NCCN胃癌临床实践指南中国版下载_PPT模板_50

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NCCN胃癌临床实践指南中国版nullNCCN胃癌临床实践指南中国版解读NCCN胃癌临床实践指南中国版解读北京大学临床肿瘤学院北京肿瘤医院消化内科沈琳 2008 肿瘤学临床实践指南（中国版）2008年第一版胃癌nullCopyright ©2005 American Cancer SocietyAge-standardized Incidence Rates for Stomach Cancer in world.From Parkin...

nullNCCN胃癌临床实践指南中国版解读NCCN胃癌临床实践指南中国版解读北京大学临床肿瘤学院北京肿瘤医院消化内科沈琳 2008 肿瘤学临床实践指南（中国版）2008年第一版胃癌nullCopyright ©2005 American Cancer SocietyAge-standardized Incidence Rates for Stomach Cancer in world.From Parkin, D. M. et al. CA Cancer J Clin 2005;55:74-108.世界胃癌年龄调整发病率对1990-1992年中国的1/10万人口死因抽样调查资料中胃癌死亡情况进行

分析

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对1990-1992年中国的1/10万人口死因抽样调查资料中胃癌死亡情况进行分析胃癌粗死亡率(crude mortality rate) 25.2/10 万（M：32.8/10 万，F：17.0/10 万），占全部恶性肿瘤死亡的23.2%，恶性肿瘤死亡中第一位。（男性是女性1.9倍）中国胃癌世界人口调整死亡率(mortality rates adjusted by the world population)男性：40.8/10 万，女性：18.6/10 万，分别是欧美发达国家的4.2-7.9 倍，3.8-8.0 倍有明显的地区差异和城乡差别。全国抽样调查263个点，胃癌调整死亡率在2.5-153.0 /10万之间，Urban areas:15.3/10 万; Rural areas:24.4/10万，是城市的1.6 倍 NCCN共识分类NCCN共识分类1类：基于高水平的证据，NCCN达成共识，推荐应用 2A类：基于包括临床经验在内的稍低水平证据，NCCN达成共识，推荐应用。 2B类：基于包括临床经验在内的稍低水平证据，NCCN未达成统一共识（但无较大分歧）。 3类：NCCN对该建议的适宜性存在较大分歧。除非特别说明，本指南中所有的建议均达成2A类共识。 NCCN 胃癌临床实践指南 2008第1版指南更新主要变化总结NCCN 胃癌临床实践指南 2008第1版指南更新主要变化总结（GAST-1）：workup：PET/CT扫描和EUS作为可选的检查项目。（GAST－ 2）：要求多学科会议讨论患者所有三个治疗途径的抉择 T2以上分期患者将术前化疗作为一类推荐首选治疗手段。术前放化疗作为2B类的首选治疗手段。（GAST－3）： R0术后分期T2 N0M0及以上者，如术前采用ECF

方案

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化疗，术后可选择ECF继续（1类）（GAST－5）： follow up：近端胃大部或全胃切除者，应监测并补充Vit B12 （GAST－A）：增加综合治疗模式原则新页（GAST－B、C）：更新外科及系统化疗原则（GAST－A）：新增放疗原则新页NCCN guidelines ----Gastric Cancer Chinese version 1. 2008在整个治疗指南中将chemotherapy/RT 更改为 chemoradiation 将salvage 改为palliative与2007版类似与2007版类似注意：除了特别指出的情况，所有推荐的治疗都是2A证据的。临床试验：NCCN认为对于任何一个肿瘤病人参加临床实验都获得最佳治疗. 要特别鼓励参与临床试验。 null强调多学科评估和协作！null多学科综合治疗模式有益于局部进展期胃癌患者（1类证据） NCCN专家组基本观点：不鼓励单一学科成员单方面进行治疗决策。具备以下条件，可能给局部进展期胃癌患者以最佳的综合治疗：例会形势实用（一周或2周一次），相关学科的机构和个人定期来共同回顾患者的详细资料。每次例会，各相关学科都要积极参与，包括肿瘤外科，肿瘤内科，消化科，放射科，病理科。此外，最好还能包括营养科，社工，护理以及其他支持学科。所有长期的治疗策略要在全面分期检查完成后再进行，最好在所有治疗开始之前。决策前共同回顾原始的医学数据而非单纯阅读

