grant

Phase resolved ARF optical coherence elastography for intravascular imaging

Organization UNIVERSITY OF CALIFORNIA-IRVINELocation IRVINE, UNITED STATESPosted 15 Aug 2014Deadline 30 Jun 2026
NIHUS FederalResearch GrantFY2023AcousticAcousticsAcute Coronary EventAdipose tissueAlgorithmsAmericanAnimal Disease ModelsAnimal ModelAnimal Models and Related StudiesArterial Fatty StreakArterial Fatty StreaksArteriesArtifactsAtheromaAtheromatousAtheromatous degenerationAtheromatous plaqueBasic ResearchBasic ScienceBenchmarkingBest Practice AnalysisBiomechanicsBlood VesselsBody TissuesCalibrationCardiologyCardiovascularCardiovascular Body SystemCardiovascular DiseasesCardiovascular Organ SystemCardiovascular systemCathetersCause of DeathCessation of lifeCharacteristicsChemicalsClinicalConsultationsDeathDevelopmentDiagnosisDisease ManagementDisease ProgressionDisorder ManagementDistalDomestic RabbitDoppler OCTEarly DiagnosisEchographyEchotomographyElasticityEvaluationFatty TissueFundingHeart VascularHistologicHistologicallyImageImaging ProceduresImaging TechnicsImaging TechniquesImaging technologyLaser ElectromagneticLaser RadiationLasersLengthLesionLightMapsMeasurementMedical DeviceMedical UltrasoundMethodsModalityMonitorMorphologic artifactsMorphologyMotionNIR SpectroscopyNear-Infrared SpectrometryNear-Infrared SpectroscopyOCT TomographyOptical Coherence TomographyOpticsOryctolagus cuniculusOutcomePathogenesisPathologistPenetrationPersonsPhasePhotoradiationPhysiciansProceduresPropertyProtocolProtocols documentationRabbitsRabbits MammalsRadiationResolutionRiskRoentgen RaysRuptureSafetyScanningSchemeSourceSpeedStressSystemTechniquesTechnologyTherapeutic InterventionTimeTissuesUltrasonicUltrasonic ImagingUltrasonicsUltrasonogramUltrasonographyUltrasound DiagnosisUltrasound Medical ImagingUltrasound TestUnited StatesValidationVisualizationWorkX-RadiationX-Ray RadiationX-rayXrayadiposeatherosclerosis plaqueatherosclerotic lesionsatherosclerotic plaqueatherosclerotic plaque rupturebenchmarkbiomechanicalcardiovascular disordercirculatory systemclinical translationclinically translatableconsultationcostdesign and constructdesign and constructiondevelopmentaldiagnostic ultrasoundearly detectionelastic imagingelasticity imagingelastographyhuman errorimage-based methodimagingimaging in vivoimaging methodimaging modalityimaging probeimaging systemimprovedin vivoin vivo imaginginstrumentintervention therapymetermodel of animalmulti-modalitymultimodalityoptic imagingopticaloptical Doppler tomographyoptical coherence Doppler tomographyoptical imagingpig modelpiglet modelplaque lesionporcine modelresolutionssonogramsonographysound measurementswine modeltoolultrasoundultrasound imagingultrasound scanningvalidationsvascularvulnerable plaquewhite adipose tissueyellow adipose tissue
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Full Description

PROJECT SUMMARY
Cardiovascular disease is responsible for 1 in 4 deaths, or 650,000 Americans, every year. It is the

leading cause of death in the United States. Ruptured atherosclerotic plaques are the main cause of acute

coronary events, and it is of lethal consequence. Clinically, early detection of the latent vulnerability of plaques

is the first line of defense against such deadly circumstances, and it relies on visualizing both tissue structural

and biomechanical properties. Accurate characterization of a plaque lesion can facilitate better treatment

management by further our understanding in the disease progression.

The long-term objective of this proposal is to develop a multimodal intravascular imaging system that

combines optical coherence tomography (OCT), ultrasound imaging (US), and shear-wave-based optical

coherence elastography (OCESW) for studying and characterizing plaque vulnerability. The proposed system,

IVOCT-US-OCESW, is built upon the ARF-OCE technology developed in the preceding proposal, with several

significant technical advancements that will further facilitate its clinical translation. The proposed IVOCT-US-

OCESW system unifies the high spatial resolution and extended penetration depth of the 1.7-µm OCT, the broad

imaging depth of US, and the enhanced biomechanical contrast of OCESW. It will provide physicians a powerful

clinical instrument for studying, diagnosing, and managing vulnerable plaques. The multimodal probe only

requires a single disposable guide wire and catheter, thereby reducing the costs, procedure length, associated

risks, and X-ray exposure. Our specific aims are to: 1) Design and construct a multimodal IVOCT-US-OCESW

imaging probe; 2) Develop the IVOCT-US-OCESW system featuring a 4-MHz, 1.7-µm laser; 3) Establish a

scanning protocol and algorithms for biomechanical property quantification; 4) Demonstrate the efficacy of the

proposed system in normal and diseased animal models.

We expect the development of the proposed high-speed, high-penetration-depth, and high-sensitivity

IVOCT-US-OCESW system and probe to have significant impact to both basic science and clinical understanding

of plaque pathogenesis. This will enhance the clinicians’ ability to identify vulnerable lesions, tailor interventional

therapy, and monitor disease progression. More importantly, it will be a powerful tool that provides a quantitative

means to benchmark and evaluate new medical devices and therapies.

Grant Number: 5R01HL125084-12
NIH Institute/Center: NIH

Principal Investigator: ZHONGPING CHEN

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