Wu Xiangru, Dagar Vinod, Algar Elizabeth, Muscat Andrea, Bandopadhayay Pratiti, Ashley David, Wo Chow Chung
Department of Anatomical Pathology, Royal Children's Hospital, Flemington Road, Parkville, Vic 3052, Australia.
Pathology. 2008 Dec;40(7):664-70. doi: 10.1080/00313020802436451.
To correlate the immunostaining for INI1 protein and mutations in INI1 gene in possible rhabdoid tumours (RT) and atypical teratoid/rhabdoid tumours (AT/RT) seen at the Royal Children's Hospital in the last 10 years, and to study the clinicopathological features of those patients with negative nuclear staining.
Twenty tumours showing suggestive histological and/or immunohistochemical features of RT and AT/RT were selected. Immunohistochemistry for INI1 and molecular investigations for INI1 mutations were performed. The clinical features, histology and immunohistochemistry in those patients with negative nuclear staining were studied.
In seven tumours the nuclei stained uniformly for INI1. In none of these was an INI1 mutation detected. In 13 tumours nuclei showed no staining. In only ten of these was material available for molecular studies. Mutations were detected in nine. In these 13 patients, the primary tumour was in the central nervous system (CNS) in seven, in the soft tissue in three, in the liver in two and in the kidney in one. The age of presentation varied from 19 days to 7 years. Only five tumours showed large areas of rhabdoid cells. Most showed extensive non-diagnostic areas. In two an alternative diagnosis, ependymoma or myoepithelial carcinoma of soft tissue, was initially suggested. All the CNS tumours were positive for EMA, GFAP, and SMA. There were no long term survivors, but an occasional patient showed excellent response to intensive chemotherapy.
In this small series, there is a strong correlation between the loss of INI1 immunostaining and the presence of an INI1 mutation suggesting that the former is a reliable marker for RT and AT/RT in children. As relatively few tumours showed uniform populations of rhabdoid cells, and some showed features suggesting another diagnosis, INI1 staining should be checked in all high grade CNS tumours and malignant extraCNS tumours where the diagnosis is unclear. The prognosis of RT is poor but medium term remission can be achieved in some patients with aggressive treatment.
将过去10年在皇家儿童医院所见的可能的横纹肌样瘤(RT)和非典型畸胎样/横纹肌样瘤(AT/RT)中INI1蛋白免疫染色与INI1基因突变进行关联,并研究核染色阴性患者的临床病理特征。
选取20例显示RT和AT/RT提示性组织学和/或免疫组化特征的肿瘤。进行INI1免疫组化及INI1基因突变的分子研究。研究核染色阴性患者的临床特征、组织学及免疫组化情况。
7例肿瘤INI1核染色均匀。这些肿瘤均未检测到INI1突变。13例肿瘤核无染色。其中仅10例有材料可用于分子研究。9例检测到突变。在这13例患者中,原发肿瘤位于中枢神经系统(CNS)7例,软组织3例,肝脏2例,肾脏1例。发病年龄从19天至7岁不等。仅5例肿瘤有大片横纹肌样细胞。多数显示广泛的非诊断性区域。2例最初提示为其他诊断,即室管膜瘤或软组织肌上皮癌。所有CNS肿瘤EMA、GFAP和SMA均为阳性。无长期存活者,但偶尔有患者对强化化疗反应良好。
在这个小系列研究中,INI1免疫染色缺失与INI1突变存在之间有很强的相关性,提示前者是儿童RT和AT/RT的可靠标志物。由于相对较少的肿瘤显示均匀的横纹肌样细胞群体,且有些显示提示其他诊断的特征,对于所有诊断不明确的高级别CNS肿瘤和恶性CNS外肿瘤均应检查INI1染色。RT预后较差,但部分积极治疗的患者可实现中期缓解。
Zotero 插件