Sex-Specific Role for SLIT1 in Regulating Stress Susceptibility

Yentl Y. van der Zee; Casey K. Lardner; Eric M. Parise; Philipp Mews; Aarthi Ramakrishnan; Vishwendra Patel; Collin D. Teague; Marine Salery; Deena M. Walker; Caleb J. Browne; Benoit Labonté; Lyonna F. Parise; Hope Kronman; Catherine J. Penã; Angélica Torres-Berrío; Julia E. Duffy; Laurence de Nijs; Lars M.T. Eijssen; Li Shen; Bart Rutten; Orna Issler; Eric J. Nestler

doi:10.1016/j.biopsych.2021.01.019

Sex-Specific Role for SLIT1 in Regulating Stress Susceptibility

Yentl Y. van der Zee, Casey K. Lardner, Eric M. Parise, Philipp Mews, Aarthi Ramakrishnan, Vishwendra Patel, Collin D. Teague, Marine Salery, Deena M. Walker, Caleb J. Browne, Benoit Labonté, Lyonna F. Parise, Hope Kronman, Catherine J. Penã, Angélica Torres-Berrío, Julia E. Duffy, Laurence de Nijs, Lars M.T. Eijssen, Li Shen, Bart RuttenOrna Issler, Eric J. Nestler

Research output: Contribution to journal › Article › peer-review

12 Scopus citations

Abstract

Background: Major depressive disorder is a pervasive and debilitating syndrome characterized by mood disturbances, anhedonia, and alterations in cognition. While the prevalence of major depressive disorder is twice as high for women as men, little is known about the molecular mechanisms that drive sex differences in depression susceptibility. Methods: We discovered that SLIT1, a secreted protein essential for axonal navigation and molecular guidance during development, is downregulated in the adult ventromedial prefrontal cortex (vmPFC) of women with depression compared with healthy control subjects, but not in men with depression. This sex-specific downregulation of Slit1 was also observed in the vmPFC of mice exposed to chronic variable stress. To identify a causal, sex-specific role for SLIT1 in depression-related behavioral abnormalities, we performed knockdown (KD) of Slit1 expression in the vmPFC of male and female mice. Results: When combined with stress exposure, vmPFC Slit1 KD reflected the human condition by inducing a sex-specific increase in anxiety- and depression-related behaviors. Furthermore, we found that vmPFC Slit1 KD decreased the dendritic arborization of vmPFC pyramidal neurons and decreased the excitability of the neurons in female mice, effects not observed in males. RNA sequencing analysis of the vmPFC after Slit1 KD in female mice revealed an augmented transcriptional stress signature. Conclusions: Together, our findings establish a crucial role for SLIT1 in regulating neurophysiological and transcriptional responses to stress within the female vmPFC and provide mechanistic insight into novel signaling pathways and molecular factors influencing sex differences in depression susceptibility.

Original language	English (US)
Pages (from-to)	81-91
Number of pages	11
Journal	Biological Psychiatry
Volume	91
Issue number	1
DOIs	https://doi.org/10.1016/j.biopsych.2021.01.019
State	Published - Jan 1 2022
Externally published	Yes

Keywords

Chronic variable stress
Major depressive disorder
Prefrontal cortex
RNA sequencing
SLIT1

ASJC Scopus subject areas

Biological Psychiatry

Access to Document

10.1016/j.biopsych.2021.01.019

Cite this

van der Zee, Y. Y., Lardner, C. K., Parise, E. M., Mews, P., Ramakrishnan, A., Patel, V., Teague, C. D., Salery, M., Walker, D. M., Browne, C. J., Labonté, B., Parise, L. F., Kronman, H., Penã, C. J., Torres-Berrío, A., Duffy, J. E., de Nijs, L., Eijssen, L. M. T., Shen, L., ... Nestler, E. J. (2022). Sex-Specific Role for SLIT1 in Regulating Stress Susceptibility. Biological Psychiatry, 91(1), 81-91. https://doi.org/10.1016/j.biopsych.2021.01.019

van der Zee, YY, Lardner, CK, Parise, EM, Mews, P, Ramakrishnan, A, Patel, V, Teague, CD, Salery, M, Walker, DM, Browne, CJ, Labonté, B, Parise, LF, Kronman, H, Penã, CJ, Torres-Berrío, A, Duffy, JE, de Nijs, L, Eijssen, LMT, Shen, L, Rutten, B, Issler, O & Nestler, EJ 2022, 'Sex-Specific Role for SLIT1 in Regulating Stress Susceptibility', Biological Psychiatry, vol. 91, no. 1, pp. 81-91. https://doi.org/10.1016/j.biopsych.2021.01.019

