The DMT1 IVS4+44C>A polymorphism and the risk of iron deficiency anemia in children with celiac disease

PloS one

A Genetic Variation Linked to Iron Deficiency Anemia Risk in Children with Celiac Disease

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Abstract

The IVS4+44-AA genotype is associated with a four-fold increased risk of developing anemia in 387 Italian celiac children.

  • Anemia risk is significantly higher in individuals with the DMT1 IVS4+44-AA genotype, regardless of the degree of villous atrophy.
  • Total DMT1 expression is upregulated in cases of mild atrophy but not in severe atrophy, independent of the IVS4+44C>A variant.
  • The A-allele of the DMT1 polymorphism is linked to increased expression of DMT1 transcripts that do not respond to iron levels, potentially limiting iron absorption.
  • Dysregulation of DMT1 expression related to the IVS4+44-AA genotype may not affect iron absorption under normal conditions but could contribute to iron deficiency when combined with severe villous atrophy.

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Key numbers

Increase in Anemia Risk
Risk of developing anemia associated with IVS4+44-AA genotype.
387
Cohort Size
Number of Italian celiac children included in the study.

Full Text

What this is

  • This research investigates the role of the IVS4+44C>A polymorphism in () among children with ().
  • The study examines a cohort of 387 Italian celiac children, focusing on the genetic variant's impact on anemia risk and expression.
  • Findings suggest that the AA genotype of the polymorphism significantly increases the risk of in these patients.

Essence

  • The IVS4+44-AA genotype increases the risk of anemia in children with by 4×. The A-allele is linked to reduced expression of iron-responsive transcripts, which may hinder iron absorption.

Key takeaways

  • The IVS4+44-AA genotype confers a 4× increased risk of developing anemia in celiac children, regardless of the degree of intestinal atrophy.
  • A-allele carriers show preferential expression of transcripts lacking iron-responsive elements, which limits the transporter’s ability to adapt to iron deficiency.

Caveats

  • Results may not be generalizable beyond the Southern Italian population studied, limiting broader applicability.
  • The study's cohort did not represent all possible combinations of genotypes and villous atrophy stages, which may affect findings.

Definitions

  • Celiac Disease (CD): A chronic autoimmune disorder triggered by gluten, leading to inflammation and damage in the small intestine.
  • Iron Deficiency Anemia (IDA): A condition characterized by a lack of sufficient iron, leading to reduced hemoglobin levels and impaired oxygen transport.
  • DMT1: Divalent metal transporter 1, a protein that facilitates iron uptake in the intestinal cells.

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