Differential mucin phenotypes and their significance in a variation of colorectal carcinoma

来源 :World Journal of Gastroenterology | 被引量 : 0次 | 上传用户:moneyNUMBER_1
下载到本地 , 更方便阅读
声明 : 本文档内容版权归属内容提供方 , 如果您对本文有版权争议 , 可与客服联系进行内容授权或下架
论文部分内容阅读
AIM: To investigate mucin expression profiles in colorectal carcinoma (CRC) histological subtypes with regard to clinicopathologic variables and prognosis. METHODS: Mucin (MUC)2 and MUC5AC expressions were assessed by immunohistochemistry for a total of 250 CRC cases that underwent surgical resection. CRCs included 63 well-to-moderately differentiated adenocar-cinomas (WMDAs), 91 poorly differentiated adenocarcinomas (PDAs), 81 mucinous adenocarcinoma (MUAs), and 15 signet-ring cell carcinomas (SRCCs). MUC2 and MUC5AC were scored as positive when ≥ 25% and ≥ 1% of cancer cells were stained positive, respectively. The human mutL homolog 1 and human mutS homolog 2 expressions were assessed by immunohistochemistry in PDAs to investigate mismatch-repair (MMR) status.Tumors that did not express either of these two were considered MMR-deficient. Results were analyzed for associations with clinicopathologic variables and the prognosis in individual histological CRC subtypes. RESULTS: MUC2-positive and MUC5AC-positive WMDA percentages were 49.2% and 30.2%, respectively. In contrast, MUC2-positive and MUC5AC-positive PDA percentages were 9.5% and 51.6%, respectively. MUC2 levels tended to decrease and MUC5AC levels tended to increase from WMDA to PDA. In 21 tumors comprising both adenoma and adenocarcinoma components in a single tumor (4 WMDAs, 7 PDAs, and 10 MUAs), MUC2 was significantly downregulated in PDA and MUC5AC was downregulated in PDA and MUA in the adenoma-carcinoma sequence. These results suggested that MUC2 levels might be associated with malignant potential and that MUC5AC expression was an early event in tumorigenesis. Despite worse prognoses than WMDA, high MUC2 expression levels were maintained in MUA (95.1%) and SRCC (71.5%), which suggested a pathogenesis for these subtypes distinct from that of WMDA. No significant associations were found between MUC2 expression and any clinicopathologic variables in any histological subtype. MUC5AC expression in PDA was closely associated with right-sided location (P = 0.017), absence of nodal metastasis (P = 0.010), low tumor node metastasis stage (P = 0.010), and MMR deficiency (P = 0.003). MUC2 expression in WMDA was a marginal prognostic factor for recurrence/metastasis-free survival (RFS) by univariate Cox analysis (P = 0.077) but not by multivariate Cox analysis (P = 0.161). MUC5AC expression in PDA was a significant prognostic factor for RFS by univariate Cox analysis (P = 0.007) but not by multivariate Cox analysis (P = 0.104). Kaplan-Meier curves and log-rank tests revealed that MUC2 expression was marginally associated with a better WMDA prognosis [P = 0.064 for RFS and P = 0.172 for overall survival (OS)] but not for PDA. In contrast, MUC5AC expression was significantly and marginally associated with a better PDA prognosis in terms of RFS and OS, respectively(P = 0.004 for RFS and P = 0.100 for OS), but not for WMDA and MUA. CONCLUSION: Mucin core protein expression profiles and clinical significance differ according to histological CRC subtypes. This may reflect different pathogeneses for these tumors. AIM: To investigate mucin expression profiles in colorectal carcinoma (CRC) histological subtypes with regard to clinicopathologic variables and prognosis. METHODS: Mucin (MUC) 2 and MUC5AC expressions were assessed by immunohistochemistry for a total of 250 CRC cases that underwent surgical resection. CRCs included 63 well-to-moderately differentiated adenocar-cinomas (WMDAs), 91 poorly differentiated adenocarcinomas (PDAs), 81 mucinous adenocarcinoma (MUAs), and 15 signet-ring cell carcinomas The human mutL homolog 1 and human mutS homolog 2 expressions were assessed by immunohistochemistry in PDAs to investigate mismatch-repair (MMR) status.Tumors that did not express either of these. 