Journal List > J Korean Soc Radiol > v.74(4) > 1087646

Roh, Yeom, Kim, Yoon, Park, Park, and Baik: Change of Apparent Diffusion Coefficient Immediately after Recanalization through Intra-Arterial Revascularization Therapy in Acute Ischemic Stroke

Abstract

Purpose

Intra-arterial revascularization therapy (IART) for acute ischemic stroke has become increasingly popular recently. However, early change in apparent diffusion coefficient (ADC) values after full recanalization in human stroke has not received much attention. The aim of this study was to evaluate ADC changes immediately after interventional full-recanalization in patients with acute ischemic stroke.

Materials and Methods

ADC values of 25 lesions from 18 acute ischemic stroke patients were recorded with both pre- and post-recanalization ADC maps. Measurement was done by placing region of interests over the representative images of the lesion. For analysis, lesions were divided into territorial infarction (TI) and watershed infarction (WI).

Results

Mean ADC values of the overall 25 lesions before IART were 415.12 × 10-6 mm2/sec, and increased to 619.08 × 10-6 mm2/sec after the IART. Average relative ADC (rADC) value for 22 TI increased from 0.59 to 0.92 (p < 0.000), whereas, average rADC value for 3 WI did not change significantly.

Conclusion

There was a conspicuous increase of ADC values immediately after full-recanalization in TI lesions. On the other hand, WI lesions did not show significant change in ADC values after recanalization.

INTRODUCTION

In human cerebral ischemia, the temporal evolution of signal intensity on magnetic resonance imaging (MRI), especially on diffusion weighted imaging (DWI), has been documented in the literature (12345). Apparent diffusion coefficient (ADC) values typically decrease sharply shortly after stroke onset, remain low for at least 72 to 96 hours, and then gradually increase, reaching and surpassing normal levels. Many animal studies, especially in rodent models, have shown imaging and pathologic changes after ischemic injury with or without subsequent reperfusion (67891011). Such studies provide information on the mechanism of tissue injury in ischemic stroke and implications on clinical treatment of ischemic stroke patients.
Over the past decades, the development of endovascular procedures to achieve recanalization aims at salvage of ischemic penumbra and better clinical outcome in patients (12). Signal evolution on MRI after recanalization of ischemic stroke lesions may reflect tissue change from reperfusion, and helps to clarify critical pathophysiology of acute ischemic stroke.
Though post-procedural MR imaging is not performed routinely, information on changes in MR imaging findings in the early reperfusion state may attribute to our understanding of pathophysiology of ischemic stroke and reperfusion injury after recanalization of occluded intracranial arteries.
There are only a few studies with human subjects probably due to the impracticality of serial imaging follow up in humans; however, changes on DWI finding after reperfusion or recanalization are reported (1314). The purpose of this study was to evaluate ADC changes immediately after interventional full-recanalization in patients with acute cerebral ischemia.

MATERIALS AND METHODS

Study Population

Study population was selected among the patients who received intra-arterial revascularization therapy (IART) in our institution for hyperacute to acute ischemic stroke, from January 2010 to December 2013. Institutional Review Board approval was obtained for this retrospective study, and informed consent was waived. Only a small number of patients underwent post-recanalization diffusion weighted MR imaging immediately after the procedure.
Inclusion criteria for this study were as follows: 1) patients who had both pre- and post-procedural DWI, 2) patients who received endovascular mechanical thrombectomy (either with stent retrieval or direct aspiration), intra-arterial thrombolysis, and/or stent insertion as treatment, 3) patients who showed successful recanalization with thrombolysis in cerebral infarction (TICI) grade 2b or more. Definition of TICI categories were according to that of Higashida et al. (15). The initial TICI grades were 0 and post-treatment TICI grades were 3 in all cases, except for a single case of TICI grade 2b; a detailed discussion of this exceptional case was provided later in the manuscript.
Exclusion criteria included: 1) hemorrhagic transformation that may attribute to signal change on DWI, seen as dark signal intensity on susceptibility weighted images acquired after the recanalization, 2) more than 4 hours of time interval between recanalization and post-recanalization DWI. Recanalization time was recorded for each case, as the time stated on images of the first angiography obtained after retrieval of Solitaire stent, aspiration of thrombus, or IA tirofiban injection demonstrating fully-recanalized artery. The average time interval between recanalization and post-recanalization DWI was 72 minutes for the overall study population.
Finally, a total of 18 patients were included in the study. Clinical characteristics of the cases, including initial National Institutes of Health Stroke Scale (NIHSS) and onset time, were collected through review of electronic medical record system of our hospital.

