Capillary morphogenesis protein-2 is the major receptor mediating lethality of anthrax toxin in vivo

Liu, Shihui; Crown, Devorah; Miller-Randolph, Sharmina; Moayeri, Mahtab; Wang, Hailun; Hu, Hao; Morley, Thomas J.; Leppla, Stephen H.

doi:10.1073/pnas.0905409106

Cited by 147 publications

(234 citation statements)

References 34 publications

(41 reference statements)

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“…TEM8 was the first toxin receptor to be described (4) and continues to receive attention as a potential tumor marker. CMG2 appears to be expressed more widely in tissues, has a higher affinity for PA (6), and in our work has been found to be more important for both bacterial pathogenesis (8,22) and tumor targeting (16,21).…”

Section: Discussionmentioning

confidence: 83%

“…Lethality of PA Variants for Receptor-deficient Mice-The CMG2 Ϫ/Ϫ and TEM8 Ϫ/Ϫ C57BL/6 mice used here were described previously (6,8). These mice and littermate control mice (all 8 -10 weeks old) were challenged intraperitoneally with two doses of PA or PA variants along with FP59 (in 0.5 ml of PBS; doses indicated in the tables and figures) with a 2-day interval.…”

Section: Methodsmentioning

confidence: 99%

“…CHO cells were grown in minimum essential medium ␣ with 5% FBS, 2 mM glutamine, 5 mM HEPES, pH 7.4, and 50 g/ml gentamicin, with or without 300 g/ml hygromycin B. HeLa cells were cultured in Dulbecco's modified Eagle's medium with 10% FBS, 2 mM glutamine, and 50 g/ml gentamicin. MEF cells were isolated from embryonic day 13.5 embryos of the wild type, CMG2 Ϫ/Ϫ , TEM8 Ϫ/Ϫ and CMG2 Ϫ/Ϫ /TEM8 Ϫ/Ϫ mice (described below) as described previously (6) and cultured in Dulbecco's modified Eagle's medium with 10% FBS, 2 mM glutamine, and 50 g/ml gentamicin. MEF cells were passaged at 85-90% confluence by splitting 1:4 and used within the first six passages.…”

Section: Methodsmentioning

confidence: 99%

“…Measurement of PA Affinity for Receptors-Schild plot analyses were used as described previously (6,29) to determine the affinity (apparent K d ) of PA variant proteins for cellular receptors. Briefly, the nontoxic PA-U7, PA-U7 I656Q, PA-U7 I656V, and PA-U7 TSR proteins were used as competitors to block the toxicity of wild type PA to CHO cells.…”

Section: Methodsmentioning

confidence: 99%

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Anthrax Toxin Protective Antigen Variants That Selectively Utilize either the CMG2 or TEM8 Receptors for Cellular Uptake and Tumor Targeting

Chen

Liu

Leysath

et al. 2016

Journal of Biological Chemistry

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The protective antigen (PA) moiety of anthrax toxin binds to cellular receptors and mediates the translocation of the two enzymatic moieties of the toxin to the cytosol. Two PA receptors are known, with capillary morphogenesis protein 2 (CMG2) being the more important for pathogenesis and tumor endothelial marker 8 (TEM8) playing a minor role. The C-terminal PA domain 4 (PAD4) has extensive interactions with the receptors and is required for binding. Our previous study identified PAD4 variants having enhanced TEM8 binding specificity. To obtain PA variants that selectively bind to CMG2, here we performed phage display selections using magnetic beads having bound CMG2. We found that PA residue isoleucine 656 plays a critical role in PA binding to TEM8 but has a much lesser effect on PA binding to CMG2. We further characterized the role of residue 656 in distinguishing PA binding to CMG2 versus TEM8 by substituting it with the other 19 amino acids. Of the resulting variants, PA I656Q and PA I656V had significantly reduced activity on TEM8-expressing CHO cells but maintained their activity on CMG2-expressing CHO cells. The preference of these PA mutants for CMG2 over TEM8 was further demonstrated using mouse embryonic fibroblast cells and mice deficient in the CMG2 and/or the TEM8 receptors. The structural basis of the alterations in the receptor binding activities of these mutants is also discussed.Anthrax toxin is composed of three nontoxic proteins: protective antigen (PA), 3 lethal factor (LF), and edema factor (EF), which are released from Bacillus anthracis as monomers and assemble into toxic complexes on the surface of animal cells (1-3). PA is the moiety which binds to cell surface receptors and facilitates entry of the enzymatic EF and LF moieties into the host cell cytosol. Two anthrax toxin receptors have been identified; capillary morphogenesis protein 2 (CMG2, or anthrax toxin receptor 2) is the physiologically relevant toxin receptor mediating most of the in vivo toxicity of the toxin, whereas tumor endothelial marker 8 (TEM8, or anthrax toxin receptor 1) functions only as a minor anthrax toxin receptor (4 -8). Upon binding to the toxin receptors, PA is cleaved at the sequence 164 RKKR 167 by cell surface furin or furin-like proteases (9, 10), yielding the C-terminal 63-kDa fragment (PA63), which assembles to form a ring-shaped oligomer. The PA63 oligomer then binds LF and/or EF, and the toxin complex is internalized by receptor-mediated endocytosis. LF and EF are translocated into the cytosol from early or late endosomes to exert their cytotoxic effects. Therefore, PA plays the crucial role in anthrax toxin pathogenesis, serving as the delivery vehicle for translocation of LF and EF into the cytosol of the cell.The absolute requirement for cell surface proteolytic activation of PA for the toxin's action prompted our group and others to reengineer PA to make it depend on tumor-associated proteases for activation, thereby achieving high specificity for tumors (11)(12)(13)(14)(15). In a recent example, ...

