Abstract

<b>Background:</b> This paper outlines a multiparametric renal MRI acquisition and analysis protocol to allow non-invasive assessment of hemodynamics (renal artery blood flow and perfusion), oxygenation (BOLD T₂^*), and microstructure (diffusion, T₁ mapping). <b>Methods:</b> We use our multiparametric renal MRI protocol to provide (1) a comprehensive set of MRI parameters [renal artery and vein blood flow, perfusion, T₁, T₂^*, diffusion (ADC, D, D^*, f_p), and total kidney volume] in a large cohort of healthy participants (127 participants with mean age of 41 ± 19 years) and show the MR field strength (1.5 T vs. 3 T) dependence of T₁ and T₂^* relaxation times; (2) the repeatability of multiparametric MRI measures in 11 healthy participants; (3) changes in MRI measures in response to hypercapnic and hyperoxic modulations in six healthy participants; and (4) pilot data showing the application of the multiparametric protocol in 11 patients with Chronic Kidney Disease (CKD). <b>Results:</b> Baseline measures were in-line with literature values, and as expected, T₁-values were longer at 3 T compared with 1.5 T, with increased T₁ corticomedullary differentiation at 3 T. Conversely, T₂^* was longer at 1.5 T. Inter-scan coefficients of variation (CoVs) of T₁ mapping and ADC were very good at <2.9%. Intra class correlations (ICCs) were high for cortex perfusion (0.801), cortex and medulla T₁ (0.848 and 0.997 using SE-EPI), and renal artery flow (0.844). In response to hypercapnia, a decrease in cortex T₂^* was observed, whilst no significant effect of hyperoxia on T₂^* was found. In CKD patients, renal artery and vein blood flow, and renal perfusion was lower than for healthy participants. Renal cortex and medulla T₁ was significantly higher in CKD patients compared to healthy participants, with corticomedullary T₁ differentiation reduced in CKD patients compared to healthy participants. No significant difference was found in renal T₂^*. <b>Conclusions:</b> Multiparametric MRI is a powerful technique for the assessment of changes in structure, hemodynamics, and oxygenation in a single scan session. This protocol provides the potential to assess the pathophysiological mechanisms in various etiologies of renal disease, and to assess the efficacy of drug treatments.