Your search keyword '"Emily J Yao"' showing total 7 results

1. Systems genetic analysis of binge‐like eating in a <scp>C57BL</scp> / <scp>6J</scp> x <scp>DBA</scp> / <scp>2J‐F2</scp> cross

Author

Richard K Babbs, Emily J Yao, Julia C Kelliher, Kimberly P. Luttik, Kristyn N. Borrelli, Camron D. Bryant, Megan K. Mulligan, and M. Imad Damaj

Subjects

0301 basic medicine, Genetics, Candidate gene, Binge eating, Bulimia nervosa, Genome-wide association study, Quantitative trait locus, Biology, medicine.disease, Article, 03 medical and health sciences, Behavioral Neuroscience, Eating disorders, 030104 developmental biology, 0302 clinical medicine, Neurology, Binge-eating disorder, Expression quantitative trait loci, medicine, medicine.symptom, 030217 neurology & neurosurgery

Abstract

Binge eating is a heritable trait associated with eating disorders and refers to the rapid consumption of a large quantity of energy-dense food that is, associated with loss of control and negative affect. Binge eating disorder is the most common eating disorder in the United States; however, the genetic basis is unknown. We previously identified robust mouse inbred strain differences between C57BL/6J and DBA/2J in binge-like eating of sweetened palatable food in an intermittent access, conditioned place preference paradigm. To map the genetic basis of changes in body weight and binge-like eating (BLE) and to identify candidate genes, we conducted quantitative trait locus (QTL) analysis in 128 C57BL/6J x DBA/2J-F2 mice combined with PheQTL and trait covariance analysis in GeneNetwork2 using legacy BXD-RI trait datasets. We identified a QTL on Chromosome 18 influencing changes in body weight across days in females (log of the odds [LOD] = 6.3; 1.5-LOD: 3-12 cM) that contains the candidate gene Zeb1. We also identified a sex-combined QTL influencing initial palatable food intake on Chromosome 5 (LOD = 5.8; 1.5-LOD: 21-28 cM) that contains the candidate gene Lcorl and a second QTL influencing escalated palatable food intake on Chromosome 6 in males (LOD = 5.4; 1.5-LOD: 50-59 cM) that contains the candidate genes Adipor2 and Plxnd1. Finally, we identified a suggestive QTL in females for slope of BLE on distal Chromosome 18 (LOD = 4.1; p = 0.055; 1.5-LOD: 23-35 cM). Future studies will use BXD-RI strains to fine map loci and support candidate gene nomination for gene editing.

Published

2021

2. Sex differences in behavioral and brainstem transcriptomic neuroadaptations following neonatal opioid exposure in outbred mice

Author

Julia L. Scotellaro, Ryan W. Logan, Elisha M. Wachman, William Evan Johnson, Jacob C. Beierle, Emily J Yao, Julia C Kelliher, Carly R. Langan, Melanie M Chen, Camron D. Bryant, Will W. Yen, Richard K Babbs, Qiu T Ruan, Kristyn N. Borrelli, and Alberto Cruz-Martín

Subjects

business.industry, Physiology, Irritability, Pons, Sexual dimorphism, Opioid, Hyperalgesia, medicine, Morphine, Circadian rhythm, Brainstem, medicine.symptom, business, medicine.drug

Abstract

The opioid epidemic led to an increase in the number of Neonatal Opioid Withdrawal Syndrome (NOWS) cases in infants born to opioid-dependent mothers. Hallmark features of NOWS include weight loss, severe irritability, respiratory problems, and sleep fragmentation. Mouse models provide an opportunity to identify brain mechanisms that contribute to NOWS. Neonatal outbred Swiss Webster Cartworth Farms White (CFW) mice were administered morphine (15mg/kg, s.c.) twice daily for postnatal days (P) 1-14, an approximate of the third trimester of human gestation. Male and female mice underwent behavioral testing on P7 and P14 to determine the impact of opioid exposure on anxiety and pain sensitivity. Ultrasonic vocalizations (USVs) and daily body weights were also recorded. Brainstems containing pons and medulla were collected during morphine withdrawal on P14 for RNA-sequencing. Morphine induced weight loss from P2-14, which persisted during adolescence (P21) and adulthood (P50). USVs markedly increased at P7 in females, emerging earlier than males. On P7 and P14, both morphine exposed female and male mice displayed hyperalgesia on the hot plate and tail flick assays, with females having greater hyperalgesia than males. Morphine-exposed mice exhibited increased anxiety-like behavior in the open-field arena at P21. Transcriptome analysis of the brainstem (medulla plus pons), an area implicated in opioid withdrawal and NOWS, identified pathways enriched for noradrenergic signaling in females and males. We also found sex-specific pathways related to mitochondrial function and neurodevelopment in females and circadian entrainment in males. Sex-specific transcriptomic neuroadaptations implicate unique neurobiological mechanisms underlying NOWS-like behaviors.SIGNIFICANCE STATEMENTNeonatal opioid withdrawal syndrome (NOWS) is a poorly understood condition that has both a genetic and environmental component and is thought to be mechanistically distinct from opioid withdrawal in adults. The development of murine models for measuring neurobehavioral responses is critical for informing the neurobiological adaptations underlying NOWS. Using outbred mice that more closely model human genetic variation, we discovered a surprising degree of sexual dimorphism in behavioral timing and severity of NOWS-model behaviors as well as transcriptomic adaptations in brain tissue that together suggest distinct mechanisms and sex-specific therapeutics for reversing withdrawal symptoms and restoring brain function.

