Prevention of metastasis to liver by using 5-FU intraperitoneal chemotherapy in nude mice inoculated with human colonic cancer cells

AIMS Using a new approach of regional adjuvant chemotherapy to prevent cancer cells hepatic metasta- sis after radical surgery of large bowel cancer. METHODS A model of liver with metastasis of hu- man colonic cancer (HCC) cells in nude mice was used to observe the effect in prevention of metastasis of HCC cells inoculated via spleen applied with early postoper- ative intraperitoneal (IP) chemotherapy using large dose of 5-FU. RESULTS The incidence of metastasis to liver was decreased by 40%,the mean number of metastatic liv- er nodules in each animal was reduced by 50.89% and the mean survival times of each animal was prolonged by 48.21% by using 5-FU 40 mg/NS 40 ml/kg IP for two consecutive days as compared with the controls. CONCLUSIONS IP is a new and more effective re- gional adjuvant chemotheraputic approach in the pre- vention of liver metastasis HCC cells after radical surgery of large bowel cancer.

Adeno-associated virus mediated endostatin gene therapy in combination with topoisomerase inhibitor effectively controls liver tumor in mouse model

AIM:rAAV mediated endostatin gene therapy has been examined as a new method for treating cancer.However, a sustained and high protein delivery is required to achieve the desired therapeutic effects.We evaluated the impact of topoisomerase inhibitors in rAAV delivered endostatin gene therapy in a liver tumor model. METHODS:rAAV containing endostatin expression cassettes were transduced into hepatoma cell lines.To test whether the topoisomerase inhibitor pretreatment increased the expression of endostatin,Western blotting and ELISA were performed.The biologic activity of endostatin was confirmed by endothelial cell proliferation and tube formation assays. The anti-tumor effects of the rAAV-endostatin vector combined with a topoisomerase inhibitor,etoposide,were evaluated in a mouse liver tumor model. RESULTS:Topoisomerase inhibitors,including camptothecin and etoposide,were found to increase the endostatin exPression level in vitro.The over-expressed endostatin, as a result of pretreatment with a topoisomerase inhibitor, was also biologically active.In animal experiments,the combined therapy of topoisomerase inhibitor,etoposide with the rAAV-endostatin vector had the best tumor- suppressive effect and tumor foci were barely observed in livers of the treated mice.Pretreatment with an etoposide increased the level of endostatin in the liver and serum of rAAV-endostatin treated mice.Finally,the mice treated With rAAV-endostatin in combination with etoposide showed the longest survival among the experimental models. CONCLUSION:rAAV delivered endostatin gene therapy in combination with a topoisomerase inhibitor pretreatment is an effective modality for anticancer gene therapy.

Immunotherapy for recurrent hepatocellular carcinoma

Hepatocellular carcinoma(HCC)is presented frequently in late stages that are not amenable for curative treatment.Even for patients who can undergo resection for curative treatment of HCC,up to 50%recur.For patients who were not exposed to systemic therapy prior to recurrence,recurrence frequently cannot be subjected to curative therapy or local treatments.Such patients have several options of immunotherapy(IO).This includes programmed cell death protein 1(PD-1)and cytotoxic T-lymphocyte associated protein 4 treatment,combination of PD-1 and vascular endothelial growth factor inhibitor or single agent PD-1 therapy when all other options are deemed inappropriate.There are also investigational therapies in this area that explore either PD-1 and tyrosine kinase inhibitors or a novel agent in addition to PD-1 with vascular endothelial growth factor inhibitors.This minireview explored IO options for patients with recurrent HCC who were not exposed to systemic therapy at the initial diagnosis.We also discussed potential IO options for patients with recurrent HCC who were exposed to first-line therapy with curative intent at diagnosis.

