Your search keyword '"Siyang Liu"' showing total 16 results

1. Correction: Recombination Pattern Reanalysis of Some HIV-1 Circulating Recombination Forms Suggest the Necessity and Difficulty of Revision.

Author

Lei Jia, Lin Li, Hanping Li, Siyang Liu, Xiaolin Wang, Zuoyi Bao, Tianyi Li, Daomin Zhuang, Yongjian Liu, Jingyun Li, and PLOS ONE Editors

Subjects

Medicine, Science

Abstract

[This corrects the article DOI: 10.1371/journal.pone.0107349.].

Published

2016

2. The Antiviral Activity of Approved and Novel Drugs against HIV-1 Mutations Evaluated under the Consideration of Dose-Response Curve Slope.

Author

Shuai Chang, Daomin Zhuang, Wei Guo, Lin Li, Wenfu Zhang, Siyang Liu, Hanping Li, Yongjian Liu, Zuoyi Bao, Jingwan Han, Hongbin Song, and Jingyun Li

Subjects

Medicine, Science

Abstract

OBJECTIVES:This study was designed to identify common HIV-1 mutation complexes affecting the slope of inhibition curve, and to propose a new parameter incorporating both the IC50 and the slope to evaluate phenotypic resistance. METHODS:Utilizing site-directed mutagenesis, we constructed 22 HIV-1 common mutation complexes. IC50 and slope of 10 representative approved drugs and a novel agent against these mutations were measured to determine the resistance phenotypes. The values of new parameter incorporating both the IC50 and the slope of the inhibition curve were calculated, and the correlations between parameters were assessed. RESULTS:Depending on the class of drug, there were intrinsic differences in how the resistance mutations affected the drug parameters. All of the mutations resulted in large increases in the IC50s of nucleoside reverse transcriptase inhibitors. The effects of the mutations on the slope were the most apparent when examining their effects on the inhibition of non-nucleoside reverse transcriptase inhibitors and protease inhibitors. For example, some mutations, such as V82A, had no effect on IC50, but reduced the slope. We proposed a new concept, termed IIPatoxic, on the basis of IC50, slope and the maximum limiting concentrations of the drug. The IIPatoxic values of 10 approved drugs and 1 novel agent were calculated, and were closely related to the IIPmax values (r > 0.95, p < 0.001). CONCLUSIONS:This study confirms that resistance mutations cannot be accurately assessed by IC50 alone, because it tends to underestimate the degree of resistance. The slope parameter is of very importance in the measurement of drug resistance and the effect can be applied to more complex patterns of resistance. This is the most apparent when testing the effects of the mutations on protease inhibitors activity. We also propose a new index, IIPatoxic, which incorporates both the IC50 and the slope. This new index could complement current IIP indices, thereby enabling predict the efficacy of pre-clinical drugs for which human pharmacokinetic is not available.

Published

2016

3. Development of an HIV-1 Subtype Panel in China: Isolation and Characterization of 30 HIV-1 Primary Strains Circulating in China.

Author

Jingwan Han, Siyang Liu, Wei Guo, Zuoyi Bao, Xiaolin Wang, Lin Li, Yongjian Liu, Daomin Zhuang, Hanping Li, Lei Jia, Tao Gui, Hongshuai Sui, Tianyi Li, and Jingyun Li

Subjects

Medicine, Science

Abstract

The complex epidemic and significant diversity of HIV-1 strains in China pose serious challenges for surveillance and diagnostic assays, vaccine development and clinical management. There is a lack of HIV-1 isolates in current canonical HIV-1 subtype panels that can represent HIV-1 diversity in China; an HIV-1 subtype panel for China is urgently needed.Blood samples were collected from HIV-1 infected patients participating in the drug-resistance surveillance program in China. The samples were isolated, cultured and stored as neat culture supernatant. The HIV-1 isolates were fully characterized. The panel was used to compare 2 viral load assays and 2 p24 assays as the examples of how this panel could be used.An HIV-1 subtype panel for China composed of 30 HIV-1 primary strains of four subtypes (B [including Thai-B], CRF01_AE, CRF07_BC and G) was established. The samples were isolated and cultured to a high-titer (10(6)-10(9) copies/ml)/high-volume (40 ml). The HIV-1 isolates were fully characterized by the final viral load, p24 concentration, gag-pol and envC2V3 sequencing, co-receptor prediction, determination of the four amino acids at the tip of the env V3-loop, glycosylation sites in the V3 loop and the drug-resistance mutations. The comparison of two p24 assays and two viral load assays on the isolates illustrated how this panel may be used for the evaluation of diagnostic assay performance. The Pearson value between p24 assays were 0.938. The viral load results showed excellent concordance and agreement for samples of Thai-B, but lower correlations for samples of CRF01_AE.The current panel of 30 HIV-1 isolates served as a basis for the development of a comprehensive panel of fully characterized viral isolates, which could reflect the current dynamic and complex HIV-1 epidemic in China. This panel will be available to support HIV-1 research, assay evaluation, vaccine and drug development.

