ABCA4 p.Val2050Leu
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PMID: 9666097
[PubMed]
Allikmets R et al: "Organization of the ABCR gene: analysis of promoter and splice junction sequences."
No.
Sentence
Comment
122
acceptors (G863A, 5585+1G/A, V2050L), and six in The mean of the distribution of individual information donors (4253+5G/T, 5196+1G/A, 5196+2T/C, contents (R i values, R sequence ) for splice acceptor and 5714+5G/A, 5898+1G/T, 6005+1G/T).
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ABCA4 p.Val2050Leu 9666097:122:29
status: NEW130 The V2050L muta-For the 50 splice acceptor and donor sites of the tion lowered the information content of the spliceABCR gene, the average R i values were 9.49±0.37 and acceptor site in exon 45 insignificantly, suggesting that7.45±0.32, respectively, in good correlation with those this variant did not affect splicing but represented apredicted.
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ABCA4 p.Val2050Leu 9666097:130:4
status: NEW135 The individual information R i acceptor at position 365 by two bits and created an Table 2 Analysis of ABCR splice site variants Exon Mutation Disease Number of patients wt R i mt R i Predicted effect on the ABCR protein 17A G863A STGD/AMD 11/1 11.6 9.7 Change of aa or deletion of one aaa 28D 4253+5G/T STGD 1 8.2 4.3 Partially functioning splice site 36D 5196+1G/A AMD 1 6.8 -6.0 Non-functional protein 36D 5196+2T/C STGD 1 6.8 -0.7 Non-functional protein 40A 55851G/A STGD 1 5.9 -1.6 Non-functional protein 40D 5714+5G/A STGD 8 7.2 3.7 Partially functioning splice site 42D 5898+1G/T STGD 3 8.6 0.8 Non-functional protein 43D 6005+1G/T STGD 1 11.2 3.4 Partially functioning splice site 45A V2050L STGD 2 12.5 10.6 Change of aa, no effect on splicing 'A` or 'D` after the exon number indicates splice acceptor or donor sequences, respectively.
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ABCA4 p.Val2050Leu 9666097:135:4
status: NEWX
ABCA4 p.Val2050Leu 9666097:135:695
status: NEW126 acceptors (G863A, 5585+1G/A, V2050L), and six in The mean of the distribution of individual information donors (4253+5G/T, 5196+1G/A, 5196+2T/C, contents (R i values, R sequence ) for splice acceptor and 5714+5G/A, 5898+1G/T, 6005+1G/T).
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ABCA4 p.Val2050Leu 9666097:126:29
status: NEW141 The individual information R i acceptor at position 365 by two bits and created an Table 2 Analysis of ABCR splice site variants Exon Mutation Disease Number of patients wt R i mt R i Predicted effect on the ABCR protein 17A G863A STGD/AMD 11/1 11.6 9.7 Change of aa or deletion of one aaa 28D 4253+5G/T STGD 1 8.2 4.3 Partially functioning splice site 36D 5196+1G/A AMD 1 6.8 -6.0 Non-functional protein 36D 5196+2T/C STGD 1 6.8 -0.7 Non-functional protein 40A 55851G/A STGD 1 5.9 -1.6 Non-functional protein 40D 5714+5G/A STGD 8 7.2 3.7 Partially functioning splice site 42D 5898+1G/T STGD 3 8.6 0.8 Non-functional protein 43D 6005+1G/T STGD 1 11.2 3.4 Partially functioning splice site 45A V2050L STGD 2 12.5 10.6 Change of aa, no effect on splicing 'A` or 'D` after the exon number indicates splice acceptor or donor sequences, respectively.
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ABCA4 p.Val2050Leu 9666097:141:695
status: NEW
PMID: 22427542
[PubMed]
Fritsche LG et al: "A subgroup of age-related macular degeneration is associated with mono-allelic sequence variants in the ABCA4 gene."
No.
Sentence
Comment
93
These patients were heterozygous for variants c.634C>T (p.R212C), c.4556C>G (p.T1519R), and c.6148G>C (p.V2050L), respectively.
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ABCA4 p.Val2050Leu 22427542:93:105
status: NEW91 These patients were heterozygous for variants c.634C>T (p.R212C), c.4556C>G (p.T1519R), and c.6148G>C (p.V2050L), respectively.
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ABCA4 p.Val2050Leu 22427542:91:105
status: NEW
PMID: 20335603
[PubMed]
Poloschek CM et al: "ABCA4 and ROM1: implications for modification of the PRPH2-associated macular dystrophy phenotype."
No.
Sentence
Comment
9
Patients with heterozygous sequence alterations only in ROM1 (p.R229H) or ABCA4 (p.V2050L) showed a mild ocular phenotype and were otherwise asymptomatic.
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ABCA4 p.Val2050Leu 20335603:9:83
status: NEW73 It is predicted to lead to an amino acid substitution (valine to leucine at position 2050, p.V2050L).
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ABCA4 p.Val2050Leu 20335603:73:55
status: NEWX
ABCA4 p.Val2050Leu 20335603:73:93
status: NEW103 Group 3: Mutations in PRPH2, ROM1, and ABCA4 (p.R172W, p.R229H, and p.V2050L).
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ABCA4 p.Val2050Leu 20335603:103:70
status: NEW124 Group 5: Mutation of ABCA4 (p.V2050L).
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ABCA4 p.Val2050Leu 20335603:124:30
status: NEW141 TABLE1.DetailedPhenotypicDataofAllExaminedFamilyMembersSortedbyGroups Patient Group Genotype Age AtEx. VA OD/OS Age(y)at Onsetof SymptomsVisualField ColorVision (PanelD15)FundusFAF ERG Scotopic 1.8B-Wave Amplitude ERG30-Hz Flicker AmplitudemfERG EOG Arden Ratio V-21 p.R172W 221.25/1.25AsymptomaticOP:ODnasalsup smallscotoma, OSnormal;GP: ODnormal ODdesaturated:2 unspecific defects OU:ONdrusen, perifoveolar drusenODϾOS OU:ONdrusen, peri-foveolar punctual increase ODϾOS P1NNODN OSdesaturated:1 unspecific defect OSNA IV-71 p.R172W 450.2/0.140;VAloss35; photophobia GP:OUcentral scotoma40° (I/2) OD:mildprotan, deutanand tritandefects, OS:unspecific defects OU:macularRPE granularity,OS: 0.5ODD temporalMA OU:speckled beyondarcades; OS:reducedat lowerarcade indicating atrophy,1ODD NNZ5ND* III-41 p.R172W 750.05/0.0742;VAloss photophobia (onset unknown) GP:OUcentral scotoma30° (I/3) OU:marked protanand deutandefects OU:severeMA, 4ODD OU:reduced CTA,4ODD, surrounding speckles NP2AP1 V-12 p.R172W, p.R229H 260.9/0.922;flickering lightsensation OP:ODnormal OSparacentral defects10° fromcenter OU:normalOU:mildmacular RPEclumping OU:speckled, 2ODD, surrounding increase,OD: reticular increase P1P1Z3N 21AsymptomaticNReNReNReNDNDNDZ1ND IV-12 p.R172W, p.R229H 560.8/0.7501adaptation difficulties GP:OUparacentral scotoma:1-10° radius(I/2,I/3 inf,I/4sup) OU:mild unspecific defectsOS:1 tritandefect OU:mildRPE atrophy OU:speckled, 3ODD NP1Z4P1 32;photophobiaOP:asinGPOD:moderate temporaloptic nerveatrophy 30;flickering lightsensation, relative paracentral scotoma 471.0/1.032;photophobiaGP:OUstableNDOU:mildRPE irregularity NDNDNDZ3ND 430.9/0.930;flickering lightsensation, relative paracentral scotoma GP:OU paracentral scotoma:3-10° radius(I/2inf, I/4sup) OU:moderate tetartandefects OU:minorRPE irregularity NDP2NNDP1 (continues) TABLE1(continued).DetailedPhenotypicDataofAllExaminedFamilyMembersSortedbyGroups Patient Group Genotype Age AtEx. VA OD/OS Age(y)at Onsetof SymptomsVisualField ColorVision (PanelD15)FundusFAF ERG Scotopic 1.8B-Wave Amplitude ERG30-Hz Flicker AmplitudemfERG EOG Arden Ratio III-22 p.R172W, p.R229H 840.05/0.0256;photophobia 30;VAloss GPstableOU:notpossibleOU:severeMAOU:NRdueto dense cataracts P2P2Z4P2 710.02/0.03GP:OUsupVF loss,OSinf,VF constriction to70° OU:notpossibleOU:severeMANDNDNDNDND V-43 p.R172W, p.V2050L, p.R229H 221.0/1.222;photophobia inbrightlight 22;mild nyctalopia GP:OUsupmild constriction (I/3,I/2,I/1), OSparacentral scotoma5° (I/1),OP: reduction central20° OU:normalOU:mild- moderateMA OU:speckled,3 ODD, encircling increase P1NZ3N IV-43 p.R172W, p.V2050L, p.R229H 500.2/0.349;nyctalopia 40;photophobia 35;VFdefects 13;mildVAloss GP:OD paracentral scotoma(III/4) 10°,sensitivity lossforI/1,I/2, OScentral scotoma40° (I/3)extending temporally OU:marked protanand deutandefects OU:moderateMA extendingbeyond arcades; temporallyϾ1 ODDsevereMA; midperipheral RPEclumping; moderate temporalON atrophy OU:speckled beyond arcades, reducedCTA (mild progression) P3P2Z5P1 480.2/0.540;photophobia 35;VFdefects 13;mildVAloss GP:ODcentral scotoma35° (I/3)extending temporally,OS centralscotoma 40°(I/3) OD:marked protanand deutandefects OS:marked protan,deutan, andtritan defects OU:mild pericentralMAto arcades;mid- peripheralRPE clumping;nasally 1ODDRPE atrophy; moderate temporalON atrophy OU:speckled beyond arcades, reducedCTA P2P2Z5ND IV-94 p.R229H 361.25/1.25AsymptomaticOPandGP: normal OS:unsaturated:2 unspecific defects OU:normalOU:normalNNZ1N (continues) nantly affected with stable rod function.
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ABCA4 p.Val2050Leu 20335603:141:2383
status: NEWX
ABCA4 p.Val2050Leu 20335603:141:2654
status: NEW155 The ABCA4 p.V2050L heterozygous carrier reported herein (group 5, V-3) showed centrally reduced mfERG amplitudes and additional minor fundus abnormalities.
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ABCA4 p.Val2050Leu 20335603:155:12
status: NEWX
ABCA4 p.Val2050Leu 20335603:155:33
status: NEW156 This finding suggests that the p.V2050L mutation in the heterozygous state is capable of mildly reducing macular function without an additional mutation on the second allele.
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ABCA4 p.Val2050Leu 20335603:156:33
status: NEWX
ABCA4 p.Val2050Leu 20335603:156:246
status: NEW157 Indeed, heterozygous mutations in ABCA4 have been reported to cause electrophysiologically detectable dysfunction in individuals who had no obvious clinical signs: Maia-Lopes et al.40 described and clinically characterized a heterozygous ABCA4 p.V2050L carrier within a family with Stargardt disease.
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ABCA4 p.Val2050Leu 20335603:157:246
status: NEW160 In contrast, normal flicker amplitudes and stable rod function as shown in a follow-up examination 13 years after the initial presentation was found in her brother (group 2, IV-1) not carrying ABCA4 p.V2050L.
