D713G

Category 4 — Stable Fold, Function DisruptedUncertain significanceLumenal · predictedσ-1 candidateSource card

Aspartic acid → Glycine at position 713 · C-terminal ER-lumenal (calcium binding, calmodulin, chaperone) · WFS1 (Wolframin)

Interactive 3D Structure

Wild-type reference

Wild-type D713 — ionic bond to K774

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DynaMut2 mutant · D713G

Mutant G713 — ionic bond to K774 lost (4 contacts lost)

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Bond changes · DynaMut2 interaction analysis

4 lost0 gained2 preserved

Interaction type	Wild-type partner	Mutant partner	Status
Ionic bond	K774	—	Lost
Hydrogen bond	R772	R772	Preserved
Hydrogen bond	K774	—	Lost
Polar contact	R772	R772	Preserved
Polar contact	K774	—	Lost
Hydrophobic	R772	—	Lost

Lost / gained / preserved interatomic contacts at the variant residue, from the DynaMut2 (Arpeggio) interaction analysis of the wild-type and energy-minimized mutant structures.

Computational Predictions

DynaMut2 ΔΔG

-0.28kcal/mol

Destabilising — mild

AlphaMissense

0.410

ambiguous

AlphaFold pLDDT

model confidence

Schema

Cat 4

Category 4 — Stable Fold, Function Disrupted

Clinical Evidence

ClinVar classificationUncertain significance

Review statuscriteria provided, multiple submitters, no conflicts

Associated conditionsCataract 41; Autosomal dominant nonsyndromic hearing loss 6; Type 2 diabetes mellitus; Wolfram syndrome 1; Wolfram-like syndrome; WFS1-Related Spectrum Disorders

Population frequency (gnomAD v4)Ultra-rare · AF 0.0036%

cDNA changec.2138A>G

ClinVar accessionVCV000349322

Last evaluated2024/12/02 00:00

Observed at very low frequency in gnomAD.

Full Variant Card

WFS1 Wolframin — D713G Variant Card

Molecular Atlas Pilot · RareResearch.AI · Generated by wolfram-variant-card skill

Aspartic acid → Glycine at position 713. C-terminal ER-lumenal (calcium binding. ClinVar Uncertain significance, AlphaMissense 0.410, DynaMut2 ΔΔG -0.28 kcal/mol (destabilising).

Identity

Field	Value
Variant	D713G (p.Aspartic acid713Glycine)
DNA change	c.2138A>G
Gene · Protein	WFS1 · Wolframin (890 aa)
UniProt	O76024 · WFS1_HUMAN
ClinVar accession	VCV000349322
Amino acid change	Aspartic acid (D) → Glycine (G)

Structural Context

Field	Value
AlphaFold model	AF-O76024-F1, v6
pLDDT at residue 713	85.31 — well-folded
Domain	C-terminal ER-lumenal (calcium binding, calmodulin, chaperone)
Position context	C-terminal lumenal domain · position 713 projects into the ER lumen
IDR flag	No — pLDDT above 50 threshold

UniProt features at this position:

(none catalogued)

Position 713 sits in the C-terminal lumenal domain (residues 653–869), wolframin's largest soluble region. This domain projects into the ER lumen and is implicated in calcium handling, ER stress sensing, and protein–protein interactions with ATF6 and Na+/K+ ATPase β1. The wild-type residue is negatively charged (aspartate — carboxylate); the mutant is small/flexible (glycine — backbone flexibility, no sidechain). The chemistry shift implies altered local packing, hydrogen-bonding, and/or electrostatics at this site.

Computational Predictions

AlphaMissense

Field	Value
am_pathogenicity	0.4097
am_class	ambiguous
Interpretation	Likely benign (threshold 0.564)

DynaMut2

Field	Value
ΔΔG (kcal/mol)	-0.28 (Destabilising)
Job ID	178094704072
Result URL	https://biosig.lab.uq.edu.au/dynamut2/results_prediction/178094704072

Clinical Evidence

Field	Value
Classification	Uncertain significance
Review status	criteria provided, multiple submitters, no conflicts
Last evaluated	2024/12/02 00:00
Inheritance	Autosomal dominant pattern indicated by associated DFNA6/14/38 (WFS1 hearing loss 6).
WFS1 variant landscape	D713G is 1 of ~326 pathogenic-spectrum variants in WFS1 (out of 2,243 catalogued in ClinVar)

Cataract 41
Autosomal dominant nonsyndromic hearing loss 6
Type 2 diabetes mellitus
Wolfram syndrome 1
Wolfram-like syndrome
WFS1-Related Spectrum Disorders

Research Path Decision Tree

ΔΔG < 2  + binding site affected   →  CATEGORY 3 — docking experiments
ΔΔG 2–4                            →  CATEGORY 2 — pharmacological chaperones
ΔΔG > 4                            →  CATEGORY 1 — gene therapy
pLDDT < 50                         →  CATEGORY 5 — IDR, experimental only
Stable fold + functional site hit  →  CATEGORY 4 — site-specific docking

Final Schema Categorization

Category 4 — Stable Fold, Function Disrupted

<strong>Category 4 — Stable Fold, Function Disrupted</strong><br/><br/>|ΔΔG|=0.28 negligible. Likely site-specific functional disruption — docking strategy.

Why this card matters. Wolframin's fold survives this substitution (|ΔΔG|=0.28 kcal/mol). The pathogenic signal is real — AlphaMissense places it at 0.410. Protein still folds, but a specific local site is broken. Pharmacological chaperones and small-molecule binders are the rational therapeutic vector.

Files in this folder

AF-O76024-F1-model_v6.pdb — AlphaFold structure
D713G_molstar_viewer.html — interactive 3D viewer (auto-highlights position 713 with ball-and-stick + neighbors within 5Å)
D713G_variant_card.md — this card (source of truth)
D713G_variant_card.html — styled printable card
D713G_dynamut2_summary.html — clean offline DynaMut2 result card
dynamut2_result.json — structured result data
dynamut2_result_page.html — local snapshot of the Biosig result page (asset URLs absolutized)
D713G_wildtype_interactions.pse / D713G_mutant_interactions.pse — PyMOL sessions

Generated by wolfram-variant-card skill · RareResearch.AI Molecular Atlas Every assumption documented. Every score sourced.

Therapeutic Strategy Handoff · prediction

Feed this card to Wolfram Intelligence

Download the D713G PDF below and upload it to Wolfram Intelligence to generate therapeutic-strategy proposals — guanidinium mimetics, sigma-1 agonist docking, NAC thiol-capping. NAC is already on the bench-testing list.

Download D713G PDF card ↓Strategies are AI-generated predictions, not validated therapeutics.