Your search keyword '"Liu, Haican"' showing total 25 results

1. Polymorphisms of human T cell epitopes of Mycobacterium tuberculosis indicate divergence of host immune pressure on different categories of proteins.

Author

Jiang, Yi, Liu, Haican, Dou, Xiangfeng, Zhao, Xiuqin, Li, Machao, Li, Guilian, Bai, Yun, Zhang, Wen, Lian, Lulu, Yu, Qin, Zhang, Jingrui, and Wan, Kanglin

Subjects

*GENETIC polymorphisms, *T cells, *EPITOPES, *MYCOBACTERIUM tuberculosis, *IMMUNE response

Abstract

Abstract Mycobacterium tuberculosis is the most successful pathogen with multiple mechanisms to subvert host immune response, resulting in insidious disease. There are few studies on whether the bacteria undergo antigenic variation in response to host immune pressure. Studies on T cell epitopes of M. tuberculosis can help us further understand the mechanism of interaction between the bacteria and host immune system. Here, we selected 180 M. tuberculosis complex in China, amplified 462 experimentally verified human T cell epitopes, sequenced and compared the results to analyze the diversity of those epitopes. It proved that a large majority human T cell epitopes of M. tuberculosis are conserved. However, polymorphisms of T cell epitopes indicated different categories of proteins suffered divergence from host immune pressure. Moreover, Beijing strains are more conservative than non-Beijing strains in T cell epitopes, which might make them easier to transmit than non-Beijing strains. [ABSTRACT FROM AUTHOR]

Published

2018

2. IncA/C plasmids conferring high azithromycin resistance in vibrio cholerae.

Author

Wang, Ruibai, Liu, Haican, Zhao, Xiuqin, Li, Jie, and Wan, Kanglin

Subjects

*AZITHROMYCIN, *VIBRIO cholerae, *CHOLERA treatment, *ERYTHROMYCIN, *ANTIBIOTICS

Abstract

Azithromycin (AZM) is a clinically important antibiotic against Vibrio cholerae , especially for inhibiting V. cholerae colonisation of the intestine and for the treatment of severe cholera in children and pregnant women. An IncA/C plasmid was isolated from two high minimum inhibitory concentration (MIC) AZM-resistant V. cholerae strains of the two mainly pathogenic serogroups (O1 and O139) isolated in China. In the 172 predicted open reading frames (ORFs), 16 genes were related to antibiotic resistance, of which 5 were well-defined genes associated with macrolide resistance. The five macrolide resistance genes distributed in two clusters, mphR–mrx–mph (K) and mel–mph2 , flanked by insertion sequence elements and involving two kinds of resistance mechanism. Deletion of the complete region of the two clusters deceased the AZM MIC from ≥64 µg/mL to ≤0.5 µg/mL. This IncA/C plasmid shows great ability to accumulate antibiotic resistance genes. In addition to 11 resistance genes to other antibiotics, 5 macrolide resistance genes with different function were gathered repeatedly through transposition on one plasmid. This genotype could not be simply explained by antibiotic stress applied on the host from the environment or treatment. These phosphorylases and transmembrane transporters might be involved in the transport and metabolism of other non-antibiotic substances, enabling this kind of plasmid to propagate better in the host. [ABSTRACT FROM AUTHOR]

Published

2018

3. Identification of Species of Nontuberculous Mycobacteria Clinical Isolates from 8 Provinces of China.

Author

Liu, Haican, Lian, Lulu, Jiang, Yi, Huang, Mingxiang, Tan, Yunhong, Zhao, Xiuqin, Zhang, Jingrui, Yu, Qin, Liu, Jiao, Dong, Haiyan, Lu, Bing, Wu, Yimou, and Wan, Kanglin

Subjects

*LUNG disease prevention, *DNA analysis, *CHI-squared test, *ELECTROPHORESIS, *GENETIC techniques, *GRAM-positive bacteria, *LUNG diseases, *MYCOBACTERIUM, *POLYMERASE chain reaction, *PROBABILITY theory, *RESEARCH funding, *TUBERCULOSIS, *DATA analysis software, *DESCRIPTIVE statistics, *GRAM-negative aerobic bacteria

Abstract

Pulmonary diseases caused by nontuberculous mycobacteria (NTM) are increasing in incidence and prevalence worldwide. In this study, we identified NTM species of the clinical isolates from 8 provinces in China, in order to preliminarily provide some basic scientific data in the different species and distribution of NTM related to pulmonary disease in China. A total of 523 clinical isolates from patients with tuberculosis (TB) diagnosed clinically from 2005 to 2012 were identified to the species using conventional and molecular methods, including multilocus PCR, rpoB and hsp65 PCR-PRA, hsp65, rpoB, and 16S-23S internal transcribed spacer region sequencing. The isolates were identified into 3 bacterium genera, including NTM, Gordonia bronchialis, and Nocardia farcinica, and, for the 488 NTM isolates, 27 species were identified. For all the 27 species of NTM which were found to cause pulmonary infections in humans, the most prevalent species was M. intracellulare, followed by M. avium and M. abscessus. And seven other species were for the first time identified in patients with TB in China. NTM species identification is very important for distinguishing between tuberculosis and NTM pulmonary diseases, and the species diversity drives the creation of diverse and integrated identification methods with higher accuracy and efficacy. [ABSTRACT FROM AUTHOR]

Published

2016

4. Comparative Analysis of Human B Cell Epitopes Based on BCG Genomes.

Author

Li, Machao, Liu, Haican, Zhao, Xiuqin, and Wan, Kanglin

Subjects

*ANTIGEN analysis, *NUCLEIC acid analysis, *TUBERCULOSIS prevention, *DNA analysis, *B cells, *BCG vaccines, *COMPARATIVE studies, *GENES, *GENOMES, *MYCOBACTERIUM, *POLYMERASE chain reaction, *DRUG development, *DESCRIPTIVE statistics, *SEQUENCE analysis

Abstract

Background. Tuberculosis is a huge global health problem. BCG is the only vaccine used for about 100 years against TB, but the reasons for protection variability in populations remain unclear. To improve BCG efficacy and develop a strategy for new vaccines, the underlying genetic differences among BCG subtypes should be understood urgently. Methods and Findings. Human B cell epitope data were collected from the Immune Epitope Database. Epitope sequences were mapped with those of 15 genomes, including 13 BCGs, M. bovis AF2122/97, and M. tuberculosis H37Rv, to identify epitopes distribution. Among 398 experimentally verified B cell epitopes, 321 (80.7%) were conserved, while the remaining 77 (19.3%) were lost to varying degrees in BCGs. The variable protective efficacy of BCGs may result from the degree of B cell epitopes deficiency. Conclusions. Here we firstly analyzed the genetic characteristics of BCGs based on B cell epitopes and found that B cell epitopes distribution may contribute to vaccine efficacy. Restoration of important antigens or effective B cell epitopes in BCG could be a useful strategy for vaccine development. [ABSTRACT FROM AUTHOR]

Published

2016

5. Immunogenicity and efficacy analyses of EPC002, ECA006, and EPCP009 protein subunit combinations as tuberculosis vaccine candidates.