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ABCA4 p.Val2050Leu 20335603:160:51
status: NEWX
ABCA4 p.Val2050Leu 20335603:160:201
status: NEW161 This finding may hint at an additional effect of p.V2050L on generalized cone function and an acceleration of loss of rod function if the genotype also contains ROM1 p.R229H and PRPH2 TABLE1(continued).DetailedPhenotypicDataofAllExaminedFamilyMembersSortedbyGroups Patient Group Genotype AgeAt Ex. VA OD/OS Age(y)at Onsetof SymptomsVisualField ColorVision (PanelD15)FundusFAF ERG Scotopic 1.8B-Wave Amplitude ERG30-Hz Flicker AmplitudemfERG EOG Arden Ratio III-64 p.R229H 681.0/1.0AsymptomaticOPandGP: normal OS:unsaturated:1 unspecific defect OU:mildarteriolar narrowing; arteriovenous nipping OU:normalNNZ2N V-35 p.V2050L 241.25/1.25AsymptomaticOPandGP: Normal ODdesaturated:1 unspecific defect OU:minimal perifoveolarRPE irregularity OU:subtle perifoveolar increase NNZ2N A,globalamplitudereduction;arcades,temporalvasculararcades;CTA,correspondingtoatrophy;EOG,electrooculogram;ERG,full-fieldelectroretinogram;ex.,examination;FAF,fundus autofluorescence;GP,Goldmannperimetry;inf,inferior;MA,macularatrophy;mfERG,multifocalelectroretinogram;NA,notanalyzableduetoartifact;N,normal;ND,notdone;ND*,notdonebecause patientrefusedtheexamination;NL,normallimit;NR,notrecordable;NR,norecords;ON,opticnerve;OP,Octopusperimetry;P1-3,amplitude(ERG)orArdenratio(EOG,normalrange1.7-3.3) belowthelowernormallimit(increasingreduction);ODD,opticdiscdiameter;sup,superior;VA,visualacuity;VF,visualfield;Z1-5,pleaseseeMethodsforanexplanation.Alldegreesindicate diameterunlessotherwiseindicated.
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ABCA4 p.Val2050Leu 20335603:161:51
status: NEWX
ABCA4 p.Val2050Leu 20335603:161:456
status: NEWX
ABCA4 p.Val2050Leu 20335603:161:617
status: NEW163 In support of this idea, it has been reported previously that ABCA4 p.V2050L can be associated with a rod-cone pattern of functional loss as described in one patient with RP who bears a heterozygous p.V2050L mutation.
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ABCA4 p.Val2050Leu 20335603:163:70
status: NEWX
ABCA4 p.Val2050Leu 20335603:163:201
status: NEW70 It is predicted to lead to an amino acid substitution (valine to leucine at position 2050, p.V2050L).
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ABCA4 p.Val2050Leu 20335603:70:55
status: NEWX
ABCA4 p.Val2050Leu 20335603:70:93
status: NEW100 Group 3: Mutations in PRPH2, ROM1, and ABCA4 (p.R172W, p.R229H, and p.V2050L).
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ABCA4 p.Val2050Leu 20335603:100:70
status: NEW121 Group 5: Mutation of ABCA4 (p.V2050L).
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ABCA4 p.Val2050Leu 20335603:121:30
status: NEW140 Detailed Phenotypic Data of All Examined Family Members Sorted by Groups Patient Group Genotype Age At Ex. VA OD/OS Age (y) at Onset of Symptoms Visual Field Color Vision (Panel D 15) Fundus FAF ERG Scotopic 1.8 B-Wave Amplitude ERG 30-Hz Flicker Amplitude mfERG EOG Arden Ratio III-2 2 p.R172W, p.R229H 84 0.05/0.02 56; photophobia 30; VA loss GP stable OU: not possible OU: severe MA OU: NR due to dense cataracts P 2 P 2 Z 4 P 2 71 0.02/0.03 GP: OU sup VF loss, OS inf, VF constriction to 70&#b0; OU: not possible OU: severe MA ND ND ND ND ND V-4 3 p.R172W, p.V2050L, p.R229H 22 1.0/1.2 22; photophobia in bright light 22; mild nyctalopia GP: OU sup mild constriction (I/3, I/2, I/1), OS paracentral scotoma 5&#b0; (I/1), OP: reduction central 20&#b0; OU: normal OU: mild-moderate MA OU: speckled, 3 ODD, encircling increase P 1 N Z 3 N IV-4 3 p.R172W, p.V2050L, p.R229H 50 0.2/0.3 49; nyctalopia 40; photophobia 35; VF defects 13; mild VA loss GP: OD paracentral scotoma (III/4) 10&#b0;, sensitivity loss for I/1, I/2, OS central scotoma 40&#b0; (I/3) extending temporally OU: marked protan and deutan defects OU: moderate MA extending beyond arcades; temporally b0e;1 ODD severe MA; midperipheral RPE clumping; moderate temporal ON atrophy OU: speckled beyond arcades, reduced CTA (mild progression) P 3 P 2 Z 5 P 1 48 0.2/0.5 40; photophobia 35; VF defects 13; mild VA loss GP: OD central scotoma 35&#b0; (I/3) extending temporally, OS central scotoma 40&#b0; (I/3) OD: marked protan and deutan defects OS: marked protan, deutan, and tritan defects OU: mild pericentral MA to arcades; mid-peripheral RPE clumping; nasally 1 ODD RPE atrophy; moderate temporal ON atrophy OU: speckled beyond arcades, reduced CTA P 2 P 2 Z 5 ND IV-9 4 p.R229H 36 1.25/1.25 Asymptomatic OP and GP: normal OS: unsaturated: 2 unspecific defects OU: normal OU: normal N N Z 1 N (continues) nantly affected with stable rod function.
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ABCA4 p.Val2050Leu 20335603:140:563
status: NEWX
ABCA4 p.Val2050Leu 20335603:140:858
status: NEW154 The ABCA4 p.V2050L heterozygous carrier reported herein (group 5, V-3) showed centrally reduced mfERG amplitudes and additional minor fundus abnormalities.
X
ABCA4 p.Val2050Leu 20335603:154:12
status: NEW159 In contrast, normal flicker amplitudes and stable rod function as shown in a follow-up examination 13 years after the initial presentation was found in her brother (group 2, IV-1) not carrying ABCA4 p.V2050L.
X
ABCA4 p.Val2050Leu 20335603:159:201
status: NEW164 In support of this idea, it has been reported previously that ABCA4 p.V2050L can be associated with a rod-cone pattern of functional loss as described in one patient with RP who bears a heterozygous p.V2050L mutation.
X
ABCA4 p.Val2050Leu 20335603:164:70
status: NEWX
ABCA4 p.Val2050Leu 20335603:164:201
status: NEW
PMID: 18977788
[PubMed]
Riveiro-Alvarez R et al: "Frequency of ABCA4 mutations in 278 Spanish controls: an insight into the prevalence of autosomal recessive Stargardt disease."
No.
Sentence
Comment
96
These Table 1 ABCA4 sequence variants identified in Spanish control population Mutant alleles Nucleotide change Amino acid change Number of cases Number of alleles Frequency (%) Homozygous individuals Mutations* c.661G.A p.Gly221Arg 1 1 0.64 None c.1140T.A p.Asn380Lys 1 1 0.64 None c.2588G.C p.Gly863Ala 1 1 0.64 None c.3113C.T p.Ala1038Val 1 1 0.64 None c.3899G.A p.Arg1300Gln 1 1 0.64 None c.5882G.A p.Gly1961Glu 1 1 0.64 None c.5908C.T p.Leu1970Phe 1 1 0.64 None c.6148G.C p.Val2050Leu 1 1 0.64 None c.6529G.A p.Asp2177Asn 2 2 1.28 None Total 10 Polymorphisms{ c.466A.G p.Ile156Val 5 5 3.2 None c.635G.A p.Arg212His 5 6 3.84 1 c.1268A.G p.His423Arg 43 48 30.7 5 c.1269C.T p.His423His 2 2 1.28 None IVS10+5delG 34 36 23 2 c.2828G.A p.Arg943Gln 1 1 0.64 None c.4203C.A p.Pro1401Pro 3 3 1.9 None IVS33+48C.T 59 75 48 16 c.5603A.T p.Asn1868Ile 4 4 2.5 None c.5682G.C p.Leu1894Leu 29 35 22.4 6 c.5814A.G p.Leu1938Leu 27 33 21.1 6 c.5843 C.T p.Pro1948Leu 9 10 6.4 1 c.5844A.G p.Pro1948Pro 27 32 20.5 5 c.6069C.T p.Ile2023Ile 11 12 7.7 1 c.6249C.T p.Ile2083Ile 12 14 8.9 2 c.6285T.C p.Asp2095Asp 24 26 16.6 2 c.6764G.T p.Ser2255Ile 12 13 8.3 1 *A total of 15 mutant alleles were detected.
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ABCA4 p.Val2050Leu 18977788:96:479
status: NEW97 These Table 1 ABCA4 sequence variants identified in Spanish control population Mutant alleles Nucleotide change Amino acid change Number of cases Number of alleles Frequency (%) Homozygous individuals Mutations* c.661G.A p.Gly221Arg 1 1 0.64 None c.1140T.A p.Asn380Lys 1 1 0.64 None c.2588G.C p.Gly863Ala 1 1 0.64 None c.3113C.T p.Ala1038Val 1 1 0.64 None c.3899G.A p.Arg1300Gln 1 1 0.64 None c.5882G.A p.Gly1961Glu 1 1 0.64 None c.5908C.T p.Leu1970Phe 1 1 0.64 None c.6148G.C p.Val2050Leu 1 1 0.64 None c.6529G.A p.Asp2177Asn 2 2 1.28 None Total 10 Polymorphisms{ c.466A.G p.Ile156Val 5 5 3.2 None c.635G.A p.Arg212His 5 6 3.84 1 c.1268A.G p.His423Arg 43 48 30.7 5 c.1269C.T p.His423His 2 2 1.28 None IVS10+5delG 34 36 23 2 c.2828G.A p.Arg943Gln 1 1 0.64 None c.4203C.A p.Pro1401Pro 3 3 1.9 None IVS33+48C.T 59 75 48 16 c.5603A.T p.Asn1868Ile 4 4 2.5 None c.5682G.C p.Leu1894Leu 29 35 22.4 6 c.5814A.G p.Leu1938Leu 27 33 21.1 6 c.5843 C.T p.Pro1948Leu 9 10 6.4 1 c.5844A.G p.Pro1948Pro 27 32 20.5 5 c.6069C.T p.Ile2023Ile 11 12 7.7 1 c.6249C.T p.Ile2083Ile 12 14 8.9 2 c.6285T.C p.Asp2095Asp 24 26 16.6 2 c.6764G.T p.Ser2255Ile 12 13 8.3 1 *A total of 15 mutant alleles were detected.
X
ABCA4 p.Val2050Leu 18977788:97:479
status: NEW
PMID: 18285826
[PubMed]
Kitiratschky VB et al: "ABCA4 gene analysis in patients with autosomal recessive cone and cone rod dystrophies."
No.
Sentence
Comment
70
of alleles Reference Missense: 6 c.731T4Ca p.L244P 2 23 12 c.1622T4Cb p.L541P 1 5 13 c.1928T4G p.V643G 1 9 17 c.2588G4C p.G863A and p.G863del 2 4 21 c.3113C4Tb p.A1038V 1 4 25 c.3608G4A p.G1203E 1 24 28 c.4139C4T p.P1380L 2 25 30 c.4457C4T p.P1486L 1 25 30 c.4462T4C p.C1488R 1 25 37 c.5285C4A p.A1762D 1 24 41 c.5819T4C p.L1940P 1 26 42 c.5882G4A p.G1961E 1 9 45 c.6148G4C p.V2050L 1 25 45 c.6229C4T p.R2077W 1 25 Nonsense: 6 c.700C4T p.Q234X 1 This study 6 c.735T4G p.Y245X 2 24 28 c.4234C4T p.Q1412X 1 10 Deletion: 24 c.3539_3554del p.S1181PfsX8 1 This study 43 c.5917delG p.V1973X 3 27 Splice site/intronic: 26 c.5196+1G4A Splicing 1 9 34 c.4848+2T4C Splicing 1 This study 36 c.5196+1_5196+4del Splicing 1 15 39 c.5461À10T4C Unknown 8 14 40 c.5714+5G4A Splicing?
X
ABCA4 p.Val2050Leu 18285826:70:376
status: NEW
PMID: 18326749
[PubMed]
Maia-Lopes S et al: "Evidence of widespread retinal dysfunction in patients with stargardt disease and morphologically unaffected carrier relatives."
No.
Sentence
Comment
150
Several other sequence changes that have been significantly correlated to the STGD phenotype (M1V, N96D, R290W, L2027F, R2030Q, V2050L, 3211insGT, and IVS40ϩ5GϾA) were also identified.
X
ABCA4 p.Val2050Leu 18326749:150:128
status: NEW134 Several other sequence changes that have been significantly correlated to the STGD phenotype (M1V, N96D, R290W, L2027F, R2030Q, V2050L, 3211insGT, and IVS40af9;5Gb0e;A) were also identified.
