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Characterization of the conserved features of the NSE6 subunit of the Physcomitrium patens SMC5/6 complex.

Edit LelkesJitka JemelkováMarcela HoláBarbora ŠtefanoviePeter KolesárRadka VágnerováEva Dvořák TomaštíkováAles PecinkaKarel J AngelisJan J Paleček
Published in: The Plant journal : for cell and molecular biology (2023)
Structural Maintenance of Chromosome (SMC) complexes are molecular machines ensuring chromatin organization at higher levels. They play direct roles in cohesion, condensation, replication, transcription, and DNA repair. Their cores are composed of long-armed SMC, kleisin, and kleisin-associated subunits. Additional factors, like NSE6 within SMC5/6, bind to SMC core complexes and regulate their activities. In the human HsNSE6/SLF2, we recently identified a new CANIN domain. Here we tracked down its sequence homology to lower plants, selected bryophyte Physcomitrium patens (Pp), and analyzed PpNSE6 protein-protein interactions to explore its conservation in detail. We identified a previously unrecognized core sequence motif conserved from yeasts to humans within the NSE6 CANIN domain. This motif mediates the interaction between NSE6 and its NSE5 partner in yeasts and plants. In addition, the CANIN domain and its preceding PpNSE6 sequences bind both PpSMC5 and PpSMC6 arms. Interestingly, we mapped the PpNSE6-binding site at the PpSMC5 arm right next to the PpNSE2-binding surface. The position of NSE6 at SMC arms suggests its role in SMC5/6 dynamics regulation. Consistent with the regulatory role of NSE6 subunits, Ppnse6 mutant lines were viable, sensitive to the DNA-damaging drug bleomycin and lost a large portion of rDNA copies. These moss mutants also exhibited reduced growth and developmental aberrations. Altogether, our data showed the conserved function of the NSE6 subunit and architecture of the SMC5/6 complex across species.
Keyphrases
  • transcription factor
  • dna repair
  • dna damage
  • endothelial cells
  • single molecule
  • oxidative stress
  • dna damage response
  • dna methylation
  • copy number
  • dna binding
  • protein kinase
  • hepatitis c virus
  • data analysis