Reactions of Pyridine N-oxide and 4-picoline N-oxide

Cavitt, Stanley Bruce

08 1900

In this paper, some of the work by Talbott has been repeated and other reactions of 4-picoline and pyridine N-oxides with aromatic halogen compounds have been investigated.

reactions

pyridine N-oxide

4-picoline N-oxide

Pyridine.

Picoline-N-oxide.

Die kationisch induzierte Oligomerisation von N-Vinylformamid

Madl, Alexander

24 May 2000

Gegenstand der vorliegenden Arbeit ist die Untersuchung der kationisch initiierten Oligomerisation von N-Vinylformamid mit Iod, Brom, Trifluormethansulfonsäure und Trifluormethansulfonsäure-trimethylsilylester. Quantenchemische Berechnungen zur Konformation und zur Elektronendichteverteilung von N-Vinylformamid, sowie zu seiner Reaktion mit Elektrophilen werden vorgestellt. Die Struktur der erhaltenen Oligomere wird mittels 1H- und 13C-NMR-Spektroskopie, MALDI-TOF-MS, GPC, IR-Spektroskopie, Thermogravimetrie und quantitativer Elementaranalyse untersucht. Die Abhängigkeit von Ausbeute, mittleren Polymerisationsgrad und Kopfgruppenfunktionalität der erhaltenen Oligo(N-vinylformamide) vom Initiator, sowie von der Polarität des Lösemittels, dem eingesetzten Monomer/Initiator-Verhältnis und der Reaktionstemperatur wird vorgestellt. Im Vergleich zum N-Vinylformamid werden N-Vinylacetamid, N-Methyl-N-vinylformamid, N-Methyl-N-vinylacetamid und N-Vinylpyrrolidon auf ihre Fähigkeit untersucht, mit Initiatoren der kationischen Polymerisation Oligomere zu bilden. Mit N-Deutero-N-vinylformamid als Monomer und der 2H-NMR-Analyse der erhaltenen Oligomere wird der Einfluß der NH-Eliminierung während der Oligomerisation von N-Vinylformamid untersucht. Ausgehend von den experimentellen Ergebnissen wird ein für die Vinylpolymerisation neuer Mechanismus für die Oligomerisation von N-Vinylformamid vorgeschlagen und diskutiert. / The topic of the dissertation is the survey of the cationically initiated oligomerization of N-vinylformamide with iodine, bromine, trifluoromethanesulfonic acid, and trifluoromethanesulfonic acid trimethylsilylester as initiators. Quantum chemical calculations on the conformation and the electron density of N-vinylformamide, as well as on its reaction with electrophiles are presented. The structure of the obtained oligomers is investigated with 1H- and 13C NMR spectroscopy, MALDI-TOF-MS, GPC, IR spectroscopy, thermal decomposition, and quantitative combustion analysis. The influence of the polarity of the solvent, of the initiator, of the reaction temperature, and of the monomer/initiator ratio on yield, degree of polymerization, head group functionality, and chain structures of the obtained oligo(N-vinylformamide) is investigated. In comparison with N-vinylformamide, the ability of N-vinylacetamide, N-methyl-N-vinylformamide, N-methyl-N-vinylacetamide, and N-vinylpyrrolidone in undergoing a cationically induced polymerization to oligomeric products is investigated. The influence of the NH-elimination on the oligomerization process is investigated with N-deutero-N-vinylformamide as monomer and the 2H NMR analysis of the obtained oligomers. From the results, a new mechanism for the oligomerization of N-vinylformamide is proposed and discussed.

