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1. Functional characterization of Trip10 in cancer cell growth and survival

Author

Yan Pearlly S, Chu Pei-Yi, Yeh Kun-Tu, Chen Chien-Min, Sun Wei-Sheng, Hung Yi-Chen, Lai Yen-Ling, Yen Jia-Yi, Kuo Tzen-Yu, Lee Kuan-Der, Tseng Min-Jen, Leu Yu-Wei, Hsu Chia-Chen, Chang Yu-Sun, Huang Tim H-M, and Hsiao Shu-Huei

Subjects
Medicine
Abstract

Abstract Background The Cdc42-interacting protein-4, Trip10 (also known as CIP4), is a multi-domain adaptor protein involved in diverse cellular processes, which functions in a tissue-specific and cell lineage-specific manner. We previously found that Trip10 is highly expressed in estrogen receptor-expressing (ER+) breast cancer cells. Estrogen receptor depletion reduced Trip10 expression by progressively increasing DNA methylation. We hypothesized that Trip10 functions as a tumor suppressor and may be involved in the malignancy of ER-negative (ER-) breast cancer. To test this hypothesis and evaluate whether Trip10 is epigenetically regulated by DNA methylation in other cancers, we evaluated DNA methylation of Trip10 in liver cancer, brain tumor, ovarian cancer, and breast cancer. Methods We applied methylation-specific polymerase chain reaction and bisulfite sequencing to determine the DNA methylation of Trip10 in various cancer cell lines and tumor specimens. We also overexpressed Trip10 to observe its effect on colony formation and in vivo tumorigenesis. Results We found that Trip10 is hypermethylated in brain tumor and breast cancer, but hypomethylated in liver cancer. Overexpressed Trip10 was associated with endogenous Cdc42 and huntingtin in IMR-32 brain tumor cells and CP70 ovarian cancer cells. However, overexpression of Trip10 promoted colony formation in IMR-32 cells and tumorigenesis in mice inoculated with IMR-32 cells, whereas overexpressed Trip10 substantially suppressed colony formation in CP70 cells and tumorigenesis in mice inoculated with CP70 cells. Conclusions Trip10 regulates cancer cell growth and death in a cancer type-specific manner. Differential DNA methylation of Trip10 can either promote cell survival or cell death in a cell type-dependent manner.

Published
2011
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2. A role of ygfZ in the Escherichia coli response to plumbagin challenge

Author

Chen Tai-Hung, Chen Jenn-Wei, Sun Wei-Sheng W, Syu Wan-Jr, Lin Ching-Nan, Don Ming-Jaw, and Wang Shao-Hung

Subjects
Medicine
Abstract

Abstract Plumbagin is found in many herbal plants and inhibits the growth of various bacteria. Escherichia coli strains are relatively resistant to this drug. The mechanism of resistance is not clear. Previous findings showed that plumbagin treatment triggered up-regulation of many genes in E. coli including ahpC, mdaB, nfnB, nfo, sodA, yggX and ygfZ. By analyzing minimal inhibition concentration and inhibition zones of plumbagin in various gene-disruption mutants, ygfZ and sodA were found critical for the bacteria to resist plumbagin toxicity. We also found that the roles of YgfZ and SodA in detoxifying plumbagin are independent of each other. This is because of the fact that ectopically expressed SodA reduced the superoxide stress but not restore the resistance of bacteria when encountering plumbagin at the absence of ygfZ. On the other hand, an ectopically expressed YgfZ was unable to complement and failed to rescue the plumbagin resistance when sodA was perturbed. Furthermore, mutagenesis analysis showed that residue Cys228 within YgfZ fingerprint region was critical for the resistance of E. coli to plumbagin. By solvent extraction and HPLC analysis to follow the fate of the chemical, it was found that plumbagin vanished apparently from the culture of YgfZ-expressing E. coli. A less toxic form, methylated plumbagin, which may represent one of the YgfZ-dependent metabolites, was found in the culture supernatant of the wild type E. coli but not in the ΔygfZ mutant. Our results showed that the presence of ygfZ is not only critical for the E coli resistance to plumbagin but also facilitates the plumbagin degradation.