Published

2015

4. Recombination pattern reanalysis of some HIV-1 circulating recombination forms suggest the necessity and difficulty of revision.

Author

Lei Jia, Lin Li, Hanping Li, Siyang Liu, Xiaolin Wang, Zuoyi Bao, Tianyi Li, Daomin Zhuang, Yongjian Liu, and Jingyun Li

Subjects

Medicine, Science

Abstract

Recombination is one of the major mechanisms underlying the generation of HIV-1 variability. Currently 61 circulating recombinant forms of HIV-1 have been identified. With the development of recombination detection techniques and accumulation of HIV-1 reference stains, more accurate mosaic structures of circulating recombinant forms (CRFs), like CRF04 and CRF06, have undergone repeated analysis and upgrades. Such revisions may also be necessary for other CRFs. Unlike previous studies, whose results are based primarily on a single recombination detection program, the current study was based on multiple recombination analysis, which may have produced more impartial results.Representative references of 3 categories of intersubtype recombinants were selected, including BC recombinants (CRF07 and CRF08), BG recombinants (CRF23 and CRF24), and BF recombinants (CRF38 and CRF44). They were reanalyzed in detail using both the jumping profile hidden Markov model and RDP3.The results indicate that revisions and upgrades are very necessary and the entire re-analysis suggested 2 types of revision: (i) length of inserted fragments; and (ii) number of inserted fragments. The reanalysis also indicated that determination of small regions of about 200 bases or fewer should be performed with more caution.Results indicated that the involvement of multiple recombination detection programs is very necessary. Additionally, results suggested two major challenges, one involving the difficulty of accurately determining the locations of breakpoints and the second involving identification of small regions of about 200 bases or fewer with greater caution. Both indicate the complexity of HIV-1 recombination. The resolution would depend critically on development of a recombination analysis algorithm, accumulation of HIV-1 stains, and a higher sequencing quality. With the changes in recombination pattern, phylogenetic relationships of some CRFs may also change. All these results may be critical to understand the role of recombination in a complex and dynamic HIV evolution.

Published

2014

5. Prevalence and mutation patterns of HIV drug resistance from 2010 to 2011 among ART-failure individuals in the Yunnan Province, China.

Author

Hanping Li, Min Zhong, Wei Guo, Daomin Zhuang, Lin Li, Yongjian Liu, Zuoyi Bao, Siyang Liu, Xiaolin Wang, Tianyi Li, Shaomin Yang, and Jingyun Li

Subjects

Medicine, Science

Abstract

BackgroundAssessing the prevalence of HIV-1 drug-resistance and the mutation patterns associated with resistance in the geographical regions implementing free antiretroviral therapy (ART) in China is necessary for preventing the spread of resistant strains and designing the regimens for the subsequent therapies with limited resources.MethodsPlasma samples in different cities/prefectures were collected at Yunnan Provincial Hospital of Infectious Disease from January 2010 to December 2011. Genotyping of drug-resistant individuals was conducted using an in-house assay on plasma samples. Viral load, CD4 T cell counts and demographic data were obtained from medical records and an administered questionnaire.ResultsA total of 609 pol sequences (515 ART-failure and 94 therapy-naïve individuals) derived from 664 samples were obtained. The prevalence of drug-resistance was 45.1% in the ART-failure individuals. Of these, 26.8% harbored HIV strains dually resistant to nucleoside reverse transcriptase inhibitors and non-nucleoside reverse transcriptase inhibitors, and 14.8% harbored HIV strains resistant to only one drug category. Mutations such as M184V/I, K103N, V106A, Y181C and G190A were common among the ART-failure individuals, and the frequencies of M184V/I, K103N and V106A were 28.2%, 19.2%, and 22.1%, respectively. The percentages of individuals exhibiting intermediate or high-level resistance to 3TC, FTC, EFV and NVP drugs were 28.4%, 28.2%, 37.3%, and 37.5%, respectively. Factors such as ethnicity, transmission route, CD4 counts, viral load and the duration of ART were significantly correlated with development of drug resistance in the ART-failure individuals.ConclusionsThe high prevalence of HIV drug-resistance observed among the ART-failure individuals from 2010 to 2011 in Yunnan province should be of increasing concern in regions where the implementation of ART is widespread. Education about the risk factors associated with HIV drug resistance is important for preventing and controlling the spread of HIV drug-resistant strains.

