1,698 research outputs found
AL Amyloidosis for Cardiologists: Awareness, Diagnosis, and Future Prospects: JACC: CardioOncology State-of-the-Art Review
Amyloid light chain (AL) amyloidosis is a rare, debilitating, often fatal disease. Symptoms of cardiomyopathy are common presenting features, and patients often are referred to cardiologists. Cardiac amyloid infiltration is the leading predictor of death. However, the variable presentation and perceived rarity of the disease frequently lead to delay in suspecting amyloidosis as a cause of heart failure, leading to misdiagnoses and a marked delay in diagnosis, with devastating consequences for the patient. A median time from symptom onset to correct diagnosis of about 2 years is often too long when median survival from diagnosis for patients with AL amyloidosis and cardiomyopathy is 4 months to 2 years. The authors highlight the challenges to diagnosis, identify gaps in the current knowledge, and summarize novel treatments on the horizon to raise awareness about the critical need for early recognition of symptoms and diagnosis of AL amyloidosis aimed at accelerating treatment and improving outcomes for patients
Intrinsic ankle stiffness is associated with paradoxical calf muscle movement but not postural sway or age
Due to Achilles tendon compliance, passive ankle stiffness is insufficient to stabilise the body when standing. This results in ‘paradoxical’ muscle movement, whereby calf muscles tend to shorten during forward body sway. Natural variation in stiffness may affect this movement. This may have consequences for postural control, with compliant ankles placing greater reliance upon active neural control rather than stretch reflexes. Previous research also suggests ageing reduces ankle stiffness, possibly contributing to reduced postural stability. Here we determine the relationship between ankle stiffness and calf muscle movement during standing, and whether this is associated with postural stability or age. Passive ankle stiffness was measured during quiet stance in 40 healthy volunteers ranging from 18 to 88 years of age. Medial gastrocnemius muscle length was also recorded using ultrasound. We found a significant inverse relationship between ankle stiffness and paradoxical muscle movement, that is, more compliant ankles were associated with greater muscle shortening during forward sway (r ≥ 0.33). This was seen during both quiet stance as well as voluntary sway. However, we found no significant effects of age upon stiffness, paradoxical motion or postural sway. Furthermore, neither paradoxical muscle motion nor ankle stiffness was associated with postural sway. These results show that natural variation in ankle stiffness alters the extent of paradoxical calf muscle movement during stance. However, the absence of a clear relationship to postural sway suggests that neural control mechanisms are more than capable of compensating for a lack of inherent joint stiffness
The World Will Never be the Same: The Russia-Ukraine Conflict as a Trigger Point for Deglobalisation
This paper makes the case for why we believe that the Russia-Ukraine crisis signals the end of a global era defined by globalisation. Even though Russia’s economy is only a fraction of the US, EU or China, its role in the world is much more relevant and the events in Ukraine are triggering a cascade of effects that will redefine the political, social and economic thinking and interactions among nations long into the future. With the Russian invasion of Ukraine, the “peace dividend” of recent decades is gone as military budgets are increasing significantly around the world. Energy and raw material dependency on other countries is considered a strategic weakness. The war has disrupted global supply chains and nations are now shunning the exposure to other countries, especially ones that do not share similar values. The macroeconomic environment has changed as growth prospects are depressed and inflation is on the rise. The world is moving to a period of reorganisation and instability
Претензионная работа по топливу для предприятий энергетики
