A genetic strategy to identify targets for the development of drugs that prevent bacterial persistence

Kim, Jee Hyun; O’Brien, Kathryn M.; Sharma, Ritu; Boshoff, Helena I.; Rehren, Germán; Chakraborty, Sumit; Wallach, Joshua B.; Monteleone, Mercedes; Wilson, Daniel J.; Aldrich, Courtney C.; Barry, Clifton E.; Rhee, Kyu Y.; Ehrt, Sabine; Schnappinger, Dirk

doi:10.1073/pnas.1315860110

Cited by 136 publications

(158 citation statements)

References 43 publications

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“…pGMCH-T38S38-P750-mmpL3-DAS ϩ 4 achieves transcriptional regulation of DAS-tagged MmpL3 as mmpL3-DAS is transcribed using a promoter (P750), which contains a tet operator (tetO4C5G) that is recognized by TetR38. TetR38 is a reverse TetR that binds tetO4C5G in the presence of ATc (20) and thus transcriptionally represses mmpL3-DAS with ATc. pGMCH-T38S38-P750-mmpL3-DAS ϩ 4 causes hygromycin resistance and integrates into the L5 attachment site.…”

Section: Methodsmentioning

confidence: 99%

“…To investigate whether MmpL3 is required for the growth and persistence of M. tuberculosis in vitro and in vivo, we generated M. tuberculosis knockdown strains in which MmpL3 levels are regulated either exclusively at the transcriptional level or by a dual control (DUC) switch so that the chemical compound, ATc or doxycycline, triggers transcriptional repression of the mmpL3 gene and simultaneous degradation of the MmpL3 protein (20). Conditional knockdowns in the virulent (ATCC 25618) and avirulent (mc 2 6206) M. tuberculosis H37Rv backgrounds were generated as follows.…”

Section: Construction Of M Tuberculosis Conditional Mmpl3 Knockdown mentioning

confidence: 99%

“…1), MmpL3-DUC knockdowns were generated by transforming the merodiploid H37Rv strains with plasmid pGMCgSq19-TSC10M1-sspB, allowing for the expression of the E. coli adaptor protein SspB under the control of an ATc-inducible (TET-ON) promoter. The presence of a DAS ϩ 4 tag on MmpL3 is expected to target the cytosolic C-terminal domain of MmpL3 for proteolytic degradation by the ClpX protease upon coexpression of sspB, which allows the tagged proteins to be delivered to the protease (20,27). Because sspB is expressed under the control of a TET-ON promoter and mmpL3-DAS ϩ 4 under the control of a TET-OFF promoter in MmpL3-DUC, the addition of ATc to the culture medium is expected to simultaneously silence mmpL3-DAS ϩ 4 expression and turn on the expression of sspB, resulting in the C-terminal proteolytic degradation of MmpL3-DAS ϩ 4.…”

Section: Construction Of M Tuberculosis Conditional Mmpl3 Knockdown mentioning

confidence: 99%

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Therapeutic Potential of the Mycobacterium tuberculosis Mycolic Acid Transporter, MmpL3

Obregón-Henao

Wallach

et al. 2016

Antimicrob Agents Chemother

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103

122

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Section: Methodsmentioning

confidence: 99%

Section: Construction Of M Tuberculosis Conditional Mmpl3 Knockdown mentioning

confidence: 99%

Section: Construction Of M Tuberculosis Conditional Mmpl3 Knockdown mentioning

confidence: 99%

See 1 more Smart Citation

Therapeutic Potential of the Mycobacterium tuberculosis Mycolic Acid Transporter, MmpL3

Obregón-Henao

Wallach

et al. 2016

Antimicrob Agents Chemother

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103

122

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“…Recently, the hipAB system of Shewanella oneidensis was characterized, and a ternary HipAB-DNA complex different from the one from E. coli was observed (46). Since persister cells are highly problematic with respect to antibiotic treatments of infectious diseases, much emphasis has been placed on the development of drugs that suppress the development and survival of persister cells (47)(48)(49)(50)(51)(52)(53).…”

Section: Persister Cells As a Classical Model For Phenotypic Heterogementioning

confidence: 99%

Phenotypic Heterogeneity, a Phenomenon That May Explain Why Quorum Sensing Does Not Always Result in Truly Homogenous Cell Behavior

