RUFY1 binds Arl8b and mediates endosome-to-TGN CI-M6PR retrieval for cargo sorting to lysosomes.

Arl8b, an Arf-like GTP-binding protein, regulates cargo trafficking and positioning of lysosomes. However, it is unknown whether Arl8b regulates lysosomal cargo sorting. Here, we report that Arl8b binds to the Rab4 and Rab14 interaction partner, RUN and FYVE domain-containing protein (RUFY) 1, a known regulator of cargo sorting from recycling endosomes. Arl8b determines RUFY1 endosomal localization through regulating its interaction with Rab14. RUFY1 depletion led to a delay in CI-M6PR retrieval from endosomes to the TGN, resulting in impaired delivery of newly synthesized hydrolases to lysosomes. We identified the dynein-dynactin complex as an RUFY1 interaction partner, and similar to a subset of activating dynein adaptors, the coiled-coil region of RUFY1 was required for interaction with dynein and the ability to mediate dynein-dependent organelle clustering. Our findings suggest that Arl8b and RUFY1 play a novel role on recycling endosomes, from where this machinery regulates endosomes to TGN retrieval of CI-M6PR and, consequently, lysosomal cargo sorting.

Reversible Stimuli-Dependent Aggregation-Induced Emission from a "Nonfluorescent" Amphiphilic PVDF Graft Copolymer.

A poly(vinylidine fluoride) graft random copolymer of t-butyl aminoethyl methacrylate (tBAEMA) and oligo(ethylene glycol) methyl ether methacrylate (OEGMA, Mn = 300) [PVDF-g-P(tBAEMA-ran-OEGMA), PVBO] is synthesized by atom transfer radical polymerization (ATRP), and PVBO is fractionated to get a highly water-soluble fraction (PVBO-1) showing a reversible on/off fluorescence behavior with gradual increase and decrease in pH, respectively, achieving a maximum quantum yield of 0.18 at pH = 12. PVBO-1 dissolved in water shows large multimicellar aggregates (MMcA), but at pH 12, crumbling of larger aggregates to much smaller micelles occurs, forming nonconjugated polymer dots (NCPDs), as supported by transmission electron microscopy and dynamic light scattering study. The reversible fluorescence on/off behavior also occurs with the decrease and increase of temperature. Theoretical study indicates that, at high pH, most of the amino groups become neutral and exhibit a strong tendency to form aggregates from crowding of a large number of carbonyl and amine groups, minimizing the HOMO-LUMO gap, showing an absorption peak at the visible region, and generating aggregation-induced emission.

Fluorescence in "Nonfluorescent" Polymers.

Recently, a great deal of research has been started on generating fairly strong photoluminescence from organic molecules without having any conjugated π-system or fluorophore. Discrete chromophores or auxochromophores termed as "subfluorophores" may undergo "space conjugation" via co-operative intramolecular conformation followed by intermolecular aggregation to generate fluorescence or sometimes phosphorescence emission. Polymeric materials are important in this regard as nonconjugated polymers self-assemble/aggregate in a moderately concentrated solution and also in the solid state, producing membranes, films, and so forth with good physical and mechanical properties. Therefore, promoting fluorescence in these commodity polymers is very much useful for sensing, organic light emitting diodes (OLED), and biological applications. In this perspective, we have discussed the aggregation-induced emission from four different types of architectures, for example, (i) dendrimers or hyperbranched polymers, (ii) entrapped polymeric micellar self-assembly, (iii) cluster formation, and (iv) stretching-induced aggregation, begining with the genesis of fluorescence from aggregation of propeller-shaped small organic molecules. The mechanism of induced fluorescence of polymers with subfluorophoric groups is also discussed from the theoretical calculations of the energy bands in the aggregated state. Also, an attempt has been made to highlight some useful applications in the sensing of surfactants, bacteria, cell imaging, drug delivery, gene delivery, OLED, and so forth.

Zwitterionic Poly(vinylidene fluoride) Graft Copolymer with Unexpected Fluorescence Property.

