Diffusion tensor MRI is sensitive to fibrotic injury in a mouse model of oxalate-induced chronic kidney disease.

Rohan S Virgincar, Aaron K Wong, Kai H Barck, Joshua D Webster, Jeffrey Hung, Patrick Caplazi, Man Kin Choy, William F Forrest, Laura C Bell, Alex J de Crespigny, Debra Dunlap, Charles Jones, Dong Eun Kim, Robby M Weimer, Andrey S Shaw, Hans D Brightbill, Luke Xie
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Abstract

Chronic kidney disease (CKD) is characterized by inflammation and fibrosis in the kidney. Renal biopsies and estimated glomerular filtration rate (eGFR) remain the standard of care, but these endpoints have limitations in detecting the stage, progression, and spatial distribution of fibrotic pathology in the kidney. MRI diffusion tensor imaging (DTI) has emerged as a promising noninvasive technology to evaluate renal fibrosis in vivo both in clinical and preclinical studies. However, these imaging studies have not systematically identified fibrosis particularly deeper in the kidney where biopsy sampling is limited, or completed an extensive analysis of whole organ histology, blood biomarkers, and gene expression to evaluate the relative strengths and weaknesses of MRI for evaluating renal fibrosis. In this study, we performed DTI in the sodium oxalate mouse model of CKD. The DTI parameters fractional anisotropy, apparent diffusion coefficient, and axial diffusivity were compared between the control and oxalate groups with region of interest (ROI) analysis to determine changes in the cortex and medulla. In addition, voxel-based analysis (VBA) was implemented to systematically identify local regions of injury over the whole kidney. DTI parameters were found to be significantly different in the medulla by both ROI analysis and VBA, which also spatially matched with collagen III immunohistochemistry (IHC). The DTI parameters in this medullary region exhibited moderate to strong correlations with histology, blood biomarkers, hydroxyproline, and gene expression. Our results thus highlight the sensitivity of DTI to the heterogeneity of renal fibrosis and importance of whole kidney noninvasive imaging.NEW & NOTEWORTHY Chronic kidney disease (CKD) can be characterized by inflammation and fibrosis of the kidney. Although standard of care methods have been limited in scope, safety, and spatial distribution, MRI diffusion tensor imaging (DTI) has emerged as a promising noninvasive technology to evaluate renal fibrosis in vivo. In this study, we performed DTI in an oxalate mouse model of CKD to systematically identify local kidney injury. DTI parameters strongly correlated with histology, blood biomarkers, hydroxyproline, and gene expression.

弥散张量核磁共振成像对草酸盐诱导的慢性肾病小鼠模型中的纤维损伤很敏感。
慢性肾脏病(CKD)以肾脏炎症和纤维化为特征。肾活检和估计肾小球滤过率(eGFR)仍然是治疗的标准,但这些终点在检测肾脏纤维化病变的阶段、进展和空间分布方面存在局限性。在临床和临床前研究中,核磁共振弥散张量成像(DTI)已成为评估体内肾脏纤维化的一种很有前途的非侵入性技术。然而,这些成像研究并没有系统地确定纤维化,尤其是在活检取样有限的肾脏深部,也没有完成对整个器官组织学、血液生物标记物和基因表达的广泛分析,以评估 MRI 在评估肾脏纤维化方面的相对优势和劣势。在本研究中,我们在草酸钠小鼠 CKD 模型中进行了 DTI 分析。通过感兴趣区(ROI)分析比较了对照组和草酸盐组的 DTI 参数分数各向异性、表观扩散系数和轴向扩散率,以确定皮质和髓质的变化。此外,还实施了基于体素的分析(VBA),以系统识别整个肾脏的局部损伤区域。通过 ROI 分析和 VBA 发现,髓质的 DTI 参数有显著差异,这也与胶原 III IHC 的空间匹配。该髓质区域的 DTI 参数与组织学、血液生物标记物、羟脯氨酸和基因表达呈中度至高度相关。因此,我们的研究结果凸显了 DTI 对肾脏纤维化异质性的敏感性以及全肾无创成像的重要性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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