Author

Wang, Ruihuan, Fan, Xueting, Jiang, Yi, Li, Guilian, Li, Machao, Zhao, Xiuqin, Luan, Xiuli, Deng, Yunli, Chen, Zixin, Liu, Haican, and Wan, Kanglin

Subjects

*COMBINED vaccines, *IMMUNE response, *TUBERCULOSIS vaccines, *MYCOBACTERIUM tuberculosis, *HUMORAL immunity, *IMMUNOGLOBULINS, *TICK infestations

Abstract

Tuberculosis (TB) is the leading cause of death from infectious diseases worldwide, and developing a new TB vaccine is a priority for TB control. Combining multiple immunodominant antigens to form a novel multicomponent vaccine with broad-spectrum antigens to induce protective immune responses is a trend in TB vaccine development. In this study, we used T-cell epitope-rich protein subunits to construct three antigenic combinations: EPC002, ECA006, and EPCP009. Fusion expression of purified protein EPC002f (CFP-10-linker-ESAT-6-linker-nPPE18), ECA006f (CFP-10-linker-ESAT-6-linker-Ag85B), and EPCP009f (CFP-10-linker-ESAT-6-linker-nPPE18-linker-nPstS1) and recombinant purified protein mixtures EPC002m (mix of CFP-10, ESAT-6, and nPPE18), ECA006m (mix of CFP-10, ESAT-6, and Ag85B), and EPCP009m (mix of CFP-10, ESAT-6, nPPE18, and nPstS1) were used as antigens, formulated with alum adjuvant, and the immunogenicity and efficacy were analyzed using immunity experiments with BALB/c mice. All protein-immunized groups elicited higher levels of humoral immunity, including IgG and IgG1. The IgG2a/IgG1 ratio of the EPCP009m-immunized group was the highest, followed by that of the EPCP009f-immunized group, which was significantly higher than the ratios of the other four groups. The multiplex microsphere-based cytokine immunoassay revealed that EPCP009f and EPCP009m induced the production of a wider range of cytokines than EPC002f, EPC002m, ECA006f, and ECA006m, which included Th1-type (IL-2, IFN-γ, TNF-α), Th2-type (IL-4, IL-6, IL-10), Th17-type (IL-17), and other proinflammatory cytokines (GM-CSF, IL-12). The enzyme-linked immunospot assays demonstrated that the EPCP009f- and EPCP009m-immunized groups had significantly higher amounts of IFN-γ than the other four groups. The in vitro mycobacterial growth inhibition assay demonstrated that EPCP009m inhibited Mycobacterium tuberculosis (Mtb) growth most strongly, followed by EPCP009f, which was significantly better than that of the other four vaccine candidates. These results indicated that EPCP009m containing four immunodominant antigens exhibited better immunogenicity and Mtb growth inhibition in vitro and may be a promising candidate vaccine for the control of TB. [ABSTRACT FROM AUTHOR]

Published

2023

6. Omics analysis of Mycobacterium tuberculosis isolates uncovers Rv3094c, an ethionamide metabolism-associated gene.

Author

Wan, Li, Hu, Peilei, Zhang, Lili, Wang, Zhao-Xi, Fleming, Joy, Ni, Bo, Luo, Jianjun, Guan, Cha-Xiang, Bai, Liqiong, Tan, Yunhong, Liu, Haican, Li, Na, Xiao, Tongyang, Bai, Hua, Zhang, Yong-An, Zhang, Xian-En, Wan, Kanglin, Bi, Lijun, Ouyang, Songying, and Zhang, Hongtai

Subjects

*MYCOBACTERIUM tuberculosis, *FLAVIN mononucleotide, *GENE expression, *DRUG resistance, *GENES, *FUNGICIDE resistance

Abstract

Global control of the tuberculosis epidemic is threatened by increasing prevalence of drug resistant M. tuberculosis isolates. Many genome-wide studies focus on SNP-associated drug resistance mechanisms, but drug resistance in 5–30% of M. tuberculosis isolates (varying with antibiotic) appears unrelated to reported SNPs, and alternative drug resistance mechanisms involving variation in gene/protein expression are not well-studied. Here, using an omics approach, we identify 388 genes with lineage-related differential expression and 68 candidate drug resistance-associated gene pairs/clusters in 11 M. tuberculosis isolates (variable lineage/drug resistance profiles). Structural, mutagenesis, biochemical and bioinformatic studies on Rv3094c from the Rv3093c-Rv3095 gene cluster, a gene cluster selected for further investigation as it contains a putative monooxygenase/repressor pair and is associated with ethionamide resistance, provide insights on its involvement in ethionamide sulfoxidation, the initial step in its activation. Analysis of the structure of Rv3094c and its complex with ethionamide and flavin mononucleotide, to the best of our knowledge the first structures of an enzyme involved in ethionamide activation, identify key residues in the flavin mononucleotide and ethionamide binding pockets of Rv3094c, and F221, a gate between flavin mononucleotide and ethionamide allowing their interaction to complete the sulfoxidation reaction. Our work broadens understanding of both lineage- and drug resistance-associated gene/protein expression perturbations and identifies another player in mycobacterial ethionamide metabolism. A multi-omic analysis of 11 Mycobacterium tuberculosis (Mtb) isolates with different drug resistance profiles leads to the discovery of Rv3094c, an enzyme capable of activating the clinically relevant Mtb drug, ethionamide. [ABSTRACT FROM AUTHOR]

Published

2023

7. Deep N-terminomics of Mycobacterium tuberculosis H37Rv extensively correct annotated encoding genes.

Author

Shi, Jiahui, Meng, Shuhong, Wan, Li, Zhang, Zhenpeng, Jiang, Songhao, Zhu, Huiming, Dai, Erhei, Chang, Lei, Gao, Huiying, Wan, Kanglin, Zhang, Liqun, Zhao, Xiuqin, Liu, Haican, Lyu, Zhitang, Zhang, Yao, and Xu, Ping

