Your search keyword '"Basler N"' showing total 17 results

1. Cellular localisation of NADPH oxidases in rat renal resistance arteries: P126

Author

Basler, N., Schlüter, T., Schlüter, R., Rettig, R., and Grisk, O.

Published

2014

2. Das Mistelpräparat Iscucin Crataegi : Option für die Installationstherapie bei Harnblasenkarzinom

Author

Simoes-Wüst, P., Hunziker-Basler, N., Zuzak, T., Pally, Jenny, Simoes-Wüst, P., Hunziker-Basler, N., Zuzak, T., and Pally, Jenny

Abstract

Wässrige Mistelextrakte wie die Iscucin®-Präparate der WALA werden im Rahmen einer komplementärmedizinischen Krebsbehandlung häufig eingesetzt. Es stehen Iscucine® von acht verschiedenen Wirtsbäumen zur Verfügung. In vitro durchgeführte Zytotoxizitätstests zeigten, dass die Iscucin®-Präparate konzentrationsabhängige, wachstumshemmende Effekte auf verschiedene Tumorzelllinien ausübten. Bei der Blasenkrebszelllinie VM-CUB1 war die Hemmung durch Iscucin® Crataegi am stärksten ausgeprägt. In weiteren Versuchen wurden fünf Blasenkrebszelllinien mit verschiedenen Iscucin-Präparaten unter Bedingungen behandelt, die der therapeutischen Instillationstherapie beim oberflächlichen Blasenkrebs ähneln. Die Blasenkarzinomzelllinien VM-CUB1, TCC-SUP, T-24, J82 und UM-UC-3 wurden mit Iscucin® Abietis, Crataegi, Populi, Quercus und Tiliae inkubiert, und mit dem MTT-Zytotoxizitäts-Test wurde der Einfluss der Behandlung auf das Zellwachstum gemessen. Eine nur zweistündige Inkubation der Blase Krebszellen führte mit einer Mistelextraktkonzentration von 8 mg/ml aus Iscucin® Crataegi beziehungsweise Iscucin® Tiliae bei allen Zelllinien zu einem starken und mindestens sechs Tage anhaltenden zytotoxischen Effekt.

Published

2019

3. Prolonged cytotoxic effect of aqueous extracts from dired Viscum album on bladder cancer cells

Author

Hunziker-Basler, N., Zuzak, T., Eggenschwiler, Jenny, Rist, L., Simoes-Wüst, A.P., Viviani, A., Hunziker-Basler, N., Zuzak, T., Eggenschwiler, Jenny, Rist, L., Simoes-Wüst, A.P., and Viviani, A.

Abstract

Aqueous extracts from whole dried mistletoe (Viscum album L., Iscucin®) are often used in anti-cancer treatment. We studied the effect of extracts obtained from mistletoe bushes that grew on different host trees on bladder cancer cells by means of MTT-colorimetric cell proliferation/survival assays. The extracts possessed concentration-dependent cytotoxic properties whose extent varied with the host tree, but did not always correlate with the corresponding mistletoe lectin content. A 2-hours treatment of bladder cancer cells triggered a later, strong cytotoxic effect. This prolonged effect suggests that instillation with Iscucin® has therapeutic potential for bladder cancer patients.

Published

2019

4. Prolonged cytotoxic effect of aqueous extracts from dired Viscum album on bladder cancer cells

Author

Hunziker-Basler, N., Zuzak, T., Eggenschwiler, Jenny, Rist, L., Simoes-Wüst, A.P., and Viviani, A.

Subjects

615: Pharmakologie und Therapeutik

Abstract

Aqueous extracts from whole dried mistletoe (Viscum album L., Iscucin®) are often used in anti-cancer treatment. We studied the effect of extracts obtained from mistletoe bushes that grew on different host trees on bladder cancer cells by means of MTT-colorimetric cell proliferation/survival assays. The extracts possessed concentration-dependent cytotoxic properties whose extent varied with the host tree, but did not always correlate with the corresponding mistletoe lectin content. A 2-hours treatment of bladder cancer cells triggered a later, strong cytotoxic effect. This prolonged effect suggests that instillation with Iscucin® has therapeutic potential for bladder cancer patients.

