The challenge of molecular selection in liver-limited metastatic colorectal cancer for surgical resection: a systematic review and meta-analysis in the context of current and future approaches

Objectives:Treatment of metastatic colorectal cancer(mCRC)includes resection of liver metastases(LM),however,no validated biomarker identifies patients most likely to benefit from this procedure.This meta-analysis aimed to assess the impact of the most relevant molecular alterations in cancer-related genes of CRC(i.e.,RAS,BRAF,SMAD4,PIK3CA)as prognostic markers of survival and disease recurrence in patients with mCRC surgically treated by LM resection.Methods:A systematic literature review was performed to identify studies reporting data regarding survival and/or recurrence in patients that underwent complete liver resection for CRC LM,stratified according to RAS,BRAF,PIK3CA,and SMAD4 mutational status.Hazard ratios(HRs)from multivariate analyses were pooled in the meta-analysis and various adjustment strategies for confounding factors were combined.The search was conducted in numerous databases,including MEDLINE(PubMed),Embase,Cumulative Index to Nursing and Allied Health Literature(CINAHL)(EBSCO host),and WHO Global Index Medicus,through March 18th,2022.Meta-analyses,editorials,letters to the editor,case reports,studies on other primary cancers,studies with primary metastatic sites other than the liver,studies lacking specific oncological outcome variables or genetic data,non-English language studies,and studies omitting residual disease data from liver metastasectomy were excluded.The remaining 47 studies were summarized in a descriptive table which outlines the key characteristics of each study and final results were graphically presented.Results:RAS mutation status was negatively associated with overall survival(OS)(HR,1.68;95%CI,1.54–1.84)and recurrence free survival(RFS)(HR,1.46;95%CI,1.33–1.61).A negative association was also found for BRAF regarding OS(HR,2.64;95%CI,2.15–3.24)and RFS(HR,1.89;95%CI,1.32–2.73)and SMAD4 regarding OS(HR,1.93;95%CI,1.56–2.38)and RFS(HR,1.95;95%CI,1.31–2.91).For PIK3CA only three studies were eligible and no significant association with either OS or RFS could be highlighted.Conclusion:RAS,BRAF,and SMAD4 are negatively associated with OS and RFS in patients undergoing curative liver metastasectomy from colorectal cancer.No conclusion can be drawn for PIK3CA due to the limited literature availability.These data support the integration of RAS,BRAF,and SMAD4 mutational status in the surgical decision-making for colorectal liver metastasis.Nevertheless,we have to consider several limitations,the major ones being the pooling of results from studies that evaluated patient outcomes as either disease-free survival(DFS)or RFS;the inclusion of patients with minimal residual disease and unconsidered potential confounding factors,such as variability in resectability definitions,chemotherapy use,and a potential interaction between biological markers and pre-and post-resection pharmacological treatments.

Yu Gan Long Ameliorates Hepatic Fibrosis by Inhibiting PI3K/AKT,Ras/ERK and JAK1/STAT3 Signaling Pathways in CCl4-induced Liver Fibrosis Rats

Yu Gan Long(YGL)is a Chinese traditional herbal formula which has been reported to attenuate liver fibrosis for many years and we have explored its anti-fibrotic mechanism through blocking transforming growth factor(TGF-β)in the previous study.But the mechanisms associated with platelet-derived growth factor(PDGF)-BB remain obscure.In this study,we further investigated the mechanism of YGL reducing carbon tetrachloride(CCl4)-induced liver fibrosis in rats.Our results showed that YGL suppressed CCl4-induced upregulation of collagen IV(Col IV),type HI precollagen(PCHI),hyaluronuc acid(HA)and laminin(LN),which are implicated in liver fibrosis.Also,YGL reduced theα-smooth muscle actin(α-SMA)expression,which acts as the indicator of liver fibrosis.Furthermore,YGL decreased the serum levels of hepatic stellate cell(HSC)mitogen PDGF-BB and inflammation cytokines,including TNF-α,IL-1β,IL-6.Markers involved in liver fibrosis,such as Ras,p-Raf-1,p-ERK1/2,p-JNK,p-P38,p-PI3K,p-AKT,p-JAKl,p-STAT3 were downregulated significantly after treatment with YGL.Our results indicated that YGL ameliorated CCl4-induced liver fibrosis by reducing inflammation cytokines production,and suppressing Ras/ERK,PI3K/AKT,and JAK1/STAT3 signaling pathways,which provided further evidence towards elucidation of the anti-fibrotic mechanism of YGL.

