Segura-Roman Ashley, Citron Y Rose, Shin Myungsun, Sindoni Nicole, Maya-Romero Alex, Rapp Simon, Goul Claire, Mancias Joseph D, Zoncu Roberto
bioRxiv. 2024 Aug 6:2024.08.06.606738. doi: 10.1101/2024.08.06.606738.
Protein Kinase A (PKA) is regulated spatially and temporally via scaffolding of its catalytic (Cα/β) and regulatory (RI/RII) subunits by the A-kinase-anchoring proteins (AKAP). PKA engages in poorly understood interactions with autophagy, a key degradation pathway for neuronal cell homeostasis, partly via its AKAP11 scaffold. Mutations in AKAP11 drive schizophrenia and bipolar disorders (SZ-BP) through unknown mechanisms. Through proteomic-based analysis of immunopurified lysosomes, we identify the Cα-RIα-AKAP11 holocomplex as a prominent autophagy-associated protein kinase complex. AKAP11 scaffolds Cα-RIα to the autophagic machinery via its LC3-interacting region (LIR), enabling both PKA regulation by upstream signals, and its autophagy-dependent degradation. We identify Ser83 on the RIα linker-hinge region as an AKAP11-dependent phospho-residue that modulates RIα-Cα binding and cAMP-induced PKA activation. Decoupling AKAP11-PKA from autophagy alters Ser83 phosphorylation, supporting an autophagy-dependent checkpoint for PKA signaling. Ablating AKAP11 in induced pluripotent stem cell-derived neurons reveals dysregulation of multiple pathways for neuronal homeostasis. Thus, the autophagosome is a novel platform that modulate PKA signaling, providing a possible mechanistic link to SZ/BP pathophysiology.
蛋白激酶A(PKA)通过A激酶锚定蛋白(AKAP)对其催化亚基(Cα/β)和调节亚基(RI/RII)进行时空调控。PKA与自噬存在着尚不清楚的相互作用,自噬是神经元细胞稳态的关键降解途径,部分是通过其AKAP11支架实现的。AKAP11中的突变通过未知机制导致精神分裂症和双相情感障碍(SZ-BP)。通过基于蛋白质组学的免疫纯化溶酶体分析,我们确定Cα-RIα-AKAP11全复合物是一种突出的自噬相关蛋白激酶复合物。AKAP11通过其LC3相互作用区域(LIR)将Cα-RIα支架连接到自噬机制上,既使PKA能受上游信号调控,又能实现其依赖自噬的降解。我们确定RIα连接子-铰链区域的Ser83是一个依赖AKAP11的磷酸化残基,它调节RIα-Cα结合和cAMP诱导的PKA激活。将AKAP11-PKA与自噬解偶联会改变Ser83的磷酸化,支持PKA信号传导的自噬依赖性检查点。在诱导多能干细胞衍生的神经元中敲除AKAP11会揭示神经元稳态的多种途径失调。因此,自噬体是调节PKA信号传导的一个新平台,为SZ/BP病理生理学提供了可能的机制联系。
