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Primary topic: TNFAIP3 celiac immune gene

TNFAIP3 Gene and Metabolism: What It Can Mean in a Pathway Report

TNFAIP3 is tracked as small-effect non-HLA immune susceptibility context for celiac risk.

What is the TNFAIP3 gene?

TNFAIP3 helps regulate inflammatory signaling. In this report it is treated as immune-risk context, not gluten intolerance evidence.

How TNFAIP3 affects metabolism

TNFAIP3-linked celiac signals add modest susceptibility context after HLA and serology remain the main clinical anchors.

What happens when TNFAIP3 is altered

A TNFAIP3 signal cannot diagnose celiac disease and should not drive dietary restriction by itself.

Curated SNP evidence for TNFAIP3

These SNPs come from the approved study-level evidence model. Each claim is scored from curated study rows, then gated before it can influence pathway scoring.

Gluten / celiac immune risk

Evidence-backed report connection

TNFAIP3 currently has 1 curated SNPs, 1 claim-level scores, and 1 claims eligible for pathway scoring.

Open the sample report
rs2327832TNFAIP3 celiac susceptibility signal1 claims · 3 study rows

disease trait · AG

Non-HLA TNFAIP3 celiac susceptibility context

Moderate

rs2327832 AG carries one GWAS Catalog celiac disease risk G allele at the TNFAIP3 immune-regulation locus.

TNFAIP3 rs2327832 AG is scored as small non-HLA celiac susceptibility context.

Likely effectHigher trait association
Signal sizeSmall signal
Evidence supportStrong support
Report useIncluded in pathway scoring
Show study evidence
dbSNP rs2327832identity only · unknowndbSNP confirms rs2327832 identity; identity evidence does not assign celiac direction.Dubois 2010 celiac GWAS TNFAIP3 locusgwas · directGWAS Catalog reports rs2327832-G associated with celiac disease, with TNFAIP3 as the author-reported gene in the Dubois 2010 celiac GWAS.PubMed record for Dubois 2010 celiac GWASgwas · directPubMed identifies the primary Dubois 2010 Nature Genetics celiac GWAS behind the GWAS Catalog rs2327832-G celiac association.

Common symptoms people report

  • digestive symptoms where celiac testing is relevant
  • family context around autoimmune disease
  • non-HLA SNP findings that require restraint

Biomarkers to validate

tTG-IgA with total IgA

First-line serology context when celiac disease is suspected.

EMA or DGP context

Adds clinician-directed follow-up when initial testing is unclear.

Formal HLA-DQ typing

Clarifies genetic background better than tag SNPs alone.

Where DNA analysis helps

DNA helps prioritize whether celiac immune context is worth discussing, but biomarkers and clinical evaluation decide what it means.

Example interpretation

TNFAIP3 may add useful context when its SNP evidence lines up with the broader pathway signal.

Suggested validation: celiac serology and HLA-DQ context.

What to do next

  • Do not remove gluten before appropriate testing if celiac disease is being evaluated.
  • Use serology and HLA context before interpreting non-HLA SNPs.
  • Treat this gene as low-impact support only.

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Related pages

HLA-DQA1

HLA-DQA1 celiac immune risk

HLA-DQB1

HLA-DQB1 celiac immune risk

Ferritin and inflammatory context

Ferritin and inflammatory context DNA follow-up

Ferritin and iron storage

Ferritin and iron storage DNA follow-up

Gluten and celiac immune risk pathway

gluten celiac immune risk pathway

Inflammation and immune signaling pathway

inflammation immune signaling pathway

Can DNA predict metabolism?

can DNA predict metabolism

23andMe vs Metastate metabolism report

23andMe vs Metastate metabolism report

Related symptom angle

Slow metabolism genetics

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