Rapid identification of a major diffusion/perfusion mismatch in distal internal carotid artery or middle cerebral artery ischemic stroke

This study consisted of retrospective and prospective components. Both components were compliant with the Health Insurance Portability and Accountability Act (HIPAA) and were approved by our institutional review board (IRB).

The retrospective study utilized data from a published study by Copen et al. [8], which demonstrated that a clinically significant diffusion/perfusion mismatch is common among acute ischemic stroke patients imaged within 24 hours of stroke onset, and most commonly occurs in patients with a proximal artery occlusion. In that study, all patients who presented to the emergency department (ED) of our hospital from June 2005 through December 2006 with symptoms suggesting an acute stroke syndrome were screened. Inclusion criteria for the present analysis were:

In the second study, we prospectively identified patients who presented to our hospital ED with stroke symptoms in 2008. Patients were included in this study if they met the same criteria as in the retrospective study. Patients who received intravenous thrombolytic prior to imaging were included if their imaging demonstrated a diffusion/perfusion mismatch consistent with persistent occlusion.

All imaging studies were requested by ED physicians based on clinical need and were not influenced by these studies.

In the retrospective study, CTA was performed from the C6 vertebral body level through the circle of Willis following injection of 100–140 ml of Isovue 61.2 g/100 mL (Bracco Diagnostics, Princeton, NJ) at a rate of 3 ml/s. Imaging was triggered 25 seconds after contrast material injection (40 seconds for patients with atrial fibrillation). Immediately afterward, a second set of images was obtained from the aortic arch to the skull base. The parameters were 2.5-mm slice thickness, 1.25-mm reconstruction interval, 140 kV, 220–250 mA, and 0.75:1 pitch.

In the prospective study, CT angiography was performed from the vertex to the aortic arch following injection of 80–120 ml of Isovue 370 (Bracco Diagnostics, Princeton, NJ) at a rate of 3.5 ml/s. SmartPrep (GE Medical Systems) was used with a region of interest 1 cm below the carina covering the entire lumen of the ascending aorta. Scanning began with a 10-second delay after the region of interest reached 75 HU. The parameters were 1.25-mm slice thickness, 0.625-mm reconstruction interval, 120 kV, 350–800 mA, and 0.516:1 pitch.

MR imaging was performed on a 1.5 T Signa whole body scanner (GE Medical Systems) with echo-planar capabilities. Axial DWI were obtained using single-shot, spin echo echoplanar imaging with the following parameters: TR 5000 ms; TE 80 to 110 ms; b-value 1000 s/mm2; field of view 22 cm; matrix size 128_128, zero-filled to 256_256, and slice thickness of 5 mm with a 1-mm inter-slice gap. As many slices as needed to cover the entire brain were acquired. For each slice a sequence including an image without diffusion gradients plus high-gradient-factor images in six directions were acquired. This was repeated five times and resulted in 35 images for each slice and a total imaging time of less than 4 minutes. Double inversion pulses were used to help reduce eddy current effects.

The perfusion-weighted imaging (PWI) was a serial gradient echo echoplanar sequence with TR/TE of 1500/40 ms. The field of view, section orientation, slice thickness, and spacing were as specified previously in the DWI sequence. Ten seconds after the beginning of image acquisition, 20 mL gadopentetate dimeglumine 0.5 mol/L (Magnevist; Bayer HealthCare Pharmaceuticals) was injected at a rate of 5 mL/s followed by 20 mL normal saline at the same rate. Sixteen slices were acquired every 1.5 seconds and this was repeated 46 times, which resulted in 69 seconds of imaging time.

MRA images of the head were acquired using a three-dimensional time-of-flight technique with 25° flip angle, TR/TE of 36/6.8 ms, 18-cm field of view, and a 512 _ 512 matrix. One hundred eleven transverse images were reconstructed with a section thickness of 1.4 mm and spacing of 0.7 mm.

In the retrospective study, the mean transit time (MTT) map was calculated using singular value decomposition deconvolution [9] with the arterial input function (AIF) derived from the middle cerebral artery ipsilateral to the infarct. This map was used as its clinical utility has been demonstrated in multiple successful trials [10, 11]. We used the time to peak (TTP) map in the prospective study because it is more commonly used. It has been shown to have the highest predictive performance when compared to standard MTT, circular MTT, and time to maximum (Tmax) maps [6]. Image processing usually consumes approximately 5 to 10 minutes; however exact processing time was not available in our studies.

In the retrospective study, lesions on DWI and MTT maps were outlined visually by a research technologist and were edited by a neuroradiologist (P.W.S.) using a semi-automated commercially available image analysis program (Analyze 7.0; AnalyzeDirect, Overland Park, Kan). These were done blinded to time of stroke onset and the locations of arterial occlusion. In the prospective study, DWI abnormalities were outlined visually by a research fellow and were checked by a neuroradiologist (R.G.G.). After coregistration, PWI lesions were outlined using a TTP delay threshold of greater than four seconds relative to the contralateral hemisphere, which was found to be the best estimate of penumbral tissue in a correlative study of MRI and positron emission tomography [12]. The mean value of a region of interest covering the contralateral MCA territory at the level of the basal ganglia was the reference for identifying tissue with TTP delay beyond the 4 second threshold [12]. Perfusion map artifacts such as those arising within the ventricles were excluded manually. Final outlines were checked by the same neuroradiologist. All analyses were performed using a semi-automated commercially available image analysis program (Analyze 8.0; AnalyzeDirect, Overland Park, Kan) and blinded to the clinical data of the patients and the site of arterial occlusion.

The absolute volume of the diffusion-perfusion mismatch was calculated as the difference between the respective volumes. Areas of DWI abnormalities which were not covered by PWI lesions were added to the total perfusion abnormality volume for mismatch calculation. A mismatch was considered zero if the PWI lesion was smaller than the DWI lesion. Absolute mismatch volume was divided by DWI lesion volume to yield relative mismatch volume in percent, a value that has been used in different clinical trials to recruit patients who may benefit from thrombolytic therapies [10, 11].

Patients with DWI lesions ≤ 70 ml were compared to those with lesions > 70 ml for the likelihood of the presence of a 100% diffusion/perfusion mismatch using two-tailed Fisher’s Exact Test. This analysis was repeated using a DWI lesion volume threshold of 100 ml. Two-tailed Spearman’s rank analyses were performed to assess for a significant correlation between time from ictus and DWI lesion volume, and between time from ictus and relative mismatch values. A finding was deemed significant if the P value was <0.05.