2Department of Radiology, Kayseri City Hospital, Kayseri-Turkey
3Department of Genaral Surgery, Kayseri City Hospital, Kayseri-Turkey
4Department of Pathology, Kayseri City Hospital, Kayseri-Turkey
5Department of Medical Oncology, Kayseri City Hospital, Kayseri-Turkey
6Department of Radiation Oncology, Nevsehir State Hospital, Nevsehir-Turkey DOI : 10.5505/tjo.2021.2873
Summary
OBJECTIVEThe compatibility between magnetic resonance imaging tumor regression grade (mrTRG) and pathological tumor regression grade (pTRG) was examined in patients with locally advanced rectal cancer (LARC) who underwent neoadjuvant chemoradiotherapy (nCRT). The primary endpoint of the study was to evaluate the relationship between mrTRG and pTRG after nCRT. The secondary endpoint of the study was to evaluate the variables that affect mrTRG and pTRG.
METHODS
Forty-one patients with LARC treated with nCRT were analyzed. Magnetic resonance imaging (MRI)
performed after nCRT was compared with MRI taken before nCRT. Changes in T and N stages and
extramural vascular invasion positivity were investigated. TRG was divided into five groups in terms
of pathological and MRI. The Dworak pTRG system was used for compatibility testing. MRI sensitivity
and specificity were evaluated by comparing MRI-based response assessment with pathological assessment
after nCRT.
RESULTS
Median patient age was 61 years (range, 26?79 years), and 18 (43.9%) were female. The relationship
between mrTRG and pTRG was evaluated with the Cohen kappa coefficient. Significant compatibility
was observed between pTRG and mrTRG (p=0.002), but the compatibility was low (kappa compatibility,
0.319). The sensitivity of mrTRG was 90% (18/20); specificity was 14.3% (3/21); positive predictive value
was 85.7% (18/21); and negative predictive value was 90% (18/20). While pTRG was negatively affected
by advanced age (p=0.037), mrTRG was adversely affected by advanced post-nCRT N stage (p=0.048).
CONCLUSION
As age increased, pTRG was negatively affected; as the post-nCRT N stage increased, mrTRG was negatively
affected. There was compatibility between mrTRG and pTRG, as expected, but this compatibility
was found to be low.
Introduction
Magnetic resonance imaging (MRI) is the most commonly used diagnostic method for radiologically imaging rectal cancer. MRI has advantages in the evaluation of locally advanced stage rectal cancer (LARC). With rectal MRI, it is possible to determine many tumor lesion features, including size, morphology, and borders, which are useful in treatment planning.[1,2] MRI is used both before and after neoadjuvant chemoradiotherapy (nCRT). Significant progress has been made in controlling the local disease using nCRT in cases with LARC detected by MRI. At present, the most preferred imaging method for local staging of rectal cancer is rectal MRI.[3,4] Due to the increasing prominence of nCRT in recent years, the importance of imaging techniques has been studied, for both staging and accurately evaluating radiological response. Tumor volume reduction and fibrotic transformation are the two primary response markers that can be appreciated on morphological (T2 weighted) MRI and can help guide the treatment strategy after nCRT. However, research has indicated that morphological MRI is unable to differentiate between sterile fibrosis and fibrosis-containing tumor tissue, which is a significant clinical limitation. Researchers have concluded that it would be appropriate to add diffusion-weighted imaging to the MRI protocol, stating that diffusion-weighted MRI successfully distinguishes between tumor and fibrosis.[5]Pathological tumor regression grade (pTRG) is a system used in the histological evaluation of tumor response to nCRT that was initially used in other cancers of the gastrointestinal system, bladder, head, and neck. [6-9] Overtime, studies were carried out on the use of pTRG in determining the prognosis of LARC.[10,11] The most well-known pTRG systems are Mandard, Rödel, Dworak, and the American Joint Committee on Cancer (AJCC) scoring systems.[7,12-14] Recently, a pTRG-like MRI tumor regression grade (mrTRG) system was developed.[15,16] The basic principle of both the mrTRG and pTRG systems is related to tumor fibrosis rate following nCRT. Radiological interpretation requires the comparison of high-resolution oblique images with basal scans to determine the proportions of the tumor with fibrotic low signal intensity and residual medium signal intensity. There has been a lack of consensus in previous studies on the compatibility of mrTRG and pTRG in patients with LARC. In the study by Sclafani et al.,[16] agreement between mrTRG and pTRG was found to be poor, and mrTRG was seen as a complementary prognostic tool for surgical decision-making and pTRG. In contrast, Rengo et al.[17] found the compatibility between mrTRG and pTRG to be excellent. Ko et al.[18] recommended combining MRI and endoscopic biopsy to detect complete remission.
