Application of immune checkpoint inhibitors and microsatellite instability in gastric cancer

In this editorial we comment on the article by Li published in the recent issue of the World Journal of Gastroenterology.We focus specifically on the application of immune checkpoint inhibitors(ICIs)and microsatellite instability(MSI)in gastric cancer(GC).The four pillars of GC management have long been considered,including surgery,chemotherapy,radiotherapy and targeted therapy.However,immunotherapy has recently emerged as a“fifth pillar”,and its use is rapidly expanding.There are four principal strategies for tumor immunotherapy:ICIs,tumor vaccines,adoptive immunotherapy and nonspecific immunomodulators.Of them,ICIs are the most advanced and widespread type of cancer immunotherapy for GC.Recent breakthrough results for ICIs have paved the way to a new era of cancer immunotherapy.In particular,inhibition of the PD-1/PD-L1 axis with ICIs,including nivolumab and pembrolizumab,has emerged as a novel treatment strategy for advanced GC.Unfortunately,these therapies are sometimes associated with often subtle,potentially fatal immune-related adverse events(irAEs),including dermatitis,diarrhea,colitis,endocrinopathy,hepatotoxicity,neuropathy and pneumonitis.We must be aware of these irAEs and improve the detection of these processes to prevent inappropriate discharges,emergency department revisits,and downstream complications.Recent studies have revealed that MSI-high or mismatch-repair-deficient tumors,regardless of their primary site,have a promising response to ICIs.So,it is important to detect MSI before applying ICIs for treatment of GC.

Tislelizumab in previously treated,locally advanced unresectable/metastatic microsatellite instability-high/mismatch repair-deficient solid tumors

Objective:The open-label,phase II RATIONALE-209 study evaluated tislelizumab(anti-programmed cell death protein 1 antibody)as a tissue-agnostic monotherapy for microsatellite instability-high(MSI-H)/mismatch repair-deficient(dMMR)tumors.Methods:Adults with previously treated,locally advanced unresectable or metastatic MSI-H/dMMR solid tumors were enrolled.Patients received tislelizumab 200 mg intravenously every 3 weeks.Objective response rate(ORR;primary endpoint),duration of response(DoR),and progression-free survival(PFS)were assessed by independent review committee(Response Evaluation Criteria in Solid Tumors v1.1).Results:Eighty patients were enrolled and treated;75(93.8%)patients had measurable disease at baseline.Most had metastatic disease and received at least one prior therapy for advanced/metastatic disease(n=79;98.8%).At primary analysis(data cutoff July 8,2021;median follow-up 15.2 months),overall ORR[46.7%;95%confidence interval(95%CI),35.1−58.6;one-sided P<0.0001]and ORR across tumor-specific subgroups[colorectal(n=46):39.1%(95%CI,25.1–54.6);gastric/gastroesophageal junction(n=9):55.6%(95%CI,21.2−86.3);others(n=20):60.0%(95%CI,36.1−80.9)]were significantly greater with tislelizumab vs.a prespecified historical control ORR of 10%;five(6.7%)patients had complete responses.Median DoR,PFS,and overall survival were not reached with long-term follow-up(data cutoff December 5,2022;median follow-up 28.9 months).Tislelizumab was well tolerated with no unexpected safety signals.Treatment-related adverse events(TRAEs)of grade≥3 occurred in 53.8%of patients;7.5%of patients discontinued treatment due to TRAEs.Conclusions:Tislelizumab demonstrated a significant ORR improvement in patients with previously treated,locally advanced unresectable or metastatic MSI-H/dMMR tumors and was generally well tolerated.

Comparative effectiveness of immunotherapy and chemotherapy in patients with metastatic colorectal cancer stratified by microsatellite instability status

