[ Rock y Pop ] : q grupo de estos ta chido o cool??

Elegis a tu favorito o en todo caso haced una lista de q orden te gustaria o q grupos faltarian? !! Poison http://www.youtube.com/watch?v=sMqjGywYOI8 Bon Jovi http://www.youtube.com/watch?v=nE11Zrrp24I Guns and Roses http://www.youtube.com/watch?v=VlzptZ9wieQ&feature=related Dire Straits http://www.youtube.com/watch?v=aNaKWXqXkhw Nirvana http://www.youtube.com/watch?v=wY3oEvaq71A de estos 5 grupos elegid entre los 3 primeros cual ha sido el mejor o el q te ha llamado mas la atencion, de ahi despues elegid tu favorito o haced un top 5 !! esperad sus opiniones please!! byeee y como dice alex lora "Y Q VIVA EL ROCK AND ROLLLLLLLLLL" !!!!!!!!!!!!!!!!!!!!! a verdad me falto aerosmith http://www.youtube.com/watch?v=t4u5om4xihU solo son los grupos cuyos cantantes eran reconocidos o por sus voces o sus peinados en aquella epoca sigan opinando !!!!!!!!!! por favor kiero saber cual es su favorito realmente !!!!!!jejeje y despues lesdigo cuales son mis favoritos pero por favor q de los 3 primeros digan cual es mejor y de ahi hacen el top5 !!!!!!!!!!!!!!!!!!!!!!!!!!!

[ Otros - Música y Ocio ] : hola alguien que sepa ingles me puede traducir esta cancion ???

porque las traducciones de internet estan mal traducidas Letra de la cancion "Ready, Set, Don't Go" de Billy Ray y Miley Cyrus She's gotta do what she's gotta do And I've gotta like it or not She's got dreams too big for this town And she needs to give 'em a shot Whatever they are Looks like she's all ready to leave Nothing left to pack There ain't no room for me in that car Even if she asked me to tag along God I gotta be strong [Chorus] She's at the startin' line of the rest of her life As ready as she's ever been Got the hunger and the stars in her eyes The prize is hers to win She's waitin' on my blessings before she hits that open road Baby get ready Get set Don't go She says things are fallen into place Feels like they're fallen apart I painted this big ol' smile on my face To hide my broken heart If only she knew This is where I don't say what I want so bad to say This is where I want to but I won't get in the way Of her and her drea

Distinct Olfactory Cross-Modal Effects on the Human Motor System

by Simone Rossi, Alberto De Capua, Patrizio Pasqualetti, Monica Ulivelli, Luciano Fadiga, Vincenzo Falzarano, Sabina Bartalini, Stefano Passero, Daniele Nuti, Paolo M. Rossini

Background

Converging evidence indicates that action observation and action-related sounds activate cross-modally the human motor system. Since olfaction, the most ancestral sense, may have behavioural consequences on human activities, we causally investigated by transcranial magnetic stimulation (TMS) whether food odour could additionally facilitate the human motor system during the observation of grasping objects with alimentary valence, and the degree of specificity of these effects.

Methodology/Principal Findings

In a repeated-measure block design, carried out on 24 healthy individuals participating to three different experiments, we show that sniffing alimentary odorants immediately increases the motor potentials evoked in hand muscles by TMS of the motor cortex. This effect was odorant-specific and was absent when subjects were presented with odorants including a potentially noxious trigeminal component.

The smell-induced corticospinal facilitation of hand muscles during observation of grasping was an additive effect which superimposed to that induced by the mere observation of grasping actions for food or non-food objects. The odour-induced motor facilitation took place only in case of congruence between the sniffed odour and the observed grasped food, and specifically involved the muscle acting as prime mover for hand/fingers shaping in the observed action.

Conclusions/Significance

Complex olfactory cross-modal effects on the human corticospinal system are physiologically demonstrable. They are odorant-specific and, depending on the experimental context, muscle- and action-specific as well. This finding implies potential new diagnostic and rehabilitative applications.