Published
2010
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4. PrgE: an OB-fold protein from plasmid pCF10 with striking differences to prototypical bacterial SSBs

Author

Breidenstein, Annika, Lamy, Anaïs, Bader P.J., Cyrielle, Sun, Wei-Sheng, Wanrooij, Paulina H., Berntsson, Ronnie P.-A., Breidenstein, Annika, Lamy, Anaïs, Bader P.J., Cyrielle, Sun, Wei-Sheng, Wanrooij, Paulina H., and Berntsson, Ronnie P.-A.

Abstract

A major pathway for horizontal gene transfer is the transmission of DNA from donor to recipient cells via plasmid-encoded type IV secretion systems (T4SSs). Many conjugative plasmids encode for a single-stranded DNA-binding protein (SSB) together with their T4SS. Some of these SSBs have been suggested to aid in establishing the plasmid in the recipient cell, but for many, their function remains unclear. Here, we characterize PrgE, a proposed SSB from the Enterococcus faecalis plasmid pCF10. We show that PrgE is not essential for conjugation. Structurally, it has the characteristic OB-fold of SSBs, but it has very unusual DNA-binding properties. Our DNA-bound structure shows that PrgE binds ssDNA like beads on a string supported by its N-terminal tail. In vitro studies highlight the plasticity of PrgE oligomerization and confirm the importance of the N-terminus. Unlike other SSBs, PrgE binds both double- and single-stranded DNA equally well. This shows that PrgE has a quaternary assembly and DNA-binding properties that are very different from the prototypical bacterial SSB, but also different from eukaryotic SSBs.

Published
2024
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5. Breaking barriers : pCF10 type 4 secretion system relies on a self-regulating muramidase to modulate the cell wall

Author

Sun, Wei-Sheng, Torrens, Gabriel, ter Beek, Josy, Cava, Felipe, Berntsson, Ronnie P.-A., Sun, Wei-Sheng, Torrens, Gabriel, ter Beek, Josy, Cava, Felipe, and Berntsson, Ronnie P.-A.

Abstract

Conjugative type 4 secretion systems (T4SSs) are the main driver for the spread of antibiotic resistance genes and virulence factors in bacteria. To deliver the DNA substrate to recipient cells, it must cross the cell envelopes of both donor and recipient bacteria. In the T4SS from the enterococcal conjugative plasmid pCF10, PrgK is known to be the active cell wall degrading enzyme. It has three predicted extracellular hydrolase domains: metallo-peptidase (LytM), soluble lytic transglycosylase (SLT), and cysteine, histidine-dependent amidohydrolases/peptidases (CHAP). Here, we report the structure of the LytM domain and show that its active site is degenerate and lacks the active site metal. Furthermore, we show that only the predicted SLT domain is functional in vitro and that it unexpectedly has a muramidase instead of a lytic transglycosylase activity. While we did not observe any peptidoglycan hydrolytic activity for the LytM or CHAP domain, we found that these domains downregulated the SLT muramidase activity. The CHAP domain was also found to be involved in PrgK dimer formation. Furthermore, we show that PrgK interacts with PrgL, which likely targets PrgK to the rest of the T4SS. The presented data provides important information for understanding the function of Gram-positive T4SSs. IMPORTANCE: Antibiotic resistance is a large threat to human health and is getting more prevalent. One of the major contributors to the spread of antibiotic resistance among different bacteria is type 4 secretion systems (T4SS). However, mainly T4SSs from Gram-negative bacteria have been studied in detail. T4SSs from Gram-positive bacteria, which stand for more than half of all hospital-acquired infections, are much less understood. The significance of our research is in identifying the function and regulation of a cell wall hydrolase, a key component of the pCF10 T4SS from Enterococcus faecalis. This system is one of the best-studied Gram-positive T4SSs, and this added knowledge a

