Designed ankyrin repeat proteins are effective targeting elements for chimeric antigen receptors

Hammill, Joanne A.; VanSeggelen, Heather; Helsen, Christopher W.; Denisova, Galina; Evelegh, Carole; Tantalo, Daniela; Bassett, Jennifer; Bramson, Jonathan L.

doi:10.1186/s40425-015-0099-4

Cited by 64 publications

(52 citation statements)

References 30 publications

(36 reference statements)

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“…Indeed, they contain ankyrin repeats (ARs) which are one of the most common protein binding motifs found in nature (usually stretches of 33 aminoacid forming a β-turn and two anti-parallel α-helices). These can be engineered to bind efficiently Her2 providing an alternative to the 4D5 murine scFv-based CAR [176,177]. Similarly, adnectins are affinity molecules derived from a fibronectin domain and can serve as an alternative to scFv in CAR configuration [178] though the complex structure of the two last examples may trigger immunogenicity.…”

Section: Non Scfv-based Carsmentioning

confidence: 98%

T-cells “à la CAR-T(e)” – Genetically engineering T-cell response against cancer

Eisenberg

Hoogi

Shamul

et al. 2019

Advanced Drug Delivery Reviews

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Section: Non Scfv-based Carsmentioning

confidence: 98%

T-cells “à la CAR-T(e)” – Genetically engineering T-cell response against cancer

Eisenberg

Hoogi

Shamul

et al. 2019

Advanced Drug Delivery Reviews

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“…Conversely, a disadvantage of using scFv-binding domains is their tendency for oligomerization, which can lead to tonic signalling and T-cell exhaustion 17 . Alternative binding domains have been used in preclinical studies, including receptors 18 , ligands 19 , cytokines 20,21 , DARPins (designed ankyrin repeat proteins) 22 , adnectins 23 , Fc receptor fragments 24 , nanobodies 25 , peptides 26 and variable lymphocyte receptors 27 . The relative efficacy, safety and immunogenicity of these alternative binders have not yet been fully investigated and are the focus of substantial ongoing work.…”

Section: Review Articlementioning

confidence: 99%

Programming CAR-T cells to kill cancer

2018

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T cells engineered to express chimeric antigen receptors (CARs) that are specific for tumour antigens have led to high complete response rates in patients with haematologic malignancies. Despite this early success, major challenges to the broad application of CAR-T cells as cancer therapies remain, including treatment-associated toxicities and cancer relapse with antigen-negative tumours. Targeting solid tumours with CAR-T cells poses additional obstacles because of the paucity of tumourspecific antigens and the immunosuppressive effects of the tumour microenvironment. To overcome these challenges, T cells can be programmed with genetic modules that increase their therapeutic potency and specificity. In this Review Article, we survey major advances in the engineering of next-generation CAR-T therapies for haematologic cancers and solid cancers, with particular emphasis on strategies for the control of CAR specificity and activity and on approaches for improving CAR-T-cell persistence and overcoming immunosuppression. We also lay out a roadmap for the development of off-the-shelf CAR-T cells.

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“…DARPins are more compact than scFv and are thermodynamically stable. They do not need VH‐VL pairing to bind targets specifically . They do not contain cysteine; hence, they are resistant to protease and can be expressed in bacteria.…”

Section: Anit‐her2 Mabs and Derivativesmentioning

confidence: 99%

“…They do not need VH-VL pairing to bind targets specifically. [95] They do not contain cysteine; hence, they are resistant to protease and can be expressed in bacteria. Because of their small size, penetrate better in tumour cells.…”

Section: Darpin-pe40 and 4d5 Scfv-pe40mentioning

confidence: 99%

Monoclonal antibody-based therapeutics, targeting the epidermal growth factor receptor family: from herceptin to Pan HER

Moradi‐Kalbolandi

Hosseinzade

Salehi

et al. 2018

Journal of Pharmacy and Pharmacology

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Objectives Monoclonal antibody-based of cancer therapy has been considered as one of the most successful therapeutic strategies for both haematologic malignancies and solid tumours in the last two decades. Epidermal growth factor receptor (EGFR) family signalling pathways play a key role in the regulation of cell proliferation, survival and differentiation. Hence, anti-EGFR family mAbs is one of the most promising approaches in cancer therapy. Key findings Here, recent advances in anti-EGFR mAb including approved or successfully tested in preclinical and clinical studies have been reviewed. Although we focus on monoclonal antibodies against the EGF receptor, but the mechanisms underlying the effects of EGFR-specific mAb in cancer therapy, to some extend the resistance to existing anti-EGFR therapies and some therapeutic strategies to overcome resistance such as combination of mAbs on different pathways are briefly discussed as well. Summary The EGFR family receptors, is considered as an attractive target for mAb development to inhibit their consecutive activities in tumour growth and resistance. However, due to resistance mechanisms, the combination therapies may become a good candidate for targeting EGFR family receptors.

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Designed ankyrin repeat proteins are effective targeting elements for chimeric antigen receptors

Cited by 64 publications

References 30 publications

T-cells “à la CAR-T(e)” – Genetically engineering T-cell response against cancer

T-cells “à la CAR-T(e)” – Genetically engineering T-cell response against cancer

Programming CAR-T cells to kill cancer

Monoclonal antibody-based therapeutics, targeting the epidermal growth factor receptor family: from herceptin to Pan HER

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