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encyclopedia of Rare Disease Annotation for Precision Medicine



   best vitelliform macular dystrophy
  

Disease ID 568
Disease best vitelliform macular dystrophy
Definition
Autosomal dominant hereditary maculopathy with childhood-onset accumulation of LIPOFUSION in RETINAL PIGMENT EPITHELIUM. Affected individuals develop progressive central acuity loss, and distorted vision (METAMORPHOPSIA). It is associated with mutations in bestrophin, a chloride channel.
Synonym
best disease
best macular dystrophy
best's disease
disease, best
disease, best's
dystrophies, vitelliform macular
dystrophy, best macular
dystrophy, vitelliform macular
macular degeneration, polymorphic vitelline
macular dystrophies, vitelliform
macular dystrophy, best
macular dystrophy, vitelliform
macular dystrophy, vitelliform, 2
vitelliform dystrophy (disorder)
vitelliform macular dystrophies
vitelliform macular dystrophy
vitelliform macular dystrophy [disease/finding]
vmd2
Orphanet
OMIM
DOID
UMLS
C0339510
MeSH
SNOMED-CT
Comorbidity
UMLS | Disease | Sentences' Count(Total Sentences:2)
C0024441  |  macular hole  |  3
C0456909  |  vision loss  |  1
Curated Gene
Entrez_id | Symbol | Resource(Total Genes:2)
5961  |  PRPH2  |  CTD_human;GHR
7439  |  BEST1  |  CLINVAR;CTD_human;GHR;ORPHANET;UNIPROT
Inferring Gene(Waiting for update.)
Text Mined Gene
Entrez_id | Symbol | Score | Resource(Total Genes:41)
24  |  ABCA4  |  4.204  |  DISEASES
55107  |  ANO1  |  2.221  |  DISEASES
7439  |  BEST1  |  8.279  |  DISEASES
144453  |  BEST3  |  4.588  |  DISEASES
266675  |  BEST4  |  5.143  |  DISEASES
659  |  BMPR2  |  1.261  |  DISEASES
65250  |  C5orf42  |  2.394  |  DISEASES
778  |  CACNA1F  |  1.608  |  DISEASES
23066  |  CAND2  |  2.023  |  DISEASES
629  |  CFB  |  1.093  |  DISEASES
9635  |  CLCA2  |  1.973  |  DISEASES
22802  |  CLCA4  |  2.071  |  DISEASES
1382  |  CRABP2  |  1.74  |  DISEASES
23418  |  CRB1  |  1.499  |  DISEASES
2202  |  EFEMP1  |  1.746  |  DISEASES
6785  |  ELOVL4  |  1.943  |  DISEASES
346007  |  EYS  |  2.19  |  DISEASES
2189  |  FANCG  |  1.318  |  DISEASES
2875  |  GPT  |  3.473  |  DISEASES
84706  |  GPT2  |  2.122  |  DISEASES
283120  |  H19  |  2.83  |  DISEASES
3005  |  H1F0  |  1.156  |  DISEASES
3033  |  HADH  |  1.543  |  DISEASES
3617  |  IMPG1  |  4.268  |  DISEASES
83552  |  MFRP  |  2  |  DISEASES
27030  |  MLH3  |  2.033  |  DISEASES
4519  |  MT-CYB  |  1.059  |  DISEASES
4593  |  MUSK  |  1.017  |  DISEASES
4647  |  MYO7A  |  1.476  |  DISEASES
5015  |  OTX2  |  2.562  |  DISEASES
5339  |  PLEC  |  1.456  |  DISEASES
5515  |  PPP2CA  |  1.866  |  DISEASES
117177  |  RAB3IP  |  3.166  |  DISEASES
6103  |  RPGR  |  1.361  |  DISEASES
6171  |  RPL41  |  2.746  |  DISEASES
6247  |  RS1  |  1.776  |  DISEASES
6663  |  SOX10  |  1.054  |  DISEASES
6427  |  SRSF2  |  1.468  |  DISEASES
6430  |  SRSF5  |  2.601  |  DISEASES
6905  |  TBCE  |  2.779  |  DISEASES
4308  |  TRPM1  |  1.96  |  DISEASES
Locus
Symbol | Locus(Total Locus:1)
BEST1  |  11q12.3
Disease ID 568
Disease best vitelliform macular dystrophy
Integrated Phenotype
HPO | Name(Total Integrated Phenotypes:6)
HP:0012508  |  Metamorphopsia
HP:0000505  |  Visual impairment
HP:0001123  |  Visual field defect
HP:0000551  |  Abnormality of color vision
HP:0001139  |  Choroideremia
HP:0008028  |  Cystoid macular degeneration
Text Mined Phenotype
HPO | Name | Sentences' Count(Total Phenotypes:5)
HP:0011508  |  Macular hole  |  3
HP:0000572  |  Visual loss  |  2
HP:0200056  |  Macular scar  |  1
HP:0100699  |  Scarring  |  1
HP:0011510  |  Drusen  |  1
Disease ID 568
Disease best vitelliform macular dystrophy
Manually Symptom(Waiting for update.)
