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Publication DateTraffic, ISSN 1398-9219, 12/2013, Volume 14, Issue 12, pp. 1255 - 1271
Eph receptors, a complex subfamily of receptor tyrosine kinases, are rapidly endocytosed following ligand‐mediated activation and traffic through endocytic...
Tiam1 | endocytosis | recycling | signaling endosomes | EphA2 | Signaling endosomes | Endocytosis | Recycling | LIGAND-BINDING | C-CBL | NUCLEOTIDE EXCHANGE FACTORS | CELL BIOLOGY | PDGF BETA-RECEPTOR | TRANSFERRIN RECEPTOR | NEURITE OUTGROWTH | CELL-MIGRATION | EPIDERMAL-GROWTH-FACTOR | RHO-GTPASES | INTRACELLULAR TRAFFICKING | Guanine Nucleotide Exchange Factors - genetics | Signal Transduction | Humans | Receptor, EphA2 - metabolism | Animals | Lysosomes - metabolism | Guanine Nucleotide Exchange Factors - metabolism | Receptor, EphA2 - genetics | Cell Line, Tumor | Cell Membrane - metabolism | Mice | T-Lymphoma Invasion and Metastasis-inducing Protein 1 | rac1 GTP-Binding Protein - metabolism | Cell adhesion & migration | signalling endosomes
Tiam1 | endocytosis | recycling | signaling endosomes | EphA2 | Signaling endosomes | Endocytosis | Recycling | LIGAND-BINDING | C-CBL | NUCLEOTIDE EXCHANGE FACTORS | CELL BIOLOGY | PDGF BETA-RECEPTOR | TRANSFERRIN RECEPTOR | NEURITE OUTGROWTH | CELL-MIGRATION | EPIDERMAL-GROWTH-FACTOR | RHO-GTPASES | INTRACELLULAR TRAFFICKING | Guanine Nucleotide Exchange Factors - genetics | Signal Transduction | Humans | Receptor, EphA2 - metabolism | Animals | Lysosomes - metabolism | Guanine Nucleotide Exchange Factors - metabolism | Receptor, EphA2 - genetics | Cell Line, Tumor | Cell Membrane - metabolism | Mice | T-Lymphoma Invasion and Metastasis-inducing Protein 1 | rac1 GTP-Binding Protein - metabolism | Cell adhesion & migration | signalling endosomes
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Loading RightsAmerican Journal of Transplantation, ISSN 1600-6135, 07/2018, Volume 18, Issue 7, pp. 1636 - 1645
Calcineurin inhibitor toxicity (CNT) is a frequent occurrence in transplanted renal grafts and autochthone kidneys from patients undergoing long‐term treatment...
interstitial fibrosis and tubular atrophy | animal models | immunosuppressant ‐ calcineurin inhibitor (CNI) | translational research/science | kidney transplantation/nephrology | pharmacology | kidney (allograft) function/dysfunction | fibrosis | basic (laboratory) research/science | immunosuppressant - calcineurin inhibitor (CNI) | SURGERY | basic (laboratory) research | kidney transplantation | INJURY | MECHANISMS | MATRIX PROTEINS | NEPHROPATHY | dysfunction | TRANSPLANTATION | nephrology | CHRONIC CYCLOSPORINE NEPHROTOXICITY | GROWTH-FACTOR-BETA | science | DISEASE | NEPHRITIS | kidney (allograft) function | translational research | MULTIFUNCTIONAL CYTOKINE | Analysis | Immunosuppressive agents | Kidneys | Toxicity | Epithelial cells | Pathogenesis | Calcineurin | Calcineurin inhibitors | Inflammation | Cyclosporin A | Metastases | Tacrolimus | Tumor necrosis factor | Tumor necrosis factor-TNF | Apoptosis | Kidney transplantation
interstitial fibrosis and tubular atrophy | animal models | immunosuppressant ‐ calcineurin inhibitor (CNI) | translational research/science | kidney transplantation/nephrology | pharmacology | kidney (allograft) function/dysfunction | fibrosis | basic (laboratory) research/science | immunosuppressant - calcineurin inhibitor (CNI) | SURGERY | basic (laboratory) research | kidney transplantation | INJURY | MECHANISMS | MATRIX PROTEINS | NEPHROPATHY | dysfunction | TRANSPLANTATION | nephrology | CHRONIC CYCLOSPORINE NEPHROTOXICITY | GROWTH-FACTOR-BETA | science | DISEASE | NEPHRITIS | kidney (allograft) function | translational research | MULTIFUNCTIONAL CYTOKINE | Analysis | Immunosuppressive agents | Kidneys | Toxicity | Epithelial cells | Pathogenesis | Calcineurin | Calcineurin inhibitors | Inflammation | Cyclosporin A | Metastases | Tacrolimus | Tumor necrosis factor | Tumor necrosis factor-TNF | Apoptosis | Kidney transplantation
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Loading RightsJournal of inherited metabolic disease, ISSN 0141-8955, 08/2019
Fabry disease (FD) is a rare X-linked lysosomal storage disorder caused by α-galactosidase A (α-Gal A) deficiency. The progressive accumulation of...