Recently, there has been a growth of research on the nonconjugated polymer exhibiting fluorescence property and it would be exciting if fluorescence property is developed in zwitterionic polymers because of their good water solubility. Poly(vinylidene fluoride) (PVDF) grafted with poly(dimethyl amino ethyl methacrylate) (PDMAEMA) is fractionated and a highly water-soluble fraction (PVDM-1) is quaternized with 1,3-propane sultone, producing a zwitterionic polymer, PVDF- g-PDMAEMA-sultone (PVDMS). PVDM-1 shows the fluorescence property with very low quantum yield (1%) in water, but on quaternization, fluorescence quantum yield increases to 8%. Transmission electron microscopy results indicate that the PVDM-1 cast from water has vesicular morphology, whereas PVDMS exhibits aggregated vesicular morphology. The 1H NMR spectra indicate the presence of 72 mol % DMAEMA in PVDM-1 wherein 66% of -NMe2 groups is quaternized upon postpolymerization modification. PVDM-1 exhibits absorption peaks at 210, 276, and 457 nm with a hump at 430 nm, whereas PVDMS exhibits two absorption peaks at 203 and 297 nm. PVDM-1 exhibits a broad emission peak at 534 nm, whereas PVDMS exhibits a sharp emission peak at 438 nm. An attempt has been made from density functional theory calculations to shed light on the origin of fluorescence in both PVDM-1 and in the zwitterionic PVDMS. The excitonic decay occurs from the lowest unoccupied molecular orbital (LUMO) of carbonyl group to the highest occupied molecular orbital (HOMO) of tertiary amine group for PVDM-1, whereas in PVDMS, the excitonic transition occurs from the LUMO situated over the quaternary ammonium group to the HOMO located on the electron-rich terminal sulfonate group.

Light-Induced Conformational Change of Uracil-Anchored Polythiophene-Regulating Thermo-Responsiveness.

Tuning the electronic structure of a π-conjugated polymer from the responsive side chains is generally done to get desired optoelectronic properties, and it would be very fruitful when light is used as an exciting tool that can also affect the backbone chain conformation. For this purpose, polythiophene- g-poly-[ N-(6-methyluracilyl)- N, N-dimethylamino chloride]ethyl methacrylate (PTDU) is synthesized. On exposure to diffuse sunlight, the uracil moieties of the grafted chains cause the absorption maximum of PTDU solution to show gradual blue shift of 87 nm and a gradual blue shift of 46 nm in the emission maximum, quenching its fluorescence with time. These effects occur specifically at the absorption range of polythiophene (PT) chromophore on direct exposure of light of different wavelengths, and the optimum wavelength is found to be 420 nm. Impedance study suggests a decrease in charge transfer resistance upon exposure because of conformational change of PTDU. Theoretical study indicates that on exposure to visible light, uracil moieties move toward the backbone to facilitate photoinduced electron transfer between the PT and the uracil, attributing to the variation in optoelectronic properties. Morphological and light-scattering studies exhibit a decrease in particle size because of coiling of the PT backbone and squeezing of the grafted chain on light exposure. The transparent orange-colored PTDU solution becomes hazy with a hike in emission intensity on addition of sodium halides and becomes reversibly transparent or hazy on heating or cooling. The screening of cationic centers of PTDU by varying halide anion concentration tunes the phase transition temperature. Thus, the light-induced variation in the backbone conformation is responsible for tuning the optoelectronic properties and regulates the thermos-responsiveness of the PTDU solution in the presence of halide ions.

Influence of Hofmeister I- on Tuning Optoelectronic Properties of Ampholytic Polythiophene by Varying pH and Conjugating with RNA.

