55 research outputs found
The Age of the Galactic Disk
I review different methods devised to derive the age of the Galactic Disk,
namely the Radio-active Decay (RD), the Cool White Dwarf Luminosity Function
(CWDLF), old opne clusters (OOC) and the Color Magnitude Diagram (CMD) of the
stars in the solar vicinity. I argue that the disk is likely to be 8-10 Gyr
old. Since the bulk of globulars has an age around 13 Gyr, the possibility
emerges that the Galaxy experienced a minimum of Star Formation at the end of
the halo/bulge formation. This minimum might reflect the time at which the
Galaxy started to acquire material to form the disk inside-out.Comment: 10 pages, 4 figure, invited review, in "The chemical evolution of the
Milky Way : Stars vs Clusters, Vulcano (Italy), 20-24 September 199
Coupling of kinesin ATP turnover to translocation and microtubule regulation: one engine, many machines
The cycle of ATP turnover is integral to the action of motor proteins. Here we discuss how variation in this cycle leads to variation of function observed amongst members of the kinesin superfamily of microtubule associated motor proteins. Variation in the ATP turnover cycle among superfamily members can tune the characteristic kinesin motor to one of the range of microtubule-based functions performed by kinesins. The speed at which ATP is hydrolysed affects the speed of translocation. The ratio of rate constants of ATP turnover in relation to association and dissociation from the microtubule influence the processivity of translocation. Variation in the rate-limiting step of the cycle can reverse the way in which the motor domain interacts with the microtubule producing non-motile kinesins. Because the ATP turnover cycle is not fully understood for the majority of kinesins, much work remains to show how the kinesin engine functions in such a wide variety of molecular machines
Protocol for the Foot in Juvenile Idiopathic Arthritis trial (FiJIA): a randomised controlled trial of an integrated foot care programme for foot problems in JIA
<b>Background</b>:
Foot and ankle problems are a common but relatively neglected manifestation of juvenile idiopathic arthritis. Studies of medical and non-medical interventions have shown that clinical outcome measures can be improved. However existing data has been drawn from small non-randomised clinical studies of single interventions that appear to under-represent the adult population suffering from juvenile idiopathic arthritis. To date, no evidence of combined therapies or integrated care for juvenile idiopathic arthritis patients with foot and ankle problems exists.
<b>Methods/design</b>:
An exploratory phase II non-pharmacological randomised controlled trial where patients including young children, adolescents and adults with juvenile idiopathic arthritis and associated foot/ankle problems will be randomised to receive integrated podiatric care via a new foot care programme, or to receive standard podiatry care. Sixty patients (30 in each arm) including children, adolescents and adults diagnosed with juvenile idiopathic arthritis who satisfy the inclusion and exclusion criteria will be recruited from 2 outpatient centres of paediatric and adult rheumatology respectively. Participants will be randomised by process of minimisation using the Minim software package. The primary outcome measure is the foot related impairment measured by the Juvenile Arthritis Disability Index questionnaire's impairment domain at 6 and 12 months, with secondary outcomes including disease activity score, foot deformity score, active/limited foot joint counts, spatio-temporal and plantar-pressure gait parameters, health related quality of life and semi-quantitative ultrasonography score for inflammatory foot lesions. The new foot care programme will comprise rapid assessment and investigation, targeted treatment, with detailed outcome assessment and follow-up at minimum intervals of 3 months. Data will be collected at baseline, 6 months and 12 months from baseline. Intention to treat data analysis will be conducted.