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Loading RightsJournal of Separation Science, ISSN 1615-9306, 11/2018, Volume 41, Issue 21, pp. 4067 - 4074
Cefepime monitoring in urine by micellar electrokinetic capillary chromatography with UV detection and liquid chromatography coupled to mass spectrometry via...
cefepime | micellar electrokinetic capillary chromatography | capillary electrophoresis | therapeutic drug monitoring | DIRECT SAMPLE INJECTION | CHEMISTRY, ANALYTICAL | HUMAN PLASMA | HEALTHY-SUBJECTS | VALIDATION | CEREBROSPINAL-FLUID | HUMAN SERUM | INHIBITOR COMBINATIONS | IN-VITRO | PHARMACOKINETICS | BETA-LACTAM ANTIBIOTICS | Liquid chromatography | Precipitation (Meteorology) | Mass spectrometry | Analysis | Urine | Spectroscopy | Electrokinetics | Ions | Stability analysis | Chromatography | Proteins | Dilution | Ionization | Scientific imaging | Monitoring
cefepime | micellar electrokinetic capillary chromatography | capillary electrophoresis | therapeutic drug monitoring | DIRECT SAMPLE INJECTION | CHEMISTRY, ANALYTICAL | HUMAN PLASMA | HEALTHY-SUBJECTS | VALIDATION | CEREBROSPINAL-FLUID | HUMAN SERUM | INHIBITOR COMBINATIONS | IN-VITRO | PHARMACOKINETICS | BETA-LACTAM ANTIBIOTICS | Liquid chromatography | Precipitation (Meteorology) | Mass spectrometry | Analysis | Urine | Spectroscopy | Electrokinetics | Ions | Stability analysis | Chromatography | Proteins | Dilution | Ionization | Scientific imaging | Monitoring
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Reduced β-catenin expression affects patterning of bone primordia, but not bone maturation
Biology Open, ISSN 2046-6390, 05/2017, Volume 6, Issue 5, pp. 582 - 588
Wnt/beta-catenin signaling is involved in patterning of bone primordia, but also plays an important role in the differentiation of chondrocytes and...
Limb patterning | β-catenin dosage | Bone development | Canonical wnt signaling | ENDOCHONDRAL OSSIFICATION | OSTEOBLAST DIFFERENTIATION | APICAL ECTODERMAL RIDGE | beta-catenin dosage | MOUSE EMBRYO | CHONDROCYTE DIFFERENTIATION | CARTILAGE | LIMB DEVELOPMENT | SIGNALING PATHWAY | Canonical Wnt signaling | BIOLOGY | GENE-EXPRESSION | MICE | Transcription factors | Wnt protein | Bone diseases | Dosage | Osteoblasts | Cartilage | Osteoporosis | β-catenin | Biomedical materials | Mineralization | Extracellular matrix | Biocompatibility | Primordia | Chondrogenesis | Maturation | Abnormalities | Medical treatment | Embryos | Signaling | Skeletogenesis | Bone mass | Osteoblastogenesis | Chondrocytes | Calcification | Bone | Differentiation
Limb patterning | β-catenin dosage | Bone development | Canonical wnt signaling | ENDOCHONDRAL OSSIFICATION | OSTEOBLAST DIFFERENTIATION | APICAL ECTODERMAL RIDGE | beta-catenin dosage | MOUSE EMBRYO | CHONDROCYTE DIFFERENTIATION | CARTILAGE | LIMB DEVELOPMENT | SIGNALING PATHWAY | Canonical Wnt signaling | BIOLOGY | GENE-EXPRESSION | MICE | Transcription factors | Wnt protein | Bone diseases | Dosage | Osteoblasts | Cartilage | Osteoporosis | β-catenin | Biomedical materials | Mineralization | Extracellular matrix | Biocompatibility | Primordia | Chondrogenesis | Maturation | Abnormalities | Medical treatment | Embryos | Signaling | Skeletogenesis | Bone mass | Osteoblastogenesis | Chondrocytes | Calcification | Bone | Differentiation
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Loading RightsNephrology Dialysis Transplantation, ISSN 0931-0509, 05/2018, Volume 33, Issue suppl_1, pp. i623 - i623
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Loading RightsPflügers Archiv - European Journal of Physiology, ISSN 0031-6768, 8/2016, Volume 468, Issue 8, pp. 1433 - 1448
Acute kidney injury (AKI) is common in hospitalized patients and has a poor prognosis, the severity of AKI being linked to progression to chronic kidney...
