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Synthèse de mimes peptidiques pyrrolo[3,2-e][1,4]diazépin-2-oneDeaudelin, Philippe January 2008 (has links)
Mémoire numérisé par la Division de la gestion de documents et des archives de l'Université de Montréal.
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X-ray Crystallographic Characterization Of Designed Peptides Containing Heterochiral And Homochiral Diproline Segments And Database AnalysisSaha, Indranil 07 1900 (has links)
Understanding the relation between amino acid sequences and protein structures is one of the most important problems in modern molecular biology. However, due to the complexities in the protein structure, this task is really daunting. Hence, understanding the structural features of proteins and the rules of folding is central to the design of novel and more effective biomaterials. With the inception of the de novo design of synthetic mimetics for protein structural elements, the study of designed peptides is a subject of intense current research. The de novo design of polypeptide structures provides insights into the factors that govern the folding of peptides and proteins. The rational design of synthetic peptide models for secondary structural motifs in proteins depends on the ability to control the polypeptide chain stereochemistry. An approach, which seems to be useful, is the introduction of constrained genetically coded amino acids like Proline or the introduction of non-protein constrained amino acids like Aib which are capable of restricting the range of available backbone conformations of the polypeptide chain. The use of such residues would then permit the design of well defined and intended structural motifs like the β-turns which serve as chain reversal areas of the polypeptide chain. Templates incorporating multiple repeats of such conformationally constrained residues would in turn further enhance the choice of conformational parameters for the polypeptide chain towards folding. Crystal structure determination of the oligopeptides by X-ray diffraction gives insight into the specific conformational states, modes of aggregation, hydrogen bond interactions and solvation of peptides. Precise structural analysis and good characterization of geometrical parameters and stereochemical details of these molecules provide valuable inputs for peptide design and are indispensable for exploring strategies to design peptide sequences which serve as synthetic mimics for folding motifs in proteins. Many of the above points have been investigated in this thesis which incorporates study of designed peptides containing heterochiral and homochiral diproline segments followed by protein database analysis.
This thesis reports results of x-ray crystallographic studies of twenty two (22) oligopeptides containing heterochiral or homochiral diproline segments. Apart from the crystal data, protein database analysis has also been carried out to investigate what actually is found in nature. Given in brackets are the compound names used in the thesis for the peptides solved.
1) Piv-DPro-LPro-NHMe ( DPPN ) [C16H27N3O3 ] 2) Piv-DPro-LPro-LVal-OMe ( DPPV ) [C21H35N3O5 . 0.09 H2O] 3) Piv-DPro-LPro-LPhe-OMe ( DPPF ) [C25H35N3O5 . H2O] 4) Piv-DPro-LPro-DAla-OMe ( DPPDA ) [C19H31N3O5] 5) Piv-LPro-DPro-LAla-OMe ( PDPA ) [C19H31N3O5] 6) Piv-DPro-LPro-LVal-NHMe ( DPPVN ) [C21H36N4O4 . H2O] 7) Piv-DPro-LPro-LLeu-NHMe ( DPPLN ) [C22H38N4O4 . 0.34H2O] 8) Piv-DPro-LPro-LPhe-NHMe ( DPPFN ) [C25H36N4O4 . H2O] 9) Piv-DPro-LPro-Aib-NHMe ( DPPUN ) [C20H34N4O4] 10) Piv-DPro-LPro-DAla-NHMe ( DPPDAN ) [C19H32N4O4] 11) Piv-DPro-LPro-DVal-NHMe ( DPPDVN ) [C21H36N4O4 .1.43 H2O] 12) Piv-DPro-LPro-DLeu-NHMe ( DPPDLN ) [C22H38N4O4 . H2O] 13) Piv-LPro-DPro-LAla-NHMe ( PDPAN ) [C19H32N4O4] 14) Piv-LPro-DPro-LVal-NHMe ( PDPVN ) [C21H36N4O4] 15) Piv-LPro-DPro-LLeu-NHMe ( PDPLN ) [C22H38N4O4 . H2O] 16) Piv-LPro-DPro-LVal-OMe ( PDPVO ) [C21H35N3O5 . H2O] 17) Racemic mixture of Piv-DPro-LPro-DVal-NHMe + Piv-LPro-DPro-LVal-NHMe
( PPVVN ) [C21H36N4O4 . 0.74H2O] 18) Racemic mixture of Piv-DPro-LPro-DLeu-NHMe + Piv-LPro-DPro-LLeu-NHMe ( PPLLN ) [C22H38N4O4 . H2O] 19) Racemic mixture of Piv-DPro-LPro-DPhe-NHMe + Piv-LPro-DPro-LPhe-NHMe
( PPFFN ) [C25H36N4O4 . 2 H2O] 20) Piv-LPro-LPro-LPhe-OMe ( PPFO ) [C25H35N3O5 . 0.5 H2O] 21) Piv-LPro-LPro-LVal-NHMe ( PPVN ) [C21H36N4O4 . H2O] 22) Piv-LPro-LPro-Aib-NHMe ( PPUN ) [C20H34N4O4. H2O]
Results from the X-ray crystallographic analysis of the above peptides provided substantial information regarding role of diproline templates on the folding of the polypeptide chain.
