Sugi Atlas

Atlas / Disease / neuronopathy, distal hereditary motor, type 7A

neuronopathy, distal hereditary motor, type 7A

disease
On this page

Also known as HMN7Aneuronopathy, distal hereditary motor caused by mutation in SLC5A7neuronopathy, distal hereditary motor, type VIIASLC5A7 neuronopathy, distal hereditary motor

Summary

neuronopathy, distal hereditary motor, type 7A (MONDO:0008024) is a disease caused by SLC5A7 (GenCC Strong), with 3 cohort genes.

At a glance

  • Causal gene: SLC5A7 (GenCC Strong)
  • Cohort genes: 3
  • ClinVar variants: 499

Clinical features

No curated clinical features (Orphanet) for this disease.

Identifiers

Disease identifiers

FieldValue
Canonical nameneuronopathy, distal hereditary motor, type 7A
Mondo IDMONDO:0008024
MeSHC563562
OMIM158580
DOIDDOID:0111201
UMLSC1834703
MedGen322474
GARD0018269
Is cancer (heuristic)no

Also known as: HMN7A · neuronopathy, distal hereditary motor caused by mutation in SLC5A7 · neuronopathy, distal hereditary motor, type VIIA · SLC5A7 neuronopathy, distal hereditary motor

Data availability: 499 ClinVar variants · 4 GenCC gene-disease records.

Disease family

Classification path: disease › human disease › disease by etiologic mechanism › disease of genetic or genomic mechanism › hereditary disease › autosomal genetic disease › autosomal dominant disease › neuronopathy, distal hereditary motor, autosomal dominantdistal hereditary motor neuropathy type 7neuronopathy, distal hereditary motor, type 7A

Related subtypes (1): neuronopathy, distal hereditary motor, type 7B

Genetics & variants

GWAS landscape

No GWAS associations recorded — common-variant (GWAS) studies don’t cover this disease (typical for Mendelian / rare diseases). See the curated gene cohort and Mendelian overlap below.

Variant details and genetic-evidence tiers

ClinVar germline variants

499 retrieved; paginated sample, class counts are floors:

276 uncertain significance, 185 likely benign, 17 conflicting classifications of pathogenicity, 6 likely pathogenic, 5 benign, 5 pathogenic, 5 benign/likely benign

