From ea46f42ee640928b92947bfb204c41a482d80937 Mon Sep 17 00:00:00 2001 From: root Date: Tue, 8 May 2012 18:39:56 -0500 Subject: Add all the source codes into the github. --- .../webqtl_demo2_part1.ppt_files/Slide0001.gif | Bin 0 -> 89129 bytes .../webqtl_demo2_part1.ppt_files/Slide0002.gif | Bin 0 -> 88189 bytes .../webqtl_demo2_part1.ppt_files/Slide0003.gif | Bin 0 -> 79744 bytes .../webqtl_demo2_part1.ppt_files/Slide0004.gif | Bin 0 -> 99835 bytes .../webqtl_demo2_part1.ppt_files/Slide0005.gif | Bin 0 -> 87507 bytes .../webqtl_demo2_part1.ppt_files/Slide0006.gif | Bin 0 -> 99731 bytes .../webqtl_demo2_part1.ppt_files/Slide0007.gif | Bin 0 -> 74135 bytes .../webqtl_demo2_part1.ppt_files/Slide0008.gif | Bin 0 -> 72580 bytes .../webqtl_demo2_part1.ppt_files/Slide0009.gif | Bin 0 -> 46338 bytes .../webqtl_demo2_part1.ppt_files/Slide0010.gif | Bin 0 -> 53010 bytes .../webqtl_demo2_part1.ppt_files/Slide0011.gif | Bin 0 -> 87161 bytes .../webqtl_demo2_part1.ppt_files/Slide0012.gif | Bin 0 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This presentation contains content that your browser is unable to display. This presentation was optimized for the recent version of Microsoft Internet Explorer and Netscape Navigator 4.

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Memphis Microarray 2003
June 11, 2003, Rob Williams
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GeneNetwork and WebQTL:
Slide 2
Slide 3
Search results
"First page of data:"
"Data sources:"
"Expression estimates for App on..."
"Critiquing the App data the..."
"App expression after windsorizing"
"Discovering shared expression patterns"
"Transcript neighborhoods"
"App and Atcay transcript scatterplot"
"App transcript and eight of..."
App transcript coexpression neighborhood
"Correlations of App with classical..."
"Network Graph of App with..."
"Summary of Part 1:"
Contact for comments and improvements:
\ No newline at end of file diff --git a/web/tutorial/ppt/html/webqtl_demo2_part1.ppt_files/outline_expand.gif b/web/tutorial/ppt/html/webqtl_demo2_part1.ppt_files/outline_expand.gif new file mode 100755 index 00000000..c8c72b13 Binary files /dev/null and b/web/tutorial/ppt/html/webqtl_demo2_part1.ppt_files/outline_expand.gif differ diff --git a/web/tutorial/ppt/html/webqtl_demo2_part1.ppt_files/outline_expanded.htm b/web/tutorial/ppt/html/webqtl_demo2_part1.ppt_files/outline_expanded.htm new file mode 100755 index 00000000..a45e9c0c --- /dev/null +++ b/web/tutorial/ppt/html/webqtl_demo2_part1.ppt_files/outline_expanded.htm @@ -0,0 +1,5 @@ +
GeneNetwork and WebQTL:
Part 1: How to study expression variation and covariation (slides 2–16)
Part 2. Discovering upstream modulators (slides 17–30)

Slide 2
Slide 3
Search results
"First page of data:"
First page of data: The Trait Data and Analysis Form

"Data sources:"
Data sources: Metadata for each resource

"Expression estimates for App on..."
Expression estimates for App on the Trait Data form

"Critiquing the App data the..."
Critiquing the App data the Trait Data

"App expression after windsorizing"
App expression after windsorizing

"Discovering shared expression patterns"
Discovering shared expression patterns

"Transcript neighborhoods"
Transcript neighborhoods

"App and Atcay transcript scatterplot"
App and Atcay transcript scatterplot

"App transcript and eight of..."
App transcript and eight of its neighbors

App transcript coexpression neighborhood
"Correlations of App with classical..."
Correlations of App with classical traits

"Network Graph of App with..."
Network Graph of App with classical traits

"Summary of Part 1:"
Summary of Part 1:

Contact for comments and improvements:
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' + ENDSHOW_MESG + '

