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251. Parthenolide protects human lens epithelial cells from oxidative stress-induced apoptosis via inhibition of activation of caspase-3 and caspase-9

Author

Hangping Yao, Xueting Shao, Ke Yao, Nanping Wu, Xiajing Tang, and Lei Feng

Subjects
Caspase 3, Apoptosis, medicine.disease_cause, chemistry.chemical_compound, Western blot, Annexin, Lens, Crystalline, medicine, Animals, Humans, Parthenolide, Molecular Biology, Caspase, Cells, Cultured, Caspase-9, medicine.diagnostic_test, biology, Anti-Inflammatory Agents, Non-Steroidal, Epithelial Cells, Cell Biology, Molecular biology, Caspase Inhibitors, Caspase 9, Enzyme Activation, Oxidative Stress, Biochemistry, chemistry, biology.protein, sense organs, Rabbits, Sesquiterpenes, Oxidative stress
Abstract

The apoptosis of lens epithelial cells has been proposed as the common basis of cataract formation, with oxidative stress as the major cause. This study was performed to investigate the protective effect of the herbal constituent parthenolide against oxidative stress-induced apoptosis of human lens epithelial (HLE) cells and the possible molecular mechanisms involved. HLE cells (SRA01-04) were incubated with 50 microM H(2)O(2) in the absence or presence of different doses of parthenolide (10, 20 and 50 microM). To study apoptosis, the cells were assessed by morphologic examination and Annexin V-propidium iodide double staining flow cytometry; to investigate the underlying molecular mechanisms, the expression of caspase-3 and caspase-9 were assayed by Western blot and quantitative RT-PCR, and the activities of caspase-3 and caspase-9 were measured by a Chemicon caspase colorimetric activity assay kit. Stimulated with H(2)O(2) for 18 h, a high fraction of HLE cells underwent apoptosis, while in the presence of parthenolide of different concentrations, dose-dependent blocking of HLE cell apoptosis was observed. The expression of caspase-3 and caspase-9 induced by H(2)O(2) in HLE cells was significantly reduced by parthenolide both at the protein and mRNA levels, and the activation of caspase-3 and caspase-9 was also suppressed by parthenolide in a dose-dependent manner. In conclusion, parthenolide prevents HLE cells from oxidative stress-induced apoptosis through inhibition of the activation of caspase-3 and caspase-9, suggesting a potential protective effect against cataract formation.

Published
2007

252. Development of striatal fast-spiking GABAergic interneurons

Author

Nanping Wu, Joshua L. Plotkin, Marie-Françoise Chesselet, and Michael Levine

Subjects
education.field_of_study, Population, Striatum, Biology, Neurotransmission, Medium spiny neuron, gamma-Aminobutyric acid, medicine.anatomical_structure, nervous system, Cerebral cortex, Basal ganglia, medicine, GABAergic, education, Neuroscience, medicine.drug
Abstract

Fast-spiking GABAergic interneurons represent a very small portion of striatal neurons, yet they play a critical role in modulating cortical input and mediating inhibition of striatal medium-sized spiny projection neurons. Considering their pivotal role in the adult striatum, it is of importance to determine when during development these neurons acquire their characteristic properties and function. In this review we describe recent work from our laboratories indicating that fast-spiking GABAergic interneurons are under stronger cortical control than efferent neurons at postnatal day 12 but mature considerably between postnatal days 12-19 in the rat striatum. During this time period, their molecular development is under the control of GABAergic and cholinergic mechanisms. Thus, fast-spiking interneurons are poised to influence striatal function and perhaps development during the postnatal period in rats, and their properties could be influenced by commonly used pharmacological agents during a protracted developmental window. These findings point to the need for future research to better understand the functional maturation of this critical population of striatal GABAergic neurons, and the consequences of abnormal maturation of these cells.

Published
2007

253. Abstract B18: MicroRNA-21 is involved in pancreatic cancer fibroblast tumor supportiveness

Author

Andrew Nguyen, Timothy R. Donahue, Nanping Wu, Paul A. Toste, and Luyi Li

Subjects
Oncology, Cancer Research, medicine.medical_specialty, Gene knockdown, Tumor microenvironment, business.industry, Cancer, medicine.disease, Fibroblast migration, Metastasis, Small hairpin RNA, Internal medicine, Pancreatic cancer, microRNA, Medicine, business
Abstract

Background: Pancreatic ductal adenocarcinoma (PDAC) is characterized by poor survival despite current medical and surgical therapies and has a propensity towards subclinical metastasis even with resectable disease. The tumor microenvironment consists of a network of supporting cells, including tumor-associated fibroblasts (TAFs), which promote tumor invasion and metastasis, and contribute to PDAC’s extremely poor prognosis. MicroRNAs (miRs) have recently emerged as critical players in post-transcriptional regulation of pathways in cancer biology. In this study, we identified miRs in fibroblasts induced by PDAC tumor cells (TCs). Further, we study the stable suppression of one of these miRs in TAFs and the effects upon fibroblast migration and invasion, as well as tumor cell proliferation. Methods: Primary pancreatic fibroblasts were cultured with MIA PaCa-2 TC conditioned media and RNA was analyzed by the NanoString MicroRNA Expression Assay. Stable miR knockdown (KD) was achieved with a stably expressed shRNA anti-microRNA by lentiviral vector. Migration was determined by an 18 hour scratch assay and 24 hour invasion by modified Boyden chamber. TC proliferation was measured by MTT assay. In vivo tumor growth was evaluated by subcutaneous TC and TAF co-implantation in NSG mice. Results: In primary pancreatic fibroblasts, MIA PaCa-2 tumor cells induced 62 miRs >50% increase or 30% decrease in expression. The most prevalent induced miR with 2-fold increase in expression was miR-21. miR-21 KD in TAFs was achieved by introducing stable expression of anti-miR-21, which resulted in a 75% decrease in expression (P50% decreased ability to migrate (p Conclusions: Pancreatic cancer TCs can induce tumor supportive miRs in TAFs. miR-21 KD in PDAC TAFs results in decreased TAF migration and invasion, as well as reduced ability to support in vitro and in vivo tumor growth. Citation Format: Andrew Hieu Nguyen, Luyi Li, Paul Toste, Nanping Wu, Timothy R. Donahue. MicroRNA-21 is involved in pancreatic cancer fibroblast tumor supportiveness. [abstract]. In: Proceedings of the AACR Special Conference on Pancreatic Cancer: Innovations in Research and Treatment; May 18-21, 2014; New Orleans, LA. Philadelphia (PA): AACR; Cancer Res 2015;75(13 Suppl):Abstract nr B18.

Published
2015

254. The Corticostriatal Pathway in Huntington’s Disease

Author

Nanping Wu, Véronique M. André, Michael Levine, Damian M. Cummings, and Carlos Cepeda

Subjects
Cerebral Cortex, General Neuroscience, Glutamate receptor, Long-term potentiation, Striatum, medicine.disease, Phenotype, Article, Corpus Striatum, Glutamatergic, medicine.anatomical_structure, Huntington Disease, Huntington's disease, nervous system, Cerebral cortex, Activity-dependent plasticity, Neural Pathways, medicine, Animals, Humans, Psychology, Neuroscience
Abstract

The corticostriatal pathway provides most of the excitatory glutamatergic input into the striatum and it plays an important role in the development of the phenotype of Huntington's disease (HD). This review summarizes results obtained from genetic HD mouse models concerning various alterations in this pathway. Evidence indicates that dysfunctions of striatal circuits and cortical neurons that make up the corticostriatal pathway occur during the development of the HD phenotype, well before there is significant neuronal cell loss. Morphological changes in the striatum are probably primed initially by alterations in the intrinsic functional properties of striatal medium-sized spiny neurons. Some of these alterations, including increased sensitivity of N-methyl-D-aspartate receptors in subpopulations of neurons, might be constitutively present but ultimately require abnormalities in the corticostriatal inputs for the phenotype to be expressed. Dysfunctions of the corticostriatal pathway are complex and there are multiple changes as demonstrated by significant age-related transient and more chronic interactions with the disease state. There also is growing evidence for changes in cortical microcircuits that interact to induce dysfunctions of the corticostriatal pathway. The conclusions of this review emphasize, first, the general role of neuronal circuits in the expression of the HD phenotype and, second, that both cortical and striatal circuits must be included in attempts to establish a framework for more rational therapeutic strategies in HD. Finally, as changes in cortical and striatal circuitry are complex and in some cases biphasic, therapeutic interventions should be regionally specific and take into account the temporal progression of the phenotype.

