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Research ArticleADULT BRAIN
Open Access

Differentiation of Low- and High-Grade Gliomas Using High b-Value Diffusion Imaging with a Non-Gaussian Diffusion Model

Y. Sui, Y. Xiong, J. Jiang, M.M. Karaman, K.L. Xie, W. Zhu and X.J. Zhou
American Journal of Neuroradiology September 2016, 37 (9) 1643-1649; DOI: https://doi.org/10.3174/ajnr.A4836

Abstract

BACKGROUND AND PURPOSE: Imaging-based tumor grading is highly desirable but faces challenges in sensitivity, specificity, and diagnostic accuracy. A recently proposed diffusion imaging method by using a fractional order calculus model offers a set of new parameters to probe not only the diffusion process itself but also intravoxel tissue structures, providing new opportunities for noninvasive tumor grading. This study aimed to demonstrate the feasibility of using the fractional order calculus model to differentiate low- from high-grade gliomas in adult patients and illustrate its improved performance over a conventional diffusion imaging method using ADC (or D).

MATERIALS AND METHODS: Fifty-four adult patients (18–70 years of age) with histology-proved gliomas were enrolled and divided into low-grade (n = 24) and high-grade (n = 30) groups. Multi-b-value diffusion MR imaging was performed with 17 b-values (0–4000 s/mm2) and was analyzed by using a fractional order calculus model. Mean values and SDs of 3 fractional order calculus parameters (D, β, and μ) were calculated from the normal contralateral thalamus (as a control) and the tumors, respectively. On the basis of these values, the low- and high-grade glioma groups were compared by using a Mann-Whitney U test. Receiver operating characteristic analysis was performed to assess the performance of individual parameters and the combination of multiple parameters for low- versus high-grade differentiation.

RESULTS: Each of the 3 fractional order calculus parameters exhibited a statistically higher value (P ≤ .011) in the low-grade than in the high-grade gliomas, whereas there was no difference in the normal contralateral thalamus (P ≥ .706). The receiver operating characteristic analysis showed that β (area under the curve = 0.853) produced a higher area under the curve than D (0.781) or μ (0.703) and offered a sensitivity of 87.5%, specificity of 76.7%, and diagnostic accuracy of 82.1%.

CONCLUSIONS: The study demonstrated the feasibility of using a non-Gaussian fractional order calculus diffusion model to differentiate low- and high-grade gliomas. While all 3 fractional order calculus parameters showed statistically significant differences between the 2 groups, β exhibited a better performance than the other 2 parameters, including ADC (or D).

ABBREVIATIONS:

AUC
area under the curve
FROC
fractional order calculus
ROC
receiver operating characteristic
WHO
World Health Organization

Gliomas are the most common primary brain tumors seen in adults, accounting for approximately one-third to one-half of all cases diagnosed1 and 82% of malignant brain tumors.2 According to the latest classification by the World Health Organization (WHO), gliomas can be divided into 4 grades, spanning a broad spectrum of biologic aggressiveness.3 Accurate grading of gliomas is essential to patient management, not only for selecting the most effective therapy for malignant tumors but also for avoiding unnecessary aggressive treatment for low-grade tumors before malignant transformation, maximizing the quality of life for patients.

MR imaging has been widely used for the initial diagnosis of brain tumors. Its role for tumor grading, however, is less established.4 Conventional MR imaging techniques, including precontrast T1-weighted, T2-weighted, T2-weighted FLAIR, and postcontrast T1-weighted imaging, have limited sensitivity (eg, 72.5%) and specificity (eg, 65.0%) for differentiating low- and high-grade gliomas.4,5 Perfusion imaging (eg, CBV) can improve the sensitivity to >90%,6 but the specificity (eg, 57.5%) remains inadequate and is subject to the choice of CBV threshold values, depending on tumor types.79 With the ability to reveal tumor metabolic changes, MR spectroscopy has also been used for tumor grading.6,10,11 The long data-acquisition times, poor spatial resolution, and magnetic susceptibility perturbations at specific locations (eg, near the sinus and the skull) have hindered its widespread clinical application.6,10,11 Because of the aforementioned challenges and limitations faced by MR imaging/MR spectroscopy, tissue biopsy remains the criterion standard for tumor classification and grading, despite its sampling errors, invasiveness, and inability to evaluate residual tumor tissue after cytoreductive surgery.5