Subjects

*MYCOBACTERIUM tuberculosis, *GENES, *COMPARATIVE genomics, *MYCOBACTERIA, *TUBERCULOSIS, *MASS spectrometers

Abstract

Mycobacterium tuberculosis (MTB) is a severe causing agent of tuberculosis (TB). Although H37Rv, the type strain of M. tuberculosis was sequenced in 1998, annotation errors of encoding genes have been frequently reported in hundreds of papers. This phenomenon is particularly severe at the 5′ end of the genes. Here, we applied a TMPP [(N -Succinimidyloxycarbonylmethyl) tris (2,4,6-trimethoxyphenyl) phosphonium bromide] labeling combined with StageTip separating strategy on M. tuberculosis H37Rv to characterize the N-terminal start sites of its annotated encoding genes. Totally, 1047 proteins were identified with 2058 TMPP labeled N-terminal peptides from all the 2625 mass spectrometer (MS) sequenced proteins. Comparative genomics analysis allowed the re-annotation of 43 proteins' N-termini in H37Rv and 762 proteins in Mycobacteriaceae. All revised N-termini start sites were distributed in 5'-UTR of annotated genes due to over-annotation of previous N-terminal initiation codon, especially the ATG. In addition, we identified and verified a novel gene Rv1078A in +3 frame different from the annotated gene Rv1078 in +2 frame. Altogether, our findings contribute to the better understanding of N-terminal of H37Rv and other species from Mycobacteriaceae that can assist future studies on biological study. • TMPP labeling combined with StageTip separating strategy can extensively correct annotated encoding genes. • 43 proteins' N-termini in H37Rv and 762 proteins in Mycobacteriaceae are wrongly annotated. • Over-prediction of initiation codon with ATG is one of the main reasons for genome mis-annotation. • A novel gene Rv1078A can be added in H37Rv annotation. [ABSTRACT FROM AUTHOR]

Published

2022

8. Quantitative proteomics reveals that dormancy-related proteins mediate the attenuation in mycobacterium strains.

Author

Wang, Hong, Wan, Li, Shi, Jiahui, Zhang, Tao, Zhu, Huiming, Jiang, Songhao, Meng, Shuhong, Wu, Shujia, Sun, Jinshuai, Chang, Lei, Zhang, Liqun, Wan, Kanglin, Yang, Jiaqi, Zhao, Xiuqin, Liu, Haican, Zhang, Yao, Dai, Erhei, and Xu, Ping

Subjects

*PROTEOMICS, *MYCOBACTERIUM, *TUBERCULOSIS, *DORMANCY in plants, *MYCOBACTERIUM bovis, *BCG vaccines, *VIRULENCE of bacteria, *PROTEINS

Abstract

Although members of the Mycobacterium tuberculosis complex (MTBC) exhibit high similarity, they are characterized by differences with respect to virulence, immune response, and transmissibility. To understand the virulence of these bacteria and identify potential novel therapeutic targets, we systemically investigated the total cell protein contents of virulent H37Rv, attenuated H37Ra, and avirulent M. bovis BCG vaccine strains at the log and stationary phases, based on tandem mass tag (TMT) quantitative proteomics. Data analysis revealed that we obtained deep-coverage protein identification and high quantification. Although 272 genetic variations were reported in H37Ra and H37Rv, they showed very little expression difference in log and stationary phase. Quantitative comparison revealed H37Ra and H37Rv had significantly dysregulation in log phase (227) compared with stationary phase (61). While BCG and H37Rv, and BCG and H37Ra showed notable differences in stationary phase (1171 and 1124) with respect to log phase (381 and 414). In the log phase, similar patterns of protein abundance were observed between H37Ra and BCG, whereas a more similar expression pattern was observed between H37Rv and H37Ra in the stationary phase. Bioinformatic analysis revealed that the upregulated proteins detected for H37Rv and H37Ra in log phase were virulence-related factors. In both log and stationary phases, the dysregulated proteins detected for BCG, which have also been identified as M. tuberculosis response proteins under dormancy conditions. We accordingly describe the proteomic profiles of H37Rv, H37Ra, and BCG, which we believe will potentially provide a better understanding of H37Rv pathogenesis, H37Ra attenuation, and BCG immuno protection. [ABSTRACT FROM AUTHOR]

Published

2021

9. Construction and immunogenicity of a T cell epitope-based subunit vaccine candidate against Mycobacterium tuberculosis.

Author

Fan, Xueting, Li, Xiaoyan, Wan, Kanglin, Zhao, Xiuqin, Deng, Yunli, Chen, Zixin, Luan, Xiuli, Lu, Shuangshuang, and Liu, Haican

Subjects

*MYCOBACTERIUM tuberculosis, *T cells, *TUBERCULOSIS, *TUBERCULOSIS vaccines, *RECOMBINANT proteins, *IMMUNOGLOBULIN G, *CELLULAR inclusions, *ANTIBODY formation

Abstract

• This study is the first to design a tuberculosis vaccine based on T cell epitopes. • T cell epitope-based subunit vaccinestimulated strong Th1-type cellular immune response. • The used approach could be useful against latent TB. Despite antibiotic treatment and Bacille Calmette-Guérin (BCG) vaccination, Mycobacterium tuberculosis remains a major public health burden in most developing countries. Therefore, developing an improved vaccine is high priority. In this study, we cloned the genes of the immunodominant antigen of M. tuberculosis viz. its 38-kDa antigen (Pst homolog) (Rv0934, PstS1), and its T cell epitopes (amino acid [aa]169–405 and [aa]802–1119), which we termed PstS1p. Prokaryotic expression showed that the two recombinant proteins were mainly in the form of inclusion bodies. We also evaluated the immunity and immunogenicity of PstS1 and PstS1p. Both PstS1 and its T cell epitopes elicited significantly higher antigen-specific immunoglobulin G (IgG) antibodies in mouse serum, indicating that they enhanced antibody response. They also elicited the T helper 1 (Th1)-type response and promoted CD4+ T cell proliferation. Compared to PstS1, PstS1p promoted stronger cell-mediated immune response. These data indicate that PstS1p is highly immunogenic in mice, and may be a promising candidate vaccine for controlling tuberculosis. [ABSTRACT FROM AUTHOR]

Published

2021

10. Exploring the immunogenicity of Rv2201-519: A T-cell epitope-based antigen derived from Mycobacterium tuberculosis AsnB with implications for tuberculosis infection detection and vaccine development.