MR Imaging

One patient had pre-recanalization MR imaging in outside hospitals, in a 1.5T system (Genesis Signa, GE Healthcare, Milwaukee, WI, USA). The other 17 patients' pre-recanalization MR exams and all post-recanalization MR exams were performed in our own institution, using 1.5T or 3T MR imaging systems (Avanto, Verio, or Skyra, Siemens Medical Systems, Erlangen, Germany).
Overall, 36 MR exams were reviewed, of which, 18 pre-recanalization included images from an outside hospital and 18 post-recanalization images were obtained in our hospital.

Lesion Classification

Some of the patients had multifocal infarction, and the lesions were considered separately. Lesions that were not in the territory of the recanalized vessels (i.e., acute infarction in the posterior cerebral artery territory when the interventional treatment of anterior circulation was successfully applied) were not included in the analysis. Some small cortical infarctions, in which ADC value could not be obtained, were also disregarded.
Overall, 25 lesions of 18 patients were included in the study. The lesions were divided into either territorial infarction (TI) or watershed infarction (WI) according to pathophysiologic differences. WI is an ischemic lesion that occurs at the junction between 2 non-anastamosing distal arterial distributions. Two of 18 patients showed both TI and WI lesions and 1 patient presented with WI alone. All 3 lesions of WI were located in the internal watershed zone, deep white matter.

Means of Recanalization

Three patients were given intravenous tissue plasminogen activator (tPA) infusion in emergency room before endovascular treatment, since they satisfied indications at the time of arrival and first examination by the neurologist. Two of the 3 patients had completed tPA infusion, but did not show any clinically significant improvement i.e., NIHSS was unchanged and were referred to the angioroom for endovascular treatment. One of 3 patients had persistently high blood pressure (BP) from the beginning of the tPA infusion and the infusion was discontinued due to increased risk of hemorrhage associated with uncontrollably high BP. The other 15 patients were treated with endovascular intervention alone.

ADC Value Measurement

For each lesion, a representative image that could best demonstrate characteristics of the entire lesion was selected. Small region of interests (ROIs) that were as small as possible but large enough to generate meaningful ADC value for analysis were selected in representative images of the lesion. Another ROI of the same size was also placed on the contralateral anatomic location for comparison. The selected locations of ROIs were based on ease of sampling and to minimize interference of cerebrospinal fluid signal.
Review of MRI images and measurement was performed by 2 authors, a radiology trainee (J.E.R) and an experienced neuroradiologist (S.K.B), in consensus. ADC values of the infarcted area and the contralateral normal structure were recorded for pre- and post-recanalization DWI in each case. Subsequently, differences between pre- and post-recanalization ADC values were calculated. Also, relative ADC (rADC) values (ADC value of the lesion divided by ADC value of the normal contralateral region) were generated, and changes in rADC values were also recorded.

Statistical Analysis

The difference between pre-recanalization and post-recanalization ADC values were compared with paired t-test. The change of ADC values in TI and WI was compared with Mann-Whitney-U test. All statistical analyses were conducted with SPSS 21.0 (IBM SPSS., Statistics, IBM Corp, Armonk, NY, USA). A p-value < 0.05 was considered statistically significant.

