762 research outputs found
Magnetic resonance imaging analysis of the bioabsorbable Milagroâą interference screw for graft fixation in anterior cruciate ligament reconstruction
Ligament graft fixation with bioabsorbable interference screws is a standard procedure in cruciate ligament replacement. Previous screw designs may resorb incompletely, and can cause osteolysis and sterile cysts despite being implanted for several years. The aim of this study was to examine the in vivo degradation and biocompatibility of the new Milagroâą interference screw (Mitek, Norderstedt, Germany). The Milagroâą interference screw is made of 30% Ă-TCP (TriCalcium phosphate) and 70% PLGA (Poly-lactic-co-glycolic acid). In the period between June 2005 and February 2006, 38 patients underwent graft fixation with Milagroâą screws in our hospital. Arthroscopic ACL reconstruction was performed using hamstring tendon grafts in all the patients. MR imaging was performed on 12 randomly selected patients out of the total of 38 at 3, 6 and 12 months after surgery. During the examination, the volume loss of the screw, tunnel enlargement, presence of osteolysis, fluid lines, edema and postoperative screw replacement by bone tissue were evaluated. There was no edema or signs of inflammation around the bone tunnels. At 3, 6 and 12 months, the tibial screws showed an average volume loss of 0, 8.1% (±7.9%) and 82.6% (±17.2%, P < 0.05), respectively. The femoral screws showed volume losses of 2.5% (±2.1%), 31.3% (±21.6%) and 92.02% (±6.3%, P < 0.05), respectively. The femoral tunnel enlargement was 47.4% (±43.8%) of the original bone tunnel volume after 12 months, and the mean tunnel volume of the tibial tunnel was â9.5% (±58.1%) compared to the original tunnel. Bone ingrowth was observed in all the patients. In conclusion, the resorption behaviour of the Milagroâą screw is closely linked to the graft healing process. The screws were rapidly resorbed after 6 months and, at 12 months, only the screw remnants were detectable. Moreover, the Milagroâą screw is biocompatible and osteoconductive, promoting bone ingrowth during resorption. Tunnel enlargement is not prevented in the first months but is reduced by bone ingrowth after 12 months
Dual equipoise shared decision making: definitions for decision and behaviour support interventions
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80919.pdf (publisher's version ) (Open Access)ABSTRACT: BACKGROUND: There is increasing interest in interventions that can support patients who face difficult decisions and individuals who need to modify their behaviour to achieve better outcomes. Evidence for effectiveness is used to categorise patients care. Effective care is where evidence of benefit outweighs harm: patients should always receive this type of care, where indicated. Preference-sensitive care describes a situation where the evidence for the superiority of one treatment over another is either not available or does not allow differentiation; in this situation, there are two or more valid approaches, and the best choice depends on how individuals value the risks and benefits of treatments. DISCUSSION: Preference-sensitive decisions are defined by equipoise: situations where options need to be deliberated. Moreover, where both healthcare professionals and patients agree that equipoise exists, situations may be regarded as having 'dual equipoise'. Such conditions are ideal for shared decision making. However, there are many situations in medicine where dual equipoise does not exist, where health professionals hold the view that scientific evidence for benefit strongly outweighs harm. This is often the case where people suffer from chronic conditions, and where behaviour change is recommended to improve outcomes. However, some patients, are either ambivalent or find it difficult to sustain optimal behaviours, i.e., patients will be in varying degrees of equipoise. Therefore, situations where dual equipoise exists (or not) help to clarify the definitions of two classes of support, namely, decision and behaviour change support interventions. Decision support interventions help people think about choices they face; they describe where and why choice exists, in short, conditions of dual equipoise; they provide information about options, including, where reasonable, the option of taking no action. These interventions help people to deliberate, independently or in collaboration with others, about options by considering relevant attributes; they support people to forecast how they might feel about short, intermediate, and long-term outcomes that have relevant consequences, in ways that help the process of constructing preferences and eventual decision making appropriate to their individual situation. Whereas, behavioural support interventions describe, justify, and recommend actions that, over time, lead to predictable outcomes over short, intermediate, and long-term timeframes, and that have relevant and important consequences for those who are considering behaviour change. SUMMARY: Decision and behaviour support interventions have divergent aims, different relationships to equipoise, and form two classes of interventions
