Bestimmung von Tal-Rücken-Umschlagpunkten auf Potentialenergieflächen mittels eines Variationsansatzes für Newtontrajektiorien

Schmidt, Benjamin

20 October 2017

Das Konzept des Minimum-Energie-Pfades (MEP) dient als grundlegendes Modell, um den Ablauf chemischer Reaktionen zu verstehen. Es basiert auf der Theorie des Übergangszustandes, derzufolge Ausgangsstoffe und Reaktionsprodukte energetisch stabile Zustände bilden, die durch eine Potentialbarriere voneinander getrennt sind. Beim Übergang der Reaktanten in die Produkte gilt es, diese Barriere zu ¨uberwinden.

info:eu-repo/classification/ddc/000

ddc:000

Current BIM Practices of Commercial MEP Contractors

Kent, Bryan John

04 June 2014

Building Information Modeling (BIM) use in the contracting industry has grown significantly in recent years. With this change in the construction industry, consensus has not been reached as to what BIM is, who is using it and what they are using it for. The purpose of this research was to determine current BIM practices of US-based commercial MEP contractors. Executive, middle management, and field personnel were interviewed to determine the current BIM practices in their companies. The majority of companies interviewed were using BIM and most were using it on a significant portion of their projects. The majority of MEP contractors using BIM were seeing positive results in many of six key performance indicators, profitability, schedule duration, field efficiency, change orders, rework, and safety. The top uses of BIM for MEP contractors were clash detection coordination, prefabrication, design creation, and quantity take-off/cost estimating. Most MEP contractors have not yet incorporated BIM for scheduling, sequencing, or safety analysis. Additionally most MEP contractors did not have a formal BIM training program in their company.

building information modeling

BIM

MEP

current practices

clash detection

prefabrication

Construction Engineering and Management

A New Approach to Measuring Market Expectations and Term Premia

Ye, Xiaoxia

January 2015

No / This article develops a novel approach for measuring market expectations and term premia in the term structure of interest rates. Key components of this approach are generic impact measures of state variables in a Gaussian dynamic term structure model. These measures are inherent in a particular state variable regardless of how other state variables are defined within the model. With the help of these measures, the approach gives rise to market expectations that predict yield changes well, and term premia with a legitimate impact on the forward curve. In my empirical analysis, I show the generic impact of the short rate on the yield curve, and present observations of the historical dynamics of market expectations and term premia. The calibrated model is also employed to study the impacts of recent unconventional monetary policies.

Monoclonal Antibody Expression and Novel Purification in Nicotiana benthamiana

Fulton, Andrew Dale

28 June 2011

Over the past few decades researchers and industrial professionals alike have realized the vast potential of monoclonal antibodies to treat diseases ranging from arthritis, immune and infectious diseases to cancer. There are a number of antibodies on the market that constitute a large portion of the biopharmaceutical niche in the drug industry. Blockbuster drugs (selling greater than $1 billion/year), include antibodies such as Avastin (bevacizumab), Herceptin (trastuzumab), Rituxan (rituximab), Humira (adalimumab) and Remicade (infliximab), which are cornerstones in this type of sector. With the cost of development to market approval rising astronomically for a new drug, new ways to produce and process these molecules becomes a paramount objective to ultimately help both patients and drug developers. Plants, such as Nicotiana benthamiana, offer a unique production platform due to their recently found ability to produce large amounts of therapeutic proteins in a quick manner. While production would be simple and cheap, purification would not be due to the presence of toxic compounds in ground plant tissue. The current methods to purify these molecules from plant extract include expensive affinity column steps (Protein A/G) that are difficult to scale-up to bed volumes that would be necessary for this technology. In the following paper, a method to purify a monoclonal antibody by non-Protein A/G resins is accomplished and compared to purification by Protein A. The modified process involved an UF/DF step, a precipitation of native impurities step using a charged polymer, hydrophobic interaction chromatography and hydrophobic charge induction chromatography. The yield of this modified process was 19.0%. This process compared favorably with Protein A due to the fact that even with washing steps including NaCl and Tween-20, the Protein A elution fraction still contained a large portion of host cell impurities. A chromatography step would need to be included before Protein A to both protect the column resin and provide a more purified immunoglobulin. / Master of Science