Published

2007

5. 44. Long-lasting cytotoxic effects of a single application of aqueous extracts from dried Viscum album L. on bladder cancer cells in an in vitro system

Author

Simoes-Wust, A.P., Hunziker-Basler, N., Zuzak, T.J., Eggenschwiler, J., Rist, L., and Viviani, A.

Subjects

Materia medica, Vegetable -- Health aspects -- Chemical properties -- Methods, Bladder cancer -- Care and treatment, Cancer -- Care and treatment, Mistletoe -- Health aspects -- Chemical properties -- Methods, Plant extracts -- Health aspects -- Chemical properties -- Methods, Biological sciences, Health, Science and technology

Abstract

Viscum album (mistletoe) extracts are often used as a cancer therapy in the complementary medicine, with the patients reporting an improvement in quality of life upon treatment. Besides possessing immunomodulatory [...]

Published

2007

6. Wnt8 is required in lateral mesendodermal precursors for neural posteriorization in vivo.

Author

Erter, C E, Wilm, T P, Basler, N, Wright, C V, and Solnica-Krezel, L

Abstract

The dorsal ectoderm of the vertebrate gastrula was proposed by Nieuwkoop to be specified towards an anterior neural fate by an activation signal, with its subsequent regionalization along the anteroposterior (AP) axis regulated by a graded transforming activity, leading to a properly patterned forebrain, midbrain, hindbrain and spinal cord. The activation phase involves inhibition of BMP signals by dorsal antagonists, but the later caudalization process is much more poorly characterized. Explant and overexpression studies in chick, Xenopus, mouse and zebrafish implicate lateral/paraxial mesoderm in supplying the transforming influence, which is largely speculated to be a Wnt family member. We have analyzed the requirement for the specific ventrolaterally expressed Wnt8 ligand in the posteriorization of neural tissue in zebrafish wild-type and Nodal-deficient embryos (Antivin overexpressing or cyclops;squint double mutants), which show extensive AP brain patterning in the absence of dorsal mesoderm. In different genetic situations that vary the extent of mesodermal precursor formation, the presence of lateral wnt8-expressing cells correlates with the establishment of AP brain pattern. Cell tracing experiments show that the neuroectoderm of Nodal-deficient embryos undergoes a rapid anterior-to-posterior transformation in vivo during a short period at the end of the gastrula stage. Moreover, in both wild-type and Nodal-deficient embryos, inactivation of Wnt8 function by morpholino (MO(wnt8)) translational interference dose-dependently abrogates formation of spinal cord and posterior brain fates, without blocking ventrolateral mesoderm formation. MO(wnt8) also suppresses the forebrain deficiency in bozozok mutants, in which inactivation of a homeobox gene causes ectopic wnt8 expression. In addition, the bozozok forebrain reduction is suppressed in bozozok;squint;cyclops triple mutants, and is associated with reduced wnt8 expression, as seen in cyclops;squint mutants. Hence, whereas boz and Nodal signaling largely cooperate in gastrula organizer formation, they have opposing roles in regulating wnt8 expression and forebrain specification. Our findings provide strong support for a model of neural transformation in which a planar gastrula-stage Wnt8 signal, promoted by Nodal signaling and dorsally limited by Bozozok, acts on anterior neuroectoderm from the lateral mesoderm to produce the AP regional patterning of the CNS.

Published

2001

7. Known and novel viruses in Belgian honey bees: yearly differences, spatial clustering, and associations with overwintering loss.

Author

Deboutte W, De Smet L, Brunain M, Basler N, De Rycke R, Smets L, de Graaf DC, and Matthijnssens J

Subjects

Animals, Bees virology, Bees parasitology, Belgium, Viral Load, Phylogeny, RNA Viruses genetics, RNA Viruses isolation & purification, RNA Viruses classification, Viruses genetics, Viruses isolation & purification, Viruses classification, Seasons, Insect Viruses genetics, Insect Viruses isolation & purification, Insect Viruses physiology