Published

2013

6. Altered lipid metabolism in residual white adipose tissues of Bscl2 deficient mice.

Author

Weiqin Chen, Hongyi Zhou, Siyang Liu, Cassie J Fhaner, Bethany C Gross, Todd A Lydic, and Gavin E Reid

Subjects

Medicine, Science

Abstract

Mutations in BSCL2 underlie human congenital generalized lipodystrophy type 2 disease. We previously reported that Bscl2 (-/-) mice develop lipodystrophy of white adipose tissue (WAT) due to unbridled lipolysis. The residual epididymal WAT (EWAT) displays a browning phenotype with much smaller lipid droplets (LD) and higher expression of brown adipose tissue marker proteins. Here we used targeted lipidomics and gene expression profiling to analyze lipid profiles as well as genes involved in lipid metabolism in WAT of wild-type and Bscl2(-/-) mice. Analysis of total saponified fatty acids revealed that the residual EWAT of Bscl2(-/-) mice contained a much higher proportion of oleic 18:1n9 acid concomitant with a lower proportion of palmitic 16:0 acid, as well as increased n3- polyunsaturated fatty acids (PUFA) remodeling. The acyl chains in major species of triacylglyceride (TG) and diacylglyceride (DG) in the residual EWAT of Bscl2(-/-) mice were also enriched with dietary fatty acids. These changes could be reflected by upregulation of several fatty acid elongases and desaturases. Meanwhile, Bscl2(-/-) adipocytes from EWAT had increased gene expression in lipid uptake and TG synthesis but not de novo lipogenesis. Both mitochondria and peroxisomal β-oxidation genes were also markedly increased in Bscl2(-/-) adipocytes, highlighting that these machineries were accelerated to shunt the lipolysis liberated fatty acids through uncoupling to dissipate energy. The residual subcutaneous white adipose tissue (ScWAT) was not browning but displays similar changes in lipid metabolism. Overall, our data emphasize that, other than being essential for adipocyte differentiation, Bscl2 is also important in fatty acid remodeling and energy homeostasis.

Published

2013

7. Recombination form and epidemiology of HIV-1 unique recombinant strains identified in Yunnan, China.

Author

Lin Li, Lili Chen, Shaomin Yang, Tianyi Li, Jianjian Li, Yongjian Liu, Lei Jia, Bihui Yang, Zuoyi Bao, Hanping Li, Xiaolin Wang, Daomin Zhuang, Siyang Liu, and Jingyun Li

Subjects

Medicine, Science

Abstract

Several studies identified HIV-1 recombination in some distinct areas in Yunnan, China. However, no comprehensive studies had been fulfilled in the whole province up to now. To illustrate the epidemiology and recombination form of Unique Recombinant Forms (URFs) circulating in Yunnan, 788 HIV-1 positive individuals residing in 15 prefectures of Yunnan were randomly enrolled into the study. Full-length gag and pol genes were amplified and sequenced. Maximum likelihood tree was constructed for phylogenetic analysis. Recombinant breakpoints and genomic schematics were identified with online software jpHMM. 63 (10.2%) unique recombinant strains were identified from 617 strains with subtypes. The URFs distributed significantly differently among prefectures (Pearson chi-square test, P

Published

2012

8. Screening for and verification of novel mutations associated with drug resistance in the HIV type 1 subtype B(') in China.

