Your search keyword '"Qian, Yongchang"' showing total 22 results

1. HSPA5 Forms Specific Complexes with Copper.

Author

Qian, Yongchang, Meng, Bingchao, Zhang, Xuchu, Zheng, Ying, Taylor, Robert, and Tiffany-Castiglioni, Evelyn

Subjects

*COPPER, *METAL complexes, *ASTROCYTES, *HOMEOSTASIS, *SPECTROPHOTOMETRY, *ETHYLENEDIAMINETETRAACETIC acid, *METAL ions

Abstract

Our previous study indicated that Hspa5 directly interacts with copper (Cu) to maintain Cu homeostasis in astrocytes. In this study, we explored the possibility that Cu forms a specific complex with Hspa5 by assaying stoichiometric binding of Cu and other metals to recombinant human HSPA5 (rh-HSPA5) in silico. Spectrophotometric analysis showed that incubation of rh-HSPA5 with Cu but not with Fe, Mn, Zn, or Pb in the presence of ascorbic acid produced an absorbance peak at 470 nm. Furthermore, the absorbance peak was absent when bovine serum albumin was incubated with Cu and when another recombinant protein YWHAZ-14-3-3-Zeta carrying a 6× histidine tag identical to the tag in the rh-HSPA5 was incubated with Cu. The absorbance peak produced by Cu and rh-HSPA5 was abolished by EDTA treatment and was stabilized at pH levels above 6.5. Assay of the stoichiometry of metal binding to the purified rh-HSPA5 showed that one molecule of the rh-HSPA5 could chelate 1 or 2 Cu, 13 iron (Fe), 5 zinc (Zn) and 10 lead (Pb) ions but not manganese (Mn). These data further support our previous finding that HSPA5 specifically forms a complex with Cu to help maintain Cu homeostasis. [ABSTRACT FROM AUTHOR]

Published

2013

2. ER chaperone–metal interactions: Links to protein folding disorders

Author

Tiffany-Castiglioni, Evelyn and Qian, Yongchang

Subjects

*ENDOPLASMIC reticulum, *MOLECULAR chaperones, *PROTEIN folding, *POST-translational modification, *ETIOLOGY of Alzheimer's disease, *CELLULAR signal transduction, *OXIDATIVE stress, *NEUROTOXICOLOGY, *PHYSIOLOGY

Abstract

Abstract: Chaperones in the endoplasmic reticulum play vital roles in the folding, assembly, and post-translational modification of secretory proteins and also recycle, refold, or initiate degradation of misfolded proteins. Chaperone deficiencies in either amount or function are implicated in the etiology or pathogenesis of Alzheimer''s disease and other protein folding disorders of the central nervous system. In this review, we discuss evidence that chaperones become pathologic through deleterious interactions with metals and then promote protein folding disorders. The “master regulator” chaperone GRP78 in the endoplasmic reticulum is a compelling subject for investigation in this context because it is located at the hub of signaling pathways in a complex chaperone network. It has therefore been studied by several laboratories in conjunction with exposure to toxic metals. The key points of this review are that metals are implicated in the etiology or pathogenesis of Alzheimer''s disease and other protein folding disorders, metals induce the expression GRP78, often associated with oxidative stress, some metals bind to GRP78, and lead (Pb) impairs GRP78 function when it binds to GRP78. If certain metals do indeed cause or promote the aggregation of toxic proteins in the central nervous system, as the available evidence indicates, the identification of the mechanisms by which they act would provide valuable leads for the development of therapies to prevent or reverse toxic protein aggregation. [Copyright &y& Elsevier]

Published

2012

3. Involvement of the molecular chaperone Hspa5 in copper homeostasis in astrocytes

Author

Qian, Yongchang, Zheng, Ying, Taylor, Robert, and Tiffany-Castiglioni, Evelyn

Subjects

*MOLECULAR chaperones, *HEAT shock proteins, *RNA interference, *HOMEOSTASIS, *ASTROCYTES, *COPPER in the body, *LABORATORY rats, *GENE expression, *PROTEIN binding