N-Vinylformamid

Oligo(N-vinylformamid)

En-Reaktion

Wachstumsmechanismus

N-Formyl-imin

dimeres N-Methyl-N-vinylformamid

N-Vinylacetamid

Oligo(N-vinylacetamid)

ddc:540

Kationische Polymerisation

Enamide

Übertragungsreaktion

Oligomerisation

Oligomere

Polyvinylamide

Die kationisch induzierte Oligomerisation von N-Vinylformamid

Madl, Alexander

16 May 2000

Gegenstand der vorliegenden Arbeit ist die Untersuchung der kationisch initiierten Oligomerisation von N-Vinylformamid mit Iod, Brom, Trifluormethansulfonsäure und Trifluormethansulfonsäure-trimethylsilylester. Quantenchemische Berechnungen zur Konformation und zur Elektronendichteverteilung von N-Vinylformamid, sowie zu seiner Reaktion mit Elektrophilen werden vorgestellt. Die Struktur der erhaltenen Oligomere wird mittels 1H- und 13C-NMR-Spektroskopie, MALDI-TOF-MS, GPC, IR-Spektroskopie, Thermogravimetrie und quantitativer Elementaranalyse untersucht. Die Abhängigkeit von Ausbeute, mittleren Polymerisationsgrad und Kopfgruppenfunktionalität der erhaltenen Oligo(N-vinylformamide) vom Initiator, sowie von der Polarität des Lösemittels, dem eingesetzten Monomer/Initiator-Verhältnis und der Reaktionstemperatur wird vorgestellt. Im Vergleich zum N-Vinylformamid werden N-Vinylacetamid, N-Methyl-N-vinylformamid, N-Methyl-N-vinylacetamid und N-Vinylpyrrolidon auf ihre Fähigkeit untersucht, mit Initiatoren der kationischen Polymerisation Oligomere zu bilden. Mit N-Deutero-N-vinylformamid als Monomer und der 2H-NMR-Analyse der erhaltenen Oligomere wird der Einfluß der NH-Eliminierung während der Oligomerisation von N-Vinylformamid untersucht. Ausgehend von den experimentellen Ergebnissen wird ein für die Vinylpolymerisation neuer Mechanismus für die Oligomerisation von N-Vinylformamid vorgeschlagen und diskutiert. / The topic of the dissertation is the survey of the cationically initiated oligomerization of N-vinylformamide with iodine, bromine, trifluoromethanesulfonic acid, and trifluoromethanesulfonic acid trimethylsilylester as initiators. Quantum chemical calculations on the conformation and the electron density of N-vinylformamide, as well as on its reaction with electrophiles are presented. The structure of the obtained oligomers is investigated with 1H- and 13C NMR spectroscopy, MALDI-TOF-MS, GPC, IR spectroscopy, thermal decomposition, and quantitative combustion analysis. The influence of the polarity of the solvent, of the initiator, of the reaction temperature, and of the monomer/initiator ratio on yield, degree of polymerization, head group functionality, and chain structures of the obtained oligo(N-vinylformamide) is investigated. In comparison with N-vinylformamide, the ability of N-vinylacetamide, N-methyl-N-vinylformamide, N-methyl-N-vinylacetamide, and N-vinylpyrrolidone in undergoing a cationically induced polymerization to oligomeric products is investigated. The influence of the NH-elimination on the oligomerization process is investigated with N-deutero-N-vinylformamide as monomer and the 2H NMR analysis of the obtained oligomers. From the results, a new mechanism for the oligomerization of N-vinylformamide is proposed and discussed.

info:eu-repo/classification/ddc/540

ddc:540

Kationische Polymerisation

Enamide

Übertragungsreaktion

Oligomerisation

Oligomere

Polyvinylamide

N-Vinylformamid

Oligo(N-vinylformamid)

En-Reaktion

Wachstumsmechanismus

N-Formyl-imin

dimeres N-Methyl-N-vinylformamid

N-Vinylacetamid

Oligo(N-vinylacetamid)

Synthesis of Novel Extremely Sterically Hindered Tertiary Alkylamines

Shoker, Tharallah A.