Text Mined Symptom(Waiting for update.)
Manually Genotype(Total Text Mining Genotypes:0)
(Waiting for update.)
Text Mining Genotype(Total Genotypes:0)
(Waiting for update.)
All Snps(Total Genotypes:40)
snpId pubmedId geneId geneSymbol diseaseId sourceId sentence score Year geneSymbol_dbSNP CHROMOSOME POS REF ALT
rs1129649236911202784GNB3umls:C0339510BeFreeThe 3-locus MDR model comprising FTO rs8050136C/A and GNB3 rs1129649T/C and rs5443C/T emerged as the best disease conferring model.0.0002714422013GNB3;P3H3126839304TC
rs11296492369112079068FTOumls:C0339510BeFreeThe 3-locus MDR model comprising FTO rs8050136C/A and GNB3 rs1129649T/C and rs5443C/T emerged as the best disease conferring model.0.0002714422013GNB3;P3H3126839304TC
rs121918283NA7439BEST1umls:C0339510CLINVARNA0.577100838NABEST11161959513ATC-
rs121918284181798817439BEST1umls:C0339510UNIPROTHowever, unlike two other alleles previously associated with Best disease, cotransfection with wild-type bestrophin-1 did not impair the formation of active wild-type bestrophin-1 channels, consistent with the recessive nature of the condition.0.5771008382008BEST11161955892GA
rs121918284NA7439BEST1umls:C0339510CLINVARNA0.577100838NABEST11161955892GA
rs121918285NA7439BEST1umls:C0339510CLINVARNA0.577100838NABEST11161951893CG,T
rs1800995104537317439BEST1umls:C0339510UNIPROTHowever, our results suggest that, in addition to Best disease, mutations within the bestrophin gene could be responsible for other forms of maculopathy with phenotypic characteristics similar to Best disease and for other diseases not included in the VMD category.0.5771008381999NANANANANA
rs1800995NA7439BEST1umls:C0339510CLINVARNA0.577100838NANANANANANA
rs1805142NA7439BEST1umls:C0339510CLINVARNA0.577100838NABEST11161955825GC
rs1805143104537317439BEST1umls:C0339510UNIPROTHowever, our results suggest that, in addition to Best disease, mutations within the bestrophin gene could be responsible for other forms of maculopathy with phenotypic characteristics similar to Best disease and for other diseases not included in the VMD category.0.5771008381999BEST11161959519CG,T
rs1805144103319517439BEST1umls:C0339510UNIPROTBest vitelliform macular dystrophy (VMD2) is an autosomal dominant dystrophy with a juvenile age of onset.0.5771008381999BEST11161959530GC
rs200277476114493207439BEST1umls:C0339510BeFreeBest's vitelliform macular dystrophy caused by a new mutation (Val89Ala) in the VMD2 gene.0.5771008382001BEST11161956946CT
rs200277476NA7439BEST1umls:C0339510UNIPROTNA0.577100838NABEST11161956946CT
rs267606677NA7439BEST1umls:C0339510CLINVARNA0.577100838NABEST11161957430AG
rs281865238NA7439BEST1umls:C0339510CLINVARNA0.577100838NABEST11161957402CA,T
rs281865528NA7439BEST1umls:C0339510CLINVARNA0.577100838NABEST11161962624CA-
rs28940273103319517439BEST1umls:C0339510UNIPROTBest vitelliform macular dystrophy (VMD2) is an autosomal dominant dystrophy with a juvenile age of onset.0.5771008381999BEST11161955749GC
rs28940273NA7439BEST1umls:C0339510CLINVARNA0.577100838NABEST11161955749GC
rs28940274NA7439BEST1umls:C0339510CLINVARNA0.577100838NABEST11161955723TC
rs28940274184009857439BEST1umls:C0339510UNIPROTBestrophin Cl- channels are highly permeable to HCO3-.0.5771008382008BEST11161955723TC
rs28940274171103747439BEST1umls:C0339510BeFreeFurthermore, we show that three out of 18 disease-associated alterations investigated (I73N, Y85H, F281del) reveal measurable effects on membrane insertion suggesting that defective membrane integration of bestrophin-1 may represent a potential disease mechanism for a small subset of Best macular dystrophy-related mutations.0.5771008382007BEST11161955723TC
rs28940275NA7439BEST1umls:C0339510CLINVARNA0.577100838NABEST11161951822AC
rs28940275193575577439BEST1umls:C0339510UNIPROTA broad phenotypic variability may be observed in BVMD, even with a single BEST1 mutation.0.5771008382009BEST11161951822AC
rs28940276NA7439BEST1umls:C0339510CLINVARNA0.577100838NABEST11161951831GA
rs28940276NA7439BEST1umls:C0339510UNIPROTNA0.577100838NABEST11161951831GA
rs28940278NA7439BEST1umls:C0339510CLINVARNA0.577100838NABEST11161951946GA
rs28940278NA7439BEST1umls:C0339510UNIPROTNA0.577100838NABEST11161951946GA
rs28940570107986427439BEST1umls:C0339510UNIPROTAllelic variation in the VMD2 gene in best disease and age-related macular degeneration.0.5771008382000BEST11161958159CT
rs28940570193575577439BEST1umls:C0339510UNIPROTA broad phenotypic variability may be observed in BVMD, even with a single BEST1 mutation.0.5771008382009BEST11161958159CT
