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4. Poly(ethylene glycol) Cross-Linked Antibody Nanoparticles for Tunable Biointeractions

Author

Hu, Y, Cortez-Jugo, C, Ju, Y, Zheng, T, Zhou, J, Lin, Z, De Rose, R, Hagemeyer, CE, Alt, K, Caruso, F, Hu, Y, Cortez-Jugo, C, Ju, Y, Zheng, T, Zhou, J, Lin, Z, De Rose, R, Hagemeyer, CE, Alt, K, and Caruso, F

Abstract

Liver accumulation of nanoparticles is a major challenge in nanoparticle-mediated delivery as it can reduce the delivery of the nanoparticles to their intended site and lead to liver damage and toxicity. Recent studies have shown that particle engineering, e.g., nanoparticle composition, can influence liver uptake and allow homing of nanoparticles to specific organs or tissues. Herein, we investigated the role of nanoparticle cross-linking on liver uptake. We developed a series of antibody nanoparticles (AbNPs) using various poly(ethylene glycol) (PEG) molecule (e.g., different arm numbers and arm lengths) cross-linkers. Specifically, AbNPs based on Herceptin were engineered with PEG cross-linker architectures ranging from 2-arm (at molecular weights of 600 Da, 2.5 kDa, and 5 kDa) to 4-arm and 8-arm via a mesoporous silica templating method. The molecular architecture of PEG modulated not only the targeting ability of the AbNPs in model cell lines but also their interaction with phagocytes in human blood. Increasing the PEG arm length from 600 Da to 5 kDa also reduced the uptake of the nanoparticles in the liver by 85%. Tumor accumulation of Herceptin AbNPs cross-linked with a 5 kDa 2-arm-PEG was 50% higher compared with control AbNPs and displayed similar liver uptake as free Herceptin. This study highlights the role of PEG cross-linking in receptor targeting and liver uptake, which influence tumor targeting, and combined with the versatility and multifunctionality of the antibody nanoparticle platform could lead to the development of organ-selective targeted antibody nanoparticle assemblies.

Published
2023

5. An Engineered Nanosugar Enables Rapid and Sustained Glucose-Responsive Insulin Delivery in Diabetic Mice

Author

Xu, R, Bhangu, SK, Sourris, KC, Vanni, D, Sani, M-A, Karas, JA, Alt, K, Niego, B, Ale, A, Besford, QA, Dyett, B, Patrick, J, Carmichael, I, Shaw, JE, Caruso, F, Cooper, ME, Hagemeyer, CE, Cavalieri, F, Xu, R, Bhangu, SK, Sourris, KC, Vanni, D, Sani, M-A, Karas, JA, Alt, K, Niego, B, Ale, A, Besford, QA, Dyett, B, Patrick, J, Carmichael, I, Shaw, JE, Caruso, F, Cooper, ME, Hagemeyer, CE, and Cavalieri, F

Abstract

Glucose-responsive insulin-delivery platforms that are sensitive to dynamic glucose concentration fluctuations and provide both rapid and prolonged insulin release have great potential to control hyperglycemia and avoid hypoglycemia diabetes. Here, biodegradable and charge-switchable phytoglycogen nanoparticles capable of glucose-stimulated insulin release are engineered. The nanoparticles are "nanosugars" bearing glucose-sensitive phenylboronic acid groups and amine moieties that allow effective complexation with insulin (≈95% loading capacity) to form nanocomplexes. A single subcutaneous injection of nanocomplexes shows a rapid and efficient response to a glucose challenge in two distinct diabetic mouse models, resulting in optimal blood glucose levels (below 200 mg dL-1 ) for up to 13 h. The morphology of the nanocomplexes is found to be key to controlling rapid and extended glucose-regulated insulin delivery in vivo. These studies reveal that the injected nanocomplexes enabled efficient insulin release in the mouse, with optimal bioavailability, pharmacokinetics, and safety profiles. These results highlight a promising strategy for the development of a glucose-responsive insulin delivery system based on a natural and biodegradable nanosugar.

Published
2023

6. Missing Lactase Persistence in Late Iron Age Central Europe

Author

Warnberg, O., Knipper, C., Röder, B., Lassau, G., Spichtig, N., Ramsl, P., Novotny, F., Teschler-Nicola, M., Marion, S., Schönfelder, M., Pare, C., Szécsényi-Nagy, A., Schibler, J., Schiffels, S., https://orcid.org/0000-0002-1017-9150, Alt, K., and Pichler, S.

Abstract

Missing Lactase Persistence in Late Iron Age Central Europe Being able to digest milk sugar beyond the age of weaning is a rather new trait in humans. The calculated age of the responsible mutations largely coincides with the introduction of dairy farming. Recent European populations exhibit a gradient of high levels of lactose tolerance in the north and lower numbers in the south. Lactase persistence is believed to have co-evolved with farming or livestock keeping as a selective advantage. Palaeogenetic data of prehistoric individuals, however, have so far not provided any clear evidence that the spread of the lactase persistence mutation predates the Roman period, while persistence increases throughout the Middle Ages. In contrast, evidence of dairy processing reaches back to the introduction of farming in the Neolithic. In this paper, we investigate lactase persistence in the La Tène period of the European Iron Age. 39 individuals from Austria, France, Hungary and Switzerland have been successfully genotyped for the two single nucleotide polymorphisms (SNPs) 13910C/T and 22018G/A, which are associated with lactose tolerance. None of those individuals carries the homozygous variant of either of the two SNPs, while four individuals are heterozygous at 22018G/A. This implies that during the Iron Age processed dairy products like cheese and yoghurt still represented the common supply of milk-derived nutrients while fresh milk played only a minor role in the regions studied here. The population-wide spread of the lactose tolerance trait in Europe therefore clearly post-dates the Iron Age., Archäologisches Korrespondenzblatt, Bd. 52 Nr. 2 (2022): Archäologisches Korrespondenzblatt

Published
2023
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8. Socio-cultural practices affect sexual dimorphism in stature in Early Neolithic Europe

Author

Cox, S., Nicklisch, N., Francken, M., Wahl, J., Meller, H., Haak, W., https://orcid.org/0000-0003-2475-2007, Alt, K., Rosenstock, E., and Mathieson, I.

