Severity of the <scp>TGN</scp>1412 trial disaster cytokine storm correlated with <scp>IL</scp>‐2 release

Eastwood, David; Bird, Christopher; Dilger, Paula; Hockley, Jason; Findlay, Lucy; Poole, Stephen; Thorpe, Susan J.; Wadhwa, Meenu; Thorpe, Robin; Stebbings, Richard

doi:10.1111/bcp.12165

Cited by 54 publications

(48 citation statements)

References 38 publications

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“…In our study, we confirmed the absence of induced proliferation with CD28.2, but recorded significant levels of IFNγ, TNF, IL-6 and IL-12 release. Otherwise, whereas the severity of the adverse response of TGN1412 was correlated with the level of IL-2 release, 30 we observed that level of IFNγ release could be more predictive of agonist properties of divalent anti-CD28 mAbs.…”

Section: Mabs Volume 6 Issuementioning

confidence: 57%

Advantages ofPapio anubisfor preclinical testing of immunotoxicity of candidate therapeutic antagonist antibodies targeting CD28

Poirier

Mary

Bas‐Bernardet

et al. 2014

mAbs

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Section: Mabs Volume 6 Issuementioning

confidence: 57%

Advantages ofPapio anubisfor preclinical testing of immunotoxicity of candidate therapeutic antagonist antibodies targeting CD28

Poirier

Mary

Bas‐Bernardet

et al. 2014

mAbs

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“…7A, 7B). In a recent study the severity of the TGN1412-induced cytokine storm was correlated with the IL-2 release, suggesting that IL-2 production might be used as a prognostic factor in upcoming trials of new biologicals (34). Thus, in addition to cytokine secretion, analysis of costimulatory molecules expression may be also informative for the evaluation of new biologicals.…”

Section: Discussionmentioning

confidence: 99%

“…1). Because Eastwood et al (34) showed that IL-2 is a marker associated with the induction of a cytokine storm, we addressed whether under the above conditions T cells were present that secreted TNF-a, IFN-g, and IL-2 in parallel. Irrespective of whether T cells derived from PBMCs or HDC-PBMCs, polyfunctional T cells were detected (Fig.…”

Section: Upon Tgn1412 Treatment T Cells Isolated From High-density Prmentioning

confidence: 99%

Cell Contact–Dependent Priming and Fc Interaction with CD32+ Immune Cells Contribute to the TGN1412-Triggered Cytokine Response

Bartholomaeus

Semmler

Bukur

et al. 2014

The Journal of Immunology

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Following inconspicuous preclinical testing, the superagonistic anti-CD28 mAb TGN1412 was applied to six study participants who all developed a devastating cytokine storm. We verified that TGN1412 treatment of fresh PBMCs induced only moderate responses, whereas restoration of tissue-like conditions by high-density preculture (HDC) allowed vigorous cytokine production. TGN1412 treatment of T cells isolated from HDC-PBMCs induced moderate cytokine responses, which upon additional anti-IgG crosslinking were significantly boosted. Moreover, coincubation of TGN1412-treated T cells with B cells expressing the intermediate affinity Fcγ receptor IIB (CD32B), or coincubation with CD32B+ transfectants, resulted in robust T cell activation. This was surprising because TGN1412 was expressed as an Ig of the subclass 4 (IgG4), which was shown before to exhibit only minor affinity to FcγRs. Transcriptome analysis of TGN1412-treated T cells revealed that similar gene signatures were induced irrespective of whether T cells derived from fresh or HDC-PBMCs were studied. Collectively, these data indicate that HDC-PBMCs and HDC-PBMC–derived T cells mount rapid TGN1412 responses, which are massively boosted by FcγR crosslinking, in particular by CD32-expressing B cells. These results qualify HDC-PBMCs as a valuable in vitro test system for the analysis of complex mAb functions.

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“…However, IL2 was combined with an F(ab 0 ) 2 fragment of an anti-CD3/ EpCAM quadroma in a clinical trial (40), but treatment was limited because of considerable toxicity most likely caused by induction of secondary cytokines, known as CRS or cytokine storm. Systemic administration of IL2 is known to induce a cytokine storm (41), and the severity of adverse events associated with CRS, such as with the TGN1412 catastrophic trial, is correlated with IL2 release (42). Although it is not without side effects, immunotherapy with IFNa, which is not produced by T cells, is not typically associated with cytokine storm.…”

Section: Discussionmentioning

confidence: 99%

Redirected T-Cell Killing of Solid Cancers Targeted with an Anti-CD3/Trop-2–Bispecific Antibody Is Enhanced in Combination with Interferon-α

Rossi

Chang

et al. 2014

Molecular Cancer Therapeutics

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Trop-2 has limited presence on normal tissues but is highly expressed in diverse epithelial cancers. (E1)-3s is a T-cell-redirecting trivalent bispecific antibody (bsAb), comprising an anti-CD3 scFv covalently linked to a stabilized dimer of a Trop-2-targeting Fab using Dock-and-Lock. We show for the first time that bsAbmediated bidirectional trogocytosis occurs between target and T cells and involves immunologic synapses. We studied the effects of interferon-a (INFa) on (E1)-3s-mediated T-cell killing of human gastric and pancreatic cancer cell lines. T-cell activation, cytokine induction, and cytotoxicity were evaluated ex vivo using peripheral blood mononuclear cells (PBMC) or T cells with NCI-N87 gastric cancer as target cells. In vivo activity was assayed with NCI-N87 and Capan-1 (pancreatic) xenografts. In the presence of target cells and PBMCs, (E1)-3s did not cause excess cytokine production. When combined with (E1)-3s, peginterferonalfa-2a-which alone did not increase T-cell activation or raise cytokine levels over baseline-increased CD69 expression but did not significantly increase cytokine induction. (E1) 3s mediated a highly potent T-cell lysis of NCI-N87 target cells in vitro. Inclusion of peginterferonalfa-2a or a more potent form of INFa, 20 Ã -2b, significantly potentiated the activity of (E1)-3s by more than 2.5-or 7-fold, respectively. In vivo, combining peginterferonalfa-2a with (E1)-3s delayed Capan-1 growth longer than each single agent. Similarly, combination therapy delayed tumor proliferation of NCI-N87 compared with (E1)-3s or peginterferonalfa-2a single-treatment groups. (E1)-3s effectively induced T-cell-mediated killing of Trop-2-expressing pancreatic and gastric cancers, which was enhanced with INFa.

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Severity of the TGN1412 trial disaster cytokine storm correlated with IL‐2 release

Cited by 54 publications

References 38 publications

Advantages ofPapio anubisfor preclinical testing of immunotoxicity of candidate therapeutic antagonist antibodies targeting CD28

Advantages ofPapio anubisfor preclinical testing of immunotoxicity of candidate therapeutic antagonist antibodies targeting CD28

Cell Contact–Dependent Priming and Fc Interaction with CD32+ Immune Cells Contribute to the TGN1412-Triggered Cytokine Response

Redirected T-Cell Killing of Solid Cancers Targeted with an Anti-CD3/Trop-2–Bispecific Antibody Is Enhanced in Combination with Interferon-α

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