Abstract

Abstract: Copper (Cu) ion availability in tissues and cells must be closely regulated within safe limits by Cu transporters and chaperones. Astrocytes play key roles in metal homeostasis and distribution in the brain that are only partially understood. The purpose of this study was to define the role that the protein chaperone Hspa5, also known as Grp78, plays in Cu homeostasis in astrocytes. First passage cultures of primary astrocytes from neonatal rats and cultures of the C6 rat glioma cells were used as models. We found that the level of Cu accumulation in astrocyte cultures increased with Cu concentrations in the medium, and Cu treatment significantly reduced cellular levels of iron (Fe), manganese (Mn) and zinc (Zn). Cu accumulation specifically induced protein expression of Hspa5 but not metallothioneins (MTs) in astrocytes. In C6 cells, Hspa5 was identified as one component of a Cu-binding complex and shown to directly bind Cu. However, the level of Hspa5 expression was not proportional to Cu accumulation in astrocytes and C6 cells: astrocytes expressed low protein levels of Hspa5 compared to C6 cells but accumulated significantly more Cu than did C6 cells. Consistent with this finding, astrocytes expressed a lower level of the Cu-extruding protein Atp7a than did C6 cells, and depletion of Hspa5 by RNA interference resulted in significantly increased Cu accumulation and induction of MT1/2 expression. These data demonstrate that Hspa5 is involved in Cu homeostasis in astrocytes but not as a Cu storage protein. [Copyright &y& Elsevier]

Published

2012

4. Image analysis of Ca2+ signals as a basis for neurotoxicity assays: Promises and challenges

Author

Barhoumi, Rola, Qian, Yongchang, Burghardt, Robert C., and Tiffany-Castiglioni, Evelyn

Subjects

*NEUROTOXICOLOGY, *IMAGE analysis, *BIOLOGICAL assay, *INTRACELLULAR calcium, *CYTOSOL, *CELL physiology, *PHYSIOLOGICAL effects of poisons, *TOXICITY testing

Abstract

Abstract: Free intracellular calcium ([Ca2+] i ) controls a wide range of cellular functions such as contraction, neurotransmitter and hormone release, metabolism, cell division and differentiation. Cytosolic Ca2+ levels are abnormal in cells exposed to toxicants and understanding how these levels become altered may improve our ability to design high-throughput methods for the sensitive detection of cellular responses to a toxic exposure. Because Ca2+ is involved in multiple aspects of cellular function, its role in signaling is complex. It is therefore necessary to identify the individual pathways targeted during toxicant exposure in order to use them as a tool for predictive measurements of toxicity and as targets for prevention or reversal of injury. This review illustrates several methods available for analysis of Ca2+ responses in vitro and their applicability for understanding mechanisms of toxicity at the molecular and cellular levels. The review will also consider the usefulness of Ca2+ imaging for predicting a unique signature for classes of toxicants. Towards this end, two methodological approaches for assessment of Ca2+ responses to toxicants are examined: steady state measurements and complex spatial and/or temporal measurements. Each of the methods described and appropriately used results in reliable and reproducible measurements which may be applied in a high-throughput fashion to individualize in vitro assessment of cellular responses caused by toxicants. [Copyright &y& Elsevier]

Published

2010

5. Valproate reversibly reduces neurite outgrowth by human SY5Y neuroblastoma cells

Author

Qian, Yongchang, Zheng, Ying, and Tiffany-Castiglioni, Evelyn

Subjects

*VALPROIC acid, *NEUROBLASTOMA, *MOOD stabilizers, *PARKINSON'S disease, *CYTOPLASMIC filaments, *GENE expression, *COGNITION disorders, *PEOPLE with bipolar disorder

Abstract

Abstract: Valproate (VPA) is a commonly prescribed mood stabilizer. However, emerging evidence indicates that VPA administration may cause reversible symptoms of Parkinsonism and cognitive decline (P/CD) in some manic patients. The mechanism of this phenomenon is unknown. In this study, we used human SY5Y neuroblastoma cells as a neuronal model to investigate the effects of VPA on neurite outgrowth and neurofilament expression. Data showed that the treatment with VPA at therapeutic plasma levels (0.5 mM) significantly reduced cell proliferation from day 4 through day 6, and neurite outgrowth length from day 1 through day 6. Conversely, VPA had no effect on cell proliferation of human CCF astrocytoma cells but stimulated nerve growth factor (NGF)-induced neurite outgrowth from rat PC12 pheochromocytoma cells. In parallel to these alterations in human SY5Y cells, both mRNA and protein levels of neurofilament 160 (NF160) were significantly reduced, starting at day 2 and day 3, respectively, by the treatment. The inhibition of neurite outgrowth by VPA was completely reversed 2 days after cessation of VPA exposure. Furthermore, NF160 protein levels also rebounded to control levels after VPA removal. NGF application significantly alleviated the inhibition of neurite outgrowth by VPA. These data suggest that VPA-modulated NF160 expression was involved in the inhibition and the reversal of neurite outgrowth in human neuronal cells. [Copyright &y& Elsevier]

