APC and K-ras gene mutation in aberrant crypt foci of human colon

AIM:To study the genetic alteration in ACF and to define the possibility that ACF may be a very early morphological lesion with molecular changes,and to explore the relationship between ACF and colorectal adenoma even carcinoma. METHODS: DNA from 35 CRC, 15 adenomas, 34 ACF and 10 normal mucus was isolated by means of microdissection. Direct gene sequencing of K-ras gene including codon 12, 13 and 61 as well as the mutation cluster region (MCR) of APC gene was performed. RESULTS: K-ras gene mutation frequency in ACF, adenoma and carcinoma was 17.6% (6/34), 13.3% (2/15), and 14.3% (5/35) respectively, showing no difference (P 】 0.05) in K-ras gene mutation among three pathologic procedures. The K-ras gene mutation in adenoma, carcinoma and 4 ACF restricted in codon 12 (GGT GAT), but the other 2 mutations from ACF located in codon 13 (GGC GAC). K-ras gene mutation was found more frequently in older patients and patients with polypoid cancer. No mutation in codon 61 was found in the three tissue types. Mutation rate of APC gene in adenoma and carcinoma was 22.9% (8/35) and 26.7% (4/15), which was higher than ACF (2.9%) (P 【0.05). APC gene mutation in carcinoma was not correlated with age of patients, location, size and differentiation of tumor. CONCLUSION: ACF might be a very early morphological lesion in the tumorogenesis of colorectal tumor. The morphological feature and gene mutation status was different in ACF and adenoma. ACF is possibly putative microadenoma that might be the precursor of adenoma. In addition, the development of a subgroup of colorectal carcinomas might undergo a way of normal epithelium ACF carcinomas .

Azoxymethane-induced rat aberrant crypt foci:Relevance in studying chemoprevention of colon cancer

The pathogenesis of colon cancer involves sequential and multistep progression of epithelial cells initiated to a cancerous state with defined precancerous intermediaries. Aberrant crypt foci （ACF） represent the earliest identifiable intermediate precancerous lesions during colon carcinogenesis in both laboratory animals and humans. ACF are easily induced by colon-specific carcinogens in rodents and can be used to learn more about the process of colon carcinogenesis. For over two decades, since its first discovery, azoxymethane （AOM）-induced rodent ACF have served as surrogate biomarkers in the screening of various anticarcinogens and carcinogens. Several dietary constituents and phytochemicals have been tested for their colon cancer chemopreventive efficacy using the ACF system. There has been substantial effort in defining and refining ACF in terms of understanding their molecular make-up, and extensive research in this field is currently in progress. In chemoprevention studies, AOM-induced rat ACF have been very successful as biomarkers, and have provided several standardized analyses of data. There have been several studies that have reported that ACF data do not correlate to actual colon tumor outcome, however, and hence there has been an ambiguity about their role as biomarkers. The scope of this mini-review is to provide valuable insights and limitations of AOM-induced rat ACF as biomarkers in colon cancer chemoprevention studies. The role of the dynamics and biological heterogeneity of ACF is critical in understanding them as biomarkers in chemoprevention studies.

Relationship of human rectal aberrant crypt foci and formation of colorectal polyp:One-year following up after polypectomy

AIM:To clarify the relationship of human rectal aberrant crypt foci and formation of colorectal polyp.METHODS:Eighty-nine subjects were recruited from the population of Japanese individuals who underwent polypectomy at Yokohama City University Hospital.All patients had baseline adenomas removed at year 0 colonoscopy.Aberrant crypt foci(ACF) were defined as lesions in which the crypts were more darkly stained with methylene blue than normal crypts and had larger diameters,often with oval or slit-like lumens and a thicker epithelial lining.RESULTS:A total of 366 ACFs were identified in 89 patients;all had baseline adenomas removed at the first examination(year 0) colonoscopy and returned for the second(year 1).ACF in the lower rectum were assessed at year 0 and study group were divided into two groups depend on ACF numbers,0-3 or over 3.All participants were examined in the number and maximum size of adenoma.There was no statistical difference in number and maximum size of ACF at year 0,however,maximum size of adenoma was larger in over 3 group than 0-3 group at year 1.CONCLUSION:The number of ACF may be a predictive factor of relatively large adenoma incidence in the pilot phase study.