X
ABCA4 p.Val2050Leu 18326749:134:128
status: NEW
PMID: 16303926
[PubMed]
Hargitai J et al: "Correlation of clinical and genetic findings in Hungarian patients with Stargardt disease."
No.
Sentence
Comment
89
Summarized Clinical and Genetic Data of Patients with STGD Patient Allele 1 Allele 2 Fishman OU Gender Age Duration VA OD VA OS FT OD (m) FT OS (m) MV OD (mm3 ) MV OS (mm3 ) 1 ND ND I M 18 10 0.42 0.50 90.00 76.00 1.70 1.67 2 L541P/A1038V ND III F 27 15 0.06 0.08 43.00 58.00 1.27 1.28 3 5917delG 5917delG II F 29 8 0.17 0.17 54.00 20.00 1.38 1.35 4 ND ND III F 42 14 0.10 0.10 91.00 71.00 1.60 1.59 5 V2050L ND II F 22 5 0.20 0.33 28.00 77.00 1.64 1.68 6 ND ND II F 17 2 1.00 0.71 156.00 141.00 2.55 2.6 7 IVS40ϩ5GϾA ND III M 28 13 0.10 0.06 71.00 92.00 1.61 1.61 8 L541P/A1038V G1961E II M 37 15 0.10 0.10 87.00 97.00 1.95 1.95 9 106delT G1961E II M 32 7 0.08 0.08 51.00 32.00 1.59 1.66 10 ND ND I F 55 17 0.25 0.56 160.00 170.00 1.72 1.82 11 L541P/A1038V G863A II F 15 3 0.25 0.33 67.00 68.00 1.78 1.76 12 IVS40ϩ5GϾA 5917delG III M 15 6 0.20 0.20 107.00 117.00 1.93 1.92 13 ND ND I M 27 2 0.38 0.33 56.00 86.00 2.01 1.97 14 G1886E G1961E II F 37 9 0.12 0.16 92.00 46.00 1.55 1.59 15 G1961E ND III F 20 5 0.30 0.20 49.00 34.00 1.43 1.53 16 ND ND II M 28 14 0.32 0.08 52.00 60.00 1.46 1.52 17 IVS40ϩ5GϾA 5917delG III M 27 5 0.10 0.10 97.00 92.00 1.76 1.71 18 L541P/A1038V D1532N III M 28 12 0.25 0.10 49.00 46.00 1.83 1.86 19 ND ND II F 31 11 0.10 0.13 67.00 72.00 1.55 1.49 20 L541P L541P/A1038V II F 15 5 0.10 0.10 28.00 34.00 1.63 1.65 21 L541P/A1038V G863A II F 25 2 0.20 0.62 94.00 81.00 1.92 1.94 22 L541P/A1038V ND II M 18 9 0.08 0.10 63.00 72.00 1.40 1.43 23 G1961E ND III F 34 9 0.16 0.16 16.00 23.00 1.31 1.56 24 ND ND II F 52 14 0.16 0.16 122.00 113.00 1.90 1.99 25 P68L L541P/A1038V III M 37 22 0.10 0.12 40.00 40.00 1.41 1.42 26 ND ND II F 18 11 0.20 0.25 59.00 72.00 1.42 1.47 27 L541P/A1038V G1961E II F 24 7 0.18 0.18 83.00 100.00 1.72 1.77 28 IVS40ϩ5GϾA 5917delG III M 15 7 0.10 0.16 38.00 46.00 1.30 1.41 29 R1108C R1108C II M 31 14 0.10 0.10 41.00 44.00 1.95 1.96 30 G1961E ND II M 28 6 0.33 0.56 91.00 129.00 1.98 2.04 31 ND ND II F 28 11 0.08 0.10 55.00 63.00 1.52 1.59 32 L541P/A1038V G863A II M 32 15 0.20 0.20 92.00 86.00 1.80 1.75 33 ND ND II F 27 4 0.25 0.20 66.00 75.00 1.72 1.76 34 ND ND II F 36 8 0.12 0.10 58.00 69.00 1.59 1.56 35 IVS40ϩ5GϾA IVS40ϩ5GϾA III F 19 6 0.10 0.10 62.00 53.00 1.67 1.65 Fishman OU, classification of patients by fundus photos in three categories according to Fishman et al.25 ND, not determined.
X
ABCA4 p.Val2050Leu 16303926:89:418
status: NEW87 Summarized Clinical and Genetic Data of Patients with STGD Patient Allele 1 Allele 2 Fishman OU Gender Age Duration VA OD VA OS FT OD (òe;m) FT OS (òe;m) MV OD (mm3 ) MV OS (mm3 ) 1 ND ND I M 18 10 0.42 0.50 90.00 76.00 1.70 1.67 2 L541P/A1038V ND III F 27 15 0.06 0.08 43.00 58.00 1.27 1.28 3 5917delG 5917delG II F 29 8 0.17 0.17 54.00 20.00 1.38 1.35 4 ND ND III F 42 14 0.10 0.10 91.00 71.00 1.60 1.59 5 V2050L ND II F 22 5 0.20 0.33 28.00 77.00 1.64 1.68 6 ND ND II F 17 2 1.00 0.71 156.00 141.00 2.55 2.6 7 IVS40af9;5Gb0e;A ND III M 28 13 0.10 0.06 71.00 92.00 1.61 1.61 8 L541P/A1038V G1961E II M 37 15 0.10 0.10 87.00 97.00 1.95 1.95 9 106delT G1961E II M 32 7 0.08 0.08 51.00 32.00 1.59 1.66 10 ND ND I F 55 17 0.25 0.56 160.00 170.00 1.72 1.82 11 L541P/A1038V G863A II F 15 3 0.25 0.33 67.00 68.00 1.78 1.76 12 IVS40af9;5Gb0e;A 5917delG III M 15 6 0.20 0.20 107.00 117.00 1.93 1.92 13 ND ND I M 27 2 0.38 0.33 56.00 86.00 2.01 1.97 14 G1886E G1961E II F 37 9 0.12 0.16 92.00 46.00 1.55 1.59 15 G1961E ND III F 20 5 0.30 0.20 49.00 34.00 1.43 1.53 16 ND ND II M 28 14 0.32 0.08 52.00 60.00 1.46 1.52 17 IVS40af9;5Gb0e;A 5917delG III M 27 5 0.10 0.10 97.00 92.00 1.76 1.71 18 L541P/A1038V D1532N III M 28 12 0.25 0.10 49.00 46.00 1.83 1.86 19 ND ND II F 31 11 0.10 0.13 67.00 72.00 1.55 1.49 20 L541P L541P/A1038V II F 15 5 0.10 0.10 28.00 34.00 1.63 1.65 21 L541P/A1038V G863A II F 25 2 0.20 0.62 94.00 81.00 1.92 1.94 22 L541P/A1038V ND II M 18 9 0.08 0.10 63.00 72.00 1.40 1.43 23 G1961E ND III F 34 9 0.16 0.16 16.00 23.00 1.31 1.56 24 ND ND II F 52 14 0.16 0.16 122.00 113.00 1.90 1.99 25 P68L L541P/A1038V III M 37 22 0.10 0.12 40.00 40.00 1.41 1.42 26 ND ND II F 18 11 0.20 0.25 59.00 72.00 1.42 1.47 27 L541P/A1038V G1961E II F 24 7 0.18 0.18 83.00 100.00 1.72 1.77 28 IVS40af9;5Gb0e;A 5917delG III M 15 7 0.10 0.16 38.00 46.00 1.30 1.41 29 R1108C R1108C II M 31 14 0.10 0.10 41.00 44.00 1.95 1.96 30 G1961E ND II M 28 6 0.33 0.56 91.00 129.00 1.98 2.04 31 ND ND II F 28 11 0.08 0.10 55.00 63.00 1.52 1.59 32 L541P/A1038V G863A II M 32 15 0.20 0.20 92.00 86.00 1.80 1.75 33 ND ND II F 27 4 0.25 0.20 66.00 75.00 1.72 1.76 34 ND ND II F 36 8 0.12 0.10 58.00 69.00 1.59 1.56 35 IVS40af9;5Gb0e;A IVS40af9;5Gb0e;A III F 19 6 0.10 0.10 62.00 53.00 1.67 1.65 Fishman OU, classification of patients by fundus photos in three categories according to Fishman et al.25 ND, not determined.
X
ABCA4 p.Val2050Leu 16303926:87:416
status: NEW
PMID: 16103129
[PubMed]
Wiszniewski W et al: "ABCA4 mutations causing mislocalization are found frequently in patients with severe retinal dystrophies."
No.
Sentence
Comment
39
arRP patients from five families (AR168, AR192, AR194, AR554 and AR591) were heterozygous for various missense ABCA4 mutations that by conceptual translation would lead to either an amino acid change (G1961E, V2050L and D2177 N) or splicing alteration (36IVSþ1G .
X
ABCA4 p.Val2050Leu 16103129:39:209
status: NEW44 A WT 168-05 24 20/25 OD; 20/30 OS;VF , 308 OU RP N/A N/A 168-06 26 N/A RP N/A N/A AR192 192-03 9 20/20 OD; 20/25 OS;VF , 58 OU RP D2177N WT 192-04 19 20/30 OD; 20/40 OS;VF , 58 OU RP WT WT 192-05 19 20/30 OD; 20/40 OS;VF , 58 OU RP WT WT AR194 194-03 30 N/A RP D2177N WT 194-05 Childhood 20/25 OD; 20/40 OS RP N/A N/A 194-06 5 N/A RP D2177N WT 194-07 4 or 5 20/80 OU RP N/A N/A AR197 197-05 7 CF 3 feet OD; CF 2 feet OS RP [L541P; A1038V] [L541P; A1038V] 197-06 9 CF 5 feet OD; HM OS RP [L541P; A1038V] [L541P; A1038V] AR554 554-03 2 10/12 20/60 OU RP V2050L WT 554-04 1 9/12 N/A RP N/A N/A AR591 591-03 20 20/25 OU RP N/A N/A 591-04 8 20/20 OD; 20/25 OS;VF , 108 OU RP G1961E WT AR689 689-03 7 N/A RP R408X R602W 689-08 7 N/A RP N/A N/A OD, right eye; OS, left eye; OU, both eyes; VF, visual field; RP, retinitis pigementosa, WT, wild type; N/A, not available; CF, counting fingers; HM, hand motions.
X
ABCA4 p.Val2050Leu 16103129:44:552
status: NEW131 In subjects from five RP families (9% of disease alleles), we found heterozygous missense ABCA4 mutations (G1961E, V2050L, D2177 N and 36IVSþ1) that are suggested to have functional consequences for ABCA4 activity (29,36).
X
ABCA4 p.Val2050Leu 16103129:131:115
status: NEW
PMID: 15614538
[PubMed]
Lorenz B et al: "Age matters--thoughts on a grading system for ABCA4 mutations."
No.
Sentence
Comment
33
All carry mutations which have been reported mostly in AMD (D2177N, V2050L [1, 16, 18]) or STGD (L541P+A1038V [3]).
X
ABCA4 p.Val2050Leu 15614538:33:68
status: NEW34 All carry mutations which have been reported mostly in AMD (D2177N, V2050L [1, 16, 18]) or STGD (L541P+A1038V [3]).
X
ABCA4 p.Val2050Leu 15614538:34:68
status: NEW
PMID: 15494742
[PubMed]
Klevering BJ et al: "Microarray-based mutation analysis of the ABCA4 (ABCR) gene in autosomal recessive cone-rod dystrophy and retinitis pigmentosa."
No.
Sentence
Comment
101
Likewise, the known Table 2 ABCA4 sequence variants in RP patients RP patient number Inheritance Allele 1 Allele 2 Nucleotide change Effect Nucleotide change Effect 9304 Aut. Rec. 2588G4C; 2828G4Aa DG863/G863A; R943Q 5888delG R1963fs 9444 Aut. Rec. 6529G4A D2177N Not identified 9545 Isolated 6529G4A D2177N Not identified 14753 Isolated 1622T4C; 3113C4T L541P; A1038V Not identified 17597 Isolated 6148G4C V2050L Not identified a Polymorphic variants 4203A, 5603 T, and 5682C also present.
X
ABCA4 p.Val2050Leu 15494742:101:407
status: NEW114 For two conservative missense mutations (V1433I and V2050L), the pathologic nature can be questioned.