RESULTS

A total of 18 patients were analyzed in this study, including 9 female patients and 9 male patients. The mean age of the study population was 64.39 years old (range from 45 to 77 years old), and the initial NIHSS on arrival time ranged from 1 to 28. The occlusion site of the cases and devices/method used for recanalization for each case were listed in Table 1.
The overall results were shown in Table 2. ADC values were expressed in 10 to minus 6th power of square millimeter per second (× 10-6 mm2/sec). Mean ADC values of the overall 25 lesions before IART were 415.12 × 10-6 mm2/sec, and after the IART, it was 619.08 × 10-6 mm2/sec.

TI

There was a marked increase of ADC value after recanalization of TI lesions (Fig. 1). Average ADC value for 22 TI lesions before thrombectomy was 436.09 × 10-6 mm2/sec and increased to 666.45 × 10-6 mm2/sec after the endovascular intervention (p < 0.000). Consequently, the relative ADC value (the ADC value measured on the infarction lesion divided by the ADC value measured at the contralateral anatomy of the infarction lesion) was also increased from 0.59 to 0.92 (p < 0.000).
One of the cases showed interesting features in the course of treatment. A 77-year-old male patient presented with dysarthria and right hemiparesis, after only 1hour from symptom onset. Acute infarction was noted in left middle cerebral artery (MCA) territory. Intravenous tPA was indicated, but infusion could not be completed due to his uncontrollably high BP. Stenosis in distal M1 was noted on digital subtraction angiography. Recanalization of inferior division was achieved after intra-arterial injection of tirofiban. However, the patient's BP was still too unstable, so further thrombolysis was suspended after TICI 2b recanalization to prevent catastrophic hemorrhage. Follow up DWI at 50 minutes post-partial recanalization showed increased ADC in recanalized inferior division territory alone. The ADC change was well correlated with reperfusion (Fig. 2).

WI

Of the 3 WI lesions included in the study, none showed prominent increase in ADC value after IART. Mean ADC value for the 3 WI lesions was 261.33 × 10-6 mm2/sec and increased to 271.67 × 10-6 mm2/sec after the intervention (p = 0.498). WI did not show significant increase in ADC value after IART, whereas TI lesions presented marked increase in ADC values. An example case from the WI subgroup was shown in Fig. 3.