Abstract

In recent years, managed honey bee colonies have been suffering from an increasing number of biotic and abiotic stressors, resulting in numerous losses of colonies worldwide. A pan-European study, EPILOBEE, estimated the colony loss in Belgium to be 32.4% in 2012 and 14.8% in 2013. In the current study, absolute viral loads of four known honey bee viruses (DWV-A, DWV-B, AmFV, and BMLV) and three novel putative honey bee viruses (Apis orthomyxovirus 1, apthili virus, and apparli virus) were determined in 300 Flemish honey bee samples, and associations with winter survival were determined. This revealed that, in addition to the known influence of DWV-A and DWV-B on colony health, one of the newly described viruses (apthili virus) shows a strong yearly difference and is also associated with winter survival. Furthermore, all scrutinized viruses revealed significant spatial clustering patterns, implying that despite the limited surface area of Flanders, local virus transmission is paramount. The vast majority of samples were positive for at least one of the seven investigated viruses, and up to 20% of samples were positive for at least one of the three novel viruses. One of those three, Apis orthomyxovirus 1, was shown to be a genuine honey bee-infecting virus, able to infect all developmental stages of the honey bee, as well as the Varroa destructor mite. These results shed light on the most prevalent viruses in Belgium and their roles in the winter survival of honey bee colonies., Importance: The western honey bee ( Apis mellifera ) is a highly effective pollinator of flowering plants, including many crops, which gives honey bees an outstanding importance both ecologically and economically. Alarmingly high annual loss rates of managed honey bee colonies are a growing concern for beekeepers and scientists and have prompted a significant research effort toward bee health. Several detrimental factors have been identified, such as varroa mite infestation and disease from various bacterial and viral agents, but annual differences are often not elucidated. In this study, we utilize the viral metagenomic survey of the EPILOBEE project, a European research program for bee health, to elaborate on the most abundant bee viruses of Flanders. We complement the existing metagenomic data with absolute viral loads and their spatial and temporal distributions. Furthermore, we identify Apis orthomyxovirus 1 as a potentially emerging pathogen, as we find evidence for its active replication honey bees., Competing Interests: The authors declare no conflict of interest.

Published

2024

8. Successful application of ancient DNA extraction and library construction protocols to museum wet collection specimens.

Author

Straube N, Lyra ML, Paijmans JLA, Preick M, Basler N, Penner J, Rödel MO, Westbury MV, Haddad CFB, Barlow A, and Hofreiter M

Subjects

DNA, Mitochondrial genetics, Sequence Analysis, DNA, Specimen Handling, DNA, Ancient, Museums

Abstract

Millions of scientific specimens are housed in museum collections, a large part of which are fluid preserved. The use of formaldehyde as fixative and subsequent storage in ethanol is especially common in ichthyology and herpetology. This type of preservation damages DNA and reduces the chance of successful retrieval of genetic data. We applied ancient DNA extraction and single stranded library construction protocols to a variety of vertebrate samples obtained from wet collections and of different ages. Our results show that almost all samples tested yielded endogenous DNA. Archival DNA extraction was successful across different tissue types as well as using small amounts of tissue. Conversion of archival DNA fragments into single-stranded libraries resulted in usable data even for samples with initially undetectable DNA amounts. Subsequent target capture approaches for mitochondrial DNA using homemade baits on a subset of 30 samples resulted in almost complete mitochondrial genome sequences in several instances. Thus, application of ancient DNA methodology makes wet collection specimens, including type material as well as rare, old or extinct species, accessible for genetic and genomic analyses. Our results, accompanied by detailed step-by-step protocols, are a large step forward to open the DNA archive of museum wet collections for scientific studies., (© 2021 The Authors. Molecular Ecology Resources published by John Wiley & Sons Ltd.)

Published

2021

9. Neoadjuvant rituximab modulates the tumor immune environment in patients with high risk prostate cancer.

Author

Ryan ST, Zhang J, Burner DN, Liss M, Pittman E, Muldong M, Shabaik A, Woo J, Basler N, Cunha J, Shalapour S, Estrada MV, Karin M, Messer K, Howell S, Kane CJ, and Jamieson CAM

Subjects

Animals, B7-H1 Antigen, Humans, Lymphocytes, Tumor-Infiltrating, Male, Mice, Prostatectomy, Rituximab therapeutic use, T-Lymphocytes, Tumor Microenvironment, Neoadjuvant Therapy, Prostatic Neoplasms drug therapy, Prostatic Neoplasms surgery