The value of postoperative hepatic regional chemotherapy in prevention of recurrence after radical resection of primary liver cancer

INTRODUCTIONIn China,primary liver cancer (PLC) ranks secondin cancer mortality since the 1990s.In the field ofPLC treatment,surgical resection remains the best,which includes large PLC resection,small PLCresection,re-resection of subclinical recurrence,aswell as cytoreduction and sequential resection forunresectable PLC.However,recurrence

Liver-first approach of colorectal cancer with synchronous hepatic metastases: A reverse strategy

Recently, there has been a change in the strategy of how synchronous colorectal hepatic metastases are attributed to the development of more valuable protocols of chemotherapy and radiotherapy for neoadjuvant treatment of colorectal neoplasms and their hepatic metastases. There is a consensus that patients with synchronous colorectal hepatic metastases have lower survival than those with metachronous colorectal hepatic metastases. Currently, controversy remains concerning the best approach is sequence in a patient with colorectal cancer and synchronous hepatic metastases resection. To obtain a better patient selection, the authors have suggested the initial realization of systemic chemotherapy in the circumstance of patients with colorectal tumor stage Ⅳ, since these patients have a systemic disease. The rationale behind this liver-first strategy is initially the control of synchronous hepatic metastases of colorectal carcinoma, which can optimize a potentially curative hepatic resection and longstanding survival. The liver-first strategy procedure is indicated for patients with colorectal hepatic metastases who require downstaging therapy to make a curative liver resection possible. Thus, the liver-first strategy is considered an option in cases of rectal carcinoma in the early stage and with limited or advanced synchronous colorectal hepatic metastases or in case of patients with asymptomatic colorectal carcinoma, but with extensive liver metastases. Patients undergoing systemic chemotherapy and with progression of neoplastic disease should not undergo hepatic resection, because it does not change the prognosis and may even make it worse. To date, there have been no randomized controlled trials on surgical approach of colorectal synchronous hepatic metastases, despite the relatively high number of available manuscripts on this subject. All of these published studies are observational, usually retrospective, and often non-comparative. The patient selection criteria for the liver-first strategy should be individualized, and the approach of these patients should be performed by a multidisciplinary team so its benefits will be fully realized.

Preliminary Investigation on Regulating Effects of Different TCM Treatments on Transcription of the Correlated Genes of Liver Cancer in Rats

The regulating effects of TCM treatments including clearing away heat and toxic materials,promoting blood circulation and removing blood stasis,and strengthening the spleen and regulating qi on the oncogene transcription were observed in the liver cancer model rats.The preliminary results indicated that the mRNA levels of H-ras N-ras and K-ras,and signal molecules correlated with the ras/MAPK signal transduction pathway were down-regulated by the different TCM treatments in varying degrees.Also,the regulating effects of the treatments on differently-displayed genes were discrepant.It is suggested that the molecular mechanisms of the TCM treatments for liver cancer was complex with different target genes.

EFFECT OF DRUG-RESISTANCE REVERSORS ON EXPRESSIONS OF ONCOGENES OR TUMOR SUPPRESSOR ONCOGENES OF HUMAN TUMOR CELL LINES

MIT method was applied to assay the cytotoxicityof three reversors, verapamil (VER), dipyridamole (DPM)and cyclosporin (CSA) in K562, K562/ADM and KB celllines. S-P immunocytochemical technique was applied todetect cxpressions of oncoproteins or tumor suppressoroncoproteins in these tumor cell lines before or aftertreatment with these reversors. Results showed that threereversors were capable of inhibiting to a certain extentgrowth of K562 or KB cell lines and reversing greatlyadriamycin (ADM)-resistance in K562/ADM cell line.DPM and CsA were observed to inhibit, partly or wholly,expressions of p53, p16, bcl-2, p21 or cerbB-2oncoproteins. VER showed whole inhibition ofexpressions of P53, p16, p21 and bcl-2 and partlyexpression of p53 oncoprotein in K562 cell line. Theseresults suggest that growth inhibition in K562 or KB celllines by the reversors may be associated with partial orwhole inhibition or expressions of p53, p16, p21 or c-erbB-2 oncoproteins. Inhibitions of expressions p53, p16,p21 oncoproteins by VER but not DPM or CsA, may berespossible for reversing activity of VER for ADM-resistance in K562/ADM cell line.

