Substrate Promiscuity and Hyperoxidation Susceptibility as Potential Driving Forces for the Co-evolution of Prx5-Type and Prx6-Type 1‑Cys Peroxiredoxin Mechanisms

Substrate Promiscuity and Hyperoxidation Susceptibility as Potential Driving Forces for the Co-evolution of Prx5-Type and Prx6-Type 1‑Cys Peroxiredoxin Mechanisms

So-called 1-Cys peroxiredoxins (Prx) employ only one cysteine residue for the reduction of hydroperoxides and require an external thiol for the reduction of a reactive sulfenic acid during the catalytic cycle. Hence, 1-Cys Prx, which often belong to the structural Prx5- or the Prx6-type subfamily, a...

Ausführliche Beschreibung

Gespeichert in:
Bibliographische Detailangaben
Veröffentlicht in:ACS catalysis 2023-03, Vol.13 (6), p.3627-3643
Hauptverfasser: Lang, Lukas, Wolf, Ann-Cathrin, Riedel, Mareike, Thibol, Lea, Geissel, Fabian, Feld, Kristina, Zimmermann, Jannik, Morgan, Bruce, Manolikakes, Georg, Deponte, Marcel
Format: Artikel
Sprache:eng
Online-Zugang:Volltext
Tags: Tag hinzufügen
Keine Tags, Fügen Sie den ersten Tag hinzu!
container_end_page 3643
container_issue 6
container_start_page 3627
container_title ACS catalysis
container_volume 13
creator Lang, Lukas
Wolf, Ann-Cathrin
Riedel, Mareike
Thibol, Lea
Geissel, Fabian
Feld, Kristina
Zimmermann, Jannik
Morgan, Bruce
Manolikakes, Georg
Deponte, Marcel
description So-called 1-Cys peroxiredoxins (Prx) employ only one cysteine residue for the reduction of hydroperoxides and require an external thiol for the reduction of a reactive sulfenic acid during the catalytic cycle. Hence, 1-Cys Prx, which often belong to the structural Prx5- or the Prx6-type subfamily, are potentially promiscuous enzymes that could react with a variety of thiols. Furthermore, the dependence on an external thiol could affect the susceptibility of 1-Cys Prx to hyperoxidation, i.e., the formation of a sulfinic or sulfonic acid. Here, we compared the reaction mechanisms and kinetics of the Prx5- and Prx6-type enzymes PfAOP and PfPrx6 from the malaria parasite Plasmodium falciparum to address the hyperoxidation susceptibility and potential substrate promiscuity of 1-Cys Prx. While PfAOP did not react with common thiol-disulfide oxido­reductases, the enzyme turned out to be promiscuous regarding the reduction by synthesized glutathione analogues and other low-molecular-weight thiols. Furthermore, we established a complete single turnover experiment for PfAOP with glutathione and the glutaredoxin PfGrx and identified the rapid H2O2-dependent hyperoxidation of PfAOP as the cause for the apparent preference of this Prx5-type enzyme for alkylhydroperoxides in vitro. Unlike promiscuous PfAOP, PfPrx6 was inactive with ascorbate, the physiological low-molecular-weight thiols glutathione, cysteine, cysteamine, coenzyme A, and dihydrolipoamide, as well as physiological protein thiols, including PfTrx1, PfGrx, and the resolving cysteine of the Prx1-type enzyme PfPrx1a in potential hetero-oligomers. Reduction of PfPrx6 was only observed with dithiothreitol and required the presence of a histidine residue, which protects the enzyme from hyperoxidation and is the major structural difference between the active sites of Prx5- and Prx6-type enzymes. We propose two alternative evolutionary adaptations of the 1-Cys Prx mechanism to hyperoxidation and the formation of alternative mixed disulfides that could explain the co-existence of promiscuous Prx5- and protected Prx6-type enzymes in a variety of organisms and subcellular compartments.