Author

Hanping Li, Qingmao Geng, Wei Guo, Daomin Zhuang, Lin Li, Yongjian Liu, Zuoyi Bao, Siyang Liu, and Jingyun Li

Subjects

Medicine, Science

Abstract

OBJECTIVE: Mutations associated with HIV drug resistance have been extensively characterized at the HIV-1 polymerase domain, but more studies have verified that mutations outside of the polymerase domain also results in resistance to antiviral drugs. In this study, mutations were identified in 354 patients experiencing antiretroviral therapy (ART) failure and in 97 naïve-therapy patients. Mutations whose impact on antiviral drugs was unknown were verified by phenotypic testing. METHODS: Pol sequences of HIV subtype B(') obtained from patients experiencing ART failure and from naïve-therapy patients were analyzed for mutations distinct between two groups. Mutations that occurred at a significantly higher frequency in the ART failure than the naïve-therapy group were submitted to the Stanford HIV Drug Resistance Database (SHDB) to analyze the correlation between HIV mutations and drug resistance. For mutations whose impact on the antiviral drug response is unknown, the site-directed mutagenesis approach was applied to construct plasmids containing the screened mutations. 50% inhibitory concentration (IC(50)) to AZT, EFV and NVP was measured to determine the response of the genetically constructed viruses to antiviral drugs. RESULTS: 7 mutations at 6 positions of the RT region, D123E, V292I, K366R, T369A, T369V, A371V and I375V, occurred more frequently in the ART failure group than the naïve-therapy group. Phenotypic characterization of these HIV mutants revealed that constructed viruses with mutations A371V and T369V exhibited dual resistance to AZT and EFV respectively, whereas the other 5 mutations showed weak resistance. Although the impact of the other six mutations on response to NVP was minimal, mutation T369V could enhance resistance to NVP. CONCLUSIONS: This study demonstrated that mutations at the RT C-terminal in subtype B' could result in resistance to RT inhibitors if the mutations occurred alone, but that some mutations could promote susceptibility to antiviral drugs.

Published

2012

9. Genetically dependent ERBB3 expression modulates antigen presenting cell function and type 1 diabetes risk.

Author

Hongjie Wang, Yulan Jin, M V Prasad Linga Reddy, Robert Podolsky, Siyang Liu, Ping Yang, Bruce Bode, John Chip Reed, R Dennis Steed, Stephen W Anderson, Leigh Steed, Diane Hopkins, Yihua Huang, and Jin-Xiong She

Subjects

Medicine, Science

Abstract

Type 1 diabetes (T1D) is an autoimmune disease resulting from the complex interaction between multiple susceptibility genes, environmental factors and the immune system. Over 40 T1D susceptibility regions have been suggested by recent genome-wide association studies; however, the specific genes and their role in the disease remain elusive. The objective of this study is to identify the susceptibility gene(s) in the 12q13 region and investigate the functional link to the disease pathogenesis. A total of 19 SNPs in the 12q13 region were analyzed by the TaqMan assay for 1,434 T1D patients and 1,865 controls. Thirteen of the SNPs are associated with T1D (best p = 4x10(-11)), thus providing confirmatory evidence for at least one susceptibility gene in this region. To identify candidate genes, expression of six genes in the region was analyzed by real-time RT-PCR for PBMCs from 192 T1D patients and 192 controls. SNP genotypes in the 12q13 region are the main factors that determine ERBB3 mRNA levels in PBMCs. The protective genotypes for T1D are associated with higher ERBB3 mRNA level (p

Published

2010

10. Development of an HIV-1 Subtype Panel in China: Isolation and Characterization of 30 HIV-1 Primary Strains Circulating in China

Author

Daomin Zhuang, Tianyi Li, Zuoyi Bao, Tao Gui, Wei Guo, Jingwan Han, Hongshuai Sui, Lei Jia, Jingyun Li, Xiaolin Wang, Lin Li, Yongjian Liu, Siyang Liu, and Hanping Li

Subjects

Male, China, Multidisciplinary, Concordance, lcsh:R, Human immunodeficiency virus (HIV), virus diseases, lcsh:Medicine, HIV Infections, Drug resistance, Viral Load, V3 loop, Biology, medicine.disease_cause, Isolation (microbiology), Virology, HIV-1, medicine, Humans, Female, lcsh:Q, lcsh:Science, Viral load, Phylogeny, Research Article