18 April 2018

Three advanced methodologies for the preparation of extremely sterically hindered tertiary alkyl amines have been developed. The syntheses of 28 novel tertiary alkylamines that accommodate unusual steric hindrance are detailed. The electrophilic amination of alkyl Grignard reagents with N-chlorodialkylamines, in the presence of N,N,N′,N′-tetramethylethylenediamine (TMEDA) as a key additive, gives a variety of unprecedentedly sterically hindered tertiary alkylamines in good yields. Alternative strategy to 1-adamantyl-substituted (1-Ad) sterically hindered tertiary amines, which involved instead an SN1 reaction between 1-Ad cation with various secondary amines, is described. A complementary strategy to 1-Ad-based sterically hindered tertiary amines, which involves an iminium salt intermediate, is also reported. Salient features of the three protocols that are detailed here include unusual tolerance of steric hindrance, mild reaction conditions employed, ease of product isolation-purification, and absence of catalysts/transition metals. The molecular structures of two faithful examples of extremely sterically hindered tertiary alkylamines were determined by single crystal X-ray diffraction, and the height “h” of nitrogen pyramid of these compounds were measured. The NMR spectra show a restriction in rotation at room temperature among many hindered tertiary amines, and some of them exhibit two complete sets of peaks for two non-equivalent rotamers at room temperature. 15N NMR has been applied to study the structural changes in highly sterically hindered tertiary amines. Most of these compounds have been shown to undergo Hofmann type elimination reaction upon thermolysis at 100 degree in inert solvents, like toluene. / In der vorliegenden Arbeit wurden drei Methoden zur Synthese von tertitären Aminen mit extremer sterischer Hinderung entwickelt und zur Synthese von 28 neuen tertiären Alkylaminen mit entsprechender sterischer Hinderung angewendet. Die elektrophile Aminierung von Grignard-Reagenzien mit N-Chlordialkylaminen, unter Zusatz von N,N,N′,N′-Tetramethylethylendiamin (TMEDA) als Schlüsselkomponente, ermöglicht einen einfachen Zugang zu einer Vielzahl von tertiären Aminen mit extremer sterischer Hinderung mit guten Ausbeuten. Eine alternative Synthesestrategie unter SN1-Bedingungen führt zu sterisch-gehinderten 1-Adamantyl-substituierten (1-Ad) tertiären Aminen durch die Reaktion eines 1-Ad-Kations mit unterschiedlichen sterisch-gehinderten sekundären Aminen. Angelehnt an die zuvor beschriebene Reaktion können auch sterisch gehinderte Imine über eine Iminium-Salz-Zwischenstufe zu sterisch-gehinderten 1-Ad-substituierten tertiären Aminen umgesetzt werden. Auch in diesen Fall zeichnet sich die Reaktion durch eine bemerkenswerte Toleranz gegenüber sterischer Hinderung, milden Reaktionsbedingungen, leichte Produktisolierbarkeit und die Abwesenheit von Übergangsmetallkatalysatoren aus. Die molekulare Struktur zweier repräsentativer tertiärer Alkylamine mit extremer sterischer Hinderung wurde mittels Röntgeneinkristallstrukturanalyse untersucht und die Höhe “h” ihrer Stickstoff-Pyramide bestimmt. Die NMR-Spektren zeigen bei RT eine Einschränkung der freien Rotation um die N-C-Bindungsachse, teilweise führt dies zu vollständig getrennten Signalsätzen für die einzelnen Rotamere. 15N-NMR-Spektroskopie wurde ebenfalls zur Untersuchung von Strukturveränderungen genutzt. In inerten Lösungsmitteln, wie Toluol, zeigen die Verbindungen bei 100 °C in den meisten Fällen eine Hofmann-Eliminierung.

info:eu-repo/classification/ddc/540

ddc:540

Amine

Beitrag von Ackerbohne (Vicia faba L.), Luzerne (Medicago sativa L.) und Saatwicke (Vicia sativa L.) zur Selbstregelung der N-Zufuhr in leguminosenbasierten Fruchtfolgen. / The contribution of faba bean (Vicia faba L.), alfalfa (Medicago sativa L.) and vetch (Vicia sativa L.) to the self-regulation of N input in legume-based cropping systems.

