Toward magnetic resonance fingerprinting for low-field MR-guided radiation therapy

Nikolai J Mickevicius; Joshua P Kim; Jiwei Zhao; Zachary S Morris; Newton J Hurst Jr; Carri K Glide-Hurst

doi:10.1002/mp.15202

Toward magnetic resonance fingerprinting for low-field MR-guided radiation therapy

Med Phys. 2021 Nov;48(11):6930-6940. doi: 10.1002/mp.15202. Epub 2021 Sep 18.

Authors

Nikolai J Mickevicius¹, Joshua P Kim², Jiwei Zhao³, Zachary S Morris¹, Newton J Hurst Jr¹, Carri K Glide-Hurst¹

Affiliations

¹ Department of Human Oncology, University of Wisconsin-Madison, Madison, Wisconsin, USA.
² Department of Radiation Oncology, Henry Ford Cancer Institute, Detroit, Michigan, USA.
³ Department of Biostatistics and Medical Informatics, University of Wisconsin-Madison, Madison, Wisconsin, USA.

Abstract

Purpose: The acquisition of multiparametric quantitative magnetic resonance imaging (qMRI) is becoming increasingly important for functional characterization of cancer prior to- and throughout the course of radiation therapy. The feasibility of a qMRI method known as magnetic resonance fingerprinting (MRF) for rapid T₁ and T₂ mapping was assessed on a low-field MR-linac system.

Methods: A three-dimensional MRF sequence was implemented on a 0.35T MR-guided radiotherapy system. MRF-derived measurements of T₁ and T₂ were compared to those obtained with gold standard single spin echo methods, and the impacts of the radiofrequency field homogeneity and scan times ranging between 6 and 48 min were analyzed by acquiring between 1 and 8 spokes per time point in a standard quantitative system phantom. The short-term repeatability of MRF was assessed over three measurements taken over a 10-h period. To evaluate transferability, MRF measurements were acquired on two additional MR-guided radiotherapy systems. Preliminary human volunteer studies were performed.

Results: The phantom benchmarking studies showed that MRF is capable of mapping T₁ and T₂ values within 8% and 10% of gold standard measures, respectively, at 0.35T. The coefficient of variation of T₁ and T₂ estimates over three repeated scans was < 5% over a broad range of relaxation times. The T₁ and T₂ times derived using a single-spoke MRF acquisition across three scanners were near unity and mean percent errors in T₁ and T₂ estimates using the same phantom were < 3%. The mean percent differences in T₁ and T₂ as a result of truncating the scan time to 6 min over the large range of relaxation times in the system phantom were 0.65% and 4.05%, respectively.

Conclusions: The technical feasibility and accuracy of MRF on a low-field MR-guided radiation therapy device has been demonstrated. MRF can be used to measure accurate T₁ and T₂ maps in three dimensions from a brief 6-min scan, offering strong potential for efficient and reproducible qMRI for future clinical trials in functional plan adaptation and tumor/normal tissue response assessment.

Keywords: 0.35T; MR fingerprinting; MR-guided radiotherapy; MRF; low-field; quantitative imaging; relaxometry.

MeSH terms

Benchmarking*
Brain
Humans
Image Processing, Computer-Assisted
Magnetic Resonance Imaging*
Magnetic Resonance Spectroscopy
Phantoms, Imaging

Abstract

MeSH terms

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