') + doc.close() +} +function SetSldVisited(){ gDocTable[gCurSld-1].mVisited=true } +function IsSldVisited(){ return gDocTable[gCurSld-1].mVisited } +function hrefList( sldHref, visible, sldIdx ) +{ + this.mSldHref= this.mNtsHref = sldHref + this.mSldIdx = sldIdx + this.mOrigVis= this.mVis = visible + this.mVisited= false +} +var gDocTable = new Array( + new hrefList("slide0001.htm", 1, 1), + new hrefList("slide0002.htm", 1, 2), + new hrefList("slide0003.htm", 1, 3), + new hrefList("slide0004.htm", 1, 4), + new hrefList("slide0005.htm", 1, 5), + new hrefList("slide0006.htm", 1, 6), + new hrefList("slide0007.htm", 1, 7), + new hrefList("slide0008.htm", 1, 8), + new hrefList("slide0009.htm", 1, 9), + new hrefList("slide0010.htm", 1, 10), + new hrefList("slide0011.htm", 1, 11), + new hrefList("slide0012.htm", 1, 12), + new hrefList("slide0013.htm", 1, 13), + new hrefList("slide0014.htm", 1, 14), + new hrefList("slide0015.htm", 1, 15), + new hrefList("slide0016.htm", 1, 16), + new hrefList("slide0017.htm", 1, 17), + new hrefList("slide0018.htm", 1, 18) +); + +function ImgBtn( oId,bId,w,action ) +{ + var t=this + t.Perform = _IBP + t.SetActive = _IBSetA + t.SetInactive= _IBSetI + t.SetPressed = _IBSetP + t.SetDisabled= _IBSetD + t.Enabled = _IBSetE + t.ChangeIcon = null + t.UserAction = action + t.ChgState = _IBUI + t.mObjId = oId + t.mBorderId= bId + t.mWidth = w + t.mIsOn = t.mCurState = 0 +} +function _IBSetA() +{ + if( this.mIsOn ) { + obj=this.ChgState( gHiliteClr,gShadowClr,2 ) + obj.style.posTop=0 + } +} +function _IBSetI() +{ + if( this.mIsOn ) { + obj=this.ChgState( gFaceClr,gFaceClr,1 ) + obj.style.posTop=0 + } +} +function _IBSetP() +{ + if( this.mIsOn ) { + obj=this.ChgState( gShadowClr,gHiliteClr,2 ) + obj.style.posLeft+=1; obj.style.posTop+=1 + } +} +function _IBSetD() +{ + obj=this.ChgState( gFaceClr,gFaceClr,0 ) + obj.style.posTop=0 +} +function _IBSetE( state ) +{ + var t=this + GetObj( t.mBorderId ).style.visibility="visible" + if( state != t.mIsOn ) { + t.mIsOn=state + if( state ) + t.SetInactive() + else + t.SetDisabled() + } +} +function _IBP() +{ + var t=this + if( t.mIsOn ) { + if( t.UserAction != null ) + t.UserAction() + if( t.ChangeIcon ) { + obj=GetObj(t.mObjId) + if( t.ChangeIcon() ) + obj.style.posLeft=obj.style.posLeft+(t.mCurState-4)*t.mWidth + else + obj.style.posLeft=obj.style.posLeft+(t.mCurState-0)*t.mWidth + } + t.SetActive() + } +} +function _IBUI( clr1,clr2,nextState ) +{ + var t=this + SetBorder( GetObj( t.mBorderId ),clr1,clr2 ) + obj=GetObj( t.mObjId ) + obj.style.posLeft=obj.style.posLeft+(t.mCurState-nextState)*t.mWidth-obj.style.posTop + t.mCurState=nextState + return obj +} +function TxtBtn( oId,oeId,action,chkState ) +{ + var t=this + t.Perform = _TBP + t.SetActive = _TBSetA + t.SetInactive= _TBSetI + t.SetPressed = _TBSetP + t.SetDisabled= _TBSetD + t.SetEnabled = _TBSetE + t.GetState = chkState + t.UserAction = action + t.ChgState = _TBUI + t.mObjId = oId + t.m_elementsId= oeId + t.mIsOn = 1 +} +function _TBSetA() +{ + var t=this + if( t.mIsOn && !t.GetState() ) + t.ChgState( gHiliteClr,gShadowClr,0,0 ) +} +function _TBSetI() +{ + var t=this + if( t.mIsOn && !t.GetState() ) + t.ChgState( gFaceClr,gFaceClr,0,0 ) +} +function _TBSetP() +{ + if( this.mIsOn ) + this.ChgState( gShadowClr,gHiliteClr,1,1 ) +} +function _TBSetD() +{ + this.ChgState( gFaceClr,gFaceClr,0,0 ) + this.mIsOn = 0 +} +function _TBSetE() +{ + var t=this + if( !t.GetState() ) + t.ChgState( gFaceClr,gFaceClr,0,0 ) + else + t.ChgState( gShadowClr,gHiliteClr,1,1 ) + t.mIsOn = 1 +} +function _TBP() +{ + var t=this + if( t.mIsOn ) { + if( t.UserAction != null ) + t.UserAction() + if( t.GetState() ) + t.SetPressed() + else + t.SetActive() + } +} +function _TBUI( clr1,clr2,lOffset,tOffset ) +{ + SetBorder( GetObj( this.mObjId ),clr1,clr2 ) + Offset( GetObj( this.m_elementsId ),lOffset,tOffset ) +} +function GetObj( objId ){ return document.all.item( objId ) } +function Offset( obj, top, left ){ obj.style.top=top; obj.style.left=left } +function SetBorder( obj, upperLeft, lowerRight ) +{ + s=obj.style; + s.borderStyle = "solid" + s.borderWidth = 1 + s.borderLeftColor = s.borderTopColor = upperLeft + s.borderBottomColor= s.borderRightColor = lowerRight +} +function GetBtnObj(){ return gBtnArr[window.event.srcElement.id] } +function BtnOnOver(){ b=GetBtnObj(); if( b != null ) b.SetActive() } +function BtnOnDown(){ b=GetBtnObj(); if( b != null ) b.SetPressed() } +function BtnOnOut(){ b=GetBtnObj(); if( b != null ) b.SetInactive() } +function BtnOnUp() +{ + b=GetBtnObj() + if( b != null ) + b.Perform() + else + Upd() +} +function GetNtsState(){ return parent.gNtsOpen } +function GetOtlState(){ return parent.gOtlOpen } +function GetOtlTxtState(){ return parent.gOtlTxtExp } +function NtsBtnSetFlag( fVal ) +{ + s=document.all.item( this.m_flagId ).style + s.display="none" + if( fVal ) + s.display="" + else + s.display="none" +} + +var gHiliteClr="THREEDHIGHLIGHT",gShadowClr="THREEDSHADOW",gFaceClr="THREEDFACE" +var gBtnArr = new Array() +gBtnArr["nb_otl"] = new TxtBtn( "nb_otl","nb_otlElem",parent.ToggleOtlPane,GetOtlState ) +gBtnArr["nb_nts"] = new TxtBtn( "nb_nts","nb_ntsElem",parent.ToggleNtsPane,GetNtsState ) +gBtnArr["nb_prev"]= new ImgBtn( "nb_prev","nb_prevBorder",30,parent.GoToPrevSld ) +gBtnArr["nb_next"]= new ImgBtn( "nb_next","nb_nextBorder",30,parent.GoToNextSld ) +gBtnArr["nb_sldshw"]= new ImgBtn( "nb_sldshw","nb_sldshwBorder",18,parent.FullScreen ) +gBtnArr["nb_voice"] = new ImgBtn( "nb_voice","nb_voiceBorder",18,parent.ToggleVNarration ) +gBtnArr["nb_otlTxt"]= new ImgBtn( "nb_otlTxt","nb_otlTxtBorder",23,parent.ToggleOtlText ) +gBtnArr["nb_nts"].m_flagId= "notes_flag" +gBtnArr["nb_nts"].SetFlag = NtsBtnSetFlag +gBtnArr["nb_otlTxt"].ChangeIcon= GetOtlTxtState +var sNext="Next",sPrev="Previous",sEnd="End Show",sFont="Arial", alwaysOn = false +function ShowMenu() +{ + BuildMenu(); + var doc=PPTSld.document.body,x=PPTSld.event.clientX+doc.scrollLeft,y=PPTSld.event.clientY+doc.scrollTop + + m = PPTSld.document.all.item("ctxtmenu") + m.style.pixelLeft=x + if( (x+m.scrollWidth > doc.clientWidth)&&(x-m.scrollWidth > 0) ) + m.style.pixelLeft=x-m.scrollWidth + + m.style.pixelTop=y + if( (y+m.scrollHeight > doc.clientHeight)&&(y-m.scrollHeight > 0) ) + m.style.pixelTop=y-m.scrollHeight + + m.style.display="" +} +function _CM() +{ + if( !parent.IsFullScrMode() && !alwaysOn) return; + + if(!PPTSld.event.ctrlKey) { + ShowMenu() + return false + } else + HideMenu() +} + +function processNavKPH(event) { + if ( PPTSld && (event.keyCode != 13 || !event.srcElement.href || event.srcElement.href == "" ) ) + return PPTSld._KPH(event); +} +function processNavClick() { + HideMenu(); + return true; +} +function BuildMenu() +{ + if( PPTSld.document.all.item("ctxtmenu") ) return + + var mObj=CreateItem( PPTSld.document.body ) +mObj.id="ctxtmenu" + var s=mObj.style + s.position="absolute" + s.cursor="default" + s.width="100px" + SetCMBorder(mObj,"menu","black") + + var iObj=CreateItem( mObj ) + SetCMBorder( iObj, "threedhighlight","threedshadow" ) + iObj.style.padding=2 + if ( self.IsFullScrMode() ) { + CreateMenuItem( iObj,sNext,M_GoNextSld,M_True ) + CreateMenuItem( iObj,sPrev,M_GoPrevSld,M_HasPrevSld ) + } + else { + CreateMenuItem( iObj,sNext, base.TP_GoToNextSld, base.HasNextSld ) + CreateMenuItem( iObj,sPrev,base.GoToPrevSld, base.HasPrevSld ) + } + var sObj=CreateItem( iObj ) + SetCMBorder(sObj,"menu","menu") + var s=sObj.style + s.borderTopColor="threedshadow" + s.borderBottomColor="threedhighlight" + s.height=1 + s.fontSize="0px" + if ( self.IsFullScrMode() ) + CreateMenuItem( iObj,sEnd,M_End,M_True ) + else + CreateMenuItem( iObj,sEnd,M_End,M_False ) +} +function Highlight() { ChangeClr("activecaption","threedhighlight") } +function Deselect() { ChangeClr("threedface","menutext") } +function Perform() +{ + e=PPTSld.event.srcElement + if( e.type=="menuitem" && e.IsActive() ) + e.Action() + else + PPTSld.event.cancelBubble=true +} +function ChangeClr( bg,clr ) +{ + e=PPTSld.event.srcElement + if( e.type=="menuitem" && e.IsActive() ) { + e.style.backgroundColor=bg + e.style.color=clr + } +} + +function M_HasPrevSld() { return( base.HasPrevSld() ) } +function M_GoNextSld() { + base.SetFSMode(1); + if( gIsEndShow ) + M_End(); + else { + if ( base.HasNextSld() ) + base.GoToNextSld(); + else if ( base.EndSlideShow ) { + StartEndShow(); + gIsEndShow = 1; + + PPTNav.location.reload(); + } + else + base.CloseFullScreen(); + } +} +function M_GoPrevSld() { + base.SetFSMode(1); + g_hideNav = 0; + if( gIsEndShow ) { + gIsEndShow = 0; + if ( base.msie > 0 && IsMac() ) + ChangeFrame( SLIDE_FRAME, GetHrefObj( g_currentSlide ).m_slideHref ); + else + PPTSld.history.back(); + + PPTNav.location.reload(); + if( PPTSld.event ) + PPTSld.event.cancelBubble=true; + } + else + base.GoToPrevSld(); +} +function M_True() { return true } +function M_False() { return false } + +function M_End() { + base.CloseFullScreen(); + /*PPTSld.event.cancelBubble=true; + window.close( self )*/ +} + +function CreateMenuItem( node,text,action,eval ) +{ + var e=CreateItem( node ) + e.type="menuitem" + e.Action=action + e.IsActive=eval + e.innerHTML=text + + if( !e.IsActive() ) + e.style.color="threedshadow" + e.onclick=Perform + e.onmouseover=Highlight + e.onmouseout=Deselect + s=e.style; + s.fontFamily=sFont + s.fontSize="8pt" + s.paddingLeft=2 +} +function CreateItem( node ) +{ + var elem=PPTSld.document.createElement("DIV") + node.insertBefore( elem ) + return elem +} +function SetCMBorder( o,ltClr,rbClr ) +{ + var s=o.style + s.backgroundColor="menu" + s.borderStyle="solid" + s.borderWidth=1 + s.borderColor=ltClr+" "+rbClr+" "+rbClr+" "+ltClr +} + +/* netscape context menu */ +g_ctxmenu = 0; +function setRect( obj, X, Y, W, H ) { + obj.top = Y; + obj.left = X; + obj.clip.top = 0; + obj.clip.left = 0; + obj.clip.bottom = H; + obj.clip.right = W; +} + +function KPH(event) { + if ( ! base.IsFullScrMode() && !alwaysOn ) + return true; + + if ( (!IsMac() &&event.which == 3) || ( IsMac() && (event.modifiers & Event.CONTROL_MASK) && event.which == 1 ) ) { + PPTSld.g_ctxmenu = 1; + PPTSld.stripUobj.visibility = "show"; + PPTSld.stripDobj.visibility = "show"; + PPTSld.shadeUobj.visibility = "show"; + PPTSld.shadeDobj.visibility = "show"; + PPTSld.panelobj.visibility = "show"; + PPTSld.Fobj.visibility = "show"; + PPTSld.Bobj.visibility = "show"; + PPTSld.Eobj.visibility = "show"; + + setRect(PPTSld.shadeUobj, event.pageX-2, event.pageY-2, 82, 67 ); + setRect(PPTSld.shadeDobj, event.pageX, event.pageY, 82, 67 ); + setRect(PPTSld.panelobj, event.pageX, event.pageY, 80, 65 ); + setRect(PPTSld.Fobj, event.pageX, event.pageY, 80, 20 ); + setRect(PPTSld.Bobj, event.pageX, event.pageY+20, 80, 20 ); + setRect(PPTSld.stripUobj, event.pageX, event.pageY+41, 80, 1 ); + setRect(PPTSld.stripDobj, event.pageX, event.pageY+43, 80, 1 ); + setRect(PPTSld.Eobj, event.pageX, event.pageY+45, 80, 20 ); + return false; + } + if ( HitOK( event ) ) { + PPTSld.g_ctxmenu = 0; + PPTSld.stripUobj.visibility = "hide"; + PPTSld.stripDobj.visibility = "hide"; + PPTSld.shadeUobj.visibility = "hide"; + PPTSld.shadeDobj.visibility = "hide"; + PPTSld.panelobj.visibility = "hide"; + PPTSld.Fobj.visibility = "hide"; + PPTSld.Bobj.visibility = "hide"; + PPTSld.Eobj.visibility = "hide"; + } + return true; +} + +function overMe() { + this.bgColor = "blue"; +} + +function outMe() { + this.bgColor = "#AAAAAA"; +} + +function makeElement( whichEl, whichContainer ) { + if ( arguments.length == 1 ) { + whichContainer = PPTSld; + } + tmp = new Layer(100,whichContainer); + eval( whichEl + " = tmp" ); + return eval(whichEl); +} + +function initMe( obj, clr, text ) { + obj.bgColor = clr; +// obj.document.write("" + text + ""); + obj.document.write( "   " + text +" "); + obj.document.close(); + obj.captureEvents(Event.CLICK); + obj.color = "black"; +} + +function createCM() { + if ( base.IsFullScrMode() ) { + var clr = "#AAAAAA"; + PPTSld.shadeUobj = makeElement("SHADEU"); + PPTSld.shadeDobj = makeElement("SHADED"); + PPTSld.panelobj = makeElement("PANEL"); + PPTSld.stripUobj = makeElement("STRIPU"); + PPTSld.stripDobj = makeElement("STRIPD"); + PPTSld.shadeUobj.bgColor = "#BBBBBB"; + PPTSld.shadeDobj.bgColor = "#888888"; + PPTSld.stripUobj.bgColor = "#777777"; + PPTSld.stripDobj.bgColor = "#CCCCCC"; + PPTSld.panelobj.bgColor = clr; + PPTSld.Fobj = makeElement("Next"); + PPTSld.Bobj = makeElement("Previous"); + PPTSld.Eobj = makeElement("EndShow"); + initMe( PPTSld.Fobj, clr, "Next" ); + PPTSld.Fobj.onclick = M_GoNextSld; + + initMe( PPTSld.Bobj, clr, "Previous" ); + PPTSld.Bobj.onclick = M_GoPrevSld; + + initMe( PPTSld.Eobj, clr, "End Show"); + PPTSld.Eobj.onclick = base.CloseFullScreen; + } +} + +function IsContextMenu() { + return (g_ctxmenu == 1) +} +var g_notesTable = new Array() +var g_hiddenSlide = new Array() +makeSlide( 0,1,1); +makeSlide( 1,1,1); +makeSlide( 2,1,1); +makeSlide( 3,1,1); +makeSlide( 4,1,1); +makeSlide( 5,1,1); +makeSlide( 6,1,1); +makeSlide( 7,1,1); +makeSlide( 8,1,1); +makeSlide( 9,1,1); +makeSlide( 10,1,1); +makeSlide( 11,1,1); +makeSlide( 12,1,1); +makeSlide( 13,1,1); +makeSlide( 14,1,1); +makeSlide( 15,1,1); +makeSlide( 16,0,1); +makeSlide( 17,1,1); + +var END_SHOW_HREF = "endshow.htm", + OUTLINE_EXPAND_HREF = "outline_expanded.htm", + OUTLINE_COLLAPSE_HREF = "outline_collapsed.htm", + OUTLINE_NAVBAR_HREF = "outline_navigation_bar.htm", + NAVBAR_HREF = "navigation_bar.htm", + BLANK_NOTES_HREF = "blank_notes.htm", + NUM_VISIBLE_SLIDES = 18, + SIMPLE_FRAMESET = 0, + SLIDE_FRAME = "PPTSld", + NOTES_FRAME = "PPTNts", + OUTLINE_FRAME = "PPTOtl", + OUTLINE_NAVBAR_FRAME = "PPTOtlNav", + NAVBAR_FRAME = "PPTNav", + MAIN_FRAME = "MainFrame", + FS_NAVBAR_HREF = "fs_navigation_bar.htm", + isIEFiles = 2, + isNAVFiles = 8, + isFLATFiles = 16, + includeNotes = 1, + PPTPRESENTATION = 1; +var INITSLIDENUM = 1; + +var EndSlideShow = 0; +var g_outline_href = OUTLINE_COLLAPSE_HREF; +var g_fullscrMode = 0; +var FSWin = null; +var gtmpstr = document.location.href; +var g_baseURL = gtmpstr.substr(0, gtmpstr.lastIndexOf("/") ) + "/" + "webqtl_demo2_part1.ppt_files"; +var g_showoutline = 1; +var g_shownotes = includeNotes; +var g_currentSlide = INITSLIDENUM, g_prevSlide = INITSLIDENUM; +var saveFSSlideNum = saveTPSlideNum = g_currentSlide; +var saveFSprevSlide = saveTPprevSlide = g_prevSlide; +var g_slideType="ie"; +var appVer = navigator.appVersion; +var msie = appVer.indexOf( "MSIE " ) + appVer.indexOf( "Internet Explorer " ); +var isnav = ( navigator.appName.indexOf( "Netscape" ) >= 0 ); +var msieWin31 = (appVer.indexOf( "Windows 3.1" ) > 0); +var ver = 0; +var g_done = 0; +var g_prevotlobjidx = 0; +var g_ShowFSDefault = 0; +var g_lastVisibleSld = 1; +var g_allHidden = false; +function IsIE() { + return (msie >= 0 ); +} + +function IsNav() { + return (isnav); +} +var msiePos = appVer.indexOf( "MSIE " ); +var inexPos = appVer.indexOf( "Internet Explorer " ); +if ( msiePos >= 0 ) + ver = parseFloat( appVer.substring( msiePos+5, appVer.indexOf ( ";", msiePos ) ) ); +else if( inexPos >= 0 ) + ver=parseFloat( appVer.substring( inexPos+18, appVer.indexOf(";",inexPos) ) ) +else + ver = parseInt( appVer ); + +//var g_supportsPPTHTML = 0; //!msieWin31 && ( ( msie >= 0 && ver >= 3.02 ) || ( msie < 0 && ver >= 3 ) ); + +function GetCurrentSlideNum() +{ + obj = GetHrefObj( g_currentSlide ); + if ( GetHrefObj( g_currentSlide ).m_origVisibility == 1 ) + return obj.m_slideIdx; + else + return g_currentSlide; +} + +function GetNumSlides() +{ + if ( GetHrefObj( g_currentSlide ).m_origVisibility == 1 ) + return NUM_VISIBLE_SLIDES; + else + return g_docTable.length; +} + +function GetHrefObj( slideIdx ) +{ return g_docTable[slideIdx - 1]; +} + +function GetSlideNum( slideHref ) +{ + for (ii=0; ii 0 ) { + obj = GetHrefObj( targetIdx ); + while ( ( obj.m_visibility == 0 ) && ( targetIdx>0 ) ) + obj = GetHrefObj( targetIdx-- ); + GoToSld( obj.m_slideHref ); + } +} + +function GoToLast() +{ + targetIdx = g_docTable.length; + if ( targetIdx != g_currentSlide ) + GoToSld( GetHrefObj( targetIdx ).m_slideHref ); +} + +function GoToFirst() +{ GoToSld( GetHrefObj(1).m_slideHref ); +} + +function highlite() { + if ( IsFullScrMode() ) + return; + index = GetCurrentSlideNum(); + if ( !frames[MAIN_FRAME].frames[OUTLINE_FRAME] ) + return; + if ( msie < 0 ) { + if ( g_prevotlobjidx != 0 ) { + eval( "otlobj = frames[MAIN_FRAME].frames[OUTLINE_FRAME].document.LAYERID" + g_prevotlobjidx ); + otlobj.hidden = true; + } + else + index = GetCurrentSlideNum(); + eval( "otlobj = frames[MAIN_FRAME].frames[OUTLINE_FRAME].document.LAYERID" + index ); + otlobj.hidden = false; + + g_prevotlobjidx = index; + + return; + } + if ( !g_showoutline ) + return; + + backclr = frames[MAIN_FRAME].frames[OUTLINE_FRAME].document.body.bgColor; + textclr = frames[MAIN_FRAME].frames[OUTLINE_FRAME].document.body.text; + if ( g_prevotlobjidx != 0 ) { + eval( "otlobj = frames[MAIN_FRAME].frames[OUTLINE_FRAME].document.all.p" + g_prevotlobjidx ); + otlobj.style.backgroundColor = backclr; + otlobj.style.color = textclr; + otlobj.all.AREF.style.color = textclr; + } + else + index = GetCurrentSlideNum(); + eval( "otlobj = frames[MAIN_FRAME].frames[OUTLINE_FRAME].document.all.p" + index ); + otlobj.style.backgroundColor = textclr; + otlobj.style.color = backclr; + otlobj.all.AREF.style.color = backclr; + g_prevotlobjidx = index; +} + +function ChangeFrame( frame, href ) +{ +if ( IsFramesMode() ) { + if ( NAVBAR_FRAME == frame || OUTLINE_NAVBAR_FRAME == frame ) { + frames[frame].location.replace(href); + } + else if( ! ( ( OUTLINE_FRAME == frame && !g_showoutline) || (NOTES_FRAME == frame && !g_shownotes ) ) ){ + frames[MAIN_FRAME].frames[frame].location.href = href; + } + } + else { + if ( frame == NAVBAR_FRAME || frame == SLIDE_FRAME ) { + if( frame == NAVBAR_FRAME ) { + href = FS_NAVBAR_HREF; + + } + if( frame == NAVBAR_FRAME ) + window.frames[frame].location.replace(href); + else + window.frames[frame].location.href = href; + } + } + +} + +function shutEventPropagation() { + if ( IsNav() ) + return; + + var slideFrame; + if ( IsFramesMode() ) + slideFrame = frames[MAIN_FRAME].frames[SLIDE_FRAME]; + else + slideFrame = window.frames[SLIDE_FRAME]; + if ( slideFrame.event ) + slideFrame.event.cancelBubble=true; +} + +function GoToSld( slideHref ) +{ + shutEventPropagation(); + if ( slideHref != GetHrefObj( g_currentSlide ).m_slideHref || g_slideType != GetHrefObj( g_currentSlide ).type) { + g_prevSlide = g_currentSlide; + g_currentSlide = GetSlideNum( slideHref ); + g_slideType = GetHrefObj( g_currentSlide ).type; + obj = GetHrefObj( g_currentSlide ); + obj.m_visibility = 1; + ChangeFrame( SLIDE_FRAME, slideHref ); + if( !SIMPLE_FRAMESET ) + ChangeFrame( NOTES_FRAME, obj.m_notesHref ); + ChangeFrame( NAVBAR_FRAME, NAVBAR_HREF ); + + } +} + +function PrevSldViewed() +{ GoToSld( GetHrefObj( g_prevSlide ).m_slideHref ); +} + +function NoHref() {} + +function ExpandOutline( ) +{ + g_outline_href = OUTLINE_EXPAND_HREF; + ChangeFrame( OUTLINE_FRAME, OUTLINE_EXPAND_HREF ); + frames[OUTLINE_NAVBAR_FRAME].location.replace( OUTLINE_NAVBAR_HREF); +} + +function CollapseOutline() +{ + g_outline_href = OUTLINE_COLLAPSE_HREF; + ChangeFrame( OUTLINE_FRAME, OUTLINE_COLLAPSE_HREF ); + frames[OUTLINE_NAVBAR_FRAME].location.replace( OUTLINE_NAVBAR_HREF); + } + +function SlideUpdated( id ) +{ + if ( id != GetHrefObj( g_currentSlide ).m_slideHref ) { + g_prevSlide = g_currentSlide; + g_currentSlide = GetSlideNum( id ); + obj = GetHrefObj( g_currentSlide ); + if( !SIMPLE_FRAMESET ) + ChangeFrame( NOTES_FRAME, obj.m_notesHref ); + ChangeFrame( NAVBAR_FRAME, NAVBAR_HREF ); + } +} + +function hrefList( slideHref, notesHref, visible, slideIdx, type ) +{ + this.m_slideHref = slideHref; + this.m_notesHref = notesHref; + this.m_navbarHref = NAVBAR_HREF; + this.m_origVisibility = visible; + this.m_visibility = visible; + this.m_slideIdx = slideIdx; + this.type = type; +} + +function IsFullScrMode() { + return g_fullscrMode; +} + + +function IsFramesMode() { + return (1 - g_fullscrMode); +} + +function SldUpdated( id ) +{ + if ( ( id != GetHrefObj( g_currentSlide ).m_slideHref ) || ( g_currentSlide == g_lastVisibleSld ) ){ + g_prevSlide = g_currentSlide; + g_currentSlide = GetSlideNum( id ); + obj = GetHrefObj( g_currentSlide ); + if( !SIMPLE_FRAMESET ) + ChangeFrame( NOTES_FRAME, obj.m_notesHref ); + ChangeFrame( NAVBAR_FRAME, NAVBAR_HREF ); + } +} + +function ToggleOutline() { + g_showoutline = 1 - g_showoutline; + writeMyFrame(); +} + +function ShowHideNotes() { + g_shownotes = 1 - g_shownotes; + writeMyFrame(); +} + +function writeMyFrame() { + SetFSMode(0); + obj = frames[MAIN_FRAME]; + + var curslide = g_baseURL + "/" + GetHrefObj( g_currentSlide ).m_slideHref; + var curnotes = g_baseURL + "/" + GetHrefObj( g_currentSlide ).m_notesHref; + var otlhref = g_baseURL + "/" + g_outline_href; + if ( msie < 0 ) { + if ( ! g_showoutline && g_shownotes ) { + obj.document.write( ' \ No newline at end of file diff --git a/web/tutorial/ppt/html/webqtl_demo2_part1.ppt_files/slide0001_image001.png b/web/tutorial/ppt/html/webqtl_demo2_part1.ppt_files/slide0001_image001.png new file mode 100755 index 00000000..a1cb20e4 Binary files /dev/null and b/web/tutorial/ppt/html/webqtl_demo2_part1.ppt_files/slide0001_image001.png differ diff --git a/web/tutorial/ppt/html/webqtl_demo2_part1.ppt_files/slide0001_notes_pane.htm b/web/tutorial/ppt/html/webqtl_demo2_part1.ppt_files/slide0001_notes_pane.htm new file mode 100755 index 00000000..7c670210 --- /dev/null +++ b/web/tutorial/ppt/html/webqtl_demo2_part1.ppt_files/slide0001_notes_pane.htm @@ -0,0 +1,5 @@ +
Welcome to a short demonstration of the GeneNetwork and its WebQTL module. Please adjust the size of the windows on your monitor so that you can see part of this page, as well as GeneNetwork windows. WebQTL produces a large number of new windows, so you may need to modify your browser preferences to permit pop-ups. In this demonstration, we explore one important transcript expressed in the brain: the amyloid beta precursor protein messenger RNA. A protein product of this mRNA, the APP protein, is associated with AlzheimerƠs disease.