Author

Luan, Xiuli, Fan, Xueting, Li, Guilian, Li, Mchao, Li, Na, Yan, Yuhan, Zhao, Xiuqin, Liu, Haican, and Wan, Kanglin

Subjects

*MYCOBACTERIUM tuberculosis, *VACCINE development, *IMMUNE response, *T cells, *TUBERCULOSIS, *ANTIGENS

Abstract

• Rv2201-519 is a T-cell epitope-rich fragment of MTB antigen Rv2201. • Rv2201-519 shows promising sensitivity in TB detection with ELISpot. • Rv2201-519 induces potent Th1-type immune responses in mice. • Rv2201-519 is an immunodominant antigen and may serves as vaccine candidate for TB. Research dedicated to diagnostic reagents and vaccine development for tuberculosis (TB) is challenging due to the paucity of immunodominant antigens that can predict disease risk and exhibit protective potential. Therefore, it is crucial to identify T-cell epitope-based Mycobacterium tuberculosis (MTB) antigens characterized by specific and prominent recognition by the immune system. In this study, we constructed a T-cell epitope-rich tripeptide-splicing fragment (nucleotide positions 131–194, 334–377, and 579–643) of Rv2201 (also known as the 72 kDa AsnB) from the MTB genome, ultimately yielding the recombinant protein Rv2201-519 in Escherichia coli BL21 (DE3). Subsequently, we gauged the recombinant protein's ability to detect tuberculosis infection through ELISpot and assessed its immunostimulatory effect on mouse models using flow cytometry and ELISA. Our results indicated that Rv2201-519 possessed promising sensitivity; however, the sensitivity was lower than that of a commercial diagnostic kit containing ESAT-6, CFP-10, and Rv3615c (80.56 % vs. 94.44 %). The Rv2201-519 group exhibited a propensity for a CD4+ Th1 cell immune response in inoculated BALB/c mice that manifested as higher levels of antigen-specific IgG production (IgG2a/IgG1 > 1). In comparison to Ag85B, Rv2201-519 induced a more robust Th1-type cellular immune response as evidenced by a notable rise in the ratio of IFN-γ/IL-4 and IL-12 cytokine production and increased CD4+ T cell activation with a higher percentage of CD4+IFN-γ+ T cells. Rv2201-519 also induced a higher level of IL-6 compared with Ag85B, a higher percentage of CD8+ T cells specific for Rv2201-519, and a lower percentage of CD8+IL-4+ T cells. Collectively, the current evidence suggests that Rv2201-519 could potentially serve as an immunodominant protein for tuberculosis infection screening, laying the groundwork for further evaluation in recombinant Bacillus Calmette-Guérin (BCG) and subunit vaccines against MTB challenges in future studies. [ABSTRACT FROM AUTHOR]

Published

2024

11. Synergistic activities of clofazimine with moxifloxacin or capreomycin against Mycobacterium tuberculosis in China.

Author

Li, Guilian, Xu, Zhengquan, Jiang, Yi, Liu, Haican, Zhao, Li-li, Li, Machao, Xu, Donglei, Zhao, Xiuqin, Liu, Zhiguang, Wang, Ruibai, and Wan, Kanglin

Subjects

*MYCOBACTERIUM tuberculosis, *MULTIDRUG-resistant tuberculosis, *MOXIFLOXACIN, *DRUG abuse, *TUBERCULOSIS

Abstract

• Clofazimine/moxifloxacin combinations showed excellent synergism against Mycobacterium tuberculosis. • Moxifloxacin showed better synergism than capreomycin when combined with clofazimine. • Multidrug-/extensively drug-resistant isolates more likely to show antagonism than drug-resistant/pan-sensitive strains. • Difference in antagonism relevant for clofazimine/moxifloxacin and clofazimine/capreomycin. Clofazimine (CFZ) is a promising candidate drug for use in the management of multidrug-resistant tuberculosis (MDR-TB) patients. In this study, the minimum inhibitory concentration (MIC) method and checkerboard method were used to investigate potential synergies between CFZ and moxifloxacin (MOX) or capreomycin (CAP). Thirty Mycobacterium tuberculosis strains were collected, including 13 MDR strains, 2 extensively drug-resistant (XDR) strains, 3 pan-sensitive strains and 12 strains resistant to other drugs. When the minimum fractional inhibitory concentration indexes (FICIs) were calculated, synergy was found in 21 (70.00%) M. tuberculosis strains against the CFZ/CAP combination and 29 (96.67%) against the CFZ/MOX combination. When the maximum FICIs were calculated, 10 of 15 MDR/XDR strains and 2 of 15 other drug-resistant or pan-sensitive strains showed antagonism against the CFZ/CAP combination, whilst 8 of 15 MDR/XDR strains and 1 of 15 other drug-resistant or pan-sensitive strains showed antagonism against the CFZ/MOX combination, respectively. In conclusion, these findings demonstrate that the combination of CFZ and MOX shows better synergism than the combination of CFZ and CAP. The MDR/XDR isolates are more likely to show antagonism than the other drug-resistant or pan-sensitive strains in both the CFZ/MOX and CFZ/CAP combinations. CFZ in combination with MOX may be a promising drug regimen for the treatment of MDR-TB, particularly for susceptible M. tuberculosis infections. [ABSTRACT FROM AUTHOR]

Published

2019

12. Ribokinase screened from T7 phage displayed Mycobacterium tuberculosis genomic DNA library had good potential for the serodiagnosis of tuberculosis.