doi_str_mv 10.1021/acscatal.2c04896
format Article
fullrecord <record><control><sourceid>acs_cross</sourceid><recordid>TN_cdi_crossref_primary_10_1021_acscatal_2c04896</recordid><sourceformat>XML</sourceformat><sourcesystem>PC</sourcesystem><sourcerecordid>b855480467</sourcerecordid><originalsourceid>FETCH-LOGICAL-a322t-2e7793df3546932bf9c3517419c18a41e0d0f4030c899c4c7781f8ebbd55b18e3</originalsourceid><addsrcrecordid>eNp1UEtOwzAQtRBIVKV7lj4AKXZs57NEgVKkIiq1rCPHsamrNK5sp2p3XIE7cDJOgkmLxIZZzMzTzHszegBcYzTGKMa3XDjBPW_GsUA0y5MzMIgxYxGjhJ3_6S_ByLk1CkFZkqVoAD4XXeW85V7CuTUb7USn_QHytobTw1Zas9c199q0cNE5IbdeV7rpNxycGy9br3kD763e6fYNTowV0kFlLPQrCQsTyZ1pup5vVLiwZ9EyyPb6ASVHhL_eP4pDEOzvWVmH3MJnKVa81W7jrsCF4o2To1MdgtfJw7KYRrOXx6fibhZxEsc-imWa5qRWhNEkJ3GlckEYTinOBc44xRLVSFFEkMjyXFCRphlWmayqmrEKZ5IMATrqCmucs1KVW6s33B5KjMofo8tfo8uT0YFyc6SESbk2nW3Dg_-vfwNS4YY-</addsrcrecordid><sourcetype>Aggregation Database</sourcetype><iscdi>true</iscdi><recordtype>article</recordtype></control><display><type>article</type><title>Substrate Promiscuity and Hyperoxidation Susceptibility as Potential Driving Forces for the Co-evolution of Prx5-Type and Prx6-Type 1‑Cys Peroxiredoxin Mechanisms</title><source>ACS Publications</source><creator>Lang, Lukas ; Wolf, Ann-Cathrin ; Riedel, Mareike ; Thibol, Lea ; Geissel, Fabian ; Feld, Kristina ; Zimmermann, Jannik ; Morgan, Bruce ; Manolikakes, Georg ; Deponte, Marcel</creator><creatorcontrib>Lang, Lukas ; Wolf, Ann-Cathrin ; Riedel, Mareike ; Thibol, Lea ; Geissel, Fabian ; Feld, Kristina ; Zimmermann, Jannik ; Morgan, Bruce ; Manolikakes, Georg ; Deponte, Marcel</creatorcontrib><description>So-called 1-Cys peroxiredoxins (Prx) employ only one cysteine residue for the reduction of hydroperoxides and require an external thiol for the reduction of a reactive sulfenic acid during the catalytic cycle. Hence, 1-Cys Prx, which often belong to the structural Prx5- or the Prx6-type subfamily, are potentially promiscuous enzymes that could react with a variety of thiols. Furthermore, the dependence on an external thiol could affect the susceptibility of 1-Cys Prx to hyperoxidation, i.e., the formation of a sulfinic or sulfonic acid. Here, we compared the reaction mechanisms and kinetics of the Prx5- and Prx6-type enzymes PfAOP and PfPrx6 from the malaria parasite Plasmodium falciparum to address the hyperoxidation susceptibility and potential substrate promiscuity of 1-Cys Prx. While PfAOP did not react with common thiol-disulfide oxido­reductases, the enzyme turned out to be promiscuous regarding the reduction by synthesized glutathione analogues and other low-molecular-weight thiols. Furthermore, we established a complete single turnover experiment for PfAOP with glutathione and the glutaredoxin PfGrx and identified the rapid H2O2-dependent hyperoxidation of PfAOP as the cause for the apparent preference of this Prx5-type enzyme for alkylhydroperoxides in vitro. Unlike promiscuous PfAOP, PfPrx6 was inactive with ascorbate, the physiological low-molecular-weight thiols glutathione, cysteine, cysteamine, coenzyme A, and dihydrolipoamide, as well as physiological protein thiols, including PfTrx1, PfGrx, and the resolving cysteine of the Prx1-type enzyme PfPrx1a in potential hetero-oligomers. Reduction of PfPrx6 was only observed with dithiothreitol and required the presence of a histidine residue, which protects the enzyme from hyperoxidation and is the major structural difference between the active sites of Prx5- and Prx6-type enzymes. We propose two alternative evolutionary adaptations of the 1-Cys Prx mechanism to hyperoxidation and the formation of alternative mixed disulfides that could explain the co-existence of promiscuous Prx5- and protected Prx6-type enzymes in a variety of organisms and subcellular compartments.