Ebola virus

monoclonal antibodies

MEP HyperCelTM

transgenic plants

antibody purification

Protein A

MMV008138 and analogs: potential novel antimalarial agents for P. falciparum

Liu, Lixuan

15 May 2018

Malaria is a severe and deadly mosquito-borne disease. Although treatable, the continuous emergence of multi-drug resistant parasite strains urgently calls for the development of novel antimalarial agents. P. falciparum parasites synthesize essential isoprenoid precursors, isopentenyl pyrophosphate (IPP) and dimethylallyl pyrophosphate (DMAPP), via a non-mevalonate pathway: the methylerythritol phosphate (MEP) pathway. This pathway is not utilized by humans. Thus, compounds that target the MEP pathway and disrupt isoprenoid biosynthesis in P. falciparum hold promise as potent and safe new antimalarial agents, that engage new targets. Previously, we and others identified MMV008138 from the Malaria Box as a MEP pathway targeting compound. Later work revealed that it targets the IspD enzyme within the MEP pathway. Work in the Carlier group has established preliminary structure-activity relationship (SAR) of MMV008138: 1) (1R,3S)-configuration is required; 2) 2', 4'-disubstitution of the D-ring with small, electronegative substituents; 3) functional importance of carboxylate acid at C3. In this work, I aim to gain further insight into the C3 SAR and A-ring SAR of lead compound MMV008138. Synthesized acid bioisosteres and A-ring analogs of MMV008138 were evaluated in their ability to inhibit P. falciparum parasite growth. We showed that the C3 substituent of MMV008138 has a very tight SAR, and likely interacts with a very constricted pocket within the PfIspD enzyme. A-ring modifications are limited to certain positions of MMV001838 and need to be sterically small. However, we have yet to identify a modification that significantly improves drug lead potency. Future work will continue towards understanding the A-ring SAR of MMV008138, as well as D-ring SAR and C1-SAR. Efforts will also be directed towards finding analogs with improved potency, transport and metabolic stability. / MS

malaria

antimalarial

P. falciparum

MEP pathway

IspD

MMV008138

structure-activity relationship

Avaliação do álcool perílico como potencial antimalárico em Plasmodium falciparum e Plasmodium berghei. / Evaluation of perillyl alcohol as potential antimalarial in Plasmodium falciparum and Plasmodium berghei.

