Design and Synthesis of Beta-Hairpin Peptidomimetics for Modulating Integrin Mediated Cell Adhesion, Abeta Fibrillogenesis and p53-MDM2 Protein-Protein Interactions

Jain, Priyesh

31 December 2010

Inhibiting therapeutically important protein-protein interactions has been a tremendous challenge for medicinal chemists. The folded 3D structures of peptides and proteins, mainly comprise secondary structural elements i.e α-helices and β-sheet have created an opportunity to design small molecules and peptidomimetic inhibitors of protein-protein interaction (PPI). Hence, information about the formation and stabilization of these secondary structures is vital for designing future drugs. In this dissertation, several cyclic beta-hairpin peptidomimetics that mimic the recognition surface have been designed and synthesized as inhibitors for different targets such as integrin mediated extracellular matrix -cell adhesion in multiple myeloma, p53-MDM2 PPI, amyloid beta fibrillogenesis inhibitor. Cyclization of linear peptides to restrict the number of conformations available to the linear peptide can increase its affinity for the target as well as increase its proteolytic resistance. In this study, different beta turn promoters that increase the propensity of cyclic peptides to adopt beta-sheet structures have been designed and synthesized. Chapter two discusses the design and synthesis of several cyclic III (Integrin Interaction Inhibitor) peptides that block adhesion of integrins to extracellular matrix components in Multiple Myeloma tumor cells. These cyclic peptides, as assayed by TOPRO 3 assay were more potent than the parent linear peptide with a bio-activity of 1.08 μM. We have also studied structure activity relationships (SAR) of these cyclic III peptide analogs to increase the potency and bioavailability of these peptides. Chapter three describes the application of cyclic beta-hairpin peptidomimetics to inhibit abeta fibrillogenesis that is responsible for Alzheimer’s disease. We have successfully designed and synthesized cyclic peptides that target the hydrophobic region (17-21) of abeta fibril which is believed to cause self aggregation and plaque formation. We have also successfully explored these cyclic beta-hairpin peptides to disrupt p53-MDM2 interactions. Chapter five discusses the design and synthesis of novel cysteine based Peptide Nucleic Acid (PNA) monomers that are aimed to increase cellular uptake by introducing positively charged species attached to the cysteine side chain. We have successfully synthesized CPNA monomers and made efforts to make PNA oligomers.

β-sheet conformation

Cyclic Peptides

Cyclic III peptide

Multiple Myeloma

Peptide Nucleic Acids

American Studies

Arts and Humanities

Chemistry

Supramolecular organisation, conformation and electronic properties of porphyrin molecules on metal substrates

Weber, Alexander

05 1900

The investigation and control of molecular properties is currently a dynamic research field. Here I present molecular level studies of porphyrin molecules adsorbed on metal surfaces via Low Temperature Scanning Tunneling Microscopy/Spectroscopy (STM/STS), supported by complementary X-ray absorption experiments. Intermolecular and molecule-surface interactions of tetrapyrdil porphyrin (TPyP) on Ag(111) and Cu(111) were investigated. TPyP self-assembles on Ag(111) over a wide sample temperature range into large, highly-ordered 2D chiral domains. By contrast, adsorption of TPyP on the more reactive Cu(111) leads to temperature dependent assemblies, governed decisively by the strong substrate influence. The increased metal-surface interactions on Cu(111) are accompanied by a conformational distortion of the porphyrin macrocycle. The TPyP’s pyridil groups were coordinated with single iron molecules, forming metal-organic complexes. Furthermore, the porphyrin’s macrocycle was metalated by exposing a layer of well-ordered TPyP to an iron atom beam, demonstrating a novel approach towards the fabrication of metallo-tetraaryl porphyrins performed in two dimensions under ultrahigh vacuum conditions. This method was similarly used to form lanthanideporphyrinates by coordinating tetraphenyl porphyrin (TPP) macrocycles with cerium. The influence of the metal center on the porphyrins’ electronic structure was investigated via STS for TPP, TPyP,Fe−TPyP, Fe−TPP, Ce−TPP, and Co−TPP, whereby the inhomogenous electron density distribution associated with individual frontier orbitals were imaged via dI/dV mapping. The symmetry and form of the molecular orbitals could be directly correlated to the saddle-shaped conformational adaptation for the case of Co −TPP.

supramolecular nanostructures

electronic structure molecules

molecular conformation

Scanning Tunneling Microscopy

Scanning Tunneling Microscopy

porphyrin metalation

electronic properties

molecular manipulation

Ąžuolo žėlimo ypatumai mišriuose brandžiuose ąžuolo - minkštųjų lapuočių medynuose / The peculiarities of oak sprout at mixed mature arboretum of oaks- soft leafy trees

