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1
Titration of transport and modifier sites in the red cell anion transport system.红细胞阴离子转运系统中转运位点和修饰位点的滴定法
J Gen Physiol. 1982 Feb;79(2):253-82. doi: 10.1085/jgp.79.2.253.
2
The human erythrocyte anion transport protein, band 3. Characterization of exofacial alkaline titratable groups involved in anion binding/translocation.人类红细胞阴离子转运蛋白,带3。参与阴离子结合/转运的胞外碱性可滴定基团的特性。
J Gen Physiol. 1992 Aug;100(2):301-39. doi: 10.1085/jgp.100.2.301.
3
Chloride--bicarbonate exchange in red blood cells: physiology of transport and chemical modification of binding sites.红细胞中的氯-碳酸氢根交换:转运生理学及结合位点的化学修饰
Philos Trans R Soc Lond B Biol Sci. 1982 Dec 1;299(1097):383-99. doi: 10.1098/rstb.1982.0139.
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Irreversible inactivation of red cell chloride exchange with phenylglyoxal, and arginine-specific reagent.用苯乙二醛(一种精氨酸特异性试剂)使红细胞氯交换发生不可逆失活。
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Relationship of net chloride flow across the human erythrocyte membrane to the anion exchange mechanism.跨人红细胞膜的净氯流与阴离子交换机制的关系。
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N-(4-azido-2-nitrophenyl)-2-aminoethylsulfonate (NAP-taurine) as a photoaffinity probe for identifying membrane components containing the modifier site of the human red blood cell anion exchange system.N-(4-叠氮基-2-硝基苯基)-2-氨基乙磺酸盐(NAP-牛磺酸)作为一种光亲和探针,用于鉴定含有人类红细胞阴离子交换系统修饰位点的膜成分。
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Bicarbonate exchange through the human red cell membrane determined with [14C] bicarbonate.用[14C]碳酸氢盐测定的通过人红细胞膜的碳酸氢盐交换。
J Physiol. 1979 Sep;294:521-39. doi: 10.1113/jphysiol.1979.sp012944.
8
Asymmetry of the red cell anion exchange system. Different mechanisms of reversible inhibition by N-(4-azido-2-nitrophenyl)-2-aminoethylsulfonate (NAP-taurine) at the inside and outside of the membrane.红细胞阴离子交换系统的不对称性。膜内外N-(4-叠氮基-2-硝基苯基)-2-氨基乙磺酸盐(NAP-牛磺酸)可逆抑制的不同机制。
J Gen Physiol. 1978 Nov;72(5):607-30. doi: 10.1085/jgp.72.5.607.
9
Phosphate transport in human red blood cells: concentration dependence and pH dependence of the unidirectional phosphate flux at equilibrium conditions.人类红细胞中的磷酸盐转运:平衡条件下单向磷酸盐通量的浓度依赖性和pH依赖性。
J Membr Biol. 1981;61(3):173-92. doi: 10.1007/BF01870522.
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Asymmetry in the mechanism for anion exchange in human red blood cell membranes. Evidence for reciprocating sites that react with one transported anion at a time.人类红细胞膜中阴离子交换机制的不对称性。一次仅与一种转运阴离子反应的往复位点的证据。
J Gen Physiol. 1979 Sep;74(3):351-74. doi: 10.1085/jgp.74.3.351.

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Modification of C1- transport in skeletal muscle of Rana temporaria with the arginine-binding reagent phenylglyoxal.用精氨酸结合试剂苯乙二醛对林蛙骨骼肌中C1-转运的修饰
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Electrodiffusion, barrier, and gating analysis of DIDS-insensitive chloride conductance in human red blood cells treated with valinomycin or gramicidin.缬氨霉素或短杆菌肽处理的人红细胞中对4,4'-二异硫氰基二苯乙烯-2,2'-二磺酸(DIDS)不敏感的氯电导的电扩散、屏障及门控分析
J Gen Physiol. 1997 Feb;109(2):201-16. doi: 10.1085/jgp.109.2.201.
7
Effects of external pH on binding of external sulfate, 4.4-dinitro-stilbene-2,2'-disulfonate (DNDS), and chloride to the band 3 anion exchange protein.外部pH值对外部硫酸盐、4,4'-二硝基芪-2,2'-二磺酸盐(DNDS)和氯离子与带3阴离子交换蛋白结合的影响。
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8
Effects of external pH on substrate binding and on the inward chloride translocation rate constant of band 3.外部pH值对带3蛋白底物结合及氯离子内向转运速率常数的影响。
J Gen Physiol. 1996 Feb;107(2):271-91. doi: 10.1085/jgp.107.2.271.
9
Selective phenylglyoxalation of functionally essential arginyl residues in the erythrocyte anion transport protein.红细胞阴离子转运蛋白中功能必需精氨酰残基的选择性苯乙二醛化
J Gen Physiol. 1983 Apr;81(4):453-84. doi: 10.1085/jgp.81.4.453.
10
Irreversible inactivation of red cell chloride exchange with phenylglyoxal, and arginine-specific reagent.用苯乙二醛(一种精氨酸特异性试剂)使红细胞氯交换发生不可逆失活。
J Gen Physiol. 1982 Feb;79(2):283-312. doi: 10.1085/jgp.79.2.283.

