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Publication DateInternational Immunopharmacology, ISSN 1567-5769, 09/2018, Volume 62, p. 287
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Scientific Reports, ISSN 2045-2322, 12/2018, Volume 8, Issue 1, pp. 1621 - 11
Trichostatin A (TSA) possess histone deacetylase (HDAC) inhibitory potential, can reverse the deactivation of tumor suppressor genes and inhibit tumor cell...
THERAPY | ACETYLATION | CYTOTOXICITY | MULTIDISCIPLINARY SCIENCES | BIOLOGY | Cell Survival - drug effects | Neoplastic Stem Cells - drug effects | Humans | Pancreatic Neoplasms - pathology | Histone Deacetylases - metabolism | Hydroxamic Acids - metabolism | Deoxycytidine - metabolism | Cell Line, Tumor | Histone Deacetylase Inhibitors - metabolism | Antimetabolites, Antineoplastic - metabolism | Deoxycytidine - analogs & derivatives | Neoplastic Stem Cells - physiology | Apoptosis | Vimentin | Cell proliferation | Histone deacetylase | Chromatin | Deactivation | Gemcitabine | Oct-4 protein | Exploration | mRNA | siRNA | E-cadherin | Cell growth | Lysine | Pancreatic cancer | Cell lines | Stem cells | Tumor suppressor genes | Trichostatin A | Methylation
THERAPY | ACETYLATION | CYTOTOXICITY | MULTIDISCIPLINARY SCIENCES | BIOLOGY | Cell Survival - drug effects | Neoplastic Stem Cells - drug effects | Humans | Pancreatic Neoplasms - pathology | Histone Deacetylases - metabolism | Hydroxamic Acids - metabolism | Deoxycytidine - metabolism | Cell Line, Tumor | Histone Deacetylase Inhibitors - metabolism | Antimetabolites, Antineoplastic - metabolism | Deoxycytidine - analogs & derivatives | Neoplastic Stem Cells - physiology | Apoptosis | Vimentin | Cell proliferation | Histone deacetylase | Chromatin | Deactivation | Gemcitabine | Oct-4 protein | Exploration | mRNA | siRNA | E-cadherin | Cell growth | Lysine | Pancreatic cancer | Cell lines | Stem cells | Tumor suppressor genes | Trichostatin A | Methylation
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Loading RightsInternational Immunopharmacology, ISSN 1567-5769, 09/2018, Volume 62, pp. 287 - 292
Sepsis is a major cause of mortality among critically ill patients in the intensive care unit (ICU). Alterations in serum amyloid A (SAA) and nitric oxide (NO)...
Serum amyloid A nitric oxide | CRP | Sepsis | Septic shock | APACHE II score | Mortality | MANAGEMENT | IMMUNOLOGY | DEFINITIONS | SIRS | PHARMACOLOGY & PHARMACY | INFECTION | DYSFUNCTION | EPIDEMIOLOGY | Nitric Oxide - blood | Predictive Value of Tests | Prospective Studies | Humans | Middle Aged | Critical Illness | Male | Biomarkers - blood | Shock, Septic - mortality | Sepsis - mortality | Sensitivity and Specificity | Shock, Septic - blood | Female | Sepsis - blood | APACHE | Serum Amyloid A Protein - analysis | Medical research | Care and treatment | Prognosis | C-reactive protein | Nitric oxide | Analysis | Medicine, Experimental | Biological markers
Serum amyloid A nitric oxide | CRP | Sepsis | Septic shock | APACHE II score | Mortality | MANAGEMENT | IMMUNOLOGY | DEFINITIONS | SIRS | PHARMACOLOGY & PHARMACY | INFECTION | DYSFUNCTION | EPIDEMIOLOGY | Nitric Oxide - blood | Predictive Value of Tests | Prospective Studies | Humans | Middle Aged | Critical Illness | Male | Biomarkers - blood | Shock, Septic - mortality | Sepsis - mortality | Sensitivity and Specificity | Shock, Septic - blood | Female | Sepsis - blood | APACHE | Serum Amyloid A Protein - analysis | Medical research | Care and treatment | Prognosis | C-reactive protein | Nitric oxide | Analysis | Medicine, Experimental | Biological markers
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Loading RightsOncotarget, ISSN 1949-2553, 12/2017, Issue 5
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Loading RightsNature Cell Biology, ISSN 1465-7392, 04/2019, Volume 21, Issue 4, pp. 498 - 510
Metabolic reprogramming is a hallmark of cancer. Here, we demonstrate that tumour-associated macrophages (TAMs) enhance the aerobic glycolysis and apoptotic...
