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Effect of PTU treatment on histone acetylation pattern in the developing rat brain.

机译:PTU处理对发育中大鼠脑中组蛋白乙酰化模式的影响。

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The effect of hypothyroidism induced m female rats on histone acetylation pattern m the neonatal rat brain was studied. It is likely that thyroid hormone regulates the acetylation of histones and thereby influence their interaction with DNA and modulates transcription. Propylthiouracil (PTU), administered to induce hypothyroidism, resulted in a significant reduction m the thyroid and brain weight of neonatal rats. The circulating thyroxine levels were undetectable in both 14 and 21 day old pups. The hypothyroid condition was further confirmed by low levels of T4 (94.31 ng/g brain tissue vs 1811.29 ng/g in controls and 144.67 ng/g vs 1087.72 ng/g in controls at 14 and 21 days, respectively) and T3 (42.19 ng/g brain tissue vs 879.97 ng/g in controls and 60.62 ng/g vs 766.68 ng/g in controls at 14 and 21 days, respectively) in the neonatal rat brain. Histone acetylation pattern was similar in treated and control groups m the 14 day old rats. PTU treatment, however, resulted in significant (p<0.01) reduction in acetylation in the H3 fraction at 21 days whereas no such changes were recorded in other histone fractions. Lower histone acetylation in the 21 day old pups suggest a reduction m the transcriptional activity due to fewer initiation sites for RNA polymerase. It may be concluded that thyroid hormone may stimulate transcription of specific genes by increasing the acetylation of nucleosomal histones.
机译:研究了甲减引起的雌性大鼠对新生大鼠脑中组蛋白乙酰化模式的影响。甲状腺激素可能会调节组蛋白的乙酰化,从而影响其与DNA的相互作用并调节转录。丙硫氧嘧啶(PTU)可以诱导甲状腺功能减退,可显着降低新生大鼠的甲状腺和脑重量。在14和21日龄的幼犬中均未检测到循环甲状腺素水平。通过低水平的T4(分别在14天和21天时的脑组织为94.31 ng / g vs对照的1811.29 ng / g和144.67 ng / g vs对照1087.72 ng / g)和T3的低水平进一步证实了甲状腺功能低下。在新生大鼠脑中,分别在14天和21天时,大脑组织的/ g脑组织vs对照的879.97 ng / g和对照的60.62 ng / g vs 766.68 ng / g。在14日龄大鼠的治疗组和对照组中,组蛋白乙酰化模式相似。然而,PTU处理在21天时导致H3馏分中乙酰化的显着降低(p <0.01),而其他组蛋白馏分中未记录到此类变化。在21天大的幼仔中较低的组蛋白乙酰化表明转录活性降低,因为RNA聚合酶的起始位点较少。可以得出结论,甲状腺激素可以通过增加核小体组蛋白的乙酰化来刺激特定基因的转录。

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