P67T — LYFE SCIENCES

Genetic Information

Gene & Transcript Details

Gene

MSH6

Transcript

NM_000179.3 MANE Select

Total Exons

—

Reference Sequence

NC_000002.11

Alternative Transcripts

ID	Status	Details
NM_000179.3	MANE Select	4265 nt \| 90–4172
NM_000179.2	RefSeq Select	4435 nt \| 153–4235
NM_000179.1	Alternative	4264 nt \| 88–4170

Variant Details

HGVS Notation

NM_000179.3:c.199C>A

Protein Change

P67T

Location

Exon 1 (Exon 1 of )

5'Exon Structure3'

Functional Consequence

Loss of Function

Alternate Identifiers

—

Clinical & Population Data

Population Frequency

gnomAD

Global Frequency

0.00095 in 100,000

Extremely Rare

ACMG Criteria Applied PM2

This variant is absent or extremely rare in population databases (PM2 criteria applies).

ClinVar

Open

Classification

Uncertain Significance (VUS)

3 publications

Clinical Statement

"This variant has been reported in ClinVar as Benign (1 clinical laboratories) and as Uncertain significance (4 clinical laboratories) and as Uncertain Significance (1 clinical laboratories)."

COSMIC Somatic Evidence

Open

COSMIC ID

Recurrence

0 occurrences

PM1 Criteria

Not Applied

COSMIC Database Preview

Accessing full COSMIC database details requires institutional login or subscription.

Functional Impact & Domains

Functional Domain

Hotspot Status

Not a hotspot

Domain Summary

This variant is not located in a mutational hotspot or critical domain.

Related Variants in This Domain

No evidence of other pathogenic variants at this position in gene MSH6.

Functional Studies & Therapeutic Relevance

OncoKB JAX-CKB

Functional Summary

Error in OpenAI Consolidation. OncoKB: MSH6P67TMSH6P67TSomaticNCBI Gene:2956|Show additional gene information Variant OverviewMSH6, a DNA mismatch repair protein, is frequently mutated in colorectal, small bowel, and endometrial cancers.The MSH6 P67T mutation has not specifically been reviewed by the OncoKB team, and therefore its biological significance is unknown. JAX-CKB: No results found

Database Previews

OncoKB

JAX-CKB

Click on previews to view full database entries. External databases may require institutional access.

Computational Analysis

Pathogenicity Predictions

SpliceAI

Predictor Consensus

Mixed/VUS

PP3 Applied

REVEL Score

0.0

Threshold: ≥0.75 = PP3 applied

SpliceAI Scores

Window: ±500bp

Effect Type	Score	Position
- Acceptor Loss (AL)	0.0	257 bp
- Donor Loss (DL)	0.06	-201 bp
+ Acceptor Gain (AG)	0.0	246 bp
+ Donor Gain (DG)	0.0	38 bp

High impact (≥0.5) Medium impact (0.2-0.49) Low impact (<0.2)

VCEP Guidelines

Applied ACMG/AMP Criteria (VCEP Specific)

Filter Criteria:

PM2

PM2 (Unknown (Pre-LLM))

From pre-LLM assessment (LLM Failed)

BP4

BP4 (Unknown (Pre-LLM))

From pre-LLM assessment (LLM Failed)