首页> 美国卫生研究院文献>The Journal of Physiology >Cations that alter surface potentials of lipid bilayers increase the calcium requirement for exocytosis in sea urchin eggs.
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Cations that alter surface potentials of lipid bilayers increase the calcium requirement for exocytosis in sea urchin eggs.

机译:改变脂质双层表面电位的阳离子会增加海胆鸡蛋胞吐作用所需的钙。

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摘要

1. We examined the effects of cations that bind to phospholipid bilayers on the calcium requirement for exocytosis in vitro. 2. Tetracaine and trifluoperazine, two monovalent cations that bind hydrophobically to lipid bilayers, decreased the zeta-potential of lipid vesicles with a phospholipid composition similar to sea urchin plasma membranes; the decrease in the magnitude of the negative zeta-potential was consistent with the Gouy-Chapman-Stern theory. 3. Trifluoperazine and tetracaine also increased the concentration of calcium required to produce half-maximal exocytosis (Ca50) in isolated fragments of plasma membranes from sea urchin eggs. 4. The effects of trifluoperazine and tetracaine on the Ca50 of egg fragments can be explained quantitatively from the zeta-potential data obtained with phospholipid vesicles if we assume the calcium binding sites responsible for triggering exocytosis lie within a Debye length (less than 1 nm) of the surface of the plasma membranes, such that the concentration of calcium at the sites is affected by the surface potential of the membrane. 5. The divalent cation magnesium, which binds specifically to the phosphate group of lipids, affected Ca50 in a manner that can also be explained quantitatively from its effects on the zeta-potential of phospholipid vesicles. 6. The polyvalent cation neomycin, which adsorbs to the lipid phosphatidylinositol 4,5-bisphosphate with high affinity, also binds co-operatively to phosphatidylinositol; its effect on Ca50 can be explained quantitatively from its effects on the zeta-potential of vesicles containing the latter lipid. 7. A decrease in the ionic strength increases the magnitude of the surface potential of membranes; the effect of ionic strength on Ca50 can be explained qualitatively from its effect on the zeta-potential of phospholipid vesicles. 8. All our results are consistent with the hypothesis that calcium binding sites lie within a Debye length of the plasma membrane; they also indicate that drugs with specific, high-affinity sites may affect exocytosis by a non-specific mechanism.
机译:1.我们研究了与磷脂双层结合的阳离子对体外胞吐所需钙的影响。 2. Tetracaine和trifluoperazine,这两种单价阳离子与脂质双层疏水结合,通过类似于海胆质膜的磷脂成分降低了脂质囊泡的Zeta电位。负ζ电位的幅度减小与Gouy-Chapman-Stern理论一致。 3. Trifluoperazine和丁卡因还增加了海胆卵质膜分离片段中产生半数最大胞吐作用(Ca50)所需的钙浓度。 4.如果我们假设负责触发胞吐作用的钙结合位点在Debye长度(小于1 nm)之内,那么三氟拉嗪和丁卡因对卵片段Ca50的影响可以从磷脂囊泡获得的ζ电位数据中定量解释。质膜表面的“电势”,使得位点处的钙浓度受膜表面电势的影响。 5.与脂质的磷酸基团特异性结合的二价阳离子镁以一种也可以从其对磷脂囊泡的ζ电位的影响进行定量解释的方式影响Ca50。 6.多价阳离子新霉素,其以高亲和力吸附于脂质磷脂酰肌醇4,5-双磷酸酯上,也与磷脂酰肌醇结合。它对Ca50的作用可以从其对含有后者脂质的囊泡的Zeta电位的影响进行定量解释。 7.离子强度的降低会增加膜表面电势的大小;离子强度对Ca50的影响可以从其对磷脂囊泡的Zeta电位的影响进行定性解释。 8.我们所有的结果均与钙结合位点位于质膜的德拜长度之内的假设相符。它们还表明具有特异性,高亲和力位点的药物可能通过非特异性机制影响胞吐作用。

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