Visible-Light-Driven Photocatalytic H2 Production Using Composites of Co-Al Layered Double Hydroxides and Graphene Derivatives.

The direct conversion of solar energy into chemical energy represents an enormous challenge for current science. One of the commonly proposed photocatalytic systems is composed of a photosensitizer (PS) and a catalyst, together with a sacrificial electron donor (ED) when only the reduction of protons to H2 is addressed. Layered double hydroxides (LDH) have emerged as effective catalysts. Herein, two Co-Al LDH and their composites with graphene oxide (GO) or graphene quantum dots (GQD) have been prepared by coprecipitation and urea hydrolysis, which determined their structure and so their catalytic performance, giving H2 productions between 1409 and 8643 µmol g-1 using a ruthenium complex as PS and triethanolamine as ED at 450 nm. The influence of different factors, including the integration of both components, on their catalytic behavior, has been studied. The proper arrangement between the particles of both components seems to be the determining factor for achieving a synergistic interaction between LDH and GO or GQD. The novel Co-Al LDH composite with intercalated GQD achieved an outstanding catalytic efficiency (8643 µmol H2 g-1) and exhibited excellent reusability after 3 reaction cycles, thus representing an optimal integration between graphene materials and Co-Al LDH for visible light driven H2 photocatalytic production.

Basal and Stress-Induced Network Activity in the Adrenal Medulla In Vivo.

The adrenal medulla plays a critical role in mammalian homeostasis and the stress response. It is populated by clustered chromaffin cells that secrete epinephrine or norepinephrine along with peptides into the bloodstream affecting distant target organs. Despite been heavily studied, the central control of adrenal medulla and in-situ spatiotemporal responsiveness remains poorly understood. For this work, we continuously monitored the electrical activity of individual adrenomedullary chromaffin cells in the living anesthetized rat using multielectrode arrays. We measured the chromaffin cell activity under basal and physiological stress conditions and characterized the functional micro-architecture of the adrenal medulla. Under basal conditions, chromaffin cells fired action potentials with frequencies between ~0.2 and 4 Hz. Activity was almost completely driven by sympathetic inputs coming through the splanchnic nerve. Chromaffin cells were organized into independent local networks in which cells fired in a specific order, with latencies from hundreds of microseconds to a few milliseconds. Electrical stimulation of the splanchnic nerve evoked almost exactly the same spatiotemporal firing patterns that occurred spontaneously. Hypoglycemic stress, induced by insulin administration resulted in increased activity of a subset of the chromaffin cells. In contrast, respiratory arrest induced by lethal anesthesia resulted in an increase in the activity of virtually all chromaffin cells before cessation of all activity. These results suggest a stressor-specific activation of adrenomedullary chromaffin cell networks and revealed a surprisingly complex electrical organization that likely reflects the dynamic nature of the adrenal medulla's neuroendocrine output during basal conditions and during different types of physiological stress.

Copper-complexed dipyridyl-pyridazine functionalized periodic mesoporous organosilica as a heterogeneous catalyst for styrene epoxidation.

A new heterogeneous catalyst has been synthesized by immobilization of a copper complex on dipyridyl-pyridazine functionalized periodic mesoporous organosilica (dppz-vPMO). This ordered support was first prepared by a co-condensation reaction between vinyltriethoxysilane and 1,2-bis(trimethoxysilyl)ethane and further post-functionalized through a hetero Diels-Alder reaction with 3,6-di-2-pyridyl-1,2,4,5-tetrazine. Techniques such as XRD, N2 isotherms, TEM, 13C NMR, XPS and DRIFT, among others, were employed to characterize the surface functionalized materials. These results have proven the ordered mesostructure of the materials as well as the presence of novel nitrogen-chelating heterocyclic compounds on the pore surface after the post-modification process. Additionally, the successful anchoring of a copper complex on the dipyridyl-pyridazine (dppz) ligands has been confirmed. The resulting material was evaluated as a heterogeneous catalyst in the epoxidation of styrene using tert-butylhydroperoxide (TBHP) as an oxidant. Under the optimized reaction conditions, Cu@dppz-vPMO showed a high styrene conversion (86.0%) and a remarkable selectivity to styrene oxide (41.9%). Indeed, this catalyst provided excellent catalytic results in terms of stability, reaction rate, conversion and selectivity compared to other bipyridine-like copper catalysts.

Ru- and Ir-complex decorated periodic mesoporous organosilicas as sensitizers for artificial photosynthesis.

