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<div style="position:absolute;right:10px;top:10px;font-size: 
75%"><em>Last original <tt>PLINK</tt> release is <b>v1.07</b>
(10-Oct-2009); <b>PLINK 1.9</b> is now <a href="plink2.shtml"> available</a> for beta-testing</em></div>

<h1>Whole genome association analysis toolset</h1>

<font size="1" color="darkgreen">
<em>
<a href="index.shtml">Introduction</a> |
<a href="contact.shtml">Basics</a> |
<a href="download.shtml">Download</a> |
<a href="reference.shtml">Reference</a> |
<a href="data.shtml">Formats</a> |
<a href="dataman.shtml">Data management</a> |
<a href="summary.shtml">Summary stats</a> |
<a href="thresh.shtml">Filters</a> |
<a href="strat.shtml">Stratification</a> |
<a href="ibdibs.shtml">IBS/IBD</a> |
<a href="anal.shtml">Association</a> |
<a href="fanal.shtml">Family-based</a> |
<a href="perm.shtml">Permutation</a> |
<a href="ld.shtml">LD calcualtions</a> |
<a href="haplo.shtml">Haplotypes</a> |
<a href="whap.shtml">Conditional tests</a> |
<a href="proxy.shtml">Proxy association</a> |
<a href="pimputation.shtml">Imputation</a> |
<a href="dosage.shtml">Dosage data</a> |
<a href="metaanal.shtml">Meta-analysis</a> |
<a href="annot.shtml">Result annotation</a> |
<a href="clump.shtml">Clumping</a> |
<a href="grep.shtml">Gene Report</a> |
<a href="epi.shtml">Epistasis</a> |
<a href="cnv.shtml">Rare CNVs</a> |
<a href="gvar.shtml">Common CNPs</a> |
<a href="rfunc.shtml">R-plugins</a> |
<a href="psnp.shtml">SNP annotation</a> |
<a href="simulate.shtml">Simulation</a> |
<a href="profile.shtml">Profiles</a> |
<a href="ids.shtml">ID helper</a> |
<a href="res.shtml">Resources</a> |
<a href="flow.shtml">Flow chart</a> | 
<a href="misc.shtml">Misc.</a> |
<a href="faq.shtml">FAQ</a> |
<a href="gplink.shtml">gPLINK</a> 
</em></font>
</p>


<table border=0>
<tr>


<td bgcolor="lightblue" valign="top" width=20%>

<font size="1">

<a href="index.shtml">1. Introduction</a> </p>

<a href="contact.shtml">2. Basic information</a> </p>
<ul> 
 <li> <a href="contact.shtml#cite">Citing PLINK</a>
 <li> <a href="contact.shtml#probs">Reporting problems</a>
 <li> <a href="news.shtml">What's new?</a>
 <li> <a href="pdf.shtml">PDF documentation</a>
</ul>


<a href="download.shtml">3. Download and general notes</a> </p>
<ul> 
 <li> <a href="download.shtml#download">Stable download</a>
 <li> <a href="download.shtml#latest">Development code</a>
 <li> <a href="download.shtml#general">General notes</a>
 <li> <a href="download.shtml#msdos">MS-DOS notes</a>
 <li> <a href="download.shtml#nix">Unix/Linux notes</a>
 <li> <a href="download.shtml#compilation">Compilation</a>
 <li> <a href="download.shtml#input">Using the command line</a>
 <li> <a href="download.shtml#output">Viewing output files</a>
 <li> <a href="changelog.shtml">Version history</a>
</ul>

<a href="reference.shtml">4. Command reference table</a> </p>
<ul> 
 <li> <a href="reference.shtml#options">List of options</a>
 <li> <a href="reference.shtml#output">List of output files</a> 
 <li> <a href="newfeat.shtml">Under development</a>
</ul>