DISCUSSION

The key findings of our study were as follows: first, there was a substantial increase of ADC value in acute infarction lesion immediately after IART i.e., less than 4 hours after the procedure, and secondly, there was no significant change in ADC values of WI lesions, whereas TI lesions showed marked increase. The results of our study indicated changes in ADC values at the earliest stage after recanalization in human ischemic stroke; furthermore, it is the first to show different profile in changes of ADC values between TI and WI, to the best of our knowledge.
In an early study on rat MCA occlusion model, Neumann-Haefelin et al. (9) reported dynamic change of MRI characteristics of transient ischemic lesions during the reperfusion period. In the 0.5 and 1.0 hours occlusion groups, ADC value of the ischemic region increased sharply after reperfusion with secondary decline at day 1, and (pseudo) normal level at 2–3 days. However, early increase in ADC value was absent in the 2.5 hours group and started to increase at day 1 and normalized between day 2 and 7.
In another animal study of Li et al. (16), which included 16 rats with temporary MCA occlusion or sham operation, ADC values decreased significantly during occlusion, as compared with those in the contralateral regions but fully recovered after reperfusion. The ADC values remained normal thereafter in the 10-min group but declined secondarily 12 hours after reperfusion in the 30-min group. The transient or permanent resolution of DWI lesions does not necessarily indicate full tissue recovery from ischemic injury. In addition, selective neuronal necrosis was seen in the selected ROI of the rats undergoing 10 minutes of transient MCA occlusion.
Despite the relatively long time interval between onset and recanalization (average of 379 minutes, over 6 hours), the remarkable increase in ADC values after recanalization seen in our study may be comparable to those of short-term occlusion group. This discrepancy may have resulted from differences between primate and rodent, and sex and age differences of subjects included in the studies. Human ischemic strokes are usually small in volume and collateralization may affect outcome; however, rodent models may simulate malignant infarction in many cases (17). Also, molecular differences in thrombotic, inflammatory, and DNA repair cascades, as compared with primates (18) can limit direct comparison of human and rodent studies.
Secondary ADC decline could not be confirmed in our study, as in previous rodent studies (916), because patients could not undergo serial MR imaging follow up as in animal studies. Subacute phase MR images might provide additional information, though it has limited use in daily practice.
DWI changes after reperfusion in ischemic stroke has been reported in human subjects. In 2000, Kidwell et al. (13) showed reversal of lesions on DWI and perfusion weighted images immediately after thrombolysis, in 7 patients treated with intravenous or intraarterial tPA.
Their study included a small number of cases treated with IA or combined IV/IA thrombolysis. Moreover, mainstream endovascular treatment for ischemic stroke is currently changed to mechanical thrombectomy. The change was described as a reversal indicating that thrombolysis could potentially normalize the ischemic lesion. Increase of ADC value after recanalization does not mean normalization of the infarcted tissue. In support, some animal studies showed that normalization of DWI lesion does not necessarily indicate tissue salvage from ischemic injury, but is associated with neuronal damage (161920).
Recently, Inoue et al. (14) demonstrated transient reversal of DWI immediately after IART in most of the study population, using DWI Evaluation for Understanding Stroke Evolution Study-2 data. They analyzed DWI before, within 12 hours of IART and follow-up MR on day 5. In their study, early DWI reversibility was not uncommon but typically transient, and the authors suggested that early DWI reversal may result from the transient rise in ADC values after reperfusion, which is possibly related to vasogenic edema (21).
On the other hand, subjects included in our study were imaged in less than 4 hours after recanalization, so we evaluated changes in ADC values at the earlier reperfusion state. We observed a prominent ADC increase in the majority of the patients (in TI lesions); furthermore, we demonstrated different profile of ADC changes between TI and WI. However, we could not assess if the change of ADC values were transient or permanent because the small subset of patients with follow-up MR imaging were not included in the analysis.
The early increase in ADC value observed in our study may reflect vasogenic edema after reperfusion. Recanalization of occluded vessels could result in reperfusion hyperemia due to the loss of autoregulation, the release of vasodilating substances, and the process of neovascularization (22). Delayed reperfusion injury may occur in the setting of reperfusion hyperemia due to oxidants or free radical damage (23).
Relationship between perfusion changes and cellular damage was investigated by Lee et al. (24), in a study using cats with 1 hour transient occlusion of MCA by clipping. They reported significant increase in TUNEL (terminal dUTP nick end labeling)-positive cells, which indicates nonspecific cellular damage including necrosis, in the groups of continuous hyperperfusion and early hyperperfusion with gradual decrease, as compared to normal perfusion and persistent hypoperfusion groups.
The second key finding of this work was that the prominent increase in ADC value seen on TI was not seen on WI lesions. Different evolution profile between WI and TI has been reported previously. Huang et al. (25) reported that ADC value increased more rapidly in the 14 TI patients, as compared to the 9 WI patients included in their study on temporal evolution of ADC values. The different pathophysiologic and hemodynamic features of the 2 infarction types are the likely cause of this difference.
In our study, the change of ADC value immediately after full recanalization in WI were not as significant as in cases of TI. While the exact pathophysiology underlying the increase of ADC value after full-recanalization remains to be determined, the change was not observed in WI as much as TI. This difference could possibly be due to the difference in pathophysiologic and hemodynamic features of the 2 types.
Our study had several limitations. The retrospective nature of the study possibly caused some degree of selection bias. Secondly, 2 patients had acquired pre-recanalization DWIs at 2 different outside hospitals, which were analyzed in the same manner as the images acquired in our own institution.
In addition, the ADC value measurement was conducted through ROI selection by the reviewer on a representative image of the case, hence the analysis was subjective. Overall average change of the ADC value of the lesion could not be assessed. Fourth, a relatively small number of WI lesions were analyzed.
Lastly, the final infarct core could not be compared with the initial lesions because only a small number of patients had follow up MR images, and thus, clinical outcome of the patients included in this study was not assessed. Further investigation with long term outcome and follow up MR imaging findings of patients who were treated with IART, as compared to untreated patients or patients treated with other methods will provide additional information.
In conclusions, ADC value was increased in acute ischemic stroke immediately after full-recanalization, on images acquired in less than 4 hours after recanalization. TI lesions showed a substantial increase in ADC values, but the increase was not seen in WI lesions.

