There has been much recent debate regarding the role of advanced imaging in general—and CT perfusion (CTP) in particular—in acute stroke management.1 Typical questions include the following:
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1) CT versus MR imaging: which technique is essential/sufficient/preferred for patient selection for lytic and endovascular stroke therapies?
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2) Vascular/collateral imaging: is there a role for CTA or MRA in acute triage to lytic and/or endovascular stroke therapies; are they worth the time required?
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3) Core or penumbra: what measures of admission stroke severity (both depth and extent of ischemia) best predict tissue and clinical outcome and the potential risks and benefits of treatment, and how can one best determine these?
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4) Perfusion imaging: when is it indicated, does it have added value for acute stroke assessment, and, if so, how should it be technically performed (acquisition and postprocessing) and optimally interpreted (which map, what threshold)?
The response to these queries depends critically on the sensitivity, specificity, and reproducibility of the various imaging techniques, which not only vary in a nonlinear manner with time post-ictus but also reflect a “snapshot” in time of a rapidly changing hemodynamic and physiologic process. We define “core” as critically ischemic brain tissue likely to be irreversibly infarcted despite early robust reperfusion and “penumbra” as severely ischemic but still viable tissue, likely to infarct in the absence of early robust reperfusion.
In brief, the answers are the following:
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1) An unenhanced head CT excluding hemorrhage is necessary and sufficient screening for standard IV thrombolytic therapy.
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2) A CTA to detect proximal large-vessel occlusion
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a) Is quick and highly accurate (more than MRA) for identifying candidates for endovascular stroke treatment; and
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b) Can be obtained without slowing IV thrombolysis.
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3) “Core is critical” for determining endovascular treatment eligibility.
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a) Patients with admission core volume >70–100 mL are highly likely to have poor clinical outcome despite early robust reperfusion (and more likely to bleed following recanalization).
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b) The most accurate practical way to determine core, with strong level 1 evidence, is with DWI.
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c) Despite the superiority of DWI for sensitive core detection—especially at early (<3 hours) times postonset—many neurointerventionalists consider an unenhanced CT good enough for endovascular triage (yet-to-be validated).
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4) If MR imaging is unavailable, appropriately thresholded CT cerebral blood flow (CBF) maps can distinguish small (<70–100 mL) from large (>70–100 mL) admission cores
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a) With high specificity for poor outcome, and
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b) With greater accuracy than other CTP maps, including cerebral blood volume (CBV).
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c) However, thresholds vary by postprocessing platform.
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5) Advanced imaging, most notably CT or MR perfusion, can facilitate accurate diagnosis, patient selection, outcome prediction, and other management decisions, but
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a) Most patients with proximal large-vessel occlusion and small core have mismatch (so mismatch does not add much to the endovascular triage decision).
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b) Penumbral imaging has not been validated for extending the time window for IV thrombolysis; and, most important
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c) The time needed for perfusion scanning must never slow the administration of definitive reperfusion therapies.
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For triage to IV-tPA, opponents of advanced imaging argue—convincingly, on the basis of level 1 evidence—that 1) IV lysis is FDA-approved ≤3 hours post-ictus on the basis of prospective randomized trials proving clinical benefit; 2) IV lysis is safe and effective, albeit with a high “number needed to treat,” ≤4.5 hours post-ictus; 3) “Time-Brain”; delays in IV lysis result in the death, on average, of almost 2 million neurons/minute2; and 4) an unenhanced head CT showing no hemorrhage is sufficient for deciding tPA eligibility.1
Once the decision to administer thrombolysis has been made, a rapid head and neck CTA can be obtained immediately during the 10 minutes required to mix the IV-tPA, without slowing treatment. The CTA identifies vascular occlusions that are targets for endovascular approaches (including FDA-approved clot retrieval ≤8 hours post-ictus) and can characterize both collateral flow and parenchymal “first pass” perfusion (from the CTA source images [SI]).3 This approach presupposes that despite FDA approval for a variety of clot-retrieval devices, endovascular therapy is indeed indicated. Some evidence-based purists counter that “until and unless the Interventional Management of Stroke 3 trial is completed … management of proximal occlusions remains speculative and thus patients should be offered the trial or be informed of the unproven nature of the proffered ‘rescue’ treatment.”1
What other imaging is required to weigh the risks versus benefits of treatment? Expert recommendations4 suggest that the admission core lesion volume >70–100 mL, together with admission NIHSS score, is one of the most important independent predictors of poor outcome5 and hence a necessary exclusion for endovascular treatment.5,6 This makes sense; why risk a large hemorrhage by attempting “futile” recanalization of already dead tissue?