Author

Luo, Dan, Wang, Li, Li, Lingling, Liao, Yating, Yan, Xiaoliang, Zeng, Yanhua, Liu, Haican, Wan, Kanglin, and Yi, Xiaomei

Subjects

*GENE libraries, *TUBERCULOSIS, *SERODIAGNOSIS, *MYCOBACTERIUM tuberculosis, *IMMUNOBLOTTING, *BACTERIOPHAGES

Abstract

Tuberculosis caused by Mycobacterium tuberculosis (M. tuberculosis) is the leading cause of death among infectious diseases in the worldwide. Lack of more sensitive and effective diagnostic reagents has increased the awareness of rapid diagnosis for tuberculosis. In this study, T7 phage displayed genomic DNA library of M. tuberculosis was constructed to screen the antigens that specially bind with TB-positive serum from the whole genome of M. tuberculosis and to improve the sensitivity and specificity of tuberculosis serological diagnosis. After three rounds of biopanning, results of DNA sequencing and BLAST analysis showed that 19 positive phages displayed four different proteins and the occurrence frequency of the phage which displayed ribokinase was the highest. The results of indirect ELISA and dot immunoblotting indicated that representative phages could specifically bind to tuberculosis-positive serum. The prokaryotic expression vector containing the DNA sequence of ribokinase gene was then constructed and the recombinant protein was expressed and purified to evaluate the serodiagnosis value of ribokinase. The reactivity of the recombinant ribokinase with different clinical serum was detected and the sensitivities and specificities in tuberculosis serodiagnosis were 90% and 86%, respectively by screening serum from tuberculosis patients (n = 90) and uninfected individuals (n = 90) based on ELISA. Therefore, this study demonstrated that ribokinase had good potential for the serodiagnosis of tuberculosis. [ABSTRACT FROM AUTHOR]

Published

2019

13. In Vitro Activity of β-Lactams in Combination with β-Lactamase Inhibitors against Mycobacterium tuberculosis Clinical Isolates.

Author

Li, Fu, Wan, Li, Xiao, Tongyang, Liu, Haican, Jiang, Yi, Zhao, Xiuqin, Wang, Ruibai, and Wan, Kanglin

Subjects

*ANTIBIOTICS, *BETA lactam antibiotics, *CLAVULANIC acid, *DRUG resistance in microorganisms, *ENZYME inhibitors, *GENETIC polymorphisms, *MICROBIAL sensitivity tests, *GENETIC mutation, *MYCOBACTERIUM tuberculosis, *SEQUENCE analysis, *IN vitro studies, *PHARMACODYNAMICS

Abstract

Objectives. Evaluating the activity of nineteen β-lactams in combination with different β-lactamase inhibitors to determine the most potent combination against Mycobacterium tuberculosis (MTB) in vitro. Methods. Drug activity was examined by drug susceptibility test with 122 clinical isolates from China. Mutations of blaC and drug targets ldtMt1, ldtMt2, dacB2, and crfA were analyzed by nucleotide sequencing. Results. Tebipenem (TBM) in combination with clavulanate (CLA) exhibited the highest anti-TB activity. The MIC of β-lactam antibiotics was reduced most evidently in the presence of CLA, compared to avibactam (AVI) and sulbactam (SUB). Eight polymorphism sites were identified in blaC, which were not associated with β-lactams resistance. Interestingly, one strain carrying G514A mutation in blaC was highly susceptible to β-lactams regardless of the presence of inhibitors. The transpeptidase encoding genes, ldtMt1, ldtMt2, and dacB2, harboured three mutations, two mutations, and one mutation, respectively, but no correlation was found between these mutations and drug resistance. Conclusion. The activity of β-lactams against MTB and different synergetic effect of β-lactamase inhibitors were indicated. TBM/CLA exhibited the most activity and has a great prospect in developing novel anti-TB regimen; however, further clinical research is warranted. Moreover, the resistance to the β-lactam antibiotics might not be conferred by single target mutation in MTB and requires further studies. [ABSTRACT FROM AUTHOR]

Published

2018

14. Antimicrobial susceptibility and MIC distribution of 41 drugs against clinical isolates from China and reference strains of nontuberculous mycobacteria.

Author

Li, Guilian, Pang, Hui, Guo, Qian, Huang, Mingxiang, Tan, Yanhong, Li, Chao, Wei, Jianhao, Xia, Yuanzhi, Jiang, Yi, Zhao, Xiuqin, Liu, Haican, Zhao, Li-li, Liu, Zhiguang, Xu, Donglei, and Wan, Kanglin

Subjects

*MYCOBACTERIA, *ANTI-infective agents, *MICROBIAL sensitivity tests, *CEFOXITIN

Abstract

To treat nontuberculous mycobacteria (NTM) infections more optimally, further research pertaining to mycobacterial susceptibility to antimicrobial agents is required. A total of 82 species of NTM reference strains and 23 species of NTM clinical isolates were included. Minimum inhibitory concentrations (MICs) for 41 drugs were determined using the microdilution method in cation-adjusted Mueller–Hinton broth. The results showed that most of the NTM were susceptible to aminoglycosides, quinolones, three macrolides (clarithromycin, azithromycin and roxithromycin), cefmetazole, linezolid and capreomycin. Rapidly growing mycobacterium strains were additionally susceptible to cefoxitin, clofazimine, rifapentine, doxycycline, minocycline, tigecycline, meropenem and sulfamethoxazole, whereas slowly growing mycobacterium strains were additionally susceptible to rifabutin. This study on the susceptibility of NTM includes the largest sample size of Chinese clinical isolates and reference strains. NTM species-specific drug susceptibility patterns suggested that it is urgent to identify the species of NTM, to normalise the treatment of NTM infectious disease and to clarify the resistance mechanisms of NTM. [ABSTRACT FROM AUTHOR]

Published

2017

15. Genotypic Diversity of Mycobacterium tuberculosis Clinical Isolates in the Multiethnic Area of the Xinjiang Uygur Autonomous Region in China.

Author

Liu, Jie, Li, Junlian, Liu, Jiao, Zhao, Xiuqin, Lian, Lulu, Liu, Haican, Lu, Bing, Yu, Qin, Zhang, Jingrui, Qi, Yingcheng, and Wan, Kanglin

Subjects

*BACTERIOPHAGE typing, *CHI-squared test, *ETHNIC groups, *MYCOBACTERIUM tuberculosis, *CULTURAL pluralism, *POLYMERASE chain reaction, *RESEARCH funding, *DATA analysis software, *OLIGONUCLEOTIDE arrays, *DESCRIPTIVE statistics, *GENOTYPES

Abstract

Objectives. We studied the genetic diversity of clinical isolates from patients with tuberculosis in the multiethnic area of Xinjiang autonomous region in China. A total of 311 clinical M. tuberculosis isolates were collected in 2006 and 2011 and genotyped by two genotyping methods. All isolates were grouped into 68 distinct spoligotypes using the spoligotyping method. The Beijing family was dominant, followed by T1 and CAS. MIRU-VNTR results showed that a total of 195 different VNTR types were identified. Ten of the 15 loci were highly or moderately discriminant according to their HGDI scores, and 13 loci had good discriminatory power in non-Beijing family strains, whereas only two loci had good discriminatory power in Beijing family strains. Chi-square tests demonstrated that there were no correlations between four characteristics (sex, age, type of case, and treatment history) and the Beijing family. In summary, Beijing family strains were predominant in Xinjiang, and the VNTR-15China locus-set was suitable for genotyping all Xinjiang strains, but not for the Beijing family strains. Thus, these data suggested that different genotype distributions may exist in different regions; MLVA locus-sets should be adjusted accordingly, with newly added loci to increase resolution if necessary. [ABSTRACT FROM AUTHOR]

Published

2017

16. Locked Nucleic Acid Probe-Based Real-Time PCR Assay for the Rapid Detection of Rifampin-Resistant Mycobacterium tuberculosis.

