Modulation of anxiety by cortical serotonin 1A receptors

Piszczek, Łukasz; Piszczek, Agnieszka; Kuczmanska, Joanna; Audero, Enrica; Gross, Cornelius

doi:10.3389/fnbeh.2015.00048

Cited by 19 publications

(16 citation statements)

References 70 publications

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“…Related to the hypothesis that 5-HT functions to moderate aversive mental states ( Deakin and Graeff, 1991 ) and promote patience ( McDannald, 2015 ) is the notion that 5-HT plays an important role in negatively modulating anxiety ( Piszczek et al, 2015 ). Selective reductions of 5-HT in the forebrain have been found to enhance anxiety-related behaviours ( Pum et al, 2009 ; Tu et al, 2014 ), whereas chronically administered SSRIs have been found to reduce anxiety ( Blanco et al, 2013 ).…”

Section: Psychological Functions Associated With Brain 5-htmentioning

confidence: 99%

“…Selective reductions of 5-HT in the forebrain have been found to enhance anxiety-related behaviours ( Pum et al, 2009 ; Tu et al, 2014 ), whereas chronically administered SSRIs have been found to reduce anxiety ( Blanco et al, 2013 ). Like impulsivity and aggression, anxiety appears to be negatively modulated by 5-HT1AR stimulation ( Heisler et al, 1998 ; Parks et al, 1998 ; Schreiber and De Vry, 1993 ; Toth, 2003 ), and although there are some contradictory findings ( File et al, 1996 ), this effect appears to be mediated by postsynaptic 5-HT1AR signalling ( Celada et al, 2013a ; Gross et al, 2002 ; Piszczek et al, 2015 ; Stefanski et al, 1993 ; Tauscher et al, 2001 ; Tu et al, 2014 ; Zhou et al, 2008 , 2014 ).…”

Section: Psychological Functions Associated With Brain 5-htmentioning

confidence: 99%

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Serotonin and brain function: a tale of two receptors

2017

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Previous attempts to identify a unified theory of brain serotonin function have largely failed to achieve consensus. In this present synthesis, we integrate previous perspectives with new and older data to create a novel bipartite model centred on the view that serotonin neurotransmission enhances two distinct adaptive responses to adversity, mediated in large part by its two most prevalent and researched brain receptors: the 5-HT1A and 5-HT2A receptors. We propose that passive coping (i.e. tolerating a source of stress) is mediated by postsynaptic 5-HT1AR signalling and characterised by stress moderation. Conversely, we argue that active coping (i.e. actively addressing a source of stress) is mediated by 5-HT2AR signalling and characterised by enhanced plasticity (defined as capacity for change). We propose that 5-HT1AR-mediated stress moderation may be the brain’s default response to adversity but that an improved ability to change one’s situation and/or relationship to it via 5-HT2AR-mediated plasticity may also be important – and increasingly so as the level of adversity reaches a critical point. We propose that the 5-HT1AR pathway is enhanced by conventional 5-HT reuptake blocking antidepressants such as the selective serotonin reuptake inhibitors (SSRIs), whereas the 5-HT2AR pathway is enhanced by 5-HT2AR-agonist psychedelics. This bipartite model purports to explain how different drugs (SSRIs and psychedelics) that modulate the serotonergic system in different ways, can achieve complementary adaptive and potentially therapeutic outcomes.

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Section: Psychological Functions Associated With Brain 5-htmentioning

confidence: 99%

Section: Psychological Functions Associated With Brain 5-htmentioning

confidence: 99%

Serotonin and brain function: a tale of two receptors

2017

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“…Stimulation of HTR1A within the hippocampus or amygdala was known to produce an anxiogenic effect, while HTR1A agonist injection into the dorsal raphe nucleus was anxiolytic . Findings from transgenic animals showed that overexpression of HTR1A in forebrain and even in cortical principal neurons could reverse the anxiety phenotype of HTR1A knockout mice . Therefore, we speculate that increasing HTR1A in ACC is likely associated with decreasing anxiety in rats, which need to be researched further.…”

Section: Discussionmentioning

confidence: 99%

“…6,31,32 Findings from transgenic animals showed that overexpression of HTR1A in forebrain and even in cortical principal neurons could reverse the anxiety phenotype of HTR1A knockout mice. 33,34 Therefore, we speculate that increasing HTR1A in ACC is likely associated with decreasing anxiety in rats, which need to be researched further.…”

Section: Consistent Withmentioning

confidence: 91%

Down‐regulation of HTR1A‐modulated ACC activation contributes to stress‐induced visceral hyperalgesia in rats