HETEROGENEITY | INHIBITION | MICROENVIRONMENT | GLUCOSE-METABOLISM | GROWTH | RESISTANCE | METASTATIC NICHE FORMATION | HYPOXIA | PROMOTE | PROGRESSION | CELL BIOLOGY | Transducers | Hydroxylation | Chemoresistance | Breast cancer | Macrophages | Ribonucleic acid--RNA | Glycolysis | Breast | Lactic acid | Feedforward | Tumors | Apoptosis | Cancer
HETEROGENEITY | INHIBITION | MICROENVIRONMENT | GLUCOSE-METABOLISM | GROWTH | RESISTANCE | METASTATIC NICHE FORMATION | HYPOXIA | PROMOTE | PROGRESSION | CELL BIOLOGY | Transducers | Hydroxylation | Chemoresistance | Breast cancer | Macrophages | Ribonucleic acid--RNA | Glycolysis | Breast | Lactic acid | Feedforward | Tumors | Apoptosis | Cancer
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Loading RightsJournal of Human Evolution, ISSN 0047-2484, 08/2013, Volume 65, Issue 2, pp. 162 - 167
Most researchers believe that anatomically modern humans (AMH) first appeared in Africa 160-190 ka ago, and would not have reached eastern Asia until ∼50 ka...
Anatomically modern humans | Huanglong Cave | U-series dating | China | SOUTHERN CHINA | GUANGXI | ETHIOPIA | VARIABILITY | AFRICA | EVOLUTIONARY BIOLOGY | EVOLUTION | HOMINID SITE | ANTHROPOLOGY | REMAINS | AGE | Biological Evolution | Caves - chemistry | Radiometric Dating | Humans | Mass Spectrometry | Geologic Sediments - chemistry | Tooth - chemistry | Uranium - chemistry | Chronology as Topic | Fossils | Human evolution | Fossil hominids | Mass spectrometry | Analysis
Anatomically modern humans | Huanglong Cave | U-series dating | China | SOUTHERN CHINA | GUANGXI | ETHIOPIA | VARIABILITY | AFRICA | EVOLUTIONARY BIOLOGY | EVOLUTION | HOMINID SITE | ANTHROPOLOGY | REMAINS | AGE | Biological Evolution | Caves - chemistry | Radiometric Dating | Humans | Mass Spectrometry | Geologic Sediments - chemistry | Tooth - chemistry | Uranium - chemistry | Chronology as Topic | Fossils | Human evolution | Fossil hominids | Mass spectrometry | Analysis
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Loading RightsACS APPLIED MATERIALS & INTERFACES, ISSN 1944-8244, 07/2019, Volume 11, Issue 26, pp. 23093 - 23101
Bacterial infections pose mounting public health concerns and cause an enormous medical and financial burden today. Rapid and sensitive detection of pathogenic...
GENETIC DETECTION | SYSTEM | INFECTIONS | QUANTIFICATION | MATERIALS SCIENCE, MULTIDISCIPLINARY | chronic wound healing | NANOSCIENCE & NANOTECHNOLOGY | MECHANISMS | COLORIMETRIC DETECTION | nanofibers | biofilm eradication | pH-switchable drug release | antimicrobial hydrogel | STAPHYLOCOCCUS-AUREUS | PATHOGENS
GENETIC DETECTION | SYSTEM | INFECTIONS | QUANTIFICATION | MATERIALS SCIENCE, MULTIDISCIPLINARY | chronic wound healing | NANOSCIENCE & NANOTECHNOLOGY | MECHANISMS | COLORIMETRIC DETECTION | nanofibers | biofilm eradication | pH-switchable drug release | antimicrobial hydrogel | STAPHYLOCOCCUS-AUREUS | PATHOGENS
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Loading RightsJournal of Experimental and Clinical Cancer Research, ISSN 1756-9966, 07/2018, Volume 37, Issue 1, pp. 151 - 11
Background: Colorectal cancer (CRC) is one of the most prevalent malignancies in the world and developed drug resistance has represented one of the most...
