Feasibility study of computed high b-value diffusion-weighted magnetic resonance imaging for pediatric posterior fossa tumors
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Pediatric Radiology – Original Article
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Feasibility study of computed high b-value diffusion-weighted magnetic resonance imaging for pediatric posterior fossa tumors

1. Acıbadem Mehmet Ali Aydınlar University Faculty of Medicine Atakent Hospital, Department of Radiology, İstanbul, Türkiye
2. Ondokuz Mayıs University Faculty of Medicine Department of Radiology, Samsun, Türkiye
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Received Date: 07.03.2024
Accepted Date: 22.07.2024
Online Date: 02.09.2024
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ABSTRACT

PURPOSE

To evaluate the diagnostic efficacy of computed diffusion-weighted imaging (DWI) in pediatric posterior fossa tumors generated using high b-values.

METHODS

We retrospectively performed our study on 32 pediatric patients who had undergone brain magnetic resonance imaging for a posterior fossa tumor between January 2016 and January 2022. The DWIs were evaluated for each patient by two blinded radiologists. The computed DWI (cDWI) was mathematically derived using a mono-exponential model from images with b = 0 and 1,000 s/mm2 and high b-values ​​of 1,500, 2,000, 3,000, and 5,000 s/mm2. The posterior fossa tumors were divided into two groups, low grade and high grade, and the tumor/thalamus signal intensity (SI) ratios were compared. The Mann–Whitney U test and receiver operating characteristic (ROC) curves were used to compare the diagnostic performance of the acquired DWI (DWI1000), apparent diffusion coefficient (ADC)1000 maps, and cDWI (cDWI1500, cDWI2000, cDWI3000,andcDWI5000).

RESULTS

The comparison of the two tumor groups revealed that the tumor/thalamus SI ratio on the DWI1000 and cDWI (cDWI1500, cDWI2000, cDWI3000,and cDWI5000) was statistically significantly higher in high-grade tumors (P < 0.001). In the ROC curve analysis, higher sensitivity and specificity were detected in the cDWI1500, cDWI2000, cDWI3000, and ADC1000 maps (100%, 90.90%) compared with the DWI1000 (80%, 81.80%). cDWI3000 had the highest area under the curve (AUC) value compared with other parameters (AUC: 0.976).

CONCLUSION

cDWI generated using high b-values ​​was successful in differentiating between low-grade and high-grade posterior fossa tumors without increasing imaging time.

CLINICAL SIGNIFICANCE

cDWI created using high b-values can provide additional information about tumor grade in pediatric posterior fossa tumors without requiring additional imaging time.

Main points

• Compared with images generated using existing b-values, synthetic diffusion-weighted imaging (DWI) with high b-values exhibits greater diffusion effects at a higher signal-to-noise ratio and may be produced without additional scanning time.

• The use of computed DWI (cDWI) with high b-values can help distinguish between low-grade and high-grade tumors without requiring more imaging time.

• For differentiating between low-grade and high-grade posterior fossa tumors, cDWI1500, cDWI2000, and cDWI3000 perform better as diagnostic tools than the acquired DWI1000 and apparent diffusion coefficient1000 maps.

Pediatric brain tumors are the most common childhood solid tumors and are frequently located in the posterior fossa.1, 2 The most common tumors in the posterior fossa in children are medulloblastoma (MB), pilocytic astrocytoma (PA), and ependymoma.3, 4