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.

A randomized trial of iron depletion in patients with nonalcoholic fatty liver disease and hyperferritinemia

AIM: To compare iron depletion to lifestyle changes alone in patients with severe nonalcoholic fatty liver disease (NAFLD) and hyperferritinemia, a frequent feature associated with more severe liver damage, despite at least 6 mo of lifestyle changes.

Role of mitogen activated protein kinase cascade pathway and anti-stress response in liver transplantation

OBJECTIVE: To explore the changes of mitogen activated protein kinase (MAPK) cascade pathway and anti-stress response of hepatocytes after liver transplantation. METHODS: Ten normal liver specimens and 18 punctured donor liver specimens were divided into 3 groups: A (control: 10), B (no rejection: 10) and C (acute rejection:8). MAPK, Ras, Jun and heat shock protein 70 (HSP70) were tested immunohistochemically while Ras and HSP70 were tested by in situ hybridization. All sections were subjected to image analysis. RESULTS: Protein expressions of MAPK, Ras and Jun were increased by an ascending order of groups A, B and C. The protein expression of HSP70 was the highest in group B but lower in group C. Expressions of Ras and HSP7O mRNA were consistent with those of protein. CONCLUSIONS: The changes of the MAPK cascade pathway and anti-stress response of hepatocytes after liver transplantation are one of regulation mechanisms for protecting the hepatocytes from damage after liver transplantation. This mechanism is active to support individual survival.

枳葛口服液通过Syk/Ras/ERK信号通路防治酒精性肝损伤机制研究

目的:基于Syk/Ras/ERK信号通路观察枳葛口服液含药血清对酒精性肝损伤大鼠BRL3A肝细胞炎症反应的影响,探讨枳葛口服液防治酒精性肝损伤的相关机制。方法:将正常大鼠BRL3A肝细胞接种于6孔板,贴壁后分为正常对照组、模型组(2.5%乙醇处理)、阳性对照组(美他多辛含药血清加2.5%乙醇)和不同浓度枳葛口服液含药血清(2.5%、5%、10%枳葛口服液含药血清加2.5%乙醇)干预组,24h后酶标法检测各组细胞上清液中GGT(γ-谷氨酰转肽酶)、LDH(乳酸脱氢酶)含量;RT-PCR法测定各组细胞内Syk、Ras、MEK1/2、ERK1/2、c-Fos mRNA表达情况。结果:与正常对照组比较,模型组细胞上清液中GGT、LDH含量显著升高(P<0.01);Syk、Ras、MEK1/2、ERK1/2、c-Fos mRNA表达显著升高(P<0.01)。与模型组比较,各干预组以上指标均呈现不同程度的好转,其中10%枳葛口服液含药血清及阳性对照组作用最显著(P<0.01),二者之间未见明显差异(P>0.05)。结论:一定浓度的枳葛口服液含药血清对大鼠肝细胞酒精性肝损伤具有防治作用,其机制可能与抑制Syk/Ras/ERK信号通路活化,从而减轻肝脏炎症相关。