Cancer stem-like cells | Regorefanib | 5-fluouracil resistant colon cancer | WNT/β-catenin signaling and miR-34a | INVASION | METASTASIS | ONCOLOGY | WNT/beta-catenin signaling and miR-34a | SUSCEPTIBILITY | PROLIFERATION | MICRORNA-34A | EXPRESSION | Genetic aspects | Colon cancer | Research | Drug resistance | Drug therapy | Colorectal cancer | Breast cancer | Metastasis | Kinases | Cancer therapies | Proteins | Cell growth | Chemotherapy | MicroRNAs | Pancreatic cancer | Stem cells | Tumorigenesis | Prostate cancer
Cancer stem-like cells | Regorefanib | 5-fluouracil resistant colon cancer | WNT/β-catenin signaling and miR-34a | INVASION | METASTASIS | ONCOLOGY | WNT/beta-catenin signaling and miR-34a | SUSCEPTIBILITY | PROLIFERATION | MICRORNA-34A | EXPRESSION | Genetic aspects | Colon cancer | Research | Drug resistance | Drug therapy | Colorectal cancer | Breast cancer | Metastasis | Kinases | Cancer therapies | Proteins | Cell growth | Chemotherapy | MicroRNAs | Pancreatic cancer | Stem cells | Tumorigenesis | Prostate cancer
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Loading RightsONCOTARGET, ISSN 1949-2553, 01/2018, Volume 9, Issue 3, pp. 3267 - 3277
Chronic myeloid leukemia (CML) is a myeloproliferative pathology, originating from the hematopoietic cancer stem cells (hCSCs) due to the Bcl-Abl Philadelphia...
CML | diterpenoid ovatodiolide | TYROSINE KINASE | CD34(+)/CD38(-) | MICRORNAS | CANCER | CELL BIOLOGY | PI3K/AKT/mTOR | THERAPY | COMPLETE CYTOGENETIC REMISSION | IMATINIB MESYLATE TREATMENT | STAT5 | DIFFERENTIATION | hematopoietic stem cells | INHIBITOR | TUMORIGENESIS
CML | diterpenoid ovatodiolide | TYROSINE KINASE | CD34(+)/CD38(-) | MICRORNAS | CANCER | CELL BIOLOGY | PI3K/AKT/mTOR | THERAPY | COMPLETE CYTOGENETIC REMISSION | IMATINIB MESYLATE TREATMENT | STAT5 | DIFFERENTIATION | hematopoietic stem cells | INHIBITOR | TUMORIGENESIS
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Loading RightsOncotarget, 2018, Volume 9, Issue 3, pp. 3267 - 3277
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Loading RightsEuropean Journal of Medicinal Chemistry, ISSN 0223-5234, 06/2014, Volume 81, pp. 277 - 288
A novel class of small-molecule inhibitors of MDM2–p53 interaction with a ( )-3-benzylideneindolin-2-one scaffold was identified using an integrated virtual...