Author

Zhao, Yong, Li, Guilian, Sun, Chongyun, Li, Chao, Wang, Xiaochen, Liu, Haican, Zhang, Pingping, Zhao, Xiuqin, Wang, Xinrui, Jiang, Yi, Yang, Ruifu, Wan, Kanglin, and Zhou, Lei

Subjects

*TUBERCULOSIS diagnosis, *NUCLEIC acid probes, *POLYMERASE chain reaction, *RIFAMPIN, *DRUG resistance, *NUCLEIC acid amplification techniques, *THERAPEUTICS

Abstract

Drug-resistant Mycobacterium tuberculosis can be rapidly diagnosed through nucleic acid amplification techniques by analyzing the variations in the associated gene sequences. In the present study, a locked nucleic acid (LNA) probe-based real-time PCR assay was developed to identify the mutations in the rpoB gene associated with rifampin (RFP) resistance in M. tuberculosis. Six LNA probes with the discrimination capability of one-base mismatch were designed to monitor the 23 most frequent rpoB mutations. The target mutations were identified using the probes in a “probe dropout” manner (quantification cycle = 0); thus, the proposed technique exhibited superiority in mutation detection. The LNA probe-based real-time PCR assay was developed in a two-tube format with three LNA probes and one internal amplification control probe in each tube. The assay showed excellent specificity to M. tuberculosis with or without RFP resistance by evaluating 12 strains of common non-tuberculosis mycobacteria. The limit of detection of M. tuberculosis was 10 genomic equivalents (GE)/reaction by further introducing a nested PCR method. In a blind validation of 154 clinical mycobacterium isolates, 142/142 (100%) were correctly detected through the assay. Of these isolates, 88/88 (100%) were determined as RFP susceptible and 52/54 (96.3%) were characterized as RFP resistant. Two unrecognized RFP-resistant strains were sequenced and were found to contain mutations outside the range of the 23 mutation targets. In conclusion, this study established a sensitive, accurate, and low-cost LNA probe-based assay suitable for a four-multiplexing real-time PCR instrument. The proposed method can be used to diagnose RFP-resistant tuberculosis in clinical laboratories. [ABSTRACT FROM AUTHOR]

Published

2015

17. Multicenter clinical evaluation of three commercial reagent kits based on the interferon-gamma release assay for the rapid diagnosis of tuberculosis in China.

Author

Qiu, Yan, Wang, Yansen, Lin, Nan, Huang, Mingxiang, Tan, Yunhong, Wang, Qing, Jiang, Yi, Liu, Haican, Liu, Jiao, Zhang, Jingrui, Wang, Jue, Chen, Xinchan, Wang, Dongping, Li, Guilian, Chen, Zhongnan, Zhang, Lishui, Bao, Dixun, Zhao, Lili, Guan, Chaxiang, and Wan, Kanlgin

Subjects

*TUBERCULOSIS diagnosis, *INTERFERON gamma, *BIOLOGICAL assay, *MEDICAL care, *CLINICAL trials

Abstract

Summary Objective To evaluate the performance of three interferon-gamma release assay (IGRA) kits in detecting Mycobacterium tuberculosis infection in China. Methods A multicenter clinical trial was used to compare the effectiveness and application of the three kits. A total of 1026 participants were enrolled at three hospitals, including 597 tuberculosis (TB) patients diagnosed clinically (517 patients with pulmonary TB and 80 patients with extrapulmonary TB) and 429 negative controls (244 patients with pulmonary disease but not TB, or with non-tuberculosis mycobacterial lung diseases, and 185 healthy people). Detection performance indicators including sensitivity, specificity, and the Youden index (YI) were used to evaluate performance. Results Through bacterial culture evaluation, 224 of the 517 pulmonary TB patients were positive and all 429 negative controls were negative. When the gold standard bacterial methods were used, the sensitivity, specificity, and YI were 89.7% (201/224), 91.1% (391/429), and 0.81 for T-SPOT.TB, 86.2% (193/224), 87.2% (374/429), and 0.73 for QB-SPOT, and 83.9% (188/224), 88.6% (380/429), and 0.73 for TB-IGRA, respectively. There were no significant differences in the sensitivity and specificity of the three kits. Conclusions The results showed that the three kits had very high sensitivity and specificity and exhibited a good performance for the detection of M. tuberculosis infection. [ABSTRACT FROM AUTHOR]

Published

2015

18. Drug Susceptibility Testing of 31 Antimicrobial Agents on Rapidly Growing Mycobacteria Isolates from China.

Author

Pang, Hui, Li, Guilian, Zhao, Xiuqin, Liu, Haican, Wan, Kanglin, and Yu, Ping

Subjects

*ANTI-infective agents, *CULTURE media (Biology), *CULTURES (Biology), *DRUG resistance in microorganisms, *MICROBIOLOGICAL techniques, *MYCOBACTERIUM, *RESEARCH funding, *SPUTUM, *DESCRIPTIVE statistics, *IN vitro studies

Abstract

Objectives. Several species of rapidly growing mycobacteria (RGM) are now recognized as human pathogens. However, limited data on effective drug treatments against these organisms exists. Here, we describe the species distribution and drug susceptibility profiles of RGM clinical isolates collected from four southern Chinese provinces from January 2005 to December 2012. Methods. Clinical isolates (73) were subjected to in vitro testing with 31 antimicrobial agents using the cation-adjusted Mueller-Hinton broth microdilution method. The isolates included 55 M. abscessus, 11 M. fortuitum, 3 M. chelonae, 2 M. neoaurum, and 2 M. septicum isolates. Results. M. abscessus (75.34%) and M. fortuitum (15.07%), the most common species, exhibited greater antibiotic resistance than the other three species. The isolates had low resistance to amikacin, linezolid, and tigecycline, and high resistance to first-line antituberculous agents, amoxicillin-clavulanic acid, rifapentine, dapsone, thioacetazone, and pasiniazid. M. abscessus and M. fortuitum were highly resistant to ofloxacin and rifabutin, respectively. The isolates showed moderate resistance to the other antimicrobial agents. Conclusions. Our results suggest that tigecycline, linezolid, clofazimine, and cefmetazole are appropriate choices for M. abscessus infections. Capreomycin, sulfamethoxazole, tigecycline, clofazimine, and cefmetazole are potentially good choices for M. fortuitum infections. Our drug susceptibility data should be useful to clinicians. [ABSTRACT FROM AUTHOR]

Published

2015

19. First Insight into the Genotypic Diversity of Clinical Mycobacterium tuberculosis Isolates from Gansu Province, China.