@article{24049862eb9b4245ae8190c8e61fa7a2,

title = "Sex-Specific Role for SLIT1 in Regulating Stress Susceptibility",

abstract = "Background: Major depressive disorder is a pervasive and debilitating syndrome characterized by mood disturbances, anhedonia, and alterations in cognition. While the prevalence of major depressive disorder is twice as high for women as men, little is known about the molecular mechanisms that drive sex differences in depression susceptibility. Methods: We discovered that SLIT1, a secreted protein essential for axonal navigation and molecular guidance during development, is downregulated in the adult ventromedial prefrontal cortex (vmPFC) of women with depression compared with healthy control subjects, but not in men with depression. This sex-specific downregulation of Slit1 was also observed in the vmPFC of mice exposed to chronic variable stress. To identify a causal, sex-specific role for SLIT1 in depression-related behavioral abnormalities, we performed knockdown (KD) of Slit1 expression in the vmPFC of male and female mice. Results: When combined with stress exposure, vmPFC Slit1 KD reflected the human condition by inducing a sex-specific increase in anxiety- and depression-related behaviors. Furthermore, we found that vmPFC Slit1 KD decreased the dendritic arborization of vmPFC pyramidal neurons and decreased the excitability of the neurons in female mice, effects not observed in males. RNA sequencing analysis of the vmPFC after Slit1 KD in female mice revealed an augmented transcriptional stress signature. Conclusions: Together, our findings establish a crucial role for SLIT1 in regulating neurophysiological and transcriptional responses to stress within the female vmPFC and provide mechanistic insight into novel signaling pathways and molecular factors influencing sex differences in depression susceptibility.",

keywords = "Chronic variable stress, Major depressive disorder, Prefrontal cortex, RNA sequencing, SLIT1",

author = "{van der Zee}, {Yentl Y.} and Lardner, {Casey K.} and Parise, {Eric M.} and Philipp Mews and Aarthi Ramakrishnan and Vishwendra Patel and Teague, {Collin D.} and Marine Salery and Walker, {Deena M.} and Browne, {Caleb J.} and Benoit Labont{\'e} and Parise, {Lyonna F.} and Hope Kronman and Pen{\~a}, {Catherine J.} and Ang{\'e}lica Torres-Berr{\'i}o and Duffy, {Julia E.} and {de Nijs}, Laurence and Eijssen, {Lars M.T.} and Li Shen and Bart Rutten and Orna Issler and Nestler, {Eric J.}",

note = "Publisher Copyright: {\textcopyright} 2021 Society of Biological Psychiatry",

year = "2022",

month = jan,

day = "1",

doi = "10.1016/j.biopsych.2021.01.019",

language = "English (US)",

volume = "91",

pages = "81--91",

journal = "Biological Psychiatry",

issn = "0006-3223",

publisher = "Elsevier USA",

number = "1",

}

TY - JOUR

T1 - Sex-Specific Role for SLIT1 in Regulating Stress Susceptibility

AU - van der Zee, Yentl Y.

AU - Lardner, Casey K.

AU - Parise, Eric M.

AU - Mews, Philipp

AU - Ramakrishnan, Aarthi

AU - Patel, Vishwendra

AU - Teague, Collin D.

AU - Salery, Marine

AU - Walker, Deena M.

AU - Browne, Caleb J.

AU - Labonté, Benoit

AU - Parise, Lyonna F.

AU - Kronman, Hope

AU - Penã, Catherine J.

