中华肿瘤杂志
中華腫瘤雜誌
중화종류잡지
CHINESE JOURNAL OF ONCOLOGY
2010年
11期
850-854
,共5页
李玲%宋丽华%丁士超%张晓君%强玲%韩春燕%袁香婷%徐丹丹
李玲%宋麗華%丁士超%張曉君%彊玲%韓春燕%袁香婷%徐丹丹
리령%송려화%정사초%장효군%강령%한춘연%원향정%서단단
癌胚抗原%细胞角蛋白19片段%癌,非小细胞肺%治疗效果%预后
癌胚抗原%細胞角蛋白19片段%癌,非小細胞肺%治療效果%預後
암배항원%세포각단백19편단%암,비소세포폐%치료효과%예후
CEA%CYFRA21-1%Carcinoma,non-small cell luns%Treatment outcome%Prognosis
目的 研究癌胚抗原(CEA)和细胞角蛋白19片段(CYFRA21-1)作为晚期非小细胞肺癌(NSCLC)疗效评价指标的价值.方法 以血清肿瘤标志物CEA和(或)CYFRA21-1升高的228例初治NSCLC患者为研究对象,所有患者均采用以化疗为主的治疗手段.采用回顾性研究方法,按照实体瘤疗效评价标准(RECIST)判断疗效,并分析治疗前后血清肿瘤标志物的变化与近期疗效及无进展生存时间(PFS)的关系.结果 228例患者中,部分缓解(PR)40例,稳定(SD)151例,进展(PD)37例.按照血清肿瘤标志物的变化率将患者分为下降组、升高组和稳定组,CEA下降组90例,稳定组49例,升高组66例;CYFRA21~1下降组84例,稳定组26例,升高组37例.PR患者在CEA和CYFRA21-1下降组中分别占68.4%和88.9%,在升高组中分别占7.9%和5.6%;PD患者在CEA和CYFRA21-1升高组分别占59.4%和76.2%,而下降组中无PD患者;SD患者介于两者之间.血清肿瘤标志物的变化率与影像学疗效评价显著相关(rCEA=0.45,PCEA=0.00;rCYFRA21-1=0.44,PCYFRA21-1=0.00).不同肿瘤标志物变化组患者的PFS差异有统计学意义(均P<0.05),并可区分SD亚组患者的预后.结论 治疗前后CEA和CYFRA21-1的变化可以预测NSCLC患者的影像学疗效及PFS,并可将SD患者进一步划分为不同的疗效及预后亚组,有利于SD患者的个体化治疗.
目的 研究癌胚抗原(CEA)和細胞角蛋白19片段(CYFRA21-1)作為晚期非小細胞肺癌(NSCLC)療效評價指標的價值.方法 以血清腫瘤標誌物CEA和(或)CYFRA21-1升高的228例初治NSCLC患者為研究對象,所有患者均採用以化療為主的治療手段.採用迴顧性研究方法,按照實體瘤療效評價標準(RECIST)判斷療效,併分析治療前後血清腫瘤標誌物的變化與近期療效及無進展生存時間(PFS)的關繫.結果 228例患者中,部分緩解(PR)40例,穩定(SD)151例,進展(PD)37例.按照血清腫瘤標誌物的變化率將患者分為下降組、升高組和穩定組,CEA下降組90例,穩定組49例,升高組66例;CYFRA21~1下降組84例,穩定組26例,升高組37例.PR患者在CEA和CYFRA21-1下降組中分彆佔68.4%和88.9%,在升高組中分彆佔7.9%和5.6%;PD患者在CEA和CYFRA21-1升高組分彆佔59.4%和76.2%,而下降組中無PD患者;SD患者介于兩者之間.血清腫瘤標誌物的變化率與影像學療效評價顯著相關(rCEA=0.45,PCEA=0.00;rCYFRA21-1=0.44,PCYFRA21-1=0.00).不同腫瘤標誌物變化組患者的PFS差異有統計學意義(均P<0.05),併可區分SD亞組患者的預後.結論 治療前後CEA和CYFRA21-1的變化可以預測NSCLC患者的影像學療效及PFS,併可將SD患者進一步劃分為不同的療效及預後亞組,有利于SD患者的箇體化治療.
목적 연구암배항원(CEA)화세포각단백19편단(CYFRA21-1)작위만기비소세포폐암(NSCLC)료효평개지표적개치.방법 이혈청종류표지물CEA화(혹)CYFRA21-1승고적228례초치NSCLC환자위연구대상,소유환자균채용이화료위주적치료수단.채용회고성연구방법,안조실체류료효평개표준(RECIST)판단료효,병분석치료전후혈청종류표지물적변화여근기료효급무진전생존시간(PFS)적관계.결과 228례환자중,부분완해(PR)40례,은정(SD)151례,진전(PD)37례.안조혈청종류표지물적변화솔장환자분위하강조、승고조화은정조,CEA하강조90례,은정조49례,승고조66례;CYFRA21~1하강조84례,은정조26례,승고조37례.PR환자재CEA화CYFRA21-1하강조중분별점68.4%화88.9%,재승고조중분별점7.9%화5.6%;PD환자재CEA화CYFRA21-1승고조분별점59.4%화76.2%,이하강조중무PD환자;SD환자개우량자지간.혈청종류표지물적변화솔여영상학료효평개현저상관(rCEA=0.45,PCEA=0.00;rCYFRA21-1=0.44,PCYFRA21-1=0.00).불동종류표지물변화조환자적PFS차이유통계학의의(균P<0.05),병가구분SD아조환자적예후.결론 치료전후CEA화CYFRA21-1적변화가이예측NSCLC환자적영상학료효급PFS,병가장SD환자진일보화분위불동적료효급예후아조,유리우SD환자적개체화치료.
Objective To investigate the value of carcinoembryonic antigen (CEA) or cytokeratin 19 fragment ( CYFRA21-1 ) as an assessment indicator of therapeutic efficacy in advanced non-small cell lung cancer (NSCLC) patients. Methods 228 cases of advanced NSCLC with chemotherapy were enrolled into this retrospective study. The serum CEA or CYFRA21-1 levels of all patients were above the cut-off limit before treatment. The relationship between changes of tumor markers (TMs) and imaging therapeutic efficacy or progression-free survival (PFS) was analyzed, and the value of TMs in therapeutic efficacy assessment was evaluated. Results According to RECIST criteria, partial response (PR) occurred in 40 cases, stable disease (SD) in 151 and PD (progressive disease) in 37. The cut-off values of the changes of TMs between pre- and post-treatment were determined according to the above mentioned criteria. The CEA down (D), stable (S), above (A) groups were 90, 49 and 66 cases, respectively. CYFRA21-1 down (D), stable (S), above (A) groups were 84, 26 and 37 cases, respectively. PR groups were 68.4% and 88.9% in CEA and cyfra21-1 down groups, respectively, 7. 9% and 5. 6% in the above groups,respectively. PD groups were 59.4% and 76.2% in CEA and CYFRA21-1 above groups, respectively. No PD cases were in the down groups. The changes of TMs in SD group were between them. Statistically significant correlations were observed between changes of TMs and imaging therapeutic efficacy (rCEA =0.45, P =0. 00;rCYFRA21-1 =0.44,P =0. 00). PFS among different TMs groups were significantly different (all P <0. 05), which can be used to further distinguish the prognosis among SD subgroups. Conclusion Changes of TMs can be used to predict the imaging therapeutic effect and PFS of the patients, and if the SD group is divided into subgroups according to different therapeutic efficacy and prognosis, it may help the patients to receive individualized treatment.