异变腺窝病灶(ACF)

从ACF概念、与结肠癌的关系、相关的基因和指标、研究方法和研究意义等几个方面对近年来异变腺窝病灶(ACF)的研究进行了概述。可以看出:ACF是结肠癌的癌前病变,可以作为结肠癌早期诊断指标。异变腺窝病灶(ACF);

窄带内镜、染色内镜与常规内镜对远端大肠ACF发现率的对比研究

目的比较常规内镜与窄带内镜(NBI)、染色内镜对远端大肠异常隐窝灶(aberrant cryptfoci,ACF)的发现率。方法选择2011年8月至12月就诊于江西省萍乡市人民医院准备接受结肠镜检查的患者670例,用随机数字表法将患者分为3组:其中常规内镜组228例、NBI组220例、染色内镜组222例。比较三种方法对远端大肠ACF检出率及各组间所用操作时间。结果在三组中,共发现155例ACF病例数。常规内镜、NBI组及染色内镜组发现ACF病例数分别为5例(2.19%)、25例(11.36%),125例(56.31%),三组组间比较有显著性统计学差异(P<0.01)。但是与常规内镜相比,NBI组、染色内镜组操作时间有所延长。结论染色内镜能大幅提高远端大肠ACF发现率。NBI内镜较常规白光内镜能提高远端结肠ACF发现率,但比染色内镜低。常规白光内镜对远端结肠ACF发现率低。

Accumulation of aberrant DNA methylation during colorectal cancer development

Despite the recent advances in the therapeutic modalities,colorectal cancer(CRC)remains to be one of the most common causes of cancer-related death.CRC arises through accumulation of multiple genetic and epigenetic alterations that transform normal colonic epithelium into adenocarcinomas.Among crucial roles of epigenetic alterations,gene silencing by aberrant DNA methylation of promoter regions is one of the most important epigenetic mechanisms.Recent comprehensive methylation analyses on genome-wide scale revealed that sporadic CRC can be classified into distinct epigenotypes.Each epigenotype cooperates with specific genetic alterations,suggesting that they represent different molecular carcinogenic pathways.Precursor lesions of CRC,such as conventional and serrated adenomas,already show similar methylation accumulation to CRC,and can therefore be classified into those epigenotypes of CRC.In addition,specific DNA methylation already occurs in the normal colonic mucosa,which might be utilized for prediction of the personal CRC risk.DNA methylation is suggested to occur at an earlier stage than carcinoma formation,and may predict the molecular basis for future development of CRC.Here,we review DNA methylation and CRC classification,and discuss the possible clinical usefulness of DNA methylation as biomarkers for the diagnosis,prediction of the prognosis and the response to therapy of CRC.

饮茶对大鼠大肠变性隐窝病灶及大肠肿瘤的影响

以二甲基肼诱发Wistar大鼠大肠癌为模型,研究了绿茶和茶色素(红茶的主要成分)大肠癌的化学预防作用和对大肠肿瘤的影响。结果表明,在第16周2个饮茶组动物的变性隐窝病灶(ACF)形成数比阳性对照组显著减少(P< 0.01);在第32周时阳性对照组100% 发生了肿瘤(平均瘤数为2.6个/只,平均瘤体积为294.7m m 3/瘤)。绿茶组和茶色素组的平均瘤数抑制率分别为47.1% 和43.1% ,平均瘤体积抑制率分别为77.1% 和68.1% 。表明绿茶和茶色素对实验性大肠肿瘤具有预防作用。