Antiproliferative activity | Small-molecule inhibitors | MDM2–p53 interaction | MDM2-p53 interaction | ACTIVATION | DOMAIN | CHEMISTRY, MEDICINAL | PROTEIN-PROTEIN INTERACTION | P53 PATHWAY | DISCOVERY | OPTIMIZATION | ANTAGONISTS | BINDING | EFFICIENCY | Molecular Weight | Antineoplastic Agents - chemical synthesis | HCT116 Cells | Humans | Tumor Suppressor Protein p53 - metabolism | Models, Molecular | Structure-Activity Relationship | Antineoplastic Agents - chemistry | Dose-Response Relationship, Drug | Neoplasms, Experimental - pathology | Animals | Protein Binding - drug effects | Drug Design | Antineoplastic Agents - pharmacology | Cell Proliferation - drug effects | Mice | Mice, Inbred BALB C | Molecular Structure | Cell Cycle - drug effects | Neoplasms, Experimental - drug therapy | Proto-Oncogene Proteins c-mdm2 - metabolism | Drug Screening Assays, Antitumor | Tumor proteins | Colorectal cancer | Index Medicus
Antiproliferative activity | Small-molecule inhibitors | MDM2–p53 interaction | MDM2-p53 interaction | ACTIVATION | DOMAIN | CHEMISTRY, MEDICINAL | PROTEIN-PROTEIN INTERACTION | P53 PATHWAY | DISCOVERY | OPTIMIZATION | ANTAGONISTS | BINDING | EFFICIENCY | Molecular Weight | Antineoplastic Agents - chemical synthesis | HCT116 Cells | Humans | Tumor Suppressor Protein p53 - metabolism | Models, Molecular | Structure-Activity Relationship | Antineoplastic Agents - chemistry | Dose-Response Relationship, Drug | Neoplasms, Experimental - pathology | Animals | Protein Binding - drug effects | Drug Design | Antineoplastic Agents - pharmacology | Cell Proliferation - drug effects | Mice | Mice, Inbred BALB C | Molecular Structure | Cell Cycle - drug effects | Neoplasms, Experimental - drug therapy | Proto-Oncogene Proteins c-mdm2 - metabolism | Drug Screening Assays, Antitumor | Tumor proteins | Colorectal cancer | Index Medicus
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Loading RightsOMICS A Journal of Integrative Biology, ISSN 1536-2310, 03/2019, Volume 23, Issue 3, pp. 167 - 179
Chronic hepatitis B (CHB) is a major global health burden. Liver fibrosis, an insidious process, is the main histopathological change in CHB that might lead to...
precision medicine | microbial proteomics | diagnostic medicine | liver fibrosis biomarkers | hepatitis B | Proteomics | TAFI DEFICIENCY | proteomics | MODELS | BIOTECHNOLOGY & APPLIED MICROBIOLOGY | DISEASE | GENETICS & HEREDITY | EPIDEMIOLOGY
precision medicine | microbial proteomics | diagnostic medicine | liver fibrosis biomarkers | hepatitis B | Proteomics | TAFI DEFICIENCY | proteomics | MODELS | BIOTECHNOLOGY & APPLIED MICROBIOLOGY | DISEASE | GENETICS & HEREDITY | EPIDEMIOLOGY
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Quaternary Geochronology, ISSN 1871-1014, 10/2014, Volume 23, pp. 56 - 62
Maba hominin, one of the key representatives of archaic in China, was originally attributed to around the Middle-Late Pleistocene transition (∼130 ka) based on...
Middle Pleistocene | Maba hominin | Speleothem calcite | Southern China | U-series dating | Archaic Homo sapiens | URANIUM | MODERN HUMANS | HUMAN-EVOLUTION | ETHIOPIA | MODEL | HOMO HEIDELBERGENSIS | AFRICA | ORIGIN | GEOGRAPHY, PHYSICAL | GEOSCIENCES, MULTIDISCIPLINARY | ASIA | Archaeology
Middle Pleistocene | Maba hominin | Speleothem calcite | Southern China | U-series dating | Archaic Homo sapiens | URANIUM | MODERN HUMANS | HUMAN-EVOLUTION | ETHIOPIA | MODEL | HOMO HEIDELBERGENSIS | AFRICA | ORIGIN | GEOGRAPHY, PHYSICAL | GEOSCIENCES, MULTIDISCIPLINARY | ASIA | Archaeology
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Loading RightsEuropean Journal of Medicinal Chemistry, ISSN 0223-5234, 08/2014, Volume 83, pp. 409 - 418
Based on the chemical structure of Pyrroloquinoline quinone (PQQ), a novel class of indole-2-carboxylate derivatives was designed, synthesized and assayed for...
