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I型生长因子受体:现状与未来研究方向

Type I growth factor receptors: current status and future work.

作者信息

Gullick W J

机构信息

ICRF Oncology Unit, Hammersmith Hospital, London, U.K.

出版信息

Biochem Soc Symp. 1998;63:193-8.

PMID:9513723
Abstract

The type 1 family of growth factor receptors consists of the epidermal growth factor receptor (EGFR), and ErbB-2, ErbB-3 and ErbB-4. Six ligands are known to bind directly to EGFR, none (at present) to ErbB-2, and a family of ligands collectively called the neuregulins bind to both ErbB-3 and ErbB-4. It is now apparent that the receptors function in various heterodimeric pairs, depending on their concentrations, the concentrations of particular ligands in the environment and some intrinsic degree of dimer selectivity. Overexpression of EGFR, ErbB-2 and ErbB-3 has been found commonly in solid human tumours. ErbB-4 has not yet been examined. The EGFR is also activated by various mutations in brain tumours and possibly in other tumour types. These changes appear to be one of the causes of malignant transformation. They may also provide information regarding the course of disease and response to current treatments. Finally, they are targets for a variety of new forms of treatment being developed in the laboratory, in preclinical models and in a few cases in clinical trials.

摘要

1型生长因子受体家族由表皮生长因子受体(EGFR)、ErbB-2、ErbB-3和ErbB-4组成。已知有六种配体可直接与EGFR结合,目前尚无配体与ErbB-2直接结合,而一类统称为神经调节蛋白的配体可与ErbB-3和ErbB-4两者结合。现在很明显,这些受体以各种异源二聚体对的形式发挥作用,这取决于它们的浓度、环境中特定配体的浓度以及某种内在的二聚体选择性程度。在人类实体瘤中普遍发现EGFR、ErbB-2和ErbB-3过表达。尚未对ErbB-4进行检测。EGFR在脑肿瘤以及可能在其他肿瘤类型中也会因各种突变而被激活。这些变化似乎是恶性转化的原因之一。它们还可能为疾病进程和对当前治疗的反应提供信息。最后,它们是实验室、临床前模型以及少数临床试验中正在研发的各种新型治疗方法的靶点。

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