A versatile and facile strategy based on an inverse electron demand Diels-Alder reaction between 5-norbornen-2-yltriethoxysilane and a tetrazine derivative has been established for the synthesis of a new triethoxysilane precursor containing dipyridylpyridazine units. Such a precursor has been incorporated into the mesostructure of an ethylene-bridged periodic mesoporous organosilica (PMO) material through a one-pot synthesis via a co-condensation method. Upon attachment of Ru- and Ir-complexes to the pendant N-chelating heterocyclic ligands, the resulting decorated PMOs have acted as photosensitizers in artificial photosynthetic systems. The deposition of Pt on these PMOs has allowed us to obtain efficient photocatalytic materials for the hydrogen evolution reaction as a result of electron transfer from the light harvesting Ru- and Ir-complexes to the supported Pt nanoparticles through methyl viologen as an electron relay. They have exhibited total turnover number values of 573 and 846, respectively, under visible light irradiation. The role played by each component and the stability of the photocatalytic systems have been discussed. The present approach paves the way to the synthesis of different materials with coordination sites capable of forming surface complexes to be applied as sensitizers and catalysts.

A hands-free stool sampling system for monitoring intestinal health and disease.

Analysis of stool offers simple, non-invasive monitoring for many gastrointestinal (GI) diseases and access to the gut microbiome, however adherence to stool sampling protocols remains a major challenge because of the prevalent dislike of handling one's feces. We present a technology that enables individual stool specimen collection from toilet wastewater for fecal protein and molecular assay. Human stool specimens and a benchtop test platform integrated with a commercial toilet were used to demonstrate reliable specimen collection over a wide range of stool consistencies by solid/liquid separation followed by spray-erosion. The obtained fecal suspensions were used to perform occult blood tests for GI cancer screening and for microbiome 16S rRNA analysis. Using occult blood home test kits, we found overall 90% agreement with standard sampling, 96% sensitivity and 86% specificity. Microbiome analysis revealed no significant difference in within-sample species diversity compared to standard sampling and specimen cross-contamination was below the detection limit of the assay. Furthermore, we report on the use of an analogue turbidity sensor to assess in real time loose stools for tracking of diarrhea. Implementation of this technology in residential settings will improve the quality of GI healthcare by facilitating increased adherence to routine stool monitoring.

TLR4 activates the ß-catenin pathway to cause intestinal neoplasia.

Colonic bacteria have been implicated in the development of colon cancer. We have previously demonstrated that toll-like receptor 4 (TLR4), the receptor for bacterial lipopolysaccharide (LPS), is over-expressed in humans with colitis-associated cancer. Genetic epidemiologic data support a role for TLR4 in sporadic colorectal cancer (CRC) as well, with over-expression favoring more aggressive disease. The goal of our study was to determine whether TLR4 played a role as a tumor promoter in sporadic colon cancer. Using immunofluorescence directed to TLR4, we found that a third of sporadic human colorectal cancers over-express this marker. To mechanistically investigate this observation, we used a mouse model that over-expresses TLR4 in the intestinal epithelium (villin-TLR4 mice). We found that these transgenic mice had increased epithelial proliferation as measured by BrdU labeling, longer colonic crypts and an expansion of Lgr5+ crypt cells at baseline. In addition, villin-TLR4 mice developed spontaneous duodenal dysplasia with age, a feature that is not seen in any wild-type (WT) mice. To model human sporadic CRC, we administered the genotoxic agent azoxymethane (AOM) to villin-TLR4 and WT mice. We found that villin-TLR4 mice showed an increased number of colonic tumors compared to WT mice as well as increased ß-catenin activation in non-dysplastic areas. Biochemical studies in colonic epithelial cell lines revealed that TLR4 activates ß-catenin in a PI3K-dependent manner, increasing phosphorylation of ß-catenin(Ser552), a phenomenon associated with activation of the canonical Wnt pathway. Our results suggest that TLR4 can trigger a neoplastic program through activation of the Wnt/ß-catenin pathway. Our studies highlight a previously unexplored link between innate immune signaling and activation of oncogenic pathways, which may be targeted to prevent or treat CRC.

Falcipain inhibitors: optimization studies of the 2-pyrimidinecarbonitrile lead series.

Falcipain-2 and falcipain-3 are papain-family cysteine proteases of the malaria parasite Plasmodium falciparum that are responsible for host hemoglobin hydrolysis to provide amino acids for parasite protein synthesis. Different heteroarylnitrile derivatives were studied as potential falcipain inhibitors and therefore potential antiparasitic lead compounds, with the 5-substituted-2-cyanopyrimidine chemical class emerging as the most potent and promising lead series. Through a sequential lead optimization process considering the different positions present in the initial scaffold, nanomolar and subnanomolar inhibitors at falcipains 2 and 3 were identified, with activity against cultured parasites in the micromolar range. Introduction of protonable amines within lead molecules led to marked improvements of up to 1000 times in activity against cultured parasites without noteworthy alterations in other SAR tendencies. Optimized compounds presented enzymatic activities in the picomolar to low nanomolar range and antiparasitic activities in the low nanomolar range.

