Glasgow Prognostic Score (GPS) Can Be a Useful Indicator to Determine Prognosis of Patients With Colorectal Carcinoma

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Int Surg 2014;99:512 517 DOI: 10.9738/INTSURG-D-13-00118.1 Glasgow Prognostic Score (GPS) Can Be a Useful Indicator to Determine Prognosis of Patients With Colorectal Carcinoma Tadahiro Nozoe, Rumi Matono, Hideki Ijichi, Takefumi Ohga, Takahiro Ezaki Department of Surgery, Fukuoka Higashi Medical Center, Koga, Japan The Glasgow Prognostic Score (GPS), an inflammation-based score, has been used to predict the biologic behavior of malignant tumors. The aim of the current study was to elucidate a further significance of GPS in colorectal carcinoma. Correlation of GPS and modified GPS (mgps), which are composed of combined score provided for serum elevation of C-reactive protein and hypoalbuminemia examined before surgical treatment, with clinicopathologic features was investigated in 272 patients with colorectal carcinoma. Survival of GPS 1 patients was significantly worse than that of GPS 0 patients (P ¼ 0.009), and survival of GPS 2 patients was significantly worse than that of GPS 1 patients (P, 0.0001). Similarly, survival of mgps 1 patients was significantly worse than that of mgps 0 patients (P ¼ 0.009), and survival of mgps 2 patients was significantly worse than that of mgps 1 patients (P ¼ 0.0006). Multivariate analysis demonstrated that GPS (P, 0.0001) as well as tumor stage (P¼0.004) and venous invasion (P ¼ 0.011) were factors independently associated with worse prognosis. Both GPS and mgps could classify outcome of patients with a clear stratification, and could be applied as prognostic indicators in colorectal carcinoma. Key words: Colorectal carcinoma Glasgow prognostic score (GPS) Prognostic indicator Although many tumor-environmental elements, including both tumor-related and host-related factors, have been linked with tumor progression, host inflammatory response is one of the more important factors that has a role in the progression and/or development of tumors. 1 Serum elevation of C-reactive protein (CRP), an acute phase protein, has been shown to be a prognostic indicator in a variety of neoplasms, including colorectal carcinoma. 2 5 Moreover, hypoalbuminemia brought about by malnutrition and related to cachexic condition has been reported to Reprint requests: Tadahiro Nozoe, Department of Surgery, Fukuoka Higashi Medical Center, 1-1-1, Chidori, Koga, 811-3195, Japan. Tel.: þ81 92 943 2331; Fax: þ81 92 943 8775; E-mail: paper7777@yahoo.co.jp or nozoet@fukuokae2.hosp.go.jp 512 Int Surg 2014;99

GPS IN COLORECTAL CARCINOMA NOZOE Table 1 Relationship between GPS and patients clinicopathologic characteristics GPS 0 (n ¼ 179) GPS 1 (n ¼ 62) GPS 2 (n ¼ 31) P value Sex Male 105 (58.7) 35 (56.5) 20 (64.5) 0.756 Female 74 (41.3) 27 (43.5) 11 (35.5) Age 69.8 6 11.0 70.4 6 12.5 71.3 6 9.1 0.130 Location of tumor Colon 121 (67.6) 47 (75.8) 25 (80.6) 0.212 Rectum 58 (32.4) 15 (24.2) 6 (19.4) Depth of tumor T1 31 (17.3) 3 (4.8) 0,0.0001 T2 36 (20.1) 8 (12.9) 1 (3.2) T3 111 (62.0) 48 (77.5) 26 (83.9) T4 1 (0.6) 3 (4.8) 4 (12.9) Histology Well 60 (33.5) 15 (24.2) 7 (22.6) 0.127 Moderately 110 (61.5) 41 (66.1) 19 (61.3) Poorly 9 (5.0) 6 (9.7) 5 (16.1) Nodal metastasis No 107 (59.8) 33 (53.2) 12 (38.7) 0.083 Yes 72 (40.2) 29 (46.8) 19 (61.3) Lymphatic invasion No 107 (59.8) 40 (64.5) 13 (41.9) 0.103 Yes 72 (40.2) 22 (35.5) 18 (58.1) Venous invasion No 138 (77.1) 46 (74.2) 23 (74.2) 0.868 Yes 41 (22.9) 16 (25.8) 8 (25.8) Tumor stage I 59 (33.0) 10 (16.1) 0 0.0009 II 46 (25.7) 20 (32.3) 12 (38.7) III 59 (33.0) 21 (33.9) 12 (38.7) IV 15 (8.3) 11 (17.7) 7 (22.6) Resection Curative 164 (91.6) 51 (82.3) 24 (77.4) 0.025 Noncurative 15 (8.4) 11 (17.7) 7 (22.6) Proportion of lymphocytes in the peripheral blood, % 29.6 6 9.1 24.4 6 10.0 17.8 6 7.0,0.0001 GPS, Glasgow Prognostic Score. Values in parentheses are percentages. be correlated with an unfavorable prognosis of some gastrointestinal tumors. 