Bispecific antibodies targeting CD40 and tumor-associated antigens promote cross-priming of T cells resulting in an antitumor response superior to monospecific antibodies

Hägerbrand, Karin; Varas, Laura; Deronic, Adnan; Nyesiga, Barnabas; Sundstedt, Anette; Ljung, Lill; Sakellariou, Christina; Werchau, Doreen; Thagesson, Mia; Jimenez, David Gomez; Greiff, Lennart; Celander, Mona; Smedenfors, Kristine; Rosén, Anna; Bölükbas, Deniz A.; Carlsson, Fredrika; Levin, Mattias; Säll, Anna; Schantz, Laura von; Lindstedt, Malin; Ellmark, Peter

doi:10.1136/jitc-2022-005018

Cited by 11 publications

(17 citation statements)

References 28 publications

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“…The functionality of RUBY bsAbs was evaluated in a variety of assays. It was shown that a CD40-EpCAM RUBY bsAb displayed conditional CD40 activation in a reporter assay, similar to what has been shown by Hägerbrand et al 29 The bsAb induced activation of CD40-expressing cells only in the presence of EpCAM expressed on CHO cells whereas no activation was observed in a similar set up with CHO cells lacking EpCAM expression ( Figure 3(b) ). Additionally, a CD137-5T4 RUBY bsAb induced potent T cell activation as measured by a dose-dependent increase in interferon (IFN)-gamma release in the presence of 5T4.…”

Section: Resultssupporting

confidence: 83%

“…These results are in line with efficient tumor localization of a RUBY bsAb previously seen in vivo in tumor-bearing mice. 29 …”

Section: Resultsmentioning

confidence: 99%

“…The safety of RUBY has been partly evaluated in a study by Hägerbrand et al 29 where non-human primates were administered up to 37.5 mg/mL repeated doses of a CEAxCD40 RUBY, which showed no pathological findings related to either format or compound. Additional prerequisites for appropriate safety and immunogenicity profiles are good physiological stress and low presence of product-related impurities, as it is known that these can increase the drug toxicity and patient immunogenic responses.…”

Section: Discussionmentioning

confidence: 99%

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RUBY® – a tetravalent (2+2) bispecific antibody format with excellent functionality and IgG-like stability, pharmacology and developability properties

Nyesiga,

Levin,

Säll

et al. 2024

mAbs

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Despite the large number of existing bispecific antibody (bsAb) formats, the generation of novel bsAbs is still associated with development and bioprocessing challenges. Here, we present RUBY, a novel bispecific antibody format that allows rapid generation of bsAbs that fulfill key development criteria. The RUBY TM format has a 2 + 2 geometry, where two Fab fragments are linked via their light chains to the C-termini of an IgG, and carries mutations for optimal chain pairing. The unique design enables generation of bsAbs with mAb-like attributes. Our data demonstrate that RUBY bsAbs are compatible with small-scale production systems for screening purposes and can be produced at high yields (>3 g/L) from stable cell lines. The bsAbs produced are shown to, in general, contain low amounts of aggregates and display favorable solubility and stress endurance profiles. Further, compatibility with various IgG isotypes is shown and tailored Fc gamma receptor binding confirmed. Also, retained interaction with FcRn is demonstrated to translate into a pharmacokinetic profile in mice and non-human primates that is comparable to mAb controls. Functionality of conditional active RUBY bsAbs is confirmed in vitro. Anti-tumor effects in vivo have previously been demonstrated, and shown to be superior to a comparable mAb, and here it is further shown that RUBY bsAbs penetrate and localize to tumor tissue in vivo. In all, the RUBY format has attractive mAb-like attributes and offers the possibility to mitigate many of the development challenges linked to other bsAb formats, facilitating both high functionality and developability.

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Section: Resultssupporting

confidence: 83%

“…These results are in line with efficient tumor localization of a RUBY bsAb previously seen in vivo in tumor-bearing mice. 29 …”

Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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RUBY® – a tetravalent (2+2) bispecific antibody format with excellent functionality and IgG-like stability, pharmacology and developability properties

Nyesiga,

Levin,

Säll

et al. 2024

mAbs

Self Cite

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“…It has been reported the immunostimulators mainly focus on the tumor necrosis factor receptor (TNFR) family and B7-CD28 family. Currently, a number of agonistic antibodies have entered the clinical stage (44)(45)(46). TNFRSF4, also known as OX40, activates the PI3K/PKB, NF-kB1 and NFAT pathways and enhances T cell-mediated antitumor immunity, thereby improving survival in several preclinical cancer models, including B16 melanoma and lung cancer (47).…”

Section: Discussionmentioning

confidence: 99%

RASGRP2 is a potential immune-related biomarker and regulates mitochondrial-dependent apoptosis in lung adenocarcinoma

Liu

Ouyang²,

Feng³

et al. 2023

Front. Immunol.