报告

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。多学科团队做出共识推荐并摘要

记录

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在案，对每位患者是有益的。特定患者的主要治疗小组或医生应尊重以及考虑多学科团队所做出的共识推荐。反馈部分患者的治疗随访结果，对整个多学科团队是有效的实例教育方式。在例会期间，正式的定期复习相关文献，对整个多学科团队是高效的教育方式。nullnull分期 CT扫描±EUS判断病灶范围腹腔镜有助于部分患者的分期不能根治性切除标准局部进展期:3/4站淋巴结转移, 大血管受侵或被包绕远处转移或腹膜种植(包括腹腔脱落细胞学阳性可切除肿瘤 T1者在有经验者可采用内镜下胃粘膜切除 T1-T3合适的肿瘤切缘≥4 cm（5 cm）, 镜下阴性推荐D1/D2淋巴结清扫, 应至少检查15个淋巴结，并结合位置清扫到2站淋巴结 T4应切除受累部位不做常规脾切除, 除非脾脏受累或脾门受侵可考虑留置空肠营养管姑息手术可以接受切缘阳性，淋巴结不强求清扫胃肠短路或营养管外科治疗原则NCCN v.1.2008 Gastric Cancernull结合淋巴结数目以及累及区域分期Japanese Gastric cancer associati（JGCA)Japanese Gastric cancer associati（JGCA)腹腔细胞学（CY） CY0 腹腔细胞学良性或无法确定 CY1 腹腔细胞学未见癌细胞 CYx 未作其它远处转移（M）§ M0 腹膜、肝、腹腔细胞学外无远处转移 M1 腹膜、肝、腹腔细胞学外有远处转移 Mx 不清楚分期