Published

2009

6. Comparative non-cholinergic neurotoxic effects of paraoxon and diisopropyl fluorophosphate (DFP) on human neuroblastoma and astrocytoma cell lines

Author

Qian, Yongchang, Venkatraj, Jijayanagaram, Barhoumi, Rola, Pal, Ranadip, Datta, Aniruddha, Wild, James R., and Tiffany-Castiglioni, Evelyn

Subjects

*NEUROBLASTOMA, *CELL culture, *ASTROCYTOMAS, *PARAOXONASE

Abstract

Abstract: The objective of this study was to evaluate the comparative non-cholinergic neurotoxic effects of paraoxon, which is acutely neurotoxic, and diisopropyl fluorophosphate (DFP), which induces OPIDN, in the human neuroblastoma SY5Y and the human astrocytoma cell line CCF-STTG1. SY5Y cells have been studied extensively as a model for OP-induced neurotoxicity, but CCF cells have not previously been studied. We conducted a preliminary human gene array assay of OP-treated SY5Y cells in order to assess at the gene level whether these cells can distinguish between OP compounds that do and do not cause OPIDN. Paraoxon and DFP induced dramatically different profiles of gene expression. Two genes were upregulated and 13 downregulated by at least 2-fold in paraoxon-treated cells. In contrast, one gene was upregulated by DFP and none was downregulated at the 2-fold threshold. This finding is consistent with current and previous observations that SY5Y cells can distinguish between OPs that do or do not induce OPIDN. We also examined gene array results for possible novel target proteins or metabolic pathways for OP neurotoxicity. Protein levels of glucose regulated protein 78 (GRP78) revealed that paraoxon exposure at 3 μM for 24 h significantly reduced GRP78 levels by 30% in neuroblastoma cells, whereas DFP treatment had no effect. In comparison with SY5Y neuroblastoma cells, paraoxon and DFP (3 μM for 24 h) each significantly increased GRP78 levels by 23–24% in CCF astrocytoma cells. As we have previously evaluated intracellular changes in Ca2+ levels in SY5Y cells, we investigated the effects of paraoxon and DFP on cellular Ca2+ homeostasis in CCF by studying cytosolic and mitochondrial basal calcium levels. A significant decrease in the ratio of mitochondrial to cytosolic Ca2+ fluorescence was detected in CCF cultures treated for either 1 or 3 days with 1, 3, 10, or 30 μM paraoxon. In contrast, treatment with DFP for 1 day had no significant effect on the ratio of mitochondrial to cytosolic Ca2+ fluorescence; after 3 days treatment, only 30 μM decreased the ratio. These results are consistent with the finding that paraoxon induced a greater decrease than did DFP of intracellular esterase activity in CCF cells. The changes seen in the ratio of mitochondrial to cytosolic Ca2+ represent a good indicator of the degree of injury induced by each chemical tested. This work further develops in vitro models that distinguish between compounds that cause OPIDN and those that induce acute neurotoxicity only. The study also exposes additional OP-induced toxicities that may be obscured in vivo. [Copyright &y& Elsevier]

Published

2007

7. Differential profiles of copper-induced ROS generation in human neuroblastoma and astrocytoma cells

Author

Qian, Yongchang, Zheng, Ying, Abraham, Liz, Ramos, Kenneth S., and Tiffany-Castiglioni, Evelyn