肝癌患者血浆RASSF1A异常甲基化检测的意义

目的采用甲基化特异性PCR法(MSP)检测41例原发性肝癌(HCC)患者血浆中游离Ras相关结构域家族蛋白1A(RASSF1A)异常高甲基化情况,探讨血浆RASSF1A检测在肝癌诊断中的意义.方法收集患者血浆,提取游离DNA,亚硫酸氢钠修饰并纯化,以甲基化特异性引物及非甲基化引物进行PCR.结果41例患者血浆中有17例RASSF1A呈现异常高甲基化(41.5%),对照血浆均为阴性.患者一般情况、临床病理资料等与血浆中RASSF1A异常高甲基化检测结果无关(P>0.05);在10例AFP阴性的HCC患者中,有7例结果为阳性.结论血浆RASSF1A甲基化检测对肝癌的早期诊断及筛选有重要意义,并有助于判断预后.

IGF-Ⅱ和HBxAg及ras基因在树鼠句实验性肝癌组织中的表达

用免疫组化方法观察胰岛素样生长因子Ⅱ（ＩＧＦ－Ⅱ）、ＨＢｘＡｇ及ｒａｓ基因的表达蛋白ｐ２１在乙肝病毒（ＨＢＶ）和黄曲霉素Ｂ１（ＡＦＢ１）致树鼠句肝癌过程中的表达。发现这三种基因蛋白的表达与肝癌发生呈正相关系。即接受ＨＢＶ和ＡＦＢ１双因素的树鼠句的肝癌发生率与ＩＧＦ－Ⅱ、ＨＢｘＡｇ及ｐ２１的表达阳性率均显著高于只暴露于单一因素ＨＢＶ或ＡＦＢ１的动物。同时，在带瘤树鼠句中，这三种基因的表达又显著高于无瘤者。提示：ＨＢＶ与ＡＦＢ１能协同激发这些基因的异常表达；

新制抗癌方对AFB_1染毒的HBV转基因小鼠肝癌前病变组织PCNA、P21^(ras)和NF-KBP65表达的影响

Objectives:This study is to investigate the effects of new anti-tumor formular(NAF)on expression of PCNA,P21 ras and NF-KB P65 in liver precancerous lesions of HBV large envelope transgenic mice injected by aflatoxin B1(AFB1).Methods:The precancerous HBV large envelope transgenic mouse injected by AFB1 liver model was used.Mice was given water,NAF concentrated water solution throughout the whole experiment(48 weeks).PCNA,P21 ras and NF-KB P65 protein expression were detected by immunohistochemical method.Results: PCNA,P21 ras and NF-KB P65 expressions were significantly inhibited by NAF treatment.Conclusion NAF inhibited PCNA,P21 ras and NF-KB P65 protein expressions,therefore,NAF could show obvious effects on protecting against synergistic hepatoearcinogenesis of HBV and AFB1.

TC 21/R-Ras 2在肝癌中的表达、亚细胞定位及意义

目的:探讨TC21基因在肝癌细胞、肝癌及癌旁组织中的表达、亚细胞定位及意义。方法:用RT-PCR检测TC 21在肝癌细胞系及人肝癌及癌旁组织中mRNA水平的表达,用免疫组化及Western印迹检测TC21蛋白在肝癌相关组织中的表达差异,用组织芯片技术结合免疫组化检测TC21蛋白的亚细胞定位。结果:RT-PCR检测结果表明TC21 mRNA在SMMC-7721、BEL-7402、Huh-7、Hep3B、HepG2、MHCC-97L、MHCC-LM3 7个肝癌细胞系及L-02和Chang liver 2株永生化人肝细胞系、7对肝癌及对应癌旁肝组织中均有较高表达;Western印迹结果表明上述细胞系中TC21蛋白表达与mRNA表达一致,TC21在4对肝癌及癌旁组织中均呈较高水平的表达;免疫组化检测结果表明TC21在人原发性肝癌、癌旁组织、硬化肝组织与正常肝组织中的表达阳性率分别为84.2%、77.2%、41.7%、0%,肝癌与肝硬化、正常肝相比显著高表达(P<0.05,P<0.01),与癌旁组织比无统计学意义(P>0.05);统计学分析结果表明TC21蛋白表达与肿瘤大小呈正相关(P<0.05),与是否肝硬化呈负相关(P<0.05);肝癌组织中TC21主要定位于肝癌细胞核,部分定位于胞质,膜定位不明显,TC21蛋白在肝癌细胞中的核定位显著高于癌旁肝细胞(P<0.001)。结论:本研究首次揭示TC21蛋白在肝癌组织中的高表达及核定位预示其在肝细胞恶性转化及肝癌发生发展中发挥重要作用。

