1.Epidemiologic analysis of 399 patients with organophosphorus pesticide poisoning.
Zhi-Wei SUN ; Xiao-Ling CHEN ; Pei-Fen FANG
Chinese Journal of Industrial Hygiene and Occupational Diseases 2007;25(12):753-754
Adolescent
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Adult
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Aged
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Aged, 80 and over
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Child
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Child, Preschool
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China
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epidemiology
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Female
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Humans
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Male
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Middle Aged
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Organophosphate Poisoning
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Pesticides
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poisoning
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Young Adult
2.Value of Friedman clinical staging systems in management with uvulopalatopharyngoplasty for obstructive sleep apnea hypopnea syndrome.
Pei-Jie HE ; Kuan-Lin XIAO ; Fang-Lu CHI
Chinese Journal of Otorhinolaryngology Head and Neck Surgery 2007;42(2):154-155
Adult
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Female
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Humans
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Male
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Middle Aged
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Palatine Tonsil
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pathology
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Sleep Apnea, Obstructive
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pathology
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surgery
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Tongue
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pathology
3.Phenylethanoid glycosides distribution in medicinal plants of Gesneriaceae.
Zhen-Fang BAI ; Xiao-Qin WANG ; Pei-Gen XIAO ; Yong LIU
China Journal of Chinese Materia Medica 2013;38(24):4267-4270
To investigate the role of distribution and phylogeny of phenylethanoid glycoside in medicinal plants of Gesneriaceae, five phenylpropanoid glycosides, acteoside, paraboside B, isonuomioside A, paraboside II, and paraboside III were quantitatively determined in 12 species of Gesneriaceae by HPLC. The existence and content of these compounds were analyzed. The results showed that phenylethanoid glycosides were found in the most of those plants, but the kind of phenylethanoid glycosides varied in different species. Acteoside distribute in most of this plant group, paraboside B, isonuomioside A, paraboside II, and paraboside III were rare in those plants. The results of this study support morphological viewpoint that Trib. Trichosporeae is more developmental than Trib. Didymocarpeae.
Glucosides
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chemistry
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metabolism
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Magnoliopsida
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metabolism
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Phenylethyl Alcohol
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chemistry
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Plants, Medicinal
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metabolism
4.Investigation on the Use of Essential Medicine System Variety in Children’s Medicines and the Medication in Drug Instructions in Our Hospital
Tieqiao WANG ; Yongqian LIU ; Pei LU ; Dali XIAO ; Rui FANG ; Suiqiong WANG
China Pharmacy 2016;27(24):3334-3336
OBJECTIVE:To provide reference for the safe and rational drug use for children. METHODS:Information manage-ment system was used to investigate the use of essential medicines system variety in stock in 2015 and analyze the medication infor-mation for children in the drug instructionsin our hospital in 2015. RESULTS:Only 201 kinds of medicines belonged to children’s medicines in all the 685 kinds of medicines in our hospital. And 89 kinds (44.28%) of medicines belonged to essential medicine system among the 201 kinds of children’s medicines,in which,78 (87.60%) showed complete medication information for chil-dren;112 kinds(55.72%)of medicines belonged to non-essential medicine system,in which,38(33.93%)showed complete medi-cation information for children. The proportions of showing complete medication information for children in the essential medicines and in its chemicals,biological products,injections and oral preparations were higher than non-essential medicines,the differences were statistically significant(P<0.05). Only 41 kinds of medicines belonged to child-specific medicines among the 201 children’s medicines;62 showed complete medication information for children in the 73 kinds of essential medicines among the non-child-spe-cific medicines;only 13 showed complete medication information for children in the 87 kinds of non-essential medicines,the pro-portion of showing complete medication information for children in essential medicines among the non-child-specific medicines was higher than non-essential medicines,the difference was statistically significant(P<0.05). CONCLUSIONS:The use proportion of essential medicine system variety for children’s medicines is high in our hospital;but there are lacking of child-specific medicines and the medication information for children is insufficient. However,compared with non-essential medicines for children,the essen-tial medicines show better medication information for children in aspects of types,dosage form distribution and non-child-specific medicines,and it is suitable for children.
5.Insulin Autoimmune Syndrome: 73 Cases of Clinical Analysis.
Yun-Lin WANG ; Pei-Wei YAO ; Xiao-Ting ZHANG ; Zhuo-Zhang LUO ; Pei-Qiang WU ; Fang XIAO
Chinese Medical Journal 2015;128(17):2408-2409
Adult
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Aged
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Autoimmune Diseases
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diagnosis
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metabolism
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Female
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Humans
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Insulins
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metabolism
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Male
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Middle Aged
6.Research on application of determination of MMP-13 in osteoarthritis.
Wen-Xiao CHEN ; Fang-Jun SHAN ; Hong-Ting JIN ; Ping-Er WANG ; Lu-Wei XIAO ; Pei-Jian TONG
China Journal of Orthopaedics and Traumatology 2014;27(7):617-620
Osteoarthritis (OA) is a complex chronic progressive disease attacked by biological and mechanical factors and a result from the anabolic and catabolic imbalance in chondrocyte, subchondral bone and extracellular matrix(ECM). Etiology and pathological of OA are not yet entirely clear. The degradation and destruction of collagen II caused by matrix metalloproteinase -13 (MMP-13) is considered the core factor in the occurrence and development of OA. The research of MMP-13 inhibitor provide ideas and methods for the treatment of OA. In this article,the role and determination of MMP-13 in OA and the development prospect of MMP-13 inhibitor in the treatment of OA research progress were reviewed.