Subjects

*NEUROBLASTOMA, *TUMORS in children, *ASTROCYTOMAS, *SUPEROXIDE dismutase

Abstract

Abstract: To determine neuronal and glial responses to copper (Cu) elevation in the CNS, human neuroblastoma and astrocytoma cells were used to compare their responses to Cu in terms of reactive oxygen species (ROS) generation and expression of enzymes responsible for anti-oxidation. Astrocytoma cells, not neuroblastoma cells, were responsive to Cu and Cu elevation was associated with ROS generation. Intracellular Cu levels as determined by inductively coupled plasma-mass spectrometry (ICP-MS), and expression levels of copper-transporting ATPase (ATP7A) and human copper transporter 1 (hCtr1) as detected by quantitative reverse transcription–polymerase chain reaction (RT-PCR), were comparable in both cell lines. Differences in Cu-induced ROS between two cell lines paralleled superoxide dismutase (SOD)-catalase expression as detected by Western blot analysis. Copper,zinc-SOD (Cu,Zn-SOD) and catalase protein levels were upregulated by Cu in neuroblastoma cells while Cu,Zn-SOD was down-regulated by Cu and catalase level was not changed in astrocytoma cells. Manganese-SOD (Mn-SOD) was not responsive to Cu in either cell line. Furthermore, 78-kDa glucose-regulated protein aggregation and upregulation were observed in Cu-treated astrocytoma cells, but not neuroblastoma cells. These data suggest that neurons use the SOD-catalase system to scavenge Cu-induced ROS while glia rely on the endoplasmic reticulum stress response to compensate for the reduction of ROS scavenging capacity. [Copyright &y& Elsevier]

Published

2005

8. GRP78 Compartmentalized Redistribution in Pb-treated Glia: Role of GRP78 in Lead-induced Oxidative Stress

Author

Qian, Yongchang, Zheng, Ying, Ramos, Kenneth S., and Tiffany-Castiglioni, Evelyn

Subjects

*OXIDATIVE stress, *GLUCOSE, *PROTEINS, *ASTROCYTOMAS, *BIOMOLECULES

Abstract

Abstract: Glucose-regulated protein of 78kDa (GRP78) is an endoplasmic reticulum (ER) molecular chaperone functioning in protein folding, assembly and trafficking. GRP78 also plays a role in protection against cytotoxicity and apoptosis induced by environmental insults. Our previous study showed that lead (Pb) directly targets GRP78 by binding to the protein and increasing GRP78 levels. In this study, the effect of Pb on compartmentalized distribution of GRP78 in living cells was examined. A rat GRP78–EGFP fusion protein and EGFP were transiently expressed in astrocytoma cells exposed to 5μM Pb acetate or 50μM CuSO4 and fluorescence signals were captured. Control cells expressing EGFP showed a homogeneous distribution of EGFP that was not changed by Pb or Cu treatment. Cells expressing GRP78–EGFP showed a compartmentalized, non-homogeneous distribution of GRP78–EGFP in the cytosol. The redistribution of GRP78–EGFP fluorescent bodies was observed in cells exposed to Pb for 10h, but not 5h. Redistribution was also observed in cells exposed to 50μM Cu for 5 or 10h. To assess GRP78 function, GRP78 was depleted with dsRNAi oligos in rat C6 glioma cells. GRP78 depletion significantly increased the sensitivity of cells to Pb exposure as indicated by the generation of reactive oxygen species (ROS). These data suggest that Pb directly targets GRP78 and induces its compartmentalized redistribution in living cells and that GRP78 plays a protective role in Pb neurotoxicity. [Copyright &y& Elsevier]

Published

2005

9. Functional analysis of a genetic defect of copper transport (Menkes disease) in different cell...

Author

Qian, Yongchang and Tiffany-Castiglioni, Evelyn

Subjects

*COPPER in the body

Abstract

Presents a functional analysis of a genetic defect of copper transport, Menkes disease, in different cell lines. Effects of sulfhydryl reagents on copper accumulation in cultured cells; Kinetics of cellular copper uptake; Reverse transcription-polymerase chain reaction analysis of the Menkes gene transcript.

Published

1996

10. Coincident expression of Menkes gene with copper efflux in human placental cells.

Author

Qian, Yongchang and Majimdar, Sudeep

Subjects

*PLACENTA, *COPPER, *PHYSIOLOGY

Abstract

Studies the coincident expression of Menkes gene with copper efflux in human placental cells. Preparation of a 67Cu-ceruloplasmin complex; Cell culture; Cell polarization; BeWo cells.

