Characterization of focal liver lesions with half-Fourier acquisition single-shot turbo-spin-echo (HASTE) and inversion recovery (IR)-HASTE sequences
✍ Scribed by Yi Tang; Yasuyuki Yamashita; Tomohiro Namimoto; Mutsumasa Takahashi
- Book ID
- 102905598
- Publisher
- John Wiley and Sons
- Year
- 1998
- Tongue
- English
- Weight
- 992 KB
- Volume
- 8
- Category
- Article
- ISSN
- 1053-1807
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✦ Synopsis
Abstract
The half‐Fourier acquisition single‐shot turbo‐spinecho (HASTE) sequence allows for heavily T2‐weighted images, and the inversion recovery (IR)‐HASTE sequence represents the T1 value of the tissue in a very short time. This study was undertaken to determine whether characterizing focal liver lesions can be made by combination with these very fast sequences. Seventy‐four patients (33 cysts, 28 hemangiomas, and 33 malignant solid liver masses [15 metastatic tumors, 14 hepatocellular carcinomas, and 4 cholangiocarcinomasl]) underwent dynamic CT and breath‐hold abdominal MRI using turbo‐spin‐echo (TSE), HASTE, and IR‐HASTE sequences with variable TI values on a 1.5‐T MR unit. The imaging time for each slice was 2 seconds for HASTE imaging and 2 to 4 seconds for IR‐HASTE imaging. Lesion detection and qualitative characterization were evaluated. Quantitative analysis was performed by measuring the contrast‐to‐noise ratios (CNRs) as well as visual analysis. The inversion time (TI) nulling values were also statistically analyzed. All cystic lesions were detected on both TSE and HASTE imagings. For solid lesions, TSE failed to detect one small solid lesion and HASTE sequence failed to detect three lesions. With HASTE sequences, all cysts and hemangiomas were markedly hyperintense in comparison with malignant solid masses. CNRs of hemangiomas or cysts were significantly higher than those of malignant solid masses (P < .01), and there was no overlap. The TI nulling value was 1,100 ± 100 msec for hemangiomas, 1,900 ± 110 msec for cysts, and 740 ± 140 msec for malignant solid masses. There was no overlap between the TI nulling values of hemangiomas and cysts (P < .01). By combining the CNR from the HASTE sequence and the TI nulling value from the IR‐HASTE sequence, complete discrimination among malignant solid masses, hemangiomas, and cysts of the liver could be made. Application of HASTE (representing T2 values) and IR‐HASTE (representing T1 values) sequences provided a rapid and reliable imaging method for characterizing focal liver lesions without the use of contrast medium.
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