PQQ | ROS generation | Antiproliferative activities | Indole-2-carboxylate derivatives | PYRROLOQUINOLINE QUINONE PQQ | NORTOPSENTIN | COENZYME | CHEMISTRY, MEDICINAL | PHYSIOLOGICAL IMPORTANCE | ANALOGS | ANTITUMOR-ACTIVITY | INHIBITOR | Chemistry Techniques, Synthetic | Intracellular Space - drug effects | Reactive Oxygen Species - metabolism | Antineoplastic Agents - chemical synthesis | Humans | Indoles - chemical synthesis | Structure-Activity Relationship | Antineoplastic Agents - chemistry | Proteolysis - drug effects | Poly(ADP-ribose) Polymerases - metabolism | Intracellular Space - metabolism | Drug Design | Cell Line, Tumor | Inhibitory Concentration 50 | Indoles - pharmacology | Antineoplastic Agents - pharmacology | Cell Proliferation - drug effects | Cell Cycle - drug effects | Indoles - chemistry | Drug Screening Assays, Antitumor | Etoposide | Quinone | Lead compounds
PQQ | ROS generation | Antiproliferative activities | Indole-2-carboxylate derivatives | PYRROLOQUINOLINE QUINONE PQQ | NORTOPSENTIN | COENZYME | CHEMISTRY, MEDICINAL | PHYSIOLOGICAL IMPORTANCE | ANALOGS | ANTITUMOR-ACTIVITY | INHIBITOR | Chemistry Techniques, Synthetic | Intracellular Space - drug effects | Reactive Oxygen Species - metabolism | Antineoplastic Agents - chemical synthesis | Humans | Indoles - chemical synthesis | Structure-Activity Relationship | Antineoplastic Agents - chemistry | Proteolysis - drug effects | Poly(ADP-ribose) Polymerases - metabolism | Intracellular Space - metabolism | Drug Design | Cell Line, Tumor | Inhibitory Concentration 50 | Indoles - pharmacology | Antineoplastic Agents - pharmacology | Cell Proliferation - drug effects | Cell Cycle - drug effects | Indoles - chemistry | Drug Screening Assays, Antitumor | Etoposide | Quinone | Lead compounds
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Loading RightsMolecular Therapy - Nucleic Acids, ISSN 2162-2531, 06/2019, Volume 16, pp. 745 - 757
Atherosclerosis (AS) is a chronic inflammatory disease characterized by accumulating deposition of lipids in the arterial intima. Notably, macrophages...
atherosclerosis | Notch-signaling pathway | macrophage | plaque formation | microRNA-133b | Animal models | Immune response | Leukocyte migration | Therapeutic applications | Genes | MiRNA | Lipids | Smooth muscle | Macrophages | Manuscripts | Cholesterol | Inflammatory diseases | Signal transduction | Lipoproteins | Arteriosclerosis | MicroRNAs | Apoptosis
atherosclerosis | Notch-signaling pathway | macrophage | plaque formation | microRNA-133b | Animal models | Immune response | Leukocyte migration | Therapeutic applications | Genes | MiRNA | Lipids | Smooth muscle | Macrophages | Manuscripts | Cholesterol | Inflammatory diseases | Signal transduction | Lipoproteins | Arteriosclerosis | MicroRNAs | Apoptosis
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Loading RightsBMC Molecular and Cell Biology, ISSN 2661-8850, 06/2019, Volume 20, Issue 1, p. 15
Background To investigate the effects of serum amyloid A1 (SAA1) on lipopolysaccharide (LPS) -induced inflammation in vascular smooth muscle cells (VSMCs)....
Vascular smooth muscle cell | Inflammation | p38MAPK/NF-κB | Serum amyloid A1 | NOX-4/ROS | LPS | PHYSIOLOGY | p38MAPK/NF-kappa B | INVOLVEMENT | ATHEROSCLEROSIS | VARIANT | CELL BIOLOGY | SERUM AMYLOID-A | LIPOPOLYSACCHARIDE | LOW-GRADE INFLAMMATION | DYSFUNCTION | EXPRESSION | NADPH OXIDASES | Oxidative stress | Toxicity | Smooth muscle | Cardiovascular disease | Kinases | NAD(P)H oxidase | Western blotting | Lipopolysaccharides | Interleukin 6 | Proteins | Signal transduction | NOX4 protein | Atherosclerosis | Physiology | Amyloid | Interleukin 8 | NF-κB protein | Superoxide | siRNA | Chemiluminescence | Tumor necrosis factor-α | IL-1β | Interleukin 17 | Polymerase chain reaction | Protein expression | Monocyte chemoattractant protein 1
Vascular smooth muscle cell | Inflammation | p38MAPK/NF-κB | Serum amyloid A1 | NOX-4/ROS | LPS | PHYSIOLOGY | p38MAPK/NF-kappa B | INVOLVEMENT | ATHEROSCLEROSIS | VARIANT | CELL BIOLOGY | SERUM AMYLOID-A | LIPOPOLYSACCHARIDE | LOW-GRADE INFLAMMATION | DYSFUNCTION | EXPRESSION | NADPH OXIDASES | Oxidative stress | Toxicity | Smooth muscle | Cardiovascular disease | Kinases | NAD(P)H oxidase | Western blotting | Lipopolysaccharides | Interleukin 6 | Proteins | Signal transduction | NOX4 protein | Atherosclerosis | Physiology | Amyloid | Interleukin 8 | NF-κB protein | Superoxide | siRNA | Chemiluminescence | Tumor necrosis factor-α | IL-1β | Interleukin 17 | Polymerase chain reaction | Protein expression | Monocyte chemoattractant protein 1
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Loading RightsArchaeology in Oceania, ISSN 0728-4896, 07/2016, Volume 51, Issue 2, p. 158
Polynesian adze sourcing studies that rely on geochemical analyses to assign distant artefacts to a source or quarry have been undertaken for more than three...
