DNA-templated assembly of droplet-derived PEG microtissues

Patterning multiple cell types is a critical step for engineering functional tissues, but few methods provide three-dimensional positioning at the cellular length scale. Here, we present a "bottom-up" approach for fabricating multicellular tissue constructs that utilizes DNA-templated assembly of 3D cell-laden hydrogel microtissues. A flow focusing-generated emulsion of photopolymerizable prepolymer is used to produce 100 μm monodisperse microtissues at a rate of 100 Hz (10(5) h(-1)). Multiple cell types, including suspension and adherently cultured cells, can be encapsulated into the microtissues with high viability (~97%). We then use a DNA coding scheme to self-assemble microtissues "bottom-up" from a template that is defined using "top-down" techniques. The microtissues are derivatized with single-stranded DNA using a biotin-streptavidin linkage to the polymer network, and are assembled by sequence-specific hybridization onto spotted DNA microarrays. Using orthogonal DNA codes, we achieve multiplexed patterning of multiple microtissue types with high binding efficiency and >90% patterning specificity. Finally, we demonstrate the ability to organize multicomponent constructs composed of epithelial and mesenchymal microtissues while preserving each cell type in a 3D microenvironment. The combination of high throughput microtissue generation with scalable surface-templated assembly offers the potential to dissect mechanisms of cell-cell interaction in three dimensions in healthy and diseased states, as well as provides a framework for templated assembly of larger structures for implantation.     

Investigating the role of c-Jun N-terminal kinases in the proliferation of Werner syndrome fibroblasts using diaminopyridine inhibitors

ABSTRACT: Fibroblasts derived from the progeroid Werner syndrome show reduced replicative lifespan and a "stressed" morphology, both alleviated using the MAP kinase inhibitor SB203580. However, interpretation of these data is problematical because although SB203580 has the stress-activated kinases p38 and JNK1/2 as its preferred targets, it does show relatively low overall kinase selectivity. Several lines of data support a role for both p38 and JNK1/2 activation in the control of cellular proliferation and also the pathology of diseases of ageing, including type II diabetes, diseases to which Werner Syndrome individuals are prone, thus making the use of JNK inhibitors attractive as possible therapeutics. We have thus tested the effects of the widely used JNK inhibitor SP600125 on the proliferation and morphology of WS cells. In addition we synthesised and tested two recently described aminopyridine based inhibitors. SP600125 treatment resulted in the cessation of proliferation of WS cells and resulted in a senescent-like cellular phenotype that does not appear to be related to the inhibition of JNK1/2. In contrast, use of the more selective aminopyridine CMPD 6o at concentrations that fully inhibit JNK1/2 had a positive effect on cellular proliferation of immortalised WS cells, but no effect on the replicative lifespan of primary WS fibroblasts. In addition, CMPD 6o corrected the stressed WS cellular morphology. The aminopyridine CMPD 6r, however, had little effect on WS cells. CMDP 6o was also found to be a weak inhibitor of MK2, which may partially explain its effects on WS cells, since MK2 is known to be involved in regulating cellular morphology via HSP27 phosphorylation, and is thought to play a role in cell cycle arrest. These data suggest that total JNK1/2 activity does not play a substantial role in the proliferation control in WS cells.     

Automated parallel anionic polymerizations: Enhancing the possibilities of a widely used technique in polymer synthesis

Anionic polymerization techniques have been implemented successfully in a commercial automated synthesizer. The main problems for a successful adaptation of the experimental technique in the automated synthesizer are addressed, as well as some simple potential applications, such as the anionic polymerization of styrene, isoprene, and methyl methacrylate. The obtained results were reproducible and in concordance with literature knowledge. The apparent rate constant of the anionic polymerization of styrene in cyclohexane initiated by sec‐butyllithium could be determined at two different concentrations of the monomer and initiator in a temperature range of 10–60 °C. All the synthesis and characterization experiments of the polymers were performed within a short time period. Moreover, the syntheses of poly(styrene‐b‐isoprene) and poly(styrene‐b‐methyl methacrylate) block copolymers were also successfully carried out within the automated synthesizer. © 2005 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 43: 4151–4160, 2005     

The powers and pitfalls of algorithmic knowledge: a case study

This study examines one child's use of computational procedures over a period of 3 years in an urban elementary school where teachers were using a standards-based curriculum. From a sociocultural perspective, the use of standard algorithms to solve mathematical problems is viewed as a cultural tool that both enables and constrains particular practices. As this student appropriated and mastered procedures for addition, subtraction, multiplication and division, she could solve problems that involved fairly straightforward computations or where she could easily model the action to determine an appropriate computation. At the same time, her use of these algorithms, along with other readily available tools, such as her fingers or multiplication tables, constrained her ability to reflect on the tens-structure of the number system, an effect that had serious consequences for her overall mathematical achievement. The results of this study suggest that even when not directly introduced, algorithms have such strong currency that they can mediate more reform-oriented instruction.     

Thiophene systems. 11. The synthesis of novel thieno[4,3,2-de] tricyclic ring systems

The synthesis of thieno[4,3,2-de] tricyclic compounds is described. The N-1 alkylation of I produced the alkanoic ester precursors. After hydrolysis, the corresponding carboxylic acids were cyclized to the title compounds II . This cyclization step was accomplished with 1:10 phosphorus pentoxide-methanesulfonic acid. The ketones II were further modified to introduce additional functionality onto this novel tricyclic ring system.     

Liquid surface and liquid/liquid interface energies of binary subregular alloys and wetting transitions

Energetics and chemistry of liquid surfaces and liquid/liquid interfaces of binary A-B alloys are calculated using a subregular solution model. In this model, two macroscopic energetic parameters are used to produce an asymmetric miscibility gap. They are related to two microscopic parameters which describe the interaction energy between two atoms as a function of the composition of the first coordination shell of each atom. The impact of the asymmetry of the A-B interactions on the surface and interfacial energies and adsorption are analyzed by comparing the results obtained with this subregular model to those calculated for a regular solution. The role of the asymmetry on the prewetting and wetting transitions are also discussed. Calculations performed in the Co-Cu system are in good agreement with experimental data of surface energy.     

Practical asymmetric synthesis of alpha-branched 2-piperazinylbenzylamines by 1,2-additions of organometallic reagents to N-tert-butanesulfinyl imines

[reaction: see text] 2-[4-(tert-Butoxycarbonyl)piperazinyl]benzylidene-tert-butanesulfinamides underwent nucleophilic 1,2-addition with different organometallic reagents to give highly diastereomerically enriched adducts. X-ray crystallography of the resulting alpha-branched N-Boc-2-piperazinylbenzyl-tert-butanesulfinamides confirms different mechanisms depending on the organometallic reagent used. Differential deprotection of the N-Boc and the tert-butanesulfinamides was investigated, and the dehydration byproducts have been identified and characterized. To avoid the formation of byproducts in the acidic deprotection step, the N-tert-butanesulfinamide group was converted to the corresponding N-tert-butanesulfonamide (Bus), which allowed for clean orthogonal deprotection. The efficient synthesis and deprotection of the N-Boc-2-piperazinylbenzyl-tert-butanesulfinamides herein described constitutes an attractive method for extensive structure-activity studies in the search for novel ligands of the human melanocortin 4 receptor.