BACKGROUND Immunotherapy have demonstrated promising outcomes in patients with high microsatellite instability(MSI)(MSI-H)metastatic colorectal cancer.However,the comparative effectiveness of Immunotherapy and chemotherapy for patients with low MSI(MSI-L),and microsatellite stable(MSS)metastatic colorectal cancer remains unclear.AIM To investigate immunotherapy vs chemotherapy for treatment of MSI-L/MSS metastatic colorectal cancer,and to evaluate the success of immunotherapy against chemotherapy in managing MSI-H metastatic colorectal cancer during a follow-up of 50 months.METHODS We conducted a retrospective cohort study using the National Cancer Database(NCDB)to evaluate the overall survival(OS)of patients with metastatic colorectal cancer treated with immunotherapy or chemotherapy.The study population was stratified by MSI status(MSI-H,MSI-L,and MSS).Multivariable Cox proportional hazard models were used to assess the association between treatment modality and OS,adjusting for potential confounders.RESULTS A total of 21951 patients with metastatic colorectal cancer were included in the analysis,of which 2358 were MSI-H,and 19593 were MSI-L/MSS.In the MSI-H cohort,immunotherapy treatment(n=142)was associated with a significantly improved median OS compared to chemotherapy(n=860).After adjusting for potential confounders,immunotherapy treatment remained significantly associated with better OS in the MSI-H cohort[adjusted hazard ratio(aHR):0.57,95%confidence interval(95%CI):0.43-0.77,P<0.001].In the MSS cohort,no significant difference in median OS was observed between immunotherapy treatment and chemotherapy(aHR:0.94,95%CI:0.69-1.29,P=0.715).CONCLUSION In this population-based study using the NCDB,immunotherapy treatment was associated with significantly improved OS compared to chemotherapy in patients with MSI-H metastatic colorectal cancer,but not in those with MSI-L/MSS metastatic colorectal cancer.Further studies are warranted to determine the optimal therapeutic approach for patients with MSI-L/MSS metastatic colorectal cancer.

结直肠癌患者RAS、BRAF基因突变与MSI状态的相关性及其临床病理特征

目的:结直肠癌是人类最常见的恶行肿瘤之一,其发病率和病死率呈逐年上升趋势。本研究旨在分析结直肠癌患者大鼠肉瘤病毒癌基因(rat sarcoma viral oncogene,RAS)、鼠类肉瘤病毒癌基因同源物(V-Raf murine sarcoma viral oncogene homolog B,BRAF)突变与微卫星不稳定(microsatellite instability,MSI)状态相关性及其临床病理特征,为结直肠癌临床治疗及预后评估提供依据。方法:回顾性分析444例结直肠癌患者的临床病理资料,并提取肿瘤组织基因组DNA,采用荧光定量PCR法检测Kirsten大鼠肉瘤病毒癌基因同源物(Kirsten rat sarcoma viral oncogene homolog,KRAS)、Neuroblastoma大鼠肉瘤病毒癌基因同源物(neuroblastoma rat sarcoma viral oncogene homolog,NRAS)第2、3、4外显子及BRAF V600E突变;运用PCR-毛细血管电泳行MSI状态分析。结果:K(N)RAS基因突变184例(41.44%,184/444),其中KRAS突变173例(94.02%,173/184),NRAS突变11例(5.98%,11/184),K(N)RAS共突变3例。BRAF V600E突变21例(4.7%,21/444)。微卫星高度不稳定(microsatellite instability high,MSIH)48例(10.81%,48/444),微卫星低度不稳定(microsatellite instability low,MSI-L)和微卫星稳定(microsatellite stable,MSS)共396例(89.19%,396/444)。K(N)RAS基因突变右半结肠癌多于左半结肠癌,且黏液腺癌突变率高于单纯腺癌(均P<0.05)。K(N)RAS基因突变与患者性别、年龄、肿瘤大小、肉眼分型、组织学分化程度、淋巴结转移、病理分期均无关(均P>0.05)。女性BRAF V600E突变高于男性,低分化高于中分化(均P<0.05),BRAF V600E突变与患者发病年龄、肿瘤位置、大小、肉眼分型、组织学类型、淋巴结转移、病理分期均无关(均P>0.05)。发生MSI-H的患者中,右半结肠癌多于左半结肠癌,肿瘤直径≥4.5 cm病例多于直径更小病例,隆起型多于其他肉眼分型,黏液腺癌多于单纯腺癌,低分化多于高分化(均P<0.05),而与患者性别和年龄均无关(均P>0.05)。K(N)RAS突变与MSI-H发生无关(P>0.05),但RAS基因Gly位点突变与MSI-H发生相关(P<0.05)。携带RAS基因Gly位点突变的MSI-H结直肠癌患者男性多于女性,发病年龄无差异,右半结肠多于左半结肠,肉眼分型多为溃疡型,单纯腺癌比例高于黏液腺癌,多为中低分化,较多处于病理分期I~II期,常不伴淋巴结转移和BRAF V600E突变,Gly突变位点多为Gly12Ser/Asp突变。BRAF V600E突变与MSI-H发生有关(P<0.05)。与K(N)RAS突变型MSI-L/MSS结直肠癌比较,K(N)RAS突变型MSI-H结直肠癌较易发生于右半结肠,肿瘤直径≥4.5 cm的病例较多,组织学类型多为黏液腺癌,较少发生淋巴结转移,多处于病理分期I~II(均P<0.05);K(N)RAS突变型MSI-H结直肠癌与性别、年龄、肿瘤肉眼分型、组织学分化均无相关(均P>0.05)。与RAS野生型-MSI-L/MSS结直肠癌比较,RAS野生型-MSI-H结直肠癌多发生于右半结肠,肿瘤直径≥4.5 cm,多为溃疡型和隆起型,较多为黏液腺癌,且多为中低分化(均P<0.05),而RAS野生型-MSI-H结直肠癌与性别、年龄、淋巴结转移、病理分期均无关(均P>0.05)。结论:结直肠癌KRAS基因Gly位点突变、BRAF V600E突变与MSI-H发生相关;MSI-H-RAS基因Gly点突变结直肠癌患者有其独特的临床病理特征;RAS-MSI基因状态与临床病理特征相关;K(N)RAS、BRAF V600E、MSI检测有利于结直肠癌患者个体化治疗及预后评估。