The thesis is divided into the following eight chapters :
Chapter 1 gives a general introduction to the stereochemistry of polypeptide chains and the secondary structure classification: helices, β-sheets and β-turns. This section also provides a brief overview of the use of non standard and D-amino acids into peptide design. Discussions on DProline, puckering states of the Proline ring, diproline segments and racemic mixtures of peptides are also presented. A brief discussion on X-ray diffraction and solution to the phase problem is also given.
Chapter 2 describes the structural characterization in crystals of the five following designed peptides: Piv-DPro-LPro-NHMe (DPPN), Piv-DPro-LPro-Xxx-OMe [Xxx = LVal (DPPV); LPhe (DPPF); DAla (DPPDA)] and Piv-LPro-DPro-LAla-OMe (PDPA) containing the heterochiral diproline segment with an aim towards understanding the directive influence of
short range interaction on polypeptide folding. Except PDPA, in all the structures, a type II’ β-turn was observed at the DPro-LPro segment with the formation of a 4→1 intramolecular hydrogen bond between the atoms of the polypeptide backbone. In PDPA, the expected type II β-turn occurred at the LPro-DPro segment. Thus, the DPro-LPro segment preferably adopts a
type II’ β-turn conformation when present at the C-terminus which is mimicked by the methyl ester group. The use of pivalyol group at the N-terminus is to ensure the trans geometry of the peptide bond between pivalyol and the first Proline.
Crystal parameters
DPPN: C16H27N3O3; P21; a = 10.785(1) Å, b = 15.037(1) Å, c = 11.335(1) Å; β = 109.96(1)°;
Z = 4; R = 0.0388, wR2 = 0.1047.
DPPV: C21H35N3O5 . 0.09 H2O; P212121; a =10.676(1) Å, b = 16.608(1) Å, c = 39.887(1) Å, Z = 12; R = 0.0688, wR2 = 0.1701.
DPPF: C25H35N3O5 . H2O; P21; a = 9.538(1) Å, b = 10.367(1) Å, c = 13.102(1) Å; β = 93.04(1) °; Z = 2; R = 0.0504, wR2 = 0.1455.
DPPDA: C19H31N3O5; P21; a = 11.269(1) Å, b = 9.945(1) Å, c = 18.550(2) Å; β = 97.46(1)°; Z = 4; R = 0.0563, wR2 = 0.1249.
PDPA: C19H31N3O5; P212121; a = 9.043(1) Å, b = 10.183(2) Å, c = 23.371(1) Å; Z = 4; R = 0.0753, wR2 = 0.1603.
Chapter 3 describes the crystal structures of the four following designed peptides containing the heterochiral diproline segment followed by a L-residue or an achiral amino acid residue like Aib : Piv-DPro-LPro-Xxx-NHMe [Xxx = LVal (DPPVN); LLeu (DPPLN); LPhe (DPPFN) and Aib (DPPUN)]. In the first three peptides the DPro-LPro segennt adopts a type II’ β-turn conformation with the formation of a type I β-turn at the LPro-Xxx segment. The peptide backbone overall therefore adopts a consecutive β-turn structure. When the L-amino acids at the C-terminus are replaced by the achiral amino acid Aib, the overall folded structure adopted by the peptide backbone still remains unchanged with the formation of a consecutive
β-turn. All the structures are stabilized by two intramolecular 4→1 hydrogen bonds between the C=O group and the nitrogen atom of the polypeptide backbone.
Crystal parameters
DPPVN: C21H36N4O4 . H2O; P21; a = 9.386(1) Å, b = 12.112(1) Å, c = 10.736(1) Å; β = 99.53(1) °; Z = 2; R = 0.0528, wR2 = 0.1337.
DPPLN: C22H38N4O4 . 0.34H2O; P21; a =9.231(1) Å, b = 17.558(1) Å, c = 15.563(1) Å; β = 91.94(1) °; Z = 4; R = 0.0555, wR2 = 0.1422.
DPPFN: C25H36N4O4 . H2O; P212121; a = 10.473(1) Å, b = 15.980(1) Å, c = 15.994(1) Å; Z = 4; R = 0.0620, wR2 = 0.1826.
DPPUN: C20H34N4O4; P212121; a = 10.571(2) Å, b = 11.063(1) Å, c = 18.536(1) Å; Z = 4; R = 0.0578, wR2 = 0.1256.
