Efficacy comparison of fruquintinib,regorafenib monotherapy or plus programmed death-1 inhibitors for microsatellite stable metastatic colorectal cancer

BACKGROUND Regorafenib(R)and fruquintinib(F)are the standard third-line regimens for colorectal cancer(CRC)according to the National Comprehensive Cancer Network guidelines,but both have limited efficacy.Several phase 2 trials have indicated that R or F combined with immune checkpoint inhibitors can reverse immunosuppression and achieve promising efficacy for microsatellite stable or proficient mismatch repair(MSS/pMMR)CRC.Due to the lack of studies comparing the efficacy between F,R,F plus programmed death-1(PD-1)inhibitor,and R plus PD-1 inhibitors(RP),it is still unclear whether the combination therapy is more effective than monotherapy.AIM To provide critical evidence for selecting the appropriate drugs for MSS/pMMR metastatic CRC(mCRC)patients in clinical practice.METHODS A total of 2639 CRC patients were enrolled from January 2018 to September 2022 in our hospital,and 313 MSS/pMMR mCRC patients were finally included.RESULTS A total of 313 eligible patients were divided into F(n=70),R(n=67),F plus PD-1 inhibitor(FP)(n=95)and RP(n=81)groups.The key clinical characteristics were well balanced among the groups.The median progression-free survival(PFS)of the F,R,FP,and RP groups was 3.5 months,3.6 months,4.9 months,and 3.0 months,respectively.The median overall survival(OS)was 14.6 months,15.7 months,16.7 months,and 14.1 months.The FP regimen had an improved disease control rate(DCR)(P=0.044)and 6-month PFS(P=0.014)and exhibited a better trend in PFS(P=0.057)compared with F,and it was also significantly better in PFS than RP(P=0.030).RP did not confer a significant survival benefit;instead,the R group had a trend toward greater benefit with OS(P=0.080)compared with RP.No significant differences were observed between the R and F groups in PFS or OS(P>0.05).CONCLUSION FP is superior to F in achieving 6-month PFS and DCR,while RP is not better than R.FP has an improved PFS and 6-month PFS compared with RP,but F and R had similar clinical efficacy.Therefore,FP may be a highly promising strategy in the treatment of MSS/pMMR mCRC.

Extended survival with metastatic pancreatic cancer under fruquintinib treatment after failed chemotherapy:Two case reports

BACKGROUND Pancreatic cancer is a highly malignant disease.After decades of treatment progress,the current five-year survival rate for patients is still less than 10%.For later-line treatment,the treatment options are even more limited.Anti-angiogenic drugs can improve progression-free survival in patients with advanced pancreatic cancer.Preclinical data show that fruquintinib might improve the prognosis of advanced pancreatic cancer by targeting angiogenesis and lymphopoiesis,improving the abnormal vascular structure,and modulating the tumour immune microenvironment.CASE SUMMARY We present two cases of third-line fruquintinib monotherapy that brought an extraprolonged progress-free survival(PFS)of 10 months.Patient 1 took adjuvant gemcitabine-based and first-line nab-paclitaxel-based chemotherapy and then used local radiotherapy combined with programmed cell death 1 receptor(PD-1).Each line lasted approximately 7 months.Moreover,the patient took third-line fruquintinib,which was followed by stable disease for 10 months,during which no additional adverse effect was observed.The patient later refused to take fruquintinib due to difficulty urinating and lower abdominal pain after the coronavirus disease 2019(COVID-19)infection.The patient died in February 2023.Patient 2 also took two prior lines of chemotherapy and then local radiotherapy combined with S-1.After confirmed disease progression,the patient experienced a continuous partial response after using fruquintinib monotherapy in the third line.After the patient had COVID-19 in December 2022,fruquintinib was discontinued.The patient died in January 2023 due to disease progression.CONCLUSION Both cases achieved a PFS benefit from later-line single-agent fruquintinib therapy.With its better safety profile,fruquintinib may be worth exploring and studying in more depth as a later-line treatment for pancreatic cancer patients.