纳武利尤单抗联合伊匹木单抗治疗MSI-H晚期结肠癌1例报道

本文报告1例晚期结肠癌患者,既往术后标本免疫组化结果提示错配修复完整(proficient mismatch repair, pMMR),予术后化疗等全身治疗后病情进展。随后行二代测序(next-generation sequencing, NGS)提示该患者微卫星高度不稳定(microsatellite instability-high, MSI-H)以及高水平的肿瘤突变负荷值(tumor mutation burden, TMB)。

PD-1单抗治疗一例dMMR/MSI-H/TMB-H型结肠癌伴颅内转移瘤患者临床完全缓解

一例70岁男性患者,在接受右半肠癌根治性手术1年后出现了记忆丧失和认知功能下降的症状,头颅磁共振成像检查发现脑部肿块,手术后经病理检查确诊为结肠腺癌转移。原发灶及颅内转移瘤免疫组织化学检测均提示为错配修复缺陷。原发结肠肿瘤组织基因检测证实为微卫星高度不稳定伴有高肿瘤突变负荷,肿瘤突变负荷为77.7 muts/Mb。患者结肠癌根治术和颅内转移瘤术后均接受了辅助化疗,但在颅内转移瘤切除术和化疗结束后1个月颅内转移复发。患者接受帕博利珠单抗治疗后结果颅内转移瘤消退并达到临床完全缓解。

Discrepancy among microsatellite instability detection methodologies in non-colorectal cancer:Report of 3 cases

BACKGROUND Microsatellite instability(MSI)is a predictive biomarker for cancer immunotherapy.The tumor-agnostic nature of MSI makes it a denominator for immunotherapy in several solid tumors.It can be assessed using next-generation sequencing(NGS),fluorescent multiplex PCR,and immunohistochemistry(IHC).CASE SUMMARY Here,we report 3 cases with discordant MSI results detected using different methods.A cholangiocellular carcinoma case revealed proficient mismatch repair(MMR)by IHC but high MSI(MSI-H)by liquid NGS.A cervical cancer case revealed deficient MMR by IHC,microsatellite stable by PCR,and MSI-H by NGS.Lastly,an endometrial cancer case revealed proficient MMR by IHC but MSI-H by NGS.CONCLUSION IHC for MMR status is the first choice due to several advantages.However,in cases of indeterminate IHC results,molecular testing by MSI-PCR is preferred.Recently,NGS-based MSI assays are being widely used to detect MSI-H tumors.All three methods have high accuracy;however,the inconsistencies between them may lead to misdiagnosis.

