We compared variant allele counts for Asian and Oceania samples from the GenomeAsia cohort to allele counts present in non-Asian gnomAD samples (European (non-Finnish), European (Finnish), Latino, African or other) for variants found in a set of 124 medically relevant genes. The genes used were 115 genes used for prenatal screening70 as well as the cancer-associated genes BRCA1, BRCA2, TP53, MEN1, MLH1, MSH2, MSH6, PMS1 and PMS2A. A Fisher’s exact test was used to calculate variations that were significantly overrepresented in the GenomeAsia subsamples and corrected for multiple testing using the Bonferroni method. We further accessed variants for these genes that had not previously been reported. All variants were further filtered as being damaging as determined by having a high impact on the protein (stop codon, essential splice site or frameshift mutation) or were predicted to be damaging by the Polyphen2 program. A cumulative comparison of allele counts for all over-represented and novel variants was performed and compared to non-Asian gnomAD to calculate a P value, odds ratio and relative difference in cumulative allele frequency (GenomeAsia cumulative allele frequency minus gnomAD non-Asian allele frequency). Reported P values were corrected for multiple testing using the Bonferroni method.