表

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2 日本胃癌学会（JGCA）分期（1998年第13版*）原发肿瘤（T） T1 肿瘤侵犯粘膜层和/或粘膜肌层(M)和/或粘膜下层(SM) T2 肿瘤侵犯固有肌层(MP)或浆膜下层(SS) † T3 肿瘤穿透浆膜(SE) † T4 肿瘤侵犯邻近结构(SI) ‡ Nx 不明局部淋巴结（N）淋巴结分站分组（见ST-3）淋巴结转移程度 N0 无淋巴结转移证据 N1 第一站淋巴结有转移，第二、三站淋巴结无转移 N2 第二站淋巴结有转移，第三站淋巴结无转移 N3 第三站淋巴结有转移 Nx 区域淋巴结无法评估肝转移（H） H0 无肝转移 H1 有肝转移 Hx 不清楚腹膜转移（P） P0 无腹膜转移 P1 有腹膜转移*本分期源自 Japanese Gastric Cancer Association. Japanese Classification of Gastric Carcinoma - 2nd English Edition. Gastric Cancer (1998) 1: 10–24 †肿瘤可以穿透固有肌层达胃结肠韧带或肝胃韧带或大小网膜，但没有穿透这些结构的脏层腹膜。在这种情况下，原发肿瘤的分期为T2。如果穿透覆盖胃韧带或网膜的脏层腹膜，则应当被分为T3期。 ‡肿瘤侵犯大、小网膜、食管和十二指肠不作为T4,经胃壁内扩展至十二指肠或食管的肿瘤分期取决于包括胃在内的这些部位的最大浸润深度。 §M1的种类应注明：LYM: 淋巴结；PLE: 胸膜；MAR: 骨髓；OSS: 骨；BRA:脑；MEN: 脑膜；SKI: 皮肤；OTH: 其它Regional LN Group According to Location of TumorRegional LN Group According to Location of TumorLD/LnullSasako et al : the long-term outcome of survival ：D2 vs D2+, no statistically significant difference 69% vs 70%, p=0.57, HR:1.03, ( 95% CI: 0.77-1.37). Sasako M, Sano T, Yamamoto S, et al. Randomized phase III trial of standard D2 versus D2 + para-aortic lymph node (PAN) dissection (D) for clinically M0 advanced gastric cancer: JCOG9501. J Clin Oncol 2006.24(18S):LBA4015.扩大根治 or D2 ? ——循证医学证据nullA prospective randomized controlled clinical trial in Taiwan : D2 vs D1 5-year survival D2 dissection was superior to D1 dissection 59.5% vs 53.6%, p=0.041; HR: 0.49, p=0.002 Wu CW, Hsiung CA, Lo SS, et al. Nodal dissection for patients with gastric cancer: A randomized controlled trial. Lancet Oncol 2006;7:309-315 进一步的临床试验，特别是观察手术前后的辅助治疗应该基于D2式手术！ D1 or D2 ? ——循证医学证据null适合于所有胃癌胃切除标本原发性胃癌胃切除标本的检查原发性肿瘤* 外科切缘评估† 淋巴结评估‡ 原发性胃癌的组织学类型§ Lauren分类，1965 日本胃癌研究协会（JRSGC）分类，1981 WHO分类，2000 病理学分期（pTNM）应包括下列参数：肿瘤的恶性程度（分级）ξ 浸润的深度淋巴结的部位、数目及阳性数远端及近端外科切缘状况注释胃癌原发肿瘤检查应包括：肿瘤在胃粘膜确切位置及肿瘤范围；肿瘤距近端和远端外科切缘的距离；肿瘤大体形态，包括肿瘤大小、早期胃癌的形态类型；肿瘤切面，浸润胃壁情况。 † 外科切缘评估：胃切除标本有远端及近端切缘：部分切除标本，远端切缘是十二指肠，近端切缘是胃体；全胃切除标本，远端切缘是十二指肠，近端切缘是食管。外科切缘有3种情况：R0：外科切缘干净；R1：外科切缘镜下阳性；R2：外科切缘肉眼阳性。建议切除的近端切缘应距肿瘤边缘5cm，同时应常规术中切缘冰冻检查。 ‡ 淋巴结评估：见ST-1/2/3。根据胃切除时淋巴结清扫的范围分为：D0：淋巴结清扫的范围不包括所有N1淋巴结；D1：淋巴结清扫的范围不包括所有N2淋巴结；D2：淋巴结清扫的范围不包括所有N3淋巴结。按照AJCC标准，因为被检查淋巴结的数量和淋巴结阳性率之间有正相关，应检查至少15个淋巴结。§ 胃癌组织学类型 Lanren分类（1965）：肠型；弥漫型 JRSGC分类（1981）：乳头状型管状型低分化型粘液型印戒细胞型 WHO分类（2000）腺癌肠型弥漫型乳头状腺癌管状腺癌粘液腺癌印戒细胞癌腺鳞癌鳞状细胞癌小细胞癌未分化癌其它 ξ 胃腺癌组织学分级：高分化；中分化；低分化；未分化病理学分期（pTNM）病理学分期与胃癌预后极其相关，早期胃癌预后极好，5年生存率达90%。建议使用AJCC/UICC分类，在病理报告中N分期可增加标注JRSGC要求的淋巴结部位。病理诊断原则系统化疗原则 NEW系统化疗原则 NEW遵照原始文献报道的药物剂量/方案, 合理用药并进行适当调整患者合适的器官功能和体力状况充分考虑化疗的毒性和益处, 并始终与患者及家属讨论/交流, 并进行患者教育, 警示并防治不良反应, 避免严重合并症及缩短持续时间患者化疗期间仔细观察, 及时治疗合并症, 并适当监测患者血液学改变化疗阶段及时评估疗效和长期合并症 nullUpdate of 2008.v.1 NCCN version可切除胃癌围手术期化疗 ---MAGIC trial可切除胃癌围手术期化疗 ---MAGIC trial胃癌（占85%）或低位食管癌（15%）ECF* 3cs-手术-ECF 3cs单一手术N=250 5Y 38%N=253 5Y 23%ECF: E 50mg/m2 C 60mg/m2 FU 200mg/m2/d civD.Cuuningham 2005 ASCO abs 4001 Cunningham et al, NEJM 2006可切除胃癌围手术期化疗 ---MAGIC trial*No pathologic complete responses可切除胃癌围手术期化疗 ---MAGIC trialCunningham et al, NEJM 2006可切除胃癌围手术期化疗 ---MAGIC trialCunningham et al, NEJM 2006可切除胃癌围手术期化疗 ---MAGIC trialnullOverall Survival可切除胃癌围手术期化疗 5-FU+DDP in AGC/LE ---FFCD 9703 trial可切除胃癌围手术期化疗 5-FU+DDP in AGC/LE ---FFCD 9703 trialFP 2～3cs（98例） -手术- FP 2～ 3cs (RR+SD n+)（54例）单一手术N=113 5Y DFS 34%N=111 5Y DFS 