IVIM全容积定量参数与直肠腺癌神经脉管侵犯、MSI状态及Ki-67指数的相关性研究

目的探讨体素内不相干运动(intravoxel incoherent motion,IVIM)全肿瘤容积参数与直肠腺癌患者神经侵犯(perineural invasion,PNI)、脉管侵犯(lymphovascular invasion,LVI)、微卫星不稳定性(microsatellite instability,MSI)状态及Ki-67指数的相关性。材料与方法回顾性分析136例直肠腺癌患者的影像资料和临床资料,测量病灶IVIM全容积参数包括真实扩散系数(D)、伪扩散系数(D*)及灌注分数(f)。根据病理报告中的LVI状态、PNI状态、MSI及Ki-67指数进行分组,采用独立样本t检验或Mann-Whitney U检验分析各定量参数与肿瘤病理学特征的关系。结果直肠腺癌PNI阴性组D值[(1.174±0.164)×10^(-3) mm^(2)/s]显著低于阳性组[(1.270±0.206)×10^(-3) mm^(2)/s](t=-3.033,P=0.003),LVI阴性组f值0.172(0.158,0.193)显著低于阳性组0.188(0.168,0.237)(Z=-2.435,P=0.015),Ki-67低表达组f值(0.175±0.035)显著低于高表达组(0.188±0.038)(t=-2.097,P=0.038),MSI高组和MSI低组的D、D*、f值差异无统计学意义(P>0.05)。结论IVIM全容积定量参数能够在一定程度上反映直肠腺癌的病理学特征,可作为术前评估直肠腺癌生物学行为的重要影像学指标。

Bat 26 Microsatellite Instability in Oral Cavity Cancers in Senegal

Oral cavity cancers are part of head and neck cancers. They have become frequent in the world in general and Senegal in particular. This study evaluates microsatellite instability tumors in oral cavity cancers in Senegal. Forty cancerous tissues, 20 healthy tissues, and 12 blood tissues were included in this study. These tissues were collected from each patient during the biopsy after obtaining consent. DNA extraction, Polymerase Chain Reaction (PCR) and sequencing were carried out to obtain sequences. Mutation surveyor, Bioedit and Dnasp software were used to perform our analyses. High instability was found in 57.5% of patients with cancer. Moreover, 90% of the patients had the same motif on healthy and cancerous tissue. Furthermore, 26.12%, 20.72%, and 11.71% polymorphic sites were found in cancerous, healthy and blood tissue respectively. Thus, a similarity between cancerous and healthy tissues seems to exist. This implies that instability of the Bat 26 microsatellite could occur early in the occurrence of oral cavity cancers.

结直肠癌患者KRAS、NRAS、BRAF、HER2基因突变及MSI状态与临床特征的相关性分析

目的探讨结直肠癌患者的Kirsten大鼠肉瘤病毒癌基因同源物(KRAS)、神经母细胞瘤病毒癌基因RAS同源物(NRAS)、鼠类肉瘤滤过性毒菌致癌同源体B(BRAF)、人表皮生长因子受体2(HER2)基因突变及微卫星不稳定性(MSI)状态与临床病理特征之间的关系。方法收集2019年10月至2022年3月在该院接受治疗的226例结直肠癌患者的临床资料,采用二代测序技术检测KRAS、NRAS、BRAF、HER2基因突变情况和MSI状态,应用免疫组化法评估错配修复系统(MMR)状态,采用多因素Logistic回归分析KRAS、NRAS、BRAF、HER2与临床病理特征的关系。结果在226例结直肠癌患者中,KRAS基因突变频率为54.9%,NRAS基因突变频率为5.3%,BRAF基因突变频率为8.4%,HER2基因扩增突变频率为1.8%。黏液腺癌KRAS基因的突变频率高于普通腺癌(P<0.05),右半结肠癌KRAS基因突变的风险增加(OR=2.145,P=0.012)。而NRAS基因突变在左半结肠和直肠癌频率较高(P<0.05)。BRAF基因突变在低分化类型及微卫星高度不稳定(MSI-H)的结直肠癌中突变频率均较高(P<0.05),右半结肠BRAF基因突变的风险增加(OR=2.844,P=0.042)。HER2基因扩增突变表现肝肺等远处转移(P<0.05)。KRAS基因突变与NRAS、BRAF、HER2扩增突变是相互排斥的,差异有统计学意义(P<0.05)。MSI-H在右半结肠中的发生频率更高(P<0.05)。226例标本检出10例标本错配修复缺陷(dMMR)/MSI-H,8例标本dMMR/微卫生稳定,5例标本错配修复正常/MSI-H,dMMR和MSI-H之间存在中等程度的一致性(Kappa=0.575)。结论结直肠癌患者中,KRAS、NRAS、BRAF、HER2基因及MSI状态与临床病理特征有关,联合检测能够提供更准确、有效的数据,以指导患者的治疗临床用药和预后判断。

