690 research outputs found
O plastocrono e o filocrono em Araucaria angustifolia (Bert.) O. Ktze., no municĂpio de Colombo, ParanĂĄ.
EVINCI. Resumo 014
Oral malodor in Special Care Patients: current knowledge
Epidemiological studies report that about 50% of the population may have oral malodor
with a strong social and psychological impact in their daily life. When intra-oral causes are
excluded, referral to an appropriate medical specialist is paramount for management and
treatment of extra-oral causes. The intra-oral causes of halitosis are highly common, and the
dentist is the central clinician to diagnose and treat them. Pseudohalitosis or halitophobia
may occur and an early identification of these conditions by the dentist is important in order
to avoid unnecessary dental treatments for patients who need psychological or psychiatric
therapy. The organoleptic technique is still considered the most reliable examination method
to diagnose genuine halitosis. Special needs patients are more prone than others to have
oral malodor because of concurrent systemic or metabolic diseases, and medications.
The present report reviews halitosis, its implications, and the management in special care
dentistry
Micropropagation of Ocotea porosa (Nees & Martius) Barroso
The objective of this work was the establishment of a micropropagation protocol for Ocotea porosa by multiplication of shoots from axillary buds. Different concentration of BAP (0; 2.5; 5 or 10 ĂŹM) or BAP+KIN (0; 1.25; 2.5 or 5 ĂŹM) were investigated to optimize the multiplication. Shoot growth was stimulated with reduced concentration of BAP (0; 0.5; 1 or 1.5 ĂŹM) or KIN (0.5 or 1ĂŹM) or activated charcoal (0.5; 1; 2 or 3 gl-1). For root induction different concentrations of IBA (0; 1.25; 2.5; 5 or 10 ĂŹM) or (0; 2.5; 5 or 10 mM) were applied. The highest mean multiplication rate was observed in the fourth subculture with 5 ĂŹM BAP, reaching 5.3 shoots per explant. The shoots elongated in culture medium supplemented with 2 gl-1 activated charcoal and presented bigger leaves than on medium with reduced concentration of BAP. The shoots rooted on medium contains 10 ĂŹM IBA or after pulse treatment of 10 mM (68.7 and 62.6% of rooting, respectively). The survival rate of the plants was 56.7%. This study showed that O. porosa micropropagation is feasible; however it needs further research in order to increase plant survival.Key words: 6-Benzylaminopurine, multiplication, rooting, in vitro culture, apical shoots, native specie
Analgesic and Antidepressant Effects of the Clinical Glutamate Modulators Acetyl-L-Carnitine and Ketamine
Pain and depression are leading causes of disability and of profound social and economic burden. Their impact is aggravated by their chronicity and comorbidity and the insufficient efficacy of current treatments. Morphological and functional metabolism studies link chronic pain and depressive disorders to dysfunctional neuroplastic changes in fronto-limbic brain regions that control emotional responses to painful injuries and stressful events. Glutamate modulators are emerging new therapies targeting dysfunctional brain areas implicated in the generation and maintenance of chronic pain and depression. Here, we report the effects of two clinically approved glutamate modulators: acetyl-L-carnitine (ALCAR) and S, R(±)ketamine (KET). ALCAR is a natural neurotrophic compound currently marketed for the treatment of neuropathies. KET is the prototypical non-competitive antagonist at N-methyl-D-aspartate glutamate receptors and a clinically approved anesthetic. Although they differ in pharmacological profiles, ALCAR and KET both modulate aminergic and glutamatergic neurotransmissions and pain and mood. We assessed in rats the effects of ALCAR and KET on cerebral metabolic rates for glucose (rCMRglc) and assessed clinically the effects of ALCAR in chronic pain and of KET in post-operative pain. ALCAR and KET increased rCMRglc at similar degrees in prefrontal, somatosensory, and cingulate cortices, and KET increased rCMRglc at a different, much larger, degree in limbic and dopaminergic areas. While rCMRglc increases in prefrontal cortical areas have been associated with analgesic and antidepressant effects of ALCAR and KET, the marked metabolic increases KET induces in limbic and dopaminergic areas have been related to its psychotomimetic and abuse properties. In patients with chronic neuropathic pain, ALCAR (1,000 mg/day) yielded to a fast (2 weeks) improvement of mood and then of pain and quality of life. In day-surgery patients, KET improved dischargeability and satisfaction. In obese patients undergoing bariatric surgery, a single, low dose of KET (0.5 mg/kg) at induction of anesthesia determined a very fast (hours) amelioration of post-operative depression and pain and an opioid-sparing effect. These findings indicate that ALCAR and KET, two non-selective glutamate modulators, still offer viable therapeutic options in comorbid pain and depression
