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Infection and Immunity, April 2006, p. 2449-2452, Vol. 74, No. 4
0019-9567/06/$08.00+0     doi:10.1128/IAI.74.4.2449-2452.2006
Copyright © 2006, American Society for Microbiology. All Rights Reserved.

Boosting of Cellular Immunity against Mycobacterium tuberculosis and Modulation of Skin Cytokine Responses in Healthy Human Volunteers by Mycobacterium bovis BCG Substrain Moreau Rio de Janeiro Oral Vaccine

St George's Vaccine Institute, St George's Hospital Medical School, London, United Kingdom,¹ Fundação Ataulpho de Paiva/IOC-FIOCRUZ, Rio de Janeiro, Brazil,² Center for Molecular Microbiology and Immunology, Imperial College, London, United Kingdom,³ Wellcome Trust Genome Campus, Sanger Institute, Cambridge, United Kingdom⁴

Received 30 August 2005/ Returned for modification 13 November 2005/ Accepted 23 January 2006

	ABSTRACT

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Oral immunization of healthy adults with 10⁷ CFU BCG Moreau Rio de Janeiro was well tolerated and significantly boosted gamma interferon responses to purified protein derivative, Ag85, and MPB70 from previous childhood intradermal BCG immunization. Oral BCG offers the possibility of a needle-free tuberculosis vaccine and of boosting the protective immunity from intradermal tuberculosis vaccines.

	TEXT

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DNA, recombinant viruses (13), subunit proteins, and genetically modified mycobacteria (2, 4, 5, 15) are being developed as vaccines against adult pulmonary tuberculosis, but down-selection of candidates will be slow, expensive, and contentious. A vaccine based on an adaptation of existing technology that could enter the market rapidly is therefore attractive. As a booster vaccine for infants, or immunocompetent adults or adolescents, to extend the protection afforded by neonatal BCG (19) will almost certainly be required, a "BCG-plus" strategy is gaining attention. M. bovis naturally spreads via the gastrointestinal tract, and BCG was developed by Calmette and Guérin as an oral vaccine. In Brazil, Assis demonstrated that repeated oral doses of BCG Moreau were highly effective in preventing tuberculosis (1), and Brazil routinely employed single-dose oral immunization with 100 mg of BCG Moreau up to the mid-1970s. We used the oral vaccine, still licensed for children and adults in Brazil, prepared from a World Health Organization-defined seed lot designated Mycobacterium bovis BCG substrain Moreau Rio de Janeiro, cultured in a proprietary Sauton medium, suspended in 5 ml 1.5% sodium glutamate solution, and presented as a single 100-mg dose that we found to contain between 3.4 x 10⁷ and 7.3 x 10⁷ CFU viable bacilli. BCG Moreau substrains retain the RD2 sequence deleted from BCG Pasteur but have a unique RD16 deletion and characteristically do not produce cervical adenitis, otitis media, or retropharyngeal abscess after oral delivery (12), even after repeated high doses during cancer chemotherapy (18).

Subjects, immunization, and reactogenicity. The phase 1 study protocol was approved by the Wandsworth Local Research Ethics Committee (reference 00.60.03) and the UK MCA/MHRA (MF8000/10030). All subjects provided written informed consent. Fifteen minutes after receiving 100 ml of 2% sodium bicarbonate buffer, 29 healthy volunteers (12 male, 17 female; mean age, 25), all of whom had received intradermal BCG in childhood or adolescence, received a single oral 100-mg dose of BCG, mixed with bicarbonate buffer. The vaccine was extremely well tolerated with no vaccine-related serious adverse events. Eight subjects (28%) reported mild to moderate, transient odynophagia, 9 (29%) reported headache, and 6 (21%) reported gastrointestinal symptoms related to bicarbonate buffer (which we used to abolish gastric acid but which the manufacturer's data sheet does not routinely recommend, and its omission could increase palatability and eliminate the requirement for clean water to dispense). Clinical examination, including ear, nose, and throat inspection, and C-reactive protein levels of subjects reporting odynophagia after immunization were normal.

