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Reference values for healthy human myocardium using a T1 mapping methodology: results from the International T1 Multicenter cardiovascular magnetic resonance study
Authors:Darius Dabir  Nicholas Child  Ashwin Kalra  Toby Rogers  Rolf Gebker  Andrew Jabbour  Sven Plein  Chung-Yao Yu  James Otton  Ananth Kidambi  Adam McDiarmid  David Broadbent  David M Higgins  Bernhard Schnackenburg  Lucy Foote  Ciara Cummins  Eike Nagel  Valentina O Puntmann
Institution:.Cardiovascular Imaging Department, King’s College London, The Rayne Institute, 4th Floor Lambeth Wing, St. Thomas’ Hospital Campus, London, SE1 UK ;.German Heart Institute Berlin, Berlin, Germany ;.St Vincent’s Hospital and The Victor Chang Cardiac Research Institute, Sydney, NSW Australia ;.Leeds University, Leeds, UK ;.Philips Healthcare, Guildford, UK ;.Philips Healthcare, Hamburg, Germany
Abstract:

Background

T1 mapping is a robust and highly reproducible application to quantify myocardial relaxation of longitudinal magnetisation. Available T1 mapping methods are presently site and vendor specific, with variable accuracy and precision of T1 values between the systems and sequences. We assessed the transferability of a T1 mapping method and determined the reference values of healthy human myocardium in a multicenter setting.

Methods

Healthy subjects (n = 102; mean age 41 years (range 17–83), male, n = 53 (52%)), with no previous medical history, and normotensive low risk subjects (n=113) referred for clinical cardiovascular magnetic resonance (CMR) were examined. Further inclusion criteria for all were absence of regular medication and subsequently normal findings of routine CMR. All subjects underwent T1 mapping using a uniform imaging set-up (modified Look- Locker inversion recovery, MOLLI, using scheme 3(3)3(3)5)) on 1.5 Tesla (T) and 3 T Philips scanners. Native T1-maps were acquired in a single midventricular short axis slice and repeated 20 minutes following gadobutrol. Reference values were obtained for native T1 and gadolinium-based partition coefficients, λ and extracellular volume fraction (ECV) in a core lab using standardized postprocessing.

Results

In healthy controls, mean native T1 values were 950 ± 21 msec at 1.5 T and 1052 ± 23 at 3 T. λ and ECV values were 0.44 ± 0.06 and 0.25 ± 0.04 at 1.5 T, and 0.44 ± 0.07 and 0.26 ± 0.04 at 3 T, respectively. There were no significant differences between healthy controls and low risk subjects in routine CMR parameters and T1 values. The entire cohort showed no correlation between age, gender and native T1. Cross-center comparisons of mean values showed no significant difference for any of the T1 indices at any field strength. There were considerable regional differences in segmental T1 values. λ and ECV were found to be dose dependent. There was excellent inter- and intraobserver reproducibility for measurement of native septal T1.

Conclusion

We show transferability for a unifying T1 mapping methodology in a multicenter setting. We provide reference ranges for T1 values in healthy human myocardium, which can be applied across participating sites.

Electronic supplementary material

The online version of this article (doi:10.1186/s12968-014-0069-x) contains supplementary material, which is available to authorized users.
Keywords:T1 mapping  Reference values  Multicenter study  MOLLI  Native T1  ECV
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