21%FP: 5-FU 800mg/m2 d1-5 ci DDP 100mg/m2 d1 Q4w 随访 5.7Y贲门、胃89％食管11％可切除胃癌围手术期化疗 5-FU+DDP in AGC/LE ---FFCD 9703 trial可切除胃癌围手术期化疗 5-FU+DDP in AGC/LE ---FFCD 9703 trialHR 0.65V. Boige et al, ASCO 2007 abstr 4510可切除胃癌围手术期化疗 Patient data-based meta-analysis: CT+S vs S可切除胃癌围手术期化疗 Patient data-based meta-analysis: CT+S vs S从12随机试验, 2284 患者中筛选出2102患者,涉及9个试验, 中位随访时间5.3年 CT+S vs S HR 0.87 P=0.003 转化为5年绝对生存率提高4% R0切除率 67% vs 62% p=0.03P.G.Thirion et al, ASCO 2007 abstr 4512GAST-C 1 of 2: preoperative chemoradiationGAST-C 1 of 2: preoperative chemoradiation2008.v.1NCCN guideline： Paclitaxel/docetaxel + fluoropyrimidine(5-FU or capecitabine) category 2B； Recommendation of Chinese version: Docetaxel might be changed; Category 2B to 3.Reason: Study about Paclitaxel/5FU+RT is only phase II. No prospective studies has been searched on docetaxel/5-FU +RT(medline).nullPreoperative chemoradiation: phase II Phase II Trial of Preoperative Chemoradiation in Patients With Localized Gastric Adenocarcinoma (RTOG 9904): Quality of Combined Modality Therapy and Pathologic Response ——Jaffer A. Ajani JCO 2006：24（24）：3593Phase: II Patients： 43 cases with localized GC (12% IB; 37% II; 52% III).，20 center Methods: 2cys of 5FU+CF+DDP——CRT (infusional 5FU+weekly paclitaxel) Resection （5 to 6 weeks after chemoradiotherapy was completed.） Result： path CR： 26% R0 resection ：77%, 1 year：more patients with path CR (82%) are living than those with less than path CR (69%）GAST-C 1 of 2: preoperative chemoradiationGAST-C 1 of 2: preoperative chemoradiation2008.v.1NCCN guideline： Paclitaxel/docetaxel + fluoropyrimidine(5-FU+capecitabine) category 2B； Recommendation of Chinese version: Docetaxel might be changed; Category 2B to 3.nullUpdate of 2008.v.1 NCCN versionPostoperative chemotherapy?nullStage IB-IV(M0) D0 和 D1占90%nullnullGAST-3:T3,T4 or any T,N1 after R0 resectionGAST-3:T3,T4 or any T,N1 after R0 resection2008.v.1NCCN guideline：RT,45-50.4Gy+concurrent 5-FU based radiosensitization(preferred)+5-FU±leucovorin or ECF if received preoperatively（category 1） Recommendation of Chinese version: Add foot note If D0/D1 resection: agreed the above; If D2 resection: postoperative chemotherapy recommended.Evidence： D0/D1 operation consists more than 90% in INT0116； 2 Meta analysis about adjuvant chemotherapy GASC-studynullPatients: 23 trials， 4919 pts Methods: Adjuvant chemotherapy arm(Arm A): 2441 Observation arm(Arm B): 2478 Results: 3y Survival rate: 60.6% in Arm A, 53.4% in Arm B (RR: 0.85,95%CI: 0.80–0.90 ) DFS: Arm B had a shorter DFS (RR: 0.88, 95%CI: 0.77–0.99) Recurrence rate: Arm A had a lower recurrence rate (RR: 0.78, 95%CI: 0.710.86) Grade 3/4 of AE(myelosuppression and GI): more frequently in Arm A. Conclusion: Adjuvant chemotherapy could improve the survival rate and disease-free survival rate in gastric cancer after curative resection and reduce the relapse rate. META analysis of Adjuvant chemotherapy 1 An updated meta-analysis of adjuvant chemotherapy after curative resection for gastric cancer ——European Journal of Surgical Oncology (EJSO) 2008.02.002 nullMETA analysis of Adjuvant chemotherapy 2 The role of postoperative adjuvant chemotherapy following curative resection for gastric cancer: