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This Article Free to Access Abstract Full Text (PDF) All Versions of this Article: jnnp.2006.099077v1 jnnp.2006.099077v2 78/6/581    most recent Submit a response Alert me when this article is cited Alert me when eLetters are posted Alert me if a correction is posted Citation Map Services Email this link to a friend Similar articles in this journal Similar articles in PubMed Add article to my folders Download to citation manager Request Permissions Citing Articles Citing Articles via HighWire Citing Articles via Google Scholar Google Scholar Articles by Liang, Z. Articles by Ling, L. Search for Related Content PubMed PubMed Citation Articles by Liang, Z. Articles by Ling, L. Topic Collections Relevant Article

A prospective study of secondary degeneration following subcortical infarction using diffusion tensor imaging

¹ Department of Neurology and Stroke Centre, The First Affiliated Hospital, Sun Yat-Sen University, Guangzhou, China
² Medical Imaging Centre, The First Affiliated Hospital, Jinan University, Guangzhou, China
³ Department of Neurology, The First Affiliated Hospital, Jinan University, Guangzhou, China

Correspondence to:
Correspondence to:
Professor Jinsheng Zeng
Department of Neurology and Stroke Centre, The First Affiliated Hospital, Sun Yat-Sen University, No 58 Zhongshan Road II, Guangzhou, 510080, PR China; zengjs{at}pub.guangzhou.gd.cn

Received 1 June 2006
In final revised form 4 January 2007

Accepted for publication 5 January 2007

	ABSTRACT

TOP ABSTRACT MATERIAL AND METHODS RESULTS DISCUSSION REFERENCES

 
Background: Secondary degeneration of the pyramidal tract distal to the primary lesion after a stroke has been detected by some studies using diffusion tensor imaging (DTI) but its potential clinical significance and the degeneration of the fibre tract proximal to the primary lesion have received little attention.

Methods: Twelve patients underwent DTI on the 1st, 4th and 12th week following a subcortical infarct involving the posterior limb of the internal capsule, and 12 age and sex matched controls underwent DTI once. The DTI parameters mean diffusivity and fractional anisotropy (FA), and the clinical scores before DTI examination, including the National Institutes of Health Stroke Scale (NIHSS), the Fugl–Meyer (FM) scale and the Barthel index (BI), were assessed. The relations between the per cent changes in DTI parameters and clinical scores were analysed.

Results: From the 1st to the 12th week after stroke onset, FA values decreased (p<0.01, respectively) in the fibre tract above and below the internal capsule, and the NIHSS decreased (p<0.01) but the FM scale and BI increased (p<0.01, respectively) progressively. The per cent reductions in FA value in the fibre tract above and below the internal capsule were negatively correlated with the per cent changes in NIHSS and FM scale (p<0.05, respectively).

Conclusions: Secondary degeneration of the fibre tract proximal and distal to a primary lesion can be detected by DTI clearly and quantitatively and deteriorates with time progressively, which may hamper functional recovery after a subcortical cerebral infarct.

Abbreviations: BI, Barthel Index; DTI, diffusion tensor imaging; FA, fractional anisotropy; FLAIR, fluid attenuated inversion recovery; FM, Fugl–Meyer; MD, mean diffusivity; NIHSS, National Institutes of Health Stroke Scale; ROI, region of interest; WD, Wallerian degeneration

Animal experiments and post-mortem examinations have demonstrated that a focal cerebral infarct can cause secondary degeneration in fibre pathways remote from the primary lesion. Delayed disintegration of such a fibre tract is considered to be Wallerian degeneration (WD), defined as anterograde degeneration of a nerve tract distal to an injury.^1–5 Conventional MRI can detect the ipsilateral cerebral peduncle atrophy during the chronic stage of a focal cortical infarct^6–8 but cannot reveal the delayed degeneration in the pyramidal tract on other regions clearly or quantitatively. Diffusion tensor imaging (DTI), which uses diffusion sensitive gradients applied in at least six non-collinear directions, can determine the diffusivity of every voxel and fully depict tissue diffusion characteristics. DTI has been used to detect and quantify the secondary degeneration in the fibre tract in vivo.^9,10

Thomalla et al¹¹ reported that secondary degeneration revealed by DTI occurred in the pyramidal tract distal to the primary lesion from the acute (5 days from onset) to the chronic (288 days) stage in two patients with ischaemic stroke. In some cross sectional studies, fractional anisotropy (FA) values were found to be generally reduced along the pyramidal tract on the infarct side distal to the primary lesion.^9,12,13 After middle cerebral artery territory infarction, lower FA values in the cerebral peduncle were associated with a greater neurological deficit acutely, with worse outcomes 3 months later.¹³ However, to date, no prospective, controlled, contrast enhanced studies have monitored secondary degeneration, and the potential clinical significance of the degeneration distal to the primary lesion has not been confirmed. In addition, only one case report revealed that a pontine infarct can cause retrograde degeneration in the fibre pathway proximal to the primary lesion.¹⁴ However, there has been little research on the retrograde degeneration of the fibre tract after subcortical infarction, and its impact on the patient’s outcome is not well understood.