<a href="data.shtml">5. Basic usage/data formats</a> 
<ul> 
 <li> <a href="data.shtml#plink">Running PLINK</a>
 <li> <a href="data.shtml#ped">PED files</a>
 <li> <a href="data.shtml#map">MAP files</a>
 <li> <a href="data.shtml#tr">Transposed filesets</a>
 <li> <a href="data.shtml#long">Long-format filesets</a>
 <li> <a href="data.shtml#bed">Binary PED files</a>
 <li> <a href="data.shtml#pheno">Alternate phenotypes</a>
 <li> <a href="data.shtml#covar">Covariate files</a>
 <li> <a href="data.shtml#clst">Cluster files</a>
 <li> <a href="data.shtml#sets">Set files</a>
</ul>

<a href="dataman.shtml">6. Data management</a> </p>
<ul>
 <li>  <a href="dataman.shtml#recode">Recode</a>
 <li>  <a href="dataman.shtml#recode">Reorder</a>
 <li>  <a href="dataman.shtml#snplist">Write SNP list</a>
 <li>  <a href="dataman.shtml#updatemap">Update SNP map</a>
 <li>  <a href="dataman.shtml#updateallele">Update allele information</a>
 <li>  <a href="dataman.shtml#refallele">Force reference allele</a>
 <li>  <a href="dataman.shtml#updatefam">Update individuals</a>
 <li>  <a href="dataman.shtml#wrtcov">Write covariate files</a>
 <li>  <a href="dataman.shtml#wrtclst">Write cluster files</a>
 <li>  <a href="dataman.shtml#flip">Flip strand</a>
 <li>  <a href="dataman.shtml#flipscan">Scan for strand problem</a>
 <li>  <a href="dataman.shtml#merge">Merge two files</a>
 <li>  <a href="dataman.shtml#mergelist">Merge multiple files</a>
 <li>  <a href="dataman.shtml#extract">Extract SNPs</a>
 <li>  <a href="dataman.shtml#exclude">Remove SNPs</a>
 <li>  <a href="dataman.shtml#zero">Zero out sets of genotypes</a>
 <li>  <a href="dataman.shtml#keep">Extract Individuals</a>
 <li>  <a href="dataman.shtml#remove">Remove Individuals</a>
 <li>  <a href="dataman.shtml#filter">Filter Individuals</a>
 <li>  <a href="dataman.shtml#attrib">Attribute filters</a>
 <li>  <a href="dataman.shtml#makeset">Create a set file</a>
 <li>  <a href="dataman.shtml#tabset">Tabulate SNPs by sets</a>
 <li>  <a href="dataman.shtml#snp-qual">SNP quality scores</a>
 <li>  <a href="dataman.shtml#geno-qual">Genotypic quality scores</a>
</ul>
 
<a href="summary.shtml">7. Summary stats</a>
<ul>
 <li> <a href="summary.shtml#missing">Missingness</a>
 <li> <a href="summary.shtml#oblig_missing">Obligatory missingness</a>
 <li> <a href="summary.shtml#clustermissing">IBM clustering</a>
 <li> <a href="summary.shtml#testmiss">Missingness by phenotype</a>
 <li> <a href="summary.shtml#mishap">Missingness by genotype</a>
 <li> <a href="summary.shtml#hardy">Hardy-Weinberg</a>
 <li> <a href="summary.shtml#freq">Allele frequencies</a>
 <li> <a href="summary.shtml#prune">LD-based SNP pruning</a>
 <li> <a href="summary.shtml#mendel">Mendel errors</a>
 <li> <a href="summary.shtml#sexcheck">Sex check</a>
 <li> <a href="summary.shtml#pederr">Pedigree errors</a>
</ul>

<a href="thresh.shtml">8. Inclusion thresholds</a>
<ul>
 <li> <a href="thresh.shtml#miss2">Missing/person</a>
 <li> <a href="thresh.shtml#maf">Allele frequency</a>
 <li> <a href="thresh.shtml#miss1">Missing/SNP</a>
 <li> <a href="thresh.shtml#hwd">Hardy-Weinberg</a>
 <li> <a href="thresh.shtml#mendel">Mendel errors</a>
</ul>


