Notes

Adaptable Pendant Polymer pertaining to Selective Charge Provider Transfer through Controlling the Supramolecular Self-Assembly.
The use of radical bridging ligands to facilitate strong magnetic exchange between paramagnetic metal centers represents a key step toward the realization of single-molecule magnets with high operating temperatures. Moreover, bridging ligands that allow the incorporation of high-anisotropy metal ions are particularly advantageous. Toward these ends, we report the synthesis and detailed characterization of the dinuclear hydroquinone-bridged complexes [(Me6tren)2MII 2(C6H4O2 2-)]2+ (Me6tren = tris(2-dimethylaminoethyl)amine; M = Fe, Co, Ni) and their one-electron-oxidized, semiquinone-bridged analogues [(Me6tren)2MII 2(C6H4O2 -˙)]3+. Single-crystal X-ray diffraction shows that the Me6tren ligand restrains the metal centers in a trigonal bipyramidal geometry, and coordination of the bridging hydro- or semiquinone ligand results in a parallel alignment of the three-fold axes. We quantify the p-benzosemiquinone-transition metal magnetic exchange coupling for the first time and find that the nickel(ii) complex exhibits a substantial J less then -600 cm-1, resulting in a well-isolated S = 3/2 ground state even as high as 300 K. The iron and cobalt complexes feature metal-semiquinone exchange constants of J = -144(1) and -252(2) cm-1, respectively, which are substantially larger in magnitude than those reported for related bis(bidentate) semiquinoid complexes. Finally, the semiquinone-bridged cobalt and nickel complexes exhibit field-induced slow magnetic relaxation, with relaxation barriers of U eff = 22 and 46 cm-1, respectively. Remarkably, the Orbach relaxation observed for the Ni complex is in stark contrast to the fast processes that dominate relaxation in related mononuclear NiII complexes, thus demonstrating that strong magnetic coupling can engender slow magnetic relaxation.Isoenriched poly-3-hydroxybutyrate (P3HB) is a biodegradable material with properties similar to isotactic polypropylene, yet efficient routes to this material are lacking after 50+ years of extensive efforts in catalyst design. In this contribution, a novel lanthanum aminobisphenolate catalyst (1-La) can access isoenriched P3HB through the stereospecific ring-opening polymerization (ROP) of rac-β-butyrolactone (rac-BBL). Replacing the tethered donor group of a privileged supporting ligand with a non-coordinating benzyl substituent generates a catalyst whose reactivity and selectivity can be tuned with inexpensive achiral neutral donor ligands (e.g. see more phosphine oxides, OPR3). The 1-La/OPR3 (R = n-octyl, Ph) systems display high activity and are the most isoselective homogeneous catalysts for the ROP of rac-BBL to date (0 °C P m = 0.8, TOF ∼190 h-1). Combined reactivity and spectroscopic studies provide insight into the active catalyst structure and ROP mechanism. Both 1-La(TPPO)2 and a structurally related catalyst with a tethered donor group (2-Y) operate under chain-end stereocontrol; however, 2-RE favors formation of P3HB with opposite tacticity (syndioenriched) and its ROP activity and selectivity are totally unaffected by added neutral donor ligands. Our studies uncover new roles for neutral donor ligands in stereospecific ROP, including suppression of chain-scission events, and point to new opportunities for catalyst design.Understanding the origin and structural basis of the photoluminescence (PL) phenomenon in thiolate-protected metal nanoclusters is of paramount importance for both fundamental science and practical applications. It remains a major challenge to correlate the PL properties with the atomic-level structure due to the complex interplay of the metal core (i.e. the inner kernel) and the exterior shell (i.e. surface Au(i)-thiolate staple motifs). Decoupling these two intertwined structural factors is critical in order to understand the PL origin. Herein, we utilize two Au28(SR)20 nanoclusters with different -R groups, which possess the same core but different shell structures and thus provide an ideal system for the PL study. We discover that the Au28(CHT)20 (CHT cyclohexanethiolate) nanocluster exhibits a more than 15-fold higher PL quantum yield than the Au28(TBBT)20 nanocluster (TBBT p-tert-butylbenzenethiolate). Such an enhancement is found to originate from the different structural arrangement of the staple motifs in the shell, which modifies the electron relaxation dynamics in the inner core to different extents for the two nanoclusters. The emergence of a long PL lifetime component in the more emissive Au28(CHT)20 nanocluster reveals that its PL is enhanced by suppressing the nonradiative pathway. The presence of long, interlocked staple motifs is further identified as a key structural parameter that favors the luminescence. Overall, this work offers structural insights into the PL origin in Au28(SR)20 nanoclusters and provides some guidelines for designing luminescent metal nanoclusters for sensing and optoelectronic applications.Currently, bright aggregation-induced emission luminogens (AIEgens) with high photoluminescence quantum yields (PLQYs) in the NIR-II region are still limited, and thus an efficient strategy to enhance NIR-II fluorescence performance through tuning molecular aggregation is proposed here. The synthesized donor-acceptor tailored AIEgen (DTPA-TBZ) not only exhibits an excellent absorptivity in the NIR-I region, but also good fluorescence signals in the NIR-II region with an emission extending to 1200 nm. Benefiting from such improved intramolecular restriction and aggregation, a significant absolute PLQY value of 8.98% was obtained in solid DTPA-TBZ. Encouragingly, the resulting AIE dots also exhibit a high relative PLQY of up to 11.1% with IR 26 as the reference (PLQY = 0.5%). Finally, the AIE dots were applied in high performance NIR-II fluorescence imaging and NIR-I photoacoustic (PA) imaging visualization of abdominal vessels, hind limb vasculature, and cerebral vessels with high signal to background ratios was performed via NIR-II imaging; Moreover, PA imaging has also been performed to clearly observe tumors in vivo. These results demonstrate that by finely tuning molecular aggregation in DTPA-TBZ, a good NIR-I absorptivity and a highly emissive fluorescence in the NIR-II region can be achieved simultaneously, finally resulting in a promising dual-modal imaging platform for real-world applications to achieve precise cancer diagnostics.
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