X
ABCA4 p.Val2050Leu 15494742:114:52
status: NEW143 Given this clinical presentation and the fact that homozygous null mutations were not found Table 5 Functional assessment of missense (A) and splice site (B) mutations (A) Missense mutation Nature of amino-acid change Effect on ABCR functionRef R18W Nonconservative Unknown R24C Nonconservative Unknown; adjacent to first transmembrane domain G65E Nonconservative Unknown E161K Nonconservative Unknown L541P Conservative Decreased ATP binding and ATPase activity50 P597S Nonconservative Unknown G618E Nonconservative Unknown V767D Nonconservative Decreased ABCR expression10 G863A Nonconservative Decreased ATPase activity50, 51 R943Q Nonconservative Decreased ATPase activity51 A1038V Conservative Decreased ATP binding and ATPase activity50 E1087K Nonconservative Decreased ATP binding50 V1433I Conservative Unknown R1640W Nonconservative Unknown A1794D Nonconservative Introduction charged aa in 10th transmembrane domain G1961E Nonconservative Decreased ATP binding and ATPase activity 50 V2050L Conservative Unknown D2177N Nonconservative Increased ATPase activity50 (B) Splice site mutation Effect on mRNARef Predicted effect on ABCR protein 768G4T Nonsense-mediated decay33 No protein IVS36+2T4C Unknown Truncation of exon 36 resulting in V1673fs?
X
ABCA4 p.Val2050Leu 15494742:143:993
status: NEW
PMID: 15192030
[PubMed]
Stenirri S et al: "Denaturing HPLC profiling of the ABCA4 gene for reliable detection of allelic variations."
No.
Sentence
Comment
35
Exon Genotypesa Exon Genotypesa 1b M1V (1A>G) (11) 24 3523-28TϾC (12) R18W (52C>T) (11) 25 G1203D (3608G>A)b 3 250_251insCAAA (7) 27 R1300X (3898C>T) (12) N96K (288C>A) R1300Q (3899G>A) (11) 302 ϩ 26 GϾA (13) 28 P1380L (4139CϾT) (14) 4 P143L (428C>T) (10) P1401P (4203CϾA) (15) 5 R152Q (455G>A) (4) 4253 ϩ 43GϾA (12) 6 571-1GϾT (4) 29 4253 ϩ 13GϾA (12) R212H (635G>A) (16) 4354-38GϾA (4) C230S (688T>A) (12) 30a 4466 ϩ 3GϾA (4) 641delG (9) 30b C1490Y (4469G>A) (17) 10 1240-14CϾT (13) P1512R (4535C>G) (4) H423R (1268ϾG) (13) 31 T1526M (4577C>T) (14) 1357 ϩ 11delG (16) 33/34 A1598D (4793C>A) (4) H423H (1269CϾT) (13) 35 4947delC (14) 11 1387delTT (4) 5018 ؉ 2T>C (7) R500R (1500GϾA) (4) 39 H1838Y (5512C>T) (14) 12 L541P (1622T>C) (14) 40 N1868I (5603AϾT) (13) R572Q (1715G>A) (17) L1894L (5682GϾC) (15) 13 Y639X (1917C>G) (17) 5714 ؉ 5G>A C641S (1922G>C) (4) 41 L1938L (5814AϾG) (12) 14 R653C (1957C>T) (12) 42 5836-43CϾA W700X (2099G>A) (4) 5836-11GϾA (15) 3607 ϩ 49TϾC P1948I (5843CϾT) (15) 15 V767D (2300T>A) (7) P1948P (5844AϾG) (15) 16 W821R (2461T>A) (14) G1961E (5882G>A) (14) 17 2588-33CϾTb 43 L1970F (5908C>T) (11) G863A (2588G>C) (17) 44 6006-16AϾG (16) 18 2654-36CϾT (4) I2023I (6069CϾT) (14) T897I (2690C>T) (7) L2027F (6079C>T) (14) 19 R943Q (2828GϾA) (13) 45 V2050L (6148G>C) (14) Y954D (2860T>G) (4) 46 R2107H (6320G>A) (18) N965S (2894A>G) (14) 6386 ؉ 2G>C (10) 20 G978D (2933G>A) (4) 47 R2139W (6415C>T) (14) L988L (2964CϾT) (4) R2149L (6446G>T) (4) 21 E1022K (3064G>A) (4) C2150Y (6449G>A) (19) A1038V (3113C>T) (14) 48 D2177N (6529G>A) (17) G1050D (3149G>A) (4) L2241V (6721C>G) (12) 3211_3212insGT (14) 6729 ϩ 21CϾT (15) 22 E1087K (3259G>A) (14) 49 6730-3TϾC (15) R1098C (3292C>T) (12) S2255I (6764GϾT) (13) S1099P (3295T>C) (4) 6816 ϩ 28GϾC (4) R1108C (3322C>T) (14) R1129L (3386G>T) (17) a Bold indicates disease-causing mutations.
X
ABCA4 p.Val2050Leu 15192030:35:1479
status: NEW34 Exon Genotypesa Exon Genotypesa 1b M1V (1A>G) (11) 24 3523-28Tb0e;C (12) R18W (52C>T) (11) 25 G1203D (3608G>A)b 3 250_251insCAAA (7) 27 R1300X (3898C>T) (12) N96K (288C>A) R1300Q (3899G>A) (11) 302 af9; 26 Gb0e;A (13) 28 P1380L (4139Cb0e;T) (14) 4 P143L (428C>T) (10) P1401P (4203Cb0e;A) (15) 5 R152Q (455G>A) (4) 4253 af9; 43Gb0e;A (12) 6 571-1Gb0e;T (4) 29 4253 af9; 13Gb0e;A (12) R212H (635G>A) (16) 4354-38Gb0e;A (4) C230S (688T>A) (12) 30a 4466 af9; 3Gb0e;A (4) 641delG (9) 30b C1490Y (4469G>A) (17) 10 1240-14Cb0e;T (13) P1512R (4535C>G) (4) H423R (1268b0e;G) (13) 31 T1526M (4577C>T) (14) 1357 af9; 11delG (16) 33/34 A1598D (4793C>A) (4) H423H (1269Cb0e;T) (13) 35 4947delC (14) 11 1387delTT (4) 5018 d19; 2T>C (7) R500R (1500Gb0e;A) (4) 39 H1838Y (5512C>T) (14) 12 L541P (1622T>C) (14) 40 N1868I (5603Ab0e;T) (13) R572Q (1715G>A) (17) L1894L (5682Gb0e;C) (15) 13 Y639X (1917C>G) (17) 5714 d19; 5G>A C641S (1922G>C) (4) 41 L1938L (5814Ab0e;G) (12) 14 R653C (1957C>T) (12) 42 5836-43Cb0e;A W700X (2099G>A) (4) 5836-11Gb0e;A (15) 3607 af9; 49Tb0e;C P1948I (5843Cb0e;T) (15) 15 V767D (2300T>A) (7) P1948P (5844Ab0e;G) (15) 16 W821R (2461T>A) (14) G1961E (5882G>A) (14) 17 2588-33Cb0e;Tb 43 L1970F (5908C>T) (11) G863A (2588G>C) (17) 44 6006-16Ab0e;G (16) 18 2654-36Cb0e;T (4) I2023I (6069Cb0e;T) (14) T897I (2690C>T) (7) L2027F (6079C>T) (14) 19 R943Q (2828Gb0e;A) (13) 45 V2050L (6148G>C) (14) Y954D (2860T>G) (4) 46 R2107H (6320G>A) (18) N965S (2894A>G) (14) 6386 d19; 2G>C (10) 20 G978D (2933G>A) (4) 47 R2139W (6415C>T) (14) L988L (2964Cb0e;T) (4) R2149L (6446G>T) (4) 21 E1022K (3064G>A) (4) C2150Y (6449G>A) (19) A1038V (3113C>T) (14) 48 D2177N (6529G>A) (17) G1050D (3149G>A) (4) L2241V (6721C>G) (12) 3211_3212insGT (14) 6729 af9; 21Cb0e;T (15) 22 E1087K (3259G>A) (14) 49 6730-3Tb0e;C (15) R1098C (3292C>T) (12) S2255I (6764Gb0e;T) (13) S1099P (3295T>C) (4) 6816 af9; 28Gb0e;C (4) R1108C (3322C>T) (14) R1129L (3386G>T) (17) a Bold indicates disease-causing mutations.
X
ABCA4 p.Val2050Leu 15192030:34:1479
status: NEW
PMID: 12796258
[PubMed]
Fishman GA et al: "ABCA4 gene sequence variations in patients with autosomal recessive cone-rod dystrophy."
No.
Sentence
Comment
94
Patients With Cone-Rod Dystrophy Patient No./ Age, y/Sex Race/ Ethnicity Visual Acuity Visual Field Fundus Type* Mutation Cone vs Rod ERG ReductionOD OS 1/74/F AA 20/60 - 2 5/600 Central and peripheral loss 1 Gly1448Arg C = R 2/35/F W 10/350 5/400 Central and peripheral loss 1 Ala1038Val Leu541Pro C = R 3/42/F H 20/400 20/400 Central and peripheral loss 1 Ala1038Val Trp1618stop C = R 4/54/F W 10/180 10/140 Central scotoma 1 Donor splice, 5bp3Ј g-a intron 40 C = R 5/36/F W 10/120 10/60 - 1 Central scotoma 1 Leu541Pro Asp600Tyr C ↓ R 6/49/F W 5/160 5/180 Central and peripheral loss 1 Donor splice 5bp3Ј g-a intron 40 C = R 7/49/F W 10/350 4/350 Central and peripheral loss 1 Glu328Stop Val767Asp C = R 8/40/M W 10/225 20/400 Central and peripheral loss 1 Ala1038Val C = R 9/36/M W 5/600 5/350 Central and peripheral loss 1 Gly550Arg C = R 10/39/F AA 20/100 - 2 20/400 Central scotoma 1 Ala1038Val C = R 11/26/F W 20/200 20/200 Central and peripheral loss 1 Val2050Leu C ↓ R 12/36/M W 20/200 20/80+1 Central scotoma 1 Donor splice 5bp3Ј g-a intron 40 C = R 13/43/M AA 20/400 20/200 Central and peripheral loss 2 Leu1201Arg C = R (ND) 14/33/M P 20/40+1 20/50 Central scotoma 2 Leu2027Phe C ↓ R 15/44/M AA CF 20/400 Central and peripheral loss 2 Leu1201Arg C = R (ND) 16/56/M AA 20/40 20/40 Central scotoma 2 Leu2027Phe C = R Abbreviations: AA, African American; C ↓ R, cone responses more reduced than rod amplitudes; C = R, cone and rod amplitudes were similarly reduced; CF, counting fingers; ERG, electroretinogram; H, Hispanic; ND, nondetectable; P, Palestinian; W, white.
X
ABCA4 p.Val2050Leu 12796258:94:981
status: NEW
PMID: 11726554
[PubMed]
Shroyer NF et al: "Cosegregation and functional analysis of mutant ABCR (ABCA4) alleles in families that manifest both Stargardt disease and age-related macular degeneration."
No.
Sentence
Comment
46
The complex allele [H1406Y; V2050L] was identified in STGD-affected AR215-4 (Fig. 1).
X
ABCA4 p.Val2050Leu 11726554:46:28
status: NEW97 Pedigree Maternal allele Paternal allele AMD relative A priori Cosegregation AR19 pGM, -6 0.5 - AR33 [W1408R; R1640W] R24H and D1532N mA, -16 0.5 Yes AR59 4232insTATG C1488R pGM, -6 0.5 No AR80 T1526M pGF, -5 0.5 - AR80 T1526M mGF, -7 0.5 Yes AR125 4947delC C1488R pGM, -7 0.5 Yes AR215 [H1406Y; V2050L] pGM, -5 0.5 - AR218 2160+1G→C G1961E mA, -8 0.5 No AR262 W821R pGGF, -7 0.25 No AR271 P68R E1087K mGA, -6 0.25 No AR335 D645N F608I mGM, -9 0.5 Yes AR382 R1108C mGM, -6 0.5 Yes AR389 E2096K 5714+5G→A pGM, -8 0.5 Yes AR397 5196+1G→A 5585-1G→A mA, -5 0.5 No AR410 A1038V 768G→T pC, -5 0.25 Yes AR422 pGM, -6 0.5 - AR423 P1380L D1532N pGF, -4 0.5 No AR468 P1380L P1380L mU, -9 0.5 Yes AR484 L2027F G550R mGU, -5 0.25 Yes AR562 R2107H 3050+5G→A pGU, -5 0.25 No AR643 5196+2T→C L2027F mU, -4 0.5 Yes AR661 P1380L C54Y mGF, -6 0.5 Yes AR669 664del13 pGF, -4 0.5 No AR534 W821R P1380L pGM, -7 0.5 Yes (17) Family 1 R212C I2113M mGM, I-2 0.5 Yes (27) Family 2 R1108C R2107H mGM, I-2 0.5 Yes (27) Family 3 R212C G1977S mGF, I-1 0.5 Yes (27) 10.25 15 unlikely to account for many of the remaining alleles (our unpublished observations).