Rodriguez, Adriana Alejandra Marin

23 November 2015

A malária mata mais de um milhão de pessoas por ano, sendo uma das doenças infecciosas mais relevantes e um grande problema de saúde pública. Além disso, o surgimento de cepas resistentes aos quimioterápicos utilizados faz necessário o estudo de novos alvos para tratamentos contra esta doença. No nosso laboratório foi demonstrada a biossíntese de isoprenóides, em P. falciparum pela via MEP. Sabe-se que substâncias inibidoras da biossíntese de isoprenóides, dentre essas os terpenos, apresentam atividade antimalárica. Levando em consideração o anterior, nós avaliamos o potencial antimalárico do álcool perilico (POH) em P. falciparum e P. berghei. Nossos resultados demonstraram que o POH teve efeito inibitório contra o crescimento do P. falciparum in vitro, nas cepas 3D7 e K1 com uma IC50 de 4,8 ± 0,5 &mu;M, e 10,41±2,33 &mu;M, respectivamente. Além disso, o POH não teve efeito tóxico na linhagem celular Vero. Ainda, Comprovamos que o POH inibiu a farnesilação de proteinas entre 20 e 37 KDa de P. falciparum. Por outro lado, os experimentos in vivo não mostraram eficácia do tratamento do POH contra PbGFP em camundongos Balb/c. Em contraste, foi demostrada a eficácia do POH na de malária cerebral experimental (MCE), , indicando uma redução na taxa de incidência da MCE no grupo tratado com POH, comparado o não tratado ( P<0,05). Além disso, o POH reduziu a inflamação no cérebro dos animais tratados, uma vez que teve uma redução significativa na adesão de leucócitos aos vasos cerebrais (P<0.001), como também, o numero de hemorragias foi menor comparados com os animais não tratados. (P<0.0001). Portanto, os resultados obtidos nesta pesquisa abrem novas alternativas no estudo do mecanismo de ação do POH como um terpeno com grande potencial para tratar MC. / Malaria kills over one million people a year worldwide, and is one of the most important infectious diseases and a major public health problem. Furthermore, the emergence of resistant strains to chemotherapeutic agents used, make it necessary to study new targets for treatments against this disease. In our laboratory we have demonstrated the isoprenoids biosynthesis in P. falciparum, by the MEP pathway. It is known that the substances that inhibit isoprenoid biosynthesis, among these terpenes, have antimalarial activity in vitro and in vivo. Considering this, we evaluate the antimalarial potential of PA (POH) in P. falciparum and P. berghei. Our results showed that the POH had inhibitory effect against the growth of strains 3D7 and K1 of P. falciparum in vitro, with an IC50 of 4.8 &mu;M ± 0.5, and 10.41 ± 2.33 &mu;M, respectively. Furthermore, the POH had no toxic effect on cell line Vero. Moreover, the POH proved that inhibited proteins farnesylation from 20 to 37 kDa of P.falciparum. On the other hand, in vivo experiments did not show efficacy on treatment against POH PbGFP in BALB/c mice. In contrast, the effectiveness of POH in the experimental cerebral malaria (MCE) was demonstrated, indicating a reduction in the incidence rate of MCE in the group treated with POH, compared with of untreated animals (P <0.05). In addition, the POH reduced inflammation in the brain of treated animals, since it had a significant reduction in leukocyte adhesion to cerebral vessels (P <0.001), as also the number of bleeding was lower compared to untreated animals (P<0.0001). Therefore, the results obtained in this work provide new alternatives to study the POH\'s mechanism of action as a terpene with great potential to treat MC.

Plasmodium berghei

Plasmodium berghei

Plasmodium falciparum

Plasmodium falciparum

Álcool perílico

Experimental cerebral malária

Intranasally

Isoprenilação de proteínas

Isoprenoides

Isoprenoids

Malaria cerebral experimental

MEP pathway

Perillyl alcohol

Proteins isoprenylation

Via intranasal

Via MEP

Avaliação do álcool perílico como potencial antimalárico em Plasmodium falciparum e Plasmodium berghei. / Evaluation of perillyl alcohol as potential antimalarial in Plasmodium falciparum and Plasmodium berghei.

