Cyclic nucleotide signalling systems in vascular smooth muscle cells and immune cells with special reference to phosphodiesterases PDE3 and PDE4

Ekholm, Dag.

January 1998

Thesis (doctoral)--Lund University, 1998. / Added t.p. with thesis statement inserted. Errata slip inserted. Includes bibliographical references.

Modulation of the sonic hedgehog response in dorsoventral neutral tube patterning /

Robertson, Christie Portia.

January 2002

Thesis (Ph. D.)--University of Washington, 2002. / Vita. Includes bibliographical references (leaves 160-188).

Type VII phosphodiesterase in regulation of T cell function /

Li, Linsong,

January 1999

Thesis (Ph. D.)--University of Washington, 1999. / Vita. Includes bibliographical references (leaves 81-91).

CHARACTERIZATION OF THE EFFECT OF N(6),0(2')-DIBUTYRYL CYCLIC ADENOSINE 3':5'-MONOPHOSPHATE UPON INFLUENZA VIRUS REPLICATION IN PRIMARY CHICK KIDNEY CELLS.

SOLTYSIAK, ROBERT MARION

January 1976

DISSERTATION (PH.D.)--THE UNIVERSITY OF MICHIGAN

CHARACTERIZATION OF THE EFFECT OF N(6),0(2')-DIBUTYRYL CYCLIC ADENOSINE 3':5'-MONOPHOSPHATE UPON INFLUENZA VIRUS REPLICATION IN PRIMARY CHICK KIDNEY CELLS

SOLTYSIAK, ROBERT MARION.

January 1976

Thesis (Ph. D.)--University OF MICHIGAN.

Cyclic GMP-inhibited cAMP phosphodiesterase further characterization and identification of the phophorylation site for cAMP-dependent protein kinase /

Rascón, Ana.

January 1992

Thesis (Ph. D.)--University of Lund, 1992. / Published dissertation. Includes bibliographical references.

Structural and biochemical studies on the biosynthetic pathways of cyanobactins

Bent, Andrew F.

January 2016

Cyclic peptides have potential as scaffolds for novel pharmaceuticals, however their chemical synthesis can be challenging and as such natural sources are often explored. Several species of cyanobacteria produce a family of cyclic peptides, the cyanobactins, through the ribosomal synthesis of precursor peptides and post-translational tailoring. The patellamides, a member of the cyanobactin family, are cyclic octapeptides containing D-stereo centres and heterocyclised amino acids. A single gene cluster, patA - patG, contains the genes for the expression of the precursor peptide and the enzymes responsible for post-translational modifications including a heterocyclase, protease, macrocyclase and oxidase. Biochemical and structural analysis on the patellamide and related cyanobactin pathways has been carried out. The crystal structure of PatF, a proposed prenyl transferase, has been determined, highlighting that it is likely evolutionary inactive due to changes to key residues when compared to active homologues. This is in agreement with the knowledge that no naturally prenylated patellamides have been discovered to date. The crystal structure of the macrocyclase domain of PatG has been determined in complex with a substrate analogue peptide. The structure, together with biochemical analysis has allowed a mechanism of macrocyclisation to be proposed, confirming the requirement of a specific substrate conformation to enable macrocyclisation. Using isolated enzymes from the patellamide and related pathways, a small scale library of macrocycles made up of diverse sequences has been created in vitro and characterised by mass spectrometry and in certain cases NMR. In order to further enhance diversity, macrocycles containing unnatural amino acids have been created using three approaches; SeCys derived precursor peptides, intein-mediated peptide ligation and pEVOL amber codon technology. Finally, two oxidase enzymes from cyanobactin pathways have been purified, characterised and confirmed active for thiazoline oxidation. Native X-ray datasets on crystals of the oxidase CyaGox have been collected and phasing trials are on-going.

572

A Sythetic Study of a Cyclic Siloxydiyne and its Iron Carbonyl Complex / A Synthetic Study of a Cyclic Siloxydiyne and its Iron Carbonyl Complex

Chi, Xiang-yong

12 1900

The synthetic studies include the synthesis of the cyclic siloxydiyne, 3,3,5,5,8,8,10,10-octamethyl-4,9-dioxa-3,5,8,10-tetrasilacyclodeca-1,6- diyne [VI] and its novel iron carbonyl complex. In the preparation of [VI] by HBr promoted condensation of bis (methoxydimethylsilyl) acetylene, a minor product, a cyclic trimer was always formed along with the major product [VI]. No evidence of an equilibrium between the trimerization product and the dimerization product was found. Compound [VI] can react with iron carbonyl reagents to produce a novel binuclear iron complex of trimethylenemethane [VII] in very low yield either in a thermal or photo-reaction. The key step proposed by us in the formation of [VII] is a I,2-silyl shift in a complexed bis (silyl) acetylene to form a vinylidene intermediate. Experiments aimed at isolating this intermediate were not successful.

cyclic siloxydiyne syntheses

iron carbonyl complex

Cyclic compounds -- Synthesis.

Silicones -- Synthesis.

Carbonyl compounds.

Conformational Studies On Cyclic Pentapeptides And Structural Features In Globular Proteins

Nagarajaram, H A

01 1900

No description available.

Pentapeptides - Biochemistry

Proteins - Biochemistry

Peptides - Biochemistry

Cyclic Peptide

cyclic Pentapeptide

Cis Peptlde

Globular Proteins

Biochemistry

Comparison of retentive properties of two attachment systems in mandibular overdentures - an in vitro study

Satti, Asim Alsadig

January 2013

>Magister Scientiae - MSc / Aim: The aim of this study is to test and compare the retentive properties of two types of attachments i.e. Locator® and OT equator in a mandibular overdenture placed over 2 implants.

Overdenture

Implant overdentures

Implants

Mandibular overdenture

Retention

Locator®

OT equator

Cyclic dislodgement

Cyclic fatigue

In-vitro