Results show that more than half of the snow CHON molecules may be related to the oxidized and hydrolyzed processes of atmospheric organics. Potential formation processes of atmospheric organics on a molecular level provide a new concept to better understand the sources and scavenging mechanisms of organic nitrogen species in the atmosphere.Despite the recent advances in cancer therapeutics, highly aggressive cancer forms, such as glioblastoma (GBM), still have very low survival rates. The intracellular scaffold protein syntenin, comprising two postsynaptic density protein-95/discs-large/zona occludens-1 (PDZ) domains, has emerged as a novel therapeutic target in highly malignant phenotypes including GBM. Here, we report the development of a novel, highly potent, and metabolically stable peptide inhibitor of syntenin, KSL-128114, which binds the PDZ1 domain of syntenin with nanomolar affinity.  https://www.selleckchem.com/products/taurochenodeoxycholic-acid.html  KSL-128114 is resistant toward degradation in human plasma and mouse hepatic microsomes and displays a global PDZ domain selectivity for syntenin. An X-ray crystal structure reveals that KSL-128114 interacts with syntenin PDZ1 in an extended noncanonical binding mode. Treatment with KSL-128114 shows an inhibitory effect on primary GBM cell viability and significantly extends survival time in a patient-derived xenograft mouse model. Thus, KSL-128114 is a novel promising candidate with therapeutic potential for highly aggressive tumors, such as GBM.In this work, a tetradentate N,O-hybrid 2,9-bis(diphenylphosphine oxide)-1,10-phenanthroline (Ph2-BPPhen) ligand was studied for the coextraction of trivalent f-block elements from nitric acid media. The extraction as well as the complexation behaviors of Ph2-BPPhen with f-block elements were thoroughly investigated using 31P and 1H NMR spectrometry, UV-vis spectrophotometry, single crystal X-ray diffraction, and density functional theoretical (DFT) calculation. Ph2-BPPhen exhibits remarkably extraction ability for both Am(III) and Eu(III) and more than 99.5% of Am(III) and Eu(III) were extracted from 1.0 M HNO3 solution. Slope analysis suggests that both 21 and 11 ligand/metal complexes were probably formed during the extraction. The 11 and 21 Ln(III) complexes with Ph2-BPPhen were also identified in CH3OH solution by NMR spectrometry, and the stability constants were determined via UV-vis spectrophotometry. Structures of the 11 Eu(Ph2-BPPhen)(NO3)3 and Am(Ph2-BPPhen)(NO3)3 complexes were further elucidated by single X-ray crystallography and DFT calculations. The higher extractability of Ph2-BPPhen toward trivalent Am(III) and Eu(III) compared with the previously reported phenanthroline-derived amide and phosphonate ligands was attributed to the stronger affinity of the -P═O(R)2 group to metal ions. The results from this work indicate that the N,O-hybrid 1,10-phenanthroline derived phosphine oxide ligand can serve as a new and promising candidate for coextraction of trivalent f-block elements in the treatment of nuclear waste.We report a palladium-catalyzed, ligand promoted, C-H fluorine-containing olefination of anilides with 4-bromo-3,3,4,4-tetrafluorobutene as the fluorinated reagent, which has a potential transformation into other compounds due to its -CF2CF2Br functional group. -CF2CF2H was obtained by using the mild reducing agent sodium borohydride. Bioactive compounds such as aminoglutethimide derivative and propham were well-tolerated in this reaction, both of which highlight the synthetic importance of this method.The specific recognition of AT-rich DNA sequences opens up the door to promising diagnostic and/or therapeutic strategies against gene-related diseases. Here, we demonstrate that amphiphilic PtII complexes of the type [Pt(dmba)(N∧N)]NO3 (dmba = N,N-dimethylbenzylamine-κN, κC; N∧N = dpq (3), dppz (4), and dppn (5)) recognize AT-rich oligonucleotides over other types of DNA, RNA, and model proteins. The crystal structure of 4 shows the presence of significant π-stacking interactions and a distorted coordination sphere of the d8 PtII atom. Complex 5, containing the largest π-conjugated ligand, forms supramolecular assemblies at high concentrations under aqueous environment. However, its aggregation can be promoted in the presence of DNA at concentrations as low as 10 μM in a process that "turns on" its excimer emission around 600 nm. Viscometry, gel electrophoresis, and theoretical calculations demonstrate that 5 binds to minor groove when self-assembled, while the monomers of 3 and 4 intercalate into the DNA. The complexes also inhibit cancer cell growth with low-micromolar IC50 values in 2D tissue culture and suppress tumor growth in 3D tumor spheroids with a multicellular resistance (MCR) index comparable to that of cisplatin.Characterizing the surfaces of colloidal semiconductor nanocrystals (NCs) remains a key challenge for understanding and controlling their physical properties and chemical behavior. For this reason, the development of new methods to study NC surfaces is of great interest. In this paper, we report the use of (Me3Si)2Fe(CO)4 and Et3SiCo(CO)4 as reagents for functionalizing CdSe NC surfaces with organometallic metal tetracarbonyl fragments. This method avoids NC surface reduction and can achieve high metal carbonyl surface densities. Surface reduction or oxidation, as well as changes to the surface stoichiometry, was shown to shift the metal carbonyl CO stretching frequencies, making these surface-bound metal carbonyl fragments useful spectroscopic reporters of NC surface chemistry. Normal coordinate analysis was used on the metal carbonyl CO stretching vibrations to study the electronic influence of the CdSe NCs on the transition-metal center of the metal carbonyl fragments. These studies demonstrate the utility of organometallic spectroscopic reporters in studying the surface chemistry of NCs.Cholestatic liver injury is frequently associated with drug inhibition of bile salt transporters, such as the bile salt export pump (BSEP). Reliable in silico models to predict BSEP inhibition directly from chemical structures would significantly reduce costs during drug discovery and could help avoid injury to patients. We report our development of classification and regression models for BSEP inhibition with substantially improved performance over previously published models. We assessed the performance effects of different methods of chemical featurization, data set partitioning, and class labeling and identified the methods producing models that generalized best to novel chemical entities.