Adriana Alejandra Marin Rodriguez

23 November 2015

A malária mata mais de um milhão de pessoas por ano, sendo uma das doenças infecciosas mais relevantes e um grande problema de saúde pública. Além disso, o surgimento de cepas resistentes aos quimioterápicos utilizados faz necessário o estudo de novos alvos para tratamentos contra esta doença. No nosso laboratório foi demonstrada a biossíntese de isoprenóides, em P. falciparum pela via MEP. Sabe-se que substâncias inibidoras da biossíntese de isoprenóides, dentre essas os terpenos, apresentam atividade antimalárica. Levando em consideração o anterior, nós avaliamos o potencial antimalárico do álcool perilico (POH) em P. falciparum e P. berghei. Nossos resultados demonstraram que o POH teve efeito inibitório contra o crescimento do P. falciparum in vitro, nas cepas 3D7 e K1 com uma IC50 de 4,8 ± 0,5 &mu;M, e 10,41±2,33 &mu;M, respectivamente. Além disso, o POH não teve efeito tóxico na linhagem celular Vero. Ainda, Comprovamos que o POH inibiu a farnesilação de proteinas entre 20 e 37 KDa de P. falciparum. Por outro lado, os experimentos in vivo não mostraram eficácia do tratamento do POH contra PbGFP em camundongos Balb/c. Em contraste, foi demostrada a eficácia do POH na de malária cerebral experimental (MCE), , indicando uma redução na taxa de incidência da MCE no grupo tratado com POH, comparado o não tratado ( P<0,05). Além disso, o POH reduziu a inflamação no cérebro dos animais tratados, uma vez que teve uma redução significativa na adesão de leucócitos aos vasos cerebrais (P<0.001), como também, o numero de hemorragias foi menor comparados com os animais não tratados. (P<0.0001). Portanto, os resultados obtidos nesta pesquisa abrem novas alternativas no estudo do mecanismo de ação do POH como um terpeno com grande potencial para tratar MC. / Malaria kills over one million people a year worldwide, and is one of the most important infectious diseases and a major public health problem. Furthermore, the emergence of resistant strains to chemotherapeutic agents used, make it necessary to study new targets for treatments against this disease. In our laboratory we have demonstrated the isoprenoids biosynthesis in P. falciparum, by the MEP pathway. It is known that the substances that inhibit isoprenoid biosynthesis, among these terpenes, have antimalarial activity in vitro and in vivo. Considering this, we evaluate the antimalarial potential of PA (POH) in P. falciparum and P. berghei. Our results showed that the POH had inhibitory effect against the growth of strains 3D7 and K1 of P. falciparum in vitro, with an IC50 of 4.8 &mu;M ± 0.5, and 10.41 ± 2.33 &mu;M, respectively. Furthermore, the POH had no toxic effect on cell line Vero. Moreover, the POH proved that inhibited proteins farnesylation from 20 to 37 kDa of P.falciparum. On the other hand, in vivo experiments did not show efficacy on treatment against POH PbGFP in BALB/c mice. In contrast, the effectiveness of POH in the experimental cerebral malaria (MCE) was demonstrated, indicating a reduction in the incidence rate of MCE in the group treated with POH, compared with of untreated animals (P <0.05). In addition, the POH reduced inflammation in the brain of treated animals, since it had a significant reduction in leukocyte adhesion to cerebral vessels (P <0.001), as also the number of bleeding was lower compared to untreated animals (P<0.0001). Therefore, the results obtained in this work provide new alternatives to study the POH\'s mechanism of action as a terpene with great potential to treat MC.

Plasmodium berghei

Plasmodium falciparum

Álcool perílico

Isoprenilação de proteínas

Isoprenoides

Malaria cerebral experimental

Via intranasal

Via MEP

Plasmodium berghei

Plasmodium falciparum

Experimental cerebral malária

Intranasally

Isoprenoids

MEP pathway

Perillyl alcohol

Proteins isoprenylation

Steigerung der Effektivität repetitiver Doppelpuls-TMS mit I-Wellen-Periodizität (iTMS) durch individuelle Adaptation des Interpulsintervalls

Sewerin, Sebastian

01 December 2014

Die transkranielle Magnetstimulation (TMS) ist ein nichtinvasives Hirnstimulationsverfahren, mit welchem sowohl die funktionelle Untersuchung umschriebener kortikaler Regionen als auch die Modulation der Erregbarkeit ebendieser sowie die Induktion neuroplastischer Phänomene möglich ist. Sie wurde in der Vergangenheit insbesondere bei der Erforschung des humanen zentralmotorischen Systems angewandt. Dabei zeigte sich, dass ein einzelner über dem primärmotorischen Areal (M1) applizierter TMS-Puls multiple deszendierende Erregungswellen im Kortikospinaltrakt induzieren kann. Von diesen Undulationen besitzt die D-Welle (direkte Welle) die kürzeste Latenz und sie rekurriert auf eine direkte Aktivierung kortikospinaler Neurone, wohingegen I-Wellen (indirekte Wellen) längere Latenzen besitzen und durch transsynaptische Aktivierung dieser Zellen entstehen. Bemerkenswert ist das periodische Auftreten der letztgenannten Erregungswellen mit einer Periodendauer von etwa 1,5 ms. Zwar sind die genauen Mechanismen noch unbekannt, welche der Entstehung dieser I-Wellen sowie dem Phänomen der I-Wellen-Fazilitierung, das sich in geeigneten TMS-Doppelpulsprotokollen offenbart, zugrunde liegen, jedoch existieren hierzu verschiedene Erklärungsmodelle. Im Mittelpunkt der vorliegenden Arbeit steht die repetitive Anwendung eines TMS-Doppelpulsprotokolls, bei dem das Interpulsintervall (IPI) im Bereich der I-Wellen-Periodizität liegt (iTMS) und das gleichsam durch eine Implementierung der I-Wellen-Fazilitierung in der repetitiven TMS charakterisiert ist. Da gezeigt werden konnte, dass iTMS mit einem IPI von 1,5 ms (iTMS_1,5ms) die kortikospinale Erregbarkeit signifikant intra- und postinterventionell zu steigern vermag, und die I-Wellen-Periodizität interindividuellen Schwankungen unterliegt, wurde in der hier vorgestellten Studie an Normalprobanden der Einfluss einer individuellen Anpassung des IPIs (resultierend in der iTMS_adj) auf die intrainterventionelle kortikospinale Erregbarkeit untersucht. In der Tat stellte sich heraus, dass die iTMS_adj der iTMS_1,5ms diesbezüglich überlegen ist. Dieses Ergebnis unterstreicht das Potential einer Individualisierung der interventionellen TMS für erregbarkeitsmodulierende Effekte und macht dasjenige der ohnehin auf physiologische Prozesse abgestimmten iTMS explizit, was insbesondere für klinische Anwendungen relevant sein mag.