a meta-analysis Shu-Liang Zhao; Jing-Yuan Fang. Renji Hospital, Shanghai, China. Cancer Investigation, May2008, Vol. 26 Issue 3, p317-325,Patients: 15 trials， 3212 pts， Methods: Surgery+adjuvant chemotherapy vs Surgery only Results: RR for death in the treated group was 0.90 (P = 0.0010). Little or no significant benefits were suggested in subgroup analyses between different population and regimens either. Conclusion: Postoperative adjuvant chemotherapy for gastric cancer confers slightly significant benefits compared to the surgery only group. nullPostoperative adjuvant chemotherapy ——S1 monotherapy Adjuvant chemotherapy for gastric cancer with S-1, an oral fluoropyrimidine. —— Sakuramoto, S N Engl J Med，2007，357：1810-1820 1004 cases (stage II/III ，D2,3 years follow up*Randomized phase III trial comparing S-1 monotherapy versus surgery alone for stage II/III gastric cancer patients (pts) after curative D2 gastrectomy (ACTS-GC study). 2007Gastrointestinal cancer symposium, sasako M*12/2005 showed that HR of death for S-1 to C was 0.57, trial was recommended to stop. 09/2006 HR of death for S-1 was 0.68. Conclusions: Adjuvant chemotherapy with S-1 for gastric cancer is feasible and effective. This regimen can be the standard treatment for stage II/III gastric cancer pts after curative D2 dissection. ACTS-GC study JCOGnullPostoperative chemoradiation might be a good option to compensate the insufficiency of the surgery such as D0/D1 resection. Adjuvant chemotherapy shows survival benefit compared with surgery alone, especially after D2 resection for patients with stage II or higher.Postoperative adjuvant chemotherapy Conclusion:GAST-3：after R1 resectionGAST-3：after R1 resection2008.v.1NCCN guideline： RT,45-50.4Gy+concurrent 5-FU-based radiosensitization (preferred) +5-FU±leucovorin Recommendation of Chinese version: To add “Clinical trials” as another option.Reason： R1 resection is not radical, till now, no standard therapy has been accepted, it should be better to find the appropriate ones by clinical studies.nullUpdate of 2008.v.1 NCCN versionNo DDP+fluoropyrimidine (5-FU or capecitabine or S－1 ) 2B No paclitaxel-based regimens；V325 研究结果V325 研究结果TCF(多西紫杉醇、顺铂、5FU)是用于预后较好的患者的一项新的治疗选择Moiseyenko et al, JCO 2007, *3－4级毒性包括：81％的非血液学毒性反应， 75％的血液学毒性反应中30％伴有中性粒细胞减少性发热CPT-11 for AGC——Ⅱ期多中心临床研究（2003 ASCO）FFCD 9803 法国CPT-11 for AGC——Ⅱ期多中心临床研究（2003 ASCO）FFCD 9803 法国Bouche O et al. J Clin Oncol2004;22:4319–27CPT-11联合5-FU治疗AGC ----III期临床试验（2005 ASCO）CPT-11联合5-FU治疗AGC ----III期临床试验（2005 ASCO）N=170 CPT-11 80mg/m2 CF 500mg/m2 5FU 2000mg/m2 civ 1/W x 6w N=163 CDDP 100mg/m2 d1 5FU 1000mg/m2/d d1-5 Q4W N=333 AGCRR 54（31.8%） 42（25.8%） TTP 5.0m 4.2m (p=0.088) TTF 4.0m 3.4m (p=0.002) OS 9.0m 8.7m p＝0.53M. Dank 2005 ASCO abs 4003REAL-2: 疗效（Efficacy）REAL-2: 疗效（Efficacy）Cunningham et al. ASCO 2006 LBA 4017REAL 2: 安全性 safety outcomesREAL 2: 安全性 safety outcomesOxaliplatin联合EPI、5-FU/CF治疗晚期胃癌的临床多中心研究—— chinaOxaliplatin联合EPI、5-FU/CF治疗晚期胃癌的临床多中心研究—— china用药方法乐沙定 100mg/m2 d1 EPI 50mg/m2 d1 CF 200mg/m2 d1-3 5-FU 500mg/m2 CIV d1-3 每3周重复，治疗至少3个周期评价疗效及毒性反应CR 2例（5.6%） PR 13例（36.1%） SD 17例（47.2%）总有效率41.7%。其中初治患者9/20（45%）复治患者6/16（37.5%）]主要不良反应：骨髓抑制： Ⅲ-ⅣOANC7/36（19.4%）， ⅢOPLT3/36（8.3%），ⅢO Hb4/36（11.1%），ⅢO神经末梢毒性 4/36（11.1%），以EPI为基础的三药联合可行！ EOX有明显生存优势！ML17032 : CAPE vs 5-FU in AGC trial designML17032 : CAPE vs 5-FU in AGC trial designFP Cisplatin 80 mg/m2 3-hour i.v. infusion 5-FU c.i. 800 mg/m2/day; d1–5 q3wXP Cisplatin 80 mg/m2 3-hour i.v. infusion Capecitabine 1000 mg/m2 twice daily; d1–14 q3w KPS ≥70% 18–75 years Advanced and/or metastatic gastric cancer (AGC) ≥1 measurable lesion No prior treatment for AGCR A N D O M I Z A T I O NSuperior response rate with XP vs. FPSuperior response rate with XP vs. FPML17032 : XP vs FP progression-free survival.HR 0.81 ML17032 : XP vs FP progression-free survival.HR 0.81 Estimated probabilityHR=0.81 (95% CI: 0.63–1.04) Compared to HR upper limit 1.25, p=0.00081.00.80.60.40.20.0Per protocol analysis相似的血液学不良发应 XP vs. FP相似的血液学不良发应 XP vs. FPA Phase II Trial of Capecitabine plus DDP in AGC－－ChinaA Phase II Trial of Capecitabine plus DDP in AGC－－China2002.6-2003.5, N=145, Cape 1000mg/m2 Bid d1-14 DDP 20mg/m2 iv d1-5 q3W 130pts evaluable : 98M/32F Age: 53.7ysResultsCR 10 (8%) PR 48(37%) SD 51(39%) PD 21(16%) OS 12m Safety：grade 3-4 adverse event < 5% -----2005,2006 ASCOfirst-line chemotherapy with fluorouracil, leucovorin and oxaliplatin (FLO) versus fluorouracil, leucovorin and cisplatin (FLP)first-line chemotherapy with fluorouracil, leucovorin and oxaliplatin (FLO) versus fluorouracil, leucovorin and cisplatin (FLP)FLO F 2600mg/m2 24h infusion, L 200mg/m2, oxaliplatin 85mg/m2 q2wFLP F 2000mg/m2 24h infusion, qw L 200mg/m2, qw cisplatin 50mg/m2, q2w. Total 220 pts Median age 64 yrs Advanced and/or metastatic gastric cancer (AGC)R A N D O M I Z A T I O NS. Al-Batran, J. Hartmann, ASCO 2006The primary end point was TTPSuperior Performance with FLO vs. FLPSuperior Performance with FLO vs. FLPS. Al-Batran, J. Hartmann, ASCO 2006Phase II Study of S-1 ±DDP vs 5-FU+DDP for Gastric Cancer (PI:ML Jin)Phase II Study of S-1 ±DDP vs 5-FU+DDP for Gastric Cancer (PI:ML Jin)Pathologically confirmed，unrectable，measurable leasionsC:5-FU+DDPA:S-1B:S-1+DDPrandomizationAssumed 180 cases，60 cases per arm，enrollment completed Objective：RR, TTPEvidence ：SC-101 study —— 2008 ASCO meetingEvidence ：SC-101 study —— 2008 ASCO meeting※: Arm B compared with Arm C , P<0.05 ★: Arm B compared with Arm A and C , P<0.05 ＃: Arm B compared with Arm A and C , P<0.05* : Arm B compared with Arm A , P>0.05Evidence ：SC-101 study —— 2008 ASCO meeting A randomized multi-center phase II trial： capecitabine (X) versus S-1 (S) as first-line treatment in elderly patients with mAGC A randomized multi-center phase II trial： capecitabine (X) versus S-1 (S) as first-line treatment in elderly patients with mAGCElderly chemo-naïve pts (>= 65 years) with measurable metastatic or recurrent gastric cancer armX (N=46, Median age=71.0 years ) Capecitabine (1,250 mg/m2 bid, D1-14 every 3 weeks) arm S (N=45, Median age= 70.5 years ) S-1 (40~60 mg bid D1-28 every 6 weeks) randomly10/2004-4/2006Y. Kang, D. Shin 2007 ASCO Annual MeetingA randomized study: the activity and safety of capecitabine vs S-1 in elderly pts with AGC phase II Y. Kang, JCO, 2007 ASCO Meetings Proceedings Part I.Vol 25, No. 18S: 4546) A randomized study: the activity and safety of capecitabine vs S-1 in elderly pts with AGC phase II Y. Kang, JCO, 2007 ASCO Meetings Proceedings Part I.Vol 25, No. 18S: 4546) Evidence ：capecitabine vs S-1 Evidence ：capecitabine vs S-1 toxity Evidence ：capecitabine vs S-1 toxity nullUpdate of 2008.v.1 NCCN versionDDP+fluoropyrimidine (5-FU or capecitabine or S－1 ) 2Bnulla randomized phase II trial of the Swiss Group for Clinical Cancer Research. Chemotherapy-naive patients ECF vs DC vs DCFEvidence 1: docetaxel ——Roth AD, Fazio N, et al, J Clin Oncol. 