Your search keyword '"Yentl Y. van der Zee"' showing total 13 results

1. The long noncoding RNA FEDORA is a cell type- and sex-specific regulator of depression

Author

Orna Issler, Yentl Y. van der Zee, Aarthi Ramakrishnan, Sunhui Xia, Alexander K. Zinsmaier, Chunfeng Tan, Wei Li, Caleb J. Browne, Deena M. Walker, Marine Salery, Angélica Torres-Berrío, Rita Futamura, Julia E. Duffy, Benoit Labonte, Matthew J. Girgenti, Carol A. Tamminga, Jeffrey L. Dupree, Yan Dong, James W. Murrough, Li Shen, and Eric J. Nestler

Subjects

Multidisciplinary

Abstract

Women suffer from depression at twice the rate of men, but the underlying molecular mechanisms are poorly understood. Here, we identify marked baseline sex differences in the expression of long noncoding RNAs (lncRNAs), a class of regulatory transcripts, in human postmortem brain tissue that are profoundly lost in depression. One such human lncRNA, RP11-298D21.1 (which we termed FEDORA), is enriched in oligodendrocytes and neurons and up-regulated in the prefrontal cortex (PFC) of depressed females only. We found that virally expressing FEDORA selectively either in neurons or in oligodendrocytes of PFC promoted depression-like behavioral abnormalities in female mice only, changes associated with cell type–specific regulation of synaptic properties, myelin thickness, and gene expression. We also found that blood FEDORA levels have diagnostic implications for depressed women and are associated with clinical response to ketamine. These findings demonstrate the important role played by lncRNAs, and FEDORA in particular, in shaping the sex-specific landscape of the brain and contributing to sex differences in depression.

Published

2022

2. Blood miR-144-3p: a novel diagnostic and therapeutic tool for depression

Author

Yentl Y. van der Zee, Lars M. T. Eijssen, Philipp Mews, Aarthi Ramakrishnan, Kelvin Alvarez, Casey K. Lardner, Hannah M. Cates, Deena M. Walker, Angélica Torres-Berrío, Caleb J. Browne, Ashley Cunningham, Flurin Cathomas, Hope Kronman, Eric M. Parise, Laurence de Nijs, Li Shen, James W. Murrough, Bart P. F. Rutten, Eric J. Nestler, Orna Issler, RS: MHeNs - R3 - Neuroscience, Psychiatrie & Neuropsychologie, Basic Neuroscience 1, and MUMC+: MA Psychiatrie (3)

Subjects

EXPRESSION, Depressive Disorder, Major, STRESS, MICRORNA, MAJOR DEPRESSION, PERIPHERAL-BLOOD, SUSCEPTIBILITY, RESILIENCE, CELL DISTRIBUTION WIDTH, Antidepressive Agents, Article, Epigenesis, Genetic, Cellular and Molecular Neuroscience, Psychiatry and Mental health, Mice, MicroRNAs, SOCIAL DEFEAT, TARGET, Animals, Ketamine, Molecular Biology, Biomarkers

Abstract

Major depressive disorder (MDD) is the leading cause of disability worldwide. There is an urgent need for objective biomarkers to diagnose this highly heterogeneous syndrome, assign treatment, and evaluate treatment response and prognosis. MicroRNAs (miRNAs) are short non-coding RNAs, which are detected in body fluids that have emerged as potential biomarkers of many disease conditions. The present study explored the potential use of miRNAs as biomarkers for MDD and its treatment. We profiled the expression levels of circulating blood miRNAs from mice that were collected before and after exposure to chronic social defeat stress (CSDS), an extensively validated mouse model used to study depression, as well as after either repeated imipramine or single-dose ketamine treatment. We observed robust differences in blood miRNA signatures between stress-resilient and stress-susceptible mice after an incubation period, but not immediately after exposure to the stress. Furthermore, ketamine treatment was more effective than imipramine at re-establishing baseline miRNA expression levels, but only in mice that responded behaviorally to the drug. We identified the red blood cell-specific miR-144-3p as a candidate biomarker to aid depression diagnosis and predict ketamine treatment response in stress-susceptible mice and MDD patients. Lastly, we demonstrate that systemic knockdown of miR-144-3p, via subcutaneous administration of a specific antagomir, is sufficient to reduce the depression-related phenotype in stress-susceptible mice. RNA-sequencing analysis of blood after such miR-144-3p knockdown revealed a blunted transcriptional stress signature as well. These findings identify miR-144-3p as a novel target for diagnosis of MDD as well as for antidepressant treatment, and enhance our understanding of epigenetic processes associated with depression.