During the past 2 decades, diffusion imaging based on ADC has been evaluated for tumor grading.1214 Despite the potential, several studies indicate that ADC values overlap considerably among different tumor grades in both adult1517 and pediatric patients.14,1820 The ADC values of tumor tissues are obtained by characterizing the diffusion MR imaging signals with a monoexponential function, also known as a Gaussian diffusion model, which assumes that the diffusion process within a voxel is homogeneous.21 Unlike low-grade gliomas, high-grade gliomas have an increased degree of tissue heterogeneity,22,23 which is not adequately captured by ADC. To overcome this limitation, a number of non-Gaussian diffusion models2432 have been developed to extract tissue microstructural information, including tissue heterogeneity, beyond what ADC can provide. The fractional order calculus (FROC) model,26,29 for example, can produce a set of parameters, including diffusion coefficient D (in square millimeters/second), fractional order derivative in space β, and a spatial parameter μ (in micrometers). These parameters provide additional avenues to probing not only the diffusion process itself (D) but also the intravoxel tissue heterogeneity (β) that can be used to improve tumor characterization.26,29,33 In this study, we demonstrate the feasibility of using a new set of parameters from the FROC model to improve MR imaging–based differentiation of low- and high-grade gliomas in adult patients.

Materials and Methods

Patients

The institutional review board of the performing hospital (Tongji Hospital, Wuhan, China) approved this prospective study, and written informed consent was obtained from all participating patients. Fifty-six adult patients (18–70 years of age) with an initial diagnosis of gliomas were recruited and underwent multi-b-value diffusion MR imaging before biopsy or surgical treatment. Two patients were excluded from the analysis due to excessive motion. Among the 54 patients included in the study, histopathology revealed 24 low-grade gliomas, including 1 pilocytic astrocytoma (WHO I), 2 oligodendrogliomas (WHO I and II), 20 astrocytomas (WHO II, predominantly diffuse tumors), 1 ganglioglioma (WHO II), and 30 high-grade gliomas, including 2 anaplastic oligodendrogliomas (WHO III), 10 anaplastic astrocytomas (WHO III), and 18 glioblastoma multiformes (WHO IV), according to the WHO guideline of 2007.3

Image Acquisition

All MR imaging examinations were performed on a 3T scanner (MR750; GE Healthcare, Milwaukee, Wisconsin) with a 32-channel phased-array head coil. The imaging protocol included precontrast T1-weighted FLAIR, T2-weighted FLAIR, T2-weighted PROPELLER, and multi-b-value diffusion-weighted sequences, followed by postcontrast T1-weighted imaging. Susceptibility-weighted imaging was performed on selected patients when the conventional sequences were inadequate to characterize hemorrhage within tumors. In all sequences, an FOV of 24 cm and a section thickness of 5 mm were used. The parameters specific to each anatomic imaging sequence were the following: T1-weighted FLAIR: TR/TE = 1750/32.4 ms, TI = 860 ms, flip angle = 90°, and matrix size = 320 × 320; T2-weighted PROPELLER: TR/TE = 4260/102 ms, echo-train length = 32, and matrix size = 320 × 224; T2-weighted FLAIR: TR/TE = 8400/150 ms, TI = 2100 ms, echo-train length = 26, and matrix size = 256 × 256. The DWIs were produced by using a single-shot echo-planar imaging sequence with 17 b-values (01, 201, 501, 1001, 2001, 4001, 6001, 8001, 10001, 12001, 16001, 20002, 24002, 28002, 32004, 36004 and 40004 s/mm2, in which the subscript denotes the number of averages). At each b-value, a Stejskal-Tanner diffusion gradient was successively applied along the x-, y-, and z-axes to obtain a trace-weighted image to minimize the influence of diffusion anisotropy. The key data acquisition parameters were TR/TE = 3025/94.5 ms, sensitivity encoding acceleration factor = 2, separation between 2 diffusion gradient lobes Δ = 38.6 ms, duration of each diffusion gradient δ = 32.2 ms, matrix size = 160 × 160 (reconstructed with a 256 × 256 matrix), and scan time = 4 minutes 30 seconds.

Image Analysis

Equation 1 was used to fit the intensity (S) of the multi-b-value diffusion images voxel-by-voxel, according to the FROC diffusion model26,29: Embedded Image where S0 is the signal intensity without diffusion weighting, Gd is the diffusion gradient amplitude, and δ and Δ are defined earlier. The β parameter (dimensionless; 0 < β ≤ 1) is a fractional order derivative with respect to space, and μ (in units of micrometers) is a spatial constant to preserve the nominal units of the diffusion coefficient D (in square millimeters/second). In the fitting, D (which reflects the intrinsic diffusivity) was estimated by a monoexponential model by using the data acquired at lower b-values (≤1000 s/mm2), in an attempt to make D equivalent to conventional ADC. After D was determined, β and μ were subsequently obtained from a voxelwise nonlinear fitting by using a Levenberg-Marquardt algorithm34 with all b-values.

ROIs were first placed on the normal contralateral thalamus, which served as an internal control, followed by placing ROIs on the solid region of tumors by 2 neuroradiologists (Y.X. and K.L.X. with 8 and 15 years of clinical experience, respectively) blinded to the histology grades. Guided by the high-resolution anatomic images, regions of hemorrhage, cystic change, and/or necrosis were excluded. In the solid region of tumors, the enhancing components and the nonenhancing (or not-so-obvious enhancing) components were measured and averaged. The ROI-based image analysis was performed with customized software developed in Matlab (MathWorks, Natick, Massachusetts).