A significant tuning of optoelectronic properties of polythiophene (PT) chains due to Hofmeister iodide (I-) ion is demonstrated in ampholytic polythiophene [polythiophene-g-poly{(N,N,N-trimethylamino iodide)ethyl methacrylate-co-methacrylic acid}, APT] at different pHs. In acidic medium, the absorption and emission signals of PT chromophore exhibit appreciable blue shift in the presence of I- as counteranion only. The cooperative effect of undissociated -COOH and quaternary ammonium groups immobilize I- near the apolar PT chain causing threading of grafted chains and hence twisting of the backbone attributing to the blue shift. As medium pH is increased, dethreading of the PT backbone occurs due to ionization of -COOH group, releasing quencher iodide ions from the vicinity of the PT chains resulting in a red shift in absorption and a sharp hike in fluorescence intensity (390 times) for an increase of excitons lifetime. With an increase of pH, morphology changes from a multivesicular aggregate with vacuoles to smaller size vesicles and finally to nanofibrillar network structure. Dethreading is also found when APT interacts with RNA showing a significant hike of fluorescence (22 times) for displacing iodide ions forming a nanofibrillar network morphology. Threading and dethreading also affect the resistance, capacitance, and Warburg impedance values of APT. Molecular dynamics simulation of a model APT chain in a water box supports the threading at lower pH where the iodide ions pose nearer to the PT chain than that at higher pH causing dethreading. So the influence of Hofmeister I- ion is established for tuning the optoelectronic properties of a novel PT based polyampholyte by changing pH or by conjugating with RNA.

Surfactant-Triggered Fluorescence Turn "on/off" Behavior of a Polythiophene-graft-Polyampholyte.

Polythiophene-graft-polyampholyte (PTP) is synthesized using N,N-dimethylaminoethyl methacrylate and tert-butyl methacrylate monomers by grafting from polythiophene backbone, followed by hydrolysis. The resulting polymer exhibits aqueous solubility via formation of small-sized miceller aggregates with hydrophobic polythiophene at the center and radiating polyionic side chains (cationic or anionic depending on the pH of the medium) at the outer periphery. The critical micelle concentration of PTP in acidic solution (0.025 mg/mL, pH = 2.7) is determined from fluorescence spectroscopy. PTP exhibits reversible fluorescence on and off response in both acidic and basic medium with the sequential addition of differently charged ionic surfactants, repeatedly. The fluorescence intensity of PTP at pH 2.7 increases with the addition of an anionic surfactant, sodium dodecyl benzenesulfonate (SDBS), due to the self-aggregation forming compound micelles. The fluorescence intensity of these solutions again decreases on addition of a cationic surfactant, cetyltrimethylammonium bromide (CTAB), because of assembling of SDBS with CTAB, thus deassembling the PTP-SDBS aggregates. At pH 9.2, these turn on and turn off responses are also shown by PTP with the sequential addition of cationic surfactant (CTAB) and anionic surfactant (SDBS), respectively. This result shows that PTP has potential for surfactant-induced reversible fluorescence turn on and off using ionic surfactant (SDBS and CTAB) through self-assembling and deassembling of the ionic aggregates. The reversible aggregation and disaggregation process of PTP with the surfactants at both acidic and basic pH is supported from dynamic light scattering and Fourier transform infrared spectroscopy. The morphology of the above systems studied by transmission and scanning electron microscopy also supports the above aggregation and disaggregation process.

Phase Behavior of Poly(vinylidene fluoride)-graft-poly(diethylene glycol methyl ether methacrylate) in Alcohol-Water System: Coexistence of LCST and UCST.

