Baran Irina
Biophysics Department, Faculty of Medicine, University of Medicine and Pharmacy Carol Davila, Bucharest, Romania.
Biophys J. 2005 Aug;89(2):979-98. doi: 10.1529/biophysj.105.059238. Epub 2005 May 20.
A large amount of data and observations on inositol 1,4,5-trisphosphate (IP(3)) binding to the IP(3) receptor/Ca(2+) channel, the steady-state activity of the channel, and its inactivation by IP(3) can be explained by assuming one activation and one inhibition module, both allosterically operated by Ca(2+), IP(3), and ATP, and one adaptation element, driven by IP(3), Ca(2+), and the interconversion between two possible conformations of the receptor. The adaptation module becomes completely insensitive to a second IP(3) pulse within 80 s. Observed kinetic responses are well reproduced if, in addition, two module open states are rendered inactive by the current charge carrier Mn(2+). The inactivation time constants are 59 s in the activation, and 0.75 s in the adaptation module. The in vivo open probability of the channel is predicted to be almost in coincidence with the behavior in lipid bilayers for IP(3) levels of 0.2 and 2 microM and one-order-higher at 0.02 microM IP(3), whereas at 180 microM IP(3) the maximal in vivo activity may be 2.5-orders higher than in bilayers and restricted to a narrower Ca(2+) domain (approximately 10 microM-wide versus approximately 100 microM-wide). IP(3) is likely to inhibit channel activity at < or =120 nM Ca(2+) in vivo.
关于肌醇1,4,5 -三磷酸(IP(3))与IP(3)受体/Ca(2+)通道的结合、通道的稳态活性及其被IP(3)灭活的大量数据和观察结果,可以通过假设一个激活模块和一个抑制模块来解释,这两个模块均由Ca(2+)、IP(3)和ATP进行变构调节,还有一个适应元件,由IP(3)、Ca(2+)以及受体两种可能构象之间的相互转化驱动。该适应模块在80秒内对第二个IP(3)脉冲完全不敏感。此外,如果当前的电荷载体Mn(2+)使两个模块开放状态失活,那么观察到的动力学响应就能得到很好的重现。激活模块中的失活时间常数为59秒,适应模块中为0.75秒。对于0.2和2微摩尔的IP(3)水平,通道在体内的开放概率预计几乎与在脂质双层中的行为一致,而在0.02微摩尔IP(3)时则高一阶;然而,在180微摩尔IP(3)时,体内的最大活性可能比在双层中高2.5阶,并且局限于更窄的Ca(2+)域(约10微摩尔宽,而双层中约100微摩尔宽)。在体内,IP(3)在Ca(2+)浓度≤120纳摩尔时可能会抑制通道活性。