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神经营养因子受体TrkA和TrkB在神经母细胞瘤中的预后及生物学作用

Prognostic and biological role of neurotrophin-receptor TrkA and TrkB in neuroblastoma.

作者信息

Eggert A, Ikegaki N, Liu X G, Brodeur G M

机构信息

Children's Hospital of Philadelphia/Department of Pediatrics, University of Pennsylvania 19104, USA.

出版信息

Klin Padiatr. 2000 Jul-Aug;212(4):200-5. doi: 10.1055/s-2000-9677.

Abstract

Expression of different neurotrophin receptors of the tyrosine kinase (Trk) family plays an important role in the biology and clinical behavior of neuroblastomas (NB). Observations from several independent studies suggest that high expression of TrkA is present in NB with favorable biological features and highly correlated with patient survival, whereas TrkB is mainly expressed on unfavorable, aggressive NB with MYCN-amplification. To determine expression of Trk receptors and ligands in primary NB, we developed a reliable semiquantitative duplex RT-PCR protocol, that requires only 1 microgram RNA per tumor sample. Activation of TrkA by its ligand nerve growth factor (NGF) initiates a cascade of signaling events and promotes neuronal differentiation in vitro. Activation of TrkB by its ligand brain derived neurotrophic factor (BDNF) has been associated with proliferation and survival of NB cells. To study Trk signal transduction pathways and their biological effects in NB, we stably expressed TrkA and TrkB cDNA in the human NB cell line SH-SY5Y. Introduction of TrkA and TrkB restored responsiveness of SH-SY5Y cells to the ligands NGF and BDNF, respectively, and resulted in morphological differentiation. Expression of TrkA resulted in growth inhibition of the transfectants compared to parental cells, whereas TrkB transfectants demonstrated an increased proliferation rate. Further insight into the differences of TrkA and TrkB signaling may suggest new options for the treatment of NB. As expression of TrkA is a strong prognostic factor especially in MYCN non-amplified NB, a prospective study of Trk receptor expression using RT-PCR should be performed for German neuroblastoma patients.

摘要

酪氨酸激酶(Trk)家族不同神经营养因子受体的表达在神经母细胞瘤(NB)的生物学特性和临床行为中起着重要作用。几项独立研究的观察结果表明,TrkA高表达存在于具有良好生物学特征的NB中,且与患者生存率高度相关,而TrkB主要表达于具有MYCN扩增的不良、侵袭性NB中。为了确定原发性NB中Trk受体和配体的表达,我们开发了一种可靠的半定量双重RT-PCR方案,每个肿瘤样本仅需1微克RNA。其配体神经生长因子(NGF)激活TrkA会引发一系列信号事件,并在体外促进神经元分化。其配体脑源性神经营养因子(BDNF)激活TrkB与NB细胞的增殖和存活有关。为了研究NB中Trk信号转导途径及其生物学效应,我们在人NB细胞系SH-SY5Y中稳定表达了TrkA和TrkB cDNA。引入TrkA和TrkB分别恢复了SH-SY5Y细胞对配体NGF和BDNF的反应性,并导致形态分化。与亲本细胞相比,TrkA的表达导致转染细胞生长受到抑制,而TrkB转染细胞显示增殖率增加。对TrkA和TrkB信号差异的进一步深入了解可能为NB的治疗提供新的选择。由于TrkA的表达是一个强有力的预后因素,尤其是在MYCN未扩增的NB中,因此应对德国神经母细胞瘤患者进行使用RT-PCR的Trk受体表达的前瞻性研究。

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