Dependences of the Casimir-Polder interaction between an atom and a cavity wall on atomic and material properties
The Casimir-Polder and van der Waals interactions between an atom and a flat
cavity wall are investigated under the influence of real conditions including
the dynamic polarizability of the atom, actual conductivity of the wall
material and nonzero temperature of the wall. The cases of different atoms near
metal and dielectric walls are considered. It is shown that to obtain accurate
results for the atom-wall interaction at short separations, one should use the
complete tabulated optical data for the complex refractive index of the wall
material and the accurate dynamic polarizability of an atom. At relatively
large separations in the case of a metal wall, one may use the plasma model
dielectric function to describe the dielectric properties of wall material. The
obtained results are important for the theoretical interpretation of
experiments on quantum reflection and Bose-Einstein condensation.Comment: 5 pages, 1 figure, iopart.cls is used, to appear in J. Phys. A
(special issue: Proceedings of QFEXT05, Barcelona, Sept. 5-9, 2005
Evolution of surname distribution under gender-equality measurements
We consider a model for the evolution of the surnames distribution under a
gender-equality measurement presently discussed in the Spanish parliament (the
children take the surname of the father or the mother according to alphabetical
order). We quantify how this would bias the alphabetical distribution of
surnames, and analyze its effect on the present distribution of the surnames in
Spain
Pharmacological treatment for familial amyloid neuropathy
This is a protocol for a Cochrane Review (Intervention). The objectives are as follows: To assess and compare the efficacy, acceptability, and tolerability of pharmacologic diseaseâmodifying agents for familial amyloid neuropathy (FAP)
Pharmacological treatment for familial amyloid polyneuropathy
Background:
Diseaseâmodifying pharmacological agents for transthyretin (TTR)ârelated familial amyloid polyneuropathy (FAP) have become available in the last decade, but evidence on their efficacy and safety is limited. This review focuses on diseaseâmodifying pharmacological treatment for TTRârelated and other FAPs, encompassing amyloid kinetic stabilisers, amyloid matrix solvents, and amyloid precursor inhibitors.
Objectives:
To assess and compare the efficacy, acceptability, and tolerability of diseaseâmodifying pharmacological agents for familial amyloid polyneuropathies (FAPs).
Search methods:
On 18 November 2019, we searched the Cochrane Neuromuscular Specialised Register, the Cochrane Central Register of Controlled Trials, MEDLINE, and Embase. We reviewed reference lists of articles and textbooks on peripheral neuropathies. We also contacted experts in the field. We searched clinical trials registries and manufacturers' websites.
Selection criteria:
We included randomised clinical trials (RCTs) or quasiâRCTs investigating any diseaseâmodifying pharmacological agent in adults with FAPs.
Disability due to FAP progression was the primary outcome. Secondary outcomes were severity of peripheral neuropathy, change in modified body mass index (mBMI), quality of life, severity of depression, mortality, and adverse events during the trial.
Data collection and analysis:
We followed standard Cochrane methodology.
Main results:
The review included four RCTs involving 655 people with TTRâFAP. The manufacturers of the drugs under investigation funded three of the studies. The trials investigated different drugs versus placebo and we did not conduct a metaâanalysis.
One RCT compared tafamidis with placebo in earlyâstage TTRâFAP (128 randomised participants). The trial did not explore our predetermined disability outcome measures. After 18 months, tafamidis might reduce progression of peripheral neuropathy slightly more than placebo (Neuropathy Impairment Score (NIS) in the lower limbs; mean difference (MD) â3.21 points, 95% confidential interval (CI) â5.63 to â0.79; P = 0.009; lowâcertainty evidence). However, tafamidis might lead to little or no difference in the change of quality of life between groups (Norfolk Quality of LifeâDiabetic Neuropathy (Norfolk QOLâDN) total score; MD â4.50 points, 95% CI â11.27 to 2.27; P = 0.19; very lowâcertainty evidence). No clear betweenâgroup difference was found in the numbers of participants who died (risk ratio (RR) 0.65, 95% CI 0.11 to 3.74; P = 0.63; very lowâcertainty evidence), who dropped out due to adverse events (RR 1.29, 95% CI 0.30 to 5.54; P = 0.73; very lowâcertainty evidence), or who experienced at least one severe adverse event during the trial (RR 1.16, 95% CI 0.37 to 3.62; P = 0.79; very lowâcertainty evidence).
