Evidence Repository - Clinical Genome Resources

The ClinGen Evidence Repository is an FDA-recognized human genetic variant database containing expert-curated assertions regarding variants' pathogenicity and supporting evidence summaries. [Disclaimer]

Variant: NM_001126112.2(TP53):c.998G>A (p.Arg333His)

Curation Version - 2.0
Curation History
JSON LD for Version 2.0

CA000533

142273 (ClinVar)

Gene: TP53

Condition: Li-Fraumeni syndrome

Inheritance Mode: Autosomal dominant inheritance

Link to MONDO

UUID: d8de06fc-22f0-4978-9c21-a8d7b365d2c9

Approved on: 2025-03-04

Published on: 2025-06-23

HGVS expressions

NM_001126112.2:c.998G>A

NM_001126112.2(TP53):c.998G>A (p.Arg333His)

NC_000017.11:g.7670711C>T

CM000679.2:g.7670711C>T

NC_000017.10:g.7574029C>T

CM000679.1:g.7574029C>T

NC_000017.9:g.7514754C>T

NG_017013.2:g.21840G>A

ENST00000503591.2:c.998G>A

ENST00000508793.6:c.998G>A

ENST00000509690.6:c.602G>A

ENST00000514944.6:c.719G>A

ENST00000604348.6:c.977G>A

ENST00000269305.9:c.998G>A

ENST00000269305.8:c.998G>A

ENST00000359597.8:c.993+2824G>A

ENST00000413465.6:c.782+3470G>A

ENST00000420246.6:c.*105G>A

ENST00000445888.6:c.998G>A

ENST00000455263.6:c.*17G>A

ENST00000504290.5:c.*17G>A

ENST00000504937.5:c.602G>A

ENST00000510385.5:c.*105G>A

ENST00000576024.1:c.54-1021G>A

ENST00000610292.4:c.881G>A

ENST00000610538.4:c.*17G>A

ENST00000610623.4:c.*17G>A

ENST00000615910.4:c.965G>A

ENST00000617185.4:c.*105G>A

ENST00000618944.4:c.*105G>A

ENST00000619186.4:c.521G>A

ENST00000619485.4:c.881G>A

ENST00000620739.4:c.881G>A

ENST00000622645.4:c.*105G>A

ENST00000635293.1:c.881G>A

NM_000546.5:c.998G>A

NM_001126113.2:c.*17G>A

NM_001126114.2:c.*105G>A

NM_001126115.1:c.602G>A

NM_001126116.1:c.*105G>A

NM_001126117.1:c.*17G>A

NM_001126118.1:c.881G>A

NM_001276695.1:c.*17G>A

NM_001276696.1:c.*105G>A

NM_001276697.1:c.521G>A

NM_001276698.1:c.*105G>A

NM_001276699.1:c.*17G>A

NM_001276760.1:c.881G>A

NM_001276761.1:c.881G>A

NM_001276695.2:c.*17G>A

NM_001276696.2:c.*105G>A

NM_001276697.2:c.521G>A

NM_001276698.2:c.*105G>A

NM_001276699.2:c.*17G>A

NM_001276760.2:c.881G>A

NM_001276761.2:c.881G>A

NM_000546.6:c.998G>A

NM_001126112.3:c.998G>A

NM_001126113.3:c.*17G>A

NM_001126114.3:c.*105G>A

NM_001126115.2:c.602G>A

NM_001126116.2:c.*105G>A

NM_001126117.2:c.*17G>A

NM_001126118.2:c.881G>A

NM_001276695.3:c.*17G>A

NM_001276696.3:c.*105G>A

NM_001276697.3:c.521G>A

NM_001276698.3:c.*105G>A

NM_001276699.3:c.*17G>A

NM_001276760.3:c.881G>A

NM_001276761.3:c.881G>A

Benign

BS2 BS3 BP4

PM2 PM1 PM5 BA1 BS4 BS1 PS2 PS4 PS3 PS1 PP1 PP3

Evidence Links 0

Expert Panel

TP53 VCEP

Criteria Specification Information

Criteria Specification: ClinGen TP53 Expert Panel Specifications to the ACMG/AMP Variant Interpretation Guidelines for TP53 Version 2.3.0

Criteria Specification Approval History

Criteria Specifications for this VCEP

Evidence submitted by expert panel

TP53 VCEP

The NM_000546.6: c.998G>A variant in TP53 is a missense variant predicted to cause substitution of arginine by histidine at amino acid 333 (p.Arg333His). This variant has been observed in 4-7 heterozygous unrelated females from the same data source with no personal history of cancer prior to age 60 years and no personal history of sarcoma at any age (BS2_Moderate; ClinVar SCVs: SCV000285219.10). In vitro assays performed in yeast and/or human cell lines showed functional transactivation and retained growth suppression activity indicating that this variant does not impact protein function (BS3; PMIDs: 12826609, 29979965, 30224644). Computational predictor scores (BayesDel = -0.0924; Align GVGD Class C0) are below the recommended thresholds (BayesDel ≤ -0.008 and an Align GVGD Class ≤ 55), evidence that does not predict a damaging effect on TP53 via protein change. SpliceAI predicts that the variant has no impact on splicing (BP4_Moderate). In summary, this variant meets the criteria to be classified as benign for Li Fraumeni syndrome based on the ACMG/AMP criteria applied, as specified by the ClinGen TP53 VCEP: BS2_Moderate, BS3, BP4_Moderate. (Bayesian Points: -8; VCEP specifications version 2.3; 3/4/2025).

BS2

MODERATE. This variant has been observed in 4-7 heterozygous unrelated females from the same data source with no personal history of cancer prior to age 60 years and no personal history of sarcoma at any age (BS2_Moderate; ClinVar SCVs: SCV000285219.10).

BS3

In vitro assays performed in yeast and/or human cell lines showed functional transactivation and retained growth suppression activity indicating that this variant does not impact protein function(BS3; PMIDs: 12826609, 29979965, 30224644).

BP4

MODERATE. Computational predictor scores (BayesDel = -0.0924; Align GVGD Class C0) are below the recommended thresholds (BayesDel ≤ -0.008 and an Align GVGD Class ≤ 55), evidence that does not predict a damaging effect on TP53 via protein change. SpliceAI predicts that the variant has no impact on splicing. (BP4_Moderate).

PM2

The highest population minor allele frequency in gnomAD v4.1.0 is 0.00008789 (8/91026 alleles) in the South Asian population (PM2, BS1, and BA1 are not met).

PM1

This variant does not reside within a region of TP53 that is defined as a mutational hotspot by the ClinGen TP53 VCEP (PM1 not met).

PM5

Another missense variant (c.997C>T, p.Arg333Cys) in the same codon has been reported (ClinVar Variation ID: 184745). However, the variants have not yet been curated to determine if they would be classified as pathogenic or likely pathogenic by the ClinGen TP53 VCEP’s specifications (PM5 not evaluated).

BA1

The highest population minor allele frequency in gnomAD v4.1.0 is 0.00008789 (8/91026 alleles) in the South Asian population (PM2, BS1, and BA1 are not met).

BS4