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A Novel Glycerophosphodiester Phosphodiesterase,GDE5, Controls Skeletal Muscle Development via a Non-enzymatic Mechanism
Authors:Yuri Okazaki  Noriyasu Ohshima  Ikumi Yoshizawa  Yasutomi Kamei  Stefania Mariggiò   Keiko Okamoto  Masahiro Maeda  Yoshihito Nogusa  Yuichiro Fujioka  Takashi Izumi  Yoshihiro Ogawa  Yoshitsugu Shiro  Masanobu Wada  Norihisa Kato  Daniela Corda  Noriyuki Yanaka
Abstract:Mammalian glycerophosphodiester phosphodiesterases (GP-PDEs) have been identified recently and shown to be implicated in several physiological functions. This study isolated a novel GP-PDE, GDE5, and showed that GDE5 selectively hydrolyzes glycerophosphocholine (GroPCho) and controls skeletal muscle development. We show that GDE5 expression was reduced in atrophied skeletal muscles in mice and that decreasing GDE5 abundance promoted myoblastic differentiation, suggesting that decreased GDE5 expression has a counter-regulatory effect on the progression of skeletal muscle atrophy. Forced expression of full-length GDE5 in cultured myoblasts suppressed myogenic differentiation. Unexpectedly, a truncated GDE5 construct (GDE5ΔC471), which contained a GP-PDE sequence identified in other GP-PDEs but lacked GroPCho phosphodiesterase activity, showed a similar inhibitory effect. Furthermore, transgenic mice specifically expressing GDE5ΔC471 in skeletal muscle showed less skeletal muscle mass, especially type II fiber-rich muscle. These results indicate that GDE5 negatively regulates skeletal muscle development even without GroPCho phosphodiesterase activity, providing novel insight into the biological significance of mammalian GP-PDE function in a non-enzymatic mechanism.
Keywords:Cell Differentiation   Glycerolipid   Glycerophospholipid   Phosphodiesterases   Skeletal Muscle   Glycerophosphocholine   Glycerophosphodiester   Myogenesis
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