Blinatumomab induces autologous T-cell killing of chronic lymphocytic leukemia cells

Wong, Ryan; Pepper, Chris; Brennan, Paul; Nagorsen, Dirk; Man, Stephen; Fegan, Christopher

doi:10.3324/haematol.2012.082248

Cited by 67 publications

(58 citation statements)

References 49 publications

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“…Final products had mostly a central memory and effective memory phenotype within both helper and cytotoxic T cell subsets. These results are consistent with previous reports showing induction of effector memory CD4 + and CD8 + T cells following blinatumomab treatment in vitro and in vivo (18,31,32). Interestingly, BET cells expressed CD27, the receptor for CD70, in .70% of CD4 + and CD8 + subsets.…”

Section: Discussionsupporting

confidence: 82%

“…To expand T cells, freshly isolated PBMC from untreated CLL patients or normal donors were plated at 3 3 10 6 /ml in serum-free X-VIVO 15 medium (Lonza) containing 0.1 mM gentamicin (Fisiopharma, Palomonte, Italy), 10 ng/ml blinatumomab (AMG103; Amgen) (17,18), and 500 IU/ml rhIL-2 (Bayer HealthCare Pharmaceuticals, Berlin, Germany). In two CLL cases, frozen PBMC were used.…”

Section: Expansion Of T Cells Using Blinatumomab and Rhil-2mentioning

confidence: 99%

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A Novel Method Using Blinatumomab for Efficient, Clinical-Grade Expansion of Polyclonal T Cells for Adoptive Immunotherapy

Golay

D'Amico

Borleri

et al. 2014

The Journal of Immunology

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Current treatment of chronic lymphocytic leukemia (CLL) patients often results in life-threatening immunosuppression. Furthermore, CLL is still an incurable disease due to the persistence of residual leukemic cells. These patients may therefore benefit from immunotherapy approaches aimed at immunoreconstitution and/or the elimination of residual disease following chemotherapy. For these purposes, we designed a simple GMP-compliant protocol for ex vivo expansion of normal T cells from CLL patients’ peripheral blood for adoptive therapy, using bispecific Ab blinatumomab (CD3 × CD19), acting both as T cell stimulator and CLL depletion agent, and human rIL-2. Starting from only 10 ml CLL peripheral blood, a mean 515 × 106 CD3+ T cells were expanded in 3 wk. The resulting blinatumomab-expanded T cells (BET) were polyclonal CD4+ and CD8+ and mostly effector and central memory cells. The Th1 subset was slightly prevalent over Th2, whereas Th17 and T regulatory cells were <1%. CMV-specific clones were detected in equivalent proportion before and after expansion. Interestingly, BET cells had normalized expression of the synapse inhibitors CD272 and CD279 compared with starting T cells and were cytotoxic against CD19+ targets in presence of blinatumomab in vitro. In support of their functional capacity, we observed that BET, in combination with blinatumomab, had significant therapeutic activity in a systemic human diffuse large B lymphoma model in NOD-SCID mice. We propose BET as a therapeutic tool for immunoreconstitution of heavily immunosuppressed CLL patients and, in combination with bispecific Ab, as antitumor immunotherapy.

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Section: Discussionsupporting

confidence: 82%

Section: Expansion Of T Cells Using Blinatumomab and Rhil-2mentioning

confidence: 99%

A Novel Method Using Blinatumomab for Efficient, Clinical-Grade Expansion of Polyclonal T Cells for Adoptive Immunotherapy

Golay

D'Amico

Borleri

et al. 2014

The Journal of Immunology

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“…MGD011, however, was able to eliminate leukemic cells in CLL patient samples by engaging and expanding the patient's residual T cells in vitro from a low E:T cell ratio to one exceeding the target cell population. These data also confirm that CLL T cells can be redirected to become cytolytic against leukemic cells in the presence of MGD011, as previously reported for blinatumomab (19), even though T-cell dysfunction in CLL, such as defects in immune synapse formation, co-stimulatory/accessory molecule expression, and cytokine release have been reported (20)(21)(22).…”