Sun

Zhang

et al. 2019

Neurogastroenterology Motil

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Background Long‐term stress was suggested to cause visceral hypersensitivity and promote functional gastrointestinal disorders (FGIDs). Some brain regions such as the anterior cingulate cortex (ACC) may play an important role for generating visceral hypersensitivity; however, its molecular mechanisms are not clear. This study aimed to explore the role of 5‐HT1A receptors (HTR1As) in activating ACC and corresponding mechanism, in stress‐induced visceral hyperalgesia rats. Methods The VH rat model was established by chronic water avoidance stress (WAS), and the visceral sensitivity was measured by electromyogram. Rat's anxiety‐like behaviors were evaluated by the open field test (OFT) and elevated plus maze (EPM). To overexpress or down‐regulate HTR1A expression, HTR1A‐specific lentivirus expressing the green fluorescent protein was administered into the ACC. Protein expression levels were observed by Western blot. Results The protein expression of HTR1A in bilateral ACC in WAS group was significantly lower than that in normal control (NC) and Sham‐WAS groups, while the levels of c‐fos in the ACC of WAS rats were significantly higher. Down‐regulation of HTR1As could induce VH in control rats with the increased expression of c‐fos, p‐ERK, and p‐Akt in ACC, while up‐regulation of HTR1As in the ACC could partly inhibit ACC sensitization and stress‐induced visceral hyperalgesia. Conclusions & Inferences Down‐regulation of HTR1As modulates ACC activation probably through activating ERK and Akt pathways, thus contributes to the formation of stress‐induced visceral hyperalgesia.

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“…As reported in other papers. (62)(63)(64) Activation of serotonin receptors may result in anxiolytic response (65), and estrogen may modulate this response (66). Other neurotransmitters and hormones may participate in this response.…”

Section: Discussionmentioning

confidence: 99%

Efeitos da corticosterona e do estrógeno na atividade do eixo HPA de ratas: comportamento e comprimento dos telômeros

Filho¹,

de²

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Agradeço a Deus, por ter me dado serenidade e calma em todos os momentos. Aos meus pais Maria Lúcia e Procópio Barcellos, e minhas irmãs Milene e Mariel, por sempre me apoiarem em todos os momentos da minha vida, me dando apoio, conselhos e amor. Foi bem difícil ficar longe todos esses anos, mas não teve um dia que deixei de sentir saudade de vocês. Tudo que consegui nesse momento, é graças a educação que me proporcionaram ao longo desses anos. Sem o apoio e carinho, não teria conseguido chegar aqui. Amo muito vocês. Ao professor Franci, que sempre me tratou com muita educação e respeito. Agradeço a confiança, convívio e ensinamentos ao longos desses sete anos no laboratório. O seu exemplo me fez crescer tanto profissionalmente como pessoalmente. Gratidão por tudo. Ao professor Rodrigo Tocantins Calado, que sem a usa ajuda nas análises dos telômeros, esse projeto não poderia ser feito. E a todos que convivi no laboratório de hematologia do Hospital das Clínicas de Ribeirão Preto. Em especial ao Leonardo, Barbara e Rita. Muito obrigado por toda ajuda, desde as extrações de DNA, até ao final das análises. Aos meus amigos do laboratório Bruno e Iracema, em especial a querida Fabiana, que sempre trouxe muita alegria para o laboratório. A Larissa, pela amizade ao longo desses anos. Ao Guillermo, por toda a ajuda e conselhos durante o meu mestrado. A Nathália, que tive o prazer de conviver durante os primeiros anos do doutorado. E a Luana (Lucy), minha grande amiga e companheira no laboratório, apesar de estar longe nesses últimos anos, sempre pude contar com você para tudo, muito obrigado por me ajudar a me aceitar e amar. A minha querida Aline (Linete), minha grande companheira de pós-graduação e amiga. Seu apoio em todos os momentos foram imprescindíveis para a conclusão da tese. Você não foi apenas a minha amiga, mas minha irmã de coração. Sua alegria de viver é linda e exemplar. Cada momento passado com você me trouxe muito carinho e amor. E agradeço também a sua família, por sempre me tratar tão bem e me acolher. A querida Ana Omoto (Aninha), um dos melhores presentes que eu tive nesse últimos anos. Sua amizade trouxe muita luz e paz na minha vida. Agradeço muito a Deus por ter me dado uma grande amiga irmã. Seu companheirismo na reta final me ajudou a ter serenidade para concluir o trabalho. Agradeço a sua família também, que sempre me trataram com muito carinho. A minha goiana favorita, Ludmila, seu apoio e amizade nesses últimos meses me trouxe muita força e coragem. Uma pessoa muito verdadeira, gentil e amável. Sentirei muita falta de tomar um cafezinho na cantina com você. Espero algum dia conhecer Goiânia com você. Aos amigos que a pós-graduação trouxe, onde sempre pude conversar e partilhar das nossas experiências, sou muito grato, em especial a Mariana Benício,

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Modulation of anxiety by cortical serotonin 1A receptors

Cited by 19 publications

References 70 publications

Serotonin and brain function: a tale of two receptors

Serotonin and brain function: a tale of two receptors

Down‐regulation of HTR1A‐modulated ACC activation contributes to stress‐induced visceral hyperalgesia in rats

Efeitos da corticosterona e do estrógeno na atividade do eixo HPA de ratas: comportamento e comprimento dos telômeros

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