%0 Generic %A Apostolidis, Leonidas %A Schwarz, Daniel %A Xia, Annie %A Weiler, Markus %A Heckel, Andreas %A Godel, Tim %A Heiland, Sabine %A Schlemmer, Heinz-Peter %A Jäger, Dirk %A Bendszus, Martin %A Bäumer, Philipp %D 2017 %T Dorsal root ganglia hypertrophy as in vivo correlate of oxaliplatin-induced polyneuropathy %U https://plos.figshare.com/articles/dataset/Dorsal_root_ganglia_hypertrophy_as_i_in_vivo_i_correlate_of_oxaliplatin-induced_polyneuropathy/5343430 %R 10.1371/journal.pone.0183845 %2 https://plos.figshare.com/ndownloader/files/9185158 %2 https://plos.figshare.com/ndownloader/files/9185176 %K DRG volume %K sciatic nerves %K RD %K Conclusion OXA-PNP manifests %K oxaliplatin-induced polyneuropathy Purpose %K 3.0 Tesla %K MRN %K nerve lesions %K non-significant decrease %K Dorsal root ganglia hypertrophy %K mm %K tibial nerves %K nT 2 signal %K Results DRG hypertrophy %K T 2 %K neurophysiological examination %K postmortem studies %K resonance neurography %K MD %K imaging protocol %K dorsal root ganglia %K FA %K vivo %K vs %K Quantitative assessment %K report hypertrophy %K AD %K diffusion tensor imaging %K T 2-weighted fat-saturated sequences %K lumbosacral plexus %X

Purpose

To investigate in vivo morphological and functional correlates of oxaliplatin-induced peripheral neuropathy (OXA-PNP) by magnetic resonance neurography (MRN).

Methods

Twenty patients (7 female, 13 male, 58.9±10.0 years) with mild to moderate OXA-PNP and 20 matched controls (8 female, 12 male, 55.7±15.6 years) were prospectively enrolled. All patients underwent a detailed neurophysiological examination prior to neuroimaging. A standardized imaging protocol at 3.0 Tesla included the lumbosacral plexus and both sciatic nerves and their branches using T2-weighted fat-saturated sequences and diffusion tensor imaging. Quantitative assessment included volumetry of the dorsal root ganglia (DRG), sciatic nerve normalized T2 (nT2) signal and caliber, and fractional anisotropy (FA), mean diffusivity (MD), axial (AD) and radial diffusivity (RD). Additional qualitative evaluation of sciatic, peroneal, and tibial nerves evaluated the presence, degree, and distribution of nerve lesions.

Results

DRG hypertrophy in OXA-PNP patients (207.3±47.7mm3 vs. 153.0±47.1mm3 in controls, p = 0.001) was found as significant morphological correlate of the sensory neuronopathy. In contrast, peripheral nerves only exhibited minor morphological alterations qualitatively. Quantitatively, sciatic nerve caliber (27.3±6.7mm2 vs. 27.4±7.4mm2, p = 0.80) and nT2 signal were not significantly changed in patients (1.32±0.22 vs. 1.22±0.26, p = 0.16). AD, RD, and MD showed a non-significant decrease in patients, while FA was unchanged.

Conclusion

OXA-PNP manifests with morphological and functional correlates that can be detected in vivo by MRN. We report hypertrophy of the DRG that stands in contrast to experimental and postmortem studies. DRG volume should be further investigated as a biomarker in other sensory peripheral neuropathies and ganglionopathies.

%I PLOS ONE