Research on the preparation and performance of Ni2P@MOF composite nanomaterials.

The present study employed a solvothermal method utilizing triphenylphosphine and nickel acetylacetonate as precursors for phosphide preparation, followed by analysis and characterization. The Ni-MOF precursor was prepared using benzene diacid, triethylenediamine, and nickel sulfate as raw materials. Ni2P was introduced into the Ni-MOF precursor during its preparation while maintaining the synthesis conditions, allowing for the adsorption of Ni2P nanoparticles during Ni-MOF synthesis to produce Ni2P@MOF composite materials. The materials underwent individual testing for UV, magnetic, and microwave absorption properties. Magnetic testing results demonstrated that the incorporation of Ni2P led to an increase in the saturation magnetization (Ms) of Ni2P@MOFs compared to the Ni-MOF, thereby enhancing its electromagnetic loss capability. Microwave absorption property testing indicated that the Ni2P@MOFs exhibited enhanced dielectric and electromagnetic loss capabilities compared to the Ni-MOF, optimizing impedance matching properties and increasing effective absorption bandwidth compared to pure Ni2P materials.

Real-time imaging of RNA polymerase I activity in living human cells.

RNA polymerase I (Pol I) synthesizes about 60% of cellular RNA by transcribing multiple copies of the ribosomal RNA gene (rDNA). The transcriptional activity of Pol I controls the level of ribosome biogenesis and cell growth. However, there is currently a lack of methods for monitoring Pol I activity in real time. Here, we develop LiveArt (live imaging-based analysis of rDNA transcription) to visualize and quantify the spatiotemporal dynamics of endogenous ribosomal RNA (rRNA) synthesis. LiveArt reveals mitotic silencing and reactivation of rDNA transcription, as well as the transcriptional kinetics of interphase rDNA. Using LiveArt, we identify SRFBP1 as a potential regulator of rRNA synthesis. We show that rDNA transcription occurs in bursts and can be altered by modulating burst duration and amplitude. Importantly, LiveArt is highly effective in the screening application for anticancer drugs targeting Pol I transcription. These approaches pave the way for a deeper understanding of the mechanisms underlying nucleolar functions.