Characterization of human HtrA2, a novel serine protease involved in the mammalian cellular stress response

Gray, Charles A.; Ward, Robin V.; Karran, Eric; Turconi, Sandra; Rowles, Alison; Viglienghi, Daniela; Southan, Christopher; Barton, A.J.L.; Fantom, Kenneth; West, Andrew B.; Savopoulos, John; Hassan, Namir J.; Clinkenbeard, Helen; Hanning, Charles R.; Amegadzie, Bernard Y.; Davis, John B.; Dingwall, Colin; Livi, George P.; Creasy, Caretha L.

doi:10.1046/j.1432-1327.2000.01589.x

Cited by 244 publications

(223 citation statements)

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“…Maintenance of autophagy at a basal level in most cells contributes to the routine turnover of cytoplasmic components, and autophagy is rapidly upregulated when cells need to generate intracellular nutrients and energy. As previously reported, ER stress can activate autophagy 18 and increase Omi expression 4 (confirmed in Supplementary Figure S2a), indicating that endogenous Omi might be involved in regulating constitutive basal autophagy. We therefore examined whether endogenous Omi levels were related to stress-induced autophagy activation.…”

Section: Resultssupporting

confidence: 86%

“…Omi is reported to be upregulated by severalfold after heat shock or tunicamycin treatment. 4 In our report, both mRNA and protein levels increased under tunicamycin treatment (Figure 2a; Supplementary Figure S2b). In a mouse model of kidney ischemia/ reperfusion, protease activity of Omi obviously increased.…”

Section: Discussionsupporting

confidence: 55%

“…3 Most Omi resides in the intermembrane space of the mitochondria; however, endoplasmic reticulum (ER) and Golgi localization have also been reported. 4 Under apoptotic stimulation, a mature processed form of Omi is released into the cytosol where it binds to the cytosolic inhibitor of apoptosis proteins (IAPs) and inactivates their caspase-inhibitory activity 5 by direct cleavage. 3 Mature Omi that lacks the mitochondrial targeting sequence induces dramatic apoptosis-like morphological changes and cell death that is not blocked by caspase inhibitors.…”

mentioning

confidence: 99%

“…These mice died within 30 days after birth, similarly to mnd2 mice. 10 Furthermore, many other neurodegenerative disease proteins, such as presenilin-1 4,11 or amyloid precursor protein, 12 were reported to be associated with Omi.…”

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confidence: 99%

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Omi/HtrA2 is a positive regulator of autophagy that facilitates the degradation of mutant proteins involved in neurodegenerative diseases

Wang

et al. 2010

Cell Death Differ

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Omi, also known as high temperature requirement factor A2 (HtrA2), is a serine protease that was originally identified as a proapoptotic protein. Like Smac/Diablo, it antagonizes inhibitor of apoptosis proteins when released into the cytosol on apoptotic stimulation. Loss of its protease activity in mnd2 (motor neuron degeneration 2) mice is associated with neurodegeneration. However, the detailed mechanisms by which Omi regulates the pathogenesis of neurodegenerative disease remain largely unknown. We report here that Omi participates in the pivotal cellular degradation process known as autophagy. It activates autophagy through digestion of Hax-1, a Bcl-2 family-related protein that represses autophagy in a Beclin-1 (mammalian homologue of yeast ATG6)-dependent pathway. Moreover, Omi-induced autophagy facilitates the degradation of neurodegenerative proteins such as pathogenic A53T a-synuclein and truncated polyglutamine-expanded huntingtin, as well as the endogenous autophagy substrate p62. Knockdown of Omi decreases the basal level of autophagy and increases the level of the above target proteins. Furthermore, S276C Omi, the protease-defective mutant found in mnd2 mice, fails to regulate autophagy. Increased autophagy substrates and the formation of aggregate structures are observed in the brains of mnd2 mice. These results identify Omi as a novel regulator of autophagy and suggest that Omi might be important in the cellular quality control of proteins involved in neurodegenerative diseases.

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Section: Resultssupporting

confidence: 86%

Section: Discussionsupporting

confidence: 55%

mentioning

confidence: 99%

mentioning

confidence: 99%

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Omi/HtrA2 is a positive regulator of autophagy that facilitates the degradation of mutant proteins involved in neurodegenerative diseases

Wang

et al. 2010

Cell Death Differ

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“…The serine protease Omi (also known as high temperature requirement (HtrA2)) was identified first as an interactor of mxi2 or presenilin in human cells (Faccio et al, 2000;Gray et al, 2000) Thereafter, Omi was found to interact with XIAP(X-linked inhibitor of apoptosis). As XIAP was thought to be a direct inhibitor of caspases, the apoptotic function of Omi was extensively investigated.…”

Section: Introductionmentioning

confidence: 99%

Serine protease Omi/HtrA2 targets WARTS kinase to control cell proliferation

et al. 2006

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The serine protease Omi/HtrA2 was initially regarded as a proapoptotic molecule that proteolyses several proteins to induce cell death. Recent studies, however, indicate that loss of Omi protease activity increases susceptibility to stress-induced cell death. These complicated findings suggest that the protease activity of Omi is involved not only in apoptosis but also in cellular homeostasis. However, the targets which Omi uses to mediate this novel process are unknown. Previously, we showed that WARTS (WTS)/large tumor-suppressor 1 mitotic kinase interacts with the protein/discs-large protein/zonula (PDZ) domain of Omi and promotes its protease activity. We now report that WTS is a substrate for Omi protease activity, thus it is not only a regulator but also a downstream target of this protease. Interaction with Omi PDZ domain is required for WTS to be proteolysed. When caspase-9-deficient mouse embryonic fibroblasts (MEFs) were treated with staurosporine, WTS was proteolysed by activated endogenous Omi without induction of cell death. Therefore, protease activity of Omi and proteolysis of WTS are not necessarily required for cell death. We found that depletion of Omi from HeLa cells results in accelerated cell proliferation despite no significant change in the duration of mitosis. The depletion of WTS showed the same effect on S phase progression. Therefore, WTS proteolytic fragment(s) generated by Omi may act as an inhibitor of G1/S progression. Our data reveal a role for Omi-mediated processing of WTS in negative regulation of cell cycle progression at interphase, suggesting a novel function of Omi other than apoptosis.

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The Chloroplast Proteolytic Machinery

Adam

2018

Annual Plant Reviews Online

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Characterization of human HtrA2, a novel serine protease involved in the mammalian cellular stress response

Cited by 244 publications

References 44 publications

Omi/HtrA2 is a positive regulator of autophagy that facilitates the degradation of mutant proteins involved in neurodegenerative diseases

Omi/HtrA2 is a positive regulator of autophagy that facilitates the degradation of mutant proteins involved in neurodegenerative diseases

Serine protease Omi/HtrA2 targets WARTS kinase to control cell proliferation

The Chloroplast Proteolytic Machinery

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