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Single-molecule tracking in live cells reveals distinct target-search strategies of transcription factors in the nucleus

  • Ignacio Izeddin
  • , Vincent Récamier
  • , Lana Bosanac
  • , Ibrahim I. Cissé
  • , Lydia Boudarene
  • , Claire Dugast-Darzacq
  • , Florence Proux
  • , Olivier Bénichou
  • , Raphaël Voituriez
  • , Olivier Bensaude
  • , Maxime Dahan
  • , Xavier Darzacq
  • CNRS
  • PSL research University & IPSL
  • Laboratory Imaging
  • Howard Hughes Medical Institute
  • Massachusetts Institute of Technology
  • Laboratoire de Probabilités et Modèles Aléatoires
  • Université Pierre et Marie Curie
  • Institut Curie
  • University of California, Berkeley

Résultats de recherche: Contribution à un journalArticleRevue par des pairs

Résumé

Gene regulation relies on transcription factors (TFs) exploring the nucleus searching their targets. So far, most studies have focused on how fast TFs diffuse, underestimating the role of nuclear architecture. We implemented a single-molecule tracking assay to determine TFs dynamics. We found that c-Myc is a global explorer of the nucleus. In contrast, the positive transcription elongation factor P-TEFb is a local explorer that oversamples its environment. Consequently, each c-Myc molecule is equally available for all nuclear sites while P-TEFb reaches its targets in a position-dependent manner. Our observations are consistent with a model in which the exploration geometry of TFs is restrained by their interactions with nuclear structures and not by exclusion. The geometry-controlled kinetics of TFs target-search illustrates the influence of nuclear architecture on gene regulation, and has strong implications on how proteins react in the nucleus and how their function can be regulated in space and time.

langue originaleAnglais
Numéro d'articlee02230
journaleLife
Volume2014
Numéro de publication3
Les DOIs
étatPublié - 12 juin 2014
Modification externeOui

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