Author:
Bagher-Ebadian Hassan,Brown Stephen L.,Ghassemi Mohammad M.,Nagaraja Tavarekere N.,Valadie Olivia Grahm,Acharya Prabhu C.,Cabral Glauber,Divine George,Knight Robert A.,Lee Ian Y.,Xu Jun H.,Movsas Benjamin,Chetty Indrin J.,Ewing James R.
Abstract
AbstractWe introduce and validate four adaptive models (AMs) to perform a physiologically based Nested-Model-Selection (NMS) estimation of such microvascular parameters as forward volumetric transfer constant, Ktrans, plasma volume fraction, vp, and extravascular, extracellular space, ve, directly from Dynamic Contrast-Enhanced (DCE) MRI raw information without the need for an Arterial-Input Function (AIF). In sixty-six immune-compromised-RNU rats implanted with human U-251 cancer cells, DCE-MRI studies estimated pharmacokinetic (PK) parameters using a group-averaged radiological AIF and an extended Patlak-based NMS paradigm. One-hundred-ninety features extracted from raw DCE-MRI information were used to construct and validate (nested-cross-validation, NCV) four AMs for estimation of model-based regions and their three PK parameters. An NMS-based a priori knowledge was used to fine-tune the AMs to improve their performance. Compared to the conventional analysis, AMs produced stable maps of vascular parameters and nested-model regions less impacted by AIF-dispersion. The performance (Correlation coefficient and Adjusted R-squared for NCV test cohorts) of the AMs were: 0.914/0.834, 0.825/0.720, 0.938/0.880, and 0.890/0.792 for predictions of nested model regions, vp, Ktrans, and ve, respectively. This study demonstrates an application of AMs that quickens and improves DCE-MRI based quantification of microvasculature properties of tumors and normal tissues relative to conventional approaches.
Funder
Varian Medical Systems
Health Sciences Center - Pilot Grant from Michigan State University and Henry Ford Health System
Dykstra Steel Family -Philanthropic grant
National Cancer Institute
Publisher
Springer Science and Business Media LLC
Cited by
2 articles.
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