Anthes, Johann

03 February 2005

No description available.

630 Landwirtschaft

Veterinärmedizin

Agricultural Sciences

Ackerbohne

Luzerne

Saatwicke

Dauerfeldversuch

Reinsaat

Gemengesaat

N-Fixierung

N-Transfer

N-Flächenbilanz

Selbstregulation

Faba bean

alfalfa

vetch

long term trial

sole crop

intercropped

N-fixation

N-transfer

N-balance

self-regulation

48.16

YA

Nitrogen availability and transformation in soils of acidified and nitrogen saturated mountain forest ecosystems / Nitrogen availability and transformation in soils of acidified and nitrogen saturated mountain forest ecosystems

TAHOVSKÁ, Karolina

January 2012

Nitrogen availability and transformation in acidified and N saturated soils of Czech (The Bohemian Forest, Ore Mountains) and Ukraine (Pop Ivan massif) mountain forest ecosystems were investigated. The study was primarily focused on the role of microbial immobilization in soil N retention. The study was based on field measurements (ion exchange resins), analyses of selected soil biochemical and microbial characteristics, and on laboratory experiments (15N labelling).

Use of the N,N-dialkyl-N’-benzoyl(thio)selenoureas as single source precursors for the synthesis of semiconducting quantum dots

Bruce, Jocelyn Catherine

12 1900

Thesis (PhD (Chemistry and Polymer Science))--Stellenbosch University, 2008. / The successful preparation and structural characterization of a number of N,N-dialkyl-N’-benzoyl(thio)selenourea ligands is described; where the intermolecular interactions are characterized by the presence of Resonance Assisted Hydrogen Bonding (RAHB), π- π interactions between neighbouring benzene residues only being evident amongst the longer alkyl chain derivatives. The first structural characterization of an asymmetrically substituted N,N-dialkyl- N’-benzoylselenourea ligand reveals an increased stability of the Z isomer in the solid state, this being reflected by the sulfur analogue. Attempts to synthesise N,N-dicyclohexyl-N’-benzoylselenourea led to the isolation and structural characterization of a novel 1,3,5-oxaselenazine salt and dicyclohexylaminobenzoate. The first structural characterization of a “bipodal” N,N-dialkyl-N’-benzoylselenourea ligand, 3,3,3’,3’-tetrabutyl-1,1’- isophthaloylbis(selenourea), reveals RAHB in the crystal lattice similar to that exhibited by the “monopodal” analogue, N,N-dibutyl-N’-benzoylselenourea. The successful complexation of the N,N-dialkyl-N’-benzoyl(thio)selenourea ligands to a number of different transition metal ions is reported allowing the preparation of several potential single source precursors. Coordination through the O and Se/S donor atoms to Pd(II) results in the formation of square planar metal complexes, with a cis conformation, several of which could be structurally characterized. In particular, the first structural elucidation of an asymmetrically substituted N,N-dialkyl-N’-benzoylselenourea metal complex, cis-bis(N-benzyl-N-methyl-N’- benzoylselenoureato)palladium(II) indicates the increased stability of the EZ isomer in the solid state. Structural elucidation of the novel (N,N-diphenyl-N’-benzoylselenoureato)cadmium(II) reveals a bimetallic complex in the solid state, where the expected 2:1 ligand : metal ratio is maintained, and the two