Â鶹AV

Michael B. Reed

Michael B. Reed, Ph.D.
Associate Professor

Research Institute of the Â鶹AV Health Centre
Glen Site
1001 Boulevard Décarie
Block E
Office EM3.3226
IDIGH Mail Drop Point #EM33211
Montréal, Québec, Canada H4A 3J1

Tel: (514) 934-1934 Ext. 43641
michael.reed [at] mcgill.ca

Research


Focus

The research of my laboratory focuses on molecular aspects of the pathogenesis of Mycobacterium tuberculosis, the bacterial agent responsible for the infectious disease, tuberculosis (TB). Despite the existence of effective antibacterial drugs and a partially effective vaccine for more than half a century, TB still remains the cause of 2 million deaths worldwide each year - the most due to any single infectious agent. This situation reflects very poorly on the current level of understanding of the pathogenic processes associated with this important pathogen.

Although early studies considered TB strains to be restricted in terms of their genetic and antigenic variability, more recent evidence indicates that M. tuberculosis has evolved into several genetically diverse lineages of strains that are likely to possess unique attributes related to the transmission and development of disease. My laboratory utilizes a combination of microbial genetics, biochemistry and whole animal (mouse) in vivo infection studies to investigate the array of metabolic and virulence strategies available to this phenotypically diverse pathogen. Increasing our knowledge and understanding of this diversity will greatly enhance future efforts aimed at developing new strategies to successfully diagnose and treat TB disease.

Keywords

ÌýTuberculosis, Mycobacterium tuberculosis, molecular microbiology, bacterial pathogenesis

Selected PublicationsÌý- Ìý Ìý Ìý Ìý Ìý Ìý Ìý Ìý

Ìý

  1. Lee RS, Radomski N, Proulx JF, Manry J, McIntosh F, Desjardins F, Soualhine H, DomenechP, Reed MB, Menzies D & Behr MA (2015).Ìý Re-emergence and amplification of tuberculosis in the Canadian arctic. The Journal of Infectious Diseases [doi: 10.1093/infdis/jiv011; Epub ahead of print].
  2. Domenech P, Rog A, Moolji J, Radomski N, Fallow A, Leon-Solis L, Bowes J, Behr MA & ReedÌýMB (2014).Ìý The origins of a 350-kilobase genomic duplication in MycobacteriumÌýtuberculosis and its impact on virulence.Ìý Infection and Immunity 82: 2902-2912.

  3. Hansen JM, Golchin SA, Veyrier FJ, Domenech P, Boneca IG, Azad AK, Rajaram MV,ÌýSchlesinger LS, Divangahi M, Reed MB & Behr MA (2014).Ìý N-glycolylated peptidoglycanÌýcontributes to the immunogenicity but not pathogenicity of Mycobacterium tuberculosis. The Journal of Infectious Diseases 209: 1045-1054.

  4. Albanna AS, Reed MB, Kotar KV, Fallow A, McIntosh FA, Behr MA & Menzies D (2011).ÌýReduced transmissibility of East African Indian strains of Mycobacterium tuberculosis.Ìý PLoSÌýONE 6: e25075.

  5. Domenech P, Kolly GS, Leon-Solis L, Fallow A & Reed MB (2010).Ìý Massive gene duplicationÌýevent among clinical isolates of the Mycobacterium tuberculosis W/Beijing family. JournalÌýof Bacteriology 192: 4562-4570.

  6. Fallow A, Domenech P & Reed MB (2010).Ìý Strains of the East Asian (W/Beijing) lineage ofÌýMycobacterium tuberculosis are DosS/DosT-DosR two-component regulatory systemÌýnatural mutants. Journal of Bacteriology 192: 2228-2238.

  7. Domenech P & Reed MB (2009).Ìý Rapid and spontaneous loss of phthiocerolÌýdimycocerosate (PDIM) from Mycobacterium tuberculosis grown in vitro: implications forÌývirulence studies.Ìý Microbiology 155: 3532-3543.

External Links

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