<a href="strat.shtml">9. Population stratification</a>
<ul>
 <li> <a href="strat.shtml#cluster">IBS clustering</a>
 <li> <a href="strat.shtml#permtest">Permutation test</a>
 <li> <a href="strat.shtml#options">Clustering options</a>
 <li> <a href="strat.shtml#matrix">IBS matrix</a>
 <li> <a href="strat.shtml#mds">Multidimensional scaling</a>
 <li> <a href="strat.shtml#outlier">Outlier detection</a>
</ul>

<a href="ibdibs.shtml">10. IBS/IBD estimation</a>
<ul>
 <li> <a href="ibdibs.shtml#genome">Pairwise IBD</a>
 <li> <a href="ibdibs.shtml#inbreeding">Inbreeding</a>
 <li> <a href="ibdibs.shtml#homo">Runs of homozygosity</a>
 <li> <a href="ibdibs.shtml#segments">Shared segments</a>
</ul>


<a href="anal.shtml">11. Association</a>
<ul>
 <li> <a href="anal.shtml#cc">Case/control</a>
 <li> <a href="anal.shtml#fisher">Fisher's exact</a>
 <li> <a href="anal.shtml#model">Full model</a>
 <li> <a href="anal.shtml#strat">Stratified analysis</a>
 <li> <a href="anal.shtml#homog">Tests of heterogeneity</a>
 <li> <a href="anal.shtml#hotel">Hotelling's T(2) test</a>
 <li> <a href="anal.shtml#qt">Quantitative trait</a>
 <li> <a href="anal.shtml#qtmeans">Quantitative trait means</a>
 <li> <a href="anal.shtml#qtgxe">Quantitative trait GxE</a>
 <li> <a href="anal.shtml#glm">Linear and logistic models</a>
 <li> <a href="anal.shtml#set">Set-based tests</a>
 <li> <a href="anal.shtml#adjust">Multiple-test correction</a>
</ul>

<a href="fanal.shtml">12. Family-based association</a>
<ul>
 <li> <a href="fanal.shtml#tdt">TDT</a>
 <li> <a href="fanal.shtml#ptdt">ParenTDT</a>
 <li> <a href="fanal.shtml#poo">Parent-of-origin</a>
 <li> <a href="fanal.shtml#dfam">DFAM test</a>
 <li> <a href="fanal.shtml#qfam">QFAM test</a>
</ul>

<a href="perm.shtml">13. Permutation procedures</a>
<ul>
 <li> <a href="perm.shtml#perm">Basic permutation</a>
 <li> <a href="perm.shtml#aperm">Adaptive permutation</a>
 <li> <a href="perm.shtml#mperm">max(T) permutation</a>
 <li> <a href="perm.shtml#rank">Ranked permutation</a>
 <li> <a href="perm.shtml#genedropmodel">Gene-dropping</a>
 <li> <a href="perm.shtml#cluster">Within-cluster</a>
 <li> <a href="perm.shtml#mkphe">Permuted phenotypes files</a>
</ul>

<a href="ld.shtml">14. LD calculations</a>
<ul>
 <li> <a href="ld.shtml#ld1">2 SNP pairwise LD</a>
 <li> <a href="ld.shtml#ld2">N SNP pairwise LD</a>
 <li> <a href="ld.shtml#tags">Tagging options</a>
 <li> <a href="ld.shtml#blox">Haplotype blocks</a>
</ul>

<a href="haplo.shtml">15. Multimarker tests</a>
<ul>
 <li> <a href="haplo.shtml#hap1">Imputing haplotypes</a>
 <li> <a href="haplo.shtml#precomputed">Precomputed lists</a>
 <li> <a href="haplo.shtml#hap2">Haplotype frequencies</a>
 <li> <a href="haplo.shtml#hap3">Haplotype-based association</a>
 <li> <a href="haplo.shtml#hap3c">Haplotype-based GLM tests</a>
 <li> <a href="haplo.shtml#hap3b">Haplotype-based TDT</a>
 <li> <a href="haplo.shtml#hap4">Haplotype imputation</a>
 <li> <a href="haplo.shtml#hap5">Individual phases</a>
</ul>

