AbstractObjectiveDiagnosing tumor progression and pseudoprogression remains challenging for many clinicians. Accurate recognition of these findings remains paramount given necessity of prompt treatment. However, no consensus has been reached on the optimal technique to discriminate tumor progression. We sought to investigate the role of magnetic resonance perfusion (MRP) to evaluate tumor progression in glioma patients.
MethodsAn institutional retrospective review of glioma patients undergoing MRP with concurrent clinical follow up visit was performed. MRP was evaluated in its ability to predict tumor progression, defined clinically or radiographically, at concurrent clinical visit and at follow up visit. The data was then analyzed based on glioma grade and subtype.
ResustsA total of 337 scans and associated clinical visits were reviewed from 64 patients. Sensitivity, specificity, positive and negative predictive value were reported for each tumor subtype and grade. The sensitivity and specificity for high-grade glioma were 60.8% and 87.8% respectively, compared to low-grade glioma which were 85.7% and 89.0% respectively. The value of MRP to assess future tumor progression within 90 days was 46.9% (sensitivity) and 85.0% (specificity).
ConclusionBased on our retrospective review, we concluded that adjunct imaging modalities such as MRP are necessary to help diagnose clinical disease progression. However, there is no clear role for stand-alone surveillance MRP imaging in glioma patients especially to predict future tumor progression. It is best used as an adjunctive measure in patients in whom progression is suspected either clinically or radiographically.
INTRODUCTIONDifferentiating post-treatment changes in high-grade gliomas remains a challenging clinical task due to their radiological similarities (recurrent enhancing lesions). The prompt diagnosis of tumor progression and radiation necrosis remains paramount due to the apparent therapeutic and prognostic implications. Accurate diagnoses with conventional MR imaging are limited, as tumor progression appears to strongly mimic entities such as radiation necrosis and pseudoprogression as outlined by the MacDonald criteria19). Over the last decade, Response Assessment in Neuro-Oncology criteria has replaced the McDonald criteria to help discriminate these entities more clearly by dividing tumor response into four sets (complete, partial, stable, and progression)25). Recently, it has been demonstrated that accurate identification of tumor progression may be enhanced by adjunct imaging modalities such as magnetic resonance perfusion (MRP), Single photon emission computed tomography (SPECT) or positron emission tomography (PET) imaging3-5,7,11,12,15,24).
MRP is a unique imaging modality that utilizes gadolinium contrast to expand upon conventional MRI sequencing in order to approximate the blood flow/volume of selected tissues. Neoplasms, due to their high vascularity, tend to demonstrate higher cerebral blood volume (CBV) measurements than normal brain. Radiation necrosis on the other hand tends to demonstrate lower CBV values due to the lower cellularity and lack of neovascularization8,16,22). Because of its availability at most hospitals, MRP may be an effective tool for rapidly distinguishing these two entities.
Many patients in our institution receive surveillance MRP imaging to evaluate for glioma recurrence. In our institution, it is used in three different scenarios: First, it is used contemporaneously with MR and/or clinical findings suggestive of TP in patients with treated high grade glioma, as an adjunct to determine whether there is true TP or RN or pseudo-progression (PP). Second, it is used contemporaneously with MR and/or clinical findings suggestive of tumor progression in patients with low grade glioma, as an adjunct to determine whether there has been progression to a higher grade of tumor. Finally, it is used as a “screening tool” in patients with any type of glioma and stable clinical and imaging findings, to try to predict progression at a later date. Since there is no consensus in the literature on the utility of MRP in confirming clinical tumor progression for any of the three scenarios, we aimed to elucidate the clinical accuracy of MRP more closely by reviewing our own institutional experience.
MATERIALS AND METHODSSelection criteriaFollowing approval for our institutional review board (IRB), we conducted a retrospective chart review of patients who received MRP for surveillance of TP. Patients were included who had histopathologically proven glioma ([World Health Organization, WHO] II-VI) and who received neuro-oncology care and surveillance MRP imaging in conjunction with their follow-up visit at our institution. Patients who received MRP imaging for diagnoses other than glioma were excluded. Patients with less than two MRP studies were also excluded. Patients with follow up clinical visits without concordant imaging, or vice versa, were also excluded.
