Kazuya Nakagomi scite author profile

The nuclear matrix attachment DNA (MAR) binding protein SATBI is a sequence context-specific binding protein that binds in the minor groove, making virtually no contact with the DNA bases. The SATB1 binding sites consist of a special AT-rich sequence context in which one strand is well-mixed A's, T's, and C's, excluding G's (ATC sequences), which is typically found in clusters within different MARs. To determine the extent of conservation of the SATB1 gene among different species, we cloned a mouse homolog of the human SATB1cDNA from a cDNA expression library of the mouse thymus, the tissue in which this protein is predominantly expressed. This mouse cDNA encodes a 764-amino-acid protein with a 98% homology in amino acid sequence to the human SATB1 originally cloned from testis. To characterize the DNA binding domain of this novel class of protein, we used the mouse SATBI cDNA and delineated a 150-amino-acid polypeptide as the binding domain. This region confers full DNA binding activity, recognizes the specific sequence context, and makes direct contact with DNA at the same nucleotides as the whole protein. This DNA binding domain contains a novel DNA binding motif: when no more than 21 amino acids at either the N-or C-terminal end of the binding domain are deleted, the majority of the DNA binding activity is lost. The concomitant presence of both terminal sequences is mandatory for binding. These two terminal regions consist of hydrophilic amino acids and share homologous sequences that are different from those of any known DNA binding motifs. We propose that the DNA binding region of SATB1 extends its two terminal regions toward DNA to make direct contact with DNA.

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Angiotensin I-converting enzyme inhibitor derived from an enzymatic hydrolysate of casein. II. Isolation and bradykinin-potentiating activity on the uterus and the ileum of rats.

Maruyama

Nakagomi

Tomizuka

et al. 1985

Agricultural and Biological Chemistry

145

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Inhibitors of angiotensin I-converting enzyme were isolated from an enzymatic hydrolysate of bovine casein. The amino acid sequences of these inhibitors were Phe-Phe-Val-Ala-Pro-Phe-Pro-Glu-Val-Phe-Gly-Lys (CEI12), Phe-Phe-Val-Ala-Pro (CEI5), and Ala-Val-Pro-Tyr-Pro-Gln-Arg (CEI^). CEI5 is a penta-peptide derived from the hydrolysate of CEI12 with proline-specific endopeptidase, and CEI^is a hepta-peptide derived from /2-casein. These inhibitors potentiated bradykinin in the contraction of the uterus and the ileum of rats. The ileum was more sensitive to these inhibitors than the uterus. The bradykinin-potentiating activity of these inhibitors on the ileum lasted for more than 90min even after washing the organ.

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Quantification of the isomerization of Asp residue in recombinant human αA-crystallin by reversed-phase HPLC

Sadakane

Yamazaki

Nakagomi

et al. 2003

Journal of Pharmaceutical and Biomedical Analysis

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Inhibitory Effect of Alginic Acids on Hyaluronidase and on Histamine Release from Mast Cells

Asada

Sugie

Inoue

et al. 1997

Bioscience, Biotechnology, and Biochemistry

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Kazuya Nakagomi

A novel DNA-binding motif in the nuclear matrix attachment DNA-binding protein SATB1.

Angiotensin I-converting enzyme inhibitor derived from an enzymatic hydrolysate of casein. II. Isolation and bradykinin-potentiating activity on the uterus and the ileum of rats.

Quantification of the isomerization of Asp residue in recombinant human αA-crystallin by reversed-phase HPLC

Inhibitory Effect of Alginic Acids on Hyaluronidase and on Histamine Release from Mast Cells

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