Abstract

Eukaryotic nuclei are subdivided into subnuclear structures. Among the most prominent of these structures are the nucleolus and the PML nuclear bodies (PML‐NBs). PML‐NBs are spherical multiprotein aggregates of varying size localized in the interchromosomal area. PML‐NB formation is dependent on the presence of the promyelocytic leukemia protein (PML) as well as on post‐translational modification of core components by covalent attachment of the small ubiquitin‐like modifier (SUMO). So far, PML‐NBs as well as PML have been described in mammalian cells only, whereas no orthologs are known in the plant kingdom. In order to investigate conserved mechanisms in PML targeting, we expressed human PML (hPML) fused to the GFP in Nicotiana benthamiana. Using confocal laser scanning microscopy and coimmunoprecipitation followed by mass spectrometric analysis, we found the fusion protein in association with nucleolar constituents. Importantly, mutants of hPML, which are no longer SUMOylated, showed altered localizations, implying SUMO‐dependent targeting of hPML in plants as has previously been shown for mammalian cells. Interestingly, in the presence of proteasome inhibitors, hPML could also be found in the nucleolus of mammalian cells suggesting conserved targeting mechanisms of PML across kingdoms. Finally, Solanum tuberosum COP1, a proposed PML‐like protein from plants, was fused to the red fluorescent protein (RFP) and coexpressed with hPML::eGFP. Microscopic analysis confirmed the localization of COP1::RFP in nuclear speckles. However, hPML::eGFP did not colocalize with COP1::RFP. Hence, we conclude that plants do not possess specialized PML‐NBs, but that their functions may be covered by other subnuclear structures like the nucleolus. Database Proteomics data have been deposited to the ProteomeXchange Consortium with the identifier PXD004254.

Highlights

  • Eukaryotic nuclei are subdivided into subnuclear structures

  • The subnuclear structures known as PML nuclear bodies (PML-NB) are intensively studied and implicated in various cellular processes

  • Upon expression of an human PML (hPML)::eGFP construct, we could show targeting of the human protein to subnuclear interchromosomal regions associated with the nucleolus, but not to punctuate structures comparable to PML-NBs in the mammalian system [3]

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Summary

Introduction

Eukaryotic nuclei are subdivided into subnuclear structures. Among the most prominent of these structures are the nucleolus and the PML nuclear bodies (PML-NBs). Abbreviations COP1, constitutive photomorphogenic protein 1; FIB2, fibrillarin 2; hPML, human promyelocytic leukemia protein; PML-NB, PML nuclear bodies; SUMO, small ubiquitin-like modifier. One prominent example for a subnuclear domain characterized in metazoans but not in plants are structures termed PML nuclear bodies (PML-NBs) These dot-like structures of varying size, which are known as nuclear domain 10 (ND10) or PML oncogenic domains (POD), are localized to the interchromosomal area and are characterized by a subset of interacting core proteins [3]. Among these is the eponymous tumor-suppressor protein, promyelocytic leukemia protein (PML), as well as Sp100 and Daxx [1,4,5]. Based on the described inconsistencies, a functional commonality of hPML and AtCOP1 seemed unlikely and it has been suggested that PML is not evolutionarily conserved [20]

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