From d0911a04958a04042da02a334ccc528dae79cc17 Mon Sep 17 00:00:00 2001
From: zsloan
Date: Fri, 27 Mar 2015 20:28:51 +0000
Subject: Removed everything from 'web' directory except genofiles and renamed
 the directory to 'genotype_files'

---
 web/tutorial/ppt/WebQTLDemo_files/slide0043.htm | 112 ------------------------
 1 file changed, 112 deletions(-)
 delete mode 100755 web/tutorial/ppt/WebQTLDemo_files/slide0043.htm

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color:#E9EB5D'><i>Having ÒconfirmedÓ these known relations, we can </i></span></span></layer><script>
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   <td align=left colspan=1><font face=Helvetica size=3>Having worked with
   WebQTL now for 30 minutes, do we know anything new? The hypothesis that we
   have generated (but not validated) is that three transcripts: Atp6l, Gnas,
   and Ndr4 are part of a family of genes that are coregulated in normal mouse
   forebrain with App and Hsp84-1. We need to add functional and mechanistic
   significance to this hypothesis to make it biologically vibrant. But from a
   statiistical standpoint it is a strong inference.</font><br>
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  </tr>
  <tr>
   <td colspan=1></td>
   <td align=left colspan=1><br>
   </td>
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   <td align=left colspan=1><font face=Helvetica size=3>Please donÕt say: But
   these are mere correlations. A high correlation in this context has a
   biological basis. The real question is are we smart enough to understand the
   web (not chain) of causality that produced the correlation. Once we
   understand the web of causality, does it have utility? Very often the answer
   will be NO. This will often be the case when a high correlation is generated
   by linkage disequilibrium of sets of polymorphisms that modulate a set of
   mechanistically separated traits. Chromosomal linkage can produce
   correlations that are not mechanistic in the conventional sense used by
   molecular biologists. For example, clusters<span style="mso-spacerun:
   yes">&nbsp; </span>of hox transcription factor genes tend to be close
   physically to keratin gene clusters, and one might expect shared patterns of
   variance produced by this linkage in a mapping panel, no matter how large.</font><br>
   </td>
  </tr>
  <tr>
   <td colspan=1></td>
   <td align=left colspan=1><br>
   </td>
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   <td align=left colspan=1><font face=Helvetica size=3>If Affymetrix designed
   probe sets with reasonable care, if we did the experiments correctly, if we
   sampled animals appropriately, then a correlation of 0.70 or higher between
   transcripts in the brain tells you that these two transcripts are
   effectively coupled in this set of animals under this set of conditions.
   More than 50% the variance in the expression of one transcript can be
   predicted from the other. That is a major piece of information that could be
   of significant clinical, economic, and predictive value, whatever its
   causes. Yes, correlation coefficients are noisy and have large error terms,
   but we have larger n of strains coming to the rescue. Expect more than 50
   BXD lines soon.</font><br>
   </td>
  </tr>
  <tr>
   <td colspan=1></td>
   <td align=left colspan=1><br>
   </td>
  </tr>
  <tr>
   <td colspan=1></td>
   <td align=left colspan=1><font face=Helvetica size=3>This is a thin veneer
   of functional genomics. It is enough to generate some marvelous hypotheses
   in a semi-automated way.</font><br>
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