Statistical Analysis

The mean and SD of D, β, and μ for each patient were calculated from the normal contralateral thalamus and the tumor ROIs, respectively. On the basis of these values, the low-grade and high-grade glioma groups were compared by using a Mann-Whitney U test with a statistical significance set at P < .05.

To investigate the potential value of using combinations of the FROC parameters (D, β, and μ) for differentiation of low- and high-grade gliomas, we employed a logistic regression model: Embedded Image where a0 is a constant, and a1, a2, and a3 are the regression coefficients for D, β, and μ, respectively. The regression coefficients were estimated by using a maximum-likelihood method.35 Receiver operating characteristic (ROC) analysis was performed to determine the area under the ROC curve (AUC) for assessing the performance of tumor differentiation by using each of the 3 FROC parameters individually and the combination of FROC parameters represented by P0. The best cutoff values in the ROC analysis were determined by using the Youden index. To determine the generalizability of the proposed method, we used a holdout cross-validation algorithm by applying the logistic regression model, Equation 2, on a “training dataset” and a “test dataset” (randomly and equally split from the samples). The Pearson correlation coefficients were then determined between the predicted values and the “true” histopathologic results. All statistical analyses were performed by using SPSS software (IBM, Armonk, New York).

Results

Comparison among Representative Patients in Each Group

Figure 1 shows a set of axial images from a representative patient (oligodendroglioma, WHO I) in the low-grade glioma group, including T2-weighted EPI (Fig 1A), and the FROC maps (color images in Fig 1B–D). The precontrast and postcontrast T1-weighted FLAIR, precontrast T2-weighted FLAIR, and T2-weighted PROPELLER images are available in On-line Fig 1. The D, β, and μ maps (Fig 1B–D, respectively) all exhibited higher values in the tumor than in the surrounding brain parenchyma. Figure 2 shows a set of axial images from a representative patient (glioblastoma multiforme, WHO IV) in the high-grade glioma group by using a layout similar to that of Fig 1. The FROC parameters D, β, and μ (Fig 2B–D, respectively) were considerably lower compared with those in Fig 1B–D, leading to a distinct difference between the high- and low-grade tumors. Additional anatomic images are available (On-line Fig 2).

Fig 1.
Fig 1.

A 41-year-old female patient with a low-grade glioma (oligodendroglioma, WHO grade I). T2-weighted EPI at b=0 with the tumor ROI encircled in green (A), and FROC parameter maps of D (B), β (C), and μ (D) with the tumor ROIs indicated by the black contours (see On-line Fig 1 for a complete set of images, including axial precontrast T1-weighted FLAIR, postcontrast T1-weighted FLAIR, precontrast T2-weighted FLAIR, and precontrast T2WI PROPELLER images). Compared with the patient with glioblastoma multiforme in Fig 2, all 3 FROC parameters exhibited higher values. a.u. indicates arbitrary units. The color scale in (B) is expressed in square micrometers/millisecond.

Fig 2.
Fig 2.

A 38-year-old male patient with a high-grade glioma (glioblastoma multiforme, WHO grade IV). T2-weighted EPI at b=0 with the tumor ROI encircled in green (A) and FROC parameter maps of D (B), β (C), and μ (D) with the tumor ROIs indicated by the black contours (see On-line Fig 2 for a complete set of images including axial precontrast T1-weighted FLAIR, postcontrast T1-weighted FLAIR, T2-weighted FLAIR, and T2-weighted PROPELLER images). Compared with the patient with an oligodendroglioma in Fig 1, all 3 FROC parameters exhibited lower values. a.u. indicates arbitrary units. The color scale in (B) is expressed in square micrometers/millisecond.

Group Comparison Based on the FROC Parameters

After calculating the mean values of the FROC parameters from each tumor ROI, we obtained the means and SDs from each patient group; they are listed in Table 1. Because D is the mathematic equivalent to the conventional ADC (see “Materials and Methods”), an agreement of >96% was observed between D from the FROC model and ADC from a monoexponential fitting by using 2 b-values (b = 0 and 1000 s/mm2), as is typical in clinical studies. Thus, ADC and D are used interchangeably in this study. Comparison of the FROC parameters between the 2 tumor groups is shown in a set of boxplots (Fig 3). Consistent with the representative cases in Figs 1 and 2, the group analysis exhibited statistically higher values (P ≤ .011) in the low-grade than the high-grade gliomas for each of the 3 FROC parameters. In comparison, the internal control by using a normal contralateral thalamus showed no significant differences (P ≥ .706) in the FROC parameters between the 2 patient groups, as summarized in Table 1.

View this table:
Table 1:

FROC parameters of gliomas and normal contralateral thalamus of patients with low-grade and high-grade gliomas

Fig 3.
Fig 3.

