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结直肠癌中癌胚抗原组成员CGM2、CD66a(胆汁糖蛋白)和非特异性交叉反应抗原的失调。Northern印迹法和原位杂交的比较分析。

Dysregulation of carcinoembryonic antigen group members CGM2, CD66a (biliary glycoprotein), and nonspecific cross-reacting antigen in colorectal carcinomas. Comparative analysis by northern blot and in situ hybridization.

作者信息

Nollau P, Prall F, Helmchen U, Wagener C, Neumaier M

机构信息

Abteilung für Klinische Chemie, Universitätskrankenhaus Eppendorf, Hamburg, Germany.

出版信息

Am J Pathol. 1997 Aug;151(2):521-30.

Abstract

Genes coding for CD66a (biliary glycoprotein), carcinoembryonic antigen (CEA) group member 2 (CGM2), and nonspecific cross-reacting antigen (NCA) are members of the human CEA gene subgroup. We investigated a series of 11 colorectal carcinomas by Northern blot and isotopic in situ hybridization (ISH), demonstrating underexpression of CD66a and CGM2 in the majority of the carcinomas as compared with the normal mucosa, whereas NCA was overexpressed. ISH for CD66a and CGM2 mRNA revealed that large areas of the carcinomas remained without or with only faint hybridization signals. However, in every carcinoma, at least some positive foci were observed, indicating remaining cell populations that actively transcribe CD66a and CGM2. In contrast, ISH for NCA displayed strong and extensive autoradiographic signals. By analysis of step sections, foci of CD66a and CGM2 expression were shown to co-localize. Furthermore, these foci contained relatively few nuclei immunohistochemically positive for the proliferation-associated nuclear antigen Ki-67. Our data indicate a dysregulation of the three genes possibly with a common transcriptional control for CD66a and CGM2 and a different control for NCA. The focal expression of CD66a and CGM2 could be interpreted as due to a focal, incomplete, and abortive differentiation or, alternatively, as a consequence of genetic heterogeneity with foci of slow-proliferating subclones.

摘要

编码CD66a(胆汁糖蛋白)、癌胚抗原(CEA)组成员2(CGM2)和非特异性交叉反应抗原(NCA)的基因是人类CEA基因亚组的成员。我们通过Northern印迹法和同位素原位杂交(ISH)研究了11例结直肠癌,结果显示与正常黏膜相比,大多数癌组织中CD66a和CGM2表达下调,而NCA过表达。CD66a和CGM2 mRNA的ISH显示,癌组织的大片区域没有杂交信号或只有微弱的杂交信号。然而,在每例癌组织中,至少观察到一些阳性灶,表明仍有活跃转录CD66a和CGM2的细胞群体。相比之下,NCA的ISH显示出强烈而广泛的放射自显影信号。通过连续切片分析,CD66a和CGM2表达灶显示共定位。此外,这些灶中增殖相关核抗原Ki-67免疫组化阳性的细胞核相对较少。我们的数据表明这三个基因存在失调,可能对CD66a和CGM2有共同的转录调控,而对NCA有不同的调控。CD66a和CGM2的灶性表达可解释为由于局灶性、不完全和夭折的分化,或者是由于具有缓慢增殖亚克隆灶的遗传异质性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/38e5/1857996/7bccf18534d0/amjpathol00020-0206-a.jpg

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