My thanks to Dr. Robert F. Clark and Wenli Cai for testing this PowerPoint demonstration and making many improvements.

(Initial version of June 2003 by Rob Williams. Edits July 13, 2005 by RW and RFC. Edit July 14, 2005 by WC. Final edits by RF Clark, July 22, 2005.
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Please link to the web site:  http://www.genenetwork.org
To begin a search you make choices about what species, group, and database to explore.

For this demonstration enter APP as above and click on the SEARCH button. Make sure that the DEFAULT SETTINGS are species = Mouse, Group = BXD, Type = Whole Brain, and Database = INIA BRAIN mRNA M430 (Apr05) PDNN.

Notes:
1. The GeneNetwork and WebQTL are often used to work with public data sets. However, it is possible to enter and analyze your own data for specific genetic reference populations such as the BXD genetic reference population of mice or the HXB strains of rat. Entering your own data is a more advanced topic, but if you click on the HOME pop-down menu (upper left), you will see ̉Enter Trait DataÓ that will explain the process.
2. For help on advanced searching methods read the left side of the page (INTRODUCTION).  If you make a search term too complex, you may get no hits (try entering ̉amyloid betaÓ for example). If you make it too simple, you may also get too many.
3. Use the asterisk * as a wildcard. For example, to find all Hoxb transcripts, search for Hoxb*.
4. In some cases you can also research for transcripts and genes using special search strings such as ̉Mb = (Chr1, 100 102)Ó to find all genes on Chromosome 1 between 98 and 104 megabases (donƠt actually use the quotes). Details are described at http://www.genenetwork.org/searchHelp.html.
5.   These INFO buttons provide links to data about the different data types. Try them.
6.  The SET TO DEFAULT button is used to change the database default setting to match your typical search categories.
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SHORT DETOUR to the HELP menu. If you are new to the GeneNetwork, you may find it helpful to review the The Glossary and FAQ pages shown above. We are in the process of making ̉liveÓ demos for some of the key modules in the GeneNetwork. Check the NEWS every month or two to find out about new features.