X
ABCA4 p.Val2050Leu 11726554:97:296
status: NEW
PMID: 11702214
[PubMed]
Fumagalli A et al: "Mutational scanning of the ABCR gene with double-gradient denaturing-gradient gel electrophoresis (DG-DGGE) in Italian Stargardt disease patients."
No.
Sentence
Comment
37
DNA samples (n=22) carrying previously identified mutations in the ABCR gene were employed as controls for evaluating the efficacy of the DG-DGGE approach in detecting sequence variations R572Q (Lewis et al. 1999), Y639X (Lewis et al. 1999), G863A (Lewis et al. 1999; Maugeri et al. 1999), A1038V (Rozet et al. 1998), T1019M (Rozet et al. 1998), 3211insGT (Lewis et al. 1999), P1380L (Lewis et al. 1999), H1406Y (Lewis et al. 1999), 4947delC (Lewis et al. 1999), H1838Y (Lewis et al. 1999), 5714+5G→A (Cremers et al. 1998), N1868I (De La Paz et al. 1999), L1938L (Rivera et al. 2000), G1961E (Allikmets et al. 1997a, 1997b), L1970F (Lewis et al. 1999), L2027F (Nasonkin et al. 1998), V2050L (Lewis et al. 1999), E2131K (Lewis et al. 1999), R2139W (Lewis et al. 1999), 6709insG (Lewis et al. 1999), D2177N (Allikmets et al. 1997a, 1997b), 2181del12 (Lewis et al. 1999).
X
ABCA4 p.Val2050Leu 11702214:37:691
status: NEW
PMID: 11527935
[PubMed]
Briggs CE et al: "Mutations in ABCR (ABCA4) in patients with Stargardt macular degeneration or cone-rod degeneration."
No.
Sentence
Comment
147
Missense Changes Found in Patients with No Other Detected ABCR Changes Patient ID Missense Change Mouse abc134 Mouse abc234 Human ABCC35 032-069 Ala60Val Ala N/A Glu 032-028 Gly65Glu Gly N/A Leu 032-044 Gly550Arg* Gly N/A N/A 032-038 Trp821Arg‡ Trp N/A Trp 035-019, 032-097 Glu1122Lys Glu Glu Glu 032-063, 032-093 Arg2030Gln† Arg Arg Arg 071-002 Leu2035Pro Phe Leu Met 032-064 Val2050Leu Phe Val Cys 032-061 Arg2107His Arg Arg Arg 007-009 Gly2146Asp‡ Gly Gly Gly Residues at homologous locations in other ABCR proteins.
X
ABCA4 p.Val2050Leu 11527935:147:391
status: NEW144 Missense Changes Found in Patients with No Other Detected ABCR Changes Patient ID Missense Change Mouse abc134 Mouse abc234 Human ABCC35 032-069 Ala60Val Ala N/A Glu 032-028 Gly65Glu Gly N/A Leu 032-044 Gly550Arg* Gly N/A N/A 032-038 Trp821Argߥ Trp N/A Trp 035-019, 032-097 Glu1122Lys Glu Glu Glu 032-063, 032-093 Arg2030Glnߤ Arg Arg Arg 071-002 Leu2035Pro Phe Leu Met 032-064 Val2050Leu Phe Val Cys 032-061 Arg2107His Arg Arg Arg 007-009 Gly2146Aspߥ Gly Gly Gly Residues at homologous locations in other ABCR proteins.
X
ABCA4 p.Val2050Leu 11527935:144:389
status: NEW
No.
Sentence
Comment
102
Thirty-Three Truncated and 98 Amino Acid-Changing Variants in the ABCA4 Gene Exon Nucleotide Change Effect (A) (B) AMD (n ؍ 182) Control (n ؍ 96) STGD (n ؍ 374) Allele Prevalence 2 106delT FS NS 0 0 1 Ͻ0.01 2 160 ϩ 1g 3 a Splice site NS 0 0 1 Ͻ0.01 3 161G 3 A Cys54Tyr NS 0 0 6 Ͻ0.01 3 179C 3 T Ala60Val NS 0 0 2 Ͻ0.01 3 194G 3 A Gly65Glu NS 0 0 2 Ͻ0.01 3 223T 3 G Cys75Gly NS 0 0 2 Ͻ0.01 3 247delCAAA FS NS 0 0 2 Ͻ0.01 3 298C 3 T Ser100Pro NS 0 0 1 Ͻ0.01 5 454C 3 T Arg152Stop NS 0 0 2 Ͻ0.01 6 574G 3 A Ala192Thr NS 0 0 1 Ͻ0.01 6 618C 3 G Ser206Arg NS 0 0 3 Ͻ0.01 6 634C 3 T Arg212Cys 0.02 Yes 0 0 7 0.01 6 635G 3 A Arg212His NS 2 2 6 0.01 6 658C 3 T Arg220Cys NS 0 0 2 Ͻ0.01 6 661delG FS NS 0 0 1 Ͻ0.01 666delAAAGACGGTGC 6 GC FS NS 0 0 1 Ͻ0.01 6 746A 3 C Asp249Gly NS 0 0 1 Ͻ0.01 8 899C 3 A Thr300Asn NS 0 0 1 Ͻ0.01 8 997C 3 T Arg333Trp NS 0 0 1 Ͻ0.01 9 1140T 3 A Asn380Lys NS 0 0 1 Ͻ0.01 9 1222C 3 T Arg408Stop NS 0 0 1 Ͻ0.01 10 1268A 3 G His423Arg NS 1 0 7 0.01 10 1335C 3 G Ser445Arg NS 0 0 1 Ͻ0.01 10 1344delG FS NS 0 0 1 Ͻ0.01 11 1411G 3 A Glu471Lys NS 0 0 3 Ͻ0.01 11 1513delATCAC FS NS 0 0 1 Ͻ0.01 12 1622T 3 C Leu541Pro 0.001 Yes 0 0 11 0.01 13 1804C 3 T Arg602Trp NS 0 0 3 Ͻ0.01 13 1805G 3 A Arg602Gln NS 0 0 1 Ͻ0.01 13 1819G 3 T Gly607Trp NS 0 0 1 Ͻ0.01 13 1823T 3 A Phe608Ile NS 0 0 1 Ͻ0.01 13 1927G 3 A Val643Met NS 0 0 1 Ͻ0.01 14 1989G 3 T Trp663Stop NS 0 0 1 Ͻ0.01 14 2005delAT FS NS 0 0 3 Ͻ0.01 14 2041C 3 T Arg681Stop NS 0 0 2 Ͻ0.01 14 2147C 3 T Thr716Met NS 0 0 1 Ͻ0.01 15 2291G 3 A Cys764Tyr NS 0 0 1 Ͻ0.01 15 2294G 3 A Ser765Asn NS 0 0 1 Ͻ0.01 15 2300T 3 A Val767Asp NS 0 0 2 Ͻ0.01 16 2385del16bp FS NS 0 0 1 Ͻ0.01 16 2453G 3 A Gly818Glu NS 0 0 1 Ͻ0.01 16 2461T 3 A Trp821Arg NS 0 0 1 Ͻ0.01 16 2546T 3 C Val849Ala NS 0 0 4 Ͻ0.01 16 2552G 3 A Gly851Asp NS 0 0 1 Ͻ0.01 16 2560G 3 A Ala854Thr NS 0 0 1 Ͻ0.01 17 2588G 3 C Gly863Ala 0.0006 No 2 2 28 0.02 17 2617T 3 C Phe873Leu NS 0 0 1 Ͻ0.01 18 2690C 3 T Thr897Ile NS 0 0 1 Ͻ0.01 18 2701A 3 G Thr901Ala NS 0 1 0 Ͻ0.01 18 2703A 3 G Thr901Arg NS 0 0 2 Ͻ0.01 19 2828G 3 A Arg943Gln NS 20 13 37 0.05 19 2883delC FS NS 0 0 1 Ͻ0.01 20 2894A 3 G Asn965Ser NS 0 0 3 Ͻ0.01 19 2912C 3 A Thr971Asn NS 0 0 1 Ͻ0.01 19 2915C 3 A Thr972Asn NS 0 0 1 Ͻ0.01 20 2920T 3 C Ser974Pro NS 0 0 1 Ͻ0.01 20 2966T 3 C Val989Ala NS 0 0 2 Ͻ0.01 20 2977del8bp FS NS 0 0 1 Ͻ0.01 20 3041T 3 G Leu1014Arg NS 0 0 1 Ͻ0.01 21 3055A 3 G Thr1019Ala NS 0 0 1 Ͻ0.01 21 3064G 3 A Glu1022Lys NS 0 0 1 Ͻ0.01 21 3091A 3 G Lys1031Glu NS 0 0 1 Ͻ0.01 21 3113G 3 T Ala1038Val 0.001 Yes 1 0 17 0.01 22 3205insAA FS NS 0 0 1 Ͻ0.01 22 3261G 3 A Glu1087Lys NS 0 0 2 Ͻ0.01 22 3322C 3 T Arg1108Cys 0.04 Yes 0 0 6 Ͻ0.01 22 3323G 3 A Arg1108His NS 0 0 1 Ͻ0.01 23 3364G 3 A Glu1122Lys NS 0 0 1 Ͻ0.01 (continues) Exon Nucleotide Change Effect (A) (B) AMD (n ؍ 182) Control (n ؍ 96) STGD (n ؍ 374) Allele Prevalence 23 3386G 3 T Arg1129Leu NS 0 0 3 Ͻ0.01 24 3531C 3 A Cys1158Stop NS 0 0 1 Ͻ0.01 25 3749T 3 C Leu1250Pro NS 0 0 1 Ͻ0.01 26 3835delGATTCT FS NS 0 0 1 Ͻ0.01 27 3940C 3 A Pro1314Thr NS 0 1 0 Ͻ0.01 28 4139C 3 T Pro1380Leu 0.001 Yes 0 0 10 0.01 28 4222T 3 C Trp1408Arg NS 0 0 2 Ͻ0.01 28 4223G 3 T Trp1408Leu NS 0 0 2 Ͻ0.01 28 4234C 3 T Gln1412stop NS 0 0 1 Ͻ0.01 29 4297G 3 A Val1433Ile NS 1 0 0 Ͻ0.01 29 4319T 3 C Phe1440Ser NS 0 0 1 Ͻ0.01 30 4353 - 1g 3 t Splice site NS 0 0 1 Ͻ0.01 30 4457C 3 T Pro1486Leu NS 0 0 1 Ͻ0.01 30 4462T 3 C Cys1488Arg NS 0 0 3 Ͻ0.01 30 4463G 3 T Cys1488Phe NS 0 0 2 Ͻ0.01 30 4469G 3 A Cys1490Tyr NS 0 0 3 Ͻ0.01 30 4531insC FS NS 0 0 2 Ͻ0.01 32 4538A 3 G Gln1513Arg NS 0 0 1 Ͻ0.01 30 4539 ϩ 1g 3 t Splice site NS 0 0 1 Ͻ0.01 31 4574T 3 C Leu1525Pro NS 0 0 1 Ͻ0.01 33 4733delGTTT FS NS 0 0 1 Ͻ0.01 4859delATAACAinsTCC 35 T FS NS 0 0 1 Ͻ0.01 36 4909G 3 A Ala1637Thr NS 0 0 1 Ͻ0.01 35 4918C 3 T Arg1640Trp NS 0 0 1 Ͻ0.01 35 4919G 3 A Arg1640Gln NS 0 0 1 Ͻ0.01 35 4954T 3 G Tyr1652Asp NS 0 0 1 Ͻ0.01 36 5077G 3 A Val1693Ile NS 0 0 1 Ͻ0.01 36 5186T 3 C Leu1729Pro NS 0 0 2 Ͻ0.01 36 5206T 3 C Ser1736Pro NS 0 0 1 Ͻ0.01 36 5212del11bp FS NS 0 0 1 Ͻ0.01 37 5225delTGGTGGTGGGC FS NS 0 0 1 Ͻ0.01 del LPA 37 5278del9bp 1760 NS 0 0 1 Ͻ0.01 37 5288delG FS NS 0 0 1 Ͻ0.01 38 5395A 3 G Asn1799Asp NS 0 0 1 Ͻ0.01 38 5451T 3 G Asp1817Glu NS 1 0 4 Ͻ0.01 39 5584 ϩ 5g 3 a Splice site 0.02 Yes 0 0 6 Ͻ0.01 40 5603A 3 T Asn1868Ile 0.0006 No 20 7 79 0.08 40 5651T 3 A Val1884GLu NS 0 0 1 Ͻ0.01 40 5657G 3 A Gly1886Glu NS 0 0 1 Ͻ0.01 40 5687T 3 A Val1896Asp NS 0 0 1 Ͻ0.01 40 5693G 3 A Arg1898His NS 0 0 1 Ͻ0.01 40 5714 ϩ 5g 3 a Splice site NS 0 0 1 Ͻ0.01 42 5843CA 3 TG Pro1948Leu NS 11 7 28 0.04 42 5882G 3 A Gly1961Glu Ͻ0.0001 Yes 1 0 43 0.03 43 5908C 3 T Leu1970Phe NS 1 0 1 Ͻ0.01 43 5917delG FS NS 0 0 1 Ͻ0.01 44 6079C 3 T Leu2027Phe 0.01 Yes 0 0 9 0.01 44 6088C 3 T Arg2030Stop NS 0 0 2 Ͻ0.01 44 6089G 3 A Arg2030Gln NS 0 0 1 Ͻ0.01 44 6112A 3 T Arg2038Trp NS 0 0 1 Ͻ0.01 45 6148A 3 C Val2050Leu NS 1 0 0 Ͻ0.01 46 6212A 3 T Tyr2071Phe NS 0 0 1 Ͻ0.01 45 6229C 3 T Arg2077Trp NS 0 0 2 Ͻ0.01 46 6320G 3 A Arg2107His 0.01 Yes 0 0 10 0.01 46 6383A 3 G His2128Arg NS 0 0 1 Ͻ0.01 47 6446G 3 T Arg2149Leu NS 0 0 1 Ͻ0.01 47 6449G 3 A Cys2150Tyr NS 0 0 5 Ͻ0.01 48 6529G 3 A Asp2177Asn NS 2 0 0 Ͻ0.01 48 6686T 3 C Leu2229Pro NS 0 0 1 Ͻ0.01 48 6707delTCACACAG FS NS 0 0 1 Ͻ0.01 48 6729 ϩ 1g 3 a Splice site NS 0 0 1 Ͻ0.01 49 6764G 3 T Ser2255Ile 0.009 No 16 4 54 0.06 49 6788G 3 T Arg2263Leu NS 0 0 1 Ͻ0.01 (A) The probability under the null hypothesis of similar prevalence of each variant in Stargardt (STGD) compared with non-STGD alleles (two-tailed Fisher`s exact test); (B) compatability of the variant existing in a ratio of 100:1 in STGD to control alleles, calculated using the binomial distribution.
