Laura Marianne Huckins, PhD
Cards
About
Research
Overview
Research Areas of Focus:
Transcriptomic Imputation
Transcriptomic Imputation approaches use eQTL reference data to create predictors of gene expression in specific tissues. These models may then be applied to genotype data to calculate predicted genetically regulated gene expression (GREX), and to test for associations between GREX and a trait of interest. These models may also be applied to summary statistics to translate GWAS data into GREX associations.
The Huckins Lab develops and applies these models; in particular, we focus on (1) improvement of statistical methodology underlying model creation; (2) probing spatio-temporal specificity of these models; (3) expansion to multi-omic prediction. We apply these models to psychiatric traits and disorders.
Disorders of Interest
The Huckins Lab focuses on understudied psychiatric disorders. In particular, we are interested in disorders affecting women, children, and vulnerable populations.
Eating Disorders
Eating Disorders are highly complex, dangerous, and understudied neuropsychiatric disorders. EDs have significant heritability (50-80%), in line with other psychiatric disorders, and have the highest mortality rates of any psychiatric disorders. Despite this, ED research receives ~$1 for every $70 spent on other major mental disorders.
EDs affect all genders, races, ethnic groups, and people of all ages. EDs may disproportionately affect members of the LGBTQIA community (16% of transgender college students report having an eating disorder, as do 3.5% of sexual minority women, and 2.1% of sexual minority men) and active duty personnel (~9% of women and ~7.5% of men have or develop an eating disorder during active duty).
The Huckins Lab is dedicated to addressing this dearth of ED research. Dr. Huckins has been involved in ED research since her PhD- including work on the first GWAS for Anorexia Nervosa, the first study of low-frequency variation, and the first study of transcriptomic imputation. Our work focuses on elucidating the tissues and systems involved in EDs, and studying multi-omic involvement, including gene expression, histone modifications, and microbiome involvement.
Post-traumatic Stress Disorder (PTSD)
Following a life-threatening traumatic exposure, about 10% of those exposed are at considerable risk for developing posttraumatic stress disorder (PTSD), a severe and disabling syndrome characterized by uncontrollable intrusive memories, nightmares, avoidance behaviours, and hyperarousal in addition to impaired cognition and negative emotion symptoms.
The Huckins Lab is interested in understanding the genetic basis of susceptibility/resilience to PTSD following trauma. A key focus of our group is understanding differing genetic aetiologies and risk factors for PTSD according to trauma type, in particular sexual assault.
Our analyses include a range of genetic, genomic, and multi-omic investigations into (1) predicting PTSD trajectory; (2) identifying shared and distinct genetic aetiologies for military and civilian PTSD; (3) identifying biological systems involved in PTSD using multi-omic imputation.
Publications
2025
Implications of gene × environment interactions in post-traumatic stress disorder risk and treatment
Seah C, Sidamon-Eristoff A, Huckins L, Brennand K. Implications of gene × environment interactions in post-traumatic stress disorder risk and treatment. Journal Of Clinical Investigation 2025, 135: e185102. PMID: 40026250, PMCID: PMC11870735, DOI: 10.1172/jci185102.Peer-Reviewed Original ResearchConceptsPost-traumatic stress disorderGene x environment interactionsGenetic component of riskLimitations of genetic studiesTreating post-traumatic stress disorderExposure to traumatic stressPost-traumatic stress disorder riskInteraction of traumaGenetic screeningGenetic studiesGenetic componentEnvironment interactionMolecular mechanismsStress disorderPTSD riskTraumatic exposureTraumatic stressTraumatic experiencesDisorder riskGenetic factorsNovel therapeuticsBiological mechanismsGWASGeneral populationGenesHarnessing precision nutrition to individualize weight restoration in anorexia nervosa