6,7 The Glasgow prognostic score (GPS), which is a cumulative inflammation-based cancer-prognostic marker composed of serum elevation of CRP and decrease in albumin concentration, is likely to reflect host systemic inflammatory response and has been reported to be significant as a prognostic indicator in cancer-bearing patients. 8 10 Moreover, it has been found that hypoalbuminemia alone is unlikely to be associated with reduced survival likelihood in patients with colorectal carcinoma 11 ; therefore, the GPS has been modified (mgps), providing a score of 1 only for a case with serum elevation of CRP, and score of 0 for a case only with hypoalbuminemia or where neither was elevated. Although, until now, there have been some reports regarding the significance of GPS as a prognostic indicator in colorectal carcinoma, 9,11 16 the aim of this study was to elucidate further the significance of GPS and mgps in colorectal carcinoma. Patients and Methods Patients, collection of blood samples, and laboratory measurement Two hundred and seventy-two patients with colorectal carcinoma that had been treated by resection Int Surg 2014;99 513

NOZOE GPS IN COLORECTAL CARCINOMA Clinicopathologic investigation The clinicopathologic factors were determined according to the TNM classification of malignant tumors prescribed by the International Union Against Cancer. 17 Follow-up for the patients Fig. 1 Comparison of the patients survival between GPS 0, 1, and 2. Significant differences were observed between GPS 0 and GPS 1 patients (P ¼ 0.009) and between GPS 1 and GPS 2 patients (P, 0.0001). and lymph node dissection in our institute from 2003 to 2012 were included in this study. Patients who have had malignant tumors in other organs or have been suffering from other chronic inflammatory diseases causing serum elevation of CRP were excluded from this study. Patient ages ranged from 24 to 90 years, with a mean of 70.4, and were composed of 160 men and 112 women. No neoadjuvant therapy had been given for the patients who had been enrolled in this study. All blood samples were collected and the laboratory measurements of serum values of CRP and albumin were performed just before the operation. Patients who had both a serum elevation of CRP (.1.0 mg/dl) and hypoalbuminemia (,3.5 g/dl) were allocated a GPS of 2. Patients with only one of the abnormal values were allocated a GPS of 1, and patients who had neither were allocated a GPS of 0. Moreover, patients who had both abnormal values were allocated an mgps of 2. Patients who had only serum elevation of CRP but not hypoalbuminemia were allocated an mgps of 1, and patients who had neither or only hypoalbuminemia were allocated a mgps of 0. Correlation of preoperative values of GPS and mgps with clinicopathologic characteristics were examined. The follow-up for patients was continued until their death, and only patients who died of colorectal carcinoma were included in the tumor-related deaths. The period from the operation to the date of death was defined to be the survival time. The interval of the follow-up after operation ranged from 2 months to 8 years and 5 months. Statistical analysis All statistical analyses were performed using Stat- View (SAS Institute Inc, Cary, NC). Chi-square and t tests were used to compare the difference regarding values in each GPS score. Survival curves were made by the Kaplan-Meier method, and the Mantel- Cox test was used to analyze the equality of the survival curves. The Cox proportional hazards model in a forward stepwise manner was used in the multivariate analysis to determine the independent prognostic indicators. P, 0.05 was considered significant. Results The