ClinVarVariant (HGVS)GeneClassificationReview
1426671NM_021815.5(SLC5A7):c.364dup (p.Tyr122fs)SLC5A7Pathogeniccriteria provided, single submitter
3752933NM_021815.5(SLC5A7):c.719G>A (p.Trp240Ter)SLC5A7Pathogeniccriteria provided, single submitter
3756992NM_021815.5(SLC5A7):c.134del (p.Gly45fs)SLC5A7Pathogeniccriteria provided, single submitter
4784269NM_021815.5(SLC5A7):c.836del (p.Phe279fs)SLC5A7Pathogeniccriteria provided, single submitter
4788433NM_021815.5(SLC5A7):c.101dup (p.Ser34fs)SLC5A7Pathogeniccriteria provided, single submitter
1009672NM_021815.5(SLC5A7):c.292+1G>ASLC5A7Likely pathogeniccriteria provided, single submitter
1027324NM_021815.5(SLC5A7):c.895+1G>CSLC5A7Likely pathogeniccriteria provided, multiple submitters, no conflicts
1415144NM_021815.5(SLC5A7):c.179-2A>GSLC5A7Likely pathogeniccriteria provided, single submitter
2500960NM_021815.5(SLC5A7):c.742-2A>GSLC5A7Likely pathogeniccriteria provided, single submitter
265763NM_021815.5(SLC5A7):c.1082G>A (p.Arg361Gln)SLC5A7Likely pathogeniccriteria provided, single submitter
2691886NM_021815.5(SLC5A7):c.1503_1506del (p.Phe502fs)SLC5A7Likely pathogeniccriteria provided, single submitter
1042814NM_021815.5(SLC5A7):c.1177A>G (p.Thr393Ala)SLC5A7Conflicting classifications of pathogenicitycriteria provided, conflicting classifications
1476505NM_021815.5(SLC5A7):c.81G>A (p.Trp27Ter)SLC5A7Conflicting classifications of pathogenicitycriteria provided, conflicting classifications
1596627NM_021815.5(SLC5A7):c.742-5C>TSLC5A7Conflicting classifications of pathogenicitycriteria provided, conflicting classifications
1810255NM_021815.5(SLC5A7):c.320G>A (p.Arg107His)SLC5A7Conflicting classifications of pathogenicitycriteria provided, conflicting classifications
2542724NM_021815.5(SLC5A7):c.1480A>G (p.Ile494Val)SLC5A7Conflicting classifications of pathogenicitycriteria provided, conflicting classifications
39495NM_021815.5(SLC5A7):c.1497del (p.Lys499fs)SLC5A7Conflicting classifications of pathogenicityno assertion criteria provided
440281NM_021815.5(SLC5A7):c.1306G>A (p.Val436Met)SLC5A7Conflicting classifications of pathogenicitycriteria provided, conflicting classifications
464174NM_021815.5(SLC5A7):c.46C>T (p.Leu16Phe)SLC5A7Conflicting classifications of pathogenicitycriteria provided, conflicting classifications
532814NM_021815.5(SLC5A7):c.1643G>A (p.Arg548Gln)SLC5A7Conflicting classifications of pathogenicitycriteria provided, conflicting classifications
532824NM_021815.5(SLC5A7):c.1237G>A (p.Val413Ile)SLC5A7Conflicting classifications of pathogenicitycriteria provided, conflicting classifications
549706NM_021815.5(SLC5A7):c.1549G>A (p.Val517Ile)SLC5A7Conflicting classifications of pathogenicitycriteria provided, conflicting classifications
572646NM_021815.5(SLC5A7):c.385C>T (p.Leu129Phe)SLC5A7Conflicting classifications of pathogenicitycriteria provided, conflicting classifications
580407NM_021815.5(SLC5A7):c.1246G>A (p.Val416Ile)SLC5A7Conflicting classifications of pathogenicitycriteria provided, conflicting classifications
648681NM_021815.5(SLC5A7):c.1478G>T (p.Cys493Phe)SLC5A7Conflicting classifications of pathogenicitycriteria provided, conflicting classifications
650165NM_021815.5(SLC5A7):c.973C>A (p.Gln325Lys)SLC5A7Conflicting classifications of pathogenicitycriteria provided, conflicting classifications
782193NM_021815.5(SLC5A7):c.1529A>C (p.Lys510Thr)SLC5A7Conflicting classifications of pathogenicitycriteria provided, conflicting classifications
945469NM_021815.5(SLC5A7):c.1496A>C (p.Lys499Thr)SLC5A7Conflicting classifications of pathogenicitycriteria provided, conflicting classifications
464169Single alleleCCDC138Uncertain significancecriteria provided, single submitter
833287NC_000002.12:g.(?107988146)(108963283_?)dupCCDC138Uncertain significancecriteria provided, single submitter

Genes & proteins

Mendelian disease overlap and somatic drivers

GenCC: 10 · Orphanet: 2 · OMIM-shared: 0 · Dual-evidence (GWAS+Mendelian): 0

GenCC gene–disease validity (cohort genes)

the Disease column is the GenCC-asserted condition — a cohort gene’s strongest validity may be for a related predisposition syndrome.

GeneClassificationInheritanceDiseaseRecords
SLC5A7StrongAutosomal dominantneuronopathy, distal hereditary motor, type 7A10

Orphanet rare-disease linkage (cohort genes)

GeneOrphanet IDRare disease
SLC5A7Orphanet:139589Distal hereditary motor neuropathy type 7
SLC5A7Orphanet:98914Presynaptic congenital myasthenic syndromes

Cohort genes → proteins

3 cohort genes, 3 distinct canonical proteins.

Evidence partition

SubsetGenes
multi_evidence3

Cohort genes (full)

SymbolHGNCEnsemblUniProtNameEvidence
SLC5A7HGNC:14025ENSG00000115665Q9GZV3High affinity choline transporter 1gencc,clinvar
SULT1C2HGNC:11456ENSG00000198203O00338Sulfotransferase 1C2clinvar
CCDC138HGNC:26531ENSG00000163006Q96M89Coiled-coil domain-containing protein 138clinvar

Cohort function summary

Lead sentence per gene, UniProt-curated.

