Evidence Repository - Clinical Genome Resources

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Variant: NM_000546.6(TP53):c.733G>A (p.Gly245Ser)

CA000367

12365 (ClinVar)

Gene: TP53

Condition: Li-Fraumeni syndrome

Inheritance Mode: Autosomal dominant inheritance

Link to MONDO

UUID: ed201831-1d8d-4c6d-ad13-1055f8d3407b

Approved on: 2024-08-05

Published on: 2024-08-05

HGVS expressions

NM_000546.6:c.733G>A

NM_000546.6(TP53):c.733G>A (p.Gly245Ser)

NC_000017.11:g.7674230C>T

CM000679.2:g.7674230C>T

NC_000017.10:g.7577548C>T

CM000679.1:g.7577548C>T

NC_000017.9:g.7518273C>T

NG_017013.2:g.18321G>A

ENST00000503591.2:c.733G>A

ENST00000508793.6:c.733G>A

ENST00000509690.6:c.337G>A

ENST00000514944.6:c.454G>A

ENST00000604348.6:c.712G>A

ENST00000269305.9:c.733G>A

ENST00000269305.8:c.733G>A

ENST00000359597.8:c.733G>A

ENST00000413465.6:c.733G>A

ENST00000420246.6:c.733G>A

ENST00000445888.6:c.733G>A

ENST00000455263.6:c.733G>A

ENST00000504290.5:c.337G>A

ENST00000504937.5:c.337G>A

ENST00000509690.5:c.337G>A

ENST00000510385.5:c.337G>A

ENST00000514944.5:c.454G>A

ENST00000610292.4:c.616G>A

ENST00000610538.4:c.616G>A

ENST00000610623.4:c.256G>A

ENST00000615910.4:c.700G>A

ENST00000617185.4:c.733G>A

ENST00000618944.4:c.256G>A

ENST00000619186.4:c.256G>A

ENST00000619485.4:c.616G>A

ENST00000620739.4:c.616G>A

ENST00000622645.4:c.616G>A

ENST00000635293.1:c.616G>A

NM_000546.5:c.733G>A

NM_001126112.2:c.733G>A

NM_001126113.2:c.733G>A

NM_001126114.2:c.733G>A

NM_001126115.1:c.337G>A

NM_001126116.1:c.337G>A

NM_001126117.1:c.337G>A

NM_001126118.1:c.616G>A

NM_001276695.1:c.616G>A

NM_001276696.1:c.616G>A

NM_001276697.1:c.256G>A

NM_001276698.1:c.256G>A

NM_001276699.1:c.256G>A

NM_001276760.1:c.616G>A

NM_001276761.1:c.616G>A

NM_001276695.2:c.616G>A

NM_001276696.2:c.616G>A

NM_001276697.2:c.256G>A

NM_001276698.2:c.256G>A

NM_001276699.2:c.256G>A

NM_001276760.2:c.616G>A

NM_001276761.2:c.616G>A

NM_001126112.3:c.733G>A

NM_001126113.3:c.733G>A

NM_001126114.3:c.733G>A

NM_001126115.2:c.337G>A

NM_001126116.2:c.337G>A

NM_001126117.2:c.337G>A

NM_001126118.2:c.616G>A

NM_001276695.3:c.616G>A

NM_001276696.3:c.616G>A

NM_001276697.3:c.256G>A

NM_001276698.3:c.256G>A

NM_001276699.3:c.256G>A

NM_001276760.3:c.616G>A

NM_001276761.3:c.616G>A

Pathogenic

PM2_Supporting PS2_Moderate PM1 PS4 PS3 PP3 PP4_Moderate

BA1 PM5 BS2 BS4 BS1 BS3 BP4 PVS1 PS1 PP1

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 2.0.0

Criteria Specification Approval History

Criteria Specifications for this VCEP

Evidence submitted by expert panel

TP53 VCEP

The NM_000546.6: c.733G>A variant in TP53 is a missense variant predicted to cause substitution of glycine by serine at amino acid 245 (p.Gly245Ser). This variant has been identified as a de novo occurrence with unconfirmed parental relationships in 1 individual with a strongly LFS-associated cancer totaling 2 phenotype points (PS2_Moderate; Internal lab contributor: SCV000184981.8). This variant has been reported in an additional individual meeting Classical criteria and 11 individuals meeting Revised Chompret criteria. Based on this evidence, this variant scores 8 total points meeting the TP53 VCEP phenotype scoring criteria of ≥ 8 points. (PS4_Very Strong; PMIDs: 11370630, 32156018, 32888145, 33245408, 34670578, 35974385, 20522432, 24122735, Internal