EphrinA1 | Biomedicine | Bidirectional | Human Physiology | Kidney repair | EPO | EphA2 | VITRO | ACUTE KIDNEY INJURY | INDUCIBLE FACTOR | ACTIVATION | PHYSIOLOGY | MESENCHYMAL STEM-CELLS | ISCHEMIA-REPERFUSION INJURY | GENE | IN-VIVO | ENDOTHELIAL-CELLS | RECEPTORS | Ephrin-A1 - metabolism | Humans | Cells, Cultured | Receptor, EphA2 - metabolism | Rats | Male | Coculture Techniques - methods | RNA, Messenger - metabolism | Rats, Sprague-Dawley | Hypoxia - metabolism | Animals | Up-Regulation - physiology | Cell Line, Tumor | Signal Transduction - physiology | Erythropoietin - metabolism | Laminin - metabolism | Acute Kidney Injury - metabolism | Physiological aspects | Laminin | Kidney diseases | Erythropoietin | RNA | Analysis | Life Sciences | Cancer
EphrinA1 | Biomedicine | Bidirectional | Human Physiology | Kidney repair | EPO | EphA2 | VITRO | ACUTE KIDNEY INJURY | INDUCIBLE FACTOR | ACTIVATION | PHYSIOLOGY | MESENCHYMAL STEM-CELLS | ISCHEMIA-REPERFUSION INJURY | GENE | IN-VIVO | ENDOTHELIAL-CELLS | RECEPTORS | Ephrin-A1 - metabolism | Humans | Cells, Cultured | Receptor, EphA2 - metabolism | Rats | Male | Coculture Techniques - methods | RNA, Messenger - metabolism | Rats, Sprague-Dawley | Hypoxia - metabolism | Animals | Up-Regulation - physiology | Cell Line, Tumor | Signal Transduction - physiology | Erythropoietin - metabolism | Laminin - metabolism | Acute Kidney Injury - metabolism | Physiological aspects | Laminin | Kidney diseases | Erythropoietin | RNA | Analysis | Life Sciences | Cancer
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Loading RightsMolecular Genetics and Metabolism, ISSN 1096-7192, 02/2019, Volume 126, Issue 2, pp. S110 - S111
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Loading RightsPLoS one, ISSN 1932-6203, 2017, Volume 12, Issue 4, Art. e0175161, pp. 17 - 12:4, Art. e0175161<17
Background Return to work with or after a chronic disease is a dynamic process influenced by a variety of interactions between personal, work, societal and...
