恶性脑肿瘤的化疗方案ppt课件
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恶性脑肿瘤的化学治疗,Cerebrum and Cerebellum,流行病学趋势,2005 (US) 18,500* 12,760Incidence 11.47 per 100,000 (annual rate)Adjusted 5 yr survival rate (1995-2000)33% adults73% children 2nd leading cause of cancer deaths in persons 肿瘤,正常脑组织暴露化疗药物,高渗性BBB开放,Blood brain barrier disruption (BBBD) and intra-arterial methotrexate based therapy for newly diagnosed primary CNS lymphoma: The BBBD Consortium Experience.,2007 ASCO Annual Meeting Proceedings Part I. Vol 25, No. 18S,4 institutions: 1982-2005, 177 PCNSL,BBBD/IA MTX ;2,469 procedures,PtsCRPRORRM OS(y)MPFS(y)PFS-5(y),1771014180.2%3.11.640%,A Phase II Trial Involving Patients with Recurrent PCNSL Treated with Carboplatin/BBBD, by Adding Rituxan (Rituximab), an anti CD-20 Antibody, to the Treatment RegimenPhase I/II Study of Carboplatin, Melphalan and Etoposide Phosphate in Conjunction with Osmotic Opening of the Blood-Brain Barrier and Delayed Intravenous Sodium Thiosulfate Chemoprotection, in Subjects with Anaplastic Oligodendroglioma or OligoastrocytomaPhase II Clinical Trial of Patients with High-Grade Glioma Treated with Intra-arterial Carboplatin-based Chemotherapy, Randomized to Treatment with or without Delayed Intravenous Sodium Thiosulfate as a Potential Chemoprotectant against Severe ThrombocytopeniaIntra-arterial Melphalan (L-phenylalanine mustard) Administered in Conjunction with Osmotic Blood-Brain Barrier Disruption in Patients with Brain Malignancies: A Phase I Study,Neuro-Oncology Blood-Brain Barrier Program,Oregon Health & Science UniversityBlood Brain Barrier and Neuro-Oncology Program,替尼泊苷联合尼莫司汀治疗转移性脑肿瘤,治疗方法:VM26100mg,iv,gtt,D1-3,4周重复ACNU2-3mg/kg,iv,gtt,D1,4-6周重复化疗前20%甘露醇250ml,iv,gtt,DXM10mg,iv,ACNU共计47周期,平均2.3VM26共计49周期,平均2.5,中国癌症杂志Vol9, No2, June,1999,替尼泊苷联合尼莫司汀治疗转移性脑肿瘤,研究对象男性: 11例女性: 9例年龄: 33-70岁原发肿瘤病理类型:肺癌 12例乳腺癌 1例恶性淋巴瘤 3例鼻咽癌 1例滑膜肉瘤 1例不明肿瘤 2例,中国癌症杂志Vol9, No2, June,1999,替尼泊苷联合尼莫司汀治疗转移性脑肿瘤,临床表现症状 例次头痛 13恶心,呕吐 11意识改变6肢体肌力感觉异常 10颅脑神经受损7共济失调1合计 48,中国癌症杂志Vol9, No2, June,1999,替尼泊苷联合尼莫司汀治疗转移性脑肿瘤,结果:症状缓解率:完全缓解CR:60.4%部份缓解PR:31.6%症状总缓解率:91.7%颅脑CT复查:脑水肿减轻或消失 100%(16/16)完全缓解CR10%(2/20)部份缓解PR50%(10/20)总有效率(CR+PR)60%(12/20)颅脑外病灶缩小52.9%(9/17),中国癌症杂志Vol9, No2, June,1999,替尼泊苷联合尼莫司汀治疗转移性脑肿瘤,结果患者存活时间1-17月,平均6.5月超过6个月者11例,中国癌症杂志Vol9, No2, June,1999,避开BBB的方式,椎管内化疗:主要用于CNS淋巴瘤,脑膜转移肿瘤,白血病的脑膜侵犯。