Abstract

The rules and structure of human culture impact health and disease as much as genetics or the natural environment. Studying the origins and evolution of these patterns in the archaeological record is challenging as it is difficult to tease apart the effects of genetics, culture, and environment. We take a multidisciplinary approach by combining published ancient DNA, skeletal metrics, paleopathology, and dietary stable isotopes to analyze cultural, environmental, and genetic contributions to variation in stature in four geographically defined populations of Early Neolithic Europe: North Central, South Central, Southern (Mediterranean), and Southeastern (Balkan) Europeans. In individuals from Central Europe, female stature is low, despite polygenic scores for height identical to males and to neighboring regions. Dietary and skeletal stress markers indicate environmental stress that is equal in both sexes, but the high stature sexual dimorphism ratio suggests that these stresses were exacerbated in females by cultural factors, likely associated with male preference and sex-biased allocation of resources. In contrast, shorter average stature in Mediterranean Neolithic populations have been previously reported to be associated with genetic differences; however, this is likely an artifact of residual population structure in the genome-wide association studies (GWAS). Instead, we suggest that reduced sexual dimorphism in the region indicates a degree of male vulnerability in response to general environmental stress. We conclude that while population-level stature trends may in some cases reflect genetic factors, differences in sexual dimorphism are largely driven by culture, or the interaction of culture and environment. Our analysis indicates that biological effects of sex-specific inequities can be linked to cultural influences at least as early as 7000 years before present. Understanding these patterns is key to interpreting the evolution of genetic and sociocultural determinants of health and our results show that culture, more than environment or genetics, drove height disparities in Early Neolithic Europe.Competing Interest StatementThe authors have declared no competing interest. 1 Introduction 2 Materials and Methods 2.1 Genetic data 2.2 Osteology and stable isotope data 2.3 Statistical models 3 Results 3.1 Distribution of stature, polygenic scores and stable isotope values 3.2 Patterns of non-genetic factors in Central Europe 3.3 Patterns of genetic ancestry in the Mediterranean 4 Discussion 4.1 Sexual dimporphism in Central Europe reflects the effects of culture 4.2 Mediterranean differences may have both genetic and environmental bases 4.3 Conclusion

Published
2023

10. Template-Assisted Antibody Assembly: A Versatile Approach for Engineering Functional Antibody Nanoparticles

Author

Hu, Y, Li, J, Ju, Y, Houston, ZH, Fletcher, NL, De Rose, R, Fernandes, S, Hagemeyer, CE, Alt, K, Thurecht, KJ, Cortez-Jugo, C, Caruso, F, Hu, Y, Li, J, Ju, Y, Houston, ZH, Fletcher, NL, De Rose, R, Fernandes, S, Hagemeyer, CE, Alt, K, Thurecht, KJ, Cortez-Jugo, C, and Caruso, F

Abstract

The clinical success of monoclonal antibody therapy has inspired research in understanding the fundamental molecular basis of antibody-antigen interactions and the engineering of antibodies and antibody assemblies with enhanced or novel properties. In particular, colloidally stable antibody assemblies can enhance dosing strategies and enable combined therapy of a mixture of antibodies or biologics. Herein, nanoassemblies of therapeutic antibodies were fabricated with controlled physicochemical properties using a versatile template-mediated assembly method. The antibody nanoparticles (AbNPs) cross-linked with poly(ethylene glycol)-N-hydroxysuccinimide were monodispersed, with particle diameters consistent with the template size (250 nm). When assembled using Herceptin or Kadcyla as a model antibody and antibody-drug conjugate, respectively, the nanoparticles retained the selectivity of the monoclonal antibody and recognized >98% of cells expressing the target receptors on cell membranes. Unlike the free Herceptin antibody, which was predominantly localized at the surface, the AbNPs were internalized via receptor-mediated endocytosis, presenting opportunities for delivering monoclonal antibodies intracellularly at high concentrations and/or against intracellular targets. With the vast array of antibodies that could be applied and different cross-linking chemistries possible, the reported antibody assembly strategy provides a versatile platform for the development of antibody assemblies for therapeutic, diagnostic, and clinical applications.

Published
2022

11. PIGN encephalopathy: Characterizing the epileptology

Author

Bayat, A, Valles-Ibanez, G, Pendziwiat, M, Knaus, A, Alt, K, Biamino, E, Bley, A, Calvert, S, Carney, P, Caro-Llopis, A, Ceulemans, B, Cousin, J, Davis, S, Portes, V, Edery, P, England, E, Ferreira, C, Freeman, J, Gener, B, Gorce, M, Heron, D, Hildebrand, MS, Jezela-Stanek, A, Jouk, P-S, Keren, B, Kloth, K, Kluger, G, Kuhn, M, Lemke, JR, Li, H, Martinez, F, Maxton, C, Mefford, HC, Merla, G, Mierzewska, H, Muir, A, Monfort, S, Nicolai, J, Norman, J, O'Grady, G, Oleksy, B, Orellana, C, Orec, LE, Peinhardt, C, Pronicka, E, Rosello, M, Santos-Simarro, F, Schwaibold, EMC, Stegmann, APA, Stumpel, CT, Szczepanik, E, Terczynska, I, Thevenon, J, Tzschach, A, Van Bogaert, P, Vittorini, R, Walsh, S, Weckhuysen, S, Weissman, B, Wolfe, L, Reymond, A, De Nittis, P, Poduri, A, Olson, H, Striano, P, Lesca, G, Scheffer, IE, Moller, RS, Sadleir, LG, Bayat, A, Valles-Ibanez, G, Pendziwiat, M, Knaus, A, Alt, K, Biamino, E, Bley, A, Calvert, S, Carney, P, Caro-Llopis, A, Ceulemans, B, Cousin, J, Davis, S, Portes, V, Edery, P, England, E, Ferreira, C, Freeman, J, Gener, B, Gorce, M, Heron, D, Hildebrand, MS, Jezela-Stanek, A, Jouk, P-S, Keren, B, Kloth, K, Kluger, G, Kuhn, M, Lemke, JR, Li, H, Martinez, F, Maxton, C, Mefford, HC, Merla, G, Mierzewska, H, Muir, A, Monfort, S, Nicolai, J, Norman, J, O'Grady, G, Oleksy, B, Orellana, C, Orec, LE, Peinhardt, C, Pronicka, E, Rosello, M, Santos-Simarro, F, Schwaibold, EMC, Stegmann, APA, Stumpel, CT, Szczepanik, E, Terczynska, I, Thevenon, J, Tzschach, A, Van Bogaert, P, Vittorini, R, Walsh, S, Weckhuysen, S, Weissman, B, Wolfe, L, Reymond, A, De Nittis, P, Poduri, A, Olson, H, Striano, P, Lesca, G, Scheffer, IE, Moller, RS, and Sadleir, LG

