Redirected Activity of Human Antitumor Chimeric Immune Receptors is Governed by Antigen and Receptor Expression Levels and Affinity of Interaction

Turatti, Fabio; Figini, Mariangela; Balladore, Emanuela; Alberti, Paola; Casalini, Patrizia; Marks, James D.; Canevari, Silvana; Mezzanzanica, Delia

doi:10.1097/cji.0b013e3180de5d90

Cited by 70 publications

(59 citation statements)

References 35 publications

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“…4). These results suggest that the advantages of serial engagement initially proposed for TCR-peptide/ MHC interaction can also apply to CARs, as has been proposed by others for CARs against cancer (71,72,73) as well as HIV (37).…”

Section: Discussionsupporting

confidence: 66%

Novel CD4-Based Bispecific Chimeric Antigen Receptor Designed for Enhanced Anti-HIV Potency and Absence of HIV Entry Receptor Activity

Liu

Patel

Ghanem

et al. 2015

J Virol

101

133

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Adoptive transfer of CD8 T cells genetically engineered to express "chimeric antigen receptors" (CARs) represents a potential approach toward an HIV infection "functional cure" whereby durable virologic suppression is sustained after discontinuation of antiretroviral therapy. We describe a novel bispecific CAR in which a CD4 segment is linked to a single-chain variable fragment of the 17b human monoclonal antibody recognizing a highly conserved CD4-induced epitope on gp120 involved in coreceptor binding. We compared a standard CD4 CAR with CD4-17b CARs where the polypeptide linker between the CD4 and 17b moieties is sufficiently long (CD4-35-17b CAR) versus too short (CD4-10-17b) to permit simultaneous binding of the two moieties to a single gp120 subunit. When transduced into a peripheral blood mononuclear cell (PBMC) or T cells thereof, all three CD4-based CARs displayed specific functional activities against HIV-1 Env-expressing target cells, including stimulation of gamma interferon (IFN-␥) release, specific target cell killing, and suppression of HIV-1 pseudovirus production. In assays of spreading infection of PBMCs with genetically diverse HIV-1 primary isolates, the CD4-10-17b CAR displayed enhanced potency compared to the CD4 CAR whereas the CD4-35-17b CAR displayed diminished potency. Importantly, both CD4-17b CARs were devoid of a major undesired activity observed with the CD4 CAR, namely, rendering the transduced CD8 ؉ T cells susceptible to HIV-1 infection. Likely mechanisms for the superior potency of the CD4-10-17b CAR over the CD4-35-17b CAR include the greater potential of the former to engage in the serial antigen binding required for efficient T cell activation and the ability of two CD4-10-17b molecules to simultaneously bind a single gp120 subunit. IMPORTANCEHIV research has been energized by prospects for a cure for HIV infection or, at least, for a "functional cure" whereby antiretroviral therapy can be discontinued without virus rebound. This report describes a novel CD4-based "chimeric antigen receptor" (CAR) which, when genetically engineered into T cells, gives them the capability to selectively respond to and kill HIV-infected cells. This CAR displays enhanced features compared to previously described CD4-based CARs, namely, increased potency and avoidance of the undesired rendering of the genetically modified CD8 T cells susceptible to HIV infection. When adoptively transferred back to the individual, the genetically modified T cells will hopefully provide durable killing of infected cells and sustained virus suppression without continued antiretroviral therapy, i.e., a functional cure. C ombination antiretroviral therapy (cART) (1) today offers the promise of near-normal life expectancy for HIV-infected individuals (2), most of whom would previously have succumbed to the lethal consequences of immune system demise. Nevertheless, even under conditions of plasma viral load suppression below the limits of detection, CD4 T-cell recovery is often incomplete. The pathogenic sequel...

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Section: Discussionsupporting

confidence: 66%

Novel CD4-Based Bispecific Chimeric Antigen Receptor Designed for Enhanced Anti-HIV Potency and Absence of HIV Entry Receptor Activity

Liu

Patel

Ghanem

et al. 2015

J Virol

101

133

View full text Add to dashboard Cite

show abstract

“…Because the threshold may be influenced by many other factors, such as affinity (42), structure (43), epitope localization of individual CAR-Ag pairs (44,45), and the expression of a coreceptor on target cells (46), the threshold may vary among mAbs and target Ags. We also could not investigate the relationship between the expression of CD20 and the ADCC activity of mAbs because NK cell activity is predominant in the CD20-CEM system, and a clear threshold has not been observed (28).…”

