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Featured researches published by Tadashi Umemoto.


Bioorganic & Medicinal Chemistry | 2017

Investigation on cellular uptake and pharmacodynamics of DOCK2-inhibitory peptides conjugated with cell-penetrating peptides

Yusuke Adachi; Kotaro Sakamoto; Tadashi Umemoto; Yasunori Fukuda; Akiyoshi Tani; Taiji Asami

Protein-protein interaction between dedicator of cytokinesis 2 (DOCK2) and Ras-related C3 botulinum toxin substrate 1 (Rac1) is an attractive intracellular target for transplant rejection and inflammatory diseases. Recently, DOCK2-selective inhibitory peptides have been discovered, and conjugation with oligoarginine cell-penetrating peptide (CPP) improved inhibitory activity in a cell migration assay. Although a number of CPPs have been reported, oligoarginine was only one example introduced to the inhibitory peptides. In this study, we aimed to confirm the feasibility of CPP-conjugation approach for DOCK2-inhibitory peptides, and select preferable sequences as CPP moiety. First, we evaluated cell permeability of thirteen known CPPs and partial sequences of influenza A viral protein PB1-F2 using an internalization assay system based on luciferin-luciferase reaction, and then selected four CPPs with efficient cellular uptake. Among four conjugates of these CPPs and a DOCK2-inhibitory peptide, the inhibitory activity of a novel CPP, PB1-F2 fragment 5 (PF5), conjugate was comparable to oligoarginine conjugate and higher than that of the non-conjugated peptide. Finally, internalization assay revealed that oligoarginine and PF5 increased the cellular uptake of inhibitory peptides to the same extent. Hence, we demonstrated that CPP-conjugation approach is applicable to the development of novel anti-inflammatory drugs based on DOCK2 inhibition by investigating both cellular uptake and bioactivity.


Archive | 2010

Process for producing nucleoside

Tadashi Umemoto; Yoji Hayase; Shumpei Murata; Kenichi Miyata


Biochemical and Biophysical Research Communications | 2016

Discovery of an artificial peptide agonist to the fibroblast growth factor receptor 1c/βKlotho complex from random peptide T7 phage display

Kotaro Sakamoto; Yayoi Kawata; Yasushi Masuda; Tadashi Umemoto; Takashi Ito; Taiji Asami; Shiro Takekawa; Tetsuya Ohtaki; Hiroshi Inooka


Archive | 2010

Fgf21 cis-element binding substance

Shungo Adachi; 足達 俊吾; Kazunori Nishi; 一紀 西; Tadashi Umemoto; 忠士 梅本; Masahiro Nogami; 真宏 野上; Shoichi Nakao; 勝一 中尾


Bioorganic & Medicinal Chemistry Letters | 2017

Discovery of peptidic miR-21 processing inhibitor by mirror image phage display: A novel method to generate RNA binding D-peptides

Kotaro Sakamoto; Kentaro Otake; Tadashi Umemoto


Archive | 2010

Method for synthesizing nucleic acid

Shumpei Murata; Tadashi Umemoto; Kenichi Miyata; Yoji Hayase


Tetrahedron | 2017

Direct and practical synthesis of 2′-O,4′-C-aminomethylene-bridged nucleic acid purine derivatives by transglycosylation

Tadashi Umemoto; Shinichi Masada; Kenichi Miyata; Mari Ogasawara-Shimizu; Shumpei Murata; Kazunori Nishi; Kazuhiro Ogi; Yoji Hayase; Nobuo Cho


Chemistry Letters | 2017

A Glutamic Acid Analog Bearing an Ethylenediamine Moiety Promotes the Cytosolic Delivery of TAT Peptides

Tadashi Umemoto; Kotaro Sakamoto; Yasunori Fukuda; Yusuke Adachi; Akiyoshi Tani; Taiji Asami


Archive | 2013

Acide nucléique modifié inédit

Shumpei Murata; 俊平 村田; Shinichi Masada; 眞一 政田; N. Miyamoto; 宮本 直樹; Tadashi Umemoto; 忠士 梅本


Archive | 2010

A process for the preparation of nucleoside

Tadashi Umemoto; Yoji Hayase; Shumpei Murata; Kenichi Miyata

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Shumpei Murata

Takeda Pharmaceutical Company

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Kenichi Miyata

Takeda Pharmaceutical Company

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Yoji Hayase

Takeda Pharmaceutical Company

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Kotaro Sakamoto

Takeda Pharmaceutical Company

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Taiji Asami

Takeda Pharmaceutical Company

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Akiyoshi Tani

Takeda Pharmaceutical Company

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Kazunori Nishi

Takeda Pharmaceutical Company

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Shinichi Masada

Takeda Pharmaceutical Company

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Yasunori Fukuda

Takeda Pharmaceutical Company

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Yusuke Adachi

Kyoto Pharmaceutical University

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