Abstract

OBJECTIVE: Epilepsy is common in patients with PIGN diseases due to biallelic variants; however, limited epilepsy phenotyping data have been reported. We describe the epileptology of PIGN encephalopathy. METHODS: We recruited patients with epilepsy due to biallelic PIGN variants and obtained clinical data regarding age at seizure onset/offset and semiology, development, medical history, examination, electroencephalogram, neuroimaging, and treatment. Seizure and epilepsy types were classified. RESULTS: Twenty six patients (13 female) from 26 families were identified, with mean age 7 years (range = 1 month to 21 years; three deceased). Abnormal development at seizure onset was present in 25 of 26. Developmental outcome was most frequently profound (14/26) or severe (11/26). Patients presented with focal motor (12/26), unknown onset motor (5/26), focal impaired awareness (1/26), absence (2/26), myoclonic (2/26), myoclonic-atonic (1/26), and generalized tonic-clonic (2/26) seizures. Twenty of 26 were classified as developmental and epileptic encephalopathy (DEE): 55% (11/20) focal DEE, 30% (6/20) generalized DEE, and 15% (3/20) combined DEE. Six had intellectual disability and epilepsy (ID+E): two generalized and four focal epilepsy. Mean age at seizure onset was 13 months (birth to 10 years), with a lower mean onset in DEE (7 months) compared with ID+E (33 months). Patients with DEE had drug-resistant epilepsy, compared to 4/6 ID+E patients, who were seizure-free. Hyperkinetic movement disorder occurred in 13 of 26 patients. Twenty-seven of 34 variants were novel. Variants were truncating (n = 7), intronic and predicted to affect splicing (n = 7), and missense or inframe indels (n = 20, of which 11 were predicted to affect splicing). Seven variants were recurrent, including p.Leu311Trp in 10 unrelated patients, nine with generalized seizures, accounting for nine of the 11 patients in this cohort with generalized seizures. SIGNIFICANCE: PIGN encephalopathy is a complex

Published
2022

12. Im Blickpunkt

Author

Spitzing, T., Nicklisch, N., Steuer, H., and Alt, K. W.

Published
2008

17. A clinical trial of non-invasive imaging with an anti-HIV antibody labelled with copper-64 in people living with HIV and uninfected controls.

Author

Chang J., McMahon J.H., Zerbato J.M., Lau J.S.Y., Wichmann C.W., Scott F.E., Guo N., Lee S.-T., Liu Z., Caskey M., Nussenzweig M.C., Donnelly P.S., Egan G., Hagemeyer C.E., Scott A.M., Lewin S.R., Lange J.L., Roche M., Tumpach C., Dantanarayana A., Rhodes A., Rasmussen T.A., Mackenzie C.A., Alt K., Hagenauer M., Roney J., O'Bryan J., Carey A., McIntyre R., Beech P., O'Keefe G.J., Chang J., McMahon J.H., Zerbato J.M., Lau J.S.Y., Wichmann C.W., Scott F.E., Guo N., Lee S.-T., Liu Z., Caskey M., Nussenzweig M.C., Donnelly P.S., Egan G., Hagemeyer C.E., Scott A.M., Lewin S.R., Lange J.L., Roche M., Tumpach C., Dantanarayana A., Rhodes A., Rasmussen T.A., Mackenzie C.A., Alt K., Hagenauer M., Roney J., O'Bryan J., Carey A., McIntyre R., Beech P., and O'Keefe G.J.

Abstract

Background: A research priority in finding a cure for HIV is to establish methods to accurately locate and quantify where and how HIV persists in people living with HIV (PLWH) receiving suppressive antiretroviral therapy (ART). Infusing copper-64 (64Cu) radiolabelled broadly neutralising antibodies targeting HIV envelope (Env) with CT scan and positron emission tomography (PET) identified HIV Env in tissues in SIV infected non-human primates. We aimed to determine if a similar approach was effective in people living with HIV (PLWH). Method(s): Unmodified 3BNC117 was compared with 3BNC117 bound to the chelator MeCOSar and 64Cu (64Cu-3BNC117) in vitro to assess binding and neutralization. In a clinical trial 64Cu-3BNC117 was infused into HIV uninfected (Group 1), HIV infected and viremic (viral load, VL >1000 c/mL; Group 2) and HIV infected aviremic (VL <20 c/mL; Group 3) participants using two dosing strategies: high protein (3mg/kg unlabeled 3BNC117 combined with <5mg 64Cu-3BNC117) and trace (<5mg 64Cu-3BNC117 only). All participants were screened for 3BNC117 sensitivity from virus obtained from viral outgrowth. Magnetic resonance imaging (MRI)/PET and pharmacokinetic assessments (ELISA for serum 3BNC117 concentrations and gamma counting for 64Cu) were performed 1, 24- and 48-hours post dosing. The trial (clincialtrials.gov NCT03063788) primary endpoint was comparison of PET standard uptake values (SUVs) in regions of interest (e.g lymph node groups and gastrointestinal tract). Finding(s): Comparison of unmodified and modified 3BNC117 in vitro demonstrated no difference in HIV binding or neutralisation. 17 individuals were enrolled of which 12 were dosed including Group 1 (n=4, 2 high protein, 2 trace dose), Group 2 (n=6, 2 high protein, 4 trace) and Group 3 (n=2, trace only). HIV+ participants had a mean CD4 of 574 cells/microL and mean age 43 years. There were no drug related adverse effects and no differences in tissue uptake in regions of interest (e.g lymph nod

Published
2021

18. A clinical trial of non-invasive imaging with an anti-HIV antibody labelled with copper-64 in people living with HIV and uninfected controls