Published

2021

3. H3K79me2 dynamics in medium spiny neurons mediate long-term behavioral and cell type-specific molecular effects of early life stress

Author

Simone Sidoli, Eric J. Nestler, Deena M. Walker, Orna Issler, Hope Kronman, Caleb J. Browne, Benjamin A. Garcia, Arthur Godino, Catherine Jensen Pena, Philipp Mews, Yentl Y. van der Zee, Eric M. Parise, Rachael L. Neve, Aarthi Ramakrishnan, Angélica Torres-Berrío, Brittany F. Boyce, Li Shen, and Casey K. Lardner

Subjects

Male, 0301 basic medicine, Jumonji Domain-Containing Histone Demethylases, Nucleus accumbens, Medium spiny neuron, Nucleus Accumbens, Article, Histones, Social defeat, Mice, 03 medical and health sciences, Histone H3, 0302 clinical medicine, Transcriptional regulation, Animals, Histone Demethylases, Neurons, Regulation of gene expression, biology, Receptors, Dopamine D2, F-Box Proteins, Receptors, Dopamine D1, General Neuroscience, Histone-Lysine N-Methyltransferase, DOT1L, 030104 developmental biology, Histone, Gene Expression Regulation, biology.protein, Neuroscience, Stress, Psychological, 030217 neurology & neurosurgery

Abstract

Animals susceptible to chronic social defeat stress (CSDS) exhibit depression-related behaviors, and show aberrant transcription across several limbic brain regions. The nucleus accumbens (NAc) in particular shows unique susceptible versus resilient phenotypes at the transcriptional, neuroanatomical, and physiological levels. Early life stress (ELS) promotes susceptibility to CSDS in adulthood, but associated enduring changes in transcriptional control mechanisms in NAc have not yet been investigated. Here, we examined long-lasting changes in histone modifications induced in NAc by ELS and studied their underlying mechanisms in mediating heightened lifelong stress susceptibility in male and female mice. We identify dimethylation of lysine 79 of histone H3 (H3K79me2) and the enzymes that control this modification, selectively in D2-type medium spiny neurons, as crucial for the expression of ELS-induced stress susceptibility. We also map the site-specific regulation of this histone mark genome-wide, and reveal the transcriptional networks it modulates. Finally, we demonstrate the potential clinical relevance of this epigenetic mechanism by showing that systemic delivery of a small molecule inhibitor of H3K79me2 deposition reverses ELS-induced behavioral deficits.

Published

2021

4. Sex-specific role for SLIT1 in regulating stress susceptibility

Author

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

Subjects

0301 basic medicine, Male, medicine.medical_specialty, Anhedonia, Ventromedial prefrontal cortex, Prefrontal Cortex, Anxiety, Article, 03 medical and health sciences, Mice, 0302 clinical medicine, Downregulation and upregulation, Internal medicine, Medicine, Animals, Prefrontal cortex, Biological Psychiatry, Depression (differential diagnoses), Gene knockdown, Depressive Disorder, Major, Sex Characteristics, business.industry, medicine.disease, 030104 developmental biology, medicine.anatomical_structure, Endocrinology, Major depressive disorder, Female, medicine.symptom, business, 030217 neurology & neurosurgery

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.

Published

2021

5. Gene-Targeted, CREB-Mediated Induction of ΔFosB Controls Distinct Downstream Transcriptional Patterns Within D1 and D2 Medium Spiny Neurons

Author

Arthur Godino, Marine Salery, Molly Estill, Li Shen, Ashley M. Cunningham, Eric J. Nestler, Casey K. Lardner, Hope Kronman, Peter J. Hamilton, Eric M. Parise, Rachael L. Neve, Yentl Y. van der Zee, and Jee Hyun Kim