Qualifikation | Rehabilitand | Dialyse | Erwerbsquote | Medizin | Medizinische Rehabilitation | Erwerbsbeteiligung | Schweiz | Berufliche Reintegration | Depression (Psy) | Psychosozialer Faktor | Gesundheitszustand | Chronische Krankheit | DEPRESSION | DONOR RENAL-TRANSPLANTATION | MULTIDISCIPLINARY SCIENCES | WORK | LIVER-TRANSPLANT | QUALITY-OF-LIFE | HEALTH | RECIPIENTS | ACCESS | PARTICIPATION | UNEMPLOYMENT | Employment - statistics & numerical data | Humans | Middle Aged | Male | Kidney Transplantation - statistics & numerical data | Models, Statistical | Switzerland | Social Class | Young Adult | Kidney Transplantation - psychology | Adolescent | Adult | Female | Aged | Employment - psychology | Cohort Studies | Psychological aspects | Care and treatment | Kidneys | Chronic kidney failure | Patient outcomes | Organ transplant recipients | Transplantation | Research | End-stage renal disease | Transplants & implants | Liver | Mental health | Social factors | Mental depression | Demographics | Employment | Education | Surgery | Population | Occupational health | Age | Chronic illnesses | Diabetes mellitus | Patients | Quality of life | Studies | Anxieties | Social analysis | Dialysis | Diabetes | Society | Kidney diseases | Kidney transplantation | Life Sciences | Human health and pathology | Santé publique et épidémiologie | Urology and Nephrology
Qualifikation | Rehabilitand | Dialyse | Erwerbsquote | Medizin | Medizinische Rehabilitation | Erwerbsbeteiligung | Schweiz | Berufliche Reintegration | Depression (Psy) | Psychosozialer Faktor | Gesundheitszustand | Chronische Krankheit | DEPRESSION | DONOR RENAL-TRANSPLANTATION | MULTIDISCIPLINARY SCIENCES | WORK | LIVER-TRANSPLANT | QUALITY-OF-LIFE | HEALTH | RECIPIENTS | ACCESS | PARTICIPATION | UNEMPLOYMENT | Employment - statistics & numerical data | Humans | Middle Aged | Male | Kidney Transplantation - statistics & numerical data | Models, Statistical | Switzerland | Social Class | Young Adult | Kidney Transplantation - psychology | Adolescent | Adult | Female | Aged | Employment - psychology | Cohort Studies | Psychological aspects | Care and treatment | Kidneys | Chronic kidney failure | Patient outcomes | Organ transplant recipients | Transplantation | Research | End-stage renal disease | Transplants & implants | Liver | Mental health | Social factors | Mental depression | Demographics | Employment | Education | Surgery | Population | Occupational health | Age | Chronic illnesses | Diabetes mellitus | Patients | Quality of life | Studies | Anxieties | Social analysis | Dialysis | Diabetes | Society | Kidney diseases | Kidney transplantation | Life Sciences | Human health and pathology | Santé publique et épidémiologie | Urology and Nephrology
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Loading RightsJournal of Oncology, ISSN 1687-8450, 2012, Volume 2012, pp. 1 - 11
During the past 20 years, the phosphatase and tensin homolog PTEN has been shown to be involved in major physiological processes, and its mutation or loss is...
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Loading RightsTherapeutische Umschau. Revue therapeutique, ISSN 0040-5930, 03/2015, Volume 72, Issue 3, p. 139
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Journal of Cellular and Molecular Medicine, ISSN 1582-1838, 08/2009, Volume 13, Issue 8b, pp. 1620 - 1631
Oxidized low‐density lipoprotein (oxLDL) induced‐apoptosis of vascular cells may participate in plaque instability and rupture. We have previously shown that...
