Does intravoxel incoherent motion reliably stage hepatic fibrosis, steatosis, and inflammation?

كلية الطب

جامعة أسيوط

Does intravoxel incoherent motion reliably stage hepatic fibrosis, steatosis, and inflammation?

مؤلف البحث
Kumaresan Sandrasegaran ,1 Paul Territo,1 Reem M. Elkady,1,2 Yuning Lin,1,3 Pauley Gasparis,1 Gitasree Borthakur,1 Chen Lin1
تاريخ البحث
قسم البحث
قسم الأشعة التشخيصية
مستند البحث
sand 2017.pdf
مجلة البحث
Abdominal Radiology
المشارك في البحث
Reem Mostafa Mohamed-AliEl Kady
الناشر
springer
تصنيف البحث
hh
عدد البحث
43
موقع البحث
doi: 10.1007/s00261-017-1263-8.
سنة البحث
2017
صفحات البحث
600-606
ملخص البحث

Objective: To investigate the usefulness of intravoxel incoherent motion (IVIM) in determining the severity of hepatic fibrosis, steatosis, and inflammation in patients with chronic liver disease.

Methods: Forty-nine patients who had liver MRI with IVIM sequence and liver biopsy within three months of MRI were enrolled. A reviewer, blinded to histology, placed regions of interest of 1–2 cm2 in the right liver lobe. In addition, the first twenty patients were assessed with a second reviewer. Perfusion fraction (f), pseudodiffusion coefficient (Dfast), true diffusion coefficient (Dslow), and apparent diffusion coefficient (ADC) were calculated from normalized signal intensities that were fitted into a biexponential model. Errors in the model were minimized with global stochastic optimization using Simulated Annealing. ANOVA with post hoc Tukey–Kramer test and multivariate generalized linear model analysis were performed, using histological findings as the gold standard.

Results: The most common etiologies for liver disease were hepatitis C and alcohol, accounting together for 76% (37/ 49) of patients. Low-grade fibrosis (F0, F1), hepatic steatosis, and inflammation were seen in 24% (12/49), 31% (15/49), and 29% (14/49) of patients, respectively. The interobserver correlation was poor for Dfast and Dslow (0.105, 0.173) and moderate for f and ADC (0.461, 0.418). ANOVA showed a strong inverse association between Dfast and liver fibrosis grade (p = 0.001). A weak inverse association was seen between ADC and hepatic steatosis (p = 0.059). Multivariate general linear model revealed that the only significant association between IVIM parameters and pathological features was between Dfast and fibrosis. On ROC curve analysis, Dfast< 23.4 9 10-3 mm2 /s had a sensitivity of 82.8% and a specificity of 64.3% in predicting high-grade fibrosis.

Conclusion: Dfast has the strongest association with hepatic fibrosis but has weak interobserver correlation. IVIM parameters were not significantly associated with hepatic inflammation or steatosis.

Key words: MRI—Hepatic fibrosis—Hepatic steatosis—Hepatitis—IVIM