Possible tally stones at Mnajdra, Malta

This article describes the investigation of the orientations of the temple complexes of Malta and Gozo, which date from the period 3600-2500 B.C. It was accepted only those axes that were clearly axes of symmetry, and which were directed towards an entrance with a view of the terrain external to the temple. 15 such axes were identified, and it was found that the orientations of the axes were far from random. Indeed, with one exception, they faced in a southerly direction, between 125.5° and 2040 azimuth. The exception is Temple I at Mnajdra, Malta.peer-reviewe

Linking protein-protein interactions to the diversity of amyloid-like aggregates

Protein aggregation is often studied in the context of neurodegenerative diseases. Deposits of supramolecular aggregates, often appearing as ordered fibrils, are associated with the onset of devastating pathologies as Alzheimer´s and Parkinson´s diseases. Equally important is the impact that the formation of protein aggregates may have in the quality of a protein drug product. The presence of the so-called sub-visible particles (SVP) and visible particles in protein drug product is indeed considered one of the risk factors potentially inducing immune response in patients. Finally yet importantly, protein aggregates, and particularly amyloid fibrils, have unique structural, physico-chemical, mechanical and optical properties, making them appealing bio-inspired materials for several applications. Either one looks at protein aggregation in the context of diseases, drug development or biomaterials, understanding how protein-protein (PPIs) and protein-solvent interactions (PSI) determine aggregation kinetics and the morphology/structures of the final aggregates is a conditio sine qua non for unraveling the molecular mechanisms ruling the self-assembly reaction and for controlling it. In our group, we have reported the possibility for a large group of proteins under specific destabilizing conditions to form a variety of protein aggregates, being it not limited to the formation of amyloid fibrils (Figure 1) [1]. In line with the scope of the conference, I will present our unique approach based on advanced fluorescence microscopy, small angle X-ray scattering and spectroscopy and aimed at identifying the key PPIs and PSIs responsible for such variability in structures and morphologies [2-6]. We use surfactants, salts, alcohols in bulk and microfluidic setups to finely tune the interactions between proteins and, consequently, control the self-assembly process. Our results show that subtle changes in the PPIs and PSI do not only affect the kinetics, but they may also have a dramatic effect on the 3D arrangement, microscopic structures, mechanical properties and stability of the final self-assembled structures. Our findings provide a scenario in which a pool of highly heterogeneous structures can be generated as a result of interconnected aggregation pathways, being this aspect of key relevance especially for protein drug product development and optimization. Please click Additional Files below to see the full abstract

Sucrose modulates insulin amyloid-like fibril formation: effect on the aggregation mechanism and fibril morphology

Sucrose modifies the human insulin fibrillation pathways, affecting the fibril morphology.</p

Radiation Hardness and Defects Activity in PEA2PbBr4 Single Crystals

Metal halide perovskites (MHPs) are low-temperature processable hybrid semiconductor materials with exceptional performances that are revolutionizing the field of optoelectronic devices. Despite their great potential, commercial deployment is hindered by MHPs lack of stability and durability, mainly attributed to ions migration and chemical interactions with the device electrodes. To address these issues, 2D layered MHPs have been investigated as possible device interlayers or active material substitutes to reduce ion migration and improve stability. Here we consider the 2D perovskite PEA2PbBr4 that was recently discussed as very promising candidate for X-ray direct detection. While the increased resilience of PEA2PbBr4 detectors have already been reported, the physical mechanisms responsible for such improvement compared to the standard "3D" perovskites are not still fully understood. To unravel the charge transport process in PEA2PbBr4 crystals thought to underly the device better performance, we adapted an investigation technique previously used on highly resistive inorganic semiconductors, called photo induced current transient spectroscopy (PICTS). We demonstrate that PICTS can detect three distinct trap states (T1, T2, and T3) with different activation energies, and that the trap states evolution upon X-ray exposure can explain PEA2PbBr4 superior radiation tolerance and reduced aging effects. Overall, our results provide essential insights into the stability and electrical characteristics of 2D perovskites and their potential application as reliable and direct X-ray detectors

Early Stage Alpha-Synuclein Amyloid Fibrils are Reservoirs of Membrane-Binding Species

Abstract The presence of αSN fibrils indisputably associates with the development of synucleinopathies. However, while certain fibril morphologies have been linked to downstream pathological phenotypes, others appear less harmful, leading to the concept of fibril strains, originally described in relation to prion disease. Indeed, the presence of fibrils does not associate directly with neurotoxicity. Rather, it has been suggested that the toxic compounds are soluble amyloidogenic oligomers, potentially co-existing with fibrils. Here, combining synchrotron radiation circular dichroism, transmission electron microscopy and binding assays on native plasma membrane sheets, we reveal distinct biological and biophysical differences between initial and matured fibrils, transformed within the timespan of few days. Immature fibrils are reservoirs of membrane-binding species, which in response to even gentle experimental changes release into solution in a reversible manner. In contrast, mature fibrils, albeit macroscopically indistinguishable from their less mature counterparts, are structurally robust, shielding the solution from the membrane active soluble species. We thus show that particular biological activity resides transiently with the fibrillating sample, distinct for one, but not the other, spontaneously formed fibril polymorph. These results shed new light on the principles of fibril polymorphism with consequent impact on future design of assays and therapeutic development