Oral fruquintinib combined with tegafur-gimeracil-oteracil potassium for advanced colorectal cancer to obtain longer progression-free survival:A case report

BACKGROUND After the failure of second-line standard therapy,effective treatment options for metastatic colorectal cancer are limited,and the duration of remission cannot meet clinical needs.In addition,associated drug toxicity may lead to treatment interruption that may affect patient outcomes.Therefore,more safe,effective and convenient treatments are urgently needed.CASE SUMMARY Here,we describe a patient with advanced colorectal cancer with multiple metastases in both lungs.Oxaliplatin combined with 5-fluorouracil or capecitabine was given as the first-line treatment,and bevacizumab combined with irinotecan was given as the second-line treatment after disease progression.However,treatment was interrupted due to recurrent grade 2 nausea and grade 1 diarrhea.He received targeted therapy with fruquintinib starting on August 26,2020 and responded well for 12 mo.After slow progression of the lung metastases,progression-free survival was again achieved over 13.5 mo by continued treatment of fruquintinib in combination with tegafur-gimeracil-oteracil potassium chemotherapy.Overall treatment duration was more than 25.5 mo.The treatments delayed tumor progression,reduced drug side effects,maintained a good quality of life,and further extended overall survival.CONCLUSION This case report detailed preliminary evidence showing that the combination of fruquintinib with tegafur-gimeracil-oteracil potassium chemotherapy double oral therapy may result in longer progression-free survival in patients with advanced colorectal cancer.

PD-1 inhibitor in combination with fruquintinib therapy for initial unresectable colorectal cancer:A case report

BACKGROUND PD-1 inhibitors in combination with fruquintinib have not previously been reported as neoadjuvant therapy for patients with colorectal cancer.In this case report,the combination of a PD-1 inhibitor and fruquintinib demonstrated good efficacy in patients with MSI-H colorectal cancer.CASE SUMMARY The patient was a young man in his 30s who had MSI-H type colon cancer.The patient underwent four cycles of neoadjuvant therapy with a PD-1 inhibitor combined with fruquintinib before surgery,resulting in regression of the mass and a successful surgery.CONCLUSION Some patients with colorectal cancer have the MSI-H type,and the first-line chemotherapy regimen is not effective.However,PD-1 monoclonal antibody immunotherapy has a good therapeutic effect,which can be improved by combination therapy with fruquintinib.We recommend that patients with a history of colon or rectal cancer receive universal MSI testing;then,neoadjuvant therapy should be used.

Fruquintinib beneficial in elderly patient with neoplastic pericardial effusion from rectal cancer:A case report

BACKGROUND Neoplastic pericardial effusion(NPE)is a rare consequence of rectal cancer and carries a poor prognosis.Optimal management has yet to be determined.Fruquintinib is an oral anti-vascular endothelial growth factor receptor tyrosine kinase inhibitor approved by the China Food and Drug Administration in September 2018 as third-line treatment of metastatic colorectal cancer.CASE SUMMARY Herein,we report an elderly patient with NPE from rectal cancer who responded to the use of fruquintinib.In March 2015,a 65-year-old Chinese woman diagnosed with KRAS-mutated adenocarcinoma of the rectum was subjected to proctectomy,adjuvant concurrent chemoradiotherapy,and adjuvant chemotherapy.By October 2018,a mediastinal mass was detected via computed tomography.The growth had invaded parietal pericardium and left hilum,displaying features of rectal adenocarcinoma in a bronchial biopsy.FOLFIRI and FOLFOX chemotherapeutic regimens were administered as first-and second-line treatments.After two cycles of second-line agents,a sizeable pericardial effusion resulting in tamponade was drained by pericardial puncture.Fluid cytology showed cells consistent with rectal adenocarcinoma.Single-agent fruquintinib was initiated on January 3,2019,as a third-line therapeutic.Ten cycles were delivered before the NPE recurred and other lesions progressed.The recurrence-free interval for NPE was 9.2 mo,attesting to the efficacy of fruquintinib.Ultimately,the patient entered a palliative care unit for best supportive care.CONCLUSION Fruquintinib may confer good survival benefit in elderly patients with NPEs due to rectal cancer.