transkranielle Magnetstimulation (TMS)

I-Wellen-Periodizität

motorisch evoziertes Potential (MEP)

primärmotorischer Kortex (M1)

kortikospinale Erregbarkeit

Doppelpulsstimulation

transcranial magnetic stimulation (TMS)

I-wave periodicity

motor evoked potential (MEP)

primary motor cortex (M1)

corticospinal excitability

paired-pulse stimulation

ddc:612

A global search algorithm for phase transition pathways in computer-aided nano-design

He, Lijuan

13 January 2014

One of the most important design issues for phase change materials is to engineer the phase transition process. The challenge of accurately predicting a phase transition is estimating the true value of transition rate, which is determined by the saddle point with the minimum energy barrier between stable states on the potential energy surface (PES). In this thesis, a new algorithm for searching the minimum energy path (MEP) is presented. The new algorithm is able to locate both the saddle point and local minima simultaneously. Therefore no prior knowledge of the precise positions for the reactant and product on the PES is needed. Unlike existing pathway search methods, the algorithm is able to search multiple transition paths on the PES simultaneously, which gives us a more comprehensive view of the energy landscape than searching individual ones. In this method, a Bézier curve is used to represent each transition path. During the searching process, the reactant and product states are located by minimizing the two end control points of the curve, while the shape of the transition pathway is refined by moving the intermediate control points of the curve in the conjugate directions. A curve subdivision scheme is developed so that multiple transitions paths can be located. The algorithm is demonstrated by examples of LEPS potential, LEPS plus harmonic oscillator potential, and PESs defined by Rastrigin function and Schwefel function.

Saddle point

Multiple transition pathway

MEP

Bézier curve

Curve subdivision scheme

Nanotechnology

Nanostructures

Algorithms

Creating Interactive Visualizations for Twitter Datasets using D3

Björck, Olof

January 2018

Project Meme Evolution Programme (Project MEP) is a research program directed by Raazesh Sainudiin, Uppsala University, Sweden, that collects and analyzes datasets from Twitter. Twitter can be used to understand how ideas spread in social media. This project aims to produce interactive visualizations for datasets collected in Project MEP. Such interactive visualizations will facilitate exploratory data analysis in Project MEP. Several technologies had to be learned to produce the visualizations, most notably JavaScript, D3, and Scala. Three interactive visualizations were produced; one that allows for exploration of a Twitter user timeline and two that allows for exploration and understanding of a Twitter retweet network. The interactive visualizations are accessible as Scala functions and in a website developed in this project and uploaded to GitHub. The interactive visulizations contain some known bugs but they still allow for useful exploratory data analysis of Project MEP datasets and the project goal is therefore considered met. / Project Meme Evolution Programme

D3

JavaScript

Interactive Visualizations

Visualization

Visualizations

Project MEP

Computational Mathematics

Beräkningsmatematik

Other Computer and Information Science

Annan data- och informationsvetenskap