Wallerian degeneration in cervical spinal cord tracts is commonly seen in routine T2-weighted MRI after traumatic spinal cord injury and is associated with impairment in a retrospective study

This retrospective study included patients with tSCI that underwent MRI of the cervical spine from January 2004 until August 2019 and was approved by the local ethics committee. A total of 61 patients with tSCI were initially included with at least 3 follow-up MRI examinations (time interval between trauma and most recent MRI examination being at least 1 year) who were referred to our institution for rehabilitation. Scoring of trauma severity was done according to American Spinal Injury Association Impairment Scale (AIS) which is based on clinical examination according to the International Standards for Neurological Classification of Spinal Cord Injury [16]. These clinical and additional neurophysiological assessments by sensory (SEP) and motor evoked potentials (MEP) were performed between 2 and 20 days after trauma.

The study design is presented in Fig. 1. Cervical spine MRIs were evaluated for T2w signal hyperintensity in the anatomical region of specific tracts, consistent with WD. Signal intensity change was assessed in the anatomical region of the dorsal column (DC), the lateral corticospinal tract (CS), and the lateral spinothalamic tract (ST) [17‐19]. T2w signal hyperintensity was evaluated in at least three successive MRI examinations after trauma. If a specific hyperintense signal was visible in one or more MRI examinations, the signal was evaluated as positive, even if a subsequent MRI was read negative for signal change in the same location. When no signal change was visible in all available MRI examinations for at least 1 year, this patient was evaluated negative for WD.

Most patients underwent MRI of the cervical spine on a 3T Magnetom Skyra fit system (Siemens Healthineers). Image evaluation was performed on sagittal and axial T2w turbo spin-echo images. Following settings were used: axial: repetition time (TR) 5510 ms, echo time (TE) 93 ms, echo train length (ETL) 16, field of view: (FOV) 160 × 160 mm, matrix 320 × 320, slice thickness 3 mm, spacing 3.6 mm. Sagittal: repetition time (TR) 3760 ms, echo time (TE) 87 ms, echo train length (ETL) 17, field of view (FOV) 220 × 220 mm, matrix 384 × 384, slice thickness 2.5 mm, spacing 2.75 mm. In cases with significant metal artifacts or before the 3T system was installed, imaging was done on a 1.5T Avanto fit system (Siemens Healthineers), using the following settings: Axial: repetition time (TR) 3390 ms, echo time (TE) 112 ms, echo train length (ETL) 15, field of view (FOV) 200 × 200 mm, matrix 320 × 320, slice thickness 3 mm, spacing 3.5 mm. Sagittal: repetition time (TR) 3440 ms, echo time (TE) 107 ms, echo train length (ETL) 16, field of view (FOV) 240 × 240mm, matrix 512 × 512, slice thickness 2.5 mm, spacing 2.75 mm. In both systems, a standard radiofrequency neck coil (20 channels) is used. Our 1.5T and 3T systems received a technical update (Verio to Skyra fit and Avanto to Avanto fit) in 2013. Systems originally were installed in 2004 (Avanto) and 2010 (Verio).

Axial T2w images had to cover at least two segments above and below the injury. Two fellowship trained radiologists with 6 and 7 years of experience in radiology and at least 1 year exclusively in neuroradiology evaluated all patients on our institution’s Merlin PACS (Phoenix-PACS GmbH).

First, in the trauma MRI, the level of the injury and sagittal expansion were evaluated on sagittal T2w images; clinical information was withheld from the readers. Transverse cord involvement was evaluated, using the Brain and Spinal Injury Center score (BASIC) grade 0–4. Grade 0: No appreciable cord signal abnormality; grade 1: Intramedullary T2w hyperintensity is approximately confined to central gray matter; grade 2: Intramedullary T2w hyperintensity extends beyond expected gray matter margin to involve spinal white matter, but does not involve entire transverse extent of the spinal cord; grade 3: intramedullary T2w hyperintensity involves entire transverse extent of spinal cord; grade 4: Grade 3 injury plus discrete T2w hypointense foci, consistent with macrohemorrhage [20].

