Displaying 20 results from an estimated 186 matches for "genotypic".
2007 Oct 02
1
Trouble obtaining results from a loop
#Hello,
#I have a question about obtaining results from a loop I have written.
#Below is a sample of individual genotypes from a genetic question I am
working on called "P.genotype.sample ".
P.genotype.sample<-matrix(10,10,10)
P.genotype.sample[,1]<-c(2,2,1,5,1,1,5,6,1,3)
P.genotype.sample[,2]<-c(6,3,3,6,8,1,6,7,2,3)
P.genotype.sample[,3]<-c(2,2,2,3,3,2,2,2,3,3)
2007 Sep 26
1
Paste a matrix column in pairwise fashion with other columns?
#Hello,
#I have would like to paste a single column of a matrix
# in pair wise fashion with other columns based upon
# even and odd column numbers.
# I can do it in a very clunky fashion and I know there
# must be a better way. below is a sample matrix and my extremely
# clunky code that gets the job done for a small matrix, but i plan to
# do this on a much grander scale. any help would be very
2006 Feb 15
1
no convergence using lme
Hi. I was wondering if anyone might have some suggestions about how I can
overcome a problem of "iteration limit reached without convergence" when
fitting a mixed effects model.
In this study:
Outcome is a measure of heart action
Age is continuous (in weeks)
Gender is Male or Female (0 or 1)
Genotype is Wild type or knockout (0 or 1)
Animal is the Animal ID as a factor
2008 Aug 20
4
Looping over groups
Hello,
My R skills are somewhere between novice and intermediary, and I am hoping that some of you very helpful forum members, whom I've seen work your magic on other peoples' problems/questions, can help me here.
I have a matrix with the following format:
(i) individual plants comprising many different genotype groups (i.e., a plant is genotype 1 or genotype 2 or genotype 3, etc). The
2010 Oct 09
1
question related to multiple regression
Hi,
I am conducting an association analysis of genotype and a phenotype such as
cholesterol level as an outcome and the genotype as a regressor using
multiple linear regression. There are 3 possibilities for the genotype AA,
AG, GG. There are 5 people with the AA genotype, 100 with the AG genotype
and 900 with the GG genotype. I coded GG genotype as 1, AG as 2 and AA as 3
and the p-value for the
2005 Apr 21
2
ANOVA model
Hi,
Could someone tell me if this is the correct model syntax for the
following dataset:
lme(height~treatment+genotype+treatment*genotype,drought,random=~genotyp
e)
The dataset has two factors: one fixed - treatment, and one random -
genotype. I need to test the effect of both factors to identify their
significance. There are multiple (but not equal) replicates at each
level of genotype (the
2011 Mar 08
1
NaNs in Nested Mixed Model
Dear R users,
I have a problem with something called "NaNs" in a nested mixed model.
The background is that I have studied the number of insect nymphs
emerging from replicated Willow genotypes in the field. I have 15
replicates each of 4 Willow genotypes belonging two 2 Willow species.
Now I want to elucidate the effect of Willow genotype on the number of
emerging nymphs. Previously I
2010 Sep 03
3
define colors for groups in lattice xyplot
Dear all,
Lattice provides automatic coloring for subgroups on each panel by the
simple use of a groups statement. For an application I want to change
these colors to a predifined set. This works well using a panel function
in stead of the default as long as there are only points in the graphs.
When I set type="b" things get messed up. Any idea why? I include sample
code for
2005 Jul 05
0
plot legend outside the grid
Thanks Bert for all the help. I got the legend figured out Friday but left early becoz of long weekend so didn't get a chance to reply.. I modified the plot margins a little bit and Here's what I finally had...
par(mar=c(c(10, 6, 6, 10) + 0.1));
par(xpd=FALSE);
with (dataFrame, stripchart(marbles_buried ~ genotype, method="jitter", vertical=TRUE, col = c('blue',
2005 Jun 30
1
FW: plot legend outside the grid
-----Original Message-----
From: Ghosh, Sandeep
Sent: Thursday, June 30, 2005 5:43 PM
To: 'Berton Gunter'
Subject: plot legend outside the grid
Thanks for the pointers... I managed to get everything to look and feel the way I want except for the legend to plot outside the grid... Thanks for the note on the par, but I'm not able to it to plot outside the plot grid..
dataFrame <-
2004 Nov 21
1
Two factor ANOVA in lme
I want to specify a two-factor model in lme, which should be easy?