Author

McMahon, JH, Zerbato, JM, Lau, JSY, Lange, JL, Roche, M, Tumpach, C, Dantanarayana, A, Rhodes, A, Chang, J, Rasmussen, TA, Mackenzie, CA, Alt, K, Hagenauer, M, Roney, J, O'Bryan, J, Carey, A, McIntyre, R, Beech, P, O'Keefe, GJ, Wichmann, CW, Scott, FE, Guo, N, Lee, S-T, Liu, Z, Caskey, M, Nussenzweig, MC, Donnelly, PS, Egan, G, Hagemeyer, CE, Scott, AM, Lewin, SR, McMahon, JH, Zerbato, JM, Lau, JSY, Lange, JL, Roche, M, Tumpach, C, Dantanarayana, A, Rhodes, A, Chang, J, Rasmussen, TA, Mackenzie, CA, Alt, K, Hagenauer, M, Roney, J, O'Bryan, J, Carey, A, McIntyre, R, Beech, P, O'Keefe, GJ, Wichmann, CW, Scott, FE, Guo, N, Lee, S-T, Liu, Z, Caskey, M, Nussenzweig, MC, Donnelly, PS, Egan, G, Hagemeyer, CE, Scott, AM, and Lewin, SR

Abstract

BACKGROUND: A research priority in finding a cure for HIV is to establish methods to accurately locate and quantify where and how HIV persists in people living with HIV (PLWH) receiving suppressive antiretroviral therapy (ART). Infusing copper-64 (64Cu) radiolabelled broadly neutralising antibodies targeting HIV envelope (Env) with CT scan and positron emission tomography (PET) identified HIV Env in tissues in SIV infected non-human primates . We aimed to determine if a similar approach was effective in people living with HIV (PLWH). METHODS: Unmodified 3BNC117 was compared with 3BNC117 bound to the chelator MeCOSar and 64Cu (64Cu-3BNC117) in vitro to assess binding and neutralization. In a clinical trial 64Cu-3BNC117 was infused into HIV uninfected (Group 1), HIV infected and viremic (viral load, VL >1000 c/mL; Group 2) and HIV infected aviremic (VL <20 c/mL; Group 3) participants using two dosing strategies: high protein (3mg/kg unlabeled 3BNC117 combined with <5mg 64Cu-3BNC117) and trace (<5mg 64Cu-3BNC117 only). All participants were screened for 3BNC117 sensitivity from virus obtained from viral outgrowth. Magnetic resonance imaging (MRI)/PET and pharmacokinetic assessments (ELISA for serum 3BNC117 concentrations and gamma counting for 64Cu) were performed 1, 24- and 48-hours post dosing. The trial (clincialtrials.gov NCT03063788) primary endpoint was comparison of PET standard uptake values (SUVs) in regions of interest (e.g lymph node groups and gastrointestinal tract). FINDINGS: Comparison of unmodified and modified 3BNC117 in vitro demonstrated no difference in HIV binding or neutralisation. 17 individuals were enrolled of which 12 were dosed including Group 1 (n=4, 2 high protein, 2 trace dose), Group 2 (n=6, 2 high protein, 4 trace) and Group 3 (n=2, trace only). HIV+ participants had a mean CD4 of 574 cells/microL and mean age 43 years. There were no drug related adverse effects and no differences in tissue uptake in regions of interest (e.g lymph node g

Published
2021

19. Stealth nanorods via the aqueous living crystallisation-driven self-assembly of poly(2-oxazoline)s

Author

Finnegan, JR, Pilkington, EH, Alt, K, Rahim, MA, Kent, SJ, Davis, TP, Kempe, K, Finnegan, JR, Pilkington, EH, Alt, K, Rahim, MA, Kent, SJ, Davis, TP, and Kempe, K

Abstract

The morphology of nanomaterials critically influences their biological interactions. However, there is currently a lack of robust methods for preparing non-spherical particles from biocompatible materials. Here, we combine 'living' crystallisation-driven self-assembly (CDSA), a seeded growth method that enables the preparation of rod-like polymer nanoparticles, with poly(2-oxazoline)s (POx), a polymer class that exhibits 'stealth' behaviour and excellent biocompatibility. For the first time, the 'living' CDSA process was carried out in pure water, resulting in POx nanorods with lengths ranging from ∼60 to 635 nm. In vitro and in vivo study revealed low immune cell association and encouraging blood circulation times, but little difference in the behaviour of POx nanorods of different length. The stealth behaviour observed highlights the promising potential of POx nanorods as a next generation stealth drug delivery platform.

Published
2021

20. The occurrence of intersex in different populations of the marine amphipod Echinogammarus marinus in north-west Brittany – A longterm-study

Author

Oetken, M., Adler, M., Alt, K., Bachmann, J., Dombrowski, A., Duhme, F., Gabriel, A.-L., Grünewald, J., Jourdan, J., Lück, Maren, Mensch, C., Rösch, D., Ruthemann, A., Terres, S., Völker, M.L., Wilhelm, F., Oehlmann, J., Oetken, M., Adler, M., Alt, K., Bachmann, J., Dombrowski, A., Duhme, F., Gabriel, A.-L., Grünewald, J., Jourdan, J., Lück, Maren, Mensch, C., Rösch, D., Ruthemann, A., Terres, S., Völker, M.L., Wilhelm, F., and Oehlmann, J.

Abstract

In the past two decades, an increasing body of studies has been published on the intersex phenomenon in separate-sexed crustaceans from marine and freshwater ecosystems. Various causes are being considered that could have an influence on the occurrence of intersex. Besides genetic factors, environmental conditions such as photoperiodicity, temperature, salinity and parasitism, but also environmental pollution with endocrine disrupting chemicals (EDCs) are discussed. As part of a long-term monitoring (2012 – 2020) in north-west Brittany, we recorded the occurrence of intersex in the marine amphipod Echinogammarus marinus. We quantified the intersex incidence at marine and estuarine sites and analyzed the incidence in relation to the endocrine potential of the sediments. Intersex occurred with mean frequencies between 0.87% and 12%. It was striking that the incidence of intersex increased with increasing distance from the sea. Since the highest incidence was observed at the range boundary of this stenohaline species, we assume that intersex is triggered by endocrine potential and increasing stress due to increasing freshwater content − and thus an interplay of different environmental factors.

Published
2021

25. An X-band GaN HEMT power amplifier design using an artificial neural network modeling technique

Author

Lee, Sang Yun, Cetiner, Bedri Artug, Torpi, Hamid, Cai, S.J., Li, Jiang, Alt, K., Chen, Y.L., Wen, Cheng P., Wang, Kang L., and Itoh, Tatsuo

Subjects
High-electron-mobility transistors -- Research, Neural networks -- Usage, Transistors -- Research, Business, Electronics, Electronics and electrical industries
Abstract

A novel gallium nitride-based high electron mobility transistor power amplifier design is presented that uses an artificial neural network modeling technique.