本文引用的文献

1
Irreversible inactivation of red cell chloride exchange with phenylglyoxal, and arginine-specific reagent.用苯乙二醛(一种精氨酸特异性试剂)使红细胞氯交换发生不可逆失活。
J Gen Physiol. 1982 Feb;79(2):283-312. doi: 10.1085/jgp.79.2.283.
2
Transport and interactions of anions and protons in the red blood cell membrane.红细胞膜中阴离子与质子的转运及相互作用。
Ann N Y Acad Sci. 1980;341:394-418. doi: 10.1111/j.1749-6632.1980.tb47186.x.
3
The kinetics of the titratable carrier for anion exchange in erythrocytes.红细胞中可滴定阴离子交换载体的动力学。
Ann N Y Acad Sci. 1980;341:384-93. doi: 10.1111/j.1749-6632.1980.tb47185.x.
4
The reaction of phenylglyoxal with arginine residues in proteins.苯乙二醛与蛋白质中精氨酸残基的反应。
J Biol Chem. 1968 Dec 10;243(23):6171-9.
5
A quantitative estimate of the non-exchange-restricted chloride permeability of the human red cell.对人体红细胞非交换限制氯离子通透性的定量估计。
J Physiol. 1971 Oct;218 Suppl:49P-50P.
6
Temperature dependence of chloride, bromide, iodide, thiocyanate and salicylate transport in human red cells.人体红细胞中氯离子、溴离子、碘离子、硫氰酸盐和水杨酸盐转运的温度依赖性
J Physiol. 1972 Aug;224(3):583-610. doi: 10.1113/jphysiol.1972.sp009914.
7
Passive ion permeability of the erythrocyte membrane.红细胞膜的被动离子通透性。
Prog Biophys Mol Biol. 1969;19(2):423-67.
8
Membrane proteins related to anion permeability of human red blood cells. I. Localization of disulfonic stilbene binding sites in proteins involved in permeation.与人类红细胞阴离子通透性相关的膜蛋白。I. 二磺酸芪结合位点在参与通透的蛋白质中的定位。
J Membr Biol. 1974;15(3):207-26. doi: 10.1007/BF01870088.
9
Selective solubilization of proteins from red blood cell membranes by protein perturbants.通过蛋白质扰动剂从红细胞膜中选择性溶解蛋白质。
J Supramol Struct. 1973;1(3):220-32. doi: 10.1002/jss.400010307.
10
Characteristics of chloride transport in human red blood cells.人类红细胞中氯离子转运的特征
J Gen Physiol. 1973 Feb;61(2):185-206. doi: 10.1085/jgp.61.2.185.

红细胞阴离子转运系统中转运位点和修饰位点的滴定法

Titration of transport and modifier sites in the red cell anion transport system.

作者信息

Wieth J O, Bjerrum P J

出版信息

J Gen Physiol. 1982 Feb;79(2):253-82. doi: 10.1085/jgp.79.2.253.

DOI:10.1085/jgp.79.2.253
PMID:6276496
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2215494/
Abstract

This work demonstrates the existence of titratable transport and modifier sites in the anion transport system of human red cells. Effects of alkaline extracellular pH on chloride exchange were studied up to pH 13 at 0 degrees C. The studies revealed two sets of reversible titratable groups. One set, having a pK of or approximately 11, appeared to be identical with the inhibitory halide-binding modifier site. Deprotonation of this site stimulated anion transport. The apparent dissociation constants of chloride and iodide at this modifier site were 0.3 and 0.06 M, respectively, and it was confirmed that the organic sulfonate NAP-taurine inhibits anion transport reversibly by a high-affinity interaction with halide-binding modifier sites at the extracellular side of the membrane. Other groups, with apparent pK of or approximately 12 at chloride concentrations above 0.1 M, were named as "transport sites" because transport function depended totally on their protonation. The apparent pK decreased when extracellular halide concentrations was lowered below 0.1 M. It was dependent of the intracellular chloride concentration, and was equally sensitive to extracellular pH of 13, was fully reversible. Hydroxyl ions were not transported to an appreciable extent by the anion exchange system. The pK values of both sets of groups make it likely that they are both arginyl residues, functioning as anion recognition sites similar to the role of functionally essential arginyl residues observed with numerous enzymes.

摘要

这项研究证明了人类红细胞阴离子转运系统中存在可滴定的转运位点和修饰位点。在0℃下,研究了细胞外碱性pH对氯离子交换的影响,直至pH值达到13。研究揭示了两组可逆的可滴定基团。一组的pK值约为11,似乎与抑制性卤化物结合修饰位点相同。该位点的去质子化刺激了阴离子转运。氯离子和碘离子在该修饰位点的表观解离常数分别为0.3 M和0.06 M,并且证实有机磺酸盐NAP-牛磺酸通过与膜外侧卤化物结合修饰位点的高亲和力相互作用可逆地抑制阴离子转运。在氯离子浓度高于0.1 M时,其他基团的表观pK值约为12,被称为“转运位点”,因为转运功能完全取决于它们的质子化状态。当细胞外卤化物浓度降低到0.1 M以下时,表观pK值降低。它依赖于细胞内氯离子浓度,对细胞外pH值为13同样敏感,且完全可逆。阴离子交换系统不会大量转运氢氧根离子。这两组基团的pK值表明它们可能都是精氨酰残基,起着阴离子识别位点的作用,类似于在许多酶中观察到的功能必需精氨酰残基的作用。