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RESULTS OF THE APP SEARCH.  A search of the INIA Brain database generates 18 matches, 10 of which are shown above. The GeneNetwork will display several hundred matches in pages of 40 each. If a search generates a larger numbers of hits, then you will need to refine search terms.

Notes:
1. APP is a great transcript to introduce you to the complexity and power of new array platforms that often provide ̉alternativeÓ expression estimates for single genes. There are seven probe sets that target different parts of the APP transcript. Which of the alternative measurements is most appropriate and informative? Have a look at the FAQ page for more on this topic, but general advice: 1. be skeptical and try to validate that the correct transcript and gene is being measured; 2. check what part of the transcript is complementary to the probes; 3. evaluate the performance of individual probes based on expression level, signal-to-noise and other error terms such as the standard deviation and error.
2. In this particular case we have highlighted and selected # 5 on this SEARCH RESULTS page. The annotation for this probe set mentions that it targets the last three exons and the 3Ơ untranslated region (UTR) of the amyloid precursor protein (APP).  That is just what we want.
3. Most probe sets have not been annotated in as much detail as App. Refer tot the FAQ to learn how to annotate probe sets yourself.
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The Trait Data and Analysis Form is the single most important page from the point of view of working with GeneNetwork data. Please read the text carefully. Explore the links, but do not close this page. We will need it many more times in this demonstration.
Notes:
1. What is this database? It is called INIA Brain mRNA M430 (Apr05) PDNN, but what does that actually mean. How much of the brain was used? How were the animals processed? Most of these types of questions can be answered by clicking on the DATABASE link.
2. Transcript/gene LOCATION data is usually from the most recent assembly. You can VERIFY the location of the probes and probe set using the two VERIFY buttons. VERIFY UCSC performs a sequence alignment (BLAT analysis) of the probes to the most recent assembly.
3. The PROBE TOOL button provides you with highly detailed information on the probe sequences used to assemble the probe set. For example, in this case you can find out which probes correspond to which of the three exons. You can also review the performance of the individual probes. Please check the GLOSSARY for additional details on probes.
4. The identifiers (IDs) provide links to other key resources.