Abstract

Background The complex epidemic and significant diversity of HIV-1 strains in China pose serious challenges for surveillance and diagnostic assays, vaccine development and clinical management. There is a lack of HIV-1 isolates in current canonical HIV-1 subtype panels that can represent HIV-1 diversity in China; an HIV-1 subtype panel for China is urgently needed. Methods Blood samples were collected from HIV-1 infected patients participating in the drug-resistance surveillance program in China. The samples were isolated, cultured and stored as neat culture supernatant. The HIV-1 isolates were fully characterized. The panel was used to compare 2 viral load assays and 2 p24 assays as the examples of how this panel could be used. Results An HIV-1 subtype panel for China composed of 30 HIV-1 primary strains of four subtypes (B [including Thai-B], CRF01_AE, CRF07_BC and G) was established. The samples were isolated and cultured to a high-titer (106-109 copies/ml)/high-volume (40ml). The HIV-1 isolates were fully characterized by the final viral load, p24 concentration, gag-pol and envC2V3 sequencing, co-receptor prediction, determination of the four amino acids at the tip of the env V3-loop, glycosylation sites in the V3 loop and the drug-resistance mutations. The comparison of two p24 assays and two viral load assays on the isolates illustrated how this panel may be used for the evaluation of diagnostic assay performance. The Pearson value between p24 assays were 0.938. The viral load results showed excellent concordance and agreement for samples of Thai-B, but lower correlations for samples of CRF01_AE. Conclusion The current panel of 30 HIV-1 isolates served as a basis for the development of a comprehensive panel of fully characterized viral isolates, which could reflect the current dynamic and complex HIV-1 epidemic in China. This panel will be available to support HIV-1 research, assay evaluation, vaccine and drug development.

Published

2015

11. Prevalence and mutation patterns of HIV drug resistance from 2010 to 2011 among ART-failure individuals in the Yunnan Province, China

Author

Shaomin Yang, Daomin Zhuang, Xiaolin Wang, Tianyi Li, Min Zhong, Hanping Li, Yongjian Liu, Jingyun Li, Lin Li, Wei Guo, Siyang Liu, and Zuoyi Bao

Subjects

Adult, Male, China, Nevirapine, Efavirenz, Adolescent, Genotype, Anti-HIV Agents, Science, HIV Infections, Drug resistance, Microbial Sensitivity Tests, chemistry.chemical_compound, Young Adult, Acquired immunodeficiency syndrome (AIDS), Risk Factors, Antiretroviral Therapy, Highly Active, Drug Resistance, Viral, medicine, Prevalence, Humans, Treatment Failure, Child, Aged, Multidisciplinary, Geography, business.industry, Lamivudine, virus diseases, Middle Aged, Resistance mutation, medicine.disease, Virology, chemistry, Child, Preschool, Mutation, HIV-1, Medicine, Female, business, Viral load, HIV drug resistance, medicine.drug, Research Article

Abstract

BackgroundAssessing the prevalence of HIV-1 drug-resistance and the mutation patterns associated with resistance in the geographical regions implementing free antiretroviral therapy (ART) in China is necessary for preventing the spread of resistant strains and designing the regimens for the subsequent therapies with limited resources.MethodsPlasma samples in different cities/prefectures were collected at Yunnan Provincial Hospital of Infectious Disease from January 2010 to December 2011. Genotyping of drug-resistant individuals was conducted using an in-house assay on plasma samples. Viral load, CD4 T cell counts and demographic data were obtained from medical records and an administered questionnaire.ResultsA total of 609 pol sequences (515 ART-failure and 94 therapy-naïve individuals) derived from 664 samples were obtained. The prevalence of drug-resistance was 45.1% in the ART-failure individuals. Of these, 26.8% harbored HIV strains dually resistant to nucleoside reverse transcriptase inhibitors and non-nucleoside reverse transcriptase inhibitors, and 14.8% harbored HIV strains resistant to only one drug category. Mutations such as M184V/I, K103N, V106A, Y181C and G190A were common among the ART-failure individuals, and the frequencies of M184V/I, K103N and V106A were 28.2%, 19.2%, and 22.1%, respectively. The percentages of individuals exhibiting intermediate or high-level resistance to 3TC, FTC, EFV and NVP drugs were 28.4%, 28.2%, 37.3%, and 37.5%, respectively. Factors such as ethnicity, transmission route, CD4 counts, viral load and the duration of ART were significantly correlated with development of drug resistance in the ART-failure individuals.ConclusionsThe high prevalence of HIV drug-resistance observed among the ART-failure individuals from 2010 to 2011 in Yunnan province should be of increasing concern in regions where the implementation of ART is widespread. Education about the risk factors associated with HIV drug resistance is important for preventing and controlling the spread of HIV drug-resistant strains.