能谱CT影像组学预测结直肠癌MSI状态的应用研究

目的研究基于能谱CT成像静脉期单能量序列影像组学模型,用于预测结直肠癌微卫星不稳定(MSI)状态。方法回顾性收集2019年7月至2022年8月在泰州市人民医院经手术切除或穿刺活检病理确诊为结直肠癌患者97例(男性57例、女性40例)。根据免疫组化MSI表达结果进行分组:MSI组34例、微卫星稳定(MSS)组63例。以DICOM格式将静脉期1.25mm原始图像数据传至GEAW4.7后处理工作站,生成碘基物质分解图、70keV、100keV单能量图,导入ITK-SNAP开源软件,手动勾画感兴趣区(ROI),利用Pyradiomics工具进行影像组学特征提取,采用mRMR(最大相关和最小冗余)和LASSO(最小绝对收缩选择算子)算法对训练组的影像组学特征进行降维,获取关键的影像组学特征,建立预测肿瘤生物学行为的影像组学模型。采用受试者工作特征(ROC)曲线下面积(AUC)来评估模型的诊断效能。使用校正曲线对模型的校正性能进行评估,应用决策曲线评价模型在训练组中的临床实用性。结果静脉期单能量70keV序列、100keV序列、碘基物质分解图共三种模型各提取了1218个特征,其中70keV单能量序列特征分类性能最佳。结论基于能谱CT成像的单能量模型可以有效地区分结直肠癌MSI和MSS状态患者,可以作为术前预测结直肠癌患者MSI状态的重要影像生物标志物,为指导临床医生制定个体化治疗方案及评估患者预后提供新思路。

结直肠癌组织中MMR蛋白表达、MSI、RAS和BRAF基因突变与临床病理特征的关系

目的 探讨结直肠癌患者癌组织中错配修复(MMR)蛋白表达、微卫星不稳定性(MSI)、大鼠肉瘤(RAS)基因和致癌同源体B1(BRAF)基因突变与临床病理特征的关系。方法 选取该院2022年1-12月接受根治手术治疗的352例结直肠癌患者的肿瘤组织和血液标本、42例非肠癌患者的实体瘤组织和血液标本,采用免疫组化法检测MMR蛋白表达,一代测序片段分析法检测MSI,实时荧光定量聚合酶链反应检测KRAS、NRAS和BRAF基因突变状态,分析MMR蛋白表达、MSI和3种基因突变状态与结直肠癌临床病理特征的关系。结果 352例CRC患者肿瘤组织中检出MMR缺陷(dMMR)29例(8.2%),高度微卫星不稳定(MSI-H)26例(7.4%),KRAS基因突变161例(45.7%),NRAS基因突变13例(3.7%),BRAF基因突变11例(3.1%)。与dMMR有关因素为低龄、黏液腺癌、原发于右半结肠癌(P<0.05);与MSI-H相关因素包括低龄、肿瘤家族史、原发于右半结肠癌(P<0.05);KRAS和NRAS基因高突变率分别与黏液腺癌和淋巴结转移有关(P<0.05);BRAF基因高突变率与低分化和原发于右半结肠癌有关(P<0.05)。BRAF基因突变与dMMR和MSI-H有关(P<0.05)。结论 MMR蛋白表达,MSI,以及KRAS、NRAS和BRAF基因突变与不同的临床病理特征有关。通过这5种分子标志物的联合检测可以对肿瘤进行分子分型,进一步为结直肠癌患者的个体化精准诊疗提供理论依据。

Study on the Correlation between the Expression of Angiogenic Factor VEGF and Microsatellite Instability in Gastric Adenocarcinoma

Objective: To investigate the correlation between the microsatellite instability (MSI) and the expression of vascular endothelial growth factor (VEGF) in gastric adenocarcinoma. Methods: PCR SSCP method was used to detect MSI of thirty cases with gastric adenocarcinoma at five loci in each patient. Expression of VEGF was examined by the method of immunohistochemistry. Results: The positive of MSI was in 13 patients out of 30 patients (43.4%) in our study. Positive VEGF Immunostaining was detected in 18 patients (60.0%). VEGF was decreased in microsatellite instability high (MSI H) gastric adenocarcinoma. Conclusion: MSI H and microsatellite stable (MSS) gastric adenocarcinoma may follow a different pathway of angiogenesis. The low frequency of VEGF expression among MSI H cancer may partially explain why these cancers are less aggressive.

