Background Cardiac magnetic resonance (CMR) T1 mapping indices, including T1 time, partition coefficient (l), and extracellular volume fraction (ECV) measurements, are a group of emerging noninvasive, quantitative imaging biomarkers that can be used to assess diffuse myocardial fibrosis. Similar to other quantitative MRI measurements, T1 mapping results can be influenced by multiple scanner dependent factors, such as field strength, gradient systems, coil configuration, pulse sequence design, and artifacts related to field inhomogeneity and eddy currents. The purpose of this ex-vivo phantom, multicenter study was to investigate how scanner and field strength variation affected the accuracy and precision of T1 mapping indices. Methods MR studies were performed on two 1.5T (1 Philips, 1 Siemens) and three 3T (2 Philips, 1 Siemens) scanners. Two sets of four phantoms were made to mimic the T1/T2 of pre- and post-contrast myocardium and blood at 1.5T and 3T. T1 mapping using modified look locker with inversion recovery (MOLLI) was performed with simulated heart rate of 40-100bpm using a standard 17 heart beat and a shorter 11 heart beat MOLLI protocol. Inversion recovery spin echo (IR-SE) sequence with TR = 10 sec was acquired during the same session to estimate the reference T1. The phantoms were taken out the magnet after IR-SE and all MOLLI protocols were re-scanned after 10 min to evaluate inter-scan reproducibility. The partition coefficient (l) was estimated by ΔR1myocardium/ΔR1blood. General linear model was used to compare the accuracy and reproducibility of T1 and l across field strength, scanners and protocols. Results The IR-SE T1 values were significantly different across scanners within the same field strength. The average partition coefficient estimated from IR-SE was 43.7% (1.5T) and 46.0% (3T), similar to normal in-vivo values. Accuracy was defined as the percent error between MOLLI and IR-SE, and scan/re-scan reproducibility was reported as the relative percent mean difference between the two back to back MOLLI scans. T1 and l accuracy both varied significantly between different scanners (p<0.0001 for both T1 and l) and across heart rates (p<0.0001 for T1 and p=0.001 for l). However, neither varied across the standard 17HB and 11HB protocols (p=0.177 for T1 and p=0.574 for lamda). Additionally, field strength significantly affected T1 accuracy but not l accuracy (p<0.0001 for T1 vs. p=0.109 for l). In addition to less variability in accuracy, l also had lower percent error overall between scan repetitions, or higher scan/re-scan reproducibility, than T1 measurements (4.59% vs. 5.54%).