Immune responses induced by immunization. Antigen-specific peripheral blood mononuclear cells (PBMCs) secreting gamma interferon (IFN-) were detected by ELISPOT based on that reported by Lalvani et al. (10), in which unfractionated PBMCs are stimulated for 18 h with M. tuberculosis antigens (purified protein derivative [PPD], Statens Serum Institute, Copenhagen, Denmark; MPB70 recombinant protein, Lionex, Braunschweig, Germany; ESAT-6 recombinant protein, antigen 85 complex, gift from NIH, NIAID, Tuberculosis Research Materials and Vaccine Testing contract no. NO1 AI-75320). The background activity of IFN--secreting cells in control wells was constant (data not shown). As all subjects had previously received intradermal BCG, PBMCs secreting IFN- in response to PPD were detectable prior to immunization (Fig. 1), and boosting of this baseline frequency was observed from day 7 after a single oral dose of liquid vaccine, sustained throughout the 9 months of follow-up, and significantly raised from baseline at months 1 and 3 in a strict per-protocol analysis. MPB70 accounts for as much as 10% of BCG Moreau culture filtrate but is expressed to a much lower level in BCG Glaxo (14), which would have been the strain subjects had previously received. Consequently, IFN--secreting cells responding to MPB70 were not detectable before immunization but appeared following oral immunization, peaking at day 28 (P < 0.01 from day 0), followed by a gradual decline to a plateau, which was still raised from baseline at 9 months. The ability of oral BCG to stimulate an immune response to this internal secreted antigen provides encouragement for development of recombinant BCG (rBCG) vaccines expressing heterologous antigens. Ag85 is a highly immunogenic major secretion product of many mycobacterial strains (20) and is being exploited in subunit and recombinant live tuberculosis vaccine candidates. PBMCs secreting IFN- in response to Ag85 were detectable prior to immunization, and there were increases to peak mean numbers of 460 per 10⁶ on day 7 after immunization for the whole group and 373 per 10⁶ at 3 months when only per-protocol subjects were analyzed (Fig. 1). This is similar to that obtained recently with modified vaccinia Ankara-Ag85 as a single-antigen delivery system to boost prior intradermal BCG immunization (peak 783 per 10⁶), although in that study the numbers fell sharply after day 7 (13). ESAT-6 is coded in the RD1 gene segment, which has been deleted from BCG, and an immune response to this antigen has been used to differentiate exposure to M. tuberculosis from that to BCG (10). Although sporadic low-level background activity could be detected, there was no discernible increase in the frequency of IFN--secreting cells after immunization (Fig. 1), indicating that exposure to other mycobacteria was not the cause of the immune responses we observed.

View larger version (30K): [in this window] [in a new window]   FIG. 1. Frequency of PBMCs secreting IFN- in response to mycobacterial antigens at primary protocol time points after oral immunization with BCG. Values are frequency of IFN--secreting cells per 106 PBMCs (corrected for background activity in wells without antigen) for 13 subjects with complete data sets at primary protocol time points after oral immunization. Columns are group means. Error bars are standard errors of the means. Differences from day 0 were analyzed using GraphPad Prism by repeated-measures one-way analysis of variance and corrected by Dunnett's test for multiple comparisons.

View larger version (25K): [in this window] [in a new window]   FIG. 2. Relative quantity of cytokine mRNA in skin biopsies of Heaf tests before and after oral liquid BCG vaccine. Values indicate relative amounts of cytokine RNA extracted from skin biopsies taken 7 days after a standard tuberculin Heaf test, either before oral BCG immunization or 1 month after. Subject V039, diamonds; subject V040, circles; subject V041, squares; subject V043, triangles. ND, not detected. All cytokine mRNAs were assessed relative to a standard control RNA except V039 IFN-, which used a different control RNA (indicated by dotted line). No preimmunization results on V041 for IL-1 and -ß, IL-2, IL-12p40, and IL-15 were available due to insufficient sample. The y axes are plotted on a logarithmic scale.

	ACKNOWLEDGMENTS

 
This work was supported by Wellcome Trust Programme grant 043139 and the Commission of the European Union Integrated Project ‘MUVAPRED,’ contract number LSHP-CT-2003-503240.

	FOOTNOTES

 
* Corresponding author. Mailing address: CMM (Infectious Diseases), St George's Hospital Medical School, Cranmer Terrace, London SW17 0RE, United Kingdom. Phone: 44 208 7255826. Fax: 44 208 7253487. E-mail: d.lewis{at}sghms.ac.uk.

Editor: J. L. Flynn

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This Article Abstract Full Text (PDF) Alert me when this article is cited Alert me if a correction is posted Services Similar articles in this journal Similar articles in PubMed Alert me to new issues of the journal Download to citation manager Reprints and Permissions Copyright Information Books from ASM Press MicrobeWorld Citing Articles Citing Articles via Google Scholar Google Scholar Articles by Cosgrove, C. A. Articles by Lewis, D. J. M. Search for Related Content PubMed PubMed Citation Articles by Cosgrove, C. A. Articles by Lewis, D. J. M.