The histopathological definition of extramural vascular invasion (EMVI) is tumor cells invading vessels beyond the muscularis propria, which indicates a poor prognosis in patients with rectal cancer.[19] MRI can provide accurate guidance in detecting EMVI (mr- EMVI).[20] Several studies have shown that mr-EMVI is one of the risk factors for distant metastasis in rectal cancer.[21,22] Particularly in patients with a baseline T3 stage, defining EMVI may be important in predicting patients" response to nCRT and long-term results.[23]
In this study, changes in T and N stages and the positivity of EMVI were investigated. In addition, the compatibility of mrTRG and pTRG was examined to investigate the reliability of MRI in the diagnosis and treatment of rectal cancer.
Methods
Patient SelectionA total of 72 patients with a diagnosis of rectal cancer who received nCRT in the radiation oncology clinic of our hospital between June 2014 and July 2019 were evaluated. Patient interview information, patient files, and electronic system data were used for data collection. The patients" demographic status, primary diagnosis, disease stage, tumor localization, distance to the anal sphincter, MRI examination, treatment method, treatment response, and final status were noted.
Patients older than 18 years of age with pathological evidence of rectum adenocarcinoma, Eastern Cooperative Oncology Group 1-2, locally advanced stage according to AJCC eighth edition, complete imaging and treatment information, and nCRT treatment were included in the study. Ten patients with missing files, follow-up information, or MRI imaging were excluded from the study. In addition, 21 patients who were prescribed nCRT but were not operated on for any reason were excluded from the study. The remaining 41 patients were included in the study.
Imaging and Treatment Details
Before treatment, all patients were evaluated by the
multidisciplinary treatment council including general
surgery, medical oncology, and radiation oncology.
Digital examination of the rectum, colonoscopy, multislice
triphasic thorax, abdominal, and pelvic computed tomography, endorectal ultrasonography (USG),
and pelvic MRI was ordered in the initial evaluation.
Pelvic MRIs were obtained with pelvic phased-array
coils and 1.5 T MRI. Pelvic MRI consisted of sagittal
fast spin-echo T2-weighted images, coronal short-au
inversion recovery, axial fast spin-echo T2-weighted
images, axial T2-weighted images with fat saturation,
axial T1-weighted images, axial T1-weighted images
with gadolinium, and sagittal T1-weighted images with
gadolinium. Table 1 shows the parameters for pelvic
MRI sequences.
;){kind=link}
Table 1: Technical information on pre-nCRT and post-nCRT MRIs
First, sagittal T2-weighted images were obtained, and after a segment containing tumor tissue was detected, this segment was scanned transversely. EMVI was evaluated with axial T2-weighted images and axial T1-weighted images with gadolinium. On MRI, EMVI is characterized by focal enlargement of the vessel, wall irregularity, and loss of flow void. Diffusion-weighted MRI was not obtained. Fibrosis was evaluated with T2- weighted and post-contrast T1-weighted images.
The nCRT treatment was performed with Varian DHX and IX devices at Kayseri Training and Research Hospital and Kayseri City Hospital. A total dose of 45 Gy with a fraction dose of 180 cGy was administered 5 days a week for 5 weeks. For the radiotherapy (RT) technique, 3-field 3-dimensional conformal RT (3DCRT), double-arc volumetric arc therapy, and 7-field intensity-modulated RT were used. No additional dose was administered to the mesorectum due to the feedback regarding the difficulties experienced in surgical operations due to RT. RT was applied to the rectum and mesorectum as well as to the internal iliac, obturator, and presacral lymph nodes. Capecitabine was administered as a chemotherapy (ChT) agent at a dose of 825 mg/m2 twice a day, 5 days a week concurrent with RT. Patients underwent surgical operation an average of 68 days (range, 33-385 days) after nCRT. Total mesorectal excision (TME) was performed on all patients. Capecitabine plus oxaliplatin, oxaliplatin plus leucovorin plus 5-FU, and capecitabine were administered to the patients as adjuvant ChT. The patients were evaluated before treatment, 1 and 2 months after the end of nCRT, and every 3 months after the operation. During the evaluation, blood tests were performed and the tumor markers carcinoembryonic antigen and carbohydrate antigen 19-9 were evaluated. Abdominal USG and pelvic MRIs were performed for all patients.
