论文信息 - Evidence for early neurodegeneration in the cervical cord of patients with primary progressive multiple sclerosis.

Evidence for early neurodegeneration in the cervical cord of patients with primary progressive multiple sclerosis.

Spinal neurodegeneration is an important determinant of disability progression in patients with primary progressive multiple sclerosis. Advanced imaging techniques, such as single-voxel (1)H-magnetic resonance spectroscopy and q-space imaging, have increased pathological specificity for neurodegeneration, but are challenging to implement in the spinal cord and have yet to be applied in early primary progressive multiple sclerosis. By combining these imaging techniques with new clinical measures, which reflect spinal cord pathology more closely than conventional clinical tests, we explored the potential for spinal magnetic resonance spectroscopy and q-space imaging to detect early spinal neurodegeneration that may be responsible for clinical disability. Data from 21 patients with primary progressive multiple sclerosis within 6 years of disease onset, and 24 control subjects were analysed. Patients were clinically assessed on grip strength, vibration perception thresholds and postural stability, in addition to the Expanded Disability Status Scale, Nine Hole Peg Test, Timed 25-Foot Walk Test, Multiple Sclerosis Walking Scale-12, and Modified Ashworth Scale. All subjects underwent magnetic resonance spectroscopy and q-space imaging of the cervical cord and conventional brain and spinal magnetic resonance imaging at 3 T. Multivariate analyses and multiple regression models were used to assess the differences in imaging measures between groups and the relationship between magnetic resonance imaging measures and clinical scores, correcting for age, gender, spinal cord cross-sectional area, brain T2 lesion volume, and brain white matter and grey matter volume fractions. Although patients did not show significant cord atrophy when compared with healthy controls, they had significantly lower total N-acetyl-aspartate (mean 4.01 versus 5.31 mmol/l, P = 0.020) and glutamate-glutamine (mean 4.65 versus 5.93 mmol/l, P = 0.043) than controls. Patients showed an increase in q-space imaging-derived indices of perpendicular diffusivity in both the whole cord and major columns compared with controls (P < 0.05 for all indices). Lower total N-acetyl-aspartate was associated with higher disability, as assessed by the Expanded Disability Status Scale (coefficient = -0.41, 0.01 < P < 0.05), Modified Ashworth Scale (coefficient = -3.78, 0.01 < P < 0.05), vibration perception thresholds (coefficient = -4.37, P = 0.021) and postural sway (P < 0.001). Lower glutamate-glutamine predicted increased postural sway (P = 0.017). Increased perpendicular diffusivity in the whole cord and columns was associated with increased scores on the Modified Ashworth Scale, vibration perception thresholds and postural sway (P < 0.05 in all cases). These imaging findings indicate reduced structural integrity of neurons, demyelination, and abnormalities in the glutamatergic pathways in the cervical cord of early primary progressive multiple sclerosis, in the absence of extensive spinal cord atrophy. The observed relationship between imaging measures and disability suggests that early spinal neurodegeneration may underlie clinical impairment, and should be targeted in future clinical trials with neuroprotective agents to prevent the development of progressive disability.

[1] O. Ciccarelli,et al. Spinal cord spectroscopy and diffusion-based tractography to assess acute disability in multiple sclerosis. , 2007, Brain : a journal of neurology.

[2] Jerry L Prince,et al. Spinal cord quantitative MRI discriminates between disability levels in multiple sclerosis , 2013, Neurology.

[3] J. Moffett,et al. N-Acetylaspartate in the CNS: From neurodiagnostics to neurobiology , 2007, Progress in Neurobiology.

[4] A J Thompson,et al. Measuring the impact of MS on walking ability , 2003, Neurology.

[5] Yoram Cohen,et al. q‐Space diffusion MRI (QSI) of the disease progression in the spinal cords of the Long Evans shaker: diffusion time and apparent anisotropy , 2013, NMR in biomedicine.

[6] A. F. Marliani,et al. Quantitative proton magnetic resonance spectroscopy of the human cervical spinal cord at 3 tesla , 2007, Magnetic resonance in medicine.

[7] David H. Miller,et al. Reducing the impact of white matter lesions on automated measures of brain gray and white matter volumes , 2010, Journal of magnetic resonance imaging : JMRI.

[8] B. Meier,et al. Computer Simulations in Magnetic Resonance. An Object-Oriented Programming Approach , 1994 .

[9] David Bonekamp,et al. Regional apparent metabolite concentrations in young adult brain measured by 1H MR spectroscopy at 3 Tesla , 2008, Journal of magnetic resonance imaging : JMRI.

[10] R. Hughes,et al. Electromyography-Controlled Exoskeletal Upper-Limb–Powered Orthosis for Exercise Training After Stroke , 2007, American journal of physical medicine & rehabilitation.

[11] J. Kurtzke. Rating neurologic impairment in multiple sclerosis , 1983, Neurology.

