Analytical and preparative separation of PEGylated lysozyme for the characterization of chromatography media

The effect of PEGylation on cation exchange chromatography was studied with poly(ethylene glycol) of different chain lengths (5 kDa, 10 kDa and 30 kDa) using lysozyme as a model system. A stable binding via reduction of a Schiff base was formed during random PEGylation on lysine residues with methoxy-PEG-aldehyde. A purification method for PEGylated proteins using cation exchange chromatography was developed, and different isoforms of mono-PEGylated lysozyme were isolated. TSKgel SP-5PW and Toyopearl GigaCap S-650M showed the best performance of all tested cation exchange resins, and the separation of PEGylated lysozyme could be also scaled up to semi-preparative level. Size-exclusion chromatography, SDS-PAGE and MALDI-TOF mass spectrometry were used for analysis. Separated mono-PEGylated lysozyme of different sizes was used to determine dynamic binding capacities (DBC) and selectivity of cation exchange chromatography resins. An optimization of binding conditions resulted in a more than 20-fold increase of DBC for Toyopearl GigaCap S-650M with 30 kDa mono-PEGylated lysozyme.     

Lanthanide versus Actinide Reactivity in the Formation of Sterically Crowded [(C5Me5)3MLn] Nitrile and Isocyanide Complexes

The limits of steric crowding in organometallic metallocene complexes have been examined by studying the synthesis of [(C₅Me₅)₃ML_n] complexes as a function of metal in which L=Me₃CCN, Me₃CNC, and Me₃SiCN. The bis(tert‐butyl nitrile) complexes [(C₅Me₅)₃Ln(NCCMe₃)₂] (Ln=La, 1 ; Ce, 2 ; Pr, 3 ) can be isolated with the largest lanthanide metal ions, La³⁺, Ce³⁺, and Pr³⁺. The Pr³⁺ ion also forms an isolable mono‐nitrile complex, [(C₅Me₅)₃Pr(NCCMe₃)] ( 4 ), whereas for Nd³⁺ only the mono‐adduct [(C₅Me₅)₃Nd(NCCMe₃)] ( 5 ) was observed. With smaller metal ions, Sm³⁺ and Y³⁺, insertion of Me₃CCN into the M? C(C₅Me₅) bond was observed to form the cyclopentadiene‐substituted ketimide complexes [(C₅Me₅)₂Ln{NC(C₅Me₅)(CMe₃)}(NCCMe₃)] (Ln=Sm, 6 ; Y, 7 ). With tert‐butyl isocyanide ligands, a bis‐isocyanide product can be isolated with lanthanum, [(C₅Me₅)₃La(CNCMe₃)₂] ( 8 ), and a mono‐isocyanide product with neodymium, [(C₅Me₅)₃Nd(CNCMe₃)] ( 9 ). Silicon–carbon bond cleavage was observed in reactions between [(C₅Me₅)₃Ln] complexes and trimethylsilyl cyanide, Me₃SiCN, to produce the trimeric cyanide complexes [{(C₅Me₅)₂Ln(μ‐CN)(NCSiMe₃)}₃] (Ln=La, 10 ; Pr, 11 ). With uranium, a mono‐nitrile reaction product, [(C₅Me₅)₃U(NCCMe₃)] ( 12 ), which is analogous to 5 , was obtained from the reaction between [(C₅Me₅)₃U] and Me₃CCN, but [(C₅Me₅)₃U] reacts with Me₃CNC through C? N bond cleavage to form a trimeric cyanide complex, [{(C₅Me₅)₂U(μ‐CN)(CNCMe₃)}₃] ( 13 ).     

A Disulfide Intercalator Toolbox for the Site‐Directed Modification of Polypeptides

A disulfide intercalator toolbox was developed for site‐specific attachment of a broad variety of functional groups to proteins or peptides under mild, physiological conditions. The peptide hormone somatostatin (SST) served as model compound for intercalation into the available disulfide functionalization schemes starting from the intercalator or the reactive SST precursor before or after bioconjugation. A tetrazole–SST derivative was obtained that undergoes photoinduced cycloaddition in mammalian cells, which was monitored by live‐cell imaging.     