</description><identifier>ISSN: 2155-5435</identifier><identifier>EISSN: 2155-5435</identifier><identifier>DOI: 10.1021/acscatal.2c04896</identifier><language>eng</language><publisher>American Chemical Society</publisher><ispartof>ACS catalysis, 2023-03, Vol.13 (6), p.3627-3643</ispartof><rights>2023 The Authors. Published by American Chemical Society</rights><lds50>peer_reviewed</lds50><oa>free_for_read</oa><woscitedreferencessubscribed>false</woscitedreferencessubscribed><citedby>FETCH-LOGICAL-a322t-2e7793df3546932bf9c3517419c18a41e0d0f4030c899c4c7781f8ebbd55b18e3</citedby><cites>FETCH-LOGICAL-a322t-2e7793df3546932bf9c3517419c18a41e0d0f4030c899c4c7781f8ebbd55b18e3</cites><orcidid>0000-0002-4013-5757 ; 0000-0003-2141-917X</orcidid></display><links><openurl>$$Topenurl_article</openurl><openurlfulltext>$$Topenurlfull_article</openurlfulltext><thumbnail>$$Tsyndetics_thumb_exl</thumbnail><linktopdf>$$Uhttps://pubs.acs.org/doi/pdf/10.1021/acscatal.2c04896$$EPDF$$P50$$Gacs$$H</linktopdf><linktohtml>$$Uhttps://pubs.acs.org/doi/10.1021/acscatal.2c04896$$EHTML$$P50$$Gacs$$H</linktohtml><link.rule.ids>314,777,781,2752,27057,27905,27906,56719,56769</link.rule.ids></links><search><creatorcontrib>Lang, Lukas</creatorcontrib><creatorcontrib>Wolf, Ann-Cathrin</creatorcontrib><creatorcontrib>Riedel, Mareike</creatorcontrib><creatorcontrib>Thibol, Lea</creatorcontrib><creatorcontrib>Geissel, Fabian</creatorcontrib><creatorcontrib>Feld, Kristina</creatorcontrib><creatorcontrib>Zimmermann, Jannik</creatorcontrib><creatorcontrib>Morgan, Bruce</creatorcontrib><creatorcontrib>Manolikakes, Georg</creatorcontrib><creatorcontrib>Deponte, Marcel</creatorcontrib><title>Substrate Promiscuity and Hyperoxidation Susceptibility as Potential Driving Forces for the Co-evolution of Prx5-Type and Prx6-Type 1‑Cys Peroxiredoxin Mechanisms</title><title>ACS catalysis</title><addtitle>ACS Catal</addtitle><description>So-called 1-Cys peroxiredoxins (Prx) employ only one cysteine residue for the reduction of hydroperoxides and require an external thiol for the reduction of a reactive sulfenic acid during the catalytic cycle. Hence, 1-Cys Prx, which often belong to the structural Prx5- or the Prx6-type subfamily, are potentially promiscuous enzymes that could react with a variety of thiols. Furthermore, the dependence on an external thiol could affect the susceptibility of 1-Cys Prx to hyperoxidation, i.e., the formation of a sulfinic or sulfonic acid. Here, we compared the reaction mechanisms and kinetics of the Prx5- and Prx6-type enzymes PfAOP and PfPrx6 from the malaria parasite Plasmodium falciparum to address the hyperoxidation susceptibility and potential substrate promiscuity of 1-Cys Prx. While PfAOP did not react with common thiol-disulfide oxido­reductases, the enzyme turned out to be promiscuous regarding the reduction by synthesized glutathione analogues and other low-molecular-weight thiols. Furthermore, we established a complete single turnover experiment for PfAOP with glutathione and the glutaredoxin PfGrx and identified the rapid H2O2-dependent hyperoxidation of PfAOP as the cause for the apparent preference of this Prx5-type enzyme for alkylhydroperoxides in vitro. Unlike promiscuous PfAOP, PfPrx6 was inactive with ascorbate, the physiological low-molecular-weight thiols glutathione, cysteine, cysteamine, coenzyme A, and dihydrolipoamide, as well as physiological protein thiols, including PfTrx1, PfGrx, and the resolving cysteine of the Prx1-type enzyme PfPrx1a in potential hetero-oligomers. Reduction of PfPrx6 was only observed with dithiothreitol and required the presence of a histidine residue, which protects the enzyme from hyperoxidation and is the major structural difference between the active sites of Prx5- and Prx6-type enzymes. We propose two alternative evolutionary adaptations of the 1-Cys Prx mechanism to hyperoxidation and the formation of alternative mixed disulfides that could explain the co-existence of promiscuous Prx5- and protected Prx6-type enzymes in a variety of organisms and subcellular compartments.