From the Department of Molecular, Cellular, and Developmental Biology and Neuroscience Research Institute, University of California, Santa Barbara, California 93106-9625.
the Department of Systems Pharmacology and Translational Therapeutics, Perelman School of Medicine, University of Pennsylvania, Philadelphia, Pennsylvania 19104, and.
J Biol Chem. 2018 Apr 13;293(15):5478-5491. doi: 10.1074/jbc.RA117.000874. Epub 2018 Feb 23.
Syntaxins are a conserved family of SNARE proteins and contain C-terminal transmembrane anchors required for their membrane fusion activity. Here we show that Stx3 (syntaxin 3) unexpectedly also functions as a nuclear regulator of gene expression. We found that alternative splicing creates a soluble isoform that we termed Stx3S, lacking the transmembrane anchor. Soluble Stx3S binds to the nuclear import factor RanBP5 (RAN-binding protein 5), targets to the nucleus, and interacts physically and functionally with several transcription factors, including ETV4 (ETS variant 4) and ATF2 (activating transcription factor 2). Stx3S is differentially expressed in normal human tissues, during epithelial cell polarization, and in breast cancer normal breast tissue. Inhibition of endogenous Stx3S expression alters the expression of cancer-associated genes and promotes cell proliferation. Similar nuclear-targeted, soluble forms of other syntaxins were identified, suggesting that nuclear signaling is a conserved, novel function common among these membrane-trafficking proteins.
突触融合蛋白是 SNARE 蛋白家族的一个保守亚家族,包含 C 末端跨膜锚,这是其膜融合活性所必需的。在这里,我们发现 Stx3(突触融合蛋白 3)出人意料地也作为核基因表达的调节剂发挥作用。我们发现,选择性剪接产生了一种可溶性异构体,我们将其命名为 Stx3S,它缺乏跨膜锚。可溶性 Stx3S 与核输入因子 RanBP5(RAN 结合蛋白 5)结合,靶向细胞核,并与包括 ETV4(ETS 变体 4)和 ATF2(激活转录因子 2)在内的多种转录因子发生物理和功能相互作用。Stx3S 在正常人类组织、上皮细胞极化过程中以及乳腺癌-正常乳腺组织中差异表达。内源性 Stx3S 表达的抑制改变了与癌症相关基因的表达,并促进了细胞增殖。其他突触融合蛋白的类似核靶向可溶性形式也被鉴定出来,这表明核信号是这些膜运输蛋白共有的保守的新型功能。