Characterization of six tumorsuppressor genes and microsatellite instability in hepatocellular carcinomain southern African blacks

AIM To analyse cumulative loss of heterozygosity (LOH) of chromosomal regions and tumor suppressor genes in hepatocellular carcinomas (HCCs) from 20 southern African blacks. METHODS p53, RB1, BRCA1, BRCA2, WT1 and E cadherin genes were analysed for LOH, and p53 gene was also analysed for the codon 249 mutation, in tumor and adjacent non tumorous liver tissues using molecular techniques and 10 polymorphic microsatellite markers. RESULTS p53 codon 249 mutation was found in 25% of the subjects, as was expected, because many patients were from Mozambique, a country with high aflatoxin B 1 exposure. LOH was found at the RB1, BRCA2 and WT1 loci in 20%(4/*!20) of the HCCs, supporting a possible role of these genes in HCC. No LOH was evident in any of the remaining genes. Reports of mutations of p53 and RB1 genes in combination, described in other populations, were not confirmed in this study. Change in microsatellite repeat number was noted at 9/*!10 microsatellite loci in different HCCs, and changes at two or more loci were detected in 15%(3/*!20) of subjects. CONCLUSION We propose that microsatellite/genomic instability may play a role in the pathogenesis of a subset of HCCs in black Africans.

Potential roles of tumor suppressor genes and microsatellite instability in hepatocellular carcinogenesis in southern African blacks

MAJOR POINTS OF THE COMMENTED ARTICLECumulative loss of heterozygosity(LOH)ofchromosomal regions and tumor suppressor geneshas been reported in hepatocellular carcinomas(HCCs) from China,Japan,and Korea.In thisissue of the World Journal of Gastroenterology,Martins et al report an analysis of LOH andmicrosatellite instability in HCCs from a group of

Era of universal testing of microsatellite instability in colorectal cancer

Colorectal cancer (CRC) incidence and mortality are constantly decreasing, but CRC still remains the third most prevalent cancer and the third most common cause of cancer death in both males and females in the United States. Recent rapid declines in CRC incidence rates have largely been attributed to increases in screening that can detect and remove precancerous polyps, and the decrease in death rates for CRC largely reflects improvements in early detection, treatment and the understanding of molecular/genetic basis of CRC. One of the important molecular/genetic findings is the presence of microsatellite instability (MSI) in CRCs. Many studies have shown the importance of MSI testing in diagnosing Lynch syndrome and predicting prognosis and response to chemotherapeutic agents in CRCs. Increased emphasis has been placed on the importance of MSI testing for all newly diagnosed individuals with CRCs. Both immunohistochemical staining (IHC) and polymerase chain reaction (PCR)-based MSI testing show high sensitivity and specificity in detecting MSI. The current clinical guidelines and histopathology features are indicative of, but not reliable in diagnosing Lynch syndrome and CRCs with MSI. Currently, there are evidences that universal testing for MSI starting with either IHC or PCR-based MSI testing is cost effective, sensitive, specific and is getting widely accepted.

MSIsensor-RNA:Microsatellite Instability Detection for Bulk and Single-cell Gene Expression Data

Microsatellite instability(MSI)is an indispensable biomarker in cancer immunotherapy.Currently,MSI scoring methods by high-throughput omics methods have gained popularity and demonstrated better performance than the gold standard method for MSI detection.However,the MSI detection method on expression data,especially single-cell expression data,is still lacking,limiting the scope of clinical application and prohibiting the investigation of MSI at a single-cell level.Herein,we developed MSIsensor-RNA,an accurate,robust,adaptable,and standalone software to detect MSI status based on expression values of MSI-associated genes.We demonstrated the favorable performance and promise of MSIsensor-RNA in both bulk and single-cell gene expression data in multiplatform technologies including RNA sequencing(RNA-seq),microarray,and single-cell RNA-seq.MSIsensor-RNA is a versatile,efficient,and robust method for MSI status detection from both bulk and single-cell gene expression data in clinical studies and applications.MSIsensor-RNA is available at https://github.com/xjtu-omics/msisensor-rna.