Published
2006

255. Synaptic Alterations in Genetic Mouse Models of Huntington’s and Parkinson’s Diseases: Is there a Common Thread?

Author

Nanping Wu, Michael S. Levine, Véronique M. André, and Carlos Cepeda

Subjects
Principal function, Vesicular transport protein, Huntingtin, nervous system, Neuronal communication, Cognition, Neurotransmission, Biology, Phenotype, Neuroscience, Parkin, nervous system diseases
Abstract

The principal function of neurons is to communicate messages via the release of neurotransmitters, neuromodulators and trophic factors. Impaired synaptic transmission leads to cognitive and motor abnormalities. Huntingtin, α-synuclein and parkin play an important role in vesicle transport and synaptic transmission, so that mutations in these proteins impair neuronal communication and lead to a characteristic phenotype. Understanding the function of these proteins in physiological and pathological conditions will further our knowledge of the processes leading to neurodegenerative disorders and the possibility of finding new rational therapies.

Published
2006

256. Activation, proliferation and commitment of endogenous stem/progenitor cells to the oligodendrocyte lineage by TS1 in a rat model of dysmyelination

Author

Fernando Macias, Wole Awosika, Michael Levine, Paul M. Zhao, Jean de Vellis, Carlos Cepeda, Araceli Espinosa-Jeffrey, and Nanping Wu

Subjects
Central Nervous System, Male, Telencephalon, Subventricular zone, Nerve Tissue Proteins, Biology, Stem cell marker, Rats, Mutant Strains, Corpus Callosum, Nestin, Myelin, Developmental Neuroscience, Intermediate Filament Proteins, Cell Movement, Neurofilament Proteins, Lateral Ventricles, Glial Fibrillary Acidic Protein, medicine, Animals, Cell Lineage, Progenitor cell, Insulin-Like Growth Factor I, Rats, Wistar, Cell Proliferation, Glial fibrillary acidic protein, Stem Cells, Transferrin, Cell Differentiation, Oligodendrocyte, Cell biology, Rats, Disease Models, Animal, Oligodendroglia, medicine.anatomical_structure, nervous system, Neurology, Animals, Newborn, biology.protein, Stem cell, Neuroscience, Biomarkers, Demyelinating Diseases
Abstract

Wild-type and myelin-deficient rats received a single intraparenchymal injection of TS1, a specific combination of IGF-1 and transferrin (Tf), into their corpus callosum at postnatal day 4. The fate of endogenous stem cells in the brain was examined by the expression of the stem cell marker nestin, together with Tf, neurofilaments and glial fibrillary acidic protein from 2 to 14 days after injection. Treated mutants lacked nestin expression in the ventricular wall and had an increase in nestin-labeled radial cell processes in the subventricular regions, and extended into the parenchyma. The subventricular zone was populated by healthy new oligodendrocytes (OLs). BrdU incorporation showed that these cells originated by proliferation and were identified as OLs based upon Tf expression. Thus, TS1 is an effective treatment to promote endogenous subventricular zone progenitor proliferation, migration and OL lineage specification. This strategy offers for the first time the possibility of myelin restoration to treat myelin disorders.

Published
2005

257. Elevated expression of miR-155 is associated with the differentiation of CD8+ T cells in patients with HIV-1.

Author

CHANGZHONG JIN, LINFANG CHENG, XIANGYUN LU, TIANSHENG XIE, HAIBO WU, and NANPING WU

Subjects
MICRORNA, CYTOTOXIC T cells, T cell differentiation, HIV-positive persons, HIGHLY active antiretroviral therapy
Abstract

The differentiation and response of CD8+ T cells is vital in host defense against human immunodeficiency virus type 1 (HIV-1). MicroRNA (miR)-155 is an important regulator of T cell differentiation. However, the profile of miR-155 in HIV-1 infected individuals and its association with CD8+ T cell differentiation remain to be fully elucidated. The present cross-sectional study was performed involving 63 HIV-1-infected patients undergoing highly active antiretroviral therapy (HAART), 31 HAART-naïve patients and 35 healthy controls. The levels of miR-155 in CD8+ T cells were detected using reverse transcription-quantitative polymerase chain reaction analysis. Subsets of CD8+ T cell differentiation were detected using flow cytometry. The results revealed that the discord controllers and HAART-naïve patients showed higher percentages of effector and effector memory cells, and lower percentages of naïve cells (P<0.05). The levels of miR-155 in CD8+ T cells from the HIV-1-infected patients were higher, particularly in the discord controllers and HAART naïve patients (P<0.01). The expression levels of miR-155 were positively correlated with the percentages of effector and effector memory CD8+ T cells, and negatively correlated with the percentages of naïve and central memory CD8+ T cells (P<0.01). Taken together, these findings suggested that the levels of miR-155 in CD8+ T cells of patients with HIV-1 were increased and associated with CD8+ T cell differentiation. [ABSTRACT FROM AUTHOR]

Published
2017
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258. Metabolic rates and sulfur cycling in the geologic record

Author

Nanping Wu and James Farquhar

Subjects
Multidisciplinary, Isotope, biology, Ecology, chemistry.chemical_element, engineering.material, Geologic record, biology.organism_classification, Sulfur, chemistry.chemical_compound, chemistry, Commentaries, Environmental chemistry, Physical Sciences, engineering, Sedimentary rock, Pyrite, Sulfate, Desulfovibrio vulgaris, Cycling
Abstract

Phanerozoic levels of atmospheric oxygen relate to the burial histories of organic carbon and pyrite sulfur. The sulfur cycle remains poorly constrained, however, leading to concomitant uncertainties in O2 budgets. Here we present experiments linking the magnitude of fractionations of the multiple sulfur isotopes to the rate of microbial sulfate reduction. The data demonstrate that such fractionations are controlled by the availability of electron donor (organic matter), rather than by the concentration of electron acceptor (sulfate), an environmental constraint that varies among sedimentary burial environments. By coupling these results with a sediment biogeochemical model of pyrite burial, we find a strong relationship between observed sulfur isotope fractionations over the last 200 Ma and the areal extent of shallow seafloor environments. We interpret this as a global dependency of the rate of microbial sulfate reduction on the availability of organic-rich sea-floor settings. However, fractionation during the early/mid-Paleozoic fails to correlate with shelf area. We suggest that this decoupling reflects a shallower paleoredox boundary, primarily confined to the water column in the early Phanerozoic. The transition between these two states begins during the Carboniferous and concludes approximately around the Triassic-Jurassic boundary, indicating a prolonged response to a Carboniferous rise in O2. Together, these results lay the foundation for decoupling changes in sulfate reduction rates from the global average record of pyrite burial, highlighting how the local nature of sedimentary processes affects global records. This distinction greatly refines our understanding of the S cycle and its relationship to the history of atmospheric oxygen.

Published
2013

259. Increased GABAergic function in mouse models of Huntington's disease: reversal by BDNF

Author

Carlos, Cepeda, Amaal J, Starling, Nanping, Wu, Oanh K, Nguyen, Besim, Uzgil, Takahiro, Soda, Veronique M, André, Marjorie A, Ariano, and Michael S, Levine

Subjects
GABA Antagonists, Neurons, Disease Models, Animal, Mice, Huntington Disease, Patch-Clamp Techniques, Brain-Derived Neurotrophic Factor, Animals, Humans, In Vitro Techniques, Synaptic Transmission, gamma-Aminobutyric Acid, Membrane Potentials
Abstract

Huntington's disease (HD) is characterized by loss of striatal gamma-aminobutyric acid (GABA)ergic medium-sized spiny projection neurons (MSSNs), whereas some classes of striatal interneurons are relatively spared. Striatal interneurons provide most of the inhibitory synaptic input to MSSNs and use GABA as their neurotransmitter. We reported previously alterations in glutamatergic synaptic activity in the R6/2 and R6/1 mouse models of HD. In the present study, we used whole-cell voltage clamp recordings to examine GABAergic synaptic currents in MSSNs from striatal slices in these two mouse models compared to those in age-matched control littermates. The frequency of spontaneous GABAergic synaptic currents was increased significantly in MSSNs from R6/2 transgenics starting around 5-7 weeks (when the overt behavioral phenotype begins) and continuing in 9-14-week-old mice. A similar increase was observed in 12-15-month-old R6/1 transgenics. Bath application of brain-derived neurotrophic factor, which is downregulated in HD, significantly reduced the frequency of spontaneous GABAergic synaptic currents in MSSNs from R6/2 but not control mice at 9-14 weeks. Increased GABA current densities also occurred in acutely isolated MSSNs from R6/2 animals. Immunofluorescence demonstrated increased expression of the ubiquitous alpha1 subunit of GABA(A) receptors in MSSNs from R6/2 animals. These results indicate that increases in spontaneous GABAergic synaptic currents and postsynaptic receptor function occur in parallel to progressive decreases in glutamatergic inputs to MSSNs. In conjunction, both changes will severely alter striatal outputs to target areas involved in the control of movement.