[12] P. Boesiger,et al. Reduced field‐of‐view MRI using outer volume suppression for spinal cord diffusion imaging , 2007, Magnetic resonance in medicine.

[13] David L. Thomas,et al. Reliability of tract-specific q-space imaging metrics in healthy spinal cord , 2011 .

[14] P. Morgan,et al. Measurement of cervical spinal cord cross‐sectional area by MRI using edge detection and partial volume correction , 2005, Journal of magnetic resonance imaging : JMRI.

[15] O. Andersen,et al. Prognostic factors in a multiple sclerosis incidence cohort with twenty-five years of follow-up. , 1993, Brain : a journal of neurology.

[16] Andrew L. Alexander,et al. High b-value and diffusion tensor imaging in a canine model of dysmyelination and brain maturation , 2011, NeuroImage.

[17] David H. Miller,et al. Feasibility of grey matter and white matter segmentation of the upper cervical cord in vivo: A pilot study with application to magnetisation transfer measurements , 2012, NeuroImage.

[18] Norbert Schuff,et al. Age-related glutamate and glutamine concentration changes in normal human brain: 1H MR spectroscopy study at 4 T , 2005, Neurobiology of Aging.

[19] C. Beaulieu,et al. The basis of anisotropic water diffusion in the nervous system – a technical review , 2002, NMR in biomedicine.

[20] David H. Miller,et al. A novel approach with “skeletonised MTR” measures tract‐specific microstructural changes in early primary‐progressive MS , 2014, Human brain mapping.

[21] A. Thompson,et al. Cord atrophy separates early primary progressive and relapsing remitting multiple sclerosis , 2006, Journal of Neurology, Neurosurgery & Psychiatry.

[22] J. Baskerville,et al. The natural history of multiple sclerosis: a geographically based study. 5. The clinical features and natural history of primary progressive multiple sclerosis. , 1999, Brain : a journal of neurology.

[23] R. Rudick,et al. Neurological disability correlates with spinal cord axonal loss and reduced N‐acetyl aspartate in chronic multiple sclerosis patients , 2000, Annals of neurology.

[24] Bennett A Landman,et al. q‐space and conventional diffusion imaging of axon and myelin damage in the rat spinal cord after axotomy , 2010, Magnetic resonance in medicine.

[25] O. Ciccarelli,et al. Spinal cord repair in MS , 2010, Neurology.

[26] T. Perneger. What's wrong with Bonferroni adjustments , 1998, BMJ.

[27] Arvind Caprihan,et al. Use of tissue water as a concentration reference for proton spectroscopic imaging , 2006, Magnetic resonance in medicine.

[28] J. Marsden,et al. Stance instability in spinocerebellar ataxia type 6 , 2013, Movement disorders : official journal of the Movement Disorder Society.

[29] P. Boesiger,et al. Quantitative magnetic resonance spectroscopy in the entire human cervical spinal cord and beyond at 3T , 2008, Magnetic resonance in medicine.

[30] P. W. Stroman,et al. The current state-of-the-art of spinal cord imaging: Applications , 2014, NeuroImage.

[31] O. Ciccarelli,et al. Predicting progression in primary progressive multiple sclerosis: A 10‐year multicenter study , 2008, Annals of neurology.

[32] Y. Cohen,et al. Displacement imaging of spinal cord using q‐space diffusion‐weighted MRI , 2000, Magnetic resonance in medicine.

[33] Eliza M. Gordon-Lipkin,et al. Sensorimotor dysfunction in multiple sclerosis and column-specific magnetization transfer-imaging abnormalities in the spinal cord. , 2009, Brain : a journal of neurology.

[34] D. Leibfritz,et al. Multinuclear NMR studies on the energy metabolism of glial and neuronal cells. , 1993, Developmental neuroscience.

[35] A. F. Marliani,et al. Quantitative Cervical Spinal Cord 3T Proton MR Spectroscopy in Multiple Sclerosis , 2010, American Journal of Neuroradiology.

[36] Y. Cohen,et al. Assignment of the water slow‐diffusing component in the central nervous system using q‐space diffusion MRS: Implications for fiber tract imaging , 2000, Magnetic resonance in medicine.

[37] D. Goodkin,et al. Upper extremity function in multiple sclerosis: improving assessment sensitivity with box-and-block and nine-hole peg tests. , 1988, Archives of physical medicine and rehabilitation.

[38] David H. Miller,et al. Memory in multiple sclerosis is linked to glutamate concentration in grey matter regions , 2014, Journal of Neurology, Neurosurgery & Psychiatry.

[39] S. Provencher. Estimation of metabolite concentrations from localized in vivo proton NMR spectra , 1993, Magnetic resonance in medicine.

[40] A. Thompson,et al. Spinal cord atrophy and disability in multiple sclerosis. A new reproducible and sensitive MRI method with potential to monitor disease progression. , 1996, Brain : a journal of neurology.