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[Chinese Journal of Cancer 28:3, 240-244; March 2009]; ©2009 Landes Bioscience Clinical Research Paper Prognostic value of serum CA19-9 in patients with advanced pancreatic cancer receiving gemcitabine based chemotherapy Xin An, Yu-Hong Li,* Xu-Bin Lin, Feng-Hua Wang, Fen Feng, Rui-Hua Xu, Wen-Qi Jiang and You-Jian He State Key Laboratory of Oncology in South China; Guangzhou, Guangdong P.R. China; and Department of Medical Oncology; Cancer Center; Sun Yat-sen University; Guangzhou, Guangdong P.R. China Key words: pancreatic cancer, chemotherapy, gemcitabine, serum CA19-9, treatment efficacy, prognostic factor Background and Objective: Gemcitabine is used as an effective drug for patients with advanced pancreatic cancer. Serum CA19-9 has been proven as the most sensitive and specific serum marker for pancreatic cancer. This study was to investigate the value of serum CA19-9 in evaluating treatment efficacy and predicting prognosis of patients with pancreatic cancer treated by gemcitabine-based chemotherapy. Methods: Seventy-one patients with histologically confirmed, locally advanced or metastatic pancreatic adenocarcinoma, whose Karnofsky’s performance status (KPS) score was ≥ 70 were treated with gemcitabine alone or with gemcitabine-based chemotherapy. CA19-9 was measured before and after chemotherapy. Results: Ten out of 71 patients had normal baseline CA19-9 levels, and 61 patients had increased baseline CA19-9 levels. The overall survival of patients were similar between the two groups, which were 9.0 months and 7.9 months, respectively (p = 0.797). The median baseline CA19-9 level for patients who had increased CA19-9 was (682 ± 558) U/mL before treatment. Patients whose pretreatment CA19-9 levels were < 682 U/mL achieved better survival than those whose pretreatment CA19-9 levels were ≥ 682 U/mL (9.6 months vs. 5.1 months, p = 0.001). In addition, patients with a pretreatment CA19-9 level of < 682 U/ mL had a better tumor response (43.5% vs. 15.8%, p = 0.051) and clinical benefit response (48.1% vs. 29.2%, p = 0.125) than those whose pretreatment CA19-9 level was < 682 U/mL, but the differences were not significant. Patients with a fall of ≥25% in the baseline CA19-9 level after chemotherapy achieved a longer median overall survival (10.2 months vs. 5.0 months, p *Correspondence to: Yu-Hong Li; State Key Laboratory of Oncology in South China; and Department of Medical Oncology; Cancer Center; Sun Yat-sen University; Guangzhou, Guangdong 510060 P.R. China; Tel.: 86.20.87343486; Email: [email protected] Submitted: 06/24/08; Revised: 10/24/08; Accepted: 11/05/08 This paper was translated into English from its original publication in Chinese. Translated by: Xinglin Meditrans Center (http://www.58medtrans.com) and Hua He on 02/20/09. The original Chinese version of this paper is published in: Ai Zheng (Chinese Journal of Cancer), 28(3); http://www.cjcsysu.cn/cn/article.asp?id=15113 Previously published online as a Chinese Journal of Cancer E-publication: http://www.landesbioscience.com/journals/cjc/article/8650 240 < 0.001), better tumor response (47.8% vs. 10.5%, p = 0.002) and better clinical benefit response (69.2% vs. 8.0%, p = 0.000) than those without a decrease of baseline CA19-9 or with a fall of < 25%. Multivariate analysis revealed that the baseline CA19-9 level before chemotherapy, decreased percentage of the CA19-9 level after chemotherapy, and the differentiation degree of tumor cells were independent risk factors for patients whose baseline CA19-9 levels were increased. Conclusion: The level of pretreatment base-line CA19-9 and the decreased percentage of baseline CA19-9 after chemotherapy are of predictive values for survival of patients with advanced pancreatic cancer undergoing gemcitabine-based chemotherapy and with an increased level of baseline CA19-9. Pancreatic cancer is one of the most common malignances in China, with an increasing incidence rate in recent years. It often has latent onset and is seldom accompanied with specific symptoms and body signs. Once diagnosed, less