Wooldridge Anne A, Fortner Christopher N, Lontay Beata, Akimoto Takayuki, Neppl Ronald L, Facemire Carie, Datto Michael B, Kwon Ashley, McCook Everett, Li Ping, Wang Shiliang, Thresher Randy J, Miller Sara E, Perriard Jean-Claude, Gavin Timothy P, Hickner Robert C, Coffman Thomas M, Somlyo Avril V, Yan Zhen, Haystead Timothy A J
Department of Pharmacology, Medicine, Duke University, Medical Center, Durham, North Carolina 27710, USA.
J Biol Chem. 2008 Apr 25;283(17):11850-9. doi: 10.1074/jbc.M708628200. Epub 2008 Feb 29.
In vivo protein kinases A and G (PKA and PKG) coordinately phosphorylate a broad range of substrates to mediate their various physiological effects. The functions of many of these substrates have yet to be defined genetically. Herein we show a role for smoothelin-like protein 1 (SMTNL1), a novel in vivo target of PKG/PKA, in mediating vascular adaptations to exercise. Aortas from smtnl1(-/-) mice exhibited strikingly enhanced vasorelaxation before exercise, similar in extent to that achieved after endurance training of wild-type littermates. Additionally, contractile responses to alpha-adrenergic agonists were greatly attenuated. Immunological studies showed SMTNL1 is expressed in smooth muscle and type 2a striated muscle fibers. Consistent with a role in adaptations to exercise, smtnl1(-/-) mice also exhibited increased type 2a fibers before training and better performance after forced endurance training compared smtnl1(+/+) mice. Furthermore, exercise was found to reduce expression of SMTNL1, particularly in female mice. In both muscle types, SMTNL1 is phosphorylated at Ser-301 in response to adrenergic signals. In vitro SMTNL1 suppresses myosin phosphatase activity through a substrate-directed effect, which is relieved by Ser-301 phosphorylation. Our findings suggest roles for SMTNL1 in cGMP/cAMP-mediated adaptations to exercise through mechanisms involving direct modulation of contractile activity.
体内蛋白激酶A和G(PKA和PKG)协同磷酸化多种底物,以介导其各种生理效应。许多这些底物的功能尚未通过遗传学方法确定。在此我们展示了平滑肌样蛋白1(SMTNL1),一种PKG/PKA的新型体内靶点,在介导血管对运动的适应性方面的作用。来自smtnl1(-/-)小鼠的主动脉在运动前表现出显著增强的血管舒张,其程度与野生型同窝小鼠耐力训练后所达到的程度相似。此外,对α-肾上腺素能激动剂的收缩反应大大减弱。免疫学研究表明SMTNL1在平滑肌和2a型横纹肌纤维中表达。与在运动适应性中的作用一致,与smtnl1(+/+)小鼠相比,smtnl1(-/-)小鼠在训练前也表现出2a型纤维增加,并且在强制耐力训练后表现更好。此外,发现运动可降低SMTNL1的表达,尤其是在雌性小鼠中。在这两种肌肉类型中,SMTNL1在Ser-301位点响应肾上腺素能信号而被磷酸化。在体外,SMTNL1通过底物导向效应抑制肌球蛋白磷酸酶活性,而Ser-301磷酸化可解除这种抑制。我们的研究结果表明SMTNL1通过涉及直接调节收缩活性的机制在cGMP/cAMP介导的运动适应性中发挥作用。
