Your search keyword '"Cornelius Y. Taabazuing"' showing total 26 results

1. Inflammatory caspase substrate specificities

Author

Patrick M. Exconde, Christopher M. Bourne, Madhura Kulkarni, Bohdana M. Discher, and Cornelius Y. Taabazuing

Subjects

inflammasomes, inflammatory caspases, caspase-1, caspase-4, caspase-5, caspase-11, Microbiology, QR1-502

Abstract

ABSTRACT Caspases are a family of cysteine proteases that act as molecular scissors to cleave substrates and regulate biological processes such as programmed cell death and inflammation. Extensive efforts have been made to identify caspase substrates and to determine factors that dictate substrate specificity. Thousands of putative substrates have been identified for caspases that regulate an immunologically silent type of cell death known as apoptosis, but less is known about substrates of the inflammatory caspases that regulate an immunostimulatory type of cell death called pyroptosis. Furthermore, much of our understanding of caspase substrate specificities is derived from work done with peptide substrates, which do not often translate to native protein substrates. Our knowledge of inflammatory caspase biology and substrates has recently expanded and here, we discuss the recent advances in our understanding of caspase substrate specificities, with a focus on inflammatory caspases. We highlight new substrates that have been discovered and discuss the factors that engender specificity. Recent evidence suggests that inflammatory caspases likely utilize two binding interfaces to recognize and process substrates, the active site and a conserved exosite.

Published

2024

2. The tetrapeptide sequence of IL-18 and IL-1β regulates their recruitment and activation by inflammatory caspases

Author

Patrick M. Exconde, Claudia Hernandez-Chavez, Christopher M. Bourne, Rachel M. Richards, Mark B. Bray, Jan L. Lopez, Tamanna Srivastava, Marisa S. Egan, Jenna Zhang, William Yoo, Sunny Shin, Bohdana M. Discher, and Cornelius Y. Taabazuing

Subjects

CP: Immunology, Biology (General), QH301-705.5

Abstract

Summary: Inflammasomes are multiprotein signaling complexes that activate the innate immune system. Canonical inflammasomes recruit and activate caspase-1, which then cleaves and activates IL-1β and IL-18, as well as gasdermin D (GSDMD) to induce pyroptosis. In contrast, non-canonical inflammasomes, caspases-4/-5 (CASP4/5) in humans and caspase-11 (CASP11) in mice, are known to cleave GSDMD, but their role in direct processing of other substrates besides GSDMD has remained unknown. Here, we show that CASP4/5 but not CASP11 can directly cleave and activate IL-18. However, CASP4/5/11 can all cleave IL-1β to generate a 27-kDa fragment that deactivates IL-1β signaling. Mechanistically, we demonstrate that the sequence identity of the tetrapeptide sequence adjacent to the caspase cleavage site regulates IL-18 and IL-1β recruitment and activation. Altogether, we have identified new substrates of the non-canonical inflammasomes and reveal key mechanistic details regulating inflammation that may aid in developing new therapeutics for immune-related disorders.

Published

2023

3. Harnessing Pyroptosis for Cancer Immunotherapy

Author

Christopher M. Bourne and Cornelius Y. Taabazuing

Subjects

pyroptosis, inflammasomes, cancer immunotherapy, antitumor immunity, tumor microenvironment, caspases, Cytology, QH573-671

Abstract

Cancer immunotherapy is a novel pillar of cancer treatment that harnesses the immune system to fight tumors and generally results in robust antitumor immunity. Although immunotherapy has achieved remarkable clinical success for some patients, many patients do not respond, underscoring the need to develop new strategies to promote antitumor immunity. Pyroptosis is an immunostimulatory type of regulated cell death that activates the innate immune system. A hallmark of pyroptosis is the release of intracellular contents such as cytokines, alarmins, and chemokines that can stimulate adaptive immune activation. Recent studies suggest that pyroptosis promotes antitumor immunity. Here, we review the mechanisms by which pyroptosis can be induced and highlight new strategies to induce pyroptosis in cancer cells for antitumor defense. We discuss how pyroptosis modulates the tumor microenvironment to stimulate adaptive immunity and promote antitumor immunity. We also suggest research areas to focus on for continued development of pyroptosis as an anticancer treatment. Pyroptosis-based anticancer therapies offer a promising new avenue for treating immunologically ‘cold’ tumors.

Published

2024

4. A practical guide to graduate school interviewing for historically excluded individuals

Author

Elizabeth Ransey, Shawna Brookens, Heather K. Beasley, Andrea Marshall, Bianca J. Marlin, Piere Rodriguez-Aliaga, Colwyn Ansel Headley, Celestine Wanjalla, Arnaldo Diaz Vazquez, Sandra Murray, Steven Damo, Cornelius Y. Taabazuing, and Antentor Hinton

Subjects

Physiology, Physiology (medical), Cardiology and Cardiovascular Medicine, Perspectives

Published

2023

5. The tetrapeptide sequence of IL-1β regulates its recruitment and activation by inflammatory caspases

Author

Patrick M. Exconde, Claudia Hernandez-Chavez, Mark B. Bray, Jan L. Lopez, Tamanna Srivastava, Marisa S. Egan, Jenna Zhang, Sunny Shin, Bohdana M. Discher, and Cornelius Y. Taabazuing

Subjects

Article

Abstract

The mammalian innate immune system uses germline-encoded cytosolic pattern-recognition receptors (PRRs) to detect intracellular danger signals. At least six of these PRRs are known to form multiprotein complexes called inflammasomes which activate cysteine proteases known as caspases. Canonical inflammasomes recruit and activate caspase-1 (CASP1), which in turn cleaves and activates inflammatory cytokines such as IL-1β and IL-18, as well as the pore forming protein, gasdermin D (GSDMD), to induce pyroptotic cell death. In contrast, non-canonical inflammasomes, caspases-4/-5 (CASP4/5) in humans and caspase-11 (CASP11) in mice, are activated by intracellular LPS to cleave GSDMD, but their role in direct processing of inflammatory cytokines has not been established. Here we show that active CASP4/5 directly cleave IL-18 to generate the active species. Surprisingly, we also discovered that CASP4/5/11 cleave IL-1β at D27 to generate a 27 kDa fragment that is predicted to be inactive and cannot signal to the IL-1 receptor. Mechanistically, we discovered that the sequence identity of the P4-P1 tetrapeptide sequence adjacent to the caspase cleavage site (D116) regulates the recruitment and processing of IL-1β by inflammatory caspases to generate the bioactive species. Thus, we have identified new substrates of the non-canonical inflammasomes and reveal key mechanistic details regulating inflammation.