树舌多糖GF对HepA瘤细胞N-ras基因表达的影响

目的探明树舌多糖GF对HepA瘤组织N-ras基因表达的影响。方法运用原位杂交法、SP免疫组化染色技术及多媒体彩色病理图文分析系统测定HepA瘤细包中N-rasmRNA量及N-Ras蛋白的表达量。结果树舌多糖组、猪苓多糖组中N-rasmRNA量及Ras蛋白的表达量均显著低于荷瘤组(P<0.01),树舌多糖组与猪苓多糖组无显著性差异。结论初步认为树舌多糖GF可通过降低N-rasmRNA量及Ras蛋白的表达,而抑制HepA瘤细胞的增殖。

原发性肝癌中N-ras、c-myc癌基因的表达研究

以点杂交和原位杂交法检测了34例启东地区原发性肝癌手术切除标本N－ras、c－myc基因的表达水平和定位。点杂交结果显示：N－ras、c-myc的检出率分别为647％（22／34）和23．5％（8／34）。前期的实验表明此34例标本HBV－DNA的检出率为588％（20／34），Southernblot实验结果未见病毒DNA的整合。N－ras、c-myc阳性标本中HBV－DNA的检出率分别为54．5％（12／22）和75％（6／8），两者之间无差异，P＞0．05。原位杂交结果显示：肝癌癌组织中N－ras、c－myc基因的表达水平并没有明显增高，相反，肿瘤周围肝组织中的表达水平增高并主要位于慢性肝炎、肝硬变中的再生肝细胞中，阳性细胞呈灶性及成片分布，不伴有毛玻璃样改变（HE染色）。结论：虽然N－ras、c－myc与肝癌的发生密切相关，肝癌患者中常见其表达水平增高，但这很可能只是一种肝细胞损伤后再生时的细胞增殖性调控的表现，此种N－ras、c-myc的高表达是否直接导致肝癌发生，癌基因是否为突变型，有待进一步研究、此外，本实验中c－myc基因相对于N－ras基因的低检出率可能与c－mycMRNA极短的半衰期有关。

蛋白激酶Cα对人正常肝和肝癌细胞中Ha-ras基因表达的影响

运用基因转染技术 ,将蛋白激酶C(PKCα)cDNA正向插入的真核表达重组质粒pXJ4 1 PKCα ,导入人正常肝细胞 (L 0 2 ) ,经蛋白质免疫印迹等检验 ,表明成功构建了稳定过表达PKCα的人正常肝细胞模型 (LT3) ,用LT3和表达反义PKCα的人肝癌细胞HT6为细胞模型 ,通过RT PCR ,蛋白质印迹 (Westernblot)等分析和进一步运用自行构建的真核表达质粒prasGL3,进行荧光素酶活性检测表明 :过表达PKCα可以促进L 0 2细胞的增殖速率 ,并引起Ha ras基因转录水平上升和Ha ras启动子活性升高 ;反之 ,表达反义PKCα的BEL 74 0 2细胞增殖被抑制 ,Ha ras基因转录水平下降 ,Ha ras启动子活性降低 .通过实验我们首次观察到 ,PKCα亚类对Ha ras癌基因表达的影响与其对Ha ras启动子活性的作用有关 ,PKCα可能参与了对Ha