Heat shock protein 72 normothermic ischemia,and the impact of congested portal blood reperfusion on rat liver

INTRODUCTIONFrom the technical aspect of liver surgery ,control of bleeding during hepatic parenchymal resection is one of the most important procedures in hepatectomy .Pringle,s maneuver ,a temporary cross-clamping of the hepatoduodnal ligament ,has often been used for this purpose[1],This is the simplest and userul technique to reduce intraoperative blood loss .

High-intensity focused ultrasound extracorporeal ablation of liver tissuesin rabbits

ＨｉｇｈｉｎｔｅｎｓｉｔｙｆｏｃｕｓｅｄｕｌｔｒａｓｏｕｎｄｅｘｔｒａｃｏｒｐｏｒｅａｌａｂｌａｔｉｏｎｏｆｌｉｖｅｒｔｉｓｓｕｅｓｉｎｒａｂｂｉｔｓＣＨＥＮＧＳｈｕＱｕｎ１，ＺＨＯＵＸｉｎＤａ１，ＴＡＮＧＺｈａｏＹｏｕ１，ＹＵＹａｏ１，Ｂ...

东北菱提取物对肝癌细胞的体内外抑制作用

目的 :探索东北菱提取物对肝癌细胞体内外抑制作用。方法 :采用 3H- Td R掺入法分别测定东北菱醇提取物和水提取物对肝癌细胞的体外敏感性 ;对荷瘤小鼠进行体内实验 ,观察该提取物对肝癌细胞生长的抑制率。结果 :体外实验当剂量达 2 2 5 .0 0 g· L- 1 时 ,抑制率为 75 .4 9% ;体内实验抑瘤率为 6 0 %以上。结论 :东北菱不同溶剂提取物均具有抑制肝癌细胞的作用。

体外化疗药物敏感实验对指导原发性肝癌个体化疗的临床意义

背景与目的:肝细胞癌(肝癌)化学治疗效果差。为了提高化疗效果,本研究采用体外化疗敏感实验——三磷酸腺苷肿瘤化疗药物敏感实验(adenosinetriphosphatetumorchemosensitivityassay,ATP鄄TCA)系统评估化疗药物,并利用该系统指导肝癌患者临床个体化疗。方法:获取50个原发性肝癌手术标本,采用ATP鄄TCA系统评估5鄄氟尿嘧啶(5鄄fluorouracil,5鄄FU)、丝裂霉素(mitomycin,MMC)、顺铂(cisplatin,DDP)、草酸铂(oxaliplatin,OXA)、表阿霉素(epirubicin,EPI)、健择(gemcitabine,GEM)、伊立替康(irinotecan,CPT鄄11)、足叶乙甙(etoposide,VP鄄16)和泰素(paclitaxel,PTX)等化疗药物;23例肝癌患者术后接受ATP鄄TCA系统指导临床化疗,同时以20例接受手术及常规治疗的肝癌患者作为对照,观察162周临床疗效。结果:ATP鄄TCA系统结果可评估率为90.8%。肝癌细胞对各种化疗药物中鄄高度敏感率分别为:泰素46%、伊立替康44%、健择36%、丝裂霉素14%、表阿霉素12%、顺铂8%、足叶乙甙6%、草酸铂6%以及5鄄氟尿嘧啶4%;临床结果:临床研究观察终点ATP鄄TCA组与对照组比较,PR、CR、SD及观察期内患者死亡率两组之间无显著性差异;然而对照组有较高病情进展发生率(60.00%vs.13.04%,P=0.003);ATP鄄TCA组较对照组在总病情缓解率(60.86%vs.30.00%,P=0.043)、平均手术后总生存期(78.91周vs.27.21周,P=0.006)及手术后无疾病进展生存期(30.52周vs.4.78周,P=0.005)方面表现出明显优势。结论:ATP鄄TCA系统可以成功用于评估肝癌标本。泰素、伊立替康和健择有较高的体外抗肝癌活性。ATP鄄TCA系统指导肝癌个体化疗有可能提高患者无疾病进展生存期和总生存期。