Chapter 4 describes the crystal structures of the seven designed peptides containing
heterochiral diproline segment. Three of these contain sequences of the type DPro-LPro-DXxx [DXxx = DAla (DPPDAN); DVal (DPPDVN); DLeu (DPPDLN)] and three contains the enantiomeric peptides of the ones that are mentioned earlier in sequences of the type LPro-DPro-LXxx [LXxx = LAla (PDPAN); LVal (PDPVN); LLeu (PDPLN)]. In order to investigate the effect of the C-terminal protecting group, a final peptide Piv-LPro-DPro-LVal-OMe (PDPVO) was crystallographically characterized. All the peptides containing the DXxx residues adopted different backbone conformations. For DAla, a structure simultaneously having a β-turn and an α-turn was obtained which is the first example in designed peptides of an isolated α-turn. In the case of DVal, an open / extended structure devoid of any intramolecular hydrogen bonding was obtained whereas for DLeu, type II β-turn occurred at the LPro-DLeu segment instead of the expected type II’ turn at the DPro-LPro segment. In the case of enantiomeric peptides, all the three peptides adopted folded structures with exact mirror image conformation being generated for LAla and nearly identical mirror image conformation in the case of LLeu. The enantiomeric peptide of DVal which contained LVal residue following the diproline segment also adopted a folded conformation with the
formation of type II β-turn at the LPro-DPro segment as expected. X-ray crystallographic characterization of PDPVO resulted in the peptide adopting an overall extended / open structure. Thus, the chirality of the C-terminal residue seems to have a profound effect on the conformation of the heterochiral diproline segments. The role of the C-terminal protecting group cannot also be undermined.
Crystal parameters
DPPDAN: C19H32N4O4; P1; a = 5.964(1) Å, b = 9.354(1) Å, c = 9.961(1) Å; α = 75.44(1), β = 78.90(1) °, γ = 77.04(1); Z = 1; R = 0.0728, wR2 = 0.1528.
DPPDVN : C21H36N4O4 .1.43 H2O; P212121; a = 8.744(8) Å, b = 11.609(1) Å, c = 23.577(2)
Å; Z = 4; R = 0.0625, wR2 = 0.1856.
DPPDLN : C22H38N4O4 . H2O; P212121; a = 10.531(3) Å, b = 11.659(3) Å, c = 20.425(6) Å; Z = 4; R = 0.0444, wR2 = 0.1239.
PDPAN: C19H32N4O4; P1; a = 5.964(1) Å, b = 9.354(2) Å, c = 9.961(2) Å; α = 75.44(1), β = 78.90(1) °, γ = 77.04(1); Z = 1; R = 0.0745, wR2 = 0.1572.
PDPVN : C21H36N4O4; P212121; a = 9.743(1) Å, b = 11.423(1) Å, c = 21.664(3) Å; Z = 4; R = 0.0803, wR2 = 0.1899.
PDPLN : C22H38N4O4 . H2O; P212121; a = 10.462(4) Å, b = 11.572(4) Å, c = 20.262(7) Å; Z = 4; R = 0.0968, wR2 = 0.2418.
PDPVO : C21H35N3O5 . H2O; P212121; a = 8.784(4) Å, b = 11.587(5) Å, c = 23.328(1) Å; Z = 4; R = 0.0888, wR2 = 0.1465.
Chapter 5 describes the crystal structures of the three designed peptides containing racemic mixtures [Racemic mixture of Piv-DPro-LPro-DVal-NHMe + Piv-LPro-DPro-LVal-NHMe (PPVVN); Racemic mixture of Piv-DPro-LPro-DLeu-NHMe + Piv-LPro-DPro-LLeu-NHMe (PPLLN); Racemic mixture of Piv-DPro-LPro-DPhe-NHMe + Piv-LPro-DPro-LPhe-NHMe (PPFFN)] having the heterochiral diproline segment in their sequences and three peptides having a homochiral diproline segment [Piv-LPro-LPro-LPhe-OMe (PPFO); Piv-LPro-LPro-LVal-NHMe (PPVN); Piv-LPro-LPro-Aib-NHMe (PPUN)]. The inability of the pure enantiomers to crystallize in the case of Phe (chapter 4) invoked the use of peptide racemates for obtaining a crystal state conformation for the said compound. In all the cases, the L-enantiomer of Xxx crystallized in the asymmetric unit. A type II β-turn was obtained in the case of PPVVN at the LPro-DPro segment and a type II’ β-turn was obtained for PPLLN at the DPro-LLeu segment. in the case of Phe, an open structure devoid of any intermolecular hydrogen bonding an very similar to DPPDVN (chapter 4) was obtained. In the case of homochiral diproline segment containing peptides, PPFO crystallized with two molecules in the asymmetric unit, both of which adopted a type VIA1 hydrogen bonded β-turn conformation with a cis peptide bond between the diproline segment. In the case of Valine (PPVN) however, a structure devoid of any intramolecular hydrogen bonding was obtained. In the final peptide PPUN, a type II β-turn conformation is observed at the LPro-Aib segment. The analysis revealed that the hydration of the peptide can cause dramatic changes in its backbone conformation. In homochiral LPro-LPro sequences, the tendency to form hydrogen bonded turns competes with the formation of semi-extended polyproline structures. The results also emphasize the subtle role of sequence effects in modulating the conformations of short, constrained peptide segments. The possibility of trapping distinct conformational segments of the diproline segments in crystals by generating racemic centro-symmetric crystals in which packing effects may be appreciably different from those observed in the crystals of individual pure enantiomeric peptides has been clearly exploited in this chapter to obtain a crystal in the case of Phe. These results suggest that the energetic differences between these states is small. Conformational choice can therefore be readily influenced by environmental and sequence effects. Crystal parameters PPVVN: C21H36N4O4 . 0.74H2O; C2/c; a = 36.667(17) Å, b = 10.092(5) Å, c = 13.846(6) Å; β = 107.27(1) °; Z = 8; R = 0.1317, wR2 = 0.3141. PPLLN: C22H38N4O4 . H2O; P21/c; a = 10.555(1) Å, b = 11.687(1) Å, c = 20.108(2) Å; β = 95.47(1) °; Z = 4; R = 0.0761, wR2 = 0.2034. PPFFN: C25H36N4O4 . 2 H2O; P21/c; a = 8.883(5) Å, b = 18.811(10) Å, c = 16.033(9) Å; β = 96.28(1) °; Z = 4; R = 0.1218, wR2 = 0.2848. PPFO : C25H35N3O5 . 0.5 H2O; P212121; a = 10.199(1) Å, b = 20.702(2) Å, c = 23.970(2) Å; Z = 8; R = 0.0716, wR2 = 0.1901.
