α‐sarcin and <scp>RN</scp>ase T1 based immunoconjugates: the role of intracellular trafficking in cytotoxic efficiency

Tomé-Amat, Jaime; Ruiz-de-la-Herrán, Javier; Martínez‐del‐Pozo, Álvaro; Gavilanes, José G.; Lacadena, Javier

doi:10.1111/febs.13169

Cited by 13 publications

(33 citation statements)

References 68 publications

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“…The mechanism of action of ITs includes the binding of its target region to the tumor‐associated antigen (TAA), internalization of the complex through receptor‐mediated endocytosis, and subsequent release of toxic regions that can lead to the death of target cells 4,24 . Therefore, the antitumor effect of ITs depends on several factors: the affinity of Abs for TAA expressed on the cell surface, the rate of internalization of the complex, and the inherent efficacy and specificity of the toxin 25 .…”

Section: Discussionmentioning

confidence: 99%

Novel cucurmosin‐based immunotoxin targeting programmed cell death 1‐ligand 1 with high potency against human tumor in vitro and in vivo

et al. 2020

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Immunotoxins are Ab‐cytotoxin chimeric molecules with mighty cytotoxicity. Programmed cell death 1‐ligand 1 (PD‐L1), is a transmembrane protein expressed mainly in inflammatory tumor tissues and plays a pivotal role in immune escape and tumor progression. Although PD‐L1 immune checkpoint therapy has been successful in some cases, many patients have not benefited enough due to primary/secondary resistance. In order to optimize the therapeutic efficacy of anti‐PD‐L1 mAb, we used durvalumab as the payload and CUS245C, a type I ribosome‐inactivating protein isolated from Cucurbita moschata, as the toxin moiety, to construct PD‐L1‐specific immunotoxin (named D‐CUS245C) through the engineered cysteine residue. In vitro, D‐CUS245C selectively killed PD‐L1+ tumor cells. In vivo studies also showed that D‐CUS245C had obvious antitumor effect on PD‐L1+ human xenograft tumors in nude mice. In conclusion, in the combination of the toxin with mAb, this study developed a new immunotoxin targeting PD‐L1, emphasizing a novel and promising treatment strategy and providing a valuable way to optimize cancer immunotherapy.

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Section: Discussionmentioning

confidence: 99%

Novel cucurmosin‐based immunotoxin targeting programmed cell death 1‐ligand 1 with high potency against human tumor in vitro and in vivo

et al. 2020

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“…The toxicity of an immunotoxin depends on many molecular aspects, such as the antigen binding affinity, internalization rate, intracellular processing, toxin release and intrinsic toxicity. Accordingly, the intracellular trafficking of ribotoxin-based immunotoxins has been studied, showing how they are internalized via early endosomes, following different pathways depending on the toxin used until they reach the cytosol [ 13 , 75 ]. Finally, a step further in the therapeutic use of ribotoxin-based immunotoxins has been done showing the efficiency of the α-sarcin-based immunotoxin IMTXA33αs, which inhibits tumor growth as well as angiogenesis in nude mice harboring colon cancer xenografts [ 14 ] ( Figure 4 B).…”

Section: The Potential Biotechnological Uses Of Fungal Ribotoxinsmentioning

confidence: 99%

Fungal Ribotoxins: A Review of Potential Biotechnological Applications

Olombrada

Lázaro-Gorines

López-Rodríguez

et al. 2017

Toxins

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Fungi establish a complex network of biological interactions with other organisms in nature. In many cases, these involve the production of toxins for survival or colonization purposes. Among these toxins, ribotoxins stand out as promising candidates for their use in biotechnological applications. They constitute a group of highly specific extracellular ribonucleases that target a universally conserved sequence of RNA in the ribosome, the sarcin-ricin loop. The detailed molecular study of this family of toxic proteins over the past decades has highlighted their potential in applied research. Remarkable examples would be the recent studies in the field of cancer research with promising results involving ribotoxin-based immunotoxins. On the other hand, some ribotoxin-producer fungi have already been studied in the control of insect pests. The recent role of ribotoxins as insecticides could allow their employment in formulas and even as baculovirus-based biopesticides. Moreover, considering the important role of their target in the ribosome, they can be used as tools to study how ribosome biogenesis is regulated and, eventually, may contribute to a better understanding of some ribosomopathies.

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“…). Previous studies with other immunoconjugates based on scFvA33 have revealed how, when fused to RNaseT1, they follow a pathway via lysosomes and the Golgi apparatus, whereas, when using α‐sarcin, the immunotoxin is only internalized via the Golgi apparatus . In the case of IMTXA33HtA3ΔW, the immunotoxin follows a pathway involving both systems, as shown by the confocal microscopy assays (Fig.…”

Section: Resultsmentioning

confidence: 71%

“…Colocalization of IMTXA33HtA3DW with both the Golgi and lysosomes was observed ( Fig. 6), which would affect release to the cytosol, as described for scFvA33 immunoconjugates based on a-sarcin and RNase T1 [27]. IMTXA33HtA3DW showed specific cytotoxicity against GPA33-positive cells with an IC 50 of approximately 0.5 lM (Fig.…”

Section: Discussionmentioning

confidence: 69%

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Preparation of an engineered safer immunotoxin against colon carcinoma based on the ribotoxin hirsutellin A

et al. 2015

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Immunotoxins are chimeric proteins composed of an antibody domain that specifically directs the action of the toxic domain, resulting in the death of the targeted cells. Over recent years, immunotoxins have been widely studied and the number of different constructions has increased exponentially. Protein engineering has allowed the design of optimized versions of immunotoxins with an improved tumor binding affinity, stability or cytotoxic efficacy, although sometimes this has compromised the safety of the patient in terms of undesirable adverse secondary reactions. A triple mutant at three Trp residues (HtA3ΔW) of the ribotoxin hirsutellin A retains its specific ribonucleolytic activity, although cell internalization capacity is lacking. This toxin variant has been fused to the single chain variable fragment A33 (scFvA33). This immunoconjugate (IMTXA33HtA3ΔW) was produced in the methylotrophic yeast Pichia pastoris and purified using nickel‐nitrilotriacetic acid affinity chromatography. Both target and toxic domains were characterized. The immunotoxin showed an exquisite specific binding against GPA33‐positive culture cells, which results in the death of the targeted cells because of specific ribonucleolytic activity against ribosomes of the engineered hirsutellin A variant. IMTXA33HtA3ΔW represents a promising structure in the search for an improved immunotoxin without compromising the safety of patients.

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α‐sarcin and RNase T1 based immunoconjugates: the role of intracellular trafficking in cytotoxic efficiency

Cited by 13 publications

References 68 publications

Novel cucurmosin‐based immunotoxin targeting programmed cell death 1‐ligand 1 with high potency against human tumor in vitro and in vivo

Novel cucurmosin‐based immunotoxin targeting programmed cell death 1‐ligand 1 with high potency against human tumor in vitro and in vivo

Fungal Ribotoxins: A Review of Potential Biotechnological Applications

Preparation of an engineered safer immunotoxin against colon carcinoma based on the ribotoxin hirsutellin A

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