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Research:
The Smith Lab are pursuing the mechanisms by which genetic variation in the host alters the immune pressures experienced by Mycobacterium tuberculosis. By understanding how these interactions drive specific arms of immunity, new host-pathogen paired vaccines and therapeutics can be rationally designed.
We leverage host diversity in mice and macrophages from wild-derived mouse strains and diverse mouse panels, including the Collaborative Cross, Diversity Outbred and BxD resources. In parallel, we define the bacterial requirements for growth and adaptation in these diverse host environments through bacterial genetics approaches, including libraries of transposon mutants (TnSeq), CRISPRi and knockouts generated through ORBIT (“oligonucleotide-mediated recombineering followed by Bxb1 integrase targeting”).
Altogether, using these Systems Genetics approaches, we aim to identify host loci that control specific aspects of the host-pathogen microenvironment, that can potentially be targeted by new vaccination strategies and therapeutic intervention.
The Smith Lab are pursuing the mechanisms by which genetic variation in the host alters the immune pressures experienced by Mycobacterium tuberculosis. By understanding how these interactions drive specific arms of immunity, new host-pathogen paired vaccines and therapeutics can be rationally designed.
We leverage host diversity in mice and macrophages from wild-derived mouse strains and diverse mouse panels, including the Collaborative Cross, Diversity Outbred and BxD resources. In parallel, we define the bacterial requirements for growth and adaptation in these diverse host environments through bacterial genetics approaches, including libraries of transposon mutants (TnSeq), CRISPRi and knockouts generated through ORBIT (“oligonucleotide-mediated recombineering followed by Bxb1 integrase targeting”).
Altogether, using these Systems Genetics approaches, we aim to identify host loci that control specific aspects of the host-pathogen microenvironment, that can potentially be targeted by new vaccination strategies and therapeutic intervention.
研究兴趣
论文共 48 篇作者统计合作学者相似作者
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Adrian Jinich,Anisha Zaveri,Michael A DeJesus, Amanda Spencer, Ricardo Almada-Monter,Emanuel Flores-Bautista,Clare M Smith,Christopher M Sassetti,Jeremy M Rock,Sabine Ehrt,Dirk Schnappinger,Thomas R Ioerger,Kyu Y Rhee
Molecular microbiology (2025)
Rachel K Meade, Oyindamola O Adefisayo, Marco T P Gontijo, Summer J Harris,Charlie J Pyle, Kaley M Wilburn, Alwyn M V Ecker, Erika J Hughes, Paloma D Garcia, Joshua Ivie,Michael L McHenry, Penelope H Benchek,Harriet Mayanja-Kizza, Jadee L Neff,Dennis C Ko,Jason E Stout,Catherine M Stein,Thomas R Hawn,David M Tobin,Clare M Smith
bioRxiv the preprint server for biology (2025)
Matthew W. Blanchard,John Sebastian Sigmon,Jennifer Brennan, Chidima Ahulamibe, Michelle E. Allen, Sam Ardery,Ralph S. Baric,Timothy A. Bell,Joseph Farrington,Dominic Ciavatta,Marta C. Cruz Cisneros, Madison Drushal,Martin T. Ferris,Rebecca C. Fry,Christiann Gaines,Bin Gu,Mark T. Heise,Pablo Hock, Richard Austin Hodges, Mia Hulgin,Tal Kafri,Rachel M. Lynch,Terry Magnuson,Darla R. Miller, Caroline E. Y. Murphy,David Truong Nguyen,Kelsey E. Noll,Megan K. Proulx,Christopher M. Sassetti,Sarah A. Schoenrock,Ginger D. Shaw,Jeremy M. Simon,Clare M. Smith,Miroslav Styblo,Lisa M. Tarantino, Joyce Woo,Fernando Pardo Manuel de Villena
G3-GENES GENOMES GENETICSno. 10 (2024)
Trends in Microbiology (2024)
International Journal of Molecular Sciencesno. 3 (2023): 2861-2861
Nuria Martinez,Lorissa J. Smulan, Michael L. Jameson,Clare M. Smith,Kelly Cavallo,Michelle Bellerose, John Williams,Kim West,Christopher M. Sassetti,Amit Singhal,Hardy Kornfeld
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作者统计
#Papers: 48
#Citation: 2884
H-Index: 25
G-Index: 36
Sociability: 6
Diversity: 3
Activity: 8
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