Wistar鼠大肠癌模型中肿瘤与异常腺窝病灶关系的初步研究

目的通过阶段性观察Wistar鼠大肠癌模型中异常腺窝病灶(ACF)的发展情况,评价ACF与肿瘤的相关性。方法40只Wistar大白鼠给予二甲肼(DMH)皮下注射(20mg/kg,每周1次,连续18周),分为3组,于第8、16和24周分批处死,将美蓝染色后的大肠组织在实体镜下观察。结果ACF均分布于中段及远端大肠(大部分位距盲肠50%～80%处),共发现肿瘤10个,其中3个肿瘤为低分化黏液腺癌,均分布在近端结肠(距盲肠10%～20%)。另外7个肿瘤中有2个为腺瘤,5个为高分化腺癌,均分布在距盲肠50%～80%处。结论ACF与腺瘤癌变途径相关,而非低分化黏液腺癌的中间途径。

黄连、吴茱萸及其药对对大鼠结肠异变腺窝的影响

目的:研究黄连、吴茱萸及其药对对大鼠结肠癌前病变(异常腺窝病灶,aberrant crypt foci,ACF)的影响。方法:皮下注射二甲肼(1,2-di m-ethylhydrazine,DMH)诱发大鼠结肠ACF形成,根据形态法观察亚甲蓝染色后ACF在结肠上皮的数量和分布变化。同时通过测定肝重指标评估药物对肝的损伤情况。结果:与模型组相比,黄连、吴茱萸及其药对在大剂量和中剂量时,都能明显抑制ACF形成(P<0.01);在小剂量时,黄连组亦能抑制ACF形成(P<0.05);黄连大、中剂量组和吴茱萸大剂量组的肝重指数有所增加(P<0.01),而药对组的肝重指数小于黄连组及吴茱萸组,且3给药组间有统计学差异(P<0.01)。结论:黄连、吴茱萸及其药对在一定程度上能抑制ACF形成,且配伍后能减轻对肝的损伤。

酪蛋白糖巨肽对二甲肼干预的大鼠细胞因子网络变化的研究

目的:探讨不同剂量酪蛋白糖巨肽(casein glycomacropeptide,CGMP)干预二甲肼处理的大鼠时,外周血和结肠组织内细胞因子水平的变化情况,从而推断CGMP对二甲肼处理的大鼠细胞因子网络的影响。方法:60只Wistar雄性大鼠随机分为正常组、模型组、CGMP低剂量组、CGMP中剂量组和CGMP高剂量组。除正常组外,对每只大鼠每周腹腔注射二甲肼,剂量为30 mg/(kg?周),同时,3个剂量CGMP组注射二甲肼的同时每天灌胃CGMP,剂量分别为10、50、100 mg/(kg?d)。15周后,处死大鼠,取其结肠组织和血清,首先检测结肠末端异型隐窝灶个数,然后利用液相芯片法检测结肠组织和血清中的细胞因子的表达水平。结果:乳源CGMP对大鼠体质量影响没有显著性差异,乳源CGMP对大鼠内毒素和活性氧簇的水平具有显著的抑制作用,其抑制作用呈剂量依赖趋势。乳源CGMP可显著抑制异型隐窝灶的形成,且异型隐窝灶个数呈剂量依赖性降低。乳源CGMP可以显著抑制大鼠体内Th1/Th2类细胞因子的失衡,且呈剂量依赖趋势。结论:乳源CGMP具有改善二甲肼处理的大鼠结肠组织损伤的功能,其机制为乳源CGMP可以有效抑制二甲肼处理的大鼠体内异型隐窝灶的形成,并呈剂量依赖性,研究显示乳源CGMP可以下调大鼠体内IL-4等Th2类细胞因子的异常升高,促进IL-2等Th1类细胞因子的分泌,改善大鼠体内处于失衡状态的细胞因子网络。

放大色素结肠镜识别直肠异常隐窝病灶的可靠性及准确性

目的系统评估放大色素结肠镜(MCE)判断直肠异常隐窝病灶(ACF),尤其是伴异型增生ACF的可靠性及准确性。方法将内镜识别的ACF与活检病理学结果做对照研究,预测经病理学结果证实的内镜下伴异型增生ACF的可靠性。结果 MCE识别病理性伴异型增生ACF病变的正确百分率为88.1%,灵敏度为81.8%,特异度为89.0%。结论 MCE对判断结直肠ACF病变有较高的病理符合率,接近病理诊断,可避免过度活检,具有较高临床应用价值。