X
ABCA4 p.Val2050Leu 11328725:102:5612
status: NEW103 Thirty-Three Truncated and 98 Amino Acid-Changing Variants in the ABCA4 Gene Exon Nucleotide Change Effect (A) (B) AMD (n d1d; 182) Control (n d1d; 96) STGD (n d1d; 374) Allele Prevalence 2 106delT FS NS 0 0 1 b0d;0.01 2 160 af9; 1g 3 a Splice site NS 0 0 1 b0d;0.01 3 161G 3 A Cys54Tyr NS 0 0 6 b0d;0.01 3 179C 3 T Ala60Val NS 0 0 2 b0d;0.01 3 194G 3 A Gly65Glu NS 0 0 2 b0d;0.01 3 223T 3 G Cys75Gly NS 0 0 2 b0d;0.01 3 247delCAAA FS NS 0 0 2 b0d;0.01 3 298C 3 T Ser100Pro NS 0 0 1 b0d;0.01 5 454C 3 T Arg152Stop NS 0 0 2 b0d;0.01 6 574G 3 A Ala192Thr NS 0 0 1 b0d;0.01 6 618C 3 G Ser206Arg NS 0 0 3 b0d;0.01 6 634C 3 T Arg212Cys 0.02 Yes 0 0 7 0.01 6 635G 3 A Arg212His NS 2 2 6 0.01 6 658C 3 T Arg220Cys NS 0 0 2 b0d;0.01 6 661delG FS NS 0 0 1 b0d;0.01 666delAAAGACGGTGC 6 GC FS NS 0 0 1 b0d;0.01 6 746A 3 C Asp249Gly NS 0 0 1 b0d;0.01 8 899C 3 A Thr300Asn NS 0 0 1 b0d;0.01 8 997C 3 T Arg333Trp NS 0 0 1 b0d;0.01 9 1140T 3 A Asn380Lys NS 0 0 1 b0d;0.01 9 1222C 3 T Arg408Stop NS 0 0 1 b0d;0.01 10 1268A 3 G His423Arg NS 1 0 7 0.01 10 1335C 3 G Ser445Arg NS 0 0 1 b0d;0.01 10 1344delG FS NS 0 0 1 b0d;0.01 11 1411G 3 A Glu471Lys NS 0 0 3 b0d;0.01 11 1513delATCAC FS NS 0 0 1 b0d;0.01 12 1622T 3 C Leu541Pro 0.001 Yes 0 0 11 0.01 13 1804C 3 T Arg602Trp NS 0 0 3 b0d;0.01 13 1805G 3 A Arg602Gln NS 0 0 1 b0d;0.01 13 1819G 3 T Gly607Trp NS 0 0 1 b0d;0.01 13 1823T 3 A Phe608Ile NS 0 0 1 b0d;0.01 13 1927G 3 A Val643Met NS 0 0 1 b0d;0.01 14 1989G 3 T Trp663Stop NS 0 0 1 b0d;0.01 14 2005delAT FS NS 0 0 3 b0d;0.01 14 2041C 3 T Arg681Stop NS 0 0 2 b0d;0.01 14 2147C 3 T Thr716Met NS 0 0 1 b0d;0.01 15 2291G 3 A Cys764Tyr NS 0 0 1 b0d;0.01 15 2294G 3 A Ser765Asn NS 0 0 1 b0d;0.01 15 2300T 3 A Val767Asp NS 0 0 2 b0d;0.01 16 2385del16bp FS NS 0 0 1 b0d;0.01 16 2453G 3 A Gly818Glu NS 0 0 1 b0d;0.01 16 2461T 3 A Trp821Arg NS 0 0 1 b0d;0.01 16 2546T 3 C Val849Ala NS 0 0 4 b0d;0.01 16 2552G 3 A Gly851Asp NS 0 0 1 b0d;0.01 16 2560G 3 A Ala854Thr NS 0 0 1 b0d;0.01 17 2588G 3 C Gly863Ala 0.0006 No 2 2 28 0.02 17 2617T 3 C Phe873Leu NS 0 0 1 b0d;0.01 18 2690C 3 T Thr897Ile NS 0 0 1 b0d;0.01 18 2701A 3 G Thr901Ala NS 0 1 0 b0d;0.01 18 2703A 3 G Thr901Arg NS 0 0 2 b0d;0.01 19 2828G 3 A Arg943Gln NS 20 13 37 0.05 19 2883delC FS NS 0 0 1 b0d;0.01 20 2894A 3 G Asn965Ser NS 0 0 3 b0d;0.01 19 2912C 3 A Thr971Asn NS 0 0 1 b0d;0.01 19 2915C 3 A Thr972Asn NS 0 0 1 b0d;0.01 20 2920T 3 C Ser974Pro NS 0 0 1 b0d;0.01 20 2966T 3 C Val989Ala NS 0 0 2 b0d;0.01 20 2977del8bp FS NS 0 0 1 b0d;0.01 20 3041T 3 G Leu1014Arg NS 0 0 1 b0d;0.01 21 3055A 3 G Thr1019Ala NS 0 0 1 b0d;0.01 21 3064G 3 A Glu1022Lys NS 0 0 1 b0d;0.01 21 3091A 3 G Lys1031Glu NS 0 0 1 b0d;0.01 21 3113G 3 T Ala1038Val 0.001 Yes 1 0 17 0.01 22 3205insAA FS NS 0 0 1 b0d;0.01 22 3261G 3 A Glu1087Lys NS 0 0 2 b0d;0.01 22 3322C 3 T Arg1108Cys 0.04 Yes 0 0 6 b0d;0.01 22 3323G 3 A Arg1108His NS 0 0 1 b0d;0.01 23 3364G 3 A Glu1122Lys NS 0 0 1 b0d;0.01 (continues) Exon Nucleotide Change Effect (A) (B) AMD (n d1d; 182) Control (n d1d; 96) STGD (n d1d; 374) Allele Prevalence 23 3386G 3 T Arg1129Leu NS 0 0 3 b0d;0.01 24 3531C 3 A Cys1158Stop NS 0 0 1 b0d;0.01 25 3749T 3 C Leu1250Pro NS 0 0 1 b0d;0.01 26 3835delGATTCT FS NS 0 0 1 b0d;0.01 27 3940C 3 A Pro1314Thr NS 0 1 0 b0d;0.01 28 4139C 3 T Pro1380Leu 0.001 Yes 0 0 10 0.01 28 4222T 3 C Trp1408Arg NS 0 0 2 b0d;0.01 28 4223G 3 T Trp1408Leu NS 0 0 2 b0d;0.01 28 4234C 3 T Gln1412stop NS 0 0 1 b0d;0.01 29 4297G 3 A Val1433Ile NS 1 0 0 b0d;0.01 29 4319T 3 C Phe1440Ser NS 0 0 1 b0d;0.01 30 4353 afa; 1g 3 t Splice site NS 0 0 1 b0d;0.01 30 4457C 3 T Pro1486Leu NS 0 0 1 b0d;0.01 30 4462T 3 C Cys1488Arg NS 0 0 3 b0d;0.01 30 4463G 3 T Cys1488Phe NS 0 0 2 b0d;0.01 30 4469G 3 A Cys1490Tyr NS 0 0 3 b0d;0.01 30 4531insC FS NS 0 0 2 b0d;0.01 32 4538A 3 G Gln1513Arg NS 0 0 1 b0d;0.01 30 4539 af9; 1g 3 t Splice site NS 0 0 1 b0d;0.01 31 4574T 3 C Leu1525Pro NS 0 0 1 b0d;0.01 33 4733delGTTT FS NS 0 0 1 b0d;0.01 4859delATAACAinsTCC 35 T FS NS 0 0 1 b0d;0.01 36 4909G 3 A Ala1637Thr NS 0 0 1 b0d;0.01 35 4918C 3 T Arg1640Trp NS 0 0 1 b0d;0.01 35 4919G 3 A Arg1640Gln NS 0 0 1 b0d;0.01 35 4954T 3 G Tyr1652Asp NS 0 0 1 b0d;0.01 36 5077G 3 A Val1693Ile NS 0 0 1 b0d;0.01 36 5186T 3 C Leu1729Pro NS 0 0 2 b0d;0.01 36 5206T 3 C Ser1736Pro NS 0 0 1 b0d;0.01 36 5212del11bp FS NS 0 0 1 b0d;0.01 37 5225delTGGTGGTGGGC FS NS 0 0 1 b0d;0.01 del LPA 37 5278del9bp 1760 NS 0 0 1 b0d;0.01 37 5288delG FS NS 0 0 1 b0d;0.01 38 5395A 3 G Asn1799Asp NS 0 0 1 b0d;0.01 38 5451T 3 G Asp1817Glu NS 1 0 4 b0d;0.01 39 5584 af9; 5g 3 a Splice site 0.02 Yes 0 0 6 b0d;0.01 40 5603A 3 T Asn1868Ile 0.0006 No 20 7 79 0.08 40 5651T 3 A Val1884GLu NS 0 0 1 b0d;0.01 40 5657G 3 A Gly1886Glu NS 0 0 1 b0d;0.01 40 5687T 3 A Val1896Asp NS 0 0 1 b0d;0.01 40 5693G 3 A Arg1898His NS 0 0 1 b0d;0.01 40 5714 af9; 5g 3 a Splice site NS 0 0 1 b0d;0.01 42 5843CA 3 TG Pro1948Leu NS 11 7 28 0.04 42 5882G 3 A Gly1961Glu b0d;0.0001 Yes 1 0 43 0.03 43 5908C 3 T Leu1970Phe NS 1 0 1 b0d;0.01 43 5917delG FS NS 0 0 1 b0d;0.01 44 6079C 3 T Leu2027Phe 0.01 Yes 0 0 9 0.01 44 6088C 3 T Arg2030Stop NS 0 0 2 b0d;0.01 44 6089G 3 A Arg2030Gln NS 0 0 1 b0d;0.01 44 6112A 3 T Arg2038Trp NS 0 0 1 b0d;0.01 45 6148A 3 C Val2050Leu NS 1 0 0 b0d;0.01 46 6212A 3 T Tyr2071Phe NS 0 0 1 b0d;0.01 45 6229C 3 T Arg2077Trp NS 0 0 2 b0d;0.01 46 6320G 3 A Arg2107His 0.01 Yes 0 0 10 0.01 46 6383A 3 G His2128Arg NS 0 0 1 b0d;0.01 47 6446G 3 T Arg2149Leu NS 0 0 1 b0d;0.01 47 6449G 3 A Cys2150Tyr NS 0 0 5 b0d;0.01 48 6529G 3 A Asp2177Asn NS 2 0 0 b0d;0.01 48 6686T 3 C Leu2229Pro NS 0 0 1 b0d;0.01 48 6707delTCACACAG FS NS 0 0 1 b0d;0.01 48 6729 af9; 1g 3 a Splice site NS 0 0 1 b0d;0.01 49 6764G 3 T Ser2255Ile 0.009 No 16 4 54 0.06 49 6788G 3 T Arg2263Leu NS 0 0 1 b0d;0.01 (A) The probability under the null hypothesis of similar prevalence of each variant in Stargardt (STGD) compared with non-STGD alleles (two-tailed Fisher`s exact test); (B) compatability of the variant existing in a ratio of 100:1 in STGD to control alleles, calculated using the binomial distribution.