relationship between GPS and clinicopathologic features is shown in Table 1. Significant differences were observed regarding depth of tumor (P, 0.0001), stage of the tumors (P ¼ 0.0009), and the proportion of curative resection (P ¼ 0.025). Additionally, a significant correlation of GPS with the proportion of lymphocytes in the peripheral blood was also found (P, 0.0001). The prognosis of GPS 1 patients (a 5-year survival rate of 74.9%) was significantly worse than that of GPS 0 patients [a 5-year survival rate of 92.6% (P ¼ 0.009)]; the prognosis of GPS 2 patients (a 5-year survival rate of 35.2%) was significantly worse than that of GPS 1 patients (P, 0.0001; Fig. 1). Next, the relationship between mgps and clinicopathologic features is shown in Table 2. Similarly, significant differences were found for depth of tumor (P, 0.0001), stage of the tumors (P ¼ 0.0004), the proportion of curative resection (P ¼ 514 Int Surg 2014;99

GPS IN COLORECTAL CARCINOMA NOZOE Table 2 Relationship between mgps and patients clinicopathologic characteristics mgps 0 (n ¼ 202) mgps 1 (n ¼ 39) mgps 2 (n ¼ 31) P value Sex Male 118 (58.4) 22 (56.4) 20 (64.5) 0.770 Female 84 (41.6) 17 (43.6) 11 (35.5) Age 70.2 6 11.4 68.7 6 11.7 71.3 6 9.1 0.060 Location of tumor Colon 138 (68.3) 30 (76.9) 25 (80.6) 0.251 Rectum 64 (31.7) 9 (23.1) 6 (19.4) Depth of tumor T1 34 (16.8) 0 0,0.0001 T2 38 (18.8) 6 (15.4) 1 (3.2) T3 128 (63.4) 31 (79.5) 26 (83.9) T4 2 (1.0) 2 (5.1) 4 (12.9) Histology Well 66 (32.7) 9 (23.1) 7 (22.6) 0.166 Moderately 125 (61.9) 26 (66.7) 19 (61.3) Poorly 11 (5.4) 4 (10.2) 5 (16.1) Nodal metastasis No 120 (59.4) 20 (51.3) 12 (38.7) 0.080 Yes 82 (40.6) 19 (48.7) 19 (61.3) Lymphatic invasion No 124 (61.4) 23 (59.0) 13 (41.9) 0.123 Yes 78 (38.6) 16 (41.0) 18 (58.1) Venous invasion No 155 (76.7) 29 (74.4) 23 (74.2) 0.918 Yes 47 (23.3) 10 (25.6) 8 (25.8) Tumor stage I 64 (31.7) 5 (12.8) 0 0.0004 II 53 (26.2) 13 (33.3) 12 (38.7) III 68 (33.7) 12 (30.8) 12 (38.7) IV 17 (8.4) 9 (23.1) 7 (22.6) Resection Curative 185 (91.6) 30 (76.9) 24 (77.4) 0.006 Noncurative 17 (8.4) 9 (23.1) 7 (22.6) Proportion of lymphocytes in the peripheral blood, % 29.5 6 9.4 22.0 6 8.4 17.8 6 7.0,0.0001 mgps, modified Glasgow Prognostic Score. Values in parentheses are percentages. 0.006), and lymphocyte proportion in the peripheral blood (P, 0.0001). The prognosis of mgps 1 patients (a 5-year survival rate of 72.9%) was significantly worse than that of mgps 0 patients [a 5-year survival rate of 91.5% (P ¼ 0.009)]; the prognosis of mgps 2 patients (a 5-year survival rate of 35.2%) was significantly worse than that of mgps 1 patients (P ¼ 0.0006; Fig. 2). While patients with GPS 0 or 1 are in accordance with those with mgps 0 or 1, multivariate analysis was performed by dividing GPS 2 or mgps 2 and others. This analysis revealed that GPS (P, 0.0001) as well as tumor stage (P ¼ 0.004) and venous invasion (P ¼ 0.011) proved to be factors independently associated with a worse prognosis for the patient (Table 3). Discussion GPS, which comprises solely serum concentrations of CRP and albumin, has been established as an inflammation-based score to predict the extent of aggression of the tumor and/or the prognosis of patients. It it used for a variety of malignant tumors, including carcinomas of the gastrointestinal tract 11,18 and other organs. 19,20 Int Surg 2014;99 515

