In Vitro Adsorption of Heavy Metals Using Metal-Organic Frameworks

Ngule, Chrispus M., Jr

17 August 2020

No description available.

Chemistry

Materials Science

Toxicology

Therapy

Environmental Science

Environmental Management

Environmental Health

Impact of autocrine factors on physiology and productivity in Trichoplusia ni serum-free cultures

Eriksson, Ulrika

January 2005

The aim of this study was to increase the understanding of the mechanisms regulating cell proliferation and recombinant protein production in serum-free cultures of Trichoplusia ni (T. ni) insect cells. Conditioned medium (CM) was shown to contain both stimulatory and inhibitory factors (CM factors) influencing cell growth. Metalloproteinase (MP) activity was the major factor responsible for the growth stimulating effect of CM as shown by using the specific MP inhibitor DL-thiorphan. MPs may exist in several different molecular mass forms due to autoproteolysis. Although the main band of the MP was determined to be around 48 kDa, precursor forms above 48 kDa as well as autocatalytic degradation products below the main band could be observed. It is not clear whether all forms of the MP or just the main band is involved in the growth regulation. Further, a proteinase inhibitor could be identified in the inhibitory fraction. Thus, we speculate that the proteinase inhibitor may be part of an autocrine system regulating cell proliferation. Analysis of the cell cycle phase distribution revealed a high proportion of cells in the G1 (80-90 %) and a low proportion of cells in the S and G2/M phases (10-20 %) during the whole culture, indicating that S and G2/M are short relative to G1. After inoculation, a drastic decrease in the S phase population together with a simultaneous increase of cells in G1 and G2/M could be observed as a lagphase on the growth curve and this may be interpreted as a temporary replication stop. When the cells were released from the initial arrest, the S phase population gradually increased again. This was initiated earlier in CM-supplemented cultures, and agrees with the earlier increase in cell concentration. Thus, these data suggests a correlation between CM factors and the cell cycle dynamics. In cultures supplied with CM, a clear positive effect on specific productivity was observed, with a 30 % increase in per cell productivity. The specific productivity was also maintained at a high level much longer time than in fresh-medium cultures. The positive effect observed after 20 h coincided with the time a stimulatory effect on cell growth first was seen. Thus, the productivity may be determined by the proliferation potential of the culture. A consequence of this would be that the secreted MP indirectly affects productivity. Finally, the yeast extract from Express Five SFM contains factors up to 35 kDa which are essential for T. ni cell growth. The optimal concentration was determined to be 2.5-fold that in normal medium, while higher concentrations were inhibitory. However although vital, they were not solely responsible for the growth-enhancing effect, as some other, more general, component present in yeast extract was needed for proliferation as well. / <p>QC 20101129</p>

Biotechnology

Trichoplusia ni

High Five

insect cells

BEVS

serum-free medium

yeast extract

conditioned medium

autocrine regulation of proliferation

growth factors

cell cycle

metalloproteinase

specific productivity

Bioteknik

Industrial Biotechnology

Industriell bioteknik

Systemische Wirkungen und Nebenwirkungen einer dermal verabreichten dexamethasonhaltigen Formulierung bei klinisch gesunden Pferden

