侵袭性神经母细胞瘤中缺乏高亲和力神经生长因子受体。

Lack of high-affinity nerve growth factor receptors in aggressive neuroblastomas.

作者信息

Suzuki T, Bogenmann E, Shimada H, Stram D, Seeger R C

机构信息

Department of Pediatrics, Childrens Hospital Los Angeles, University of Southern California School of Medicine 90054-0700.

出版信息

J Natl Cancer Inst. 1993 Mar 3;85(5):377-84. doi: 10.1093/jnci/85.5.377.

DOI:10.1093/jnci/85.5.377

PMID:8433391

Abstract

BACKGROUND

Neuroblastoma is a malignancy of the sympathetic nervous system. Nerve growth factor, which has a major role in development of the sympathetic nervous system, has high-affinity (gp140TRK-A) and low-affinity (gp75NGFR) cell-surface receptors. We recently reported preliminary study results showing a lack of gp140TRK-A receptors and rapid disease progression in neuroblastomas, particularly those with amplification of the N-myc (also known as MYCN) proto-oncogene.

PURPOSE

This retrospective study was designed to determine if expression of nerve growth factor receptor messenger RNA (mRNA) was associated with biologic and clinical parameters and with survival in neuroblastoma.

METHODS

We obtained 80 untreated primary neuroblastomas that had been snap-frozen and stored after surgical excision. To determine expression of gp140TRK-A and gp75NGFR, we performed Northern blot analyses on total RNA from the specimens. Samples from the same specimens were examined for N-myc proto-oncogene amplification, RNA expression, and histologic differentiation, and clinical stage at diagnosis and survival were determined.

RESULTS

Of the 80 neuroblastomas, 65 (81%) expressed gp140TRK-A RNA. However, three (27%) of the 11 tumors with genomic amplification and high expression of N-myc RNA and 62 (90%) of the 69 without genomic amplification or detectable N-myc RNA expressed gp140TRK-A mRNA. The inverse relationship between gp140TRK-A mRNA and N-myc expression had high statistical significance (P < .0001). Of the 67 tumors assessable for histologic differentiation, the 13 lacking gp140TRK-A mRNA were histologically undifferentiated, whereas 19 (35%) of the 54 expressing it were differentiated (P = .041). Only 10 (53%) of the 19 metastatic (stage IV) tumors expressed gp140TRK-A mRNA, compared with 90% for other stages (P = .0003). Survival 2 years after diagnosis was 92%, 78%, and 14% for patients whose tumors expressed high, intermediate, and no gp140TRK-A mRNA, respectively (P < .0001). Univariate and multivariate analyses demonstrated that N-myc and gp140TRK-A expression of mRNA and clinical staging were independent predictors of survival. Expression of gp75NGFR mRNA did not correlate with gp140TRK-A mRNA expression, histologic differentiation, stage, or survival.

CONCLUSIONS

The expression of gp140TRK-A mRNA correlates with distinct biologic and clinical subsets of neuroblastoma, which suggests a role for the high-affinity nerve growth factor receptors in determining the phenotype of neuroblastoma. The absence of gp140TRK-A mRNA expression, whether or not the N-myc proto-oncogene is amplified, is associated with tumor progression.

摘要

背景

神经母细胞瘤是一种交感神经系统的恶性肿瘤。神经生长因子在交感神经系统发育中起主要作用，具有高亲和力（gp140TRK - A）和低亲和力（gp75NGFR）细胞表面受体。我们最近报告的初步研究结果显示，神经母细胞瘤中缺乏gp140TRK - A受体且疾病进展迅速，尤其是那些N - myc（也称为MYCN）原癌基因扩增的肿瘤。

目的

本回顾性研究旨在确定神经生长因子受体信使核糖核酸（mRNA）的表达是否与神经母细胞瘤的生物学和临床参数以及生存相关。

方法

我们获取了80例未经治疗的原发性神经母细胞瘤，这些肿瘤在手术切除后立即速冻并保存。为了确定gp140TRK - A和gp75NGFR的表达，我们对标本的总RNA进行了Northern印迹分析。对同一标本的样本进行N - myc原癌基因扩增、RNA表达和组织学分化检测，并确定诊断时的临床分期和生存情况。

结果

在80例神经母细胞瘤中，65例（81%）表达gp140TRK - A RNA。然而，在11例基因组扩增且N - myc RNA高表达的肿瘤中，有3例（27%）表达gp140TRK - A mRNA，而在69例无基因组扩增或未检测到N - myc RNA的肿瘤中，有62例（90%）表达gp140TRK - A mRNA。gp140TRK - A mRNA与N - myc表达之间的负相关具有高度统计学意义（P <.0001）。在67例可评估组织学分化的肿瘤中，13例缺乏gp140TRK - A mRNA的肿瘤在组织学上未分化，而在54例表达该mRNA的肿瘤中有19例（35%）分化（P =.041）。19例转移性（IV期）肿瘤中只有10例（53%）表达gp140TRK - A mRNA，而其他分期的表达率为90%（P =.0003）。诊断后2年的生存率分别为：肿瘤表达高、中、无gp140TRK - A mRNA的患者，生存率分别为92%、78%和14%（P <.0001）。单因素和多因素分析表明，N - myc和gp140TRK - A mRNA的表达以及临床分期是生存的独立预测因素。gp75NGFR mRNA的表达与gp140TRK - A mRNA表达、组织学分化、分期或生存均无相关性。