Abstract

The main aims of our research program involve the synthesis of target bioactive hormones selected from results of conformational analysis and bioassays. The synthesis will be carried out in solution and by solid phase peptide methodologies. Our synthetic projects include somatostatin and oxytocin analogs emphasizing lanthionine containing structures. We will incorporate peptidomimetics such as cyclic structures, chiral methylated amino acids and peptoid structures. Specifically, the sandostatin {D-Phe-c(Cys-Phe-D-Trp-Lys-Thr-Ser-Cys]-Thr-ol} and the somatostatin related cyclohexapeptide [Pro-Phe-D-Trp-Lys-Thr-Phe] will be modified in the bridging region using lanthionine derivatives and multiple chiral methylations on the alpha-carbons and in the side chains. We will incorporate diastereomeric cyclolanthionine building units as conformationally constrained residues with cis amide bonds. We gain crucial information on the structure/bioactivity relationships using 2-D1H-NMR experiments, including 2-D total correlation spectroscopy (TOCSY) and rotating frame Overhauser enhancement spectroscopy (ROESY), in conjunction with molecular modeling techniques such as distance geometry, energy minimization, cluster analysis and molecular dynamics. We are also exploring 2-D 13C-1H heteronuclear techniques, such as the omega1 hetero half filtered TOCSY (HETLOC) and the multiple quantum coherence spectroscopy (HNQC) in order to define the backbone conformation of our analogs and measure at the rotamer populations of the side chains of the target molecules. The structural results together with bioassays carried out in the laboratories of our collaborators enable us to refine our selections of target molecules for synthesis. Currently, five different somatostatin receptors are available. Since these are genetically expressed in different organs, each receptor can be an important target for our program. Our somatostatin related ligands will be tested to determine potency and selectivity for each specific receptor type. In addition, novel lanthionine analogs of the antineoplastic somatostatin TT-232 [D-Phe-c(Cys-Trp-Lys-Cys)-Thr-NH2] will be prepared and tested for antitumor bioactivity. We intend to develop novel molecules with strong antitumor activity with low affinity to other somatostatin related receptors (SSTR1-3 and SSTR5). The results will provide crucial information to define structure requirements for recognition of each somatostatin receptor. Since there is a strong need of enzymatically stable and highly active oxytocin agonists and antagonists, we plan to synthesize and study molecules incorporating beta-methylated lanthionine building blocks. Some of our designed oxytocin analogs are expected to possess high antagonistic potency such as Atosiban {[1-deamino,Tyr2(OEt), Thr4, Orn8]vasotocin} but with higher selectivity. These compounds could be useful e.g., for the prevention of pre-term births. From this integrated approach, we hope to design and synthesize new candidate drug molecules.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
3R01DK015410-28S1
Application #
6293849
Study Section
Bio-Organic and Natural Products Chemistry Study Section (BNP)
Program Officer
Sato, Sheryl M
Project Start
1974-09-01
Project End
2000-11-30
Budget Start
2000-04-01
Budget End
2000-11-30
Support Year
28
Fiscal Year
2000
Total Cost
$102,911
Indirect Cost

  Institution

Name
University of California San Diego
Department
Chemistry
Type
Schools of Arts and Sciences
DUNS #
077758407
City
La Jolla
State
CA
Country
United States
Zip Code
92093

  Publications

Moore, Sandra Blaj; van der Hoek, Joost; de Capua, Antonia et al. (2005) Discovery of iodinated somatostatin analogues selective for hsst2 and hsst5 with excellent inhibition of growth hormone and prolactin release from rat pituitary cells. J Med Chem 48:6643-52
Moore, S B; Grant, M; Rew, Y et al. (2005) Synthesis and biologic activity of conformationally constrained analogs of L-363,301. J Pept Res 66:404-22
Kelleman, Audrey; Mattern, Ralph-Heiko; Pierschbacher, Michael D et al. (2003) Incorporation of thioether building blocks into an alphavbeta3-specific RGD peptide: synthesis and biological activity. Biopolymers 71:686-95
Del Valle, Juan R; Goodman, Murray (2003) Asymmetric hydrogenations for the synthesis of Boc-protected 4-alkylprolinols and prolines. J Org Chem 68:3923-31
Goodman, M; Zapf, C; Rew, Y (2001) New reagents, reactions, and peptidomimetics for drug design. Biopolymers 60:229-45
Li, H; Jiang, X; Goodman, M (2001) Synthesis, conformational analysis and biological activities of lanthionine analogs of a cell adhesion modulator. J Pept Sci 7:82-91
Jiang, S; Gazal, S; Gelerman, G et al. (2001) A bioactive somatostatin analog without a type II' beta-turn: synthesis and conformational analysis in solution. J Pept Sci 7:521-8
Falb, E; Salitra, Y; Yechezkel, T et al. (2001) A bicyclic and hsst2 selective somatostatin analogue: design, synthesis, conformational analysis and binding. Bioorg Med Chem 9:3255-64
Rueter, J K; Mattern, R H; Zhang, L et al. (2000) Syntheses and biological activities of sandostatin analogs containing stereochemical changes in positions 6 or 8. Biopolymers 53:497-505
Li, H; Jiang, X; Howell, S B et al. (2000) Synthesis, conformational analysis and bioactivity of Lan-7, a lanthionine analog of TT-232. J Pept Sci 6:26-35

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