MALT1 promotes necroptosis in stroke rat brain via targeting the A20/RIPK3 pathway

Necroptosis has been demonstrated to contribute to brain injury in ischemic stroke, whereas A20 can exert anti-necroptosis effect via deubiquitinating receptor-interacting protein kinase (RIPK3) at k63 and it can be cleaved by MALT1. This study aims to explore whether MALT1 is upregulated in the bra...

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Veröffentlicht in:Archives of biochemistry and biophysics 2023-02, Vol.735, p.109502-109502, Article 109502
Hauptverfasser: Peng, Zi-Mei, Zhang, Yi-Yue, Wei, Dan, Zhang, Xiao-Jie, Liu, Bin, Peng, Jun, Luo, Xiu-Ju
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Sprache:eng
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Zusammenfassung:Necroptosis has been demonstrated to contribute to brain injury in ischemic stroke, whereas A20 can exert anti-necroptosis effect via deubiquitinating receptor-interacting protein kinase (RIPK3) at k63 and it can be cleaved by MALT1. This study aims to explore whether MALT1 is upregulated in the brain during ischemic stroke and promotes brain cell necroptosis through enhancing the degradation of A20. Ischemic stroke model was established in Sprague Dawley rats by occlusion of the middle cerebral artery (MCA) for 2 h, followed by 24 h reperfusion, which showed brain injury (increase in neurological deficit score and infarct volume) concomitant with an upregulation of MALT1, a decrease in A20 level, and increases in necroptosis-associated protein levels [RIPK3, mixed lineage kinase domain-like protein (MLKL) and p-MLKL] and k63-ubiquitination of RIPK3 in brain tissues. Administration of MALT1 inhibitor (Ml-2) at 8 or 15 mg/kg (i.p.) at 1 h after ischemia significantly improved neurological function and reduced infarct volume together with a downregulation of MALT1, an increase in A20 level and decreases in necroptosis-associated protein levels and k63-ubiquitination of RIPK3. Similarly, knockdown of MALT1 could also reduce oxygen-glucose deprivation/reoxygenation (OGD/R)-induced injury in the cultured HT22 cells coincident with an increase in A20 level and decreases in necroptosis-associated protein levels and k63-ubiquitination of RIPK3. Based on these observations, we conclude that MALT1 promotes necroptosis in stroke rat brain via enhancing the degradation of A20, which leads to a decrease in the capability of A20 to deubiquitinate RIPK3 at k63 and a subsequent compromise in counteraction against the brain cell necroptosis. Upregulation of MALT1 in ischemic stroke rat brain contributes to neuronal cell necroptosis and brain injury through promoting the degradation of A20, which leads to a decrease in the capability of A20 to deubiquitinate RIPK3 at k63. [Display omitted] •Inhibition of MALT1 exerts beneficial effect on ischemic stroke rats.•MALT1 promotes necroptosis in stroke rat brain via enhancing the degradation of A20.•Ubiquitination of RIPK3 at k63 leads to a compromise in counteraction against the brain cell necroptosis.
ISSN:0003-9861
1096-0384
DOI:10.1016/j.abb.2023.109502