## Abstract Nerve growth factor (NGF) is a neurotrophic factor that plays an important role in the differentiation and growth of neuronal cells. It is also regarded as an inflammatory mediator in nonβneuronal tissues under physiological stress conditions. The mechanisms of NGF production and its ro
Role of nerve growth factor in ethylnitrosourea-induced neural carcinogenesis
β Scribed by Stanley A. Vinores; J. Regino Perez-Polo
- Publisher
- John Wiley and Sons
- Year
- 1980
- Tongue
- English
- Weight
- 692 KB
- Volume
- 5
- Category
- Article
- ISSN
- 0360-4012
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β¦ Synopsis
Abstract
The sensitivity of the rat nervous system to malignant transformation by ethylnitrosourea (ENU) is a function of age at treatment. From late gestation, nervous structures decrease in sensitivity with age as nonβneural structures increase in susceptibility. There is a decrease in the proportion of neural tumors induced by ENU and an increase in survival time when nerve growth factor (NGF) levels are elevated in the fetal or neonatal stage. If antibodies directed against mouse betaβNGF (antiβNGF) are administered prior to neonatal ENU treatment, neural tumors appear earlier, although in the same proportion as with treatment by ENU alone. This effect is not observed if the ENU is administered first. This phenomenon seems to be attributed to an increased number of trigeminal nerve neurinomas, which have a shorter latent period than other nervous system tumors. The induced neurological tumors in rats treated neonatally with antiβNGF prior to ENU seem to be almost exclusively neurinomas in the peripheral nervous system. Fetal antiβNGF treatment leads to an increased number of intracerebral gliomas and a longer survival time, which corresponds to the longer latent period of these tumors. The role of NGF in the sensitivity of the rat nervous system to carcinogenesis by ENU and its possible implications in the development of the nervous system are discussed.
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