Primary and Secondary Endpoints
The primary endpoint of the study was to evaluate
the relationship between mrTRG and pTRG after
treatment. In accordance with the literature, tumor
response grade was divided into five groups for both
pathological and MRI methods.[13,15,16] The grading
paradigms for the Dworak pTRG system and the
mrTRG system are presented in Table 2. Patel et al.[15]
demonstrated the prognostic significance of reassessing
rectal cancers using high-resolution T2-weighted
MRI after completing nCRT.[15] In our study, based
on the previous studies, the MRI response was divided
into two groups: Good response (GR; mrTRG1-2) and
poor response (PR; mrTRG3-5).
;){kind=link}
Table 2: The classification system for mrTRG and pTRG
Similarly, the pathological response was dichotomized as GR (pTRG3-4) and PR (pTRG0-2). [24,25] MRI sensitivity and specificity were evaluated by comparing the MRI-based response assessment with pathological results after neoadjuvant therapy. The secondary endpoint of the study was to evaluate the variables that affect mrTRG and pTRG.
Statistical Analysis
Descriptive statistics for continuous (quantitative) variables
were expressed as mean, standard deviation, minimum-
maximum, and median values, while categorical variables were expressed as number (n) and ratio
(%). Cohen's Kappa analysis was used for mrTRG and
pTRG compatibility (κ<0.20: poor agreement; κ=0.21-
0.40: fair agreement; κ=0.41-0.60: moderate agreement;
κ=0.61-0.80: good agreement; and κ=0.81-1.00:
very good agreement). Non-parametric tests were used
in the study, the Mann-Whitney U-test for statistical
analysis of two independent groups and the Kruskal-
Wallis test for analysis of three or more independent
groups. Significance was evaluated with post hoc analysis
after Bonferroni correction. Chi-square and Fisher's
exact tests were used to calculate the categorical demographic
characteristics of the patients. Analyses were
performed with IBM SPSS Package Program version
24.0 (IBM Corporation, Armonk, NY, USA). Statistical
significance was determined as p<0.05.
Results
The results of 41 patients diagnosed with LARC who received curative treatment in our clinic were evaluated. The patients" median age was 61 years (range, 26-79 years), and 18 (43.9%) were female. All patients had prenCRT and pre-operative comparative functional MRI results. Only 2 patients (4.9%) had high rectal localization, while 19 (46.3%) patients had midrectal localization and 20 (48.8%) patients had low rectal localization. Radiologically, EMVI was positive in 16 (39%) patients on MRI before nCRT, and pathological lymph node (pLN) was positive in 34 (82.9%) patients. A majority of patients underwent 3D-CRT (56.1%, n=23). Patient characteristics and treatment details are summarized in Table 3.;){kind=link}
Table 3: Patient characteristics and treatment details
Radiological Effect of nCRT on EMVI
While 16 patients (39%) had EMVI positivity on prenCRT
MRI, the number of EMVI-positive patients
decreased to 7 (17.1%) on post-nCRT MRI. Although
the number of EMVI-positive patients decreased after
nCRT, the difference was not statistically significant
(p>0.05).
Evaluation of mrTRG and Dworak pTRG Relationship
The relationship between mrTRG and Dworak pTRG
was assessed using the Cohen kappa fit analysis test. A
low level but significant (κ=0.319, p=0.002) compatibility
was observed between pTRG and mrTRG (Table 4).
;){kind=link}
Table 4: Detailed analysis of the relationship between mrTRG and pTRG
GR was observed in 21 (51.2%) patients and PR was observed in 20 (48.8%) patients according to basal images in the post-nCRT MRI. GR was observed in 20 (48.8%) patients and PR was observed in 21 (51.2%) patients based on the pathological evaluation.