Grote

Krysciak

Streit

2015

Appl Environ Microbiol

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Phenotypic heterogeneity describes the occurrence of "nonconformist" cells within an isogenic population. The nonconformists show an expression profile partially different from that of the remainder of the population. Phenotypic heterogeneity affects many aspects of the different bacterial lifestyles, and it is assumed that it increases bacterial fitness and the chances for survival of the whole population or smaller subpopulations in unfavorable environments. Well-known examples for phenotypic heterogeneity have been associated with antibiotic resistance and frequently occurring persister cells. Other examples include heterogeneous behavior within biofilms, DNA uptake and bacterial competence, motility (i.e., the synthesis of additional flagella), onset of spore formation, lysis of phages within a small subpopulation, and others. Interestingly, phenotypic heterogeneity was recently also observed with respect to quorum-sensing (QS)-dependent processes, and the expression of autoinducer (AI) synthase genes and other QS-dependent genes was found to be highly heterogeneous at a single-cell level. This phenomenon was observed in several Gram-negative bacteria affiliated with the genera Vibrio, Dinoroseobacter, Pseudomonas, Sinorhizobium, and Mesorhizobium. A similar observation was made for the Gram-positive bacterium Listeria monocytogenes. Since AI molecules have historically been thought to be the keys to homogeneous behavior within isogenic populations, the observation of heterogeneous expression is quite intriguing and adds a new level of complexity to the QS-dependent regulatory networks. All together, the many examples of phenotypic heterogeneity imply that we may have to partially revise the concept of homogeneous and coordinated gene expression in isogenic bacterial populations. Bacteria have evolved multiple strategies to cope with rapid and frequent changes in their environment. These survival strategies may include spore formation, increased production of polysaccharides, biofilm formation or escape from biofilms (i.e., switching from a motile into a sessile form and vice versa), altered motility, change of metabolic capabilities, response to antibiotics, and many more. In general, these switches are initiated by environmental or bacterially produced signals that are perceived by a diverse array of regulators and delegated into the corresponding regulatory networks. This presumably results in altered transcription levels of different genes or operons, which eventually causes a change in the phenotype and a response to the environmental stimulus. Within this context, it is generally assumed that the majority of a population will undergo this switch within a short time period and that the population will show a mostly homogeneous expression profile. During the last decade, it became, however, evident that a certain fraction of cells in an isogenic population behaves differently from the others, even though the environment may not have changed significantly. The term "phenotypic heterogeneity" thereby descr...

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“…Other bacteria have evolved less extreme dormant states and instead adopt cell states with low metabolic activity such that these cells are better able to tolerate stresses such as antibiotic exposure or immune system assault (6). In addition to low metabolic activity, dormant cells of all types often have a cell wall architecture that differs from that of their vegetative counterparts.…”

mentioning

confidence: 99%

Resuscitation-Promoting Factors Are Cell Wall-Lytic Enzymes with Important Roles in the Germination and Growth of Streptomyces coelicolor

et al. 2015

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Dormancy is a common strategy adopted by bacterial cells as a means of surviving adverse environmental conditions. For Streptomyces bacteria, this involves developing chains of dormant exospores that extend away from the colony surface. Both spore formation and subsequent spore germination are tightly controlled processes, and while significant progress has been made in understanding the underlying regulatory and enzymatic bases for these, there are still significant gaps in our understanding. One class of proteins with a potential role in spore-associated processes are the so-called resuscitation-promoting factors, or Rpfs, which in other actinobacteria are needed to restore active growth to dormant cell populations. The model species Streptomyces coelicolor encodes five Rpf proteins (RpfA to RfpE), and here we show that these proteins have overlapping functions during growth. Collectively, the S. coelicolor Rpfs promote spore germination and are critical for growth under nutrient-limiting conditions. Previous studies have revealed structural similarities between the Rpf domain and lysozyme, and our in vitro biochemical assays revealed various levels of peptidoglycan cleavage capabilities for each of these five Streptomyces enzymes. Peptidoglycan remodeling by enzymes such as these must be stringently governed so as to retain the structural integrity of the cell wall. Our results suggest that one of the Rpfs, RpfB, is subject to a unique mode of enzymatic autoregulation, mediated by a domain of previously unknown function (DUF348) located within the N terminus of the protein; removal of this domain led to significantly enhanced peptidoglycan cleavage. Streptomyces species are Gram-positive bacteria that abound in soil environments. They are renowned for their secondary metabolic capabilities; they produce a multitude of compounds that have found utility in both medicine and agriculture, including a vast array of antibiotics, chemotherapeutics, immunosuppressants, and antiparasitic agents (1). They are also well known for their complex, multicellular developmental cycle (2). The Streptomyces life cycle can be broadly divided into two stages: vegetative growth and reproductive development. Unlike most bacteria, Streptomyces organisms are filamentous, and during the vegetative phase of their life cycle, they grow by hyphal tip extension and branching, ultimately forming an interwoven network of cells known as the vegetative mycelium (3). Under certain as yet poorly defined stress conditions, vegetative growth ceases, and reproductive growth ensues. Here, unbranched filamentous cells, termed aerial hyphae, grow away from the vegetative mycelium and extend into the air. These cells then undergo a synchronous round of chromosome segregation, cell division, and cell wall modification to yield chains of dormant exospores (4). These spores are resistant to a wide variety of environmental insults and can be widely dispersed.A dormant cell state is not unique to the streptomycetes, and indeed many well-studied bacteria (e...

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A genetic strategy to identify targets for the development of drugs that prevent bacterial persistence

Cited by 136 publications

References 43 publications

Therapeutic Potential of the Mycobacterium tuberculosis Mycolic Acid Transporter, MmpL3

Therapeutic Potential of the Mycobacterium tuberculosis Mycolic Acid Transporter, MmpL3

Phenotypic Heterogeneity, a Phenomenon That May Explain Why Quorum Sensing Does Not Always Result in Truly Homogenous Cell Behavior

Resuscitation-Promoting Factors Are Cell Wall-Lytic Enzymes with Important Roles in the Germination and Growth of Streptomyces coelicolor

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