A recombinant trispecific single‐chain Fv derivative directed against CD123 and CD33 mediates effective elimination of acute myeloid leukaemia cells by dual targeting

Kügler, Markus; Stein, Christoph; Kellner, Christian; Mentz, Kristin; Saul, Domenica; Schwenkert, Michael; Schubert, Ingo; Singer, Heiko; Oduncu, Fuat; Stockmeyer, Bernhard; Mackensen, Andréas; Fey, Georg H.

doi:10.1111/j.1365-2141.2010.08300.x

Cited by 113 publications

(100 citation statements)

References 63 publications

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“…59 The original scFv domains were of murine origin 59 and were humanized, disulfide-stabilized and stability-engineered for incorporation into SPM-2. A final clinical candidate named SPM-2 was identified, and a production process in stably transfected human Freestyle TM 293F-cells, as well as a downstream purification process following industry standard procedures was developed.…”

Section: Resultsmentioning

confidence: 99%

“…We also urgently wish to determine, whether the dual-targeting triplebody mediates more potent lysis at lower EC50 doses in RDL experiments than the mono-targeting related proteins CD33-16 and CD123–16, either individually or in combination, similar to the studies performed earlier with the triplebodies 123-16-33, HLAII-16–19 and 33–3-19. 59,68–70 …”

Section: Discussionmentioning

confidence: 99%

“…A number of therapeutic agents with similar molecular formats as those described for CD33 have been developed, including immunoglobulins, 47–49 a radio-immunoconjugate, 50 ADCs and a fusion protein between the cytokine IL-3 and a fragment of diphtheria toxin, 51–54 bi-specific T cell-recruiting agents (BiTEs) and Dual-Antigen Recruiting T-cell engagers (DARTs), 55–58 dual-targeting triplebodies, 59,60 and CAR-transfected T cells. 61–64 Expression of CD123 is largely restricted to hematopoietic cells, but expression on endothelial cells has been reported.…”

Section: Introductionmentioning

confidence: 99%

“…8 Larger studies in patients with many different subtypes of the disease are needed to investigate, whether new dual-targeting agents simultaneously addressing both antigens on the same cell 59,60 or combinations of corresponding mono-targeting agents are promising for clinical applications for a broad group of AML patients. In a first large study pursuing this goal, the expression of CD33 and CD123 alone and in combination was investigated on cellular samples from 319 AML patients.…”

Section: Introductionmentioning

confidence: 99%

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Dual-targeting triplebody 33-16-123 (SPM-2) mediates effective redirected lysis of primary blasts from patients with a broad range of AML subtypes in combination with natural killer cells

et al. 2018

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A number of agents designed for immunotherapy of Acute Myeloid Leukemia (AML) are in preclinical and early clinical development. Most of them target a single antigen on the surface of AML cells. Here we describe the development and key biological properties of a tri-specific agent, the dual-targeting triplebody SPM-2, with binding sites for target antigens CD33 and CD123, and for CD16 to engage NK cells as cytolytic effectors. Primary blasts of nearly all AML patients carry at least one of these target antigens and the pair is particularly promising for the elimination of blasts and leukemia stem cells (LSCs) from a majority of AML patients by dual-targeting agents. The cytolytic activity of NK cells mediated by SPM-2 was analyzed in vitro for primary leukemic cells from 29 patients with a broad range of AML-subtypes. Blasts from all 29 patients, including patients with genomic alterations associated with an unfavorable genetic subtype, were lysed at nanomolar concentrations of SPM-2. Maximum susceptibility was observed for cells with a combined density of CD33 and CD123 above 10,000 copies/cell. Cell populations enriched for AML-LSCs (CD34pos and CD34pos CD38neg cells) from 2 AML patients carried an increased combined antigen density and were lysed at correspondingly lower concentrations of SPM-2 than unsorted blasts. These initial findings raise the expectation that SPM-2 may also be capable of eliminating AML-LSCs and thus of prolonging survival. In the future, patients with a broad range of AML subtypes may benefit from treatment with SPM-2.

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Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Dual-targeting triplebody 33-16-123 (SPM-2) mediates effective redirected lysis of primary blasts from patients with a broad range of AML subtypes in combination with natural killer cells

et al. 2018

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“…Several trispecific immunoconstructs targeting the FcgRIIIa receptor on NK cells have been developed and compared with their bispecific counterparts. [26][27][28] An additional tumor-specific arm in such trispecific construct increased its avidity, leading to enhanced target cell killing. [26][27][28] Moreover, increase in the construct size beyond the kidney exclusion limit of 65 kDa was an additional clinical advantage.…”

Section: Introductionmentioning

confidence: 99%

Mono- and dual-targeting triplebodies activate natural killer cells and have anti-tumor activityin vitroandin vivoagainst chronic lymphocytic leukemia

et al. 2016

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Chronic lymphocytic leukemia (CLL) is the most common form of leukemia that affects B lymphocytes in adults. Natural killer (NK) cells in CLL patients are intrinsically potent but display poor in situ effector functions. NKG2D is an activating receptor found on NK and CD8 C T cells and plays a role in immunosurveillance of CLL. In this study, we developed mono-and dual-targeting triplebodies utilizing a natural ligand for human NKG2D receptor (ULBP2) to retarget NK cells against tumor cells. Triplebodies in both formats showed better ability to induce NK-cell-dependent killing of target cells compared to bispecific counterparts. A mono-targeting triplebody ULBP2-aCD19-aCD19 successfully triggered NK cell effector functions against CLL cell line MEC1 and primary tumor cells in allogenic and autologous settings. Additionally, a dual-targeting triplebody ULBP2-aCD19-aCD33 specific for two distinct tumor-associated antigens was developed to target antigen loss variants, such as mixed lineage leukemia (MLL). Of note, this triplebody exhibited cytotoxic activity against CD19/CD33 double positive cells and retained its binding features even in the absence of one of the tumor antigens. Further, ULBP2-aCD19-aCD19 showed significant in vivo activity in immune-deficient (NSG) mouse model transplanted with CLL cell line as target cells and human immune cells as an effector population providing a proof-of-principle for this therapeutic concept.

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Bispecific Antibodies and Immune Therapy Targeting

Kiprijanov¹

2011

Drug Delivery in Oncology

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A recombinant trispecific single‐chain Fv derivative directed against CD123 and CD33 mediates effective elimination of acute myeloid leukaemia cells by dual targeting

Cited by 113 publications

References 63 publications

Dual-targeting triplebody 33-16-123 (SPM-2) mediates effective redirected lysis of primary blasts from patients with a broad range of AML subtypes in combination with natural killer cells

Dual-targeting triplebody 33-16-123 (SPM-2) mediates effective redirected lysis of primary blasts from patients with a broad range of AML subtypes in combination with natural killer cells

Mono- and dual-targeting triplebodies activate natural killer cells and have anti-tumor activityin vitroandin vivoagainst chronic lymphocytic leukemia

Bispecific Antibodies and Immune Therapy Targeting

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