Deficiency of CD73/ecto-5′-nucleotidase in mice enhances acute graft-versus-host disease

Tsukamoto, Hiroki; Chernogorova, Petya; Ayata, Cemil Korcan; Gerlach, Uwe; Rughani, Ankur; Ritchey, Jerry W.; Ganesan, Jayanthi; Follo, Marie; Zeiser, Robert; Thompson, Linda F.; Idzko, Marco

doi:10.1182/blood-2011-09-375899

Cited by 85 publications

(90 citation statements)

References 51 publications

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“…In particular, CD73 expression on Foxp3 þ T regulatory cells is important for their suppression of antitumor immunity (15). Notably, host CD73 has been shown to protect against acute graft versus host disease and to inhibit graft versus leukaemia effect (17). Taken together, these studies suggest that CD73 may be a valid therapeutic target to enhance antitumor immunity.…”

Section: Introductionmentioning

confidence: 76%

CD73-Deficient Mice Are Resistant to Carcinogenesis

Stagg

Beavis²,

Divisekera³

et al. 2012

Cancer Research

187

166

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CD73 is a cell surface 5 0 -nucleotidase that converts AMP to adenosine, an immune suppressive molecule. CD73 may promote immune escape in cancer by contributing to the degradation of extracellular ATP released by dying cancer cells in hypoxic tumors or following chemotherapy. However, whether CD73 exerts a critical oncogenic function during tumorigenesis is unknown. In this study, we used genetically deficient mice to investigate its contribution to autochthonous tumor formation. CD73 deficiency suppressed the development of 3-methylcholanthrene (MCA)-induced fibrosarcomas through a mechanism relying upon IFN-g, natural killer (NK) cells, and CD8 þ T cells. Similarly, CD73 deficiency also suppressed prostate tumorigenesis in TRAMP transgenic mice.Importantly, treatment with an anti-CD73 monoclonal antibody effectively suppressed growth of established MCA-induced tumors or TRAMP-C1 prostate tumors and inhibited the development of TRAMP-C1 lung metastases. The therapeutic activity of anti-CD73 monoclonal antibody against primary tumors was dependent on CD8 þ T cells, whereas its antimetastatic activity was dependent on host CD73 expression independent of T cells or NK cells. Taken together, our findings indicate that CD73 is a critical factor in tumorigenesis and that anti-CD73 antibodies may offer a novel generalized strategy to blunt immune escape and treat cancer. Cancer Res; 72(9); 2190-6. Ó2012 AACR.

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Section: Introductionmentioning

confidence: 76%

CD73-Deficient Mice Are Resistant to Carcinogenesis

Stagg

Beavis²,

Divisekera³

et al. 2012

Cancer Research

187

166

View full text Add to dashboard Cite

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“…However, recent experimental studies suggests a role for DAMPs such as ATP, heparan sulfate (HS), and uric acid, in enhancing allogeneic T-cell responses and in exacerbating GVHD. 15,17,32 Clinically, the data also suggests that response to DAMPs such as HMGB-1, 35 heat shock protein 70 (HSP70), 36,37 and HSP90 38 may be associated with GVHD severity in humans. In line with this notion, several pattern recognition receptors that are known to activate innate immunity in response to DAMP-mediated stimulation of APCs have been shown to exacerbate GVHD.…”

Section: Discussionmentioning

confidence: 99%

“…Host tissue damage after conditioning is known to lead to the release of not only proinflammatory cytokines, but also DAMPs and PAMPs. 6,15,27,[32][33][34] Both DAMPs and PAMPs can activate APCs and enhance T-cell responses. 7 The role of PAMPs in exacerbating GVHD may be model/context dependent.…”