Published
2024
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9. Structural foundation for the role of enterococcal PrgB in conjugation, biofilm formation, and virulence

Author

Sun, Wei-Sheng, Lassinantti, Lena, Järvå, Michael A., Schmitt, Andreas, ter Beek, Josy, Berntsson, Ronnie, Sun, Wei-Sheng, Lassinantti, Lena, Järvå, Michael A., Schmitt, Andreas, ter Beek, Josy, and Berntsson, Ronnie

Abstract

Type 4 Secretion Systems are a main driver for the spread of antibiotic resistance genes and virulence factors in bacteria. In Gram-positives, these secretion systems often rely on surface adhesins to enhance cellular aggregation and mating-pair formation. One of the best studied adhesins is PrgB from the conjugative plasmid pCF10 of Enterococcus faecalis, which has been shown to play major roles in conjugation, biofilm formation, and importantly also in bacterial virulence. Since prgB orthologs exist on a large number of conjugative plasmids in various different species, this makes PrgB a model protein for this widespread virulence factor. After characterizing the polymer adhesin domain of PrgB previously, we here report the structure for almost the entire remainder of PrgB, which reveals that PrgB contains four immunoglobulin (Ig)-like domains. Based on this new insight, we re-evaluate previously studied variants and present new in vivo data where specific domains or conserved residues have been removed. For the first time, we can show a decoupling of cellular aggregation from biofilm formation and conjugation in prgB mutant phenotypes. Based on the presented data, we propose a new functional model to explain how PrgB mediates its different functions. We hypothesize that the Ig-like domains act as a rigid stalk that presents the polymer adhesin domain at the right distance from the cell wall.

Published
2023
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13. Structure of the enterococcal T4SS protein PrgL reveals unique dimerization interface in the VirB8 protein family

Author

Jäger, Franziska, Lamy, Anaïs, Sun, Wei-Sheng, Guerini, Nina, Berntsson, Ronnie, Jäger, Franziska, Lamy, Anaïs, Sun, Wei-Sheng, Guerini, Nina, and Berntsson, Ronnie

Abstract

Multidrug-resistant bacteria pose serious problems in hospital-acquired infections (HAIs). Most antibiotic resistance genes are acquired via conjugative gene transfer, mediated by type 4 secretion systems (T4SS). Although most multidrug-resistant bacteria responsible for HAIs are of Gram-positive origin, with enterococci being major contributors, mostly Gram-negative T4SSs have been characterized. Here, we describe the structure and organization of PrgL, a core protein of the T4SS channel, encoded by the pCF10 plasmid from Enterococcus faecalis. The structure of PrgL displays similarity to VirB8 proteins of Gram-negative T4SSs. In vitro experiments show that the soluble domain alone is enough to drive both dimerization and dodecamerization, with a dimerization interface that differs from all other known VirB8-like proteins. In vivo experiments verify the importance of PrgL dimerization. Our findings provide insight into the molecular building blocks of Gram-positive T4SS, highlighting similarities but also unique features in PrgL compared to other VirB8-like proteins.

Published
2022
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15. Enterococcal PrgA Extends Far Outside the Cell and Provides Surface Exclusion to Protect against Unwanted Conjugation

Author

Schmitt, Andreas, Hirt, Helmut, Järvå, Michael A., Sun, Wei-Sheng, ter Beek, Josy, Dunny, Gary M., Berntsson, Ronnie Per-Arne, Schmitt, Andreas, Hirt, Helmut, Järvå, Michael A., Sun, Wei-Sheng, ter Beek, Josy, Dunny, Gary M., and Berntsson, Ronnie Per-Arne

