The first thing I did when I received my genotyping results from 23andMe was log on to their website and take a look at my estimated disease risks. For most people, these estimates are one of the primary reasons for buying a direct to consumer (DTC) genetics kit. But how accurate are these disease risk estimates? How robust is the information that goes into calculating them? In a previous post I focused on how odds ratios (the ratio of the odds of disease if allele A is carried as opposed to allele B) can vary across different populations, environments and age groups and, as a consequence, affect disease risk estimates. It turns out that even if we forget about these concerns for a moment, getting an accurate estimate of disease risk is far from straightforward. One of the primary challenges is deciding which disease loci to include in the risk prediction and in this post I will investigate the effect this decision can have on risk estimates.
To help me in my quest, I will use ulcerative colitis (UC) as an example throughout the post, estimating Genomes Unzipped members’ risk for the disease as I go. Ulcerative colitis is one of two common forms of autoimmune infllammatory bowel disease and I have selected it not on the basis of any special properties (either genetic or biological) but because I am familiar with the genetics of the disease having worked on it extensively.
The table below gives our ulcerative colitis risks according to 23andMe. The numbers in the table represent the percentage of people 23andMe would expect to suffer from UC given our genotype data (after taking our sex and ethnicity into account). The colours highlight individuals who fall into 23andMe’s “increased risk” (red) or “decreased risk” (blue) categories based on comparisons with the average risk (males: 0.77%; females 0.51%). As far as I am aware none of us actually do suffer from UC.
Continue reading ‘At odds with disease risk estimates’