Published

2021

3. The Sigma-2 Receptor / Transmembrane protein 97 (σ(2)R/TMEM97) Modulator JVW-1034 Reduces Heavy Alcohol Drinking and Associated Pain States in Male Mice

Author

Luíza dos Reis Cruz, Valentina Sabino, Sean M Tanino, Emily J Yao, Sema G. Quadir, Christian D. Rohl, James J. Sahn, Stephen F. Martin, and Pietro Cottone

Subjects

0301 basic medicine, Male, medicine.medical_specialty, Alcohol Drinking, Sigma-2 receptor, Pain, Alcohol, Alcohol use disorder, Article, 03 medical and health sciences, Cellular and Molecular Neuroscience, chemistry.chemical_compound, Mice, 0302 clinical medicine, Internal medicine, medicine, Animals, Receptors, sigma, Receptor, Pain Measurement, Pharmacology, Analgesics, Ethanol, business.industry, Membrane Proteins, Lipid metabolism, medicine.disease, Mice, Inbred C57BL, 030104 developmental biology, Endocrinology, chemistry, Hyperalgesia, Neuropathic pain, medicine.symptom, business, 030217 neurology & neurosurgery, Locomotion

Abstract

Alcohol Use Disorder (AUD) is a chronic relapsing disorder characterized by compulsive alcohol intake, loss of control over alcohol intake, and a negative emotional state when access to alcohol is prevented. AUD is also closely tied to pain, as repeated alcohol drinking leads to increased pain sensitivity during withdrawal. The sigma-2 receptor, recently identified as transmembrane protein 97 (σ(2)R/TMEM97), is an integral membrane protein involved in cholesterol homeostasis and lipid metabolism. Selective σ(2)R/Tmem97 modulators have been recently shown to relieve mechanical hypersensitivity in animal models of neuropathic pain as well as to attenuate alcohol withdrawal signs in C. elegans and to reduce alcohol drinking in rats, suggesting a potential key role for this protein in alcohol-related behaviors. In this study, we tested the effects of a potent and selective σ(2)R/TMEM97 ligand, JVW-1034, on heavy alcohol drinking and alcohol-induced heightened pain states in mice using an intermittent access model. Administration of JVW-1034 decreased both ethanol intake and preference for ethanol, without affecting water intake, total fluid intake, or food intake. Notably, this effect was specific for alcohol, as JVW-1034 had no effect on sucrose intake. Furthermore, JVW-1034 reduced both thermal hyperalgesia and mechanical hypersensitivity in ethanol withdrawn mice. Our data provide important evidence that modulation of σ(2)R/TMEM97 with small molecules can mediate heavy alcohol drinking as well as chronic alcohol-induced heightened pain sensitivity, thereby identifying a promising novel pharmacological target for AUD and associated pain states.

Published

2020

4. Systems genetic analysis of binge-like eating in a C57BL/6J x DBA/2J-F2 cross

Author

Julia C Kelliher, Megan K. Mulligan, Kimberly P. Luttik, Emily J Yao, Camron D. Bryant, M I Damaj, and Richard K Babbs

Subjects

Genetics, Candidate gene, Inbred strain, Binge eating, Binge-eating disorder, Chromosome 18, medicine, Locus (genetics), Biology, medicine.symptom, Quantitative trait locus, medicine.disease, Chromosome 13