Figures and Tables

Fig. 1

Change in ADC value after full-recanalization of a TI lesion (case no. 4).

Acute infarction in right MCA territory is seen on the pre-recanalization DWI (A, B). Occluded right proximal MCA can be seen in pre-recanalization angiography (C, left), and the right MCA is recanalized after mechanical thrombectomy (C, right). After successful recanalization, increased ADC is noted on the post-recanalization image (D).
ADC = apparent diffusion coefficient, DWI = diffusion weighted imaging, MCA = middle cerebral artery, TI = territorial infarction
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Fig. 2

A 77-year-old male patient with left MCA territory infarction (case no. 10).

Initial DWI and ADC maps show acute infarction at the level of superior division territory of left MCA (A, B) and inferior division territory (C, D). Severe stenosis of left distal M1 is seen on pre-recanalization angiography (E). Angiography after IA injection of tirofiban (F) presents recanalization of inferior division and still occluded superior division. Post-recanalization ADC map (G) shows no remarkable change in superior division territory, but increased ADC in recanalized inferior division territory (H).
ADC = apparent diffusion coefficient, DWI = diffusion weighted imaging, MCA = middle cerebral artery
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Fig. 3

Change in ADC value after full-recanalization of a WI lesion (case no. 9).

Acute infarction is seen in right internal border zone (A, B). The right proximal MCA is occluded (C, left) and after successful mechanical thrombectomy (C, right), post-recanalization ADC map (D) shows no significant change in comparison with pre-recanalization image.
ADC = apparent diffusion coefficient, MCA = middle cerebral artery, WI = watershed infarction
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Table 1

Patient Demographics and Clinical Informations

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No. Age/Sex Occlusion Site Infarction Type IV tPA Outside NIHSS at ER Interval 1 Interval 2 Recanalization Method
1 69/F T-occlusion TI - - 5 373 77 Solitaire 6 × 30
2 77/F M1 TI - - 9 418 211 Wingspan 3.5 × 15
3 76/F M1 TI - o 19 289 54 Solitaire 6 × 20
4 45/F M1 TI - - 10 300 57 Solitaire 6 × 30
5 67/F M1 TI and WI - - 5 625 82 Wingspan 3 × 15
6 58/M ICA TI - - 12 391 77 Wingspan 4.5 × 20
7 56/M ICA/M1 TI - - 20 488 28 Solitaire 6 × 30
8 55/F M1 WI - - 9 680 48 Solitaire 6 × 30
9 59/M M2 TI - - 1 264 51 Solitaire 4 × 20
10 77/M M1 TI o - 20 271 55 Tirofiban IA
11 72/M M1 TI and WI - - 13 172 86 Solitaire 6 × 30
12 73/F M1 TI - - 9 229 57 Solitaire 6 × 30
13 61/M ICA/M1 TI - - 17 909 62 Solitaire 6 × 30
14 62/M ICA/M1 TI - - 20 279 55 Aspiration
15 75/F BA TI - - 28 166 148 Solitaire 6 × 30
16 59/M CCA/T/M1 TI o - 17 341 40 Aspiration/solitaire 6 × 30
17 67/F ICA/M1 TI - - 22 353 67 Aspiration/solitaire 6 × 30
18 51/M M2 TI o - 24 274 33 Aspiration/solitaire 4 × 20

