Synthesis of #alpha#-functionalised tryptophan derivatives and their incorporation into cholecystokinin ligands

Bourne, Gregory Thomas

January 1992

No description available.

572

Non-peptide surrogates

CONFORMATIONALLY CONSTRAINED ANALOGUES OF THE NEUROHYPOPHYSEAL HORMONE OXYTOCIN.

HILL, PATRICIA ANNE SCHROEDER.

January 1986

The synthesis of seventeen novel conformationally constrained analogues of the neurohypophyseal peptide hormone oxytocin is described. Synthesis of the peptides was accomplished using solid-phase synthesis techniques on either Merrifield or p-methyl-benzhydrylamine resin. Cleavage of peptides from the solid support and deprotection were carried out by either ammonolysis followed by treatment with sodium in liquid ammonia or anhydrous HF. Disulfide formation was accomplished by treatment of the deprotected peptide with aqueous potassium ferricyanide. Purification of the peptide analogues involved a combination of either partition and/or size exclusion chromatography followed by reverse-phase high-performance liquid chromatography. Several conformationally constrained unnatural amino acids were incorporated into the synthetic peptides. Two were prepared and incorporated as a mixture of isomers and the resulting peptides were separated and purified by HPLC. The types of analogues prepared fall into three categories: analogues incorporating conformational restrictions in positions 1 and 2; bicyclic oxytocin peptides; oxytocin antagonists with changes at the Asn⁵ residue. The peptides with conformational restrictions at position 1 or 2 are: [Tic²]OT, [DTic²]OT, [DTic²,Thr⁴]OT, [β-MePhe²]OT, [ΔPhe²]OT, [Cys(CH₂)₅¹,Phe²,Thr⁴,Orn⁸]OT and [Pen¹,DPhe²,Thr⁴,Orn⁸]OT. Bicyclic peptide analogues and their monocyclic precursors include: [Mpa¹,Lys⁴,Glu⁵]OT, [Mpa¹,Lys⁴,Glu⁵]OT, [Mpa¹,Glu⁴,Lys⁸]OT, and [Mpa¹,Glu⁴,Lys⁸]OT. Antagonists with changes in the Asn⁵ residue are: [Pen¹,DPhe²,Thr⁴,Thr⁵,Orn⁸]OT; [Pen¹,DPhe²,Thr⁴,Leu⁵,Orn⁸]OT; [Pen¹,DPhe²,Thr⁴,Asp⁵,Orn⁸]OT; and [Pen¹,DPhe²,Thr⁴,Tyr⁵,Orn⁸]OT. Biological assays of these analogues for oxytocic activity in the rat uterus model have shown one of the β-MePhe²-containing peptides, [L-threo-β-MePhe²]OT, to be a very potent agonist and one bicyclic, [Mpa¹,Glu⁴,Lys⁸]OT to be an extremely potent oxytocin antagonist. Initial biophysical investigations employing 250 MHz nuclear magnetic resonance spectroscopy were also undertaken in order to determine possible solution conformations of these peptide analogues.

Oxytocin.

Peptide hormones.

Oligopeptides.

The role of adrenomedullin in the anaesthetised rat model of myocardial ischaemia and reperfusion

Looi, Yee Hoo

January 2003

No description available.

612

Hypotensive peptide

Novel peptide discovery : isolation and characterisation of peptides with antidiabetic properties from the skin secretions of amphibians

Marenah, Lamin

January 2001

No description available.

615.9

Peptide sequencing

Diazopeptide chemistry

Potterton, Michael Andrew

January 1997

No description available.

547

Peptide nitrosation

Synthesis and structure-activity studies of novel potassium ion channel blockers

Fletcher, David Ian

January 1997

No description available.

615.9

Peptide toxins

Organometallic derivatives of amino acids and peptides

Stewart, A. S. J.

January 1987

No description available.

547

Peptide synthesis

Thermolysin catalysed peptide bond synthesis

Durrant, I.

January 1986

No description available.

572

Catalysed peptide bond

Molecular mechanisms of altered gastrointestinal function in gastrin deficient mice

Khan, Zara Ellen

January 2001

No description available.

572

Peptide hormones

Modulation of intestinal permeability with special reference to the absorption of bioactive peptides

Foster, Russell

January 1995

No description available.

615.1

Peptide drugs; Zoladex