than 20% of these patients have surgical opportunity. Even if radical surgical resection is performed, the recurrence and metastatic rates remain as high as 85%. For locally advanced, recurrent, and metastatic pancreatic cancer, gemcitabine monotherapy is the standard front-line chemotherapy. However the median survival of patients receiving this regimen is only 5 to 10 months.1,2 Serum carbohydrate antigen 19-9 (CA19-9) is a tumor-associated antigen which has been shown to be a highly specific and sensitive serum marker for pancreatic cancer, thus it is recommended for the diagnosis, staging, and postoperative surveillance of patients with pancreatic cancer.3,4 A few studies showed that the level of serum CA19-9 could predict the survival for patient with advanced pancreatic cancer undergoing systemic chemotherapy, although the results are disparate. This study was to determine the value of serum CA19-9 in evaluating therapeutic efficacy and predicting prognosis in pancreatic cancer treated with gemcitabine-based regimens. Patients and Methods Study subjects. A total of 71 patients with unresectable or metastatic pancreatic adenocarcinoma treated at Sun-Yet Sun University Cancer Center from January 2000 to January 2008 were enrolled. All patients met the following criteria: 1) Pathologically confirmed pancreatic cancer; 2) No history of previous treatment and Chinese Journal of Cancer 2009; Vol. 28 Issue 3 Prognostic value of serum CA19-9 in patients with advanced pancreatic cancer receiving gemcitabine based chemotherapy receiving first-line gemicitabine based chemotherapy; 3) Karnofsky performers status (KPS) score ≥ 70; 4) Dynamic measurement of serum CA19-9 before and after chemotherapy; 5) No jaundice. The median age of patients was 55 years (40–79 years). Fortyseven patients were males and 24 were females. The primary tumor was located in pancreatic head in 21 cases, in pancreatic body and tail in 49 cases, and in the whole pancreas in one patient. Thirteen patients had locally advanced disease, and 58 patients had evidence of metastatic disease. The most common metastatic site was liver (55 cases), followed by posterior peritoneal lymph nodes and lung. Twelve cases were treated with gemcitabine monotherapy, 35 cases with gemcitabine plus oxaliplatin, 16 cases with gemcitabine plus 5-FU/CF in bolus, and the rest eight cases with gemcitabine plus capecitabine or docetaxel. The accumulated dosage for gemcitabine was 5.3 g/ m2 (2–16g/m2). Measurement of serum CA19-9. Serum CA19-9 was measured one week before starting chemotherapy (baseline level) and every 3–4 weeks after each cycle of chemotherapy. The concentration of CA19-9 was measured by commercially available enzyme immunoassay (Electrochemilumnescenceimmunoassay, Elecsys 1010, Roche Diagnostics GmbH, Mannheim, Germany). The normal value of CA19-9 was < 35 U/mL, and the detectable range was from 0.6 to 500,000 U/mL. Evaluation standard for therapeutic effects. Overall survival (OS). OS was defined as the time from beginning of the treatment until the date of death. Objective remission rate (ORR). The Response Evaluation Criteria in Solid Tumor (RECIST) was used to determine the therapeutic effect. Complete remission (CR) was defined as complete disappearance of all target lesions without occurrence of new lesions, a decrease in the level of tumor markers to the normal level which was maintained for four weeks. Partial remission (PR) was defined as a decrease in the sum of the longest lengths of all baseline target lesions ≥ 30% which was maintained for four weeks. Stable disease (SD) was defined as a decrease in the sum of the longest lengths of all baseline target lesions less than PR, or enlargement of the lesions without progression. Progressive disease (PD) was defined as an increase in the sum of the longest lengths of the detected smallest target lesion ≥ 20%, or occurrence of one or more new lesion sites. Clinical benefit response (CBR). CBR is a comprehensive assessment for cancer related pain, body strength, and weight. The standard is as the followings: 1) Improvement of at least