Therapy-induced senescence upregulates antigen presentation machinery and triggers anti-tumor immunity in Acute Myeloid Leukemia

Gilioli, Diego; Fusco, Simona; Tavella, Teresa; Giannetti, Kety; Conti, Anastasia; Santoro, Antonella; Carsana, Edoardo; Beretta, Stefano; Gambacorta, Valentina; Aletti, Federico; Carraba, Matteo Giovanni; Bonini, Chiara; Ciceri, Fabio; Merelli, Ivan; Vago, Luca; Schmitt, Clemens A.; Micco, Raffaella Di

doi:10.1101/2022.11.17.515658

Cited by 5 publications

(3 citation statements)

References 51 publications

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“…The activation of IFN signaling is propaedeutic for MHC-I overexpression and subsequent CD8 T cell mediated killing 16 . These results are further supported by a recent preprint by Di Micco and colleagues who also report high levels of MHC-I in chemotherapy-treated primary human senescent leukemia cells 17 . Also, these findings are aligned with previous data from the Van Deursen and Schmitt labs placing macrophages at the interface between stressed/senescent cells and CD8 T cell mediated clearance 18,19 .…”

supporting

confidence: 75%

Recent insights into the crosstalk between senescent cells and CD8 T lymphocytes

2023

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Recent reports in oncological and non-oncological experimental setups provide strong evidence that senescent cells are under the surveillance of CD8 T cell-mediated adaptive immunity. These new data also shed light on the mechanisms that sensitize senescent cells to CD8 T cell-dependent killing, as well as those that enable senescent cells to evade CD8 T cell immunosurveillance. Understanding the interplay between cellular senescence and the adaptive immune system may open new strategies to ameliorate aging and aging-associated diseases.

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supporting

confidence: 75%

Recent insights into the crosstalk between senescent cells and CD8 T lymphocytes

2023

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“…Combining Abemaciclib with anti-PD-L1, an immune checkpoint inhibitor, results in further tumor suppression [211]. Senescent AML cells triggered by cytosine arabinoside also display increased MHC expression, effectively activating T cell proliferation [212]. This effect can be enhanced by the anti-PD-1 antibody Nivolumab [212].…”

Section: Adaptive Immune Responses Activated By Sncsmentioning

confidence: 99%

“…Senescent AML cells triggered by cytosine arabinoside also display increased MHC expression, effectively activating T cell proliferation [212]. This effect can be enhanced by the anti-PD-1 antibody Nivolumab [212]. These synergies suggest a potential combination strategy of senescence-inducing therapies with immune checkpoint inhibitors to achieve enhanced cancer control.…”

Section: Adaptive Immune Responses Activated By Sncsmentioning

confidence: 99%

Therapy-induced cellular senescence: Potentiating tumor elimination or driving cancer resistance and recurrence?

Liu,

Lomeli,

Kron

2024

Preprint

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Cellular senescence has recently been recognized as a hallmark of cancer, reflecting its association with aging and inflammation, its role as a response to deregulated proliferation and oncogenic stress, and its induction by cancer therapies such as radiation, chemotherapy, and targeted agents. While such therapy-induced senescence (TIS) has been linked to resistance, recurrence, metastasis and normal tissue toxicity, TIS has the potential to enhance therapy response and stimulate anti-tumor immunity. In this review, we examine the Jekyll and Hyde nature of senescent cells (SnCs), with a particular focus on how their persistence while expressing the senescence-associated secretory phenotype (SASP) modulates the tumor microenvironment through autocrine and paracrine mechanisms. Via the SASP, the formation of SnCs may alternately mediate resistance or response to conventional therapy. Further, toward fulfilling the unmet potential of cancer immunotherapy, we consider how SnCs may influence tumor inflammation and serve as a source of antigen to potentiate anti-tumor immunity. This new view suggests treatment strategies based on inducing TIS to enhance immune checkpoint blockade. Finally, we describe strategies for mitigating the detrimental effects of senescence, such as modulating the SASP or targeting SnC persistence, toward enhancing the benefits of cancer treatment.

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PRMT9 inhibition sparks immune responses in AML

Santoro,

Di Micco

2024

Nat Cancer

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Therapy-induced senescence upregulates antigen presentation machinery and triggers anti-tumor immunity in Acute Myeloid Leukemia

Cited by 5 publications

References 51 publications

Recent insights into the crosstalk between senescent cells and CD8 T lymphocytes

Recent insights into the crosstalk between senescent cells and CD8 T lymphocytes

Therapy-induced cellular senescence: Potentiating tumor elimination or driving cancer resistance and recurrence?

PRMT9 inhibition sparks immune responses in AML

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