2021
DOI: 10.1002/sctm.21-0135
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CAR-NK Cells from Engineered Pluripotent Stem Cells: Off-the-shelf Therapeutics for all Patients

Abstract: Clinical success of adoptive cell therapy with chimeric antigen receptor (CAR) T cells for treating hematological malignancies has revolutionized the field of cellular immunotherapy. However, due to the nature of utilizing autologous T cells, affordability and availability are major hurdles, in addition to scientific challenges relating to CAR-T therapy optimization. Natural killer (NK) cell is a specialized immune effector cell type that recognizes and kills targets without human leukocyte antigen (HLA) restr… Show more

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Cited by 20 publications
(14 citation statements)
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References 59 publications
(119 reference statements)
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“…On the one hand, CAR-NK cells can be conveniently prepared from a wider range of autogenous and allogeneic sources without causing severe adverse reaction (e.g., aGVHD, CRS) by CAR-T-based implantation. On the other hand, CAR-NK cells are adequate for cell immunosurveillance dispense with pre-sensitization and thus have more flexible killing capacity upon both hematologic and solid tumor cells over CAR-T cells via both the CAR-dependent manner and CAR-independent intrinsic mechanisms, which thus provide alternative strategies for conquering tumor escape and varied adverse events (e.g., “on-target, off-tumor toxicity” during CAR-T application) [ 5 , 112 , 117 , 147 ].…”
Section: Conclusion and Perspectivementioning
confidence: 99%
“…On the one hand, CAR-NK cells can be conveniently prepared from a wider range of autogenous and allogeneic sources without causing severe adverse reaction (e.g., aGVHD, CRS) by CAR-T-based implantation. On the other hand, CAR-NK cells are adequate for cell immunosurveillance dispense with pre-sensitization and thus have more flexible killing capacity upon both hematologic and solid tumor cells over CAR-T cells via both the CAR-dependent manner and CAR-independent intrinsic mechanisms, which thus provide alternative strategies for conquering tumor escape and varied adverse events (e.g., “on-target, off-tumor toxicity” during CAR-T application) [ 5 , 112 , 117 , 147 ].…”
Section: Conclusion and Perspectivementioning
confidence: 99%
“…It was frequently objected that NK cells are never antigen-specific, an argument that is no longer valid with the arrival of CAR-NK cells in preclinical studies and clinical trials. Adult iPSC allow to obtain high numbers of NK cells, are easily accessible (theoretically, any somatic cell type might be reprogrammable into iPSC) because mostly skin fibroblasts or PBMC are used [ 74 , 75 ], and avoid the ethically highly debatable approach with embryonic stem cells. Once suitable homogeneous iPSC clones are selected, they can be banked and are further expandable and differentiable into the desired end product.…”
Section: Adoptive Transfer Of Nk Cellsmentioning
confidence: 99%
“…Once suitable homogeneous iPSC clones are selected, they can be banked and are further expandable and differentiable into the desired end product. Several methods and protocols to end up with NK cells have been published, although they are not yet entirely problem-free [ 74 , 75 ].…”
Section: Adoptive Transfer Of Nk Cellsmentioning
confidence: 99%
“…Examples of cell types that can be cultured as aggregates include PSCs, neural stem cells [11], and mammary epithelial stem cells [12]. In contrast, hematopoietic stem/progenitor cells and immune cells like T cells and NK cells are typically grown as single cells or loose clumps [13].…”
Section: Scale Up Of Optimal Hydrodynamic Conditionsmentioning
confidence: 99%