Boxplots of FROC parameters D (A), β (B), and μ (C) between the low- (L) and high-grade (H) gliomas. Boxes represent the 25th and 75th percentiles with the median indicated by the middle line in the box. Vertical end bars denote the range of data except for the outliers (ie, values larger than the 75th percentile or smaller than the 25th percentile) represented by a red asterisk. The black asterisk indicates a significant difference (P < .05) between the low- and high-grade gliomas.

ROC Analysis

Figure 4 illustrates the ROC curves using individual FROC parameters for differentiating low- (positive) from high-grade (negative) gliomas. Because D and μ were strongly correlated (see the results in Fig 5), μ was excluded from the logistic regression to avoid overweighting. The constant and regression coefficients of D and β were 19.936, −0.012, and −24.145, respectively (see Equation 2), and the corresponding P0 was used in ROC analysis to represent the combination of D and β. Table 2 summarizes the cutoff values with the corresponding sensitivity, specificity, accuracy, positive and negative predictive values, and asymptotic significance (P value). Although D offered the highest sensitivity (91.7%), its specificity was the lowest (63.3%), leading to moderate accuracy (77.5%). The sensitivity was noticeably improved by β or the combination of β and D, which resulted in the best accuracy (82.1%). The AUC values of the ROC analyses together with their 95% confidence intervals and standard errors are given in Table 3. The parameter β had a higher AUC (0.853) than D (0.781) or μ (0.703), indicating a better performance for glioma differentiation. The combination of D and β did not improve the sensitivity, specificity, accuracy, or AUC compared with β.

Fig 4.
Fig 4.

ROC curves for β (in red), D (in green), and μ (in blue) for differentiating low- and high-grade gliomas. The diagonal line serves as a reference.

Fig 5.
Fig 5.

Scatterplots of D versus μ (A) and D versus β (B) from all patients (the blue diamonds represent low-grade and the red triangles denote high-grade gliomas). A very strong correlation between D and μ (A) (Pearson correlation coefficient r = 0.930; P < .001) and a weaker correlation between D and β (B) (Pearson correlation coefficient r = 0.766; P < .001) are illustrated. B, The dashed lines indicate the cutoff values for D (red), β (green), and the combination of D and β (black; linear equation: β = 0.000497D + 0.798).

View this table:
Table 2:

Cutoff, sensitivity, specificity, diagnostic accuracy, and asymptotic significance (P value) using D, β, μ, and a combination of D and β for differentiating low- (positive) from high-grade (negative) gliomasa

View this table:
Table 3:

AUC values of the ROC analyses with their 95% confidence intervals and standard errors using D, β, μ, and a combination of D and β for differentiating low- (positive) from high-grade (negative) gliomas

The cross-validation analysis showed that the Pearson correlation coefficients between the predicted values and the “true” histopathologic results were 0.529 (P < .01) for the training set and 0.625 (P < .01) for the test set. The significance test for the difference between the 2 correlations (Fisher Z-test) resulted in a P value of .617, suggesting that the training and test datasets did not produce statistically different correlations.

The scatterplots in Fig 5 illustrate the possible (or lack of) correlation among the FROC parameters using all patient data. A very strong correlation between D and μ was observed (Fig 5A) with a Pearson correlation coefficient of r = 0.930 (P < .001). In contrast, a noticeably weaker correlation was seen between D and β (r = 0.766, P < .001). In Fig 5B, the best cutoff values of D and β are indicated by the vertical (red) and the horizontal (green) lines, respectively. The oblique black line in Fig 5B corresponds to the cutoff probability of P0 = .662 for the combination of D and β. The close proximity between the black and green lines is a reflection of the fact that D has a considerably smaller role than β in the equation P0 = exp(19.936 − 0.012 D − 24.145 β) / [1 + exp(19.936 − 0.012D − 24.145 β)].

Discussion

We have investigated the feasibility of using a set of novel FROC diffusion parameters to differentiate low- from high-grade gliomas in adults and demonstrated that D, β, and μ exhibited significant differences between the 2 tumor groups. When used individually, β outperformed the other 2 parameters. These results are important because they demonstrate that new parameters from the FROC diffusion model can contribute positively to glioma differentiation and extend the capability of diffusion imaging beyond conventional ADC.