Published
2001

29. Effect of doping density on capacitance of resonant tunneling diodes

Author

Jo, J.., Alt, K., and Wang, K.L.

Subjects
Diodes -- Research, Semiconductor doping -- Research, Physics
Abstract

A study was conducted on the influence of doping density in the collector and emitter regions of resonant tunneling diodes on parallel resistance and capacitance. Results show that doping density affect capacitance values and that the dependence was caused by the electron density modulation near the barriers. Results may be used in designing resonant tunneling diodes with excellent high frequency performance.

Published
1997

30. Observation of new type resonances in triple barrier resonant tunneling diodes

Author

Jo, J., Alt, K., and Wang, K.L.

Subjects
Resonance -- Research, Superlattices as materials -- Research, Tunnel diodes -- Research, Physics
Abstract

New features about energy level alignment in a superlattice are revealed by current-voltage characteristics measured in triple resonant tunneling diodes. Obtained data indicate that energy levels in the two quantum wells are not aligned at current peaks. Current peaks are seen when one of the energy levels in the two wells becomes resonant with the emitter level. A current peak, which was thermally activated, revealed inverted bistability at 77 K temperature. X state assisted tunneling is discussed.

Published
1997

31. Ligand-Functionalized Poly(ethylene glycol) Particles for Tumor Targeting and Intracellular Uptake.

Author

Cui, J, Alt, K, Ju, Y, Gunawan, ST, Braunger, JA, Wang, T-Y, Dai, Y, Dai, Q, Richardson, JJ, Guo, J, Björnmalm, M, Hagemeyer, CE, Caruso, F, Cui, J, Alt, K, Ju, Y, Gunawan, ST, Braunger, JA, Wang, T-Y, Dai, Y, Dai, Q, Richardson, JJ, Guo, J, Björnmalm, M, Hagemeyer, CE, and Caruso, F

Abstract

Drug carriers typically require both stealth and targeting properties to minimize nonspecific interactions with healthy cells and increase specific interaction with diseased cells. Herein, the assembly of targeted poly(ethylene glycol) (PEG) particles functionalized with cyclic peptides containing Arg-Gly-Asp (RGD) (ligand) using a mesoporous silica templating method is reported. The influence of PEG molecular weight, ligand-to-PEG molecule ratio, and particle size on cancer cell targeting to balance stealth and targeting of the engineered PEG particles is investigated. RGD-functionalized PEG particles (PEG-RGD particles) efficiently target U-87 MG cancer cells under static and flow conditions in vitro, whereas PEG and cyclic peptides containing Arg-Asp-Gly (RDG)-functionalized PEG (PEG-RDG) particles display negligible interaction with the same cells. Increasing the ligand-to-PEG molecule ratio improves cell targeting. In addition, the targeted PEG-RGD particles improve cell uptake via receptor-mediated endocytosis, which is desirable for intracellular drug delivery. The PEG-RGD particles show improved tumor targeting (14% ID g-1) when compared with the PEG (3% ID g-1) and PEG-RDG (7% ID g-1) particles in vivo, although the PEG-RGD particles show comparatively higher spleen and liver accumulation. The targeted PEG particles represent a platform for developing particles aimed at balancing nonspecific and specific interactions in biological systems.

Published
2019

37. The genetic prehistory of the Greater Caucasus

Author

Wang, C., Reinhold, S., Kalmykov, A., Wissgott, A., Brandt, G., Jeong, C., Cheronet, O., Ferry, M., Harney, E., Keating, D., Mallick, S., Rohland, N., Stewardson, K., Kantorovich, A., Maslov, V., Petrenko, V., Erlikh, V., Atabiev, B., Magomedov, R., Kohl, P., Alt, K., Pichler, S., Gerling, C., Meller, H., Vardanyan, B., Yeganyan, L., Rezepkin, A., Mariaschk, D., Berezina, N., Gresky, J., Fuchs, K., Knipper, C., Schiffels, S., Balanovska, E., Balanovsky, O., Mathieson, I., Higham, T., Berezin, Y., Buzhilova, A., Trifonov, V., Pinhasi, R., Belinskiy, A., Reich, D., Hansen, S., Krause, J., and Haak, W.

Abstract

Archaeogenetic studies have described the formation of Eurasian ’}steppe ancestry{’ as a mixture of Eastern and Caucasus hunter-gatherers. However, it remains unclear when and where this ancestry arose and whether it was related to a horizon of cultural innovations in the 4th millennium BCE that subsequently facilitated the advance of pastoral societies likely linked to the dispersal of Indo-European languages. To address this, we generated genome-wide SNP data from 45 prehistoric individuals along a 3000-year temporal transect in the North Caucasus. We observe a genetic separation between the groups of the Caucasus and those of the adjacent steppe. The Caucasus groups are genetically similar to contemporaneous populations south of it, suggesting that - unlike today - the Caucasus acted as a bridge rather than an insurmountable barrier to human movement. The steppe groups from Yamnaya and subsequent pastoralist cultures show evidence for previously undetected Anatolian farmer-related ancestry from different contact zones, while Steppe Maykop individuals harbour additional Upper Palaeolithic Siberian and Native American related ancestry.

