193 research outputs found

    Intersubject Regularity in the Intrinsic Shape of Human V1

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    Previous studies have reported considerable intersubject variability in the three-dimensional geometry of the human primary visual cortex (V1). Here we demonstrate that much of this variability is due to extrinsic geometric features of the cortical folds, and that the intrinsic shape of V1 is similar across individuals. V1 was imaged in ten ex vivo human hemispheres using high-resolution (200 Ī¼m) structural magnetic resonance imaging at high field strength (7 T). Manual tracings of the stria of Gennari were used to construct a surface representation, which was computationally flattened into the plane with minimal metric distortion. The instrinsic shape of V1 was determined from the boundary of the planar representation of the stria. An ellipse provided a simple parametric shape model that was a good approximation to the boundary of flattened V1. The aspect ration of the best-fitting ellipse was found to be consistent across subject, with a mean of 1.85 and standard deviation of 0.12. Optimal rigid alignment of size-normalized V1 produced greater overlap than that achieved by previous studies using different registration methods. A shape analysis of published macaque data indicated that the intrinsic shape of macaque V1 is also stereotyped, and similar to the human V1 shape. Previoud measurements of the functional boundary of V1 in human and macaque are in close agreement with these results

    MinimizaciĆ³n de la tardanza en problemas de programaciĆ³n de tareas en maquinas paralelas con deterioro de los recursos

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    En ambientes de manufactura y de servicios es frecuente encontrar diferentes tareas que son realizadas en paralelo empleando recursos heterogĆ©neos, los cuales tienen la caracterĆ­stica de sufrir deterioro a medida que transcurre el tiempo. Ese deterioro tiene un impacto significativo en el desempeƱo de dichos recursos, lo que se puede medir de diferentes formas tales, como: calidad, tiempo de proceso, entre otros. Esta investigaciĆ³n cientĆ­fica utiliza un modelo donde el deterioro de los recursos es una funciĆ³n de las tareas especĆ­ficas previamente realizadas por el recurso. La formulaciĆ³n del problema se presenta por medio de un modelo de programaciĆ³n matemĆ”tica. Este trabajo presenta dos heurĆ­sticas para resolver el problema en un tiempo razonable, donde cada heurĆ­stica emplea diferentes reglas y criterios para identificar la mejor soluciĆ³n. Un anĆ”lisis de sensibilidad, que comprende 2700 casos, es llevado a cabo para evaluar la eficacia de las heurĆ­sticas. Los resultados comprueban que las heurĆ­sticas son eficientes y generan soluciones Ćŗtiles para el tomador de decisiones.In manufacturing and service environments it is common to find processes that are performed in parallel by different resources, which have the characteristic that their performance deteriorates with time. This deterioration has a significant effect on the performance of the resources that can be measured in different forms such as quality and process time. This research utilizes a model where resource deterioration is a function of the specific jobs previously completed by the resource. The problemā€™s formulation is presented as a mathematical program. The paper presents two heuristics to solve the problem, where each has different rules to find the best solution. A sensitivity analysis that includes 2700 cases is performed to evaluate the performance of the heuristics. The results demonstrate that the heuristics are efficient and generate useful solutions for decision makers

    MinimizaciĆ³n de la tardanza en problemas de programaciĆ³n de tareas en maquinas paralelas con deterioro de los recursos

    Get PDF
    En ambientes de manufactura y de servicios es frecuente encontrar diferentes tareas que son realizadas en paralelo empleando recursos heterogĆ©neos, los cuales tienen la caracterĆ­stica de sufrir deterioro a medida que transcurre el tiempo. Ese deterioro tiene un impacto significativo en el desempeƱo de dichos recursos, lo que se puede medir de diferentes formas tales, como: calidad, tiempo de proceso, entre otros. Esta investigaciĆ³n cientĆ­fica utiliza un modelo donde el deterioro de los recursos es una funciĆ³n de las tareas especĆ­ficas previamente realizadas por el recurso. La formulaciĆ³n del problema se presenta por medio de un modelo de programaciĆ³n matemĆ”tica. Este trabajo presenta dos heurĆ­sticas para resolver el problema en un tiempo razonable, donde cada heurĆ­stica emplea diferentes reglas y criterios para identificar la mejor soluciĆ³n. Un anĆ”lisis de sensibilidad, que comprende 2700 casos, es llevado a cabo para evaluar la eficacia de las heurĆ­sticas. Los resultados comprueban que las heurĆ­sticas son eficientes y generan soluciones Ćŗtiles para el tomador de decisiones. In manufacturing and service environments it is common to find processes that are performed in parallel by different resources, which have the characteristic that their performance deteriorates with time. This deterioration has a significant effect on the performance of the resources that can be measured in different forms such as quality and process time. This research utilizes a model where resource deterioration is a function of the specific jobs previously completed by the resource. The problemā€™s formulation is presented as a mathematical program. The paper presents two heuristics to solve the problem, where each has different rules to find the best solution. A sensitivity analysis that includes 2700 cases is performed to evaluate the performance of the heuristics. The results demonstrate that the heuristics are efficient and generate useful solutions for decision makers