Published

2012

12. Altered Lipid Metabolism in Residual White Adipose Tissues of Bscl2 Deficient Mice

Author

Cassie J. Fhaner, Siyang Liu, Gavin E. Reid, Weiqin Chen, Bethany C. Gross, Hongyi Zhou, and Todd A. Lydic

Subjects

Male, Mouse, lcsh:Medicine, Gene Expression, Adipose tissue, White adipose tissue, Biochemistry, Mice, chemistry.chemical_compound, 0302 clinical medicine, GTP-Binding Protein gamma Subunits, Adipocyte, Lipid droplet, Molecular Cell Biology, Brown adipose tissue, Adipocytes, Signaling in Cellular Processes, Homeostasis, lcsh:Science, Mice, Knockout, chemistry.chemical_classification, 0303 health sciences, Adipogenesis, Multidisciplinary, Cell Differentiation, Animal Models, Lipids, Heterotrimeric GTP-Binding Proteins, medicine.anatomical_structure, Lipid Signaling, Research Article, Signal Transduction, Polyunsaturated fatty acid, medicine.medical_specialty, Adipose Tissue, White, Lipolysis, 030209 endocrinology & metabolism, Biology, 03 medical and health sciences, Model Organisms, Internal medicine, medicine, Animals, 030304 developmental biology, Gene Expression Profiling, lcsh:R, Fatty acid, Lipid metabolism, Lipid Metabolism, Metabolism, Endocrinology, Gene Expression Regulation, chemistry, lcsh:Q

Abstract

Mutations in BSCL2 underlie human congenital generalized lipodystrophy type 2 disease. We previously reported that Bscl2 (-/-) mice develop lipodystrophy of white adipose tissue (WAT) due to unbridled lipolysis. The residual epididymal WAT (EWAT) displays a browning phenotype with much smaller lipid droplets (LD) and higher expression of brown adipose tissue marker proteins. Here we used targeted lipidomics and gene expression profiling to analyze lipid profiles as well as genes involved in lipid metabolism in WAT of wild-type and Bscl2(-/-) mice. Analysis of total saponified fatty acids revealed that the residual EWAT of Bscl2(-/-) mice contained a much higher proportion of oleic 18:1n9 acid concomitant with a lower proportion of palmitic 16:0 acid, as well as increased n3- polyunsaturated fatty acids (PUFA) remodeling. The acyl chains in major species of triacylglyceride (TG) and diacylglyceride (DG) in the residual EWAT of Bscl2(-/-) mice were also enriched with dietary fatty acids. These changes could be reflected by upregulation of several fatty acid elongases and desaturases. Meanwhile, Bscl2(-/-) adipocytes from EWAT had increased gene expression in lipid uptake and TG synthesis but not de novo lipogenesis. Both mitochondria and peroxisomal β-oxidation genes were also markedly increased in Bscl2(-/-) adipocytes, highlighting that these machineries were accelerated to shunt the lipolysis liberated fatty acids through uncoupling to dissipate energy. The residual subcutaneous white adipose tissue (ScWAT) was not browning but displays similar changes in lipid metabolism. Overall, our data emphasize that, other than being essential for adipocyte differentiation, Bscl2 is also important in fatty acid remodeling and energy homeostasis.

Published

2013

13. Screening for and Verification of Novel Mutations Associated with Drug Resistance in the HIV Type 1subtype B′ in China

Author

Qing-mao Geng, Jingyun Li, Daomin Zhuang, Zuoyi Bao, Siyang Liu, Wei Guo, Lin Li, Yongjian Liu, and Hanping Li

Subjects

Male, Non-Clinical Medicine, Epidemiology, Mutant, lcsh:Medicine, HIV Infections, Drug resistance, medicine.disease_cause, lcsh:Science, Genetics, Mutation, Multidisciplinary, Middle Aged, Antivirals, Phenotype, HIV Reverse Transcriptase, Medicine, Infectious diseases, Female, HIV drug resistance, Research Article, Adult, China, medicine.drug_class, Mechanisms of Resistance and Susceptibility, HIV prevention, Molecular Sequence Data, Retrovirology and HIV immunopathogenesis, Mutagenesis (molecular biology technique), Viral diseases, Biology, Microbiology, Antiviral Agents, Young Adult, Genetic Mutation, Virology, Drug Resistance, Viral, medicine, Humans, Amino Acid Sequence, lcsh:R, Computational Biology, HIV, Reverse transcriptase, HIV-1, lcsh:Q, Antiviral drug