Activity of Basic Catalysts in the Meerwein-Ponndorf-Verley Reaction of Benzaldehyde with Ethanol.

The Meerwein-Ponndorf-Verley (MPV) reaction of benzaldehyde with ethanol in the liquid phase in the presence of basic catalysts consisting of magnesium oxide, calcium oxide, and mixed oxides obtained by calcination of layered double hydroxides, was studied. The catalysts were characterized using various techniques including X-ray diffraction and gas adsorption (viz nitrogen physisorption to determine textural properties and carbon dioxide chemisorption to elucidate surface basic properties). The catalyst consisting of calcium oxide, which was that possessing the highest density of basic sites, was found to be the most active in the process; the MPV reaction was accompanied by two other, competing reactions (viz aldol condensation and the Tishchenko cross-reaction). The MPV reaction of benzaldehyde with other alcohols was also examined, the highest conversion being obtained with secondary alcohols as hydrogen sources. Copyright 2001 Academic Press.

Antifungal sordarins. part 3: synthesis and structure-activity relationships of 2',3'-fused oxirane derivatives.

A number of new 2',3'-fused oxirane derivatives were synthesized for structure-activity relationship study. Many of these derivatives exhibit high potency against Candida spp. In addition, sordarin manno epoxide derivative 6 presents in vivo therapeutic effect in mice and is considered a promising antifungal lead within this series.

Antifungal sordarins. Synthesis and structure-activity relationships of 3'-O-substituted derivatives.

A number of novel 3'-O-acyl and alkyl sordarins were synthesised for structure-activity relationship studies. Many of these derivatives exhibit high activity against Candida albicans, Candida pseudotropicalis, Candida tropicalis and Cryptococcus neoformans.

Identification and activity of a series of azole-based compounds with lactate dehydrogenase-directed anti-malarial activity.

Plasmodium falciparum, the causative agent of malaria, relies extensively on glycolysis coupled with homolactic fermentation during its blood-borne stages for energy production. Selective inhibitors of the parasite lactate dehydrogenase (LDH), central to NAD(+) regeneration, therefore potentially provide a route to new antimalarial drugs directed against a novel molecular target. A series of heterocyclic, azole-based compounds are described that preferentially inhibit P. falciparum LDH at sub-micromolar concentrations, typically at concentrations about 100-fold lower than required for human lactate dehydrogenase inhibition. Crystal structures show these competitive inhibitors form a network of interactions with amino acids within the active site of the enzyme, stacking alongside the nicotinamide ring of the NAD(+) cofactor. These compounds display modest activity against parasitized erythrocytes, including parasite strains with known resistance to existing anti-malarials and against Plasmodium berghei in BALB/c mice. Initial toxicity data suggest the azole derivatives have generally low cytotoxicity, and preliminary pharmoco-kinetic data show favorable bioavailability and circulation times. These encouraging results suggest that further enhancement of these structures may yield candidates suitable for consideration as new therapeutics for the treatment of malaria. In combination these studies also provide strong support for the validity of targeting the Plasmodium glycolytic pathway and, in particular, LDH in the search for novel anti-malarials.

Rehidratación oral: experiencia en el manejo de pacientes con gastroenteritis aguda en la sala de emergencia Hospital Pediátrica Dr. Antonio Ortiz / Oral rehydration: experience in the handling of patients with acute gastroenteritis in the emergency room at the Dr. Antonio Ortiz Pediatric Hospital

Las soluciones orales de rehidratación que contienen de 50-90mEq/L de sodio han sido recomendadas recientemente para el manejo ambulatorio de niños con diarrea en los Estados Unidos. Nosotros llevamos a cabo un estudio randomizado comparando el uso de una solución comercial para rehidratación oral (Rehydralyte), que contiene 75 mEq/L de sodio con la forma usual de rehidratación con una solución endovenosa. Los pacientes tratados en la Sala de Emergencia del Hospital Pediótrico Universitario Dr. Antonio Ortíz, con diarrea aguda fueron escogidos al azar para administrárseles la solución de rehidratación oral (Rehydralyte) (Gripo A), pacientes controles (Grupo B) fueron hidratados con fluidos endovenosos de la manera usual, ie, Lactato de Ringer y luego una solución de 56 mEq/L de sodio. Todos los pacientes recibieron orientación sobre esta modalidad de tratamiento. Ambos grupos fueron comparados para ganancia en peso, parámetros metabólicos, duración de la diarrea, impacto de complicaciones asociadas al uso de solución endovenosa e impacto de costo. Cuando ambos grupos fueron comparados, no hubo diferencias en las medidas de la data clínica, de la rehidratación oral tanto en costo qomo en menos sufrimiento humano. Podemos concluir que en niños puertorriqueños la solución de rehidratación oral que contiene 75 mEq/L de sodio se puede usar con seguridad en el tratamiento de diarrea aguda en base ambulatoria