How best to measure core? Here, opinion diverges on the basis of local practice and available resources. The most accurate, but least practical, is carbon 11 flumazenil PET.7 Unenhanced CT is rapid, convenient, and affordable but insensitive for the detection of early (<3–6 hours) ischemia. Many consider CT good enough for endovascular triage—at least for later times post-ictus—by using a “one-third MCA territory hypoattenuation” or “Alberta Stroke Program Early CT score ≤7” (corresponding to a >70–100-mL core) as the cutoffs for poor outcome. CTA-SI is more sensitive than unenhanced CT for ischemia detection at <3–6 hours, although the source images obtained by using fast current-generation multidetector row scanners tend to be flow- rather than volume-weighted and hence less well-correlated with DWI core.8 CTA-SI also allows collateral vessel assessment; a “malignant” (near-zero) collateral pattern has recently been shown to be both highly specific for poor outcome and strongly correlated with a large DWI core.9
DWI, based on Level 1 evidence, is unequivocally the most accurate practical imaging test for core, as early as 30 minutes post-ictus. However, what if MR imaging is unavailable? Which CT parameters can accurately estimate core? As already noted, the “jury is still out” on the use of standard unenhanced CT for endovascular triage; it's sensitivity at very early time post-ictus (<3hr) may be insufficient. Moreover, the paradigm that admission CT-CBV maps optimally correlate with DWI has recently been challenged; ongoing studies by multiple groups suggest that appropriately thresholded CT-CBF maps, obtained by using updated current-generation acquisition and postprocessing protocols, provide the most accurate estimate of core.10,11 Ideally, CTP acquisitions should be sufficiently long (>60–90 seconds) to avoid truncation of the contrast time-attenuation curves and postprocessed by using delay-insensitive software.
An important caveat is that the quantitative thresholds used for CTP map interpretation vary widely, not only among software of different vendors but also among different software versions from the same vendor, limiting their generalizability. This problem is one of standardization; effort is currently underway within the stroke community to address this.12 It is equally noteworthy, however, that for the purpose of selecting patients for endovascular stroke therapy, the correlation between CTP and DWI ischemic lesion volumes need not be perfect: CTP should only be able to accurately distinguish large (>70–100 mL) from small (<70–100 mL) admission ischemic lesion volumes. Preliminary data suggest that this is indeed the case.13
On the basis of these considerations, our neuroradiology section, in a consensus symposium led by Gil Gonzalez, developed the following acute stroke imaging algorithm delineating the imaging evaluation that we consider to be essential and sufficient for determining stroke treatment eligibility in our practice:6
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1) Unenhanced head CT to exclude hemorrhage
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2) Head and neck CTA, performed immediately following head CT (while the IV-tPA is being mixed, so as not to slow thrombolysis administration)
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a) Axial, coronal, and sagittal thick-slab maximum intensity projections (3-cm section thickness at 0.5-cm overlapping intervals) reviewed in real-time at the scanner console
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b) If MR imaging is contraindicated and endovascular therapy will not immediately to be performed, CT perfusion imaging should be considered.
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3) DWI
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a) If large-vessel occlusion is present and infarct core is <70–100 mL, proceed immediately to endovascular treatment.
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b) If the patient is not an endovascular candidate, MR perfusion imaging should be considered.
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With regard to perfusion imaging, which is not required for either IV lysis or endovascular treatment selection, valid indications include the following: 1) excluding stroke mimics; 2) identifying high-risk patients following TIA; 3) specifying stroke subtype and hemodynamics; 4) clarifying/confirming the presence/site of vessel occlusion; 5) assessment of vasospasm; 6) determining the need for blood pressure management; 7) guiding disposition decisions, such as transfer to an intensive care unit; and 8) establishing prognosis, especially of large “malignant” perfusion patterns at early time points, for which the risks of treatment may outweigh the benefits (ie, too bad to treat). For these reasons, perfusion imaging is routine in our institutional acute stroke imaging algorithm, provided that definitive standard of care IV or endovascular reperfusion therapy will not be delayed.
References
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- © 2012 by American Journal of Neuroradiology