One RCT compared diflunisal with placebo (130 randomised participants). At month 24, diflunisal might reduce progression of disability (Kumamoto Score; MD â4.90 points, 95% CI â7.89 to â1.91; P = 0.002; lowâcertainty evidence) and peripheral neuropathy (NIS plus 7 nerve tests; MD â18.10 points, 95% CI â26.03 to â10.17; P < 0.001; lowâcertainty evidence) more than placebo. After 24 months, changes from baseline in the quality of life measured by the 36âItem ShortâForm Health Survey score showed no clear difference between groups for the physical component (MD 6.10 points, 95% CI 2.56 to 9.64; P = 0.001; very lowâcertainty evidence) and the mental component (MD 4.40 points, 95% CI â0.19 to 8.99; P = 0.063; very lowâcertainty evidence). There was no clear betweenâgroup difference in the number of people who died (RR 0.46, 95% CI 0.15 to 1.41; P = 0.17; very lowâcertainty evidence), in the number of dropouts due to adverse events (RR 2.06, 95% CI 0.39 to 10.87; P = 0.39; very lowâcertainty evidence), and in the number of people who experienced at least one severe adverse event (RR 0.77, 95% CI 0.18 to 3.32; P = 0.73; very lowâcertainty evidence) during the trial.
One RCT compared patisiran with placebo (225 randomised participants). After 18 months, patisiran reduced both progression of disability (Raschâbuilt Overall Disability Scale; leastâsquares MD 8.90 points, 95% CI 7.00 to 10.80; P < 0.001; moderateâcertainty evidence) and peripheral neuropathy (modified NIS plus 7 nerve tests â Alnylam version; leastâsquares MD â33.99 points, 95% CI â39.86 to â28.13; P < 0.001; moderateâcertainty evidence) more than placebo. At month 18, the change in quality of life between groups favoured patisiran (Norfolk QOLâDN total score; leastâsquares MD â21.10 points, 95% CI â27.20 to â15.00; P < 0.001; lowâcertainty evidence). There was little or no betweenâgroup difference in the number of participants who died (RR 0.61, 95% CI 0.21 to 1.74; P = 0.35; lowâcertainty evidence), dropped out due to adverse events (RR 0.33, 95% CI 0.13 to 0.82; P = 0.017; lowâcertainty evidence), or experienced at least one severe adverse event (RR 0.91, 95% CI 0.64 to 1.28; P = 0.58; lowâcertainty evidence) during the trial.
One RCT compared inotersen with placebo (172 randomised participants). The trial did not explore our predetermined disability outcome measures. From baseline to week 66, inotersen reduced progression of peripheral neuropathy more than placebo (modified NIS plus 7 nerve tests â Ionis version; MD â19.73 points, 95% CI â26.50 to â12.96; P < 0.001; moderateâcertainty evidence). At week 65, the change in quality of life between groups favoured inotersen (Norfolk QOLâDN total score; MD â10.85 points, 95% CI â17.25 to â4.45; P < 0.001; lowâcertainty evidence). Inotersen may slightly increase mortality (RR 5.94, 95% CI 0.33 to 105.60; P = 0.22; lowâcertainty evidence) and occurrence of severe adverse events (RR 1.48, 95% CI 0.85 to 2.57; P = 0.16; lowâcertainty evidence) compared to placebo. More dropouts due to adverse events were observed in the inotersen than in the placebo group (RR 8.57, 95% CI 1.16 to 63.07; P = 0.035; lowâcertainty evidence).
There were no studies addressing apolipoprotein AIâFAP, gelsolinâFAP, and betaâ2âmicroglobulinâFAP.
Authors' conclusions
Evidence on the pharmacological treatment of FAPs from RCTs is limited to TTRâFAP. No studies directly compare diseaseâmodifying pharmacological treatments for TTRâFAP. Results from placeboâcontrolled trials indicate that tafamidis, diflunisal, patisiran, and inotersen may be beneficial in TTRâFAP, but further investigations are needed. Since direct comparative studies for TTRâFAP will be hampered by sample size and costs required to demonstrate superiority of one drug over another, longâterm nonârandomised openâlabel studies monitoring their efficacy and safety are needed
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