呋喹替尼治疗转移性结直肠癌的真实世界观察

目的 探讨呋喹替尼治疗转移性结直肠癌(metastatic colorectal cancer,mCRC)的临床疗效和安全性。方法 收集本院2019年1月至2021年12月接受呋喹替尼三线或后线治疗的48例m CRC患者资料。分析其临床治疗、无进展生存期(progression-free survival,PFS)和不良反应发生情况。结果 48例mCRC患者接受呋喹替尼治疗2~17个周期,完全缓解(complete response,CR) 0例(0.0%),部分缓解(partial response,PR) 3例(6.2%),疾病稳定(stable disease,SD) 32例(66.7%),疾病进展(progressive disease,PD) 13例(27.1%),疾病控制率(disease control rate,DCR)为72.9%,客观缓解率(objective response rate,ORR)为6.2%,中位PFS为4.9个月。呋喹替尼单药治疗和联合治疗患者的中位PFS分别为4.7个月和6.2个月(P=0.445)。48例患者常见不良反应有高血压、手足皮肤反应、甲状腺功能异常、蛋白尿、乏力和肝功能异常。31.3%(15/48)的患者发生3~4级不良反应,主要是高血压和手足皮肤反应。结论 呋喹替尼在mCRC三线或后线治疗中有明确的临床获益,且耐受性良好,总体不良反应可控,与免疫治疗的联合值得进一步探索。

呋喹替尼联合免疫检查点抑制剂在微卫星稳定型转移性结直肠癌患者后线治疗中的疗效和安全性

目的评估呋喹替尼单药或联合免疫检查点抑制剂(immune checkpoint inhibitor,ICI)在微卫星稳定(microsatellitestable,MSS)型转移性结直肠癌(metastatic colorectal cancer,mCRC)患者三线及以上治疗中的疗效和安全性。方法选择2020年1月至2024年4月在武汉大学人民医院肿瘤科接受治疗的pMMR/MSS型mCRC患者为研究对象。在未调整模型和倾向性匹配中比较呋喹替尼单药或呋喹替尼联合ICI的预后、疗效以及安全性。结果共104例患者纳入分析,其中呋喹替尼组33例,呋喹替尼联合ICI组71例。与呋喹替尼组相比,呋喹替尼联合ICI组的中位无进展生存期更长(3.0个月vs 4.5个月;HR=0.55,95%CI:0.33~0.89);但两组的中位总生存期(10.1个月vs 13.1个月)、客观缓解率(9.1%vs 11.3%)、疾病控制率(51.5%vs 66.2%)比较,差异均无统计学意义(均P>0.05)。倾向性匹配分析亦获得类似的结果。两组3级及以上不良事件均主要包括手足皮肤反应、血小板减少和白细胞减少;其中呋喹替尼组3级及以上不良事件的发生率为30.3%,呋喹替尼联合ICI组为36.6%(P=0.529)。结论相比于呋喹替尼,呋喹替尼联合ICI可为pMMR/MSS型mCRC患者的三线及以上治疗带来无进展生存期获益,安全性可控,值得进一步研究。

