Publications by authors named "Kei Nagatoshi"

Article Synopsis
  • Cells can communicate and exert forces on the extracellular matrix (ECM), with fibronectin (FN) being a key component that helps form structures called FN pillars in developing quail embryos.
  • FN pillars form between the somitic mesoderm and endoderm and are linked to long filopodia from somite epithelial cells; their formation relies on specific proteins like Ena/VASP, α5β1-integrins, and talin.
  • The study reveals that the formation and alignment of FN pillars are influenced by the pulsatile blood flow from the dorsal aorta, suggesting a novel mechanism for how these pillars develop and contribute to somite morphogenesis.
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N-myristoylation of eukaryotic cellular proteins has been recognized as a modification that occurs mainly on cytoplasmic proteins. In this study, we examined the membrane localization, membrane integration, and intracellular localization of four recently identified human N-myristoylated proteins with predicted transmembrane domains. As a result, it was found that protein Lunapark, the human ortholog of yeast protein Lnp1p that has recently been found to be involved in network formation of the endoplasmic reticulum (ER), is an N-myristoylated polytopic integral membrane protein.

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To establish a strategy for the comprehensive identification of human N-myristoylated proteins, the susceptibility of human cDNA clones to protein N-myristoylation was evaluated by metabolic labeling and MS analyses of proteins expressed in an insect cell-free protein synthesis system. One-hundred-and-forty-one cDNA clones with N-terminal Met-Gly motifs were selected as potential candidates from approximately 2000 Kazusa ORFeome project human cDNA clones, and their susceptibility to protein N-myristoylation was evaluated using fusion proteins, in which the N-terminal ten amino acid residues were fused to an epitope-tagged model protein. As a result, the products of 29 out of 141 cDNA clones were found to be effectively N-myristoylated.

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