SymbolProtein nameFunction (lead sentence)
SLC5A7High affinity choline transporter 1High-affinity Na(+)-coupled choline transmembrane symporter.
SULT1C2Sulfotransferase 1C2Sulfotransferase that utilizes 3’-phospho-5’-adenylyl sulfate (PAPS) to catalyze the sulfate conjugation of phenolic compounds.

Protein-family classification

Druggable: 1 · Difficult: 0 · Unknown: 2 · Druggable fraction: 0.33

Family distribution

Cohort families vs a genome-wide background (hypergeometric, BH-FDR; fold = observed/expected). Counts kept; sorted by enrichment, so the catch-all Other/Unknown bucket no longer leads.

FamilyGenesFoldFDR
Transporter125.9×0.076
Other/Unknown21.2×0.587

Per-gene assignment

SymbolFamilyDruggable?ECInterPro (top 3)
SLC5A7TransporteryesNa/solute_symporter, Na/Glc_symporter_sf, Choline_transporter
SULT1C2Other/UnknownnoSulfotransferase_dom, P-loop_NTPase
CCDC138Other/UnknownnoCCDC138, CCDC138_C, CCDC138_CC

Expression context

Cohort genes with no expression data: 0.

3 cohort genes are a single-cell marker in ≥1 SCXA experiment.

Breadth distribution (Bgee present_calls)

BucketGenes
narrow (1-5 tissues)0
moderate (6-20)0
broad (>20)3
unknown0

Top tissues across cohort

TissueCohort genes
male germ line stem cell (sensu Vertebrata) in testis2
pancreatic ductal cell1
primordial germ cell in gonad1
nephron tubule1
pylorus1
renal medulla1
sperm1
ventricular zone1

Per-gene tissue summary (top 30)

SymbolBgee breadthFANTOM5 breadthSCXATop tissues
SLC5A7101tissue_specificmarkermale germ line stem cell (sensu Vertebrata) in testis, pancreatic ductal cell, primordial germ cell in gonad
SULT1C2191broadmarkerpylorus, nephron tubule, renal medulla
CCDC138178ubiquitousmarkermale germ line stem cell (sensu Vertebrata) in testis, sperm, ventricular zone

Protein interactions among cohort

Intra-cohort edges: 0.

Hub genes (top 10 by interactor count)

SymbolInteractor count
SLC5A71,536
CCDC138829
SULT1C2620

Structural data

PDB: 2 · AlphaFold-only: 1 · No structure: 0

Cohort genes with PDB structures (top 30)

SymbolUniProtPDB entries
SLC5A7Q9GZV312
SULT1C2O003381

AlphaFold-only cohort genes (top 30 by pLDDT)

SymbolUniProtpLDDT
CCDC138Q96M8973.25

Function

Pathway analysis

Distinct Reactome pathways touched by cohort: 17. Enrichment computed across 3 evidence-associated genes (2 with Reactome annotation).

Pathways by enrichment

Over-representation of cohort genes vs the genome-wide background (hypergeometric test, Benjamini-Hochberg FDR; fold = observed/expected over 2 annotated cohort genes). Counts and members are kept as ground-truth; sorted by enrichment.

PathwayCohort genesFoldFDRSample cohort genes
Defective SLC5A7 in the neurotransmitter release cycle causes distal hereditary motor neuronopathy 7A (HMN7A)15710.0×0.001SLC5A7
Defective transport by SLC5A7 causes distal hereditary motor neuronopathy 7A (HMN7A)15710.0×0.001SLC5A7
SLC-mediated bile acid transport1815.7×0.007SLC5A7
Acetylcholine Neurotransmitter Release Cycle1335.9×0.013SLC5A7
Cytosolic sulfonation of small molecules1259.6×0.013SULT1C2
Neurotransmitter release cycle1219.6×0.013SLC5A7
Phase II - Conjugation of compounds1139.3×0.017SULT1C2
SLC transporter disorders1102.0×0.021SLC5A7
R-HSA-425366190.6×0.021SLC5A7
Disorders of transmembrane transporters169.6×0.024SLC5A7
Biological oxidations164.9×0.024SULT1C2
Transmission across Chemical Synapses138.1×0.037SLC5A7
SLC-mediated transmembrane transport129.6×0.044SLC5A7
Neuronal System122.1×0.054SLC5A7
Transport of small molecules112.6×0.088SLC5A7
Disease16.5×0.156SLC5A7
Metabolism15.8×0.165SULT1C2

GO biological processes by enrichment

Over-representation of cohort genes vs the genome-wide background (hypergeometric test, Benjamini-Hochberg FDR; fold = observed/expected over 2 annotated cohort genes). Counts and members are kept as ground-truth; sorted by enrichment.

