Increasing LFA-1 Expression Enhances Immune Synapse Architecture and T Cell Receptor Signaling in Jurkat E6.1 Cells

Cassioli, Chiara; Bálint, Štefan; Compeer, Ewoud B.; Felce, James H.; Gamberucci, Alessandra; Bella, Chiara Della; Felce, Suet Ling; Brunetti, Jlenia; Valvo, Salvatore; Pende, Daniela; D’Elios, M M; Moretta, Lorenzo; Dustin, Michael L.; Baldari, Cosima T.

doi:10.3389/fcell.2021.673446

Cited by 14 publications

(10 citation statements)

References 54 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…For this purpose, we have used the Jurkat human T cell line, which has been widely used to study T cell activation, signaling, and IS assembly. 36 Contrary to primary T cells, Jurkat cells can be easily expanded and long-term cultured after transduction without losing CAR expression or BiTE secretion, avoiding transduction-to-transduction differences and loss of transgene expression. In addition, clonal stimulation by superantigens provides a proper control that mimics the canonical IS and, together with the high transduction efficiency achieved in Jurkat cells, allows to perform experiments with a high number of T cell-target cell interactions.…”

Section: Discussionmentioning

confidence: 99%

Synapse topology and downmodulation events determine the functional outcome of anti-CD19 T cell-redirecting strategies

et al. 2022

View full text Add to dashboard Cite

Cancer immunotherapy strategies based on the endogenous secretion of T cell-redirecting bispecific antibodies by engineered T lymphocytes (STAb-T) are emerging as alternative or complementary approaches to those based on chimeric antigen receptors (CAR-T). The antitumor efficacy of bispecific anti-CD19 × anti-CD3 (CD19×CD3) T cell engager (BiTE)-secreting STAb-T cells has been demonstrated in several mouse models of B-cell acute leukemia. Here, we have investigated the spatial topology and downstream signaling of the artificial immunological synapses (IS) that are formed by CAR-T or STAb-T cells. Upon interaction with CD19-positive target cells, STAb-T cells form IS with structure and signal transduction, which more closely resemble those of physiological cognate IS, compared to IS formed by CAR-T cells expressing a second-generation CAR bearing the same CD19-single-chain variable fragment. Importantly, while CD3 is maintained at detectable levels on the surface of STAb-T cells, indicating sustained activation mediated by the secreted BiTE, the anti-CD19 CAR was rapidly downmodulated, which correlated with a more transient downstream signaling. Furthermore, CAR-T cells, but not STAb-T cells, provoke an acute loss of CD19 in target cells. Such differences might represent advantages of the STAb-T strategy over the CAR-T approach and should be carefully considered in order to develop more effective and safer treatments for hematological malignancies.

show abstract

Section: Discussionmentioning

confidence: 99%

Synapse topology and downmodulation events determine the functional outcome of anti-CD19 T cell-redirecting strategies

et al. 2022

View full text Add to dashboard Cite

show abstract

“…Our data show that SARS-CoV-2 Spike protein binding to ACE2 interferes with the assembly of a functional IS in CTLs by inhibiting the process at an early step, concomitant with ACE2 exclusion from the IS. Potential targets of the ACE2-Spike axis are integrins, such as LFA-1, which are essential for the generation of well-structured immune synapses characterized by the tight accumulation of TCR/CD3 complexes at the center of the contact area with the APC ( Cassioli et al, 2021a ). ACE2 has been reported to constitutively interact with β1 and α5 integrins, promoting cell adhesion and modulating downstream signaling ( Clarke et al, 2012 ; Lin et al, 2004 ).…”

Section: Resultsmentioning

confidence: 99%

SARS-CoV-2 Spike protein suppresses CTL-mediated killing by inhibiting immune synapse assembly

Onnis

Andreano

Cassioli

et al. 2022

Journal of Experimental Medicine

Self Cite

View full text Add to dashboard Cite

CTL-mediated killing of virally infected or malignant cells is orchestrated at the immune synapse (IS). We hypothesized that SARS-CoV-2 may target lytic IS assembly to escape elimination. We show that human CD8+ T cells upregulate the expression of ACE2, the Spike receptor, during differentiation to CTLs. CTL preincubation with the Wuhan or Omicron Spike variants inhibits IS assembly and function, as shown by defective synaptic accumulation of TCRs and tyrosine phosphoproteins as well as defective centrosome and lytic granule polarization to the IS, resulting in impaired target cell killing and cytokine production. These defects were reversed by anti-Spike antibodies interfering with ACE2 binding and reproduced by ACE2 engagement by angiotensin II or anti-ACE2 antibodies, but not by the ACE2 product Ang (1-7). IS defects were also observed ex vivo in CTLs from COVID-19 patients. These results highlight a new strategy of immune evasion by SARS-CoV-2 based on the Spike-dependent, ACE2-mediated targeting of the lytic IS to prevent elimination of infected cells.

show abstract

“…We tested suspension CHO-ES cells to compare against adherent CHO-K1 cells. Lastly, we also tested Jurkat cells which were isolated in 1977 and have become an in vitro system useful to study T-cell biology and MCF-7 which is a breast cancer cell line that was established in 1973 and has been used to study estrogen responses, hormone resistance, and testing of potential cancer therapeutics such as tamoxifen (Cassioli et al 2021 ; Lee et al 2015 ). Additionally, MCF-7 has been used to investigate the importance of the interaction between cancer cells, angiogenesis, cellular metabolism, and respiration (Comşa et al 2015 ).…”

Section: Resultsmentioning

confidence: 99%

High efficiency sorting and outgrowth for single-cell cloning of mammalian cell lines

Munoz

Morachis

2022

Biotechnol Lett

View full text Add to dashboard Cite

Single-cell selection and cloning is required for multiple bioprocessing and cell engineering workflows. Dispensing efficiency and outgrowth were optimized for multiple common suspension (CHO ES, Expi293F, and Jurkat) and adherent (MCF-7, A549, CHO-K1, and HEK293) cell lines. Single-cell sorting using a low pressure microfluidic cell sorter, the WOLF Cell Sorter, was compared with limiting dilution at 0.5 cells/well to demonstrate the increased efficiency of using flow cytometry selection of cells. In this work, there was an average single cell deposition on Day 0 of 89.1% across all the cell lines tested compared to 41.2% when using limiting dilution. After growth for 14 days, 66.7% of single-cell clones sorted with the WOLF Cell Sorter survived and only 23.8% when using limiting dilution. Using the WOLF Cell Sorter for cell line development results in higher viable single-cell colonies and the ability to select subpopulations of single-cells using multiple parameters.

show abstract

Increasing LFA-1 Expression Enhances Immune Synapse Architecture and T Cell Receptor Signaling in Jurkat E6.1 Cells

Cited by 14 publications

References 54 publications

Synapse topology and downmodulation events determine the functional outcome of anti-CD19 T cell-redirecting strategies

Synapse topology and downmodulation events determine the functional outcome of anti-CD19 T cell-redirecting strategies

SARS-CoV-2 Spike protein suppresses CTL-mediated killing by inhibiting immune synapse assembly

High efficiency sorting and outgrowth for single-cell cloning of mammalian cell lines

Contact Info

Product

Resources

About