Rodriguez I, Huckins L, Bulik C, Xu J, Igudesman D. Harnessing precision nutrition to individualize weight restoration in anorexia nervosa. Journal Of Eating Disorders 2025, 13: 29. PMID: 39962541, PMCID: PMC11834214, DOI: 10.1186/s40337-025-01209-x.Peer-Reviewed Original ResearchWeight restorationPrecision nutritionAnorexia nervosaGut microbiotaIndividualized nutrition therapyPsychiatric comorbiditiesHabitual lifestyle behaviorsPrecision nutrition approachesDuration of illnessRestore microbial diversityNutrition therapySevere psychiatric disordersNutrition prescriptionKeystone taxaDietary interventionGenetic markersMicrobial diversityWeight outcomesMetabolic profileEffective treatmentDietary planNutritional approachFecal energy lossPatient recoveryMortality rateGenetics of Anorexia Nervosa Translation to Future Personalized Therapies
Xu J, Igudesman D, Huckins L, Bulik C. Genetics of Anorexia Nervosa Translation to Future Personalized Therapies. Psychiatric Clinics Of North America 2025 DOI: 10.1016/j.psc.2025.01.007.Peer-Reviewed Original Research
2024
Evaluation of imputation performance of multiple reference panels in a Pakistani population
Xu J, Liu D, Hassan A, Genovese G, Cote A, Fennessy B, Cheng E, Charney A, Knowles J, Ayub M, Peterson R, Bigdeli T, Huckins L. Evaluation of imputation performance of multiple reference panels in a Pakistani population. Human Genetics And Genomics Advances 2024, 6: 100395. PMID: 39696820, PMCID: PMC11759560, DOI: 10.1016/j.xhgg.2024.100395.Peer-Reviewed Original ResearchGenome-wide association studiesReference panelImputation accuracyMultiple reference panelsPakistani individualsGenotype imputationAssociation studiesGenotype dataAncestry compositionEuropean individualsSample sizeTOPMedDiverse populationsPakistani populationImputationGenomeAncestryIndividualsGenotypesPopulationVariantsFuture panelsAuthor Correction: Modeling gene × environment interactions in PTSD using human neurons reveals diagnosis-specific glucocorticoid-induced gene expression
Seah C, Breen M, Rusielewicz T, Bader H, Xu C, Hunter C, McCarthy B, Deans P, Chattopadhyay M, Goldberg J, Dobariya S, Desarnaud F, Makotkine I, Flory J, Bierer L, Staniskyte M, Noggle S, Huckins L, Paull D, Brennand K, Yehuda R. Author Correction: Modeling gene × environment interactions in PTSD using human neurons reveals diagnosis-specific glucocorticoid-induced gene expression. Nature Neuroscience 2024, 28: 214-214. PMID: 39633181, PMCID: PMC11706769, DOI: 10.1038/s41593-024-01854-6.Peer-Reviewed Original ResearchChronic overlapping pain conditions and nociplastic pain
Johnston K, Signer R, Huckins L. Chronic overlapping pain conditions and nociplastic pain. Human Genetics And Genomics Advances 2024, 6: 100381. PMID: 39497418, PMCID: PMC11617767, DOI: 10.1016/j.xhgg.2024.100381.Peer-Reviewed Original ResearchGenome wide association studiesTranscriptome-wide associationChronic overlapping pain conditionsTissue enrichment analysisSingle nucleotide polymorphismsEnrichment analysisNociplastic painPain conditionsIndependent single nucleotide polymorphismsMultisite chronic painGene set enrichment analysisSNP heritabilityUnique genesNeuropathic pain phenotypesAssociation studiesPolygenic traitChronic pain conditionsGene setsNucleotide polymorphismsMetabolic traitsHeritable traitGenetic overlapPain phenotypesPain descriptorsPain experience42. STRESS EXPOSURE DYNAMICALLY REGULATES EQTL ACTIVITY IN THE POST-MORTEM BRAIN AND IN HIPSC-DERIVED NEURONS