Abstract

Horizontal gene transfer between Gram-positive bacteria leads to a rapid spread of virulence factors and antibiotic resistance. This transfer is often facilitated via type 4 secretion systems (T4SS), which frequently are encoded on conjugative plasmids. However, donor cells that already contain a particular conjugative plasmid resist acquisition of a second copy of said plasmid. They utilize different mechanisms, including surface exclusion for this purpose. Enterococcus faecalis PrgA, encoded by the conjugative plasmid pCF10, is a surface protein that has been implicated to play a role in both virulence and surface exclusion, but the mechanism by which this is achieved has not been fully explained. Here, we report the structure of full-length PrgA, which shows that PrgA protrudes far out from the cell wall (approximately 40 nm), where it presents a protease domain. In vivo experiments show that PrgA provides a physical barrier to cellular adhesion, thereby reducing cellular aggregation. This function of PrgA contributes to surface exclusion, reducing the uptake of its cognate plasmid by approximately one order of magnitude. Using variants of PrgA with mutations in the catalytic site we show that the surface exclusion effect is dependent on the activity of the protease domain of PrgA. In silico analysis suggests that PrgA can interact with another enterococcal adhesin, PrgB, and that these two proteins have co-evolved. PrgB is a strong virulence factor, and PrgA is involved in post-translational processing of PrgB. Finally, competition mating experiments show that PrgA provides a significant fitness advantage to plasmid-carrying cells.

Published
2020
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23. Functional characterization of Trip10 in cancer cell growth and survival

Author

Hsu, Chia-Chen, primary, Leu, Yu-Wei, additional, Tseng, Min-Jen, additional, Lee, Kuan-Der, additional, Kuo, Tzen-Yu, additional, Yen, Jia-Yi, additional, Lai, Yen-Ling, additional, Hung, Yi-Chen, additional, Sun, Wei-Sheng, additional, Chen, Chien-Min, additional, Chu, Pei-Yi, additional, Yeh, Kun-Tu, additional, Yan, Pearlly S, additional, Chang, Yu-Sun, additional, Huang, Tim H-M, additional, and Hsiao, Shu-Huei, additional

Published
2011
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26. DNA methylation of the Trip10 promoter accelerates mesenchymal stem cell lineage determination

Author

Hsiao, Shu-Huei, primary, Lee, Kuan-Der, additional, Hsu, Chia-Chen, additional, Tseng, Min-Jen, additional, Jin, Victor X., additional, Sun, Wei-Sheng, additional, Hung, Yi-Chen, additional, Yeh, Kun-Tu, additional, Yan, Pearlly S., additional, Lai, Yen-Yu, additional, Sun, H. Sunny, additional, Lu, Yen-Jung, additional, Chang, Yu-Sun, additional, Tsai, Shaw-Jenq, additional, Huang, Tim H.-M., additional, and Leu, Yu-Wei, additional

Published
2010
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27. Macrobenthic community structure and bioassessment for water quality of Banqiao Reservoir in Huaihe River basin.

Author

SUN Wei-sheng, GU Qian-hong, DONG Jing, CHENG Qing-qing, LI Xue-jun, and ZHANG Man

Abstract

In order to demonstrate macrobenthic community structure dynamics and conduct a biological evaluation of water quality in Banqiao Reservoir, we collected seasonal samples from January to November 2014 across 15 sampling sites. A total of 17 species belonging to five families, four classes, and 3 phyla were identified, including 8 chironomidae, 4 oligochaeta and 5 mollusc. Bellamya aeruginosa, Corbicula fluminea, Branchiura sowerbyi, Pelopia sp. and Glyptotendipes sp. were the important species in Banqiao Reservoir. The total density, biomass and biodiversity of macrobenthos showed significant spatial and temporal differences. ANOSIM analysis indicated that the macrobenthic community structure also differed significantly among regions and seasons, and the main contributing species were Glyptotendipes sp., Pelopia sp. and B. sowerbyi. The abundance-biomass comparison curves (ABC curves) indicated that the current macrobenthic community in Banqiao Reservoir was stable. Combined with the biodiversity index, biological pollution index (BPI) and Hilsenhoff biotic index (BI), it was suggested that Banqiao Reservoir suffered slight pollution. [ABSTRACT FROM AUTHOR]