Abstract

Background: Immunotherapeutic regulation of the tumor microenvironment in prostate cancer patients is not understood. Most antibody immunotherapies have not succeeded in prostate cancer. We showed previously that high-risk PCa patients have a higher density of tumor infiltrating B-cells in prostatectomy specimens. In mouse models, anti-CD20 antibody ablation of B-cells delayed PCa regrowth post-treatment. We sought to determine whether neoadjuvant anti-CD20 immunotherapy with rituximab could reduce CD20+ B cell infiltration of prostate tumors in patients., Methods: An open label, single arm clinical trial enrolled eight high-risk PCa patients to receive one cycle of neoadjuvant rituximab prior to prostatectomy. Eleven clinical specimens with similar characteristics were selected as controls. Treated and control samples were concurrently stained for CD20 and digitally scanned in a blinded fashion. A new method of digital image quantification of lymphocytes was applied to prostatectomy sections of treated and control cases. CD20 density was quantified by a deconvolution algorithm in pathologist-marked tumor and adjacent regions. Statistical significance was assessed by one sided Welch's t-test, at 0.05 level using a gatekeeper strategy. Secondary outcomes included CD3+ T-cell and PD-L1 densities., Results: Mean CD20 density in the tumor regions of the treated group was significantly lower than the control group (p = 0.02). Mean CD3 density in the tumors was significantly decreased in the treated group (p = 0.01). CD20, CD3 and PD-L1 staining primarily occurred in tertiary lymphoid structures (TLS). Neoadjuvant rituximab was well-tolerated and decreased B-cell and T-cell density within high-risk PCa tumors compared to controls., Conclusions: This is the first study to treat patients prior to surgical prostate removal with an immunotherapy that targets B-cells. Rituximab treatment reduced tumor infiltrating B and T-cell density especially in TLSs, thus, demonstrating inter-dependence between B- and T-cells in prostate cancer and that Rituximab can modify the immune environment in prostate tumors. Future studies will determine who may benefit from using rituximab to improve their immune response against prostate cancer. Trial registration NCT01804712, March 5th, 2013 https://clinicaltrials.gov/ct2/show/NCT01804712?cond=NCT01804712&draw=2&rank=1.

Published

2020

10. Paleogenome Reveals Genetic Contribution of Extinct Giant Panda to Extant Populations.

Author

Sheng GL, Basler N, Ji XP, Paijmans JLA, Alberti F, Preick M, Hartmann S, Westbury MV, Yuan JX, Jablonski NG, Xenikoudakis G, Hou XD, Xiao B, Liu JH, Hofreiter M, Lai XL, and Barlow A

Subjects

Animals, China, Endangered Species, Male, DNA, Ancient analysis, Genetic Variation, Genome, Ursidae genetics

Abstract

Historically, the giant panda was widely distributed from northern China to southwestern Asia [1]. As a result of range contraction and fragmentation, extant individuals are currently restricted to fragmented mountain ranges on the eastern margin of the Qinghai-Tibet plateau, where they are distributed among three major population clusters [2]. However, little is known about the genetic consequences of this dramatic range contraction. For example, were regions where giant pandas previously existed occupied by ancestors of present-day populations, or were these regions occupied by genetically distinct populations that are now extinct? If so, is there any contribution of these extinct populations to the genomes of giant pandas living today? To investigate these questions, we sequenced the nuclear genome of an ∼5,000-year-old giant panda from Jiangdongshan, Tengchong County in Yunnan Province, China. We find that this individual represents a genetically distinct population that diverged prior to the diversification of modern giant panda populations. We find evidence of differential admixture with this ancient population among modern individuals originating from different populations as well as within the same population. We also find evidence for directional gene flow, which transferred alleles from the ancient population into the modern giant panda lineages. A variable proportion of the genomes of extant individuals is therefore likely derived from the ancient population represented by our sequenced individual. Although extant giant panda populations retain reasonable genetic diversity, our results suggest that this represents only part of the genetic diversity this species harbored prior to its recent range contractions., (Copyright © 2019 Elsevier Ltd. All rights reserved.)