PPVN : C21H36N4O4 . H2O; P212121; a = 9.454(1) Å, b = 11.119(1) Å, c = 23.021(2) Å; Z = 4;
R = 0.0551, wR2 = 0.1587.
PPUN: C20H34N4O4. H2O; P21; a = 6.276(1) Å, b = 14.011(2) Å, c = 12.888(1) Å; β =
96.80(1) °; Z = 2; R = 0.0475, wR2 = 0.1322.
Chapter 6 describes the pyrrolidine ring puckering states of the Proline residue present in diproline segments in the peptides solved in this thesis, the Cambridge structural database
(CSD) [only acyclic diproline containing peptides have been taken into account] and in a non-redundant dataset of proteins in the Protein Data Bank (PDB). The five membered pyrrolidine ring of Proline can be best characterized in terms of the following five endocyclic torsion
angles χ1, χ2, χ3,χ4 and θ. Using various values of these endocyclic torsion angles the following puckering states were identified : [1] Cγ-exo (A) [2] Cγ-endo (B) [3] Cβ-exo (C) [4] Cβ-endo (D) [5] Twisted Cγ-exo-Cβ-endo (E) [6] Twisted Cγ-endo-Cβ-exo (F) [7] Planar (G) [8] Cα-distorted (H) [9] Twisted Cβ-exo-Cα-endo (I) [10] Cδ-endo (K) [11] N-distorted (L) [12] Twisted Cδ-endo- Cγ-exo (N). In the case of peptides solved in this thesis for heterochiral diproline segments, the Cγ-exo / Cβ-exo (AC) combination turns out to more preferred than the other combinations. The Cγ-endo / Cγ-endo (BB) state is the second most populated state. The overall investigation of Proline rings in peptides show that the states Cγ-exo (A), Cβ-exo
(C) and Twisted Cγ-endo-Cβ-exo (F) are the most preferred states of occurrence of the pyrrolidine ring conformation. In the case of proteins, the overall percentage distribution of various combinations indicates that the AA (Cγ-exo / Cγ-exo), AE (Cγ-exo / Twisted Cγ-exo-Cβ-endo) and FF (Twisted Cγ-endo-Cβ-exo / Twisted Cγ-endo-Cβ-exo) categories are the most preferred combinations. For Proline rings in proteins, the states Cγ-exo (A), Twisted Cγ-exo-Cβ-endo (E) and Twisted Cγ-endo-Cβ-exo (F) are the most preferred states of occurrence of the pyrrolidine ring conformation.