Published
2015

28. Protein Interactions and Regulation of EscA in Enterohemorrhagic E. coli.

Author

Lin, Ching-Nan, Sun, Wei-Sheng W., Lu, Hui-Yin, Ng, Swee-Chuan, Liao, Ying-Shu, and Syu, Wan-Jr

Subjects
*PROTEIN-protein interactions, *ESCHERICHIA coli diseases, *DIARRHEA, *ABDOMINAL pain, *HEMOLYTIC-uremic syndrome, *PROTEIN stability, *PROTEIN synthesis
Abstract

Infections caused by enterohemorrhagic Escherichia coli (EHEC) can lead to diarrhea with abdominal cramps and sometimes are complicated by severe hemolytic uremic syndrome. EHEC secretes effector proteins into host cells through a type III secretion system that is composed of proteins encoded by a chromosomal island, locus for the enterocyte effacement (LEE). EspA is the major component of the filamentous structure connecting the bacteria and the host's cells. Synthesis and secretion of EspA must be carefully controlled since the protein is prone to polymerize. CesAB, CesA2, and EscL have been identified as being able to interact with EspA. Furthermore, the intracellular level of EspA declines when cesAB, cesA2, and escL are individually deleted. Here, we report a LEE gene named l0033, which also affects the intracellular level of EspA. We renamed l0033 as escA since its counterpart in enteropathogenic E. coli has been recently described. Similar to CesAB, EscL, and CesA2, EscA interacts with EspA and enhances the protein stability of EspA. However, EscA is also able to interact with inner membrane-associated EscL, CesA2, and EscN, but not with cytoplasmic CesAB. In terms of gene organizations, escA locates in LEE3. Expression of EscA is faithfully regulated via Mpc, the first gene product of LEE3. Since Mpc is tightly regulated to low level, we suggest that EscA is highly synchronized and critical to the process of escorting EspA to its final destination. [ABSTRACT FROM AUTHOR]

Published
2014
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29. Protein Interactions and Regulation of EscA in Enterohemorrhagic E. coli.

Author

Lin, Ching-Nan, Sun, Wei-Sheng W., Lu, Hui-Yin, Ng, Swee-Chuan, Liao, Ying-Shu, and Syu, Wan-Jr

Subjects
PROTEIN-protein interactions, ESCHERICHIA coli diseases, DIARRHEA, ABDOMINAL pain, HEMOLYTIC-uremic syndrome, PROTEIN stability, PROTEIN synthesis
Abstract

Infections caused by enterohemorrhagic Escherichia coli (EHEC) can lead to diarrhea with abdominal cramps and sometimes are complicated by severe hemolytic uremic syndrome. EHEC secretes effector proteins into host cells through a type III secretion system that is composed of proteins encoded by a chromosomal island, locus for the enterocyte effacement (LEE). EspA is the major component of the filamentous structure connecting the bacteria and the host's cells. Synthesis and secretion of EspA must be carefully controlled since the protein is prone to polymerize. CesAB, CesA2, and EscL have been identified as being able to interact with EspA. Furthermore, the intracellular level of EspA declines when cesAB, cesA2, and escL are individually deleted. Here, we report a LEE gene named l0033, which also affects the intracellular level of EspA. We renamed l0033 as escA since its counterpart in enteropathogenic E. coli has been recently described. Similar to CesAB, EscL, and CesA2, EscA interacts with EspA and enhances the protein stability of EspA. However, EscA is also able to interact with inner membrane-associated EscL, CesA2, and EscN, but not with cytoplasmic CesAB. In terms of gene organizations, escA locates in LEE3. Expression of EscA is faithfully regulated via Mpc, the first gene product of LEE3. Since Mpc is tightly regulated to low level, we suggest that EscA is highly synchronized and critical to the process of escorting EspA to its final destination. [ABSTRACT FROM AUTHOR]

Published
2014
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30. A role of ygfZ in the Escherichia coli response to plumbagin challenge.