Published

1996

11. Copper transport and kinetics in cultured C6 rat glioma cells.

Author

Qian, Yongchang and Tiffany-Castiglioni, Evelyn

Subjects

*COPPER, *GLIOMAS, *PHYSIOLOGY

Abstract

Characterizes the Cu transport system, using rapidly growing C6 rat glioma cells. Cell culture; Kinetics of 67Cu uptake; Time and temperature dependence of Cu uptake; Treatment with transport inhibitors; Treatment with Pb; Measurement of Cu efflux.

Published

1995

12. Functional analysis of a genetic detect of copper transport (Menkes disease) in different cell...

Author

Qian, Yongchang and Tiffany-Castiglioni, Evelyn

Subjects

*ADENOSINE triphosphatase

Abstract

Defines the function of the copper (Cu)-transporting ATPase in Menkes disease by incubating Menkes and normal fibroblasts with 67Cu before and after brief exposure to -SH reagents, p-chloromercuribenzoate and dithiothreitol. Kinetics of 67Cu uptake; Double reciprocal plots of initial rates of Cu uptake.

Published

1996

13. Copper efflux from murine microvascular cells requires expression of the menkes disease Cu-ATPase.

Author

Qian, Yongchang, Tiffany-Castiglioni, Evelyn, Welsh, Jane, Harris, Edward D., Qian, Y, Tiffany-Castiglioni, E, Welsh, J, and Harris, E D

Subjects

*COPPER metabolism, *CEREBRAL circulation

Abstract

Previously, we showed that the transport of Cu by PC12 pheochromocytoma cells and C6 glioma cells correlated with the expression of a Cu-transporting ATPase (Atp7a) that has been linked to Menkes disease. Here, we show that cerebrovascular endothelial (CVE) cells that comprise the blood-brain barrier (BBB) also express the gene for the Cu-ATPase. By using reverse transcription-polymerase chain reaction (RT-PCR) and primers designed from mouse Atp7a cDNA, we amplified a 925-bp and a 760-bp cDNA fragment from two extreme regions of Atp7a mRNA from murine CVE cells; 777 bp of the 925-bp fragment and 677 bp of the 760-bp fragment had a 99.7 and 100% sequence homology, respectively, with mouse Atp7a cDNA. The 777-bp sequences covered the heavy metal binding (Hmb) domain and the 677-bp fragment coded for residues at the -COOH terminus of Atp7a. A functional analysis showed that Cu efflux was blocked by the sulfhydryl reagent p-chloromercuribenzoate (p-CMB), a potential inhibitor of Atp7a function. This study provides strong evidence that a Cu-ATPase in the BBB controls the penetration of Cu into the brain and that lesions to the Cu-ATPase in CVE cells are a primary cause of low brain Cu levels in Menkes disease. [ABSTRACT FROM AUTHOR]

Published

1998

14. Copper handling by astrocytes: Insights into neurodegenerative diseases

Author

Tiffany-Castiglioni, Evelyn, Hong, Sandra, and Qian, Yongchang

Subjects

*NEURODEGENERATION, *COPPER poisoning, *ALZHEIMER'S disease, *ASTROCYTES, *TRACE elements in the body, *GENETIC models

Abstract

Abstract: Copper (Cu) is an essential trace element in the brain that can be toxic at elevated levels. Cu accumulation is a suspected etiology in several neurodegenerative diseases, including Alzheimer''s disease, Parkinson''s disease, and prion-induced disorders. Astrocytes are a proposed depot in the brain for Cu and other metals, including lead (Pb). This article describes the physiological roles of Cu in the central nervous system and in selected neurodegenerative diseases, and reviews evidence that astrocytes accumulate Cu and protect neurons from Cu toxicity. Findings from murine genetic models of Menkes disease and from cell culture models concerning the molecular mechanisms by which astrocytes take up, store, and buffer Cu intracellularly are discussed, as well as potential mechanistic linkages between astrocyte functions in Cu handling and neurodegenerative diseases. [Copyright &y& Elsevier]

Published

2011

15. Effects of propofol on intracellular Ca2+ homeostasis in human astrocytoma cells

Author

Barhoumi, Rola, Burghardt, Robert C., Qian, Yongchang, and Tiffany-Castiglioni, Evelyn