Section: Discussionsupporting

confidence: 71%

MGD011, A CD19 x CD3 Dual-Affinity Retargeting Bi-specific Molecule Incorporating Extended Circulating Half-life for the Treatment of B-Cell Malignancies

Liu

Lam

Long

et al. 2017

Clinical Cancer Research

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Purpose: CD19, a B-cell lineage-specific marker, is highly represented in B-cell malignancies and an attractive target for therapeutic interventions. MGD011 is a CD19 x CD3 DART bispecific protein designed to redirect T lymphocytes to eliminate CD19-expressing cells. MGD011 has been engineered with a modified human Fc domain for improved pharmacokinetic (PK) properties and designed to cross-react with the corresponding antigens in cynomolgus monkeys. Here, we report on the preclinical activity, safety and PK properties of MGD011.Experimental Design: The activity of MGD011 was evaluated in several in vitro and in vivo models. PK, safety and pharmacodynamic activity was also assessed in dose-escalation and repeatdose studies of MGD011 administered once weekly in cynomolgus monkeys.Results: MGD011 mediated killing of human B-cell lymphoma lines by human or cynomolgus monkey PBMCs as well as autologous B-cell depletion in PBMCs from both species. MGD011-mediated killing was accompanied by target-dependent T-cell activation and expansion, cytokine release and upregulation of perforin and granzyme B. MGD011 demonstrated antitumor activity against localized and disseminated lymphoma xenografts reconstituted with human PBMCs. In cynomolgus monkeys, MGD011 displayed a terminal half-life of 6.7 days; once weekly intravenous infusion of MGD011 at doses up to 100 mg/kg, the highest dose tested, was well tolerated and resulted in dose-dependent, durable decreases in circulating B cells accompanied by profound reductions of B lymphocytes in lymphoid organs.Conclusions: The preclinical activity, safety and PK profile support clinical investigation of MGD011 as a therapeutic candidate for the treatment of B-cell malignancies.

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“…In a study using peripheral blood mononuclear cells from either treatment-naïve or previously-treated patients with chronic lymphocytic leukaemia (CLL), blinatumomab induced T-cell proliferation and activation, cytokine secretion and granzyme B release, and induced tumour cell death at very low T-cell: tumour cell ratios [21]. These findings suggest that blinatumomab may be of use in overcoming immunodeficiency in the treatment of CLL [21].…”

Section: Pharmacodynamicsmentioning

confidence: 95%

“…These findings suggest that blinatumomab may be of use in overcoming immunodeficiency in the treatment of CLL [21]. Blinatumomab may also have therapeutic potential in acute myeloid leukaemia (AML), as in blast cell cultures from patients with AML, the presence of blinatumomab resulted in a decrease in CD33?…”

Section: Pharmacodynamicsmentioning

confidence: 96%

Blinatumomab: First Global Approval

Sanford

2015

Drugs

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Blinatumomab (BLINCYTO™) is a novel, bispecific T-cell engaging antibody that binds cluster of differentiation (CD) 19 antigens on blast cells while also binding and activating the CD3/T cell receptor complex, causing cell lysis. The antibody is being developed by Amgen as a treatment for haematological cancers that originate from B cell lines. Blinatumomab was approved by the US FDA in December 2014 for the treatment of adults with Philadelphia chromosome (Ph)-negative relapsed/refractory B-cell precursor acute lymphoblastic leukaemia (BCP-ALL). It is awaiting approval for this indication in the EU and is in phase III development in various countries. This article summarizes the milestones in the development of blinatumomab leading to its first approval for the treatment of Ph-negative BCP-ALL.

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Blinatumomab induces autologous T-cell killing of chronic lymphocytic leukemia cells

Cited by 67 publications

References 49 publications

A Novel Method Using Blinatumomab for Efficient, Clinical-Grade Expansion of Polyclonal T Cells for Adoptive Immunotherapy

A Novel Method Using Blinatumomab for Efficient, Clinical-Grade Expansion of Polyclonal T Cells for Adoptive Immunotherapy

MGD011, A CD19 x CD3 Dual-Affinity Retargeting Bi-specific Molecule Incorporating Extended Circulating Half-life for the Treatment of B-Cell Malignancies

Blinatumomab: First Global Approval

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