When the accuracy of mrTRG in treatment response evaluation was compared with pTRG, mrTRG was determined to have a sensitivity of 90% (18/20), specificity of 14.3% (3/21), positive predictive value of 85.7% (18/21), and negative predictive value of 90% (18/20) (Table 5).
;){kind=link}
Table 5: MRI pathological response relationship after neoadjuvant therapy
Analysis of Variables and pTRG
No significant relationships were found between pTRG
and gender, tumor localization, pre-nCRT EMVI,
post-nCRT EMVI, pre-nCRT pLN, post-nCRT pLN, pre-nCRT T stage, post-nCRT T stage, pre-nCRT N
stage, post-nCRT N stage, pre-nCRT tumor length,
post-nCRT tumor length, pre-nCRT tumor diameter,
post-nCRT tumor diameter, RT technique, pathological subtype, and time between the end of RT and the
operation (p>0.05).
The median age of patients with GR based on pTRG was 57 years (range, 26-73 years), and the median age of patients with PR based on pTRG was 64 years (range, 41-79 years). As age increased, a significantly higher rate of PR was observed (p=0.037) (Fig. 1).
;){kind=link}
Analysis of Variables and mrTRG
No significant relationships were found between
mrTRG and age, gender, tumor location, pre-nCRT
EMVI, post-nCRT EMVI, pre-nCRT pLN, post-nCRT
pLN, pre-nCRT T stage, post-nCRT T stage, prenCRT
N stage, pre-nCRT tumor length, post-nCRT
tumor length, pre-nCRT tumor diameter, post-nCRT tumor diameter, RT technique, pathological subtype,
and time between the end of RT and MRI (p>0.05).
The relationship between response based on mrTRG and post-nCRT N stage was significant (p=0.048); as the N stage progressed, the ratio of patients with PR increased significantly (Table 6).
;){kind=link}
Discussion
The stage of the disease and surgical margins largely determines the prognosis of patients with rectal cancer.[24] In addition, venous invasion, perineural invasion, and tumor grade impact prognosis.[26] EMVI is defined histologically as the involvement of veins other than the muscularis propria.[25] The presence of EMVI is an independent predictor of local or distant recurrence, nodal disease, and lower overall survival. Comparing pre-treatment and post-treatment scans, it has been shown that MRI has a high sensitivity even when advanced histopathological techniques are used to define EMVI.[27] MRI is currently the standard method for post-nCRT local staging of rectal cancer and has demonstrated good accuracy in identifying EMVI.[28] In our study, the prognostic value of EMVI was not examined, but the effect of nCRT on EMVI was examined to emphasize the importance of EMVI presence. The number of EMVI-positive patients decreased when prenCRT and post-nCRT MRIs were compared. The number of patients with positive EMVI on MRI decreased from 16 (39%) pre-nCRT to 7 (17.1%) post-nCRT.In recent years, compatibility between mrTRG and pTRG has been the subject of multiple studies. Particularly in rectal cancer, the watch-and-wait approach has increased the importance of mrTRG. However, mrTRG is not a routinely offered service in every center. In addition, mrTRG findings have not been as consistent as pTRG findings, and studies have produced conflicting results regarding compatibility.
In the study by Siddiqui et al.,[29] mrTRG evaluation of the images of 12 patients by 35 radiologists was compared. Eight radiologists showed very good to near-perfect agreement (? >0.8), 6 showed good agreement (0.8≥ κ>0.6), and 12 showed moderate agreement (0.6≥κ> 0.4). The radiologists identified good responders in 65.9% of cases and poor responders in 90% of cases. Although there was a trend toward good agreement among the radiologists, it is clear that there were still differing assessments. Since our study was retrospective, mrTRG evaluation by a single radiologist was specifically requested. Evaluation of all 41 cases by the same radiologist was deemed appropriate for the stability of the study. The conclusion of the previous study emphasized that radiologists can be taught mrTRG measurement and that good agreement can be achieved between radiologists.
