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Clusterin expression in normal mucosa and colorectal cancer.

机译:Clusterin在正常黏膜和结直肠癌中的表达。

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The gene Clusterin is a target for cancer therapy in clinical trials. The indication for intervention is up-regulated Clusterin expression. Clusterin has been reported to be deregulated in multiple cancer types, including colorectal cancer (CRC). However, for CRC the studies have disagreed on whether Clusterin is up- or down-regulated by neoplastic cells. In the present study we sought to clarify the expression and distribution of Clusterin mRNAs and proteins in normal and neoplastic colorectal tissue through laser microdissection, variant-specific real time RT-PCR, immunohistochemistry, immunofluorescence, Western blotting, and array-based transcriptional profiling. At the transcript level we demonstrated the expression of two novel Clusterin transcripts in addition to the known transcript, and at the protein level we demonstrated two Clusterin isoforms. Our analysis of normal epithelial cells revealed that among these, Clusterin was only expressed by rare neuroendocrine subtype. Furthermore our analysis showed that in the normal mucosa the majority of the observed Clusterin protein originated from the stromal compartment. In tumors we found that Clusterin was de novo synthesized by non-neuroendocrine cancer cells in approximately 25% of cases. Moreover we found that the overall Clusterin level in tumors often appeared to be lower than in normal mucosa due to the stromal compartment often being suppressed in tumors. Although Clusterin in normal neuroendocrine cells showed a basal localization, the localization in cancer cells was often apical and in some cases associated with apical secretion. Collectively our results indicate that Clusterin expression is very complex. We conclude that Clusterin expression is associated with neuroendocrine differentiation in normal epithelia and that the Clusterin observed in neoplastic cells is de novo synthesized. The cases with de novo synthesized Clusterin define a distinct subgroup of CRC that may be of clinical importance as anti-Clusterin therapeutics are now in clinical trials.
机译:Clusterin基因是临床试验中癌症治疗的靶标。干预的指标是Clusterin表达上调。据报道,簇蛋白在包括结直肠癌(CRC)在内的多种癌症类型中被解除调节。然而,对于CRC,关于簇状蛋白是由肿瘤细胞上调还是下调的研究,其研究结果并不相同。在本研究中,我们试图通过激光显微切割,变体特异性实时R​​T-PCR,免疫组织化学,免疫荧光,蛋白质印迹和基于阵列的转录谱来阐明Clusterin mRNA和蛋白在正常和赘生性结直肠组织中的表达和分布。在转录本水平上,我们证明了除已知转录本外还有两种新型Clusterin转录本的表达,在蛋白质水平上,我们证实了两种Clusterin同工型。我们对正常上皮细胞的分析表明,在这些细胞中,簇蛋白仅由罕见的神经内分泌亚型表达。此外,我们的分析表明,在正常的粘膜中,观察到的大多数Clusterin蛋白起源于基质区室。在肿瘤中,我们发现,大约25%的病例是非神经内分泌癌细胞从头合成了Clusterin。此外,我们发现肿瘤中的总体簇蛋白水平通常似乎低于正常粘膜,这是由于基质区室通常在肿瘤中被抑制。尽管簇蛋白在正常神经内分泌细胞中显示出基础定位,但癌细胞中的定位通常是顶端的,在某些情况下与顶端的分泌有关。总体而言,我们的结果表明Clusterin表达非常复杂。我们得出结论,Clusterin表达与正常上皮细胞的神经内分泌分化有关,并且在新生细胞中观察到的Clusterin是从头合成的。从头合成Clusterin的病例定义了一个明显的CRC亚组,由于抗Clusterin治疗药物目前正在临床试验中,因此可能具有重要的临床意义。

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