Abstract

ObjectiveBinge eating is a heritable quantitative trait associated with eating disorders (ED) and refers to the rapid consumption of a large quantity of energy-dense food that is associated with loss of control, anxiety, and depression. Binge Eating Disorder is the most common ED in adults in the US; however, the genetic basis is unknown. We previously identified robust mouse inbred strain differences between C57BL/6J and DBA/2J in binge-like eating (BLE) of sweetened palatable food (PF) in an intermittent access, conditioned place preference paradigm.MethodsTo map the genetic basis of BLE, we phenotyped and genotyped 128 C57BL/6J x DBA/2J-F2 mice.ResultsWe identified a quantitative trait locus (QTL) on chromosome 13 influencing progressive changes in body weight across training days (LOD = 5.5; 26-39 cM). We also identified two sex-combined QTLs influencing PF intake on chromosome 5 (LOD = 5.6; 1.5-LOD interval = 21-28 cM) and 6 (LOD = 5.3; 1.5-LOD interval = 50-59 cM). Furthermore, sex-specific analyses revealed that the chromosome 6 locus was driven by males (1.5-LOD interval: 52-59 cM) and identified a female-selective QTL for BLE on chromosome 18 (LOD = 4.1; 1.5-LOD interval: 23-35 cM). Systems genetic analysis of the chromosome 6 locus for BLE using GeneNetwork legacy trait datasets from BXD recombinant inbred strains identified Adipor2 and Plxnd1 as two positional, functional, biological candidate genes.DiscussionWe identified genetic loci influencing BLE. Future studies will phenotype BXD recombinant inbred strains to fine map loci and support candidate gene nomination and validation.

Published

2020

5. The effect of the demyelinating agent cuprizone on binge-like eating of sweetened palatable food in female and male C57BL/6 substrains

Author

William Evan Johnson, Melanie M Chen, Julia C Kelliher, Jeya Anandakumar, Arthurine R. Medeiros, Jacob A Beierle, Camron D. Bryant, Emily J Yao, Richard K Babbs, and Anyaa A. Shah

Subjects

C57BL/6, Male, medicine.medical_specialty, Nerve Tissue Proteins, Striatum, Biology, Article, Myelin, Cuprizone, Mice, Binge-eating disorder, Weight loss, Internal medicine, medicine, Animals, General Psychology, Myelin Sheath, Sex Characteristics, Nutrition and Dietetics, Binge eating, medicine.disease, biology.organism_classification, Corpus Striatum, Myelin basic protein, Mice, Inbred C57BL, Eating disorders, Disease Models, Animal, Endocrinology, medicine.anatomical_structure, biology.protein, Female, medicine.symptom, Binge-Eating Disorder

Abstract

Binge eating is a heritable symptom of eating disorders with an unknown genetic etiology. Rodent models for binge-like eating (BLE) of palatable food permit the study of genetic and biological mechanisms. We previously genetically mapped a coding mutation in Cyfip2 associated with increased BLE of sweetened palatable food in the C57BL/6NJ versus C57BL/6J substrain. The increase in BLE in C57BL/6NJ mice was associated with a decrease in transcription of genes enriched for myelination in the striatum. Here, we tested the hypothesis that decreasing myelin levels with the demyelinating agent cuprizone would enhance BLE. Mice were treated with a 0.3% cuprizone home cage diet for two weeks. Cuprizone induced similar weight loss in both substrains and sexes that recovered within 48 h after removal of cuprizone. Following a three-week recovery period, mice were trained for BLE in an intermittent, limited access procedure. Surprisingly, cuprizone significantly reduced BLE in male but not female C57BL/6NJ mice while having no effect in C57BL/6J mice. Cuprizone also reduced myelin basic protein (MBP) at seven weeks post-cuprizone removal while having no effect on myelin-associated glycoprotein at this time point. C57BL/6NJ mice also showed less MBP than C57BL/6J mice. There were no statistical interactions of Treatment with Sex on MBP levels, indicating that differences in MBP reduction are unlikely to account for sex differences in BLE. To summarize, cuprizone induced an unexpected, significant reduction in BLE in C57BL/6NJ males, which could indicate genotype-dependent sex differences in the biological mechanisms of BLE.

Published

2020

6. The demyelinating agent cuprizone induces a male-specific reduction in binge eating in the binge-prone C57BL/6NJ strain

Author

Arthurine R. Medeiros, Richard K Babbs, Jeya Anandakumar, Jacob A Beierle, Emily J Yao, Julia C Kelliher, Camron D. Bryant, Anyaa A. Shah, and Melanie M Chen

Subjects

0303 health sciences, medicine.medical_specialty, Binge eating, biology, Rodent, Striatum, 3. Good health, Myelin basic protein, Transcriptome, 03 medical and health sciences, Myelin, 0302 clinical medicine, medicine.anatomical_structure, Endocrinology, Weight loss, Internal medicine, biology.animal, CYFIP2, medicine, biology.protein, medicine.symptom, 030217 neurology & neurosurgery, 030304 developmental biology