信迪利单抗联合呋喹替尼对结直肠癌肝转移的疗效及安全性

目的探讨信迪利单抗联合呋喹替尼对结直肠癌肝转移的疗效及安全性。方法将台州市中心医院2021年1月至2023年12月收治的90例结直肠癌肝转移患者,根据随机数字表法分为对照组(n=45)和联合组(n=45)。对照组予以呋喹替尼胶囊口服,联合组加用信迪利单抗静脉滴注,治疗12周后评价两组患者的临床疗效,比较两组治疗前后肿瘤标志物[癌胚抗原(CEA)、糖类抗原125(CA-125)、糖类抗原199(CA-199)水平],记录两组胃肠道不良反应、手足皮肤反应、高血压、天冬氨酸氨基转移酶(AST)升高、蛋白尿等不良反应发生情况。结果治疗12周后,联合组ORR(20.00%)与DCR(88.89%)均高于对照组ORR(4.44%)与DCR(68.89%)(χ^(2)=5.075,5.404,均P<0.05);治疗12周后,联合组CEA、CA-125、CA-199[分别为(19.44±2.18)μg·L^(-1)、(35.82±4.66)U·mL^(-1)、(31.23±4.15)kU·mL^(-1)]均低于对照组[分别为(23.68±2.89)μg·L^(-1)、(40.29±5.07)U·mL^(-1)、(36.49±4.54)kU·mL^(-1)](t=7.857,4.354,5.737,均P<0.05)。两组胃肠道不良反应、手足皮肤反应、高血压、AST升高、蛋白尿不良反应发生情况差异均无统计学意义(χ^(2)=0.257,0.476,0.800,0.104,0.304,均P>0.05)。结论对于结直肠癌肝转移患者,信迪利单抗与呋喹替尼联合应用疗效显著,可降低患者肿瘤标志物水平,且不会增加不良反应的发生,安全可控。

呋喹替尼单药及联合PD-1抑制剂用于晚期转移性结肠癌后线治疗的疗效及安全性

目的 探讨PD-1单抗联合及呋喹替尼单药对晚期转移性结直肠癌的效果、安全性及预后影响因素。方法 纳入自2018年6月至2021年12月在医院接受呋喹替尼联合PD-1抑制剂治疗的31例、呋喹替尼单药治疗的42例及四线化疗35例患者为研究对象,回顾性地分析患者的疗效、生存期及主要不良反应,探讨无进展生存期(PFS)及总生存期(OS)的危险因素。结果 联合用药组与化疗组及单药组PFS比较存在差异,与化疗组比较OS差异显著。分化程度及治疗方案是影响联合用药组与化疗组患者PFS的独立危险因素,治疗方案是影响患者OS的独立危险因素。分化程度是影响联合用药与单药组患者PFS的独立危险因素。呋喹替尼单药或联合PD-1较传统化疗多项不良反应发生率降低,而高血压发生率升高。结论 呋喹替尼联合PD-1单抗后线治疗晚期CRC患者具有潜在的疗效和可控的安全性,分化程度可能是影响患者PFS的独立危险因素。