益肝煎剂对实验性肝纤维化大鼠Ⅰ,Ⅲ型胶原蛋白表达的影响

目的探讨益肝煎剂对实验性肝纤维化大鼠肝脏Ⅰ、Ⅲ型胶原蛋白表达的影响。方法采用400 mL·L^(-1)四氯化碳(CCl_4)sc制备大鼠实验性肝纤维化模型,将80只(雌雄各半)Wistar大鼠随机分成正常对照组(A组)、模型对照组(B组)、秋水仙碱组(C组)和益肝煎剂组(D组)各20只,后两组于造模的同时开始给药,观察10wk。采用苦味酸-天狼星红(Picric acid-Sirius red)染色显示Ⅰ,Ⅲ型胶原,偏振光显微镜下区分Ⅰ,Ⅲ型胶原。用半定量评分方法判断细胞变性程度和纤维化程度。结果益肝煎剂组大鼠肝组织的脂肪变性程度较模型组明显减轻,脂肪变性积分分别为2.00±1.36和3.17±0.75(P<0.01);Ⅰ,Ⅲ型胶原蛋白含量明显少于模型组,纤维化程度积分分别为1.32±0.57和2.33±0.82(P<0.01)。结论益肝煎剂对大鼠实验性肝纤维化的形成有明显抑制作用。

经导管肝动脉化疗栓塞联合经皮无水乙醇注射治疗肝癌的长期疗效观察

背景与目的肝癌的介入治疗中,经导管肝动脉化疗栓塞(transcatheterarterialchemoembolization,TACE)与经皮无水乙醇注射(percutaneousethanolinjection,PEI)是开展最广泛、效果最显著的两项治疗措施。TACE联合PEI可明显提高肝癌的近效疗效,但远期随访结果报道较少。本研究拟探讨TACE联合PEI治疗肝癌的长期效果及价值。方法675例肿瘤直径为2～15cm(平均9.6cm)、不能切除的原发性肝细胞癌(hepatocellularcarcinoma,HCC)接受介入治疗,其中179例行TACE联合PEI治疗(联合组),496例行单纯TACE治疗(TACE组)。两组中各有10例介入治疗后行Ⅱ期手术切除,标本送病理研究。其他病例随访5～7年以上(平均6.6年),分别统计1、3、5、7年累计生存率。联合组与TACE组两组无论是手术切除病例,还是随访病例,介入治疗前的一般资料均具有可比性。结果病理研究显示,虽然治疗前后肿块缩小程度两组无显著性差异,但联合组肿瘤平均坏死程度[(100.0±0.0)%]及完全坏死率(100%)均显著高于TACE组[分别为(91.5±7.1)%和20%,P<0.05或0.01]。随访结果显示,联合组1、3、5、7年生存率分别为80.5%、58.6%、29.6%和16.5%,TACE组分别为68.5%、27.8%、7.2%和5.2%,统计学处理均有显著性差异(P<0.01)。

丹参酮ⅡA及其纳米粒诱导肝癌细胞凋亡及对p38MAPK、TGFβ1信号蛋白表达的影响

目的:探讨丹参酮ⅡA(Tanshinone ⅡA,TSⅡA)及其纳米粒(Tanshinone ⅡA nanoparticles,TS-NP)治疗小鼠肝癌的作用及机制。方法:采用乳化溶剂挥发法制备TS-NP,建立小鼠肝癌模型,采用TUNEL标记法检测细胞凋亡率,免疫组织化学SP法检测p38促分裂原活化蛋白激酶(p38 mitogen-activated protein kinase,p38 MAPK)、肿瘤生长因子(tumor growth factorβ1,TGFβ1)的表达。结果:与对照组比较,TSⅡA组、TS-NP各剂量组瘤体质量显著降低(P<0.01),生存期均明显延长,肝癌细胞凋亡率升高(P<0.01)。其中与对照组比较,TS-NP组治疗作用优于等剂量的TSⅡA组,p38 MAPK表达明显高于其他各组(P<0.01),但TGFβ1的表达低于其他各组(P<0.01);肝癌组织中p38 MAPK与TGFβ1表达呈负相关(r=-0.873,P<0.001)。结论:TSⅡA及其纳米微粒能够抑制小鼠肝癌生长,延长生存期,而TS-NP的疗效优于等剂量的TSⅡA。其治疗肝癌的机制与抑制TGFβ1、上调p38 MAPK的表达从而抑制肝癌细胞增殖、诱导细胞凋亡有关质类。

