Fragment-based discovery of selective inhibitors of the Mycobacterium tuberculosis protein tyrosine phosphatase PtpA

Rawls, Katherine A.; Lang, P. Therese; Takeuchi, Jun; Imamura, Shinichi; Baguley, Tyler D.; Grundner, Christoph; Alber, Tom; Ellman, Jonathan A.

doi:10.1016/j.bmcl.2009.10.090

Cited by 47 publications

(50 citation statements)

References 30 publications

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“…Chiradia et al identified synthetic chalcones as inhi bitors of PtpA, and in follow-up work elucidated structure-activity relationships and demonstrated inhibition by one compound of M. bovis BCG in human macrophages but not in axenic culture ( 108 – 110 ). A group that had previously identified PtpB inhibitors using a fragment-based approach applied this method to identify inhibitors of PtpA ( 111 ). The most potent of these ( K i = 1.4 μM) was also selective relative to human Tyr and dual-specificity kinases.…”

Section: Tuberculosis Stpks and Phosphatases As Potential Drug Tarmentioning

confidence: 99%

Mycobacterium tuberculosis Serine/Threonine Protein Kinases

Prisic

Husson

2014

Microbiol Spectr

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The Mycobacterium tuberculosis genome encodes 11 serine/threonine protein kinases (STPKs). A similar number of two-component systems are also present, indicating that these two signal transduction mechanisms are both important in the adaptation of this bacterial pathogen to its environment. The M. tuberculosis phosphoproteome includes hundreds of Ser- and Thr-phosphorylated proteins that participate in all aspects of M. tuberculosis biology, supporting a critical role for the STPKs in regulating M. tuberculosis physiology. Nine of the STPKs are receptor type kinases, with an extracytoplasmic sensor domain and an intracellular kinase domain, indicating that these kinases transduce external signals. Two other STPKs are cytoplasmic and have regulatory domains that sense changes within the cell. Structural analysis of some of the STPKs has led to advances in our understanding of the mechanisms by which these STPKs are activated and regulated. Functional analysis has provided insights into the effects of phosphorylation on the activity of several proteins, but for most phosphoproteins the role of phosphorylation in regulating function is unknown. Major future challenges include characterizing the functional effects of phosphorylation for this large number of phosphoproteins, identifying the cognate STPKs for these phosphoproteins, and determining the signals that the STPKs sense. Ultimately, combining these STPK-regulated processes into larger, integrated regulatory networks will provide deeper insight into M. tuberculosis adaptive mechanisms that contribute to tuberculosis pathogenesis. Finally, the STPKs offer attractive targets for inhibitor development that may lead to new therapies for drug-susceptible and drug-resistant tuberculosis.

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Section: Tuberculosis Stpks and Phosphatases As Potential Drug Tarmentioning

confidence: 99%

Mycobacterium tuberculosis Serine/Threonine Protein Kinases

Prisic

Husson

2014

Microbiol Spectr

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“…Compounds 6 and 7 can compete well with the potency and selectivity of earlier MptpA inhibitors. [25][26][27] …”

Section: Resultsmentioning

confidence: 98%

Dynamic Substrate Enhancement for the Identification of Specific, Second‐Site‐Binding Fragments Targeting a Set of Protein Tyrosine Phosphatases

2011

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Protein tyrosine phosphatases (PTPs) are key regulators in living systems and thus are attractive drug targets. The development of potent, selective PTP inhibitors has been a difficult challenge mainly due to the high homology of the phosphotyrosine substrate pockets. Here, a strategy of dynamic substrate enhancement is described targeting the secondary binding sites of PTPs. By screening four different PTPs from bacterial (MptpA) and human origin (PTP1B, HePtp, Shp2) with this assay, specific fragments were identified. One highly specific fragment that binds to the secondary site of Mycobacterium tuberculosis protein tyrosine phosphatase A (MptpA) was characterized in order to validate the assay concept. Finally by covalently linking the secondary fragment to a phosphotyrosine mimetic, a moderately active but highly specific inhibitor of MptpA was obtained.

