Optimized three‐dimensional ultrashort echo time: Magnetic resonance fingerprinting for myelin tissue fraction mapping

Author:

Zhou Zihan12,Li Qing13,Liao Congyu45ORCID,Cao Xiaozhi45,Liang Hui6,Chen Quan45,Pu Run7,Ye Huihui8,Tong Qiqi9ORCID,He Hongjian1210ORCID,Zhong Jianhui111

Affiliation:

1. Center for Brain Imaging Science and Technology, College of Biomedical Engineering and Instrument Science Zhejiang University Hangzhou Zhejiang China

2. Key Laboratory for Biomedical Engineering of Ministry of Education Zhejiang University Hangzhou Zhejiang China

3. MR Collaborations Siemens Healthineers Ltd Shanghai China

4. Department of Radiology Stanford University Stanford California USA

5. Department of Electrical Engineering Stanford University Stanford California USA

6. Department of Neurology, The First Affiliated Hospital Zhejiang University School of Medicine Hangzhou Zhejiang China

7. Neusoft Medical Systems Shanghai China

8. State Key Laboratory of Modern Optical Instrumentation, College of Optical Science and Engineering Zhejiang University Hangzhou Zhejiang China

9. Research Center for Healthcare Data Science Zhejiang Lab Hangzhou Zhejiang China

10. School of Physics Zhejiang University Hangzhou Zhejiang China

11. Department of Imaging Sciences University of Rochester Rochester New York USA

Abstract

AbstractQuantitative assessment of brain myelination has gained attention for both research and diagnosis of neurological diseases. However, conventional pulse sequences cannot directly acquire the myelin‐proton signals due to its extremely short T2 and T2* values. To obtain the myelin‐proton signals, dedicated short T2 acquisition techniques, such as ultrashort echo time (UTE) imaging, have been introduced. However, it remains challenging to isolate the myelin‐proton signals from tissues with longer T2. In this article, we extended our previous two‐dimensional ultrashort echo time magnetic resonance fingerprinting (UTE‐MRF) with dual‐echo acquisition to three dimensional (3D). Given a relatively low proton density (PD) of myelin‐proton, we utilized Cramér–Rao Lower Bound to encode myelin‐proton with the maximal SNR efficiency for optimizing the MR fingerprinting design, in order to improve the sensitivity of the sequence to myelin‐proton. In addition, with a second echo of approximately 3 ms, myelin‐water component can be also captured. A myelin‐tissue (myelin‐proton and myelin‐water) fraction mapping can be thus calculated. The optimized 3D UTE‐MRF with dual‐echo acquisition is tested in simulations, physical phantom and in vivo studies of both healthy subjects and multiple sclerosis patients. The results suggest that the rapidly decayed myelin‐proton and myelin‐water signal can be depicted with UTE signals of our method at clinically relevant resolution (1.8 mm isotropic) in 15 min. With its good sensitivity to myelin loss in multiple sclerosis patients demonstrated, our method for the whole brain myelin‐tissue fraction mapping in clinical friendly scan time has the potential for routine clinical imaging.

Funder

Fundamental Research Funds for the Central Universities

Major Scientific Project of Zhejiang Laboratory

National Natural Science Foundation of China

Publisher

Wiley

Subject

Neurology (clinical),Neurology,Radiology, Nuclear Medicine and imaging,Radiological and Ultrasound Technology,Anatomy

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