β-catenin和MMP-7在异常腺窝病灶中的表达差异的初步探讨

目的检测β-catenin及MMP-7在Wistar鼠大肠癌模型异常腺窝病灶中的表达差异,探讨其与大肠肿瘤的相关性及其发生途径。方法 20只Wistar鼠给予二甲肼经典造模处理,于24周处死,取其大肠组织进行病理和免疫组化检查。结果发现两种不同病理类型的ACF:hACF和dACF,两者β-catenin的表达异常率分别为4.84%和100%,在MMP-7的阳性表达率分别为7.87%和81.82%,而肿瘤的β-catenin的表达异常率和MMP-7的阳性表达率均为100%。dACF与肿瘤在两个癌基因表达率的差异均没有统计学意义。结论单纯增生型ACF与肿瘤发生无明显相关,非典型性增生型ACF与肿瘤发生关系密切,并且其发生可能遵循Wnt途径。

256例大肠异常隐窝灶的内镜与病理特征分析

目的了解大肠异常隐窝灶的内镜和病理特点,探讨ACF与结直肠肿瘤的关系。方法随机选择2011年8月-2012年3月就诊于江西省萍乡市人民医院准备接受结肠镜检查的患者370例,在距肛门25～30 cm以下给予0.4%靛胭脂染色后观察、记录发现远端大肠ACF病例数及ACF数目,并且行病理检查。结果 370例患者共发现256例ACF病例(69.19%)。正常黏膜组、增生性息肉组、腺瘤组、结肠癌组ACF患病率分别为58.21%、78.18%、82.05%、88.89%。256例ACF患者Ⅰ级106例(41.41%)、Ⅱ级82例(32.03%)、Ⅲ级68例(26.56%)。病理有异型增生病例数39例(10.54%),均为轻度异型增生;病理无异型增生217例(58.65%)。有ACF组增生性息肉的发生率为16.8%,腺瘤的发生率25.0%,结直肠癌的发生率12.5%;而无ACF组分别为10.53%、12.58%、3.51%。结论异常隐窝灶是常见结肠镜下病变,异型增生ACF病变并不少见。ACF可能是结肠腺瘤和大肠癌的独立预测因素。

结直肠异常隐窝灶中BAI1、VEGF蛋白表达及意义

目的观察BAI1、VEGF在结肠异型增生性异常隐窝灶(aberrant crypt foci,ACF)、管状腺瘤及腺瘤癌变中的表达。方法联合放大内镜窄带成像(narrow-band imaging,NBI)技术观察ACF,采用免疫组化法检测40例异型增生性ACF、40例结肠管状腺瘤伴异型增生、35例管状腺瘤癌变及32例结直肠正常黏膜标本中BAI1和VEGF的表达。结果 BAI1蛋白在结直肠正常黏膜、异型增生性ACF、结肠管状腺瘤伴异型增生及管状腺瘤癌变组中的阳性率逐步降低,分别为93.8%、72.5%、45%、11.4%,且异型增生性ACF组阳性率明显低于结直肠正常黏膜组(P<0.05),结肠管状腺瘤伴异型增生组阳性率明显低于异型增生性ACF组(P<0.05),管状腺瘤癌变组阳性率明显低于管状腺瘤伴异型增生组(P<0.05);VEGF蛋白在结直肠正常黏膜、异型增生性ACF、管状腺瘤伴异型增生及管状腺瘤癌变组中的阳性率逐步升高,分别为9.4%、52.5%、62.5%、94.3%,且异型增生性ACF组阳性率明显高于结直肠正常黏膜组(P<0.05),管状腺瘤癌变组阳性率明显高于异型增生性ACF组及管状腺瘤伴异型增生组(P<0.05);在异型增生性ACF、管状腺瘤及管状腺瘤癌变过程中BAI1和VEGF表达呈负相关(rs=-0.656,P<0.05)。结论 BAI1低表达与VEGF高表达可能在结直肠癌前病变中起一定作用,可能为结直肠肿瘤的早期诊治提供新的作用靶点。