Cd(II) centres are 5 and 6 coordinated, with O and Se donor atoms. Multinuclear Nuclear Magnetic Resonance (NMR) Spectroscopy has been employed in the thorough characterisation of the potential single source precursors, 77Se NMR spectroscopy indicating a decreased shielding of the 77Se nucleus as the “hardness” of the central metal ion increases i.e. Pd(II) > Zn(II) > Cd(II). Use of 113Cd NMR spectroscopy indicates the preferential binding of N,N-diethyl-N’- benzoylselenourea to Cd(II) over that of its sulfur analogue, and initial studies suggest a form of chelate metathesis taking place in solution. 31P NMR spectroscopy is used to gain insight into the formation of cis-bis(N,N-diethyl-N’- benzoylselenoureato)Pt(II). Thermolysis of (N,N-diethyl-N’-benzoylselenoureato)cadmium(II) and its sulfur analogue led to the successful synthesis of CdSe and CdS quantum dots respectively, where thermolysis over a range of temperatures allows a degree of size control over the resulting nanoparticles. The effect of precursor alkyl chain length on nanoparticle morphology was investigated for both the N,N-dialkyl-N’-benzoylthio- and –selenoureas. A correlation between the two for the (N,N-dialkyl-N’-benzoylselenoureato)Cd(II) complexes is described and possible growth mechanisms are discussed. Preliminary investigations into the use of other N,N-dialkyl-N’-benzoyl(thio)selenourea metal complexes as single source precursors reveal that both (N,N-diethyl-N’-benzoylselenoureato)Zn(II) and its sulfur analogue show potential as single source precursors for the formation of ZnO and ZnS nanoparticles respectively. Initial studies into the use of N,N-dialkyl-N’-benzoyl(thio)selenourea metal complexes as single source precursors for the synthesis of core-shell nanoparticles is briefly described. The Aerosol Assisted Chemical Vapour Deposition (AACVD) of several N,N-dialkyl-N’-benzoyl(thio)selenourea metal complexes is reported, where both (N,N-diethyl-N’-benzoylselenoureato)Cd(II) and its sulfur analogue allow the deposition of crystalline CdSe and CdS respectively. The AACVD of (N,N-diethyl-N’- benzoylselenoureato)Zn(II) leads to the deposition of crystalline ZnSe, ZnS being deposited by (N,N-diethyl-N’-benzoylthioureato)Zn(II). The deposition of heazelwoodite (Ni3S2) with varying morphologies results from the AACVD of cis-bis(N,N-diethyl-N’-benzoylthioureato)Ni(II). Thermal annealing of the amorphous material deposited by the AACVD of cis-bis(N,N-diethyl-N’-benzoylthioureato)Pd(II), allows the formation of highly crystalline palladium. The deposition of metallic platinum using cis-bis(N,N-diethyl-N’-benzoylthioureato)Pt(II) is described as well as the deposition of crystalline Pd17Se15 from cis-bis(N,N-diethyl-N’-benzoylselenoureato)Pd(II). This, to the best of our knowledge, is the first time that AACVD has been performed, using the N,N-dialkyl-N’- benzoyl(thio)selenourea metal complexes as single source precursors, in addition, we believe it to be the first time that palladium selenide has been deposited using the AACVD technique.

Nanoparticles

N,N-dialkyl-N'-aryl(thio)selenoureas

Single source precursors

Chemical vapour deposition

Dissertations -- Chemistry

Theses -- Chemistry

Plan de negocios para el ingreso al mercado chileno de empresa nutricional espa?ola