Published

2023

6. Noncanonical inflammasome assembly requires caspase-11 catalytic activity and intra-molecular autoprocessing

Author

Daniel C. Akuma, Daniel Grubaugh, Chukwuma E. Odunze, Sunny Shin, Cornelius Y. Taabazuing, and Igor E. Brodsky

Abstract

Inflammatory caspases are cysteine protease zymogens whose activation following infection or cellular damage occurs within supramolecular organizing centers (SMOCs) known as inflammsasomes. Inflammasomes are large oligomeric complexes that recruit caspases to undergo proximity-induced autoprocessing, leading to formation of the enzymatically active form that cleaves downstream targets. Binding of bacterial LPS to its cytosolic sensor, caspase-11 (Casp11), promotes Casp11 aggregation within a high molecular weight complex known as the noncanonical inflammasome, where it is activated to cleave gasdermin D and induce pyroptosis. However, the cellular correlates of Casp11 oligomerization and whether Casp11 forms an LPS-induced SMOC within cells remain unknown. Using fluorescently labeled Casp11, we found that LPS transfection of macrophages induced Casp11 speck formation, providing direct evidence that Casp11 forms LPS-induced specks in macrophages. Unexpectedly, we found that catalytic activity was required for Casp11 to form LPS-induced specks in macrophages. Importantly, both catalytic activity and autoprocessing were required for Casp11 speck formation in an ectopic expression system, and Casp11 processing via an exogenous protease was sufficient to induce Casp11 speck formation. These data reveal a previously-undescribed role for Casp11 catalytic activity and self-cleavage in non-canonical inflammasome assembly and indicate that Casp11 catalytic activity and autoprocessing occur upstream of, and mediate, Casp11 oligomerization. Our data provide new insight into the molecular requirements for assembly of Casp11 noncanonical inflammasome complexes.

Published

2022

7. A ubiquitin-independent proteasome pathway controls the CARD8 inflammasome

Author

Jeffrey C. Hsiao, Atara R. Neugroschl, Ashley J. Chui, Cornelius Y. Taabazuing, Andrew R. Griswold, Qinghui Wang, Hsin-Che Huang, Elizabeth L. Orth-He, Daniel P. Ball, Giorgos Hiotis, and Daniel A. Bachovchin

Abstract

CARD8 is a pattern-recognition receptor that forms a caspase-1-activating inflammasome. CARD8 undergoes autoproteolysis, generating an N-terminal (NT) fragment with a disordered region and a ZU5 domain and a C-terminal (CT) fragment with UPA and CARD domains. DPP8 and DPP9 (DPP8/9) inhibitors, including Val-boroPro (VbP), accelerate the degradation of the NT fragment via a poorly characterized proteasome-mediated pathway, thereby releasing the inflammatory CT fragment from autoinhibition. Here, we show that the core 20S proteasome, which degrades disordered and misfolded proteins independent of ubiquitin, controls CARD8 activation. In unstressed cells, the 20S proteasome degrades just the NT disordered region, leaving behind the folded ZU5, UPA, and CARD domains to act as an inhibitor of inflammasome assembly. In VbP-stressed cells, the 20S proteasome degrades the entire NT fragment, perhaps due to ZU5 domain unfolding, freeing the CT fragment from autoinhibition. Overall, this work shows that the susceptibility of the CARD8 NT to 20S proteasome-mediated degradation controls inflammasome activation.

Published

2022

8. A ubiquitin-independent proteasome pathway controls activation of the CARD8 inflammasome

Author

Jeffrey C. Hsiao, Atara R. Neugroschl, Ashley J. Chui, Cornelius Y. Taabazuing, Andrew R. Griswold, Qinghui Wang, Hsin-Che Huang, Elizabeth L. Orth-He, Daniel P. Ball, Giorgos Hiotis, and Daniel A. Bachovchin

Subjects

CARD Signaling Adaptor Proteins, Proteasome Endopeptidase Complex, Inflammasomes, Humans, Cell Biology, Dipeptidyl-Peptidases and Tripeptidyl-Peptidases, Molecular Biology, Biochemistry, Ubiquitins, Neoplasm Proteins

Abstract

CARD8 is a pattern-recognition receptor that forms a caspase-1-activating inflammasome. CARD8 undergoes constitutive autoproteolysis, generating an N-terminal (NT) fragment with a disordered region and a ZU5 domain and a C-terminal (CT) fragment with UPA and CARD domains. Dipeptidyl peptidase 8 and dipeptidyl peptidase 9 inhibitors, including Val-boroPro, accelerate the degradation of the NT fragment via a poorly characterized proteasome-mediated pathway, thereby releasing the inflammatory CT fragment from autoinhibition. Here, we show that the core 20S proteasome, which degrades disordered and misfolded proteins independent of ubiquitin modification, controls activation of the CARD8 inflammasome. In unstressed cells, we discovered that the 20S proteasome degrades just the NT disordered region, leaving behind the folded ZU5, UPA, and CARD domains to act as an inhibitor of inflammasome assembly. However, in Val-boroPro-stressed cells, we show the 20S proteasome degrades the entire NT fragment, perhaps due to ZU5 domain unfolding, freeing the CT fragment from autoinhibition. Taken together, these results show that the susceptibility of the CARD8 NT domain to 20S proteasome-mediated degradation controls inflammasome activation.

Published

2022

9. DPP9’s Enzymatic Activity and Not Its Binding to CARD8 Inhibits Inflammasome Activation

Author

Sahana D. Rao, Cornelius Y. Taabazuing, Daniel A. Bachovchin, Andrew R. Griswold, Ashley J. Chui, Abir Bhattacharjee, and Daniel P. Ball

Subjects

0301 basic medicine, Dipeptidases, Inflammasomes, Protein Conformation, Mutant, NLR Proteins, Plasma protein binding, 01 natural sciences, Biochemistry, Organofluorophosphonates, Serine, 03 medical and health sciences, medicine, Humans, Protease Inhibitors, Letters, Dipeptidyl-Peptidases and Tripeptidyl-Peptidases, Adaptor Proteins, Signal Transducing, chemistry.chemical_classification, 010405 organic chemistry, HEK 293 cells, Signal transducing adaptor protein, Inflammasome, General Medicine, Neoplasm Proteins, 0104 chemical sciences, Cell biology, CARD Signaling Adaptor Proteins, HEK293 Cells, 030104 developmental biology, Enzyme, chemistry, Mutation, Molecular Medicine, Signal transduction, Apoptosis Regulatory Proteins, Protein Binding, Signal Transduction, medicine.drug

