Wadsworth Center, New York State Department of Health, Albany, NY 12201, USA.
J Biol Chem. 2012 Aug 31;287(36):30328-35. doi: 10.1074/jbc.M112.383109. Epub 2012 Jul 6.
Ryanodine receptor types 1 (RyR1) and 2 (RyR2) are calcium release channels that are highly enriched in skeletal and cardiac muscle, respectively, where they play an essential role in excitation-contraction coupling. Apocalmodulin (apo-CaM) weakly activates RyR1 but inhibits RyR2, whereas Ca(2+)-calmodulin inhibits both isoforms. Previous cryo-EM studies showed distinctly different binding locations on RyR1 for the two states of CaM. However, recent studies employing FRET appear to challenge these findings. Here, using cryo-EM, we have determined that a CaM mutant that is incapable of binding calcium binds to RyR1 at the apo site, regardless of the calcium concentration. We have also re-determined the location of RyR1-bound Ca(2+)-CaM using uniform experimental conditions. Our results show the existence of the two overlapping but distinct binding sites for CaM in RyR1 and imply that the binding location switch is due to Ca(2+) binding to CaM, as opposed to direct effects of Ca(2+) on RyR1. We also discuss explanations that could resolve the apparent conflict between the cryo-EM and FRET results. Interestingly, apo-CaM binds to RyR2 at a similar binding location to that of Ca(2+)-CaM on RyR1, in seeming agreement with the inhibitory effects of these two forms of CaM on their respective receptors.
兰尼碱受体 1 型 (RyR1) 和 2 型 (RyR2) 是钙释放通道,分别在骨骼肌和心肌中高度富集,在兴奋-收缩耦联中发挥着重要作用。钙调蛋白 (apo-CaM) 对 RyR1 的激活作用较弱,但对 RyR2 具有抑制作用,而 Ca2+-钙调蛋白则抑制两种同工酶。先前的冷冻电镜研究显示,在两种 CaM 状态下,RyR1 上的结合位置明显不同。然而,最近采用 FRET 的研究似乎对这些发现提出了挑战。在这里,我们使用冷冻电镜确定了一种不能结合钙离子的 CaM 突变体,无论钙离子浓度如何,它都与 RyR1 的 apo 位点结合。我们还使用统一的实验条件重新确定了 RyR1 结合的 Ca(2+)-CaM 的位置。我们的结果表明,RyR1 中存在两个重叠但不同的 CaM 结合位点,并暗示结合位置的切换是由于 CaM 结合钙离子,而不是钙离子对 RyR1 的直接影响。我们还讨论了可以解决冷冻电镜和 FRET 结果之间明显冲突的解释。有趣的是,apo-CaM 与 RyR2 的结合位置与 RyR1 上 Ca(2+)-CaM 的结合位置相似,这似乎与这两种形式的 CaM 对各自受体的抑制作用一致。