In this study, DTI was used to prospectively quantify and monitor changes in diffusivity in the fibre pathway both proximal and distal to a recent subcortical infarct in 12 patients. The relation between the per cent changes in DTI parameters and clinical scores were analysed.

	MATERIAL AND METHODS

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Subjects
We selected 12 consecutive patients within 7 days of stroke onset who had unilateral subcortical cerebral infarct involving the posterior limb of the internal capsule. Patients were excluded if they had other signal abnormalities on T1 and T2 weighted images and fluid attenuated inversion recovery (FLAIR) images on magnetic resonance. No patient had a history of brain or spinal cord disease. Following a predefined protocol, all patients had DTI in the first week (W1, 5 (2) days), at the end of the fourth week (W4, 28 (2) days) and at the end of the 12th week (W12, 88 (2) days).

Patient demographics and vascular risk factors were obtained. All patients had a detailed neurological examination 2 h before the magnetic resonance examination, including an evaluation of neurological deficits using the National Institutes of Health Stroke Scale (NIHSS), motor deficits using the Fugl–Meyer (FM) scale and a life independence assessment using the Barthel Index (BI). The volume of the initial lesion was estimated on magnetic resonance FLAIR images at the end of the third month (volume = /6 x length x width x the number of slice involved). Twelve age and sex matched healthy volunteers underwent DTI using the same MRI protocol.

The research protocol was approved by the local ethics committee for clinical research and all procedures involving the participant were conducted according to institutional guidelines in compliance with the regulations. Oral and written informed consent was obtained from all participants.

Magnetic resonance imaging
MRI was performed using a 1.5 T MRI system (Signa General Electric Medical Systems, Milwaukee, USA) equipped with gradient hardware allowing up to 23 mT/m gradients. The baseline scan was in the anteroposterior plane, using a standard head coil. Prior to scanning, head movement was limited by vacuum fixation cushions. Axial T1 weighted FLAIR, fast spin echo T2 weighted imaging, traditional FLAIR and DTI were used. Consecutive slices were acquired in an identical location for all sequences, with a 5 mm slice thickness. Typical acquisition parameters were: T1-FLAIR (TR 2250 ms/TE 7.7 ms), fast spin echo T2 (TR 3800/TE120 ms) and traditional FLAIR (TR 9000/TE 120/TI 2200 ms). For DTI, an echo planar imaging sequence was used (TR10000/TE115 ms, NEX = 2, matrix 128 x 128, field of view 24 x 24 cm). Diffusion weighted images were obtained with b = 1000 s/mm² and diffusion sensitive gradients were applied along 13 gradient directions. In addition, a reference image without diffusion weighting (b = 0 s/mm²) was acquired. Acquisitions were repeated 20 times, and the results were averaged. The maximum strength of the diffusion gradients was 23 MT/m.

Image post-processing
To correct for distortions related to eddy currents associated with the large diffusion sensitive gradients, we applied an unwrapping algorithm to the diffusion weighted data set before the tensor estimation was performed. With this correction, the diffusion tensor parameters were calculated on a pixel-by-pixel basis. With the software Fuctool 2.3.1 (Signa General Electric Medical Systems), regions of interest (ROIs) were manually defined as an ellipse with an area of 36 mm², first on T2 weighted images and then on the corresponding DTI images. ROIs were symmetrically placed on axial slices in the left and right centrum semiovale (at the mid-point of the anterior two-thirds part on the second slice over the bottom of the lateral ventricle); in the coronal radiata (at the mid-point of the anterior two-thirds part on the second slice below the bottom of the lateral ventricle); in the middle part of the posterior limb of the internal capsule along its longitudinal direction; in the anterior part of the cerebral peduncle; and in the pons and medulla. All ROI positions were determined according to the scanning baseline and the anatomical structure. The ROIs in the fibre tract both above and below the internal capsule had no abnormal signal on T2 weighted or FLAIR images, and therefore all were not involved with the ischaemic damage. The mean diffusivity (MD) (derived from the trace of the diffusion tensor (MD = trace [D]/3) and measured on ADC images) and the fractional anisotropy index (FA value) (measured on the anisotropy images) were analysed.