<a href="whap.shtml">16. Conditional haplotype tests</a>
<ul>
 <li> <a href="whap.shtml#whap1">Basic usage</a>
 <li> <a href="whap.shtml#whap2">Specifying type of test</a>
 <li> <a href="whap.shtml#whap3">General haplogrouping</a>
 <li> <a href="whap.shtml#whap4">Covariates and other SNPs</a>
</ul>

<a href="proxy.shtml">17. Proxy association</a>
<ul>
 <li> <a href="proxy.shtml#proxy1">Basic usage</a>
 <li> <a href="proxy.shtml#proxy2">Refining a signal</a>
 <li> <a href="proxy.shtml#proxy2b">Multiple reference SNPs</a>
 <li> <a href="proxy.shtml#proxy3">Haplotype-based SNP tests</a>
</ul>

<a href="pimputation.shtml">18. Imputation (beta)</a>
<ul>
 <li> <a href="pimputation.shtml#impute1">Making reference set</a>
 <li> <a href="pimputation.shtml#impute2">Basic association test</a>
 <li> <a href="pimputation.shtml#impute3">Modifying parameters</a>
 <li> <a href="pimputation.shtml#impute4">Imputing discrete calls</a>
 <li> <a href="pimputation.shtml#impute5">Verbose output options</a>
</ul>

<a href="dosage.shtml">19. Dosage data</a>
<ul>
 <li> <a href="dosage.shtml#format">Input file formats</a>
 <li> <a href="dosage.shtml#assoc">Association analysis</a>
 <li> <a href="dosage.shtml#output">Outputting dosage data</a>
</ul>

<a href="metaanal.shtml">20. Meta-analysis</a>
<ul>
 <li> <a href="metaanal.shtml#basic">Basic usage</a>
 <li> <a href="metaanal.shtml#opt">Misc. options</a>
</ul>

<a href="annot.shtml">21. Annotation</a>
<ul>
 <li> <a href="annot.shtml#basic">Basic usage</a>
 <li> <a href="annot.shtml#opt">Misc. options</a>
</ul>

<a href="clump.shtml">22. LD-based results clumping</a>
<ul>
 <li> <a href="clump.shtml#clump1">Basic usage</a>
 <li> <a href="clump.shtml#clump2">Verbose reporting</a>
 <li> <a href="clump.shtml#clump3">Combining multiple studies</a>
 <li> <a href="clump.shtml#clump4">Best single proxy</a>
</ul>

<a href="grep.shtml">23. Gene-based report</a>
<ul>
 <li> <a href="grep.shtml#grep1">Basic usage</a>
 <li> <a href="grep.shtml#grep2">Other options</a>
</ul>

<a href="epi.shtml">24. Epistasis</a>
<ul>
 <li> <a href="epi.shtml#snp">SNP x SNP</a>
 <li> <a href="epi.shtml#case">Case-only</a>
 <li> <a href="epi.shtml#gene">Gene-based</a>
</ul>

<a href="cnv.shtml">25. Rare CNVs</a>
<ul>
 <li> <a href="cnv.shtml#format">File format</a>
 <li> <a href="cnv.shtml#maps">MAP file construction</a>
 <li> <a href="cnv.shtml#loading">Loading CNVs</a>
 <li> <a href="cnv.shtml#olap_check">Check for overlap</a>
 <li> <a href="cnv.shtml#type_filter">Filter on type </a>
 <li> <a href="cnv.shtml#gene_filter">Filter on genes </a> 
 <li> <a href="cnv.shtml#freq_filter">Filter on frequency </a>
 <li> <a href="cnv.shtml#burden">Burden analysis</a>
 <li> <a href="cnv.shtml#burden2">Geneset enrichment</a>
 <li> <a href="cnv.shtml#assoc">Mapping loci</a>
 <li> <a href="cnv.shtml#reg-assoc">Regional tests</a>
 <li> <a href="cnv.shtml#qt-assoc">Quantitative traits</a>
 <li> <a href="cnv.shtml#write_cnvlist">Write CNV lists</a>
 <li> <a href="cnv.shtml#report">Write gene lists</a>
 <li> <a href="cnv.shtml#groups">Grouping CNVs </a>
</ul>