,Phase 2 study of BCNU and temozolomide for recurrent glioblastoma multiforme: North American Brain Tumor Consortium study,Neuro-oncol. 2004 January; 6(1): 3337,可评价病人数PRSDMTTP(w)PFS-6MS(w)MPFS(w)OS-61Year,532211721%341168%26%,可评价病人数CRPRMTTP(w)PFS-6(m),42091730.3%,Second-line chemotherapy with irinotecan plus carmustine in glioblastoma recurrent or progressive after first-line temozolomide chemotherapy: a phase II study of the Gruppo Italiano Cooperativo di Neuro-Oncologia (GICNO).,J Clin Oncol. 2004 Dec 1;22(23):4779-86,2007年ASCO有关Gliomas的文献有36篇,病人数可评价病人数PRMPFS(w)MOS(w)PFS-6,685959%234043%,In grade III patients the median PFS was 42 weeks, the 6 month PFS was 61% the medial overall survival was 60 weeks Conclusion: The combination of bevacizumab and irinotecan is safe and demonstrates superior activity against malignant gliomas.,Phase II trial of bevacizumab and irinotecan in the treatment of malignant gliomas,A phase II, randomized, non-comparative clinical trial of the effect of bevacizumab (BV) alone or in combination with irinotecan (CPT) on 6-month progression free survival (PFS6) in recurrent, treatment-refractory glioblastoma (GBM).,J Clin Oncol 26: 2008 (May 20 suppl; abstr 2010b,Bevacizumab plus irinotecan in recurrent glioblastoma multiforme,J Clin Oncol. 2007 Oct 20;25(30):4722-9,可评价病人数PRPFS-6OS-6,3557%46%77%,Phase II trial of irinotecan and thalidomide in adults with recurrent glioblastoma multiforme,可评价病人数CRPRSDMPFS(w)MOS(w)1Year,3211119133634%,Neuro Oncol. 2008 Feb 26,Bevacizumab and irinotecan for recurrent oligodendroglial tumors.,Conclusions: This regimen is effective in recurrent oligodendrogliomas,and the overall tolerance is acceptable.,ASCO 2009,Abstract 2054,25Pts.CRPRM-PFS(d)MOS(d)6-PFS(ms),20%52%17432842%,ASCO 2009,Abstract 2037,2009年ASCO有关神经系统肿瘤的文献80余篇,A phase II study of XL184 in patients (pts) with progressive glioblastomamultiforme (GBM) in first or second relapse.,Conclusions: XL184at a dose of 175 mg PO qd, has demonstrated substantial activity in ptswith progressive or recurrent GBM.,ASCO 2009, Abstract 2047,26Pts.PRSDPD6-PFS(ms),38%35%27%,(9pts received bevacizumab),脑胶质瘤和转移性瘤耐药的研究,1) 6-甲基鸟嘌呤DNA甲基转移酶 (MGMT) (6-methylguanine-DNA hyltransferase )2) P-glycoprotein,Fruehauf, J. P. et al. Clin Cancer Res 2006;12:4523-4532,脑胶质瘤和转移性瘤耐药的研究,Fruehauf, J. P. et