Statistical analysis
Data are presented as median and quartile range. A Mann–Whitney test was used first for comparison between the left and right sides for median MD and FA values of any of the regions studied in controls. As the infarction appeared in either the left or right side in patients, we used median MD and FA values from both sides of the control subjects to compare with the quantitative DTI data of the patients from either the infarct side or the contralateral side to avoid any possible bias. A Mann–Whitney test was used for each comparison. To reveal the time progressive effect, liner regression for each patient was first established to describe the trend in clinical scores and DTI quantitative data obtained at W1, W4 and W12. The medians of within subject regression coefficients of all patients were then tested using Wilcoxon’s signed ranks test to determine whether the population within subject regression coefficient was equal to zero. Finally, Spearman correlation analysis was used to assess the association between the absolute value of per cent change (((W12 – W1)/W1) x 100%) of FA values and clinical scores, and the correlation between the within subject regression coefficient of the FA values and clinical scores. Values of p<0.05 were considered statistically significant. Statistical analysis was performed using SPSS 13.0 (Abacus Concepts Inc., Chicago, Illinois, USA).

	RESULTS

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Subject characteristics
Six patients had only one vascular risk factor, and one patient had no known risk factors (table 1). In all patients, on T2 weighted and FLAIR images, the primary subcortical lesion involved the posterior limb of the internal capsule, and the volume of the initial lesion was obtained. All patients and controls were right handed.

View larger version (26K): [in this window] [in a new window] [PowerPoint for Teaching]   Figure 1  An example of magnetic resonance images obtained from a patient with a left subcortical infarct on the first week after the onset of stroke. From axial T2 weighted images (A–F) and the coronal fluid attenuated inversion recovery image (G), the subcortical infarct involving the posterior limb of the internal capsule is observed (white arrows). Beyond the primary lesion, there is no hyperintense signal.

View larger version (52K): [in this window] [in a new window] [PowerPoint for Teaching]   Figure 2  An example of diffusion tensor images obtained from the same patient as in fig 1. From the axial fractional anisotropy (FA) images (A–F), reduced FA signals are observed not only at the primary lesion (C, white arrow) but in the fibre tract above the primary lesion including the centrum semiovale and coronal radiata (A, B, black arrows), and below the primary lesion including the cerebral peduncle, pons and medulla ipsilaterally (D–F, black arrows). In (G), a coronal view shows the reduced FA signals at the infarct region (white arrow) and in the fibre tract proximal and distal to the infarct lesion (black arrows).

Compared with controls, MD in the infarct was decreased at W1 (0.86 (0.85, 0.87) mm²/s in patients vs 1.04 (1.02, 1.05) mm²/s in controls; p<0.01) but it was increased at W4 (1.24 (1.20, 1.26) mm²/s in patients vs 1.04 (1.02, 1.05) mm²/s in controls; p<0.01) and at W12 (1.82 (1.72, 1.91) mm²/s in patients vs 1.04 (1.02, 1.05) mm²/s in controls; p<0.01). However, from W1 to W12, there was no significant change in MD in any region beyond the infarct area, either on the infarct side or on the contralateral side, compared with matched regions in controls.

Clinical scores
All patients had some degree of motor deficits. The FM scale ranged from 4 to 79 (21.00 (11.50, 61.50)) in the first examination; 11 patients had hemiplegia and one had a minor upper limb motor deficit and Broca’s aphasia. Four patients had one or two limb sensory disturbances. All patients received similar therapy for stroke, and each vascular risk factor was treated appropriately. By the end of the third month, all patients recovered somewhat; 8 patients returned to work, 3 were partially dependent and 1 was completely dependent. Table 3 shows the median clinical scores at the three time points. The Wilcoxon signed ranks test showed that the population medians of the within subject regression coefficients of the clinical scores were not equal to zero. That means the NIHSS decreased but the FM scale and BI increased progressively with time.

	DISCUSSION

TOP ABSTRACT MATERIAL AND METHODS RESULTS DISCUSSION REFERENCES

Some cross sectional studies have shown that at early or chronic stages, there is a reduction in the FA value with the MD remaining unchanged on the infarct side in the fibre tract distal to the infarct foci. In a small group of patients with a middle cerebral artery territory ischaemic stroke, 2–16 days after onset, the FA value was reduced but MD was unchanged at the cerebral peduncle on the infarct side.¹³ Werring et al⁹ reported a 15% decrease in the FA value and an unchanged MD in the fibre tract distal to the primary lesion in patients 2–6 months after a stroke. Another study found a 32% decrease in the FA value with MD unchanged in the fibre tract distal to the cerebral infarction in patients more than 1 year after a stroke.¹⁶ Only a longitudinal DTI study involving two patients with striatocapsular infarction showed that the FA value of the cerebral peduncle decreased from 16% to 25% over more than 9 months in one case, and from 17% to 48% over 3 months in another case, with a slight rise in MD.¹² In this study, we prospectively observed secondary degeneration in the fibre tract distal to the primary infarction in 12 stroke patient from W1 to W12 and in controls, and confirmed that the FA value decreased progressively with MD unchanged during the observation time period. Our data illustrate the course of secondary structural degradation more clearly, which defined WD over time in the fibre tract distal to the primary lesions.^17,18