Author

Ching-Nan Lin, Wan-Jr Syu, Sun, Wei-Sheng W., Jenn-Wei Chen, Tai-Hung Chen, Ming-Jaw Don, and Shao-Hung Wang

Subjects
METABOLIC detoxification, PLANT metabolites, PLUMBAGINALES, ANTIBACTERIAL agents, ESCHERICHIA coli
Abstract

Plumbagin is found in many herbal plants and inhibits the growth of various bacteria. Escherichia coli strains are relatively resistant to this drug. The mechanism of resistance is not clear. Previous findings showed that plumbagin treatment triggered up-regulation of many genes in E. coli including ahpC, mdaB, nfnB, nfo, sodA, yggX and ygfZ. By analyzing minimal inhibition concentration and inhibition zones of plumbagin in various gene-disruption mutants, ygfZ and sodA were found critical for the bacteria to resist plumbagin toxicity. We also found that the roles of YgfZ and SodA in detoxifying plumbagin are independent of each other. This is because of the fact that ectopically expressed SodA reduced the superoxide stress but not restore the resistance of bacteria when encountering plumbagin at the absence of ygfZ. On the other hand, an ectopically expressed YgfZ was unable to complement and failed to rescue the plumbagin resistance when sodA was perturbed. Furthermore, mutagenesis analysis showed that residue Cys228 within YgfZ fingerprint region was critical for the resistance of E. coli to plumbagin. By solvent extraction and HPLC analysis to follow the fate of the chemical, it was found that plumbagin vanished apparently from the culture of YgfZ-expressing E. coli. A less toxic form, methylated plumbagin, which may represent one of the YgfZ-dependent metabolites, was found in the culture supernatant of the wild type E. coli but not in the ΔygfZ mutant. Our results showed that the presence of ygfZ is not only critical for the E coli resistance to plumbagin but also facilitates the plumbagin degradation. [ABSTRACT FROM AUTHOR]

Published
2010
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33. Breaking barriers: pCF10 type 4 secretion system relies on a self-regulating muramidase to modulate the cell wall.

Author

Sun W-S, Torrens G, Ter Beek J, Cava F, and Berntsson RP-A

Subjects
Plasmids genetics, Bacterial Proteins metabolism, Bacterial Proteins genetics, Conjugation, Genetic, Catalytic Domain, Cell Wall metabolism, Type IV Secretion Systems metabolism, Type IV Secretion Systems genetics, Enterococcus faecalis genetics, Enterococcus faecalis enzymology, Enterococcus faecalis metabolism, Muramidase metabolism, Muramidase genetics
Abstract

Conjugative type 4 secretion systems (T4SSs) are the main driver for the spread of antibiotic resistance genes and virulence factors in bacteria. To deliver the DNA substrate to recipient cells, it must cross the cell envelopes of both donor and recipient bacteria. In the T4SS from the enterococcal conjugative plasmid pCF10, PrgK is known to be the active cell wall degrading enzyme. It has three predicted extracellular hydrolase domains: metallo-peptidase (LytM), soluble lytic transglycosylase (SLT), and cysteine, histidine-dependent amidohydrolases/peptidases (CHAP). Here, we report the structure of the LytM domain and show that its active site is degenerate and lacks the active site metal. Furthermore, we show that only the predicted SLT domain is functional in vitro and that it unexpectedly has a muramidase instead of a lytic transglycosylase activity. While we did not observe any peptidoglycan hydrolytic activity for the LytM or CHAP domain, we found that these domains downregulated the SLT muramidase activity. The CHAP domain was also found to be involved in PrgK dimer formation. Furthermore, we show that PrgK interacts with PrgL, which likely targets PrgK to the rest of the T4SS. The presented data provides important information for understanding the function of Gram-positive T4SSs.IMPORTANCEAntibiotic resistance is a large threat to human health and is getting more prevalent. One of the major contributors to the spread of antibiotic resistance among different bacteria is type 4 secretion systems (T4SS). However, mainly T4SSs from Gram-negative bacteria have been studied in detail. T4SSs from Gram-positive bacteria, which stand for more than half of all hospital-acquired infections, are much less understood. The significance of our research is in identifying the function and regulation of a cell wall hydrolase, a key component of the pCF10 T4SS from Enterococcus faecalis . This system is one of the best-studied Gram-positive T4SSs, and this added knowledge aids in our understanding of horizontal gene transfer in E. faecalis as well as other medically relevant Gram-positive bacteria., Competing Interests: The authors declare no conflict of interest.