[ Otros - Relaciones Familiares ] : hacer un comic para alguien que me gusta es buena idea con una cancion qque me guste!!?

bueno, lo quiero hacer en vez de escribir una cancion que me gusta para una chava, hacer como un comic lo que dice la cancion en vez de poner letras!! a ver si entienden mi pregunta! International You Day" i'm sorry that it took so long to write this song but i gave up you see one million words can't describe how it feels to know your love where did i go wrong? i should have told you from the start that i'm closer then you think when we're apart nothing that i've tried is as simple as this line but without you my life is incomplete my days are absolutely gray and so I'll try let your heart know for sure that i have so much more to tell you every single day i swear i'm giving up my inside to the one that i adorded i know this world is big enough for you and i but i'll give you more i'm coming home today to wipe the tears right from your eyes i'm totally enamored by your life nothing that i've done has ever been for one but without you my life is incomplete my days are absolutely gray and so I'll try let your heart know for sure that i have so much more to tell you every single day my life is incomplete my rites are absolutely gone so wake me up before you leave today something i need to say cause they'll be nothing when you're gone

Aβ42 Mutants with Different Aggregation Profiles Induce Distinct Pathologies in

by Koichi Iijima, Hsueh-Cheng Chiang, Stephen A. Hearn, Inessa Hakker, Anthony Gatt, Christopher Shenton, Linda Granger, Amy Leung, Kanae Iijima-Ando, Yi Zhong

Aggregation of the amyloid-β-42 (Aβ42) peptide in the brain parenchyma is a pathological hallmark of Alzheimer's disease (AD), and the prevention of Aβ aggregation has been proposed as a therapeutic intervention in AD. However, recent reports indicate that Aβ can form several different prefibrillar and fibrillar aggregates and that each aggregate may confer different pathogenic effects, suggesting that manipulation of Aβ42 aggregation may not only quantitatively but also qualitatively modify brain pathology. Here, we compare the pathogenicity of human Aβ42 mutants with differing tendencies to aggregate. We examined the aggregation-prone, EOFAD-related Arctic mutation (Aβ42Arc) and an artificial mutation (Aβ42art) that is known to suppress aggregation and toxicity of Aβ42 in vitro. In the Drosophila brain, Aβ42Arc formed more oligomers and deposits than did wild type Aβ42, while Aβ42art formed fewer oligomers and deposits. The severity of locomotor dysfunction and premature death positively correlated with the aggregation tendencies of Aβ peptides. Surprisingly, however, Aβ42art caused earlier onset of memory defects than Aβ42. More remarkably, each Aβ induced qualitatively different pathologies. Aβ42Arc caused greater neuron loss than did Aβ42, while Aβ42art flies showed the strongest neurite degeneration. This pattern of degeneration coincides with the distribution of Thioflavin S-stained Aβ aggregates: Aβ42Arc formed large deposits in the cell body, Aβ42art accumulated preferentially in the neurites, while Aβ42 accumulated in both locations. Our results demonstrate that manipulation of the aggregation propensity of Aβ42 does not simply change the level of toxicity, but can also result in qualitative shifts in the pathology induced in vivo.

[ Idiomas ] : Nesesito la traduccion de esta rola porfa ayudenme?

Title: Take It Like A Man I get a little bit vicious Thats why you love me Because you can't resist it You do anything for me You want out but we're off the ground So pick out your parachute Cause I'm not gonna let you down I won't let you get away its not that easy anyway I don't want to know and I want you for the cause How does anybody get anything done? You depend on us You'll never get to heaven as the radical son Just keep it up you soldier You won't help I can't help I've got to make you understand You gotta take it like a man Do you need a dozen roses Would you like a box of chocolate? Is it really such a deep cut That I have to come and stitch it up Yeah I get a little crazy with the razor blades Go on and call your mama if you need a band-aid But everything worth it hurts a little bit You don't want to run away, and I wont let you anyway 'Cause were doing it for the cause How do you suppose I get anything done? You're making it so hard You'll never get to heaven as the radical son Keep it up soldier You won't help I cant help I've got to make you understand You gotta take it like a man I want you for the cause How does anybody get anything done? You depend on us You'll never get to heaven as the radical son Don't be running off Cause this is love What did you think it was? Ooh.The thing is love, love So don't go! You won't help I cant help I've got to make you understand You gotta take it like a man Take it like a man You gotta take it like a man

Generalization Mediates Sensitivity to Complex Odor Features in the Honeybee

by Geraldine A. Wright, Sonya M. Kottcamp, Mitchell G. A. Thomson

Animals use odors as signals for mate, kin, and food recognition, a strategy which appears ubiquitous and successful despite the high intrinsic variability of naturally-occurring odor quantities. Stimulus generalization, or the ability to decide that two objects, though readily distinguishable, are similar enough to afford the same consequence [1], could help animals adjust to variation in odor signals without losing sensitivity to key inter-stimulus differences. The present study was designed to investigate whether an animal's ability to generalize learned associations to novel odors can be influenced by the nature of the associated outcome. We use a classical conditioning paradigm for studying olfactory learning in honeybees [2] to show that honeybees conditioned on either a fixed- or variable-proportion binary odor mixture generalize learned responses to novel proportions of the same mixture even when inter-odor differences are substantial. We also show that the resulting olfactory generalization gradients depend critically on both the nature of the stimulus-reward paradigm and the intrinsic variability of the conditioned stimulus. The reward dependency we observe must be cognitive rather than perceptual in nature, and we argue that outcome-dependent generalization is necessary for maintaining sensitivity to inter-odor differences in complex olfactory scenes.

