando imposta no 3° dia de vida (antes do início) ou no 11° dia (no vale) do PHRE, resulta em padrões de atividade do eixo HPA distintos. A PM no 3° dia induz à hiperatividade do eixo, enquanto que no 11° dia, resulta na hipoatividade, alterações estas observadas em animais jovens. Assim, os principais objetivos do presente trabalho foram os de estudar como a PM afetaria a atividade do eixo HPA durante o PHRE, e verificar se essas alterações teriam conseqüências duradouras. Os resultados mostraram que os efeitos da PM na liberação de ACTH mantiveram o mesmo padrão de atividade relatado na adolescência, ou seja, hiperresponsividade no grupo submetido à PM no 3o dia de vida e hiporresponsividade no grupo submetido à mesma manipulação no 11o dia de vida. No entanto, essa alteração não se refletiu na liberação da corticosterona (CORT), pois não se observou diferença na secreção deste hormônio entre os grupos. Além disso, a PM não alterou a liberação de CORT em resposta ao Teste de supressão à Dexametasona, indicando que não houve alterações no sistema de retroalimentação negativa no nível hipofisário do eixo HPA. A PM afetou o comportamento do tipo ansioso nos animais de ambos os grupos PM, sendo que tal alteração parece não ter sido mediada por mudanças na densidade do sítio benzodiazepínico do receptor GABAA. Os resultados indicaram que, embora a PM não leve a alterações permanentes na secreção da corticosterona, este pode ser um modelo animal interessante para se estudar o substrato neurobiológico que faz com que um evento adverso durante o desenvolvimento aumente a vulnerabilidade aos transtornos relacionados à ansiedade. / Adverse events in childhood have been associated to the development of psychopathologies, such as depression and anxiety disorders. In rats, stressful events during neonatal period, like 24h Maternal Deprivation (MD), may be an interesting tool to understand how stress during early life leads to changes in behavior and stress response in adulthood. According to some studies, MD on the 3rd day (MD 3-4) or 11th day (MD 11- 12) of life results in opposite changes in the activity of the Hypothalamus-Pituitary- Adrenal (HPA) axis, i.e., hyper and hyporresponsiveness, respectively. Since in human beings psychopathologies has been related to impairment in resilience to stress the aim of this work was to investigate whether MD leads to long lasting changes in HPA axis functioning and differential behavioral features in animal models of anxiety. The results obtained indicate that only the ACTH release presented the pattern we hypothesized. Conversely the corticosterone (CORT) plasmatic levels do not reflect this pattern. Moreover, MD did not affect the CORT release in response to the Dexamethasone Suppression Test, indicating that there are MD did not alter the negative feedback system. Although MD did not lead to convincing alteration to CORT levels it did change anxiety-like behavior in the group MD 11-12. However this behavioral change did not seem to be mediated by expression of benzodiazepine site in GABAA receptors. The results indicate that even though the MD procedure does not lead to consistent changes in the peripheral component of the HPA axis it could still be an interesting animal model to study the neurobiological underpinnings of how adverse events in early life increase the vulnerability to psychopathologies. / FAPESP: 2006/06415-4 / TEDE / BV UNIFESP: Teses e dissertações

Transtornos de ansiedade

Privação materna

Estresse

HPA axis e receptores GABAA

Maternal deprivation

Stress

Anxiety

HPA axis and GABAA receptors

Maternal Separation in Rats : An Experimental Model for Long-Term Effects of Early Life Experiences on Neurochemistry, Voluntary Ethanol Intake and Exploration and Risk Assessment Behavior

Roman, Erika

January 2004

The period of early life is important for the development of individual brain function and behavior. Human studies have shown altered vulnerability to develop psychopathology and/or excessive drug intake, possibly leading to dependence, as a consequence of early life experiences. In the present thesis, maternal separation (MS), an experimental model for studies of early environmental influences, was used to investigate long-term effects on neurochemistry, voluntary ethanol intake and exploration and risk assessment behavior in rats. Rat pups were assigned to one of three different rearing conditions: daily 15 min (MS15) or 360 min (MS360) of MS and normal animal facility rearing (AFR) during the first three weeks of life. Measurements of adult endogenous opioid peptide levels, opioid- and dopamine receptor density revealed minor MS-induced effects on the opioid system whereas interesting alterations were found in dopamine receptor density. Long-term effects on voluntary ethanol intake showed distinct MS-induced alterations in male Wistar and ethanol-preferring AA (Alko, Alcohol) rats. Female Wistar rats were unaffected, indicating sex differences in the effects of MS on ethanol intake. Male MS15 rats generally had a slower acquisition phase and a low subsequent ethanol intake whereas male MS360 rats had a high ethanol intake. MS15 is therefore suggested to protect against a high voluntary ethanol intake in male rats whereas MS360 may serve as a risk factor. The recently established concentric square field test indicated alterations in risk assessment as well as an increased exploratory drive and somewhat higher risk-taking behavior in adult MS360 rats, while minor effects were seen in MS15 rats. Altogether, these results demonstrate that environmental influences during the period of early life can have long-term effects on neurochemistry and behavior. Of special interest is the finding that MS altered the inherited high ethanol intake in adult ethanol-preferring AA rats.

