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Creators/Authors contains: "Reveillaud, Julie"

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  1. null (Ed.)
  2. Abstract Despite the f0(980) hadron having been discovered half a century ago, the question about its quark content has not been settled: it might be an ordinary quark-antiquark ($${{\rm{q}}}\overline{{{\rm{q}}}}$$ q q ¯ ) meson, a tetraquark ($${{\rm{q}}}\overline{{{\rm{q}}}}{{\rm{q}}}\overline{{{\rm{q}}}}$$ q q ¯ q q ¯ ) exotic state, a kaon-antikaon ($${{\rm{K}}}\overline{{{\rm{K}}}}$$ K K ¯ ) molecule, or a quark-antiquark-gluon ($${{\rm{q}}}\overline{{{\rm{q}}}}{{\rm{g}}}$$ q q ¯ g ) hybrid. This paper reports strong evidence that the f0(980) state is an ordinary$${{\rm{q}}}\overline{{{\rm{q}}}}$$ q q ¯ meson, inferred from the scaling of elliptic anisotropies (v2) with the number of constituent quarks (nq), as empirically established using conventional hadrons in relativistic heavy ion collisions. The f0(980) state is reconstructed via its dominant decay channel f0(980) →π+π, in proton-lead collisions recorded by the CMS experiment at the LHC, and itsv2is measured as a function of transverse momentum (pT). It is found that thenq= 2 ($${{\rm{q}}}\overline{{{\rm{q}}}}$$ q q ¯ state) hypothesis is favored overnq= 4 ($${{\rm{q}}}\overline{{{\rm{q}}}}{{\rm{q}}}\overline{{{\rm{q}}}}$$ q q ¯ q q ¯ or$${{\rm{K}}}\overline{{{\rm{K}}}}$$ K K ¯ states) by 7.7, 6.3, or 3.1 standard deviations in thepT< 10, 8, or 6 GeV/cranges, respectively, and overnq= 3 ($${{\rm{q}}}\overline{{{\rm{q}}}}{{\rm{g}}}$$ q q ¯ g hybrid state) by 3.5 standard deviations in thepT< 8 GeV/crange. This result represents the first determination of the quark content of the f0(980) state, made possible by using a novel approach, and paves the way for similar studies of other exotic hadron candidates. 
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    Free, publicly-accessible full text available December 1, 2026
  3. The EIC Comprehensive Chromodynamics Experiment (ECCE) detector has been designed to address the full scope of the proposed Electron Ion Collider (EIC) physics program as presented by the National Academy of Science and provide a deeper understanding of the quark–gluon structure of matter. To accomplish this, the ECCE detector offers nearly acceptance and energy coverage along with excellent tracking and particle identification. The ECCE detector was designed to be built within the budget envelope set out by the EIC project while simultaneously managing cost and schedule risks. This detector concept has been selected to be the basis for the EIC project detector. 
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    Free, publicly-accessible full text available April 1, 2026
  4. Abstract Neural circuit function is shaped both by the cell types that comprise the circuit and the connections between those cell types1. Neural cell types have previously been defined by morphology2, 3, electrophysiology4, 5, transcriptomic expression6–8, connectivity9–13, or even a combination of such modalities14–16. More recently, the Patch-seq technique has enabled the characterization of morphology (M), electrophysiology (E), and transcriptomic (T) properties from individual cells17–20. Using this technique, these properties were integrated to define 28, inhibitory multimodal, MET-types in mouse primary visual cortex21. It is unknown how these MET-types connect within the broader cortical circuitry however. Here we show that we can predict the MET-type identity of inhibitory cells within a large-scale electron microscopy (EM) dataset and these MET-types have distinct ultrastructural features and synapse connectivity patterns. We found that EM Martinotti cells, a well defined morphological cell type22, 23known to be Somatostatin positive (Sst+)24, 25, were successfully predicted to belong to Sst+ MET-types. Each identified MET-type had distinct axon myelination patterns and synapsed onto specific excitatory targets. Our results demonstrate that morphological features can be used to link cell type identities across imaging modalities, which enables further comparison of connectivity in relation to transcriptomic or electrophysiological properties. Furthermore, our results show that MET-types have distinct connectivity patterns, supporting the use of MET-types and connectivity to meaningfully define cell types. 
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  5. null (Ed.)
  6. Free, publicly-accessible full text available September 1, 2026
  7. Free, publicly-accessible full text available September 1, 2026
  8. Free, publicly-accessible full text available September 1, 2026