CMG–Pol epsilon dynamics suggests a mechanism for the establishment of leading-strand synthesis in the eukaryotic replisome

Zhou, Jin; Janska, Agnieszka; Goswami, Panchali; Renault, Ludovic; Ali, Ferdos Abid; Kotecha, Abhay; Diffley, John F.X.; Costa, Alessandro

doi:10.1073/pnas.1700530114

Cited by 94 publications

(117 citation statements)

References 54 publications

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“…In line with these findings, Pol δ can take over leading‐strand synthesis in a dysfunctional Pol ϵ background . Additionally, structural evidence has emerged showing two conformations of Pol ϵ in complex with CMG, suggestive of a Pol δ‐Pol ϵ switch on the leading strand . In this model, initial leading‐strand synthesis is uncoupled from CMG unwinding activity.…”

Section: Staged Assembly Ensures Robust Eukaryotic Dna Replicationsupporting

confidence: 56%

“…The prevailing view in the field is that eukaryotic replication proceeds with continuous synthesis of the leading strand and discontinuous synthesis of the lagging strand. However, a closer look at leading‐strand synthesis also shows discontinuous synthesis, as the leading‐strand polymerase is not always stably attached to DNA . In the past, a variety of studies using biochemical and genetic techniques generated the widely accepted view that Pol ϵ performs leading‐strand synthesis and Pol δ performs lagging‐strand synthesis (reviewed in Ref …”

Section: Staged Assembly Ensures Robust Eukaryotic Dna Replicationmentioning

confidence: 99%

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Noise in the Machine: Alternative Pathway Sampling is the Rule During DNA Replication

2017

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The astonishing efficiency and accuracy of DNA replication has long suggested that refined rules enforce a single highly reproducible sequence of molecular events during the process. This view was solidified by early demonstrations that DNA unwinding and synthesis are coupled within a stable molecular factory, known as the replisome, which consists of conserved components that each play unique and complementary roles. However, recent single-molecule observations of replisome dynamics have begun to challenge this view, revealing that replication may not be defined by a uniform sequence of events. Instead, multiple exchange pathways, pauses, and DNA loop types appear to dominate replisome function. These observations suggest we must rethink our fundamental assumptions and acknowledge that each replication cycle may involve sampling of alternative, sometimes parallel, pathways. Here, we review our current mechanistic understanding of DNA replication while highlighting findings that exemplify multi-pathway aspects of replisome function and considering the broader implications.

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Section: Staged Assembly Ensures Robust Eukaryotic Dna Replicationsupporting

confidence: 56%

Section: Staged Assembly Ensures Robust Eukaryotic Dna Replicationmentioning

confidence: 99%

Noise in the Machine: Alternative Pathway Sampling is the Rule During DNA Replication

2017

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“…These studies show that the catalytic domain of Pol ε is flexibly attached to its noncatalytic domain (which is engaged in complex with the CMG helicase). The catalytic domain adopts two conformations: it is proposed that in one conformation the catalytic domain is actively engaged with the DNA and in the other one it is disengaged [168,169]. In the context of the human replisome, we envisage that encounter with replication blocks stalls Pol ε, leading to the disengagement of the catalytic domain, followed by a switch to Pol δ4/PDIP46 which performs the bypass synthesis (Figure 7).…”

Section: Roles Of Pol δ4 and Pdip46 In Leading Strand Synthesismentioning

confidence: 98%

“…The model shown in Figure 7 incorporates recent structural and functional studies of the yeast replisome from the Diffley laboratory [168][169][170][171]. These studies show that the catalytic domain of Pol ε is flexibly attached to its noncatalytic domain (which is engaged in complex with the CMG helicase).…”

Section: Roles Of Pol δ4 and Pdip46 In Leading Strand Synthesismentioning

confidence: 99%

“…It was proposed that Pol could also disengage from the DNA during replication  stress [168,169]. Replication stress, broadly defined as encounter with replication barriers due to template lesions or complex DNA structures might be addressed by similar mechanisms to that which are well established in relation to Pol  [88,179,180] and are based on the switching of specialized polymerases such as the TLS polymerases.…”

