Synthesis and characterization of high-molecular-weight syndiotactic amorphous polypropylene

Heterocycle-fused titanium indenyl silylamido dimethyl complexes produce very high molecular weight polypropylene having a prevailingly syndiotactic microstructure with syndiotactic pentad contents rrrr up to 40-55% (sam-PP). The samples are basically amorphous and may slowly develop a low level of crystallinity (16-20%) at room temperature. A structural characterization has shown that sam-PP samples crystallize in disordered modifications of the helical form I of syndiotactic polypropylene (s-PP). The stretching of compression-molded films of sam-PP samples produce oriented crystalline fibers in the trans-planar mesomorphic form of s-PP. The low stereoregularity prevents the formation of the ordered trans-planar form III of s-PP, which instead is obtained in stretched fibers of the highly stereoregular and crystalline s-PP. The trans-planar mesomorphic form, obtained in stretched fibers, in turn transforms into the helical form I upon releasing the tension. The analysis of the mechanical properties has shown that sam-PP samples show good elastic behavior in a large range of deformation with remarkable strength, due to the presence of crystallinity. A comparison with the mechanical properties of less syndiotactic and fully amorphous samples is reported. These fully amorphous samples present lower strength and experience rapid viscous flow of the chains at high deformations and/or by application of stresses for long times. The higher strength in the semicrystalline sam-PP samples makes these materials interesting thermoplastic elastomers showing high toughness and ductility.     

In-source fragmentation and analysis of polysaccharides by capillary electrophoresis/mass spectrometry

In order to develop a robust and easy-to-use technique for characterization of bacterial polysaccharides, a pseudo-hydrolysis strategy was investigated. Based on in-source collision-induced dissociation, polysaccharide molecular ions were fragmented within the orifice-skimmer region of an electrospray ionization (ESI) mass spectrometer. The fragment ions thus generated were then analyzed similarly to the conventional ESI mass spectrometry approach. MS/MS scanning was applied to obtain product-ion spectra of the primary fragments for sequencing. To further improve the sensitivity and separation of polysaccharides from other components in the samples, a pressure-assisted capillary electrophoresis/mass spectrometry (CE/MS) system was employed. Using bacterial polysaccharides as model compounds, the mass spectra obtained for polysaccharide repeating units generated through chemical hydrolysis and in-source fragmentation were directly compared, both in positive and negative ion modes. With the additional separation of impurities provided by CE, the success of this technique has been demonstrated for structural analysis of O-chain polysaccharides (O-PS) and capsular polysaccharides (CPS). In-source fragmentation was applied to promote the formation of structurally relevant repeating units of heterogeneous CPS that would remain undetected using conventional ESI conditions. This approach was proven to be particularly useful for probing the subtle structural differences in monosaccharide composition and functionalities arising across bacterial serotypes.     

Structure and properties of ZnS nanoclusters

Earlier studies have shown that the most stable structures for (ZnS)n clusters with n = 10-47 are hollow polyhedral clusters ("bubbles"). We report a detailed study of larger clusters, where n = 50, 60, 70, and 80, for which onionlike or "double bubble" structures are predicted. We report calculations of the vibrational spectra and the electronic structure of bubble and double bubble clusters, which may assist in their experimental identification.     

Diiron-aminocarbyne complexes with amine or imine ligands: C-N coupling between imine and aminocarbyne ligands promoted by tolylacetylide addition to [Fe2{μ-CN(Me)R}(μ-CO)(CO)(NHCPh2)(Cp)2][SO3CF3]

A terminally coordinated CO ligand in the complexes [Fe₂{μ-CN(Me)R}(μ-CO)(CO)₂(Cp)₂][SO₃CF₃] (R = Me, 1a; R = Xyl, 1b; Xyl = 2,6-Me₂C₆H₃), is readily displaced by primary and secondary amines (L), in the presence of Me₃NO, affording the complexes [Fe₂{μ-CN(Me)R}(μ-CO)(CO)(L)(Cp)₂][SO₃CF₃] (R = Me, L = NH₂Et, 4a; R = Xyl, L = NH₂Et, 4b; R = Me, L = NH₂Prⁱ, 5a; R = Xyl, L = NH₂Prⁱ, 5b; R = Xyl, L = NH₂C₆H₁₁, 6; R = Xyl, L = NH₂Ph, 7; R = Xyl, L = NH₃, 8; R = Me, L = NHMe₂, 9a; R = Xyl, L = NHMe₂, 9b; R = Xyl, = NH(CH₂)₅, 10). In the absence of Me₃NO, NH₂Et gives addition at the CO ligand of 1b, yielding [Fe₂{μ-CN(Me)(Xyl)}(μ-CO)(CO){C(O)NHEt}(Cp)₂] (11). Carbonyl replacement is also observed in the reaction of 1a-b with pyridine and benzophenone imine, affording [Fe₂{μ-CN(Me)R}(μ-CO)(CO)(L)(Cp)₂][SO₃CF₃] (R = Me, L = Py, 12a; R = Xyl, L = Py, 12b; R = Me, L = HNCPh₂, 13a; R = Xyl, L = HNCPh₂, 13b). The imino complex 13b reacts with p-tolylacetylide leading to the formation of the μ-vinylidene-diaminocarbene compound [Fe₂{μ-η¹:η²- CC(Tol)C(Ph)₂N(H)CN(Me)(Xyl){(μ-CO)(CO)(Cp₂)] (15) which has been studied by X-ray diffraction.     

