Epidemiology

There are four main types of hemochromatosis.[4][7]​​ The most common form, type 1, is caused by mutations in the HFE gene (hemostatic iron regulator) and occurs primarily in people of northern European descent.[2][3]​​[4][7]​​​[8]​​​​​​[9]​ While precise estimates vary, the prevalence of HFE-related hemochromatosis is similar in the US, Europe, and Australia, at approximately 1 case per 200 to 400 people.[4][7][10]​ The major HFE mutation (C282Y) is common in the US: 1 in 10 white people is heterozygous for this mutation, while approximately 1 in 200 is a C282Y homozygote.[3][11]​ The frequency of C282Y homozygosity is much lower in other ethnicities including Hispanic people (0.27 per 1000), Pacific Islanders (0.12 per 1000), and black people (0.14 per 1000).[3][11]​ The homozygous C282Y mutation is present in approximately 80% to 90% of patients of northern European origin who have type 1 hemochromatosis.[2][8]

The rarer forms of hemochromatosis (types 2-4), involving mutations in other genes, have been reported worldwide.

Although type 1 hemochromatosis is an autosomal-recessive condition, with approximately equal numbers of male and female homozygotes, it shows heterogeneous clinical expression, which is more common in men.[9]​ Iron loss through menses and pregnancy is thought to attenuate disease manifestations in female homozygotes, although other factors may also be involved.[12] One large study of patients of northern European descent (ages 40-69 years) showed that among C282Y homozygotes, iron overload-related disease was seen in 28% of men and 1.2% of women.[13]​​​

The risk of clinical disease increases with age.[8][14] In classic hemochromatosis, symptoms become clinically apparent in the fourth or fifth decade of life.​

Use of this content is subject to our disclaimer