Abstract

Inflammasomes are multiprotein complexes formed in response to pathogens. NLRP1 and CARD8 are related proteins that form inflammasomes, but the pathogen-associated signal(s) and the molecular mechanisms controlling their activation have not been established. Inhibitors of the serine dipeptidyl peptidases DPP8 and DPP9 (DPP8/9) activate both NLRP1 and CARD8. Interestingly, DPP9 binds directly to NLRP1 and CARD8, and this interaction may contribute to the inhibition of NLRP1. Here, we use activity-based probes, reconstituted inflammasome assays, and mass spectrometry-based proteomics to further investigate the DPP9–CARD8 interaction. We show that the DPP9–CARD8 interaction, unlike the DPP9–NLRP1 interaction, is not disrupted by DPP9 inhibitors or CARD8 mutations that block autoproteolysis. Moreover, wild-type, but not catalytically inactive mutant, DPP9 rescues CARD8-mediated cell death in DPP9 knockout cells. Together, this work reveals that DPP9’s catalytic activity and not its binding to CARD8 restrains the CARD8 inflammasome and thus suggests the binding interaction likely serves some other biological purpose.

Published

2019

10. The NLRP1 and CARD8 inflammasomes

Author

Andrew R. Griswold, Cornelius Y. Taabazuing, and Daniel A. Bachovchin

Subjects

CARD8, Inflammasomes, Immunology, NLR Proteins, DPP8/9, Biology, Proinflammatory cytokine, NLRP1, Shigella flexneri, inflammasome, medicine, Immunology and Allergy, Humans, Invited Reviews, Adaptor Proteins, Signal Transducing, Invited Review, pyroptosis, Pyroptosis, Pattern recognition receptor, Inflammasome, biology.organism_classification, Small molecule, anthrax lethal toxin, Cell biology, Neoplasm Proteins, CARD Signaling Adaptor Proteins, proteasome, Proteasome, Val‐boroPro, Apoptosis Regulatory Proteins, medicine.drug

Abstract

Inflammasomes are multiprotein complexes that activate inflammatory cytokines and induce pyroptosis in response to intracellular danger‐associated signals. NLRP1 and CARD8 are related germline‐encoded pattern recognition receptors that form inflammasomes, but their activation mechanisms and biological purposes have not yet been fully established. Both NLRP1 and CARD8 undergo post‐translational autoproteolysis to generate two non‐covalently associated polypeptide chains. NLRP1 and CARD8 activators induce the proteasome‐mediated destruction of the N‐terminal fragment, liberating the C‐terminal fragment to form an inflammasome. Here, we review the danger‐associated stimuli that have been reported to activate NLRP1 and/or CARD8, including anthrax lethal toxin, Toxoplasma gondii, Shigella flexneri and the small molecule DPP8/9 inhibitor Val‐boroPro, focusing on recent mechanistic insights and highlighting unresolved questions. In addition, we discuss the recently identified disease‐associated mutations in NLRP1 and CARD8, the potential role that DPP9’s protein structure plays in inflammasome regulation, and the emerging link between NLRP1 and metabolism. Finally, we summarize all of this latest research and consider the possible biological purposes of these enigmatic inflammasomes.

Published

2020

11. Caspase-1 interdomain linker cleavage is required for pyroptosis

Author

Darren C. Johnson, Elizabeth L. Orth, Andrew R. Griswold, Cornelius Y. Taabazuing, Lauren E Vostal, Daniel A. Bachovchin, Ilana B. Kotliar, Daniel P. Ball, and Sahana D. Rao

Subjects

0301 basic medicine, Inflammasomes, THP-1 Cells, animal diseases, Health, Toxicology and Mutagenesis, Caspase 1, Apoptosis, Plant Science, Biochemistry, Genetics and Molecular Biology (miscellaneous), 03 medical and health sciences, 0302 clinical medicine, Zymogen, NLR Family, Pyrin Domain-Containing 3 Protein, medicine, Pyroptosis, Humans, Research Articles, Adaptor Proteins, Signal Transducing, Ecology, Chemistry, NLRP1, HEK 293 cells, Signal transducing adaptor protein, Inflammasome, Cell biology, CARD Signaling Adaptor Proteins, 030104 developmental biology, HEK293 Cells, Signal transduction, Apoptosis Regulatory Proteins, Carrier Proteins, 030217 neurology & neurosurgery, medicine.drug, Research Article, Signal Transduction

Abstract

The related human NLRP1 and CARD8 form ASC-dependent and ASC-independent inflammasomes, respectively, both of which require pro-caspase-1 interdomain linker processing for the induction of pyroptosis., Pathogen-related signals induce a number of cytosolic pattern-recognition receptors (PRRs) to form canonical inflammasomes, which activate pro-caspase-1 and trigger pyroptotic cell death. All well-studied inflammasome-forming PRRs oligomerize with the adapter protein ASC (apoptosis-associated speck-like protein containing a CARD) to generate a large structure in the cytosol, which induces the dimerization, autoproteolysis, and activation of the pro-caspase-1 zymogen. However, several PRRs can also directly interact with pro-caspase-1 without ASC, forming smaller “ASC-independent” inflammasomes. It is currently thought that little, if any, pro-caspase-1 autoproteolysis occurs during, and is not required for, ASC-independent inflammasome signaling. Here, we show that the related human PRRs NLRP1 and CARD8 exclusively form ASC-dependent and ASC-independent inflammasomes, respectively, identifying CARD8 as the first canonical inflammasome-forming PRR that does not form an ASC-containing signaling platform. Despite their different structures, we discovered that both the NLRP1 and CARD8 inflammasomes require pro-caspase-1 autoproteolysis between the small and large catalytic subunits to induce pyroptosis. Thus, pro-caspase-1 self-cleavage is a required regulatory step for pyroptosis induced by human canonical inflammasomes.

