Fluorescence Lifetime Imaging (FLIm): a method to evaluate colon inflammation in vivo
Project Number5R21DK133773-03
Contact PI/Project LeaderALFONSO-GARCIA, ALBA
Awardee OrganizationUNIVERSITY OF CALIFORNIA AT DAVIS
Description
Abstract Text
PROJECT SUMMARY/ABSTRACT
Inflammatory bowel disease (IBD) is an umbrella term for gastrointestinal (GI) diseases where chronic
inflammation and its sequelae significantly impact a patient’s physical health, quality of life, and healthcare
utilization. Early diagnosis of GI inflammation could prompt earlier medical intervention with a direct impact on
patient’s prognosis and quality of life. There is a need for novel methods capable of detecting early and low-
grade GI inflammation. The goal of this proposal is to demonstrate the feasibility of fluorescence lifetime imaging
(FLIm) for detecting early colorectal inflammation in vivo. Without requiring exogenous labeling agents, FLIm is
sensitive to changes in cellular metabolism, which is altered at the onset of inflammatory processes.
Our specific aims focus on establishing FLIm as a research tool to quantify and monitor inflammation at the
tissue level using the in vivo murine colon as a model. In Aim 1 we will (sub-aim 1.1) fabricate a side-viewing
endoscopic probe for nondestructive, in situ, and in vivo intraluminal imaging of the full length of the colon and
(sub-aim 1.2) show that FLIm is sensitive to epithelial metabolism using wild-type and PPAR-g knockout mice
treated with antibiotic (streptomycin) to generate transient dysbiosis and with 5-ASA to protect against antibiotic
effects. In Aim 2 we will test the relevance of FLIm for detecting early inflammatory changes with a model that
recapitulates aspects of pre-IBD (high-fat diet and antibiotics). Using image processing and statistical analysis,
we will validate the FLIm parameters with histopathology and biochemical assays (H&E, tissue hypoxia,
intracellular lactate, NAD+/NADH, ADP/ATP, PDH activity) performed after necropsy (n = 6 animals/group for
both male and female mice). The broad range of inflammatory responses generated with this study will
demonstrate the sensitivity of FLIm as a research tool for label-free, nondestructive, in vivo intraluminal detecting
and monitoring the host response to GI inflammation.
Results from this research are expected to provide convincing preliminary data for subsequent R01-type
research grant applications that build on the proposed concept. The long-term goal of the PI is to establish FLIm
as a nondestructive and label-free, in situ and in vivo, mesoscopic imaging modality to study 1) pathogenesis
and treatment of GI inflammation over time, 2) the host-microbiota relationship with pharmacological and dietary
changes, and 3) to translate this approach into a clinical tool for in vivo endoscopic imaging of the human GI
tract. We anticipate that the applications of the proposed implementation of FLIm range from early detection of
inflammatory and infectious diseases and cancer to the close monitoring of pharmacological and nutritional
treatments on the GI tract.
Public Health Relevance Statement
PROJECT NARRATIVE
Novel imaging technologies are needed to facilitate the study and visualization of the early and low-grade
gastrointestinal (GI) inflammation. Our proposal aims to establish fluorescence lifetime imaging (FLIm) as a
nondestructive and label-free research tool to visualize and quantify the tissue-level response to microbiome-
mediated inflammation using the in vivo murine colon as a study model. The long-term goal of this research
seeks to translate FLIm as a clinical tool for the early diagnosis of human GI inflammatory diseases.
NIH Spending Category
No NIH Spending Category available.
Project Terms
AbscessAdultAgonistAnimal ModelAnimalsAntibiotic TherapyAntibioticsApplications GrantsAutopsyBiochemicalBiological AssayBiopsyCharacteristicsChronicClinicalColonColonic inflammationColonoscopyColorectalCommunicable DiseasesContrast MediaDataDiagnosisDiameterDiseaseDisease ProgressionDysplasiaEarly DiagnosisEndoscopyEnergy MetabolismEnvironmentEpitheliumExhibitsFemaleFiberFistulaFluorescenceFundingGastrointestinal DiseasesGastrointestinal tract structureGlycolysisGoalsHigh Fat DietHistopathologyHourHumanHypoxiaImageImaging DeviceImaging TechniquesImmune responseIn SituInflammationInflammatoryInflammatory Bowel DiseasesInflammatory ResponseInterventionIntestinesKnockout MiceLabelLaboratoriesLateralLengthLinkMagnetic ResonanceMalignant NeoplasmsMediatingMedicalMetabolicMetabolismMethodsModalityModelingMonitorMotionMusNADHNutritionalOperative Surgical ProceduresOpticsOutcomeOxygenPPAR gammaPathogenesisPatientsPerforationPersonal SatisfactionProcessPropertyQuality of lifeRecording of previous eventsResearchResearch Project GrantsResolutionSideSpeedStatistical Data InterpretationStreptomycinStructureStudy modelsSymptomsTechnologyTestingThickTimeTissuesTranslatingUnited StatesVisualVisualizationWild Type MouseX-Ray Computed Tomographycofactordietarydisease diagnosisdisease modeldysbiosisfluorescence lifetime imaginggastrointestinalgastrointestinal imaginggut dysbiosishealth care service utilizationhost microbiotahuman imagingimage processingimaging detectionimaging modalityimaging probein vivoin vivo fluorescencein vivo imagingintestinal epitheliummalemetermicrobiomemicrobiotanovelnovel imaging technologyoperationoptical fiberoxidationpatient prognosispharmacologicphysical conditioningresponsetooltreatment response
National Institute of Diabetes and Digestive and Kidney Diseases
CFDA Code
847
DUNS Number
047120084
UEI
TX2DAGQPENZ5
Project Start Date
15-September-2022
Project End Date
31-May-2026
Budget Start Date
01-June-2024
Budget End Date
31-May-2026
Project Funding Information for 2024
Total Funding
$193,200
Direct Costs
$120,000
Indirect Costs
$73,200
Year
Funding IC
FY Total Cost by IC
2024
National Institute of Diabetes and Digestive and Kidney Diseases
$193,200
Year
Funding IC
FY Total Cost by IC
Sub Projects
No Sub Projects information available for 5R21DK133773-03
Publications
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The Project Outcomes shown here are displayed verbatim as submitted by the Principal Investigator (PI) for this award. Any opinions, findings, and conclusions or recommendations expressed are those of the PI and do not necessarily reflect the views of the National Institutes of Health. NIH has not endorsed the content below.
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