Effect of cholesterol on the interaction between amphyphylic peptides and liposomes

With the rise of antibiotic resistance, antimicrobial peptides (AMPs) have been proposed as an alternative novel class of therapeutic agents. They are polycationic, with a net positive charge of more than +2, and they are characterized by amphipathic structures, with both a hydrophobic and a hydrophilic domain. These characteristics allow them to selectively bind to negatively charged lipids (largely present in bacteria, not in mammalian cells), via hydrophobic and electrostatic interactions. Moreover, mammalian cells are characterized by a high content of cholesterol. For this reason, here we present an experimental study on the effect of the presence of cholesterol on the capability of amphyphylic peptide Trasportant 10 (TP10) to interact with model membranes with selected composition. The study was performed by means of fluorescence spectroscopy and fluorescence confocal microscopy measurements also exploiting the advantages of phasor plot analysis of Fluorescence Lifetime Imaging (FLIM) measurements. Our results show that the presence of cholesterol inhibits TP-10 interaction with lipid vesicles, the extent of the observed effect being dependent on the cholesterol concentration in the membrane

Novel Combination of Sorafenib and Celecoxib Provides Synergistic Anti-Proliferative and Pro-Apoptotic Effects in Human Liver Cancer Cells

Molecular targeted therapy has shown promise as a treatment for advanced hepatocellular carcinoma (HCC). Sorafenib, a multikinase inhibitor, recently received FDA approval for the treatment of advanced HCC. However, although sorafenib is well tolerated, concern for its safety has been expressed. Celecoxib (Celebrex®) is a selective cyclooxygenase-2 (COX-2) inhibitor which exhibits antitumor effects in human HCC cells. The present study examined the interaction between celecoxib and sorafenib in two human liver tumor cell lines HepG2 and Huh7. Our data showed that each inhibitor alone reduced cell growth and the combination of celecoxib with sorafenib synergistically inhibited cell growth and increased apoptosis. To better understand the molecular mechanisms underlying the synergistic antitumor activity of the combination, we investigated the expression profile of the combination-treated liver cancer cell lines using microarray analysis. Combination treatment significantly altered expression levels of 1,986 and 2,483 transcripts in HepG2 and Huh7 cells, respectively. Genes functionally involved in cell death, signal transduction and regulation of transcription were predominantly up-regulated, while genes implicated in metabolism, cell-cycle control and DNA replication and repair were mainly down-regulated upon treatment. However, combination-treated HCC cell lines displayed specificity in the expression and activity of crucial factors involved in hepatocarcinogenesis. The altered expression of some of these genes was confirmed by semi-quantitative and quantitative RT-PCR and by Western blotting. Many novel genes emerged from our transcriptomic analyses, and further functional analyses may determine whether these genes can serve as potential molecular targets for more effective anti-HCC strategies

Observation of the Early Structural Changes Leading to the Formation of Protein Superstructures.

Formation of superstructures in protein aggregation processes has been indicated as a general pathway for several proteins, possibly playing a role in human pathologies. There is a severe lack of knowledge on the origin of such species in terms of both mechanisms of formation and structural features. We use equine lysozyme as a model protein, and by combining spectroscopic techniques and microscopy with X-ray fiber diffraction and ab initio modeling of Small Angle X-ray Scattering data, we isolate the partially unfolded state from which one of these superstructures (i.e., particulate) originates. We reveal the low-resolution structure of the unfolded state and its mechanism of formation, highlighting the physicochemical features and the possible pathway of formation of the particulate structure. Our findings provide a novel detailed knowledge of such a general and alternative aggregation pathway for proteins, this being crucial for a basic and broader understanding of the aggregation phenomena.This is the author's accepted manuscript and will be under embargo until the 3rd of September 2015. The final version is published by ACS in The Journal of Physical Chemistry Letters here: http://pubs.acs.org/doi/abs/10.1021/jz501614e

Subtle pH variation around pH 4.0 affects aggregation kinetics and aggregate characteristics of recombinant human insulin

Insulin is a biotherapeutic protein, which, depending on environmental conditions such as pH, has been shown to form a large variety of aggregates with different structures and morphologies. This work focuses on the formation and characteristics of insulin particulates, dense spherical aggregates having diameters spanning from nanometre to low-micron size. An in-depth investigation of the system is obtained by applying a broad range of techniques for particle sizing and characterisation. An interesting observation was achieved regarding the formation kinetics and aggregate characteristics of the particulates; a subtle change in the pH from pH 4.1 to pH 4.3 markedly affected the kinetics of the particulate formation and led to different particulate sizes, either nanosized or micronsized particles. Also, a clear difference between the secondary structure of the protein particulates formed at the two pH values was observed, where the nanosized particulates had an increased content of aggregated β-structure compared to the micronsized particles. The remaining characteristics of the particles were identical for the two particulate populations. These observations highlight the importance of carefully studying the formulation design space and of knowing the impact of parameters such as pH on the aggregation to secure a drug product in control. Furthermore, the identification of particles only varying in few parameters, such as size, are considered highly valuable for studying the effect of particle features on the immunogenicity potential.Drug Delivery Technolog