</description><issn>2155-5435</issn><issn>2155-5435</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2023</creationdate><recordtype>article</recordtype><recordid>eNp1UEtOwzAQtRBIVKV7lj4AKXZs57NEgVKkIiq1rCPHsamrNK5sp2p3XIE7cDJOgkmLxIZZzMzTzHszegBcYzTGKMa3XDjBPW_GsUA0y5MzMIgxYxGjhJ3_6S_ByLk1CkFZkqVoAD4XXeW85V7CuTUb7USn_QHytobTw1Zas9c199q0cNE5IbdeV7rpNxycGy9br3kD763e6fYNTowV0kFlLPQrCQsTyZ1pup5vVLiwZ9EyyPb6ASVHhL_eP4pDEOzvWVmH3MJnKVa81W7jrsCF4o2To1MdgtfJw7KYRrOXx6fibhZxEsc-imWa5qRWhNEkJ3GlckEYTinOBc44xRLVSFFEkMjyXFCRphlWmayqmrEKZ5IMATrqCmucs1KVW6s33B5KjMofo8tfo8uT0YFyc6SESbk2nW3Dg_-vfwNS4YY-</recordid><startdate>20230317</startdate><enddate>20230317</enddate><creator>Lang, Lukas</creator><creator>Wolf, Ann-Cathrin</creator><creator>Riedel, Mareike</creator><creator>Thibol, Lea</creator><creator>Geissel, Fabian</creator><creator>Feld, Kristina</creator><creator>Zimmermann, Jannik</creator><creator>Morgan, Bruce</creator><creator>Manolikakes, Georg</creator><creator>Deponte, Marcel</creator><general>American Chemical Society</general><scope>AAYXX</scope><scope>CITATION</scope><orcidid>https://orcid.org/0000-0002-4013-5757</orcidid><orcidid>https://orcid.org/0000-0003-2141-917X</orcidid></search><sort><creationdate>20230317</creationdate><title>Substrate Promiscuity and Hyperoxidation Susceptibility as Potential Driving Forces for the Co-evolution of Prx5-Type and Prx6-Type 1‑Cys Peroxiredoxin Mechanisms</title><author>Lang, Lukas ; Wolf, Ann-Cathrin ; Riedel, Mareike ; Thibol, Lea ; Geissel, Fabian ; Feld, Kristina ; Zimmermann, Jannik ; Morgan, Bruce ; Manolikakes, Georg ; Deponte, Marcel</author></sort><facets><frbrtype>5</frbrtype><frbrgroupid>cdi_FETCH-LOGICAL-a322t-2e7793df3546932bf9c3517419c18a41e0d0f4030c899c4c7781f8ebbd55b18e3</frbrgroupid><rsrctype>articles</rsrctype><prefilter>articles</prefilter><language>eng</language><creationdate>2023</creationdate><toplevel>peer_reviewed</toplevel><toplevel>online_resources</toplevel><creatorcontrib>Lang, Lukas</creatorcontrib><creatorcontrib>Wolf, Ann-Cathrin</creatorcontrib><creatorcontrib>Riedel, Mareike</creatorcontrib><creatorcontrib>Thibol, Lea</creatorcontrib><creatorcontrib>Geissel, Fabian</creatorcontrib><creatorcontrib>Feld, Kristina</creatorcontrib><creatorcontrib>Zimmermann, Jannik</creatorcontrib><creatorcontrib>Morgan, Bruce</creatorcontrib><creatorcontrib>Manolikakes, Georg</creatorcontrib><creatorcontrib>Deponte, Marcel</creatorcontrib><collection>CrossRef</collection><jtitle>ACS catalysis</jtitle></facets><delivery><delcategory>Remote Search Resource</delcategory><fulltext>fulltext</fulltext></delivery><addata><au>Lang, Lukas</au><au>Wolf, Ann-Cathrin</au><au>Riedel, Mareike</au><au>Thibol, Lea</au><au>Geissel, Fabian</au><au>Feld, Kristina</au><au>Zimmermann, Jannik</au><au>Morgan, Bruce</au><au>Manolikakes, Georg</au><au>Deponte, Marcel</au><format>journal</format><genre>article</genre><ristype>JOUR</ristype><atitle>Substrate Promiscuity and Hyperoxidation Susceptibility as Potential Driving Forces for the Co-evolution of Prx5-Type and Prx6-Type 1‑Cys Peroxiredoxin Mechanisms</atitle><jtitle>ACS catalysis</jtitle><addtitle>ACS Catal</addtitle><date>2023-03-17</date><risdate>2023</risdate><volume>13</volume><issue>6</issue><spage>3627</spage><epage>3643</epage><pages>3627-3643</pages><issn>2155-5435</issn><eissn>2155-5435</eissn><abstract>So-called 