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Putative Cooperative ATP–DnaA Binding to Double-Stranded DnaA Box and Single-Stranded DnaA-Trio Motif upon Helicobacter pylori Replication Initiation Complex Assembly

oriC is a region of the bacterial chromosome at which the initiator protein DnaA interacts with specific sequences, leading to DNA unwinding and the initiation of chromosome replication. The general architecture of oriCs is universal; however, the structure of oriC and the mode of orisome assembly d...

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Autores principales: Jaworski, Pawel, Zyla-Uklejewicz, Dorota, Nowaczyk-Cieszewska, Malgorzata, Donczew, Rafal, Mielke, Thorsten, Weigel, Christoph, Zawilak-Pawlik, Anna
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8235120/
https://www.ncbi.nlm.nih.gov/pubmed/34205762
http://dx.doi.org/10.3390/ijms22126643
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author Jaworski, Pawel
Zyla-Uklejewicz, Dorota
Nowaczyk-Cieszewska, Malgorzata
Donczew, Rafal
Mielke, Thorsten
Weigel, Christoph
Zawilak-Pawlik, Anna
author_facet Jaworski, Pawel
Zyla-Uklejewicz, Dorota
Nowaczyk-Cieszewska, Malgorzata
Donczew, Rafal
Mielke, Thorsten
Weigel, Christoph
Zawilak-Pawlik, Anna
author_sort Jaworski, Pawel
collection PubMed
description oriC is a region of the bacterial chromosome at which the initiator protein DnaA interacts with specific sequences, leading to DNA unwinding and the initiation of chromosome replication. The general architecture of oriCs is universal; however, the structure of oriC and the mode of orisome assembly differ in distantly related bacteria. In this work, we characterized oriC of Helicobacter pylori, which consists of two DnaA box clusters and a DNA unwinding element (DUE); the latter can be subdivided into a GC-rich region, a DnaA-trio and an AT-rich region. We show that the DnaA-trio submodule is crucial for DNA unwinding, possibly because it enables proper DnaA oligomerization on ssDNA. However, we also observed the reverse effect: DNA unwinding, enabling subsequent DnaA–ssDNA oligomer formation—stabilized DnaA binding to box ts1. This suggests the interplay between DnaA binding to ssDNA and dsDNA upon DNA unwinding. Further investigation of the ts1 DnaA box revealed that this box, together with the newly identified c-ATP DnaA box in oriC1, constitute a new class of ATP–DnaA boxes. Indeed, in vitro ATP–DnaA unwinds H. pylori oriC more efficiently than ADP–DnaA. Our results expand the understanding of H. pylori orisome formation, indicating another regulatory pathway of H. pylori orisome assembly.
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spelling pubmed-82351202021-06-27 Putative Cooperative ATP–DnaA Binding to Double-Stranded DnaA Box and Single-Stranded DnaA-Trio Motif upon Helicobacter pylori Replication Initiation Complex Assembly Jaworski, Pawel Zyla-Uklejewicz, Dorota Nowaczyk-Cieszewska, Malgorzata Donczew, Rafal Mielke, Thorsten Weigel, Christoph Zawilak-Pawlik, Anna Int J Mol Sci Article oriC is a region of the bacterial chromosome at which the initiator protein DnaA interacts with specific sequences, leading to DNA unwinding and the initiation of chromosome replication. The general architecture of oriCs is universal; however, the structure of oriC and the mode of orisome assembly differ in distantly related bacteria. In this work, we characterized oriC of Helicobacter pylori, which consists of two DnaA box clusters and a DNA unwinding element (DUE); the latter can be subdivided into a GC-rich region, a DnaA-trio and an AT-rich region. We show that the DnaA-trio submodule is crucial for DNA unwinding, possibly because it enables proper DnaA oligomerization on ssDNA. However, we also observed the reverse effect: DNA unwinding, enabling subsequent DnaA–ssDNA oligomer formation—stabilized DnaA binding to box ts1. This suggests the interplay between DnaA binding to ssDNA and dsDNA upon DNA unwinding. Further investigation of the ts1 DnaA box revealed that this box, together with the newly identified c-ATP DnaA box in oriC1, constitute a new class of ATP–DnaA boxes. Indeed, in vitro ATP–DnaA unwinds H. pylori oriC more efficiently than ADP–DnaA. Our results expand the understanding of H. pylori orisome formation, indicating another regulatory pathway of H. pylori orisome assembly. MDPI 2021-06-21 /pmc/articles/PMC8235120/ /pubmed/34205762 http://dx.doi.org/10.3390/ijms22126643 Text en © 2021 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
Jaworski, Pawel
Zyla-Uklejewicz, Dorota
Nowaczyk-Cieszewska, Malgorzata
Donczew, Rafal
Mielke, Thorsten
Weigel, Christoph
Zawilak-Pawlik, Anna
Putative Cooperative ATP–DnaA Binding to Double-Stranded DnaA Box and Single-Stranded DnaA-Trio Motif upon Helicobacter pylori Replication Initiation Complex Assembly
title Putative Cooperative ATP–DnaA Binding to Double-Stranded DnaA Box and Single-Stranded DnaA-Trio Motif upon Helicobacter pylori Replication Initiation Complex Assembly
title_full Putative Cooperative ATP–DnaA Binding to Double-Stranded DnaA Box and Single-Stranded DnaA-Trio Motif upon Helicobacter pylori Replication Initiation Complex Assembly
title_fullStr Putative Cooperative ATP–DnaA Binding to Double-Stranded DnaA Box and Single-Stranded DnaA-Trio Motif upon Helicobacter pylori Replication Initiation Complex Assembly
title_full_unstemmed Putative Cooperative ATP–DnaA Binding to Double-Stranded DnaA Box and Single-Stranded DnaA-Trio Motif upon Helicobacter pylori Replication Initiation Complex Assembly
title_short Putative Cooperative ATP–DnaA Binding to Double-Stranded DnaA Box and Single-Stranded DnaA-Trio Motif upon Helicobacter pylori Replication Initiation Complex Assembly
title_sort putative cooperative atp–dnaa binding to double-stranded dnaa box and single-stranded dnaa-trio motif upon helicobacter pylori replication initiation complex assembly
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8235120/
https://www.ncbi.nlm.nih.gov/pubmed/34205762
http://dx.doi.org/10.3390/ijms22126643
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