lab contributor: SCV000184981.8). At least two individuals with this variant were found to have a variant allele fraction of 5-25%, which is a significant predictor of variant pathogenicity (PP4_Moderate, PMID: 34906512, Internal lab contributors: SCV000184981.8). This variant has an allele frequency of 0.000002543 (3/1179926 alleles) in the European (non-Finnish) population in gnomAD v4.1.0 which is lower than the Clingen TP53 VCEP threshold (<0.00004) for PM2_Supporting, and therefore meets this criterion (PM2_Supporting). In vitro assays performed in yeast and/or human cell lines showed non-functional transactivation and loss of growth suppression activity indicating that this variant impacts protein function (PMIDs: 12826609, 30224644, 29979965) (PS3). This variant resides within a codon (NM_00546.4: 175, 245, 248, 249, 273, 282) of TP53 that is defined as a mutational hotspot by the ClinGen TP53 VCEP (PMID: 8023157 ) (PM1). Computational predictor scores (BayesDel = 0.5536; Align GVGD = Class C55) are above recommended thresholds (BayesDel > 0.16 and an Align GVGD Class of > 15), evidence that correlates with impact to TP53 via protein change (PP3). In summary, this variant meets the criteria to be classified as Pathogenic for Li Fraumeni Syndrome based on the ACMG/AMP criteria applied, as specified by the ClinGen TP53 VCEP: PS2_Moderate, PS4_Very Strong, PP4_Moderate, PM2_Supporting, PS3, PM1, PP3. (Bayesian Points: 20; VCEP specifications version 2.0; 7/24/2024)

PM2_Supporting

This variant has an allele frequency of 0.000002543 (3/1179926 alleles) in the European (non-Finnish) population in gnomAD v4.1.0 which is lower than the Clingen TP53 VCEP threshold (<0.00004) for PM2_Supporting, and therefore meets this criterion (PM2_Supporting).

PS2_Moderate

This variant has been identified as a de novo occurrence with unconfirmed parental relationships in 1 individual with a strongly LFS-associated cancer totaling 2 phenotype points (PS2_Moderate; Internal lab contributor: SCV000184981.8).

PM1

This variant resides within a codon (NM_00546.4: 175, 245, 248, 249, 273, 282) of TP53 that is defined as a mutational hotspot by the ClinGen TP53 VCEP (PMID: 8023157 ) (PM1).

PS4

PS4_VERY STRONG APPLIED This variant has been reported in 1 individual meeting Classical criteria and 11 individuals meeting Revised Chompret criteria. Based on this evidence, this variant scores 8 total points meeting the TP53 VCEP phenotype scoring criteria of ≥ 8 points. (PS4_Very Strong; PMIDs: 11370630, 32156018, 32888145, 33245408, 34670578, 35974385, 20522432, 24122735, Internal lab contributor: SCV000184981.8).

PS3

In vitro assays performed in yeast and/or human cell lines showed non-functional transactivation and loss of growth suppression activity indicating that this variant impacts protein function (PMIDs: 12826609, 30224644, 29979965) (PS3).

PP3

Computational predictor scores (BayesDel = 0.5536; Align GVGD = Class C55) are above recommended thresholds (BayesDel > 0.16 and an Align GVGD Class of > 15), evidence that correlates with impact to TP53 via protein change (PP3).

PP4_Moderate

At least two individuals with this variant were found to have a variant allele fraction of 5-25%, which is a significant predictor of variant pathogenicity (PP4_Moderate, PMID: 34906512, Internal lab contributors: SCV000184981.8).

BA1