During the past 2 decades, ADC has been applied to differentiating a number of brain tumors,14,16,18,36 including gliomas. Although the sensitivity of using ADC to detect neoplastic changes has been demonstrated, considerable overlap in ADC values exists between low- and high-grade brain tumors,14,16,17 compromising the specificity and diagnostic accuracy. The suboptimal performance of ADC for tumor grading originates, at least in part, from the use of a Gaussian diffusion model (ie, the monoexponential model), which assumes a homogeneous diffusion process in the tumor, despite overwhelming evidence of tumor heterogeneity.3739 In the presence of heterogeneity, non-Gaussian diffusion models can be more effective in characterizing the complex diffusion process, particularly at high b-values (eg, b ≥ 1500 s/mm2).15,2132,36,40

Like other non-Gaussian diffusion models, the FROC diffusion model provides new parameters complementary to ADC. In the FROC model, correlation between β and intravoxel tissue heterogeneity has been suggested in several studies on phantoms and tissue specimens.26,29,41,42 This correlation is also supported by in vivo studies indicating that tissues with a smaller β-value exhibit a larger degree of intravoxel heterogeneity.22,27,33,43 Tissue heterogeneity is also a contributing factor to the WHO tumor grading system.44 Thus, the β parameter may provide a link between an MR imaging measurement and WHO grades. The lower β values (ie, a high degree of intravoxel heterogeneity) seen in high-grade gliomas (Figs 2 and 3) are consistent with the increased degree of tissue heterogeneity due to the presence of edema, necrosis, hemorrhage, microcalcification, and so forth. This observation is also consistent with a recent study on pediatric brain tumors33,43 in which high-grade tumors showed significantly lower β values compared with their low-grade counterparts. Further studies on well-controlled excised tissues are needed to directly establish and validate the correlation between diffusion heterogeneity suggested by β and structural heterogeneity revealed by histopathology.

Kwee et al27 recently studied high-grade gliomas by using an alternative non-Gaussian diffusion model based on a stretched-exponential formulism.28 Although this model is similar to the FROC model, the stretched-exponential is developed empirically instead of using the fractionalized Fick diffusion equation. The heterogeneity index α in the stretched-exponential model resembles β in this study. The α value for high-grade gliomas was reported to be 0.58 ± 0.08, which is lower than β = 0.77 ± 0.06 in our study. This finding is most likely due to the different diffusion times (Δ) used in these studies.45 Compared with the study of Kwee et al, our study produced a noticeably smaller SD in β because of the relatively large number of b-values used. Although a minimum of 4 b-values is needed to obtain the 3 FROC parameters, a larger number of b-values improves the robustness of the nonlinear fitting, particularly when the SNR is low.

Using all the patient data in this study, we observed a strong linear correlation between D and μ (Fig 5A). Because μ has been related to the dimension of free diffusion space,26 the correlation in Fig 5A reflects the classic relationship between the diffusion rate and mean free length. β was less correlated with D or μ. This weaker correlation can be exploited to improve specificity and diagnostic accuracy because these 2 parameters act more independently. In this study, we have seen evidence suggesting that β is more dominant than D for differentiating low- from high-grade gliomas because the combination of β with D did not improve the performance compared with using β alone. This finding suggests the important role of tumor heterogeneity in various tumor grades.

Our study has several limitations. First, despite the improvement offered by the FROC model in glioma grading, the sensitivity, specificity, and diagnostic accuracy remain suboptimal. An extension of the FROC model to quantifying temporal heterogeneity, as demonstrated recently,42,43 suggests new opportunities to further improve the performance. These non-Gaussian diffusion imaging techniques may eventually help in complementing surgical biopsy in situations in which tissue biopsy is difficult or risky. Second, the number of patients enrolled in the study is moderate. As such, we did not attempt to further distinguishing glioma subtypes or individual grades. Finally, limited by the SNR, the highest b-value attempted in this study was 4000 s/mm2, though an even higher b-value may further improve the reliability of extracting the FROC diffusion parameters.26,29,45

Conclusions

We have demonstrated the feasibility of using high-b-value diffusion MR imaging with the FROC diffusion model to improve differentiation between low- and high-grade gliomas. In particular, the new parameter β offers a higher diagnostic accuracy than using the diffusion coefficient (D or ADC) alone and is the most useful and dominant parameter among the 3 FROC parameters for differentiating glioma grades. Although the focus of this study is on gliomas, the non-Gaussian diffusion imaging approach demonstrated herein is expected to have applications in other disease processes that involve tissue-heterogeneity changes.

Acknowledgments

The authors are grateful to Drs Keith R. Thulborn, Kejia Cai, and Frederick C. Damen for helpful discussions.

Footnotes

  • Yi Sui and Ying Xiong contributed equally and share the first authorship.

  • Disclosures: Yi Sui—UNRELATED: Employment: GE Healthcare, Comments: joined GE Healthcare after the work was done. Xiaohong Joe Zhou—RELATED: Grant: National Institutes of Health grant No. 1S10RR028898*; UNRELATED: Consultancy: Horizon Medical Physics Services, Comments: consulting fees and ownership; Grants/Grants Pending: National Institutes of Health Grant No. 1R21EB023050–01,* AbbVie Pharmaceuticals,* Comments: federal or industrial grant support; Royalties: Elsevier Publishing, Comments: royalty payment for a book I coauthored. *Money paid to the institution.

