Liu Ying, Bunston Carly, Hodson Nicholas, Resaul Jeyna, Sun Ping-Hui, Cai Shuo, Chen Gang, Gu Yanan, Satherley Lucy K, Bosanquet David C, Al-Sarireh Bilal, Tian Xiuyun, Hao Chunyi, Jiang Wen G, Ye Lin
Metastasis and Angiogenesis Research Group, Cardiff China Medical Research Collaborative, Division of Cancer and Genetics, Cardiff University School of Medicine, Cardiff, CF14 4XN, UK.
Department of Surgery, Morriston Hospital, ABM University Health Board, Swansea, SA6 6NL, UK.
Int J Oncol. 2017 May;50(5):1491-1500. doi: 10.3892/ijo.2017.3953. Epub 2017 Apr 5.
Psoriasin (S100A7) is an 11-kDa small calcium binding protein initially isolated from psoriatic skin lesions. It belongs to the S100 family of proteins which play an important role in a range of cell functions including proliferation, differentiation, migration and apoptosis. Aberrant Psoriasin expression has been implicated in a range of cancers and is often associated with poor prognosis. This study examined the role of Psoriasin on pancreatic cancer cell functions and the implication in progression of the disease. Expression of Psoriasin was determined in a cohort of pancreatic tissues comprised of 126 pancreatic tumours and 114 adjacent non-tumour pancreatic tissues. Knockdown and overexpression of Psoriasin in pancreatic cancer cells was performed using specifically constructed plasmids, which either had anti-Psoriasin ribozyme transgene or the full length human Psoriasin coding sequence. Psoriasin knockdown and overexpression was verified using conventional RT-PCR and qPCR. The effect of manipulating Psoriasin expression on pancreatic cancer cell functions was assessed using several in vitro cell function assays. Local invasive pancreatic cancers extended beyond the pancreas expressed higher levels of Psoriasin transcripts compared with the cancers confined to the pancreas. Primary tumours with distant metastases exhibited a reduced expression of Psoriasin. Psoriasin overexpression cell lines exhibited significantly increased growth and migration compared to control cells. In addition, Psoriasin overexpression resulted in increased pancreatic cancer cell invasion which was associated with upregulation of matrix metalloproteinase-2 (MMP-2) and MMP-9. Overexpression of Psoriasin also promoted aggregation and survival of pancreatic cancer cells when they lost anchorage. Taken together, higher expression of Psoriasin was associated with local invasion in pancreatic cancers. Psoriasin expression is associated with pancreatic cancer cell growth, migration, cell-matrix adhesion, and invasion via regulation of MMPs. As such, the proposed implications of Psoriasin in invasion, disease progression and as a potential therapeutic target warrant further investigation.
银屑素(S100A7)是一种11千道尔顿的小钙结合蛋白,最初从银屑病皮肤病变中分离出来。它属于S100蛋白家族,该家族在包括增殖、分化、迁移和凋亡在内的一系列细胞功能中发挥重要作用。银屑素的异常表达与多种癌症有关,并且常与预后不良相关。本研究探讨了银屑素在胰腺癌细胞功能中的作用及其在疾病进展中的意义。在一组由126个胰腺肿瘤和114个相邻非肿瘤胰腺组织组成的胰腺组织中测定了银屑素的表达。使用特异性构建的质粒在胰腺癌细胞中进行银屑素的敲低和过表达,这些质粒要么含有抗银屑素核酶转基因,要么含有全长人银屑素编码序列。使用常规RT-PCR和qPCR验证银屑素的敲低和过表达。使用几种体外细胞功能测定法评估操纵银屑素表达对胰腺癌细胞功能的影响。与局限于胰腺的癌症相比,超出胰腺的局部浸润性胰腺癌表达更高水平的银屑素转录本。有远处转移的原发性肿瘤银屑素表达降低。与对照细胞相比,银屑素过表达细胞系的生长和迁移显著增加。此外,银屑素过表达导致胰腺癌细胞侵袭增加,这与基质金属蛋白酶-2(MMP-2)和MMP-9的上调有关。银屑素的过表达还促进了胰腺癌细胞在失去锚定后的聚集和存活。综上所述,银屑素的高表达与胰腺癌的局部浸润有关。银屑素表达与胰腺癌细胞的生长、迁移、细胞-基质粘附以及通过调节基质金属蛋白酶的侵袭有关。因此,银屑素在侵袭、疾病进展中的潜在意义以及作为潜在治疗靶点值得进一步研究。
Zotero 插件