Published
2004

260. Preliminary research on the co-infection of human immunodeficiency virus and hepatitis virus in intravenous drug users

Author

Nanping, Wu, Dan, Li, Biao, Zhu, and Wei, Zou

Subjects
Hepatitis, Viral, Human, Humans, HIV Infections, Substance Abuse, Intravenous
Abstract

To confirm the close relationship of high co-infection rate between HIV and hepatitis virus in intravenous drug users (i.v.DUs).Anti-HIV, HBV and HCV were detected by ELISA in the serum from 35 scattered and 15 massed i.v.DUs. PCR and RT-PCR were performed to confirm the infection of HIV, HBV, HCV, HGV and TTV among the 15 massed intravenous drug abusers.Among the 50 i.v.DUs, the positive rates of anti-HCV1 HBsAg, anti-HBe and anti-HBc were 92% (46/50), 12% (6/50), 10% (5/50) and 66% (33/50), respectively. In the samples of HBsAg positive, their HBeAg was also positive. Although the positive rate of serum markers was different in the massed i.v.DUs compared to the scattered i.v.DUs, no significant difference was shown. In the cases of massed i.v.DUs, the positive rates of HIV DNA, HBV-DNA, HCV-RNA, HGV-RNA, and TTV-DNA were 100% (15/15), 26.6% (4/15), 53.3% (8/15), 33.3% (5/15) and 26.6% (4/15), respectively. Among the 15 massed intravenous drug users, one was infected with HIV, HBV, HCV, HGV and TTV; two were infected with HIV, HBV, HCV and HGV; three were infected only with HIV; and the remaining had other forms of co-infection.The co-infection rate of HIV, HBV, HCV, HGV and TTV in intravenous drug users is very high.

Published
2003

261. Parkin-deficient mice exhibit nigrostriatal deficits but not loss of dopaminergic neurons

Author

Nigel T. Maidment, Mahadevan Gajendiran, Marie-Françoise Chesselet, Jie Shen, Matthew S. Goldberg, Sheila M. Fleming, Anushree Bhatnagar, Larry C. Ackerson, Gloria J. Klapstein, Edward G. Meloni, Michael Levine, Carlos Cepeda, Bryan L. Roth, James Palacino, Nanping Wu, and Hoa A. Lam

Subjects
Microdialysis, Time Factors, Dopamine, Ubiquitin-Protein Ligases, Blotting, Western, Nigrostriatal pathway, Substantia nigra, Mice, Transgenic, Striatum, Biochemistry, Parkin, Receptors, Dopamine, Mice, medicine, Animals, Molecular Biology, Alleles, Chromatography, High Pressure Liquid, Germ-Line Mutation, Neurons, biology, Behavior, Animal, Models, Genetic, Dopaminergic, Brain, Parkinson Disease, Cell Biology, Anatomy, nervous system diseases, Ubiquitin ligase, Electrophysiology, Substantia Nigra, Disease Models, Animal, medicine.anatomical_structure, nervous system, biology.protein, Neuroscience, medicine.drug
Abstract

Loss-of-function mutations in parkin are the major cause of early-onset familial Parkinson's disease. To investigate the pathogenic mechanism by which loss of parkin function causes Parkinson's disease, we generated a mouse model bearing a germline disruption in parkin. Parkin-/- mice are viable and exhibit grossly normal brain morphology. Quantitative in vivo microdialysis revealed an increase in extracellular dopamine concentration in the striatum of parkin-/- mice. Intracellular recordings of medium-sized striatal spiny neurons showed that greater currents are required to induce synaptic responses, suggesting a reduction in synaptic excitability in the absence of parkin. Furthermore, parkin-/- mice exhibit deficits in behavioral paradigms sensitive to dysfunction of the nigrostriatal pathway. The number of dopaminergic neurons in the substantia nigra of parkin-/- mice, however, is normal up to the age of 24 months, in contrast to the substantial loss of nigral neurons characteristic of Parkinson's disease. Steady-state levels of CDCrel-1, synphilin-1, and alpha-synuclein, which were identified previously as substrates of the E3 ubiquitin ligase activity of parkin, are unaltered in parkin-/- brains. Together these findings provide the first evidence for a novel role of parkin in dopamine regulation and nigrostriatal function, and a non-essential role of parkin in the survival of nigral neurons in mice.

Published
2003

262. MicroRNAs in Pancreatic Fibroblast Induced by Tumor Cells

Author

Nanping Wu, Timothy R. Donahue, Andrew Nguyen, Luyi Li, and Paul A. Toste

Subjects
medicine.anatomical_structure, business.industry, microRNA, Cancer research, medicine, Surgery, Tumor cells, Fibroblast, business
Published
2014

264. The Impact of Cytotoxic Chemotherapy on Pancreatic Stellate Cells

Author

Brian E. Kadera, Paul A. Toste, Luyi Li, Nanping Wu, Timothy R. Donahue, M. Duong, and Andrew Nguyen

Subjects
Oncology, medicine.medical_specialty, business.industry, Internal medicine, Hepatic stellate cell, Medicine, Surgery, Cytotoxic chemotherapy, business
Published
2014

265. Membrane Resonance and Subthreshold Membrane Oscillations in Mesencephalic V Neurons: Participants in Burst Generation

Author

Scott H. Chandler, Chie-Fang Hsiao, and Nanping Wu

Subjects
Aging, Patch-Clamp Techniques, Potassium Channels, Subthreshold membrane potential oscillations, Tetrodotoxin, In Vitro Techniques, Sodium Channels, Membrane Potentials, Rats, Sprague-Dawley, Bursting, Biological Clocks, Mesencephalon, medicine, Potassium Channel Blockers, Animals, ARTICLE, 4-Aminopyridine, Neurons, Subthreshold conduction, Chemistry, Oscillation, General Neuroscience, Cell Membrane, Resonance, Signal Processing, Computer-Assisted, Rats, Nap, medicine.anatomical_structure, Amplitude, nervous system, Sensory Thresholds, Soma, Neuroscience, Sodium Channel Blockers
Abstract

Trigeminal mesencephalic (Mes V) neurons are critical components of the circuits controlling oral-motor activity. The possibility that they can function as interneurons necessitates a detailed understanding of the factors controlling their soma excitability. Using whole-cell patch-clamp recording,in vitro, we investigated the development of the ionic mechanisms responsible for the previously described subthreshold membrane oscillations and rhythmical burst discharge in Mes V neurons from rats ages postnatal day (P) 2–12. We found that the oscillation amplitude and frequency increased during development, whereas bursting emerged after P6. Furthermore, when bursting was initiated, the spike frequency was largely determined by the oscillation frequency. Frequency domain analysis indicated that these oscillations emerged from the voltage-dependent resonant properties of Mes V neurons. Low doses of 4-aminopyridine (m) reduced the oscillations and abolished resonance in most neurons, suggesting that the resonant current is a steady-state K+current (I4-AP). Sodium ion replacement or TTX reduced substantially the oscillations and peak amplitude of the resonance, suggesting the presence of a persistent Na+current (INaP) that functions to amplify the resonance and facilitate the emergence of subthreshold oscillations and bursting.