程序性死亡受体1抑制剂联合呋喹替尼后线治疗转移性结直肠癌的临床疗效和安全性研究

背景结直肠癌发病率较高,转移性结直肠癌(mCRC)已进入靶向免疫治疗新时代,由于mCRC有效的后线治疗选择十分有限,而且经历三线以上治疗的患者因长时间治疗身体素质较前大幅度下降,因此,选用毒副作用小且疗效佳的后线治疗方式有待进一步探索。目的观察呋喹替尼与程序性死亡受体1(PD-1)抑制剂联用治疗三线及以上mCRC的临床疗效和安全性。方法收集2020年6月至2022年3月郑州大学第一附属医院收治的75例mCRC患者的临床资料进行回顾性分析,根据不同的治疗方案分为呋喹替尼单药组(n=28)和PD-1抑制剂联合呋喹替尼组(n=47)。治疗方案为呋喹替尼单药组:口服呋喹替尼胶囊,1次/d,5 mg/次,连服3周,停1周,每28 d为1个治疗周期;PD-1抑制剂联合呋喹替尼组:呋喹替尼使用方法与单药组一致,PD-1抑制剂用药剂量及时间为第1天静脉滴注卡瑞利珠单抗/信迪利单抗/帕博利珠单抗200 mg、特瑞普利单抗240 mg,每21 d为1个治疗周期。主要观察指标为两组患者客观有效率(ORR)、疾病控制率(DCR)、无进展生存期(PFS)和不良反应发生率。结果截至末次随访(2022-05-31),呋喹替尼单药组患者ORR为7.1%,DCR为67.9%;PD-1抑制剂联合呋喹替尼组患者ORR为14.9%,DCR为89.4%;PD-1抑制剂联合呋喹替尼组患者DCR明显高于呋喹替尼单药组(χ^(2)=5.345,P=0.021)。PD-1抑制剂联合呋喹替尼组和呋喹替尼单药组患者中位PFS分别为6.4(4.0,13.1)个月、4.5(2.9,8.2)个月;两组患者PFS比较,差异有统计学意义(χ^(2)=5.504,P=0.019)。两组患者治疗过程中的不良反应多为1~2级。PD-1抑制剂联合呋喹替尼组患者甲状腺功能减退发生率高于呋喹替尼单药组(P<0.05);两组患者其余不良反应发生率比较,差异均无统计学意义(P>0.05)。结论PD-1抑制剂联合呋喹替尼与呋喹替尼单药治疗相比,mCRC患者的生存期延长,严重的不良反应发生率较低,是一种疗效更好的治疗方案。

呋喹替尼联合信迪利单抗治疗晚期微卫星稳定型结直肠癌疗效观察

目的观察呋喹替尼联合信迪利单抗治疗晚期微卫星稳定型结直肠癌的临床治疗效果及安全性。方法收集44例晚期微卫星稳定型结直肠癌患者,根据治疗方法分为呋喹替尼单药组(n=22)和呋喹替尼联合信迪利单抗组(n=22)。治疗方案:呋喹替尼单药组口服呋喹替尼5 mg,每日1次,服用3周停药1周,每28天为1周期;呋喹替尼联合信迪利单抗组静脉滴注信迪利单抗200 mg,每3周1次、呋喹替尼方案同单药组,并分析临床效果及不良反应。结果呋喹替尼单药组患者客观缓解率(ORR)为9.09%,疾病控制率(DCR)为45.45%;呋喹替尼联合信迪利单抗组患者ORR为18.18%,DCR为63.64%;呋喹替尼单药组中位无进展生存期(mPFS)为4.4(2.1,8.2)个月,呋喹替尼联合信迪利单抗组患者中位PFS为6.7(3.9,12.6)个月,两组差异有统计学意义(χ2=4.372,P=0.037)。两组患者治疗过程中的不良反应多为1~2级,且差异均无统计学意义(P>0.05)。结论呋喹替尼联合信迪利单抗较呋喹替尼单药治疗可给经标准治疗失败后的晚期微卫星稳定型结直肠癌患者带来更好的临床获益,且安全性良好。

信迪利单抗联合呋喹替尼治疗微卫星稳定型晚期结肠癌患者的临床疗效及对患者免疫功能的影响

目的:探索信迪利单抗联合呋喹替尼治疗微卫星稳定型(MSS)晚期结肠癌的临床疗效及对患者免疫功能的影响。方法:选取于2018年12月至2020年12月于江苏大学附属武进医院就诊的76例晚期结肠癌患者作为研究对象,随机分为对照组和观察组,每组38例。对照组给予呋喹替尼治疗,观察组给予信迪利单抗联合呋喹替尼治疗。对比两组患者治疗6个月的临床疗效,并分别于治疗前后采集外周血,采用流式细胞实验测定T淋巴细胞亚群(CD3^(+)T、CD4^(+)T、CD8^(+)T、CD4^(+)T/CD8^(+)T)变化,采用ELISA实验测定补体(C3、C4)和免疫球蛋白(IgA、IgG、IgE)水平。出院后完成2~3年随访,绘制生存曲线,比较生存与无进展生存情况。结果:治疗6个月,观察组疾病控制率(86.84%)优于对照组(60.53%);客观缓解率(36.84%)优于对照组(13.16%),差异有统计学意义(P<0.05)。治疗前,两组T淋巴细胞亚群、补体和免疫球蛋白水平差异不大;治疗后6个月,观察组CD4^(+)T/CD8^(+)T、IgA及IgG水平高于对照组,差异有统计学意义(P<0.05)。观察组治疗1年与2年的生存率优于对照组,治疗2年的无进展生存率优于对照组,截至随访结束时中位生存期和无进展生存期均高于对照组,差异有统计学意义(P<0.05)。两组患者各不良反应发生率差异均无统计学意义(P>0.05)。结论:信迪利单抗联合呋喹替尼治疗MSS晚期结肠癌的临床疗效优于呋喹替尼单药,对患者免疫功能的影响相对较小,不良反应可耐受,具有潜在应用价值。