NOZOE GPS IN COLORECTAL CARCINOMA Table 3 Variable Factors independently correlated with the prognosis Odds ratio (95% confidence interval) P value GPS, mgps (0, 1 versus 2) 7.41 (3.66 15.2),0.0001 Stage of tumor (I, II versus III, IV) 3.94 (1.54 10.1) 0.004 Venous invasion 2.25 (1.15 4.41) 0.011 GPS, Glasgow Prognostic Score; mgps, modified Glasgow Prognostic Score. Fig. 2 Comparison of the patients survival between mgps 0, 1, and 2. Significant differences were observed between mgps 0 and mgps 1 patients (P ¼ 0.009) and between mgps 1 and mgps 2 patients (P ¼ 0.0006). Initially, this combination of the clinical data of serum elevation of CRP and hypoalbuminemia was applied to possibly determine the prognosis of patients with inoperative lung cancer. 21 Thereafter, to the best of the authors knowledge, this criteria, termed GPS, has come to be used to assess the outcome of patients with malignant tumors. 19 It has been reported that GPS is a marker for the incidence of distant metastasis in colorectal carcinoma 14 and is also a significant prognostic indicator for colorectal carcinoma. 9,12 However, in an investigation by McMillan et al. 11 regarding the significance of GPS in colorectal carcinoma, survival of patients with a GPS of 1 derived from hypoalbuminemia proved to be much better than that of patients with a GPS of 1 derived from serum elevation of CRP. Therefore, patients with hypoalbuminemia but without serum elevation of CRP were classified as GPS 0, and this criteria has been come to be used as a modified GPS (mgps) to chiefly investigate the biologic behavior of colorectal carcinoma. A series of further investigations also demonstrated that mgps has proven to be a significant prognostic indicator in colorectal carcinoma. 11,13,15,16 In the current study, both GPS and mgps proved to be significant as independent prognostic indicators in colorectal carcinoma. Close correlation of serum elevation of CRP with a decrease in lymphocyte percentage in the peripheral blood, 22 which was also shown in this study, and with a decrease in T lymphocyte infiltration in patients with colorectal carcinoma 23 was previously reported. Although it should be appreciated that the identification of hypoalbuminemia in cancer-bearing patients depends on the systemic inflammatory response, 18 and the independent significance of hypoalbuminemia in determining a prognosis in colorectal carcinoma might be less reliable, 11 it has been known to be associated with an impaired immune response through macrophage activation. 24 Additionally, in the current study, a significant correlation of GPS with a decrease in the proportion of lymphocytes in the peripheral blood of the patients was found. Taken together from the panel of our investigations, GPS also has an important significance as an indicator of the nutritional and immunologic host response in patients with colorectal carcinoma. In conclusion, both GPS and mgps could be easy and useful tools to predict the outcome of patients with colorectal carcinoma. References 1. Roxburgh CS, McMillan DC. Role of systemic inflammatory response in predicting survival in patients with primary operable cancer. Future Oncol 2010;6(1):149 163 2. Nozoe T, Matsumata T, Kitamura M, Sugimachi K. Significance of preoperative elevation of serum C-reactive protein as an indicator for prognosis in colorectal cancer. Am J Surg 1998; 176(4):335 338 3. Nozoe T, Saeki H, Sugimachi K. Significance of preoperative elevation of serum C-reactive protein as an indicator of prognosis in esophageal carcinoma. Am J Surg 2001;182(2): 197 201 4. Nozoe T, Mori E, Takahashi I, Ezaki T. Preoperative elevation of serum C-reactive protein as an independent prognostic indicator of colorectal carcinoma. Surg Today 2008;38(7):597 602 5. Nozoe T, Iguchi T, Adachi E, Matsukuma A, Ezaki T. Preoperative elevation of serum C-reactive protein as an 516 Int Surg 2014;99