Published
2001

267. Subject Index Vol. 28, 2006

Author

Michael Levine, Xueliang Fan, Kang-Quan Hu, Jean de Vellis, Xin Lv, Stephen F. Matheson, Araceli Espinosa-Jeffrey, Suhail Kasim, Elena H. Chartoff, Satoshi Fujimura, R. Wayne Davies, Andrew S. McCallion, H.A. Jinnah, Kiyomi Y. Araki, Nanping Wu, Raffaella Sordella, Ellen J. Hess, Dalton James Surmeier, Fernando Macias, Bonita L. Blake, Paul Montague, Nan Wang, Madeleine R. Brouns, Kiyoshi Egami, Wole Awosika, Allison D. Ebert, T. Virag, Marcy E. MacDonald, Jun-Ying Miao, Le Su, Jeffrey Settleman, John D. VanderHeide, George R. Breese, Carlos Cepeda, Martha C. Bohn, Paul M. Zhao, Ian R. Griffiths, C.E. Rick, Pradeep G. Bhide, and Shangli Zhang

Subjects
Index (economics), Developmental Neuroscience, Neurology, Statistics, Subject (documents), Mathematics
Published
2006

268. HIV-1 downregulates the expression and phosphorylation of receptor tyrosine kinase by targeting the NF-κB pathway.

Author

TINGTING FENG, JIANHE GAN, AILAN QIN, XIAOPING HUANG, NANPING WU, HUA HU, and HANGPING YAO

Subjects
HIV-1 glycoprotein 120, PHOSPHORYLATION, PROTEIN-tyrosine kinases, MACROPHAGES, INFLAMMATION
Abstract

Macrophages are major targets of human immunodeficiency virus (HIV) and can act as long-term reservoirs of the virus. Chronic HIV-1 infection is associated with dysregulated inflammation. Recepteur d'origine nantais (RON) is expressed in tissue resident macrophages and functions to maintain inflammatory homeostasis. The present study aimed to compare the expression of RON on HIV-positive and - negative participants, and to investigate the mechanism by which HIV-1 influences the expression and function of RON in the JLTRG T cell line. The levels of RON and the RON ligand, macrophage-stimulating protein (MSP), in the peripheral blood of HIV-1-positive patients that were receiving (n=22) or not receiving highly active anti-retroviral therapy (HAART) (n=82) and 37 healthy control participants were determined by enzyme-linked immunosorbent assay. Expression of RON and MSP in the JLTRG T cell line was assessed by western blotting and the subcellular location was analyzed by fluorescence microscopy. JLTRG cells were co-cultured with a cell line that stably expresses HIV, H9/HTLV-IIIB, and alterations in the levels of RON and nuclear factor-κB (NF-κB) in JLTRG cells were assessed by western blotting. The expression of RON and MSP were significantly different in the serum of HIV-1- positive patients that were receiving HAART compared with those not receiving H AART (P<0.05) a nd healthy control patients (P<0.01). RON was detected in JLTRG cells, and was shown to be downregulated by HIV-1 infection. HIV-1 infection of JLTRG cells also reduced NF-κB phosphorylation. Thus, HIV-1 was shown to downregulate the expression and phosphorylation of RON by targeting the NF-κB pathway. [ABSTRACT FROM AUTHOR]

Published
2016
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272. A scanning electron microscopy and computer image processing morphometric study of the pharmacological regulation of patency of the peritoneal stomata

Author

Nanping Wu, Zhilian Lu, Ji-Cheng Li, Jilin Zhou, and Yuanhe Shi

Subjects
Ascitic fluid, Pathology, medicine.medical_specialty, business.industry, Scanning electron microscope, Lymphoid Tissue, fungi, Computer image, Ascites, General Medicine, Peritoneal Stomata, Mice, Materia Medica, medicine, Microscopy, Electron, Scanning, Animals, Anatomy, medicine.symptom, Peritoneum, business, Peritoneal Cavity, Developmental Biology
Abstract

The experiment on mice was carried out by injecting intraperitoneally Chinese materia medica for treating hepatocirrhosis with ascites. Observations and a quantitative analysis were carried out on the pharmacological regulation of the peritoneal stomata by using a scanning electron microscope (SEM) and a computer image processing system attached to the SEM. There was a significant increase in both the diameter (P0.05) and distribution density (P0.01) of the peritoneal stomata in the red sage root and alismatis rhizome groups, whereas the effect of poria and poria peel was not significant compared with the control group (P0.05). Our findings confirm the effect of red sage root and alismatis rhizome on the regulation of the peritoneal stomata, which can enhance the absorption of ascitic fluid, taking into consideration the absorbent function of these stomata. They indicate that the patency of peritoneal stomata can vary in response to the effect of some Chinese materia. They also suggest that the ascites is drained mainly by means of enhancing the patency of the stomata and lymphatic absorption of the stomata during the process of treatment by traditional Chinese medicine.

Published
1996

273. Penicillium marneffei infection presenting as vulv-ulcer in an HIV-infected woman

Author

Nanping Wu, C Jin, X Li, and Y Cui

Subjects
Adult, medicine.medical_specialty, Antifungal Agents, AIDS-Related Opportunistic Infections, Human immunodeficiency virus (HIV), lcsh:Medicine, Case Report, HIV Infections, medicine.disease_cause, Diagnosis, Differential, Young Adult, Hiv infected, Humans, Medicine, Ulcer, Voriconazole, biology, business.industry, lcsh:R, Penicillium, HIV, General Medicine, Triazoles, biology.organism_classification, Dermatology, Pyrimidines, Mycoses, Medicine public health, Immunology, Female, Vulvar Diseases, Penicillium marneffei, business, medicine.drug
Abstract

We report the case of an HIV-infected patient with vulv-ulcer as first manifestation associated with Penicillium marneffei, which is of special interest for healthcare workers in all fields.

Published
2011

274. Study of T Cell subsets and IL-7 protein expression in HIV-1-infected patients after 7 years HAART

Author

Norbert H. Brockmeyer, Adriane Skaletz-Rorowski, Nanping Wu, Changzhong Jin, Y. Jin, N. Weng, S Hoextermann, C. Shou, Anja Potthoff, and L. Feng

Subjects
Adult, CD4-Positive T-Lymphocytes, Male, Time Factors, CD3 Complex, T cell, CD3, Human immunodeficiency virus (HIV), lcsh:Medicine, HIV Infections, CD8-Positive T-Lymphocytes, CD38, medicine.disease_cause, Protein expression, Flow cytometry, Interleukin-7 Receptor alpha Subunit, highly active antiretroviral therapy (HAART), Antiretroviral Therapy, Highly Active, Humans, Medicine, Lymphocyte Count, Interleukin-7 receptor, Aged, IL-7, medicine.diagnostic_test, biology, business.industry, Research, Interleukin-7, lcsh:R, virus diseases, General Medicine, Middle Aged, Lymphocyte Subsets, medicine.anatomical_structure, Immunology, HIV-1, biology.protein, Female, business, T cell subsets, CD8
Abstract

Objective To study the changes in T cell subsets and IL-7 in HIV-1-infected patients after seven years of highly active antiretroviral therapy (HAART). Methods Seventy-five individuals were included in this study (25 with effective HAART, 18 with ineffective HAART, 17 untreated HIV+ patients, and 15 volunteers in the HIV negative control group). The counts of CD4+, CD8+, CD8/CD38+, and CD8/HLADR+ T cells as well as the IL-7 protein expression was measured at 5 time points during a period of seven years in patients starting HAART (baseline) and in the HIV negative control group. The expression of CD127 on CD3+ T cells was measured by flow cytometry at a single time point (after 7 years) in patients with HAART and was compared with untreated HIV+ patients and the HIV negative control group. Results At baseline CD4+ T cell counts of HIV-1-infected patients were lower than that in the control group (p < 0.01), whereas the CD8+, CD8/HLADR+ and CD8/CD38+ T cell counts were higher than those in the control group (p <0.01). After seven years of effective HAART, the CD4+ T cell counts had increased and the CD8+ T cell count had decreased, although not to the normal levels (p < 0.05). Both the CD8/HLADR+ and CD8/CD38+ T cell counts had gradually approached those of the control group (p > 0.05). In the ineffective HAART group, the CD8/CD38+ T cell count had not decreased significantly, and CD8/HLADR+ T cell count gradually decreased. Before treatment, IL-7 serum levels of patients were significantly higher than that in the control group (p < 0.01). After seven years of effective HAART, IL-7 levels had gradually decreased, but were still higher than in the control group (p < 0.01). The CD127 expression on CD3+ CD8+ T cells in effective HAART patients was higher than in untreated HIV+ patients (p < 0.05), but was lower than that in the control group (p < 0.05). CD127 expression on CD3+ CD4+ T cells was not significantly different among the control group, untreated HIV+ patients and effective HAART group. Conclusion After seven years of effective HAART, the quantity and capacity of T cell subsets and IL-7 in HIV-1-infected patients had been partially restored, and the abnormal immune activation has significantly diminished.

Published
2011

275. Comparison of a New Gold Immunochromatographic Assay for the Rapid Diagnosis of the Novel Influenza A (H7N9) Virus with Cell Culture and a Real-Time Reverse-Transcription PCR Assay.

