Anti-CD22–chimeric antigen receptors targeting B-cell precursor acute lymphoblastic leukemia

Haso, Waleed; Lee, Daniel W.; Shah, Nirali N.; Stetler‐Stevenson, Maryalice; Yuan, Constance; Pastan, Ira; Dimitrov, Dimiter S.; Morgan, Richard A.; FitzGerald, David J.; Barrett, David M.; Wayne, Alan S.; Mackall, Crystal L.; Orentas, Rimas J.

doi:10.1182/blood-2012-06-438002

Cited by 484 publications

(440 citation statements)

References 39 publications

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“…The low EC 50 value likely reflects the extremely high potency of blinatumomab. 19 Of note, TBEPC R was calculated based on the experimentally determined expression values of T cell CD3 and Nalm-6 cell CD19 and the reported blinatumomab binding affinities to CD3 and CD19 on cell surfaces following 45-minute incubations; 22,23 any potential divergence between the assay measurements and true values of receptor density and binding affinity would affect the derivation of TBEPC R values and the estimation of EC 50 . The baseline killing in the absence of the drug (Base) was fixed at 0, based on the observed data.…”

Section: Resultsmentioning

confidence: 99%

“…The effect of T cell proliferation was not considered in the current simulation since it was reported that, on average, blinatumomab caused approximately a two-fold expansion of T cells in patients, 41 which would only lead to minor changes in τ. CD19 expression level on B cells was assigned at 20,000 receptors per cell based on literature report, 42 and this value was 2- to 5-fold lower than that of B cell lines used in vitro cytotoxicity assays (20,000 vs. 40,000 – 100,000 receptors per cell). 22,33,43–45 The blood and bone marrow blinatumomab concentration-response curves predicted by the TBE model are shown in Figure 5. Blinatumomab plasma drug concentration information following the approved dosing regimen, i.e., continuous intravenous infusion at a 9 µg/day priming dose for 7 days and then 28 µg/day full dose treatments, was obtained from multiple clinical PK studies in patients with either ALL or non-Hodgkin’s lymphoma.…”

Section: Resultsmentioning

confidence: 99%

“…22,33,43,44 CD19 expression levels on B cells was assigned at 20,000 receptors per cell based on data reported in the literature. 42 The expression level of CD33 on parental OCI-AML3 cells was 500, and the expression levels of CD33 on OCI-AML3 cells transduced with low, medium, and high levels of CD33 were 1,500, 5,000, and 10,000 receptors per cell, respectively, obtained by digitization.…”

Section: Methodsmentioning

confidence: 99%

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Development of a Target cell-Biologics-Effector cell (TBE) complex-based cell killing model to characterize target cell depletion by T cell redirecting bispecific agents

Jiang

Chen

Carpenter

et al. 2018

mAbs

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T-cell redirecting bispecific antibodies (bsAbs) or antibody-derived agents that combine tumor antigen recognition with CD3-mediated T cell recruitment are highly potent tumor-killing molecules. Despite the tremendous progress achieved in the last decade, development of such bsAbs still faces many challenges. This work aimed to develop a mechanism-based pharmacokinetic/pharmacodynamic (PK/PD) modeling framework that can be used to assist the development of T-cell redirecting bsAbs. A Target cell-Biologics-Effector cell (TBE) complex-based cell killing model was developed using in vitro and in vivo data, which incorporates information on binding affinities of bsAbs to CD3 and target receptors, expression levels of CD3 and target receptors, concentrations of effector and target cells, as well as respective physiological parameters. This TBE model can simultaneously evaluate the effect of multiple system-specific and drug-specific factors on the T-cell redirecting bsAb exposure–response relationship on a physiological basis; it reasonably captured multiple reported in vitro cytotoxicity data, and successfully predicted the effect of some key factors on in vitro cytotoxicity assays and the efficacious dose of blinatumomab in humans. The mechanistic nature of this model uniquely positions it as a knowledge-based platform that can be readily expanded to guide target selection, drug design, candidate selection and clinical dosing regimen projection, and thus support the overall discovery and development of T-cell redirecting bsAbs.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

