Requirement for CD28 co-stimulation is lower in SHP-1-deficient T cells

Sathish, Jean G.; Johnson, Kenneth G.; LeRoy, Frances; Fuller, Kerenza J.; Hallett, Maurice Bartlett; Brennan, Paul; Borysiewicz, Leszek K.; Sims, Martin; Matthews, R. James

doi:10.1002/1521-4141(200112)31:12<3649::aid-immu3649>3.0.co;2-8

Cited by 20 publications

(11 citation statements)

References 35 publications

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“…Similarly, the SH2-domain-containing protein tyrosine phosphatase 1 (SHP-1) can reduce costimulation as observed in SHP-1-deficient CD4 + thymocytes. 106,107 In keeping with this, SHP-1 associates in a complex with Vav1, Grb-2 and Sos1. 105 The suppressor cytokine IL-10 has also been reported to activate SHP-1 and in the process, suppress PI3K binding to CD28.…”

Section: Cd28 and Negative Regulationmentioning

confidence: 59%

CD28 co‐signaling in the adaptive immune response

Riha¹,

Rudd²

2010

Self/Nonself

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Section: Cd28 and Negative Regulationmentioning

confidence: 59%

CD28 co‐signaling in the adaptive immune response

Riha¹,

Rudd²

2010

Self/Nonself

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“…Among these phosphatases, only PTEN and SHP-1, which were also shown to reduce IL-2 production (76, 78), have been linked to autoimmune phenomena. Specifically, mice carrying PTEN gene mutations present impaired Fas-mediated apoptosis and develop autoimmune disease (81), while SHP-1-deficient mice produce pathogenic autoantibodies and suffer from lupus-like glomerulonephritis (76). In addition, autoimmune phenomena are documented in patients with Cowden syndrome, a disease caused by germline PTEN mutations (82).…”

Section: Discussionmentioning

confidence: 99%

Protein phosphatase 2A is a negative regulator of IL-2 production in patients with systemic lupus erythematosus

Katsiari

Kyttaris²,

Juang³

et al. 2005

Journal of Clinical Investigation

140

145

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“…In order to mimic clinical adoptive transfer strategies, T-cells were subject to three rounds of in vitro antigen stimulation prior to transfer. Although this system might appear to fail to take advantage of the increased antigen-dependent proliferation of naive SHP-1 null T-cells described by Sathish et al [37,61], the authors observed increased proliferation of transferred effector T-cells in response to tumour in vivo , reduced apoptosis and improved survival of SHP-1 −/− T-cells, and, ultimately improved clearance of leukaemia. This demonstrates that abrogation of SHP-1 is beneficial in effector T-cells, not just in naive T-cells, and therefore knocking out SHP-1 in in vitro -activated, genetically modified T-cells would still add value to adoptive transfer strategies.…”

Section: Shp-1 Abrogation In Cancer Therapymentioning

confidence: 99%

“…In the absence of SHP-1, CD8 T-cells form more stable and durable synapses with antigen presenting cells (APCs) [37]. This leads to reduced activation thresholds and increased proliferation [38], which is beneficial for any kind of adoptive transfer strategy for two reasons: firstly, numbers of T-cells available for transfer are often limited, especially where genetic modification is involved; and, secondly it is known that the balance of regulatory T-cells to effector T-cells is key in tumour progression [39], so any modification that can bias towards increased effector T-cells is likely to improve treatment efficacy (Figure 2). It is worth noting that SHP-1 has also been shown to be inhibitory to T regulatory cells [40], and therefore inhibition of SHP-1 in these cells leads to increased suppressor function.…”

Section: Src Homology 2 Domain-containing Protein Tyrosine Phosphatasmentioning

confidence: 99%

SHP-1: the next checkpoint target for cancer immunotherapy?

Watson

Wehenkel

Matthews

et al. 2016

Biochemical Society Transactions

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The immense power of the immune system is harnessed in healthy individuals by a range of negative regulatory signals and checkpoints. Manipulating these checkpoints through inhibition has resulted in striking immune-mediated clearance of otherwise untreatable tumours and metastases; unfortunately, not all patients respond to treatment with the currently available inhibitors of cytotoxic T-lymphocyte-associated protein 4 (CTLA-4) and programmed cell death protein 1 (PD-1). Combinatorial studies using both anti-CTLA-4 and anti-PD-1 demonstrate synergistic effects of targeting multiple checkpoints, paving the way for other immune checkpoints to be targeted. Src homology 2 domain-containing protein tyrosine phosphatase 1 (SHP-1) is a widely expressed inhibitory protein tyrosine phosphatase (PTP). In T-cells, it is a negative regulator of antigen-dependent activation and proliferation. It is a cytosolic protein, and therefore not amenable to antibody-mediated therapies, but its role in activation and proliferation makes it an attractive target for genetic manipulation in adoptive transfer strategies, such as chimeric antigen receptor (CAR) T-cells. This review will discuss the potential value of SHP-1 inhibition in future tumour immunotherapy.

show abstract

Requirement for CD28 co-stimulation is lower in SHP-1-deficient T cells

Cited by 20 publications

References 35 publications

CD28 co‐signaling in the adaptive immune response

CD28 co‐signaling in the adaptive immune response

Protein phosphatase 2A is a negative regulator of IL-2 production in patients with systemic lupus erythematosus

SHP-1: the next checkpoint target for cancer immunotherapy?

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