Although conventional magnetic resonance imaging (MRI) is necessary for the diagnosis of brain tumors and the evaluation of their extent and location, it provides limited information on tumor type and grade.5 Advanced MRI techniques such as diffusion-weighted imaging (DWI) contribute to the differential diagnosis of these tumors. Diffusion restriction and low apparent diffusion coefficient (ADC) values ​​are found more prominently in high-grade tumors with high cellularity than in low-grade tumors.6However, when using standard b-values ​​(b = 1,000 s/mm2), overlaps can be observed in the signal intensity (SI) of high-grade and low-grade tumors.7, 8 When DW images obtained using high b-values (b = 3,000 s/mm2) and standard b-values in the differential diagnosis of high-grade and low-grade gliomas were compared, more successful results were obtained in examinations with high b-values.9 However, at a field strength of 1.5T, higher b-values result in low image quality and a low signal-to-noise ratio (SNR).10, 11 Computed DWI (cDWI) is a synthetic DWI mathematically derived from an acquired DWI with two different b-values.12 Synthetic DWI with high b-values ​​exhibits stronger diffusion effects at a higher SNR than images obtained using existing b-values ​​and can be generated without additional scanning time.13, 14 Studies have demonstrated that cDWI has improved lesion prominence compared with conventional DWI when examining the brain and other body regions.13, 15-19 To the best of our knowledge, no studies have investigated the diagnostic performance of calculated high b-values in pediatric posterior fossa tumors. In the present study, we aimed to evaluate the diagnostic performance of cDWI generated using high b-values ​​in pediatric posterior fossa tumors.

Methods

This study was approved by the Ethics Committee of Ondokuz Mayıs University Faculty of Medicine and was conducted in accordance with the Declaration of Helsinki and Good Clinical Practice guidelines (October 26, 2022, number: 2022/467). The requirement for informed consent was waived.

Patients

This study was conducted retrospectively in a single center after approval from the Ethics Committee, and the report was drafted in accordance with the Standards for Reporting of Diagnostic Accuracy Studies guidelines.20 Between January 2016 and January 2022, 32 pediatric patients who had undergone preoperative brain MRI for posterior fossa tumors and who had not received treatment were included in the study. One patient without a histopathological diagnosis was excluded from the study, and three patients were excluded from the study because artifacts affected the evaluation of the DW images. Finally, 28 patients were included in the study (Figure 1).

Based on the World Health Organization 2021 classification, the patients were divided into two groups: low grade (grade 1 and 2 tumors) and high grade (grade 3 and 4 tumors).21 The mean age of the low-grade tumor group was 7.5 ± 3.9 years (eight girls: 7 ± 3.4 years; five boys: 8.1 ± 4.0 years), and the mean age of the high-grade tumor group was 9.2 ± 4.3 years (six girls: 9.1 ± 5.1 years; nine boys: 9.2 ± 4.5 years).

Magnetic resonance imaging examination

All examinations were performed using 1.5T MRI (Achieva, Philips Healthcare, Best, Netherlands and Magnetom, SIEMENS AG, Erlangen, Germany) devices. All acquisitions were performed in the multiparametric MRI protocol, using T1WI, T2WI, fluid attenuated inversion recovery, dynamic contrast enhanced MRI, and DWI sequences. The acquisition parameters of the DWI are summarized in Table 1. cDWI was created based on images with b = 0 and 1,000 s/mm2, with high b-values ​​of 1,500, 2,000, 3,000, and 5,000 s/mm2, using the mono-exponential model established in a study produced by our team.14

Image analysis

Images were evaluated by two radiologists, with evaluations and measurements performed independently of each other’s assessment and without knowledge of the tumor pathology. Precontrast T2, precontrast T1, and postcontrast T1WIs were analyzed, and tumor boundaries were established while assessing the cystic, hemorrhagic, and necrotic components of the tumor. Using the volume of interest (VOI) approach and ITK-SNAP, measurements were taken from the solid portion of the tumor using DWI.22 Similar measurements were calculated manually using ITK-SNAP software from the acquired DWI1000, cDWI (b = 1,500, 2,000, 3,000, and 5000 s/mm2), and ADC1000 maps. In each patient, the tumor and thalamus SI ratio was calculated by measuring the right thalamus using the VOI method.

