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The Achilles heel of BCG

Ian M. OrmeCorresponding Author Informationemail address

Received 9 April 2010; received in revised form 8 June 2010; accepted 24 June 2010. published online 26 July 2010.
Corrected Proof

Summary 

There have been multiple explanations put forward to try to explain the variable efficacy of the BCG vaccine. Here I propose the new hypothesis that the primary flaw of BCG is its inability to effectively establish a population of central memory T cells. Instead, the vaccine establishes immunity represented by effector memory T cells; these distribute in the lungs and may protect humans for 10–15 years but are gradually lost. With no central memory response to compensate, the individual loses any further resistance to tuberculosis. This may have serious implications for vaccine design, given the emphasis on developing recombinant forms of BCG.

Department of Microbiology, Immunology and Pathology, Colorado State University, Fort Collins, CO 80523, USA

Corresponding Author InformationTel.: +1 970 491 5777; fax: +1 970 491 5125.

PII: S1472-9792(10)00068-5

doi:10.1016/j.tube.2010.06.002

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