A full health economic evaluation will be conducted alongside the trial and will evaluate the cost effectiveness of the intervention. This will consider the cost per improvement in Juvenile Arthritis Disability Index, and cost per quality adjusted life year gained. In addition, a discrete choice experiment will elicit willingness to pay values and a cost benefit analysis will also be undertaken
Real-Time Dynamics of Ca2+, Caspase-3/7, and Morphological Changes in Retinal Ganglion Cell Apoptosis under Elevated Pressure
Quantitative information on the dynamics of multiple molecular processes in individual live cells under controlled stress is central to the understanding of the cell behavior of interest and the establishment of reliable models. Here, the dynamics of the apoptosis regulator intracellular Ca2+, apoptosis effector caspase-3/7, and morphological changes, as well as temporal correlation between them at the single cell level, are examined in retinal gangling cell line (differentiated RGC-5 cells) undergoing apoptosis at elevated hydrostatic pressure using a custom-designed imaging platform that allows long-term real-time simultaneous imaging of morphological and molecular-level physiological changes in large numbers of live cells (beyond the field-of-view of typical microscopy) under controlled hydrostatic pressure. This examination revealed intracellular Ca2+ elevation with transient single or multiple peaks of less than 0.5 hour duration appearing at the early stages (typically less than 5 hours after the onset of 100 mmHg pressure) followed by gradual caspase-3/7 activation at late stages (typically later than 5 hours). The data reveal a strong temporal correlation between the Ca2+ peak occurrence and morphological changes of neurite retraction and cell body shrinkage. This suggests that Ca2+ elevation, through its impact on ion channel activity and water efflux, is likely responsible for the onset of apoptotic morphological changes. Moreover, the data show a significant cell-to-cell variation in the onset of caspase-3/7 activation, an inevitable consequence of the stochastic nature of the underlying biochemical reactions not captured by conventional assays based on population-averaged cellular responses. This real-time imaging study provides, for the first time, statistically significant data on simultaneous multiple molecular level changes to enable refinements and testing of models of the dynamics of mitochondria-mediated apoptosis. Further, the platform developed and the approach has direct significance to the study of a variety of signaling pathway phenomena
Improving policy coherence for food security and nutrition in South Africa: a qualitative policy analysis
Like most other low and middle-income countries, South Africa must address a rising burden of diet-related chronic disease in a
situation of persistent food insecurity and undernutrition. Supply-side policy interventions are a critical component of action to
address the double burden of malnutrition. However, the food supply is governed by a number of different policy sectors, and
policy incoherence can occur between government action to promote a healthy food supply and objectives for economic
liberalization. We analysed the coherence of food supply policy content with respect to nutrition and food security in South
Africa, and conducted 14 in-depth interviews with 22 public and private sector actors to identify opportunities to improve policy
coherence across sectors governing the food supply. Drawing on Sabatier’s conceptualization of actors as influential in shaping
policy outcomes, we identified three coalitions of actors related to food security and nutrition in South Africa: the dominant
Economic Growth coalition, the Food Security coalition, and the Health coalition. Understanding the frames, beliefs and
resources held by these coalitions offers insights into the policy tensions faced by the Government of South Africa with respect
to the food supply. The analysis indicates that the current reconsideration of economic policy agendas favouring liberalization in
SouthAfrica, including the termination of most bilateral investment treaties, may present an opportunity for increased recognition
of food security and nutrition priorities in food supply policy making. Opportunities to strengthen policy coherence across the
food supply for food security and nutrition include: specific changes to economic policy relating to the food supply that achieve
both food security/nutrition and economic objectives; creating links between producers and consumers, through markets and
fiscal incentives that make healthy / fresh foods more accessible and affordable; increasing formal avenues for engagement by
Civil Society in nutrition and food security policy making; and including consideration of the nutritional quality of the food
supply in policy objectives across sectors, to create a framework for policy coherence across sectors relating to the food supply
Stimulation‐Induced Mitochondrial [Ca 2+
Changes in mitochondrial matrix [Ca(2+)] evoked by trains of action potentials were studied in levator auris longus motor terminals using Ca(2+)-sensitive fluorescent indicator dyes (rhod-2, rhod-5F). During a 2500 impulse 50 Hz train, mitochondrial [Ca(2+)] in most wild-type terminals increased within 5–10 s to a plateau level that was sustained until stimulation ended. This plateau was not due to dye saturation, but rather reflects a powerful buffering system within the mitochondrial matrix. The amplitude of this plateau was similar for stimulation frequencies in the range 15–100 Hz. Plateau amplitude was sensitive to temperature, with no detectable stimulation-induced increase in fluorescence at temperatures below 17 °C, and increasing magnitudes as temperature was increased to near-physiological levels (38 °C). When stimulation ended, mitochondrial [Ca(2+)] decayed slowly back to prestimulation levels over a time course of hundreds of seconds. Similar measurements were also made in motor terminals of mice expressing the G93A mutation of human superoxide dismutase 1 (SOD1-G93A). In mice > 100 days old, all of whom exhibited hindlimb paralysis, some terminals continued to show wild-type mitochondrial [Ca(2+)] responses, but in other terminals mitochondrial [Ca(2+)] did not plateau, but rather continued to increase throughout most of the stimulus train. Thus mechanism(s) that limit stimulation-induced increases in mitochondrial [Ca(2+)] may be compromised in some SOD1-G93A terminals
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