AU - Torres-Berrío, Angélica

AU - Duffy, Julia E.

AU - de Nijs, Laurence

AU - Eijssen, Lars M.T.

AU - Shen, Li

AU - Rutten, Bart

AU - Issler, Orna

AU - Nestler, Eric J.

PY - 2022/1/1

Y1 - 2022/1/1

N2 - Background: Major depressive disorder is a pervasive and debilitating syndrome characterized by mood disturbances, anhedonia, and alterations in cognition. While the prevalence of major depressive disorder is twice as high for women as men, little is known about the molecular mechanisms that drive sex differences in depression susceptibility. Methods: We discovered that SLIT1, a secreted protein essential for axonal navigation and molecular guidance during development, is downregulated in the adult ventromedial prefrontal cortex (vmPFC) of women with depression compared with healthy control subjects, but not in men with depression. This sex-specific downregulation of Slit1 was also observed in the vmPFC of mice exposed to chronic variable stress. To identify a causal, sex-specific role for SLIT1 in depression-related behavioral abnormalities, we performed knockdown (KD) of Slit1 expression in the vmPFC of male and female mice. Results: When combined with stress exposure, vmPFC Slit1 KD reflected the human condition by inducing a sex-specific increase in anxiety- and depression-related behaviors. Furthermore, we found that vmPFC Slit1 KD decreased the dendritic arborization of vmPFC pyramidal neurons and decreased the excitability of the neurons in female mice, effects not observed in males. RNA sequencing analysis of the vmPFC after Slit1 KD in female mice revealed an augmented transcriptional stress signature. Conclusions: Together, our findings establish a crucial role for SLIT1 in regulating neurophysiological and transcriptional responses to stress within the female vmPFC and provide mechanistic insight into novel signaling pathways and molecular factors influencing sex differences in depression susceptibility.

AB - Background: Major depressive disorder is a pervasive and debilitating syndrome characterized by mood disturbances, anhedonia, and alterations in cognition. While the prevalence of major depressive disorder is twice as high for women as men, little is known about the molecular mechanisms that drive sex differences in depression susceptibility. Methods: We discovered that SLIT1, a secreted protein essential for axonal navigation and molecular guidance during development, is downregulated in the adult ventromedial prefrontal cortex (vmPFC) of women with depression compared with healthy control subjects, but not in men with depression. This sex-specific downregulation of Slit1 was also observed in the vmPFC of mice exposed to chronic variable stress. To identify a causal, sex-specific role for SLIT1 in depression-related behavioral abnormalities, we performed knockdown (KD) of Slit1 expression in the vmPFC of male and female mice. Results: When combined with stress exposure, vmPFC Slit1 KD reflected the human condition by inducing a sex-specific increase in anxiety- and depression-related behaviors. Furthermore, we found that vmPFC Slit1 KD decreased the dendritic arborization of vmPFC pyramidal neurons and decreased the excitability of the neurons in female mice, effects not observed in males. RNA sequencing analysis of the vmPFC after Slit1 KD in female mice revealed an augmented transcriptional stress signature. Conclusions: Together, our findings establish a crucial role for SLIT1 in regulating neurophysiological and transcriptional responses to stress within the female vmPFC and provide mechanistic insight into novel signaling pathways and molecular factors influencing sex differences in depression susceptibility.

KW - Chronic variable stress

KW - Major depressive disorder

KW - Prefrontal cortex

KW - RNA sequencing

KW - SLIT1

UR - http://www.scopus.com/inward/record.url?scp=85106265398&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=85106265398&partnerID=8YFLogxK

U2 - 10.1016/j.biopsych.2021.01.019

DO - 10.1016/j.biopsych.2021.01.019

M3 - Article

C2 - 33896623

AN - SCOPUS:85106265398

SN - 0006-3223

VL - 91

SP - 81

EP - 91

JO - Biological Psychiatry

JF - Biological Psychiatry

IS - 1

ER -

Sex-Specific Role for SLIT1 in Regulating Stress Susceptibility

Abstract

Keywords

ASJC Scopus subject areas

Access to Document

Other files and links

Fingerprint

Cite this