Kumar-Singh S, Segers K, Rodeck U, Backhovens H, Bogers J, Weyler J, Van Broeckhoven C, Van Marck E
Department of Pathology, University of Antwerp (UIA), Belgium.
J Pathol. 1997 Jan;181(1):67-74. doi: 10.1002/(SICI)1096-9896(199701)181:1<67::AID-PATH723>3.0.CO;2-Z.
The Wilms tumour 1 (WT1) gene is believed to contribute to the growth and differentiation of certain tissues, including mesothelium. This study assessed WT1 gene status by mutational screening in 42 malignant mesotheliomas (MMs) and 3 MM cell lines and detected two tumours with identical heterozygous single nucleotide deletions in intron 7, with no apparent consequence for WT1 function. Furthermore, the expression pattern of the WT1 gene was studied in MMs and related lesions using three anti-WT1 monoclonal antibodies (MAbs). Strong to moderate nuclear immunoreactivity was noted in MM in situ (54/56), cultured mesothelioma cells (4/5), and hyperplastic and normal pleural (non-neoplastic, NNM) specimens. WT1 immunoreactivity was absent in all primary tumours of lung and in pleural metastases from adenocarcinomas of breast and colon; immunoreactivity was present in pleural metastases from renal carcinomas, melanomas, and papillary carcinomas of the ovary. Expression of the WT1 protein in MM was not correlated with survival. Coordinate expression of the WT1 protein and its putative transcriptional target genes was determined by correlating WT1 immunostaining with epidermal growth factor receptor (EGF-R) and insulin-like growth factor 1 receptor (IGF-1R) expression on MM and NNM; no significant correlation was found, irrespective of p53 expression status. Finally, the putative involvement of WT1 in cell-type transition was supported by this study, in that epithelial mesothelioma showed the strongest WT1 immunoreactivity while sarcomatous mesothelioma showed the least.
肾母细胞瘤1(WT1)基因被认为有助于某些组织的生长和分化,包括间皮。本研究通过对42例恶性间皮瘤(MM)和3种MM细胞系进行突变筛查来评估WT1基因状态,检测到2例肿瘤在内含子7中有相同的杂合单核苷酸缺失,对WT1功能无明显影响。此外,使用三种抗WT1单克隆抗体(MAb)研究了MM及相关病变中WT1基因的表达模式。在MM原位(54/56)、培养的间皮瘤细胞(4/5)以及增生性和正常胸膜(非肿瘤性,NNM)标本中均观察到强至中度的核免疫反应性。在所有原发性肺癌以及乳腺癌和结肠癌的胸膜转移瘤中均未检测到WT1免疫反应性;在肾癌、黑色素瘤和卵巢乳头状癌的胸膜转移瘤中存在免疫反应性。MM中WT1蛋白的表达与生存率无关。通过将WT1免疫染色与MM和NNM上的表皮生长因子受体(EGF-R)和胰岛素样生长因子1受体(IGF-1R)表达相关联,确定了WT1蛋白及其推定的转录靶基因的协同表达;无论p53表达状态如何,均未发现显著相关性。最后,本研究支持了WT1在细胞类型转变中的推定作用,即上皮性间皮瘤显示出最强的WT1免疫反应性,而肉瘤样间皮瘤显示出最弱的免疫反应性。