The Development of BTK Inhibitors: A Five-Year Update

Bruton’s tyrosine kinase (BTK) represented, in the past ten years, an important target for the development of new therapeutic agents that could be useful for cancer and autoimmune disorders. To date, five compounds, able to block BTK in an irreversible manner, have been launched in the market, whereas many reversible BTK inhibitors (BTKIs), with reduced side effects that are more useful for long-term administration in autoimmune disorders, are under clinical investigation. Despite the presence in the literature of many articles and reviews, studies on BTK function and BTKIs are of great interest for pharmaceutical companies as well as academia. This review is focused on compounds that have appeared in the literature from 2017 that are able to block BTK in an irreversible or reversible manner; also, new promising tunable irreversible inhibitors, as well as PROTAC molecules, have been reported. This summary could improve the knowledge of the chemical diversity of BTKIs and provide information for future studies, particularly from the medicinal chemistry point of view. Data reported here are collected from different databases (Scifinder, Web of Science, Scopus, Google Scholar, and Pubmed) using “BTK” and “BTK inhibitors” as keywords.     

Longitudinal Bottom-Up Proteomics of Serum,Serum Extracellular Vesicles,and Cerebrospinal Fluid Reveals Candidate Biomarkers for Early Detection of Glioblastoma in a Murine Model

Glioblastoma Multiforme (GBM) is a brain tumor with a poor prognosis and low survival rates. GBM is diagnosed at an advanced stage, so little information is available on the early stage of the disease and few improvements have been made for earlier diagnosis. Longitudinal murine models are a promising platform for biomarker discovery as they allow access to the early stages of the disease. Nevertheless, their use in proteomics has been limited owing to the low sample amount that can be collected at each longitudinal time point. Here we used optimized microproteomics workflows to investigate longitudinal changes in the protein profile of serum, serum small extracellular vesicles (sEVs), and cerebrospinal fluid (CSF) in a GBM murine model. Baseline, pre-symptomatic, and symptomatic tumor stages were determined using non-invasive motor tests. Forty-four proteins displayed significant differences in signal intensities during GBM progression. Dysregulated proteins are involved in cell motility, cell growth, and angiogenesis. Most of the dysregulated proteins already exhibited a difference from baseline at the pre-symptomatic stage of the disease, suggesting that early effects of GBM might be detectable before symptom onset.     

From zirconium to titanium: the effect of the metal in propylene polymerisation using fluxional unbridged bicyclic catalysts

Catalytic systems based on unbridged substituted indenyl systems are becoming of interest in the production of elastomeric polypropylene. A full understanding of the structural features necessary to control this kind of behaviour has not yet been achieved, since relatively slight changes in the molecular architecture can lead to polymers with remarkably different properties. We report here our recent findings regarding the study of bicyclic zirconium and titanium complexes as fluxional catalysts in propylene polymerisation. Most of them have been synthesised according to a synthetic procedure that allowed us to prepare a series of complexes in which the ring fused to the cyclopentadienyl moiety is saturated and of different sizes, thus introducing a flexibility parameter that can be finely tuned. The results obtained show that the stereoselectivity induced by this class of catalysts strongly depends both on the structure of the ligand and on the nature of metal atom (Zr vs. Ti). The titanium-based catalysts yield polypropylenes with new and interesting microstructures, in particular when an higher stability is achieved through a careful choice of the substitution pattern of the ligands.     

Tetrameric aggregate of 1,c‐3‐diphenyltetran‐r‐1‐ol via an R44(8) homodromic ring

The compound 1,c‐3‐diphenyltetran‐r‐1‐ol (systematic name: 1,c‐3‐diphenyl‐1,2,3,4‐tetrahydro‐r‐1‐naphthol), C₂₂H₂₀O, which possesses the tetrahydronaphthalene core that is found in a large number of natural products, crystallizes with Z′ = 4 and with the four molecules forming a hydrogen‐bonded cyclic aggregate. The aliphatic six‐membered rings are present with two different conformations in the molecules of the asymmetric unit. A comparison with similar fragments reveals their conformational flexibility. In addition, the structure demonstrates the relative stereochemistries of the chiral centers, which are important since the title compound is used in the stereoselective synthesis of compounds with therapeutic activity.