Subjects

Male, Neurons, Addiction, media_common.quotation_subject, Receptors, Dopamine D1, Gene Expression, Mice, Transgenic, Biology, Nucleus accumbens, CREB, Medium spiny neuron, Nucleus Accumbens, Cell biology, Mice, Inbred C57BL, Mice, Cocaine, Gene expression, biology.protein, Epigenome editing, Transcriptional regulation, Animals, Female, Transcription factor, Biological Psychiatry, media_common

Abstract

Background The onset and persistence of addiction phenotypes are, in part, mediated by transcriptional mechanisms in the brain that affect gene expression and, subsequently, neural circuitry. ΔFosB is a transcription factor that accumulates in the nucleus accumbens (NAc)—a brain region responsible for coordinating reward and motivation—after exposure to virtually every known rewarding substance, including cocaine and opioids. ΔFosB has also been shown to directly control gene transcription and behavior downstream of both cocaine and opioid exposure, but with potentially different roles in D1 and D2 medium spiny neurons (MSNs) in NAc. Methods To clarify MSN subtype-specific roles for ΔFosB and investigate how these coordinate the actions of distinct classes of addictive drugs in NAc, we developed a CRISPR (clustered regularly interspaced short palindromic repeats)/Cas9-based epigenome editing tool to induce endogenous ΔFosB expression in vivo in the absence of drug exposure. After inducing ΔFosB in D1- or D2-MSNs or both, we performed RNA sequencing on bulk male and female NAc tissue (n = 6–8/group). Results We found that ΔFosB induction elicits distinct transcriptional profiles in NAc by MSN subtype and by sex, establishing for the first time that ΔFosB mediates different transcriptional effects in males versus females. We also demonstrated that changes in D1-MSNs, but not those in D2-MSNs or both, significantly recapitulate changes in gene expression induced by cocaine self-administration. Conclusions Together, these findings demonstrate the efficacy of a novel molecular tool for studying cell type–specific transcriptional mechanisms and shed new light on the activity of ΔFosB, a critical transcriptional regulator of drug addiction.

Published

2020

6. Adolescent Social Isolation Reprograms the Medial Amygdala: Transcriptome and Sex Differences in Reward

Author

Hannah M. Cates, Andrew P. Lipschultz, Li Shen, Georgia E. Hodes, Bin Zhang, Ashley M. Cunningham, Arthur Godino, Orna Issler, Yentl Y. van der Zee, Eric M. Parise, Aarthi Ramakrishnan, Catherine Jensen Pena, Angélica Torres-Berrío, Xianxiao Zhou, Eric J. Nestler, Deena M. Walker, Caleb J. Browne, Pamela J. Kennedy, and Rosemary C. Bagot

Subjects

0303 health sciences, Period (gene), CRYM, Crystallin mu, Biology, Amygdala, Transcriptome, 03 medical and health sciences, 0302 clinical medicine, medicine.anatomical_structure, Gene expression, medicine, Anxiety, Social isolation, medicine.symptom, Neuroscience, 030217 neurology & neurosurgery, 030304 developmental biology

Abstract

Adolescence is a sensitive window for reward- and stress-associated behavior. Although stress during this period causes long-term changes in behavior in males, how females respond is relatively unknown. Here we show that social isolation stress in adolescence, but not adulthood, induces persistent but opposite effects on anxiety- and cocaine-related behaviors in male vs. female mice, and that these effects are reflected in transcriptional profiles within the adult medial amygdala (meA). By integrating differential gene expression with co-expression network analyses, we identified crystallin mu (Crym), a thyroid-binding protein, as a key driver of these transcriptional profiles. Manipulation of Crym specifically within adult meA neurons recapitulates the behavioral and transcriptional effects of social isolation and re-opens a window of plasticity that is otherwise closed. Our results establish that meA is essential for sex-specific responses to stressful and rewarding stimuli through transcriptional programming that occurs during adolescence.