Allersmeier, Maren

23 November 2010

Da topische Glucocorticoide im Vergleich zur parenteralen Anwendung weniger systemische (Neben)Wirkungen haben können, werden sie bevorzugt in der Human- und Veterinärmedizin eingesetzt. Jedoch konnte bei vielen Untersuchungen gezeigt werden, dass topische Glucocorticoide je nach Applikationsdauer, -ort, Wirkstoffpotenz, -dosis und Behandlungsfläche ausgeprägte messbare Reaktionen wie Suppression der HHNA und der Immunzellen hervorrufen können. Beim Pferd wurden jedoch dahingehend bisher keine Untersuchungen durchgeführt. Da Glucocorticoide im Pferdesport auch dopingrelevant sind wurde der Frage nachgegangen, ob nach der dermalen Applikation eines niederpotenten Glucocorticoidpräparates auf die Haut gesunder Pferde systemische Effekte auftreten können und ob ein, nach perkutaner Resorption auftretender, Wirkstoffspiegel im Blut gemessen werden kann. Im Rahmen dieser Dissertation standen 10 erwachsene, klinisch gesunde Versuchspferde zur Verfügung. Die Versuchsdurchführung erfolgte in 3 Phasen. Vor Behandlungsbeginn (Tag 0) wurden von jedem Pferd die Kontrolldaten erfasst. Die Applikation der Dexamethasonformulierung erfolgte über einen Zeitraum von 10 Tagen. 2 mal täglich wurden 50 g einer 0,017 %igen Dexamethasonemulsion auf eine definierte Hautfläche (30 x 50 cm) aufgetragen. Die Blutentnahmen zur Gewinnung der Proben erfolgten am 2., 6., 8., und 10. Tag der Behandlung. Die Nachbehandlungsphase erstreckte sich über einen Zeitraum von 20 Tagen ohne die Dexamethasonanwendung. Hier erfolgte die Probengewinnung an den Tagen 3, 7, 11, 14 und 20 nach Absetzen der Behandlung. Aus den gewonnenen Plasmaproben wurden die Konzentrationen von Cortisol, Insulin, T3 und T4 mittels Radioimmunoassay bestimmt, sowie die ACTH-Konzentrationen mittels Chemilumineszenz-Enzymimmunometrischem Assay. Darüber hinaus wurden die hämatologischen und blutchemischen Parameter gemessen. Die Funktion des negativen Feetback-Mechanismus der Hypothalamus-Hypophysen-Nebennierenrinden-Achse wurde mittels eines ACTH-Stimulationstests überprüft. Während der Behandlung konnte eine ausgeprägte Suppression der Nebennierenrindenfunktion, gekennzeichnet durch die signifkante Abnahme der basalen Cortisolkonzentration, auf weniger als 10 % der Ausgangswerte vor der Behandlung gemessen werden. Auch der ACTH-Stimulationstest am 8. Behandlungstag zeigte einen signifikant geringeren Anstieg des Kortisolspiegels (< 50 %) als vor der Behandlung. Weiterhin kam es während der dermalen Verabreichung von Dexamethason zu einer progressiven, signifikanten Zunahme des Serumglucosespiegels bis um das 1,5 fache des Kontrollwertes. Parallel dazu stieg der Plasmainsulinspiegel um das 3-fache des Ausgangswertes vor Behandlungsbeginn. Die Plasmakonzentration von T3 zeigte einen leichten behandlungsbedingten Abfall, wohingegen der Plasma-T4-Spiegel einen deutlichen Rückgang auf 50 % des Ausgangswertes zeigte. Die endokrinologischen Veränderungen waren nach Absetzen der Behandlung alle reversibel. Weiterhin kam es zu einer signifikanten Reduktion der eosinophilen Granulozyten und der Lymphozyten, während die Zahl der Neutrophilen zunahm. Plasmakonzentrationen von Dexamethason konnten mit einem Maximalwert am 8. Tag der Behandlung (1542,10 ± 567 pg/ml) gemessen werden. Diese Ergebnisse belegen, dass bei der dermalen Applikation von Dexamethason eine perkutane Wirkstoffresorption in einem Umfang stattfindet, dass die typischen systemischen Glucocorticoidwirkungen auftreten. Es kann somit auch davon ausgegangen werden, dass die topische Verabreichung schwach wirksamer Glucocorticoidformulierungen eine gewisse Dopingrelevanz besitzt.

info:eu-repo/classification/ddc/636.089

ddc:636.089

The Cancer Recognition (CARE) Antibody Test

Thornthwaite, Jerry T., McDuffee, Emily C., Harris, Robert B., Secor McVoy, Julie R., Lane, I. W.

28 December 2004

The cancer recognition (CARE) antibody (Ab) test is a serologic assay for a specific IgM that is elevated in cancer patients. All tests are measured using an indirect enzyme-linked immunosorbent assay (ELISA) of human serum. The target polypeptide in the CARE Ab test is the IgM binding epitope (LT-11) of the CARE antigen (Ag) consisting of a 16 mer structure that has been produced synthetically. The mean relative concentration (MRC) is determined relative to standard, normalized human plasma. Non-parametric analysis showed median MRC values of healthy volunteers (HVs) with no history of cancer (n=47), family history of cancer (n=126) and a previous cancer history (n=24) to be 26, 34 and 46, respectively. It was determined that there was no significance found among the medians of the three HV groups (P=0.53). The specificity of the HV types was between 87 and 98%. Benign/non-cancer surgical patients (n=27) had a median value of 20 with a specificity of 96%. The cancer patients (n=61) had a median value of 246 with a sensitivity of 89%. There was a significant difference between the HV and cancer patients (P<0.0001) as well as between the benign/surgical non-cancerous group and cancer patients (P<0.0001). The IgM antibody is heat stable at room temperature for two days versus being frozen at -80°C (r2=0.97). Either serum or plasma samples may be used in the CARE Ab test (r2=0.92). The CARE Ab was almost exclusively IgM with no serum conversion to IgG in sequential measurements of patients with cancer over a six-month period. Preliminary data from patients undergoing post-operative cancer treatment showed that decreasing Ab levels revealed patients negative for residual cancer or undergoing remission, while relapsing patients show an increase in Ab levels. A return to a positive Ab level shortly after treatment is a poor prognostic sign while in advanced cancers the Ab levels may be depressed significantly.

