Litcius/Paper detail

RhoA-GTPase Modulates Neurite Outgrowth by Regulating the Expression of Spastin and p60-Katanin

Dandan Tan, Haowen Zhang, Junyao Deng, Jingmin Liu, Jinkun Wen, Li-xia Li, Xianghai Wang, Mengjie Pan, Xiaofang Hu, Jiasong Guo

2020Cells28 citationsDOIOpen Access PDF

Abstract

RhoA-GTPase (RhoA) is widely regarded as a key molecular switch to inhibit neurite outgrowth by rigidifying the actin cytoskeleton. However, during neurite outgrowth, whether and how microtubule dynamics are regulated by RhoA remains to be elucidated. Herein, CT04 and Y27632 were used to inactivate RhoA and its downstream effector Rho-associated coiled coil-forming kinase (ROCK), while the RhoAQ63L lentiviral vector was utilized to overexpress the constitutively activated RhoA in dorsal root ganglion (DRG) neurons or neuronal differentiated PC12 cells. The current data illustrate that the RhoA signaling pathway negatively modulates neurite outgrowth and elevates the expression of Glu-tubulin (a marker for a stabilized microtubule). Meanwhile, the microtubule-severing proteins spastin and p60-katanin were downregulated by the RhoA signaling pathway. When spastin and p60-katanin were knocked down, the effects of RhoA inhibition on neurite outgrowth were significantly reversed. Taken together, this study demonstrates that the RhoA pathway-mediated inhibition of neurite outgrowth is not only related to the modulation of microfilament dynamics but is also attributable to the regulation of the expression of spastin and p60-katanin and thus influences microtubule dynamics.

Topics & Concepts

RHOANeuriteCell biologyMicrotubuleSmall GTPaseGTPaseCytoskeletonChemistryActinActin cytoskeletonSignal transductionBiologyBiochemistryCellIn vitroCellular Mechanics and InteractionsNerve injury and regenerationCellular transport and secretion
RhoA-GTPase Modulates Neurite Outgrowth by Regulating the Expression of Spastin and p60-Katanin | Litcius