Published

2020

7. Author Correction: Long-term behavioral and cell-type-specific molecular effects of early life stress are mediated by H3K79me2 dynamics in medium spiny neurons

Author

Eric M. Parise, Li Shen, Orna Issler, Eric J. Nestler, Deena M. Walker, Caleb J. Browne, Benjamin A. Garcia, Casey K. Lardner, Catherine Jensen Pena, Simone Sidoli, Arthur Godino, Hope Kronman, Aarthi Ramakrishnan, Yentl Y. van der Zee, Rachael L. Neve, Philipp Mews, Brittany F. Boyce, and Angélica Torres-Berrío

Subjects

General Neuroscience, Cell type specific, Early life stress, Biology, Medium spiny neuron, Neuroscience, Term (time)

Published

2021

8. Sex-Specific Role for the Long Non-coding RNA LINC00473 in Depression

Author

Yentl Y. van der Zee, Li Shen, Catherine Jensen Pena, Yan Dong, Orna Issler, Angélica Torres-Berrío, Benoit Labonté, Zachary S. Lorsch, Chunfeng Tan, Julia E. Duffy, Brigham J. Hartley, Kristen J. Brennand, Eric M. Parise, Erin Flaherty, Junshi Wang, Peter J. Hamilton, Yong-Hwee E. Loh, Immanuel Purushothaman, Rachael L. Neve, Eric J. Nestler, Deena M. Walker, Hope Kronman, Aarthi Ramakrishnan, Molly Estill, Erin S. Calipari, Carol A. Tamminga, Psychiatrie & Neuropsychologie, and RS: MHeNs - R3 - Neuroscience

Subjects

Male, 0301 basic medicine, STRESS, PREFRONTAL CORTEX, SUSCEPTIBILITY, Social defeat, Mice, 0302 clinical medicine, SOCIAL DEFEAT, Gene expression, RNA-Seq, TRANSCRIPTION, Prefrontal cortex, Aged, 80 and over, Neurons, Behavior, Animal, biology, Depression, Effector, General Neuroscience, LOCALIZATION, Middle Aged, Resilience, Psychological, Phenotype, Long non-coding RNA, Female, RNA, Long Noncoding, Adult, medicine.medical_specialty, Down-Regulation, UNIQUE FEATURES, Mice, Transgenic, CREB, Young Adult, 03 medical and health sciences, Sex Factors, Internal medicine, medicine, Animals, Humans, Gene, Aged, Depressive Disorder, Major, GENOME-WIDE, EVOLUTION, 030104 developmental biology, Endocrinology, CELLS, biology.protein, Stress, Psychological, 030217 neurology & neurosurgery

Abstract

Depression is a common disorder that affects women at twice the rate of men. Here, we report that long non-coding RNAs (lncRNAs), a recently discovered class of regulatory transcripts, represent about one-third of the differentially expressed genes in the brains of depressed humans and display complex region- and sex-specific patterns of regulation. We identified the primate-specific, neuronal-enriched gene LINC00473 as downregulated in prefrontal cortex (PFC) of depressed females but not males. Using viral-mediated gene transfer to express LINC00473 in adult mouse PFC neurons, we mirrored the human sex-specific phenotype by inducing stress resilience solely in female mice. This sex-specific phenotype was accompanied by changes in synaptic function and gene expression selectively in female mice and, along with studies of human neuron-like cells in culture, implicates LINC00473 as a CREB effector. Together, our studies identify LINC00473 as a female-specific driver of stress resilience that is aberrant in female depression. Issler et al. demonstrate that long non-coding RNAs are robustly regulated in the brains of postmortem depressed humans in a brain site- and sex-specific manner. LINC00473 is highlighted as key regulator of mood in females only, where it acts in prefrontal cortex by regulating gene expression, neurophysiology, and behavior.

Published

2020

9. Cell type-specific epigenetic priming of gene expression in nucleus accumbens by cocaine.

Author

Mews P, Van der Zee Y, Gurung A, Estill M, Futamura R, Kronman H, Ramakrishnan A, Ryan M, Reyes AA, Garcia BA, Browne CJ, Sidoli S, Shen L, and Nestler EJ

Subjects

Animals, Mice, Male, Gene Expression Regulation drug effects, Cocaine-Related Disorders genetics, Cocaine-Related Disorders metabolism, Receptors, Dopamine D1 metabolism, Receptors, Dopamine D1 genetics, Neurons metabolism, Neurons drug effects, Chromatin metabolism, Chromatin genetics, Nucleus Accumbens metabolism, Nucleus Accumbens drug effects, Cocaine pharmacology, Epigenesis, Genetic drug effects, Histones metabolism