25% and ≥ 1% of cancer cells were stained positive, respectively. Two were considered MMR-deficient. Results were analyzed for associations with clinicopathologic variables and the prognosis in individual histological CRC subtypes. RESULTS: MUC2 MUC2-positive and MUC5AC-positive PDA percentages were 49.2% and 30.2%, respectively. In contrast, MUC2-positive and MUC5AC-positive PDA percentages were 9.5% and 51.6%, respectively. MUC2 levels tended to decrease and MUC5AC levels tended to increase from WMDA to PDA. MUC2 was significantly downregulated in PDA and MUC5AC was downregulated in PDA and MUA in the adenoma-carcinoma sequence. All of the 21 adenomas and adenocarcinoma components in a single tumor (4 WMDAs, 7 PDAs, and 10 MUAs) These results suggest that MUC2 levels might be associated with malignant potential and that MUC5AC expression was an early event in tumorigenesis. However, MUC5AC expression was an early event in tumorigenesis. a pathogenesis for these subtypes distinct from that of WMDA. No significant associations were found between MUC2 expression and any clinicopathologic variables in any histological subtype. MUC5AC expression in PDA wasabsence of nodal metastasis (P = 0.010), low tumor node metastasis stage (P = 0.010), and MMR deficiency (P = 0.003). MUC2 expression in WMDA was a marginal MUC5AC expression in PDA was a significant prognostic factor for RFS by univariate Cox analysis (P = 0.077) but not by multivariate Cox analysis (P = 0.161). The prognostic factor for recurrence / metastasis-free survival = 0.007) but not by multivariate Cox analysis (P = 0.104). Kaplan-Meier curves and log-rank tests revealed that MUC2 expression was marginally associated with a better WMDA prognosis [P = 0.064 for RFS and P = 0.172 for overall survival ( OS)] but not for PDA. In contrast, MUC5AC expression was significantly and marginally associated with a better PDA prognosis in terms of RFS and OS, respectively (P = 0.004 for RFS and P = 0.100 for OS), but not for WMDA and MUA. CONCLUSION: Mucin core protein expression profiles and clinical si gnificance differ according to histological CRC subtypes. This may reflect different pathogeneses for these tumors.
其他文献
  目的:开发检测TTSuV的新方法,并用于调查各年龄段猪群TTSuV流行情况。方法:从38个猪场收集265份血清样品。提供样品的猪包括胎儿(在吃母乳前,小于1日龄,34头),哺乳猪(1-20日龄,2
会议
这幅作品被认为是米开朗基罗·梅里西·达·砖拉瓦乔最杰出的代表作之一。因为此画属于大收藏家和卡拉瓦乔的仰慕者、红衣主教西皮奥内·博尔盖塞的遗产,人们不知道此画的确切
  对PCV2表现亚临床症状的猪免疫圆环疫苗,并与免疫前的猪生产性能进行比较。通过T检验、方差分析、Breslow检验及卡方检验对数据进行分析。免疫后,猪的死亡率降低,体重增加2.
传统秸秆气化炉存在三大技术问题秸秆气化炉能将农林废弃物、食用菌废渣、牛羊畜粪等转化为秸秆混合燃气,这种燃气能像液化气一样用于炊事、取暖、淋浴。然而,秸秆气化炉在使
  目的:比较国产灭活PCV 2疫苗和Ingevac CircoFLEX对保育仔猪生产性能的影响。方法:将45窝(447头仔猪14日龄)随机分为3组:A组,15窝(149头仔猪)免疫Ingevac CircoFLEX,每次剂量1
  本文研究了同一猪场中两种疫苗的免疫效果。以一个800头母猪的猪场为研究对象,仅免疫支原体疫苗后,爆发PMWS,然后开始免疫圆环疫苗(程序“MSD1”)。几个月后,换成了含有相同
  目的:进一步确认圆环疫苗、支原体疫苗及蓝耳疫苗的联合使用的安全性及效力。方法:对3周龄的小猪注射圆环和支原体联合疫苗(FLEXcombo),连续使用半年。在检测到蓝耳感染后,免
会议
  本文检测了PCV2a和PCV2b在PCVAD阴性育肥猪群血清中的存在情况,研究经免疫组化诊断为PCVAD患猪群中PCV2主的要流行基因型,并对PCV 1-2a嵌合病毒及PCV1的流行情况进行调查。
  本文通过大量的测序方法研究了一起AⅡ型先天性震颤病例。从脑部样品中提取RNA用以454测序,并通过两个real-time RT PCR同时对BVDV-1/BVDV-2和牛的未分型瘟病毒进行检测。
  本文从PMWS患猪分离PCV2 48285株,采用定点突变技术对蛋白质进行序列分析,突变株和亲本株的感染性克隆转染到PK-15细胞中后,通过间接免荧光技术计算了PCV2阳性细胞数目,并在
会议