In all available follow-up examinations, tract-specific signal change was evaluated without any clinical information. First, the level of the injury was determined on sagittal T2w. Evaluation of the axial T2w consisted of evaluation for (1) T2w hyperintense signal change in the region of the dorsal column (DC) one level above the level of the injury, (2) T2w hyperintense signal change in the region of the lateral corticospinal tract (CS) one level below the level of the injury, and (3) T2w hyperintense change in the region of the lateral spinothalamic tract (ST) one above the level of the injury. Signal abnormality was read as present or absent. Examples for signal abnormality in each tract are shown in Fig. 2.

Severity assessment of spinal cord injuries (SCI) was performed by trained rehabilitation specialists. Classification was performed based on standardized assessment of segmental motor and sensory testing according to ISNCSCI. Clinical assessments were done twice, 0 to 15 days after trauma and 16 to 40 days after trauma (stage very acute and acute 1 follow-up according to the European Multicenter Study about Spinal Cord Injury, EMSCI). This allowed to determine AIS grades which ranged from A to D (A: motor-sensory complete; B: motor complete, sensory incomplete; C: motor-sensory incomplete; and D: motor-sensory incomplete, majority of key muscles below the lesion show movement against gravity [21, 22]).

In order to objectively assess long spinal tract integrity, trained technicians and experienced physicians performed independent neurophysiological tests of lumbar dermatomes according to clinical standards on certified electromyography machines [23]. Examination was done between 16 to 40 days after trauma (stage acute 1 follow-up according to the European Multicenter Study about Spinal Cord Injury, EMSCI). Technical setup and rating was done according to Hupp et al [24]. Tibial nerve stimulation led to recordings of somatosensory evoked potentials (SEP). Motor evoked potentials (MEP) were recorded bilaterally from anterior tibial muscles following transcranial magnetic stimulation of the corresponding cortical motor areas. Latency and amplitude readings were obtained according to the used standard [24]. After normalization latencies for body height, test results were converted to a simplified score as previously described [24]: motor and sensory potentials were rated with a maximum score of 2 for each side if evoked potentials were normal with respect to latency and amplitude, one if pathological in one of these aspects, and zero if missing. In this way for both MEP and SEP assessments, a maximum of 4 points (2 points each side) could be achieved.

Statistical analysis was performed on SPSS version 21.0 (IBM Corp). For continuous data, general descriptive statistics were reported as means and standard deviation (SD). Normal distribution of patient age was evaluated with the Kolmogorov-Smirnov test. For ordinal-scaled variables (AIS grades, SEP and MEP scoring), Mann-Whitney U test was used to test for significant differences. For statistical analysis, AIS grades A–D were transferred to numeric (0–3), and results were transferred back to AIS grades (A–D) and reported as such. For effect size (r), the Cohen classification was used [25]. For r > 0.1, the effect was considered weak. R > 0.3 reflected a medium and r > 0.5 a strong effect. In all tests, a p value of < 0.05 was considered to represent statistical significance. The two-way random effects intraclass correlation coefficient (ICC) was applied for inter-reader agreement, whereas ICC values > 0.5 were moderate, > 0.75 were considered good agreement, and > 0.9 as very good [26].

Mann-Whitney U test was used to evaluate for differences in the presence or absence of WD in the different anatomical regions of the cervical cord in AIS grades as well as MEP and SEP scores. Results are given in Table 2.

AIS grades were significantly different depending on the presence or absence of signal intensity change in the DC (p < 0.001). Median in the presence of hyperintense signal change was 1 (lower quartile 0.0; upper quartile 2.0), which is equivalent to AIS B; median in the absence of hyperintense signal change was 3 (2.75; 3.0), which is equivalent to AIS D. Calculation revealed a strong effect (r = 0.62). For CS, differences were significant (p = 0.016); median in the presence of hyperintense signal change was 1 (0.0; 2.0), equivalent to AIS B; without hyperintense signal intensity change, median was 3 (1.0; 3.0), equivalent to AIS D. Effect size was medium (r = 0.41). Significant differences were observed for the ST (p = 0.015) with an abnormal signal, median was 1 (0.0; 1.5) equivalent to AIS B. When the spinal cord appeared normal, median was 2.5 (0.0; 3.0) equivalent to AIS D. Effect size was medium (r = 0.41).

MEP scores were related to hyperintense signal change in the DC (p < 0.001), where WD was associated with a median score of 0 points (0.0; 1.5); median score with normal signal was 3 points (2.0; 4.0). Effect size was strong (r = 0.58). Association of MEP score with CS was significant (p = 0.032). Median score in the presence of hyperintense signal change was 0 points (0.0; 1.75); in the absence of hyperintense signal change, median was 2 points (0.0; 3.0). Effect size was medium (r = 0.36). Statistical significance was not reached for the ST (p = 0.067).