Abstract

Binge eating (BE) is a heritable symptom of eating disorders with an unknown genetic etiology. Rodent models for BE of palatable food permit the study of genetic and biological mechanisms. We previously used genetic mapping and transcriptome analysis to map a coding mutation in Cyfip2 associated with increased BE in the BE-prone C57BL/6NJ substrain compared to the BE-resistant C57BL/6J substrain. The increase in BE in C57BL/6NJ mice was associated with a decrease in transcription of genes enriched for myelination in the striatum. Here, we tested the hypothesis that decreasing myelin levels with the demyelinating agent cuprizone would enhance BE. Mice were treated with a 0.3% cuprizone home cage diet for two weeks. Following a three-week recovery period, mice were trained for BE in an intermittent, limited access procedure. Cuprizone induced similar weight loss in both substrains and sexes that recovered within 48 h after removal of the cuprizone diet. Surprisingly, cuprizone reduced BE in male but not female C57BL/6NJ mice while having no effect in C57BL/6J mice. Cuprizone also reduced myelin basic protein (MBP) at seven weeks post-cuprizone removal while having no effect on myelin-associated glycoprotein (MAG) at this time point. C57BL/6N mice also showed less MBP than C57BL/6J mice. There were no statistical interactions of Treatment with Sex on MBP levels, indicating that differences in MBP are unlikely to account for sex differences in BE. To summarize, cuprizone induced an unexpected, male-specific reduction in BE which could indicate sex-specific biological mechanisms that depend on genetic background.

Published

2019

7. Sex Differences in Behavioral and Brainstem Transcriptomic Neuroadaptations following Neonatal Opioid Exposure in Outbred Mice

Author

Camron D. Bryant, Alberto Cruz-Martín, Jacob C. Beierle, Qiu T Ruan, Kristyn N. Borrelli, Elisha M. Wachman, Julia L. Scotellaro, William Evan Johnson, Emily J Yao, William W. Yen, Ryan W. Logan, Julia C Kelliher, Rhushikesh A. Phadke, Carly R. Langan, Melanie M Chen, and Richard K Babbs

Subjects

Adult, Male, neonatal abstinence syndrome, Physiology, Irritability, Mice, neonatal opioid withdrawal syndrome, medicine, Animals, Humans, Circadian rhythm, perinatal, Sex Characteristics, business.industry, General Neuroscience, Infant, Newborn, General Medicine, Pons, opiate, Analgesics, Opioid, Opioid, opioid dependence, rodents, Hyperalgesia, Morphine, Female, Disorders of the Nervous System, Brainstem, medicine.symptom, Opiate, Transcriptome, business, Research Article: New Research, Brain Stem, medicine.drug

Abstract

The opioid epidemic led to an increase in the number of Neonatal Opioid Withdrawal Syndrome (NOWS) cases in infants born to opioid-dependent mothers. Hallmark features of NOWS include weight loss, severe irritability, respiratory problems, and sleep fragmentation. Mouse models provide an opportunity to identify brain mechanisms that contribute to NOWS. Neonatal outbred Swiss Webster Cartworth Farms White (CFW) mice were administered morphine (15mg/kg, s.c.) twice daily for postnatal days (P) 1-14, an approximate of the third trimester of human gestation. Female and male mice underwent behavioral testing on P7 and P14 to determine the impact of opioid exposure on anxiety and pain sensitivity. Ultrasonic vocalizations (USVs) and daily body weights were also recorded. Brainstems containing pons and medulla were collected during morphine withdrawal on P14 for RNA-sequencing. Morphine induced weight loss from P2-14, which persisted during adolescence (P21) and adulthood (P50). USVs markedly increased at P7 in females, emerging earlier than males. On P7 and P14, both morphine-exposed female and male mice displayed hyperalgesia on the hot plate and tail flick assays, with females showing greater hyperalgesia than males. Morphine-exposed mice exhibited increased anxiety-like behavior in the open-field arena on P21. Transcriptome analysis of the brainstem, an area implicated in opioid withdrawal and NOWS, identified pathways enriched for noradrenergic signaling in females and males. We also found sex-specific pathways related to mitochondrial function and neurodevelopment in females and circadian entrainment in males. Sex-specific transcriptomic neuroadaptations implicate unique neurobiological mechanisms underlying NOWS-like behaviors. SIGNIFICANCE STATEMENT Neonatal opioid withdrawal syndrome (NOWS) is a poorly understood condition that has both a genetic and environmental component and is thought to be mechanistically distinct from opioid withdrawal in adults. The development of murine models for measuring neurobehavioral responses is critical for informing the neurobiological adaptations underlying NOWS. Using outbred mice that more closely model human genetic variation, we discovered several sex differences in behavioral timing and severity of NOWS-model behaviors as well as transcriptomic adaptations in brain tissue that together suggest distinct mechanisms and sex-specific therapeutics for reversing withdrawal symptoms and restoring brain function.

Published

2021