首页> 美国卫生研究院文献>The Journal of Biophysical and Biochemical Cytology >Distinct and different effects of the oncogenes v-myc and v-src on avian sympathetic neurons: retroviral transfer of v-myc stimulates neuronal proliferation whereas v-src transfer enhances neuronal differentiation
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Distinct and different effects of the oncogenes v-myc and v-src on avian sympathetic neurons: retroviral transfer of v-myc stimulates neuronal proliferation whereas v-src transfer enhances neuronal differentiation

机译:癌基因v-myc和v-src对禽交感神经元的不同影响:v-myc的逆转录病毒转移刺激神经元增殖而v-src转移促进神经元分化

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摘要

Immature avian sympathetic neurons are able to proliferate in culture for a limited number of divisions albeit expressing several neuron- specific properties. The effect of avian retroviral transfer of oncogenes on proliferation and differentiation of sympathetic neurons was investigated. Primary cultures of 6-d-old quail sympathetic ganglia, consisting of 90% neuronal cells, were infected by Myelocytomatosis virus (MC29), which contains the oncogene v-myc, and by the v-src-containing Rous sarcoma virus (RSV). RSV infection, in contrast to findings in other cellular systems, resulted in a reduction of neuronal proliferation as determined by 3H-thymidine incorporation (50% of control 4 d after infection) and in increased morphological differentiation. This is reflected by increased neurite production, cell size, and expression of neurofilament protein. In addition, RSV- infected neurons, unlike uninfected cells, are able to survive in culture for time periods up to 14 d in the absence of added neurotrophic factors. In contrast, retroviral transfer of v-myc stimulated the proliferation of immature sympathetic neurons preserving many properties of uninfected cells. The neuron-specific cell surface antigen Q211 and the adrenergic marker enzyme tyrosine hydroxylase were maintained in MC29-infected cells and in the presence of chick embryo extract the cells could be propagated over several weeks and five passages. Within 7 d after infection, the number of Q211-positive neurons increased approximately 100-fold. These data demonstrate distinct and different effects of v-src and v-myc-containing retroviruses on proliferation and differentiation of sympathetic neurons: v-src transfer results in increased differentiation, whereas v- myc transfer maintains an immature status reflected by proliferation, immature morphology, and complex growth requirements. The possibility of expanding immature neuronal populations by transfer of v-myc will be of considerable importance for the molecular analysis of neuronal proliferation and differentiation.
机译:未成熟的禽交感神经元能够在培养物中增殖有限的分裂,尽管它表达了几种神经元特有的特性。研究了禽逆转录病毒转移致癌基因对交感神经元增殖和分化的影响。由90%的神经元细胞组成的6日龄鹌鹑交感神经节的原代培养物感染了含有致癌基因v-myc的骨髓增生病病毒(MC29)和含v-src的劳斯肉瘤病毒(RSV) 。与其他细胞系统中的发现相反,RSV感染可导致神经元增殖减少(如感染3H-胸腺嘧啶核苷)(感染后4 d为对照的50%),并导致形态分化增加。这通过增加的神经突产生,细胞大小和神经丝蛋白的表达来反映。此外,与RSV感染的神经元不同,与未感染的细胞不同,在没有添加神经营养因子的情况下,其能够在培养物中存活长达14 d。相比之下,v-myc的逆转录病毒转移刺激未成熟的交感神经元的增殖,从而保留了未感染细胞的许多特性。神经元特异性细胞表面抗原Q211和肾上腺素标记酶酪氨酸羟化酶在感染了MC29的细胞中得以维持,并且在存在鸡胚提取物的情况下,这些细胞可以繁殖数周和五代。感染后7天内,Q211阳性神经元的数量增加了约100倍。这些数据证明了v-src和含v-myc的逆转录病毒对交感神经元增殖和分化的不同影响:v-src转移导致分化增加,而v-myc转移则保持增殖,未成熟形态反映的未成熟状态,以及复杂的增长要求。通过v-myc转移来扩大不成熟神经元种群的可能性对于神经元增殖和分化的分子分析具有相当重要的意义。

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