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“…Although the deletion of any of the two PTPs does not affect the pathogen growth in cell culture, the identical deletions severely attenuate growth in infected host macrophages [90,94]. As the PTPs are not essential for the growth of the pathogen itself, but are essential for the modulation of host signaling pathways to allow the persistence of the pathogen in the infected host, the pharmacotherapeutic targeting of PtpA and PtpB must focus on the drug permeability in the host macrophage, but not in the M. tuberculosis (carrying the cell wall and efficient pump-mediated drug efflux systems [95]). …”

Section: Mycobacterium Tuberculosis -Two Ptps With Known Inhibitorsmentioning

confidence: 99%

“…(3)) (K i = 1.4 µM against PtpA) is selective when tested against a panel of human PTPs and DUSPs (>70-fold selective over human PTP1B, TC-PTP, VHR, CD45, and LAR; 11-fold selective over human LMW-PTP), and does not inhibit M. tuberculosis PtpB (>100-fold selectivity). Molecular modeling highlighted the importance of pi-stacking with Trp48 of PtpA for high-affinity binding [95]. Regarding PtpB inhibition, isoxazole carboxylic acid isostere 433 Da analogue (13) has K i 220 nM against PtpB (>100-fold selectivity over M. tuberculosis PtpA, as well as over human VHR and TC-PTP, 98-fold selectivity over human LAR, 35-fold selectivity over human CD45) [97].…”

Section: Mycobacterium Tuberculosis -Two Ptps With Known Inhibitorsmentioning

confidence: 99%

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Finding the Smoking Gun: Protein Tyrosine Phosphatases as Tools and Targets of Unicellular Microorganisms and Viruses

Heneberg

2012

CMC

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Protein tyrosine phosphatases (PTPs) are increasingly recognized as important effectors of host-pathogen interactions. Since Guan and Dixon reported in 1990 that phosphatase YopH serves as an essential virulence determinant of Yersinia, the field shifted significantly forward, and dozens of PTPs were identified in various microorganisms and even in viruses. The discovery of extensive tyrosine signaling networks in non-metazoan organisms refuted the moth-eaten paradigm claiming that these organisms rely exclusively on phosphoserine/phosphothreonine signaling. Similarly to humans, phosphotyrosine signaling is thought to comprise a small fraction of total protein phosphorylation, but plays a disproportionately important role in cell-cycle control, differentiation, and invasiveness. Here we summarize the state-of-art knowledge on PTPs of important non-metazoan pathogens (Listeria monocytogenes, Staphylococcus aureus, Porphyromonas gingivalis, Caulobacter crescentus, Yersinia, Synechocystis, Leishmania, Plasmodium falciparum, Entamoeba histolytica, etc.), and focus also at the microbial proteins affecting directly or indirectly the PTPs of the host (Mycobacterium tuberculosis MTSA-10, Bacillus anthracis anthrax toxin, streptococcal β protein, Helicobacter pylori CagA and VacA, Leishmania GP63 and EF-1α, Plasmodium hemozoin, etc.). This is the first review summarizing the knowledge on biological activity and pharmacological inhibition of non-metazoan PTPs, with the emphasis of those important in host-pathogen interactions. Targeting of numerous non-metazoan PTPs is simplified by the fact that they act either as ectophosphatases or are secreted outside of the pathogen. Interfering with tyrosine phosphorylation represents a powerful pharmacologic approach, and even though the PTP inhibitors are difficult to develop, lifting the fog of phosphatase inhibition is of the great market potential and further clinical impact.

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Fragment-based discovery of selective inhibitors of the Mycobacterium tuberculosis protein tyrosine phosphatase PtpA

Cited by 47 publications

References 30 publications

Mycobacterium tuberculosis Serine/Threonine Protein Kinases

Mycobacterium tuberculosis Serine/Threonine Protein Kinases

Dynamic Substrate Enhancement for the Identification of Specific, Second‐Site‐Binding Fragments Targeting a Set of Protein Tyrosine Phosphatases

Finding the Smoking Gun: Protein Tyrosine Phosphatases as Tools and Targets of Unicellular Microorganisms and Viruses

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