Cloning, sequence determination, and expression of a 32-kilodalton-protein gene of Mycobacterium tuberculosis

Borremans, Martine; Wit, L de; Volckaert, Guido; Ooms, Josette; Bruyn, Jacqueline De; Huygen, Kris; Vooren, Jean-Paulvan; Stélandre, Martine; Verhofstadt, Roger

doi:10.1128/iai.57.10.3123-3130.1989

Cited by 118 publications

(48 citation statements)

References 33 publications

(54 reference statements)

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“…The upstream region of the BCG 85A gene, from -274 to -251. was more A/T rich than ihe BCG 85A coding region (66.7% as opposed to 32.9%). Although Martine Borremans et al and Luk De Wit et al reported the sequence of 85A genes from M. tuberculosis and BCG, they did not contain this region [14,15]. The sequence of this region is similar to the E. coli CAP-binding site consensus sequence [40], The A/T rich regions were seen near the promoter region of several genes and were binding sites for transcription factors.…”

Section: Ykasdmentioning

confidence: 99%

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Characterization of the Gene Encoding the MPB51, One of the Major Secreted Protein Antigens of Mycobacterium bovis BCG, and Identification of the Secreted Protein Closely Related to the Fibronectin Binding 85 Complex

Ohara¹,

Kitaura²,

Hotokezaka³

et al. 1995

Scand J Immunol

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The secreted protein MPB51 is one of the major proteins in the culture filtrate of Mycobacterium bovis BCG (BCG) and is a protein immunologically cross-reacting with the fibronectin binding 85 complex secreted by this bacterium. The gene encoding MPB51 (mpb51) was cloned, sequenced, and expressed in Escherichia coli. The mpb51 gene was mapped downstream of the gene for 85A component with 179 bp spaces. The mpb51 gene encoded 299 amino acids, including 33 amino acids for the signal peptide, followed by 266 amino acids for the mature protein with a molecular mass of 27807.37 Da. This is the first complete sequence of MPB51. MPB51 showed 37-43% homology to the components of 85 complex. Two-dimensional electrophoresis of culture fluids of BCG and Western blotting indicated the existence of the other novel protein(s) which strongly cross-reacted with the alpha antigen (85B) and MPB51.

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Section: Ykasdmentioning

confidence: 99%

“…The analogous gene was cloned recently from Mycobacterium leprae [12,13]. The genes for the 85A component were cloned from M. tubercuhm.s [14]. BCG [15], and M. leprae [16].…”

Section: Introductionmentioning

confidence: 99%

Characterization of the Gene Encoding the MPB51, One of the Major Secreted Protein Antigens of Mycobacterium bovis BCG, and Identification of the Secreted Protein Closely Related to the Fibronectin Binding 85 Complex

Ohara¹,

Kitaura²,

Hotokezaka³

et al. 1995

Scand J Immunol

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“…[54][55][56][57] Some of the more prominent antigens found in this fraction included the three members of the Ag85 complex (Rv3804c, Rv1886c, Rv0129c), plus Rv1196/PPE18, Rv0125/PepA, Rv0915c/PPE14 and Rv3616c. 58,59 In the lower molecular mass fraction, several proteins belonging to the ESAT-6 family (early secretory antigenic target-6) including ESAT-6/Rv3875, CFP10/ Rv3874, TB9.8/Rv0287 and Mtb9.9A/Rv1793 were isolated. [60][61][62][63] The ESAT-6 family was identified after the completion of the M. tuberculosis genome-this family is not based on homology among the members (which is quite limited) but rather on their organization on the bacterial chromosome where they are found as adjacent pairs close to a PPE or a PE gene.…”

Section: Antigen Discovery Prophylactic Vaccinesmentioning

confidence: 99%

TB vaccines: current status and future perspectives

et al. 2009

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Vaccines against intracellular pathogens such as Mycobacterium tuberculosis need to induce strong cellular immune responses. Antigen discovery programs have exploited this and used proteome studies and T‐cell recognition in PPD‐positive individuals to select proteins and after testing for protective efficacy in animals the most promising proteins have been put together in fusion molecules. Three such fusion proteins are currently in clinical trials, the two most advanced have already passed phase I trials and are entering phase II.

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“…Mycobacteria are Gram-positive bacteria, as is L. monocytogenes, but due to the highly complex, lipoid-rich cell wall structure of mycobacteria, the export machinery including signal-peptidase specificity may differ from L. monocytogenes. Yet, structural homology between BCG and Gram-positive bacterial signal peptide sequences has been reported [58,59]. The S. typhimurium aroA-strain belongs to the Gram-negative world as does E. coli.…”

Section: Improvement Of Bcg and S Typhimurium Aroaas Antigen Delivermentioning

confidence: 99%

Vaccination strategies against intracellular microbes

Hess

Kaufmann

1993

FEMS Immunology &Amp; Medical Microbiology

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Cloning, sequence determination, and expression of a 32-kilodalton-protein gene of Mycobacterium tuberculosis

Cited by 118 publications

References 33 publications

Characterization of the Gene Encoding the MPB51, One of the Major Secreted Protein Antigens of Mycobacterium bovis BCG, and Identification of the Secreted Protein Closely Related to the Fibronectin Binding 85 Complex

Characterization of the Gene Encoding the MPB51, One of the Major Secreted Protein Antigens of Mycobacterium bovis BCG, and Identification of the Secreted Protein Closely Related to the Fibronectin Binding 85 Complex

TB vaccines: current status and future perspectives

Vaccination strategies against intracellular microbes

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