Erck C, Frank R, Wehland J
Abteilung Zellbiologie, Gesellschaft fuer Biotechnologische Forschung, Braunschweig, Germany.
Neurochem Res. 2000 Jan;25(1):5-10. doi: 10.1023/a:1007523028834.
Tubulins and microtubules are subjected to several post-translational modifications of which the reversible detyrosination/tyrosination of the carboxy-terminal end of most alpha-tubulins has been extensively analysed. This modification cycle involves a specific carboxypeptidase and the activity of the tubulin-tyrosine ligase (TTL). The true physiological function of TTL has so far not been established. This review describes the purification of TTL to homogeneity by biochemical methods, its in vitro properties and the generation of monoclonal antibodies. These mabs not only enabled a very convenient and rapid purification of TTL by immunoaffinity chromatography but also its extensive characterization by protein sequencing, which led to the isolation of the full length cDNA. With this information, gene disruption should be feasible in order to determine the physiological significance of the tyrosination cycle.
微管蛋白和微管会经历多种翻译后修饰,其中大多数α-微管蛋白羧基末端的可逆去酪氨酸化/酪氨酸化已得到广泛分析。这种修饰循环涉及一种特定的羧肽酶和微管蛋白酪氨酸连接酶(TTL)的活性。迄今为止,TTL的真正生理功能尚未确定。本综述描述了通过生化方法将TTL纯化至同质状态、其体外特性以及单克隆抗体的产生。这些单克隆抗体不仅能够通过免疫亲和色谱非常方便快捷地纯化TTL,还能通过蛋白质测序对其进行广泛表征,从而分离出全长cDNA。有了这些信息,通过基因敲除来确定酪氨酸化循环的生理意义应该是可行的。