Published

2019

11. Molecular identification of late and terminal Pleistocene Equus ovodovi from northeastern China.

Author

Yuan JX, Hou XD, Barlow A, Preick M, Taron UH, Alberti F, Basler N, Deng T, Lai XL, Hofreiter M, and Sheng GL

Subjects

Animals, Biological Evolution, DNA, Ancient, Equidae classification, Equidae genetics, Genome, Mitochondrial, Haplotypes, Phylogeny

Abstract

The extant diversity of horses (family Equidae) represents a small fraction of that occurring over their evolutionary history. One such lost lineage is the subgenus Sussemionus, which is thought to have become extinct during the Middle Pleistocene. However, recent molecular studies and morphological analysis have revealed that one of their representatives, E. ovodovi, did exist in Siberia during the Late Pleistocene. Fossil materials of E. ovodovi have thus far only been found in Russia. In this study, we extracted DNA from three equid fossil specimens excavated from northeastern China dated at 12,770-12,596, 29,525-28,887 and 40,201-38,848 cal. yBP, respectively, and retrieved three near-complete mitochondrial genomes from the specimens. Phylogenetic analyses cluster the Chinese haplotypes together with previously published Russian E. ovodovi, strongly supporting the assignment of these samples to this taxon. The molecular identification of E. ovodovi in northeastern China extends the known geographical range of this fossil species by several thousand kilometers to the east. The estimated coalescence time of all E. ovodovi haplotypes is approximately 199 Kya, with the Chinese haplotypes coalescing approximately 130 Kya. With a radiocarbon age of 12,770-12,596 cal. yBP, the youngest sample in this study represents the first E. ovodovi sample dating to the terminal Pleistocene, moving the extinction date of this species forwards considerably compared to previously documented fossils. Overall, comparison of our three mitochondrial genomes with the two published ones suggests a genetic diversity similar to several extant species of the genus Equus., Competing Interests: The authors have declared that no competing interests exist.

Published

2019

12. Optimized DNA sampling of ancient bones using Computed Tomography scans.

Author

Alberti F, Gonzalez J, Paijmans JLA, Basler N, Preick M, Henneberger K, Trinks A, Rabeder G, Conard NJ, Münzel SC, Joger U, Fritsch G, Hildebrandt T, Hofreiter M, and Barlow A

Subjects

Humans, Bone and Bones chemistry, DNA, Ancient analysis, DNA, Ancient isolation & purification, Fossils, Tomography, X-Ray Computed methods

Abstract

The prevalence of contaminant microbial DNA in ancient bone samples represents the principal limiting factor for palaeogenomic studies, as it may comprise more than 99% of DNA molecules obtained. Efforts to exclude or reduce this contaminant fraction have been numerous but also variable in their success. Here, we present a simple but highly effective method to increase the relative proportion of endogenous molecules obtained from ancient bones. Using computed tomography (CT) scanning, we identify the densest region of a bone as optimal for sampling. This approach accurately identifies the densest internal regions of petrous bones, which are known to be a source of high-purity ancient DNA. For ancient long bones, CT scans reveal a high-density outermost layer, which has been routinely removed and discarded prior to DNA extraction. For almost all long bones investigated, we find that targeted sampling of this outermost layer provides an increase in endogenous DNA content over that obtained from softer, trabecular bone. This targeted sampling can produce as much as 50-fold increase in the proportion of endogenous DNA, providing a directly proportional reduction in sequencing costs for shotgun sequencing experiments. The observed increases in endogenous DNA proportion are not associated with any reduction in absolute endogenous molecule recovery. Although sampling the outermost layer can result in higher levels of human contamination, some bones were found to have more contamination associated with the internal bone structures. Our method is highly consistent, reproducible and applicable across a wide range of bone types, ages and species. We predict that this discovery will greatly extend the potential to study ancient populations and species in the genomics era., (© 2018 John Wiley & Sons Ltd.)

Published

2018

13. Ancient DNA from Giant Panda (Ailuropoda melanoleuca) of South-Western China Reveals Genetic Diversity Loss during the Holocene.