索拉非尼联合顺铂抑制肝癌HepG2细胞生长的体外研究

目的探讨索拉非尼联合顺铂(DDP)对肝癌细胞HepG2生长的抑制作用及其可能的分子机制。方法实验细胞分为4组:空白对照组、索拉非尼单药组、顺铂单药组、索拉非尼联合顺铂组。索拉非尼和顺铂单独或联合作用于细胞,以MTT法检测24、48、72、96h时间点药物对HepG2细胞的增殖抑制率,流式细胞仪检测24、48h时间点的细胞周期与凋亡率。在药物作用后24h,用荧光染料罗丹明123(Rh123)染色细胞,流式细胞仪测定线粒体跨膜电位(ΔΨm),分光光度法检测caspase-3活性。结果索拉非尼及顺铂单独应用对HepG2生长均有抑制作用,且低剂量联合具有协同作用。联合用药可以使细胞周期阻滞于G0/G1期和G2期,且凋亡率明显高于单药组(P<0.05)。单独应用顺铂和索拉非尼均能使线粒体跨膜电位降低,而联合组作用强于单药组(P<0.05)。药物作用后caspase-3活性增高,联合组高于单药组(P<0.05)。结论索拉非尼联合顺铂能更好地抑制肝癌HepG2细胞增殖,并促进其凋亡,其机制可能与细胞周期阻滞、线粒体跨膜电位降低及caspase-3活性增加有关。

螺内酯对肝纤维化大鼠Ⅰ/Ⅲ型胶原蛋白表达的影响

目的探讨螺内酯对实验性大鼠肝纤维化Ⅰ/Ⅲ型胶原蛋白表达的影响,初步揭示螺内酯对大鼠肝纤维化的预防作用及可能的机制.方法雄性 SD 大鼠81只,随机分为正常对照组(10只)、肝纤维化模型对照组(45只)及螺内酯组(26只).采用复合因素造模,螺内酯从造模开始每日1mL 100mg·kg^(-1)灌胃,共7wk.免疫组化染色及图像分析检测Ⅰ/Ⅲ型胶原含量.结果螺内酯组与肝纤维化组胶原面积比Ⅰ型胶原分别为:2.84±0.86,5.41±2.08,Ⅲ型胶原分别为:2.95±0.82,5.35±2.30.螺内酯组Ⅰ/Ⅲ型胶原增生程度明显降低(P<0.01).结论螺内酯可使肝组织Ⅰ/Ⅲ型胶原沉积明显减轻,提示螺内酯可明显预防肝纤维化的形成,ALD 在肝纤维化的发病中有一定意义.

去甲斑蝥素-泊洛沙姆407缓释剂和无水乙醇的肝癌瘤内注射疗效比较

目的 :观察去甲斑蝥素 -泊洛沙姆 40 7(NCTD- P40 7)缓释剂瘤内注射治疗中晚期肝癌的疗效。方法 :将 5 6例癌灶最大直径为 6～ 12 cm的中晚期肝癌患者随机分为 2组 ,治疗组 (2 9例 )在超声引导下经皮肝穿刺瘤内注射 NCTD- P40 7缓释剂和对照组 (2 7例 )瘤内注射无水乙醇 ,进行临床疗效观察比较研究。结果 :在生活质量、实体瘤变化及实验室指标变化方面 ,两组疗效比较无显著性差异 (P>0 .0 5 ) ;在生存期方面 ,12个月生存率治疗组为 31.0 % ,对照组为 2 2 .2 % ,有显著性差异 (P<0 .0 5 )。在毒副反应方面 ,两组均未出现明显的毒副作用。 结论 :NCTD- P40 7缓释剂局部瘤内注射治疗可高浓度长时间作用于瘤体 ,对较大的中晚期肝癌具有一定疗效 ,且综合疗效优于无水乙醇瘤内注射。