Natural Variation in as a Tool for Highlighting Differential Drought Responses

by Oumaya Bouchabke, Fengqi Chang, Matthieu Simon, Roger Voisin, Georges Pelletier, Mylène Durand-Tardif

To test whether natural variation in Arabidopsis could be used to dissect out the genetic basis of responses to drought stress, we characterised a number of accessions. Most of the accessions belong to a core collection that was shown to maximise the genetic diversity captured for a given number of individual accessions in Arabidopsis thaliana. We measured total leaf area (TLA), Electrolyte Leakage (EL), Relative Water Content (RWC), and Cut Rosette Water Loss (CRWL) in control and mild water deficit conditions. A Principal Component Analysis revealed which traits explain most of the variation and showed that some accessions behave differently compared to the others in drought conditions, these included Ita-0, Cvi-0 and Shahdara. This study relied on genetic variation found naturally within the species, in which populations are assumed to be adapted to their environment. Overall, Arabidopsis thaliana showed interesting phenotypic variations in response to mild water deficit that can be exploited to identify genes and alleles important for this complex trait.

Healthy Lifestyle Behaviour Decreasing Risks of Being Bullied, Violence and Injury

by Amelia R. Turagabeci, Keiko Nakamura, Takehito Takano

Background

Bullying and violence are problems of aggression in schools among adolescents. Basic daily healthy practices including nutritious diet, hygiene and physical activity are common approaches in comprehensive health promotion programs in school settings, however thier relationship to these aggressive behaviours is vague. We attempted to show the advantages of these healthy lifestyle behaviours in 9 developing countries by examining the association with being frequently bullied, violence and injury.

Methodology/Principal Findings

A cross-sectional cross-national survey of 9 countries using the WHO Global School Based Student Health Survey dataset was used. Measurements included experiences of "being frequently bullied" in the preceding 30 days and violence/injury in the past 12 months. Association of risk behaviours (smoking, alcohol, sexual behaviour) and healthy lifestyle (nutrition, hygiene practices, physical activity) to being bullied, and violence/injury were assessed using multivariate logistic regression. Hygiene behaviour showed lower risks of being frequently bullied [male: RR = 0.7 (97.5CI: 0.5, 0.9); female: RR = 0.6 (0.5, 0.8)], and lower risk of experiences of violence/injury [RR = 0.7 (0.5, 0.9) for males], after controlling for risk behaviours, age, education, poverty, and country.

Conclusion/Significance

Healthy lifestyle showed an association to decreased relative risk of being frequently bullied and violence/injury in developing countries. A comprehensive approach to risk and health promoting behaviours reducing bullying and violence is encouraged at school settings.

Poor Reporting of Scientific Leadership Information in Clinical Trial Registers

by Melanie Sekeres, Jennifer L. Gold, An-Wen Chan, Joel Lexchin, David Moher, Marleen L. P. Van Laethem, James Maskalyk, Lorraine Ferris, Nathan Taback, Paula A. Rochon

Background

In September 2004, the International Committee of Medical Journal Editors (ICMJE) issued a Statement requiring that all clinical trials be registered at inception in a public register in order to be considered for publication. The World Health Organization (WHO) and ICMJE have identified 20 items that should be provided before a trial is considered registered, including contact information. Identifying those scientifically responsible for trial conduct increases accountability. The objective is to examine the proportion of registered clinical trials providing valid scientific leadership information.

Methodology/Principal Findings

We reviewed clinical trial entries listing Canadian investigators in the two largest international and public trial registers, the International Standard Randomized Controlled Trial Number (ISRCTN) register, and ClinicalTrials.gov. The main outcome measures were the proportion of clinical trials reporting valid contact information for the trials' Principal Investigator (PI)/Co-ordinating Investigator/Study Chair/Site PI, and trial e-mail contact address, stratified by funding source, recruiting status, and register. A total of 1388 entries (142 from ISRCTN and 1246 from ClinicalTrials.gov) comprised our sample. We found non-compliance with mandatory registration requirements regarding scientific leadership and trial contact information. Non-industry and partial industry funded trials were significantly more likely to identify the individual responsible for scientific leadership (OR = 259, 95% CI: 95–701) and to provide a contact e-mail address (OR = 9.6, 95% CI: 6.6–14) than were solely industry funded trials.