BA = basilar artery, CCA = common carotid artery, ER = emergency room, ICA = internal carotid artery, Interval 1 = time interval between symptom onset and recanalization (expressed in minutes), Interval 2 = time interval between recanalization and post-recanalization imaging (expressed in minutes), IV tPA = intravenous tissue plasminogen activator, M1 = M1 segment of middle cerebral artery, M2 = M2 segment of middle cerebral artery, NIHSS = National Institutes of Health Stroke Scale, TI = territorial infarction, T-occlusion = occlusion of the carotid artery, middle and anterior cerebral artery, WI = watershed infarction

Table 2

Changes in ADC Values in TI and WI

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ADCpre ADCpost p-Value
Lesion all 415.12 619.05 0.000
 TI 436.09 666.45 0.000
 WI 261.33 271.67 0.498
Contralateral 743.40 740.80 0.571
rADCpre rADCpost p-Value
Lesion all 0.56 0.85 0.000
 TI 0.59 0.92 0.000
 WI 0.34 0.35 0.625

ADC values are expressed in × 10-6 mm2/sec.

rADC = relative apparent diffusion coefficient value (ADC value of the lesion divided by normal contralateral ADC value), TI = territorial infarction, WI = watershed (or borderzone) infarction

References

1. Schlaug G, Siewert B, Benfield A, Edelman RR, Warach S. Time course of the apparent diffusion coefficient (ADC) abnormality in human stroke. Neurology. 1997; 49:113–119.
2. An H, Ford AL, Vo K, Powers WJ, Lee JM, Lin W. Signal evolution and infarction risk for apparent diffusion coefficient lesions in acute ischemic stroke are both time- and perfusion-dependent. Stroke. 2011; 42:1276–1281.
3. Schwamm LH, Koroshetz WJ, Sorensen AG, Wang B, Copen WA, Budzik R, et al. Time course of lesion development in patients with acute stroke: serial diffusion- and hemodynamic-weighted magnetic resonance imaging. Stroke. 1998; 29:2268–2276.
4. Lansberg MG, Thijs VN, O'Brien MW, Ali JO, de Crespigny AJ, Tong DC, et al. Evolution of apparent diffusion coefficient, diffusion-weighted, and T2-weighted signal intensity of acute stroke. AJNR Am J Neuroradiol. 2001; 22:637–644.
5. Burdette JH, Ricci PE, Petitti N, Elster AD. Cerebral infarction: time course of signal intensity changes on diffusion-weighted MR images. AJR Am J Roentgenol. 1998; 171:791–795.
6. Chen F, Suzuki Y, Nagai N, Jin L, Yu J, Wang H, et al. Rodent stroke induced by photochemical occlusion of proximal middle cerebral artery: evolution monitored with MR imaging and histopathology. Eur J Radiol. 2007; 63:68–75.
7. Jiang Q, Zhang RL, Zhang ZG, Ewing JR, Divine GW, Chopp M. Diffusion-, T2-, and perfusion-weighted nuclear magnetic resonance imaging of middle cerebral artery embolic stroke and recombinant tissue plasminogen activator intervention in the rat. J Cereb Blood Flow Metab. 1998; 18:758–767.
8. Minematsu K, Li L, Sotak CH, Davis MA, Fisher M. Reversible focal ischemic injury demonstrated by diffusion-weighted magnetic resonance imaging in rats. Stroke. 1992; 23:1304–1310. discussion 1310-1311
9. Neumann-Haefelin T, Kastrup A, de Crespigny A, Yenari MA, Ringer T, Sun GH, et al. Serial MRI after transient focal cerebral ischemia in rats: dynamics of tissue injury, blood-brain barrier damage, and edema formation. Stroke. 2000; 31:1965–1972. discussion 1972-1973
