Hi, I have changed the path for subject directory. It causes the
error.Following is my SetUpFreeSurfer.csh What mistake did I made in?
#!/bin/tcsh -ef
#
# SetUpFreeSurfer.csh
#
# This is a sample SetUpFreeSurfer.csh file.
# Edit as needed for your specific setup.
# The defaults should wor
Dear all,
Open positions @ Brainntome Center.
http://brainnetome.org/en/recruitment.html
*Job 1: PhD Positions in Neuroimaging and Neuroscience, Beijing, China
Brainnetome Center*
*Applications Deadline: March 15 , 2015. *
*Brainnetome Center*
Brainnetome Center ( www.brainnetome.org) at
Wed Feb 4 11:53:21 KST 2015
/media/sf_F_DRIVE/ADHD200/Classification/Processed/TDC-51
/home/naveed-centos/freesurfer/bin/recon-all
-i
/media/sf_F_DRIVE/ADHD200/Classification/Original_selected/TDC/7407032/Pekin
g_7407032/Peking_7407032_1/scans/anat_1-anat/resources/NIfTI/files/rest.nii
-subject
sure, just draw an ROI in the volume (in e.g. freeview) and save it as a
.label file, then load it into tksurfer and it will get sampled onto the
surface (then save it)
On
Tue, 3 Feb 2015, rwlod...@uic.edu wrote:
> Hello!
> I was just wondering what the best way to find the cortical thickness
Hi all,
I'm using mri_cvs_register to warp a T1 (already in orig space) to the CVS
MNI152 template. The warped volume and surface look good, but my goal is to
get the equivalent of a list of voxel coordinates from the patient's native
orig volume in the template MNI152 space via the non-linear war
Hello!
I was just wondering what the best way to find the cortical thickness
under specific intracranial EEG leads is. Is this even possible? I know
freesurfer doesn't allow you to place leads onto the 3D model it
generates, but if I knew exactly where the lead was is there some way to
determine t
Is it world readable? You might also change its name to license.txt
On 2/3/15 12:13 PM, André Schmidt wrote:
Dear experts,
I like to see the obtained annotation files using tksurfer. However, I
already got the following error message if I use tksurfer HC001 lh
inflated in the terminal:
Fr
De inhoud van dit bericht is vertrouwelijk en alleen bestemd voor de
geadresseerde(n). Anderen dan de geadresseerde(n) mogen geen gebruik maken van
dit bericht, het niet openbaar maken of op enige wijze verspreiden of
vermenigvuldigen. Het UMCG kan niet aansprak
Dear experts,
I like to see the obtained annotation files using tksurfer. However, I already
got the following error message if I use tksurfer HC001 lh inflated in the
terminal:
FreeSurfer license file /Applications/freesurfer/.license not found
But there is a .license file in that folder.
Ca
Thanks, Doug.
On Tue, Feb 3, 2015 at 10:37 AM, Douglas Greve
wrote:
> Hi Corinna,
>
> In each iteration, the mc-full replaces your data (--y) with white
> gaussian noise, smoothes it, then computes the GLM and p-values from the t
> or F-test. The mc-z ignores your data entirely and creates a si
Hi Corinna,
In each iteration, the mc-full replaces your data (--y) with white
gaussian noise, smoothes it, then computes the GLM and p-values from the
t or F-test. The mc-z ignores your data entirely and creates a single
frame of WGN in each iteration, smoothes it, rescales it back to a z,
t
Just run mris_preproc on your healthy group, then run mri_segstats using
the cluster annotation from your first analysis and the HC stack as the
input. Does that make sense?
doug
On 2/3/15 9:18 AM, maaike rive wrote:
Hi all,
Does anyone know how to extract average (thickness/area/GI) value
On 2/3/15 4:21 AM, Schweren, LJS (med) wrote:
Thank you Doug!
One more question for clarification:
“You would remove the quadratic term from the FSGD file, then create
an image of quadradic values for each veretx and pass that with --pvr
to glmfit”.
My quadratic value (age-squared) is a c
There is not a way to do it from the command line. You can do it in
matlab, something like
sig = MRIread('sig.mgh');
sigmat = fast_vol2mat(sig);
p = 10^-abs(sigmat);
fdr = .05;
pthresh = fast_fdrthresh(p,fdr);
ind = find(p < pthresh); % This will be a list of ROI indices that
survive FDR
do
Hi all,
I am wondering what the specific reasons might be for choosing to run the
mc-z simulation compared to mc-full? What are the pros and cons for each
method for looking at group morphometry differences?
Thanks
Corinna
___
Freesurfer mailing list
Fr
Hi all,
Does anyone know how to extract average (thickness/area/GI) values of a cluster
A for subjects in a group which was NOT included in the model where this
cluster A emerged? For example: in a t-test for diagnosis1>dagnosis2 there is
an effect in an insulacluster (found with mri_glmfit
Hi Doug,
Sorry, the statistician doesn't understand it yet; we're currently building
freesurfer and SPSS models step by step to find out what's going on, but it's a
litte time consuming... so, to be continued!
Maaike
From: r_maaike@hotmail.comTo: freesur...@nmr.mgh.harvard.eduDate: Fri, 30
Dear users,
I writhe in the hope somebody encountered a similar problem.
I have individual normalized maps of intrinisc brain networks from a dual
regression. This maps are projected back into individual subject space and
further into individual surface space. Finally I normalize this maps into
Thank you Doug!
One more question for clarification:
"You would remove the quadratic term from the FSGD file, then create an image
of quadradic values for each veretx and pass that with --pvr to glmfit".
My quadratic value (age-squared) is a constant per participant. Do you mean I
should creat
Hello!
Thanks. I realized that vertices are added at the end when increasing
resolution, what I was asking about is more about the details of the
subsampling procedure, eg. what's the vertex number of the new vertex created
on the edge between vertices n and m when doing a icosahedral subdivisi
20 matches
Mail list logo
