Calculations of Monomer Conversion and Radical Concentration in Reversible Addition‐Fragmentation Chain Transfer Radical Polymerization

Simple expressions are derived for the development of monomer conversion, as well as propagating radical, adduct radical, dormant chain, and dead chain concentrations in reverse addition‐fragmentation transfer polymerization (RAFT). The relations for the profiles of propagating radical concentration and conversion versus time are derived and depend on group parameters of rate constants and chemical recipe. The analytical equations are verified against numerical solutions of the mass‐balance differential equations. This derivation involves the steady‐state hypothesis for radical and RAFT agent concentrations. The errors introduced by these assumptions are negligible when the fragmentation rate constant, k_f, is higher than 10 s⁻¹ or when the cross‐termination rate constant, k_ct, is higher than 10⁵ L · mol⁻¹ s⁻¹.

Calculated concentration profiles (points: numerical, lines: analytical) of propagating radical R, adduct radical A, dormant T, and dead D (= P + P′) chains.     

Side-chain liquid crystal copolymers containing nonmesogenic units: Dependence of the thermal behavior upon composition

The reactivity ratios have been determined for a mesogenic/nonmesogenic comonomer system, namely 5-[4-(4′-methoxyphenyl)phenoxy]pentyl methacrylate/methyl methacrylate. The reactivity ratios were found to be equal and approximately unity. The copolymerization is, therefore, azeotropic and the resulting copolymers possess a random distribution sequence of the two monomers. The thermal properties of the copolymers were evaluated using differential scanning calorimetry and polarized light microscopy. Copolymers containing 0.56 or greater mol fraction of the mesogenic side-chain exhibited liquid crystallinity, specifically smectic behavior. The glass transition temperatures exhibited a negative deviation from linear behavior on varying the composition. By contrast, the clearing temperatures decrease in essentially a linear fashion as the mol fraction of the nonmesogenic unit is increased. The behavior of these copolymers is compared with a range of materials from the literature, revealing that on increasing backbone flexibility a greater mol fraction of nonmesogenic units can be incorporated into the copolymer structure while retaining liquid crystallinity. This behavior is rationalized in terms of a microphase separated smectic phase. © 1996 John Wiley & Sons, Inc.     

Nucleobase participation in ribozyme catalysis

We constructed a modified form of the VS ribozyme containing an imidazole ring in place of adenine at position 756. The novel ribozyme is active in both cleavage and ligation reactions. The reaction is efficient, although relatively slow. The results are consistent with a role for nucleobase catalysis in the catalytic mechanism of this ribozyme.     

Systematic investigation of Saccharomyces cerevisiae enzymes catalyzing carbonyl reductions

Eighteen key reductases from baker's yeast (Saccharomyces cerevisiae) have been overproduced in Escherichia coli as glutathione S-transferase fusion proteins. A representative set of alpha- and beta-keto esters was tested as substrates (11 total) for each purified fusion protein. The stereoselectivities of beta-keto ester reductions depended both on the identity of the enzyme and the substrate structure, and some reductases yielded both L- and D-alcohols with high stereoselectivities. While alpha-keto esters were generally reduced with lower enantioselectivities, it was possible in all but one case to identify pairs of yeast reductases that delivered both alcohol antipodes in optically pure form. Taken together, the results demonstrate not only that individual yeast reductases can be used to supply important chiral building blocks, but that GST-fusion proteins allow rapid identification of synthetically useful biocatalysts (along with their corresponding genes).     

Assessment of MIST Alert,a commercial qualitative assay for detection of paralytic shellfish poisoning toxins in bivalve molluscs

A recently developed commercial rapid test kit (MIST Alert) was assessed for determination of the presence of paralytic shellfish poisoning (PSP) toxins in shellfish. Several commercially important shellfish species obtained from the UK shellfish toxin monitoring program, containing a range of total PSP toxicities as determined by the mouse bioassay (MBA), were tested. The kit detected toxin in all samples containing the European Community tolerance level of 80 microg saxitoxin (STX) equivalents/100 g shellfish flesh as determined by the MBA. With one exception, the kit detected toxin in all samples that contained >40 microg STX equivalents/100 g according to the MBA. Among samples in which the MBA did not detect toxin, the kit disagreed in 25% of the tests, although further analysis by liquid chromatography (LC) and MBA of some samples confirmed the presence of toxins. These results suggest that MIST Alert may be suitable as an initial screen for PSP toxins as part of routine monitoring programs, thereby greatly reducing the number of MBAs. Trials were also performed by nonscientific personnel to evaluate the ease of use and interpretation of results obtained by MIST Alert. The results indicated that the kits could be readily used and accurately interpreted by individuals with no technical or scientific background.     

Structural insights into the coordination and extraction of Pb(II) by disulfonamide ligands derived from o-phenylenediamine

The o-phenylenediamine-derived disulfonamide ligands 1 and 2 complex and efficiently extract Pb(II) from water into 1,2-dichloroethane via ion-exchange, in combination with 2,2'-bipyridine (97.5% and 95.0%, respectively, for 1:1 ligand-to-Pb ratios). The corresponding Pb(II)-sulfonamido binary complexes of ligands 1 and 2 (3 and 4, respectively), and ternary complexes with 2,2'-bipyridine (5 and 6, respectively), were isolated and characterized. (1)H NMR spectra of the organic phases after extraction show the formation of ternary Pb-sulfonamido-bipy complexes. X-ray characterization of 3, 4, and the ternary complex 5 consistently demonstrates four primary coordination sites and a stereochemically active lone pair on Pb. The X-ray structure of 3 shows a pseudo trigonal bipyramidal configuration on Pb, with the lone pair occupying one of the equatorial sites, and the formation of an unusual "hemidirected" coordination polymer via axial S=O-Pb coordination. The same axial S=O-Pb coordination pattern with two DMSO molecules is observed in the structure of 4.[2(CH(3))(2)SO)], thus rationalizing the high solubility of the binary complexes in strongly coordinating solvents. In contrast, the X-ray structure of the ternary complex 5 reveals a distorted four-coordinate configuration with only weak S=O-Pb coordination leading to dimer formation, thus explaining its higher solubility in weakly coordinating solvents. FT-IR spectroscopy confirms the X-ray data, since the ligand nu(S)(=)(O) stretching frequencies shift to lower values in the binary Pb(II)-sulfonamido complexes and are again altered upon formation of the ternary Pb(II)-sulfonamido-bipy complexes, as would be expected for 2,2'-bipy complexation and hindered S=O-Pb coordination.     

The Self‐Assembly of Anticancer Camptothecin–Dipeptide Nanotubes: A Minimalistic and High Drug Loading Approach to Increased Efficacy

20‐(S)‐Camptothecin (CPT)‐conjugated dipeptides are reported that preassemble into nanotubes with diameters ranging from 80–120 nm. These nanoassemblies maintain a high (～47 %) drug loading and exhibit greater drug stability (i.e., resistance to lactone hydrolysis), and consequently greater efficacy against several human cancer cells (HT‐29, A549, H460, and H23) in vitro compared with the clinically used prodrug irinotecan. A key and defining feature of this system is the use of the CPT‐conjugated dipeptide as both the drug and precursor to the nanostructured carrier, which simplifies the overall fabrication process.