See 1 more Smart Citation

Development of a Target cell-Biologics-Effector cell (TBE) complex-based cell killing model to characterize target cell depletion by T cell redirecting bispecific agents

Jiang

Chen

Carpenter

et al. 2018

mAbs

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“…(Sotillo et al 2015) Another potential solution for antigen escape is targeting multiple surface antigens on a single tumour in one product, as described in the Tumour Associated Antigen section above. Until recently, CD22-CAR targeted therapy was limited to the pre-clinical realm(Haso et al 2013). However, in addition to targeting CD22 in patients with CD19 antigen loss following CD19-directed therapy (NCT02315612), several groups are currently exploring the use of bispecific CAR T-cells in preclinical studies.…”

Section: How To Improve Car T-cell Efficacy and Increase Access To Pementioning

confidence: 99%

Recent advances in T‐cell immunotherapy for haematological malignancies

et al. 2016

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In vitro discoveries have paved the way for bench-to-bedside translation in adoptive T cell immunotherapy, resulting in remarkable clinical responses in a variety of haematological malignancies. Adoptively transferred T cells genetically modified to express CD19 CARs have shown great promise, although many unanswered questions regarding how to optimize T-cell therapies for both safety and efficacy remain. Similarly, T cells that recognize viral or tumour antigens though their native receptors have produced encouraging clinical responses. Honing manufacturing processes will increase the availability of T-cell products, while combining T-cell therapies has the ability to increase complete response rates. Lastly, innovative mechanisms to control these therapies may improve safety profiles while genome editing offers the prospect of modulating T-cell function. This review will focus on recent advances in T-cell immunotherapy, highlighting both clinical and pre-clinical advances, as well as exploring what the future holds.

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“…Multiple cell surface antigens expressed by B cell malignancies, including CD19, CD20, CD22, CD23, CD38, ROR1, and kappa light chain, have been targeted with T cells engineered to express scFv-containing CAR constructs [13,15,[20][21][22][23][24][25], and some of these antigens are now being targeted in phase I clinical trials of CAR-modified T cell therapy (Table 1). Although targeting using a scFv incorporated into a CAR has remained the most prevalent strategy to target B cell malignancies, other approaches have been used to target CAR-modified T cells to solid tumors, for example by incorporation of IL-13 into a CAR to redirect engineered T cells to IL-13Ra2-expressing tumors [26].…”

Section: Design Of Chimeric Antigen Receptorsmentioning

confidence: 99%

Chimeric antigen receptor modified T cell therapy for B cell malignancies

Turtle

2013

Int J Hematol

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Adoptive transfer of tumor-reactive T cells into cancer patients with the intent of inducing a cytotoxic antitumor effector response and durable immunity has long been proposed as a novel therapy for a broad range of malignancies; however, local and systemic tolerance mechanisms have hindered the generation of effective T cell therapies and limited the clinical efficacy of this approach in cancer patients. Chimeric antigen receptors (CARs) are recombinant receptors that comprise an extracellular antigen-targeting domain in conjunction with one or more intracellular T cell signaling domains that can be introduced into T cells by genetic modification to redirect their specificity to the CAR-targeted antigen. Administration of CD19-specific CAR-modified T cells that target B cell non-Hodgkin lymphomas and leukemia has been remarkably effective in recent clinical trials, energizing the field and stimulating new efforts to identify the critical parameters of CAR design and T cell engineering that are necessary for effective cancer therapy.

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Anti-CD22–chimeric antigen receptors targeting B-cell precursor acute lymphoblastic leukemia

Cited by 484 publications

References 39 publications

Development of a Target cell-Biologics-Effector cell (TBE) complex-based cell killing model to characterize target cell depletion by T cell redirecting bispecific agents

Development of a Target cell-Biologics-Effector cell (TBE) complex-based cell killing model to characterize target cell depletion by T cell redirecting bispecific agents

Recent advances in T‐cell immunotherapy for haematological malignancies

Chimeric antigen receptor modified T cell therapy for B cell malignancies

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