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Section: Discussionmentioning

confidence: 83%

Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

See 2 more Smart Citations

Anthrax Toxin Protective Antigen Variants That Selectively Utilize either the CMG2 or TEM8 Receptors for Cellular Uptake and Tumor Targeting

Chen

Liu

Leysath

et al. 2016

Journal of Biological Chemistry

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“…It is not known if the octameric mutants adopt (1) an identical conformation to those previously described [85,87] and (2) display enhanced serum stability relative to the more physiological octamers, though their translocase activity has been documented both in vitro and in vivo [85,87]. The PA63 (7/8) complex interacts with cellular receptors including; capillary morphogenesis protein 2 (CMG2) [88], integrin beta-1 (ITGB1) [89] and tumour endothelial marker 8 (TEM8) [90] at the cell surface (Table 2). TEM8 and CMG2 are almost ubiquitously expressed throughout the body, and drive the capture, tissue distribution and internalisation of PA [91].…”

Section: Accessing the Cytosol Via Multivesicular Bodies (Mvbs)mentioning

confidence: 99%

The potential of toxin-based drug delivery systems for enhanced nucleic acid therapeutic delivery

Shorter¹,

Gollings²,

Gorringe-Pattrick³

et al. 2016

Expert Opinion on Drug Delivery

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Abstract.Introduction: The potential of gene replacement therapy has been underscored by the market authorisation of alipogene tiparvovec (Glybera) and GSK2696273 (Strimvelis) in the EU and recombinant adenovirus-p53 (Gendicine) in China. Common to these systems is the use of attenuated viruses for "drug" delivery. Whilst viral delivery systems are being developed for siRNA, their application to antisense delivery remains problematic. Non-viral delivery remains experimental, with some notable successes. However, stability and the "PEG dilemma", balancing toxicity and limited (often liver-tropic) PK-PD, with the membrane destabilising activity, necessary for nucleocytosolic access and transfection remain a problem. Areas Covered:Here we review the use of attenuated protein toxins as a delivery vehicle for nucleic acids, their relationship to the PEG-dilemma, and their biological properties with specific reference to their intracellular trafficking. Expert opinion:The possibility of using attenuated toxins as antisense and siRNA delivery systems has been demonstrated in vitro. Systems based upon attenuated anthrax toxin have been shown to have high activity (equivalent to nucleofection) and low toxicity whilst not requiring cationic "helpers" or condensing agents, divorcing these systems from the problems associated with the PEG dilemma. It remains to be seen whether these systems can operate safely, efficiently and reproducibly, in vivo or in the clinic. Key words.Antisense, Drug Delivery, Endocytosis, Gene Therapy, siRNA, Toxin. 1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 18 19 20 21 22 23 24 25 26 27 28 29 30 31 32 33 34 35 36 37 38 39 40 41 42 43 44 45 46 47 48 49 50 51 52 53 54 55 56 57 58 59 This paper covers:1) The deferential between the challenges associated with gene and siRNA / antisense delivery.2) Why this differential is important within the context of existing rate limits to nonviral therapy i.e. the PEG dilemma.3) The use of protein toxins as part of non-viral DNA delivery systems. 4) How toxins navigate the endomembrane system. 5) Recent successes using toxins to deliver siRNA and antisense oligonucleotides.

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Effect of endosomal acidification on small ion transport through the anthrax toxin PA₆₃ channel

et al. 2017

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Tight regulation of pH is critical for the structure and function of cells and organelles. The pH environment changes dramatically along the endocytic pathway, an internalization transport process that is 'hijacked' by many intracellularly active bacterial exotoxins, including the anthrax toxin. Here we investigate the role of pH on singlechannel properties of the anthrax toxin channel, PA 63 . Using conductance and current noise analysis, blocker binding, ion selectivity, and PEG partitioning measurements, we show that the channel exists in two different open states ('maximum' and 'main') at pH  5.5, while only a maximum conductance state is detected at pH  5.5. We describe two substantially distinct patterns of PA 63 conductance dependence on KCl concentration uncovered at pH 6.5 and 4.5.

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Capillary morphogenesis protein-2 is the major receptor mediating lethality of anthrax toxin in vivo

Cited by 147 publications

References 34 publications

Anthrax Toxin Protective Antigen Variants That Selectively Utilize either the CMG2 or TEM8 Receptors for Cellular Uptake and Tumor Targeting

Anthrax Toxin Protective Antigen Variants That Selectively Utilize either the CMG2 or TEM8 Receptors for Cellular Uptake and Tumor Targeting

The potential of toxin-based drug delivery systems for enhanced nucleic acid therapeutic delivery

Effect of endosomal acidification on small ion transport through the anthrax toxin PA₆₃ channel

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Capillary morphogenesis protein-2 is the major receptor mediating lethality of anthrax toxin in vivo

Cited by 147 publications

References 34 publications

Anthrax Toxin Protective Antigen Variants That Selectively Utilize either the CMG2 or TEM8 Receptors for Cellular Uptake and Tumor Targeting

Anthrax Toxin Protective Antigen Variants That Selectively Utilize either the CMG2 or TEM8 Receptors for Cellular Uptake and Tumor Targeting

The potential of toxin-based drug delivery systems for enhanced nucleic acid therapeutic delivery

Effect of endosomal acidification on small ion transport through the anthrax toxin PA63 channel

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Product

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About

Effect of endosomal acidification on small ion transport through the anthrax toxin PA₆₃ channel