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Precise control of microtubule disassembly in living cells
Authors:Grace Y Liu  Shiau&#x;Chi Chen  Gang&#x;Hui Lee  Kritika Shaiv  Pin&#x;Yu Chen  Hsuan Cheng  Shi&#x;Rong Hong  Wen&#x;Ting Yang  Shih&#x;Han Huang  Ya&#x;Chu Chang  Hsien&#x;Chu Wang  Ching&#x;Lin Kao  Pin&#x;Chiao Sun  Ming&#x;Hong Chao  Yian&#x;Ying Lee  Ming&#x;Jer Tang  Yu&#x;Chun Lin
Institution:1. Institute of Molecular Medicine, National Tsing Hua University, Hsinchu Taiwan ; 2. Department of Physiology, College of Medicine, National Cheng Kung University, Tainan Taiwan ; 3. International Center for Wound Repair and Regeneration, National Cheng Kung University, Tainan Taiwan ; 4. Department of Medical Science, National Tsing Hua University, Hsinchu Taiwan
Abstract:Microtubules tightly regulate various cellular activities. Our understanding of microtubules is largely based on experiments using microtubule‐targeting agents, which, however, are insufficient to dissect the dynamic mechanisms of specific microtubule populations, due to their slow effects on the entire pool of microtubules. To overcome this technological limitation, we have used chemo and optogenetics to disassemble specific microtubule subtypes, including tyrosinated microtubules, primary cilia, mitotic spindles, and intercellular bridges, by rapidly recruiting engineered microtubule‐cleaving enzymes onto target microtubules in a reversible manner. Using this approach, we show that acute microtubule disassembly swiftly halts vesicular trafficking and lysosomal dynamics. It also immediately triggers Golgi and ER reorganization and slows the fusion/fission of mitochondria without affecting mitochondrial membrane potential. In addition, cell rigidity is increased after microtubule disruption owing to increased contractile stress fibers. Microtubule disruption furthermore prevents cell division, but does not cause cell death during interphase. Overall, the reported tools facilitate detailed analysis of how microtubules precisely regulate cellular architecture and functions.
Keywords:intercellular bridge  microtubule  mitotic spindle  primary cilium  spastin
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