负载呋喹替尼酸敏感靶向胶束的制备及其体外抗肿瘤活性评价

目的:构建一种负载呋喹替尼(FRU)的高选择性酸敏感靶向胶束cRGD-FRU-ASM。方法:以环状精氨酸-甘氨酸-天冬氨酸肽(cRGD)为靶头,磷脂-聚(2-乙基-2-噁唑啉)、磷脂-聚乙二醇2000-环肽为药物载体,FRU为模型药物,通过薄膜分散法制备cRGD-FRU-ASM。测定该胶束表征及临界浓度,分析药物释放情况。以人宫颈癌Hela细胞为观察对象评估该胶束的体外抗肿瘤活性。结果:cRGD-FRU-ASM为均一、乳白色混悬液,粒径约31.89 nm,呈规整的近圆形,分散性良好,分散指数为0.231,电位为-17.4 mV。临界浓度低,为4.267 mg/L。当pH为5.0时,FRU的累积释放量最多,约为80%。体外抗肿瘤活性结果显示cRGD-FRU-ASM能够抑制Hela细胞的增殖和转移,且具有抗血管生成作用(P<0.05)。结论:cRGD-FRU-ASM靶向胶束可提高FRU的利用度,增强药物对肿瘤细胞的增殖抑制作用,同时降低药物对正常组织的毒性,达到优异的抗肿瘤效果。

呋喹替尼与瑞戈非尼三线治疗亚裔晚期结直肠癌疗效与安全性的调整间接比较

目的间接比较呋喹替尼与瑞戈非尼在三线亚裔晚期结直肠癌人群中的疗效及安全性。方法按检索策略对中国生物医学文献库、中国期刊全文数据库、维普数据库、万方期刊数据库、Medline、EMBase建库以来的所有文献进行检索,检索截止时间为2019年5月10日。根据纳入标准筛选随机对照试验,以客观有效率(ORR)、疾病控制率(DCR)、中位无进展生存期(PFS)、中位总生存期(OS)以及3级及以上高血压、手足综合征和肝脏毒性发生率为研究指标,通过Bucher调整间接比较法进行分析。结果共纳入4项随机对照试验,包括接受呋喹替尼的患者325例,瑞戈非尼的患者201例。调整间接比较结果显示,呋喹替尼对比瑞戈非尼,ORR的RR为1.54(95%CI:0.08~30.56,P=0.778),DCR的RR为0.92(95%CI:0.43~1.95,P=0.825),中位OS与中位PFS的HR分别为1.10(95%CI:0.76~1.59,P=0.611)和0.72(95%CI:0.50~1.03,P=0.069),差异均无统计学意义。呋喹替尼对比瑞戈非尼,3级及以上高血压、手足综合征、谷草转氨酶升高发生率的RR分别为2.40(95%CI:0.45~12.71,P=0.302)、0.76(95%CI:0.05~12.40,P=0.847)和0.08(95%CI:0.01~1.33,P=0.079),差异均无统计学意义。结论呋喹替尼与瑞戈非尼三线治疗亚裔晚期结直肠癌的疗效与安全性相当。