Section: Roles Of Pol δ4 and Pdip46 In Leading Strand Synthesismentioning

confidence: 99%

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Regulation and Modulation of Human DNA Polymerase δ Activity and Function

Lee

Wang

Zhang

et al. 2017

Preprint

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This review focuses on the regulation and modulation of human DNA polymerase δ (Pol δ). The emphasis is on mechanisms that regulate the activity and properties of Pol δ in DNA repair and replication. The areas covered are the degradation of the p12 subunit of Pol δ, which converts it from a heterotetramer (Pol δ4) to a heterotrimer (Pol δ3), in response to DNA damage and also during the cell cycle. The biochemical mechanisms that lead to degradation of p12 are reviewed, as well as the properties of Pol δ4 and Pol δ3 that provide insights into their functions in DNA replication and repair. The second focus of the review involves the functions of two Pol δ binding proteins, PDIP46 and PDIP38, both of which are multi-functional proteins. PDIP46 is a novel activator of Pol δ4, and the impact of this function is discussed in relation to its potential roles in DNA replication. Several new models for the roles of Pol δ3 and Pol δ4 in leading and lagging strand DNA synthesis that integrate a role for PDIP46 are presented. PDIP38 has multiple cellular localizations including the mitochondria, the splicesosomes and the nucleus. It has been implicated in a number of cellular functions, including the regulation of specialized DNA polymerases, mitosis, the DNA damage response, Mdm2 alternative splicing and the regulation of the Nox4 NADPH oxidase.

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DNA Replication: Yeast

Smith

Raoof

et al. 2018

Encyclopedia of Life Sciences

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DNA replication is a complex biological process essential to maintaining the fidelity of genetic information passed to subsequent generations, while allowing for the mutations necessary for natural selection. The cellular machinery required for DNA replication must be precisely controlled throughout the cycle. A variety of DNA polymerases have proofreading and repairing capabilities to avoid catastrophic errors, thus maintaining genomic stability. Much of the mechanism involved in this process is evolutionarily conserved. Because yeast is a relatively simple and inexpensive organism to work with, much of our understanding of DNA replication in eukaryotes originates from experiments with yeast. The most thoroughly characterized model yeast systems are Saccharomyces cerevisiae (budding yeast) and Saccharomyces pombe (fission yeast). Key Concepts Yeast is a good model organism for simplifying and characterising cellular processes, such as DNA replication. The two most commonly used yeast models are S. cerevisiae and S. pombe . DNA replication is a complex biological process essential to genomic replication. DNA replication is a process that involves timely organisation of proteins and is regulated during the cell cycle by cyclin‐dependent protein kinases. Termination of DNA replication in yeast is generally not sequence specific, except in special circumstances in the cellular process.

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CMG–Pol epsilon dynamics suggests a mechanism for the establishment of leading-strand synthesis in the eukaryotic replisome

Cited by 94 publications

References 54 publications

Noise in the Machine: Alternative Pathway Sampling is the Rule During DNA Replication

Noise in the Machine: Alternative Pathway Sampling is the Rule During DNA Replication

Regulation and Modulation of Human DNA Polymerase δ Activity and Function

DNA Replication: Yeast

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CMG–Pol epsilon dynamics suggests a mechanism for the establishment of leading-strand synthesis in the eukaryotic replisome

Cited by 94 publications

References 54 publications

Noise in the Machine: Alternative Pathway Sampling is the Rule During DNA Replication

Noise in the Machine: Alternative Pathway Sampling is the Rule During DNA Replication

Regulation and Modulation of Human DNA Polymerase &delta; Activity and Function

DNA Replication: Yeast

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Regulation and Modulation of Human DNA Polymerase δ Activity and Function