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Most of the database components and resources in The GeneNetwork are linked to metadata pages that provide a human-readable summary of how, why, where, when, and with whom the data were generated. Before you get too involved with a data set, it is naturally important to read this information. While the data in The GeneNetwork may be accessible and useful, that does not always mean that the data is public domain and available for you to use in publication or for profit purposes. If you want to know more about the data ownership and usage, please read through the POLICIES pop-down menu items.
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This slide shows you the lower parts of the Trait Data and Analysis Form with the data for the first set of BXD strains
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The Basic Statistics page allows you to evaluate some aspects of the data quality. In this case, BXD8 is a potential problem. An outlier of this type may be generated by a technical artifact (bad sample?). However, it is also possible that BXD8 just has genuine low endogenous expression of App and may therefore be a particularly valuable model for research. There are different ways to treat problematic data of these types. One way is simply to discard this datum. The other way is to prevent outliers from have too much influence quantitatively, while leaving them in their low (or high positions). This is called windsorizing the data (after King Henry the VIII who had a habit of chopping heads). In this case, we have windsorized the BXD8 to a value of 16.0 and the BXD33 to a value of 16.02. Rank is retained. We are making a bet that the two lowest strains are really low, but we are hedging our bet and just making them a little lower than BXD90. This removes their ̉undueÓ influence.
Notes:
1. It turns out that BXD8 is a strain with many odd phenotypes. The whole strain is essentially an outlier for many traits. Therefore, the low App expression data may be quite accurate. Still, it would be comforting to have at least two more replicates.
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Now we get a much better feel for the variation in the error among the cases. Those without error bars are of course the ̉noisiestÓ of all. This data set is not complete yet (the aim is to acquire at least one male-female sample for each BXD strain).
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Finally, we can now start an analysis.
We ask a simple question:
Do differences in this particular App transcript steady-state abundance level correlate with those of any other transcripts in the same INIA Brain mRNA M430 data set?
Notes:
1.You can CHOOSE many other DATABASES at this point if you want, but for now letƠs stick with the default.
2. There are different ways to sort the correlations. The most obvious is by p-value (most significant values at the top of the list), but it is also interesting to sort the top 100 or top 500 by their gene symbol (gene ID) or by their chromosomal location (position).
3. If you donƠt want your analysis to be sensitive to outliers, then you may want to choose to use the Spearman Rank Order method of calculating correlations.
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The Traits Correlation output window (Correlation Results) compares App expression data with all other traits in this INIA Brain data set. The most significant 100 or 500 transcripts are sorted by their p-values. The top correlation is that of the probe set to itself (often a value of 1.0, but in this case we modified the App values manually by windsorizing the data). The next best correlation is to another App probe set. The fourth correlation is interesting and suggests that there may be a link between App and a particular type of ataxia (Atcay).
Notes:
1.Use the checkboxes to the far left to select traits that you want to study together. Once you have selected interesting traits, click on the ADD SELECTION button. This puts all of the selected traits into a SELECTIONS WINDOW for other types of analysis.
2. The p-value is not corrected for multiple tests. A conservative approach for array data would be to assume 10,000 nominally independent tests. Subtract 4 from the exponent and if the value is still smaller than 0.05 you may have a real correlation.
3. The LITERATURE CORRELATION is a data type generated by Drs. Ramin Homayouni and Michael Berry. Click on the header column by the asterisk for more information on this highly useful data type.
4. We are using Pearson product moment correlations rather that the Spearman rank order correlation. But you can select either in the previous step.
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By clicking on the CORRELATION of the Atcay transcript to the App transcript, you can generate a Correlation plot between these two transcripts. In this App and Atcay scatterplot, each point is a strain mean value. For example, BXD33 and BXD8 have low App and Atcay expressions. The two parental strains and the F1 are also included in this plot.
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A group of traits from many different databases can be selected and brought together for joint analysis. In this case all of the content of the BXD SELECTIONS is from a single BRAIN database, the top 20 neighbors of the App transcript from the Correlation Results table. Eight of these neighbors plus App is shown in the slide.
Notes:
1.All of items in the BXD SELECTIONS were selected using the SELECT ALL button
2. The buttons at the top (and bottom) of this page can do some cool stuff. We will work with NETWORK GRAPH first.
3. Think of the SELECTIONS as your shopping cart. You go to different aisles in the supermarket to acquire different types of items of interest. These could include transcripts, classical phenotypes (longevity, brain weight, prepulse inhibition, iron levels in midbrain). ̉Checking outÓ in this case involves doing some analysis with the items in the cart.
4. Different tools handle different numbers of items. Most will handle up to 100 traits.

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Output of the Network Graph. Warm colors (orange and red) are positive correlations above 0.5 whereas cool colors (green and blue) are negative correlations. Notes:
1. All of the nodes (gene/transcripts) on this graph are clickable.
2. For this graph the App expression values have ̉revertedÓ to their pre-Windsorized values.
3. To generate this graph, we used the default setting:  Size of 16 by 16 inches; Gene Symbols; Don't Show Correlations; Use curved lines (aka ̉edgesÓ).
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Going back to the Trait Data and Analysis Form window, we have computed the correlations between strain variation in App expression level and other classical phenotypes that have already been measured in many of the same BXD strains.
Notes:
1.The number of common strains varies widely--in this case from 14 to 23 strains.
2. We can add these traits (four are selected) to our BXD SELECTIONS window.
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We have computed the Network Graph, now using other types of traits.
Saline Hot Plate Latency is the green node labeled 10020.
Freezing (fear) is the green node labeled 10447.
Notes:
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END
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GeneNetwork and WebQTL:
lPart 1: How to study expression variation and covariation (slides 2–16)
lPart 2. Discovering upstream modulators (slides 17–30)
RNA

PowerPoint ̉Normal viewÓ has notes that may be useful companions to these slides.
a PowerPoint Presentation
RWW 07.23.2005
You can also download this PowerPoint at
ftp://atlas.utmem.edu/public/webqtl_demo2.ppt
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END
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Choose
database
Enter
APP
Select
search
lPART 1: How to study variation and covariation
Choose  species, group, and type
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lPlease also use the Glossary, FAQ, and News
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Highlight this probe set in red and
click. You do NOT have to select the checkbox
Search results
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lFirst page of data: The Trait Data and Analysis Form
Click here
to learn
about
data
source
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lData sources: Metadata for each resource
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lExpression estimates for App on the Trait Data form
Trait data for each strain with SE when known. For array data the scale is ~ log base 2.   F1 data = 16.723 = 2^16.723 = 108,174
These values can all be changed by the user. (Yes, there is a RESET)
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lCritiquing the App data the Trait Data
Use the BASIC STATISTICS button to evaluate the App data. You will find that App data from the different strains are not equally trustworthy. BXD8 is an obvious outlier without replication (no error bar). BXD33 is also suspiciously low. BXD5 is noisy.
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lApp expression after windsorizing
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lDiscovering shared expression patterns
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lTranscript neighborhoods
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lApp and Atcay transcript scatterplot
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lApp transcript and eight of its neighbors
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App transcript coexpression neighborhood
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lCorrelations of App with classical traits
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lNetwork Graph of App with classical traits
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lSummary of Part 1:
1. You have learned the basics about searching for traits
2. You know some methods to check data quality
3. You know how to edit bad or suspicious data
4. You know how to review the basic statistics of a trait
5. You know how to generate a scattergram between two traits using the Traits Correlation tool
6. You know how to add items to your SELECTIONS window
7. You know how to generate a Network Graph of traits that co-vary.
What does genetic covariance mean? The genetic covariance can be functional and mechanistic, but it can also be due to linkage disequilibrium. Finally, it can be due to sampling error or poor experimental design. Evaluate the biological plausibility of correlations. Test and be skeptical.
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Contact for comments and improvements:
rwilliam@nb.utmem.edu


kmanly@utmem.edu
The App findings reviewed in this presentation are part of an ongoing study by R. Williams. R. Homayouni, and R. Clark (July 15, 2005)
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