结直肠癌原发灶、门静脉血和肝转移灶K-ras基因突变的研究

目的:观察结直肠癌患者门静脉血液、原发肿瘤组织及相应肝转移灶K-ras基因突变情况,分析三者的一致性,探讨结直肠癌患者门静脉血K-ras基因突变与肝转移关系。方法:实时荧光定量PCR技术和基因测序技术检测59例结直肠癌患者门静脉血液、原发肿瘤组织及15例肝转移灶K-ras基因突变,结合其临床资料分析。结果:59例结直肠癌组织中20例(33.9%)发现K-ras基因突变,18例(30.5%)结直肠癌患者的门静脉血中也发现K-ras基因突变,15例肝转移灶中8例(53.3%)发现K-ras基因突变,与原发癌组织的基因突变率差异不明显(P>0.05)。18例门静脉血存在K-ras基因突变者,其相应的肿瘤组织中均发现K-ras突变。结直肠癌组织中无K-ras基因突变者,患者门静脉血未发现基因突变。8例肝转移灶发现K-ras基因突变者门静脉血亦均有K-ras基因突变,7例肝转移灶无K-ras突变者门静脉血也无K-ras突变。原发肿瘤组织、相应门静脉血和5例同时性、2例异时性肝转移灶的K-ras基因突变类型基本一致(即K-ras基因12密码子GGT突变为GAT或GTT),1例异时性肝转移灶K-ras基因突变类型为13密码子GGC突变为GAC。原发癌组织与门静脉血K-ras基因突变一致率为96.6%(57/59),肝转移灶与门静脉血K-ras基因突变情况基本一致,但突变类型有不同。结论:结直肠癌的原发灶、门静脉血及肝转移灶的K-ras基因突变较为一致,原发癌组织和门静脉血均有K-ras基因的突变,预示着肿瘤可能通过血行转移至肝脏。

寡脱氧核苷酸抑制N-ras癌基因表达及肝癌细胞增殖的实验研究

目的 了解三螺旋形成寡核苷酸（ＴＦＯ）、反义寡核苷酸（ＯＤＮａｓ）抑制肝癌细胞生长的作用。方法 以Ｎ－ｒａｓ第二转录起始位点及翻译起始区１－６密码为靶点，合成１２聚硫代磷酸ＴＦＯ（ＴＦＯ１２）、１９聚硫代磷酸ＯＤＮａｓ（ＯＤＮａｓ１９）、同时合成１９聚无关序列硫代磷酸寡核苷酸对照（ＯＤＮｃｏｎ）。在人肝癌Ｂｅｌ７４０２细胞观察了充代磷酸寡核苷酸对Ｎ－ｒａｓ表达ｐ２１蛋白的抑制及对细胞增殖的影响。

肝刺激因子对人肝癌细胞BEL -7402p21^(ras)表达的影响

从雄性初断乳SD大鼠肝匀浆中提取肝刺激因子 (HSS)并加以部分纯化 ,观察其促人肝癌细胞增殖活性及对p2 1ras蛋白表达的影响。结果表明 :(1)HSS具有明显的促人肝癌细胞增殖活性 ,其分子量为 14～ 2 0kD ;(2 )HSS可提高p2 1ras蛋白表达 ,具有时间 效应关系 ,并与EGF呈协同作用 ;(3)HSS调节p2 1ras蛋白表达具有剂量 效应关系 ,且呈现出饱和性。鉴于我们已报道HSS上调EGF受体蛋白和基因表达这一事实 ,本实验结果进一步说明 ,HSS促人肝癌肝细胞增殖与其调节EGF受体介导的信号分子传导过程相关。

