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首页> 外文期刊>Neurochemistry International: The International Journal for the Rapid Publication of Critical Reviews, Preliminary and Original Research Communications in Neurochemistry >Effects of acute and chronic administration of methylmalonic and propionic acids on the in vitro incorporation of 32P into cytoskeletal proteins from cerebral cortex of young rats.
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Effects of acute and chronic administration of methylmalonic and propionic acids on the in vitro incorporation of 32P into cytoskeletal proteins from cerebral cortex of young rats.

机译:急性和慢性给予甲基丙二酸和丙酸对32P体外掺入幼鼠大脑皮层细胞骨架蛋白的影响。

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We studied the effects of acute and chronic administration of methylmalonic (MMA) and propionic (PA) acids on the in vitro incorporation of 32P into neurofilament subunits (NF-M and NF-L), alpha and beta tubulins, from cerebral cortex of rats. In the chronic treatment, drugs were administered subcutaneously from day 6-17 post-partum (MMA 0.76-0.89 micromol/g body weight and PA 0.93 micromol/g body weight). In the acute treatment MMA and PA were injected (MMA 3.78 micromol/g body weight and PA 3.90 micromol/g body weight). Control animals received saline in the same volumes. The Triton-insoluble cytoskeletal fraction of control in treated animals was isolated and incubated with 32P-ATP. Our results demonstrate that both drugs were able to inhibit 32P in vitro incorporation into neurofilaments and tubulins. The acute administration of MMA decreased the in vitro 32P incorporation into NF-L and alpha-tubulin subunit, whereas PA administration decreased the 32P in vitro incorporation into NF-M, NF-L, and tubulins. On the other hand, chronic MMA administration induced a decreased 32P in vitro incorporation into NF-M, while chronic treatment with propionate decreased the in vitro phosphorylation of NF-M and alpha-tubulin. This study provides consistent evidence that a decreased phosphorylation of cytoskeletal proteins is induced by MMA and PA metabolites which accumulate in methylmalonic and propionic acidemias respectively. Therefore, it is possible that an altered brain cytoskeletal metabolism could be related with the structural alterations of CNS observed in these disorders.
机译:我们研究了急性和慢性给予甲基丙二酸(MMA)和丙酸(PA)酸对32P体外掺入大鼠大脑皮质神经丝亚基(NF-M和NF-L),α和β微管蛋白的影响。在慢性治疗中,从产后第6天到第17天皮下注射药物(MMA 0.76-0.89 micromol / g体重和PA 0.93 micromol / g体重)。在急性治疗中,注射MMA和PA(MMA 3.78微摩尔/克体重和PA 3.90微摩尔/克体重)。对照动物接受相同体积的盐水。分离治疗动物中对照的Triton不溶性细胞骨架部分,并与32P-ATP一起孵育。我们的结果表明,两种药物在体外都能抑制32P掺入神经丝和微管蛋白。 MMA的急性给药减少了32P在NF-L和α-微管蛋白亚基中的体外结合,而PA给药减少了32P在NF-M,NF-L和微管蛋白中的体外结合。另一方面,长期使用MMA诱导的32P体外掺入NF-M减少,而长期使用丙酸酯治疗会降低NF-M和α-微管蛋白的体外磷酸化。这项研究提供了一致的证据,表明分别由甲基丙二酸和丙酸血症引起的MMA和PA代谢产物诱导了细胞骨架蛋白磷酸化的降低。因此,可能在这些疾病中观察到的脑细胞骨架代谢的改变可能与中枢神经系统的结构改变有关。

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