L-Arginine Modulates T Cell Metabolism and Enhances Survival and Anti-tumor Activity

Geiger, Roger; Rieckmann, Jan C.; Wolf, Tobias; Basso, Camilla; Feng, Yuehan; Fuhrer, Tobias; Kogadeeva, Maria; Picotti, Paola; Meissner, Felix; Mann, Matthias; Zamboni, Nicola; Sallusto, Federica; Lanzavecchia, Antonio

doi:10.1016/j.cell.2016.09.031

Cited by 1,196 publications

(1,169 citation statements)

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“…15 Tcells activation consumes large amount of L-arginine, and the underlying mechanism was nicely demonstrated. 15 Given the fact that arginase-mediated L-arginine depletion profoundly suppress T-cell immune response, 20,21 L-arginine supplementation is a good idea to feed the T-cells, and to inhibit tumor growth. However, malignancies, especially solid tumors, can escape from or impair immune attack by multiple mechanisms.…”

Section: Discussionmentioning

confidence: 83%

“…13,14 Thus, following these theories, L-arginine supplementation was recently proved to enhance T-cell survival and antitumor activity. 15,16 In this study, we tried to validate our hypothesis that L-arginine supplementation and PD-1/PD-L1 pathway blockade can facilitate spontaneous immune response against osteosarcoma. We established immunocompetent mouse models using BALB/ c mice bearing in situ osteosarcoma or metastasized osteosarcoma, and then treated them with L-arginine and/or a-PD-L1 antibody.…”

Section: Introductionmentioning

confidence: 99%

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Combination therapy with L-arginine and α-PD-L1 antibody boosts immune response against osteosarcoma in immunocompetent mice

Lin

et al. 2017

Cancer Biology & Therapy

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L-arginine supplementation was recently proved to promote the function of immune cells, especially Tcells, by facilitating T-cell proliferation, differentiation and survival in vivo. Cytotoxic CD8 C plays a crucial role in modulating anti-cancer response mediated by the immune system, but was restricted by exhaustion. Thus, we hypothesized that L-arginine, in combination with a-PD-L1 antibody, may provide a favored environment for T-cell response against osteosarcoma. Immunocompetent BALB/c mouse models bearing orthotopic and metastatic osteosarcoma were established to validate this conjecture. We found that L-arginine significantly elevated the number of splenic CD8 C T-cells, the level of serum interferon-g, and CD8 C T-cell infiltration. Furthermore, a-PD-L1 antibody protected these amplified CD8 C T-cells from exhaustion, and therefore strengthened the secretion of interferon-g, granzyme B and perforin by these Tcells. As a result, this combination treatment strategy significantly prolonged survival of osteosarcoma bearing mice, suggesting that L-arginine supplementation in combination with a-PD-L1 antibody may be a promising method for osteosarcoma patients.

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Section: Discussionmentioning

confidence: 83%

Section: Introductionmentioning

confidence: 99%

Combination therapy with L-arginine and α-PD-L1 antibody boosts immune response against osteosarcoma in immunocompetent mice

Lin

et al. 2017

Cancer Biology & Therapy

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“…Considering the tight connection existing between mitochondrial metabolism and the shape of the mitochondrial network (see [209] for a review), we could expect an involvement of mitochondrial dynamics in TILs metabolism inside the tumor mass. Of note, it is still unknown whether or not differentiation to an exhausted phenotype in TILs could also affect mitochondrial dynamics, in addition to its well-established role on T EX mitochondrial metabolism [207,210]. Recently, by a microarray analysis in chronic viral-infected patients fit has been found that exhausted CD8+ T cells show significant downregulation in the expression of several genes associated with mitochondrial OXPHOS metabolism, and upregulation of the oxidative stress pathway.…”

Section: Cell Exhaustionmentioning

confidence: 99%

The mitochondrial dynamics in cancer and immune-surveillance

Simula

Nazio

Campello

2017

Seminars in Cancer Biology

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A B S T R A C TMitochondria-shaping proteins control the dynamic equilibrium between fusion and fission of the mitochondrial network. Their balance is strictly required to regulate various processes, including the quality of mitochondria, cell metabolism, cell death, proliferation and cell migration. Alterations in these processes are frequently encountered in cancer, during both its onset and later progression, as evidence emerge connecting alterations in mitochondrial dynamics with cancer development. In recent years, novel therapeutic approaches to fight against different human tumors aim at exploiting the immune system's ability to specifically recognize tumor antigens, thus killing malignant cells in a process named immune-surveillance. Interestingly, data are accumulating on the role that mitochondrial dynamics play also for the correct function of both the innate and the adaptive immune system. By this review, we overview how mitochondrial dynamics can affect various processes during cancer development, acting directly on tumor cells or indirectly on cells responsible for tumor aggression and defence.

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“…Повышенная метаболическая ак-тивность в ходе экспансии ex vivo может приводить Т-клетки к состоянию, в котором они имеют низкую способность к персистенции in vivo и, следовательно, к слабому противоопухолевому ответу. Результаты не-давнего исследования показали, что добавление арги-нина в культуральную среду в ходе экспансии ex vivo способно усилить окислительный и подавить гликоли-тический метаболизм, что позволяет добиться получе-ния большого количества более эффективных проти-воопухолевых клеток [52]. Таким образом, условия культивирования, в которых метаболическая активность противоопухолевых Т-клеток ограничивается в ходе экспансии ex vivo, могут приводить к продукции клеток с характеристиками, способствующими их использова-нию в иммунотерапии.…”

Section: т-клетки Cd8unclassified