PT - JOURNAL ARTICLE AU - Rocky Lai AU - Diana Gong AU - Travis Williams AU - Abiola F. Ogunsola AU - Kelly Cavallo AU - Cecilia S. Lindestam Arlehamn AU - Sarah Acolatse AU - Gillian L. Beamer AU - Martin T. Ferris AU - Christopher M. Sassetti AU - Douglas A. Lauffenburger AU - Samuel M. Behar TI - Host genetic background is a barrier to broadly effective vaccine protection: Relevance to BCG and <em>Mycobacterium tuberculosis</em> Infection AID - 10.1101/2022.09.19.508548 DP - 2022 Jan 01 TA - bioRxiv PG - 2022.09.19.508548 4099 - http://biorxiv.org/content/early/2022/11/29/2022.09.19.508548.short 4100 - http://biorxiv.org/content/early/2022/11/29/2022.09.19.508548.full AB - The heterogeneity of immune responses observed in humans is difficult to model in standard inbred laboratory mice. To capture the diversity inherent in mice and better understand how host variation affects BCG-induced immunity against Mycobacterium tuberculosis, 24 unique Collaborative Cross (CC) recombinant inbred mouse strains and the C57BL/6 reference strain were vaccinated with or without BCG, and then challenged with low-dose aerosolized virulent M. tuberculosis. In contrast to standard lab strains, BCG protected only half of the CC strains tested. Furthermore, BCG efficacy is dissociable from inherent susceptibility to TB. As these strains differed primarily in the genes and alleles they inherited from the CC founder strains, we conclude that the host genetic background has a major influence on whether BCG confers protection against M. tuberculosis infection and indicates that host genetics should be considered as an important barrier to vaccine-mediated protection. Importantly, we wished to identify the components of the immune response stimulated by BCG, which were subsequently recalled after Mtb infection and associated with protection. The T cell immune response following BCG vaccination and Mtb challenge was extensively characterized. Although considerable diversity was observed, BCG vaccination had little impact on the composition of T cells recruited and maintained in the lung after infection. Instead, the variability was largely shaped by the genetic background. We developed models to detect vaccine-induced differences, which identified immune signatures associated with BCG-elicited protection against TB. Importantly, even when categorized as susceptible vs. resistant, and protected vs. unprotected, many of the protected CC strains had unique flavors of immunity, indicating multiple paths to protection. Thus, CC mice can be used to define correlates of protection and to identify vaccine strategies that protect a larger fraction of genetically diverse individuals instead of optimizing protection for a single genotype.Competing Interest StatementThe authors have declared no competing interest.