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Book
Year: 2020 Publisher: Basel, Switzerland MDPI - Multidisciplinary Digital Publishing Institute
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The Hedgehog signaling pathway is an evolutionarily conserved pathway that governs complex developmental processes, including stem cell maintenance, proliferation, differentiation, and patterning. Several recent studies have shown that the aberrant activation of Hedgehog signaling is associated with neoplastic transformation, cancer cell proliferation, metastasis, multiple cancers’ drug resistance, and survival rates. This book focuses on several aspects of Hedgehog signaling in organogenesis and the tumor microenvironment, and presents reviews and original papers on recent efforts in the field of Hedgehog signaling.
Cyp26 enzymes --- congenital anomalies --- CRE/LoxP --- hedgehog signaling --- mouse models --- retinoic acid --- smoothened --- sonic hedgehog --- sonic hedgehog (SHH) --- oral squamous cell carcinoma (OSCC) --- tumor microenvironment (TME) --- tumor-associated macrophages (TAMs) --- cancer-associated fibroblasts (CAFs) --- tumor-associated angiogenesis --- hedgehog --- growth plate --- endochondral ossification --- chondrocyte --- osteoblast --- bone disease --- TMJ --- synovial joint --- articular disc --- Ihh --- PTHrP --- osteoarthritis --- epithelial–mesenchymal interaction (EMI) --- prostate cancer --- external genitalia --- androgen --- basement membrane --- bone morphogenetic protein --- stem cell --- animal experiment --- fracture healing --- cancer stem cells --- hypospadias --- urethra --- penis --- bone --- hedgehog signalling --- tooth development --- epithelial and mesenchymal interaction --- Gli1 --- mesenchymal stem cell --- lineage tracing analysis --- stem cell marker --- n/a --- epithelial-mesenchymal interaction (EMI)
Book
Year: 2021 Publisher: Basel, Switzerland MDPI - Multidisciplinary Digital Publishing Institute
Abstract | Keywords | Export | Availability | Bookmark
Loading...Choose an application
- Reference Manager
- EndNote
- RefWorks (Direct export to RefWorks)
The adult vertebrate central nervous system mainly consists of neurons, astrocytes, microglia cells, and oligodendrocytes. Oligodendrocytes, the myelin-forming cells of the CNS, are subjected to cell stress and subsequent death in a number of metabolic or inflammatory disorders, among which multiple sclerosis (MS) is included. This disease is associated with the development of large demyelinated plaques, oligodendrocyte destruction, and axonal degeneration, paralleled by the activation of astrocytes and microglia as well as the recruitment of peripheral immune cells to the site of tissue injury. Of note, viable oligodendrocytes and an intact myelin sheath are indispensable for neuronal health. For example, it has been shown that oligodendrocytes provide nutritional support to neurons, fast axonal transport depends on proper oligodendrocyte function, and mice deficient in mature myelin proteins eventually display severe neurodegeneration. This Special Issue contains a collection of highly relevant primary research articles as well as review articles focusing on the development, physiology, and pathology of the oligodendrocyte–axon–myelin unit.