apoptosis | oxidized low‐density lipoprotein | vascular smooth muscle cell | caveolin‐1 | TRPC1 | Caveolin-1 | Vascular smooth muscle cell | Oxidized low-density lipoprotein | Apoptosis | CANCER-CELLS | MEDICINE, RESEARCH & EXPERIMENTAL | LOCALIZATION | ACTIVATION | INSERTION | OPERATED CA2+ INFLUX | RECEPTOR POTENTIAL CHANNEL-1 | PLASMA-MEMBRANE | CELL BIOLOGY | caveolin-1 | CALCIUM-ENTRY | ENDOTHELIAL-CELLS | LIPID RAFTS | oxidized low-density lipoprotein | Base Sequence | Humans | Cells, Cultured | Gene Expression Regulation - physiology | Lipoproteins, LDL - physiology | RNA, Small Interfering | Apoptosis - physiology | Muscle, Smooth, Vascular - cytology | TRPC Cation Channels - genetics | Caveolin 1 - physiology | Lipoproteins (low density) | Cell culture | Membranes | Regulators | Deregulation | Toxicity | Trafficking | Homeostasis | Smooth muscle | Lipids | Kinases | Cell surface | Calcium influx | Proteins | Transient receptor potential proteins | Cell growth | Actin | Atherosclerosis | Calcium homeostasis | Translocation | Fractionation | Biotinylation | Caveolin | Muscles | Cholesterol | Arteriosclerosis | Cytoskeleton | Membrane trafficking | Calcium ions | Caveolin 1 | Muscle, Smooth, Vascular | TRPC Cation Channels | Gene Expression Regulation | Lipoproteins, LDL
apoptosis | oxidized low‐density lipoprotein | vascular smooth muscle cell | caveolin‐1 | TRPC1 | Caveolin-1 | Vascular smooth muscle cell | Oxidized low-density lipoprotein | Apoptosis | CANCER-CELLS | MEDICINE, RESEARCH & EXPERIMENTAL | LOCALIZATION | ACTIVATION | INSERTION | OPERATED CA2+ INFLUX | RECEPTOR POTENTIAL CHANNEL-1 | PLASMA-MEMBRANE | CELL BIOLOGY | caveolin-1 | CALCIUM-ENTRY | ENDOTHELIAL-CELLS | LIPID RAFTS | oxidized low-density lipoprotein | Base Sequence | Humans | Cells, Cultured | Gene Expression Regulation - physiology | Lipoproteins, LDL - physiology | RNA, Small Interfering | Apoptosis - physiology | Muscle, Smooth, Vascular - cytology | TRPC Cation Channels - genetics | Caveolin 1 - physiology | Lipoproteins (low density) | Cell culture | Membranes | Regulators | Deregulation | Toxicity | Trafficking | Homeostasis | Smooth muscle | Lipids | Kinases | Cell surface | Calcium influx | Proteins | Transient receptor potential proteins | Cell growth | Actin | Atherosclerosis | Calcium homeostasis | Translocation | Fractionation | Biotinylation | Caveolin | Muscles | Cholesterol | Arteriosclerosis | Cytoskeleton | Membrane trafficking | Calcium ions | Caveolin 1 | Muscle, Smooth, Vascular | TRPC Cation Channels | Gene Expression Regulation | Lipoproteins, LDL
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Loading RightsRheumatology, ISSN 1462-0324, 08/2018, Volume 57, Issue 8, pp. 1350 - 1357
Abstract Objectives aPL are frequently present in SLE. In a well characterized SLE cohort we aimed at investigating the prevalence of aPL and assessing their...
Antiphospholipid | Beta 2-glycoprotein 1 | Domain 1 | Systemic lupus erythematosus | Phos-phatidylserine/prothrombin complex | Lupus anticoagulant | DIAGNOSIS | ASSAY | domain 1 | phosphatidylserine/prothrombin complex | RISK | CLASSIFICATION | lupus anticoagulant | RHEUMATOLOGY | antiphospholipid | ANTIPHOSPHATIDYLSERINE/PROTHROMBIN | PATHOGENESIS | systemic lupus erythematosus | beta 2-glycoprotein 1 | ANTICARDIOLIPIN | REVISED CRITERIA | I ANTIBODIES | Immunoglobulin M | Antiphospholipid antibodies | Thrombosis | Immunoglobulin G
Antiphospholipid | Beta 2-glycoprotein 1 | Domain 1 | Systemic lupus erythematosus | Phos-phatidylserine/prothrombin complex | Lupus anticoagulant | DIAGNOSIS | ASSAY | domain 1 | phosphatidylserine/prothrombin complex | RISK | CLASSIFICATION | lupus anticoagulant | RHEUMATOLOGY | antiphospholipid | ANTIPHOSPHATIDYLSERINE/PROTHROMBIN | PATHOGENESIS | systemic lupus erythematosus | beta 2-glycoprotein 1 | ANTICARDIOLIPIN | REVISED CRITERIA | I ANTIBODIES | Immunoglobulin M | Antiphospholipid antibodies | Thrombosis | Immunoglobulin G
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14.
Editorial
Therapeutische Umschau, ISSN 0040-5930, 2015, Volume 72, Issue 3, p. 139
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PLoS ONE, ISSN 1932-6203, 08/2017, Volume 12, Issue 8, p. e0182813
Angiogenesis is a highly coordinated, extremely complex process orchestrated by multiple signaling molecules and blood flow conditions. While sprouting mode of...
