Phosphorylation of phospholamban promotes SERCA2a activation by dwarf open reading frame (DWORF)

IF 4.3 2区 生物学 Q2 CELL BIOLOGY
Elisa Bovo, Thomas Jamrozik, Daniel Kahn, Patryk Karkut, Seth L. Robia, Aleksey V. Zima
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Abstract

In cardiac myocytes, the type 2a sarco/endoplasmic reticulum Ca-ATPase (SERCA2a) plays a key role in intracellular Ca regulation. Due to its critical role in heart function, SERCA2a activity is tightly regulated by different mechanisms, including micropeptides. While phospholamban (PLB) is a well-known SERCA2a inhibitor, dwarf open reading frame (DWORF) is a recently identified SERCA2a activator. Since PLB phosphorylation is the most recognized mechanism of SERCA2a activation during adrenergic stress, we studied whether PLB phosphorylation also affects SERCA2a regulation by DWORF. By using confocal Ca imaging in a HEK293 expressing cell system, we analyzed the effect of the co-expression of PLB and DWORF using a bicistronic construct on SERCA2a-mediated Ca uptake. Under these conditions of matched expression of PLB and DWORF, we found that SERCA2a inhibition by non-phosphorylated PLB prevails over DWORF activating effect. However, when PLB is phosphorylated at PKA and CaMKII sites, not only PLB's inhibitory effect was relieved, but SERCA2a was effectively activated by DWORF. Förster resonance energy transfer (FRET) analysis between SERCA2a and DWORF showed that DWORF has a higher relative affinity for SERCA2a when PLB is phosphorylated. Thus, SERCA2a regulation by DWORF responds to the PLB phosphorylation status, suggesting that DWORF might contribute to SERCA2a activation during conditions of adrenergic stress.

Abstract Image

Abstract Image

磷酸化磷脂酰亚胺通过矮小开放阅读框(DWORF)促进 SERCA2a 的激活
在心肌细胞中,2a 型肌浆/内质网 Ca-ATP 酶(SERCA2a)在细胞内 Ca 调节中起着关键作用。由于其在心脏功能中的关键作用,SERCA2a 的活性受到不同机制(包括微肽)的严格调控。磷脂酰胆碱(PLB)是众所周知的 SERCA2a 抑制剂,而矮人开放阅读框(DWORF)则是最近发现的 SERCA2a 激活剂。由于 PLB 磷酸化是肾上腺素能应激过程中 SERCA2a 激活的最公认机制,我们研究了 PLB 磷酸化是否也会影响 DWORF 对 SERCA2a 的调控。通过在 HEK293 表达细胞系统中使用共焦钙成像技术,我们分析了使用双组分构建体共同表达 PLB 和 DWORF 对 SERCA2a 介导的钙吸收的影响。在 PLB 和 DWORF 匹配表达的条件下,我们发现非磷酸化 PLB 对 SERCA2a 的抑制作用大于 DWORF 的激活作用。然而,当 PLB 在 PKA 和 CaMKII 位点磷酸化时,不仅 PLB 的抑制作用得到缓解,而且 SERCA2a 也被 DWORF 有效激活。SERCA2a和DWORF之间的佛斯特共振能量转移(FRET)分析表明,当PLB磷酸化时,DWORF对SERCA2a的亲和力更高。因此,DWORF 对 SERCA2a 的调控响应于 PLB 的磷酸化状态,这表明 DWORF 可能有助于肾上腺素能应激条件下的 SERCA2a 激活。
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来源期刊
Cell calcium
Cell calcium 生物-细胞生物学
CiteScore
8.70
自引率
5.00%
发文量
115
审稿时长
35 days
期刊介绍: Cell Calcium covers the field of calcium metabolism and signalling in living systems, from aspects including inorganic chemistry, physiology, molecular biology and pathology. Topic themes include: Roles of calcium in regulating cellular events such as apoptosis, necrosis and organelle remodelling Influence of calcium regulation in affecting health and disease outcomes
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