Chapter 7 describes the analysis of diproline segments in a non-redundant dataset of proteins In this chapter, the possible conformational states for the diproline segment (LPro-LPro) found in proteins taken from a non-redundant dataset has been investigated an identified with an emphasis on the cis and trans states for the peptide bond between the diproline segment. The occurrence of diproline segments in type VIA1 turns (cis Pro-Pro peptide bond) and other regular secondary structures like type III β-turns and α-helices has been studied. This has been followed up by the amino acid distribution flanking the diproline segment and the conformation adopted by Xaa-Pro and Yaa-Pro segments in proteins. It is observed that for cis Pro-pro peptide bond, the conformation adopted by the first Proline lies in PII region whereas the second Proline inevitably adopts a conformation in the Bridge region, leading to the formation of the type VIA1 β-turn structure. But in the trans case, the conformation adopted by the first Proline is overwhelmingly populated in the PII (Polyproline) and right-handed α-helical region. For position i+2, the major conformation adopted by Proline is P II and α with a substantial amount of occurrences in Bridge and the C7 (γ-turn) region. The analysis also reveals that the cis-cis configuration of the peptide bond is very rare when considering the diproline segment. With a cis-trans peptide linkage, PII-PII conformation is the most stable and favoured conformation for the Pro-Pro segment in proteins. With trans peptide bond linkage between the Proline residues, α- α and PII-Bridge conformations are equally likely for the diproline segment. The population in trans-cis and cis-trans states are comparable indicating that the energy differences between these states is small. However, trans-trans is the most populated state with a percentage occurrence of 85.43%. The analysis and comparison of conformational states for the Xaa-Pro-Yaa sequence reveals that the Xaa-Pro peptide bond exists preferably as the trans conformer rather than the cis conformer. The same is valid for Pro-Yaa segment, with the cis conformer being populated to even lesser extent. The data shows that α- α, PII-α, PII-PII and extended-PII are the most populated states for Xaa-Pro and Pro-Yaa segments as compared to PII-PII and PII-α and states observed for the Pro-Pro segment.
Chapter 8 describes the analysis of single and multiple β-turns in a non-redundant dataset of proteins. The analysis on β-turns in proteins has shed a new light into the propensity values for amino acid residues at various positions of β-turns which in certain cases have undergone appreciable change in values than previously observed. One of the other notable feature of the analysis is the fact that the data displays a higher occurrence of unprimed β-turns of type I and type II as compared to their primed counterparts of type I’ and type II’ as previously observed. In fact, the results show that type I β-turn is the highest occurring turn both in isolated as well as in consecutive β-turn examples. The analysis of multiple β-turns in proteins has revealed many new categories like the (I,I+1,I+3), (I,I+2,I+3) and combination of turns which can be used for the design of the loops, especially in the case of β-hairpins. Among the multiple turns, double turns occur more frequently than the other consecutive turns like triple and quadruple turns. It is also important to note that the number of examples of a hydrogen bonded turn being followed by a hydrogen bonded turn is very less with type IV turn preceding a primed turn in most of the cases. Thus, the data available from consecutive β-turn analysis and the type-dependent amino acid positional preferences and propensities derived from the present study may be useful for modeling various single and consecutive turns, especially in designing loop regions of β-hairpins.
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Dynamic Decision Support for Regional LTL CarriersWarier, Prashant 18 May 2007 (has links)
This thesis focuses on decision support for regional LTL carriers. The basic operating characteristics of regional LTL carriers are similar to those of national LTL carriers, i.e., they operate linehaul networks with satellites, breakbulks, and relays to consolidate freight so as to be able to cost-effectively serve their customers. However, there are also key differences. Most importantly, because the area covered by a regional carrier is smaller, a regional carrier handles less freight (sometimes significantly less) and therefore typically has fewer consolidation opportunities, which results in higher handling and transportation costs per unit of freight. Consequently, competing with national carriers on price is difficult. Therefore, to gain or maintain market share, regional carriers have to provide better service. To be able to provide better service, regional carriers have to be more dynamic, e.g., they have to be able to deviate from their load plan when appropriate, which creates challenges for decision makers.
Regional carriers deliver about 60% of their shipments within a day and almost all of their shipments within two days. Furthermore, most drivers get back to their domicile at the end of each day. Therefore, the focus of the thesis is the development of effective and efficient decision models supporting daily operations of regional LTL carriers which provide excellent service at low cost.
This thesis presents an effective solution approach based on two optimization models: a dynamic load planning model and a driver assignment model. The dynamic load planning model consists of two parts: an integer program to generate the best paths for daily origin-destination freight volumes and an integer program to pack freight into trailers and trailers into loads, and to determine dispatch times for these loads. Techniques to efficiently solve these integer program solution are discussed in detail. The driver assignment model is solved in multiple stages, each stage requiring the solution of a set packing models in which columns represent driver duties. Each stages determines admissible driver duties. The quality and efficiency of the solution approach are demonstrated through a computational study with real-life data from one of the largest regional LTL carriers in the country.
An important "technique" for reducing driver requirements is the use of meet-and-turn operations. A basic meet-and-turn operation involves two drivers meeting at a location in between terminals and exchange trucks. A parking lot or a rest area suffices as a meet-and-turn location. This ensures that drivers return to the terminal where they started. More sophisticated meet-and-turn operations also exist, often called drop and hook operations. In this case, drivers do not exchange trucks, but one of their trailers. The motivation in this case is not to get drivers back to their domicile, but to reduce load-
miles. The thesis presents analytical results quantifying the maximum benefits of using meet and turn operations and optimization techniques for identifying profitable meet-and-turn opportunities.