one of the three indices, a. a decrease in the dosage of the painkiller by more than 50% compared with that given upon admission for more than four weeks without worsening any of them, b. reduction of pain severity for more than 50%, c. improvement of KPS score by more than 20 points; 2) Stable assessment scores for painkiller, pain, and body status, increase of more than 7% body weight for more than four weeks (exclusive of fluid retention). Statistical analysis. Data were analyzed by SPSS 12.0 software. Quantitative data between two groups were compared using the R*C chi-square test. Comparison among multi-groups was performed using One-Way ANOVA analysis. Survival was www.landesbioscience.com Table 1 Clinical characteristics of 71 patients with pancreatic cancer analyzed by the Kaplan-Meier test. The Cox model was used for multi-factorial analysis to screen out independent risk factors. p < 0.05 indicated statistical significance. Results Overall therapeutic effects. Until April 2008, 64 patients died and seven patients were still alive. The median OS was 7.1 months. The one- and two-year survival rates were 13.8% and 1.7%, respectively. Among 71 patients, 47 were evaluable, of which 14 patients achieved PR, 22 patients remained SD, and 11 patients had PD. The overall response rate (ORR) was 29.8% (14/47). Fifty-nine patients were able to be evaluated for clinical benefit and the total CBR rate was 39.0% (23/59). The relationship between serum CA19-9 and OS. Influence of the base-line CA19-9 level on OS. The base-line serum CA19-9 level was measured in all 71 patients one week before starting chemotherapy. Ten cases (14.1%) had normal baseline CA19-9 levels, while 61 cases (85.9%) had increased base-line CA19-9 levels. The median survival was 9.0 months for 10 patients with normal baseline CA19-9 levels and 7.9 months for 61 patients with increased baseline CA19-9 levels (p = 0.797) (Fig. 1A). Sixty-one patients with elevated CA19-9 levels were further divided into Group A (33 cases) whose baseline CA 19-9 levels were below the medium value (682 U/mL) and Group B (28 cases) whose baseline CA 19-9 concentrations were above the medium value. The OS was longer for patients in Group A (9.6 months) than in Group B (5.1 months) (p = 0.001) (Fig. 1B). Chinese Journal of Cancer 241 Prognostic value of serum CA19-9 in patients with advanced pancreatic cancer receiving gemcitabine based chemotherapy Figure 1. Correlation of scrum CA19-9 levels to the overall survival of patients with advanced pancreatic cancer Table 2 Correlation of serum CA19-9 levels to tumor response, clinical benefit response (CBR) PR: partial remission; SD: stable disease; PD: progression of disease. Table 3 Cox regression analysis for prognostic markers of pancreatic cancer Influence of changes in postchemotherapy serum CA19-9 levels on OS. Postchemotherapy serum CA19-9 levels of all the 71 patients were measured every three to four weeks after each cycle of chemotherapy. Serum CA19-9 levels of 10 patients with normal baseline CA19-9 concentrations were maintained within normal ranges after chemotherapy, while those of 61 patients with increased baseline CA19-9 levels showed different extents of changes after chemotherapy. The postchemotherapy decline rate of CA19-9 was calculated as follows: (serum baseline CA19-9 value–the lowest postchemotherapy serum CA19-9 value)/serum baseline CA19-9 value × 100%. As shown in Fig. 1C, when 25% decline in the postchemotherapy serum CA19-9 was set as the cut-off point, the median survival time of patients with a decline in postchemotherapy CA 19-9 ≥ 25% (Group C, 32 cases) was 242 significantly longer than that of the patients with a decline in postchemotherapy CA 19-9 < 25% or without decline (group D, 29 cases) (10.2 months vs. 5.0 months) (p < 0.001). Correlation of CA19-9 to objected response rate (ORR) and CBR. Among 61 patients with elevated serum CA19-9 levels, 42 were evaluable (23 from Group A and 19 from Group B; 23 from Group C and 19 from Group D) for ORR and 51 (27 from Group A and 24 from Group B; 26 from Group C and 25 from Group