Subjects

*PHYSIOLOGICAL control systems, *NEUROTOXICOLOGY, *HOMEOSTASIS, *SERUM

Abstract

Abstract: The effects of propofol, a short-acting general anesthetic, upon cell growth and Ca2+ signaling in a human astrocytic cell line were examined. Exposure of cells to graded concentrations of propofol resulted in a dose-dependent decrease in cell number with an inhibitory concentration of cell viability (IC50) of 31.7±1.2 μM. To evaluate the changes in intracellular Ca2+ homeostasis induced by propofol, cytoplasmic and mitochondrial Ca2+ were measured by fluorescence imaging. Mitochondrial Ca2+ increased while cytoplasmic Ca2+ decreased significantly at a propofol concentration lower than the IC50 (10 μM for 24 h, 1 μM for 72 h). In addition, propofol diminished the Ca2+ response induced by fetal bovine serum (FBS). To determine the source of Ca2+ alterations induced by propofol, pharmacologic agents targeting intracellular Ca2+ homeostasis mechanisms were used. Nifedipine, an L-type Ca2+ channel blocker, decreased FBS-induced Ca2+ response of control cells to a level similar to propofol treated cells. However, diazoxide (a K+-ATP channel opener) administered 1 h before FBS addition restored the FBS response in propofol treated cells to a level similar to control. In addition, diazoxide increased mitochondrial Ca2+ in control cells to a level comparable to propofol treated cells suggesting activation of these channels by propofol treatment. Addition of 1 μM RU-360 (a selective blocker of the mitochondrial Ca2+ uniporter) for 30 min prior to propofol treatment restored mitochondrial and cytoplasmic Ca2+ to control levels. These data suggest that voltage operated Ca2+ channels, mitochondrial Ca2+ and K+-ATP channels may be targets of propofol action in astrocytes. [Copyright &y& Elsevier]

Published

2007

16. In vitro models for assessing neurotoxicity of mixtures

Author

Tiffany-Castiglioni, Evelyn, Hong, Sandra, Qian, Yongchang, Tang, Yan, and Donnelly, K.C.

Subjects

*TOXICOLOGICAL chemistry, *MIXTURES, *CELL culture, *NEUROTOXICOLOGY, *TOXICOLOGY

Abstract

Abstract: Rapid and inexpensive methods are needed to investigate the interactions of complex mixtures. This commentary addresses the use of cell cultures to detect neurotoxicity of simple binary mixtures, which is a first step in the development of such methods. A small number of recent studies from our laboratory are examined. Though such studies are few, they offer guidance for optimizing the value of cell cultures as systems for chemical toxicity screening and mechanistic research. The same issues that apply to in vitro neurotoxicity studies of single agents also apply to the study of mixtures, such as relevance of endpoints tested, biological usefulness and limitations of cell culture models, and relevance of exposures tested. In this commentary we will focus on several aspects of these issues. [Copyright &y& Elsevier]

Published

2006

17. Genetic Polymorphisms and Mechanisms of Neurotoxicity: Overview

Author

Tiffany-Castiglioni, Evelyn, Venkatraj, Vijayanagaram, and Qian, Yongchang

Published

2005

18. Constructing an Efficient Bacillus subtilis Spore Display by Using Cohesin−Dockerin Interactions.

Author

Wang, He, Jiang, Xiaomin, Qian, Yongchang, Yin, Lianghong, and Fernandez-Lafuente, Roberto

Subjects

*SPORES, *GEOBACILLUS stearothermophilus, *BACILLUS subtilis, *COHESINS, *WESTERN immunoblotting

Abstract

Bacillus subtilis spore display has become a field of increasing interest in the past two decades. To improve the efficiency of B. subtilis spore display, its directed modification was performed based on the cellulosome architecture by introducing onto them divergent cohesin (Coh) modules that can specifically bind to the target enzyme bearing the matching dockerins (Doc). In this study, five different pairs of cohesins and dockerins, selected from four cellulolytic microbes, were examined for their capabilities in displaying a tetrameric enzyme β-galactosidase from Bacillus stearothermophilus IAM11001 on the surface of B. subtilis WB600 spores. Immunofluorescence microscopy, western blotting, dot blotting, and enzyme assay was applied to confirm its surface expression. All the resultant five Coh–Doc based spore display can hydrolyze o-nitrophenyl-β-D-galactopyranoside. Further, the optimized Coh–Doc based spore display exhibited the highest display efficiency. Overall, the results of current study may open new perspectives on the use of Coh–Doc interaction, which will find application in improving the efficiency of B. subtilis spore display. [ABSTRACT FROM AUTHOR]

Published

2021

19. An appropriate ratio of unsaturated fatty acids is the constituent of hickory nut extract for neurite outgrowth in human SH‐SY5Y cells.