Pharmaceutical pharmacology

Handling

Maternal Deprivation

Environment

Opioids

Dopamine

Alcohol

Stress

Concentric Square Field

Open Field

Elevated Plus-maze

Farmaceutisk farmakologi

Pharmaceutical pharmacology

Farmaceutisk farmakologi

Endogenous Opioids and Voluntary Ethanol Drinking : Consequences of Postnatal Environmental Influences in Rats

Gustafsson, Lisa

January 2007

Genetic and environmental factors interact to determine the individual vulnerability to develop ethanol dependence. The neurobiological mechanisms underlying these processes are not fully understood. Endogenous opioid peptides have been suggested to contribute. Brain opioids mediate ethanol reward and reinforcement via actions on the mesocorticolimbic dopamine system. This thesis focuses on environmental factors and investigates the impact of the early-life environment on adult voluntary ethanol consumption. The possible involvement of opioid peptides in environmental influences on adult ethanol consumption was examined using an experimental animal model. Maternal separation with short 15 min separations (MS15) was used to simulate a safe environment whereas prolonged 360 min separations (MS360) simulated an unsafe environment. Control rats were subjected to normal animal facility rearing (AFR). The separations were performed daily from postnatal day 1 to 21. Long-term ethanol consumption was registered using a two-bottle or a four-bottle free-choice paradigm in adult male and female ethanol-preferring AA (Alko, Alcohol), ethanol-avoiding ANA (Alko, Non-Alcohol) and non-preferring Wistar rats. In addition, analyses of immunoreactive Met-enkephalin-Arg6Phe7 (MEAP), dynorphin B (DYNB) and nociceptin/orphanin FQ (N/OFQ) peptide levels were performed after maternal separation as well as after voluntary ethanol drinking. In male rats, MS15 was related to lower ethanol consumption and these rats preferred lower concentrations, whereas MS360 was associated with an increased risk for higher consumption and/or preference for higher ethanol concentrations. Differences in basal opioid levels were observed in MS15 and MS360 rats. Furthermore, the ethanol-induced effects on opioid peptides in adults were dependent on the early environment. Female rats, on the other hand, were less affected or unaffected by maternal separation both in terms of ethanol consumption and neurobiological effects. Taken together, voluntary ethanol drinking, preference for low or high ethanol concentrations and opioid peptides in brain areas related to reward and reinforcement, motivation and stress were influenced by postnatal maternal separation in a sex dependent manner. The early environment thus had profound impact on the adult brain and the individual propensity for high ethanol drinking. A deranged endogenous opioid system contributed to these effects and may act as a mediator for long-term environmental influence on voluntary ethanol consumption.

Pharmaceutical pharmacology

Maternal separation

Maternal deprivation

Handling

Isolation

Alcohol

Two-bottle model

Four-bottle model

MEAP

Dynorphin B

Nociceptin/orphanin FQ

Radioimmunoassay

Farmaceutisk farmakologi

Avaliação do efeito em longo prazo do estresse neonatal causado pela separação ou privação materna em ratos sobre a expressão de comportamentos defensivos associados ao pânico / Evaluation of the long-term effect of neonatal stress caused by maternal separation or deprivation in rats on the expression of defensive behaviors associated with panic

