2012
DOI: 10.1016/j.nbd.2011.12.023
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Complete transglutaminase 2 ablation results in reduced stroke volumes and astrocytes that exhibit increased survival in response to ischemia

Abstract: Transglutaminase 2 (TG2) is a very multifunctional protein that is ubiquitously expressed in the body. It is a Ca2+-dependent transamidating enzyme, a GTPase, as well as a scaffolding protein. TG2 is the predominant form of transglutaminase expressed in the mammalian nervous system. Previously, it was shown that TG2 can affect both cell death and cell survival mechanisms depending on the cell type and the stressor. In the case of ischemic stress, TG2 was previously shown to play a protective role in the models… Show more

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Cited by 42 publications
(75 citation statements)
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“…The present finding that CHOP, GRP78, and cleaved caspase-3 were attenuated by the pretreatment with cystamine supports the previous report that the downstream activity of TG2 activates the calpain/caspase pathway (32). Also, knocking down of TG2 expression significantly attenuated their cell death (data not shown), In fact, it was reported previously that infarct volumes in TG2-knockout mice were significantly smaller compared with those in wild type mice (33), suggesting that TG2 is a potential target for development of therapeutics of brain ischemia.…”
Section: Discussionsupporting
confidence: 92%
“…The present finding that CHOP, GRP78, and cleaved caspase-3 were attenuated by the pretreatment with cystamine supports the previous report that the downstream activity of TG2 activates the calpain/caspase pathway (32). Also, knocking down of TG2 expression significantly attenuated their cell death (data not shown), In fact, it was reported previously that infarct volumes in TG2-knockout mice were significantly smaller compared with those in wild type mice (33), suggesting that TG2 is a potential target for development of therapeutics of brain ischemia.…”
Section: Discussionsupporting
confidence: 92%
“…45 Interestingly, TG1 and 2 can be upregulated by different groups of cytokines (e.g., TNFa, IL-6, and TGFb) or toxins (lipopolysachharide) in mixed astrocyte-neuronal cultures. 46 By contrast to our in vitro data that shows that both TG1 and TG2 are required for cell death from oxidative death, TG2 ablation reduced the infarct volume in a model of permanent ischemia 47 and its overexpression in neurons via a Prp promoter, showed higher number of apoptotic cells and greater susceptibility to kainate stimuli. 48 Future studies will clarify why TG2 is necessary and sufficient in some paradigms, while TG2 and TG1 are necessary in other paradigms.…”
Section: Polyamination Of Proteins By Transglutaminasecontrasting
confidence: 61%
“…Neurons from TG2 knockout mice showed decreased viability in response to oxygen-glucose deprivation, which was not observed in astrocytes, as they were resistant to oxygen-glucose deprivation in situ. Interestingly, wild type and knock out neurons were protected against oxygen glucose deprivation when they were co-cultured with astrocytes from TG2 knockout mice (Colak G 2012). Therefore, the decreased stroke volumes observed in TG2 knock out evidences that its expression is more important in astrocytes.…”
Section: Central Nervous System Resident Cells and Strokementioning
confidence: 98%