GPS IN COLORECTAL CARCINOMA NOZOE independent prognostic indicator for gastric cancer. Surg Today 2011;41(4):510 513 6. Lien YC, Hsieh CC, Wu YC, Hsu HS, Hsu WH, Wang LS et al. Preoperative serum albumin level is a prognostic indicator for adenocarcinoma of the gastric cardia. J Gastrointest Surg 2004; 8(8):1041 1048 7. Lai CC, You JF, Yeh CY, Chen JS, Tang R, Wang JY et al. Low preoperative serum albumin in colon cancer: a risk factor for poor outcome. Int J Colorectal Dis 2011;26(4):473 481 8. Proctor MJ, Morrison DS, Talwar D, Balmer SM, O Reilly DS, Foulis AK et al. An inflammation-based prognostic score (mgps) predicts cancer survival independent of tumour site: a Glasgow Inflammation Outcome Study. Br J Cancer 2011; 104(4):726 734 9. Read JA, Choy ST, Beale PJ, Clarke SJ. Evaluation of nutritional and inflammatory status of advanced colorectal cancer patients and its correlation with survival. Nutr Cancer 2006; 55(1):78 85 10. Nozoe T, Iguchi T, Egashira A, Adachi E, Matsukuma A, Ezaki T. Significance of modified Glasgow prognostic score as a useful indicator for prognosis of patients with gastric carcinoma. Am J Surg 2011;201(2):186 191 11. McMillan DC, Crozier JE, Canna K, Angerson WJ, McArdle CS. Evaluation of an inflammation-based prognostic score (GPS) in patients undergoing resection for colon and rectal cancer. Int J Colorectal Dis 2007;22(8):881 886 12. Ishizuka M, Nagata H, Takagi K, Horie T, Kubota K. Inflammation-based prognostic score is a novel predictor of postoperative outcome in patients with colorectal cancer. Ann Surg 2007;246(6):1047 1051 13. Roxburgh CS, Salmond JM, Horgan PG, Oien KA, McMillan DC. Comparison of the prognostic value of inflammationbased pathologic and biochemical criteria in patients undergoing potentially curative resection for colorectal cancer. Ann Surg 2009;249(5):788 793 14. Ishizuka M, Nagata H, Takagi K, Kubota K. Systemic inflammatory response associated with distant metastasis of T1 or T2 colorectal cancer. Dig Dis Sci 2010;55(11):3181 3187 15. Richards CH, Leitch EF, Horgan PG, Anderson JH, McKee RF, McMillan DC. The relationship between patient physiology, the systemic inflammatory response and survival in patients undergoing curative resection of colorectal cancer. Br J Cancer 2010;103(9):1356 1361 16. Roxburgh CS, Wallace AM, Guthrie GK, Horgan PG, Mc- Millan DC. Comparison of the prognostic value of tumourand patient-related factors in patients undergoing potentially curative surgery for colon cancer. Colorectal Dis 2010;12(10): 987 994 17. Sobin L, Gospodarowicz M, Wittekind C, eds. International Union Against Cancer TNM Classification of Malignant Tumours. 7th ed. New York, NY: Wiley-Blackwell, 2009:100 105 18. Crumley AB, Stuart RC, McKernan M, McMillan DC. Is hypoalbuminemia an independent prognostic factor in patients with gastric cancer? World J Surg 2010;34(10):2393 2398 19. Forrest LM, McMillan DC, McArdle CS, Angerson WJ, Dunlop DJ. Comparison of an inflammation-based prognostic score (GPS) with performance status (ECOG) in patients receiving platinum-based chemotherapy for inoperable non-small-cell lung cancer. Br J Cancer 2004;90(9):1704 1706 20. Polterauer S, Grimm C, Seebacher V, Rahhal J, Tempfer C, Reinthaller A et al. The inflammation-based Glasgow Prognostic Score predicts survival in patients with cervical cancer. Int J Gynecol Cancer 2010;20(6):1052 1057 21. Forrest LM, McMillan DC, McArdle CS, Angerson WJ, Dunlop DJ. Evaluation of cumulative prognostic scores based on the systemic inflammatory response in patients with inoperable non-small-cell lung cancer. Br J Cancer 2003;89(6):1028 1030 22. Nozoe T, Matsumata T, Sugimachi K. Preoperative elevation of serum C-reactive protein is related to impaired immunity in patients with colorectal cancer. Am J Clin Oncol 2000;23(3):263 266 23. Canna K, McArdle PA, McMillan DC, McNicol AM, Smith GW, McKee RF et al. The relationship between tumour T- lymphocyte infiltration, the systemic inflammatory response and survival in patients undergoing curative resection for colorectal cancer. Br J Cancer 2005;92(4):651 654 24. Rivadeneira DE, Grobmyer SR, Naama HA, Mackrell PJ, Mestre JR, Stapleton PP et al. Malnutrition-induced macrophage apoptosis. Surgery 2001;129(5):617 625 Int Surg 2014;99 517