Published

2020

12. DPP8/DPP9 inhibitor-induced pyroptosis for treatment of acute myeloid leukemia

Author

Cornelius Y. Taabazuing, Marian C. Okondo, Sahana D. Rao, Darren C. Johnson, Casie Reed, Elizabeth Peguero, Alex Kentsis, Elisa de Stanchina, Daniel A. Bachovchin, Ashley J. Chui, and Fiona C. Brown

Subjects

0301 basic medicine, Myeloid, Cell, Biology, Article, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Cell Line, Tumor, hemic and lymphatic diseases, Pyroptosis, medicine, Humans, Protease Inhibitors, Dipeptidyl-Peptidases and Tripeptidyl-Peptidases, Caspase 1, HEK 293 cells, Myeloid leukemia, Inflammasome, General Medicine, medicine.disease, 3. Good health, CARD Signaling Adaptor Proteins, Leukemia, Myeloid, Acute, Leukemia, HEK293 Cells, 030104 developmental biology, medicine.anatomical_structure, Cell culture, Disease Progression, Cancer research, medicine.drug

Abstract

Small-molecule inhibitors of the serine dipeptidases DPP8 and DPP9 (DPP8/9) induce a lytic form of cell death called pyroptosis in mouse and human monocytes and macrophages1,2. In mouse myeloid cells, Dpp8/9 inhibition activates the inflammasome sensor Nlrp1b, which in turn activates pro-caspase-1 to mediate cell death3, but the mechanism of DPP8/9 inhibitor-induced pyroptosis in human myeloid cells is not yet known. Here we show that the CARD-containing protein CARD8 mediates DPP8/9 inhibitor-induced pro-caspase-1 dependent pyroptosis in human myeloid cells. We further show that DPP8/9 inhibitors induce pyroptosis in the large majority of human acute myeloid leukemia (AML) cell lines and primary AML samples, but not in cells from many other lineages, and that these inhibitors inhibit human AML progression in mouse models. Overall, this work identifies the first known activator of CARD8 in human cells and indicates that its activation by small-molecule DPP8/9 inhibitors represents a new potential therapeutic strategy for AML.

Published

2018

13. The facial triad in the α-ketoglutarate dependent oxygenase FIH: A role for sterics in linking substrate binding to O2 activation

Author

Scott J. Eron, Michael J. Knapp, John A. Hangasky, Cornelius Y. Taabazuing, and Cristina B. Martin

Subjects

0301 basic medicine, Steric effects, chemistry.chemical_classification, Oxygenase, 030102 biochemistry & molecular biology, Chemistry, Stereochemistry, 010402 general chemistry, 01 natural sciences, Biochemistry, 0104 chemical sciences, Inorganic Chemistry, Hydroxylation, 03 medical and health sciences, chemistry.chemical_compound, Oxidoreductase, Enzyme kinetics, Carboxylate, Binding site, Oxidative decarboxylation

Abstract

The factor inhibiting hypoxia inducible factor-1α (FIH) is a nonheme Fe(II)/αKG oxygenase using a 2-His-1-Asp facial triad. FIH activates O2 via oxidative decarboxylation of α-ketoglutarate (αKG) to generate an enzyme-based oxidant which hydroxylates the Asn803 residue within the C-terminal transactivation domain (CTAD) of HIF-1α. Tight coupling of these two sequential reactions requires a structural linkage between the Fe(II) and the substrate binding site to ensure that O2 activation occurs after substrate binds. We tested the hypothesis that the facial triad carboxylate (Asp201) of FIH linked substrate binding and O2 binding sites. Asp201 variants of FIH were constructed and thoroughly characterized in vitro using steady-state kinetics, crystallography, autohydroxylation, and coupling measurements. Our studies revealed each variant activated O2 with a catalytic efficiency similar to that of wild-type (WT) FIH (kcataKM(O2) = 0.17 μM− 1min− 1), but led to defects in the coupling of O2 activation to substrate hydroxylation. Steady-state kinetics showed similar catalytic efficiencies for hydroxylation by WT-FIH (kcat/KM(CTAD) = 0.42 μM− 1 min− 1) and D201G (kcat/KM(CTAD) = 0.34 μM− 1 min− 1); hydroxylation by D201E was greatly impaired, while hydroxylation by D201A was undetectable. Analysis of the crystal structure of the D201E variant revealed steric crowding near the diffusible ligand site supporting a role for sterics from the facial triad carboxylate in the O2 binding order. Our data support a model in which the facial triad carboxylate Asp201 provides both steric and polar contacts to favor O2 access to the Fe(II) only after substrate binds, leading to coupled turnover in FIH and other αKG oxygenases.

Published

2017

14. Human caspase-1 autoproteolysis is required for ASC-dependent and -independent inflammasome activation

Author

Andrew R. Griswold, Elizabeth L. Orth, Ilana B. Kotliar, Sahana D. Rao, Cornelius Y. Taabazuing, Darren C. Johnson, Daniel P. Ball, and Daniel A. Bachovchin

Subjects

0303 health sciences, Programmed cell death, NLRP1, Chemistry, animal diseases, Pyroptosis, Caspase 1, Inflammasome, Cell biology, 03 medical and health sciences, Cytosol, 0302 clinical medicine, Zymogen, medicine, Receptor, 030217 neurology & neurosurgery, 030304 developmental biology, medicine.drug

Abstract

Pathogen-related signals induce a number of cytosolic pattern-recognition receptors (PRRs) to form canonical inflammasomes, which activate pro-caspase-1 and trigger pyroptotic cell death. All well-studied PRRs oligomerize with the pro-caspase-1-adapter protein ASC to generate a single large structure in the cytosol, which induces the autoproteolysis and activation of the pro-caspase-1 zymogen. However, several PRRs can also directly interact with pro-caspase-1 without ASC, forming much smaller “ASC-independent” inflammasomes. It is currently thought that pro-caspase-1 autoproteolysis does not occur during, and is not required for, ASC-independent inflammasome activation. Here, we show that the related human PRRs NLRP1 and CARD8 exclusively form ASC-dependent and ASC-independent inflammasomes, respectively, identifying CARD8 as the first PRR that cannot form an ASC-containing signaling platform. Despite their different structures, we discovered that both the NLRP1 and CARD8 inflammasomes require pro-caspase-1 autoproteolysis between the small and large catalytic subunits to induce pyroptosis. Thus, pro-caspase-1 self-cleavage is an obligate regulatory step in the activation of human canonical inflammasomes.