Abstract

A hallmark of addiction is the ability of drugs of abuse to trigger relapse after periods of prolonged abstinence. Here, we describe an epigenetic mechanism whereby chronic cocaine exposure causes lasting chromatin and downstream transcriptional modifications in the nucleus accumbens (NAc), a critical brain region controlling motivation. We link prolonged withdrawal from cocaine to the depletion of the histone variant H2A.Z, coupled with increased genome accessibility and latent priming of gene transcription, in D1 dopamine receptor-expressing medium spiny neurons (D1 MSNs) that relate to aberrant gene expression upon drug relapse. The histone chaperone ANP32E removes H2A.Z from chromatin, and we demonstrate that D1 MSN-selective Anp32e knockdown prevents cocaine-induced H2A.Z depletion and blocks cocaine's rewarding actions. By contrast, very different effects of cocaine exposure, withdrawal, and relapse were found for D2 MSNs. These findings establish histone variant exchange as an important mechanism and clinical target engaged by drugs of abuse to corrupt brain function and behavior.

Published

2024

10. Male and female variability in response to chronic stress and morphine in C57BL/6J, DBA/2J, and their BXD progeny.

Author

Morel C, Parise LF, Van der Zee Y, Issler O, Cai M, Browne C, Blando A, Leclair K, Haynes S, Williams RW, Mulligan MK, Russo SJ, Nestler EJ, and Han MH

Abstract

Drug addiction is a multifactorial syndrome in which genetic predispositions and exposure to environmental stressors constitute major risk factors for the early onset, escalation, and relapse of addictive behaviors. While it is well known that stress plays a key role in drug addiction, the genetic factors that make certain individuals particularly sensitive to stress and thereby more vulnerable to becoming addicted are unknown. In an effort to test a complex set of gene x environment interactions-specifically gene x chronic stress -here we leveraged a systems genetics resource: BXD recombinant inbred mice (BXD5, BXD8, BXD14, BXD22, BXD29, and BXD32) and their parental mouse lines, C57BL/6J and DBA/2J. Utilizing the chronic social defeat stress (CSDS) and chronic variable stress (CVS) paradigms, we first showed sexual dimorphism in the behavioral stress response between the mouse strains. Further, we observed an interaction between genetic background and vulnerability to prolonged exposure to non-social stressors. Finally, we found that DBA/2J and C57BL/6J mice pre-exposed to stress displayed differences in morphine sensitivity. Our results support the hypothesis that genetic variation in predisposition to stress responses influences morphine sensitivity and is likely to modulate the development of drug addiction.

Published

2024

11. Monomethylation of Lysine 27 at Histone 3 Confers Lifelong Susceptibility to Stress.

Author

Torres-Berrío A, Estill M, Ramakrishnan A, Kronman H, Patel V, Minier-Toribio A, Issler O, Browne CJ, Parise EM, van der Zee Y, Walker D, Martínez-Rivera FJ, Lardner CK, Cuttoli RD, Russo SJ, Shen L, Sidoli S, and Nestler EJ

Abstract

Histone post-translational modifications are critical for mediating persistent alterations in gene expression. By combining unbiased proteomics profiling, and genome-wide approaches, we uncovered a role for mono-methylation of lysine 27 at histone H3 (H3K27me1) in the enduring effects of stress. Specifically, mice exposed to early life stress (ELS) or to chronic social defeat stress (CSDS) in adulthood displayed increased enrichment of H3K27me1, and transient decreases in H3K27me2, in the nucleus accumbens (NAc), a key brain-reward region. Stress induction of H3K27me1 was mediated by the VEFS domain of SUZ12, a core subunit of the polycomb repressive complex-2, which is induced by chronic stress and controls H3K27 methylation patterns. Overexpression of the VEFS domain led to social, emotional, and cognitive abnormalities, and altered excitability of NAc D1 mediums spiny neurons. Together, we describe a novel function of H3K27me1 in brain and demonstrate its role as a "chromatin scar" that mediates lifelong stress susceptibility.

Published

2023

12. Crystallin Mu in Medial Amygdala Mediates the Effect of Social Experience on Cocaine Seeking in Males but Not in Females.