Similar to the differences seen between studies in the evaluation of mrTRG, different results have been obtained regarding the agreement between mrTRG and pTRG. In research investigating the correlation between mrTRG and pTRG, 191 patients were evaluated and mrTRG and pTRG findings were compared in two Phase-II studies (EXPERT and EXPERT-C).[16] Patients were given 4 cycles of induction capecitabine and oxaliplatin (CAPOX) ChT first, and then, capecitabinebased concurrent nCRT (54 Gy in EXPERT; 50.4 Gy in EXPERT-C) was administered. TME was administered 4-6 weeks after the end of nCRT and 4 cycles of adjuvant ChT (capecitabine in EXPERT; CAPOX in EXPERT-C) were given. High-resolution MRI was taken at the end of induction ChT and 4 weeks after concurrent nCRT. The compatibility between mrTRG and pTRG was evaluated by the weighted kappa test. Fair agreement was found between mrTRG and pTRG when the regression was classified according to standard 5-tier systems (κ=0.24) or modified 3-tier systems (κ = 0.25). The sensitivity and specificity of mrTRG1-2 (complete/good radiological regression) for the prediction of pathological complete response (pCR) were 74.4% (95% confidence interval [CI]: 58.8-86.5) and 62.8% (95% CI: 54.5-70.6), respectively. The study concluded that the compatibility between mrTRG and pTRG was low and that mrTRG could not be used as a proxy for pTRG. It was emphasized that mrTRG can provide complementary prognostic information to pTRG for improved post-operative risk stratification and identify complete pathological responders for adopting non-operative management strategies, with the need for further studies on this topic highlighted. In another study, the MRIs of 65 patients were evaluated to quantitatively assess the percentage of fibrosis developing in LARC after nCRT.[17] The patients were followed for 30 months. Fibrosis percentage was measured on T2-weighted images, and mrTRG classes were determined and compared with histopathological pTRG. The compatibility between pTRG and mrTRG was determined to be perfect (κ=0.923). The automated measurement of fibrosis detected by MRI has thus been recorded as feasible and reproducible. Significant agreement was found in our study between mrTRG and pTRG (p=0.002), though the agreement was low (κ=0.319). When compared to Sclafani et al.,[16] the number of patients in our study was markedly less. In addition, in our study, RT dose was 45 Gy, capecitabine was used as the standard ChT, and only standard 5-tier systems were used. Despite differences in methodology, our study results were similar to those of Sclafani et al.[16] in terms of the low agreement measured between mrTRG and pTRG. Our sample size of 41 was more similar to the sample size of 65 in Rengo et al.,[17] though very different results were obtained in the compatibility of mrTRG and pTRG grades. Rengo et al.[17] measured the percentage of fibrosis on T2- weighted images using the automated k-means clustering algorithm. In our study, the percentage of fibrosis was measured visually on T2-weighted MRIs by the radiologist. The reason for the differences between the two studies may be due to the differences in methodology for measuring the percentage of fibrosis.
A different approach has been employed by Ko et al.[18] In their study, 102 patients who underwent an endoscopy and MRI 2-4 weeks after nCRT were examined retrospectively.[18] A confidence interval (1-4) was established for endoscopy and MRI evaluations. Accuracy, sensitivity, and specificity were analyzed based on the findings of endoscopy, MRI, and a combination method. Patients simultaneously received a total of 50.4 Gy RT from 3 to 4 fields (45 Gy pelvic and 5.4 Gy boost) and capecitabine, and pCR was achieved in 17 (16.7%) of 102 patients. The accuracy, sensitivity, and specificity of pCR prediction from biopsy and endoscopy were 85.3%, 52.9%, and 91.8%, respectively, while from MRI, they were 91.2%, 70.6%, and 95.3%, respectively. With combined endoscopy and MRI, accuracy, sensitivity, and specificity were 89.2%, 52.9%, and 96.5%, respectively. No significant differences were found in the sensitivity and specificity of each method. The pCR prediction rate using the combination method was 92.6% after the final probability test. The study showed that the combination of endoscopic biopsy and MRI could positively predict pCR in patients with rectal cancer after nCRT.
No consensus has thus far been reached on the utility of mrTRG. In fact, mrTRG is not routinely evaluated in all centers. Therefore, more training and further studies are needed. In our study, we retrospectively investigated the compatibility of mrTRG and pTRG with a small patient group. Although compatibility was found to be low, these results are not decisive, as differing results have been obtained in other studies. At this stage, mrTRG cannot replace pTRG, but has prognostic value in the watch-and-wait patient group whose operations are delayed.