Author

Sheng GL, Barlow A, Cooper A, Hou XD, Ji XP, Jablonski NG, Zhong BJ, Liu H, Flynn LJ, Yuan JX, Wang LR, Basler N, Westbury MV, Hofreiter M, and Lai XL

Abstract

The giant panda was widely distributed in China and south-eastern Asia during the middle to late Pleistocene, prior to its habitat becoming rapidly reduced in the Holocene. While conservation reserves have been established and population numbers of the giant panda have recently increased, the interpretation of its genetic diversity remains controversial. Previous analyses, surprisingly, have indicated relatively high levels of genetic diversity raising issues concerning the efficiency and usefulness of reintroducing individuals from captive populations. However, due to a lack of DNA data from fossil specimens, it is unknown whether genetic diversity was even higher prior to the most recent population decline. We amplified complete cyt b and 12s rRNA, partial 16s rRNA and ND1 , and control region sequences from the mitochondrial genomes of two Holocene panda specimens. We estimated genetic diversity and population demography by analyzing the ancient mitochondrial DNA sequences alongside those from modern giant pandas, as well as from other members of the bear family (Ursidae). Phylogenetic analyses show that one of the ancient haplotypes is sister to all sampled modern pandas and the second ancient individual is nested among the modern haplotypes, suggesting that genetic diversity may indeed have been higher earlier during the Holocene. Bayesian skyline plot analysis supports this view and indicates a slight decline in female effective population size starting around 6000 years B.P., followed by a recovery around 2000 years ago. Therefore, while the genetic diversity of the giant panda has been affected by recent habitat contraction, it still harbors substantial genetic diversity. Moreover, while its still low population numbers require continued conservation efforts, there seem to be no immediate threats from the perspective of genetic evolutionary potential., Competing Interests: The authors declare no conflict of interest.

Published

2018

14. Reduction of the contaminant fraction of DNA obtained from an ancient giant panda bone.

Author

Basler N, Xenikoudakis G, Westbury MV, Song L, Sheng G, and Barlow A

Subjects

Animals, Base Composition, DNA Damage, Reproducibility of Results, Sequence Analysis, DNA methods, Bone and Bones metabolism, DNA, Ancient analysis, DNA, Ancient isolation & purification, Ursidae genetics

Abstract

Objective: A key challenge in ancient DNA research is massive microbial DNA contamination from the deposition site which accumulates post mortem in the study organism's remains. Two simple and cost-effective methods to enrich the relative endogenous fraction of DNA in ancient samples involve treatment of sample powder with either bleach or Proteinase K pre-digestion prior to DNA extraction. Both approaches have yielded promising but varying results in other studies. Here, we contribute data on the performance of these methods using a comprehensive and systematic series of experiments applied to a single ancient bone fragment from a giant panda (Ailuropoda melanoleuca)., Results: Bleach and pre-digestion treatments increased the endogenous DNA content up to ninefold. However, the absolute amount of DNA retrieved was dramatically reduced by all treatments. We also observed reduced DNA damage patterns in pre-treated libraries compared to untreated ones, resulting in longer mean fragment lengths and reduced thymine over-representation at fragment ends. Guanine-cytosine (GC) contents of both mapped and total reads are consistent between treatments and conform to general expectations, indicating no obvious biasing effect of the applied methods. Our results therefore confirm the value of bleach and pre-digestion as tools in palaeogenomic studies, providing sufficient material is available.

Published

2017

15. Prolonged cytotoxic effect of aqueous extracts from dried viscum album on bladder cancer cells.

Author

Hunziker-Basler N, Zuzak TJ, Eggenschwiler J, Rist L, Simões-Wüst AP, and Viviani A

Subjects

Cell Line, Tumor, Cell Proliferation drug effects, Cell Survival drug effects, Humans, Plant Extracts pharmacology, Tetrazolium Salts, Thiazoles, Urinary Bladder Neoplasms pathology, Antineoplastic Agents, Phytogenic pharmacology, Urinary Bladder Neoplasms drug therapy, Viscum chemistry

Abstract

Aqueous extracts from whole dried mistletoe (Viscum album L., Iscucin) are often used in anti-cancer treatment. We studied the effect of extracts obtained from mistletoe bushes that grew on different host trees on bladder cancer cells by means of MTT-colorimetric cell proliferation/survival assays. The extracts possessed concentration-dependent cytotoxic properties whose extent varied with the host tree, but did not always correlate with the corresponding mistletoe lectin content. A 2-hours treatment of bladder cancer cells triggered a later, strong cytotoxic effect. This prolonged effect suggests that instillation with Iscucin has therapeutic potential for bladder cancer patients.