Author

Walker DM, Zhou X, Cunningham AM, Ramakrishnan A, Cates HM, Lardner CK, Peña CJ, Bagot RC, Issler O, Van der Zee Y, Lipschultz AP, Godino A, Browne CJ, Hodes GE, Parise EM, Torres-Berrio A, Kennedy PJ, Shen L, Zhang B, and Nestler EJ

Subjects

Animals, Male, Female, Mice, mu-Crystallins, Reward, Neurons metabolism, Amygdala metabolism, Cocaine pharmacology, Cocaine metabolism

Abstract

Background: Social experiences influence susceptibility to substance use disorder. The adolescent period is associated with the development of social reward and is exceptionally sensitive to disruptions to reward-associated behaviors by social experiences. Social isolation (SI) during adolescence alters anxiety- and reward-related behaviors in adult males, but little is known about females. The medial amygdala (meA) is a likely candidate for the modulation of social influence on drug reward because it regulates social reward, develops during adolescence, and is sensitive to social stress. However, little is known regarding how the meA responds to drugs of abuse., Methods: We used adolescent SI coupled with RNA sequencing to better understand the molecular mechanisms underlying meA regulation of social influence on reward., Results: We show that SI in adolescence, a well-established preclinical model for addiction susceptibility, enhances preference for cocaine in male but not in female mice and alters cocaine-induced protein and transcriptional profiles within the adult meA particularly in males. To determine whether transcriptional mechanisms within the meA are important for these behavioral effects, we manipulated Crym expression, a sex-specific key driver gene identified through differential gene expression and coexpression network analyses, specifically in meA neurons. Overexpression of Crym, but not another key driver that did not meet our sex-specific criteria, recapitulated the behavioral and transcriptional effects of adolescent SI., Conclusions: These results show that the meA is essential for modulating the sex-specific effects of social experience on drug reward and establish Crym as a critical mediator of sex-specific behavioral and transcriptional plasticity., (Copyright © 2022 Society of Biological Psychiatry. Published by Elsevier Inc. All rights reserved.)

Published

2022

13. Gene-Targeted, CREB-Mediated Induction of ΔFosB Controls Distinct Downstream Transcriptional Patterns Within D1 and D2 Medium Spiny Neurons.

Author

Lardner CK, van der Zee Y, Estill MS, Kronman HG, Salery M, Cunningham AM, Godino A, Parise EM, Kim JH, Neve RL, Shen L, Hamilton PJ, and Nestler EJ

Subjects

Animals, Female, Gene Expression, Male, Mice, Mice, Inbred C57BL, Mice, Transgenic, Neurons metabolism, Receptors, Dopamine D1 metabolism, Cocaine, Nucleus Accumbens metabolism

Abstract

Background: The onset and persistence of addiction phenotypes are, in part, mediated by transcriptional mechanisms in the brain that affect gene expression and, subsequently, neural circuitry. ΔFosB is a transcription factor that accumulates in the nucleus accumbens (NAc)-a brain region responsible for coordinating reward and motivation-after exposure to virtually every known rewarding substance, including cocaine and opioids. ΔFosB has also been shown to directly control gene transcription and behavior downstream of both cocaine and opioid exposure, but with potentially different roles in D1 and D2 medium spiny neurons (MSNs) in NAc., Methods: To clarify MSN subtype-specific roles for ΔFosB and investigate how these coordinate the actions of distinct classes of addictive drugs in NAc, we developed a CRISPR (clustered regularly interspaced short palindromic repeats)/Cas9-based epigenome editing tool to induce endogenous ΔFosB expression in vivo in the absence of drug exposure. After inducing ΔFosB in D1- or D2-MSNs or both, we performed RNA sequencing on bulk male and female NAc tissue (n = 6-8/group)., Results: We found that ΔFosB induction elicits distinct transcriptional profiles in NAc by MSN subtype and by sex, establishing for the first time that ΔFosB mediates different transcriptional effects in males versus females. We also demonstrated that changes in D1-MSNs, but not those in D2-MSNs or both, significantly recapitulate changes in gene expression induced by cocaine self-administration., Conclusions: Together, these findings demonstrate the efficacy of a novel molecular tool for studying cell type-specific transcriptional mechanisms and shed new light on the activity of ΔFosB, a critical transcriptional regulator of drug addiction., (Copyright © 2021 Society of Biological Psychiatry. Published by Elsevier Inc. All rights reserved.)

Published

2021