变焦扩大内镜诊断结直肠癌

结直肠癌发病率的逐年增高已引起了临床医学工作者的高度重视。Brand et al发现,即使临床上无任何症状的普通人群,1/1000的患者已患有小灶性扁平腺瘤,这些腺瘤常常伴有严重的不典型增生,有的甚至伴有腺癌。日本学者Kudo应用实体显微镜,经内镜息肉切除、内镜肠粘膜切除(EMR)或外科手术,观察了14023例患者标本的结直肠粘膜凹窝腺管开口形状,认为结直肠粘膜凹窝腺管开口在不同性质的病变中有不同的形状,可籍此作为结直肠癌特别是小灶性癌或癌前小腺瘤的诊断依据,最近推出的新型变焦扩大电子结肠镜兼有常规内镜和变焦扩大内镜的功能,对小病灶变焦扩大倍数达100～150倍,作者应用最近引进的日本Pentax EC-3830FZ结肠镜开展结直肠粘膜凹窝的研究,明显提高了内镜对小病灶的肉眼诊断正确性。

结肠癌患者直肠异型隐窝灶中脂肪酸合成酶的表达及其意义

背景:异型隐窝灶(ACF)是结直肠上皮性肿瘤最早期的形态学改变,可经腺瘤进展至结直肠癌。脂肪酸合成酶(FAS)在多数人恶性肿瘤组织中呈高表达。目的:检测结肠癌患者直肠ACF中的FAS表达情况,探讨ACF中FAS表达异常在结直肠癌形成中的意义。方法:30例确诊的散发性结肠癌患者纳入研究。以0.2%亚甲蓝溶液行直肠黏膜染色,通过放大结肠镜寻找、识别ACF,选取隐窝数目超过30个的较大的ACF为研究对象。以免疫组化染色检测直肠ACF以及配对结肠癌组织和正常结肠组织中的FAS表达。结果:30例结肠癌患者共确定116个目标ACF,不伴异型增生91个,伴异型增生25个。结肠癌组织中的FAS阳性表达率显著高于ACF和正常结肠组织(76.7%对32.8%和10.0%,P<0.05),ACF与正常结肠组织间差异亦有统计学意义(P<0.05)。伴异型增生的ACF FAS阳性表达率与不伴异型增生者无明显差异(36.0%对31.9%,P>0.05)。结论:F.AS在结直肠癌腺瘤-癌发生序列的最早期即已出现表达异常,在结直肠癌的形成中发挥重要作用。以FAS抑制剂抑制ACF进展可能成为结直肠癌化学预防的手段之一。

人直肠异常隐窝病灶的2年随访研究

目的:异常隐窝病灶(aberrant crypt foci,ACF)目前被广泛认为是光镜下可视最早期的大肠癌癌前病变。本研究在2年时间通过结肠镜下动态观察ACF的变化来初步探讨ACF与结直肠癌的关系。方法:选取2013年1月至2014年12月在山西医科大学第二医院接受结肠镜检查并排除常见致癌及抑癌因素的100例患者,常规在退镜时进行直肠靛胭脂染色,观察并记录初次结肠镜检查、1年及2年复查肠镜时直肠ACF的数目及单个ACF的自然发展变化过程。结果:初次检查及1年和2年后的ACF阳性率比较,差异无统计学意义。ACF随时间的变化大部分继续存在或自行消失,少数发展为息肉、腺瘤,ACF<6枚的病例,以及腺管开口为椭圆形的ACF自行消失率更大,而腺管开口为非椭圆形者更易发展为息肉或腺瘤。结论:ACF变化呈异质性,其中部分可能为大肠癌癌前病变。