    Cerebrospinal fluid biomarkers of Alzheimer\u27s disease in a cohort of adults with Down syndrome

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    Introduction: Virtually all individuals with Down syndrome (DS) will develop Alzheimer\u27s disease (AD) pathology by age 40. Cerebrospinal fluid (CSF) biomarkers have characterized AD pathology in cohorts of late-onset AD (LOAD) and autosomal-dominant AD (ADAD). Few studies have evaluated such biomarkers in adults with DS. Methods: CSF concentrations of amyloid beta (AĪ²)40, AĪ²42, tau, phospho-tau181 (p-tau), neurofilament light chain (NfL), soluble triggering receptor expressed on myeloid cells 2 (sTREM2), chitinase-3-like protein 1 (YKL-40), alpha synuclein (Ī±Syn), neurogranin (Ng), synaptosomal-associated protein 25 (SNAP-25), and visinin-like protein 1 (VILIP-1) were assessed in CSF from 44 adults with DS from the Alzheimer\u27s Biomarker Consortium-Down Syndrome study. Biomarker levels were evaluated by cognitive status, age, and apolipoprotein E gene ( Results: Biomarker abnormalities indicative of amyloid deposition, tauopathy, neurodegeneration, synaptic dysfunction, and neuroinflammation were associated with increased cognitive impairment. Age and Discussion: The profile of many established and emerging CSF biomarkers of AD in a cohort of adults with DS was similar to that reported in LOAD and ADAD, while some differences were observed

    The Cortical Signature of Alzheimer's Disease: Regionally Specific Cortical Thinning Relates to Symptom Severity in Very Mild to Mild AD Dementia and is Detectable in Asymptomatic Amyloid-Positive Individuals

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    Alzheimer's disease (AD) is associated with neurodegeneration in vulnerable limbic and heteromodal regions of the cerebral cortex, detectable in vivo using magnetic resonance imaging. It is not clear whether abnormalities of cortical anatomy in AD can be reliably measured across different subject samples, how closely they track symptoms, and whether they are detectable prior to symptoms. An exploratory map of cortical thinning in mild AD was used to define regions of interest that were applied in a hypothesis-driven fashion to other subject samples. Results demonstrate a reliably quantifiable in vivo signature of abnormal cortical anatomy in AD, which parallels known regional vulnerability to AD neuropathology. Thinning in vulnerable cortical regions relates to symptom severity even in the earliest stages of clinical symptoms. Furthermore, subtle thinning is present in asymptomatic older controls with brain amyloid binding as detected with amyloid imaging. The reliability and clinical validity of AD-related cortical thinning suggests potential utility as an imaging biomarker. This ā€œdisease signatureā€ approach to cortical morphometry, in which disease effects are mapped across the cortical mantle and then used to define ROIs for hypothesis-driven analyses, may provide a powerful methodological framework for studies of neuropsychiatric diseases

    Shorter Telomeres May Mark Early Risk of Dementia: Preliminary Analysis of 62 Participants from the Nurses' Health Study

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    Background: Dementia takes decades to develop, and effective prevention will likely require early intervention. Thus, it is critical to identify biomarkers of preclinical disease, allowing targeting of high-risk subjects for preventive efforts. Since telomeres shorten with age and oxidative stress both of which are important contributors to the onset of dementia, telomere length might be a valuable biomarker. Methodology/Principal Findings: Among 62 participants of the Nurses' Health Study,we conducted neurologic evaluations, including patient and caregiver interviews physical exam, neurologic exam and neuropsychologic testing. We also conducted magnetic resonance imaging (MRI) in a sample of 29 of these women. In these preliminary data, after adjustment for numerous health and lifestyle factors, we found that truncated telomeres in peripheral blood leukocytes segregate with preclinical dementia states, including mild cognitive impairment (MRI); the odds of MCI were 12 fold higher (odds ratio = 12.00, 95% confidence interval 1.24-116.5) for those with shorter telomere length compared to longer telomere length. In addition, decreasing telomere length was strongly related to decreasing hippocampal volume (p=0.038). Conclusions: These preliminary data suggest that telomere length may be a possible early marker of dementia risk, and merits further study in large, prospective investigations

    The intrinsic shape of human and macaque primary visual cortex

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    Previous studies have reported considerable variability in primary visual cortex (V1) shape in both humans and macaques. Here, we demonstrate that much of this variability is due to the pattern of cortical folds particular to an individual and that V1 shape is similar among individual humans and macaques as well as between these 2 species. Human V1 was imaged ex vivo using high-resolution (200 mm) magnetic resonance imaging at 7 T. Macaque V1 was identified in published histological serial section data. Manual tracings of the stria of Gennari were used to construct a V1 surface, which was computationally flattened with minimal metric distortion of the cortical surface. Accurate flattening allowed investigation of intrinsic geometric features of cortex, which are largely independent of the highly variable cortical folds. The intrinsic shape of V1 was found to be similar across human subjects using both nonparametric boundary matching and a simple elliptical shape model fit to the data and is very close to that of the macaque monkey. This result agrees with predictions derived from current models of V1 topography. In addition, V1 shape similarity suggests that similar developmental mechanisms are responsible for establishing V1 shape in these 2 species
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