Author

Gao, Fei, Wu, Jianfeng, Zhou, Yu, Huang, Jianqin, Lu, Jidong, and Qian, Yongchang

Subjects

*NERVE growth factor, *LINOLEIC acid, *OLEIC acid, *UNSATURATED fatty acids, *LINOLENIC acids, *HICKORIES, *NUTS

Abstract

Hickory nuts (Carya cathayensis Sarg, CCS), a well‐known Chinese medicinal nut, is thought to improve memory in Chinese folks. However, functional constituents have not been scientifically identified. In this study, human SH‐SY5Y cells, combined with Q‐TOF mass spectrometry (Q‐TOF‐MS) and standard substances, were used to evaluate the function in neuronal development and to identify constituents of CCS hydrophobic extracts (CCS‐HE). Data showed that CCS‐HE but not the control induced neurite outgrowth of SH‐SY5Y cells in a dose‐dependent manner, supported by which CCS‐HE induced the expression of nerve growth factor (NGF), neurofilament 160 (NF160), and neuronal peptide Y (NPY) mRNA. Q‐TOF‐MS analysis with standard substances indicated that linolenic acid (LNA), linoleic acid (LA), and oleic acid (OA) were the main constituents in CCS‐HE. Furthermore, mixtures of these unsaturated fatty acids (UFAs) at the natural ratio (1:8:16) significantly induced neurite outgrowth and gene expression of NGF, NF160, and NPY in a dose‐dependent manner. However, the individual and alternative ratios were not effective to induce the neurite outgrowth and gene expression of NGF, NF160, and NPY. These data implicate that an appropriate ratio of UFAs is the main constituent for the neurite outgrowth. [ABSTRACT FROM AUTHOR]

Published

2020

20. Application of composite dissolving microneedles with high drug loading ratio for rapid local anesthesia.

Author

Zhan, Haohui, Ma, Fengsen, Huang, Yingcong, Zhang, Jie, Jiang, Xiayun, and Qian, Yongchang

Subjects

*MEDICAL applications of composite materials, *LOCAL anesthesia, *LIDOCAINE, *NEEDLES & pins, *STAINS & staining (Microscopy), *GUINEA pigs as laboratory animals, *METHYLCELLULOSE

Abstract

We report a type of dissolving microneedles (DMNs) which was made of composite matrix materials of hydroxypropyl methyl cellulose (HPMC) and poly(methylvinylether‑ co ‑maleic anhydride) (PMVE/MA copolymer, Gantrez S-97), and was successfully loaded with lidocaine hydrochloride. The weight of lidocaine hydrochloride loaded in the microneedles tip was 70% of the weight of the whole tip. The content was 3.43 ± 0.12 mg in weight, which was determined by high performance liquid chromatography (HPLC). The results for mechanical test showed that these microneedles were able to penetrate into the skin of the experimental animals, that was proved using organic staining, texture analyzer and histological examination. The fracture force of the microneedles was 5.442 ± 0.412 N, which was much higher than the one required for the skin penetration. The DMNs with lidocaine hydrochloride could be dissolved inside of the rat skin in 5 min. The onset time would be faster (in <5 min) when it was applied to the guinea pig model, in comparing with a commercially available anesthesia cream that had an onset time for 100 min. However, the efficacy of the DMNs for the local anesthesia only lasted for 16 min. It was shorter than that of the commercially available anesthesia cream with which the efficacy could last for about 130 min. After the DMNs was packaged under the vacuum and dark condition, it was stable for 3 months under the condition of a temperature of 40 ± 2 °C and a humidity of 75 ± 5%. The result of the experiment for the safety evaluation showed that the microneedles were non-irritating and non-allergenic to the skin. In conclusion, the DMNs with lidocaine hydrochloride could be safely administered to the skin with a quick onset time for the local anesthesia. [ABSTRACT FROM AUTHOR]

Published

2018

21. Toxicity assessment of complex mixtures remains a goal

Author

Donnelly, Kirby C., Lingenfelter, Rebecca, Cizmas, Leslie, Falahatpisheh, M.H., Qian, Yongchang, Tang, Y., Garcia, Shannon, Ramos, Kenneth, Tiffany-Castiglioni, Evelyn, and Mumtaz, Moiz M.