Published

2007

16. Effects of subtotal fasting on plasmatic coagulation, fibrinolytic status and platelet activation: a controlled pilot study in healthy subjects.

Author

Huber R, Nauck M, Basler N, Haas B, Mattern M, Lüdtke R, and Peter K

Subjects

Adult, Cardiovascular Diseases blood, Female, Flow Cytometry, Hemostasis, Humans, Male, Pilot Projects, Prothrombin Time, Risk Factors, Blood Coagulation physiology, Cardiovascular Diseases etiology, Fasting physiology, Fibrinolysis physiology, Platelet Activation physiology

Abstract

Background and Aim: There is considerable controversy as to whether fasting can be recommended to patients with cardiovascular disease. The objective of this study was to determine whether a well-known method of 1-week subtotal fasting affects hemostasis in healthy subjects., Methods and Results: Analyses were carried out before, four times during and 3 days after fasting in 12 fasting subjects (< 300 kcal/day, only from carbohydrates) (group 1), and 8 control subjects (group 2). Plasmatic coagulation (prothrombin time, partial thromboplastin time, p < or = 0.001) and fibrinolysis (plasminogen, plasmin-antiplasmin-complex, p < 0.05) increased during fasting but remained within the normal limits. While the platelet count was similar in both groups, platelet sensitivity to stimulators was reduced in group 1 (P-selectin and activated GP IIb/IIIa on ADP-stimulated platelets, p < or = 0.01). Furthermore, soluble P-selectin (p < or = 0.01) and C-reactive protein were decreased in comparison to group 2 (p < or = 0.05)., Conclusions: Hemostasis and inflammation parameters during 1-week subtotal fasting do not imply an increase in cardiovascular risk.

Published

2005

17. Adhesion of monocytes to medical steel as used for vascular stents is mediated by the integrin receptor Mac-1 (CD11b/CD18; alphaM beta2) and can be inhibited by semiconductor coating.

Author

Schuler P, Assefa D, Ylänne J, Basler N, Olschewski M, Ahrens I, Nordt T, Bode C, and Peter K

Subjects

Adhesiveness, Analysis of Variance, Animals, Biocompatible Materials chemistry, CD11b Antigen metabolism, CD18 Antigens biosynthesis, CHO Cells, Carbon Compounds, Inorganic chemistry, Cell Adhesion, Cell Line, Cricetinae, Electrochemistry, Flow Cytometry, Humans, Monocytes metabolism, Peptides chemistry, Semiconductors, Silicon Compounds chemistry, CD11b Antigen physiology, Monocytes cytology, Stainless Steel chemistry, Stents

Abstract

Implantation of stents into stenosed arteries helps to restore normal blood flow in ischemic organs. However, limited biocompatibility of the applied medical steel can cause acute thrombosis and long-term restenosis. Adhesion of monocytes to stent metal may participate in those acute and long-term complications of stent placement. Based on described prominent electrochemical properties of the interaction between the monocyte integrin receptor Mac-1 and its various ligands, we hypothesized, that this receptor is a central mediator of monocyte adhesion to stent metal and that semiconductor coating of medical steel reduces monocyte adhesion. Adhesion of monocytes on L-316 stainless steel was directly evaluated by light microscopy. Mac-1 could be identified as mediator of monocyte adhesion, since cell adhesion could be blocked by anti-Mac-1-antibodies, including the cross-reacting anti-GPIIb/IIIa antibody fragment abciximab. To further prove the central role of Mac-1, two CHO cell lines were generated expressing recombinant Mac-1 either as wild type, resulting in a low affinity receptor, or mutant with a GFFKR deletion of the alpha(M) subunit, resulting in a high affinity receptor. Indeed, adhesion was specific for Mac-1 and dependent on the affinity state of this integrin. Finally, we could demonstrate that Mac-1-mediated adhesion of monocytes to stents can be significantly inhibited by silicon carbide coating of the stent metal. In conclusion, the integrin Mac-1 and its affinity state could be identified as major mediators of monocyte adhesion on medical steel. As therapeutic strategies, the blockade of Mac-1 by antibodies or silicon carbide coating of steel inhibits monocyte adhesion on stents.

Published

2003