Author

Liu, Jie, Tong, Chongxiang, Liu, Jiao, Jiang, Yuan, Zhao, Xiuqin, Zhang, Yuanyuan, Liu, Haican, Lu, Bing, and Wan, Kanglin

Subjects

*MYCOBACTERIUM tuberculosis, *GROUP psychoanalysis, *TANDEM repeats, *GEOGRAPHY, *MICROBIOLOGY, *PATHOGENIC microorganisms

Abstract

Background: Investigations of Mycobacterium tuberculosis genetic diversity in China have indicated a significant regional distribution. The aim of this study was to characterize the genotypes of clinical M. tuberculosis isolates obtained from Gansu, which has a special geographic location in China. Methodology/Principal Findings: A total of 467 clinical M. tuberculosis strains isolated in Gansu Province were genotyped by 15-locus mycobacterial interspersed repetitive units–variable number tandem repeats (MIRU-VNTR) and spoligotyping. The results showed that 445 isolates belonged to six known spoligotype lineages, whereas 22 isolates were unknown. The Beijing genotype was the most prevalent (87.58%, n = 409), while the shared type 1 was the dominant genotype (80.94%, n = 378). The second most common lineage was the T lineage, with 25 isolates (5.35%), followed by the H lineage with 5 isolates (1.07%), the MANU family (0.64%, 3 isolates), the U family (0.43%, 2 isolates) and the CAS lineage with 1 isolate (0.21%). By using the VNTR15China method, we observed 15 groups and 228 genotypes among the 467 isolates. We found no association between the five larger groups (including the Beijing genotype) and sex, age, or treatment status, and there was no noticeable difference in the group analysis in different areas. In the present study, seven of the 15 MIRU-VNTR loci were highly or moderately discriminative according to their Hunter-Gaston discriminatory index. Conclusions/Significance: The Beijing genotype is the predominant genotype in Gansu province. We confirm that VNTR15China is suitable for typing Beijing strains in China and that it has a better discriminatory power than spoligotyping. Therefore, the use of both methods is the most suitable for genotyping analysis of M. tuberculosis. [ABSTRACT FROM AUTHOR]

Published

2014

20. Antimicrobial Susceptibility of Standard Strains of Nontuberculous Mycobacteria by Microplate Alamar Blue Assay.

Author

Li, Guilian, Lian, Lu-lu, Wan, Li, Zhang, Jingrui, Zhao, Xiuqin, Jiang, Yi, Zhao, Li-li, Liu, Haican, and Wan, Kanglin

Subjects

*MICROBIAL sensitivity tests, *MYCOBACTERIUM tuberculosis, *MICROPLATES, *BIOLOGICAL assay, *MYCOBACTERIA, *ANTI-infective agents, *FLUOROQUINOLONES

Abstract

In this study, 24 standard nontuberculous mycobacteria (NTM) species strains including 12 slowly growing mycobacteria strains and 12 rapidly growing mycobacteria strains were subjected to drug susceptibility testing using microplate Alamar Blue assay-based 7H9 broth. The most active antimicrobial agents against the 24 NTM strains were streptomycin, amikacin, the fluoroquinolones, and the tetracyclines. Mycobacterium chelonae, Mycobacterium abscessus, Mycobacterium bolletii, and Mycobacterium simiae are resistant to most antimicrobial agents. The susceptibility results of this study from 24 NTM standard strains can be referenced by clinicians before susceptibility testing for clinical isolates is performed or when conditions do not allow for susceptibility testing. The application of broth-based methods is recommended by the Clinical and Laboratory Standards Institute, and the documentation of the susceptibility patterns of standard strains of mycobacteria can improve the international standardization of susceptibility testing methods. [ABSTRACT FROM AUTHOR]

Published

2013

21. Genetic diversity of antigens Rv2945c and Rv0309 in Mycobacterium tuberculosis strains may reflect ongoing immune evasion.

Author

Jiang, Yi, Dou, Xiangfeng, Zhang, Wen, Liu, Haican, Zhao, Xiuqin, Wang, Haiyin, Lian, Lulu, Yu, Qin, Zhang, Jingrui, Li, Guilian, Chen, Chen, and Wan, Kanglin

Subjects

*ANTIGENS, *MYCOBACTERIUM tuberculosis, *PATHOGENIC bacteria, *NUCLEOTIDES, *HOST-parasite relationships

Abstract

Host immune pressure and associated immune evasion of pathogenic bacteria are key features of host-pathogen co-evolution. A previous study showed that human T-cell epitopes of Mycobacterium tuberculosis are evolutionarily hyperconserved and thus it was deduced that M. tuberculosis lacks antigenic variation and immune evasion. Here, we selected 173 clinical M. tuberculosis complex (MTBC) isolates from China, amplified the genes encoding Rv2945c and Rv0309, and compared the sequences. The results showed that genetic diversity existed in these two genes among the MTBC strains and two single nucleotide polymorphisms (SNPs) presented higher polymorphisms. Antigen Rv2945c harbored a higher number of amino acid substitutions of its T-cell epitopes, which may reflect ongoing immune evasion. In addition, the high dN/ dS value of Rv0309 suggested antigen Rv0309 might be involved in diversifying selection to evade host immunity. Finally, a small group of strains were identified based on the genetic diversity of these two genes, which might indicate that they interact differently with human T cells compared with other strains. [ABSTRACT FROM AUTHOR]

Published

2013

22. Genome Sequencing and Analysis of BCG Vaccine Strains.

Author

Zhang, Wen, Zhang, Yuanyuan, Zheng, Huajun, Pan, Yuanlong, Liu, Haican, Du, Pengcheng, Wan, Li, Liu, Jun, Zhu, Baoli, Zhao, Guoping, Chen, Chen, and Wan, Kanglin

