Wnt配体和卷曲受体在结肠黏膜及结肠癌中的表达
Expression of Wnt ligands and Frizzled receptors in colonic mucosa and in colon carcinoma.
作者信息
Holcombe R F, Marsh J L, Waterman M L, Lin F, Milovanovic T, Truong T
机构信息
Division of Hematology/Oncology and the Chao Family Comprehensive Cancer Center, University of California, Irvine Medical Center, 101 The City Drive, Building 23, Orange, CA 92868, USA.
出版信息
Mol Pathol. 2002 Aug;55(4):220-6. doi: 10.1136/mp.55.4.220.
AIMS
Signalling through the Wnt pathway is integrally associated with colon carcinogenesis. Although activating mutations in the genes for adenomatous polyposis coli (APC) and beta-catenin are clearly associated with colon cancer, less is understood about the role of the upstream secreted ligands (Wnts) and their receptors (frizzled, Fz) in this process. In other systems, increased Wnt signalling has been shown to alter the expression of components of this pathway. This study was designed to test the hypothesis that colon cancer is characterised by aberrant expression of specific Wnt genes and Fz receptors.
METHODS
The expression of Wnt genes was assessed by in situ, antisense RNA hybridisation in paraffin wax embedded samples of normal and malignant human colon tissues with probes specific for the individual Wnt genes. The expression of Fz1 and Fz2 was determined by immunoperoxidase based antibody staining on human tissues.
RESULTS
Changes in the expression of some ligands and receptors were seen in colon cancer. For example, Wnt2 mRNA was detected in colon cancer but was undetectable in normal colonic mucosa. Differential expression of Wnt5a in normal mucosa was also noted, with increased expression at the base of the crypts compared with the luminal villi and slightly increased expression in colon cancer. Wnt7a exhibited minimal expression in both normal and malignant colon tissues, whereas other Wnt ligands including Wnts 1, 4, 5b, 6, 7b, and 10b were expressed equally and strongly in both normal and malignant colon tissues. In defining cellular responses and phenotype, the type and distribution of Fz receptors may be as important as the pattern of Wnt ligand expression. No expression of Fz receptor 1 and 2 was seen in normal colonic mucosa and in well differentiated tumours. However, poorly differentiated tumours exhibited a high degree of Fz receptor expression, especially at the margin of cellular invasion.
CONCLUSIONS
These data indicate that the expression of members of the Wnt signal transduction pathway, distinct from APC and beta-catenin, is integrally associated with the process of colon carcinogenesis. Wnt2, and possibly Wnt5a, may be involved in the progression from normal mucosa to cancer and the expression of Fz1/2 receptors may be involved in processes associated with tumour invasion. Altered expression of these Wnts and Fz receptors may prove useful as prognostic or diagnostic markers for patients with colon cancer.
目的
通过Wnt信号通路进行的信号传导与结肠癌发生密切相关。虽然腺瘤性息肉病 coli(APC)和β-连环蛋白基因的激活突变与结肠癌明显相关,但对于上游分泌配体(Wnts)及其受体(卷曲蛋白,Fz)在这一过程中的作用了解较少。在其他系统中,已显示Wnt信号增加会改变该信号通路成分的表达。本研究旨在验证结肠癌的特征是特定Wnt基因和Fz受体表达异常这一假设。
方法
通过原位反义RNA杂交,使用针对各个Wnt基因的特异性探针,对正常和恶性人类结肠组织的石蜡包埋样本进行Wnt基因表达评估。通过基于免疫过氧化物酶的抗体染色检测人组织中Fz1和Fz2的表达。
结果
在结肠癌中观察到一些配体和受体表达的变化。例如,在结肠癌中检测到Wnt2 mRNA,但在正常结肠黏膜中未检测到。还注意到Wnt5a在正常黏膜中的差异表达,与管腔绒毛相比,隐窝底部表达增加,在结肠癌中略有增加。Wnt7a在正常和恶性结肠组织中均表现出极低表达,而其他Wnt配体,包括Wnts 1、4、5b、6、7b和10b在正常和恶性结肠组织中表达均一且强烈。在确定细胞反应和表型方面,Fz受体的类型和分布可能与Wnt配体表达模式同样重要。在正常结肠黏膜和高分化肿瘤中未观察到Fz受体1和2的表达。然而,低分化肿瘤表现出高度的Fz受体表达,尤其是在细胞侵袭边缘。
结论
这些数据表明,与APC和β-连环蛋白不同,Wnt信号转导通路成员的表达与结肠癌发生过程密切相关。Wnt2以及可能的Wnt5a可能参与从正常黏膜到癌症的进展,Fz1/2受体的表达可能参与与肿瘤侵袭相关的过程。这些Wnts和Fz受体的表达改变可能被证明是结肠癌患者有用的预后或诊断标志物。
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