10. Shen Q, Fisher M, Sotak CH, Duong TQ. Effects of reperfusion on ADC and CBF pixel-by-pixel dynamics in stroke: characterizing tissue fates using quantitative diffusion and perfusion imaging. J Cereb Blood Flow Metab. 2004; 24:280–290.
11. Taheri S, Candelario-Jalil E, Estrada EY, Rosenberg GA. Spatiotemporal correlations between blood-brain barrier permeability and apparent diffusion coefficient in a rat model of ischemic stroke. PLoS One. 2009; 4:e6597.
12. Liebeskind DS. Reperfusion for acute ischemic stroke: arterial revascularization and collateral therapeutics. Curr Opin Neurol. 2010; 23:36–45.
13. Kidwell CS, Saver JL, Mattiello J, Starkman S, Vinuela F, Duckwiler G, et al. Thrombolytic reversal of acute human cerebral ischemic injury shown by diffusion/perfusion magnetic resonance imaging. Ann Neurol. 2000; 47:462–469.
14. Inoue M, Mlynash M, Christensen S, Wheeler HM, Straka M, Tipirneni A, et al. Early diffusion-weighted imaging reversal after endovascular reperfusion is typically transient in patients imaged 3 to 6 hours after onset. Stroke. 2014; 45:1024–1028.
15. Higashida RT, Furlan AJ, Roberts H, Tomsick T, Connors B, Barr J, et al. Trial design and reporting standards for intra-arterial cerebral thrombolysis for acute ischemic stroke. Stroke. 2003; 34:e109–e137.
16. Li F, Liu KF, Silva MD, Omae T, Sotak CH, Fenstermacher JD, et al. Transient and permanent resolution of ischemic lesions on diffusion-weighted imaging after brief periods of focal ischemia in rats: correlation with histopathology. Stroke. 2000; 31:946–954.
17. Carmichael ST. Rodent models of focal stroke: size, mechanism, and purpose. NeuroRx. 2005; 2:396–409.
18. Tagaya M, Liu KF, Copeland B, Seiffert D, Engler R, Garcia JH, et al. DNA scission after focal brain ischemia. Temporal differences in two species. Stroke. 1997; 28:1245–1254.
19. Ringer TM, Neumann-Haefelin T, Sobel RA, Moseley ME, Yenari MA. Reversal of early diffusion-weighted magnetic resonance imaging abnormalities does not necessarily reflect tissue salvage in experimental cerebral ischemia. Stroke. 2001; 32:2362–2369.
20. Henninger N, Sicard KM, Fisher M. Spectacular shrinking deficit: insights from multimodal magnetic resonance imaging after embolic middle cerebral artery occlusion in Sprague-Dawley rats. J Cereb Blood Flow Metab. 2007; 27:1756–1763.
21. Marks MP, Tong DC, Beaulieu C, Albers GW, de Crespigny A, Moseley ME. Evaluation of early reperfusion and i.v. tPA therapy using diffusion- and perfusion-weighted MRI. Neurology. 1999; 52:1792–1798.
22. Marchal G, Young AR, Baron JC. Early postischemic hyperperfusion: pathophysiologic insights from positron emission tomography. J Cereb Blood Flow Metab. 1999; 19:467–482.
23. Macfarlane R, Moskowitz MA, Sakas DE, Tasdemiroglu E, Wei EP, Kontos HA. The role of neuroeffector mechanisms in cerebral hyperperfusion syndromes. J Neurosurg. 1991; 75:845–855.
24. Lee SK, Kim DI, Kim SY, Kim DJ, Lee JE, Kim JH. Reperfusion cellular injury in an animal model of transient ischemia. AJNR Am J Neuroradiol. 2004; 25:1342–1347.
25. Huang IJ, Chen CY, Chung HW, Chang DC, Lee CC, Chin SC, et al. Time course of cerebral infarction in the middle cerebral arterial territory: deep watershed versus territorial subtypes on diffusion-weighted MR images. Radiology. 2001; 221:35–42.
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