Barr?a Pizarro, Cecilia Daniela del Pilar

January 2017

Tesis para optar al grado de Mag?ster en Gesti?n para la Globalizaci?n / El objetivo de este trabajo es presentar un an?lisis de mercado y plan de negocios de la empresa nutricional espa?ola Nutrici?n 3G, el cual es un emprendimiento de investigadores espa?oles con amplia experiencia en el ?mbito universitario. Su servicio es vendido a los profesionales nutricionistas, quienes se los ofrecen a sus pacientes. Se toma una muestra de saliva de los pacientes y por medio de un an?lisis realizado en la casa matriz en Espa?a, entregan las probabilidades de desarrollar diversas enfermedades no transmisibles, tales como diabetes, dislipidemias, osteoporosis, ictus, etc. En Espa?a, Nutrici?n 3G ha tenido relativo ?xito y est? en condiciones financieras y de recursos de buscar nuevos clientes en otros mercados, siendo Latinoam?rica, la alternativa m?s factible. Se realiz? un an?lisis de cuatro mercados potenciales; Chile, Per?, Colombia y M?xico, resultando Chile el pa?s con mayor potencial de entrada y penetraci?n del servicio por medio de un representante en el pa?s. El mercado presenta una gran cantidad de competidores directos e indirectos y un p?blico objetivo muy espec?fico (profesionales nutricionistas) sin embargo, el an?lisis del negocio, utilizando una tasa de descuento de 10,24,%; arroj? una recuperaci?n de la inversi?n inicial al cabo de dos a?os, una tasa interna de retorno de 48% y VAN a los 5 a?os de 5.479 Euros. Situaci?n similar se dan en el an?lisis de escenario. Se evalu? la variaci?n en la venta de kits con variaciones del 10% (+10% en el caso optimista y -10% en el caso pesimista) presentando ambos casos recuperaci?n de la inversi?n de aproximadamente 2 a?os; TIR?s de 50% y 33%; ambas superiores a la tasa de descuento y con VAN?s positivas. Como conclusi?n, pese a lo competitivo del mercado, se recomienda el lanzamiento de Nutrici?n 3G en el mercado chileno.

Nutrici?n - Aspectos econ?micos

Gesti?n de negocios - Chile

Evaluation of the enzyme inhibitory effect of carboxymethylated chitosan / Ian Dewald Oberholzer

Oberholzer, Ian Dewald

January 2003

Degradation of peroral administered drugs by various enzymes in the gastrointestinal tract has proven to be troublesome for the absorption' and bioavailability of protein and peptide drugs. Mucoadhesive polymers such as poly(acrylates) have proven to inhibit protease enzymes responsible for initiating digestion of peptide drugs. Enzyme inhibitors have unique chemical properties enabling it to interact with enzymes to form complexes with such enzymes prohibiting it from functioning properly. Anionic carboxymethylated chitosan derivatives such as N,N-dicarboxymethyl chitosan and N, O-carboxymethyl chitosan display unique structural similarities to enzyme inhibitors being anionic polymers that may interact with bi-valent cations... / Thesis (M.Sc. (Pharm.))--North-West University, Potchefstroom Campus, 2004.

Mucoadhesive polymers

Protease enzymes

Enzyme inhibitors

N,N-dicarboxymethyl chitosan

N,O-carboxymethyl chitosan

Proteolytic [alpha]-chymotrypsin

Studies On The Functional Roles Of Peptidase N, A M1 Family Member, During Stress And Infection

