4.7 Article

SLAC2B-dependent microtubule acetylation regulates extracellular matrix-mediated intracellular TM4SF5 traffic to the plasma membranes

FASEB JOURNAL (2021)

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Journal

FASEB JOURNAL
Volume 35, Issue 3, Pages -

Publisher

WILEY
DOI: 10.1096/fj.202002138RR

Keywords

cell migration; fibronectin; SLAC2B; tubulin acetylation; vesicle traffic

Categories

Biochemistry & Molecular Biology Biology Cell Biology

Funding

  1. Basic Science Research Program through the National Research Foundation of Korea (NRF) - Ministry of Science, ICT & Future Planning [NRF-2020R1I1A1A01070020, NRF-2018M3A9C8020027, 2020R1A2C3008993]
  2. Tumor Microenvironment GCRC [2011-0030001]
  3. National Research Foundation of Korea [2020R1A2C3008993, 2018M3A9C8020027] Funding Source: Korea Institute of Science & Technology Information (KISTI), National Science & Technology Information Service (NTIS)

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This study showed that cell adhesion to fibronectin can enhance the translocation of TM4SF5 vesicles to the leading edges, while microtubule acetylation plays a regulatory role in this process. The coordinated actions of paxillin, SLAC2B, and HDAC6 are essential for controlling the intracellular traffic of TM4SF5 vesicles towards the leading edges, leading to TM4SF5-dependent cell migration.
Transmembrane 4 L six family member 5 (TM4SF5) translocates intracellularly and promotes cell migration, but how subcellular TM4SF5 traffic is regulated to guide cellular migration is unknown. We investigated the influences of the extracellular environment and intracellular signaling on the TM4SF5 traffic with regard to migration directionality. Cell adhesion to fibronectin (FN) but not poly-l-lysine enhanced the traffic velocity and straightness of the TM4SF5(WT) (but not palmitoylation-deficient mutant TM4SF5Pal-) toward the leading edges, depending on tubulin acetylation. Acetylated-microtubules in SLAC2B-positive cells reached mostly the juxtanuclear regions, but reached-out toward the leading edges upon SLAC2B suppression. TM4SF5 expression caused SLAC2B not to be localized at the leading edges. TM4SF5 colocalization with HDAC6 depended on paxillin expression. The trimeric complex consisting of TM4SF5, HDAC6, and SLAC2B might, thus, be enriched at the perinuclear cytosols toward the leading edges. More TM4SF5(WT) translocation to the leading edges was possible when acetylated-microtubules reached the frontal edges following HDAC6 inhibition by paxillin presumably at new cell-FN adhesions, leading to persistent cell migration. Collectively, this study revealed that cell-FN adhesion and microtubule acetylation could control intracellular traffic of TM4SF5 vesicles to the leading edges via coordinated actions of paxillin, SLAC2B, and HDAC6, leading to TM4SF5-dependent cell migration.

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