Interleukin-1α associates with the tumor suppressor p53 following DNA damage

Novak, Josef F.; Zámostná, Blanka; Vopálenský, Václav; Buryskova, Miroslava; Burýšek, Ladislav; Dolečková, Denisa; Pospíšek, Martin

doi:10.1038/s41598-020-63779-x

Cited by 3 publications

(2 citation statements)

References 83 publications

(103 reference statements)

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“…Moreover, the duration of the insult, which is not easy to predict in vitro, will be important to consider in the development of protocols based on transient immunomodulation. Links between IL-1 signaling and p53 have been reported in the context of tumor cells 45,46 , and the cGAS-STING axis is increasingly linked to DNA damage 47 , although the exact triggers of this pathway in the context of AAV-mediated CNS transduction remain to be de ned. Interestingly, the cGAS-STING signaling axis has been recently shown to drive chronic in ammation and functional decline during ageing in mice, with neuroprotective effects achieved using the H151 inhibitor 48 .…”

Section: Discussionmentioning

confidence: 99%

AAV vectors trigger DNA damage responses and STING-dependent inflammation in human CNS cells

Costa-Verdera,

Meneghini,

Fitzpatrick

et al. 2024

Preprint

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Adeno-associated viral (AAV) vector-based gene therapy is gaining foothold as a treatment option for a variety of genetic neurological diseases with encouraging clinical results. Nonetheless, dose-dependent toxicities and severe adverse events have emerged in recent clinical trials through mechanisms that remain unclear. We have modelled here the impact of AAV transduction in the context of cell models of the human central nervous system (CNS), taking advantage of induced pluripotent stem cell-based technologies. Our work uncovers vector-induced cell-intrinsic innate immune mechanisms that contribute to apoptosis in 2D and 3D models. While empty AAV capsids were well tolerated, the AAV genome triggered p53-dependent DNA damage responses across CNS cell types followed by induction of IL-1R- and STING-dependent inflammatory responses. In addition, transgene expression led to MAVS-dependent signaling and activation of type I interferon (IFN) responses. Cell-intrinsic and paracrine apoptosis onset could be prevented by inhibiting p53 or acting downstream of STING- and IL-1R-mediated responses. Activation of DNA damage, type I IFN and CNS inflammation were confirmed in vivo, in a mouse model. Together, our work identifies the cell-autonomous innate immune mechanisms of vector DNA sensing that can potentially contribute to AAV-associated neurotoxicity.

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Section: Discussionmentioning

confidence: 99%

AAV vectors trigger DNA damage responses and STING-dependent inflammation in human CNS cells

Costa-Verdera,

Meneghini,

Fitzpatrick

et al. 2024

Preprint

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“…In the Proximity Ligation Assay (PLA), a fluorescent signal is produced only when the molecules of interest are located in close proximity. In this case, the secondary antibodies, i.e., PLA probes, are not fluorescent by themselves, but they carry single stranded oligonucleotides that can synthesize fluorescent macromolecule in the simultaneous presence of the target enzymes [44,[72][73][74]. PLA in principle works when the proteins of interest are located in distances smaller than 40 nm, making it a competitive assay in terms of complex DNA damage detection.…”

Section: Proximity Ligation Assaymentioning

confidence: 99%

In Situ Detection of Complex DNA Damage Using Microscopy: A Rough Road Ahead

Nikitaki

Pariset

Sudar

et al. 2020

Cancers

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Complexity of DNA damage is considered currently one if not the primary instigator of biological responses and determinant of short and long-term effects in organisms and their offspring. In this review, we focus on the detection of complex (clustered) DNA damage (CDD) induced for example by ionizing radiation (IR) and in some cases by high oxidative stress. We perform a short historical perspective in the field, emphasizing the microscopy-based techniques and methodologies for the detection of CDD at the cellular level. We extend this analysis on the pertaining methodology of surrogate protein markers of CDD (foci) colocalization and provide a unique synthesis of imaging parameters, software, and different types of microscopy used. Last but not least, we critically discuss the main advances and necessary future direction for the better detection of CDD, with important outcomes in biological and clinical setups.

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