In the present study, we also found that the FA value decreased progressively with MD unchanged from W1 to W12 in the fibre tract proximal to the primary infarct. Several studies have demonstrated retrograde degeneration in the corticospinal tract after damage, and such a mechanism of "dying back" might be responsible in part.^19–22 An increase in MD without a change in FA value after middle cerebral artery territory infarct was observed with DTI in the ipsilateral thalamus 1 month after stroke onset.²³ Because the thalamus was remote from the primary lesion and the change in MD in the thalamus was later than in the infarct foci, it was regarded as retrograde degeneration of the thalamocortical neurons secondary to fibre damage. A case of pontine infarction with retrograde degeneration of the pyramidal tract has been detected by T2 weighted MRI and confirmed post mortem.¹⁴ It is possible that the retrograde degeneration may also occur in the coronal radiata and centrum semiovale and may be detected by DTI. In our study, the progressive reduction in the FA value in the fibre tract above the initial infarction reflects the gradual degeneration of the fibre tract proximal to the primary lesion. There are at least two fibre types in the fibre tract above the internal capsule. One is from neurons in the motor cortex, descending from the subcortex to the spinal cord and formulating the pyramidal tract. The other is derived from the relay nuclei in the thalamus that deliver somatosensory messages through the corona radiata and the centrum semiovale to sensory areas located in the frontoparietal cortex, known as the thalamic radiation. Therefore, in the fibre tract above the internal capsule, secondary degeneration in the pyramidal tract is retrograde, while in the thalamic radiation it is anterograde.

The relation between the reduction in the FA value in the fibre tract beyond the primary lesions and patient outcome is not well understood. A longitudinal study found that progressive reductions in the FA value in the pyramidal tract distal to the primary lesion were associated with persistent moderate-to-severe hemiparesis.¹² Another study reported that patients with a larger degree of FA reduction at the cerebral peduncle distal to the initial infarct had a greater motor deficit in the early stage and a worse motor outcome 3 months later. In the present study, we found that all of the stroke patients recovered gradually over 3 months, and the per cent decreases in the FA value in the fibre tract above and below the internal capsule correlated negatively with the per cent changes in NIHSS and FM scale. In addition, a significant correlation between the within subject regression coefficient of the FA value from the fibre tract below the internal capsule and NIHSS was found. These results demonstrate that during the course of neurological recovery, secondary degeneration in the fibre tract both above and below the primary lesion persists and deteriorates, and a greater extent of secondary degeneration is associated with a smaller degree of recovery. It is obvious that the secondary degeneration in the fibre tract distal and proximal to the infarction may hamper neurological recovery.

In conclusion, our study shows that secondary degeneration occurs and deteriorates not only in the fibre tract distal to but also proximal to a subcortical cerebral infarct at least 12 weeks after stroke onset, and may hamper neurological recovery. To understand the mechanism and extent of the impact of secondary degeneration on neurological recovery, future investigations with a larger sample size, more homogeneous infarcts and a longer observation period are needed.

	ACKNOWLEDGEMENTS

 
This study was supported by grants from the Teaching and Research Award Program for Outstanding Young Teachers in Higher Education Institutions of the Ministry of Education, China (2002), the National Natural Science Foundation of China (Nos 39940012 and 30271485), the Natural Science Foundation of Guangdong Province, China (Nos 990065, 21906 and 2003C30610), China Medical Board of New York Inc. (No CMB00-730), the Fund for Priority Subjects in Clinical Medicine, Chinese Ministry of Health (2004) and the Key and Scientific Project of the Natural Science Foundation of Guangdong Province, China (Nos 2003B30303 and 2003D30301).

We thank Mr Jun Liu for statistical assistance.

	FOOTNOTES

 
Published Online First 23 January 2007

The funding sources were not involved in the study design, collection, analysis or interpretation of data, writing of the report or the decision to submit the paper for publication.

Competing interests: None.

	REFERENCES

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This Article Free to Access Abstract Full Text (PDF) All Versions of this Article: jnnp.2006.099077v1 jnnp.2006.099077v2 78/6/581    most recent Submit a response Alert me when this article is cited Alert me when eLetters are posted Alert me if a correction is posted Citation Map Services Email this link to a friend Similar articles in this journal Similar articles in PubMed Add article to my folders Download to citation manager Request Permissions Citing Articles Citing Articles via HighWire Citing Articles via Google Scholar Google Scholar Articles by Liang, Z. Articles by Ling, L. Search for Related Content PubMed PubMed Citation Articles by Liang, Z. Articles by Ling, L. Topic Collections Relevant Article