Microsatellite instability,MMR gene expression and proliferation kinetics in colorectal cancer with famillial predisposition

INTRODUCTIONGenetic instability is a conunon property of manyhuman cancers,including those of HNPCC.A novel form of genetic instability involving somaticalterations,such as deletions and insertions insimple repeated sequences,has been found.Microsatellitcs are relatively short runs of tandemlyrepeated sequences scattered throughout

Helicobacter pylori and EBV in gastric carcinomas:Methylation status and microsatellite instability

AIM:To verify the methylation status of CDH1, DAPK, COX2, hMLH1 and CDKN2A genes and to evaluate their association with Helicobacter pylori (H. pylori)-cagA+ and Epstein Barr virus (EBV) infections in gastric adenocarcinomas.METHODS: Methylation-specific PCR (MSP) assay was performed in 89 primary gastric carcinomas (intestinal and diffuse types). Microsatellite instability (MSI) analysis was performed using the BAT26 primer set and PCR products were analyzed with the ABI PRISM 3100 Genetic Analyzer using Genescan 3.7 software (Applied Biosystems). Detection of H. pylori and genotyping were performed by PCR, using specifi c primers for ureaseC and cagA genes. The presence of EBV was assessed by in situ hybridization. Statistical analyses were performed using the χ2 or Fisher's exact test.RESULTS: The most frequent hypermethylated gene was COX-2 (63.5%) followed by DAPK (55.7%), CDH1 (51%), CDKN2A (36%) and hMLH1 (30.3%). Intestinal and diffuse adenocarcinomas showed different methylation profiles and there was an association between methylation of E-CDH1 and H. pylori-cagA+ in the intestinal adenocarcinoma type. MSI was correlated with hMLH1 methylation. There was an inverse correlation between DAPK hypermethylation and MSI.CONCLUSION: We found a strong association between CDH1 methylation and H. pylori-cagA+ in intestinal-type gastric cancer, association of MSI and better prognosis and an heterogeneous COX-2 overexpression.

Interrelationship between microsatellite instability and microRNA in gastrointestinal cancer

There is an increasing understanding of the roles that microsatellite instability （MSI） plays in Lynch syndrome （by mutations） and sporadic （by mainly epigenetic changes） gastrointestinal （GI） and other cancers. Defi- cient DNA mismatch repair （MMR） results in the strong mutator phenotype known as MSI, which is the hall- mark of cancers arising within Lynch syndrome. MSI is characterized by length alterations within simple repeated sequences called microsatellites. Lynch syn- drome occurs primarily because of germline mutations in one of the MMR genes, mainly MLH1 or MSH2, less frequently MSH6, and rarely PMS2. MSI is also observed in about 15% of sporadic colorectal, gastric, and en-dometrial cancers and in lower frequencies in a minor- ity of other cancers where it is often associated with the hypermethylation of the IVlLH1 gene. miRNAs are small noncoding RNAs that regulate gene expression at the posttranscriptional level and are critical in many biological processes and cellular pathways. There is accumulating evidence to support the notion that the interrelationship between MSI and miRNA plays a key role in the pathogenesis of GI cancer. As a possible new mechanism underlying MSI, overexpression of m/R-IEE has been shown to downregulate expression of MLH1, IVlSH2, and MSH6. Thus, a subset of MSI-positive （MSI＋） cancers without known MMR defects may result from m/R-1E5 overexpression. Target genes of frameshift mutation for MSI are involved in various cellular func- tions, such as DNA repair, cell signaling, and apoptosis. A novel class of target genes that included not only epi- genetic modifier genes, such as HDAC2, but also miRNA processing machinery genes, including TARBP2 and XPO5, were found to be mutated in MSI＋ GI cancers. Thus, a subset of MSI＋ colorectal cancers （CRCs） has been proposed to exhibit a mutated miRNA machinery phenotype. Genetic, epigenetic, and transcriptomic dif- ferences exist between MSI＋ and MSI- cancers. Mo- lecular signatures of miRNA expression apparently have the potential to distinguish between MSI＋ and MSI- CRCs. In this review, we summarize recent advances in the MSI pathogenesis of GI cancer, with the focus on its relationship with miRNA as well as on the potential to use MSI and related alterations as biomarkers and novel therapeutic targets.