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N-ras蛋白:在人类结直肠癌中经常出现数量和质量上的变化。

N-ras protein: frequent quantitative and qualitative changes occur in human colorectal carcinomas.

作者信息

Kim K, Kuo T, Cai J, Shuja S, Murnane M J

机构信息

Department of Pathology and Laboratory Medicine, Boston University School of Medicine, MA 02118, USA.

出版信息

Int J Cancer. 1997 May 29;71(5):767-75. doi: 10.1002/(sici)1097-0215(19970529)71:5<767::aid-ijc13>3.0.co;2-5.

Abstract

Point mutation and overexpression are recognized mechanisms for ras activation in malignancy. However, little information is available on overexpression of N-ras protein compared with H- or K-ras proteins, as N-ras-specific antibodies have only recently become available. For comparative analyses of ras protein levels, we have probed Western blots of extracts from 9 normal human tissues and 55 pairs of colorectal carcinoma and matched control mucosa, using monoclonal antibodies (MAbs) specific for H-, K- or N-ras proteins. On multi-tissue blots, N-ras protein was more highly expressed in colon than in the other human tissues analyzed, suggesting a role for N-ras in colorectal function. N-ras protein levels in multiple independent extracts of normal colon mucosa were consistently higher than either K-ras protein or H-ras protein levels. In 69% of colon carcinomas, N-ras protein levels were increased an average of 4.8-fold over normal mucosa. Overexpression of K-ras protein was also observed in colon cancers but less frequently (13% of cases) than N-ras protein. H-ras protein levels were too low for comparative studies. Alterations in N-ras protein mobility, possibly reflecting increased post-translational processing, were also detected in 42% of colon carcinomas. N-ras protein, typically present as a single 23 kDa band in normal mucosa, was expressed in some cancers as a 22 kDa band or as multiple bands of 20-23 kDa. Sequencing of N-ras DNA from 6 carcinomas with these variations in protein mobility did not reveal mutations in codons 12, 13, 59 or 61. Thus, frequent quantitative and qualitative changes in N-ras protein expression, which do not appear to correlate with the presence of typical N-ras point mutations, result in abnormal N-ras protein patterns in human colorectal carcinomas.

摘要

点突变和过表达是恶性肿瘤中Ras激活的公认机制。然而,与H-Ras或K-Ras蛋白相比,关于N-Ras蛋白过表达的信息较少,因为N-Ras特异性抗体直到最近才出现。为了对Ras蛋白水平进行比较分析,我们使用了针对H-Ras、K-Ras或N-Ras蛋白的单克隆抗体(MAb),对9种正常人体组织以及55对结直肠癌组织和配对的对照黏膜提取物进行了蛋白质印迹检测。在多组织印迹中,N-Ras蛋白在结肠中的表达高于所分析的其他人体组织,提示N-Ras在结肠功能中发挥作用。正常结肠黏膜多个独立提取物中的N-Ras蛋白水平始终高于K-Ras蛋白或H-Ras蛋白水平。在69%的结肠癌中,N-Ras蛋白水平比正常黏膜平均升高了4.8倍。在结肠癌中也观察到了K-Ras蛋白的过表达,但频率低于N-Ras蛋白(13%的病例)。H-Ras蛋白水平过低,无法进行比较研究。在42%的结肠癌中还检测到了N-Ras蛋白迁移率的改变,这可能反映了翻译后加工的增加。N-Ras蛋白在正常黏膜中通常表现为单一的23 kDa条带,在一些癌症中则表现为22 kDa条带或20 - 23 kDa的多条带。对6例具有这些蛋白迁移率变化的癌组织进行N-Ras DNA测序,未发现密码子12、13、59或61的突变。因此,N-Ras蛋白表达频繁的定量和定性变化似乎与典型的N-Ras点突变无关,导致了人类结直肠癌中N-Ras蛋白模式异常。

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