<a href="gvar.shtml">26. Common CNPs</a>
<ul>
 <li> <a href="gvar.shtml#cnv2"> CNPs/generic variants</a>
 <li> <a href="gvar.shtml#cnv2b"> CNP/SNP association</a>
</ul>


<a href="rfunc.shtml">27. R-plugins</a>
<ul>
 <li> <a href="rfunc.shtml#rfunc1">Basic usage</a>
 <li> <a href="rfunc.shtml#rfunc2">Defining the R function</a>
 <li> <a href="rfunc.shtml#rfunc2b">Example of debugging</a>
 <li> <a href="rfunc.shtml#rfunc3">Installing Rserve</a>
</ul>


<a href="psnp.shtml">28. Annotation web-lookup</a>
<ul>
 <li> <a href="psnp.shtml#psnp1">Basic SNP annotation</a>
 <li> <a href="psnp.shtml#psnp2">Gene-based SNP lookup</a>
 <li> <a href="psnp.shtml#psnp3">Annotation sources</a>
</ul>


<a href="simulate.shtml">29. Simulation tools</a>
<ul>
 <li> <a href="simulate.shtml#sim1">Basic usage</a>
 <li> <a href="simulate.shtml#sim2">Resampling a population</a>
 <li> <a href="simulate.shtml#sim3">Quantitative traits</a>
</ul>


<a href="profile.shtml">30. Profile scoring</a>
<ul>
 <li> <a href="profile.shtml#prof1">Basic usage</a>
 <li> <a href="profile.shtml#prof2">SNP subsets</a>
 <li> <a href="profile.shtml#dose">Dosage data</a>
 <li> <a href="profile.shtml#prof3">Misc options</a>
</ul>

<a href="ids.shtml">31. ID helper</a>
<ul>
 <li> <a href="ids.shtml#ex">Overview/example</a>
 <li> <a href="ids.shtml#intro">Basic usage</a>
 <li> <a href="ids.shtml#check">Consistency checks</a>
 <li> <a href="ids.shtml#alias">Aliases</a>
 <li> <a href="ids.shtml#joint">Joint IDs</a>
 <li> <a href="ids.shtml#lookup">Lookups</a>
 <li> <a href="ids.shtml#replace">Replace values</a>
 <li> <a href="ids.shtml#match">Match files</a>
 <li> <a href="ids.shtml#qmatch">Quick match files</a>
 <li> <a href="ids.shtml#misc">Misc.</a>
</ul>


<a href="res.shtml">32. Resources</a>
<ul>
 <li> <a href="res.shtml#hapmap">HapMap (PLINK format)</a>
 <li> <a href="res.shtml#teach">Teaching materials</a>
 <li> <a href="res.shtml#mmtests">Multimarker tests</a>
 <li> <a href="res.shtml#sets">Gene-set lists</a>
 <li> <a href="res.shtml#glist">Gene range lists</a>
 <li> <a href="res.shtml#attrib">SNP attributes</a>
</ul>

<a href="flow.shtml">33. Flow-chart</a>
<ul>
 <li> <a href="flow.shtml">Order of commands</a>
</ul>

<a href="misc.shtml">34. Miscellaneous</a>
<ul>
 <li> <a href="misc.shtml#opt">Command options/modifiers</a>
 <li> <a href="misc.shtml#output">Association output modifiers</a>
 <li> <a href="misc.shtml#species">Different species</a>
 <li> <a href="misc.shtml#bugs">Known issues</a>
</ul>