Ab

antibody

Ag

antigen

BSA

bovine serum albumin

CARE Ab test

CARE

cancer recognition

CHOP

cytoxan

adriamycin

ELISA

ELISA

enzyme-linked immunosorbent assay

IgM

tumor marker

Endothelial Colony Forming Cells (ECFCs): Identification, Specification and Modulation in Cardiovascular Diseases

Huang, Lan

02 February 2010

Indiana University-Purdue University Indianapolis (IUPUI) / A hierarchy of endothelial colony forming cells (ECFCs) with different levels of proliferative potential has been identified in human circulating blood and blood vessels. High proliferative potential ECFCs (HPP-ECFCs) display properties (robust proliferative potential in vitro and vessel-forming ability in vivo) consistent with stem/progenitor cells for the endothelial lineage. Corneal endothelial cells (CECs) are different from circulating and resident vascular endothelial cells (ECs). Whereas systemic vascular endothelium slowly proliferates throughout life, CECs fail to proliferate in situ and merely expand in size to accommodate areas of CEC loss due to injury or senescence. However, we have identified an entire hierarchy of ECFC resident in bovine CECs. Thus, this study provides a new conceptual framework for defining corneal endothelial progenitor cell potential. The identification of persistent corneal HPP-ECFCs in adult subjects might contribute to regenerative medicine in corneal transplantation. While human cord blood derived ECFCs are able to form vessels in vivo, it is unknown whether they are committed to an arterial or venous fate. We have demonstrated that human cord blood derived ECFCs heterogeneously express gene transcripts normally restricted to arterial or venous endothelium. They can be induced to display an arterial gene expression pattern after vascular endothelial growth factor 165 (VEGF165) or Notch ligand Dll1 (Delta1ext-IgG) stimulation in vitro. However, the in vitro Dll1 primed ECFCs fail to display significant skewing toward arterial EC phenotype and function in vivo upon implantation, suggesting that in vitro priming is not sufficient for in vivo specification. Future studies will determine whether ECFCs are amenable to specification in vivo by altering the properties of the implantation microenvironment. There is emerging evidence suggesting that the concentration of circulating ECFCs is closely related to the adverse progression of cardiovascular disorders. In a pig model of acute myocardial ischemia (AMI), we have demonstrated that AMI rapidly mobilizes ECFCs into the circulation, with a significant shift toward HPP-ECFCs. The exact role of the mobilized HPP-ECFCs in homing and participation in repair of the ischemic tissue remains unknown. In summary, these studies contribute to an improved understanding of ECFCs and suggest several possible therapeutic applications of ECFCs.

Serum reduced medium

Angiogenesis

Arteriovenous differentiation

Acute myocardial infarction

Endothelial colony forming cells

Endothelium

Vascularization

Corneal endothelium

Endothelial progenitor cells

Endothelium

Cell differentiation

Stem cells

Neovascularization

Cardiovascular system -- Diseases

Synthesis, Biological Functionalization, and Integration ofCarbon Nanotubes for Bio-Sensing Textiles

Olszewski, Amy L.

03 June 2013

No description available.

