2017
DOI: 10.1038/nrmicro.2017.59
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Engineering of obligate intracellular bacteria: progress, challenges and paradigms

Abstract: It is estimated that approximately one billion people are at risk of infection with obligate intracellular bacteria, but little is known about the underlying mechanisms that govern their life cycles. The difficulty in studying Chlamydia spp., Coxiella spp., Rickettsia spp., Anaplasma spp., Ehrlichia spp. and Orientia spp. is, in part, due to their genetic intractability Recently, genetic tools have been developed; however, optimizing the genomic manipulation of obligate intracellular bacteria remains challengi… Show more

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Cited by 138 publications
(131 citation statements)
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“…Development of the mariner transposase Himar1, which can function in many organisms Pelicic et al, 2000;Ashour and Hondalus, 2003) and the development of hyperactive Himar1 mutants have effectively diminished this last obstacle. Himar transposition provides an ideal system for global genome functional analysis of the AT-rich organism like Ehrlichia species (Munderloh et al, 2012;Cheng et al, 2013;McClure et al, 2017), since it recognizes AT sites and inserts at a single site per genome . In the present study, we constructed HF strain Himar1 transposon mutant library, and cloned selected mutants and characterized cloned mutant pathogenicity in laboratory mice.…”
Section: Introductionmentioning
confidence: 99%
“…Development of the mariner transposase Himar1, which can function in many organisms Pelicic et al, 2000;Ashour and Hondalus, 2003) and the development of hyperactive Himar1 mutants have effectively diminished this last obstacle. Himar transposition provides an ideal system for global genome functional analysis of the AT-rich organism like Ehrlichia species (Munderloh et al, 2012;Cheng et al, 2013;McClure et al, 2017), since it recognizes AT sites and inserts at a single site per genome . In the present study, we constructed HF strain Himar1 transposon mutant library, and cloned selected mutants and characterized cloned mutant pathogenicity in laboratory mice.…”
Section: Introductionmentioning
confidence: 99%
“…These techniques can only diagnose bacterial infections when there has been significant systemic tissue damage,which poses challenges in treatment owing to the high bacterial burden despite the availability of antibiotics.T oc omplicate matters,s ome bacteria are able to survive inside the host cells,w hich render the available treatments ineffective,l eading to recurrent or chronic infections. [5] These intractable infections are difficult to treat owing to the challenge in detection and high resistance towards traditional antimicrobial therapies.T ot his end, the development of new strategies for detection and elimination of intracellular bacteria is highly attractive,w hich will have as ignificant impact in the treatment against bacterial infections.…”
Section: Introductionmentioning
confidence: 99%
“…The genomic simplicity of these organisms combined with their intimate relationship with their cellular hosts makes them attractive systems for studying bacterial physiology, host–pathogen biology, and questions about how bacteria sense and respond to their environment. Obligate intracellular bacteria are difficult to propagate in the laboratory, however, and are mostly genetically intractable 9 , thus our understanding of their biology lags behind that of free-living counterparts.…”
Section: Introductionmentioning
confidence: 99%