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Synthesis and anti-influenza virus activities of a novel class of gastrodin derivatives
Molecules, ISSN 1420-3049, 04/2013, Volume 18, Issue 4, pp. 3789 - 3805
A series of substituted aryl glycoside analogues of gastrodin have been identified as potential anti-influenza agents. The most potent inhibitor 1a exhibited...
Influenza virus inhibitors | Synthesis | Aryl glycoside | Gastrodin | synthesis | influenza virus inhibitors | gastrodin | aryl glycoside | BIOCHEMISTRY & MOLECULAR BIOLOGY | RESISTANCE | ISOLATED WORLDWIDE | CHEMISTRY, MULTIDISCIPLINARY | Antiviral Agents - pharmacology | Glucosides - pharmacology | Neuraminidase - metabolism | Structure-Activity Relationship | Influenza A Virus, H1N1 Subtype - drug effects | Influenza A Virus, H1N1 Subtype - growth & development | Glucosides - chemical synthesis | Animals | Viral Matrix Proteins - antagonists & inhibitors | Benzyl Alcohols - pharmacology | Hemagglutination - drug effects | Antiviral Agents - chemical synthesis | Inhibitory Concentration 50 | Female | Neuraminidase - antagonists & inhibitors | Viral Matrix Proteins - metabolism | Mice | Benzyl Alcohols - chemical synthesis | Oseltamivir - pharmacology
Influenza virus inhibitors | Synthesis | Aryl glycoside | Gastrodin | synthesis | influenza virus inhibitors | gastrodin | aryl glycoside | BIOCHEMISTRY & MOLECULAR BIOLOGY | RESISTANCE | ISOLATED WORLDWIDE | CHEMISTRY, MULTIDISCIPLINARY | Antiviral Agents - pharmacology | Glucosides - pharmacology | Neuraminidase - metabolism | Structure-Activity Relationship | Influenza A Virus, H1N1 Subtype - drug effects | Influenza A Virus, H1N1 Subtype - growth & development | Glucosides - chemical synthesis | Animals | Viral Matrix Proteins - antagonists & inhibitors | Benzyl Alcohols - pharmacology | Hemagglutination - drug effects | Antiviral Agents - chemical synthesis | Inhibitory Concentration 50 | Female | Neuraminidase - antagonists & inhibitors | Viral Matrix Proteins - metabolism | Mice | Benzyl Alcohols - chemical synthesis | Oseltamivir - pharmacology
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Loading RightsChemical & Pharmaceutical Bulletin, ISSN 0009-2363, 11/2010, Volume 58, Issue 11, p. 1436
A series of novel glutarimide compounds were synthesized and their antiviral activities were evaluated. The compounds displaying the strongest antiviral...
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Key Engineering Materials, ISSN 1013-9826, 07/2015, Volume 655, pp. 153 - 158
The low dielectric loss ceramic-polymer composites were prepared by extrusion processing technique with high density polyethylene (HDPE) as matrix and high...
Microwave antennas | Polymer-ceramic composites | Microwave dielectrics | Dielectric loss | Ceramic powders | Polyethylenes | Dielectric constant | High density | Dielectric properties | Ceramics
Microwave antennas | Polymer-ceramic composites | Microwave dielectrics | Dielectric loss | Ceramic powders | Polyethylenes | Dielectric constant | High density | Dielectric properties | Ceramics
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