Published

2019

15. Activation of the CARD8 Inflammasome Requires a Disordered Region

Author

Cornelius Y. Taabazuing, Jeffrey C. Hsiao, Ashley J. Chui, Daniel P. Ball, Kuo Gai, Sahana D. Rao, Andrew R. Griswold, Elizabeth L. Orth, and Daniel A. Bachovchin

Subjects

0301 basic medicine, Inflammasomes, THP-1 Cells, Article, General Biochemistry, Genetics and Molecular Biology, Proinflammatory cytokine, Mice, 03 medical and health sciences, 0302 clinical medicine, medicine, Animals, Humans, Dipeptidyl-Peptidases and Tripeptidyl-Peptidases, Receptor, Chemistry, Lysine, Pyroptosis, Inflammasome, Dipeptides, Boronic Acids, Neoplasm Proteins, Cell biology, CARD Signaling Adaptor Proteins, Intrinsically Disordered Proteins, Cytosol, HEK293 Cells, RAW 264.7 Cells, 030104 developmental biology, Proteasome, Proteolysis, Proteostasis, Protein folding, 030217 neurology & neurosurgery, Intracellular, medicine.drug

Abstract

SUMMARY Several cytosolic pattern-recognition receptors (PRRs) form multiprotein complexes called canonical inflammasomes in response to intracellular danger signals. Canonical inflammasomes recruit and activate caspase-1 (CASP1), which in turn cleaves and activates inflammatory cytokines and gasdermin D (GSDMD), inducing pyroptotic cell death. Inhibitors of the dipeptidyl peptidases DPP8 and DPP9 (DPP8/9) activate both the human NLRP1 and CARD8 inflammasomes. NLRP1 and CARD8 have different N-terminal regions but have similar C-terminal regions that undergo autoproteolysis to generate two non-covalently associated fragments. Here, we show that DPP8/9 inhibition activates a proteasomal degradation pathway that targets disordered and misfolded proteins for destruction. CARD8’s N terminus contains a disordered region of ~160 amino acids that is recognized and destroyed by this degradation pathway, thereby freeing its C-terminal fragment to activate CASP1 and induce pyroptosis. Thus, CARD8 serves as an alarm to signal the activation of a degradation pathway for disordered and misfolded proteins., Graphical Abstract, In Brief Inflammasomes are multiprotein complexes that detect intracellular danger signals and stimulate powerful immune responses. DPP8/9 inhibitors activate the CARD8 inflammasome through an unknown mechanism. Here, Chui et al. show that DPP8/9 inhibitors induce the degradation of many disordered and misfolded proteins. CARD8 has an N-terminal disordered region that is degraded upon DPP8/9 inhibition, triggering inflammasome formation.

Published

2020

16. N-terminal degradation activates the NLRP1B inflammasome

Author

Andrew R. Griswold, Daniel P. Ball, Kuo Gai, Daniel A. Bachovchin, Brooke A. Vittimberga, Cornelius Y. Taabazuing, Marian C. Okondo, Elizabeth L. Orth, Ashley J. Chui, Darren C. Johnson, and Sahana D. Rao

Subjects

0301 basic medicine, Programmed cell death, Proteasome Endopeptidase Complex, Serine Proteinase Inhibitors, Inflammasomes, THP-1 Cells, Proteolysis, Ubiquitin-Protein Ligases, Bacterial Toxins, Article, 03 medical and health sciences, Gene Knockout Techniques, Mice, 0302 clinical medicine, medicine, Pyroptosis, Animals, Humans, Dipeptidyl-Peptidases and Tripeptidyl-Peptidases, Caspase, Antigens, Bacterial, Multidisciplinary, Innate immune system, medicine.diagnostic_test, biology, Chemistry, Intracellular parasite, HEK 293 cells, Caspase 1, Inflammasome, Immunity, Innate, Cell biology, 030104 developmental biology, HEK293 Cells, RAW 264.7 Cells, Host-Pathogen Interactions, biology.protein, CRISPR-Cas Systems, Apoptosis Regulatory Proteins, 030217 neurology & neurosurgery, medicine.drug

Abstract

Intracellular pathogens and danger signals trigger the formation of inflammasomes, which activate inflammatory caspases and induce pyroptosis. The anthrax lethal factor metalloprotease and small-molecule DPP8/9 inhibitors both activate the NLRP1B inflammasome, but the molecular mechanism of NLRP1B activation is unknown. In this study, we used genome-wide CRISPR-Cas9 knockout screens to identify genes required for NLRP1B-mediated pyroptosis. We discovered that lethal factor induces cell death via the N-end rule proteasomal degradation pathway. Lethal factor directly cleaves NLRP1B, inducing the N-end rule–mediated degradation of the NLRP1B N terminus and freeing the NLRP1B C terminus to activate caspase-1. DPP8/9 inhibitors also induce proteasomal degradation of the NLRP1B N terminus but not via the N-end rule pathway. Thus, N-terminal degradation is the common activation mechanism of this innate immune sensor.

Published

2018

17. Increased Turnover at Limiting O2 Concentrations by the Thr387 → Ala Variant of HIF-Prolyl Hydroxylase PHD2

Author

Cornelius Y. Taabazuing, Serap Pektas, and Michael J. Knapp

Subjects

Alanine, Oxygenase, Coordination sphere, biology, Hydrogen bond, Stereochemistry, Chemistry, Active site, Biochemistry, Cofactor, law.invention, law, biology.protein, Enzyme kinetics, Electron paramagnetic resonance

Abstract

PHD2 is a 2-oxoglutarate, non-heme Fe2+-dependent oxygenase that senses O2 levels in human cells by hydroxylating two prolyl residues in the oxygen-dependent degradation domain (ODD) of HIF1α. Identifying the active site contacts that determine the rate of reaction at limiting O2 concentrations is crucial for understanding how this enzyme senses pO2 and may suggest methods for chemically altering hypoxia responses. A hydrogen bonding network extends from the Fe(II) cofactor through ordered waters to the Thr387 residue in the second coordination sphere. Here we tested the impact of the side chain of Thr387 on the reactivity of PHD2 toward O2 through a combination of point mutagenesis, steady state kinetic experiments and {FeNO}7 EPR spectroscopy. The steady state kinetic parameters for Thr387 → Asn were very similar to those of wild-type (WT) PHD2, but kcat and kcat/KM(O2) for Thr387 → Ala were increased by roughly 15-fold. X-Band electron paramagnetic resonance spectroscopy of the {FeNO}7 centers of the (...

Published

2015

18. Oxygen sensing strategies in mammals and bacteria

Author

Michael J. Knapp, John A. Hangasky, and Cornelius Y. Taabazuing

Subjects

Heme, Biochemistry, Article, Hypoxia-Inducible Factor-Proline Dioxygenases, Inorganic Chemistry, Hydroxylation, chemistry.chemical_compound, medicine, Animals, Humans, Hypoxia, Mammals, chemistry.chemical_classification, Bacteria, biology, Chemistry, Mechanism (biology), Hypoxia (medical), biology.organism_classification, Oxygen, Enzyme, Hypoxia-inducible factors, Hypoxia-Inducible Factor 1, medicine.symptom, Signal transduction, Signal Transduction

