The DNA Damage Response and Inflammation in Cancer

Klapp, Vanessa; Álvarez-Abril, Beatriz; Leuzzi, Giuseppe; Kroemer, Guido; Ciccia, Alberto; Galluzzi, Lorenzo

doi:10.1158/2159-8290.cd-22-1220

Cited by 30 publications

(9 citation statements)

References 293 publications

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“…This particularity increases cancer antigenicity and hence influences tumor surveillance by adaptive immune effector cells as well as the response to immune checkpoint inhibitors (ICIs). 2 , 3 Along this line, the Immunoscore (IS) has been internationally validated for refining the prognosis of CRC. It consists in measuring the density of CD3 + T lymphocytes, and their cytotoxic CD8 + T cell subset, in both the center and invasive margin of the tumor.…”

Section: Main Textmentioning

confidence: 99%

Single-cell analysis of T lymphocytes infiltrating colorectal carcinoma: the dilemma of specificity

Lizarralde-Guerrero,

Zucaro,

Kroemer

et al. 2024

OncoImmunology

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Section: Main Textmentioning

confidence: 99%

Single-cell analysis of T lymphocytes infiltrating colorectal carcinoma: the dilemma of specificity

Lizarralde-Guerrero,

Zucaro,

Kroemer

et al. 2024

OncoImmunology

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“…At least in some cancers, such a propensity to accumulate mutations is driven by defects in a specific mechanism of DNA repair called mismatch repair (MMR), which is associated with the instability of specific DNA regions called microsatellites. 40 Accordingly, tumors with a molecular diagnosis of defective MMR (dMMR) or elevated (high) microsatellite instability (MSI-H) are exquisitely sensitive to ICIs, 41 which resulted in the FDA approval of pembrolizumab for use in patients with dMMR/MSI-H cancers irrespective of tissue of origin. 42 That said, TMB testing does not account for the immunological alterations imposed by genetic defects other than single nucleotide mutations, such as indels and frameshift mutations.…”

Section: Immunological Biomarkersmentioning

confidence: 99%

Immunosurveillance in clinical cancer management

Kroemer,

Chan,

Eggermont

et al. 2023

CA A Cancer J Clinicians

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The progression of cancer involves a critical step in which malignant cells escape from control by the immune system. Antineoplastic agents are particularly efficient when they succeed in restoring such control (immunosurveillance) or at least establish an equilibrium state that slows down disease progression. This is true not only for immunotherapies, such as immune checkpoint inhibitors (ICIs), but also for conventional chemotherapy, targeted anticancer agents, and radiation therapy. Thus, therapeutics that stress and kill cancer cells while provoking a tumor‐targeting immune response, referred to as immunogenic cell death, are particularly useful in combination with ICIs. Modern oncology regimens are increasingly using such combinations, which are referred to as chemoimmunotherapy, as well as combinations of multiple ICIs. However, the latter are generally associated with severe side effects compared with single‐agent ICIs. Of note, the success of these combinatorial strategies against locally advanced or metastatic cancers is now spurring successful attempts to move them past the postoperative (adjuvant) setting to the preoperative (neoadjuvant) setting, even for patients with operable cancers. Here, the authors critically discuss the importance of immunosurveillance in modern clinical cancer management.

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“…153 Defects in type I IFN signaling have also been associated with resistance to ICIs targeting cytotoxic T lymphocyte-associated protein 4 (CTLA4) or programmed cell death 1 (PDCD1, best known as PD-1) in preclinical models of melanoma, CRC, and other tumor types. 113,140 In line with this notion, ICIs and other immunotherapeutic agents have been shown to synergize with type I IFN-eliciting interventions in a variety of preclinical settings, including (but not limited to): (1) CRC-bearing mice receiving a PD-1 blocker plus a PARP7 inhibitor, 151 (2) mice with established melanomas, CRCs or mammary tumors receiving focal RT plus a number of different immunotherapeutics, 107,148,149,[154][155][156][157] (3) mammary tumor-bearing mice treated with an HER2 blocker (which at least partially relies on type I IFN signaling) or a TLR3 agonist plus an ICI targeting PD-1, 152,158 and (4) homologous recombination deficient (HRD) mouse mammary and ovarian tumors established in immunocompetent syngeneic hosts and treated with the poly(ADP-ribose) polymerase 1 (PARP1) inhibitor olaparib, which drives potent type I IFN responses, 26 and a PD-1 blocker. 159 That said, type I IFN signaling has also been associated with resistance to immunostimulatory anticancer agents including RT optionally combined with an ICI targeting PD-L1 in various preclinical tumor models, at least in part reflecting the ability of type I IFN to elicit the upregulation of serpin family B member 9 (SERPINB9), a potent cytoprotective factor.…”

Section: Response To Therapymentioning

confidence: 99%

“…Importantly, PRRs not only respond to PAMPs, but also to endogenous molecules commonly known as damage-associated molecular patterns (DAMPs). 25 The emission of these danger signals, which include a plethora of proteins, nucleic acids, and lipids that in physiological conditions are physically separated and hence cannot interact with cognate PRRs (e.g., nuclear and mitochondrial nucleic acids), [26][27][28][29] play indeed a key role in determining the immunogenicity of dying cancer cells. 30 (RAP1A).…”

Section: An Cer Cell-intrin S I C Effec Ts Of T Ype I Ifnmentioning

confidence: 99%

Type I interferon and cancer

Holicek,

Guilbaud,

Klapp

et al. 2023

Immunological Reviews

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SummaryType I interferon (IFN) is a class of proinflammatory cytokines with a dual role on malignant transformation, tumor progression, and response to therapy. On the one hand, robust, acute, and resolving type I IFN responses have been shown to mediate prominent anticancer effects, reflecting not only their direct cytostatic/cytotoxic activity on (at least some) malignant cells, but also their pronounced immunostimulatory functions. In line with this notion, type I IFN signaling has been implicated in the antineoplastic effects of various immunogenic therapeutics, including (but not limited to) immunogenic cell death (ICD)‐inducing agents and immune checkpoint inhibitors (ICIs). On the other hand, weak, indolent, and non‐resolving type I IFN responses have been demonstrated to support tumor progression and resistance to therapy, reflecting the ability of suboptimal type I IFN signaling to mediate cytoprotective activity, promote stemness, favor tolerance to chromosomal instability, and facilitate the establishment of an immunologically exhausted tumor microenvironment. Here, we review fundamental aspects of type I IFN signaling and their context‐dependent impact on malignant transformation, tumor progression, and response to therapy.

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The DNA Damage Response and Inflammation in Cancer

Cited by 30 publications

References 293 publications

Single-cell analysis of T lymphocytes infiltrating colorectal carcinoma: the dilemma of specificity

Single-cell analysis of T lymphocytes infiltrating colorectal carcinoma: the dilemma of specificity

Immunosurveillance in clinical cancer management

Type I interferon and cancer

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