外周血E-selectin、P-selection及K-ras基因突变水平在胰腺癌中的表达及意义

目的探讨外周血内皮细胞选择素(E-selectin)、血小板选择素(P-selection)及K-ras基因突变水平在胰腺癌中的表达及意义。方法选择2019年2月—2020年2月收治的胰腺癌60例作为胰腺癌组,选择同期健康体检的健康人60例作为对照组。应用双抗夹心法酶联免疫吸附试验(ELISA)检测2组外周血E-selectin及P-selection水平,使用肽核酸钳制实时定量PCR法检测外周血中K-ras基因突变情况。分析2组外周血E-selectin、P-selection水平及其与胰腺癌临床病理特征的关系。检测外周血K-ras基因突变率及与临床病理特征的关系。结果胰腺癌组外周血E-selectin水平高于对照组,P-selection水平低于对照组(P<0.01)。外周血E-selectin、P-selection水平与肿瘤分期、淋巴结转移、肝转移有关(P<0.01),与肿瘤部位无关(P>0.05)。外周血K-ras基因突变率为48.3%。胰腺癌患者外周血K-ras基因突变与性别相关(P<0.01),而与患者年龄、分期、淋巴结及肝转移和肿瘤部位无关(P>0.05)。结论外周血E-selectin和P-selection异常表达与外周血K-ras基因检测同胰腺癌发生发展及预后密切相关,对胰腺癌早期筛查、诊断、指导临床治疗起到重要作用。

Alterations in metastatic properties of hepatocellular carcinoma cell following H-ras oncogene transfection

AIM: To demonstrate the relationship between H-ras oncogene and hepatocellular carcinoma (HCC) metastasis. METHODS: Activated H-ras oncogene was transfected into SMMC 7721, a cell line derived from human HCC, by calcium phosphate transfection method. Some metastasis-related parameters were detected in vitro, including adhesion assay, migration assay, expression of collagenase IV(c IV ase) and epidermal growth factor receptor (EGFR). RESULTS: The abilities of H-ras-transfected cell clones in adhesion to laminin (LN) or fibronectin (FN), migration, c IV ase secretion increased markedly, and the expression of EGFR elevated moderately. More importantly, these alterations were consistent positively with the expression of p21, the protein product of H-ras oncogene. CONCLUSION: H-ras oncogene could induce the metastatic phenotype of HCC cell in vitro to raise its metastatic potential.

Effects of endotoxin on expression of ras, p53 and bcl-2 oncoprotein in hepatocarcinogenesis induced by thioacetamide in rats

AIM To evaluate the relationship between expression of ras, p53, bcl 2 gene products, and hepatocarcinogenesis since endotoxemia produced from lipopolysaccharide admi nistration and/or the hypophagocytic state of splenectomy significantly accelerated hepatocarcinogenesis induced by thioacetamide. 〖WTH4〗METHODS〓〖WTXFZ〗The hepatocarcinoma model was induced by oral intake of 0 03% thioacetamide for six months. During the induction of hepatocarcinoma model, rats were additionally treated with splenectomy and/or lipopolysaccharide administration. The techniques of flow cytometry, immunohistochemistry and immunoelectronmicroscopy were applied to quantitative analysis of the expression of oncogene proteins. RESULTS In this model system, overexpression of ras p21 protein mainly occurred on precancerous cell population or in early stage of hepatocyte transformation. And the levels of ras p21 declined when nuclear DNA aneuploid increased. Expression of bcl 2 protein slowly and steadily rose with more hepatocytes staying in S+G2M phases as the hepatocarcinoma became more malignant. P53 was moderately expressed during the hepatocarcinogenesis. There was no statistical correlation between endotoxemia levels and the changes of ras, p53 and bcl 2 gene products. CONCLUSION Over expression of oncogene ras p21 was likely to be a precursor of the premalignant hepatocytes and it might be responsible for the initiation of hepatocarcinogenesis. Bcl 2 protein expression is proportional to the severity of the malignancies. P53 may be a key pathway on the transformation and development of hepatocarcinoma. This study confirmed the hypothesis that there are multiple genes and multiple steps involved in hepatocarcinogenesis. Expressions of oncogene proteins reflected the properties of the premalignant and malignant cells, but not directly related to endotoxemia statistically.[JP]