al. Clin Cancer Res 2006;12:4523-4532,MGMT methylation status as a prognostic factor in anaplastic astrocytomas.,Conclusions: MGMT methylation status is an independent prognostic factor together with age in AA.,Pts.71/80(88.8%),30/71(M) 41/71(UM),MGMT methylation,M-PFS(ms),48.6 38,p=0.09,ASCO 2009 Abstract 2052,P-gp expression in brain capillary endothelial cells suggests that P-gp may restrict drug entry into brain tumors and thus be another mechanism of drug resistance.,K1735 cells,K1735 cells,MDR,The biology and mechanism of chemoresistance of brain metastases,THE UNIVERSITY OF TEXAS GRAD. SCH. OF BIOMED. SCI. AT HOUSTON 1995,BBBD(blood-brain barrier disruption)化疗高渗性、缓激肽衍生物:BBB开放选择性开放血瘤屏障(blood-tumor barrier, BTB)克服化疗耐药性多药耐药及逆转 MGMT表达预测化疗疗效,避免无效化疗。,脑胶质瘤和转移性瘤耐药的研究,联合化疗提高化疗敏感性,VM-26和BCNU联合显著提高胶质瘤对化疗的敏感性机理:抑制MDR-I或P-gp过表达PCV方案显著增强多形胶质母细胞瘤对BCNU类药制的敏感性机理:肿瘤细胞先暴露于烷化剂类药物使瘤细胞中AGT(O6-烷基鸟嘌呤-DNA烷基化转酶)活性受抑 AGT是增强肿瘤细胞对BCNU类 药物敏感性的主要靶点,Randomized Comparison of Intra-arterial Versus Intravenous Infusion of ACNU for Newly Diagnosed Patients with Glioblastoma,To compare the effectiveness of intra-arterial ACNUwith intravenous ACNU in newly diagnosed patients with supratentorial glioblastoma.,ACNU (80mg/m2) once every 6 weeks concomitant with radiotherapy.,病人数可评价病人数MS(w)PFS(w)Toxicity,8482,IA5924-,IV5645-,Journal of neuro-oncology2000,vol.49,no1,pp.63-70,2008年NCCN指南,成人侵润性低度恶性幕上星形细胞瘤/少突胶质细胞瘤辅助化疗:高剂量替莫唑胺 5/28方案复发或进展:一线方案:替莫唑胺 5/28方案(初治)二线方案:BCUN210mg/m2 iv 6w重复;,80mg/m2x3 6w重复; CCNU 110mg/m2 口服 6w重复;PCV联合化疗成人室管膜瘤:复发用vp-16,替莫唑胺 ,亚硝脲类,铂及联合方案,原发性CNS肿瘤化疗指南,多形性胶母细胞瘤辅助化疗:同步替莫唑胺 75mg/m2 daily替莫唑胺150-200mg/ m2 5/28方案复发/挽救治疗:替莫唑胺 5/28方案(初治)Bevacizumab+Irinotecan BCUN; CCNU ;PCV联合化疗间变形星形细胞瘤/少突胶质细胞瘤辅助化疗:替莫唑胺或亚硝脲复发/挽救治疗:替莫唑胺 5/28方案(初治)Bevacizumab+Irinotecan BCUN; CCNU ;PCV联合,原发性CNS肿瘤化疗原则,2008年NCCN指南,转移性脑肿瘤局限1-3或多发3个以上对原发肿瘤有效的药物替莫唑胺 5/28方案(器官特异性治疗)卡培他宾,大剂量MTX(乳腺癌,淋巴瘤),Toptecan(肺癌)癌性脑膜炎采用对脑组织穿透能力强的药物;椎管内化疗(脂质体cytarabine, MTX, cytarabine, Thiotepa )大剂量MTX治疗淋巴瘤性脑膜炎原发性中枢神经系统淋巴瘤大剂量MTX3.5g/m2 或更高剂量,或联合化疗复发或进展:再次大剂量MTX美罗华+替莫唑胺 美罗华;Toptecan 替莫唑胺MVP铂类,大剂量cytarabine, DEX,2008年NCCN指南,转移性CNS肿瘤化疗原则,恶性脑肿瘤是以外科手术、放射治疗为主的综合治疗,传统的化疗药物疗效有限,只能使部分患者受益,伴随着各类新药的诞生,特别是靶向药物和生物酶抑制剂的应用,恶性脑肿瘤的综合治疗已显露出端倪。在恶性脑肿瘤的综合治疗中,肿瘤内科所扮演的角色日显重要。随着精确放射治疗,生物靶区的确立,新型化疗药物和靶向药物的联合应用,恶性脑肿瘤的治疗必将更上新的台阶。,结 语,谢谢,- 配套讲稿:
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