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颗粒状镍化合物在组织培养中的吞噬作用、细胞分布及致癌活性

Phagocytosis, cellular distribution, and carcinogenic activity of particulate nickel compounds in tissue culture.

作者信息

Costa M, Simmons-Hansen J, Bedrossian C W, Bonura J, Caprioli R M

出版信息

Cancer Res. 1981 Jul;41(7):2868-76.

PMID:7248947
Abstract

The uptake, toxicity, and morphological transformation efficacy of various water-insoluble nickel compounds were examined in tissue culture. Particles (2.2 to 4.8 micrometers) of crystalline Ni3S2, crystalline NiS, and crystalline Ni3Se2 were actively phagocytized by cultured cells as determined by light and electron microscopy. However, particles of similar size consisting of amorphous NiS and metallic nickel were not significantly phagocytized despite long exposure periods to high concentrations. X-ray fluorescence spectrometry measurements of metal levels in subcellular fractions isolated from cells treated with crystalline Ni3S2, crystalline NiS, or amorphous NiS confirmed that amorphous NiS did not significantly enter the cells, either as a phagocytized particle or in a solubilized form, while the other two crystalline nickel compounds were actively taken up. Cells treated with amorphous NiS contained nickel levels generally less than 10% of the nickel levels in whole cells and in cytoplasmic fractions, or nuclear fractions of cells treated with either crystalline NiS or crystalline Ni3S2. The phagocytized nickel particles were always observed in the cytoplasm with light and electron microscopy, but substantial nickel levels were measured in the nuclear fraction. These and other results suggest that the nickel particles were broken down in the cytoplasm to a size range no longer detectable with the electron microscope and then subsequently entered the nucleus. Control experiments suggest that at least 20% of the nickel measured in the nucleus isolated from cells treated with Ni3S2 is no longer part of a sedimentable particle with the same particle size and/or solubility properties of the parent compound. A substantial portion of the nickel associated with the nuclear fraction coprecipitated with trichloroacetic acid-insoluble material, suggesting that nickel binds strongly to cellular macromolecules. The phagocytized particulate nickel compounds were more cytotoxic as determined by reduction of cell-plating efficiency and induced more morphological transformations in the Syrian hamster embryo cell transformation assay than did the particulate nickel compounds which were not phagocytized. Manganese dust inhibited the morphological transformation induced by Ni3S2 and also reduced the phagocytosis of Ni3S2 particles.

摘要

在组织培养中检测了各种水不溶性镍化合物的摄取、毒性及形态转化功效。通过光学显微镜和电子显微镜确定,结晶态的Ni3S2、结晶态的NiS和结晶态的Ni3Se2颗粒(2.2至4.8微米)被培养细胞积极吞噬。然而,尽管长时间暴露于高浓度环境中,由无定形NiS和金属镍组成的类似大小的颗粒却未被显著吞噬。对用结晶态Ni3S2、结晶态NiS或无定形NiS处理的细胞分离得到的亚细胞组分中的金属水平进行X射线荧光光谱测量,证实无定形NiS无论是作为吞噬颗粒还是以溶解形式都未显著进入细胞,而另外两种结晶态镍化合物则被积极摄取。用无定形NiS处理的细胞所含镍水平通常低于用结晶态NiS或结晶态Ni3S2处理的细胞的全细胞、细胞质组分或细胞核组分中的镍水平的10%。通过光学显微镜和电子显微镜始终在细胞质中观察到吞噬的镍颗粒,但在细胞核组分中检测到大量镍水平。这些及其他结果表明,镍颗粒在细胞质中分解至电子显微镜不再能检测到的大小范围,随后进入细胞核。对照实验表明,在用Ni3S2处理的细胞分离得到的细胞核中测得的镍中,至少20%不再是具有与母体化合物相同粒径和/或溶解性的可沉降颗粒的一部分。与细胞核组分相关的大部分镍与三氯乙酸不溶性物质共沉淀,表明镍与细胞大分子强烈结合。通过细胞铺板效率降低测定,吞噬的颗粒状镍化合物比未被吞噬的颗粒状镍化合物更具细胞毒性,并且在叙利亚仓鼠胚胎细胞转化试验中诱导更多形态转化。锰尘抑制了Ni3S2诱导的形态转化,也降低了Ni3S2颗粒的吞噬作用。

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