Medicine --- Neurosciences --- plasma membrane proteins --- liquid chromatography-mass spectrometry --- murine acute brain slices --- reproducibility --- rat cerebellum --- Nsun5 --- Williams-Beuren syndrome (WBS) --- corpus callosum (CC) --- oligodendrocyte (OL) --- myelination --- remyelination --- EGFR inhibitor --- smoothened agonist --- microfibers --- drug screening --- multiple sclerosis --- cuprizone --- atrophy --- design-based stereology --- 18F-FDG --- macromolecular proton fraction --- MPF --- myelin --- magnetic resonance imaging --- cuprizone model --- demyelination --- oligodendrocyte precursors --- oligodendrocytes --- immunohistochemistry --- oligodendrocyte --- epigenetics --- neurodegeneration --- laquinimod --- energy drinks --- caffeine --- taurine --- neuron --- OPC --- oligodendrocyte progenitor cells --- screening --- nanofibers --- DigiGait™ --- experimental autoimmune encephalomyelitis --- gait analysis --- schizophrenia --- interneuron --- pluripotent stem cells --- cognition --- treatment --- cre-recombinase --- experimental autoimmune encephalomyelitis (EAE) --- glial progenitor cells --- tamoxifen --- down syndrome --- white matter --- glial fate --- transient receptor potential ankyrin 1 --- astrocyte --- conditional knockout --- astrocytes --- white matter disease --- cross-talk --- CNS --- glial cells. --- age --- microglia --- plasma membrane proteins --- liquid chromatography-mass spectrometry --- murine acute brain slices --- reproducibility --- rat cerebellum --- Nsun5 --- Williams-Beuren syndrome (WBS) --- corpus callosum (CC) --- oligodendrocyte (OL) --- myelination --- remyelination --- EGFR inhibitor --- smoothened agonist --- microfibers --- drug screening --- multiple sclerosis --- cuprizone --- atrophy --- design-based stereology --- 18F-FDG --- macromolecular proton fraction --- MPF --- myelin --- magnetic resonance imaging --- cuprizone model --- demyelination --- oligodendrocyte precursors --- oligodendrocytes --- immunohistochemistry --- oligodendrocyte --- epigenetics --- neurodegeneration --- laquinimod --- energy drinks --- caffeine --- taurine --- neuron --- OPC --- oligodendrocyte progenitor cells --- screening --- nanofibers --- DigiGait™ --- experimental autoimmune encephalomyelitis --- gait analysis --- schizophrenia --- interneuron --- pluripotent stem cells --- cognition --- treatment --- cre-recombinase --- experimental autoimmune encephalomyelitis (EAE) --- glial progenitor cells --- tamoxifen --- down syndrome --- white matter --- glial fate --- transient receptor potential ankyrin 1 --- astrocyte --- conditional knockout --- astrocytes --- white matter disease --- cross-talk --- CNS --- glial cells. --- age --- microglia
Book
Year: 2020 Publisher: Basel, Switzerland MDPI - Multidisciplinary Digital Publishing Institute
Abstract | Keywords | Export | Availability | Bookmark
Loading...Choose an application
- Reference Manager
- EndNote
- RefWorks (Direct export to RefWorks)
The Hedgehog signaling pathway is an evolutionarily conserved pathway that governs complex developmental processes, including stem cell maintenance, proliferation, differentiation, and patterning. Several recent studies have shown that the aberrant activation of Hedgehog signaling is associated with neoplastic transformation, cancer cell proliferation, metastasis, multiple cancers’ drug resistance, and survival rates. This book focuses on several aspects of Hedgehog signaling in organogenesis and the tumor microenvironment, and presents reviews and original papers on recent efforts in the field of Hedgehog signaling.