Abstract

The ability to sense and adapt to changes in pO2 is crucial for basic metabolism in most organisms, leading to elaborate pathways for sensing hypoxia (low pO2). This review focuses on the mechanisms utilized by mammals and bacteria to sense hypoxia. While responses to acute hypoxia in mammalian tissues lead to altered vascular tension, the molecular mechanism of signal transduction is not well understood. In contrast, chronic hypoxia evokes cellular responses that lead to transcriptional changes mediated by the hypoxia inducible factor (HIF), which is directly controlled by post-translational hydroxylation of HIF by the non-heme Fe(II)/αKG-dependent enzymes FIH and PHD2. Research on PHD2 and FIH is focused on developing inhibitors and understanding the links between HIF binding and the O2 reaction in these enzymes. Sulfur speciation is a putative mechanism for acute O2-sensing, with special focus on the role of H2S. This sulfur-centered model is discussed, as are some of the directions for further refinement of this model. In contrast to mammals, bacterial O2-sensing relies on protein cofactors that either bind O2 or oxidatively decompose. The sensing modality for bacterial O2-sensors is either via altered DNA binding affinity of the sensory protein, or else due to the actions of a two-component signaling cascade. Emerging data suggests that proteins containing a hemerythrin-domain, such as FBXL5, may serve to connect iron sensing to O2-sensing in both bacteria and humans. As specific molecular machinery becomes identified, these hypoxia sensing pathways present therapeutic targets for diseases including ischemia, cancer, or bacterial infection.

Published

2014

19. The facial triad in the α-ketoglutarate dependent oxygenase FIH: A role for sterics in linking substrate binding to O

Author

John A, Hangasky, Cornelius Y, Taabazuing, Cristina B, Martin, Scott J, Eron, and Michael J, Knapp

Subjects

Oxygen, Repressor Proteins, Amino Acid Substitution, Catalytic Domain, Mutation, Missense, Humans, Asparagine, Crystallography, X-Ray, Hydroxylation, Catalysis, Article, Mixed Function Oxygenases

Abstract

The factor inhibiting hypoxia inducible factor-1α (FIH) is a nonheme Fe(II)/αKG oxygenase using a 2-His-1-Asp facial triad. FIH activates O2 via oxidative decarboxylation of α-ketoglutarate (αKG) to generate an enzyme-based oxidant which hydroxylates the Asn803 residue within the C-terminal transactivation domain (CTAD) of HIF-1α. Tight coupling of these two sequential reactions requires a structural linkage between the Fe(II) and the substrate binding site to ensure that O2 activation occurs after substrate binds. We tested the hypothesis that the facial triad carboxylate (Asp201) of FIH linked substrate binding and O2 binding sites. Asp201 variants of FIH were constructed and thoroughly characterized in vitro using steady-state kinetics, crystallography, autohydroxylation, and coupling measurements. Our studies revealed each variant activated O2 with a catalytic efficiency similar to that of wild-type (WT) FIH (kcat/KM(O2) = 0.17 μM−1 min−1), but led to defects in the coupling of O2 activation to substrate hydroxylation. Steady-state kinetics showed similar catalytic efficiencies for hydroxylation by WT-FIH (kcat/KM(CTAD) = 0.42 μM−1 min−1) and D201G (kcat/KM(CTAD) = 0.34 μM−1 min−1); hydroxylation by D201E was greatly impaired, while hydroxylation by D201A was undetectable. Analysis of the crystal structure of the D201E variant revealed steric crowding near the diffusible ligand site supporting a role for sterics from the facial triad carboxylate in the O2 binding order. Our data support a model in which the facial triad carboxylate Asp201 provides both steric and polar contacts to favor O2 access to the Fe(II) only after substrate binds, leading to coupled turnover in FIH and other αKG oxygenases.

Published

2016

20. Substrate Promotes Productive Gas Binding in the α-Ketoglutarate-Dependent Oxygenase FIH

Author

Michael J. Knapp, Justin T. Fermann, Scott C. Garman, and Cornelius Y. Taabazuing

Subjects

0301 basic medicine, Oxygenase, Stereochemistry, Iron, Repressor, 010402 general chemistry, Nitric Oxide, 01 natural sciences, Biochemistry, Protein Structure, Secondary, Article, Mixed Function Oxygenases, Substrate Specificity, 03 medical and health sciences, Transactivation, Histone demethylation, Oxidoreductase, Humans, chemistry.chemical_classification, Chemistry, Electron Spin Resonance Spectroscopy, Substrate (chemistry), 0104 chemical sciences, Oxygen, Repressor Proteins, 030104 developmental biology, Enzyme, Oxygenases, Ketoglutaric Acids

Abstract

The Fe(2+)/α-ketoglutarate (αKG)-dependent oxygenases use molecular oxygen to conduct a wide variety of reactions with important biological implications, such as DNA base excision repair, histone demethylation, and the cellular hypoxia response. These enzymes follow a sequential mechanism in which O2 binds and reacts after the primary substrate binds, making those structural factors that promote productive O2 binding central to their chemistry. A large challenge in this field is to identify strategies that engender productive turnover. Factor inhibiting HIF (FIH) is a Fe(2+)/αKG-dependent oxygenase that forms part of the O2 sensing machinery in human cells by hydroxylating the C-terminal transactivation domain (CTAD) found within the HIF-1α protein. The structure of FIH was determined with the O2 analogue NO bound to Fe, offering the first direct insight into the gas binding geometry in this enzyme. Through a combination of density functional theory calculations, {FeNO}(7) electron paramagnetic resonance spectroscopy, and ultraviolet-visible absorption spectroscopy, we demonstrate that CTAD binding stimulates O2 reactivity by altering the orientation of the bound gas molecule. Although unliganded FIH binds NO with moderate affinity, the bound gas can adopt either of two orientations with similar stability; upon CTAD binding, NO adopts a single preferred orientation that is appropriate for supporting oxidative decarboxylation. Combined with other studies of related enzymes, our data suggest that substrate-induced reorientation of bound O2 is the mechanism utilized by the αKG oxygenases to tightly couple O2 activation to substrate hydroxylation.

