Dynamic and coordinated single-molecular interactions at TM4SF5-enriched microdomains guide invasive behaviors in 2- and 3-dimensional environments

Membrane proteins sense extracellular cues and transduce intracellular signaling to coordinate directionality and speed during cellular migration. They are often localized to specific regions, as with lipid rafts or tetraspanin-enriched microdomains; however, the dynamic interactions of tetraspanins...

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Published in	The FASEB journal Vol. 31; no. 4; p. 1461
Main Authors	Kim, Hye-Jin, Kwon, Sojung, Nam, Seo Hee, Jung, Jae Woo, Kang, Minkyung, Ryu, Jihye, Kim, Ji Eon, Cheong, Jin-Gyu, Cho, Chang Yun, Kim, Somi, Song, Dae-Geun, Kim, Yong-Nyun, Kim, Tai Young, Jung, Min-Kyo, Lee, Kyung-Min, Pack, Chan-Gi, Lee, Jung Weon
Format	Journal Article
Language	English
Published	United States 01.04.2017
Subjects	Cell Line, Tumor Cell Movement Cholesterol - metabolism Glycosylation HEK293 Cells Hepatocytes - metabolism Hepatocytes - physiology Hepatocytes - ultrastructure Humans Integrin alpha5 - metabolism Lipoylation Membrane Microdomains - metabolism Membrane Microdomains - ultrastructure Membrane Proteins - metabolism Protein Binding Protein Processing, Post-Translational Receptor, Epidermal Growth Factor - metabolism migration 3D cell culture membrane proteins protein interaction affinity FCCS
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Abstract	Membrane proteins sense extracellular cues and transduce intracellular signaling to coordinate directionality and speed during cellular migration. They are often localized to specific regions, as with lipid rafts or tetraspanin-enriched microdomains; however, the dynamic interactions of tetraspanins with diverse receptors within tetraspanin-enriched microdomains on cellular surfaces remain largely unexplored. Here, we investigated effects of tetraspan(in) TM4SF5 (transmembrane 4 L6 family member 5)-enriched microdomains (T ERMs) on the directionality of cell migration. Physical association of TM4SF5 with epidermal growth factor receptor (EGFR) and integrin α5 was visualized by live fluorescence cross-correlation spectroscopy and higher-resolution microscopy at the leading edge of migratory cells, presumably forming TM4SF5-enriched microdomains. Whereas TM4SF5 and EGFR colocalized at the migrating leading region more than at the rear, TM4SF5 and integrin α5 colocalized evenly throughout cells. Cholesterol depletion and disruption in TM4SF5 post-translational modifications, including -glycosylation and palmitoylation, altered TM4SF5 interactions and cellular localization, which led to less cellular migration speed and directionality in 2- or 3-dimensional conditions. TM4SF5 controlled directional cell migration and invasion, and importantly, these TM4SF5 functions were dependent on cholesterol, TM4SF5 post-translational modifications, and EGFR and integrin α5 activity. Altogether, we showed that TM4SF5 dynamically interacted with EGFR and integrin α5 in migratory cells to control directionality and invasion.-Kim, H.-J., Kwon, S., Nam, S. H., Jung, J. W., Kang, M., Ryu, J., Kim, J. E., Cheong, J.-G., Cho, C. Y., Kim, S., Song, D.-G., Kim, Y.-N., Kim, T. Y., Jung, M.-K., Lee, K.-M., Pack, C.-G., Lee, J. W. Dynamic and coordinated single-molecular interactions at TM4SF5-enriched microdomains guide invasive behaviors in 2- and 3-dimensional environments.
AbstractList	Membrane proteins sense extracellular cues and transduce intracellular signaling to coordinate directionality and speed during cellular migration. They are often localized to specific regions, as with lipid rafts or tetraspanin-enriched microdomains; however, the dynamic interactions of tetraspanins with diverse receptors within tetraspanin-enriched microdomains on cellular surfaces remain largely unexplored. Here, we investigated effects of tetraspan(in) TM4SF5 (transmembrane 4 L6 family member 5)-enriched microdomains (T ERMs) on the directionality of cell migration. Physical association of TM4SF5 with epidermal growth factor receptor (EGFR) and integrin α5 was visualized by live fluorescence cross-correlation spectroscopy and higher-resolution microscopy at the leading edge of migratory cells, presumably forming TM4SF5-enriched microdomains. Whereas TM4SF5 and EGFR colocalized at the migrating leading region more than at the rear, TM4SF5 and integrin α5 colocalized evenly throughout cells. Cholesterol depletion and disruption in TM4SF5 post-translational modifications, including -glycosylation and palmitoylation, altered TM4SF5 interactions and cellular localization, which led to less cellular migration speed and directionality in 2- or 3-dimensional conditions. TM4SF5 controlled directional cell migration and invasion, and importantly, these TM4SF5 functions were dependent on cholesterol, TM4SF5 post-translational modifications, and EGFR and integrin α5 activity. Altogether, we showed that TM4SF5 dynamically interacted with EGFR and integrin α5 in migratory cells to control directionality and invasion.-Kim, H.-J., Kwon, S., Nam, S. H., Jung, J. W., Kang, M., Ryu, J., Kim, J. E., Cheong, J.-G., Cho, C. Y., Kim, S., Song, D.-G., Kim, Y.-N., Kim, T. Y., Jung, M.-K., Lee, K.-M., Pack, C.-G., Lee, J. W. Dynamic and coordinated single-molecular interactions at TM4SF5-enriched microdomains guide invasive behaviors in 2- and 3-dimensional environments.
Author	Pack, Chan-Gi Lee, Kyung-Min Lee, Jung Weon Song, Dae-Geun Ryu, Jihye Kim, Yong-Nyun Jung, Jae Woo Kang, Minkyung Cho, Chang Yun Kim, Tai Young Jung, Min-Kyo Kim, Hye-Jin Kim, Somi Nam, Seo Hee Kwon, Sojung Kim, Ji Eon Cheong, Jin-Gyu
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SubjectTerms	Cell Line, Tumor Cell Movement Cholesterol - metabolism Glycosylation HEK293 Cells Hepatocytes - metabolism Hepatocytes - physiology Hepatocytes - ultrastructure Humans Integrin alpha5 - metabolism Lipoylation Membrane Microdomains - metabolism Membrane Microdomains - ultrastructure Membrane Proteins - metabolism Protein Binding Protein Processing, Post-Translational Receptor, Epidermal Growth Factor - metabolism
Title	Dynamic and coordinated single-molecular interactions at TM4SF5-enriched microdomains guide invasive behaviors in 2- and 3-dimensional environments
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