Mycobacterium tuberculosis strains with the Beijing genotype demonstrate variability in virulence associated with transmission

被引:94
作者
Aguilar L, D. [1 ]
Hanekom, M. [2 ]
Mata, D. [1 ]
Gey van Pittius, N. C. [3 ]
van Helden, P. D. [3 ]
Warren, R. M. [3 ]
Hernandez-Pando, R. [1 ]
机构
[1] Natl Inst Med Sci & Nutr Salvador Zubiran, Expt Pathol Sect, Dept Pathol, Mexico City 14000, DF, Mexico
[2] Univ Stellenbosch, Div Anat & Histol, Dept Biomed Sci, Fac Hlth Sci, ZA-7505 Tygerberg, South Africa
[3] Univ Stellenbosch, DST NRF Ctr Excellence Biomed TB Res, MRC Ctr Mol & Cellular Biol,Fac Hlth Sci, Div Mol Biol & Human Genet,Dept Biomed Sci, ZA-7505 Tygerberg, South Africa
来源
TUBERCULOSIS | 2010年 / 90卷 / 05期
关键词
Beijing genotype; Virulence; Transmission; Murine infection model; Th1/Th2; EXPERIMENTAL PULMONARY TUBERCULOSIS; GROWTH-FACTOR-BETA; IMMUNE-RESPONSE; MURINE MODEL; EXPRESSION; PATHOGENESIS; INFECTION; PATHOLOGY; PROTEINS; KINETICS;
D O I
10.1016/j.tube.2010.08.004
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
Phylogenetic analysis has shown that Beijing genotype strains can be grouped into at least 7 different sublineages. We aimed to test the hypothesis that the virulence of Beijing genotype strains differed among members of the different sublineages and that the level of virulence correlated with their ability to spread and cause disease. BALB/c mice were infected with Beijing strains representative of the different lineages and of different epidemiological characteristics ( transmitted vs. non-transmitted). Survival times, lung pathology, bacterial load and immunology kinetics were evaluated at defined intervals post-infection. Transmissibility was determined by co-housing infected and uninfected mice in close contact for 1-2 months. The results show that mice infected with the highly transmitted Beijing strains began showing mortality 3 weeks post-infection and all had died by 5 weeks, suggesting high virulence phenotypes. In contrast, >80% of mice infected with the non-transmitted strains survived 4 months post-infection, suggesting low virulence phenotypes. Our co-housing transmission model confirmed these virulence phenotypes. Extensive tissue damage and the induction of lower levels of IFN gamma and iNOS expression, as well as high but ephemeral TNF alpha expression were associated with the high virulence phenotype. In contrast, minimal tissue damage and progressive expression of IFN gamma and TNF alpha were associated with the low virulence phenotype. Both virulence phenotypes induced similar levels of IL-4 expression during the early stages of infection after which the high virulence strain induced significantly higher levels of IL-4 expression. In conclusion, this study demonstrates that Beijing genotype strains display a spectrum of virulence phenotypes in mice which mimic their epidemiological characteristics. Both transmissible and non-transmissible strains may exist in the same sublineage. (C) 2010 Elsevier Ltd. All rights reserved.
引用
收藏
页码:319 / 325
页数:7
相关论文
共 30 条
[1]   The Beijing genotype and drug resistant tuberculosis in the Aral Sea region of Central Asia -: art. no. 134 [J].
Cox, HS ;
Kubica, T ;
Doshetov, D ;
Kebede, Y ;
Rüsch-Gerdess, S ;
Niemann, S .
RESPIRATORY RESEARCH, 2005, 6 (1)
[2]   Using a Label-free Proteomics Method to Identify Differentially Abundant Proteins in Closely Related Hypo- and Hypervirulent Clinical Mycobacterium tuberculosis Beijing Isolates [J].
de Souza, Gustavo A. ;
Fortuin, Suereta ;
Aguilar, Diana ;
Hernandez Pando, Rogelio ;
McEvoy, Christopher R. E. ;
van Helden, Paul D. ;
Koehler, Christian J. ;
Thiede, Bernd ;
Warren, Robin M. ;
Wiker, Harald G. .
MOLECULAR & CELLULAR PROTEOMICS, 2010, 9 (11) :2414-2423
[3]   Correlation of virulence, lung pathology, bacterial load and delayed type hypersensitivity responses after infection with different Mycobacterium tuberculosis genotypes in a BALB/c mouse model [J].
Dormans, J ;
Burger, M ;
Aguilar, D ;
Hernandez-Pando, R ;
Kremer, K ;
Roholl, P ;
Arend, SM ;
van Soolingen, D .
CLINICAL AND EXPERIMENTAL IMMUNOLOGY, 2004, 137 (03) :460-468
[4]  
Ewald P. W., 1994, EVOLUTION INFECT DIS
[5]   Variable host-pathogen compatibility in Mycobacterium tuberculosis [J].
Gagneux, S ;
DeRiemer, K ;
Van, T ;
Kato-Maeda, M ;
de Jong, BC ;
Narayanan, S ;
Nicol, M ;
Niemann, S ;
Kremer, K ;
Gutierrez, MC ;
Hilty, M ;
Hopewell, PC ;
Small, PM .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 2006, 103 (08) :2869-2873
[6]  
Glynn JR, 2002, EMERG INFECT DIS, V8, P843
[7]   A recently evolved sublineage of the Mycobacterium tuberculosis Beijing strain family is associated with an increased ability to spread and cause disease [J].
Hanekom, M. ;
van der Spuy, G. D. ;
Streicher, E. ;
Ndabambi, S. L. ;
McEvoy, C. R. E. ;
Kidd, M. ;
Beyers, N. ;
Victor, T. C. ;
van Helden, P. D. ;
Warren, R. M. .
JOURNAL OF CLINICAL MICROBIOLOGY, 2007, 45 (05) :1483-1490
[8]   Analysis of the local kinetics and localization of interleukin-1 alpha, tumour necrosis factor-alpha and transforming growth factor-beta, during the course of experimental pulmonary tuberculosis [J].
HernandezPando, R ;
Orozco, H ;
Arriaga, K ;
Sampieri, A ;
LarrivaSahd, J ;
MadridMarina, V .
IMMUNOLOGY, 1997, 90 (04) :607-617
[9]  
HernandezPando R, 1996, IMMUNOLOGY, V89, P26
[10]   Simultaneous detection and strain differentiation of Mycobacterium tuberculosis for diagnosis and epidemiology [J].
Kamerbeek, J ;
Schouls, L ;
Kolk, A ;
vanAgterveld, M ;
vanSoolingen, D ;
Kuijper, S ;
Bunschoten, A ;
Molhuizen, H ;
Shaw, R ;
Goyal, M ;
vanEmbden, J .
JOURNAL OF CLINICAL MICROBIOLOGY, 1997, 35 (04) :907-914
123