2007 Aug 1;25(22):3217-23. nulla randomized phase II study in Germany patients with untreated, advanced gastric adenocarcinoma.Evidence 2: docetaxel ——Thuss-Patience PC, Kretzschmar A, et al ： J Clin Oncol. 2005 Jan 20;23(3):494-501. nulla randomized phase II trial 106 patients included wDCF vs wDX wDCF : DOC 30mg/m2 d1 d8; DDP 60mg/m2; 5-Fu 200mg/m2 civ wDX DOC 30 mg/m2 d1d8; CAPE 1600 mg/m2 d1-14Evidence 3: docetaxel（Weekly） ——N.Tebbutt, et al, Asco 2007,4528. nullEvidence : paclitaxel vs docetaxel Paclitaxel versus docetaxel for advanced gastric cancer: a randomized phase II trial in combination with infusional 5-fluorouracil. ——Park SH et al, Anticancer Drugs. 2006 Feb;17(2):225-9Phase: II, randomized Patients： 77 cases with measurable metastatic gastric cancer (PF vs DF). Methods: PXL + 5-Fu vs DOC + 5-Fu Result： response rate (42 vs 33%, P=0.53) overall survival (9.9 vs 9.3 m; P=0.42) grade 3/4 toxicities (68 vs 85%; P=0.09) Global quality of life: similar pain, dyspnea, constipation and diarrhea favored PF Conclusion: Both PF and DF appear to have efficacy against metastatic gastric cancer, with different, but acceptable, safety profiles.nullUpdate of 2008.v.1 NCCN versionDCF modification： PF/DF/wDCF/DC/DX/PX should be addedGAST-C 1 of 2: metastatic or locally advanced cancerGAST-C 1 of 2: metastatic or locally advanced cancer2008.v.1NCCN guideline : Recommendation of Chinese version: To add cisplatin plus fluoropyrimidine(5-FU or capecitabine) category 2B To add fluoropyrimidine (5-FU or capecitabine) for old patients or poor performance status. Category 2BnullGAST-C 1 of 2: preoperative chemoradiation Docetaxel might be changed; Category 2B to 3. GAST-3:T3,T4 or any T,N1 after R0 resection Add foot note: If D0/D1 resection: agreed the above(CT+RT); If D2 resection: postoperative chemotherapy recommended. GAST-C 1 of 2: postoperative chemotherapy To add S-1 (category 2B) with footnote (not availabe in market now) GAST-3：after R1 resection To add “Clinical trials” as another option. GAST-C 1 of 2: metastatic or locally advanced cancer DCF modification： PF/DF/wDCF/DC/DX/PX should be added category 2B To add cisplatin plus fluoropyrimidine(5-FU or capecitabine) category 2B To add fluoropyrimidine (5-FU or capecitabine) for old patients or poor performance status. Category 2BRecommendation of Chinese version:NCCN胃癌临床指南v.1.2008重要更新概念的更新：在整个治疗指南中将chemotherapy/RT更改为chemoradiation，salvage 改为palliative 强调多学科协作在胃癌综合治疗中的重要地位，要求多学科会议讨论患者所有三个治疗途径的抉择，并增加综合治疗模式原则新页细化、更新手术、化疗、放疗原则术前分期检查PET－CT或EUS的应用强调术前新辅助化疗或放化疗的地位： T2以上分期患者将术前化疗作为一类推荐首选治疗手段。 follow up：近端胃大部或全胃切除者，应监测并补充Vit B12NCCN胃癌临床指南v.1.2008重要更新NCCN Clinical Prectice guidelines in Onco

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