bims-miptne Biomed News
on Mitochondrial permeability transition pore-dependent necrosis
Issue of 2025–10–12
four papers selected by
Oluwatobi Samuel Adegbite, University of Liverpool
  1. Mitochondrial sodium-calcium exchange-Can TMEM65 do it alone?
  2. Aging aggravated liver ischemia and reperfusion injury by promoting oxidized mtDNA mediated-macrophage pyroptosis through acetylated MCU-dependent calcium uptake.
  3. Adaptation to Elevated Mitochondrial Calcium Is Distinct in the Left and Right Ventricles.
  4. Phloretin Suppresses the mPTP Abnormal Opening via the SHP-2/JAK2/BAX Axis to Ameliorate Nonalcoholic Steatohepatitis.
  1. Cell Metab. 2025 Oct 07. pii: S1550-4131(25)00390-0. [Epub ahead of print]37(10): 1927-1928
    Mitochondrial sodium-calcium exchange-Can TMEM65 do it alone?
    Joanne F Garbincius, John W Elrod.
      The mechanisms mediating calcium transport into and out of the mitochondrial matrix have critical implications for signaling, bioenergetics, and cell death. Zhang et al.1 propose that the protein TMEM65, recently identified as a key component of the mitochondrial calcium efflux machinery, functions as the mitochondrial sodium/calcium exchanger. Their report encourages critical re-examination of the components required for mitochondrial calcium handling.
    DOI:  https://doi.org/10.1016/j.cmet.2025.09.005
  2. Cell Death Discov. 2025 Oct 07. 11(1): 449
    Aging aggravated liver ischemia and reperfusion injury by promoting oxidized mtDNA mediated-macrophage pyroptosis through acetylated MCU-dependent calcium uptake.
    Xin-Yi Wu, Rui Wang, Qi Zhang, Tao Liu, Jun-Yan Liu, Xue-Song Xu, Jun-Hua Gong.
      The shortage of liver donors for liver transplantation is currently an urgent problem. Elderly donors have become an important source of donor livers, but they are more prone to ischemia reperfusion injury (IRI) in liver transplantation. Therefore, exploring the effects and mechanisms of aging on liver IRI will provide a new theoretical basis for improving the survival rate of liver transplant patients. We constructed a mouse model of liver ischemia for 90 min and reperfusion for 6 or 24 h, and found that compared with young liver, the recovery of liver function in aged liver after IRI was slower. Detection of macrophage pyroptosis revealed that it was an important factor for aging deferring liver function restoration. Mechanistically, we demonstrated that aging triggered mitochondrial permeability transition pore (mPTP) channel opening to promote the release of Oxidized mtDNA (Ox-mtDNA), thereby inducing macrophage pyroptosis. Moreover, the activity of mPTP channel was mainly dependent on calcium uptake by acetylated mitochondrial calcium uniporter (MCU). These results illustrated that cytoplasmic Ox-mtDNA-induced macrophage pyroptosis was a key factor for aging exacerbating liver IRI. Calcium uptake via acetylated MCU triggered mPTP channel opening, which is an important mechanism for Ox-mtDNA release from mitochondria into the cytoplasm.
    DOI:  https://doi.org/10.1038/s41420-025-02746-9
  3. Circ Res. 2025 Oct 07.
    Adaptation to Elevated Mitochondrial Calcium Is Distinct in the Left and Right Ventricles.
    Shanmugasundaram Pakkiriswami, Jae Hwi Sung, Kshama R Shah, Ulas Ozkurede, Megan K Sumera, Feng Feng, Hector Chapoy Villanueva, Eun Suh Cho, Andrea Torniainen, Jop van Berlo, Gyorgy Hajnoczky, Kurt W Prins, Julia C Liu.
       BACKGROUND: Mitochondrial ATP production, essential for cardiomyocyte function, is regulated by mitochondrial Ca2+ (mtCa2+). The primary route for mtCa2+ influx is the mitochondrial calcium uniporter complex. The mitochondrial calcium uniporter complex subunit MICU (mitochondrial calcium uptake) 1 limits mtCa2+ uptake, preventing mtCa2+ overload. Although elevated mtCa2+ has been observed in multiple diseases including heart failure, its effects on heart function remain elusive.
