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携带血小板衍生生长因子受体A(PDGFRA)第14外显子突变的胃肠道间质瘤(GISTs)是具有上皮样形态的临床预后良好的胃肿瘤子集。

GISTs with PDGFRA exon 14 mutations represent subset of clinically favorable gastric tumors with epithelioid morphology.

作者信息

Lasota Jerzy, Stachura Jerzy, Miettinen Markku

机构信息

Department of Soft Tissue Pathology, Armed Forces Institute of Pathology, Washington, DC 20306-6000, USA.

出版信息

Lab Invest. 2006 Jan;86(1):94-100. doi: 10.1038/labinvest.3700360.

Abstract

Gastrointestinal stromal tumors (GISTs) are common mesenchymal tumors of the gastrointestinal tract. Activating KIT or PDGFRA (platelet-derived growth factor receptor alpha) mutations have been shown to be a major force in GIST pathogenesis. Recently, a previously undescribed N659K PDGFRA exon 14 mutation has been reported in GISTs. The purpose of this study was to evaluate the frequency of GISTs with PDGFRA exon 14 mutations and define the clinicopathologic profile of such tumors. In all, 200 GISTs negative for mutations in KIT exons 9, 11, 13 and 17 and PDGFRA exons 12 and 18 were evaluated for PDGFRA exon 14 mutations by PCR amplification and direct sequencing. Mutations were found in 11 of 119 (9%) gastric GISTs. None of the 81 GISTs from other than gastric location had such a PDGFRA mutation. A majority of these mutations (eight cases) represented simple 2125C>A or C>G missense mutations, leading to substitution of the lysine for asparagine (N659K). However, in two cases, 2123A>T missense mutations leading to substitution of the tyrosine for asparagine (N659Y) was found instead. Of 11 PDGFRA N659-mutant GISTs, 10 had pure epithelioid morphology. One tumor had mixed, predominantly spindle and focally epithelioid cell morphology. Frequency of PDGFRA N659-mutant GISTs among pure epithelioid GISTs was almost 19%. Immunohistochemically, the majority (64%) of these tumors lacked KIT expression or showed only focal scattered KIT positivity. Tumor size ranged from 2.5 to 16 cm (average 7.1 cm). Low mitotic activity, <or=5 mitoses/50 high power field was detected in six GISTs including larger, >5 cm tumors. Based on mitotic activity and tumor size, six tumors were classified as probably benign with very low malignant potential. Low to moderate malignant potential and high malignant potential was suggested in three and two tumors, respectively. In four cases with moderate or high malignant potential GISTs, a long-term follow-up (average 235.5 months) showed favorable course of disease.

摘要

胃肠道间质瘤(GISTs)是常见的胃肠道间充质肿瘤。已证实激活的KIT或血小板衍生生长因子受体α(PDGFRA)突变是GIST发病机制中的主要因素。最近,在GIST中报道了一种先前未描述的PDGFRA外显子14的N659K突变。本研究的目的是评估具有PDGFRA外显子14突变的GIST的频率,并确定此类肿瘤的临床病理特征。总共对200例KIT外显子9、11、13和17以及PDGFRA外显子12和18无突变的GIST进行了PCR扩增和直接测序,以检测PDGFRA外显子14突变。在119例(9%)胃GIST中,有11例发现突变。81例非胃部位的GIST均未发生这种PDGFRA突变。这些突变中的大多数(8例)表现为简单的2125C>A或C>G错义突变,导致赖氨酸替代天冬酰胺(N659K)。然而,在2例中,发现了导致酪氨酸替代天冬酰胺(N659Y)的2123A>T错义突变。在11例PDGFRA N659突变的GIST中,10例具有纯上皮样形态。1例肿瘤具有混合形态,主要为梭形细胞,局灶性上皮样细胞形态。在纯上皮样GIST中,PDGFRA N659突变的GIST频率近19%。免疫组化显示,这些肿瘤中的大多数(64%)缺乏KIT表达或仅显示局灶性散在的KIT阳性。肿瘤大小为2.5至16 cm(平均7.1 cm)。在6例GIST中检测到低有丝分裂活性,即每50个高倍视野中<或=5个有丝分裂象,包括较大的(>5 cm)肿瘤。根据有丝分裂活性和肿瘤大小,6例肿瘤被分类为可能良性,恶性潜能极低。分别有3例和2例肿瘤提示为低至中度恶性潜能和高恶性潜能。在4例具有中度或高度恶性潜能的GIST病例中,长期随访(平均235.5个月)显示疾病进展良好。

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