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与硫代乙酰胺相关的细胞核肿大伴随的核膜改变。

Nuclear envelope alterations accompanying thioacetamide-related enlargement of the nucleus.

作者信息

Clawson G A, Moody D E, James J, Smuckler E A

出版信息

Cancer Res. 1981 Feb;41(2):519-26.

PMID:7448799
Abstract

Treating rats with thioacetamide results in a biphasic nuclear swelling, with an initial enlargement phase (0 to 8 hr) and a secondary phase (18 to 48 hr). The swelling coincides with and may be responsible for alterations in sedimentation properties of isolated nuclei. Nuclear swelling implies increases in nuclear surface area. Total nuclear lipid increased in proportion to the increase in nuclear-envelope (NE) surface area, suggesting that intranuclear lipid was not the source of new NE phospholipid. The increased NE was apparently not derived from mass incorporation of endoplasmic reticulum into NE, as demonstrated by monitoring enzymatic composition. Significant differences were observed in the distribution of p.o. administered [14C]stearic acid and [14C]phosphatidylcholine in lipid fractions from NE as compared with those from endoplasmic reticulum. Analysis of NE phospholipid revealed little change in composition in the heavy fraction during the first 48 hr after treatment. (An early decrease in phosphatidylserine from the light nuclear fraction may reflect the upward shift of nuclei from the heavy fraction.) A significant increase in phosphatidylserine of NE from the heavy fraction was found at 96 hr. The additional phosphatidylserine in the NE might act as an acidic polymer modifying chromatin structure. Examination of fatty acids from individual NE phospholipid fractions divulged relatively few changes related to the early or the secondary nuclear swelling phases. Major changes occurred in the neutral lipid fraction of NE which apparently served as a reservoir for 18:2, with significant decreases in 18:2 noted following both nuclear swelling phases. These changes did not occur in the neutral lipid fraction from endoplasmic reticulum obtained from the same liver preparations.

摘要

用硫代乙酰胺处理大鼠会导致核肿胀呈双相性,有一个初始增大阶段(0至8小时)和一个继发阶段(18至48小时)。这种肿胀与分离细胞核沉降特性的改变同时发生,并且可能是其原因。核肿胀意味着核表面积增加。总核脂质与核膜(NE)表面积的增加成比例增加,这表明核内脂质不是新的NE磷脂的来源。增加的NE显然不是内质网大量并入NE的结果,这通过监测酶组成得以证明。与内质网的脂质部分相比,经口服给予的[14C]硬脂酸和[14C]磷脂酰胆碱在NE脂质部分中的分布存在显著差异。对NE磷脂的分析显示,处理后最初48小时内重质部分的组成变化不大。(轻核部分中磷脂酰丝氨酸的早期减少可能反映了细胞核从重质部分向上转移。)在96小时时发现重质部分的NE中磷脂酰丝氨酸显著增加。NE中额外的磷脂酰丝氨酸可能作为一种酸性聚合物修饰染色质结构。对各个NE磷脂部分的脂肪酸检查发现,与早期或继发核肿胀阶段相关的变化相对较少。主要变化发生在NE的中性脂质部分,其显然作为18:2的储存库,在两个核肿胀阶段后均观察到18:2显著减少。这些变化在从相同肝脏制剂获得的内质网的中性脂质部分中未发生。

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