Section: Discussionmentioning

confidence: 99%

Target Antigen Density Governs the Efficacy of Anti–CD20-CD28-CD3 ζ Chimeric Antigen Receptor–Modified Effector CD8+ T Cells

Watanabe

Terakura

Martens

et al. 2015

The Journal of Immunology

227

193

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The effectiveness of chimeric Ag receptor (CAR)–transduced T (CAR-T) cells has been attributed to supraphysiological signaling through CARs. Second- and later-generation CARs simultaneously transmit costimulatory signals with CD3ζ signals upon ligation, but may lead to severe adverse effects owing to the recognition of minimal Ag expression outside the target tumor. Currently, the threshold target Ag density for CAR-T cell lysis and further activation, including cytokine production, has not yet been investigated in detail. Therefore, we determined the threshold target Ag density required to induce CAR-T cell responses using novel anti-CD20 CAR-T cells with a CD28 intracellular domain and a CD20-transduced CEM cell model. The newly developed CD20CAR–T cells demonstrated Ag-specific lysis and cytokine secretion, which was a reasonable level as a second-generation CAR. For lytic activity, the threshold Ag density was determined to be ∼200 molecules per target cell, whereas the Ag density required for cytokine production of CAR-T cells was ∼10-fold higher, at a few thousand per target cell. CD20CAR–T cells responded efficiently to CD20-downregulated lymphoma and leukemia targets, including rituximab- or ofatumumab-refractory primary chronic lymphocytic leukemia cells. Despite the potential influence of the structure, localization, and binding affinity of the CAR/Ag, the threshold determined may be used for target Ag selection. An Ag density below the threshold may not result in adverse effects, whereas that above the threshold may be sufficient for practical effectiveness. CD20CAR–T cells also demonstrated significant lytic activity against CD20-downregulated tumor cells and may exhibit effectiveness for CD20-positive lymphoid malignancies.

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“…Although this provided proof-of-principle for imparting functional capacity to T-lymphocytes enabling them to recognize and respond to the HER2/neu antigen, electroporation and the use of T-cell hybridomas was not readily translatable to the clinical arena. The development of retrovirus/lentivirus vectors provided for more efficient transduction of T-lymphocytes and NK cells [272][273][274][275][276][277][278][279][280]. Various groups have sought to refine the CAR constructs, including tuning affinity of the HER2/neu antigen-recognition domain [275], utilizing the T-cell receptor peptide recognition domain instead of an antibody-based recognition domain [281] and incorporation of costimulatory elements [282] within the construct.…”

Section: Her2/neu Antigen-specific Immunotherapymentioning

confidence: 99%

“…The development of retrovirus/lentivirus vectors provided for more efficient transduction of T-lymphocytes and NK cells [272][273][274][275][276][277][278][279][280]. Various groups have sought to refine the CAR constructs, including tuning affinity of the HER2/neu antigen-recognition domain [275], utilizing the T-cell receptor peptide recognition domain instead of an antibody-based recognition domain [281] and incorporation of costimulatory elements [282] within the construct. With the identification of Heregulin as a ligand for heterodimers involving HER3 or HER4, including those with HER2/neu, a chimeric ligand molecule (heregulin and intracellular signaling component from the CD3 ζ-chain) was developed [283].…”

Section: Her2/neu Antigen-specific Immunotherapymentioning

confidence: 99%

HER2/neu: an increasingly important therapeutic target. Part 1: basic biology & therapeutic armamentarium

Nelson¹

2014

Clinical Investigation

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Redirected Activity of Human Antitumor Chimeric Immune Receptors is Governed by Antigen and Receptor Expression Levels and Affinity of Interaction

Cited by 70 publications

References 35 publications

Novel CD4-Based Bispecific Chimeric Antigen Receptor Designed for Enhanced Anti-HIV Potency and Absence of HIV Entry Receptor Activity

Novel CD4-Based Bispecific Chimeric Antigen Receptor Designed for Enhanced Anti-HIV Potency and Absence of HIV Entry Receptor Activity

Target Antigen Density Governs the Efficacy of Anti–CD20-CD28-CD3 ζ Chimeric Antigen Receptor–Modified Effector CD8+ T Cells

HER2/neu: an increasingly important therapeutic target. Part 1: basic biology & therapeutic armamentarium

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