Dr. Tanenbaum is Section Chief of Neuroradiology, MRI, and CT; and Dr. Hariharan is Director of Neuro-oncology and Neurology Residency Program Director at the NJ Neuroscience Institute, Edison, NJ.

Perfusion imaging techniques are now routinely available on high-performance magnetic resonance (MR) and helical computed tomography (CT) systems. MR and CT perfusion first-pass studies provide information analogous to that provided by Technicium D1-hemamethypropylene amine oxime (Tc-HMPAO) single-photon computed tomography (SPECT), and xenon CT, and, in many circumstances, mirror F-18 fluorodeoxyglucose (FDG) positron-emission tomography (PET) as part of a comprehensive brain examination. Perfusion information can be complementary or critical in the evaluation of patients with brain disease. These techniques are coming into widespread use in the evaluation and surveillance of patients with neoplasm, brain ischemia, neuropsychiatric disorders, and epilepsy.

Technique

High-performance, gradient-en-hanced MR scanners employ extremely fast single-shot echo planar imaging (EPI) techniques to image multiple physiologic phases at multiple (z-axis) brain locations during the first pass of a gadolinium chelate, paramagnetic contrast agent (figures 1 and 2). CT scanners can repetitively scan one or multiple (on multichannel systems) slice locations during the first pass of a standard nonionic iodinated contrast agent to obtain maps of brain perfusion (figure 3).

Perfusion CT provides information equivalent to xenon CT. ^1,2 Since xenon CT technique is more costly, personnel intensive, and more dependent on patient cooperation, it has achieved limited acceptance in the community setting.

Commercially available software is used to process first-pass data into maps of brain perfusion. Algorithms for the processing of regional cerebral blood volume (rCBV) maps are widely available for MR and CT. Calculation of mean transit time (rMTT) requires the assumption of an instantaneous contrast agent arrival in the target organ, physically impossible with first-pass techniques. Very high injection rates (10+ cc/sec) have been used to simulate instantaneous tracer arrival, but concerns about patient tolerance has limited utilization of this approach in the clinical community. Fortunately, complex deconvolution algorithms that compensate for the actual, finite arrival time of the injected first-pass contrast agent are now commercially available for CT data. Regional cerebral blood flow (rCBF) is calculated from the ratio of rCBV and rMTT. Accurate rCBF data that correlate well with xenon CT studies can therefore be obtained readily with first-pass CT. ^1,2 Quantitation of MR data is complicated by a number of factors, however. Assumptions about the relationship of signal intensity (MR)/density change (CT) with tracer concentration, well documented with iodine based contrast agents and
x-ray/CT, may not hold for the susceptibility based signal changes associated with gadolinium-based MR agents. This complicates establishment of an accurate input function for the MR first-pass data. A commercially available quantitative perfusion software package is not yet available.

Stroke

Perfusion techniques offer the most sensitive measure of the extent of brain tissue under ischemic conditions in patients with symptoms suggesting acute and subacute stroke. The deficit on a perfusion study is often greater than that seen on diffusion-weighted imaging (DWI) (and CT) in the acute setting. A reduction of cerebral blood flow (CBF) is a typical accompaniment of acute stroke. Depending on severity, this will manifest as a compensatory increase or a resultant decrease in cerebral blood volume (CBV) (figure 4), as well as a regional prolongation of MTT. The combination of MR angiography, DWI, and perfusion MR ³ (figure 5)­­or more commonly CT, CT angiography, ^4-6 and (recently) perfusion CT--are used in the triage of patients in whom thrombolytic intervention is contemplated (figures 6-8).

Quantitative assessment of CBF yields information about brain tissue viability and hemorrhagic risk, which is critical for thrombolytic therapy decision-making. Subtracting the volume of brain with restricted diffusion from the perfusion-indicated volume of tissue under ischemic conditions yields the commonly accepted MR paradigm for tissue at risk for extension of infarction. The CT analogue of DWI is not clear and is under active study.

Outside of the setting of acute stroke, perfusion imaging can yield useful information about the functionality of collateral circulation and, thus, the significance of vascular occlusive disease (figures 9 and 10).

Neuropsychiatry

Perfusion techniques are in routine use for the evaluation of neuropsychiatric disorders. Traumatic brain injuries typically manifest as regions of de-creased CBV that correlate better than structural studies with the results of neuropsychologic testing (figure 11). Positive results increase treating physicians' diagnostic confidence, often leading to more aggressive therapy. Dementia of the Alzheimer's type typically presents with decreased temporoparietal perfusion, mirroring the findings seen with SPECT and PET (figure 12). ⁷

Neuro-oncology

Characteristic patterns are evident with perfusion imaging of neoplasms. ^8,9 Certain lesions, such as meningiomas, exhibit a striking increase in relative CBV (figure 13), while schwannomas and lower grade gliomas demonstrate less impressive alterations. Generally, high-grade gliomas are very heterogeneous on perfusion studies with areas of high and low CBV. Therefore, CBV studies are useful in the characterization of focal brain lesions, particularly neoplasms.

The extent of a typically non-enhancing, low-grade primary brain neoplasm is better assessed by perfusion studies that measure capillary density, rather than disruption of the blood-brain-barrier (BBB), which typically is intact. Perhaps the most important role for perfusion MRI in the workup of tumors is in lesion surveillance. Breakdown in the BBB, seen as contrast enhancement on routine imaging sequences, is non-specific and could represent postoperative change, necrosis, or tumor. Residual or recurrent tumor will manifest an increase in CBV in contrast to gliosis or radiation necrosis, which has a low CBV (figure 14). Perfusion studies achieve a similar sensitivity to metabolic assessment with FDG-PET, with greater specificity. ^10,11

Taking advantage of the first-pass of the agent injected for the routine contrast-enhanced study, perfusion imaging poses minimal incremental cost other than the short time it takes to acquire the images. Dedicated reimbursement may be available through the use of image post-processing Current Procedural Terminology (CPT) codes.

Summary

Perfusion imaging is a powerful, clinically practical technique that provides critical information in the evaluation of patients with ischemic, neuropsychiatric, and neoplastic brain disease. AR