Synthesis and NMR studies of (13)C-labeled vitamin D metabolites

Isotope-labeled drug molecules may be useful for probing by NMR spectroscopy the conformation of ligand associated with biological hosts such as membranes and proteins. Triple-labeled [7,9,19-(13)C(3)]-vitamin D(3) (56), its 25-hydroxylated and 1 alpha,25-dihydroxylated metabolites (58 and 68, respectively), and other labeled materials have been synthesized via coupling of [9-(13)C]-Grundmann's ketone 39 or its protected 25-hydroxy derivative 43 with labeled A ring enyne fragments 25 or 26. The labeled CD-ring fragment 39 was prepared by a sequence involving Grignard addition of [(13)C]-methylmagnesium iodide to Grundmann's enone 28, oxidative cleavage, functional group modifications leading to seco-iodide 38, and finally a kinetic enolate S(N)2 cycloalkylation. The C-7,19 double labeling of the A-ring enyne was achieved by the Corey-Fuchs/Wittig processes on keto aldehyde 11. By employing these labeled fragments in the Wilson-Mazur route, the C-7,9,19 triple-(13)C-labeled metabolites 56, 58, and 68 as well as other (13)C-labeled metabolites have been prepared. In an initial NMR investigation of one of the labeled metabolites prepared in this study, namely [7,9,19-(13)C(3)]-25-hydroxyvitamin D(3) (58), the three (13)C-labeled carbons of the otherwise water insoluble steroid could be clearly detected by (13)C NMR analysis at 0.1 mM in a mixture of CD(3)OD/D(2)O (60/40) or in aqueous dimethylcyclodextrin solution and at 2 mM in 20 mM sodium dodecyl sulfate (SDS) aqueous micellar solution. In the SDS micellar solution, a double half-filter NOESY experiment revealed that the distance between the H(19Z) and H(7) protons is significantly shorter than that of the corresponding distance calculated from the solid state (X-ray) structure of the free ligand. The NMR data in micelles reveals that 58 exists essentially completely in the alpha-conformer with the 3 beta-hydroxyl equatorially oriented, just as in the solid state. The shortened distance (H(19Z))-H(7)) in micellar solutions as compared to that in the solid state is most easily rationalized on the basis that the 5(10)-torsion angle in 58 is decreased in micellar solutions as compared to that in the solid state.     

Engyodontochones,Antibiotic Polyketides from the Marine Fungus Engyodontium album Strain LF069

Six new ( 2 , 4 – 8 ) and two known polyketides with a basic structure of an anthraquinone‐xanthone were isolated from mycelia and culture broth of the fungus Engyodontium album strain LF069. The structures and relative configurations of these compounds were established by spectroscopic means, and their absolute configurations were defined mainly by comparison of quantum chemical TDDFT calculated and experimental ECD spectra. Compounds 2 and 4 – 8 were given the trivial names engyodontochone A ( 2 ) and B–F ( 4 – 8 ). Compounds 5 – 8 represent the first example of a 23,28 seco‐beticolin carbon skeleton. The relative and absolute configurations of two known substances JBIR‐97/98 ( 1 ) and JBIR‐99 ( 3 ) were determined for the first time. All isolated compounds were subjected to bioactivity assays. Compounds 1 – 4 exhibited inhibitory activity against methicillin‐resistant Staphylococcus aureus (MRSA) that was 10‐fold stronger than chloramphenicol.     

Large-area organization of pNIPAM-coated nanostars as SERS platforms for polycyclic aromatic hydrocarbons sensing in gas phase

Here, a new surface enhanced Raman spectroscopy (SERS) platform suitable for gas phase sensing based on the extended organization of poly-N-isopropylacrylamide (pNIPAM)-coated nanostars over large areas is presented. This system yields high and homogeneous SERS intensities, and simultaneously traps organic chemical agents as pollutants from the gas phase. pNIPAM-coated gold nanostars were organized into parallel linear arrays. The optical properties of the fabricated substrates are investigated, and applicability for advanced sensing is demonstrated through the detection in the gas phase of pyrene traces, a well-known polyaromatic hydrocarbon.     

Capturing the antiaromatic (#6094) C68 carbon cage in the radio-frequency furnace

Although all fullerenes do not satisfy the classical aromaticity condition, as a result of their nonplanar nature, they experience effective stabilization due to extensive cyclic π-electron delocalization and exhibit pronounced "spherical aromaticity". This feature has raised the question of the opposite phenomenon, that is, the existence of antiaromatic carbon cages. Here the first experimental evidence of the existence of antiaromatic fullerenes is reported. The elusive (#6094)C(68) was effectively captured as C(68)Cl(8) by in situ chlorination in the gas phase during radio-frequency synthesis. The chlorinated cage was separated by means of multistage HPLC, and its connectivity unambiguously determined by single-crystal X-ray analysis. Halogen-stripped pristine (#6094)C(68) was monitored by mass spectrometry of the chlorinated C(68)Cl(8) cage. Quantum chemical calculations reveal the highly antiaromatic character of (#6094)C(68), in accordance with all geometric, energetic, and magnetic criteria of aromaticity. Chlorine addition leads to substantial stabilization of the cage owing to aromatization in the resulting C(68)Cl(8), which explains its high abundance in the primary fullerene soot. This work provides new insights into the process of fullerene formation and better understanding of aromaticity phenomena in general.