D) were assessable for CBR. ORR were 43.5% (10/23) vs. 15.8% (3/19) between Group A and B (p = 0.051), and 47.8% (11/23) vs. 10.5% (2/19) between Group C and D (p = 0.002). CBR were 48.1% (13/27) vs. 29.2% (7/24) between Group A and B (p = 0.125), and 69.2% (18/26) vs. 8.0% (2/25) between Group C and D (p < 0.001) (Table 2). Multi-factorial analysis. Ten factors, including age, sex, KPS score, primary tumor site, diseases extent (locally advanced or metastatic), tumor differentiation, history of palliative therapy, chemotherapy regimen, baseline serum CA19-9 level, decreased percentage of the CA19-9 level after chemotherapy were analyzed by the univariate and COX multivariate analysis. Results revealed that baseline CA19-9 above the median value (682 U/mL), decline in CA19-9 less than 25% and poor differentiation were independent risk factors for advanced pancreatic cancers patients treated with gemcitabine based chemotherapy (Table 3). Discussion Human pancreatic cancer is one of the most malignant diseases in the world with highly poor prognosis. Gemcitabine is supe- Chinese Journal of Cancer 2009; Vol. 28 Issue 3 Prognostic value of serum CA19-9 in patients with advanced pancreatic cancer receiving gemcitabine based chemotherapy rior to 5-FU in improving CBR and prolonging the survival. The National Comprehensive Cancer Network (NCCN) panel recommends gemicitabine monotherapy as the standard frontline therapy for patients with advanced pancreatic cancer.1,2 Gemcitabine in combination with potentially synergistic agents, such as cisplatin, oxaliplatin, capecitabine, irinotecan, or 5-FU, exerts higher response rates, more favorable time to progression and higher CBR than gemicitabine momotherapy, especially for patients with good performance status whose ORR (CR + PR) is around 10% to 30%, tumor control rate is around 25% to 74%, and CBR is around 30% to 40%.5-8 In our study, most patients (83.1%) received gemcitabine based doublets. In accordance to previous studies, the objective effectiveness in our study was 29.8%; medium survival time was 7.1 months; one- and two-year survival rates were 13.8% and 1.7%, respectively. CA19-9 is a sialylated Lewis blood group antigen targeted by the monoclonal antibody 1116 NS19-9 with the molecular weight of 5 × 103 ku. The concentration of CA 19-9 is increased in more than 80% of patients with advanced pancreatic cancer. However, patients who are genotypically negative for the Lewis blood group antigen, will not express CA19-9 even in the presence of active pancreatic cancer. About 7–10% of the general population is negative for this antigen and, thus, will not express CA 19-9.10 In this study, 10 of 71 patients (14.1%) had normal ranges of CA19-9 levels, whose overall survival was not significantly different from those with elevated CA19-9 levels, consistent with that reported by Halm et al.4 We believe that serum CA19-9 could not be used as a prognostic factor for those patient with normal baseline CA19-9 levels. Maisey et al.11 conducted a retrospective study and found that the base-line CA19-9 level prior to chemotherapy was an independent predictive factor for survival of patients with advanced pancreatic cancer. Patients whose baseline CA19-9 was lowered than the average value achieved a higher one-year survival rate than those whose baseline CA19-9 was above the average. Ko et al.12 proved a positive correlation between the percentage of decline in postchemotherapy CA19-9 and the overall survival of patient with advanced pancreatic cancer. Halm et al.13 reported the survival of 43 consecutive patients with advanced pancreatic cancer treated with single-agent gemcitabine and revealed that a fall of at least 20% in the CA19-9 level following the start of chemotherapy was the only independent prognostic marker for OS. Park et al.14 conducted a phase II study and found that patients with ≥ 25% decline in serum CA19-9 achieved better outcomes in terms of time to progression and OS than those whose decline in CA19-9 was < 25%. However, a recent prospective study published in Lancet Oncol concluded that only