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BackgroundRas guanine nucleotide-releasing protein 2 (RASGRP2), one of the guanine nucleotide exchange factors (GEFs), has attracted much attention in recent years. However, the correlation between RASGRP2 and immune infiltration and malignant features in lung adenocarcinoma (LUAD) has rarely been mentioned.MethodsThe Limma package and the LASSO regression model were performed to screen for differentially expressed genes. Data from the TCGA and 5 GEO databases were used to explore the expression level of RASGRP2 in LUAD patients. A weighted co-expression network and LinkFinder module were established to find the related genes of RASGRP2. The ESTIMATE algorithm was used to analyze the correlation between RASGRP2 and immune infiltration in LUAD. Tumor-infiltrating immune cells were sorted and sequenced at the single-cell level to analyze differences in RASGRP2. Real-time PCR and immunohistochemistry were performed in the real-world cohort to verify the expression of RASGRP2 and its correlation with immune-related genes. Clone formation and EdU assays were used to verify the proliferation ability. The proportion of apoptotic cells was analyzed by flow cytometry. Observation of mitochondrial membrane potential (MMP) changes by fluorescence microscopy.ResultsOur results suggested that decreased RASGRP2 was associated with worse clinical parameters and prognosis in LUAD patients. And we constructed a FLI1-HSA-miR-1976-RASGRP2 transcriptional network to support the role of RASGRP2. Enrichment analysis revealed that RASGRP2 was involved in lymphocyte activation and leukocyte adhesion. RASGRP2 was found to be positively correlated with the infiltration of most immune cells, immunoregulators, and chemokines in a subsequent study. Meanwhile, the real-world cohort confirmed that the expression levels of PDCD1, CTLA4, CD40LG, CCL14, CXCR5, and CCR7 were higher in the high-RASGRP2 expression group. Cytological experiments proved that RASGRP2 inhibited cell proliferation in LUAD by regulating mitochondrial-dependent apoptosis.ConclusionRASGRP2 was a potential immune-related biomarker of LUAD. In addition, RASGRP2 was involved in the malignant progression of LUAD through the regulation of mitochondrial-dependent apoptosis.

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“…Therefore, it cannot be concluded whether antigen fate or DC maturation induced by CD40 targeting was the main determinant for the enhanced T cell proliferation. Of note, an exciting prospect in the context of CD40 targeting are bispecific antibodies recognizing CD40 and a TAA. , These constructs bring tumor debris in proximity to CD40 + cells, which can take up, process, and present the tumor antigens, while simultaneously being stimulated via CD40. This results in antitumor responses surpassing immune reactivity toward the initial targeted epitope …”

Section: Promoting Pan-apc Antigen Presentationmentioning

confidence: 99%

Controlling Antigen Fate in Therapeutic Cancer Vaccines by Targeting Dendritic Cell Receptors

Wijfjes,

van Dalen,

Le Gall

et al. 2023

Mol. Pharmaceutics

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Antigen-presenting cells (APCs) orchestrate immune responses and are therefore of interest for the targeted delivery of therapeutic vaccines. Dendritic cells (DCs) are professional APCs that excel in presentation of exogenous antigens toward CD4+ T helper cells, as well as cytotoxic CD8+ T cells. DCs are highly heterogeneous and can be divided into subpopulations that differ in abundance, function, and phenotype, such as differential expression of endocytic receptor molecules. It is firmly established that targeting antigens to DC receptors enhances the efficacy of therapeutic vaccines. While most studies emphasize the importance of targeting a specific DC subset, we argue that the differential intracellular routing downstream of the targeted receptors within the DC subset should also be considered. Here, we review the mouse and human receptors studied as target for therapeutic vaccines, focusing on antibody and ligand conjugates and how their targeting affects antigen presentation. We aim to delineate how targeting distinct receptors affects antigen presentation and vaccine efficacy, which will guide target selection for future therapeutic vaccine development.

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Bispecific antibodies targeting CD40 and tumor-associated antigens promote cross-priming of T cells resulting in an antitumor response superior to monospecific antibodies

Cited by 11 publications

References 28 publications

RUBY® – a tetravalent (2+2) bispecific antibody format with excellent functionality and IgG-like stability, pharmacology and developability properties

RUBY® – a tetravalent (2+2) bispecific antibody format with excellent functionality and IgG-like stability, pharmacology and developability properties

RASGRP2 is a potential immune-related biomarker and regulates mitochondrial-dependent apoptosis in lung adenocarcinoma

Controlling Antigen Fate in Therapeutic Cancer Vaccines by Targeting Dendritic Cell Receptors

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