黄芪总苷对二甲肼诱导大鼠结直肠异性隐窝灶和肝微粒体代谢酶的影响

目的观察黄芪总苷对二甲肼诱导大鼠产生异性隐窝和肝微粒体细胞色素P450(cytochrome P450s,CYP450)含量、谷胱甘肽转移酶(glutathione-S-transferase,GST)活力的影响。方法 40只SD大鼠随机分为空白对照组、黄芪组、DMH组、黄芪+DMH组,每组10只。黄芪总甙干预和二甲肼诱癌后脱颈处死动物,取结直肠和肝组织。美蓝染色结直肠后观察、计数ACF的个数,差速离心法分离出大鼠肝微粒体。采用一氧化碳还原差示光谱法测定总酶含量,通过采用分光光度计法检测GSH浓度的高低来反应GT活力的大小。结果黄芪总甙+DMH组比DMH组诱导大鼠产生ACF和大型ACF数量均显著下降(P<0.05)。DMH组与空白对照组、黄芪组、黄芪+DMH组比较,CYP450酶含量显著降低、GST酶活力显著上升(P<0.05)。结论黄芪总苷有可能通过降低肝微粒体CYP450酶含量、提高GST活力,从而减少二甲肼诱导大鼠结直肠产生异性隐窝灶数量。

荔枝核总黄酮对大鼠结直肠癌前病变的影响

目的探讨荔枝核总黄酮(TFL)对大鼠结直肠癌前病变的影响。方法将40只大鼠随机分为对照组、模型组、TFL小剂量组、TFL大剂量组。其他组大鼠给予皮下注射二甲肼20mg/kg,对照组大鼠只注射等剂量生理盐水。注射二甲肼次日起,对照组、模型组给予生理盐水灌胃,TFL小剂量组、TFL大剂量组分别按100mg/(kg·d)、200mg/(kg·d)给予TFL灌胃。造模第15周后,取大鼠全部结直肠在镜下观察异性隐窝灶(ACF)的数量,并检测ACF处黏膜程序性死亡受体1(PD-1)、核因子-кB(NF-кB)p65mRNA的表达水平,同时检测血清谷胱甘肽的含量。结果对照组未发现有ACF病变,模型组、TFL小剂量组、TFL大剂量组ACF的数量依次下降(均P<0.05)。模型组、TFL小剂量组、TFL大剂量组、对照组大鼠血清谷胱甘肽含量依次升高(均P<0.05)。模型组ACF中PD-1mRNA的表达水平高于对照组及TFL大剂量组(P<0.05),其余组间差异均无统计学意义(均P>0.05)。与对照组比较,模型组NF-κBp65mRNA的表达水平升高,而TFL大剂量组的表达水平下降(均P<0.05);模型组、TFL小剂量组、TFL大剂量组NF-κBp65mRNA的表达水平依次降低(均P<0.05)。结论TFL对二甲肼诱导的大鼠结直肠癌前病变具有良好的抑制作用,大剂量TFL的作用更佳。NF-κBp65可能为TFL抑制ACF形成的关键因子。

低聚果糖对大鼠结肠癌前期病变形成的影响

目的探讨低聚果糖对大鼠结肠癌前期病变—畸变隐窝病灶(ACF)形成的影响。方法 48只雄性Wister大鼠经适应性喂养1周后随机分为A、B、C和D组,每组12只,B、D组大鼠每周皮下注射1次二甲基肼(20 mg／kg),A、C组大鼠给予等量生理盐水,连续10周；同时A、B组大鼠给予标准鼠食,而C、D组大鼠给予含10％低聚果糖的鼠食,喂养至第12周处死,观察大鼠体重、结肠长度和ACF,以及结肠内容物重量及其丁酸含量的变化。结果各组大鼠体重增加及结肠长度差异无显著性,腹腔内脏器未见明显病灶。C、D组盲肠内容物重量显著高于A、B组,但各组近、远端结肠内容物重量差异无显著性。C、D组各肠段内容物丁酸浓度显著高于A、B组的相应肠段,D组≥4个隐窝的ACF数均显著低于B组,且丁酸浓度和ACF总数呈显著的负相关。结论低聚果糖能抑制大鼠结肠癌前期病变的形成。