Limitations of the Study
The limitations of our study are the small number of
patients and the single-center and retrospective study
design. However, the evaluation of mrTRG by a single
radiologist and the evaluation of pTRG by a single
pathologist, as well as the consistent ChT agent and
dosage used were considered strengths of the study in
terms of data balance.
Conclusion
As age increased, pTRG was negatively affected; as the post-nCRT N stage increased, mrTRG was negatively affected. There was compatibility between mrTRG and pTRG, as expected, but this compatibility was found to be low. A standard should be established for more reliable mrTRG evaluation, and further studies should be performed.Peer-review: Externally peer-reviewed.
Conflict of Interest: All authors declared no conflict of interest.
Ethics Committee Approval: Institutional Review Board approval was obtained for this study. The study was approved by the Non-Interventional Clinical Research Ethics Committee of Erciyes University Faculty of Medicine (No: 2019/837, Date: 11/12/2019).
Financial Support: None declared.
Authorship contributions: Concept - A.A., G.T., İ.P.A.; Design - A.A., S.K.E., İ.P.A.; Supervision - A.A.; Funding - None; Materials - A.A., G.T., E.A.; Data collection and/or processing - A.A., G.T., N.Ö., E.A., S.K.E.; Data analysis and/ or interpretation - A.A., G.T., E.A.; Literature search - A.A., G.T., N.Ö., E.A., S.K.E.; Writing - A.A., N.Ö., İ.P.A.; Critical review - A.A.
References
1) Horvat N, Petkovska I, Gollub MJ. MR ımaging of rectal
cancer. Radiol Clin N Am 2018;56:75.
2) Gollub MJ, Arya S, Beets-Tan RG, DePrisco G, Gonen
M, Jhaveri K, et al. Use of magnetic resonance
imaging in rectal cancer patients: Society of Abdominal
Radiology (SAR) rectal cancer disease-focused
panel (DFP) recommendations 2017. Abdom Radiol
2018;43(11):2893-902.
3) Horvat N, Rocha CC, Oliveira BC, Petkovska I, Gollub
MJ. MRI of rectal cancer: Tumor staging, ımaging
techniques, and management. Radiographics.
2019;39:367-87.
4) Sauer R, Becker H, Hohenberger W, Rödel C, Wittekind
C, Fietkau R, et al. Pre-operative versus postoperative
chemoradiotherapy for rectal cancer. N Engl J
Med 2004;351(17):1731-40.
5) Lambregts DM, Boellaard TN, Beets-Tan RG. Response
evaluation after neoadjuvant treatment for
rectal cancer using modern MR imaging: A pictorial
review. Insights Imaging 2019;10(1):15.
6) Braun OM, Neumeister B, Popp W, Scherrer R, Dobrowsky
E, Dobrowsky W, et al. Histologic tumor
regression grades in squamous cell carcinoma of the
head and neck after pre-operative radiochemotherapy.
Cancer 1989;63(6):1097-100.
7) Mandard AM, Dalibard F, Mandard JC, Marnay J,
Henry?Amar M, Petiot JF, et al. Pathologic assessment
of tumor regression after pre-operative chemoradiotherapy
of esophageal carcinoma. Clinicopathologic
correlations. Cancer 1994;73(11):2680-6.
8) Rödel C, Grabenbauer GG, Kühn R, Papadopoulos
T, Dunst J, Meyer M, et al. Combined-modality
treatment and selective organ preservation in invasive
bladder cancer: Long-term results. J Clin Oncol
2002;20(14):3061-71.
9) Becker K, Mueller JD, Schulmacher C, Ott K, Fink
U, Busch R, et al. Histomorphology and grading of
regression in gastric carcinoma treated with neoadjuvant
chemotherapy. Cancer 2003;98(7):1521-30.
10) Dhadda AS, Dickinson P, Zaitoun AM, Gandhi N,
Bessell EM. Prognostic importance of Mandard tumor
regression grade following pre-operative chemo/
radiotherapy for locally advanced rectal cancer. Eur J Cancer 2011;47(8):1138-45.
