Origem da inervação dopaminérgica da divisão central da amígdala expandida e da concha do núcleo Acumbens no rato. / Origin of dopaminergic fibers to the central extended amygdala and nucleus accumbens shell in the rat.

Renata Hydee Hasue

23 January 2001

A amígdala expandida central (EAc) inclui os núcleos central da amígdala (CeA), intersticial lateral da estria terminal (BSTl), intersticial do ramo posterior da comissura anterior (IPAC) e amígdala expandida sublenticular (SLEA). A EAc e a concha do acumbens possuem densa inervação dopaminérgica, implicada em processos motivacionais, e cuja origem foi estudada com a técnica de dupla marcação celular, combinando-se imunofluorescência para o traçador retrógrado Fluoro-Gold e para a tirosina hidroxilase. Nossos resultados indicam que a inervação dopaminérgica do CeA e BSTl é semelhante, se originando em igual proporção da área tegmental ventral (A10) e do núcleo dorsal da rafe/substância cinzenta periaquedutal (A10dc). A inervação dopaminérgica da SLEA, IPAC e concha do acumbens se origina principalmente do grupo A10. Com um anticorpo específico para dopamina vimos que parte da projeção do A10dc para o CeA é de fato dopaminérgica. Os grupos dopaminérgicos diencefálicos não inervam a EAc e a concha do acumbens. / The central extended amygdala (EAc) includes the central amygdaloid nucleus (CeA), lateral bed nucleus of the stria terminalis (BSTl), interstitial nucleus of the posterior limb of the anterior commissure (IPAC) and sublenticular extended amygdala (SLEA). The dopaminergic innervation of the EAc and nucleus accumbens shell is functionally related to motivational processes. Its origin was studied by combining immunofluorescence to tyrosine hydroxylase and Fluoro-Gold, used as retrograde tracer. Our results show that dopaminergic fibers to the CeA and BSTl derive in equal proportion from neurons in ventral tegmental area (A10) and in dorsal raphe nucleus/periaqueductal gray (A10dc). Dopaminergic inputs to SLEA, IPAC and accumbens shell arise mainly from A10 neurons. Using a dopamine antibody, we confirmed that A10dc projections to CeA are in part dopaminergic. Futhermore, the present data indicate that the diencephalic dopaminergic groups do not project to EAc and accumbens shell.

amígdala expandida

área tegmental ventral

núcleo acumbens

núcleo dorsal da rafe

substância cinzenta periaquedutal

tirosina hidroxilase

dorsal raphe nucleus

extended amygdala

nucleus accumbens

periaqueductal gray

tyrosine hydroxilase

ventral tegmental area

Female-Specific Role of Ciliary Neurotrophic Factor in the Medial Amygdala in Promoting Stress Responses

Jia, Cuihong, Gill, Wesley D., Lovins, Chiharu, Brown, Russell W., Hagg, Theo

01 March 2022

Ciliary neurotrophic factor (CNTF) is produced by astrocytes which have been implicated in regulating stress responses. We found that CNTF in the medial amygdala (MeA) promotes despair or passive coping, i.e., immobility in an acute forced swim stress, in female mice, while having no effect in males. Neutralizing CNTF antibody injected into the MeA of wildtype females reduced activation of downstream STAT3 (Y705) 24 and 48 h later. In concert, the antibody reduced immobility in the swim test in females and only after MeA injection, but not when injected in the central or basolateral amygdala. Antibody injected into the male MeA did not affect immobility. These data reveal a unique role of CNTF in female MeA in promoting despair or passive coping behavior. Moreover, 4 weeks of chronic unpredictable stress (CUS) increased immobility in the swim test and reduced sucrose preference in wildtype CNTF+/+, but not CNTF-/- littermate, females. Following CUS, 10 min of restraint stress increased plasma corticosterone levels only in CNTF+/+ females. In males, the CUS effects were present in both genotypes. Further, CUS increased CNTF expression in the MeA of female, but not male, mice. CUS did not alter CNTF in the female hippocampus, hypothalamus and bed nucleus of stria terminalis. This suggests that MeA CNTF has a female-specific role in promoting CUS-induced despair or passive coping, behavioral anhedonia and neuroendocrine responses. Compared to CNTF+/+ mice, CNTF-/- mice did not show differences in CUS-induced anxiety-like behavior and sensorimotor gating function as measured by elevated T-Maze, open field and pre-pulse inhibition of the acoustic startle response. Together, this study reveals a novel CNTF-mediated female-specific mechanism in stress responses and points to opportunities for developing treatments for stress-related disorders in women.

anhedonia

BLA

basolateral amygdala

BNST

bed nucleus of stria terminalis

CNTF

ciliary neurotrophic factor

CRF

corticotropin releasing factor

CUS

chronic unpredictable stress

CeA

central amygdala

Chronic unpredictable stress

HPA

hypothalamic-pituitary-adrenal

Hyp

hypothalamus

IL-6

interleukin-6

LIF

leukemia inhibitory factor

MeA

medial amygdala

neuroendocrine response

Neutralizing antibody

PAG

periaqueductal grey

PTSD

post-traumatic stress disorder

PVN

paraventricular nucleus

passive stress-coping

stereotaxic injection

TNF

tumor necrosis factor

mPFC

medial prefrontal cortex

Biomedical Sciences