Navickas, Nerijus

15 June 2009

Magistro darbe tiriame ąžuolo žėlimą ir jį lemiančius veiksnius. Darbo objektas – Kėdainių miškų urėdijos, Pašušvio girininkijos ąžuolo žėlimo intensyvumas ir jį lemiantys veiksniai mišriuose ąžuolo - minkštųjų lapuočių medynuose. Darbo tikslas – Ištirti ąžuolo žėlimo intensyvumą ir jį lemiančius veiksnius mišriuose ąžuolo - minkštųjų lapuočių medynuose. Darbo metodai: Tyrimai susidėjo iš dviejų etapų: girininkijos taksoraščių analizės ir tyrimo natūroje. Girininkijos taksoraščių analizė: iš girininkijos taksoraščių buvo išrinkti visi brandūs medynai pasiekę žemutinę IV grupės miškams nustatytą kirtimo amžių ir turintys pomiškio sudėtyje bent 1 ąžuolo dalį. Po to surinkta informacija apie savaiminį ąžuolo žėlimą priklausomai nuo ąžuolo kiekio medyno sudėtyje, medyno amžiaus, skalsumo, atskirai nurodant bendrą pomiškio kiekį ir atskirai ąžuoliukų kiekį juose. Medyno amžius buvo grupuojamas: 40-60; 60-80; 80-100; 100-120; 120 ir > metų Medyno sudėtis buvo grupuojama: 1-2; 3-4; 5-6; 7-8; 8-10 ąžuolų Pomiškio kieks buvo grupuojamas: 0-0,9; 1,0-1,9; 2,0-2,9; 3,0-3,9; 4,0-4,9; 5,0 ir > tukst. / ha. Girininkijos miškotvarkos medžiagos analizės metu iš viso buvo išrinkti 1956 taksaciniai sklypai. Buvo rasti 28 taksaciniai sklypai kurių pomiškio sudėtyje yra savaiminio ąžuolo. Kameralinių darbų metu buvo nustatinėjami ryšiai tarp medynų sudėties, skalsumo ir augavietės sąlygų, ąžuoliukų pomiškio kiekio. Tyrimai natūroje: atlikdami tyrimus natūroje tyrėme ąžuoliukų skaičiaus... [toliau žr. visą tekstą] / Master paper researches the sprout of oak and the factors determining it. Object of the paper - an intensity of sprout of Pasusvis forestry oak at Kedainiai forests enterprise and the factors determining it at mixed arboretums of oaks- soft leafy trees. Goal of the paper - to survey an intensity of sprout of the oak and the factors determining it at mixed arboretums of oaks- soft leafy trees. Methods of work: The researches consist of two stages: the analysis of forestry valuation register and the research in reality. Analysis of forestry valuation register: all mature arboretums that have reached bottom age set for deforesting of 4th group forest and having at least 1 part of oak at their compositions were selected from the forestry valuation register. Then the information regarding self-sprout of the oak depending on quantity of oaks at the composition of arboretum, age of arboretum, abundance were collected by separately indicating general quantity of undergrowth and the number of oaks in it. The age of arboretum was grouped: 40-60; 60-80; 80-100; 100-120; 120 and > years The composition of arboretum was grouped: 1-2; 3-4; 5-6; 7-8; 8-10 oaks The quantity of undergrowth was grouped: 0-0,9; 1,0-1,9; 2,0-2,9; 3,0-3,9; 4,0-4,9; 5,0 and > thousand. / ha. During an analysis of forestry forest management material, 1956 forest valuation lots were selected. There were 28 forest valuation lots found, whose undergrowth composition contained spontaneous oak. During soil research... [to full text]

Forestry

Ąžuolas

Ąžuolo žėlimas

Žėlimą įtakojantys veiksniai

Dirvožemio sunkumas

Augavietės kokybė

Oak

Sprout of oak

Factors determining the sprout

Conformation

Guality of habitat

Mécanismes moléculaires de l'agrégation de l'insuline induite par la surface des matériaux