体外模拟高强度聚焦超声适形扫描离体牛肝设定靶区的实验研究

目的 体外模拟高强度聚焦超声 (high- intensity focused ultrasound,HIFU )点组合扫描破坏三维立体靶区的过程 ,为 HIFU治疗肝肿瘤的临床方案提供实验依据。方法 在 B超实时监控下 ,采用从点到线 ,从线到面 ,由面到体的 HIFU立体组合扫描方式破坏离体牛肝组织内的设定靶区 ,测定凝固性坏死灶的大小、形状和体积。结果 HIFU立体组合扫描方式能使牛肝组织内预先设定的任意大小、形状的靶区出现凝固性坏死 ,受损区与正常组织边界清楚。结论 HIFU能沿设定靶区边界实时完全破坏三维立体的肝内靶区组织。

黄蘑多糖提取物的抗肝癌作用及其机制

目的:研究黄蘑多糖提取物的抗肝癌作用及其机制。方法:建立小鼠体内移植性肝癌模型,黄蘑多糖水溶性提取物(FI)腹腔连续给药,测定抑瘤率(IR);MTT法检测H22荷瘤小鼠淋巴细胞转化功能、NK细胞活性及IL-2、TNF-α的含量。结果:FI 20、40和80 mg.kg-1剂量组对肝癌H22的平均抑瘤率分别为36.1%、47.7%和57.6%,表现出较强的抗肿瘤活性;能增加体外免疫器官重量,促进T淋巴细胞转化,提高NK细胞及IL-2、TNF-α的活性。结论:FI为生物反应调节剂,通过增强机体免疫功能的作用达到抗肿瘤的功效。

贝伐珠单抗联合以5-FU为基础的双药化疗用于结直肠癌仅肝转移患者新辅助治疗:一项多中心单臂研究

目的通过开放标签的多中心探索性研究评估贝伐珠单抗联合氟尿嘧啶(5-FU)作为新辅助化疗方案对仅肝转移、转移灶初始不可切除且未经治疗的结直肠癌(colorectal cancer,CRC)患者R0切除率的影响。方法在全国7家中心招募既往未经治疗(原发灶已切除)、只存在肝转移灶且不可切除的中国转移性结直肠癌(metastatic colorectal cancer,m CRC)患者。入组患者均接受贝伐珠单抗(静脉注射,5 mg/kg,每2周1次,d1)联合以氟尿嘧啶(5-FU)为基础的双药化疗方案进行新辅助治疗。患者术前和术后共接受≤12个周期的治疗,术前最后1个周期的化疗(无贝伐珠单抗)不计入12个周期内。主要终点为R0切除率,次要终点为R1切除率、客观缓解率(objective response rate,ORR)、无进展生存(progression free survival,PFS)、无瘤生存率(disease free survival,DFS)和安全性。结果本研究共纳入50例患者,其中男性39例,女性11例;患者中位年龄57岁(范围37~73岁),R0切除率为30.0%,R1切除率为0.0%。50例患者的ORR为15.0%,中位PFS为12.06个月(95%CI:6.70~13.31),接受R0切除的15例患者中位DFS为8.57个月(95%CI:1.84~17.74)。总体安全性良好,32例患者(64.0%)共发生159次不良事件(adverse events,AE),其中24次为3级AE,无≥4级AE。最常见的与贝伐珠单抗相关的≥3级AE为高血压(8.0%)。手术安全人群(n=17)中,5例(29.4%)发生手术相关并发症,但均为肝脏局部并发症,仅1例发生肺部感染。结论对于肝脏为唯一转移灶且初始不可切除的CRC患者,使用贝伐珠单抗联合以5-FU为基础的双药化疗进行新辅助治疗可提高R0切除率,且耐受性良好。