  • This work was supported, in part, by the National Natural Science Foundation of China (grant number: 30870702), the National Program of the Ministry of Science and Technology of China during the “12th Five-year Plan” (grant No. 2011BAI08B10), and the National Institutes of Health (grant No. 1S10RR028898).

  • Paper previously presented in part at: Annual Meeting of the Radiological Society of North America, November 30 to December 5, 2014; Chicago, Illinois.

Indicates open access to non-subscribers at www.ajnr.org

References

  1. 1.
    2. Ostrom QT,
    3. Gittleman H,
    4. Liao P, et al
    . CBTRUS statistical report: primary brain and central nervous system tumors diagnosed in the United States in 2007–2011. Neuro Oncol 2014;16(suppl 4):iv163 doi:10.1093/neuonc/nou223 pmid:25304271
    FREE Full Text
  2. 2.
    2. Omuro A,
    3. DeAngelis LM
    . Glioblastoma and other malignant gliomas: a clinical review. JAMA 2013;310:184250 doi:10.1001/jama.2013.280319 pmid:24193082
    CrossRefPubMed
  3. 3.
    2. Louis DN,
    3. Ohgaki H,
    4. Wiestler OD, et al
    . The 2007 WHO classification of tumours of the central nervous system. Acta Neuropathol 2007;114:97109 pmid:17618441
    CrossRefPubMed
  4. 4.
    2. Upadhyay N,
    3. Waldman AD
    . Conventional MRI evaluation of gliomas. Br J Radiol 2011;84(Spec No 2):S10711 doi:10.1259/bjr/65711810 pmid:22433821
    Abstract/FREE Full Text
  5. 5.
    2. Law M,
    3. Yang S,
    4. Wang H, et al
    . Glioma grading: sensitivity, specificity, and predictive values of perfusion MR imaging and proton MR spectroscopic imaging compared with conventional MR imaging. AJNR Am J Neuroradiol 2003;24:198998 pmid:14625221
    Abstract/FREE Full Text
  6. 6.
    2. Poussaint TY,
    3. Rodriguez D
    . Advanced neuroimaging of pediatric brain tumors: MR diffusion, MR perfusion, and MR spectroscopy. Neuroimaging Clin N Am 2006;16:16992, ix pmid:16543091
    CrossRefPubMed
  7. 7.
    2. Law M,
    3. Young RJ,
    4. Babb JS, et al
    . Gliomas: predicting time to progression or survival with cerebral blood volume measurements at dynamic susceptibility-weighted contrast-enhanced perfusion MR imaging. Radiology 2008;247:49098 pmid:18349315
    CrossRefPubMed
  8. 8.
    2. Young GS,
    3. Setayesh K
    . Spin-echo echo-planar perfusion MR imaging in the differential diagnosis of solitary enhancing brain lesions: distinguishing solitary metastases from primary glioma. AJNR Am J Neuroradiol 2009;30:57577 doi:10.3174/ajnr.A1239 pmid:19095787
    Abstract/FREE Full Text
  9. 9.
    2. Hirai T,
    3. Murakami R,
    4. Nakamura H, et al
    . Prognostic value of perfusion MR imaging of high-grade astrocytomas: long-term follow-up study. AJNR Am J Neuroradiol 2008;29:150510 pmid:18556364
    Abstract/FREE Full Text
  10. 10.
    2. Schneider JF,
    3. Confort-Gouny S,
    4. Viola A, et al
    . Multiparametric differentiation of posterior fossa tumors in children using diffusion-weighted imaging and short echo-time 1H-MR spectroscopy. J Magn Reson Imaging 2007;26:139098 pmid:17968955
    CrossRefPubMed
  11. 11.
    2. Ishimaru H,
    3. Morikawa M,
    4. Iwanaga S, et al
    . Differentiation between high-grade glioma and metastatic brain tumor using single-voxel proton MR spectroscopy. Eur Radiol 2001;11:178491 pmid:11511902
    CrossRefPubMed
  12. 12.
    2. Kang Y,
    3. Choi SH,
    4. Kim YJ, et al
    . Gliomas: histogram analysis of apparent diffusion coefficient maps with standard- or high-b-value diffusion-weighted MR imaging–correlation with tumor grade. Radiology 2011;261:88290 doi:10.1148/radiol.11110686 pmid:21969667
    CrossRefPubMed
  13. 13.
    2. Raab P,
    3. Hattingen E,
    4. Franz K, et al
    . Cerebral gliomas: diffusional kurtosis imaging analysis of microstructural differences. Radiology 2010;254:87681 doi:10.1148/radiol.09090819 pmid:20089718
    CrossRefPubMed
  14. 14.
    2. Rumboldt Z,
    3. Camacho DL,
    4. Lake D, et al