Abstract

OBJECTIVE: Mutations associated with HIV drug resistance have been extensively characterized at the HIV-1 polymerase domain, but more studies have verified that mutations outside of the polymerase domain also results in resistance to antiviral drugs. In this study, mutations were identified in 354 patients experiencing antiretroviral therapy (ART) failure and in 97 naïve-therapy patients. Mutations whose impact on antiviral drugs was unknown were verified by phenotypic testing. METHODS: Pol sequences of HIV subtype B(') obtained from patients experiencing ART failure and from naïve-therapy patients were analyzed for mutations distinct between two groups. Mutations that occurred at a significantly higher frequency in the ART failure than the naïve-therapy group were submitted to the Stanford HIV Drug Resistance Database (SHDB) to analyze the correlation between HIV mutations and drug resistance. For mutations whose impact on the antiviral drug response is unknown, the site-directed mutagenesis approach was applied to construct plasmids containing the screened mutations. 50% inhibitory concentration (IC(50)) to AZT, EFV and NVP was measured to determine the response of the genetically constructed viruses to antiviral drugs. RESULTS: 7 mutations at 6 positions of the RT region, D123E, V292I, K366R, T369A, T369V, A371V and I375V, occurred more frequently in the ART failure group than the naïve-therapy group. Phenotypic characterization of these HIV mutants revealed that constructed viruses with mutations A371V and T369V exhibited dual resistance to AZT and EFV respectively, whereas the other 5 mutations showed weak resistance. Although the impact of the other six mutations on response to NVP was minimal, mutation T369V could enhance resistance to NVP. CONCLUSIONS: This study demonstrated that mutations at the RT C-terminal in subtype B' could result in resistance to RT inhibitors if the mutations occurred alone, but that some mutations could promote susceptibility to antiviral drugs.

Published

2012

14. Recombination Form and Epidemiology of HIV-1 Unique Recombinant Strains Identified in Yunnan, China

Author

Xiaolin Wang, Siyang Liu, Bihui Yang, Yongjian Liu, Daomin Zhuang, Jingyun Li, Tianyi Li, Shaomin Yang, Lili Chen, Lei Jia, Jianjian Li, Lin Li, Hanping Li, and Zuoyi Bao

Subjects

China, medicine.medical_specialty, Epidemiology, Sequence analysis, Population, Sexually Transmitted Diseases, Retrovirology and HIV immunopathogenesis, lcsh:Medicine, Viral diseases, Biology, Infectious Disease Epidemiology, law.invention, law, Phylogenetics, Molecular genetics, medicine, Humans, lcsh:Science, education, Gene, Phylogeny, Genetics, Molecular Epidemiology, education.field_of_study, Multidisciplinary, Population Biology, Phylogenetic tree, lcsh:R, HIV, virus diseases, Virology, Fusion Proteins, gag-pol, AIDS, HIV epidemiology, HIV-1, Recombinant DNA, Medicine, Infectious diseases, lcsh:Q, Recombination, Research Article

Abstract

Several studies identified HIV-1 recombination in some distinct areas in Yunnan, China. However, no comprehensive studies had been fulfilled in the whole province up to now. To illustrate the epidemiology and recombination form of Unique Recombinant Forms (URFs) circulating in Yunnan, 788 HIV-1 positive individuals residing in 15 prefectures of Yunnan were randomly enrolled into the study. Full-length gag and pol genes were amplified and sequenced. Maximum likelihood tree was constructed for phylogenetic analysis. Recombinant breakpoints and genomic schematics were identified with online software jpHMM. 63 (10.2%) unique recombinant strains were identified from 617 strains with subtypes. The URFs distributed significantly differently among prefectures (Pearson chi-square test, P

Published

2012

15. Bisulfite Sequencing Reveals That Aspergillus flavus Holds a Hollow in DNA Methylation

Author

Jian Qing Lin, Jian Guo He, Siyang Liu, Cheng Cheng Wang, Jun Wang, Zhu-Mei He, Hong Long Wu, Yan Feng Luo, Jian Xiang Zhou, Ji Hua Sun, Shu Jing Yan, and Shujia Huang