X
ABCA4 p.Val2050Leu 11328725:103:5522
status: NEW
PMID: 11379881
[PubMed]
Yatsenko AN et al: "Late-onset Stargardt disease is associated with missense mutations that map outside known functional regions of ABCR (ABCA4)."
No.
Sentence
Comment
111
To compare this observation directly with our previous report (Lewis et al. 1999), we replaced five mutations (A1038V, L2027F, R2030Q, R2038W, V2050L) to linker regions.
X
ABCA4 p.Val2050Leu 11379881:111:143
status: NEW
PMID: 10913642
[PubMed]
Fuse N et al: "Molecular genetic analysis of ABCR gene in Japanese dry form age-related macular degeneration."
No.
Sentence
Comment
31
Mutations Found in ABCR* Gene in 26 Exons Examined in This Study Exon AMD† Stargardt`s Disease Exon AMD Stargardt`s Disease 11 E471K 29 T1428M 15 31 R1517S 16 G818E, G863A (D847H) 33 I1562T G1578R 17 34 N1614FS 18 35 19 V931M, 2884delC N965M, (R943Q) 36 5196ϩ1G→A 5041deL15 5196ϩ2T→C 20 40 R1898H R1898H 21 A1028V 42 G1961E G1961E 22 3211insGT, V1072A E1087K 43 L1970F 6006ϩ1G→T 23 R1129L 44 L2027F, R2038W (I2023I) 24 45 V2050L, R2077W (I2083I) 25 46 R2106C (V2094V) 27 48 6519⌬11bp D2177N 6568⌬C 6519⌬11bp 6709insG *ABCR: ATP-binding cassette transporter.
X
ABCA4 p.Val2050Leu 10913642:31:468
status: NEW
PMID: 9973280
[PubMed]
Lewis RA et al: "Genotype/Phenotype analysis of a photoreceptor-specific ATP-binding cassette transporter gene, ABCR, in Stargardt disease."
No.
Sentence
Comment
76
2 0071GrA R24H 1 19 2894ArG N965S 3 36 5196ϩ1GrA Splice 2 3 0161GrA C54Y 1 21 3113CrT A1038V 16 5196ϩ2TrC Splice 1 0179CrT A60V 1 22 3211insGT FS 1 37 5281del9 PAL1761del 1 0203CrG P68R 1 3212CrT S1071L 1 38 5459GrC R1820P 1 0223TrG C75G 1 3215TrC V1072A 1 39 5512CrT H1838Y 1 6 0634CrT R212C 1 3259GrA E1087K 1 5527CrT R1843W 1 0664del13 FS 1 3322CrT R1108C 6 40 5585-1GrA Splice 1 0746ArG D249G 1 23 3364GrA E1122K 1 5657GrA G1886E 1 8 1007CrG S336C 1 3385GrT R1129C 1 5693GrA R1898H 4 1018TrG Y340D 1 3386GrT R1129L 2 5714ϩ5GrA Splice 8 11 1411GrA E471K 1 24 3602TrG L1201R 1 42 5882GrA G1961E 16 12 1569TrG D523E 1 25 3610GrA D1204N 1 5898ϩ1GrT Splice 3 1622TrC L541P 1 28 4139CrT P1380L 4 43 5908CrT L1970F 1 1715GrA R572Q 2 4216CrT H1406Y 1 5929GrA G1977S 1 1715GrC R572P 1 4222TrC W1408R 4 6005ϩ1GrT Splice 1 13 1804CrT R602W 1 4232insTATG FS 1 44 6079CrT L2027F 11 1822TrA F608I 2 4253ϩ5GrT Splice 1 6088CrT R2030X 1 1917CrA Y639X 1 29 4297GrA V1433I 1 6089GrA R2030Q 1 1933GrA D645N 1 4316GrA G1439D 2 6112CrT R2038W 1 14 2005delAT FS 1 4319TrC F1440S 1 45 6148GrC V2050L 2 2090GrA W697X 1 4346GrA W1449X 1 6166ArT K2056X 1 2160ϩ1GrC Splice 1 30a 4462TrC C1488R 2 6229CrT R2077W 1 16 2453GrA G818E 1 4457CrT P1486L 1 46 6286GrA E2096K 1 2461TrA W821R 1 30b 4469GrA C1490Y 3 6316CrT R2106C 1 2536GrC D846H 1 4539ϩ1GrT Splice 1 47 6391GrA E2131K 1 2552GrC G851D 1 31 4577CrT T1526M 7 6415CrT R2139W 1 17 2588GrC G863A 11 4594GrA D1532N 3 6445CrT R2149X 1 19 2791GrA V931M 2 35 4947delC FS 1 48 6543del36 1181del12 1 2827CrT R943W 1 36 5041del15 VVAIC1681del 2 6709insG FS 1 2884delC FS 1 5087GrA S1696N 1 NOTE.-FS ϭ frameshift.
X
ABCA4 p.Val2050Leu 9973280:76:1110
status: NEW101 For the double-mutant chromosomes in the compound heterozygous families (AR31: Y340D and R572Q; AR106: E471K and E2131K; AR128: R572Q and G863A; and AR189: L541P and A1038V) and in those families in which the second disease chromosome was not identified (AR215: H1406Y and V2050L; AR264: D1204N and L2027F; AR254: D249G and R1898H; AR265: G863A and R1898H; AR285: 2714ϩ5GrA and 2884delC; and AR305: G863A and R1898H), in three cases (AR128, AR265, and AR305) each mutation on the double-mutant chromosome had been identified independently as disease causing in other, unrelated families with STGD1 (table 1).
X
ABCA4 p.Val2050Leu 9973280:101:273
status: NEW77 2 0071GrA R24H 1 19 2894ArG N965S 3 36 5196af9;1GrA Splice 2 3 0161GrA C54Y 1 21 3113CrT A1038V 16 5196af9;2TrC Splice 1 0179CrT A60V 1 22 3211insGT FS 1 37 5281del9 PAL1761del 1 0203CrG P68R 1 3212CrT S1071L 1 38 5459GrC R1820P 1 0223TrG C75G 1 3215TrC V1072A 1 39 5512CrT H1838Y 1 6 0634CrT R212C 1 3259GrA E1087K 1 5527CrT R1843W 1 0664del13 FS 1 3322CrT R1108C 6 40 5585afa;1GrA Splice 1 0746ArG D249G 1 23 3364GrA E1122K 1 5657GrA G1886E 1 8 1007CrG S336C 1 3385GrT R1129C 1 5693GrA R1898H 4 1018TrG Y340D 1 3386GrT R1129L 2 5714af9;5GrA Splice 8 11 1411GrA E471K 1 24 3602TrG L1201R 1 42 5882GrA G1961E 16 12 1569TrG D523E 1 25 3610GrA D1204N 1 5898af9;1GrT Splice 3 1622TrC L541P 1 28 4139CrT P1380L 4 43 5908CrT L1970F 1 1715GrA R572Q 2 4216CrT H1406Y 1 5929GrA G1977S 1 1715GrC R572P 1 4222TrC W1408R 4 6005af9;1GrT Splice 1 13 1804CrT R602W 1 4232insTATG FS 1 44 6079CrT L2027F 11 1822TrA F608I 2 4253af9;5GrT Splice 1 6088CrT R2030X 1 1917CrA Y639X 1 29 4297GrA V1433I 1 6089GrA R2030Q 1 1933GrA D645N 1 4316GrA G1439D 2 6112CrT R2038W 1 14 2005delAT FS 1 4319TrC F1440S 1 45 6148GrC V2050L 2 2090GrA W697X 1 4346GrA W1449X 1 6166ArT K2056X 1 2160af9;1GrC Splice 1 30a 4462TrC C1488R 2 6229CrT R2077W 1 16 2453GrA G818E 1 4457CrT P1486L 1 46 6286GrA E2096K 1 2461TrA W821R 1 30b 4469GrA C1490Y 3 6316CrT R2106C 1 2536GrC D846H 1 4539af9;1GrT Splice 1 47 6391GrA E2131K 1 2552GrC G851D 1 31 4577CrT T1526M 7 6415CrT R2139W 1 17 2588GrC G863A 11 4594GrA D1532N 3 6445CrT R2149X 1 19 2791GrA V931M 2 35 4947delC FS 1 48 6543del36 1181del12 1 2827CrT R943W 1 36 5041del15 VVAIC1681del 2 6709insG FS 1 2884delC FS 1 5087GrA S1696N 1 NOTE.-FS afd; frameshift.
X
ABCA4 p.Val2050Leu 9973280:77:1116
status: NEW102 For the double-mutant chromosomes in the compound heterozygous families (AR31: Y340D and R572Q; AR106: E471K and E2131K; AR128: R572Q and G863A; and AR189: L541P and A1038V) and in those families in which the second disease chromosome was not identified (AR215: H1406Y and V2050L; AR264: D1204N and L2027F; AR254: D249G and R1898H; AR265: G863A and R1898H; AR285: 2714af9;5GrA and 2884delC; and AR305: G863A and R1898H), in three cases (AR128, AR265, and AR305) each mutation on the double-mutant chromosome had been identified independently as disease causing in other, unrelated families with STGD1 (table 1).
X
ABCA4 p.Val2050Leu 9973280:102:273
status: NEW
PMID: 23940504
[PubMed]
Corton M et al: "Exome sequencing of index patients with retinal dystrophies as a tool for molecular diagnosis."
No.
