Targeted delivery of an ADP-ribosylating bacterial toxin into cancer cells

Zahaf, Nour Imene; Lang, Alexander E.; Kaiser, Lars; Fichter, Christiane D.; Laßmann, Silke; McCluskey, Andrew J.; Augspach, Anke; Aktories, Klaus; Schmidt, Gudula

doi:10.1038/srep41252

Cited by 22 publications

(20 citation statements)

References 33 publications

(40 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…EGFRs are highly convenient for the targeted delivery of various drugs into cancer cells. A number of drug delivery vehicles were produced for this purpose and evaluated in vitro and in vivo [ (Chen et al, 2002;Lu et al, 2005;Liu et al, 2010;Song et al, 2016;Slastnikova et al, 2017b;Zahaf et al, 2017;Rosenkranz et al, 2018), etc.]. The main areas of EGFR-targeted drug therapy include: (1) development of drugs based on anti-EGFR antibodies binding to the extracellular EGFR domain, preventing ligand binding, and interrupting signal cascades (Herbst, 2004;Friedman and Stahl, 2009;Scott et al, 2012); (2) tyrosine kinase inhibitors binding to the intracellular EGFR domain and inhibiting the downstream effects of EGFR ligand binding (Herbst, 2004;Dassonville et al, 2007;Gazdar, 2009); and (3) delivery of drugs to cancer cells by fusion constructs containing EGF (Scott et al, 2012).…”

Section: Discussionmentioning

confidence: 99%

“…Based on the data obtained, numerous attempts have been made to create a drug where EGFR would be used as a vehicle for various agents, such as, for example, Auger-electron emitter 111 In, Staphylococcal enterotoxin A, etc. Several therapeutic approaches exploiting EGFR for this purpose have been evaluated in vitro and in vivo (Chen et al, 2002;Song et al, 2016;Zahaf et al, 2017;Liu et al, 2018).…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Targeted Delivery of 111In Into the Nuclei of EGFR Overexpressing Cells via Modular Nanotransporters With Anti-EGFR Affibody

et al. 2020

View full text Add to dashboard Cite

Since cell nucleus is one of the most vulnerable compartments, the maximum therapeutic effect from a variety of locally acting agents, such as photosensitizers, alfa-emitters, Auger electron emitters, will be expected when they get there. Therefore, the targeted delivery of these agents into the nuclei of target tumor cells is necessary for their anticancer effects and minimization of side effects. Modular nanotransporters (MNT) are artificial polypeptides comprising several predefined modules that recognize target cell, launching their subsequent internalization, escape from endosomes, and transport the drug load to the nucleus. This technology significantly enhances the cytotoxicity of locally acting drugs in vitro and in vivo. Epidermal growth factor receptors (EGFR) are useful molecular targets as they are overexpressed in glioblastoma, head-and-neck cancer, bladder cancer, and other malignancies. Here, we examined the possibility of using internalizable anti-EGFR affibody as an EGFR-targeting MNT module for drug transport into the cancer cell nuclei. It binds to both murine and human EGFR facilitating preclinical studies. We showed that MNT with affibody on the N-terminus (MNT N-affibody ) effectively delivered the Auger electron emitter 111 In to target cell nuclei and had pronounced cytotoxic efficacy against EGFR-overexpressing human A431 epidermoid carcinoma cells. Using EGFR-expressing human adenocarcinoma MCF-7 cells, we demonstrated that in contrast to MNT with N-terminal epidermal growth factor (EGF), MNT N-affibody and MNT with EGF on the C-terminus did not stimulate cancer cell proliferation.

show abstract

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Targeted Delivery of 111In Into the Nuclei of EGFR Overexpressing Cells via Modular Nanotransporters With Anti-EGFR Affibody

et al. 2020

View full text Add to dashboard Cite

show abstract

“…Recombinant wild-type and mutant Ras proteins were expressed in E. coli with an N-terminal GST-tag as described by [ 48 ]. PA and LFN-TpeL were expressed with a His-tag as described before [ 49 ].…”