Published
2024
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34. [Macrobenthic community structure and bioassessment for water quality of Banqiao Reservoir in Huaihe River basin].

Author

Sun WS, Gu QH, Dong J, Cheng QQ, Li XJ, and Zhang M

Subjects
Animals, Biodiversity, Biomass, China, Chironomidae, Ecosystem, Gastropoda, Mollusca, Oligochaeta, Seasons, Biota, Environmental Monitoring, Rivers, Water Quality
Abstract

In order to demonstrate macrobenthic community structure dynamics and conduct a biological evaluation of water quality in Banqiao Reservoir, we collected seasonal samples from January to November 2014 across 15 sampling sites. A total of 17 species belonging to five families, four classes, and 3 phyla were identified, including 8 chironomidae, 4 oligochaeta and 5 mollusc. Bellamya aeruginosa, Corbicula fluminea, Branchiura sowerbyi, Pelopia sp. and Glyptotendipes sp. were the important species in Banqiao Reservoir. The total density, biomass and biodiversity of marobenthos showed significant spatial and temporal differences. ANOSIM analysis indicated that the macrobenthic community structure also differed significantly among regions and seasons, and the main contributing species were Glyptotendipes sp., Pelopia sp. and B. sowerbyi. The abundance-biomass comparison curves (ABC curves) indicated that the current macrobenthic community in Banqiao Reservoir was stable. Combined with the biodiversity index, biological pollution index (BPI) and Hilsenhoff biotic index (BI), it was suggested that Banqiao Reservoir suffered slight pollution.

Published
2015

35. [Long distance-PCR for detection of factor VIII gene inversion in patients with severe hemophilia A].

Author

Ding PF, Sun WS, Wang QY, Liu DC, Zhang XQ, Teng B, and Shen FK

Subjects
Adolescent, Adult, Antigens analysis, Child, Child, Preschool, Hemophilia A blood, Humans, Infant, Male, von Willebrand Factor immunology, Chromosome Inversion, Factor VIII genetics, Hemophilia A genetics, Polymerase Chain Reaction methods
Abstract

The aim of current study was to detect intron 22 inversion of factor VIII gene in severe hemophilia A (HA) patients and screen the carriers of the gene inversion. Fifty-five cases of severe HA were involved and factor VIII gene inversion was detected and identified by long distance-PCR (LD-PCR) and 0.6% agarose gel electrophoresis. The 11 kb and 12 kb bands indicate the factor VIII gene inversion and non-inversion, respectively. Occurring of both 11 kb and 12 kb bands indicates a carrier of the inversion. The results showed that factor VIII gene inversion existed in 22 out of 55 cases, which accounted for about 40% of total detected patients. Five carriers of factor VIII gene inversion were diagnosed from the members in 15 families. In conclusion, LD-PCR assay is a simple, rapid and accurate method for detection of factor VIII gene inversion, and this approach is helpful in screening, carrier testing, and prenatal diagnosis of severe hemophilia A.

Published
2003

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