A thermoresponsive polymer poly(diethylene glycol methyl ether methacrylate) (PMeO2MA) is grafted from poly(vinylidene fluoride) (PVDF) backbone by using a combined ATRC and ATRP technique with a high conversion (69%) of the monomer to produce the graft copolymer (PD). It is highly soluble polymer and its solution property is studied by varying polarity in pure solvents (water, methanol, isopropanol) and also in mixed solvents (water-methanol and water-isopropanol) by measuring the hydrodynamic size (Z-average) of the particles by dynamic light scattering (DLS). The variation of Z-average size with temperature of the PD solution (0.2%, w/v) indicates a lower critical solution temperature (LCST)-type phase transition (T(PL)) in aqueous medium, an upper critical solution temperature (UCST)-type phase transition (T(PU)) in isopropanol medium, and no such phase transition for methanol solution. In the mixed solvent (water + isopropanol) at 0-20% (v/v) isopropanol the TPL increases, whereas the T(PU) decreases at 92-100% with isopropanol content. For the mixture 20-90% isopropanol, PD particles having larger sizes (400-750 nm) exhibit neither any break in Z-average size-temperature plot nor any cloudiness, indicating their dispersed swelled state in the medium. In the methanol + water mixture with methanol content of 0-30%, T(PL) increases, and at 40-60% both UCST- and LCST-type phase separations occur simultaneously, but at 70-90% methanol the swelled state of the particles (size 250-375 nm) is noticed. For 50 vol % methanol by varying polymer concentration (0.07-0.2% w/v) we have drawn a quasibinary phase diagram that indicates an approximate inverted hourglass phase diagram where a swelled state exists between two single phase boundary produced from LCST- and UCST-type phase transitions. An attempt is made to understand the phase separation process by temperature-dependent (1)H NMR spectroscopy along with transmission electron microscopy.

Light induced E-Z isomerization in a multi-responsive organogel: elucidation from (1)H NMR spectroscopy.

A multiresponsive organogel of (E)-N'-(anthracene-10-ylmethylene)-3,4,5-tris(dodecyloxy)benzohydrazide (I) showed a decrease of fluorescence intensity, decrease in mechanical strength and a change in gel morphology on irradiation with a wavelength of 365 nm. This is attributed to the E-Z isomerization across the C=N bond of I as evidenced from (1)H NMR spectroscopy.

Fate of Free Fat Dermis Graft in TMJ Interpositional Gap Arthroplasty: A Long Term MRI Study.

INTRODUCTION: Free fat dermis graft is a good interpositional material for TMJ gap arthroplasty. Analysing the fate of the graft by magnetic resonance imaging (MRI) images helps in excellent visualization of both bony and soft tissue anatomy of the operated TMJ joint as well as in assessing the changes in dermis graft which was previously placed. PURPOSE OF THIS STUDY: To investigate the radiological fate of the dermis-fat graft within the TMJ using MRI. MATERIALS AND METHODS: Five joints of five patients who had dermis-fat grafts placed in their TMJ following gap arthroplasty were recruited for this study. Each patient had undergone TMJ gap arthroplasty with immediate dermis-fat graft placement. All the patients are then subjected to MRI. RESULTS: Fat graft was identified in close proximity to the mandibular condyle in all cases, with only three joints demonstrating fat covering the entire articular surface of the mandibular condyle. In the remaining joints the interpositional material found in the MRI defined joint space with mainly grey appearance, suggesting tissue change to other than fat, i.e. scar or granulation tissue. CONCLUSION: When free fat dermis graft is placed as interpositional material the graft occupied the entire TM joint and prevented it from recurrent ankylosis. The graft placed aids in normal functioning of the temperomandibular joint without any complications.

Absence of QTc prolongation in a thorough QT study with subcutaneous liraglutide, a once-daily human GLP-1 analog for treatment of type 2 diabetes.

The objective of this study was to establish effects of liraglutide on the QTc interval. In this randomized, placebo-controlled, double-blind crossover study, 51 healthy participants were administered placebo, 0.6, 1.2, and 1.8 mg liraglutide once daily for 7 days each. Electrocardiograms were recorded periodically over 24 hours at the end of placebo and highest dosing periods. Four different models for QT correction were used: QTci, as the primary endpoint, and QTciL, QTcF, and QTcB as secondary endpoints. The upper bound of the 1-sided 95% confidence interval for time-matched, baseline-corrected, placebo-subtracted QTc intervals was <10 ms for all 4 correction methods. Moxifloxacin (400 mg) increased QTc intervals by 10.6 to 12.3 ms at 2 hours. There was no concentration-exposure dependency on QTc interval changes by liraglutide and no QTc thresholds above 500 ms or QTc increases >60 ms. The authors conclude that liraglutide caused no clinically relevant increases in the QTc interval.