Published
2018

38. The genomic history of Southeastern Europe

Author

Mathieson, I., Roodenberg, S., Posth, C., Szécsényi-Nagy, A., Rohland, N., Mallick, S., Olalde, I., Broomandkhoshbacht, N., Cheronet, O., Fernandes, D., Ferry, M., Gamarra, B., Fortes, G., Haak, W., Harney, E., Krause-Kyora, B., Kucukkalipci, I., Michel, M., Mittnik, A., Nägele, K., Novak, M., Oppenheimer, J., Patterson, N., Pfrengle, S., Sirak, K., Stewardson, K., Vai, S., Alexandrov, S., Alt, K., Andreescu, R., Antonović, D., Ash, A., Atanassova, N., Bacvarov, K., Gusztáv, M., Bocherens, H., Bolus, M., Boroneanţ, A., Boyadzhiev, Y., Budnik, A., Burmaz, J., Chohadzhiev, S., Conard, N., Cottiaux, R., Čuka, M., Cupillard, C., Drucker, D., Elenski, N., Francken, M., Galabova, B., Ganetovski, G., Gely, B., Hajdu, T., Handzhyiska, V., Harvati, K., Higham, T., Iliev, S., Janković, I., Karavanić, I., Kennett, D., Komšo, D., Kozak, A., Labuda, D., Lari, M., Lazar, C., Leppek, M., Leshtakov, K., Vetro, D., Los, D., Lozanov, I., Malina, M., Martini, F., McSweeney, K., Meller, H., Menđušić, M., Mirea, P., Moiseyev, V., Petrova, V., Price, T., Simalcsik, A., Sineo, L., Šlaus, M., Slavchev, V., Stanev, P., Starović, A., Szeniczey, T., Talamo, S., Teschler-Nicola, M., Thevenet, C., Valchev, I., Valentin, F., Vasilyev, S., Veljanovska, F., Venelinova, S., Veselovskaya, E., Viola, B., Virag, C., Zaninović, J., Zäuner, S., Stockhammer, P., Catalano, G., Krauß, R., Caramelli, D., Zariņa, G., Gaydarska, B., Lillie, M., Nikitin, A., Potekhina, I., Papathanasiou, A., Borić, D., Bonsall, C., Krause, J., Pinhasi, R., and Reich, D.

Published
2017

39. The Beaker Phenomenon and the genomic transformation of Northwest Europe

Author

Olalde, I., Brace, S., Allentoft, M., Armit, I., Kristiansen, K., Rohland, N., Mallick, S., Booth, T., Szécsényi-Nagy, A., Mittnik, A., Altena, E., Lipson, M., Lazaridis, I., Patterson, N., Broomandkhoshbacht, N., Diekmann, Y., Faltyskova, Z., Fernandes, D., Ferry, M., Harney, E., de Knijff, P., Michel, M., Oppenheimer, J., Stewardson, K., Barclay, A., Alt, K., Fernández, A., Bánffy, E., Bernabò-Brea, M., Billoin, D., Blasco, C., Bonsall, C., Bonsall, L., Allen, T., Büster, L., Carver, S., Navarro, L., Craig, O., Cook, G., Cunliffe, B., Denaire, A., Dinwiddy, K., Dodwell, N., Ernée, M., Evans, C., Kuchařík, M., Farré, J., Fokkens, H., Fowler, C., Gazenbeek, M., Pena, R., Haber-Uriarte, M., Haduch, E., Hey, G., Jowett, N., Knowles, T., Massy, K., Pfrengle, S., Lefranc, P., Lemercier, O., Lefebvre, A., Maurandi, J., Majó, T., McKinley, J., McSweeney, K., Gusztáv, M., Modi, A., Kulcsár, G., Kiss, V., Czene, A., Patay, R., Endródi, A., Köhler, K., Hajdu, T., Cardoso, J., Liesau, C., Pearson, M., Włodarczak, P., Price, T., Prieto, P., Rey, P., Ríos, P., Risch, R., Guerra, M., Schmitt, A., Serralongue, J., Silva, A., Smrčka, V., Vergnaud, L., Zilhão, J., Caramelli, D., Higham, T., Heyd, V., Sheridan, A., Sjögren, K., Thomas, M., Stockhammer, P., Pinhasi, R., Krause, J., Haak, W., Barnes, I., Lalueza-Fox, C., and Reich, D.

Published
2017

40. The early days of Neolithic Alsónyék: the Starčevo occupation

Author

Oross, K., Bánffy, E., Osztás, A., Marton, T., Nyerges, É Á, Köhler, K., Szécsényi-Nagy, A., Alt, K. W., Ramsey, C. B., Tomasz Goslar, Kromer, B., and Hamilton, D.

Abstract

The excavations at Alsónyék revealed numerous Starčevo features, over 50 in the southern part of subsite 10B and some 500 in subsite 5603. The overwhelming majority of the features uncovered were individual pits and pit complexes. Traces of houses or above-ground structures were recorded, but no certain house plans could be identified; numerous hearths and ovens were found. 25 Starčevo burials have been identified, with some in disused pits and ovens. The occupation excavated in subsite 5603 was substantial, the largest yet discovered in Transdanubia. The north-west distribution of the Early Neolithic cultural complex of the northern Balkans – the Starčevo, Körös and Criş cultures – represents the first food-producing communities in many parts of the Carpathian basin. Starčevo sites are now known in the southern part of western Hungary up to Lake Balaton, but there are many unresolved questions about the precise chronology of the Early Neolithic in Transdanubia and beyond, in the Starčevo-Körös-Criş complex as a whole, and about the character and identity of the first farmers of the region. This paper presents 34 radiocarbon dates from 33 samples, interpreted within a Bayesian framework, for the dating of the Starčevo occupation at Alsónyék. 18 samples of human and animal bone were selected as part of the OTKA-funded project Alsónyék: from the beginnings of food production to the end of the Neolithic in collaboration with the ERC- funded The Times of Their Lives project, in conjunction with 15 existing dates from human burials. The programme aimed to date Starčevo occupation and burials at Alsónyék, and in so doing to contribute to further understanding of the character and pace of the spread of the Neolithic way of life in the region. The Bayesian model presented estimates that Starčevo activity probably began in 5775–5740 cal BC (68% probability), probably lasted for 190–245 years (68% probability), and probably ended in 5560–5525 cal BC (68% probability). The transition from pottery Style group 1 to 2 probably occurred in 5760–5730 cal BC (68% probability), with the transition from pottery Style group 2 to 3 probably in 5595–5570 cal BC (68% probability).The implications of these estimates for the character of the Starčevo occupation at Alsónyék are discussed, as well as for the wider development of the Starčevo culture and of the Early Neolithic in the region as a whole. The current picture suggests the densest Starčevo presence in south-east Transdanubia within the Hungarian distribution of the culture, with a gradual spread to the north later on. The results also demonstrate that Early Neolithic settlements in western Hungary lasted for a substantial period of time, across several human generations., Bericht der Römisch-Germanischen Kommission, Bd. 94. 2013 (2016): Bericht der Römisch-Germanischen Kommission

Published
2017
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41. Parallel ancient genomic transects reveal complex population history of early European farmers

Author

Lipson, M., Szécsényi-Nagy, A., Mallick, S., Pósa, A., Stégmár, B., Keerl, V., Rohland, N., Stewardson, K., Ferry, M., Michel, M., Oppenheimer, J., Broomandkhoshbacht, N., Harney, E., Nordenfelt, S., Llamas, B., Mende, B., Köhler, K., Oross, K., Bondár, M., Marton, T., Osztás, A., Jakucs, J., Paluch, T., Horváth, F., Csengeri, P., Koós, J., Sebok, K., Anders, A., Raczky, P., Regenye, J., Barna, J., Fábián, S., Serlegi, G., Toldi, Z., Nagy, E., Dani, J., Molnár, E., Pálfi, G., Márk, L., Melegh, B., Bánfai, Z., Fernández-Eraso, J., Mujika-Alustiza, J., Fernández, C., Echevarría, J., Bollongino, R., Orschiedt, J., Schierhold, K., Meller, H., Cooper, A., Burger, J., Bánffy, E., Alt, K., Lalueza-Fox, C., Haak, W., and Reich, D.

