Highly Conserved Interaction Profiles between Clinically Relevant Mutants of the Cytomegalovirus CDK-like Kinase pUL97 and Human Cyclins: Functional Significance of Cyclin H

The complex host interaction network of human cytomegalovirus (HCMV) involves the regulatory protein kinase pUL97, which represents a viral cyclin-dependent kinase (CDK) ortholog. pUL97 interacts with the three human cyclin types T1, H, and B1, whereby the binding region of cyclin T1 and the pUL97 o...

Descripción completa

Detalles Bibliográficos
Autores principales: Schütz, Martin, Müller, Regina, Socher, Eileen, Wangen, Christina, Full, Florian, Wyler, Emanuel, Wong, Diana, Scherer, Myriam, Stamminger, Thomas, Chou, Sunwen, Rawlinson, William D., Hamilton, Stuart T., Sticht, Heinrich, Marschall, Manfred
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9569496/
https://www.ncbi.nlm.nih.gov/pubmed/36233116
http://dx.doi.org/10.3390/ijms231911814
_version_ 1784809868164595712
author Schütz, Martin
Müller, Regina
Socher, Eileen
Wangen, Christina
Full, Florian
Wyler, Emanuel
Wong, Diana
Scherer, Myriam
Stamminger, Thomas
Chou, Sunwen
Rawlinson, William D.
Hamilton, Stuart T.
Sticht, Heinrich
Marschall, Manfred
author_facet Schütz, Martin
Müller, Regina
Socher, Eileen
Wangen, Christina
Full, Florian
Wyler, Emanuel
Wong, Diana
Scherer, Myriam
Stamminger, Thomas
Chou, Sunwen
Rawlinson, William D.
Hamilton, Stuart T.
Sticht, Heinrich
Marschall, Manfred
author_sort Schütz, Martin
collection PubMed
description The complex host interaction network of human cytomegalovirus (HCMV) involves the regulatory protein kinase pUL97, which represents a viral cyclin-dependent kinase (CDK) ortholog. pUL97 interacts with the three human cyclin types T1, H, and B1, whereby the binding region of cyclin T1 and the pUL97 oligomerization region were both assigned to amino acids 231-280. We further addressed the question of whether HCMVs harboring mutations in ORF-UL97, i.e., short deletions or resistance-conferring point mutations, are affected in the interaction with human cyclins and viral replication. To this end, clinically relevant UL97 drug-resistance-conferring mutants were analyzed by whole-genome sequencing and used for genetic marker transfer experiments. The recombinant HCMVs indicated conservation of pUL97–cyclin interaction, since all viral UL97 point mutants continued to interact with the analyzed cyclin types and exerted wild-type-like replication fitness. In comparison, recombinant HCMVs UL97 Δ231-280 and also the smaller deletion Δ236-275, but not Δ241-270, lost interaction with cyclins T1 and H, showed impaired replication efficiency, and also exhibited reduced kinase activity. Moreover, a cellular knock-out of cyclins B1 or T1 did not alter HCMV replication phenotypes or pUL97 kinase activity, possibly indicating alternative, compensatory pUL97–cyclin interactions. In contrast, however, cyclin H knock-out, similar to virus deletion mutants in the pUL97–cyclin H binding region, exhibited strong defective phenotypes of HCMV replication, as supported by reduced pUL97 kinase activity in a cyclin H-dependent coexpression setting. Thus, cyclin H proved to be a very relevant determinant of pUL97 kinase activity and viral replication efficiency. As a conclusion, the results provide evidence for the functional importance of pUL97–cyclin interaction. High selective pressure on the formation of pUL97–cyclin complexes was identified by the use of clinically relevant mutants.
format Online
Article
Text
id pubmed-9569496
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher MDPI
record_format MEDLINE/PubMed
spelling pubmed-95694962022-10-17 Highly Conserved Interaction Profiles between Clinically Relevant Mutants of the Cytomegalovirus CDK-like Kinase pUL97 and Human Cyclins: Functional Significance of Cyclin H Schütz, Martin Müller, Regina Socher, Eileen Wangen, Christina Full, Florian Wyler, Emanuel Wong, Diana Scherer, Myriam Stamminger, Thomas Chou, Sunwen Rawlinson, William D. Hamilton, Stuart T. Sticht, Heinrich Marschall, Manfred Int J Mol Sci Article The complex host interaction network of human cytomegalovirus (HCMV) involves the regulatory protein kinase pUL97, which represents a viral cyclin-dependent kinase (CDK) ortholog. pUL97 interacts with the three human cyclin types T1, H, and B1, whereby the binding region of cyclin T1 and the pUL97 oligomerization region were both assigned to amino acids 231-280. We further addressed the question of whether HCMVs harboring mutations in ORF-UL97, i.e., short deletions or resistance-conferring point mutations, are affected in the interaction with human cyclins and viral replication. To this end, clinically relevant UL97 drug-resistance-conferring mutants were analyzed by whole-genome sequencing and used for genetic marker transfer experiments. The recombinant HCMVs indicated conservation of pUL97–cyclin interaction, since all viral UL97 point mutants continued to interact with the analyzed cyclin types and exerted wild-type-like replication fitness. In comparison, recombinant HCMVs UL97 Δ231-280 and also the smaller deletion Δ236-275, but not Δ241-270, lost