Evaluation of the SEP score reached statistical significance only for the dorsal column (p = 0.031); median was 1 point (0.0; 2.0) when signal was abnormal and 2 points (2.0; 3.25) when signal was normal. Effect size was moderate (r = 0.36). No correlation was found for SEP score with hyperintense signal change in CS but a trend for association of signal intensity change with ST (p = 0.092).

The presented data shows that appearance of tract-specific antegrade and retrograde degeneration, which we both refer to as WD, is a common phenomenon in routine MRI after severe tSCI. Especially WD in the DC remote from the injury can be seen in almost three quarters of the cases (71.4%) and can be appreciated with great confidence, represented by an absolute agreement between both readers. In the setting of a significant trauma history, misinterpretation is unlikely; still, mimics do exist: Deficiency syndromes, typically vitamin B₁₂ [27, 28] can result in subacute combined degeneration (SACD) that can look identical. Different pathologies include demyelination, such as multiple sclerosis [29], but especially neuromyelitis optica because of its longitudinal cord extent [30] or inflammation such as in sarcoidosis [31].

Compared to the DC, identification of pathology in the CS or the ST was more difficult to detect, which is represented by an ICC of 0.54 and 0.88, respectively. Due to tract anatomy of the CS and the ST, there is only a small area of signal change on cross-sectional imaging, if WD is present. Unlike WD in the DC, pathology in the CS and ST was often visible as dot-like hyperintensities only. Signal intensity change reflecting WD in the CS could be observed in about one-half of the cases (57.1%). Mimics of this signal change include spinal ischemia, typically affecting the anterior spinal artery represented by the owl-eyes or snake-eyes sign [32], although in most cases, only few segments are involved. In this study, in the majority of the cases, WD of the CS occurred in combination with WD of the DC and ST. WD in the ST occurred only in combination with at least WD of the DC; in most cases, all three described types of WD were present. To our knowledge, no reasonable alternative exists for this specific pattern.

Analyses showed that appearance of WD in the three different locations is associated with a higher degree of clinical impairment, reflected by the AIS grades. Median AIS without visible degeneration was D, with degeneration, AIS was B.

MEP and SEP scores were different in the presence or absence of WD in the DC (0 vs 3 and 0 vs 2 points). MEP scores were also different in the presence or absence of WD in the CS (0 vs 2 points), while there was no significant difference for the SEP scoring. This could reflect the fact that the CS is only transmitting motor signals and a degeneration would not affect sensory transmission. Because of the overlap of WD in the different tracts, this conclusion is arguable and is also in contrast with high correlation of MEP score with WD in the DC. However, coincidental occurrence of WD in more than one tract would well be in line with a high likelihood of tSCI causing diffuse, extensive white matter damage in the spinal cord.

In line with these results, previous diffusion tensor imaging data in tSCI patients and correlation with clinical and electrophysiological measures suggested WD of spinal tracts remote from the injury site [14].

This study has the following limitations: although there is some evidence for tract-specific impairment, because of the large overlap between the three investigated regions, it was not possible to correlate tract degeneration with specific types (sensory/motor) of impairment more precisely. The visual localization and specification of spinal tracts is limited by low resolution and fibers of other origin are located in close proximity to, or interspersed with, the aforementioned tracts (for example fibers from the rubrospinal and reticulospinal tracts run anterolateral to the CS [18]). Hence, we acknowledge that the anatomical description used for the regions of interest should be understood as an approximation to real tract anatomy.

In this study, the onset of visible WD in routine MRI was highly variable; unfortunately, it was not possible to identify a typical time frame, when WD first occurs or to correlate its first occurrence with clinical features. Moreover, as imaging intervals between the included patients were unequal, it was not possible to systematically evaluate how the signal progresses over the time. Both questions may be addressed in a future, prospective study design.

This study shows that WD especially in the dorsal column is a common phenomenon after severe spinal trauma, which can be detected by routine MRI with high confidence. Diagnosis in the appropriate clinical setting is straightforward. If Wallerian degeneration is present, it is associated with higher degree of clinical impairment.