Published
2017

43. Shear-sensitive nanocapsule drug release for site-specific inhibition of occlusive thrombus formation

Author

Molloy, CP, Yao, Y, Kammoun, H, Bonnard, T, Hoefer, T, Alt, K, Tovar-Lopez, F, Rosengarten, G, Ramsland, PA, van der Meer, AD, van den Berg, A, Murphy, AJ, Hagemeyer, CE, Peter, K, Westein, E, Molloy, CP, Yao, Y, Kammoun, H, Bonnard, T, Hoefer, T, Alt, K, Tovar-Lopez, F, Rosengarten, G, Ramsland, PA, van der Meer, AD, van den Berg, A, Murphy, AJ, Hagemeyer, CE, Peter, K, and Westein, E

Abstract

UNLABELLED: Essentials Vessel stenosis due to large thrombus formation increases local shear 1-2 orders of magnitude. High shear at stenotic sites was exploited to trigger eptifibatide release from nanocapsules. Local delivery of eptifibatide prevented vessel occlusion without increased tail bleeding times. Local nanocapsule delivery of eptifibatide may be safer than systemic antiplatelet therapies. SUMMARY: Background Myocardial infarction and stroke remain the leading causes of mortality and morbidity. The major limitation of current antiplatelet therapy is that the effective concentrations are limited because of bleeding complications. Targeted delivery of antiplatelet drug to sites of thrombosis would overcome these limitations. Objectives Here, we have exploited a key biomechanical feature specific to thrombosis, i.e. significantly increased blood shear stress resulting from a reduction in the lumen of the vessel, to achieve site-directed delivery of the clinically used antiplatelet agent eptifibatide by using shear-sensitive phosphatidylcholine (PC)-based nanocapsules. Methods PC-based nanocapsules (2.8 × 1012 ) with high-dose encapsulated eptifibatide were introduced into microfluidic blood perfusion assays and into in vivo models of thrombosis and tail bleeding. Results Shear-triggered nanocapsule delivery of eptifibatide inhibited in vitro thrombus formation selectively under stenotic and high shear flow conditions above a shear rate of 1000 s-1 while leaving thrombus formation under physiologic shear rates unaffected. Thrombosis was effectively prevented in in vivo models of vessel wall damage. Importantly, mice infused with shear-sensitive antiplatelet nanocapsules did not show prolonged bleeding times. Conclusions Targeted delivery of eptifibatide by shear-sensitive nanocapsules offers site-specific antiplatelet potential, and may form a basis for developing more potent and safer antiplatelet drugs.

Published
2017

44. Self-Assembled Nanoparticles from Phenolic Derivatives for Cancer Therapy

Author

Dai, Y, Guo, J, Wang, T-Y, Ju, Y, Mitchell, AJ, Bonnard, T, Cui, J, Richardson, JJ, Hagemeyer, CE, Alt, K, Caruso, F, Dai, Y, Guo, J, Wang, T-Y, Ju, Y, Mitchell, AJ, Bonnard, T, Cui, J, Richardson, JJ, Hagemeyer, CE, Alt, K, and Caruso, F

Abstract

Therapeutic nanoparticles hold clinical promise for cancer treatment by avoiding limitations of conventional pharmaceuticals. Herein, a facile and rapid method is introduced to assemble poly(ethylene glycol) (PEG)-modified Pt prodrug nanocomplexes through metal-polyphenol complexation and combined with emulsification, which results in ≈100 nm diameter nanoparticles (PtP NPs) that exhibit high drug loading (0.15 fg Pt per nanoparticle) and low fouling properties. The PtP NPs are characterized for potential use as cancer therapeutics. Mass cytometry is used to quantify uptake of the nanoparticles and the drug concentration in individual cells in vitro. The PtP NPs have long circulation times, with an elimination half-life of ≈18 h in healthy mice. The in vivo antitumor activity of the PtP NPs is systematically investigated in a human prostate cancer xenograft mouse model. Mice treated with the PtP NPs demonstrate four times better inhibition of tumor growth than either free prodrug or cisplatin. This study presents a promising strategy to prepare therapeutic nanoparticles for biomedical applications.

Published
2017

45. Reducing metal contamination in Cu-64 production

Author

Poniger, S., Tochon-Danguy, H., Sachinidis, H, Alt, K., Hagemeyer, C., Scott, A., and Ludwig Institute of Cancer Research, Melbourne branch, Australia

Subjects
64Cu, reduzierte Metallkontamination, ddc:530, 64Cu, low metal content
Abstract