Section: Discussionmentioning

confidence: 99%

Siglec-G–CD24 axis controls the severity of graft-versus-host disease in mice

Toubai

Hou

Mathewson

et al. 2014

Blood

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“…Activated Tcons proliferate and trigger release of alarmins, such as IL-33 and its soluble receptor ST2, from non-HP APCs, such as stromal cells and endothelium; these activated Tcons also express the integrin receptor α 4 β 7 , which directs their migration back to intestinal tissue after entering the villus capillaries. the absence of CD73 on either donor T cells or host APCs exacerbated GVHD (54)(55)(56). UA, a purine metabolite released from damaged cells, is an endogenous DAMP that stimulates DCs and activates CD8 + T cell cytotoxic functions (45,57).…”

Section: Immune Homeostasis In the Gi Tractmentioning

confidence: 99%

Altered homeostatic regulation of innate and adaptive immunity in lower gastrointestinal tract GVHD pathogenesis

Ferrara¹,

Smith²,

Sheets³

et al. 2017

Journal of Clinical Investigation

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Acute graft-versus-host disease (aGVHD) was noted as a complication of allogeneic bone marrow (BM) transplantation in animal models more than six decades ago (1, 2). The initial descriptions of aGVHD differentiated it from the complications of BM aplasia and focused on the severe consequences of GVHD for lower gastrointestinal (GI) tract function, as manifested by weight loss and profound diarrhea. Subsequent studies clearly identified donor T cells as the critical cells required for the induction of aGVHD (3)(4)(5). aGVHD was shown to predominantly involve the skin, liver, and lower GI tract and, later, the upper GI tract (6). In the absence of approaches to prevent aGVHD, this complication occurs in close to 100% of recipients of allogeneic BM/stem cell transplants (allogeneic hematopoietic cell transplantation, allo-HCT), greatly limiting the survival of the first cohort of patients who underwent allo-HCT. Lower GI tract GVHD: clinical findingsDespite the use of prophylaxis to prevent aGVHD, without rigorous T cell depletion this complication occurs in 30%-70% of patients undergoing allo-HCT (7-9). Standard treatment of aGVHD is the administration of systemic corticosteroids and additional immunosuppressive agents, which, as primary therapy, do not substantially improve patient outcomes (10). Thirty to seventyfive percent of patients who develop aGVHD will have a complete response to corticosteroid therapy (11).The outcome for patients with severe aGVHD (grades III-IV) of the lower GI tract is poor, with 25% overall survival (12). Four risk factors (corticosteroid resistance, age under 18 years at time of transplant, GI tract bleeding, and total bilirubin greater than 3 mg/dl) were found on multivariate analysis to be statistically associated with poor survival; no patients with all 4 factors survived, highlighting the critical need to improve survival for these patients. This Review will focus on recent findings regarding the homeostatic mechanisms of the lower GI tract that relate to the pathophysiology of aGVHD involving the distal small intestine and colon. Immune homeostasis in the GI tractThe immune balance of the human small intestine and colon is complex. There are over 100 trillion bacteria that are critical to the function of the GI tract, and individuals are exposed to a huge number of food-borne antigens on a daily basis. Thus, there must exist dynamic and robust mechanisms that mediate immune responses to pathogenic organisms but that prevent immune responses to normal flora and dietary antigens.Antigen-presenting cells in the GI tract. Specialized hematopoietic antigen-presenting cells (APCs) in the GI tract include multiple subpopulations of dendritic cells (DCs) and macrophages ( Figure 1). DCs in the lamina propria (LP) and Peyer's patch sample luminal antigens and migrate to regional lymph nodes (LNs) to activate immune responses (13,14). Macrophages are sessile and are the most abundant innate immune cells in the intestine; they maintain homeostasis by phagocytosing microorganisms and apop...

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Deficiency of CD73/ecto-5′-nucleotidase in mice enhances acute graft-versus-host disease

Cited by 85 publications

References 51 publications

CD73-Deficient Mice Are Resistant to Carcinogenesis

CD73-Deficient Mice Are Resistant to Carcinogenesis

Siglec-G–CD24 axis controls the severity of graft-versus-host disease in mice

Altered homeostatic regulation of innate and adaptive immunity in lower gastrointestinal tract GVHD pathogenesis

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