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Synthèse de mimes peptidiques pyrrolo[3,2-e][1,4]diazépin-2-oneDeaudelin, Philippe January 2008 (has links)
Mémoire numérisé par la Division de la gestion de documents et des archives de l'Université de Montréal
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En explorativ fallstudie med fokus på turtagning mellan föräldrar och unga spädbarn : Utvärdering av PEPP-modellens kartläggningsmetoder LENA och videoanalysDietmann, Rebecka, Tilde, Peltoniemi January 2021 (has links)
Interaction is an important aspect for children’s language development. The intervention model Prevention Education Program for Parents (PEPP) is currently under development within the research project Ord gör skillnad, Karolinska Institutet. PEPP is an intervention for parents to children aged 0–12 months who’s recently been diagnosed with hearing impairment. In PEPP parents receive guidance based on the child’s language environment which is mapped through Language ENvironment Analysis (LENA) and video analysis. LENA is a speech processing technological tool that analyzes the child’s language environment. The video analysis is made manually based on short video records of interactions between child and parent. The purpose of this study was to evaluate these mapping methods reliabilities to measure verbal conversational turns. The study also aimed to investigate if there’s a pattern between the amount of verbal conversational turns in a structured playtime and in the home environment. Four families with children aged 0:26–7:3 months participated. The child and parent interacted in a structured playtime that was analyzed with LENA and video analysis. Each family also made a LENA recording for an entire day in their home environment. The amount of verbal conversational turns in the structured playtime was analyzed by two assessors through video analysis. Inter-rater reliability was calculated, and a qualitative assessment was made for intervals in which the inter-rater reliability was <80%. The conformity between video analysis and LENA in the structured playtime was calculated. Further, a comparison was made between the amount of verbal conversational turns measured with LENA in home environment and structured environment. The inter-rater reliability in this study was high and in the qualitative assessment aggravating factors were identified. The conformity between video analysis and LENA analysis of the structured playtime was moderate. The amount of verbal conversational turns was higher for all participants in the structured environment compared to the home environment. This study indicates that video analysis is a reliable method. However, the aggravating aspects should be remedied in order to increase the reliability. The results confirm previous findings that demonstrate limitations with LENA’s ability to measure conversational turns in young infants. This study indicates that the number of conversational turns is higher in structured environments. To ensure the results in this study further research should be conducted. / Barn lär sig språket i interaktion med sin omgivning. Föräldrainterventionen Prevention Education Program for Parents (PEPP) utvecklas inom forskningsprojektet Ord gör skillnad, Karolinska Institutet. I PEPP handleds föräldrar till barn i åldrarna 0–12 månader med nyligen upptäckt hörselnedsättning kring samspel och kommunikation. Handledningen baseras på barnets språkmiljö som mäts med kartläggningsmetoderna Language ENvironment Analysis (LENA) och videoanalys. LENA är ett talprocessande teknologiskt verktyg som beskriver barnets språkmiljö genom automatisk analys. Videoanalysen sker manuellt av bedömare utifrån korta videoinspelningar av samspel mellan barn och förälder. Föreliggande studie syftade till att utvärdera dessa kartläggningsmetoders pålitlighet i mätning av verbala turtagningar. Vidare syftade studien till att undersöka eventuella mönster mellan antal verbala turtagningar i hemmiljö och strukturerad miljö. Fyra familjer med barn i åldrarna 0:26–7:3 månader deltog. Barn och förälder samspelade under en strukturerad leksituation som analyserades med LENA och videoanalys. Varje familj gjorde även en heldagsinspelning med LENA i hemmiljö. Antal verbala turtagningar i den strukturerade leksituationen analyserades av två bedömare med videoanalys. Interbedömarreliabilitet räknades ut och en kvalitativ bedömning genomfördes på intervall med interbedömarreliabilitet <80 %. Samstämmigheten mellan videoanalysen och LENA beräknades gällande den strukturerade leksituationen. Vidare jämfördes antal turtagningar mätt med LENA i hemmiljö och strukturerad miljö. Resultatet visade på en hög interbedömarreliabilitet i videoanalysen och i den kvalitativa bedömningen identifierades försvårande aspekter. Samstämmigheten mellan videoanalysen och LENA var måttlig. Antalet turtagningar var genomgående högre i den strukturerade leksituationen jämfört med hemmiljö. Studien tyder på att videoanalysen är en pålitlig metod. Dock identifierades försvårande aspekter som bör åtgärdas för att öka mätningens tillförlitlighet. Studien bekräftar tidigare forskning som visat på begränsningar gällande LENA:s mätning av turtagningar hos unga spädbarn. Resultatet tyder på att det sker fler turtagningar i strukturerad miljö än i hemmiljö. För att säkerställa studiens resultat krävs fortsatta studier.
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Synthesis, diversification and biomedical applications of 4,5-substitued N-aminoimidazol-2-onesPoupart, Julien 01 1900 (has links)
In peptide-based medicinal chemistry, mimicry of turn conformations is important because of the significance of such secondary structures for molecular recognition. In this context, N-aminoimidazol-2-one (Nai) residues have demonstrated ability to mimic the central residue of turn conformers. Moreover, potential to functionalize the 4- and 5-positions of the Nai heterocycle offer opportunities to add and orient side chain functionalities with constrained c-geometry.