Animals
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Collagen
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metabolism
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Humans
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Matrix Metalloproteinase 13
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analysis
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physiology
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Matrix Metalloproteinase Inhibitors
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therapeutic use
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Osteoarthritis
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drug therapy
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etiology
7.The comparison of mfVEP in normal eyes and glaucomatous eyes
Ping-Bao, WANG ; Xiao-Fang, DONG ; Zhao-Hua, XIA ; Qian, TAN ; Xiao-Bo, XIA ; Pei-Gang, HUANG
International Eye Science 2006;6(1):16-18
AIM: To test the ability of multifocal visual evoked potential (mfVEP) in the detecting of glaucoma by comparing the mfVEP recorded from normal subjects and glaucoma patients.METHODS: The mfVEP of 32 normal eyes (n =21) and of 58 eyes (n =37) with primary glaucoma were recorded with the Vision Monitor electrophysical apparatus by the second kernel analysis and to determine the correlation of the topographic location between them.RESULTS: There were significant variability (the coefficient of variation was 43.05%) in mfVEP RMS amplitude in the normal subjects; The RMS amplitude of eyes with glaucoma were smaller than that of the normal eyes and significantly statistical difference were found in the relatively center (namely the 0° -10° ring zone) and in superior nasal quadrant (P<0.05) while there were no significantly statistical differences of the latency time between them.CONCLUSION: The normal subjects have large individual variability of mfVEP responses. The RMS amplitude of the mfVEP of glaucomatous eyes descends, especially in center zone and superior nasal quadrant.
8.MiR-223-3p modulates megakaryocyte polyploidization by targeting MYH10
jing Xiao ZOU ; yi Ming QU ; Fang FANG ; Zeng FAN ; Lin CHEN ; Wen YUE ; yan Xiao XIE ; tao Xue PEI
Military Medical Sciences 2017;41(7):552-559
Objective To investigate the effect of microRNA-223-3p (miR-223-3p) on megakaryocytic differentiation and maturation, and explore the potential mechanism .Methods The endogenous expression of miR-223-3p during megakaryocyte ( MK) differentiation was detected by real-time PCR.Flow cytometry further indicated that alteration of miR-223-3p in human cell lines exerted effects on MK differentiation and maturation .By performing integrative bioinformatic analysis, the potential miR-223-3p target gene, MYH10,was identified.Real-time PCR, luciferase reporter assay and flow cytometry revealed that MYH10 was a direct target of miR-223-3p.Results Endogenous expression of miR-223-3p was in-creased with the differentiation and maturation of MK .The expression of megakaryocytic surface markers CD41 and CD61 and the ploidy were significantly increased in K562 and Meg-01 cells after transfection with miR-223-3p mimics.The expression of MYH10 decreased with the increase in miR-223-3p.Using a luciferase reporter assay ,we demonstrated that MYH10 was a direct target of MiR-223-3p.Furthermore, direct downregulation of MYH10 promoted MK polyploidization . Conclusion MiR-223-3p might regulate the polyploidization of MK by targeting MYH10.
9.Uterine adenomatoid tumors: a clinicopathologic analysis of 25 cases.
Xiao-ling LIU ; Hong-fang CHEN ; Jin-sheng SHI ; Jing-jing WEN ; Pei-jun ZONG
Chinese Journal of Pathology 2013;42(5):336-337
Adenocarcinoma
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pathology
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Adenomatoid Tumor
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metabolism
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pathology
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surgery
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Adenomyoma
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pathology
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Adult
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Antibodies, Monoclonal, Murine-Derived
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metabolism
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Biomarkers, Tumor
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metabolism
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Calbindin 2
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metabolism
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Diagnosis, Differential
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Female
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Follow-Up Studies
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Humans
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Keratins
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metabolism
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Leiomyoma
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pathology
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Lymphatic Vessel Tumors
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metabolism
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pathology
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Middle Aged
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Uterine Neoplasms
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metabolism
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pathology
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surgery
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Young Adult
10.Oligomeric interaction between ryanodine receptors: potential role in Ca(2+) release.
Xiao-Fang HU ; Pei-Hong ZHU ; Jun HU
Acta Physiologica Sinica 2006;58(4):305-308
Receptor proteins in both eukaryotic and prokaryotic cells often form regular lattice or array in the membrane. Recent theoretical analyses indicate that such arrays may provide a novel mechanism for receptor signaling regulation in cells. The functional coupling between neighboring receptors could improve the signaling performance. The ryanodine receptors (RyR)/calcium release channels usually form 2-D regular lattice in the endoplasmic/sarcoplasmic reticulum membranes. Thus, RyR is a potentially good model to study the function of receptor 2-D array. In this article, we briefly review recent progresses in this research field, including RyR-RyR interaction, RyR array's function and working mechanisms. The investigations performed by new methods in our laboratory are summarized. We demonstrate that the RyR-RyR interaction is modulated by the functional states of RyRs. Accordingly, the mechanism of "dynamic coupling" of RyR array is proposed. Its possible role in RyR-mediated Ca(2+) release is discussed.
Animals
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Calcium
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metabolism
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Cations
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Humans
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Muscle, Skeletal
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drug effects
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metabolism
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Receptor Cross-Talk
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physiology
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Ryanodine Receptor Calcium Release Channel
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physiology
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Sarcoplasmic Reticulum
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metabolism