Statistical analysis

The IBM SPSS (version 22; IBM, Armonk, NY, USA) software program was used in all calculations. The Shapiro–Wilk test was used in all statistical studies to verify normal distribution. Descriptive statistics of the data are presented as n (%), and for normalized variables, mean ± standard deviation values are provided, whereas for non-normalized variables, the median (min–max) is provided. The Mann–Whitney U test was used for data with normal distribution, comparing the tumor/thalamus SI ratios of high-grade and low-grade tumors on DWI1000, cDWI1500, cDWI2000, cDWI3000, cDWI5000, and ADC1000 maps. The receiver operating characteristic (ROC) curve was calculated for the diagnostic performance of DWI1000, cDWI1500, cDWI2000, cDWI3000, cDWI5000, and ADC1000 maps in differentiating high–low grade tumors with the area under the curve (AUC). Youden’s index was used to select the optimal predicted probability cut-off. The sensitivity and specificity of the DWI and ADC maps were calculated by determining the cut-off value using an ROC curve analysis. Interobserver correlation was evaluated using the intraclass correlation (ICC) coefficient, and κ values were interpreted as follows: κ = 0.00–0.20, slight agreement; κ = 0.21–0.40, fair agreement; κ = 0.41–0.60, moderate agreement; κ = 0.61–0.80, substantial agreement; and κ = 0.81–1.00, almost perfect agreement.23 A P value <0.05 was considered statistically significant.

Results

In total, 13 low-grade [PA = 7 (54%), posterior fossa ependymoma (grade 2) = 3 (23%), low-grade tumor-diffuse astrocytoma = 3 (23%)] and 15 high-grade [MB = 13 (87%), posterior fossa ependymoma (grade 3) = 1 (1%), glioblastoma = 1 (1%)] tumors were included in our study. The tumor/thalamus SI ratios (median and min–max values) for DWI1000, cDWI1500, cDWI2000, cDWI3000, and cDWI5000 in low-grade and high-grade tumors are reported in Table 2. The median (min–max) SI rates were higher in the high-grade tumors than in the low-grade tumors (P < 0.001). When the two tumor groups were compared, the tumor/thalamus SI ratio distributions were more clearly distinguished at higher b-values ​​than at b = 1,000 s/mm2 (Figure 2). In the ICC test, the kappa value was found to be greater than 0.75 for all parameters, with an almost perfect correlation between 0.82 and 0.95 (P < 0.001 for each comparison) (Table 2).

In the ADC1000 maps, median (min–max) ADC values ​​were found to be lower in the high-grade tumors than in the low-grade tumors [low-grade tumor: 1.1 (0.5–1.6) × 10-3 mm2/s; high-grade tumor: 0.8 (0.6–1.0) × 10-3 mm2/s, P < 0.001].

In the ROC curve analysis of the DWI1000, cDWI, and ADC1000 maps, the AUC values (Figure 3) were found to be statistically significant in all parameters. The AUC value was higher in cDWI3000 than in other parameters (AUC: 0.976, P < 0.001). In the ROC curve analysis, when optimal cut-off values ​​were used, higher sensitivity and specificity were detected in cDWI (b = 1,500, 2,000, and 3,000 s/mm2; 100%, 90.9%) than in DWI1000 (80%, 81.80%). The ADC1000 maps (100%, 90.90%) revealed higher sensitivity and specificity than DWI1000 (80%, 81.80%), whereas cDWI5000 (93%, 81.80%) displayed higher sensitivity than DWI1000 but similar specificity (80%, 81.80%) (Table 3). The DWI1000, cDWI, and ADC1000 maps of the two patients diagnosed with juvenile PA and MB are presented in Figures 4 and 5, respectively.