Sentence
Comment
105
FAMILY ID INDEX PATIENT ID GENE (OMIM entry) NUCLEOTIDE CHANGE PROTEIN CHANGE NOVEL/KNOWN REFERENCE RP-0674 01-0570 ABCA4 c.287delA p.N96Tfs*19 novel (601691) c.6148G.C p.V2050L known [43] RP-0298 95-0103 ABCA4 c.4720G.T p.E1574* known [44] c.950delG p.G317Afs*57 novel RP-1102 07-0366 ABCA4 c.2285C.A (homoz) p.A762E known [45] RP-1164 07-0360 CHM (300390) c.863dupA p.M289Y*18 novel RP-1263 08-0177 USH2A c.920_923dupGCCA p.H308Qfs*16 known [46] (608400) c.12574C.T p.R4192C novel RP-1659 10-1367 CNGB3 c.1148delC p.T383Ifs*13 known [31] (605080) c.1666G.T p.E556* novel RP-1174 04-0834 CNGB3 c.1148delC (homoz) p.T383Ifs*13 known [31] RP-0137 1601 RP1 c.1625C.G p.S542* novel (603937) c.4804C.T p.Q1602* novel RP-0235 2343 RP1 c.5173C.T (homoz) p.Q1725* novel RP-1116 06-1075 NMNAT1 c.507G.A p.W169* known [47] (608700) c.769G.A p.E257K known [47] doi:10.1371/journal.pone.0065574.t001 clinical phenotype of the patients, and/or the sequencing/ mapping methods of NGS itself.
X
ABCA4 p.Val2050Leu 23940504:105:171
status: NEW
PMID: 23953153
[PubMed]
Fujinami K et al: "Clinical and molecular analysis of Stargardt disease with preserved foveal structure and function."
No.
Sentence
Comment
142
Allele Frequencies of 72 ABCA4 Variants Identified in a Comparison Groupa With the Typical Stargardt Disease (140 Patients Without Evidence of Foveal Sparing on Autofluorescence Imaging) (Continued) Exon Nucleotide Substitution and Amino Acid Change Number of Alleles Allele Frequency Int 33 c.4773&#fe;48C>T 1 0.36% 34 c.4793C>A, p.Ala1598Asp 1 0.36% 35 c.c.4918C>T, p.Arg1640Trp 1 0.36% Int 35 c.5018&#fe;2T>C, Splice site 2 0.71% 36 c.5114G>A, p.Arg1705Gln 2 0.71% 37 c.5222_5233delTGGTGGTGGGC, p.Lys1741Hisfs 1 0.36% 37 c.5281_5289delCTT CCT GCC, p.Pro1761_Leu1763del 2 0.71% Int 38 c.5461-10T>C 23 8.21% Int 39 c.5585-1G>A, Splice site 1 0.36% Int 40 c.5714&#fe;5G>A, Splice site 5 1.79% 42 c.5882G>A, p.Gly1961Glu 17 6.07% 43 c.5908C>T, p.Leu1970Phe 2 0.71% 43 c.5917delG, p.Val1973* 1 0.36% 44 c.6079C>T, p.Leu2027Phe 10 3.57% 44 c.6089G>A, p.Arg2030Gln 3 1.07% 44 c.6118C>T, p.Arg2040* 1 0.36% 45 c.6148G>C, p.Val2050Leu 3 1.43% 46 c.6286G>A, p.Glu2096Lys 1 0.36% 46 c.6320G>A, p.Arg2107His 4 1.43% 47 c.6445C>T, p.Arg2149* 1 0.36% 47 c.6449G>A, p.Cys2150Tyr 3 1.07% 48 c.6658C>T, p.Gln2220* 3 1.07% 48 c.6709_6710insG, p.Thr2237Serfs 1 0.36% Int &#bc; Intron.
X
ABCA4 p.Val2050Leu 23953153:142:918
status: NEW
PMID: 25698705
[PubMed]
Fernandez-San Jose P et al: "Targeted Next-Generation Sequencing Improves the Diagnosis of Autosomal Dominant Retinitis Pigmentosa in Spanish Patients."
No.
Sentence
Comment
79
Spectrum of Variants Causative of the Disease Identified With the RD_NGS_Panel in Autosomal Dominant Retinitis Pigmentosa Families Family Gene NM HGVS-cdna HGVS-prot Effect Zyg dbSNP (MAF) SIFT Polyphen-2 Mutation Taster Human Splicing Finder Cosegregation (Affected/ Unaffected/ Asymptomatic) Frequency in Spanish Control Alleles Reference Known mutations RP-1875 ABCA4* NM_000350.2 c.3386G>T p.Arg1129Leu Missense Het rs1801269 (<0.01) D (0) Pr-D (0.992) DC (1.000) - Yes (2/11 ) 0/150 Allikmets et al., 28 1997 c.6148G>C p.Val2050Leu Missense Het rs41292677 (0.04) D (0.01) Pr-D (0.950) DC (0.999) - 0/150 Allikmets et al., 29 1997 RP-1688 CRX NM_000554.4 c.586_587insC p.Ala198Glyfs*38 Frameshift Het - - - DC (1.000) - NA 0/150 Sohocki et al., 30 1998 RP-1970 PRPF31 NM_015629.3 c.1146&#fe;2T>C - Splicing Het - - - DC (1.000) Decrease 5 0 donor site of exon 11 (90.88->72.59) Yes (2) 0/150 Waseem et al., 31 2007 RP-0642 RHO NM_000539.3 c.44A>G p.Asn15Ser Missense Het rs104893786 (nfd) D (0) Pr-D (0.998) DC (1.000) - Yes (1/2) 0/150 Kranich et al., 32 1993 RP-1480 SNRNP200 NM_014014.4 c.3260C>T p.Ser1087Leu Missense Het - D (0) Pr-D (0.995) DC (1.000) - Yes (4/4/4) 0/150 Zhao et al., 33 2009 Novel LOF protein mutations RP-1541 PRPF31 NM_015629.3 c.937_938insA p.Gly314Argfs*10 Frameshift Het - - - DC (1.000) - Yes (2/2) 0/150 This study RP-1176 PRPH2 NM_000322.4 c.582-1G>A - Splicing Het - - - - Decrease 3 0 acceptor site of exon 2 (82.97->54.03) Yes (2) 0/150 This study RP-2072 RP1 NM_006269.1 c.1981G>T p.Glu661* Nonsense Het - - - DC (1.000) - NA 0/150 This study RP-1890 RP1 NM_006269.1 c.2286delA p.Asn763Ilefs*12 Frameshift Het - - - DC (1.000) - Yes (2) 0/150 This study RP-1387 RP1 NM_006269.1 c.2745_2749del p.Tyr915* Nonsense Het - - - DC (1.000) - Yes (4/2) 0/150 This study RP-0631 RPGR* NM_000328.2 c.1234C>T p.Arg412* Nonsense Het - - - DC (1.000) - Yes (2) 0/150 This study Novel nonsynonymous/in-frame mutations RP-1728 GUCA1B NM_002098.5 c.131G>A p.Arg44His Missense Het - D (0.004) B (0.065) DC (0.997) - Yes (2/1) 0/300 This study RP-0422 IMPDH1 NM_000883.3 c.962C>T p.Ala321Val Missense Het - D (0) Pr-D (0.926) DC (1.000) - Yes (3/11) 0/300 This study RP-0652 PRPH2 NM_000322.4 c.536G>T p.Trp179Leu Missense Het - D (0.010) Pr-D (1.000) DC (1.000) - Yes (2) 0/300 This study RP-0948 RP1 NM_006269.1 c.4328G>A p.Arg1443Gln Missense Het - D (0) Pr-D (0.974) P (0.993) - Yes (2/1) 0/300 This study RP-1682 RP2* NM_006915.2 c.9_11del p.Phe4del In-frame Het - - - DC (0.986) - Yes (1/3) 0/300 This study LOF, loss of function; Zyg, zygosity; Het, heterozygosis; nfd, no frequency data; SIFT, deleterious (D); Polyphen2: probably damaging (Pr-D) and benign (B); Mutation Taster: disease causing (DC) and polymorphism (P); NA, not available.
X
ABCA4 p.Val2050Leu 25698705:79:526
status: NEW84 Two known compound heterozygous mutations (p.Arg1129Leu) and (p.Val2050Leu) in the ABCA4 gene were detected in one family, and two novel mutations in the chromosome X genes, RPGR (p.Arg412*) and RP2 (p.Phe4del).
X
ABCA4 p.Val2050Leu 25698705:84:64
status: NEW
PMID: 25884411
[PubMed]
Grassmann F et al: "Common synonymous variants in ABCA4 are protective for chloroquine induced maculopathy (toxic maculopathy)."
No.
Sentence
Comment
95
Table 2 Genetic variants identified in ABCA4 sequence analysis in CQ-treated patients with (cases) and without (controls) toxic maculopathy Frequency in Variant (NM_000350.2) Amino acid exchange (NP_000341.2) Cases Controls EURߤ Raw p-value FDR# c.324G > A M114I 0.00 0.04 - - - c.635G > A R212H 0.06 0.08 0.06 - - c.1268A > G* H423R 0.29 0.23 0.30 0.58783 0.58783 c.1269C > T H423H 0.13 0.04 0.07 - - c.1622T > C L541P 0.02 0.00 - - - c.2588G > C G863A 0.00 0.04 0.00 - - c.2828G > A R943Q 0.04 0.12 0.04 - - c.3113C > T A1038V 0.02 0.00 0.00 - - c.4203C > A P1401P 0.00 0.04 - - - c.4297G > A V1433I 0.00 0.04 0.00 - - c.5603A > T N1868I 0.06 0.08 0.07 - - c.5682G > C* L1894L 0.13 0.38 0.26 0.02292 0.030 c.5814A > G* L1938L 0.06 0.31 0.18 0.00722 0.014 c.5843C > T P1948L 0.04 0.08 0.04 - - c.5844A > G* P1948P 0.06 0.31 0.19 0.00722 0.014 c.6069T > C I2023I 0.04 0.08 0.06 - c.6148G > C V2050L 0.02 0.00 0.00 - - c.6249C > T I2083I 0.04 0.08 0.05 - - c.6282 + 7G > A - 0.04 0.08 0.05 - - c.6285T > C D2095D 0.08 0.15 0.10 - - c.6357A > G E2119E 0.02 0.00 - - - c.6730-3T > C - 0.02 0.12 0.02 - - c.6764G > T S2255I 0.02 0.12 0.02 - - *Common variants (combined frequency in cases and controls > 11.6%).
X
ABCA4 p.Val2050Leu 25884411:95:898
status: NEW
PMID: 26551331
[PubMed]
Duncker T et al: "Quantitative Fundus Autofluorescence and Optical Coherence Tomography in ABCA4 Carriers."
No.
Sentence
Comment
205
Heterozygous mutations in ABCA4 (p.V2050L) have also been reported to contribute to an exacerbation of the phenotype conferred by a monoallelic mutation in PRPH2 (p.R172W).41 In another study, 12 nonsymptomatic mutation-carrying relatives of STGD1 patients were found to have normal visual acuity but impaired contrast sensitivity and reduced multifocal ERG amplitudes.21 More recently, a subset of ABCA4 carriers were reported to have reduced visual acuity, fundus abnormalities that included pigmentary changes (8/18) and flecks, and multifocal ERGs of reduced amplitude and delayed implicit times.22 Some missense mutations, including the complex allele p.
X
ABCA4 p.Val2050Leu 26551331:205:35
status: NEW
PMID: 26593885
[PubMed]
Sciezynska A et al: "Next-generation sequencing of ABCA4: High frequency of complex alleles and novel mutations in patients with retinal dystrophies from Central Europe."
No.
Sentence
Comment
7
[(R152*; V2050L)].
X
ABCA4 p.Val2050Leu 26593885:7:9
status: NEW97 [(R152*; V2050L)] is a novel one.
X
ABCA4 p.Val2050Leu 26593885:97:9
status: NEW149 [(R152*; V2050L)] (8/184) (1/1172) p < 0.0001 c.
X
ABCA4 p.Val2050Leu 26593885:149:9
status: NEW172 [(R152*; V2050L)] was of immense importance for making a proper molecular diagnosis.
X
ABCA4 p.Val2050Leu 26593885:172:9
status: NEW173 A patient carrying exclusively p.R152* and p.V2050L, could have been easily misinterpreted as a compound heterozygote.
X
ABCA4 p.Val2050Leu 26593885:173:45
status: NEW174 Co-occurrence of p.R152* and p.V2050L has been previously noted in Polish patients (M. Krawczynski, unpublished data) and now the existence of the novel complex allele has been definitely confirmed.
X
ABCA4 p.Val2050Leu 26593885:174:31
status: NEW