Nault, Laurent

24 October 2012

L'agrégation protéique induite par la surface des matériaux est un phénomène important dans la stabilité des protéines thérapeutiques. En utilisant l'insuline humaine, nous avons étudié les phénomènes agrégation en présence de surfaces neutres hydrophobes ou hydrophiles et avons montré que la nucléation a lieu sur les surfaces hydrophobes que l'on soit à pH 2.5 ou 7.3. Nous avons montré que l'énergie d'activation de la nucléation est abaissée sur surface hydrophobe. De plus, il apparait que l'agitation de la solution a des effets antagonistes. En particulier, les forces hydrodynamiques de cisaillement détachent de la surface les fibres. Par Résonance Plasmonique de Surface, spectroscopie infrarouge et microscopie à fluorescence, nous avons pu définir les étapes moléculaires ayant lieu à l'interface matériaux hydrophobe/solution. L'insuline s'adsorbe tout d'abord rapidement sur la surface, puis s'accumule lentement parallèlement à une transition de la structure α initiale vers une structure β, aboutissant à la formation de fibres amyloïdes. Par la suite, nous avons étudié le mécanisme d'action d'un peptide connu pour accélérer l'agrégation de l'insuline (LVEALYL). Ce peptide s'adsorbe de façon stable sur la surface hydrophobe en structure β et facilite l'accumulation d'insuline. De plus, il apparait que la séquence du peptide n'est pas essentielle à son action car différents peptides adoptant une structure β sur la surface sont également capables d'induire l'agrégation de l'insuline. La présence de prolines aboli cette action. Ces résultats apportent d'importantes informations sur les mécanismes moléculaires d'auto-association de l'insuline. L'hydrophobicité du matériau facilite le dépliement de l'insuline adsorbée, aboutissant à l'exposition du segment LVEALYL. Cette séquence facilite la propagation du changement de conformation vers les molécules nouvellement adsorbées. Agir contre ce phénomène pourrait permettre de stabiliser les solutions protéiques.

Protéine

Agrégation

Stabilité

Surfaces

Changement de conformation

Chaperones

Diffusion and Conformational Dynamics of Semiflexible Macromolecules and Supramolecular Assemblies on Lipid Membranes

Herold, Christoph

11 December 2012

Understanding the interaction of polyelectrolytes with oppositely charged lipid membranes is an important issue of soft matter physics, which provides an insight into mechanisms of interactions between biological macromolecules and cell membranes. Despite the fact that many (bio)macromolecules and filamentous supramolecular assemblies show semiflexible behavior, prior to this work very little was known about the conformational dynamics and Brownian motion of semiflexible particles attached to freestanding lipid membranes. In order to address these issues, diffusion and conformational dynamics of semiflexible DNA molecules and filamentous fd-virus particles electrostatically adsorbed to cationic freestanding lipid membranes were studied on the single particle level by means of optical wide-field fluorescence microscopy. Supergiant unilamellar vesicles (SGUVs) with diameters larger than 100 m represent a perfect model of a freestanding membrane. In this work, a method was developed that enabled the reliable and efficient electroformation of cationic SGUVs on ITO-coated coverslips. The utilization of SGUVs as model freestanding lipid bilayers allowed for determination of the previously unknown surface viscosity of DOPC/DOTAP membranes. In particular, the analysis of the translational diffusion coefficients of small (10, 20, 50 nm) membrane-attached anionic polystyrene beads has shown that the surface viscosity of DOPC/DOTAP membranes with CDOTAP = 1–7 mol% is independent of the DOTAP concentration and equals η = (5.9 ± 0.2) × 10−10 Pa s m. The fluorescence video-microscopy investigation of single DNA molecules attached to cationic SGUVs revealed a previously unreported conformational transition of a membrane-bound DNA molecule from a 2D random coil, the original conformation in which DNA attaches to the membrane, to a compact globule. This membrane-mediated DNA condensation is favored at high cationic lipid concentrations in the membrane and long DNA contour lengths. The DNA compaction rate in the coil–globule transition is 124 ± 46 kbp/s, and the resulting DNA globule sizes were found to be 250–350 nm at DOPC membranes containing 1 mol% DOTAP and 130–200 nm for 7 mol% DOTAP, indicating a stronger compaction for higher charge densities in the membrane. Additional experiments with freestanding cationic membranes in the gel state and supported cationic lipid membranes with gel–fluid coexistence suggest that the DNA collapse on a freestanding fluid cationic membrane may be initiated by a local lipid segregation in the membrane and is accompanied by local membrane deformations, which eventually stabilize the compact DNA globule. Furthermore, in this work single molecule studies of random-coil DNA molecules and filamentous fd-virus particles on a freestanding cationic lipid bilayer with a low charge density were carried out. The experiments revealed that these particles can be described as semiflexible chains in 2D. Taken together, DNA molecules and fd-virus particles cover a broad range of the ratio of contour length and persistence length from 0.4 to 82. The results of this work demonstrate that the mobility of such membrane-attached semiflexible particles is strongly affected by hydrodynamics in the lipid membrane and the surrounding bulk fluid, and can in essence be described using a hydrodynamics-based theory for a disk-shaped solid membrane inclusion with a characteristic size approximately equal to the radii of gyration of the particles.