Author

Changzhong Jin, Nanping Wu, Xiaorong Peng, Hangping Yao, Xiangyun Lu, Yu Chen, Haibo Wu, Tiansheng Xie, Linfang Cheng, Fumin Liu, Keren Kang, Shixing Tang, and Lanjuan Li

Abstract

We assessed a colloidal gold immunochromatographic assay (GICA) for rapid detection of influenza A (H7N9) and compared it with reverse-transcription-polymerase chain reaction (RT-PCR) and viral culture. Samples from 35 H7N9 infected patients were collected, including 45 throat swab samples, 56 sputum samples, and 39 feces samples. All samples were tested by GICA, viral culture, and RT-PCR. GICA specifically reacted with recombinant HA proteins, virus lysates, and clinical samples fromH7 subtype viruses. Compared with RT-PCR, GICA demonstrated low sensitivity (33.33%) but high specificity (97.56%). The positive rate of GICA tests for samples collected in the period from 8 to 21 days after contact with poultry was much higher than those for samples collected before or after this period. Compared with viral culture, GICA showed sensitivity of 91.67% and specificity of 82.03%. Sputum specimens weremore likely to test positive for H7N9 virus than samples from throat swabs and feces. The GICA-based H7 test is a reliable, rapid, and convenient method for the screening and diagnosis of influenza A (H7N9) disease, especially for the sputum specimens with high viral load. It may be helpful in managing H7N9 epidemics and preliminary diagnosis in early stages in resource-limited settings. [ABSTRACT FROM AUTHOR]

Published
2014
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276. A reconnaissance of the Cu isotopic compositions of hydro-thermal vein-type copper deposit, Jinman, Yunnan, China

Author

Nanping Wu, Qiling Liao, Jon Woodhead, Shao-Yong Jiang, Jiayong Pan, and Jimin Yu

Subjects
chemistry.chemical_classification, Multidisciplinary, Sulfide, chemistry.chemical_element, Mineralogy, Copper, Hydrothermal circulation, Isotope fractionation, Deposition (aerosol physics), chemistry, Sedimentary rock, Organic matter, Vein (geology), Geology
Abstract

The Jinman deposit is a low-temperature hydrothermal vein-type copper deposit, which occurs along faults and fractures within Middle Jurassic sandstone and mudstone units of the Lanping-Simao Mesozoic-Cenozoic basin of Yunnan Province. In this note, we report for the first time the Cu isotopic compositions of Cu-sulfides from the Jinman deposit. The data show large variations and low δ65Cu values of −3.70‰to +0.30‰, which are in sharp contrast to the δ65Cu values of high-temperature magmatic-hydrothermal copper deposits (−0.62‰to +0.40‰) and the modern ocean-floor massive sulfide deposits (−0.48‰ to +1.15‰). It is suggested that the Cu isotope fractionation at Jinman is affected mainly by the following factors, i.e. a low temperature of ore formation (150–286°C); a sedimentary source for ore materials; various stages of ore deposition; and involvement of organic matter in the ore-forming processes.

Published
2002

277. Epidemiological and mortality analysis of older adults with HIV in eastern China.

Author

Tiansheng Xie and Nanping Wu

Subjects
OLDER HIV-positive persons, MORTALITY, EPIDEMIOLOGY, AIDS, CD4 lymphocyte count
Abstract

Objective: The aims of this study were to systematically review epidemiological characteristics in older people living with human immunodeficiency virus/acquired immunodeficiency syndrome (HIV/AIDS) (PLWHA) in low endemic areas of the People's Republic of China, analyze the causes of death and mortality, and provide a basis for targeted prevention in these populations. Methods: Nine counties representative of the distribution and epidemiological factors of the HIV epidemic in Zhejiang Province were selected, and data from 1,115 HIV-positive individuals, including 196 older people (⩾50 years), who were confirmed as PLWHA from January 1, 2000 to December 31, 2012, were retrospectively analyzed. Results: The proportion of older PLWHA increased from 0% in 2000 to 22.45% in 2012. Sexual transmission was the main route, accounting for 82.65% of infections in this group. Compared with the younger group (range from 14 to 49 years old), the older group had significantly lower CD4+ cell counts (291.64 versus 363.63; P<0.001) when first diagnosed, and more of this group presented in the AIDS state with opportunistic infections (51.02% versus 34.06%; P<0.001). In the older group, 25 (12.76%) patients died directly of AIDS and 171 (87.24%) were censored, and in the younger group 50 (5.44%) patients died directly of AIDS and 869 (94.56%) were censored. Estimated survival time since HIV diagnosis in the older group was 11.54±0.49 years (95% confidence interval [CI] 10.59-12.50), while in the younger group it was 13.85±0.46 years (95% CI 12.94-14.76), the log rank (Mantel-Cox) test gave a chi-square value of 3.83, and there was significant difference between the groups (P<0.05). Conclusion: The number of older PLWHA increased steadily over the study period in low HIV endemic provinces of a developing country. Later discovery and preexisting disease perhaps contributed to a shorter estimated survival time for older PLWHA and higher mortality. [ABSTRACT FROM AUTHOR]

Published
2013
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278. Generation of Human Immunodeficiency Virus-1 Long Terminal Repeat Reporter Genes by Rapid Polymerase Chain Reaction-Mediated Mutagenesis.

Author

Juan Wang, HangJun Lv, Ling Xu, Jin Yang, ZongXing Yang, and NanPing Wu

Subjects
POLYMERASE chain reaction methodology, GENE amplification, HIV, RESEARCH methodology, GENETIC mutation, PROBABILITY theory, RESEARCH funding, T-test (Statistics), GENE expression profiling, DESCRIPTIVE statistics
Abstract

Objective: The development of a human immunodeficiency virus (HIV)-1 promoter reporter system is critical for investigating transcription activity of the virus. We designed a modified overlap extension PCR method for single round site-directed mutagenesis of the long terminal repeat (LTR) segment of HIV-1. Methods: The procedure consists of overlap extension PCR, DpnI digestion, and product transformation. Wild-type and serial sequence deletion clones of HIV-1 LTR were constructed. βasal transcription activity was also measured. Results: The overall efficiency for obtaining the desired products was 53.2%. The reporter assay indicated the importance of the second NF-κβ cis-element and surrounding regions in mediating the regulation of HIV-1 transcription. Conclusion: The technique we investigated is suitable for highthroughput functional studies of virus-host interaction. [ABSTRACT FROM AUTHOR]

Published
2013
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279. Connections between Sulfur Cycle Evolution, Sulfur Isotopes, Sediments, and Base Metal Sulfide Deposits.

Author

FARQUHAR, JAMES, NANPING WU, CANFIELD, DONALD E., and ODURO, HARRY

Subjects
SULFUR cycle, GEOCHEMISTRY, SEDIMENTS, ORE deposits, CHEMISTRY, OXIDATION, SULFIDES
Abstract

Significant links exist between the sulfur cycle, sulfur geochemistry of sedimentary systems, and ore deposits over the course of Earth history. A picture emerges of an Archean and Paleoproterozoic stage of the sulfur cycle that has much lower levels of sulfate (<200 µM), carries a signal of mass-independent sulfur, and preserves evidence for temporal and spatial heterogeneity that reflects lower amounts of sulfur cycling than today. A second stage of ocean chemistry in the Paleoproterozoic, with higher atmospheric oxygen and oceanic sulfate at low millimolar levels, follows this stage. The isotopic record in sedimentary rocks and in sulfide-bearing ore deposits suggests abundant pyrite burial and implies a missing 34S-depleted pool that may have been lost via deep ocean deposition and possibly subduction. Proterozoic ocean chemistry appears to be quite complex. The surface waters of the Proterozoic oceans are believed to have been oxygenated, but geologic evidence from ore deposits and sedimentary rocks supports coexistence of significant anoxic, intermediate water and deep-water pools in the Mesoproterozoic. This stage in ocean chemistry ends with the second major global oxidation event in the latest Neoproterozoic (~600 Ma). This event started the transition to more oxygenated intermediate and deep waters, and higher but variable oceanic sulfate concentrations. The event set the scene for the formation in the Phanerozoic of the first significant MVT deposits and possibly is reflected in changes in other sedimentary rock-hosted base metal sulfide deposits. [ABSTRACT FROM AUTHOR]

Published
2010
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280. Immature Neurons and GABA Networks May Contribute to Epileptogenesis in Pediatric Cortical Dysplasia.