Section: Methodsmentioning

confidence: 99%

Targeting oncogenic Ras by the Clostridium perfringens toxin TpeL

et al. 2018

View full text Add to dashboard Cite

Clostridium perfringens toxin TpeL belongs to the family of large clostridial glycosylating toxins. The toxin causes N-acetylglucosaminylation of Ras proteins at threonine35 thereby inactivating the small GTPases. Here, we show that all main types of oncogenic Ras proteins (H-Ras, K-Ras and N-Ras) are modified by the toxin in vitro and in vivo. Toxin-catalyzed modification of Ras was accompanied by inhibition of the MAP kinase pathway. Importantly, TpeL inhibited the paradoxical activation of the MAP kinase pathway induced by the BRAF inhibitor Vemurafenib in the human melanoma cell line SBCL2. The toxin also blocked Ras signaling in a zebrafish embryo model expressing oncogenic H-RasG12V, resulting in a reduction of melanocyte number. By using the binding and translocation component of anthrax toxin (protective antigen), the glucosyltransferase domain of TpeL was effectively introduced into target cells that were not sensitive to native TpeL toxin. To reach a higher specificity towards cancer cells, a chimeric TpeL toxin was engineered that possessed the knob region of adenovirus serotype 35 fiber, which interacts with CD46 of target cells frequently overexpressed in cancer cells. The chimeric TpeL fusion toxin efficiently inhibited Ras and MAP kinases in human pancreatic cancer Capan-2 cells, which were insensitive to the wild-type toxin. The data reveal that TpeL and TpeL-related immunotoxins provide a new toolset as Ras-inactivating agents.

show abstract

“…More recently, the transport of a new chimeric effector via the mPA-EGF and mPA-ZHER2 transporters was shown ( Figure 3 ). This new chimera consists of the N-terminal part of LF linked to the catalytic part of an effector from the Photorhabdus luminescence toxin TccC3hvr (aa 679–960) [ 61 ]. TccC3 is an ADP-ribosyltransferase, which modifies actin at threonine 148.…”

Section: Anthrax Toxin As a Transportermentioning

confidence: 99%

“…This modification blocks the interaction of actin monomers with thymosin-β4, causing uncontrolled acting clustering and cell death. The LFN-C3 construct was transported selectively into the EGFR-overexpressing mid-esophageal cells OE21 via the mPA-EGF transporter and in the HER2 overexpressing low esophageal OE33 cells via the mPA-ZHER2 transporter, selectively eliminating the targeted cells [ 61 ]. Mouse studies are definitely required to validate the specific action of these targeted toxins in vivo.…”

Section: Anthrax Toxin As a Transportermentioning

confidence: 99%

Bacterial Toxins for Cancer Therapy

Zahaf

Schmidt

2017

Toxins

View full text Add to dashboard Cite

Several pathogenic bacteria secrete toxins to inhibit the immune system of the infected organism. Frequently, they catalyze a covalent modification of specific proteins. Thereby, they block production and/or secretion of antibodies or cytokines. Moreover, they disable migration of macrophages and disturb the barrier function of epithelia. In most cases, these toxins are extremely effective enzymes with high specificity towards their cellular substrates, which are often central signaling molecules. Moreover, they encompass the capacity to enter mammalian cells and to modify their substrates in the cytosol. A few molecules, at least of some toxins, are sufficient to change the cellular morphology and function of a cell or even kill a cell. Since many of those toxins are well studied concerning molecular mechanisms, cellular receptors, uptake routes, and structures, they are now widely used to analyze or to influence specific signaling pathways of mammalian cells. Here, we review the development of immunotoxins and targeted toxins for the treatment of a disease that is still hard to treat: cancer.

show abstract

Targeted delivery of an ADP-ribosylating bacterial toxin into cancer cells

Cited by 22 publications

References 33 publications

Targeted Delivery of 111In Into the Nuclei of EGFR Overexpressing Cells via Modular Nanotransporters With Anti-EGFR Affibody

Targeted Delivery of 111In Into the Nuclei of EGFR Overexpressing Cells via Modular Nanotransporters With Anti-EGFR Affibody

Targeting oncogenic Ras by the Clostridium perfringens toxin TpeL

Bacterial Toxins for Cancer Therapy

Contact Info

Product

Resources

About