    . Apparent diffusion coefficients for differentiation of cerebellar tumors in children. AJNR Am J Neuroradiol 2006;27:136269 pmid:16775298
    Abstract/FREE Full Text
  15. 15.
    2. Bian W,
    3. Khayal IS,
    4. Lupo JM, et al
    . Multiparametric characterization of grade 2 glioma subtypes using magnetic resonance spectroscopic, perfusion, and diffusion imaging. Transl Oncol 2009;2:27180 pmid:19956389
    CrossRefPubMed
  16. 16.
    2. Maier SE,
    3. Sun Y,
    4. Mulkern RV
    . Diffusion imaging of brain tumors. NMR Biomed 2010;23:84964 doi:10.1002/nbm.1544 pmid:20886568
    CrossRefPubMed
  17. 17.
    2. Yamasaki F,
    3. Kurisu K,
    4. Satoh K, et al
    . Apparent diffusion coefficient of human brain tumors at MR imaging. Radiology 2005;235:98591 pmid:15833979
    CrossRefPubMed
  18. 18.
    2. Bull JG,
    3. Saunders DE,
    4. Clark CA
    . Discrimination of paediatric brain tumours using apparent diffusion coefficient histograms. Eur Radiol 2012;22:44757 doi:10.1007/s00330-011-2255-67 pmid:21918916
    CrossRefPubMed
  19. 19.
    2. Poretti A,
    3. Meoded A,
    4. Huisman TA
    . Neuroimaging of pediatric posterior fossa tumors including review of the literature. J Magn Reson Imaging 2012;35:3247 doi:10.1002/jmri.22722 pmid:21989968
    CrossRefPubMed
  20. 20.
    2. Porto L,
    3. Jurcoane A,
    4. Schwabe D, et al
    . Differentiation between high and low grade tumours in paediatric patients by using apparent diffusion coefficients. Eur J Paediatr Neurol 2013;17:30207 doi:10.1016/j.ejpn.2012.12.002 pmid:23273960
    CrossRefPubMed
  21. 21.
    2. Le Bihan D
    . The ‘wet mind’: water and functional neuroimaging. Phys Med Biol 2007;52:R5790 pmid:17374909
    CrossRefPubMed
  22. 22.
    2. Pfister S,
    3. Hartmann C,
    4. Korshunov A
    . Histology and molecular pathology of pediatric brain tumors. J Child Neurol 2009;24:137586 doi:10.1177/0883073809339213 pmid:19841426
    Abstract/FREE Full Text
  23. 23.
    2. Gauvain KM,
    3. McKinstry RC,
    4. Mukherjee P, et al
    . Evaluating pediatric brain tumor cellularity with diffusion-tensor imaging. AJR Am J Roentgenol 2001;177:44954 pmid:11461881
    CrossRefPubMed
  24. 24.
    2. Le Bihan D
    . Intravoxel incoherent motion perfusion MR imaging: a wake-up call. Radiology 2008;249:74852 pmid:19011179
    CrossRefPubMed
  25. 25.
    2. Jensen JH,
    3. Helpern JA,
    4. Ramani A, et al
    . Diffusional kurtosis imaging: the quantification of non-Gaussian water diffusion by means of magnetic resonance imaging. Magn Reson Med 2005;53:143240 pmid:15906300
    CrossRefPubMed
  26. 26.
    2. Magin RL,
    3. Abdullah O,
    4. Baleanu D, et al
    . Anomalous diffusion expressed through fractional order differential operators in the Bloch-Torrey equation. J Magn Reson 2008;190:25570 pmid:18065249
    CrossRefPubMed
  27. 27.
    2. Kwee TC,
    3. Galbán CJ,
    4. Tsien C, et al
    . Intravoxel water diffusion heterogeneity imaging of human high-grade gliomas. NMR Biomed 2010;23:17987 doi:10.1002/nbm.1441 pmid:19777501
    CrossRefPubMed
  28. 28.
    2. Bennett KM,
    3. Schmainda KM,
    4. Bennett RT, et al
    . Characterization of continuously distributed cortical water diffusion rates with a stretched-exponential model. Magn Reson Med 2003;50:72734 pmid:14523958
    CrossRefPubMed
  29. 29.
    2. Zhou XJ,
    3. Gao Q,
    4. Abdullah O, et al
    . Studies of anomalous diffusion in the human brain using fractional order calculus. Magn Reson Med 2010;63:56269 doi:10.1002/mrm.22285 pmid:20187164
    CrossRefPubMed
  30. 30.
    2. Ozarslan E,
    3. Basser PJ,
    4. Shepherd TM, et al
    . Observation of anomalous diffusion in excised tissue by characterizing the diffusion-time dependence of the MR signal. J Magn Reson 2006;183:31523 pmid:16962801
    CrossRefPubMed
  31. 31.
    2. Yablonskiy DA,
    3. Bretthorst GL,
    4. Ackerman JJ
    . Statistical model for diffusion attenuated MR signal. Magn Reson Med 2003;50:66469 pmid:14523949
    CrossRefPubMed
  32. 32.
    2. Bar-Shir A,
