src/hg/makeDb/trackDb/human/covidHgeMuts.html 06d7be056190c14b85e71bc12523f18ea6815b5e

06d7be056190c14b85e71bc12523f18ea6815b5e
markd
  Mon Dec 7 00:50:29 2020 -0800
BLAT mmap index support merge with master

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-<h2>Description</h2>
-<p>
-This track shows variants associated with monogenic congenital defects of immunity to <b>SARS-CoV-2</b>, 
-with incomplete or complete penetrance from the <a target=_blank 
-href="https://www.covidhge.com/">COVID Human Genetic Effort</a>. This international consortium aims 
-to detect rare or common monogenic inborn immunity errors (IEI) underlying severe forms of COVID-19 
-in previously healthy individuals, as well as rare or common monogenic variations that make certain 
-individuals resistant to the infection by SARS-CoV2 itself despite repeated exposure.
-</p>
-
-<p>
-The major feature of the small set of  variants in this track is that they are functionally tested 
-to be <b>deleterious</b> and genetically tested to be <b>disease-causing</b>. Specifically, 
-rare variants were predicted to be loss-of-function (LOF) at 13 human loci known to govern 
-TLR3- and IRF7-dependent type I interferon (IFN) immunity to influenza virus in patients with 
-life-threatening COVID-19 pneumonia, relative to subjects with asymptomatic or benign infection. 
-These genetic defects display incomplete penetrance for influenza respiratory distress and only 
-manifested clinically upon infection with the more virulent SARS-CoV-2.
-</p>
- 
-<h2>Display Conventions</h2>
-
-
-
-<h2>Methods</h2>
-<p>
-Variant calls in 12 autosomal IFN-related genes from whole exome or genome data with a MAF lower 
-than 0.001 (gnomAD v2.1.1) and experimental demonstration of loss-of-function (LOF) were considered 
-for statistical analysis. Proportion of individuals carrying at least one pLOF variant was compared 
-between cases and controls by means of logistic regression with the likelihood ratio test. The first 
-three principal components of the PCA were included in the logistic regression model to account for 
-ethnic heterogeneity of the cohorts. Analysis of enrichment in rare (MAF &lt 0.001) synonymous 
-variants of the 12 genes was performed to check the calibration of the burden test. PCA war 
-conducted with Plink v1.9 software on whole exome and genome sequencing data and 1000 Genomes (1kG) 
-Project phase 3 public database as reference, using 27,480 exonic variants with a minor allele 
-frequency &gt0.01 and a call rate &gt0.99. The odds ratio was also estimated by logistic regression 
-and adjusted for ethnic heterogeneity. 
-</p>
-
-<h2>Data Access</h2>
-<p>
-The raw data can be explored interactively with the <a target="_blank" href="../cgi-bin/hgTables">
-Table Browser</a>, or the <a target="_blank" href="../cgi-bin/hgIntegrator">Data Integrator</a>.
-Please refer to
-our <a href="https://groups.google.com/a/soe.ucsc.edu/forum/#!forum/genome"
-target="_blank">mailing list archives</a> for questions, or our <a target="_blank"
-href="../FAQ/FAQdownloads.html#download36">Data Access FAQ</a> for more information.
-</p>
-
-<h2>Credits</h2>
-<p>
-Thanks to the COVID Human Genetic Effort contributors for making these data available, and in 
-particular to Qian Zhang at the Rockefeller University for review and input during browser track 
-development.
-</p>
-
-
-<h2>References</h2>
-<p>
-Zhang Q, Bastard P, Liu Z, Le Pen J, Moncada-Velez M, Chen J, Ogishi M, Sabli IKD, Hodeib S, Korol C
-<em>et al</em>.
-<a href="https://www.ncbi.nlm.nih.gov/pubmed/32972995" target="_blank">
-Inborn errors of type I IFN immunity in patients with life-threatening COVID-19</a>.
-<em>Science</em>. 2020 Sep 24;.
-PMID: <a href="https://www.ncbi.nlm.nih.gov/pubmed/32972995" target="_blank">32972995</a>
-</p> 
-
-    <h2>
-