Study definitionsTP, based on the revised assessment in neuro-oncology (RANO) criteria, was identified by any of the following: significant increase in size of enhancing lesions on stable or increased steroid dosage, a significant increase in T2/fluid attenuated inversion recovery (FLAIR) nonenhancing lesions, appearance of new lesions, or clear clinical deterioration not due to an apparent comorbid condition. If the patient had any evidence of clinical, radiographic RANO or histological tumor progression, it was considered tumor progression as deemed by a board-certified neuro-oncologist. Histological data was routinely not available as many patents had tumor progression but were not taken to the operating room. MRP was performed by injecting contrast agent during a dynamic susceptibility contrast scan to quantify gadolinium uptake over time. The cerebral blood flow was then qualitatively analyzed using a color gradient to compare to non-pathogenic areas. MRP was defined as positive based on a significant increase in CBV as determined qualitatively by an attending neuroradiologist blinded to the clinical data; no specific threshold values were used. MRP imaging was defined as contemporaneous if it occurred within seven days, but not after the corresponding clinical visit.
Data analysisFor contemporaneous visits, TP, defined as positive or negative by the criteria above (radiographic, histological or clinical tumor progression), was the “gold standard” and MRP, also defined above, as the “test”, i.e., a positive MRP study with a concurrent determination of clinical or radiographic progression would be deemed true positive. The positive predictive value (PPV), negative predictive value (NPV), sensitivity and specificity were calculated with subgroup analysis based on WHO grade to assess the utility of MRP in predicting tumor progression as deemed by the above criteria.
Analysis of MRP in detecting TP at the next follow up clinical visit was also analyzed, with MRP at the current visit as the “test” and TP at following follow up clinical visit as the “gold standard”. PPV, NPV, sensitivity, and specificity were then calculated. Clinical and radiographic encounters were excluded if the length from MRP study to next clinical follow up visits was greater than ninety days. Statistical analysis was performed by one author (AS) and confirmed by a second (BS). Pathological data was included when available as the definitive indication of true tumor progression.
RESULTSA total of 337 MRP studies and associated contemporaneous clinical visits were reviewed from 64 patients. 27/64 (42.1%) patients were male. Twenty-four patients had WHO II gliomas, seventeen were WHO III, and twenty-three were WHO IV. Of these patients, 20 patients had oligodendrogliomas or oligodendroglial components to their tumors, of which 14 were WHO II and 6 WHO III. 61 patients had prior surgery; 3 patients did not have adequate records of prior surgery. 50 of 59 patients underwent prior radiation, with 5 patients having insufficient documentation as to prior radiation treatment. Patient demographics are listed in Table 1.
Contemporaneous clinical visitsFor contemporaneous MRP imaging studies and clinical visits, the total PPV, NPV, sensitivity and specificity for both LGG and HGG were calculated (Table 2) from the clinical visits and concurrent imaging (Table 3). The average number of MRP imaging studies and associated visits for each patient was 5.3. The sensitivity, specificity and positive predictive value of MRP to analyze tumor progression in LGG was 85.7%, 89.0%, and 76.9% respectively. The sensitivity, specificity and positive predictive value of MRP to analyze HGG tumor progression was 60.8%, 87.8%, and 72.6% respectively.
Future clinical visitsThe ability of MRP to evaluate for tumor progression at the next clinical visit was also assessed. One-hundred and twenty-five MRP studies and associated follow-up clinical visits occurred within 90 days. The PPV, NPV, sensitivity and specificity for all glioma types were calculated (Table 2) from the imaging and next follow up visits less than ninety days. Predictive value of MRP to assess tumor progression within 90 days was 46.9% (sensitivity) and 85.0% (specificity).
DISCUSSIONThe results from our review show that as a measure of surveillance for TP, contemporaneous MRP performed in a manner similar to other adjunct imaging modalities. MRP did not perform well in its ability to predict TP at the next clinical visit. These results demonstrate that the use of MRP is likely most valuable as an adjunctive measure in patients who are already suspected of having TP, as opposed to a routine surveillance imaging modality.
MRP for high-grade gliomasThe contemporaneous use of MRP in conjunction with MR for evaluation of tumor progression in high-grade gliomas has been well characterized in the literature3,8,10,11,16,21,23). The sensitivity and specificity of MRP to predict histological tumor progression in conjunction with MR has been approximately 80% and 77% respectively24). Additionally, the utility of MRP increases if a specific cut-off parameter was used for characterizing TP. For example, Kim and Narang et al. reported near 100% diagnostic accuracy in cases when cutoff values were set for CBV (cerebral blood volume ratio) and MSIVP (maximum slope of enhancement in the vascular phase) respectively17,20). By using MRP alone, the sensitivity and specificity of detecting tumor progression in our series was approximately 61% and 88% respectively. Our series indicates that when using MRP in conjunction with both standard MR and clinical follow-up, the accuracy of MRP increases. However, in our study, specific cut-off parameters were not utilized to optimize the specificity of our study. Additionally, in comparison to other studies which only used tumor histology as evidence of progression, our study compares MRP to radiographic and clinical progression as well which is more indicative of daily decision-making for neuro-oncologists as many patients are not-reoperated everytime a MR imaging displayes progression.