Biochemistry

Biology

Chemical Engineering

Chemistry

Engineering

Materials Science

Nanoscience

Nanotechnology

Textile Research

Technology

Carbon nanotubes

CNT

human serum albumin

HSA

blood detection

covalent functionalization

carbodiimide

phage display

smart textiles

sensors

biological functionalization

peptide

Mechanistic approaches towards understanding particle formation in biopharmaceutical formations. The role of sufactant type and level on protein conformational stability, as assessed by calorimetry, and on protein size stability as assessed by dynamic light scattering, micro flow imaging and HIAC

Vaidilaite-Pretorius, Agita

January 2013

Control and analysis of protein aggregation is an increasing challenge to biopharmaceutical research and development. Therefore it is important to understand the interactions, causes and analysis of particles in order to control protein aggregation to enable successful biopharmaceutical formulations. This work investigates the role of different non-ionic surfactants on protein conformational stability, as assessed by HSDSC, and on protein size stability as assessed by Dynamic Light Scattering (DLS), HIAC and MFI. BSA and IgG2 were used as model proteins. Thermal unfolding experiments indicated a very weak surfactant-immunoglobulin IgG2 interaction, compared to much stronger interactions for the BSA surfactant systems. The DLS results showed that BSA and IgG2 with different surfactants and concentration produced different levels of particle size growth. The heat treatment and aging of samples in the presence of Tween 20, Tween 80, Brij 35 and Pluronic F-68 surfactants led to an increase in the populations of larger particles for BSA samples, whereas IgG2 systems did not notably aggregate under storage conditions MFI was shown to be more sensitive than HIAC technique for measuring sub-visible particles in protein surfactant systems. Heat treatment and storage stress showed a significant effect on BSA and IgG2 protein sub-visible particle size stability. This work has demonstrated that both proteins with different Tween 20, Tween 80, Brij 35 and Pluronic F-68 concentrations, have different level of conformational and size stability. Also aging samples and heating stress bears the potential to generate particles, but this depends on surfactant type. Poor predictive correlations between the analytical methods were determined.

Analysis of HCV Coinfections among Newly Diagnosed HIV Cases in Germany

Alemayehu, Amare Eshetu

05 March 2021

In Anbetracht der enormen Verbesserung der HCV-Therapie durch die Entwicklung hochwirksamer und direkt wirkender Virostatika (DAA) dient diese Studie der Analyse von HCV-Koinfektionen unter den gemeldeten HIV-Neudiagnosen in Deutschland. Zunächst wurde die Eignung zweier kommerzieller HCV Ag/Ab ELISAs, dem Murex (Abbott) und dem Monolisa (Bio-Rad), zum Nachweis von HCV in getrockneten Serumspots (DSS) verglichen. Der Murex-ELISA zeigte sich sensitiver bei Antigen-positiven Plasma-HCV-Serokonversionsproben während der Monolisa eine höhere Sensitivität bei HCV-Antikörper-positiven DSS-Eluaten. Des Weiteren wurde ein Aviditätstest zur Unterscheidung von neuen und bereits länger bestehenden Infektionen bei einem Aviditätsindex Cut-off von 40% und einem Zeitraum von 364 Tagen etabliert. Von den insgesamt 6.097 untersuchten Proben der Jahre 2015-2017 waren 396 HCV-ELISA-reaktiv (6,5%). Von diesen wurden 256 (64,6%) als aktive und 140 (35,4%) als ausgeheilte Infektionen identifiziert. Ein hoher Anteil der HCV-Koinfektionen wurde bei intra-venösen Drogenkonsumenten (77,8%, n=168/216), in der Altersgruppe der 30-39 Jährigen (9%, n=179/1.978) und bei Menschen osteuropäischer Herkunft (38,3%, n=124/324) beobachtet. Im Vergleich zum Jahr 2016 hat sich der Anteil der ausgeheilten Infektionen im Jahr 2017 bei der Gesamtzahl der Patienten (p<0,01) sowie insbesondere bei Personen ausländischer (p<0,01) und osteuropäischer (p<0,05) Herkunft erhöht. Die HCV Subtypen (St)-1a, St-3a und St-1b waren mit 33,9% (n=79/233), 33,5% (n=78/233) und 23,3% (n=52/233) vorherrschend. Der Anteil der St-1a- und St-1b-Proben, deren HCV-Sequenz gegen DAAs resistent ist, war in allen untersuchten Jahren hoch (25%-42,9%). Der beobachtete Anstieg des Anteils der ausgeheilten HCV-Koinfektionen kann auf die DAA-Therapie zurückgeführt werden. Es sind jedoch weitere Anstrengungen erforderlich, damit Gruppen mit weiterhin hoher HCV-Prävalenz von dieser Behandlung profitieren. / In light of the major shift in HCV therapy resulting from the availability of highly potent direct acting antivirals (DAA), this study performed a surveillance of HCV coinfections among reported HIV new diagnoses in Germany. First the suitability of two HCV Ag/Ab ELISAs, Murex (Abbott) and Monolisa (Bio-Rad) for dried serum spots (DSS) was compared. The Murex was more sensitive in antigen positive plasma HCV seroconversion samples while the Monolisa showed a higher sensitivity in HCV antibody positive DSS eluates. Furthermore, an avidity test was established to distinguish between new and already longer existing infections at an avidity index cut-off of 40% and a period of 364 days. Of the total of 6,097 samples examined for the years 2015-2017, 396 were HCV ELISA reactive (6.5%). Of these, 256 (64.6%) were identified as active and 140 (35.4%) as resolved infections. A high proportion of HCV coinfections were observed in intravenous drug users (77.8%, n=168/216), in the age group 30-39 years (9%, n=179/1,978) and in people of Eastern European origin (38.3%, n=124/324). Compared to 2016, the proportion of resolved infections in 2017 has increased in the total number of patients (p<0.01) and especially in people of foreign (p<0.01) and Eastern European (p<0.05) origin. HCV subtypes (St)-1a, St-3a, and St-1b were predominant with 33.9% (n=79/233), 33.5% (n=78/233) and 23.3% (n=52/233), respectively. The proportion of St-1a and St-1b samples whose HCV sequence has resistance to DAAs was high in all diagnoses years (25%-42.9%). The observed increase in the proportion of resolved HCV coinfections can be attributed to DAA therapy. However, further efforts are needed to ensure that groups with continued high HCV prevalence benefit from this treatment.