pretreatment base-line serum CA 19-9 concentration was an independent prognostic factor for survival, whereas a decrease in concentration during chemotherapy was not significantly associated with lengthened survival compared with those who did not have a corresponding decrease.15 We found that the median OS in patients with a baseline CA19-9 below the median value was significantly superior to those with a level above the median value. Moreover, the median OS was significantly longer in patients with a decrease in CA 19-9 ≥ 25% www.landesbioscience.com than those with a decrease < 25%. Therefore, we suppose that both pretreatment baseline CA 19-9 levels and post-treatment decline in CA19-9 levels could predict the survival of patients with advanced pancreatic cancer undergoing gemcitabine based chemotherapy. However, due to the relative small number of sample size, further prospective, large sample size studies are needed to verify the results. We also discovered that, among patients with a decline in post-treatment CA19-9 level ≥ 25%, most of which (88.9%) achieved the lowest CA19-9 value within six weeks after chemotherapy (median 5.3 weeks). We suggest that measurement of CA 19-9 after six weeks of chemotherapy may assist to decide the treatment efficacy together with other clinical parameters. RECIST is based on measuring the size changes in tumor lesions before and after chemotherapy using imaging techniques. Because pancreas is located behind the peritoneum, imaging examinations have limitations in differentiating normal pancreas, local inflammation, and fibrosis from malignant tissues, and therefore may be inaccurate in the assessment of tumor response during chemotherapy, even using 3D imaging techniques, such as CT and MRI. Carmichael J et al.16 proposed using CBR as indices to assess the treatment efficacy of pancreatic cancer. However, these parameters are too subjective, and are difficult to be quantified, which limit their clinical application. Our study indicated that dynamic measurements of CA 19-9 levels in gemcitabinebased chemotherapy are useful to assess the therapeutic effect. The ORR and CBR were significantly higher in patients whose decline in CA 19-9 was ≥ 25% than in those whose decline was < 25%. Although the ORR and CBR were higher in patients whose baseline CA 19-9 levels were below the median (682 U/ mL) than in those whose baseline CA 19-9 levels were above the median, the differences were not significant, probably due to the relatively small sample size of this study. Similar results have been reported by other groups. Micke et al. found that patients with a low level of baseline pretreatment CA19-9 (420U/mL) showed a higher response rate than those whose baseline CA19-9 was above 420 U/mL.17 An important caveat in the interpretation of CA19-9 levels in pancreatic cancer is the presence of biliary obstruction, which results in the elevation of the marker level. In the current series, patients with jaundice or hyperbilirubinemia were excluded. Therefore this potential pitfall was avoided in the interpretation of baseline CA19-9 levels. In conclusion, dynamic measurement of CA19-9 concentrations is a useful prognostic tool in predicting the survival of advanced pancreatic cancer patients with elevated serum CA19-9 levels receiving gemicitabine based chemotherapy References [1] Aapro MS, Martin C, Hatty S. Gemcitabine--a safety review [J]. Anticancer Drugs, 1998,9 (3):191-201. [2] Burris HA 3rd, Moore MJ, Andersen J, et al. 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CA 19-9 tumour-marker response to chemotherapy in patients with advanced pancreatic cancer enrolled in a randomised controlled trial [J]. Lancet Oncol, 2008,9 (2):132-138. [16] Carmichael J. Clinical response benefit in patients with advanced pancreatic cancer [J]. Role of gemcitabine. Digestion, 1997,58(6):503-507. [17] Micke O, Bruns F, Kurowski R, et al. Predictive value of carbohydrate antigen 19-9 in pancreatic cancer treated with radiochemotherapy [J]. Int J Radiat Oncol Biol Phys, 2003,57(1):90-97. 244 Chinese Journal of Cancer 2009; Vol. 28 Issue 3