Methods have been developed to employ Nai residues for peptide mimicry. Previously, Nai dipeptide esters with substituents at the imidazol-2-one 4-position were obtained as racemic mixtures. By employing alternative C-terminal groups, epimerization has now been minimized. Functionalization of the Nai 5-position after cyclization has also been achieved by novel chemistry. For example, (4-Me, 5-aldehyde)Nai residues were obtained by 5-position formylation. The aldehyde was then reduced and oxidized to provide alcohol and acid functionality. Reductive aminations on (4-Me, 5-aldehyde)Nai residues using different primary and secondary amines and amino methylation of (4-Me)Nai residues were also used to prepare constrained diaminobutyric acid analogs. In the interest to prepare Nai analogs that can serve as constrained phenylalanine residues, palladium-catalyzed chemistry was developed to cross-couple different aryl iodides at the 5-position. In model peptides, the (4-Me, 5-aryl)Nai residues were predicted by molecular dynamic calculations to be located at the i+1 position of type II’ β-turn conformations with the aryl side chain positioned in the gauche (–).
The synthesis of biologically relevant Nai peptides was next explored using methods for accessing enantioenriched residues and conditions for their 5-position arylation. Peptide derivatives of growth hormone releasing peptide-6 (GHRP-6) were targeted using the Nai residues because the corresponding semicarbazide analogs had exhibited selective and relatively high binding affinity for the cluster of differentiation receptor (CD36) receptor and potential to mediate macrophage-driven inflammation in conditions leading to age-related macular degeneration, atherosclerosis and angiogenesis. Previous studies with GHRP-6 analogs demonstrated that replacement of Trp4 with a semicarbazide possessing an aromatic side chain favored a turn conformation and selective CD36 binding affinity. Solid-phase methodology was developed to synthesize [(4-Me, 5-Aryl)Nai4]-GHRP-6 analogs and used to prepare four different Nai peptides on Rink amide resin. All four analogs were effective at mediating nitric oxide (NO) overproduction in macrophages cells treated with a Toll-like receptor 2 (TLR2) agonist. Although biological evaluation of the [(4-Me,5-Aryl)Nai4]-GHRP-6 analogs is still being performed, their ability to modulate NO overproduction strongly indicated backbone and side chain conformational requirements for biological activity.
In sum, this thesis has provided effective methods for preparing novel constrained peptide analogs for mimicry of the backbone and side chain geometry in β-turns. Enantiomerically enriched Nai residues were synthesized, introduced into peptide sequences, and functionalized at the 4- and 5-positions. Employment of the 4,5-disubstituted Nai analogs in the study of peptide medicinal chemistry offers powerful potential for exploring structure-activity relationships to identify and replicate biologically active conformers. / Le développement de mimes de tours peptidiques pose un intérêt particulier en chimie médicinale, en raison de leur importance dans la reconnaissance moléculaire. Dans ce contexte, les résidus N-aminoimidazol-2-one (Nai) ont démontré une tendance à occuper la position centrale de repliements peptidiques. De plus, la présence de l’unité imidazolone offre un potentiel de fonctionnalisation en position 4 et 5 pouvant jouer le rôle de chaînes latérales rigidifiées dans l’espace χ.
Des méthodes ont été développées pour rendre possible l’utilisation de résidus Nai en chimie peptidique. Par le passé, des esters de dipeptide Nai possédant un substituant à la position 4 de l’hétérocycle ont été synthétisés de manière racémique. L’utilisation de groupement C-terminaux a permis de grandement réduire l’épimérisation due à l’utilisation de base forte utilisée durant l’étape de cyclisation. La fonctionnalisation de la position 5 du cycle après la cyclisation a aussi été rendue possible par le développement de nouvelles conditions réactionnelles. Par exemple, des conditions de formylation ont donné des résidus (4-Me, 5-Aldéhyde)Nai. La fonction aldéhyde a été réduite et oxydée, donnant accès a des fonctions alcool et acide carboxylique. L’amination réductrice du squelette (4-Me, 5-Aldéhyde)Nai en utilisant des amines primaires et secondaires ainsi que l’amino-méthylation de résidus (4-Me)Nai ont donné accès à des résidus d’acide diaminobutyrique rigidifiés. Dans le but de préparer des analogues Nai pouvant servir de mimes rigidifiés de résidus phénylalanine, la catalyse au palladium a rendu possible l’installation de groupements 5-aryle par couplage croisé avec différents iodoaryles. Dans un modèle de peptide, le résidu (4-Me, 5-aryl)Nai a été soumis à une analyse par dynamique moléculaire qui a révélé le positionnement de la portion Nai à la position i+1 d’un tour β de type II’, avec la chaine latérale aryle adoptant une conformation gauche (-).
