1. Kim, J. et al. VDAC oligomers form mitochondrial pores to release mtDNA fragments and promote lupus-like disease. Science 366, 1531–1536 (2019). This paper reports that during oxidative stress the mtDNA is released via pores formed by voltage-dependent anion channel (VDAC) oligomers in the outer mitochondrial membrane.

2. Liu, H. et al. Prohibitin 1 regulates mtDNA release and downstream inflammatory responses. EMBO J. 41, e111173 (2022). This paper reports that PHB1 is crucial for mtDNA release and inflammatory responses by regulating mitochondrial inner membrane permeability.

3. Vargas, J. N. S., Hamasaki, M., Kawabata, T., Youle, R. J. & Yoshimori, T. The mechanisms and roles of selective autophagy in mammals. Nat. Rev. Mol. Cell Biol. 24, 167–185 (2023). A review that presents mechanisms and functions of mitophagy and other types of selective autophagy.

4. Gehrke, N. et al. Oxidative damage of DNA confers resistance to cytosolic nuclease TREX1 degradation and potentiates STING-dependent immune sensing. Immunity 39, 482–495 (2013). This paper reports that oxidative damage to DNA potentiates cytosolic immune recognition by decreasing the susceptibility of damaged DNA to TREX1-mediated degradation.

5. West, A. P. & Shadel, G. S. Mitochondrial DNA in innate immune responses and inflammatory pathology. Nat. Rev. Immunol. 17, 363–375 (2017). A review article that discusses mtDNA engagement of multiple pattern-recognition receptors in a cell-type- and context-dependent manner that triggers inflammation.