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重新激活的黑素细胞运动性:双向色素颗粒运输的差异调节和核苷酸需求

Reactivated melanophore motility: differential regulation and nucleotide requirements of bidirectional pigment granule transport.

作者信息

Rozdzial M M, Haimo L T

出版信息

J Cell Biol. 1986 Dec;103(6 Pt 2):2755-64. doi: 10.1083/jcb.103.6.2755.

Abstract

To study the molecular basis for organized pigment granule transport, procedures were developed to lyse melanophores of Tilapia mossambica under conditions in which pigment granule movements could be reactivated. Gentle lysis of the melanophores resulted in a permeabilized cell model, which, in the absence of exogenous ATP, could undergo multiple rounds of pigment granule aggregation and dispersion when sequentially challenged with epinephrine and cAMP. Both directions of transport required ATP, since aggregation or dispersion in melanophores depleted of nucleotides could be reactivated only upon addition of MgATP or MgATP plus cAMP, respectively. Differences between the nucleotide sensitivities for aggregation and dispersion were demonstrated by observations that aggregation had a lower apparent Km for ATP than did dispersion and could be initiated at a lower ATP concentration. Moreover, aggregation could be initiated by ADP, but only dispersion could be reactivated by the thiophosphate ATP analog, ATP gamma S. The direction of pigment transport was determined solely by cAMP, since pigment granules undergoing dispersion reaggregated when cAMP was removed, and those undergoing aggregation dispersed when cAMP was added. These results provide evidence that pigment granule motility may be based on two distinct mechanisms that are differentially activated and regulated to produce bidirectional movements.

摘要

为了研究有组织的色素颗粒运输的分子基础,我们开发了一些程序,以便在能够重新激活色素颗粒运动的条件下裂解莫桑比克罗非鱼的黑素细胞。对黑素细胞进行温和裂解会产生一种通透细胞模型,在没有外源ATP的情况下,当依次用肾上腺素和cAMP刺激时,该模型可经历多轮色素颗粒聚集和分散。两个运输方向都需要ATP,因为在耗尽核苷酸的黑素细胞中,聚集或分散分别只有在添加MgATP或MgATP加cAMP后才能重新激活。通过观察发现聚集对ATP的表观Km低于分散,并且可以在较低的ATP浓度下启动,从而证明了聚集和分散对核苷酸敏感性的差异。此外,ADP可以启动聚集,但只有硫代磷酸ATP类似物ATPγS可以重新激活分散。色素运输的方向仅由cAMP决定,因为当去除cAMP时,正在分散的色素颗粒会重新聚集,而当添加cAMP时,正在聚集的色素颗粒会分散。这些结果提供了证据,表明色素颗粒运动可能基于两种不同的机制,它们被不同地激活和调节以产生双向运动。

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