Author

Cepeda, Carlos, André, Véronique M., Nanping Wu, Yamazaki, Irene, Uzgil, Besim, Vinters, Harry V., Levine, Michael S., and Mathern, Gary W.

Subjects
NEURONS, GABA, DYSPLASIA, CHILDHOOD epilepsy, AMINOBUTYRIC acid, METHYL aspartate
Abstract

Cortical dysplasia (CD), a frequent pathological substrate of pediatric epilepsy surgery patients, has a number of similarities with immature cortex, such as reduced Mg2+ sensitivity of N-methyl-D-aspartate (NMDA) receptors and the persistence of subplate-like neurons and undifferentiated cells. Because γ-aminobutyric acid (GABA) is the main neurotransmitter in early cortical development, we hypothesized increased GABA receptor-mediated synaptic function in CD tissue. Infrared videomicroscopy and whole-cell patch clamp recordings were used to characterize the morphology and electrophysiological properties of immature and normal-appearing neurons in slices from cortical tissue samples resected for the treatment of pharmacoresistant epilepsy in children (0.2–14 years). In addition, we examined spontaneous and evoked synaptic activity, as well as responses to exogenous GABA application. We demonstrate both the presence of immature pyramidal neurons and networks in young CD tissue and the predominance of GABA synaptic activity. In addition, spontaneous GABA depolarizations frequently induced action potentials, supporting a potential excitatory role of GABA in CD. Evoked synaptic responses mediated by GABA were also prominent, and bath application of 4-aminopyridine induced rhythmic depolarizations that were blocked by bicuculline. Finally, responses to exogenous application of GABA had depolarized reversal potentials in severe compared to mild and non-CD cases. The present data support the hypothesis that CD shares features of immature cortex, with predominant and potentially excitatory GABAA receptor-mediated neurotransmission. These results could partially explain the increased excitability of the cortical network in pediatric CD. [ABSTRACT FROM AUTHOR]

Published
2007
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281. Altered Corticostriatal Neurotransmission and Modulation in Dopamine Transporter Knock-Down Mice.

Author

Nanping Wu

Subjects
*CORTICOSTERONE, *NEURAL transmission, *VISUAL cortex physiology, *DOPAMINERGIC neurons
Abstract

Dopamine (DA) modulates glutamate neurotransmission in the striatum. Abnormal DA modulation has been implicated in neurological and psychiatric disorders. The development of DA transporter knock-down (DAT-KD) mice has permitted modeling of these disorders and has shed new light on DA modulation. DAT-KD mice exhibit increased extracellular DA, hyperactivity, and alterations in habituation. We used whole cell patch-clamp recordings from visually identified striatal neurons in slices to examine the effects of DAT-KD on corticostriatal transmission. Electrophysiological recordings from medium-sized spiny neurons in the dorsal striatum revealed alterations in both amplitude and frequency, of spontaneous glutamate receptor-mediated synaptic currents in cells from DAT-KD mice. Furthermore, kinetic analyses revealed that these currents had shorter half-amplitude durations and faster decay times. In contrast, GABA-receptor–mediated synaptic currents were not altered. Striatal neurons from DAT-KD mice also responded differently to amphetamine, cocaine, and DA D2-receptor agonists or antagonists compared with wildtype (WT) littermate controls. In WTs amphetamine and cocaine reduced the frequency of spontaneous glutamate currents and these effects appeared to be mediated by activation of D2 receptors. In contrast, in DAT-KD mice either no changes or only small increases in frequency occurred. D2-receptor agonists or antagonists also had opposing effects in WT and DAT-KD mice. Together, these results indicate that chronically increased extracellular DA produces long-lasting changes in corticostriatal communication that may be mediated by changes in D2-receptor function. These findings have implications for understanding mechanisms underlying attention deficit hyperactivity disorder and Tourette's syndrome and may provide insights into novel therapeutic approaches. [ABSTRACT FROM AUTHOR]

Published
2007
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282. Voltage-Dependent Calcium Currents in Trigeminal Motoneurons of Early Postnatal Rats: Modulation by 5-HT Receptors.

Author

Chie-Fang Hsiao, Nanping Wu, and Chandler, Scott H.

Abstract

Trigeminal motoneurons relay the final output signals generated within the oral-motor pattern generating circuit(s) to muscles for execution of various motor patterns. In recent years, these motoneurons were shown to possess voltage dependent nonlinear membrane properties that allow them to actively participate in sculpting their final output. A complete understanding of the factors controlling trigeminal motoneuronal (TMN) discharge during oral-motor activity requires, at a minimum, a detailed understanding of the palette of ion channels responsible for membrane excitability and a determination of whether these ion channels are targets for modulation. Toward that end, we studied in detail the properties of calcium channels in TMNs and their susceptibility to modulation by 5-HT in rat brain slices. We found that based on pharmacological and voltage-dependent properties, high-voltage-activated (HVA) N-type [ω-conotoxin GVIA (ω-CgTX)]-sensitive, and to a lesser extent P/Q-type [ω-agatoxin IVA (ω-Aga IVA)]-sensitive, calcium channels make up the majority of the whole cell calcium current. 5-HT (5.0 μM) decreased HVA current by 31.3 ± 2.2%, and the majority of this suppression resulted from reduction of current flow through N- and P/Q-type calcium channels. In contrast, 5-HT had no effect on low-voltage-activated (LVA) current amplitude in TMNs. HVA calcium current inhibition was mimicked by 5-CT, a 5-HT1 receptor agonist, and by R(+)-8-hydroxydipropylaminotetralin hydrobromide (8-OH-DPAT), a specific 5-HT1A agonist. The effects of 5-HT were blocked by the 5-HT1A antagonist 1-(2-methoxyphenyl)-4-[4-(2-phthalimido)butyl]piperazine hydrobromide (NAN-190) but not by ketanserin, a 5-HT2/1C antagonist. Under current clamp, ω-CgTX and 5-HT were most effective in suppressing the mAHP and both increased the spike frequency and input/output gain in response to current injection. Calcium current modulation by 5-HT1A receptors likely is an important mechanism to fine tune the input/output gain of TMNs in response to small incoming synaptic inputs and accounts for some of the previously reported effects of 5-HT on TMN excitability during tonic and burst activity during oral-motor behavior. [ABSTRACT FROM AUTHOR]

Published
2005
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283. Persistent sodium currents in mesencephalic v neurons participate in burst generation and control of membrane excitability.

Author

Nanping Wu, Akifumi Enomoto, Susumu Tanaka, Chie-Fang Hsiao, Duane Q Nykamp, Eugene Izhikevich, and Scott H Chandler

Subjects
*NERVOUS system, *NEURONS, *BRAIN stem, *SENSORY neurons
Abstract

The functional and biophysical properties of a persistent sodium current (I(NaP)) previously proposed to participate in the generation of subthreshold oscillations and burst discharge in mesencephalic trigeminal sensory neurons (Mes V) were investigated in brain stem slices (rats, p7-p12) using whole cell patch-clamp methods. I(NaP) activated around -76 mV and peaked at -48 mV, with V1/2 of -58.7 mV. Ramp voltage-clamp protocols showed that I(NaP) undergoes time- as well as voltage-dependent inactivation and recovery from inactivation in the range of several seconds (tau(onset) = 2.04 s, tau(recov) = 2.21 s). Riluzole (< or =5 microM) substantially reduced I(NaP), membrane resonance, postinhibitory rebound (PIR), and subthreshold oscillations, and completely blocked bursting, but produced modest effects on the fast transient Na+ current (I(NaT)). Before complete cessation, burst cycle duration was increased substantially, while modest and inconsistent changes in burst duration were observed. The properties of the I(NaT) were obtained and revealed that the amplitude and voltage dependence of the resulting "window current" were not consistent with those of the observed I(NaP) recorded in the same neurons. This suggests an additional mechanism for the origin of I(NaP). A neuronal model was constructed using Hodgkin-Huxley parameters obtained experimentally for Na+ and K+ currents that simulated the experimentally observed membrane resonance, subthreshold oscillations, bursting, and PIR. Alterations in the model g(NaP) parameters indicate that I(NaP) is critical for control of subthreshold and suprathreshold Mes V neuron membrane excitability and burst generation. [ABSTRACT FROM AUTHOR]

Published
2005
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285. Triple oxygen isotope reveals insolation-forced tropical moisture cycles.