Bhosale, Manoj

09 1900

The cytosolic protein degradation pathway, performed by ATP-dependent proteases and ATP-independent peptidases, plays important roles in several cellular activities, e.g. cell division, cell cycle progression, intracellular signaling, MHC class I antigen presentation, host-pathogen interactions, etc. The roles of ATP-dependent proteases during stress and infection have been studied in great detail but the functional roles of ATP-independent peptidases are not clearly understood. In this study, the functional roles of E. coli or S. typhimurium encoded Peptidase N (PepN), an ATP-independent enzyme belonging to theM1 family of metallopeptidases, were investigated. The thesis will address four different aspects. (i) In the first part, the utility of using E coli ∆pepN to identify and characterize novel peptidases will be shown. It is known that deletion of pepN leads to inability to cleave the majority of in vitro peptidase substrates in E. coli and S. typhimurium. To study the differences between two closely related paralogs of the M17 family, E. coli encoded pepA and pepB were cloned in pBAD24 vector and introduced in E. coli ∆pepN. Peptidase A (PepA) and Peptidase B (PepB) expression increases the cleavage of several aminopeptidase substrates and partially rescues growth of ∆pepN during nutritional downshift and high temperature stress (NDHT), a dual stress involving growth in minimal media at 42°C. Purified PepA and PepB enzymes display broad substrate specificity; however, distinct differences are observed between these two paralogs: PepA is more stable at high temperature whereas PepB displays broader substrate specificity as it cleaves Asp and Insulin B chain peptide. The strategy utilized in this study, i.e. overexpression of peptidases in ∆pepN followed by screening for substrate specificities in total cell extracts, may be used to rapidly identify the substrate preferences of novel peptidases encoded in genomes of different organisms. (ii) The second aspect investigates the functional roles of PepN during stress and infection in S. typhimurium. PepN has two conserved signature motifs of the M1 family, GAMEN and HEXXH, which play roles in substrate recognition and catalysis. To address the roles of catalytic activity of PepN, the residue E-298, which is present in the HEXXH motif and acts as a general base during catalysis, was mutated to A-298 by site-specific mutagenesis and introduced into ∆pepN (pBR322/pepNE298A). Biochemical and biophysical analysis of purified PepN (WT and E298A) revealed loss of catalytic activity of E298A but no major structural changes were observed in comparison to the WT protein. The functional roles of this mutation using ∆pepN expressing pBR322/pepN or pBR322/pepNE298A were investigated using two conditions: (i) Nutritional downshift high temperature (NDHT)stress and (ii) systemic infection in mice. Monitoring growth profiles of different strains demonstrated the requirement of the enzymatic activity of PepN for adaptation and growth to NDHT stress. Earlier studies have shown that S. typhimurium ∆pepN hyper proliferates in peripheral organs during systemic infection in mice. However, expression of wild type (WT)or E298A PepN led to lower colony forming units (CFU), demonstrating that the decrease in CFU is independent of catalytic activity. These observations are consistent with lower serum amounts of inflammatory cytokines, lower tissue damage and increase in survival of mice infected with S. typhimurium expressing WT or E298A PepN. (iii) Although pathogen encoded peptidases are known to be important during infection, their roles in modulating host responses in immunocompromised individuals are not well studied. In the third part of this thesis, the roles of S. typhimurium encoded PepN were studied in mice lacking Interferon-γ (Ifnγ), a cytokine important for immunity. S. typhimurium lacking pepN displays enhanced CFU compared to WT in peripheral organs during systemic infection in C57BL/6 mice. However, Ifnγ-/-mice show higher CFU compared to C57BL/6 mice, resulting in lower fold differences between WT and ∆pepN. Concomitantly, reintroduction of pepN in ∆pepN reduces CFU, demonstrating pepN dependence. In addition, three distinct differences were observed between infection ofC57BL/6 and Ifnγ-/-mice upon infection with different S. typhimurium strains: (i) cytokine profiles, (ii) histological analysis and (iii) mice survival. Overall, the roles of the host encoded Ifnγ during infection with S. typhimurium strains with varying degrees of virulence will be highlighted. (iv) The final aspect of this study reveals differences in gene expression between S. typhimurium grown in rich medium (Luria-Bertani) versus NDHT stress. This adaptation affects several pathways and the gene expression of secretory proteins that are important for virulence in S. typhimurium are greatly reduced during NDHT stress. Also, analysis of secretory protein amounts in different media conditions shows reduction during growth in minimal media plus high temperature stress. The functional consequences of this reduction in secretory protein amounts lead to lower bacterial replication after infection of RAW cells or mice infected via the oral route. In addition, the differences in gene expression between WT and ∆pepN during these conditions were studied. Interestingly, there is reduction in expression of flagellar genes whereas the genes involved in nitrogen metabolism are upregulated in ∆pepN upon exposure to NDHT stress. Further studies were performed by quantifying the motility of different S. typhimurium strains grown in a variety of culture conditions. Overall, this part of the study attempts to compare and contrast the possible adaptive responses of WT and ∆pepN to NDHT stress. Together, this thesis addresses multiple aspects of the biochemistry and roles of the enigmatic PepN during stress and infection.

PeptidaseN

Peptidase N

Bacterium typhimurium

Typhoid Infection

E Coli Peptidase N

Salmonella typhimurium Peptidase N

PepN

Metallopeptidases

Biochemistry