GO termCohort genesFoldFDRSample cohort genes
acetylcholine biosynthetic process12808.7×0.003SLC5A7
amine metabolic process11203.7×0.004SULT1C2
choline transport1766.0×0.004SLC5A7
sulfation1526.6×0.004SULT1C2
synaptic transmission, cholinergic1401.2×0.004SLC5A7
neuromuscular synaptic transmission1300.9×0.005SLC5A7
neurotransmitter transport1210.7×0.006SLC5A7
transmembrane transport184.3×0.013SLC5A7
in utero embryonic development136.0×0.028SLC5A7

Therapeutics

Drug target analysis

Approved (phase 4): 0 · Phase ≥3: 1 · Phased (≥1): 1 · Undrugged: 2

Druggability breadth: 2 of 3 evidence-associated genes (67%) have a ChEMBL target (buckets above are over the deeply-mined display cohort).

Top cohort targets by molecule count

SymbolMoleculesMax phase
SLC5A713
SULT1C200
CCDC13800

Drugs targeting cohort genes (top 30)

MoleculeMax phaseTargets in cohort
CHOLINE CHLORIDE3SLC5A7

Bioactivity and enzyme data

Enzyme cohort genes (≥1 EC): 0.

Cohort genes with ChEMBL bioactivity (full, sorted by assay count)

SymbolAssaysType breakdown
SLC5A734Binding:24, Functional:10
SULT1C21ADMET:1

Pharmacogenomics

Cohort genes with a PharmGKB record: 3; with CPIC/DPWG dosing guidelines: 0.

No cohort gene has a CPIC/DPWG genotype-guided dosing guideline (PharmGKB).

Chemical tractability of cohort targets

1 approved/phased compounds have measured bioactivity against a cohort gene (and aren’t yet in disease-level trials). This is a research / tractability signal, NOT a therapeutic recommendation — a bioactivity row often reflects off-target or screening binding (e.g. promiscuous kinase inhibitors against a cohort kinase), implying no disease mechanism.

CompoundMax phaseCohort target (bioactivity)
CHOLINE CHLORIDE3SLC5A7

Druggability pyramid

Cohort genes binned by druggability tier (high → low):

TierDefinitionGenesSymbols
AApproved (phase 4 drug)0
BPhased (≥1) drug, not yet approved1SLC5A7
CDruggable family + PDB, no drug0
DDruggable family + AlphaFold only, no drug0
EDifficult family or no structure, no drug2SULT1C2, CCDC138

Undrugged target profiles

2 cohort genes are undrugged. Ranked by ‘starting-point quality’ (assay depth + drugged-partner adjacency).

SymbolChEMBL assaysDrugged partners (top 3)
SULT1C21
CCDC1380

Clinical trials & evidence

Clinical trials

Clinical trials: 0.

About this page

Generated deterministically by Sugi Atlas from primary biomedical databases via BioBTree. Every record on this page traces to a primary source.

Generated
Atlas version
v1.1.4
BioBTree
v2.0.2

Sources 68

This page pulls from 68 datasets indexed by BioBTree:

alphafoldantibodybgeebgee_evidencebindingdbbiogrid_interactionbrendabrenda_kineticscellosauruschembl_activitychembl_assaychembl_documentchembl_moleculechembl_targetcivic_evidenceclingen_dosageclinical_trialsclinvarctd_gene_interactiondepmapdiamond_similaritydoidefoensemblentrezesm2_similarityfantom5_genefantom5_promotergardgenccgenerifgogtopdbgtopdb_interactiongwasgwas_studyhgncintactinterpromedgenmeshmimmondomondochildmondoparentorphanetpatent_compoundpdbpfampharmgkb_clinicalpharmgkb_genepharmgkb_guidelinepharmgkb_variantpubchempubchem_activitypubchem_assayreactomerefseqrhearnacentralscxa_expressionscxa_gene_experimentsignorstring_interactiontranscriptufeatureumlsuniprot