Diffusion

Konformation

DNS

fd-Virus

Lipidmembran

diffusion

conformation

DNA

fd-virus

lipid membrane

ddc:570

rvk:WE 5300

rvk:WD 5360

Misfolded superoxide dismutase-1 in amyotrophic lateral sclerosis / Felveckat superoxiddismutas-1 i amyotrofisk lateralskelros

Zetterström, Per

January 2011

Amyotrophic lateral sclerosis (ALS) is a disease in which the motor neurons die in a progressive manner, leading to paralysis and muscle wasting. ALS is always fatal, usually through respiratory failure when the disease reaches muscles needed for breathing. Most cases are sporadic, but approximately 5–10% are familial. The first gene to be linked to familial ALS encodes the antioxidant enzyme superoxide dismutase-1 (SOD1). Today, more than 160 different mutations in SOD1 have been found in ALS patients.  The mutant SOD1 proteins cause ALS by gain of a toxic property that should be common to all. Aggregates of SOD1 in motor neurons are hallmarks of ALS patients and transgenic models carrying mutant SOD1s, suggesting that misfolding, oligomerization, and aggregation of the protein may be involved in the pathogenesis. SOD1 is normally a very stable enzyme, but the structure has several components that make SOD1 sensitive to misfolding. The aim of the work in this thesis was to study misfolded SOD1 in vivo. Small amounts of soluble misfolded SOD1 were identified as a common denominator in transgenic ALS models expressing widely different forms of mutant SOD1, as well as wild-type SOD1. The highest levels of misfolded SOD1 were found in the vulnerable spinal cord. The amounts of misfolded SOD1 were similar in all the different models and showed a broad correlation with the lifespan of the different mouse strains. The misfolded SOD1 lacked the C57-C146 intrasubunit disulfide bond and the stabilizing zinc and copper ions, and was prinsipally monomeric. Forms with higher apparent molecular weights were also found, some of which might be oligomers. Misfolding-prone monomeric SOD1 appeared to be the principal source of misfolded SOD1 in the CNS. Misfolded SOD1 in the spinal cord was found to interact mainly with chaperones, with Hsc70 being the most important. Only a minor proportion of the Hsc70 was sequestered by SOD1, however, suggesting that chaperone depletion is not involved in ALS.  SOD1 is normally found in the cytoplasm but can be secreted. Extracellular mutant SOD1 has been found to be toxic to motor neurons and glial cells. Misfolded SOD1 in the extracellular space could be involved in the spread of the disease between different areas of the CNS and activate glial cells known to be important in ALS. The best way to study the interstitium of the CNS is through the cerebrospinal fluid (CSF), 30% of which is derived from the interstitial fluid. Antibodies specific for misfolded SOD1 were used to probe CSF from ALS patients and controls for misfolded SOD1. We did find misfolded SOD1 in CSF, but at very low levels, and there was no difference between ALS patients and controls. This argues against there being a direct toxic effect of extracellular SOD1 in ALS pathogenesis. In conclusion, soluble misfolded SOD1 is a common denominator for transgenic ALS model mice expressing widely different mutant SOD1 proteins. The misfolded SOD1 is mainly monomeric, but also bound to chaperones, and possibly exists in oligomeric forms also. Misfolded SOD1 in the interstitium might promote spread of aggregation and activate glial cells, but it is too scarce to directly cause cytotoxicity.

ALS

SOD1

protein misfolding

SOD1 conformation

disulfide-reduced

transgenic mice

cerebrospinal fluid

protein-protein interaction

antibodies

Clinical chemistry

Klinisk kemi

Protein mass spectrometry in the drug discovery process /

Tjernberg, Agneta,

January 2005

Diss. (sammanfattning) Stockholm : Karolinska institutet, 2005. / Härtill 5 uppsatser.

Understanding physicochemical stability of proteins in solution and development of new analytical methods for freeze-dried protein formulations /

Bai, Shujun.

January 2008

Thesis (Ph.D. in Pharmaceutical Sciences) -- University of Colorado Denver, 2008. / Typescript. Includes bibliographical references (leaves 134-146). Free to UCD Anschutz Medical Campus. Online version available via ProQuest Digital Dissertations;

Cav1.2 pore structure using the substituted-cysteine accessibility method /

Breeze, Liam J.

January 2006

Thesis (Ph.D. in Neuroscience) -- University of Colorado at Denver and Health Sciences Center, 2006. / Typescript. Includes bibliographical references (leaves 108-118). Free to UCD Anschutz Medical Campus. Online version available via ProQuest Digital Dissertations;

Understanding physical and chemical stability of proteins in solution : relevance to therapeutic protein and monoclonal antibody formulations /

Thirumangalathu, Renuka.

January 2007

Thesis (Ph.D. in Pharmaceutical Sciences) -- University of Colorado Denver, 2007. / Typescript. Includes bibliographical references (leaves 133-143). Online version available via ProQuest Digital Dissertations.