interaction with cyclins T1 and H, showed impaired replication efficiency, and also exhibited reduced kinase activity. Moreover, a cellular knock-out of cyclins B1 or T1 did not alter HCMV replication phenotypes or pUL97 kinase activity, possibly indicating alternative, compensatory pUL97–cyclin interactions. In contrast, however, cyclin H knock-out, similar to virus deletion mutants in the pUL97–cyclin H binding region, exhibited strong defective phenotypes of HCMV replication, as supported by reduced pUL97 kinase activity in a cyclin H-dependent coexpression setting. Thus, cyclin H proved to be a very relevant determinant of pUL97 kinase activity and viral replication efficiency. As a conclusion, the results provide evidence for the functional importance of pUL97–cyclin interaction. High selective pressure on the formation of pUL97–cyclin complexes was identified by the use of clinically relevant mutants. MDPI 2022-10-05 /pmc/articles/PMC9569496/ /pubmed/36233116 http://dx.doi.org/10.3390/ijms231911814 Text en © 2022 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Schütz, Martin
Müller, Regina
Socher, Eileen
Wangen, Christina
Full, Florian
Wyler, Emanuel
Wong, Diana
Scherer, Myriam
Stamminger, Thomas
Chou, Sunwen
Rawlinson, William D.
Hamilton, Stuart T.
Sticht, Heinrich
Marschall, Manfred
Highly Conserved Interaction Profiles between Clinically Relevant Mutants of the Cytomegalovirus CDK-like Kinase pUL97 and Human Cyclins: Functional Significance of Cyclin H
title Highly Conserved Interaction Profiles between Clinically Relevant Mutants of the Cytomegalovirus CDK-like Kinase pUL97 and Human Cyclins: Functional Significance of Cyclin H
title_full Highly Conserved Interaction Profiles between Clinically Relevant Mutants of the Cytomegalovirus CDK-like Kinase pUL97 and Human Cyclins: Functional Significance of Cyclin H
title_fullStr Highly Conserved Interaction Profiles between Clinically Relevant Mutants of the Cytomegalovirus CDK-like Kinase pUL97 and Human Cyclins: Functional Significance of Cyclin H
title_full_unstemmed Highly Conserved Interaction Profiles between Clinically Relevant Mutants of the Cytomegalovirus CDK-like Kinase pUL97 and Human Cyclins: Functional Significance of Cyclin H
title_short Highly Conserved Interaction Profiles between Clinically Relevant Mutants of the Cytomegalovirus CDK-like Kinase pUL97 and Human Cyclins: Functional Significance of Cyclin H
title_sort highly conserved interaction profiles between clinically relevant mutants of the cytomegalovirus cdk-like kinase pul97 and human cyclins: functional significance of cyclin h
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9569496/
https://www.ncbi.nlm.nih.gov/pubmed/36233116
http://dx.doi.org/10.3390/ijms231911814
work_keys_str_mv AT schutzmartin highlyconservedinteractionprofilesbetweenclinicallyrelevantmutantsofthecytomegaloviruscdklikekinasepul97andhumancyclinsfunctionalsignificanceofcyclinh
AT mullerregina highlyconservedinteractionprofilesbetweenclinicallyrelevantmutantsofthecytomegaloviruscdklikekinasepul97andhumancyclinsfunctionalsignificanceofcyclinh
AT sochereileen highlyconservedinteractionprofilesbetweenclinicallyrelevantmutantsofthecytomegaloviruscdklikekinasepul97andhumancyclinsfunctionalsignificanceofcyclinh
AT wangenchristina highlyconservedinteractionprofilesbetweenclinicallyrelevantmutantsofthecytomegaloviruscdklikekinasepul97andhumancyclinsfunctionalsignificanceofcyclinh
AT fullflorian highlyconservedinteractionprofilesbetweenclinicallyrelevantmutantsofthecytomegaloviruscdklikekinasepul97andhumancyclinsfunctionalsignificanceofcyclinh
AT wyleremanuel highlyconservedinteractionprofilesbetweenclinicallyrelevantmutantsofthecytomegaloviruscdklikekinasepul97andhumancyclinsfunctionalsignificanceofcyclinh
AT wongdiana highlyconservedinteractionprofilesbetweenclinicallyrelevantmutantsofthecytomegaloviruscdklikekinasepul97andhumancyclinsfunctionalsignificanceofcyclinh
AT scherermyriam highlyconservedinteractionprofilesbetweenclinicallyrelevantmutantsofthecytomegaloviruscdklikekinasepul97andhumancyclinsfunctionalsignificanceofcyclinh
AT stammingerthomas highlyconservedinteractionprofilesbetweenclinicallyrelevantmutantsofthecytomegaloviruscdklikekinasepul97andhumancyclinsfunctionalsignificanceofcyclinh
AT chousunwen highlyconservedinteractionprofilesbetweenclinicallyrelevantmutantsofthecytomegaloviruscdklikekinasepul97andhumancyclinsfunctionalsignificanceofcyclinh
AT rawlinsonwilliamd highlyconservedinteractionprofilesbetweenclinicallyrelevantmutantsofthecytomegaloviruscdklikekinasepul97andhumancyclinsfunctionalsignificanceofcyclinh
AT hamiltonstuartt highlyconservedinteractionprofilesbetweenclinicallyrelevantmutantsofthecytomegaloviruscdklikekinasepul97andhumancyclinsfunctionalsignificanceofcyclinh
AT stichtheinrich highlyconservedinteractionprofilesbetweenclinicallyrelevantmutantsofthecytomegaloviruscdklikekinasepul97andhumancyclinsfunctionalsignificanceofcyclinh
AT marschallmanfred highlyconservedinteractionprofilesbetweenclinicallyrelevantmutantsofthecytomegaloviruscdklikekinasepul97andhumancyclinsfunctionalsignificanceofcyclinh

Ejemplares similares