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兔小肠刷状缘膜囊泡转运谷氨酸的特性。Na⁺、K⁺和H⁺梯度的影响。

Characteristics of glutamic acid transport by rabbit intestinal brush-border membrane vesicles. Effects of Na+-, K+- and H+-gradients.

作者信息

Berteloot A

出版信息

Biochim Biophys Acta. 1984 Aug 22;775(2):129-40. doi: 10.1016/0005-2736(84)90163-9.

Abstract

In the presence of a Na+-gradient (out greater than in), L-glutamic acid and L-and D-aspartic acids were equally well concentrated inside the vesicles, while no transport above simple diffusion levels was seen by replacement of Na+ by K+. Equilibrium uptake values were found inversely proportional to the medium osmolarity, thus demonstrating uptake into an osmotically sensitive intravesicular space. The extrapolation of these lines to infinite medium osmolarity (zero space) showed only a small binding component in acidic amino-acid transport. When the same experiment was performed at saturating substrate concentrations, linear relationships extrapolating through the origin but showing smaller slope values were recorded, thus indicating that the binding component could be more important than suspected above. However, binding to the membrane was neglected in our studies as it was absent from initial rate measurements. Na+-dependent uphill transport of L-glutamic acid was stimulated by K+ present on the intravesicular side only but maximal stimulation was recorded under conditions of an outward K+-gradient (in greater than out). Quantitative and qualitative differences in the K+ effect were noted between pH 6.0 and 8.0. Initial uptake rates showed pH dependency in Na+-(out greater than in) + K+-(in greater than out) gradient conditions only with a physiological pH optimum between 7.0 and 7.5. It was also found that a pH-gradient (acidic outside) could stimulate both the Na+-gradient and the Na+ + K+-gradient-dependent transport of L-glutamic acid. However, pH- or K+-gradient alone were ineffective in stimulating uptake above simple diffusion level. Finally, it was found that increased rates of efflux were always observed with an acidic pH outside, whatever the conditions inside the vesicles. From these results, we propose a channel-type mechanism of L-glutamic acid transport in which Na+ and K+ effects are modulated by the surrounding pH. The model proposes a carrier with high or low affinity for Na+ in the protonated or unprotonated forms, respectively. We also propose that K+ binding occurs only to the unprotonated carrier and allows its fast recycling as compared to the free form of the carrier. Such a model would be maximally active and effective in the intestine in the in vivo physiological situations.

摘要

在存在Na⁺梯度(胞外高于胞内)的情况下,L-谷氨酸以及L-和D-天冬氨酸在囊泡内的浓缩程度相同,而用K⁺替代Na⁺时,未观察到高于简单扩散水平的转运。平衡摄取值与介质渗透压成反比,从而证明摄取进入了对渗透压敏感的囊泡内空间。将这些直线外推至无限介质渗透压(零空间)表明,酸性氨基酸转运中仅有一个小的结合成分。当在饱和底物浓度下进行相同实验时,记录到通过原点的线性关系,但斜率值较小,因此表明结合成分可能比上述推测的更重要。然而,在我们的研究中忽略了与膜的结合,因为在初始速率测量中未出现这种情况。L-谷氨酸的Na⁺依赖性上坡转运仅受囊泡内侧存在的K⁺刺激,但在向外的K⁺梯度(胞内高于胞外)条件下记录到最大刺激。在pH 6.0和8.0之间观察到K⁺效应的定量和定性差异。初始摄取速率仅在Na⁺(胞外高于胞内)+ K⁺(胞内高于胞外)梯度条件下显示出pH依赖性,生理pH最佳值在7.0至7.5之间。还发现pH梯度(外侧酸性)可刺激L-谷氨酸的Na⁺梯度和Na⁺ + K⁺梯度依赖性转运。然而,单独的pH或K⁺梯度在刺激摄取高于简单扩散水平方面无效。最后,发现无论囊泡内的条件如何,外侧酸性pH总是会观察到流出速率增加。根据这些结果,我们提出了一种L-谷氨酸转运的通道型机制,其中Na⁺和K⁺效应受周围pH调节。该模型提出了一种载体,其对质子化或未质子化形式的Na⁺分别具有高或低亲和力。我们还提出K⁺仅与未质子化的载体结合,并使其与载体的游离形式相比能够快速循环利用。这样的模型在体内生理情况下的肠道中具有最大活性和有效性。

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