This menu gathers together those quality control, data manipulation, and modeling processes that are particularly useful for copy number analysis. These processes require
tall
data sets. (See
Tall and Wide Data Sets
.)
Experimental Design Data Set (EDDS)
use varies by process. Refer to their individual descriptions for more information.
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Adjusting copy number
intensity
or
count
data by subtracting control sample intensities or counts, either
within-subject
or
across sets
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Displaying
univariate
distribution
results for
variables
, with the option of computing and overlaying density estimates
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Standardizing
values of
numeric variables
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Computing correlations between numeric variables,
principal components
of the correlation matrix, an outlier analysis, and a
variance
components decomposition
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Binning
observations
into groups, reducing the total number of rows in a data set
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Fitting a
one-way repeated-measures ANOVA
linear
model
to rows of the input data set, using all combinations of different effects as
distinct groups
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Fitting a one-way repeated-measures analysis-of-variance linear model to
pairs
of input data set rows
Important
: The
bivariate
observations are assumed to have the same variance, and a correlation is modeled between them. If the
mean
or
covariance
structure is more complex than this, then you should run the
Mixed Model Analysis
process instead.
Note
: This process can be computationally intensive for large data sets, but runs faster than
Mixed Model Analysis
for identical models.
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Finding potential
breakpoints of copy number changes
across a
chromosome
using recursive partitioning
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See the
JMP Genomics Starter
main page for other process categories.