中期肝細(xì)胞癌TACE聯(lián)合索拉非尼治療結(jié)果SPACE研究

上傳人:kfc****60 文檔編號(hào):100742535 上傳時(shí)間:2022-06-03 格式:PPTX 頁數(shù):35 大小:7.07MB
收藏 版權(quán)申訴 舉報(bào) 下載
中期肝細(xì)胞癌TACE聯(lián)合索拉非尼治療結(jié)果SPACE研究_第1頁
第1頁 / 共35頁
中期肝細(xì)胞癌TACE聯(lián)合索拉非尼治療結(jié)果SPACE研究_第2頁
第2頁 / 共35頁
中期肝細(xì)胞癌TACE聯(lián)合索拉非尼治療結(jié)果SPACE研究_第3頁
第3頁 / 共35頁

下載文檔到電腦,查找使用更方便

20 積分

下載資源

還剩頁未讀,繼續(xù)閱讀

資源描述:

《中期肝細(xì)胞癌TACE聯(lián)合索拉非尼治療結(jié)果SPACE研究》由會(huì)員分享,可在線閱讀,更多相關(guān)《中期肝細(xì)胞癌TACE聯(lián)合索拉非尼治療結(jié)果SPACE研究(35頁珍藏版)》請(qǐng)?jiān)谘b配圖網(wǎng)上搜索。

1、讀書匯報(bào)讀書匯報(bào)Mu LuwenMu Luwen2016-04-272016-04-27Intermediate stage (Barcelona clinic liver cancer stage B) HCC Asymptomatic Non-invasive Multinodular Unresectable tumors Adequate preservation of liver function Background & Aims Transarterial chemoembolization with doxorubicin-eluting beads (DC Bead; DEB

2、-TACE) is effective in patients with Barcelona clinic liver cancer stage B hepatocellular carcinoma (HCC). The multikinase inhibitor sorafenib enhances overall survival (OS) and time-to-tumor progression (TTP) in patients with advanced HCC. This exploratory phase II trial tested the efficacy and saf

3、ety of DEB-TACE plus sorafenib in patients with intermediate stage HCC.Why choose DEB-TACE? TACE procedures can vary substantially, with regards to both the chemotherapeutic agent and embolization method, making these procedures quite heterogeneous. No consensus has been reached concerning the numbe

4、r of TACE administrations or the time between administrations. DEB-TACE reduce peak concentrations and total systemic exposure to doxorubicin, and ensure high concentrations in the tumor and adequate arterial occlusion. These beads show sustained, continuous release of doxorubicin for 14 days, with

5、a significantly lower systemic plasma concentration of doxorubicin compared with intraarterial injection. DEB-TACE reduced the rates of systemic adverse events (AE) and liver toxicity compared with conventional TACE with Lipiodol and doxorubicin.Patients were included if: Age 18 years, with a life e

6、xpectancy 12 weeks; BCLC stage B HCC with measurable lesions on CT or MRI; Child-Pugh class A and compensated liver function; ECOG performance status of 0; Bone marrow function (hemoglobin 9.0 g/dl; absolute neutrophil count (ANC) 1500/mm3; platelet count P60 109/L); Liver function (bilirubin 3 mg/d

7、l; ALT and AST5 times the upper limit of normal (ULN); no ascites; alkaline phosphatase 4 times upper limit of normal (ULN); PT-INR 2.3 or PT 6 seconds above control) kidney function (serum creatinine 1.5 times ULN; amylase and lipase 3 times ULN).Patients were excluded if: diffuse HCC; vascular inv

8、asion (including segmental portal obstruction); extrahepatic tumor spread; advanced liver disease, as shown by Child-Pugh class B or C liver function, gastrointestinal bleeding, encephalopathy, or ascites; contraindications for embolization, including known hepatofugal blood flow or portosystemic sh

9、unt. if the target lesion had previously undergone local treatment, including resection, radiofrequency ablation (RFA), percutaneous ethanol injection (PEI), or TACE; if they had received local therapy within 4 weeks of a baseline scan; had prior transarterial embolization or TACE; were previously t

10、reated with a kinase inhibitor; had received anthracyclines or radiotherapy for HCC. Study protocol Patients were randomized 1:1 to DEB-TACE (300500 lm beads; 150 mg doxorubicin) plus sorafenib (400 mg twice daily, continuously) or matching placebo. Patients were stratified by geographic region (Ame