呋喹替尼与瑞戈非尼治疗转移性结直肠癌疗效与安全性Meta分析

目的系统评价呋喹替尼与瑞戈非尼治疗转移性结直肠癌的疗效与安全性。方法计算机检索中国知网、万方、维普等中文数据库和PubMed,Elsevier ScienceDirect,Embase,Springer等外文数据库,收集国内外公开发表的呋喹替尼和瑞戈非尼治疗转移性结直肠癌的随机对照试验(RCT),检索时间为自建库至2018年12月31日。按Jadad评分系统对纳入研究进行质量评价,采用RevMan 5.3软件和加拿大药物和卫生技术局(CADTH)发布的间接比较软件进行效应量合并和间接Meta分析。结果共纳入4个RCTs,呋喹替尼组325例,瑞戈非尼组641例。Meta分析结果显示,与安慰剂比较,呋喹替尼和瑞戈非尼均显著提高患者的总生存期、无进展生存期、客观缓解率和疾病控制率;在安全性方面,虽总不良事件发生率、3级或4级不良事件发生率均高于安慰剂组,但多数可通过减量或停药得到控制;两组患者的总生存期[HR=1,95%CI(0.668,1.496)]、无疾病生存期[HR=0.65,95%CI(0.395,1.068)]、总缓解率[OR=1.99,95%CI(0.14,28.381)]、疾病控制率[OR=1.646,95%CI(0.454,5.964)]、总不良事件发生率[OR=0.714,95%CI(0.132,3.868)]、3级或4级不良事件发生率[OR=0.775,95%CI(0.442,1.357)]比较,差异均无统计学意义(P>0.05)。结论呋喹替尼与瑞戈非尼治疗转移性结肠癌的有效性和安全性均相当。

呋喹替尼与TAS-102治疗晚期结直肠癌疗效与安全性的间接比较

【目的】间接比较呋喹替尼与TAS-102治疗晚期结直肠癌的疗效与安全性。【方法】检索美国国立医学图书馆生物医学信息检索系统(PubMed)、荷兰医学文摘(EMBASE/SCOPUS)、Cochrane图书馆,以及中国知网中国知识基础设施工程(CNKI)、万方数据库等数据库发表的关于呋喹替尼与TAS-102治疗晚期结直肠癌的临床随机对照实验,检索时间从1990年1月1日截止2020年9月5日。按照Jadad评分对纳入研究进行质量评价,采用Stata 16.0软件和加拿大药物和卫生技术局发布的ITC软件进行Meta分析和间接比较。【结果】共纳入5项随机对照实验(RCT),包括1862名患者,实验组1242名患者接受呋喹替尼/TAS-102治疗,对照组620名患者接受安慰剂治疗。Meta分析显示:呋喹替尼和TAS-102皆可以提高患者的中位生存期(mOS),中位无进展生存期(mPFS)和疾病控制率(DCR),但不能改善患者的客观缓解率(ORR)。安全性方面,呋喹替尼可增加患者严重不良事件数,但血小板减少、疲劳及腹泻较安慰剂组无明显变化;TAS-102的严重不良事件数及疲劳较安慰剂组无明显变化,但血小板减少和腹泻较安慰剂组增加。间接比较显示:呋喹替尼对比TAS-102,mOS的HR为0.957(95%CI:0.72~1.26,P=0.87),mPFS的HR为0.578(95%CI:0.44~0.76,P=0.292),ORR的RR为1.447(95%CI:0.341~6.15,P=0.84),DCR的RR为1.45(95%CI:1.02~2.06,P=0.22),血小板减少的RR为0.347(95%CI:0.157~0.764,P=0.47),疲劳的RR为12.43(95%CI:7.95~19.44,P=0.14),腹泻的RR为0.97(95%CI:0.223~4.222,P=0.985),皆无统计学意义。但呋喹替尼对比TAS-102可增加严重不良事件数的发生,[RR=17(95%CI:4.96~58.28,P=0.00)]。【结论】呋喹替尼对比TAS-102治疗晚期结肠癌疗效相当,严重不良事件数的发生会增加。