Here's what I have:
factor 1 - treatment FIXED (two levels)
factor 2 - genotype RANDOM (160 genotypes in total)
I need a model that tells me whether the treatment, genotype and
interaction terms are significant. I have been reading 'Mixed effects
models in S' but in all examples the random factor is not in the main
2003 Apr 08
2
Basic LME
Hello R Users,
I am investigating the basic use of the LME function, using the following example;
Response is Weight, covariate is Age, random factor is Genotype
model.lme <- lme (Weight~Age, random=~ 1|Genotype)
After summary(model.lme), I find that the estimate of Age is 0.098 with p=0.758.
I am comparing the above model with the AOV function;
model.aov <- aov (Weight~Age + Genotype)
2003 May 22
3
How to avoid function masking
Hi All,
I've been working on updating the 'genetics' package. As a consequence of
the upgrade, .First.lib() looks like:
.First.lib <- function(libname, pkgname)
{
if (!require(combinat))
warning("Unable to load 'combinat' library. Function
`diseq.ci' will fail.")
require(gregmisc)
genotype <-
2011 Apr 20
1
avoiding if-then statements for looped chi-square tests
Hi,
I am trying to test for pairwise associations between genotypes (
Rows=individuals, Columns =genes, data are up to 4 genotypes per gene, some
with 2,3 or 4) where each chisquare comparison is different depending on the
genes tested. The test is the observed multilocus (across columns for each
individual) genotypes vs the expectation, which is the product of the
individual frequency for each
2007 Jul 23
1
problems with character objects and calls to list()
Hi All,
I have a problem trying to get a set of columns recognised as a list
and can't work out how to do it despite trawling through the mailing
list archives, and docs.
A short example...
to.convert <- NULL
n <- 6
for(x in 1:n){
to.convert <- paste(to.convert, paste((2 * x) -1, (2 * x), sep=":"), sep=",")
}
to.convert <- gsub("^,", "",
2012 Nov 03
2
reorder() in the latticeExtra library
Hello all, thanks for your time and help. Below are my commands, and it
generates a really nice plot, however I am not happy with the reorder()
function. I would like the order to be the same as they appear in the
genotype variable "genotype <- c("CJ1450 NW 4/25/12","CJ1450 BAL
4/25/12","CJ1450 NW 4/27/12","CJ1450 BAL 4/27/12","CJ1721 NW
2013 Jul 02
2
Recoding variables based on reference values in data frame
I'm new to R (previously used SAS primarily) and I have a genetics data
frame consisting of genotypes for each of 300+ subjects (ID1, ID2, ID3,
...) at 3000+ genetic locations (SNP1, SNP2, SNP3...). A small subset of
the data is shown below:
SNP_ID SNP1 SNP2 SNP3 SNP4 Maj_Allele C G C A Min_Allele T A T G ID1
CC GG CT AA ID2 CC GG CC AA ID3 CC GG
nc
AA
2002 Nov 01
0
Re: gregmisc version 0.7.3 now available
> From: kjetil halvorsen [mailto:kjetilh at umsanet.edu.bo]
>
> Martin Hoyle wrote:
> >
> > Dear Greg,
> > Thanks for the new release. The decomposition of the SSQ is
> just what I need!
> >
> I thought decomposition of the SSQ can be obtained with the split=
> argument to summary.aov? That argument seems tro be new --- it didnt
> exist two years
2006 Dec 29
1
Genotypes are not all the same
I have been merrily using the genetics package and more specifically have
been using the makeGenotypes and genotypes function. I check my
accomplishments by going
> class(g2)
[1] "genotype" "factor"
and likewise
> class(g1)
[1] "genotype" "factor"
Yet when I execute a command such as allele count I get this
> allele.count(g1)
D I
[1,]
2006 Dec 31
1
Genotype importing from Sequenom
Sequenom has an odd format of calling a SNP genotype
gg
[1] "C" "GA" "A" "C" "C" "AG" "C" "C" "T" "G"
homozygous A is called A and heterozygous is called AT
The genetics package cannot handle the fact that some genotypes are declared
with 2 letter while other are declared with only 1.