Agaram Narasimhan P, Besmer Peter, Wong Grace C, Guo Tianhua, Socci Nicholas D, Maki Robert G, DeSantis Diann, Brennan Murray F, Singer Samuel, DeMatteo Ronald P, Antonescu Cristina R
Department of Pathology, Memorial Sloan-Kettering Cancer Center, New York, NY 10021, USA.
Clin Cancer Res. 2007 Jan 1;13(1):170-81. doi: 10.1158/1078-0432.CCR-06-1508.
Gastrointestinal stromal tumor (GIST) is the most common sarcoma of the intestinal tract. Nearly all tumors express KIT protein, and most have an activating mutation in either KIT or PDGFRA. Therapy with selective tyrosine kinase inhibitors achieves a partial response or stable disease in approximately 80% of patients with advanced GIST. However, after an initial clinical response, some patients develop imatinib resistance. Our goal was to investigate the spectrum of pathologic response and molecular alterations in a group of GIST patients, clinically defined as having imatinib-stable/imatinib-responsive lesions, who underwent surgical resection.
Forty-three tumor nodules from 28 patients were available for pathologic and molecular analysis, which included genotyping for primary and secondary KIT/PDGFRA-mutations, cell cycle alterations, and biochemical activation status of KIT and downstream targets. The transcriptional changes of a subset of these tumors were compared with a group of imatinib-naive GISTs on a U133A Affymetrix expression platform.
The histologic response did not correlate with imatinib therapy duration or with proliferative activity. Second-site KIT mutation was identified in only one tumor nodule. Activation of KIT and downstream targets was consistent in all tumors analyzed. Ultrastructurally, a subset of tumors showed a smooth muscle phenotype, which correlated with overexpression of genes involved in muscle differentiation and function.
The histologic response to imatinib is heterogeneous and does not correlate well with clinical response. Second-site KIT mutations are rare in imatinib-responsive GISTs compared with imatinib-resistant tumors. The gene signature of imatinib-response in GISTs showed alterations of cell cycle control as well as up-regulation of genes involved in muscle differentiation and function.
胃肠道间质瘤(GIST)是肠道最常见的肉瘤。几乎所有肿瘤都表达KIT蛋白,且大多数在KIT或血小板衍生生长因子受体α(PDGFRA)中存在激活突变。选择性酪氨酸激酶抑制剂治疗可使约80%的晚期GIST患者获得部分缓解或病情稳定。然而,在初始临床缓解后,一些患者会出现伊马替尼耐药。我们的目标是研究一组临床上定义为伊马替尼稳定/伊马替尼敏感病变且接受手术切除的GIST患者的病理反应谱和分子改变。
来自28例患者的43个肿瘤结节可用于病理和分子分析,包括原发性和继发性KIT/PDGFRA突变的基因分型、细胞周期改变以及KIT及其下游靶点的生化激活状态。在U133A Affymetrix表达平台上,将这些肿瘤子集的转录变化与一组未接受伊马替尼治疗的GIST进行比较。
组织学反应与伊马替尼治疗持续时间或增殖活性无关。仅在一个肿瘤结节中鉴定出第二位点KIT突变。在所有分析的肿瘤中,KIT及其下游靶点的激活是一致的。超微结构上,一部分肿瘤表现出平滑肌表型,这与参与肌肉分化和功能的基因过表达相关。
对伊马替尼的组织学反应具有异质性,与临床反应相关性不佳。与伊马替尼耐药肿瘤相比,第二位点KIT突变在伊马替尼敏感的GIST中罕见。GIST中伊马替尼反应的基因特征显示细胞周期控制改变以及参与肌肉分化和功能的基因上调。