Conclusions/Significance

Despite the requirements set by WHO and ICMJE, data on scientific leadership and contact e-mail addresses are frequently omitted from clinical trials registered in the two leading public clinical trial registers. To promote accountability and transparency in clinical trials research, public clinical trials registers should ensure adequate monitoring of trial registration to ensure completion of mandatory contact information fields identifying scientific leadership

Gene Expression Profiling of a Mouse Model of Pancreatic Islet Dysmorphogenesis

by Laura Wilding Crawford, Elizabeth Tweedie Ables, Young Ah Oh, Braden Boone, Shawn Levy, Maureen Gannon

Background

In the past decade, several transcription factors critical for pancreas organogenesis have been identified. Despite this success, many of the factors necessary for proper islet morphogenesis and function remain uncharacterized. Previous studies have shown that transgenic over-expression of the transcription factor Hnf6 specifically in the pancreatic endocrine cell lineage resulted in disruptions in islet morphogenesis, including dysfunctional endocrine cell sorting, increased individual islet size, increased number of peripheral endocrine cell types, and failure of islets to migrate away from the ductal epithelium. The mechanisms whereby maintained Hnf6 causes defects in islet morphogenesis have yet to be elucidated.

Methodology/Principal Findings

We exploited the dysmorphic islets in Hnf6 transgenic animals as a tool to identify factors important for islet morphogenesis. Genome-wide microarray analysis was used to identify differences in the gene expression profiles of late gestation and early postnatal total pancreas tissue from wild type and Hnf6 transgenic animals. Here we report the identification of genes with an altered expression in Hnf6 transgenic animals and highlight factors with potential importance in islet morphogenesis. Importantly, gene products involved in cell adhesion, cell migration, ECM remodeling and proliferation were found to be altered in Hnf6 transgenic pancreata, revealing specific candidates that can now be analyzed directly for their role in these processes during islet development.

Conclusions/Significance

This study provides a unique dataset that can act as a starting point for other investigators to explore the role of the identified genes in pancreatogenesis, islet morphogenesis and mature β cell function.

Promoter Demethylation Reveals the Committed Treg Population in Humans

by Peter C. J. Janson, Malin E. Winerdal, Per Marits, Magnus Thörn, Rolf Ohlsson, Ola Winqvist

Background

Naturally occurring thymus derived regulatory T cells (Tregs) are central in the maintenance of self-tolerance. The transcription factor FOXP3 is crucial for the suppressive activity of Tregs and is considered the most specific marker for this population. However, human non regulatory T cells upregulate FOXP3 transiently upon activation which calls for other means to identify the Treg population. Since epigenetic mechanisms are involved in the establishment of stable gene expression patterns during cell differentiation, we hypothesized that the methylation profile of the FOXP3 promoter would allow the distinction of truly committed Tregs.

Methodology/Principal Findings

Human CD4⁺CD25^hi Tregs displayed a demethylated FOXP3 promoter (1.4%±0.95% SEM methylated) in contrast to CD4⁺CD25^lo T cells which were partially methylated (27.9%±7.1%). Furthermore, stimulated CD4⁺CD25^lo T cells transiently expressed FOXP3 but remained partially methylated, suggesting promoter methylation as a mechanism for regulation of stable FOXP3 expression and Treg commitment. In addition, transient FOXP3 expressing cells exhibited suppressive abilities that correlate to the methylation status of the FOXP3 promoter. As an alternative to bisulphite sequencing, we present a restriction enzyme based screening method for the identification of committed Tregs and apply this method to evaluate the effect of various culturing conditions. We show that a partial demethylation occurs in long-term cultures after activation, whereas the addition of TGF-β and/or IL-10 does not induce any additional change in methylation level.

Conclusions/Significance

The unique FOXP3 promoter methylation profile in Tregs suggests that a demethylated pattern is a prerequisite for stable FOXP3 expression and suppressive phenotype. Presently, FOXP3 is used to identify Tregs in several human diseases and there are future implications for adoptive Treg transfer in immunotherapy. In these settings there is a need to distinguish true Tregs from transiently FOXP3⁺ activated T cells. The screening method we present allows this distinction and enables the identification of cells suitable for in vitro expansions and clinical use.