CROSS-TALK | RECOVERY | CELLS | RECRUITMENT | GROWTH-FACTOR-BETA | MULTIDISCIPLINARY SCIENCES | PROSTATE-CANCER | NOTCH | PTK787/ZK222584 | PROMOTER | EXPRESSION | Blood Vessels - growth & development | Blood Vessels - metabolism | Humans | Glomerulonephritis - genetics | Rats | Receptors, Notch - genetics | Smad Proteins - genetics | Signal Transduction - genetics | Glomerulonephritis - metabolism | Chick Embryo | Intussusception - genetics | Neovascularization, Pathologic - pathology | Cell Differentiation - genetics | Animals | COUP Transcription Factor II - genetics | Gene Expression Regulation, Developmental | Glomerulonephritis - pathology | Endoglin - genetics | Intussusception - pathology | Protein Binding | Neovascularization, Pathologic - genetics | Endoglin - antagonists & inhibitors | Physiological aspects | Transcription factors | Glycoproteins | Neovascularization | Research | Glomerulonephritis | Ovalbumin | Phosphorylation | Intravenous administration | Pathogenesis | Intussusception | Pillars | Metastasis | Kinases | Blood flow | Studies | Angiogenesis | Endoglin | Signal transduction | Molecular modelling | Rodents | Microvasculature | Inhibition | Differentiation | Prostate cancer | Growth factors | CD105 antigen | Veins & arteries
CROSS-TALK | RECOVERY | CELLS | RECRUITMENT | GROWTH-FACTOR-BETA | MULTIDISCIPLINARY SCIENCES | PROSTATE-CANCER | NOTCH | PTK787/ZK222584 | PROMOTER | EXPRESSION | Blood Vessels - growth & development | Blood Vessels - metabolism | Humans | Glomerulonephritis - genetics | Rats | Receptors, Notch - genetics | Smad Proteins - genetics | Signal Transduction - genetics | Glomerulonephritis - metabolism | Chick Embryo | Intussusception - genetics | Neovascularization, Pathologic - pathology | Cell Differentiation - genetics | Animals | COUP Transcription Factor II - genetics | Gene Expression Regulation, Developmental | Glomerulonephritis - pathology | Endoglin - genetics | Intussusception - pathology | Protein Binding | Neovascularization, Pathologic - genetics | Endoglin - antagonists & inhibitors | Physiological aspects | Transcription factors | Glycoproteins | Neovascularization | Research | Glomerulonephritis | Ovalbumin | Phosphorylation | Intravenous administration | Pathogenesis | Intussusception | Pillars | Metastasis | Kinases | Blood flow | Studies | Angiogenesis | Endoglin | Signal transduction | Molecular modelling | Rodents | Microvasculature | Inhibition | Differentiation | Prostate cancer | Growth factors | CD105 antigen | Veins & arteries
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Loading RightsArthritis & Rheumatology, ISSN 2326-5191, 08/2014, Volume 66, Issue 8, pp. 2259 - 2269
Objective Despite clear advances in the treatment of systemic lupus erythematosus (SLE), many patients still present with refractory lupus nephritis, requiring...
TOPOISOMERASE-I INHIBITOR | ANTIBODIES | MORTALITY | CELLS | EFFICACY | HYBRID MICE | CAMPTOTHECIN | SENSITIVITY | RHEUMATOLOGY | ANTITUMOR-ACTIVITY | ERYTHEMATOSUS | Topoisomerase I Inhibitors - pharmacology | Animals | Topoisomerase I Inhibitors - administration & dosage | Camptothecin - administration & dosage | Female | Lupus Nephritis - drug therapy | Mice | Mice, Inbred NZB | Camptothecin - pharmacology | Disease Progression | Camptothecin - analogs & derivatives | DNA - drug effects | Lupus | Autoimmune diseases | Rodents | Deoxyribonucleic acid--DNA
TOPOISOMERASE-I INHIBITOR | ANTIBODIES | MORTALITY | CELLS | EFFICACY | HYBRID MICE | CAMPTOTHECIN | SENSITIVITY | RHEUMATOLOGY | ANTITUMOR-ACTIVITY | ERYTHEMATOSUS | Topoisomerase I Inhibitors - pharmacology | Animals | Topoisomerase I Inhibitors - administration & dosage | Camptothecin - administration & dosage | Female | Lupus Nephritis - drug therapy | Mice | Mice, Inbred NZB | Camptothecin - pharmacology | Disease Progression | Camptothecin - analogs & derivatives | DNA - drug effects | Lupus | Autoimmune diseases | Rodents | Deoxyribonucleic acid--DNA
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