    METHODS: To investigate the impact of elevated mtCa2+ in adult hearts, we generated a mouse model with cardiomyocyte-specific tamoxifen-inducible Micu1 deletion (Micu1cKO). Cardiac function was assessed through echocardiography. Mitochondria, adult cardiomyocytes, and tissue extracts were isolated from the left ventricle (LV) and right ventricle (RV) for comprehensive analysis at multiple time points ranging from 1 to 9 weeks post-tamoxifen injection.
    RESULTS: Acute MICU1 deficiency resulted in increased mtCa2+ accompanied by reduced mitochondrial respiration in both the RV and LV. Contractile function, which was diminished in both ventricles initially, remained reduced in the RV upon prolonged MICU1 deficiency. In contrast, the LV exhibited signs of recovery over time, including restored ejection fraction concurrent with normalization of mtCa2+ levels. This pattern was mirrored in cardiomyocyte contractility. In Micu1cKO RV, mtCa2+ remained elevated, likely contributing to oxidative stress. As a potential mechanism underlying LV-specific recovery, EMRE (essential MCU regulator), an mitochondrial calcium uniporter complex subunit that promotes mtCa2+ uptake, was found to be downregulated only in the LV. This suggested that the LV initiated a compensatory response to elevated mtCa2+, while the RV remained impacted. Supporting this, proteomics analysis indicated a divergent proteomic signature in Micu1cKO RV. Follow-up experiments suggested enhanced EMRE degradation in Micu1cKO LV mediated by m-AAA proteases through a PKA (protein kinase A)-regulated mechanism. In MICU1-deficient neonatal cardiomyocytes, pharmacological PKA inhibition was sufficient to decrease EMRE levels. Analysis of LV tissues from patients with dilated cardiomyopathy suggested that this pathway may be relevant in human DCM.
    CONCLUSIONS: While elevated mtCa2+ disrupted cardiac function in both ventricles, it induced an LV-specific adaptive response that suppressed mtCa2+ intake, contributing to the recovery of mitochondrial and cardiac function. The absence of this pathway in the RV has implications for therapeutics targeting RV dysfunction, a key determinant of mortality in heart failure.
    Keywords:  calcium; heart; mitochondria; myocytes, cardiac; oxidative stress
    DOI:  https://doi.org/10.1161/CIRCRESAHA.125.326221
  4. J Agric Food Chem. 2025 Oct 08.
    Phloretin Suppresses the mPTP Abnormal Opening via the SHP-2/JAK2/BAX Axis to Ameliorate Nonalcoholic Steatohepatitis.
    Yonghui Dong, Xue Wu, Jie Li, Jia Li, Yuan Lu, Caian He, Lin Han, Min Wang.
      Mitochondrial dysfunction, particularly driven by aberrant mitochondrial permeability transition pore (mPTP) opening, is a key pathogenic mechanism in nonalcoholic steatohepatitis (NASH). This study demonstrates for the first time that phloretin (Pht), a natural apple-derived dihydrochalcone, effectively inhibits this pathology by targeting SHP-2. Pht modulates the SHP-2/JAK2/BAX signaling axis, significantly suppressing the pathological mPTP opening. This action preserves mitochondrial homeostasis, evidenced by restored mitochondrial membrane potential, improved ultrastructural integrity, and the prevention of mitochondrial DNA (mtDNA) leakage into the cytosol. By blocking mtDNA escape, Pht inhibits the cytosolic mtDNA-induced activation of the cGAS-STING pathway and its downstream inflammatory cascade. Consequently, Pht ameliorates hepatic lipid metabolic dysregulation and inflammation. These findings reveal a novel SHP-2/JAK2/BAX-mPTP-mtDNA-cGAS signaling cascade through which dietary Pht alleviates NASH-associated mitochondrial inflammation. This work provides a crucial mechanistic foundation and identifies potential targets for developing functional foods or interventions aimed at promoting mitochondrial homeostasis.
    Keywords:  NASH; SHP-2; mPTP; mitochondrion; phloretin
    DOI:  https://doi.org/10.1021/acs.jafc.5c05787
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