Ayant en main des conditions de synthèse énantioenrichie ainsi que de diversification de la position 5, la construction de peptides Nai possédant un intérêt biologique a été entreprise. Des dérivés du peptide Growth hormone releasing peptide-6 (GHRP-6) ont été ciblés car les analogues semicarbazide correspondant ont précédemment démontré avoir à la fois de la sélectivité et une affinité relativement grande pour le Cluster of differentiation receptor (CD36). Ils ont ainsi le potentiel de moduler l’inflammation attribuable aux macrophages dans des conditions menant à la dégénérescence maculaire liée à l’âge, l’athérosclérose et l’angiogenèse. Des études précédentes ont démontré que le remplacement du résidu Trp4 du GHRP-6 par un semicarbazide possédant une chaîne latérale aromatique favorisait l’adoption d’un repliement de la chaîne peptidique et une affinité sélective envers le récepteur CD36. Une méthode de synthèse sur phase solide d’analogues [(4-Me, 5-Aryle)Nai4]-GHRP-6 a été développée et utilisée pour synthétiser quatre différents peptides Nai en utilisant la résine Rink amide. Les quatre analogues se sont montrés efficaces à réduire la surproduction d’oxide nitrique (NO) dans les cellules macrophages traitées avec un agoniste du Toll-like receptor 2 (TLR2). Malgré le fait que l’évaluation biologique des analogues [(4-Me, 5-Aryle)Nai4]-GHRP-6 soit toujours en cours, leur habilité à moduler la surproduction d’oxide nitrique montre qu’ils possèdent la bonne géométrie quant à la chaîne principale et la chaîne latérale aromatique pour interagir avec le récepteur.
En somme, la présente thèse a fourni des méthodes efficaces de synthèse de nouveaux analogues de peptides rigidifiés pour mimer les chaînes principale et latérales de tours β. Les résidus Nai énantioenrichis ont été synthétisés, introduits dans des séquences peptidiques d’intérêt sur phase solide et fonctionnalisés à la 4ième et 5ième position. L’utilisation de ces analogues Nai 4,5-disubstitués en chimie médicinale et peptidique offre un potentiel considérable dans l’exploration de la relation structure-activité de peptides d’intérêt biologique pour identifier et mimer les conformères bioactifs.
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Leslie Morris: The Translated Jew. German Jewish Culture outside the MarginsHahn, Hans-Joachim 17 June 2020 (has links)
Leslie Morris: The Translated Jew. German Jewish Culture outside the Margins (=Cultural Expressions of World War II). Evanston, Ill.: Northwestern University Press 2018, 235 S., ISBN: 978-0-8101-3763-9 (paper), 34,95 $. Besprochen von Hans-Joachim Hahn.
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Galerie Velké ceny města Brna / The Gallery of Brno Grand PrixSikora, Zbigniew January 2014 (has links)
The main task of this thesis was to create an architectural study of The Gallery of Brno Grand Prix based on previous urban study from previous semester works. The proposal is focused on the iconic circuit’s former glory restoration, on providing new content for raceway complex and creating decent and presentable place for the presentation of the rich history of Czech and Czechoslovak motorsport. The result is a study of an object that meets these needs while respecting the historical and morphological values of the place. The building creates new themed attraction and creates the potential for further development of near circuit.
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Study of Elastin-Like Polypeptides Grafted on Electrode SurfacesPramounmat, Nuttanit 23 May 2022 (has links)
No description available.
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Gräs blir till mjölk : Ett experiment om elevers förståelse av naturvetenskapliga fenomen / Grass turns into milk : An experiment on students' understanding of scientific phenomenaHarmouche, Wafaa January 2023 (has links)
Syftet med denna studie var att utforska hur elever i årskurs 5 utvecklar naturvetenskapliga kunskaper om hur gräs omvandlas till mjölk, där särskilt fokus läggs på sambandet mellan fotosyntes och idisslande djurs matspjälkningssystem. Studiens frågeställningar var följande: Vilka naturvetenskapliga kritiska aspekter behöver elever i årskurs 5 få möjlighet att urskilja för att förstå hur gräs kan omvandlas till mjölk. Hur kan undervisning organiseras för att elever i årskurs 5 ska förstå hur gräs kan omvandlas till mjölk? Denna studie är kvalitativ och har en variationsteoretisk och sociokulturell utgångspunkt. Dessa två teorier presenterar vad undervisningen måste handla om för att skapa bästa förutsättningar till lärande. I denna studie har variationsteorin utgångspunkt i lärandeobjektet, vilka variationsmönster som erbjudits i undervisningen samt de kritiska aspekterna av hur gräs omvandlas till mjölk. Det sociokulturella perspektivet har i denna studie bland annat fokuserat på samspelet mellan eleverna, användning av artefakter och den proximala utvecklingszonen. Resultatet i studien visar att med hjälp av en variationsteoretisk utgångspunkt går det att främja elevers lärande i de naturorienterande ämnen och skapa en variation som bidrar till att elever utvecklar naturvetenskapliga kunskaper om hur gräs omvandlas till mjölk.
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