Takahiro Kuwaki scite author profile

The processing of stress responses involves brain-wide communication among cortical and subcortical regions; however, the underlying mechanisms remain elusive. Here, we show that the claustrum (CLA) is crucial for the control of stress-induced anxiety-related behaviors. A combined approach using brain activation mapping and machine learning showed that the CLA activation serves as a reliable marker of exposure to acute stressors. In TRAP2 mice, which allow activity-dependent genetic labeling, chemogenetic activation of the CLA neuronal ensemble tagged by acute social defeat stress (DS) elicited anxiety-related behaviors, whereas silencing of the CLA ensemble attenuated DS-induced anxiety-related behaviors. Moreover, the CLA received strong input from DS-activated basolateral amygdala neurons, and its circuit-selective optogenetic photostimulation temporarily elicited anxiety-related behaviors. Last, silencing of the CLA ensemble during stress exposure increased resistance to chronic DS. The CLA thus bidirectionally controls stress-induced emotional responses, and its inactivation can serve as a preventative strategy to increase stress resilience.

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Phosphoglucomutase. V. Multiple forms of phosphoglucomutase.

Joshi¹,

Hooper²,

Kuwaki³

et al. 1967

Proc. Natl. Acad. Sci. U.S.A.

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Enzymatic Cleavage of S-(Isopropylcarboxymethyl) Glutathione into Isovalthine*

Kuwaki¹

1965

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S-(1-2-dicarboxyethyl)cysteine in urine and kidney

Kuwaki

Mizuhara

1966

Biochimica et Biophysica Acta (BBA) - General Subjects

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Critical involvement of the orbitofrontal cortex in hyperlocomotion induced by NMDA receptor blockade in mice

Seiriki

Kasai

Kuwaki

et al. 2016

Biochemical and Biophysical Research Communications

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Takahiro Kuwaki

Claustrum mediates bidirectional and reversible control of stress-induced anxiety responses

Phosphoglucomutase. V. Multiple forms of phosphoglucomutase.

Enzymatic Cleavage of S-(Isopropylcarboxymethyl) Glutathione into Isovalthine*

S-(1-2-dicarboxyethyl)cysteine in urine and kidney

Critical involvement of the orbitofrontal cortex in hyperlocomotion induced by NMDA receptor blockade in mice

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