Author

Lijuan Sha, Haowen Dang, Yue Wang, Wassenburg, Jasper A., Baker, Jonathan L., Hanying Li, Sinha, Ashish, Brahim, Yassine Ait, Nanping Wu, Zhengyao Lu, Ce Yang, Xiyu Dong, Jiayu Lu, Haiwei Zhang, Mahata, Sasadhar, Yanjun Cai, Zhimin Jian, and Hai Cheng

Subjects
*HYDROLOGIC cycle, *OXYGEN isotopes, *RADIATIVE forcing, *WATER vapor, *LATENT heat
Abstract

Tropical oceans are the main global water vapor and latent heat sources, but their responses to radiative forcing remain unclear. Here, we investigate oceanic moisture dynamics of the western tropical Pacific (WTP) over the past 210,000 years through an approach of planktonic foraminiferal triple oxygen isotope (Δ′17O). The Δ′17O record is dominated by the precession cycles (~23,000 years), with lower values reflecting higher humidity in concert with higher Northern Hemisphere summer insolation. Our empirical and modeling results, combined with other geological archives, suggest that the enhanced moisture convergence over the WTP largely intensifies changes in the meridional and zonal hydrological cycles, affecting rainfall patterns in East Asia and northern South America. We propose that the insolation-driven WTP moisture dynamics play a pivotal role in regulating tropical hydroclimate. [ABSTRACT FROM AUTHOR]

Published
2024
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286. Severe acute respiratory syndrome-associated coronavirus genotype and its characterization

Author

Lanjuan, Li, Zhigang, Wang, Yiyu, Lu, Qiyu, Bao, Suhong, Chen, Nanping, Wu, Suyun, Cheng, Jingqing, Weng, Yanjun, Zhang, Juying, Yan, Lingling, Mei, Xiaomeng, Wang, Hanping, Zhu, Yingpu, Yu, Minli, Zhang, Minhong, Li, Jun, Yao, Qunying, Lu, Pingping, Yao, Xiaochen, Bo, Jianer, Wo, Shengqi, Wang, and Songnian, Hu

Subjects
Genotype, Severe acute respiratory syndrome-related coronavirus, Mutation, Humans, Middle Aged
Abstract

To study the severe acute respiratory syndrome (SARS)-associated coronavirus genotype and its characteristics.A SARS-associated coronavirus isolate named ZJ01 was obtained from throat swab samples taken from a patient in Hangzhou, Zhejing province. The complete genome sequence of ZJ01 consisted of 29,715 bp (GenBank accession: AY297028, version: gi: 30910859). Seventeen SARS-associated coronavirus genome sequences in GenBank were compared to analyze the common sequence variations and the probability of co-occurrence of multiple polymorphisms or mutations. Phylogenetic analysis of those sequences was done.By bioinformatics processing and analysis, the 5 loci nucleotides at ZJ01 genome were found being T, T, G, T and T, respectively. Compared with other SARS-associated coronavirus genomes in the GenBank database, an A/G mutation was detected besides the other 4 mutation loci (C:G:C:C/T:T:T:T) involved in this genetic signature. Therefore a new definition was put forward according to the 5 mutation loci. SARS-associated coronavirus strains would be grouped into two genotypes (C:G:A:C:C/T:T:G:T:T), and abbreviated as SARS coronavirus C genotype and T genotype. On the basis of this new definition, the ZJ01 isolate belongs to SARS-associated coronavirus T genotype, first discovered and reported in mainland China. Phylogenetic analysis of the spike protein gene fragments of these SARS-associated coronavirus strains showed that the GZ01 isolate was phylogenetically distinct from other isolates, and compared with groups F1 and F2 of the T genotype, the isolates of BJ01 and CUHK-W1 were more closely related to the GZ01 isolate. It was interesting to find that two (A/G and C/T) of the five mutation loci occurred in the spike protein gene, which caused changes of Asp to Gly and Thr to Ile in the protein, respectively.Attention should be paid to whether these genotype and mutation patterns are related to the virus's biological activities,epidemic characteristics and host clinical symptoms.

288. Purine nucleoside phosphorylase enables dual metabolic checkpoints that prevent T cell immunodeficiency and TLR7-associated autoimmunity.

Author

Abt, Evan R., Rashid, Khalid, Le, Thuc M., Li, Suwen, Lee, Hailey R., Lok, Vincent, Luyi Li, Creech, Amanda L., Labora, Amanda N., Mandl, Hanna K., Lam, Alex K., Cho, Arthur, Rezek, Valerie, Nanping Wu, Abril-Rodriguez, Gabriel, Rosser, Ethan W., Mittelman, Steven D., Hugo, Willy, Mehrling, Thomas, and Bantia, Shanta

Abstract

Purine nucleoside phosphorylase (PNP) enables the breakdown and recycling of guanine nucleosides. PNP insufficiency in humans is paradoxically associated with both immunodeficiency and autoimmunity, but the mechanistic basis for these outcomes is incompletely understood. Here, we identify two immune lineage-dependent consequences of PNP inactivation dictated by distinct gene interactions. During T cell development, PNP inactivation is synthetically lethal with downregulation of the dNTP triphosphohydrolase SAMHD1. This interaction requires deoxycytidine kinase activity and is antagonized by microenvironmental deoxycytidine. In B lymphocytes and macrophages, PNP regulates Toll-like receptor 7 signaling by controlling the levels of its (deoxy)guanosine nucleoside ligands. Overriding this regulatory mechanism promotes germinal center formation in the absence of exogenous antigen and accelerates disease in a mouse model of autoimmunity. This work reveals that one purine metabolism gene protects against immunodeficiency and autoimmunity via independent mechanisms operating in distinct immune lineages and identifies PNP as a potentially novel metabolic immune checkpoint. [ABSTRACT FROM AUTHOR]

Published
2022
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289. Tumor-penetrating peptide enhances transcytosis of silicasome-based chemotherapy for pancreatic cancer.

Author

Xiangsheng Liu, Lin, Paulina, Perrett, Ian, Lin, Joshua, Yu-Pei Liao, Chong Hyun Chang, Jinhong Jiang, Nanping Wu, Donahue, Timothy, Wainberg, Zev, Nel, Andre E., Huan Meng, Liu, Xiangsheng, Liao, Yu-Pei, Chang, Chong Hyun, Jiang, Jinhong, Wu, Nanping, and Meng, Huan

Subjects
*TRANSCYTOSIS, *BIOLOGICAL transport, *PANCREATIC cancer, *NEUROPILINS, *CELL adhesion molecules
Abstract

Pancreatic ductal adenocarcinoma (PDAC) is almost uniformly fatal; however, some improvement in overall survival has been achieved with the introduction of nanocarriers that deliver irinotecan or paclitaxel. Although it is generally assumed that nanocarriers rely principally on abnormal leaky vasculature for tumor access, a transcytosis transport pathway that is regulated by neuropilin-1 (NRP-1) has recently been reported. NRP-1-mediated transport can be triggered by the cyclic tumor-penetrating peptide iRGD. In a KRAS-induced orthotopic PDAC model, coadministration of iRGD enhanced the uptake of an irinotecan-loaded silicasome carrier that comprises lipid bilayer-coated mesoporous silica nanoparticles (MSNPs); this uptake resulted in enhanced survival and markedly reduced metastasis. Further, ultrastructural imaging of the treated tumors revealed that iRGD coadministration induced a vesicular transport pathway that carried Au-labeled silicacomes from the blood vessel lumen to a perinuclear site within cancer cells. iRGD-mediated enhancement of silicasome uptake was also observed in patient-derived xenografts, commensurate with the level of NRP-1 expression on tumor blood vessels. These results demonstrate that iRGD enhances the efficacy of irinotecan-loaded silicasome-based therapy and may be a suitable adjuvant in nanoparticle-based treatments for PDAC. [ABSTRACT FROM AUTHOR]

Published
2017
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290. Human infections with the emerging avian influenza A H7N9 virus from wet market poultry: clinical analysis and characterisation of viral genome.