Published

2016

21. Inhibition of Dpp8/9 Activates the Nlrp1b Inflammasome

Author

Darren C. Johnson, Ashley J. Chui, Cornelius Y. Taabazuing, Marian C. Okondo, Sahana D. Rao, Sarah E. Poplawski, and Daniel A. Bachovchin

Subjects

Male, 0301 basic medicine, Dipeptidases, Proteasome Endopeptidase Complex, Proteases, Inflammasomes, Clinical Biochemistry, Caspase 1, Biology, Biochemistry, Article, Serine, Mice, 03 medical and health sciences, 0302 clinical medicine, Immune system, Drug Discovery, Pyroptosis, medicine, Animals, Humans, Molecular Biology, Pharmacology, Innate immune system, Macrophages, Pattern recognition receptor, Inflammasome, Dipeptides, Boronic Acids, Immunity, Innate, Cell biology, Mice, Inbred C57BL, HEK293 Cells, RAW 264.7 Cells, 030104 developmental biology, 030220 oncology & carcinogenesis, Proteolysis, Molecular Medicine, Female, Apoptosis Regulatory Proteins, medicine.drug

Abstract

Summary Val-boroPro (PT-100, Talabostat) induces powerful anti-tumor immune responses in syngeneic cancer models, but its mechanism of action has not yet been established. Val-boroPro is a non-selective inhibitor of post-proline-cleaving serine proteases, and the inhibition of the highly related cytosolic serine proteases Dpp8 and Dpp9 (Dpp8/9) by Val-boroPro was recently demonstrated to trigger an immunostimulatory form of programmed cell death known as pyroptosis selectively in monocytes and macrophages. Here we show that Dpp8/9 inhibition activates the inflammasome sensor protein Nlrp1b, which in turn activates pro-caspase-1 to mediate pyroptosis. This work reveals a previously unrecognized mechanism for activating an innate immune pattern recognition receptor and suggests that Dpp8/9 serve as an intracellular checkpoint to restrain Nlrp1b and the innate immune system.

Published

2018

22. Pyroptosis and Apoptosis Pathways Engage in Bidirectional Crosstalk in Monocytes and Macrophages

Author

Cornelius Y. Taabazuing, Marian C. Okondo, and Daniel A. Bachovchin

Subjects

Lipopolysaccharides, 0301 basic medicine, Programmed cell death, Clinical Biochemistry, Caspase 1, Apoptosis, Biochemistry, Caspase 7, Monocytes, Article, Cell Line, Mice, 03 medical and health sciences, Drug Discovery, Pyroptosis, Animals, Humans, Amino Acid Sequence, Dipeptidyl-Peptidases and Tripeptidyl-Peptidases, Molecular Biology, Caspase, Pharmacology, Innate immune system, biology, Caspase 3, Macrophages, Intracellular Signaling Peptides and Proteins, Phosphate-Binding Proteins, Immunity, Innate, Neoplasm Proteins, Cell biology, Crosstalk (biology), HEK293 Cells, RAW 264.7 Cells, 030104 developmental biology, Nigericin, Mutagenesis, Site-Directed, biology.protein, Molecular Medicine

Abstract

Pyroptosis is a lytic form of programmed cell death mediated by the inflammatory caspase-1, -4, and -5. We recently discovered that small-molecule inhibitors of the serine peptidases DPP8 and DPP9 (DPP8/9) induce pro-caspase-1-dependent pyroptosis in monocytes and macrophages. Notably, DPP8/9 inhibitors, unlike microbial agents, absolutely require caspase-1 to induce cell death. Therefore, DPP8/9 inhibitors are useful probes to study caspase-1 in cells. Here, we show that, in the absence of the pyroptosis-mediating substrate gasdermin D (GSDMD), caspase-1 activates caspase-3 and -7 and induces apoptosis, demonstrating that GSDMD is the only caspase-1 substrate that induces pyroptosis. Conversely, we found that, during apoptosis, caspase-3/-7 specifically block pyroptosis by cleaving GSDMD at a distinct site from the inflammatory caspases that inactivates the protein. Overall, this work reveals bidirectional crosstalk between apoptosis and pyroptosis in monocytes and macrophages, further illuminating the complex interplay between cell death pathways in the innate immune system.

Published

2017

23. Screening chelating inhibitors of HIF-prolyl hydroxylase domain 2 (PHD2) and factor inhibiting HIF (FIH)

Author

Shannon C. Flagg, Cristina B. Martin, Breanne E. Holmes, Cornelius Y. Taabazuing, and Michael J. Knapp

Subjects

Stereochemistry, Pyridines, Pyridones, Iron, Molecular Sequence Data, Catechols, Procollagen-Proline Dioxygenase, Iron Chelating Agents, Biochemistry, Article, Hypoxia-Inducible Factor-Proline Dioxygenases, Mixed Function Oxygenases, Substrate Specificity, Inorganic Chemistry, Dioxygenase, Escherichia coli, Humans, Amino Acid Sequence, Binding site, chemistry.chemical_classification, Binding Sites, biology, Chemistry, Electron Spin Resonance Spectroscopy, Active site, Hypoxia-Inducible Factor 1, alpha Subunit, Small molecule, Recombinant Proteins, Repressor Proteins, Kinetics, Enzyme, Hypoxia-inducible factors, Pyrones, biology.protein, Ketoglutaric Acids, Procollagen-proline dioxygenase, Protein Binding

Abstract

Two primary O(2)-sensors for humans are the HIF-hydroxylases, enzymes that hydroxylate specific residues of the hypoxia inducible factor-α (HIF). These enzymes are factor inhibiting HIF (FIH) and prolyl hydroxylase-2 (PHD2), each an α-ketoglutarate (αKG) dependent, non-heme Fe(II) dioxygenase. Although the two enzymes have similar active sites, FIH hydroxylates Asn(803) of HIF-1α while PHD2 hydroxylates Pro(402) and/or Pro(564) of HIF-1α. The similar structures but unique functions of FIH and PHD2 make them prime targets for selective inhibition leading to regulatory control of diseases such as cancer and stroke. Three classes of iron chelators were tested as inhibitors for FIH and PHD2: pyridines, hydroxypyrones/hydroxypyridinones and catechols. An initial screen of the ten small molecule inhibitors at varied [αKG] revealed a non-overlapping set of inhibitors for PHD2 and FIH. Dose response curves at moderate [αKG] ([αKG]~K(M)) showed that the hydroxypyrones/hydroxypyridinones were selective inhibitors, with IC(50) in the μM range, and that the catechols were generally strong inhibitors of both FIH and PHD2, with IC(50) in the low μM range. As support for binding at the active site of each enzyme as the mode of inhibition, electron paramagnetic resonance (EPR) spectroscopy were used to demonstrate inhibitor binding to the metal center of each enzyme. This work shows some selective inhibition between FIH and PHD2, primarily through the use of simple aromatic or pseudo-aromatic chelators, and suggests that hydroxypyrones and hydroxypyridones may be promising chelates for FIH or PHD2 inhibition.