Introduction In the past several years there has been a growing interest in the development of radiopharmaceuticals labeled with metallic radionuclides (Anderson et al. 1999). Of particular interest is the positron emitter Cu-64 (t½ = 12.7 h) for molecular imaging of small molecules as well as peptides and antibodies (Smith 2004). This has led us to the recent implementation of a solid target production facility using commercially available target irradiation station and chemistry modules. Routine production of Cu-64 was achieved with an average production yield of 0.32 mCi/μAh, however purification of Cu-64 has proven to be problematic; with several metallic contaminants compromising subsequent radiolabeling. We report in this work, the step by step procedure which led us to the successful production of low metal contaminant 64Cu with high specific activity and high labeling efficiency. Material and Methods Detailed implementation of our solid target was reported earlier (Poniger et al. 2012). A Nirta Solid Target from IBA was coupled to our 18/9 cyclotron using a 2-meter external beam line. A pneumatic solid target transfer system (STTS) designed by TEMA was use to deliver the irradiated target disks to a dedicated hotcell. Modules from IBA (Pinctada metal) were used for electroplating 64Ni onto a Ag disk and for acid dissolution and purification of the irradiated target. Typical irradiation parameters were 14.9 MeV at 35 μA for 5–6 hours with 64Ni plating’s ranging from 10–60 μm thickness at 6–12 mm. Radionuclidic purities were evaluated by gamma spectroscopy and traces of metallic impurities were determined by ICP-MS or ICP-AES. Labeling efficiency was evaluated by measuring the amount of 64Cu uptake per 20 μg of scFv-cage. Results and Conclusion Initial 64Cu purifications following the manufacturers recommended method resulted in high levels of Cu, Fe and Zn metal contaminants (see TABLE 1, ID 1). Note that little Ag contamination is observed nevertheless the 64Ni is plated directly on a Ag disk. After several productions, visual inspection of the module quickly revealed that the heater block used for heating the back of the Ag target disk was heavily corroded. Replacing the copper heater block with a PEEK heater block drastically reduced the levels of Cu and Fe contaminants. Unfortunately unusually high levels of Zn were still observed regardless of the stringent conditions and ultrapure reagents used during the processing (see TABLE 1, ID 5). In our quest for answers, ICP-MS analysis of the 64Ni plating solution as well as critical stock reagents such as Milli-Q water (18 MΩ cm−1) and 30% HCl TraceSelect Ultra (Sigma) was performed (see TABLE 1, ID 2,3,4). The results were surprising, with high level of Zn found not only in the 64Ni plating solution, but as well in the HCl TraceSelect Ultra. It was hypothesized that the Pinctada’s glass bottles (Kay, 2004) used to store the reagents, especially concentrated acidic solutions were the source of Zn contamination and all glass bottles were replaced by LDPE or PFA types. Our hypothesis was confirmed by subsequent ICP-MS analysis of fresh samples of HCl TraceSelect Ultra and the 64Ni plating solution prepared/stored in plastic containers (see TABLE 1, ID 6,7). We also confirmed by ICP-MS analysis that no contamination occurred when performing a non-radioactive dissolution/purification sequence on the Pinctada module using a blank PTFE target disk in conjunction with the change to plastic reagent storage bottles (see TABLE 1, ID 8). Initially the purification protocol was modified as described by Ometakova et al., 2012 to help reduce the co-elution of Zn contaminants with the 64Cu from the AG1-X8 resin. This change resulted in a significant amount of 64Cu eluting from the resin during the resin washing steps, so that protocol was abandoned and the protocol as described by Thieme et al., 2012 was adopted. By modifying the AG1-X8 resin washing protocol to this new method and eluting the 64Cu from with 0.1M HCl rather than Milli-Q water (see TABLE 1, ID 9), we were able to further reduce metal contaminants, especially Zn. During the course of these experiments, the true specific activity of 64Cu increased from as low as 12 mCi/μmol of Cu (n = 2, TABLE 1, ID 1) to 649 mCi/μmol of Cu (n = 7, TABLE 1, ID 5) and finally to 4412 mCi/μmol of Cu (n = 3, TABLE 1, ID 9). In the same time, the effective specific activity increased from 0.03 ± 0.02 mCi per 20 μg of scFv-cage, to 3.7 ± 0.3 mCi per 20 g of scFv-cage with 64Cu. In conclusion, a significant reduction in Cu, Fe and Zn contaminants was achieved when processing 64Cu using the Pinctada module: i) after replacement of the Cu heater block; ii) after elimination of glass reagent storage containers from the Pinctada module and procedures during preparation of the 64Ni plating solution and iii) after implementation of a new purification protocol (Thieme et al. 2012). Introduction of a 6M HCl wash-up cycle of the module prior to the dissolution procedure was also effective. However in recent 64Cu productions slightly elevated Ag levels have been observed and are under investigation (see TABLE 1, ID 9).

Published
2015

46. Effect of doping intensity on capacitance of resonant tunneling diodes.

Author

Jo, J., Alt, K., and Wang, K. L.

Subjects
*QUANTUM tunneling, *DIODES, *ELECTRIC capacity
Abstract

Studies capacitance and parallel resistance in resonant tunneling diodes as a function of the doping density. Capacitance as obtained by analyzing resonance in the admittance; Existence of electron density modulation around barriers; Dependence of doping density resulting from modulation.

Published
1997
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48. Polymer Capsules for Plaque-Targeted In Vivo Delivery

Author

Richardson, JJ, Choy, MY, Guo, J, Liang, K, Alt, K, Ping, Y, Cui, J, Law, LS, Hagemeyer, CE, Caruso, F, Richardson, JJ, Choy, MY, Guo, J, Liang, K, Alt, K, Ping, Y, Cui, J, Law, LS, Hagemeyer, CE, and Caruso, F

Abstract

Targeted polymer capsules can selectively bind to unstable plaques in mice after intravenous injection. Different formulations of the capsules are explored with a synthetic/biopolymer hybrid capsule showing the best stability and small-molecule drug retention. The synthetic polymer is composed of pH-sensitive blocks (PDPA), low-binding blocks (PEG), and click-groups for postfunctionalization with targeting peptides specific to plaques.

Published
2016

50. 'Celtic migrations': Fact or fiction? Strontium and oxygen isotope analysis of the Czech cemeteries of Radovesice and Kutn_a Hora in Bohemia

Author

Scheeres, M., Knipper, C., Hauschild, M., Schönfelder, Martin, Siebel, W., Pare, C., Alt, K.-W., Archéologie, Terre, Histoire, Sociétés [Dijon] ( ARTeHiS ), Ministère de la Culture et de la Communication ( MCC ) -Université de Bourgogne ( UB ) -Centre National de la Recherche Scientifique ( CNRS ), Eberhard Karls Universität Tübingen, Archéologie, Terre, Histoire, Sociétés [Dijon] (ARTeHiS), Centre National de la Recherche Scientifique (CNRS)-Université de Bourgogne (UB)-Ministère de la Culture et de la Communication (MCC), Eberhard Karls Universität Tübingen = Eberhard Karls University of Tuebingen, and Ministère de la Culture et de la Communication (MCC)-Université de Bourgogne (UB)-Centre National de la Recherche Scientifique (CNRS)

Subjects
[SHS.ARCHEO]Humanities and Social Sciences/Archaeology and Prehistory, Archéologie, [ SHS.ARCHEO ] Humanities and Social Sciences/Archaeology and Prehistory, ComputingMilieux_MISCELLANEOUS
Abstract

International audience

Published
2014

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