# WFS1 Wolframin — A307D Variant Card **Molecular Atlas Pilot · RareResearch.AI · Generated by wolfram-variant-card skill** *Alanine → Aspartic acid at position 307. N-terminal cytoplasmic (intrinsically disordered). ClinVar Uncertain significance, AlphaMissense 0.995, DynaMut2 ΔΔG -0.01 kcal/mol (destabilising).* --- ## Identity | Field | Value | |---|---| | **Variant** | A307D (p.Alanine307Aspartic acid) | | **DNA change** | c.920C>A | | **Gene · Protein** | WFS1 · Wolframin (890 aa) | | **UniProt** | O76024 · WFS1_HUMAN | | **ClinVar accession** | VCV001320779 | | **Amino acid change** | Alanine (A) → Aspartic acid (D) | --- ## Structural Context | Field | Value | |---|---| | **AlphaFold model** | AF-O76024-F1, v6 | | **pLDDT at residue 307** | **59.72** — confident | | **Domain** | N-terminal cytoplasmic (intrinsically disordered) | | **Position context** | N-terminal cytoplasmic (intrinsically disordered) | | **IDR flag** | No — pLDDT above 50 threshold | **UniProt features at this position:** (none catalogued) > Position 307 sits in N-terminal cytoplasmic (intrinsically disordered). The wild-type residue is small/hydrophobic (alanine — methyl sidechain); the mutant is negatively charged (aspartate — carboxylate). The chemistry shift implies altered local packing, hydrogen-bonding, and/or electrostatics at this site. --- ## Computational Predictions ### AlphaMissense | Field | Value | |---|---| | am_pathogenicity | **0.9953** | | am_class | **likely pathogenic** | | Interpretation | Likely pathogenic (threshold 0.564) | ### DynaMut2 | Field | Value | |---|---| | ΔΔG (kcal/mol) | **-0.01 (Destabilising)** | | Job ID | 178092086702 | | Result URL | https://biosig.lab.uq.edu.au/dynamut2/results_prediction/178092086702 | --- ## Clinical Evidence | Field | Value | |---|---| | Classification | **Uncertain significance** | | Review status | criteria provided, single submitter | | Last evaluated | 2021/04/27 00:00 | | Inheritance | Inheritance pattern not specified in ClinVar entry; WFS1 has both AD and AR presentations. | | WFS1 variant landscape | A307D is 1 of ~326 pathogenic-spectrum variants in WFS1 (out of 2,243 catalogued in ClinVar) | (no conditions catalogued) --- ## 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 3/4 — Most Druggable** Category 3/4 — Most Druggable

|ΔΔG|=0.01 < 2 kcal/mol (fold intact) + AlphaMissense 0.995 confirms functional impact. Specific local contacts disrupted — priority for docking and pharmacological chaperone screening. **Why this card matters.** Wolframin's fold survives this substitution (|ΔΔG|=0.01 kcal/mol). The pathogenic signal is real — AlphaMissense places it at 0.995. 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 - `A307D_molstar_viewer.html` — interactive 3D viewer (auto-highlights position 307 with ball-and-stick + neighbors within 5Å) - `A307D_variant_card.md` — this card (source of truth) - `A307D_variant_card.html` — styled printable card - `A307D_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) - `A307D_wildtype_interactions.pse` / `A307D_mutant_interactions.pse` — PyMOL sessions --- *Generated by wolfram-variant-card skill · RareResearch.AI Molecular Atlas* *Every assumption documented. Every score sourced.*