HCV-Subtyp

Murex

Aviditätstest

getrocknete Serumflecken

resistenzassoziierte Substitutionen

HCV subtype

Murex

Monolisa

Avidity assay

Dried serum spots

Resistance associated substitutions

570 Biologie

XD 7304

XD 7311

XD 7314

XD 7315

YC 5604

YC 5611

YC 5614

YC 5615

ddc:570

NOVEL THYROID HORMONE TARGET GENES IN THE LIVER, AND THEIR ROLES IN THYROID HORMONE SIGNALING AND PHYSIOLOGY

TALASILA, PHANI KUMAR

26 September 2012

No description available.

Biomedical Research

"Thyroid hormone

T3

liver

energy metabolism

lipid metabolism

SGK1

ANGPTL4

PI3 kinase

GSK650394

transcription

angiopoietins

oligomerization

cleavage

LPL

LDL

VLDL

HDL

serum triglycerides

PGC1a

co-activators

LPL assay

DGGR"

Signaling Cascade Involved in Rapid Stimulation of Cystic Fibrosis Transmembrane Conductance Regulator (CFTR) by Dexamethasone

Bossmann, Miriam, Ackermann, Benjamin W., Thome, Ulrich H., Laube, Mandy

15 January 2024

Impairment of mucociliary clearance with reduced airway fluid secretion leads to chronically inflamed airways. Cystic fibrosis transmembrane conductance regulator (CFTR) is crucially involved in airway fluid secretion and dexamethasone (dexa) has previously been shown to elevate CFTR activity in airway epithelial cells. However, the pathway by which dexa increases CFTR activity is largely unknown. We aimed to determine whether the increase of CFTR activity by dexa is achieved by non-genomic signaling and hypothesized that the phosphoinositide 3-kinase (PI3K) pathway is involved in CFTR stimulation. Primary rat airway epithelial cells and human bronchial submucosal gland-derived Calu-3 cells were analyzed in Ussing chambers and kinase activation was determined byWestern blots. Results demonstrated a critical involvement of PI3K and protein kinase B (AKT) signaling in the dexa-induced increase of CFTR activity, while serum and glucocorticoid dependent kinase 1 (SGK1) activity was not essential. We further demonstrated a reduced neural precursor cell expressed, developmentally downregulated 4-like (NEDD4L) ubiquitin E3 ligase activity induced by dexa, possibly responsible for the elevated CFTR activity. Finally, increases of CFTR activity by dexa were demonstrated within 30 min accompanied by rapid activation of AKT. In conclusion, dexa induces a rapid stimulation of CFTR activity which depends on PI3K/AKT signaling in airway epithelial cells. Glucocorticoids might thus represent, in addition to their immunomodulatory actions, a therapeutic strategy to rapidly increase airway fluid secretion.

info:eu-repo/classification/ddc/610

ddc:610