临床药师参与呋喹替尼致血压升高的药学监护

临床药师参与1例服用呋喹替尼后出现血压升高的结直肠癌患者药学监护,分析呋喹替尼与血压升高的关联后,对高血压进行评估,协助医生制定个体化用药方案,患者血压得到控制。临床药师参与临床药物治疗实践,有助于提高抗肿瘤药物治疗的有效性和安全性。

呋喹替尼在晚期结直肠癌中的研究进展

呋喹替尼是一种有效的、高选择性和口服VEGFR 1、2、3酪氨酸激酶抑制剂,由Hutchison MediPharma发现并开发用于治疗实体肿瘤。2018年9月,呋喹替尼在中国获得全球首个批准,用于接受至少两种系统性抗肿瘤治疗失败的转移性结直肠癌患者治疗。临床研究表明,它具有脱靶毒性低、耐药性好、疗效强等优点。本文综述了呋喹替尼的分子结构、作用机制、药代动力学、临床疗效和安全性,并讨论了其在其他肿瘤类型中的潜在临床应用。

PNI对呋喹替尼三线治疗晚期结直肠癌患者的预后生存分析

目的探讨预后营养指数(PNI)对呋喹替尼三线治疗晚期结直肠癌患者疗效的预后分析。方法选取2017年11月至2020年6月华中科技大学同济医学院附属同济医院肿瘤中心消化肿瘤科及荆州市中心医院肿瘤科收治并接受呋喹替尼三线治疗的晚期结直肠癌患者33例,计算PNI、中性粒细胞/淋巴细胞比值(NLR)、血小板/淋巴细胞比值(PLR)以及淋巴细胞/单核细胞比值(LMR)等营养免疫评估指标。采用Cox比例风险回归模型(简称Cox回归)及Kaplan-Meier曲线Log-rank检验评价相关免疫营养指标对于患者生存的影响。结果根据总生存(OS)期的受试者操作特征曲线(ROC曲线)分析,PNI最佳截止点为46.95;单因素Cox回归分析结果显示,PNI、NLR及LMR是OS的影响因素,多变量Cox分析显示PNI是OS期的独立预后因素。低PNI患者1年生存率为9.894%(95%CI=8.300~23.566),中位总生存(mOS)期为6.700个月(95%CI=5.524~7.876),高PNI患者1年生存率是42.218%(95%CI=22.496~46.378,P<0.05),mOS期为11.400个月(95%CI=6.123~16.677,P<0.05);PNI低的患者中位无进展生存(mPFS)期为2.200个月(95%CI=1.278~3.122);PNI高的患者mPFS期为3.067个月(95%CI=1.095~5.039,P>0.05)。结论PNI可作为呋喹替尼三线治疗晚期结直肠癌患者的生存预后因素。

呋喹替尼与瑞戈非尼作为转移性结直肠癌三线治疗的成本-效用分析

目的:从我国医疗卫生系统角度出发,比较呋喹替尼和瑞戈非尼三线治疗转移性结直肠癌(mCRC)的成本-效用。方法:基于两项Ⅲ期临床试验和一篇已发表的网状Meta分析,运用Markov模型模拟疾病进展状况,对两个用药方案进行药物成本效用分析。并采用单因素敏感性分析和概率敏感性分析对结果的不确定性进行评价。结果:基础分析结果显示,呋喹替尼组的总成本为121056.88元,效用值为0.60 QALYs(质量调整生命年);瑞戈非尼组的总成本为159426.06元,效用值为0.57 QALYs,增量成本效用比为负值。单因素敏感性分析显示总生存期(OS)风险比为最大影响因素。概率敏感性分析显示,呋喹替尼为优势方案的比例为100%。结论:与瑞戈非尼相比,呋喹替尼三线治疗mCRC更具成本效用优势。