Characterization of ST-4821 complex, a unique Neisseria meningitidis clone

Peng, Junping; Li, Yang; Yang, Fan; Yang, Jian; Yan, Yongliang; Nie, Hushuai; Zhang, Xiaobing; Xiong, Zhaohui; Jiang, Yan; Cheng, Fan; Xu, Xingye; Chen, Shuxia; Sun, Lu; Li, Weijun; Shen, Yan; Shao, Zhujun; Liang, Xiaofeng; Xu, Jianguo; Jin, Qi

doi:10.1016/j.ygeno.2007.10.004

Cited by 68 publications

(52 citation statements)

References 48 publications

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“…In addition, they performed an extensively CGH analysis on 28 clinical isolates belonging to the the ST-4821 complex, the most predominant and hyper virulent lineage in China [17]. The meningococcal disease-associated island was detected in almost all the ST-4821 complex clinical isolates (21 from healthy carriers and eight from patients), thus confirming its important role in meningococcal pathogenesis as reported by Bille et al [18].…”

Section: Neisserial Comparative Genome Hybridizationsupporting

confidence: 62%

“…The same authors also compared the MenC 053442 genome with those of three meningococci, MenA Z2491, MenB MC58 and MenC FAM18, defining a common backbone of genes that may be responsible for the colonization and spread among members of the human host [17]. In addition, they performed an extensively CGH analysis on 28 clinical isolates belonging to the the ST-4821 complex, the most predominant and hyper virulent lineage in China [17].…”

Section: Neisserial Comparative Genome Hybridizationmentioning

confidence: 99%

See 1 more Smart Citation

Post-genomics ofNeisseria meningitidis: an update

Bernardini¹,

Braconi²,

Lusini³

et al. 2011

Expert Review of Proteomics

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Section: Neisserial Comparative Genome Hybridizationsupporting

confidence: 62%

Section: Neisserial Comparative Genome Hybridizationmentioning

confidence: 99%

Post-genomics ofNeisseria meningitidis: an update

Bernardini¹,

Braconi²,

Lusini³

et al. 2011

Expert Review of Proteomics

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“…The Neisseria gonorrhoeae strain FA1090 genome was accessed from the University of Oklahoma website (http://www.genome.ou.edu/gono.html). The recently published sequence from the serogroup C isolate 053442 (ST-4821) (Peng et al, 2008) was also employed. CLUSTAL W version 2.0 (Larkin et al, 2007) was used to perform sequence alignments.…”

Section: Methodsmentioning

confidence: 99%

Neisseria meningitidis antigen NMB0088: sequence variability, protein topology and vaccine potential

Sardiñas

Yero

Climent

et al. 2009

Journal of Medical Microbiology

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The significance of Neisseria meningitidis serogroup B membrane proteins as vaccine candidates is continually growing. Here, we studied different aspects of antigen NMB0088, a protein that is abundant in outer-membrane vesicle preparations and is thought to be a surface protein. The gene encoding protein NMB0088 was sequenced in a panel of 34 different meningococcal strains with clinical and epidemiological relevance. After this analysis, four variants of NMB0088 were identified; the variability was confined to three specific segments, designated VR1, VR2 and VR3. Secondary structure predictions, refined with alignment analysis and homology modelling using FadL of Escherichia coli, revealed that almost all the variable regions were located in extracellular loop domains. In addition, the NMB0088 antigen was expressed in E. coli and a procedure for obtaining purified recombinant NMB0088 is described. The humoral immune response elicited in BALB/c mice was measured by ELISA and Western blotting, while the functional activity of these antibodies was determined in a serum bactericidal assay and an animal protection model. After immunization in mice, the recombinant protein was capable of inducing a protective response when it was administered inserted into liposomes. According to our results, the recombinant NMB0088 protein may represent a novel antigen for a vaccine against meningococcal disease. However, results from the variability study should be considered for designing a cross-protective formulation in future studies.

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“…It contains four rRNA operons and codes for 55 tRNAs, 1,941 protein-coding sequences (CDSs), and 135 pseudogenes. In line with a clonal population structure of serogroup A meningococci (1), the WUE2594 genome has the highest similarity to the genome of Z2491 among the seven so far completely sequenced meningococcal strains (2,7,11,12,15,16,19). Both share 1,857 CDSs, with an average nucleotide sequence identity of 98.6%, and are highly colinear, with only one inversion spanning the capsule locus regions A, C, and E (5).…”

mentioning

confidence: 97%

“…Whereas five complete genome sequences are available for serogroup B and C strains (2,7,12,15,19), which are endemic predominantly in industrialized countries (6), only a single serogroup A strain has so far been sequenced (11). However, the fact that the sequenced serogroup A strain Z2491 is not transformable in vitro has severely hindered the experimental analysis of serogroup A virulence and epidemiology.…”

mentioning

confidence: 99%