Seah C, Signer R, Young H, Hicks E, Rusielewicz T, Bader H, Xu C, Breen M, Paull D, Yehuda R, Girgenti M, Brennand K, Huckins L. 42. STRESS EXPOSURE DYNAMICALLY REGULATES EQTL ACTIVITY IN THE POST-MORTEM BRAIN AND IN HIPSC-DERIVED NEURONS. European Neuropsychopharmacology 2024, 87: 71-72. DOI: 10.1016/j.euroneuro.2024.08.156.Peer-Reviewed Original ResearchPost-mortem brainsTranscription factor binding sitesAbsence of cellular stressCombat-exposed veteransFactor binding sitesImpact gene expressionBinding sitesGR binding sitesPositive regulatory activityMotif enrichmentSequence readsCRISPRi screenOpen chromatinFunctional annotationBrain regionsTraumatic stressCRISPR screensEQTLTraumatic experiencesLeading locusPTSDPerturbed genesRegulatory architectureTranscriptomic activityTranscriptomic responseW22. EATING DISORDERS OVER THE WEIGHT SPECTRUM: DISSECTING GENETIC DIFFERENCES OF EATING DISORDERS, THINNESS, AND OBESITY
Xu J, Signer R, Hicks E, Johnston K, Termorshuizen J, Group P, Bulik C, Huckins L. W22. EATING DISORDERS OVER THE WEIGHT SPECTRUM: DISSECTING GENETIC DIFFERENCES OF EATING DISORDERS, THINNESS, AND OBESITY. European Neuropsychopharmacology 2024, 87: 112. DOI: 10.1016/j.euroneuro.2024.08.231.Peer-Reviewed Original ResearchTissue-specific mannerSignificant genesCC-GWASGenetic distanceConstitutional thinnessIdentified multiple risk variantsBonferroni significanceGenome-wide lociGenome-wide significanceMultiple risk variantsConcordant effect directionsBinge eatingClinical differencesEating disordersGTEx v8S-PrediXcanAN-BGene associationsGenetic relationshipsRisk variantsRisk genesWeight-related traitsGenetic etiologyGenesDifferential expression23. GENOME-WIDE ASSOCIATION STUDIES OF BINGE-EATING BEHAVIOUR AND ANOREXIA NERVOSA YIELD INSIGHTS INTO THE UNIQUE AND SHARED BIOLOGY OF EATING DISORDER PHENOTYPES
Huckins L, Termorshuizen J, Davies H, Lee S, Johnson J, Munn-Chernoff M, Thornton L, Källberg J, Bulik C, Breen G, Coleman J. 23. GENOME-WIDE ASSOCIATION STUDIES OF BINGE-EATING BEHAVIOUR AND ANOREXIA NERVOSA YIELD INSIGHTS INTO THE UNIQUE AND SHARED BIOLOGY OF EATING DISORDER PHENOTYPES. European Neuropsychopharmacology 2024, 87: 60. DOI: 10.1016/j.euroneuro.2024.08.137.Peer-Reviewed Original ResearchGenome-wide association studiesIdentification of novel lociGenome-wide association study meta-analysisGenetic correlationsEating Disorders Working GroupBinge-eating behaviorNovel lociGenome-wideGenomic lociAssociation studiesLociGenetic componentEating disorder phenotypesPhenotypeEarly onset obesityBE phenotypeSevere early onset obesityDisorder phenotypesTrans-diagnosticAN subtypesAN-BPAN-RAN-R.Eating disordersBinge-eating/purgingOral Contraceptives and the Risk of Psychiatric Side Effects: A Review
Ciarcia J, Huckins L. Oral Contraceptives and the Risk of Psychiatric Side Effects: A Review. Complex Psychiatry 2024, 10: 36-44. PMID: 39148498, PMCID: PMC11324216, DOI: 10.1159/000539515.Peer-Reviewed Original ResearchMood-related side effectsPsychiatric side effectsPsychiatric riskOral contraceptivesSide effectsSymptoms of depressionPrescription psychotropic medicationsOC usersMood side effectsSide effects of oral contraceptivesEffects of oral contraceptivesMood symptomsRisks of oral contraceptivesOC treatmentPsychotropic medicationsMood improvementPsychiatric disordersEating disordersProgestin-only pillsSubgroups of usersPlacebo usersRandomized controlled trialsCombination pillMoodClinical significance
Academic Achievements & Community Involvement
News & Links
Media
News
- December 07, 2023
VA/Yale Researchers Lead Multi-ancestry Study of Genetics of Problematic Alcohol Use
- September 20, 2023
Huckins to Receive 2023 International Society of Psychiatric Genetics Theodore Reich Early Career Award
- February 26, 2023
Addy, Huckins, Petrakis Elected to Connecticut Academy of Science & Engineering
- February 23, 2023Source: Connecticut Academy of Science and Engineering
Connecticut Academy of Science and Engineering Elects 35 New Members in 2023