Discussion

In our study, we evaluated the benefits of cDWI created using high b-values ​​for pediatric posterior fossa tumors compared with acquired DWI with standard b-values ​​(b = 1,000 s/mm2). We determined that the ADC1000 maps, DWI1000, cDWI1500, cDWI2000, cDWI3000, and cDWI5000 were effective in distinguishing low–high grade tumors. Notably, our study determined that cDWI3000 had a higher AUC value for diagnostic performance in the ROC curve analysis than other parameters. As demonstrated in Table 2, as b-values ​​increased, the tumor/thalamus SI ratios decreased in low-grade tumors and increased in high-grade tumors. When compared with images using b = 1,000 s/mm2, which are frequently used in standard examinations, we observed that the difference between the two groups increased with the increase in b-value. When compared with normal parenchyma areas, with the increase in b-values, a more significant signal reduction was observed in low-grade tumors (Figure 4) and a more pronounced signal in high-grade tumors (Figure 5). As a result, with the increase in b-values, a more significant contrast difference occurred between tumor and normal tissue. In a study using acquired DW images with b = 1,000 and b = 3,000 s/mm2on 3T MR to compare low-grade and high-grade differentiation in brain tumors, improved diagnostic performance (high sensitivity and specificity) was demonstrated with higher b-values.9In the present study, higher sensitivity and specificity were identified in cDWI1500, cDWI2000, and cDWI3000 ​compared with DWI1000 without increasing acquisition time.

Previous studies on pediatric posterior fossa tumors and gliomas have revealed that high-grade tumors can be effectively distinguished from low-grade tumors with minimal ADC values.8, 24-26 In the present study, the median (min–max) ADC values ​​were found to be lower in high-grade tumors than in low-grade tumors, which is consistent with the literature. In addition, in the present study, in the ROC curve analysis, we determined that cDWI1500, cDWI2000, and cDWI3000 had higher AUC values ​​than ADC1000 maps, although cDWI1500, cDWI2000, and cDWI3000 had similar sensitivity and specificity with ADC1000 maps (Table 3).

In a study comparing cDWI and acquired DWI in patients with ischemic stroke, cDWI1000 and cDWI1500 had higher image quality and lesion prominence than acquired DWI1000. However, in the present study, DWI2000 and cDWI2500 were not found to be an alternative to conventional DWI because of the low lesion detection rates.15 Kamata et al.16 reported that cDWI3000 was more useful than DWI1000 in diagnosing pediatric encephalitis/encephalopathy, and they obtained similar results for acquired DWI3000. In a study investigating synthetic b-values ​​in breast imaging, synthetic images for b1000 and b2000 were obtained and compared with acquired DWI850. The results demonstrated that lesion prominence and image quality were optimal in cDWI1200 and cDWI1800. In breast imaging, improved lesion visibility and background suppression are theoretically expected with increasing b-values.13 Similarly, in a study investigating diagnostic sensitivity in breast cancer, cDWI1500 was found to be more sensitive than acquired DWI1500.27 In addition, Daimiel Naranjo et al.28 revealed that cDWI1200 increased the visibility of the tumor without increasing the scanning time, especially in dense breast tissue. In a study on prostate cancer, cDWI with a high b-value was compared with acquired DWI to detect SI differences between cancer and normal tissue, with cDWI identified as more effective. This study verified that cDWI had a better contrast ratio than real images with a high b-value.29 This study has several limitations. First, it was retrospective and therefore cDWI at high b-values ​​could not be compared with acquired DWI at high b-values. Second, in the literature, measurements have been calculated using region of interest and compared with ADCmin values. We used VOI in our study, which might produce some differences compared with the literature. Third, our study is the first on cDWI in brain tumors, and the results should be verified through further studies.

In conclusion, the present study demonstrated that the diagnostic performance of cDWI1500, cDWI2000, and cDWI3000 is stronger in the differentiation of low-grade and high-grade posterior fossa tumors than that of acquired DWI1000 and ADC1000 maps. Moreover, the SI ratio between tumor and normal tissue became more pronounced with increasing b-values. Thus, cDWI created with high b-values ​​can contribute to the differential diagnosis of low-grade and high-grade tumors without increasing the imaging time.

Conflict of interest disclosure

Meltem Ceyhan Bilgici, MD, is Section Editor in Diagnostic and Interventional Radiology. She had no involvement in the peer-review of this article and had no access to information regarding its peer-review. Other authors have nothing to disclose.

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