11、ricas, Europe, Asia Pacific) and by serum alpha-fetoprotein (AFP) concentration (2; platelet count 60109/L. Kudo M, Matsui O, Izumi N, et al. Transarterial chemoembolization failure/refractoriness: JSH-LCSGJ criteria 2014 update. Oncology. 2014. 87 Suppl 1: 22-31.Trial profileEnrolled 307 patients a

12、t 85 centers in 13 countries.Results of the SPACE trialTTPTime to MVI/EHSOSTime to unTACEable progression (TTUP)Overall response rate (ORR) Disease control rate (DCR)SafetyTime-to-progression (TTP)Time to macrovascular invasion/extrahepatic spread (MVI/EHS)Time to unTACEable progression (TTUP) The l

13、eading cause in the sorafenib arm was deterioration of Child-Pugh status (68/110 or 61.8% of patients). In the placebo arm it was failure to achieve an objective response (50/96 or 52.1%) followed by deterioration of Child-Pugh status (41/96 or 42.7%).Overall survival (OS) The median OS not reached

14、in either group after a median follow-up of 270 days (52 events) and 272 days (49 events), respectively.Safety Four deaths in the sorafenib arm (two due to hepatobiliary/liver dysfunction and one each to constitutional (unspecified) and syndromeother (unspecified) One death in the placebo arm (due t

15、o perforation of the duodenum)Safety Summary The combination of sorafenib plus DEB-TACE was feasible, with manageable toxicities, in patients with intermediate stage HCC and good liver function. The combination did not provide meaningful clinical benefit compared with DEB-TACE alone. The regional di

16、fferences highlight that the amount of combined treatment received may have been a critical determinant of the clinical outcomes. Discordance between investigator and central radiologic review and the criteria for additional TACE also may have impacted outcomes. Whether DEB-TACE is the optimal backb

17、one for combination with sorafenib is still unresolved.ThinkingTACE and Sorafenib: A Good Marriage? The multidisciplinary approach to treating HCC. TACE causes increased hypoxia leading to an upregulation in hypoxia inducible factor-1 (HIF-1), which in turn upregulates vascular endothelial growth fa

18、ctor (VEGF), platelet-derived growth factor receptor, and increases tumor angiogenesis. The use of an antiangiogenic therapy in combination with TAE is supported in a preclinical model to cause a reduction in tumor volume and vessel density, as well as a prolongation in survival compared with TAE al

19、one.Li X, Feng GS, Zheng CS, et al: Expression of plasma vascular endothelial growth factor in patients with hepatocellular carcinoma and effect of transcatheter arterial chemoembolization therapy on plasma vascular endothelial growth factor level. World J Gastroenterol 10:2878-2882, 2004Wang B, Xu

20、H, Gao ZQ, et al: Increased expression of vascular endothelial growth factor in hepatocellular carcinoma after transcatheter arterial chemoembolization. Acta Radiol 49:523-529, 2008Jiang H, Meng Q, Tan H, et al: Antiangiogenic therapy enhances the efficacy of transcatheter arterial embolization for

21、hepatocellular carcinomas. Int J Cancer 121:416-424, 2007 The dose modification and treatment discontinuation More than one-third of patients in the sorafenib group received only one round of TACE, with the major reasons for TACE discontinuations in the sorafenib arm being worsening of liver functio

22、n and decrease of platelet count to 60,000/mm3. Such strict criteria did not take into account transient changes in liver function or platelet count and indeed at least 30% deemed ineligible for additional TACE per protocol did receive further TACE outside the study. The conservative TACE continuati

23、on rules in the SPACE trial may have contributed to the low response rate and shorter TTUP. The high biological heterogeneity across HCC Certain clinical or biological subsets of patients might be more likely to respond to sorafenib, and an unselected adjuvant population could obscure a signal of ef

24、ficacy within a subset. However, without established predictive biomarkers of sorafenib response in advanced disease, a biomarker-enriched adjuvant population cannot be defined. The timing of antiangiogenic therapy with sorafenib The first is a sequential model where the TACE is completed and then f

25、ollowed by the antiangiogenic therapy. A second model is that of an interrupted approach where antiangiogenic therapy is given throughout and is only temporarily interrupted around the time of the embolization. A third model is that of continuous administration of antiangiogrenic therapy throughout