rs28940570NA7439BEST1umls:C0339510CLINVARNA0.577100838NABEST11161958159CT
rs2894146896623957439BEST1umls:C0339510UNIPROTBest macular dystrophy (BMD), also known as vitelliform macular dystrophy (VMD2; OMIM 153700), is an autosomal dominant form of macular degeneration characterized by an abnormal accumulation of lipofuscin within and beneath the retinal pigment epithelium cells.0.5771008381998BEST11161959526GA
rs28941468NA7439BEST1umls:C0339510CLINVARNA0.577100838NABEST11161959526GA
rs28941469NA7439BEST1umls:C0339510CLINVARNA0.577100838NABEST11161957429TA
rs28941469193575577439BEST1umls:C0339510UNIPROTA broad phenotypic variability may be observed in BVMD, even with a single BEST1 mutation.0.5771008382009BEST11161957429TA
rs54432369112079068FTOumls:C0339510BeFreeThe 3-locus MDR model comprising FTO rs8050136C/A and GNB3 rs1129649T/C and rs5443C/T emerged as the best disease conferring model.0.0002714422013GNB3;CDCA3126845711CT
rs5443236911202784GNB3umls:C0339510BeFreeThe 3-locus MDR model comprising FTO rs8050136C/A and GNB3 rs1129649T/C and rs5443C/T emerged as the best disease conferring model.0.0002714422013GNB3;CDCA3126845711CT
rs672601356NA7439BEST1umls:C0339510CLINVARNA0.577100838NABEST11161955127-CA
rs74653691107986427439BEST1umls:C0339510UNIPROTAllelic variation in the VMD2 gene in best disease and age-related macular degeneration.0.5771008382000BEST11161956981CA
rs8050136236911202784GNB3umls:C0339510BeFreeThe 3-locus MDR model comprising FTO rs8050136C/A and GNB3 rs1129649T/C and rs5443C/T emerged as the best disease conferring model.0.0002714422013FTO1653782363CA
rs80501362369112079068FTOumls:C0339510BeFreeThe 3-locus MDR model comprising FTO rs8050136C/A and GNB3 rs1129649T/C and rs5443C/T emerged as the best disease conferring model.0.0002714422013FTO1653782363CA
GWASdb Annotation(Total Genotypes:0)
(Waiting for update.)
GWASdb Snp Trait(Total Genotypes:0)
(Waiting for update.)
Mapped by lexical matching(Total Items:3)
HP ID HP Name MP ID MP Name Annotation
HP:0008028Cystoid macular degenerationMP:0008584photoreceptor outer segment degenerationretrogressive pathologic change in the photoreceptor region that is rich in the visual pigment rhodopsin
HP:0001123Visual field defectMP:0010402ventricular septal defectabnormal communications between the two lower chambers of the heart, including such defects in the perimembranous, inlet, outlet (infundibular), central muscular, marginal muscular, or apical muscular regions
HP:0000551Abnormality of color visionMP:0011665d-loop transposition of the great arteriescomplete transposition of the great arteries; the d- refers to the dextroposition of the bulboventricular loop (ie, the position of the right ventricle, which is on the right side); in addition, the aorta also tends to be on the right and anterior, and th
Mapped by homologous gene(Total Items:6)
HP ID HP Name MP ID MP Name Annotation
HP:0008028Cystoid macular degenerationMP:0014059abnormal photoreceptor connecting cilium morphologyany structural anomaly of the nonmotile primary cilium that has a 9+0 microtubule array and forms the portion of the axoneme traversing the boundary between the retinal photoreceptor inner and outer segments
HP:0000551Abnormality of color visionMP:0014059abnormal photoreceptor connecting cilium morphologyany structural anomaly of the nonmotile primary cilium that has a 9+0 microtubule array and forms the portion of the axoneme traversing the boundary between the retinal photoreceptor inner and outer segments
HP:0001139ChoroideremiaMP:0013453enlarged lacrimal glandincreased size of any of the paired glands that secrete the aqueous layer of the tear film
HP:0012508MetamorphopsiaMP:0012671retinal spotsthe appearance of roundish lesions on the retina, frequently white, and may be due to inflammation, degeneration, vasculitis, exudates, edema or mineral deposits
HP:0000505Visual impairmentMP:3000003abnormal Ebner's gland morphologyany structural anomaly of the serous salivary glands which reside adjacent to the moats surrounding the circumvallate and foliate papillae just anterior to the posterior third of the tongue, anterior to the terminal sulcus; these exocrine glands secrete l
HP:0001123Visual field defectMP:0020039increased bone ossificationincrease in the formation of bone or of a bony substance, or the conversion of fibrous tissue or of cartilage into bone or a bony substance
Disease ID 568
Disease best vitelliform macular dystrophy
Case(Waiting for update.)