Subjects

*HYDROCARBONS, *RISK assessment, *HERBICIDES, *CHEMICAL terrorism

Abstract

One of the initial steps in remediating contaminated environments is to assess the human and ecological health risk associated with exposure to contaminants in a specific medium. Presented here are the results of a five-year study investigating the toxicity of simple and complex mixtures. A series of model compounds and simple mixtures including polycyclic aromatic hydrocarbons (PAHs), pentachlorophenol (PCP), and halogenated aliphatic hydrocarbons (HAHs) were analyzed. Mixture toxicity was studied using microbial genotoxicity assays and cytotoxicity assays with renal and neural cells. The majority of binary mixtures described here induced additive responses. A limited number of samples were identified where binary mixtures induced inhibitory effects. For example, benzo(a)pyrene (BAP) alone induced 30% renal cell death, whereas an equimolar dose of chrysene and BAP only produced 1.6% cellular death. In none of the mixtures tested did the mixture toxicity results deviate from the predicted results by an order of magnitude. The results from testing binary mixtures in this study indicate that the results did not deviate significantly from additivity. Complex mixture results were more difficult to interpret. The toxicity of complex mixtures could not be accurately predicted based on chemical analysis. This could be due to chemical interactions or due to the presence of unidentified chemicals, such as alkyl PAHs or high molecular weight PAHs that are not included in the standard risk assessment procedure. Even though the results from these in vitro studies indicate that additive assumptions will generally be appropriate for binary mixtures similar to the ones tested here, the risk associated with complex mixtures remains a challenge to predict. Before the results of toxicity testing can be used to adjust risk assessment calculations, it is important to fully appreciate the chemical composition and to understand the mechanism of observed chemical interactions in animals chronically exposed to low doses of chemical mixtures. This research was supported by ATSDR Grant no. ATU684505 and NIEHS SBRP Grant no. P42 ES04917. [Copyright &y& Elsevier]

Published

2004

22. Identification of angiogenesis-inhibiting peptides from Chan Su.

Author

Xia, Fengyan, Gao, Fei, Yao, Huili, Zhang, Guobing, Gao, Bo, Lu, Ying, Wang, Xiangjun, and Qian, Yongchang

Subjects

*NEOVASCULARIZATION, *RAS oncogenes, *AMINO acid sequence

Abstract

Chan Su is a traditional medicine prepared from toxic secretions from the auricular and skin glands of Chinese toads. Previous studies show that active components in Chan Su can inhibit the proliferation of tumor cells. To study the effect of Chan Su peptides on angiogenesis, fresh Chan Su was collected and its component peptides were isolated by an extraction and precipitation method. A high-performance liquid chromatography (HPLC) fingerprint of the Chan Su component peptides revealed that there were more than 18 peptide component peaks. We demonstrate that Chan Su peptides inhibit angiogenesis in vitro by inhibiting human umbilical vein endothelial cell (HUVEC) proliferation and tube formation in a dose-dependent manner. Western blots indicated that Chan Su peptides inhibited the protein expression of VEGF165 and Ras, leading us to conclude that Chan Su peptide components exert anti-angiogenic effects by suppressing the VEGF165-VEGFR2-Ras signalling pathway. Finally, we identified the partial amino acid sequences of seven Chan Su peptides using the shotgun proteomics method. • Chan Su is a traditional medicine and active components in Chan Su can inhibit the proliferation of tumor cells. • A high-performance liquid chromatography (HPLC) fingerprint of the Chan Su component peptides revealed that there were more than 18 peptide component peaks. • Peptides from Chan Su could inhibit angiogenesis in vitro via regulating the VEGF165-VEGFR2-Ras signalling pathway. • Amino acid sequences of possible anti-angiogenesis peptide from Chan Su have been identified. [ABSTRACT FROM AUTHOR]

Published

2019