Published

2011

24. Mutually exclusive binding of telomerase RNA and DNA by Ku alters telomerase recruitment model

Author

Thomas R. Cech, Pascal Chartrand, Karen J. Goodrich, Cornelius Y. Taabazuing, Faissal Ouenzar, and Jennifer S. Pfingsten

Subjects

Models, Molecular, Telomerase, Ku80, DNA End-Joining Repair, Saccharomyces cerevisiae Proteins, Mutant, Molecular Sequence Data, Biology, General Biochemistry, Genetics and Molecular Biology, Article, 03 medical and health sciences, Telomerase RNA component, chemistry.chemical_compound, Telomerase reverse transcriptase, 030304 developmental biology, Sequence Deletion, 0303 health sciences, Base Sequence, Biochemistry, Genetics and Molecular Biology(all), 030302 biochemistry & molecular biology, RNA, Telomere, Molecular biology, DNA-Binding Proteins, chemistry, Mutagenesis, Site-Directed, DNA

Abstract

Summary In Saccharomyces cerevisiae , the Ku heterodimer contributes to telomere maintenance as a component of telomeric chromatin and as an accessory subunit of telomerase. How Ku binding to double-stranded DNA (dsDNA) and to telomerase RNA (TLC1) promotes Ku's telomeric functions is incompletely understood. We demonstrate that deletions designed to constrict the DNA-binding ring of Ku80 disrupt nonhomologous end-joining (NHEJ), telomeric gene silencing, and telomere length maintenance, suggesting that these functions require Ku's DNA end-binding activity. Contrary to the current model, a mutant Ku with low affinity for dsDNA also loses affinity for TLC1 both in vitro and in vivo. Competition experiments reveal that wild-type Ku binds dsDNA and TLC1 mutually exclusively. Cells expressing the mutant Ku are deficient in nuclear accumulation of TLC1, as expected from the RNA-binding defect. These findings force reconsideration of the mechanisms by which Ku assists in recruiting telomerase to natural telomeres and broken chromosome ends. PaperClip

Published

2011

25. The second coordination sphere of FIH controls hydroxylation†

Author

Michael J. Knapp, Breanne E. Holmes, Evren Saban, Cornelius Y. Taabazuing, Yuan-Han Chen, and John A. Hangasky

Subjects

Models, Molecular, Coordination sphere, Calorimetry, Differential Scanning, Stereochemistry, Ligand, Mutant, Kinetics, Electron Spin Resonance Spectroscopy, Substrate (chemistry), Hydroxylation, Biochemistry, Article, Recombinant Proteins, Mixed Function Oxygenases, chemistry.chemical_compound, Mice, chemistry, Dioxygenase, Animals, Point Mutation, Spectrophotometry, Ultraviolet, Oxidative decarboxylation

Abstract

The factor inhibiting HIF (FIH) is a proximate oxygen sensor for human cells, hydroxylating Asn(803) within the α-subunit of the hypoxia inducible factor (HIF). FIH is an α-ketoglutatrate (αKG)-dependent, non-heme Fe(II) dioxygenase, in which Fe(II) is coordinated by a (His(2)Asp) facial triad, αKG, and H(2)O. Hydrogen bonding among the facial triad, the HIF-Asn(803) side chain, and various second-sphere residues suggests a functional role for the second coordination sphere in tuning the chemistry of the Fe(II) center. Point mutants of FIH were prepared to test the functional role of the αKG-centered (Asn(205) and Asn(294)) or HIF-Asn(803)-centered (Arg(238) and Gln(239)) second-sphere residues. The second sphere was tested for local effects on priming Fe(II) to react with O(2), oxidative decarboxylation, and substrate positioning. Steady-sate kinetics were used to test for overall catalytic effects; autohydroxylation rates were used to test for priming and positioning, and electronic spectroscopy was used to assess the primary coordination sphere and the electrophilicity of αKG. Asn(205) → Ala and Asn(294) → Ala mutants exhibited diminished rates of steady-state turnover, while minimally affecting autohydroxylation, consistent with impaired oxidative decarboxylation. Blue-shifted metal to ligand charge transfer transitions for (Fe+αKG)FIH indicated that these point mutations destabilized the π* orbitals of αKG, further supporting a slowed rate of oxidative decarboxylation. The Arg(238) → Met mutant exhibited steady-state rates too low to measure and diminished product yields, suggesting impaired substrate positioning or priming; the Arg(238) → Met mutant was capable of O(2) activation for the autohydroxylation reaction. The Gln(239) → Asn mutant exhibited significantly slowed steady-state kinetics and diminished product yields, suggesting impaired substrate positioning or priming. As HIF binding to the Gln(239) → Asn mutant stimulated autohydroxylation, it is more likely that this point mutant simply mispositions the HIF-Asn(803) side chain. This work combines kinetics and spectroscopy to show that these second-sphere hydrogen bonds play roles in promoting oxidative decarboxylation, priming Fe(II) to bind O(2), and positioning HIF-Asn(803).

Published

2011

26. Imposing function down a (cupin)-barrel: secondary structure and metal stereochemistry in the αKG-dependent oxygenases

Author

Meaghan A. Valliere, John A. Hangasky, Cornelius Y. Taabazuing, and Michael J. Knapp

Subjects

Coordination sphere, Stereochemistry, Molecular Sequence Data, Biophysics, Isopenicillin N synthase, Stereoisomerism, Biochemistry, Protein Structure, Secondary, Article, Cofactor, Substrate Specificity, Biomaterials, Protein structure, Amino Acid Sequence, Protein secondary structure, biology, Ligand, Chemistry, Metals and Alloys, Cysteine dioxygenase, Metals, Chemistry (miscellaneous), Oxygenases, biology.protein, Ketoglutaric Acids

Abstract

The Fe(II)/αketoglutarate (αKG) dependent oxygenases catalyze a diverse range of reactions significant in biological processes such as antibiotic biosynthesis, lipid metabolism, oxygen sensing, and DNA and RNA repair. Although functionally diverse, the eight-stranded β-barrel (cupin) and HX(D/E)XnH facial triad motifs are conserved in this super-family of enzymes. Crystal structure analysis of 25 αKG oxygenases reveals two stereoisomers of the Fe cofactor, Anti and Clock, which differ in the relative position of the exchangeable ligand position and the primary substrate. Herein, we discuss the relationship between the chemical mechanism and the secondary coordination sphere of the αKG oxygenases, within the constraints of the stereochemistry of the Fe cofactor. Sequence analysis of the cupin barrel indicates that a small subset of positions constitute the second coordination sphere, which has significant ramifications for the structure of the ferryl intermediate. The competence of both Anti and Clock stereoisomers of Fe points to a ferryl intermediate that is 5 coordinate. The small number of conserved close contacts within the active sites of αKG oxygenases can be extended to chemically related enzymes, such as the αKG-dependent halogenases SyrB2 and CytC3, and the non-αKG dependent dioxygenases isopenicillin N synthase (IPNS) and cysteine dioxygenase (CDO).

Published

2013