Subjects

Science, Bisulfite sequencing, Genomics, Biology, Microbiology, DNA methyltransferase, Model Organisms, Genetics, Sulfites, Methylated DNA immunoprecipitation, DNA, Fungal, RNA-Directed DNA Methylation, Epigenomics, Multidisciplinary, Computational Biology, food and beverages, Sequence Analysis, DNA, DNA Methylation, DNA methylation, Medicine, Illumina Methylation Assay, Epigenetics, Research Article, Aspergillus flavus

Abstract

Aspergillus flavus first gained scientific attention for its production of aflatoxin. The underlying regulation of aflatoxin biosynthesis has been serving as a theoretical model for biosynthesis of other microbial secondary metabolites. Nevertheless, for several decades, the DNA methylation status, one of the important epigenomic modifications involved in gene regulation, in A. flavus remains to be controversial. Here, we applied bisulfite sequencing in conjunction with a biological replicate strategy to investigate the DNA methylation profiling of A. flavus genome. Both the bisulfite sequencing data and the methylome comparisons with other fungi confirm that the DNA methylation level of this fungus is negligible. Further investigation into the DNA methyltransferase of Aspergillus uncovers its close relationship with RID-like enzymes as well as its divergence with the methyltransferase of species with validated DNA methylation. The lack of repeat contents of the A. flavus' genome and the high RIP-index of the small amount of remanent repeat potentially support our speculation that DNA methylation may be absent in A. flavus or that it may possess de novo DNA methylation which occurs very transiently during the obscure sexual stage of this fungal species. This work contributes to our understanding on the DNA methylation status of A. flavus, as well as reinforces our views on the DNA methylation in fungal species. In addition, our strategy of applying bisulfite sequencing to DNA methylation detection in species with low DNA methylation may serve as a reference for later scientific investigations in other hypomethylated species.

Published

2012

16. Screening for and Verification of Novel Mutations Associated with Drug Resistance in the HIV Type 1subtype B' in China.

Author

Hanping Li, Qingmao Geng, Wei Guo, Daomin Zhuang, Lin Li, Yongjian Liu, Zuoyi Bao, Siyang Liu, and Jingyun Li

Subjects

DRUG resistance, HIV, ANTIVIRAL agents, HIGHLY active antiretroviral therapy, PHARMACOLOGY, ANTI-infective agents

Abstract

Objective: Mutations associated with HIV drug resistance have been extensively characterized at the HIV-1 polymerase domain, but more studies have verified that mutations outside of the polymerase domain also results in resistance to antiviral drugs. In this study, mutations were identified in 354 patients experiencing antiretroviral therapy (ART) failure and in 97 naïve-therapy patients. Mutations whose impact on antiviral drugs was unknown were verified by phenotypic testing. Methods: Pol sequences of HIV subtype B9 obtained from patients experiencing ART failure and from naïve-therapy patients were analyzed for mutations distinct between two groups. Mutations that occurred at a significantly higher frequency in the ART failure than the naïve-therapy group were submitted to the Stanford HIV Drug Resistance Database (SHDB) to analyze the correlation between HIV mutations and drug resistance. For mutations whose impact on the antiviral drug response is unknown, the site-directed mutagenesis approach was applied to construct plasmids containing the screened mutations. 50% inhibitory concentration (IC50) to AZT, EFV and NVP was measured to determine the response of the genetically constructed viruses to antiviral drugs. Results: 7 mutations at 6 positions of the RT region, D123E, V292I, K366R, T369A, T369V, A371V and I375V, occurred more frequently in the ART failure group than the naïve-therapy group. Phenotypic characterization of these HIV mutants revealed that constructed viruses with mutations A371V and T369V exhibited dual resistance to AZT and EFV respectively, whereas the other 5 mutations showed weak resistance. Although the impact of the other six mutations on response to NVP was minimal, mutation T369V could enhance resistance to NVP. Conclusions: This study demonstrated that mutations at the RT C-terminal in subtype B9 could result in resistance to RT inhibitors if the mutations occurred alone, but that some mutations could promote susceptibility to antiviral drugs. [ABSTRACT FROM AUTHOR]

Published

2012