11) Fokas E, Liersch T, Fietkau R, Hohenberger W, Beissbarth
T, Hess C, et al. Tumor regression grading after
pre-operative chemoradiotherapy for locally advanced
rectal carcinoma revisited: Updated results of the CAO/
ARO/AIO-94 trial. J Clin Oncol 2014;32(15):1554-62.
12) Rodel C, Martus P, Papadoupolos T. Prognostic significant
for tumor regression after pre-operative
chemoradiotherapy for rectal cancer. J Clin Oncol
2005;23(34):8688-96.
13) Dworak O, Keilholz L, Hoffmann A. Pathological
features of rectal cancer after pre-operative radiochemotherapy.
Int J Colorectal Dis 1997;12(1):19-23.
14) AJCC Cancer Stagıng Manual. 7th ed. Germany:
Springer; 1997. p. 152.
15) Patel UB, Blomqvist LK, Taylor F, George C, Guthrie
A, Bees N, et al. MRI after treatment of locally advanced
rectal cancer: How to report tumor response-
the MERCURY experience. AJR Am J Roentgenol
2012;199(4):486-95.
16) Sclafani F, Brown G, Cunningham D, Wotherspoon
A, Mendes LS, Balyasnikova S, et al. Comparison
between MRI and pathology in the assessment of
tumor regression grade in rectal cancer. Br J Cancer
2017;117(10):1478-85.
17) Rengo M, Picchia S, Marzi S, Bellini D, Caruso D,
Caterino M, et al. Magnetic resonance tumor regression
grade (MR-TRG) to assess pathological complete
response following neoadjuvant radiochemotherapy
in locally advanced rectal cancer. Oncotarget
2017;8(70):114746-55.
18) Ko HM, Choi YH, Lee JE, Lee KH, Kim JY, Kim JS.
Combination assessment of clinical complete response
of patients with rectal cancer following chemoradiotherapy
with endoscopy and magnetic resonance
ımaging. Ann Coloproctol 2019;35(4):202-8.
19) Betge J, Pollheimer MJ, Lindtner RA, Kornprat P, Schlemmer
A, Rehak P, et al. Intramural and extramural
vascular invasion in colorectal cancer: Prognostic significance
and quality of pathology reporting. Cancer
2012;118(3):628-38.
20) Smith NJ, Shihab O, Arnaout A, Swift RI, Brown G.
MRI for detection of extramural vascular invasion in
rectal cancer. AJR Am J Roentgenol 2008;191:1517-22.
21) Bugg WG, Andreou AK, Biswas D, Toms AP, Williams
SM. The prognostic significance of MRI-detected extramural
venous invasion in rectal carcinoma. Clin
Radiol 2014;69(6):619-23.
22) Sohn B, Lim JS, Kim H, Myoung S, Choi J, Kim NK,
et al. MRI-detected extramural vascular invasion is
an independent prognostic factor for synchronous
metastasis in patients with rectal cancer. Eur Radiol 2015;25(5):1347-55.
23) Sun Y, Li J, Shen L, Wang X, Tong T, Gu, Y. Predictive
value of MRI-detected extramural vascular invasion
in stage T3 rectal cancer patients before neoadjuvant
chemoradiation. Diagn Interv Radiol 2018;24(3):128-34.
24) Balch GC, De Meo A, Guillem JG. Modern management
of rectal canser: A 2006 update. World J Gastroenterol
2006;12(20):3186-95.
25) Taylor FG, Swift RI, Blomqvist L, Brown G. A systematic
approach to the interpretation of pre-operative staging
MRI for rectal cancer. AJR 2008;191(6):1827-35.
26) Huh JW, Lee JH, Kim HR, Kim YJ. Prognostic significance
of lymphovascular or perineural invasion in
patients with locally advanced colorectal cancer. Am J Surg 2013;206(5):758-63.
27) Jhaveri KS, Hosseini-Nik H, Thipphavong S, Assarzadegan
N, Menezes RJ, Kennedy ED, et al. MRI
detection of extramural venous ınvasion in rectal
cancer: Correlation with histopathology using Elastin
Stain. AJR Am J Roentgenol 2016;206(4):747-55.