Background and aims: CREB (cAMP response element binding protein) transcription factors are key regulators of homeostatic functions in the liver, and CRE binding is increased in hepatic inflammation. During chronic hepatitis B virus (HBV) infection, mutations or deletions in the pre-S region are frequently observed. These mutations can affect the pre-S2/S promoter controlling HBV envelope protein expression (hepatitis B surface antigen (HBsAg)) and have been associated with worsened clinical outcome. We aimed to test if CREB activation impacts on HBsAg expression. Methods: The effect of the CREB inducer protein kinase A (PKA) was tested by coexpression with HBV wild-type vector in vitro. Luciferase reporter gene constructs were cloned to identify novel regulatory regions for the HBV pre-S2/S promoter. Electrophoretic mobility shift assay (EMSA) gelshift and supershift experiments were conducted to confirm DNA transcription factor binding. Results: Coexpression of HBV and PKA resulted in HBV-S mRNA induction and enhanced small envelope protein expression. We identified a CREB binding motif in the transcribed part of the pre-S2 region, contributing to basal S promoter activity via binding of activating transcription factor 2 (ATF2). A second CREB motif closely linked to the S-ATG showed a similar binding pattern involving ATF2 and CREB1, without appearing essential for basal promoter activity. Moreover, a sequence in the pre-S2 region is responsible for further transcriptional induction via CREB activators such as PKA and forskolin. EMSA experiments indicate that CREB1 and ATF4 are involved in complex formation conferring PKA dependent promoter activation. Conclusions: Our data suggest a novel mechanism by which HBV may utilise CREB/PKA signal transduction pathways of hepatocytes to enhance its HBsAg expression during homeostasis and hepatic inflammation
An antibody that prevents serpin polymerisation acts by inducing a novel allosteric behavior
Serpins are important regulators of proteolytic pathways with an antiprotease activity that involves a conformational transition from a metastable to a hyperstable state. Certain mutations permit the transition to occur in the absence of a protease; when associated with an intermolecular interaction, this yields linear polymers of hyperstable serpin molecules, which accumulate at the site of synthesis. This is the basis of many pathologies termed the serpinopathies. We have previously identified a monoclonal antibody (mAb4B12) that, in single-chain form, blocks α1-Antitrypsin (α1-AT) polymerisation in cells. Here, we describe the structural basis for this activity. The mAb4B12 epitope was found to encompass residues Glu32, Glu39 and His43 on helix A and Leu306 on helix I. This is not a region typically associated with the serpin mechanism of conformational change, and correspondingly the epitope was present in all tested structural forms of the protein. Antibody binding rendered β-sheet A - on the opposite face of the molecule - more liable to adopt an 'open' state, mediated by changes distal to the breach region and proximal to helix F. The allosteric propagation of induced changes through the molecule was evidenced by an increased rate of peptide incorporation and destabilisation of a preformed serpin-enzyme complex following mAb4B12 binding. These data suggest that prematurely shifting the β-sheet A equilibrium towards the 'open' state out of sequence with other changes suppresses polymer formation. This work identifies a region potentially exploitable for a rational design of ligands that is able to dynamically influence α1-AT polymerisation
White-light OLEDs using liquid crystal polymer networks
We have mixed nematic light-emitting liquid crystals and incorporated them as insoluble cross-linked polymer networks in a liquid crystal white-light organic light-emitting diode (LC-WOLED). The light emission is not voltage-dependent and polarized white light emission is also demonstrated. This wet-chemistry approach to WOLEDs is compatible with patterning by photolithography as well as by inkjet printing at room temperature on plastic substrates by roll-to-roll manufacturing
Reversible and Irreversible Interactions of Poly(3-hexylthiophene) with Oxygen Studied by Spin-Sensitive Methods
Understanding of degradation mechanisms in polymer:fullerene
bulk-heterojunctions on the microscopic level aimed at improving their
intrinsic stability is crucial for the breakthrough of organic photovoltaics.
These materials are vulnerable to exposure to light and/or oxygen, hence they
involve electronic excitations. To unambiguously probe the excited states of
various multiplicities and their reactions with oxygen, we applied combined
magneto-optical methods based on multifrequency (9 and 275 GHz) electron
paramagnetic resonance (EPR), photoluminescence (PL), and PL-detected magnetic
resonance (PLDMR) to the conjugated polymer poly(3-hexylthiophene) (P3HT) and
polymer:fullerene bulk heterojunctions (P3HT:PCBM; PCBM =
[6,6]-phenyl-C61-butyric acid methyl ester). We identified two distinct
photochemical reaction routes, one being fully reversible and related to the
formation of polymer:oxygen charge transfer complexes, the other one,
irreversible, being related to the formation of singlet oxygen under
participation of bound triplet excitons on the polymer chain. With respect to
the blends, we discuss the protective effect of the methanofullerenes on the
conjugated polymer bypassing the triplet exciton generation
- …