Medicine --- Cyp26 enzymes --- congenital anomalies --- CRE/LoxP --- hedgehog signaling --- mouse models --- retinoic acid --- smoothened --- sonic hedgehog --- sonic hedgehog (SHH) --- oral squamous cell carcinoma (OSCC) --- tumor microenvironment (TME) --- tumor-associated macrophages (TAMs) --- cancer-associated fibroblasts (CAFs) --- tumor-associated angiogenesis --- hedgehog --- growth plate --- endochondral ossification --- chondrocyte --- osteoblast --- bone disease --- TMJ --- synovial joint --- articular disc --- Ihh --- PTHrP --- osteoarthritis --- epithelial-mesenchymal interaction (EMI) --- prostate cancer --- external genitalia --- androgen --- basement membrane --- bone morphogenetic protein --- stem cell --- animal experiment --- fracture healing --- cancer stem cells --- hypospadias --- urethra --- penis --- bone --- hedgehog signalling --- tooth development --- epithelial and mesenchymal interaction --- Gli1 --- mesenchymal stem cell --- lineage tracing analysis --- stem cell marker --- Cyp26 enzymes --- congenital anomalies --- CRE/LoxP --- hedgehog signaling --- mouse models --- retinoic acid --- smoothened --- sonic hedgehog --- sonic hedgehog (SHH) --- oral squamous cell carcinoma (OSCC) --- tumor microenvironment (TME) --- tumor-associated macrophages (TAMs) --- cancer-associated fibroblasts (CAFs) --- tumor-associated angiogenesis --- hedgehog --- growth plate --- endochondral ossification --- chondrocyte --- osteoblast --- bone disease --- TMJ --- synovial joint --- articular disc --- Ihh --- PTHrP --- osteoarthritis --- epithelial-mesenchymal interaction (EMI) --- prostate cancer --- external genitalia --- androgen --- basement membrane --- bone morphogenetic protein --- stem cell --- animal experiment --- fracture healing --- cancer stem cells --- hypospadias --- urethra --- penis --- bone --- hedgehog signalling --- tooth development --- epithelial and mesenchymal interaction --- Gli1 --- mesenchymal stem cell --- lineage tracing analysis --- stem cell marker
Book
Year: 2021 Publisher: Basel, Switzerland MDPI - Multidisciplinary Digital Publishing Institute
Abstract | Keywords | Export | Availability | Bookmark
Loading...Choose an application
- Reference Manager
- EndNote
- RefWorks (Direct export to RefWorks)
The adult vertebrate central nervous system mainly consists of neurons, astrocytes, microglia cells, and oligodendrocytes. Oligodendrocytes, the myelin-forming cells of the CNS, are subjected to cell stress and subsequent death in a number of metabolic or inflammatory disorders, among which multiple sclerosis (MS) is included. This disease is associated with the development of large demyelinated plaques, oligodendrocyte destruction, and axonal degeneration, paralleled by the activation of astrocytes and microglia as well as the recruitment of peripheral immune cells to the site of tissue injury. Of note, viable oligodendrocytes and an intact myelin sheath are indispensable for neuronal health. For example, it has been shown that oligodendrocytes provide nutritional support to neurons, fast axonal transport depends on proper oligodendrocyte function, and mice deficient in mature myelin proteins eventually display severe neurodegeneration. This Special Issue contains a collection of highly relevant primary research articles as well as review articles focusing on the development, physiology, and pathology of the oligodendrocyte–axon–myelin unit.
plasma membrane proteins --- liquid chromatography-mass spectrometry --- murine acute brain slices --- reproducibility --- rat cerebellum --- Nsun5 --- Williams-Beuren syndrome (WBS) --- corpus callosum (CC) --- oligodendrocyte (OL) --- myelination --- remyelination --- EGFR inhibitor --- smoothened agonist --- microfibers --- drug screening --- multiple sclerosis --- cuprizone --- atrophy --- design-based stereology --- 18F-FDG --- macromolecular proton fraction --- MPF --- myelin --- magnetic resonance imaging --- cuprizone model --- demyelination --- oligodendrocyte precursors --- oligodendrocytes --- immunohistochemistry --- oligodendrocyte --- epigenetics --- neurodegeneration --- laquinimod --- energy drinks --- caffeine --- taurine --- neuron --- OPC --- oligodendrocyte progenitor cells --- screening --- nanofibers --- DigiGait™ --- experimental autoimmune encephalomyelitis --- gait analysis --- schizophrenia --- interneuron --- pluripotent stem cells --- cognition --- treatment --- cre-recombinase --- experimental autoimmune encephalomyelitis (EAE) --- glial progenitor cells --- tamoxifen --- down syndrome --- white matter --- glial fate --- transient receptor potential ankyrin 1 --- astrocyte --- conditional knockout --- astrocytes --- white matter disease --- cross-talk --- CNS --- glial cells. --- age --- microglia --- n/a
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