1-Cys peroxiredoxins (Prx) employ only one cysteine residue for the reduction of hydroperoxides and require an external thiol for the reduction of a reactive sulfenic acid during the catalytic cycle. Hence, 1-Cys Prx, which often belong to the structural Prx5- or the Prx6-type subfamily, are potentially promiscuous enzymes that could react with a variety of thiols. Furthermore, the dependence on an external thiol could affect the susceptibility of 1-Cys Prx to hyperoxidation, i.e., the formation of a sulfinic or sulfonic acid. Here, we compared the reaction mechanisms and kinetics of the Prx5- and Prx6-type enzymes PfAOP and PfPrx6 from the malaria parasite Plasmodium falciparum to address the hyperoxidation susceptibility and potential substrate promiscuity of 1-Cys Prx. While PfAOP did not react with common thiol-disulfide oxido­reductases, the enzyme turned out to be promiscuous regarding the reduction by synthesized glutathione analogues and other low-molecular-weight thiols. Furthermore, we established a complete single turnover experiment for PfAOP with glutathione and the glutaredoxin PfGrx and identified the rapid H2O2-dependent hyperoxidation of PfAOP as the cause for the apparent preference of this Prx5-type enzyme for alkylhydroperoxides in vitro. Unlike promiscuous PfAOP, PfPrx6 was inactive with ascorbate, the physiological low-molecular-weight thiols glutathione, cysteine, cysteamine, coenzyme A, and dihydrolipoamide, as well as physiological protein thiols, including PfTrx1, PfGrx, and the resolving cysteine of the Prx1-type enzyme PfPrx1a in potential hetero-oligomers. Reduction of PfPrx6 was only observed with dithiothreitol and required the presence of a histidine residue, which protects the enzyme from hyperoxidation and is the major structural difference between the active sites of Prx5- and Prx6-type enzymes. We propose two alternative evolutionary adaptations of the 1-Cys Prx mechanism to hyperoxidation and the formation of alternative mixed disulfides that could explain the co-existence of promiscuous Prx5- and protected Prx6-type enzymes in a variety of organisms and subcellular compartments.</abstract><pub>American Chemical Society</pub><doi>10.1021/acscatal.2c04896</doi><tpages>17</tpages><orcidid>https://orcid.org/0000-0002-4013-5757</orcidid><orcidid>https://orcid.org/0000-0003-2141-917X</orcidid><oa>free_for_read</oa></addata></record>
fulltext fulltext
identifier ISSN: 2155-5435
ispartof ACS catalysis, 2023-03, Vol.13 (6), p.3627-3643
issn 2155-5435
2155-5435
language eng
recordid cdi_crossref_primary_10_1021_acscatal_2c04896
source ACS Publications
title Substrate Promiscuity and Hyperoxidation Susceptibility as Potential Driving Forces for the Co-evolution of Prx5-Type and Prx6-Type 1‑Cys Peroxiredoxin Mechanisms
url https://sfx.bib-bvb.de/sfx_tum?ctx_ver=Z39.88-2004&ctx_enc=info:ofi/enc:UTF-8&ctx_tim=2025-01-18T03%3A20%3A33IST&url_ver=Z39.88-2004&url_ctx_fmt=infofi/fmt:kev:mtx:ctx&rfr_id=info:sid/primo.exlibrisgroup.com:primo3-Article-acs_cross&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.genre=article&rft.atitle=Substrate%20Promiscuity%20and%20Hyperoxidation%20Susceptibility%20as%20Potential%20Driving%20Forces%20for%20the%20Co-evolution%20of%20Prx5-Type%20and%20Prx6-Type%201%E2%80%91Cys%20Peroxiredoxin%20Mechanisms&rft.jtitle=ACS%20catalysis&rft.au=Lang,%20Lukas&rft.date=2023-03-17&rft.volume=13&rft.issue=6&rft.spage=3627&rft.epage=3643&rft.pages=3627-3643&rft.issn=2155-5435&rft.eissn=2155-5435&rft_id=info:doi/10.1021/acscatal.2c04896&rft_dat=%3Cacs_cross%3Eb855480467%3C/acs_cross%3E%3Curl%3E%3C/url%3E&disable_directlink=true&sfx.directlink=off&sfx.report_link=0&rft_id=info:oai/&rft_id=info:pmid/&rfr_iscdi=true