Rosa, Daiane Santos

30 June 2017

Diversos estudos demonstram que o estresse infantil, incluindo situações de perda dos pais, negligência e abusos, representa um forte fator de risco para o desenvolvimento de transtornos de ansiedade, sendo de especial interesse para este trabalho, o transtorno do pânico. Modelos de estresse neonatal em animais de laboratório, que se baseiam na ruptura da relação mãe-filhote, como a separação materna e a privação materna, têm sido amplamente utilizados para avaliar as consequências desse estressor sobre a expressão de comportamentos defensivos associados à ansiedade na vida adulta. No entanto, pouco se sabe sobre seus efeitos em modelos animais de ataques de pânico, mais especificamente aqueles que associam esta condição emocional à resposta defensiva de fuga em animais. Diante disso, o objetivo inicial do presente trabalho foi o de estender as investigações dos efeitos do estresse neonatal sobre o comportamento de fuga de ratos adultos (após 60 dias de nascimento) observado no labirinto em T elevado (LTE), pela estimulação elétrica da substância cinzenta periaquedutal (SCPD) e durante a exposição a um ambiente em hipóxia (7% O2). Para efeitos comparativos, esses animais também foram testados em modelos animais associados à ansiedade generalizada e a depressão. Observamos que ratos Wistar submetidos à separação materna (3h/dia, do 2º ao 21º dia pós-nascimento) não diferiram de animais controles nos parâmetros comportamentais analisados nos modelos de pânico (fuga no LTE e pela estimulação elétrica da SCPD), nos de ansiedade (resposta de esquiva no LTE e o beber punido no teste de conflito de Vogel) ou no de depressão (tempo gasto em imobilidade no teste do nado forçado). Já em ratos privados da mãe (por 24h no 11º dia pós- nascimento), embora este estressor não tenha alterada a resposta de fuga no LTE, ele aumentou a expressão deste comportamento durante a exposição à hipóxia, sugestivo de um efeito panicogênico. Ainda empregando a privação materna, observamos que a administração intraperitoneal de um inibidor da síntese de serotonina, a pclorofenilalanina metil éster (p-CPA - 100mg/Kg/dia, por 4 dias antes dos testes comportamentais) facilitou a expressão do comportamento de fuga durante o teste da hipóxia nos animais controle, de maneira semelhante ao efeito obtido somente com a privação materna. Porém este tratamento não potencializou a fuga promovida pela privação materna. Já os níveis plasmáticos de corticosterona foram aumentados pela exposição à hipóxia, independentemente dos animais terem sido previamente privados da mãe ou terem recebido o pCPA antes do teste. Por fim, também observamos, através de uma análise por Western Blotting, que nem a privação materna ou a exposição à hipóxia altera a concentração de receptores serotonérgicos do tipo 5-HT1A na SCPD ou na amígdala. Em suma, nossos resultados mostram que a privação materna promove uma facilitação da resposta de fuga na hipóxia, sugerindo uma relação entre esse estresse neonatal e o desencadeamento de ataques de pânico de um subtipo específico, o pânico respiratório. Contudo, no que diz respeito ao envolvimento da neurotransmissão serotonérgica, mais estudos são necessários para entender sua participação nessa resposta. / Early life stress (ELS), including parental loss due to death, neglect or abuse, represents a major risk factor for the late development of psychiatric disorders, such as anxiety disorders. Animal models of ELS that are based on the disruption of mother-infant relationship, such as the repeated maternal separation or maternal deprivation, have been extensively used for the investigation of the longterm effects of these stressors on the expression of defensive behaviors associated with anxiety. However, little is known about their effects on animal models of panic attacks, more specifically in those that associate this emotional condition with escape behavior in animals. Therefore, the aim of the present study was to extend the investigation on the long-term consequences of neonatal stress on the escape response of adult rats (60 days after birth) evoked by the elevated T maze (ETM), electrical stimulation of the dorsal periaqueductal gray (DPAG) or hypoxia (7% O2). For comparative reasons, these animals were also tested in animal models of anxiety and depression. The results showed that the repeated maternal separation of male Wistar (3 hours/day from day 2 to 21 after birth) did not affect the behavioral indexes measured in the panic (escape in the ETM or after DPAG electrical stimulation), anxiety (ETM inhibitory avoidance or punished licking in the Vogel conflict test) or depression (time in immobility in the forced swimming test) models. On the other hand, rats submitted to maternal deprivation (24 hs in the 11th day after birth), although not differing from the control animals on escape expression in the ETM, showed a pronounced escape response during hypoxia, indicating a panicogenic-like response. Also, using this maternal deprivation protocol, we observed that systemic administration of a 5-HT synthesis inhibitor, p-chlrophenilalanine metylester (p-CPA - 100mg/Kg/day, for 4 days before the behavioral tests), facilitated escape expression during hypoxia in non-deprived animals to a level observed in non-pharmacologically treated deprived animals. We also observed that plasma corticosterone levels were increased 30 minutes after hypoxia exposure, independently of the previous condition of the animals (deprivation or drug treatment). Finally, we observed that the number of 5-HT1A receptors in the DPAG or amygdala, measured by Western Blotting, was not affect by previous maternal deprivation or exposure to hypoxia. Taken together, our results show that a single maternal deprivation episode facilitates the expression of escape behavior during hypoxia, suggesting a relationship between this ELS with the observation of a specific subtype of panic attack, the respiratory panic. Further studies are required in order to clarify the 5- HT involvement on these responses.

Dorsal periaqueductal gray matter

Early life stress

Estresse neonatal

Hipóxia

Hypoxia

Maternal deprivation

Maternal separation

Panic

Pânico

Pânico respiratório

Privação materna

Respiratory panic attacks

Separação materna

Serotonin

Serotonina

Substancia cinzenta periaquedutal