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Horm Metab Res 1986; 18(2): 98-102
DOI: 10.1055/s-2007-1012241
ORIGINALS
Basic
© Georg Thieme Verlag, Stuttgart · New York

Development of Specific and Non-Specific Somatostatin Analogs

T. Nakano, Y. Harano, J. Emura1 , T. Kimura1 , S. Sakakibara1 , Y. Shigeta
  • Third Department of Medicine, Shiga University of Medical Science, Seta, Ohtsu, Shiga, Japan
  • 1Peptide Institute, Protein Research Foundation, Mino, Osaka, Japan
Further Information

Publication History

1984

1984

Publication Date:
14 March 2008 (online)

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Summary

Biological activity of six somatostatin analogs has been investigated. In these analogs, disulfide bond is replaced by ethylene bond cyclized with α-amino suberic acid. In addition, they contain unique D-configuration in both Trp8 and Cys14 moiety with dicarba substitution.

An analog of the short chain length, Cω7 -cyclo(Phe6 -Phe7 -D-Trp8 -Lys9 -Thr10 -Phe11 -D-Asu14) (analog 4) has suppressive effect for GH, but not for other hormones. Analog 6, Cω9 -cyclo(Asn5 -Phe6 -Phe7 -D-Trp8 -Lys9 -Thr10 -Phe11 -Thr12 -D-Asu14), has suppressed GH and insulin secretion, but not for gastrin and glucagon. Analog 1, Cω11 -cyclo(Lys4 -Asn5 -Phe6 -Phe7 -D-Trp8 -Lys9 -Thr10 -Phe11 -Thr12 -Ser13 -D-Asu14) and 5, Cω9 -cyclo(Lys4 -Asn5 -Phe6 -Phe7 -D-Trp8 -Lys9 -Thr10 -Phe11 -D-Asu14) have broad suppressive effect for GH, gastrin, insulin and glucagon release after arginine infusion.

The shortest analog, analog 2, Cω5 -cyclo(Phe7 -D-Trp8 -Lys9 -Thr10 -D-Asu14) has weak suppressive effect of GH, insulin and glucagon secretion, and it is suggested that Phe6 and Phe11 are necessary for the appearance of suppressive effect of GH. Specific analog, analog 4, may be useful for the future treatment for acromegaly and diabetic retinopathy. Non-specific analogs, 1 and 5 are candidates for the clinical application of wide variety.

Key-Words

Somatostatin - Biological Activity - Specific and Nonspecific Analog - Growth Hormone - Gastrin - IRI - IRG