Author

Yu Chen, Weifeng Liang, Shigui Yang, Nanping Wu, Hainv Gao, Jifang Sheng, Hangping Yao, Jianer Wo, Qiang Fang, Dawei Cui, Yongcheng Li, Xing Yao, Yuntao Zhang, Haibo Wu, Shufa Zheng, Hongyan Diao, Shichang Xia, Yanjun Zhang, Kwok-Hung Chan, and Hoi-Wah Tsoi

Subjects
*INFECTION, *AVIAN influenza, *ANIMAL diseases, *H7N9 Influenza, *INFLUENZA
Abstract

Summary Background Human infection with avian influenza A H7N9 virus emerged in eastern China in February, 2013, and has been associated with exposure to poultry. We report the clinical and microbiological features of patients infected with influenza A H7N9 virus and compare genomic features of the human virus with those of the virus in market poultry in Zhejiang, China. Methods Between March 7 and April 8, 2013, we included hospital inpatients if they had new-onset respiratory symptoms, unexplained radiographic infiltrate, and laboratory-confirmed H7N9 virus infection. We recorded histories and results of haematological, biochemical, radiological, and microbiological investigations. We took throat and sputum samples, used RT-PCR to detect M, H7, and N9 genes, and cultured samples in Madin-Darby canine kidney cells. We tested for co-infections and monitored serum concentrations of six cytokines and chemokines.We collected doacal swabs from 86 birds from epidemiologically linked wet markets and inoculated embryonated chicken eggs with the samples. We identified and subtyped isolates by RT-PCR sequencing. RNA extraction, complementary DNA synthesis, and PCR sequencing were done for one human and one chicken isolate. We characterised and phylogenetically analysed the eight gene segments of the viruses in the patient's and the chicken's isolates, and constructed phylogenetic trees of H, N, PB2, and NS genes. Findings We identified four patients (mean age 56 years), all of whom had contact with poultry 3-8 days before disease onset. They presented with fever and rapidly progressive pneumonia that did not respond to antibiotics. Patients were leucopenic and lymphopenic, and had impaired liver or renal function, substantially increased serum cytokine or chemokine concentrations, and disseminated intravascular coagulation with disease progression. Two patients died. Sputum specimens were more likely to test positive for the H7N9 virus than were samples from throat swabs. The viral isolate from the patient was closely similar to that from an epidemiologically linked market chicken. All viral gene segments were of avian origin. The H7 of the isolated viruses was closest to that of the H7N3 virus from domestic ducks in Zhejiang, whereas the N9 was closest to that of the wild bird H7N9 virus in South Korea. We noted Gln226Leu and Gly186Val substitutions in human virus H7 (associated with increased affinity for cx-2,6-1inked sialic acid receptors) and the PB2 Asp701Asn mutation (associated with mammalian adaptation). Ser31Asn mutation, which is associated with adamantane resistance, was noted in viral M2. Interpretation Cross species poultry-to-person transmission of this new reassortant H7N9 virus is associated with severe pneumonia and multiorgan dysfunction in human beings. Monitoring of the viral evolution and further study of disease pathogenesis will improve disease management, epidemic control, and pandemic preparedness. Fundin9 Larry Chi-Kin Yung, National Key Program for Infectious Diseases of China. [ABSTRACT FROM AUTHOR]

Published
2013
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291. Characterization of the H5N1 Highly Pathogenic Avian Influenza Virus Derived from Wild Pikas in China.

Author

Jiyong Zhou, Wenbo Sun, Junhua Wang, Junqing Guo, Wei Yin, Nanping Wu, Lanjuan Li, Yan Yan, Ming Liao, Yu Huang, Kaijian Luo, Xuetao Jiang, and Chen, Hualan

Subjects
*AVIAN influenza, *PATHOGENIC microorganisms, *VIRUS diseases, *COMMUNICABLE diseases, *RESPIRATORY infections, *MAMMALS
Abstract

The highly pathogenic H5N1 avian influenza virus emerged from China in 1996 and has spread across Eurasia and Africa, with a continuous stream of new cases of human infection appearing since the first large-scale outbreak among migratory birds at Qinghai Lake. The role of wild birds, which are the natural reservoirs for the virus, in the epidemiology of the H5N1 virus has raised great public health concern, but their role in the spread of the virus within the natural ecosystem of free-ranging terrestrial wild mammals remains unclear. In this study, we investigated H5N1 virus infection in wild pikas in an attempt to trace the circulation of the virus. Seroepidemiological surveys confirmed a natural H5N1 virus infection of wild pikas in their native environment. The hemagglutination gene of the H5N1 virus isolated from pikas reveals two distinct evolutionary clades, a mixed/Vietnam H5N1 virus sublineage (MV-like pika virus) and a wild bird Qinghai (QH)-like H5N1 virus sublineage (QH-like pika virus). The amino acid residue (glutamic acid) at position 627 encoded by the PB2 gene of the MV-like pika virus was different from that of the QH-like pika virus; the residue of the MV-like pika virus was the same as that of the goose H5N1 virus (A/GS/Guangdong [GD]/1/96). Further, we discovered that in contrast to the MV-like pika virus, which is nonpathogenic to mice, the QH-like pika virus is highly pathogenic. To mimic the virus infection of pikas, we intranasally inoculated rabbits, a species closely related to pikas, with the H5N1 virus of pika origin. Our findings first demonstrate that wild pikas are mammalian hosts exposed to H5N1 subtype avian influenza viruses in the natural ecosystem and also imply a potential transmission of highly pathogenic avian influenza virus from wild mammals into domestic mammalian hosts and humans. [ABSTRACT FROM AUTHOR]

Published
2009
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292. Parkin-deficient Mice Exhibit Nigrostriatal Deficits but Not Loss of Dopaminergic Neurons.

Author

Goldberg, Matthew S., Fleming, Sheila M., Palacino, James J., Cepeda, Carlos, Lam, Hoa A., Bhatnagar, Anushree, Meloni, Edward G., Nanping Wu, Edward G., Ackerson, Larry C., Klapstein, Gloria J., Gajendiran, Mahadevan, Roth, Bryan L., Chesselet, Marie-Françoise, Maidment, Nigel T., Levine, Michael S., and Jie Shen

Subjects
*PARKINSON'S disease, *BRAIN diseases, *DOPAMINERGIC neurons
Abstract

Loss-of-function mutations in parkin are the major cause of early-onset familial Parkinson's disease. To investigate the pathogenic mechanism by which loss of parkin function causes Parkinson's disease, we generated a mouse model bearing a germline disruption in parkin. Parkin-/- mice are viable and exhibit grossly normal brain morphology. Quantitative in vivo microdialysis revealed an increase in extracellular dopamine concentration in the striatum of parkin-/- mice. Intracellular recordings of medium-sized striatal spiny neutons showed that greater currents are required to induce synaptic responses, suggesting a reduction in synaptic excitability in the absence of parkin. Furthermore, parkin-/- mice exhibit deficits in behavioral paradigms sensitive to dysfunction of the nigrostriatal pathway. The number of dopaminergic neurons in the substantia nigra of parkin-/- mice, however, is normal up to the age of 24 months, in contrast to the substantial loss of nigral neurons characteristic of Parkinson's disease. Steady-state levels of CDCrel-1, synphilin-1, and α-synuclein, which were identified previously as substrates of the E3 ubiquitin ligase activity of parkin, are unaltered in parkin-/- brains. Together these findings provide the first evidence for a novel role of parkin in dopamine regulation and nigrostriatal function, and a non-essential role of parkin in the survival of nigral neurons in mice. [ABSTRACT FROM AUTHOR]

Published
2003
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293. HIV-1 infected Germans have more variations on neck region of DC-specific intercellular adhesion molecule-3-grabbing nonintegrin than HIV-1 infected Chinese.

Author

Li-Jun X, Brockmeyer NH, Bader A, Hang-Ping Y, Zhi-Gang W, and Nanping W

Subjects
China epidemiology, DNA Primers, Genotype, Germany epidemiology, HIV Infections epidemiology, HIV Infections pathology, Humans, RNA, Messenger genetics, RNA, Messenger metabolism, Reverse Transcriptase Polymerase Chain Reaction, Cell Adhesion Molecules genetics, Genetic Predisposition to Disease, Genetic Variation, HIV Infections genetics, HIV-1, Lectins, C-Type genetics, Receptors, Cell Surface genetics, Repetitive Sequences, Nucleic Acid genetics
Abstract

The C-type lectins DC-SIGN and DC-SIGNR bind and transmit HIV-1 depending on the tetramer formed by "neck" region and carbohydrate recognition domain (CRD). Recent studies indicated polymorphisms in neck region of DC-SIGNR were more frequent and associated with susceptibility to HIV-1 infection, whereas no similar trends were observed on DC-SIGN for rare variations of DC-SIGN among the researched subjects in those studies. In our present study, we found 9 genotype variations of DC-SIGN neck region among HIV infected Germans and 3 variations among HIV infected Chinese, respectively. Comparison of those variations between Chinese and Germans reveals strong ethnic discrepancies, and no significant evidence indicates those variations have resistance to susceptibility to HIV-1 infection.

Published
2008

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