26、the embolization period. Strebel BM, Dufour JF: Combined approach to hepatocellular carcinoma: A new treatment concept for nonresectable disease. Expert Rev Anticancer Ther 8:1743-1749, 2008 The first two models address the risk of bleeding from continuing sorafenib at the time of an invasive vascul

27、ar procedure like TACE or DEB-TACE. The third continuous administration approach, as yet untested clinically, aims at inhibiting the surge of VEGF after embolization that rises to approximately 160% of the baseline level on day 1, and falls back to 130% and 120% on days 2 and 3, respectively. The op

28、timal clinical approach will depend on the balance between safety and efficacy. Li X, Feng GS, Zheng CS, et al: Expression of plasma vascular endothelial growth factor in patients with hepatocellular carcinoma and effect of transcatheter arterial chemoembolization therapy on plasma vascular endothel

29、ial growth factor level. World J Gastroenterol 10:2878-2882, 2004 The best way to assess outcome (embolization + sorefenib) RECIST criteria the EASL guidelines modified RECIST assessment Await a prospective validation The definition of efficacy The optimal end point controversy will remain unanswere

30、d at least for now. The SPACE study has time to tumor progression as the primary end point and defines failure of therapy as an inability to achieve objective response after more than two TACE procedures in the treated tumor nodule.In conclusion There remains no established role for sorafenib as adj

31、uvant therapy for patients with hepatocellular carcinoma after liver-directed therapy. We should reassess the optimum starting dose of sorafenib to avoid these liabilities of delay and discontinuation for future trials and patients, across disease stages.THANK YOU!Sun Yat-sen University Cancer Center

展開閱讀全文
溫馨提示:
1: 本站所有資源如無特殊說明,都需要本地電腦安裝OFFICE2007和PDF閱讀器。圖紙軟件為CAD,CAXA,PROE,UG,SolidWorks等.壓縮文件請(qǐng)下載最新的WinRAR軟件解壓。
2: 本站的文檔不包含任何第三方提供的附件圖紙等,如果需要附件,請(qǐng)聯(lián)系上傳者。文件的所有權(quán)益歸上傳用戶所有。
3.本站RAR壓縮包中若帶圖紙,網(wǎng)頁內(nèi)容里面會(huì)有圖紙預(yù)覽,若沒有圖紙預(yù)覽就沒有圖紙。
4. 未經(jīng)權(quán)益所有人同意不得將文件中的內(nèi)容挪作商業(yè)或盈利用途。
5. 裝配圖網(wǎng)僅提供信息存儲(chǔ)空間,僅對(duì)用戶上傳內(nèi)容的表現(xiàn)方式做保護(hù)處理,對(duì)用戶上傳分享的文檔內(nèi)容本身不做任何修改或編輯,并不能對(duì)任何下載內(nèi)容負(fù)責(zé)。
6. 下載文件中如有侵權(quán)或不適當(dāng)內(nèi)容,請(qǐng)與我們聯(lián)系,我們立即糾正。
7. 本站不保證下載資源的準(zhǔn)確性、安全性和完整性, 同時(shí)也不承擔(dān)用戶因使用這些下載資源對(duì)自己和他人造成任何形式的傷害或損失。

相關(guān)資源

更多
正為您匹配相似的精品文檔
關(guān)于我們 - 網(wǎng)站聲明 - 網(wǎng)站地圖 - 資源地圖 - 友情鏈接 - 網(wǎng)站客服 - 聯(lián)系我們

copyright@ 2023-2025  zhuangpeitu.com 裝配圖網(wǎng)版權(quán)所有   聯(lián)系電話:18123376007

備案號(hào):ICP2024067431號(hào)-1 川公網(wǎng)安備51140202000466號(hào)


本站為文檔C2C交易模式,即用戶上傳的文檔直接被用戶下載,本站只是中間服務(wù)平臺(tái),本站所有文檔下載所得的收益歸上傳人(含作者)所有。裝配圖網(wǎng)僅提供信息存儲(chǔ)空間,僅對(duì)用戶上傳內(nèi)容的表現(xiàn)方式做保護(hù)處理,對(duì)上載內(nèi)容本身不做任何修改或編輯。若文檔所含內(nèi)容侵犯了您的版權(quán)或隱私,請(qǐng)立即通知裝配圖網(wǎng),我們立即給予刪除!