Retrovirus-mediated gene transfer in primary T lymphocytes impairs their anti–Epstein-Barr virus potential through both culture-dependent and selection process–dependent mechanisms

Sauce, Delphine; Bodinier, Marie; Garín, Marina I.; Petracca, Bruno; Tonnelier, Nicolas; Duperrier, Anne; Melo, Junia V.; Apperley, Jane F.; Ferrand, Christophe; Hervé, P.; Lang, François; Tiberghien, Pierre; Robinet, Éric

doi:10.1182/blood.v99.4.1165

Cited by 105 publications

(92 citation statements)

References 32 publications

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“…Functional analysis of protocols of polyclonal stimulation has been very limited so far, and focused on the function of CD3-stimulated GM T cells in vitro compared with CD3/CD28. 4,12 Despite PHA being a common polyclonal stimulus for transduction 2,6,13,14,16 and recent clinical data showing that the function of PHA-expanded GM T cells is poor in vivo compared with their unmanipulated counterparts, 16 no such comparative functional analysis has been published for PHA. In this study, we have explored the functional effect of PHA on T cells in vitro, compared it with iCD3/iCD28 stimulation, and then investigated the mechanisms leading to this functional effect.…”

Section: Discussionmentioning

confidence: 99%

“…12,15 To address this functional issue, we extended our analysis to explore the capacity of PHAexpanded T cells to mount antigen-specific responses against immunodominant peptides derived from Epstein-Barr virus (EBV) and cytomegalovirus (CMV). Dendritic cells (DCs) were generated from monocytes derived from CMV+/HLA-A2 and EBV+/HLA-B8 donors.…”

Section: Expansion Of Primary Human T-lymphocytes With Pha Impairs Thmentioning

confidence: 99%

“…In fact, there is evidence to suggest that the expansion process rather than the integration or expression of the transgene may have the largest effect on the function of GM T cells in vitro and in animal models. 2,4,6,[9][10][11][12][13] In humans, although the data available are still limited, a number of trials showed that GM T cells can have reduced function in vivo. [14][15][16] Phytohemagglutinin (PHA) is a common polyclonal stimulus used in protocols of retroviral transduction.…”

Section: Introductionmentioning

confidence: 99%

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Functional impairment of human T-lymphocytes following PHA-induced expansion and retroviral transduction: implications for gene therapy

et al. 2002

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Section: Discussionmentioning

confidence: 99%

Section: Expansion Of Primary Human T-lymphocytes With Pha Impairs Thmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Functional impairment of human T-lymphocytes following PHA-induced expansion and retroviral transduction: implications for gene therapy

et al. 2002

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“…In two constructs we dissected the V5 into two parts and accordingly made the two constructs as depicted in Figure 3e (second and third images). Next, we replaced the V5 peptide with a synthetic hinge region commonly used in chimeric TCR constructs 30 ((G4S)2, construct 4) or naturally occurring hinge regions from primate immunoglobulins 31 (constructs [5][6][7][8]. The original vector with the furin site plus the complete V5 peptide (construct 9) consistently displayed the highest level of TCR expression, whereas other vectors showed a performance similar to the vector where furin was linked directly to F2A (construct 10).…”

Section: Addition Of Peptide Tags Increases Tcr Expressionmentioning

confidence: 99%

“…Furthermore, the current g-retroviral vector based protocols require T cells to be fully activated for efficient transduction and this may be deleterious to their function. 7,8 We previously reported that in a murine model, prolonged ex vivo stimulation yielded fully differentiated effector T cells which were capable of in vitro tumor killing and high-level INF-g release but, exhibited inferior activity for in vivo tumor treatment compared to naive and less differentiated effectors. 9 Finally, there is a growing need for gene delivery systems to carry multiple genes in one construct, and g-retroviral vectors have a limited coding capacity (o7 kb).…”

Section: Introductionmentioning

confidence: 99%

Development of optimal bicistronic lentiviral vectors facilitates high-level TCR gene expression and robust tumor cell recognition

et al. 2008

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In human gene therapy applications, lentiviral vectors may have advantages over g-retroviral vectors in several areas, including the ability to transduce nondividing cells, resistance to gene silencing and a potentially safer integration site profile. However, unlike g-retroviral vectors it has been problematic to drive the expression of multiple genes efficiently and coordinately with approaches such as internal ribosome entry sites or dual promoters. Using different 2A peptides, lentiviral vectors expressing two-gene T-cell receptors directed against the melanoma differentiation antigens gp100 and MART-1 were constructed. We demonstrated that addition of amino-acid spacer sequences (GSG or SGSG) before the 2A sequence is a prerequisite for efficient synthesis of biologically active T-cell receptors and that addition of a furin cleavage site followed by a V5 peptide tag yielded optimal T-cell receptor gene expression. Furthermore, we determined that the furin cleavage site was recognized in lymphocytes and accounted for removal of residual 2A peptides at the post-translational level with an efficiency of 20-30%, which could not be increased by addition of multiple furin cleavage sites. The novel bicistronic lentiviral vector developed herein afforded robust antimelanoma activities to engineered peripheral blood lymphocytes, including cytokine secretion, cell proliferation and lytic activity. Such optimal vectors may have immediate applications in cancer gene therapy.

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Cellular Deformations Induced by Conical Silicon Nanowire Arrays Facilitate Gene Delivery

Chen

Aslanoglou

Gervinskas

et al. 2019

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Engineered cell–nanostructured interfaces generated by vertically aligned silicon nanowire (SiNW) arrays have become a promising platform for orchestrating cell behavior, function, and fate. However, the underlying mechanism in SiNW‐mediated intracellular access and delivery is still poorly understood. This study demonstrates the development of a gene delivery platform based on conical SiNW arrays for mechanical cell transfection, assisted by centrifugal force, for both adherent and nonadherent cells in vitro. Cells form focal adhesions on SiNWs within 6 h, and maintain high viability and motility. Such a functional and dynamic cell–SiNW interface features conformational changes in the plasma membrane and in some cases the nucleus, promoting both direct penetration and endocytosis; this synergistically facilitates SiNW‐mediated delivery of nucleic acids into immortalized cell lines, and into difficult‐to‐transfect primary immune T cells without pre‐activation. Moreover, transfected cells retrieved from SiNWs retain the capacity to proliferate—crucial to future biomedical applications. The results indicate that SiNW‐mediated intracellular delivery holds great promise for developing increasingly sophisticated investigative and therapeutic tools.

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Retrovirus-mediated gene transfer in primary T lymphocytes impairs their anti–Epstein-Barr virus potential through both culture-dependent and selection process–dependent mechanisms

Cited by 105 publications

References 32 publications

Functional impairment of human T-lymphocytes following PHA-induced expansion and retroviral transduction: implications for gene therapy

Functional impairment of human T-lymphocytes following PHA-induced expansion and retroviral transduction: implications for gene therapy

Development of optimal bicistronic lentiviral vectors facilitates high-level TCR gene expression and robust tumor cell recognition

Cellular Deformations Induced by Conical Silicon Nanowire Arrays Facilitate Gene Delivery

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