<a href="faq.shtml">35. FAQ & Hints</a>
</p>

<a href="gplink.shtml">36. gPLINK</a>
<ul>
 <li> <a href="gplink.shtml">gPLINK mainpage</a>
 <li> <a href="gplink_tutorial/index.html">Tour of gPLINK</a>
 <li> <a href="gplink.shtml#overview">Overview: using gPLINK</a>
 <li> <a href="gplink.shtml#locrem">Local versus remote modes</a>
 <li> <a href="gplink.shtml#start">Starting a new project</a>
 <li> <a href="gplink.shtml#config">Configuring gPLINK</a>
 <li> <a href="gplink.shtml#plink">Initiating PLINK jobs</a>
 <li> <a href="gplink.shtml#view">Viewing PLINK output</a>
 <li> <a href="gplink.shtml#hv">Integration with Haploview</a>
 <li> <a href="gplink.shtml#down">Downloading gPLINK</a></p>
</ul>

</font>
</td><td width=5%>


<td valign="top">


&nbsp;</p>



<h1>Meta-analysis</h1>

This page describes the basic meta-analysis functions in PLINK, in
which two or more result files can be combined in fixed-effects and
random-effects meta-analysis.

</p>

<a name="basic">
<h2>Basic usage</h2>
</a></p>

The basic command for meta-analysis is invoked as 

<h5>
 plink --meta-analysis study1.assoc study2.assoc study3.assoc
</h5></p>

PLINK expects each file to be a plain-text, rectangular white-space
delimited file, with a header row.  PLINK will search the header row 
for the columns:
<pre>
     SNP   SNP idenitifier
      OR   Odds ratio (or BETA, etc)
      SE   Standard error of OR (or user-defined weight field)
       P   (Optional) p-value from test

     CHR   (Optional) 
      BP   (Optional)
      A1   (Optional)
      A2   (Optional) 
</pre>

<strong>HINT</strong> The <tt>SE</tt> field is added as an output
field in the standard <tt>--assoc</tt>, <tt>--mh</tt>,
<tt>--linear</tt> and <tt>--logistic</tt> tests, etc, if the <tt>--ci
0.95</tt> command is specified.
</p>

For example, consider we have two association files from independent
studies, <tt>s1.assoc</tt> and <tt>s2.assoc</tt>. For example, if the
first few rows of <tt>s1.assoc</tt> were as follows:
<pre><font size="-1">
   CHR        SNP         BP   A1      F_A      F_U   A2     CHISQ       P      OR       SE      L95     U95
    22   rs915677   14433758    A   0.1522   0.1842    G    0.1538   0.695  0.7949   0.5862    0.252   2.508
    22   rs140378   15251689    G  0.02083  0.04762    C    0.4988    0.48  0.4255    1.243  0.03719   4.869
    22   rs131564   15252977    C   0.1522   0.2619    G     1.625  0.2024  0.5058   0.5401   0.1755   1.458
    22  rs4010550   15274688    G   0.1364    0.275    A     2.495  0.1142  0.4163   0.5642   0.1377   1.258
    22  rs5747361   15365080    0        0        0    G        NA      NA      NA       NA       NA      NA
    22  rs2379981   15405346    G  0.02083        0    A    0.8848  0.3469      NA       NA       NA      NA
    ...
</font></pre>

The command
<h5>
 plink --meta-analysis s1.assoc s2.assoc
</h5></p>
gives the following output
<pre>
     Performing meta-analysis of 2 files
     Reading results from [ s1.assoc ]  with 2680 read
     Reading results from [ s2.assoc ]  with 2655 read
     2778 unique SNPs, 2557 in two or more files
     Rejected 1911 SNPs, writing details to [ plink.prob ]
     Writing meta-analysis results to [ plink.meta ]
</pre>

In general, SNPs across two or more files do not need to be in the
same order; also, a SNP does not need to feature in all files. By
default, meta-analysis will be reported for any SNP in two or more
files.
</p>
In this case, a number of SNPs are reported as being rejected from
meta-analysis. The reason for this is reported in the file
<pre>
     plink.prob
</pre>
which lists the SNP, the file and the problem code, as follows:
<pre>
     BAD_CHR               Invalid chromosome code 
     BAD_BP                Invalid base-position code 
     BAD_ES                Invalid effect-size (e.g. OR) 
     BAD_SE                Invalid standard error 
     MISSING_A1            Missing allele 1 label
     MISSING_A2            Missing allele 2 label
     ALLELE_MISMATCH       Mismatching allele codes across files
</pre>

