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Diselenolane-mediated cellular uptake

机译:二硒酚烷介导的细胞摄取

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摘要

The emerging power of thiol-mediated uptake with strained disulfides called for a move from sulfur to selenium. We report that according to results with fluorescent model substrates, cellular uptake with 1,2-diselenolanes exceeds uptake with 1,2-dithiolanes and epidithiodiketopiperazines with regard to efficiency as well as intracellular localization. The diselenide analog of lipoic acid performs best. This 1,2-diselenolane delivers fluorophores efficiently to the cytosol of HeLa Kyoto cells, without detectable endosomal capture as with 1,2-dithiolanes or dominant escape into the nucleus as with epidithiodiketopiperazines. Diselenolane-mediated cytosolic delivery is non-toxic (MTT assay), sensitive to temperature but insensitive to inhibitors of endocytosis (chlorpromazine, methyl-β-cyclodextrin, wortmannin, cytochalasin B) and conventional thiol-mediated uptake (Ellman's reagent), and to serum. Selenophilicity, the extreme CSeSeC dihedral angle of 0° and the high but different acidity of primary and secondary selenols might all contribute to uptake. Thiol-exchange affinity chromatography is introduced as operational mimic of thiol-mediated uptake that provides, in combination with rate enhancement of DTT oxidation, direct experimental evidence for existence and nature of the involved selenosulfides.
机译:紧张的二硫键与硫醇介导的吸收作用的新兴力量要求从硫转移到硒。我们报道,根据荧光模型底物的结果,就效率以及细胞内定位而言,1,2-二硒代戊二烯的细胞摄取超过1,2-二硫杂环戊烷和表二硫代二酮哌嗪的摄取。硫辛酸的二硒化物类似物表现最佳。这种1,2-二硒戊烷可将荧光团有效地传递到HeLa Kyoto细胞的细胞质中,而不会像1,2-二硫杂环戊烷那样可检测到的内体捕获,也不会像表二硫代二酮哌嗪那样显着地逃逸进入细胞核。 Diselenolane介导的胞质传递是无毒的(MTT分析),对温度敏感,但对内吞作用抑制剂(氯丙嗪,甲基-β-环糊精,渥曼青霉素,细胞松弛素B)和常规硫醇介导的摄取(Ellman试剂)不敏感。血清。亲脂性,极端的CSeSeC二面角为0°以及伯硒醇和仲硒醇的酸度高但不同,都可能有助于摄取。引入硫醇交换亲和色谱作为硫醇介导的摄取的操作模拟,结合DTT氧化速率的提高,可提供有关所含硒代硫化物的存在和性质的直接实验证据。

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