Limits on Cosmological Variation of Strong Interaction and Quark Masses from Big Bang Nucleosynthesis, Cosmic, Laboratory and Oklo Data
Recent data on cosmological variation of the electromagnetic fine structure
constant from distant quasar (QSO) absorption spectra have inspired a more
general discussion of possible variation of other constants. We discuss
variation of strong scale and quark masses. We derive the limits on their
relative change from (i) primordial Big-Bang Nucleosynthesis (BBN); (ii)
Oklo natural nuclear reactor, (iii) quasar absorption spectra, and (iv)
laboratory measurements of hyperfine intervals.Comment: 10 pages 2 figurs: second version have several references added and
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Synaptic Tau Seeding Precedes Tau Pathology in Human Alzheimer's Disease Brain
Alzheimer's disease (AD) is defined by the presence of intraneuronal neurofibrillary tangles (NFTs) composed of hyperphosphorylated tau aggregates as well as extracellular amyloid-beta plaques. The presence and spread of tau pathology through the brain is classified by Braak stages and thought to correlate with the progression of AD. Several in vitro and in vivo studies have examined the ability of tau pathology to move from one neuron to the next, suggesting a âprion-likeâ spread of tau aggregates may be an underlying cause of Braak tau staging in AD. Using the HEK293 TauRD-P301S-CFP/YFP expressing biosensor cells as a highly sensitive and specific tool to identify the presence of seed competent aggregated tau in brain lysateâi.e., tau aggregates that are capable of recruiting and misfolding monomeric tauâ, we detected substantial tau seeding levels in the entorhinal cortex from human cases with only very rare NFTs, suggesting that soluble tau aggregates can exist prior to the development of overt tau pathology. We next looked at tau seeding levels in human brains of varying Braak stages along six regions of the Braak Tau Pathway. Tau seeding levels were detected not only in the brain regions impacted by pathology, but also in the subsequent non-pathology containing region along the Braak pathway. These data imply that pathogenic tau aggregates precede overt tau pathology in a manner that is consistent with transneuronal spread of tau aggregates. We then detected tau seeding in frontal white matter tracts and the optic nerve, two brain regions comprised of axons that contain little to no neuronal cell bodies, implying that tau aggregates can indeed traverse along axons. Finally, we isolated cytosolic and synaptosome fractions along the Braak Tau Pathway from brains of varying Braak stages. Phosphorylated and seed competent tau was significantly enriched in the synaptic fraction of brain regions that did not have extensive cellular tau pathology, further suggesting that aggregated tau seeds move through the human brain along synaptically connected neurons. Together, these data provide further evidence that the spread of tau aggregates through the human brain along synaptically connected networks results in the pathogenesis of human Alzheimer's disease
Effects of Short Range Correlations on Ca Isotopes
The effect of Short Range Correlations (SRC) on Ca isotopes is studied using
a simple phenomenological model. Theoretical expressions for the charge
(proton) form factors, densities and moments of Ca nuclei are derived. The role
of SRC in reproducing the empirical data for the charge density differences is
examined. Their influence on the depletion of the nuclear Fermi surface is
studied and the fractional occupation probabilities of the shell model orbits
of Ca nuclei are calculated. The variation of SRC as function of the mass
number is also discussed.Comment: 11 pages (RevTex), 6 Postscript figures available upon request at
[email protected] Physical Review C in prin
Asymmetric effects of false positive and false negative indications on the verification of alerts in different risk conditions
Dieser Beitrag ist mit Zustimmung des Rechteinhabers aufgrund einer (DFG geförderten) Allianz- bzw. Nationallizenz frei zugÀnglich.This publication is with permission of the rights owner freely accessible due to an Alliance licence and a national licence (funded by the DFG, German Research Foundation) respectively.Indications from alerts or alarm systems can be the trigger for decisions, or they can elicit further information search. We report an experiment on the tendency to collect additional information after receiving system indications. We varied the proclivity of the alarm system towards false positive or false negative indications and the perceived risk of the situation. Results showed that false alarm-prone systems led to more frequent re-checking following both alarms and non-alarms in the high risk condition, whereas miss-prone systems led to high re-checking rates only for non-alarms, representing an asymmetry effect. Increasing the risk led to more re-checks with all alarm systems, but it had a stronger impact in the false alarm-prone condition. Results regarding the relation of risk and the asymmetry effect of false negative and false positive indications are discussed
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