Vasiliy Morozov scite author profile

Abstract. This White Paper presents the science case of an Electron-Ion Collider (EIC), focused on the structure and interactions of gluon-dominated matter, with the intent to articulate it to the broader nuclear science community. It was commissioned by the managements of Brookhaven National Laboratory (BNL) and Thomas Jefferson National Accelerator Facility (JLab) with the objective of presenting a summary of scientific opportunities and goals of the EIC as a follow-up to the 2007 NSAC Long Range plan. This document is a culmination of a community-wide effort in nuclear science following a series of workshops on EIC physics over the past decades and, in particular, the focused ten-week program on "Gluons and quark sea at high energies" at the Institute for Nuclear Theory in Fall 2010. It contains a brief description of a few golden physics measurements along with accelerator and detector concepts required to achieve them. It has been benefited profoundly from inputs by the users' communities of BNL and JLab. This White Paper offers the promise to propel the QCD science program in the US, established with the CEBAF accelerator at JLab and the RHIC collider at BNL, to the next QCD frontier. Preamble Editors' note for the second editionThe first edition of this White Paper was released in 2012. In the current (second) edition, the science case for the EIC is further sharpened in view of the recent data from BNL, CERN and JLab experiments and the lessons learnt from them. Additional improvements were made by taking into account suggestions from the larger nuclear physics community including those made at the EIC Users Group meeting at Stony Brook University in July 2014, and the QCD Town Meeting at Temple University in September 2014.Abhay Deshpande, Zein-Eddine Meziani and Jian-Wei Qiu November 2014 Editors' note for the third edition Since the 2nd release of this White Paper, the NSAC's Long Range Plan (2015) was successfully completed. The EIC is a major recommendation of the US nuclear science community. In the current release (version 3) we have fixed some minor remaining errors in the text, and have added a few new references. While the core science case for the EIC remains the same, the machine designs of both options, the eRHIC at BNL and the JLEIC at JLab keep evolving. In this 3rd release of the EIC White Paper instead of making substantial changes to the machine design sections (5.1 and 5.2), we give references to the most recent machine design documents.

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Electron Ion Collider: The Next QCD Frontier - Understanding the glue that binds us all

Accardi¹,

Albacete²,

Anselmino³

et al. 2012

Preprint

302

430

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This White Paper presents the science case of an Electron-Ion Collider (EIC), focused on the structure and interactions of gluon-dominated matter, with the intent to articulate it to the broader nuclear science community. It was commissioned by the managements of Brookhaven National Laboratory (BNL) and Thomas Jefferson National Accelerator Facility (JLab) with the objective of presenting a summary of scientific opportunities and goals of the EIC as a follow-up to the 2007 NSAC Long Range plan. This document is a culmination of a community-wide effort in nuclear science following a series of workshops on EIC physics over the past decades and, in particular, the focused ten-week program on "Gluons and quark sea at high energies" at the Institute for Nuclear Theory in Fall 2010. It contains a brief description of a few golden physics measurements along with accelerator and detector concepts required to achieve them. It has been benefited profoundly from inputs by the users' communities of BNL and JLab. This White Paper offers the promise to propel the QCD science program in the U.S., established with the CEBAF accelerator at JLab and the RHIC collider at BNL, to the next QCD frontier. Editors' Note for the Second EditionThe first edition of this White Paper was released in 2012. In the current (second) edition, the science case for the EIC is further sharpened in view of the recent data from BNL, CERN and JLab experiments and the lessons learnt from them. Additional improvements were made by taking into account suggestions from the larger nuclear physics community including those made at the EIC Users Group meeting at Stony Brook University in July 2014, and the QCD Town Meeting at Temple University in September 2014.

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A Plant Caspase-Like Protease Activated during the Hypersensitive Response

Kim²,

et al. 2003

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To test the hypothesis that caspase-like proteases exist and are critically involved in the implementation of programmed cell death (PCD) in plants, a search was undertaken for plant caspases activated during the N gene-mediated hypersensitive response (HR; a form of pathogen-induced PCD in plants) in tobacco plants infected with Tobacco mosaic virus (TMV). For detection, characterization, and partial purification of a tobacco caspase, the Agrobacterium tumefaciens VirD2 protein, shown here to be cleaved specifically at two sites (TATD and GEQD) by human caspase-3, was used as a target. In tobacco leaves, specific proteolytic processing of the ectopically produced VirD2 derivatives at these sites was found to occur early in the course of the HR triggered by TMV. A proteolytic activity capable of specifically cleaving the model substrate at TATD was partially purified from these leaves. A tetrapeptide aldehyde designed and synthesized on the basis of the elucidated plant caspase cleavage site prevented fragmentation of the substrate protein by plant and human caspases in vitro and counteracted TMV-triggered HR in vivo. Therefore, our data provide a characterization of caspase-specific protein fragmentation in apoptotic plant cells, with implications for the importance of such activity in the implementation of plant PCD.

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Erratum: Unexpected enhancements and reductions of rf spin resonance strengths [Phys. Rev. ST Accel. Beams9, 051001 (2006)]

Леонова¹,

Morozov²,

Krisch³

et al. 2006

Phys. Rev. ST Accel. Beams

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Innovative applications of genetic algorithms to problems in accelerator physics

Hofler

Terzić

Krämer

et al. 2013

Phys. Rev. ST Accel. Beams

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The genetic algorithm (GA) is a powerful technique that implements the principles nature uses in biological evolution to optimize a multidimensional nonlinear problem. The GA works especially well for problems with a large number of local extrema, where traditional methods (such as conjugate gradient, steepest descent, and others) fail or, at best, underperform. The field of accelerator physics, among others, abounds with problems which lend themselves to optimization via GAs. In this paper, we report on the successful application of GAs in several problems related to the existing Continuous Electron Beam Accelerator Facility nuclear physics machine, the proposed Medium-energy Electron-Ion Collider at Jefferson Lab, and a radio frequency gun-based injector. These encouraging results are a step forward in optimizing accelerator design and provide an impetus for application of GAs to other problems in the field. To that end, we discuss the details of the GAs used, include a newly devised enhancement which leads to improved convergence to the optimum, and make recommendations for future GA developments and accelerator applications.

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Vasiliy Morozov

Electron-Ion Collider: The next QCD frontier

Electron Ion Collider: The Next QCD Frontier - Understanding the glue that binds us all

A Plant Caspase-Like Protease Activated during the Hypersensitive Response

Erratum: Unexpected enhancements and reductions of rf spin resonance strengths [Phys. Rev. ST Accel. Beams9, 051001 (2006)]

Innovative applications of genetic algorithms to problems in accelerator physics

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