MRP for low-grade gliomasLow grade-gliomas typically may or may not enhance on imaging, and when enhancement is present, anaplastic (WHO Grade III) features may be present. However, after radiation, differentiation of post-treatment enhancement on MR and tumor progression for low-grade gliomas becomes challenging due to their delayed malignant transformation and potential for radiation necrosis13). Use of perfusion imaging in these low-grade tumors may detect malignant transformation with reasonable accuracy. In our series, sensitivity and specificity remained high for these lesions using MRP. In addition, other series seem to endorse following changes in CBV for low-grade gliomas to detect anaplastic transformation as early as 1 year prior to the development of contrst-enhancement6,9,18). However, other modalities may be more efficacious in detecting progression earlier compared to MRP. Hlaihel et al. noted that magnetic resonance spectroscopy detected tumor progression (based on increased choline/creatine ratio) on average 15 months prior to increases in CBV on MRP14). Nevertheless, MRP with contemporaneous MR may be useful if careful cut-off parameters are utilized to detect clinical tumor progression.
Use of MRP as a screening toolPerfusion imaging as a screening tool to predict malignant transformation in patients with any glioma remains important. In our study, perfusion imaging did not accurately predict tumor progression at the next clinic visit, yet was functionally useful for contemporaneous evaluation of disease status. The lack of predictive value maybe linked to the fact that no specific cut-off value was employed for CBV as many studies have noted higher CBV values several months prior to tumor progression. A multi-parametric prospective study using spectroscopy and perfusion may be helpful in delineating tumor progression in glioma patients. Our study, however indicates that general increased CBV values on perfusion imaging, by itself, are not suggestive of future tumor progression. We therefore recommend combined modality screening tests including MR spectroscopy and perfusion for accurate predictions of disease status.
Study limitationsOur study was limited in several areas. First, while the criteria for TP was based on RANO criteria, significant increases in contrast enhancement, T2/FLAIR signal, and CBV were defined at the discretion of the neuroradiologist. More standardized definitions of positive MRP imaging or radiographic progression using threshold values would increase intra- and inter-observer reliability. Additionally, pathological confirmation is the accepted standard for defining true tumor progression, so our radiological association based on RANO criteria merely serves as a surrogate. Also, our mean number of days between clinical follow up was in excess of four months. Thus, only 125 of 273 follow up visits fell within 90 days. The average number of days from MRP to follow up visit, even after excluding visits greater than 90 days, was 63 days. As such, the likelihood of MRP to predict TP would have increased had the length been shorter.
Additionally, the utility of perfusion-based imaging dramatically decreases after certain types of treatment such as anti-angiogenic chemotherapeutics and brachytherapy1,2). Variations in contrast-enhancement patterns after bevacizumab treatment confounds the utility of perfusion imaging. In our study, a few recurrent tumors were treated with bevacizumab after confirmed recurrence, which may also impact the accuracy of MRP. Nevertheless, recently, studies have begun to use standardized CBV parameters and other MRI-based biomarkers to overcome these barriers to effectively monitor treatment response after bevacizumab treatment. A future prospective study to evaluate the value of these parameters in post-bevacizumab treated patients may be useful.
CONCLUSIONMRP represents a promising imaging modality in evaluating TP in glioma patients. Our study reveals that MRP performs similarly to other adjunctive diagnostic imaging studies (MRS, SPECT) in evaluating TP at contemporaneous clinic visits, but fared poorly in its ability to predict clinical or radiographic progression at the subsequent visit.
While its role has not yet been clearly defined, perhaps the use of MRP currently is best done as an adjunct with other imaging modalities, such as MRS and PET, when TP is suspected as opposed to a measure of routine stand-alone surveillance. Although our study is limited due to the lack of histological confirmation, these results remain practical for neuro-oncologists who routinely change treatment plans based on clinical/radiographic signs of progression. Further studies need to undertaken to develop standardized criteria for TP on MRP before it could be used as a surveillance measure for all glioma patients.
Table 1Table 2
Sensitivity, specificity, positive predictive value, and negative predictive value of MRP for LGG and HGG at a contemporaneous clinic visit, as well as at a delayed follow up visit within 90 days (row 3). MRP: magnetic resonance perfusion, LGG: low-grade gliomas, HGG: high-grade gliomas, PPV: positive predictive value, NPV: negative predictive value Table 3
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