The main output is in the file
<pre>
     plink.meta
</pre>
for example,
<pre>
      CHR         BP         SNP  A1  A2   N        P     P(R)      OR   OR(R)       Q       I
       22   14433758    rs915677   A   G   2   0.2217   0.2217  0.5823  0.5823  0.4184    0.00
       22   15252977    rs131564   C   G   2   0.2608   0.2608  0.6665  0.6665  0.4924    0.00
       22   15274688   rs4010550   G   A   2    0.298   0.3545  0.6748  0.6673  0.2489   24.79
       22   15462210  rs11089263   A   C   2   0.3992   0.3992  1.3108  1.3108  0.3600    0.00
       22   15462259  rs11089264   A   G   2   0.4719   0.4719  1.2606  1.2606  0.4079    0.00
       22   15475051   rs2154615   T   C   2   0.5518   0.5518  1.2876  1.2876  0.7534    0.00
       22   15476541   rs5993628   A   G   2   0.8014   0.8014  1.0948  1.0948  0.3380    0.00
       22   15549842   rs2845362   C   G   2    0.865   0.9789  0.9399  0.9854  0.1307   56.23
</pre>
which has the following fields:
<pre>
     CHR       Chromosome code
     BP        Basepair position
     SNP       SNP identifier
     A1        First allele code
     A2        Second allele code
     N         Number of valid studies for this SNP
     P         Fixed-effects meta-analysis p-value
     P(R)      Random-effects meta-analysis p-value
     OR        Fixed-effects OR estimate
     OR(R)     Random-effects OR estimate
     Q         p-value for Cochrane's Q statistic
     I         I^2 heterogeneity index (0-100)
</pre>

The effect (<tt>OR</tt>, or <tt>BETA</tt> in case of quantitative trait) is with
respect to the <tt>A1</tt> allele (i.e. if <tt>OR</tt> is greater than 1,
implies <tt>A1</tt> increases risk relative to <tt>A2</tt>).
</p>

<strong>HINT</strong> If an input file is compressed (<tt>gzip</tt>
compression) and ends in the <tt>.gz</tt> extension, PLINK will
automatically decompress it (if compiled with ZLIB support)


<a name="opt">
<h2>Misc. options</h2>
</a></p>

A number of options can be specified after the list of result
files. As <tt>--meta-analysis</tt> takes a variable number of files as
arguments, it is necessary to explicitly indicate that additional
options are specified, by a plus sign, as follows:
<h5>
 plink --meta-analysis s1.assoc s2.assoc + report-all
</h5></p>

In this example, the <tt>report-all</tt> option means that even SNPs
that are only found in a single file are reported. A full list of
options is give here:
<pre>
     study        Collate study-specific effect estimates in plink.meta (F0, F1, ...)
     no-map       Do not look for or use CHR/BP positions (i.e. if absent from files)
     no-allele    Do not look for or use A1/A2 allele codes (i.e. if absent from files)
     report-all   Report for SNPs seen only in a single file
     logscale     Indicates that effects are already on log-scale (i.e. beta from logistic regression)
     qt           Indicates that effects are from linear regression (i.e. not OR, do not take log)
</pre>

<b>Selecting subsets of SNPs</b>: One can use the <tt>--extract</tt>
option as well as <tt>--chr</tt>, etc, to input and perform
meta-analysis only on certain subsets of SNPs.
</p>

<strong>HINT</strong> If performing meta-analysis on a large number of
large files (e.g. 10+ files of imputed results, each with over 2
million entries), one might need to perform this one chromosome at a
time, with the <tt>--chr</tt> option, as all the result files might
not fit in memory in one go otherwise.


</td>
<td width=5%>&nbsp;</td>
</tr>
</table>




<hr>
<em>
 This document last modified Wednesday, 25-Jan-2017 11:39:27 EST
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