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单只大鼠肝细胞中由5',5"'-P1,P3-三磷酸二腺苷和5',5"'-P1,P4-四磷酸二腺苷诱导的胞质游离钙离子振荡分别与由ADP和ATP诱导的振荡无法区分。

Cytosolic free Ca2+ oscillations induced by diadenosine 5',5"'-P1,P3-triphosphate and diadenosine 5',5"'-P1,P4-tetraphosphate in single rat hepatocytes are indistinguishable from those induced by ADP and ATP respectively.

作者信息

Green A K, Cobbold P H, Dixon C J

机构信息

Department of Human Anatomy and Cell Biology, University of Liverpool, U.K.

出版信息

Biochem J. 1995 Sep 1;310 ( Pt 2)(Pt 2):629-35. doi: 10.1042/bj3100629.

Abstract

Diadenosine 5',5"'-P1,P3-triphosphate (Ap3A) and diadenosine 5',5"'-P1,P4-tetraphosphate (Ap4A) induce distinctive patterns of [Ca2+]i oscillations in single rat hepatocytes. We show here that [Ca2+]i oscillations induced by Ap3A and ADP are indistinguishable and that [Ca2+]i oscillations induced by Ap4A closely resemble those induced by ATP. These similarities embrace the following: (1) ADP and Ap3A invariably induce [Ca2+]i transients of short duration (approx. 9 s). Ap4A, like ATP, can induce, depending upon the individual cell, either transients of short duration (approx. 9 s), transients of much longer duration or a mixture of short and long transients within a single response. We show here that the pattern of oscillations induced by Ap4A is similar to that induced by ATP in the same hepatocyte. (2) Elevated intracellular cyclic AMP concentration modulates Ap3A-induced transients, like ADP-induced transients, through an increase in both the peak [Ca2+]i and the frequency of the transients. In contrast, Ap4A-induced transients, like ATP-induced transients, develop an increased duration or a sustained rise in [Ca2+]i, with no rise in peak [Ca2+]i. (3) Ap3A-induced transients, like ADP-induced transients, are abolished by low concentrations of the phorbol ester 4 beta-phorbol 12,13-dibutyrate (PDB; 5-10 nM), whereas long Ap4A-induced transients, like long ATP-induced transients, are refractory to high concentrations of PDB (100 nM). We propose that the [Ca2+]i oscillations induced in rat hepatocytes by Ap3A are mediated by the same purinoceptor that mediates the effects of ADP, whereas the oscillations induced by Ap4A are mediated by the same purinoceptor(s) that mediate the effects of ATP.

摘要

5',5'''-P1,P3-三磷酸二腺苷(Ap3A)和5',5'''-P1,P4-四磷酸二腺苷(Ap4A)可在单个大鼠肝细胞中诱导出独特的[Ca2+]i振荡模式。我们在此表明,Ap3A和ADP诱导的[Ca2+]i振荡无法区分,且Ap4A诱导的[Ca2+]i振荡与ATP诱导的极为相似。这些相似之处包括:(1)ADP和Ap3A总是诱导持续时间较短(约9秒)的[Ca2+]i瞬变。Ap4A与ATP一样,根据单个细胞的情况,可诱导持续时间较短(约9秒)的瞬变、持续时间长得多的瞬变或在单个反应中出现短瞬变和长瞬变的混合情况。我们在此表明,Ap4A诱导的振荡模式与同一肝细胞中ATP诱导的相似。(2)细胞内环状AMP浓度升高会像调节ADP诱导的瞬变一样,通过增加[Ca2+]i峰值和瞬变频率来调节Ap3A诱导的瞬变。相比之下,Ap4A诱导的瞬变与ATP诱导的瞬变一样,会出现持续时间增加或[Ca2+]i持续升高的情况,而[Ca2+]i峰值没有升高。(3)低浓度佛波酯4β-佛波醇12,13-二丁酸酯(PDB;5 - 10 nM)可消除Ap3A诱导的瞬变,就像消除ADP诱导的瞬变一样,而长时间的Ap4A诱导的瞬变与长时间的ATP诱导的瞬变一样,对高浓度PDB(100 nM)具有抗性。我们提出,Ap3A在大鼠肝细胞中诱导的[Ca2+]i振荡是由介导ADP作用的同一嘌呤受体介导的,而Ap4A诱导的振荡是由介导ATP作用的同一嘌呤受体介导的。

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