522 research outputs found

    Parallel analysis of tri-molecular biosynthesis with cell identity and function in single cells.

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    Cellular products derived from the activity of DNA, RNA, and protein synthesis collectively control cell identity and function. Yet there is little information on how these three biosynthesis activities are coordinated during transient and sparse cellular processes, such as activation and differentiation. Here, we describe Simultaneous Overview of tri-Molecule Biosynthesis (SOM3B), a molecular labeling and simultaneous detection strategy to quantify DNA, RNA, and protein synthesis in individual cells. Comprehensive interrogation of biosynthesis activities during transient cell states, such as progression through cell cycle or cellular differentiation, is achieved by partnering SOM3B with parallel quantification of select biomolecules with conjugated antibody reagents. Here, we investigate differential de novo DNA, RNA, and protein synthesis dynamics in transformed human cell lines, primary activated human immune cells, and across the healthy human hematopoietic continuum, all at a single-cell resolution

    Quantifying the Fraction of Missing Information for Hypothesis Testing in Statistical and Genetic Studies

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    Many practical studies rely on hypothesis testing procedures applied to data sets with missing information. An important part of the analysis is to determine the impact of the missing data on the performance of the test, and this can be done by properly quantifying the relative (to complete data) amount of available information. The problem is directly motivated by applications to studies, such as linkage analyses and haplotype-based association projects, designed to identify genetic contributions to complex diseases. In the genetic studies the relative information measures are needed for the experimental design, technology comparison, interpretation of the data, and for understanding the behavior of some of the inference tools. The central difficulties in constructing such information measures arise from the multiple, and sometimes conflicting, aims in practice. For large samples, we show that a satisfactory, likelihood-based general solution exists by using appropriate forms of the relative Kullback--Leibler information, and that the proposed measures are computationally inexpensive given the maximized likelihoods with the observed data. Two measures are introduced, under the null and alternative hypothesis respectively. We exemplify the measures on data coming from mapping studies on the inflammatory bowel disease and diabetes. For small-sample problems, which appear rather frequently in practice and sometimes in disguised forms (e.g., measuring individual contributions to a large study), the robust Bayesian approach holds great promise, though the choice of a general-purpose "default prior" is a very challenging problem.Comment: Published in at http://dx.doi.org/10.1214/07-STS244 the Statistical Science (http://www.imstat.org/sts/) by the Institute of Mathematical Statistics (http://www.imstat.org

    Functional neuroanatomy of spatial sound processing in Alzheimer's disease.

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    Deficits of auditory scene analysis accompany Alzheimer's disease (AD). However, the functional neuroanatomy of spatial sound processing has not been defined in AD. We addressed this using a "sparse" fMRI virtual auditory spatial paradigm in 14 patients with typical AD in relation to 16 healthy age-matched individuals. Sound stimulus sequences discretely varied perceived spatial location and pitch of the sound source in a factorial design. AD was associated with loss of differentiated cortical profiles of auditory location and pitch processing at the prescribed threshold, and significant group differences were identified for processing auditory spatial variation in posterior cingulate cortex (controls > AD) and the interaction of pitch and spatial variation in posterior insula (AD > controls). These findings build on emerging evidence for altered brain mechanisms of auditory scene analysis and suggest complex dysfunction of network hubs governing the interface of internal milieu and external environment in AD. Auditory spatial processing may be a sensitive probe of this interface and contribute to characterization of brain network failure in AD and other neurodegenerative syndromes

    Novel methods based on regression techniques to analyze multistate models and high-dimensional omics data.

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    The dissertation is based on four distinct research projects that are loosely interconnected by the common link of a regression framework. Chapter 1 provides an introductory outline of the problems addressed in the projects along with a detailed review of the previous works that have been done on them and a brief discussion on our newly developed methodologies. Chapter 2 describes the first project that is concerned with the identification of hidden subject-specific sources of heterogeneity in gene expression profiling analyses and adjusting for them by a technique based on Partial Least Squares (PLS) regression, in order to ensure a more accurate inference on the expression pattern of the genes over two different varieties of samples. Chapter 3 focuses on the development of an R package based on Project 1 and its performance evaluation with respect to other popular software dealing with differential gene expression analyses. Chapter 4 covers the third project that proposes a non-parametric regression method for the estimation of stage occupation probabilities at different time points in a right-censored multistate model data, using an Inverse Probability of Censoring (IPCW) (Datta and Satten, 2001) based version of the backfitting principle (Hastie and Tibshirani, 1992). Chapter 5 describes the fourth project which deals with the testing for the equality of the residual distributions after adjusting for available covariate information from the right censored waiting times of two groups of subjects, by using an Inverse Probability of Censoring weighted (IPCW) version of the Mann-Whitney U test
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