Skip Navigation
Contact Us
News + Media
Careers
Giving + Support
Referring MDs
Pediatrics
Site Search
myTuftsMed
Find a Doctor
Patient Care
+ Services
Research
+ Clinical Trials
Training
+ Education
About Tufts
Medical Center
Tufts Medical Center
Pediatrics
I Am A:
Choose One
Patient
Family or Friend of Patient
Referring Physician
Job Seeker
Researcher
Medical Student
Donor
Departments + Services
View All Patient Care + Services
View All Departments
Conditions We Treat
Your Hospital Stay
Visitor Information
Support Services
Paying Your Bill
myTuftsMed Patient Portal
Financial Assistance
Share Your Story
Patient Rights
Nursing
Close
Research Institutes + Departmental Research
View All Research + Clinical Trials
Search Clinical Trials
About Research at Tufts Medical Center
Our Researchers
Careers + Opportunities
Partnerships + Collaborations
Research Offices + Contacts
Close
Residencies + Fellowships
View All Training + Education
Meet Our Residents and Fellows
Training + Education at Tufts MC
Continuing Medical Education
Medical Libraries and Resources
Graduate Medical Education Office
Medical Staff Office
Close
About Tufts Medical Center
Learn All About Tufts Medical Center
Who We Are
Helpful Phone Numbers
History of Tufts Medical Center
Locations + Directions
Share Your Story
Policies + Public Documents
Quality + Safety
Recent Awards + Recognitions
Volunteer Services
Close
Close
Tools
Print
Text
News & Events
Dr. Elizabeth Yen Receives Three-Year K23 Award from NIH
03/13/2023
The award, from the NIH National Institute on Drug Abuse, will fund Dr. Yen’s study “Sex-specific impact of prenatal opioids on brain reward signaling and neonatal feeding regulation.”
The abstract for the award is below:
Although Neonatal Abstinence Syndrome (NAS) is an urgent public health priority, the diagnosis and management of NAS remains challenging. This is primarily due to the multifactorial nature of NAS and the highly subjective measures to assess this condition. Males and females with NAS have distinct risk profiles, yet within the current paradigm they are managed uniformly. The limited understanding of long-term outcomes further compounds the problem and predisposes this population to a myriad of health issues. To address these knowledge gaps, the current proposal expands upon the molecular and behavioral data from our K12-funded pilot study to better understand the impact of prenatal opioid exposure. An early sign of withdrawal in opioid-exposed neonates is difficulty feeding followed by hyperphagia, which often precedes severe NAS and the need for pharmacotherapy. Using saliva collected immediately after birth, we showed higher expression of a key reward gene (DRD2) in opioid-exposed males compared to females. The expression of DRD2 also correlated with the caloric intake in opioid-exposed males who later developed severe NAS and required pharmacotherapy. These transcriptomic-behavioral data indicate that prenatal opioid exposure dysregulates brain reward signaling in a sex-specific manner, resulting in hyperphagia as a reward-seeking behavior that offsets the acute loss of opioids. Furthermore, opioid-exposed neonates have heightened expression of inflammatory genes (IL6, MCP1) that correlate with the expression of DRD2, particularly in females. Expanding on these preliminary results, the current proposal will examine if prenatal opioids dysregulate brain reward signaling and modulate pro-inflammatory pathways with increased sex-specific risks for hyperphagia and associated long-term cardiometabolic disorders. Our overarching goal is to understand changes in sex-specific reward and inflammatory gene expression in opioid-exposed neonates throughout the first year of life. The hypothesis will be tested in two aims: 1) Identify sex-specific effects of prenatal opioids on reward signaling and inflammation, 2) Evaluate effects of prenatal opioids on risk for subsequent cardiometabolic disorders. We will collect serial saliva samples from 56 opioid-exposed and 56 sex- and age-matched non-exposed neonates during the initial hospitalization and then in a subset of infants post hospital discharge up to 1 year of age to evaluate the expression of reward and inflammation genes. Early cardiometabolic risk will be assessed using serum lipid panels at 1 year of age, along with growth and nutritional data. Results will be analyzed by sex. The impact of this proposed project lies in the potential to advance the field with a more comprehensive understanding of the sex-specific impact of prenatal opioid exposure on the developing brain through non-invasive molecular analyses, enabling personalized medicine and longitudinal health monitoring.
Read more on Dr. Yen’s research focus
here
.
