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肝实质细胞和非实质细胞对蓖麻毒素的摄取比较及其对蛋白质合成的抑制作用。

A comparison of the accumulation of ricin by hepatic parenchymal and non-parenchymal cells and its inhibition of protein synthesis.

作者信息

Skilleter D N, Paine A J, Stirpe F

出版信息

Biochim Biophys Acta. 1981 Nov 5;677(3-4):495-500. doi: 10.1016/0304-4165(81)90264-6.

Abstract

Rat liver non-parenchymal cells in vivo were found to accumulate 125I-labelled ricin to a much greater extent than parenchymal cells. Similarly, in monolayer cell cultures, the rate of ricin uptake by non-parenchymal Kupffer cells was several times that by parenchymal cells. Evidence is provided also to suggest that ricin is primarily recognized by Kupffer cells via terminal mannose residues in the toxin, whereas ricin uptake by parenchymal cells was consistent with a role of the previously postulated galactosyl-containing cell receptors. Protein synthesis in Kupffer cells in vitro, although observed to occur at a lower rate than in parenchymal cells, was 100--1000-times more sensitive to inhibition by ricin. The selective damage known to be caused to liver sinusoids by ricin, therefore, may reflect both the relative efficiency with which the toxin is taken up by these cells and the extreme sensitivity of protein synthesis in the cells to inhibition by ricin.

摘要

研究发现,大鼠肝脏的非实质细胞在体内积累125I标记的蓖麻毒素的程度比实质细胞大得多。同样,在单层细胞培养中,非实质库普弗细胞摄取蓖麻毒素的速率是实质细胞的几倍。有证据还表明,蓖麻毒素主要通过毒素中的末端甘露糖残基被库普弗细胞识别,而实质细胞摄取蓖麻毒素与先前假定的含半乳糖细胞受体的作用一致。体外库普弗细胞中的蛋白质合成,虽然观察到其发生速率低于实质细胞,但对蓖麻毒素抑制的敏感性要高100至1000倍。因此,已知蓖麻毒素对肝血窦造成的选择性损伤,可能既反映了这些细胞摄取毒素的相对效率,也反映了细胞内蛋白质合成对蓖麻毒素抑制的极端敏感性。

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