TRK基因高表达与人类神经母细胞瘤良好预后之间的关联。

Association between high levels of expression of the TRK gene and favorable outcome in human neuroblastoma.

作者信息

Nakagawara A, Arima-Nakagawara M, Scavarda N J, Azar C G, Cantor A B, Brodeur G M

机构信息

Department of Pediatrics, Washington University School of Medicine, St. Louis, MO 63110.

出版信息

N Engl J Med. 1993 Mar 25;328(12):847-54. doi: 10.1056/NEJM199303253281205.

DOI:10.1056/NEJM199303253281205

PMID:8441429

Abstract

BACKGROUND AND METHODS

The nerve growth factor receptor is expressed in some neuroblastomas, in which its primary component is encoded by the TRK protooncogene. To determine the relation of the expression of TRK messenger RNA in neuroblastomas to other clinical and laboratory variables, we studied frozen tumor samples from 77 patients. In addition, we tested two primary neuroblastomas that expressed TRK for responsiveness to nerve growth factor.

RESULTS

TRK expression strongly correlated with favorable tumor stage (I, II, and IVS vs. III and IV), younger age (< 1 year vs. > or = 1 year), normal N-myc copy number, and low level of N-myc expression. N-myc amplification (indicated by a high copy number) correlated with advanced tumor stage, older age, an adrenal site of the primary tumor, low level of expression of TRK, and high level of expression of N-myc. Analysis of five-year cumulative-survival rates demonstrated an association of a very favorable outcome with a high level of TRK expression (86 percent vs. 14 percent) and with normal N-myc copy number (84 percent vs. 0 percent). Univariate analysis showed that these two variables were the most powerful predictors of outcome (chi-square = 51.30, P < 0.001; and chi-square = 93.61, P < 0.001, respectively). TRK expression still had significant prognostic value when the analysis was restricted to tumors without N-myc amplification. In primary cultures of neuroblastoma cells expressing TRK, exposure to nerve growth factor induced early gene expression and neurite outgrowth, but deprivation of nerve growth factor led to neuronal cell death.

CONCLUSIONS

A high level of expression of the TRK proto-oncogene in a neuroblastoma is strongly predictive of a favorable outcome. A tumor with a functional nerve growth factor receptor may be dependent on the neurotrophin nerve growth factor for survival and may regress in its absence, allowing a new approach to the treatment of certain patients with neuroblastoma.

摘要

背景与方法

神经生长因子受体在某些神经母细胞瘤中表达，其主要成分由TRK原癌基因编码。为了确定神经母细胞瘤中TRK信使核糖核酸（mRNA）的表达与其他临床和实验室变量之间的关系，我们研究了77例患者的冷冻肿瘤样本。此外，我们检测了两个表达TRK的原发性神经母细胞瘤对神经生长因子的反应性。

结果

TRK表达与良好的肿瘤分期（I、II和IVS期与III和IV期相比）、较年轻的年龄（<1岁与≥1岁相比）、正常的N - myc拷贝数以及低水平的N - myc表达密切相关。N - myc扩增（以高拷贝数表示）与晚期肿瘤分期、较年长的年龄、原发性肿瘤的肾上腺部位、低水平的TRK表达以及高水平的N - myc表达相关。对五年累积生存率的分析表明，高水平的TRK表达（86%对14%）和正常的N - myc拷贝数（84%对0%）与非常良好的预后相关。单因素分析显示，这两个变量是预后的最有力预测因素（卡方值分别为51.30，P<0.001；和卡方值为93.61，P<0.001）。当分析仅限于无N - myc扩增的肿瘤时，TRK表达仍具有显著的预后价值。在表达TRK的神经母细胞瘤细胞的原代培养中，暴露于神经生长因子可诱导早期基因表达和神经突生长，但去除神经生长因子会导致神经元细胞死亡。