Tamotsu Furumai
Bristol-Myers Squibb
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Publication
Featured researches published by Tamotsu Furumai.
Journal of Biomolecular NMR | 1995
Keith L. Constantine; Mark S. Friedrichs; David J. Detlefsen; Maki Nishio; Mitsuaki Tsunakawa; Tamotsu Furumai; Hiroaki Ohkuma; Toshikazu Oki; Susan E. Hill; Robert E. Bruccoleri; Pin-Fang Lin; Luciano Mueller
SummaryThe 21-amino acid peptides siamycin II (BMY-29303) and siamycin I (BMY-29304), derived from Streptomyces strains AA3891 and AA6532, respectively, have been found to inhibit HIV-1 fusion and viral replication in cell culture. The primary sequence of siamycin II is CLGIGSCNDFAGCGYAIVCFW. Siamycin I differs by only one amino acid; it has a valine residue at position 4. In both peptides, disulfide bonds link Cys1 with Cys13 and Cys7 with Cys19, and the side chain of Asp9 forms an amide bond with the N-terminus. Siamycin II, when dissolved in a 50:50 mixture of DMSO and H2O, yields NOESY spectra with exceptional numbers of cross peaks for a peptide of this size. We have used 335 NOE distance constraints and 13 dihedral angle constraints to generate an ensemble of 30 siamycin II structures; these have average backbone atom and all heavy atom rmsd values to the mean coordinates of 0.24 and 0.52 Å, respectively. The peptide displays an unusual wedge-shaped structure, with one face being predominantly hydrophobic and the other being predominantly hydrophilic. Chemical shift and NOE data show that the siamycin I structure is essentially identical to siamycin II. These peptides may act by preventing oligomerization of the HIV transmembrane glycoprotein gp41, or by interfering with interactions between gp41 and the envelope glycoprotein gp120, the cell membrane or membrane-bound proteins [Frèchet, D. et al. (1994) Biochemistry, 33, 42–50]. The amphipathic nature of siamycin II and siamycin I suggests that a polar (or apolar) site on the target protein may be masked by the apolar (or polar) face of the peptide upon peptide/protein complexation.
The Journal of Antibiotics | 1995
Mitsuaki Tsunakawa; Shu-Lok Hu; Yutaka Hoshino; David J. Detlefson; Susan E. Hill; Tamotsu Furumai; Richard J. White; Maki Nishio; Kimio Kawano; Satoshi Yamamoto; Yasuo Fukagawa; Toshikazu Oki
The Journal of Antibiotics | 1993
Yoshimasa Uehara; Pei-Ming Li; Hidesuke Fukazawa; Satoshi Mizuno; Yumi Nihei; Maki Nishio; Minoru Hanada; Chii Yamamoto; Tamotsu Furumai; Toshikazu Oki
The Journal of Antibiotics | 1995
David J. Detlefsen; Susan E. Hill; Kevin J. Volk; Steven E. Klohr; Mltsuaki Tsunakawa; Tamotsu Furumai; P. F. Lin; Maki Nishio; Kimio Kawano; Toshikazu Oki; Mike S. Lee
The Journal of Antibiotics | 1993
Tamotsu Furumai; Shizuko Kakinuma; Haruaki Yamamoto; Nobujiro Komiyama; Kiyoshi Suzuki; Kyoichiro Saitoh; Toshikazu Oki
The Journal of Antibiotics | 1993
Kyoichiro Saitoh; Kiyoshi Suzuki; Minoru Hirano; Tamotsu Furumai; Toshikazu Oki
The Journal of Antibiotics | 1993
Kyoichiro Saitoh; Takashi Tsuno; Masatoshi Kakushima; Masami Hatori; Tamotsu Furumai; Toshikazu Oki
The Journal of Antibiotics | 1993
Tamotsu Furumai; Kyoichiro Saitoh; Masatoshi Kakushima; Satoshi Yamamoto; Kiyoshi Suzuki; Chiharu Ikeda; Seikichi Kobaru; Masami Hatori; Toshikazu Oki
The Journal of Antibiotics | 1992
Soichiro Toda; Yumiko Obi; Kei-Ichi Numata; Yasutaro Hamagishi; Koji Tomita; Nobujiro Komiyama; Chikako Kotake; Tamotsu Furumai; Toshikazu Oki
The Journal of Antibiotics | 1992
Chikako Kotake; Tetsuro Yamasaki; Toshio Moriyama; Mieko Shinoda; Nobujiro Komiyama; Tamotsu Furumai; Masataka Konishi; Toshikazu Oki