    3. Cohen Y
    . High b-value q-space diffusion MRS of nerves: structural information and comparison with histological evidence. NMR Biomed 2008;21:16574 pmid:17492659
    CrossRefPubMed
  33. 33.
    2. Sui Y,
    3. Wang H,
    4. Liu G, et al
    . Differentiation of low- and high-grade pediatric brain tumors with high b-value diffusion-weighted MR imaging and a fractional order calculus model. Radiology 2015;277:48996 pmid:26035586
    CrossRefPubMed
  34. 34.
    2. Press WH,
    3. Teukolsky SA,
    4. Vetterling WT, et al
    . Numerical Recipes 3rd Edition: The Art of Scientific Computing. New York: Cambridge University Press; 2007:799806
  35. 35.
    2. Menard SW
    . Applied Logistic Regression Analysis. Thousand Oaks, California: Sage Publications; 2001:1120
  36. 36.
    2. Khayal IS,
    3. McKnight TR,
    4. McGue C, et al
    . Apparent diffusion coefficient and fractional anisotropy of newly diagnosed grade II gliomas. NMR Biomed 2009;22:44955 doi:10.1002/nbm.1357 pmid:19125391
    CrossRefPubMed
  37. 37.
    2. Janiszewska M,
    3. Beca F,
    4. Polyak K
    . Tumor heterogeneity: the Lernaean hydra of oncology? Oncology (Williston Park) 2014;28:78182, 784 pmid:5224477
    PubMed
  38. 38.
    2. Burrell RA,
    3. McGranahan N,
    4. Bartek J, et al
    . The causes and consequences of genetic heterogeneity in cancer evolution. Nature 2013;501:33845 doi:10.1038/nature12625 pmid:24048066
    CrossRefPubMed
  39. 39.
    2. Marusyk A,
    3. Almendro V,
    4. Polyak K
    . Intra-tumour heterogeneity: a looking glass for cancer? Nat Rev Cancer 2012;12:32334 doi:10.1038/nrc3261 pmid:22513401
    CrossRefPubMed
  40. 40.
    2. Grinberg F,
    3. Farrher E,
    4. Kaffanke J, et al
    . Non-Gaussian diffusion in human brain tissue at high b-factors as examined by a combined diffusion kurtosis and biexponential diffusion tensor analysis. Neuroimage 2011;57:1087102 doi:10.1016/j.neuroimage.2011.04.050 pmid:21596141
    CrossRefPubMed
  41. 41.
    2. Magin RL,
    3. Akpa BS,
    4. Neuberger T, et al
    . Fractional order analysis of Sephadex gel structures: NMR measurements reflecting anomalous diffusion. Commun Nonlinear Sci Numer Simul 2011;16:458187 pmid:21804746
    CrossRefPubMed
  42. 42.
    2. Ingo C,
    3. Magin RL,
    4. Colon-Perez L, et al
    . On random walks and entropy in diffusion-weighted magnetic resonance imaging studies of neural tissue. Magn Reson Med 2014;71:61727 doi:10.1002/mrm.24706 pmid:23508765
    CrossRefPubMed
  43. 43.
    2. Karaman MM,
    3. Sui Y,
    4. Wang H, et al
    . Differentiating low- and high-grade pediatric brain tumors using a continuous-time random-walk diffusion model at high b-values. Magn Reson Med 2015 Oct 31. [Epub ahead of print] doi:10.1002/mrm.26012 pmid:26519663
    CrossRefPubMed
  44. 44.
    2. Rosenblum MK
    . The 2007 WHO Classification of Nervous System Tumors: newly recognized members of the mixed glioneuronal group. Brain Pathol 2007;17:30813 pmid:17598823
    CrossRefPubMed
  45. 45.
    2. Zhou XJ,
    3. Gao Q,
    4. Sirinivasan G, et al
    . Dependence of fractional order diffusion model parameters on diffusion time. In: Procedures of the Annual Meeting of the International Society for Magnetic Resonance in Medicine, Honolulu, Hawaii. April 18–24, 2009
  46. 46.
    2. DeLong ER,
    3. DeLong DM,
    4. Clarke-Pearson DL
    . Comparing the areas under two or more correlated receiver operating characteristic curves: a nonparametric approach. Biometrics 1988;44:83745 pmid:3203132
    CrossRefPubMed
  • Received November 25, 2015.
  • Accepted after revision February 22, 2016.
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Differentiation of Low- and High-Grade Gliomas Using High b-Value Diffusion Imaging with a Non-Gaussian Diffusion Model
Y. Sui, Y. Xiong, J. Jiang, M.M. Karaman, K.L. Xie, W. Zhu, X.J. Zhou
American Journal of Neuroradiology Sep 2016, 37 (9) 1643-1649; DOI: 10.3174/ajnr.A4836
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