Subjects

*NUCLEOTIDE sequence, *BCG vaccines, *BACTERIAL genomes, *TUBERCULOSIS vaccines, *MYCOBACTERIUM tuberculosis, *BACTERIAL diseases, *COMPARATIVE genomics

Abstract

Background: Although the Bacillus Calmette-Guérin (BCG) vaccine against tuberculosis (TB) has been available for more than 75 years, one third of the world's population is still infected with Mycobacterium tuberculosis and approximately 2 million people die of TB every year. To reduce this immense TB burden, a clearer understanding of the functional genes underlying the action of BCG and the development of new vaccines are urgently needed. Methods and Findings: Comparative genomic analysis of 19 M. tuberculosis complex strains showed that BCG strains underwent repeated human manipulation, had higher region of deletion rates than those of natural M. tuberculosis strains, and lost several essential components such as T-cell epitopes. A total of 188 BCG strain T-cell epitopes were lost to various degrees. The non-virulent BCG Tokyo strain, which has the largest number of T-cell epitopes (359), lost 124. Here we propose that BCG strain protection variability results from different epitopes. This study is the first to present BCG as a model organism for genetics research. BCG strains have a very well-documented history and now detailed genome information. Genome comparison revealed the selection process of BCG strains under human manipulation (1908–1966). Conclusions: Our results revealed the cause of BCG vaccine strain protection variability at the genome level and supported the hypothesis that the restoration of lost BCG Tokyo epitopes is a useful future vaccine development strategy. Furthermore, these detailed BCG vaccine genome investigation results will be useful in microbial genetics, microbial engineering and other research fields. [ABSTRACT FROM AUTHOR]

Published

2013

23. Comparison of transcriptional change of B. melitensis M5-90 after macrophage infection highlights the role of ribosome gene L31 in virulence.

Author

Xu, Da, Zhao, Jianlong, Jiang, Liying, Song, Jiabao, Zong, Shucheng, Yan, Xin, Liu, Haican, Zhang, Huitong, Hu, Sen, and Bu, Zhigao

Subjects

*MACROPHAGES, *BRUCELLA melitensis, *RIBOSOMES, *EPITHELIAL cells, *GENES, *INFECTION

Abstract

• RNA samples of B. melitensis M5-90 grown intracellular were isolated. • Using RNA-seq technology, we described the transcriptional change of B. melitensis M5-90 during macrophage infection. • During macrophage infection three KEGG pathways were significantly enriched. • L31 gene is required for the full virulence of avirulent strain B. melitensis M5-90 and virulent strain B. melitensis M28. Brucella , a facultative intracellular bacterium, can survive and replicate in various cell types such as epithelial cell, fibroblasts and macrophage. Macrophage is the most important sites for the survival of Brucella in vivo. The mechanisms of pathogenesis are difficult to address, since the unknown virulence genes are still exist. RNA-seq is available to study transcriptional changes that occur during disease as a way to identify important virulence-related genes. Here we described and analyzed the transcriptional change of avirulent strain Brucella melitensis M5-90 (B. melitensis M5-90) during macrophage infection using RNA-seq technology. We detected 601 significant changed genes of which 428 were upregulated after infection. The upregulated gene L31 which involved in ribosome KEGG pathway was selected to illustrate its effect on virulence in a vaccine strain B. melitensis M5-90 and a virulent strain B. melitensis M28. Deletion of L31 significant attenuates the spleen colonization in model of M5-90 or M28 infection mouse at 7, 21 and 35 days post-infection (P < 0.05). We further examine the role of L31 in a macrophage cell infection model, and the result showed a significant reduction of intracellular M28Δ L31 cells at 48 h post-infection (P < 0.001). In total, our study provided a view of transcriptional landscape of B. melitensis M5-90 intracellular, and found L31 gene is required for the full virulence of B. melitensis. [ABSTRACT FROM AUTHOR]

Published

2021

24. Correction: Locked Nucleic Acid Probe-Based Real-Time PCR Assay for the Rapid Detection of Rifampin-Resistant Mycobacterium tuberculosis.

Author

Zhao, Yong, Li, Guilian, Sun, Chongyun, Li, Chao, Wang, Xiaochen, Liu, Haican, Zhang, Pingping, Zhao, Xiuqin, Wang, Xinrui, Jiang, Yi, Yang, Ruifu, Wan, Kanglin, and Zhou, Lei

Subjects

*MYCOBACTERIUM tuberculosis, *NUCLEIC acids, *POLYMERASE chain reaction, *DIAGNOSIS

Published

2016

25. Development of Multiplex PCR Assays for the Identification of the 33 Serotypes of Streptococcus suis.

Author

Liu, Zhijie, Zheng, Han, Gottschalk, Marcelo, Bai, Xuemei, Lan, Ruiting, Ji, Shaobo, Liu, Haican, and Xu, Jianguo

Subjects

*POLYMERASE chain reaction, *SEROTYPES, *STREPTOCOCCUS suis, *ZOONOSES, *SWINE diseases

Abstract

Streptococcus suis is an important zoonotic agent causing severe diseases in pigs and humans. To date, 33 serotypes of S. suis have been identified based on antigenic differences in the capsular polysaccharide. The capsular polysaccharide synthesis (cps) locus encodes proteins/enzymes that are responsible for capsular production and variation in the capsule structures are the basis of S. suis serotyping. Multiplex and/or simplex PCR assays have been developed for 15 serotypes based on serotype-specific genes in the cps gene cluster. In this study, we developed a set of multiplex PCR (mPCR) assays to identify the 33 currently known S. suis serotypes. To identify serotype-specific genes for mPCR, the entire genomes of reference strains for the 33 serotypes were sequenced using whole genome high-throughput sequencing, and the cps gene clusters from these strains were identified and compared. We developed a set of 4 mPCR assays based on the polysaccharide polymerase gene wzy, one of the serotype-specific genes. The assays can identify all serotypes except for two pairs of serotypes: 1 and 14, and 2 and 1/2, which have no serotype-specific genes between them. The first assay identifies 12 serotypes (serotypes 1 to 10, 1/2, and 14) that are the most frequently isolated from diseased pigs and patients; the second identifies 10 serotypes (serotypes 11 to 21 except 14); the third identifies the remaining 11 serotypes (serotypes 22 to 31, and 33); and the fourth identifies a new cps cluster of S. suis discovered in this study in 16 isolates that agglutinated with antisera for serotypes 29 and 21. The multiplex PCR assays developed in this study provide a rapid and specific method for molecular serotyping of S. suis. [ABSTRACT FROM AUTHOR]

Published

2013