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Pediatric Disease Annotations & Medicines



   cone-rod dystrophy
  

Disease ID 629
Disease cone-rod dystrophy
Definition
Hereditary, progressive degeneration of the retina due to death of ROD PHOTORECEPTORS initially and subsequent death of CONE PHOTORECEPTORS. It is characterized by deposition of pigment in the retina.
Synonym
chorioretinal heredodystrophy
cone rod dystrophy
cone-rod dystrophy 2
cone-rod retinal dystrophy
cord
cord2
crd
crd2
dystrophy, peripheral tapetoretinal
pigmentary retinopathies
pigmentary retinopathy
rcrd2
retinal cone-rod dystrophy
retinitis pigmentosa
retinitis pigmentosa (disorder)
retinitis pigmentosa (rp)
retinitis pigmentosa [disease/finding]
retinopathies, pigmentary
retinopathy, pigmentary
rod cone dystrophies
rod cone dystrophy
rod-cone dystrophies
rod-cone dystrophy
rp - retinitis pigmentosa
tapetoretinal degeneration
tapetoretinal degenerations
Orphanet
OMIM
DOID
UMLS
C0035334
MeSH
SNOMED-CT
Comorbidity
UMLS | Disease | Sentences' Count(Total Sentences:7)
C0265294  |  metaphyseal dysplasia  |  6
C0700635  |  spondylometaphyseal dysplasia  |  6
C0002452  |  amelogenesis imperfecta  |  3
C0027092  |  myopia  |  2
C0456909  |  blindness  |  2
C0028754  |  obesity  |  1
C0878677  |  danon disease  |  1
Curated Gene
Entrez_id | Symbol | Resource(Total Genes:120)
MAK  |  4117  |  CLINVAR;ORPHANET;UniProtKB-KW
RIMS1  |  22999  |  ORPHANET;UniProtKB-KW
CNNM4  |  26504  |  UniProtKB-KW
WDR19  |  57728  |  GHR
CACNA1F  |  778  |  ORPHANET;UniProtKB-KW
PRPS1  |  5631  |  UniProtKB-KW
RPGR  |  6103  |  CLINVAR;CTD_human;ORPHANET;GHR;UniProtKB-KW
PDE6G  |  5148  |  ORPHANET;GHR;UniProtKB-KW
PDE6A  |  5145  |  CTD_human;ORPHANET;GHR;UniProtKB-KW
PDE6B  |  5158  |  CLINVAR;CTD_human;ORPHANET;GHR;UniProtKB-KW
POC1B  |  282809  |  ORPHANET;UniProtKB-KW
NEK2  |  4751  |  ORPHANET;UniProtKB-KW
PRCD  |  768206  |  ORPHANET;GHR;UniProtKB-KW
MT-ATP6  |  4508  |  UniProtKB-KW
RP2  |  6102  |  ORPHANET;GHR;UniProtKB-KW
BBS2  |  583  |  ORPHANET;UniProtKB-KW
KIZ  |  55857  |  ORPHANET
CDH23  |  64072  |  UniProtKB-KW
GUCY2D  |  3000  |  CTD_human;ORPHANET;UniProtKB-KW
MYO7A  |  4647  |  CLINVAR;UniProtKB-KW
ALMS1  |  7840  |  UniProtKB-KW
USH1G  |  124590  |  UniProtKB-KW
USH1C  |  10083  |  UniProtKB-KW
CA4  |  762  |  ORPHANET;GHR;UniProtKB-KW
PROM1  |  8842  |  ORPHANET;GHR;UniProtKB-KW
PCDH15  |  65217  |  UniProtKB-KW
PRPF3  |  9129  |  ORPHANET;GHR;UniProtKB-KW
PRPF6  |  24148  |  CLINVAR;ORPHANET;UniProtKB-KW
PRPF4  |  9128  |  ORPHANET;UniProtKB-KW
PRPF8  |  10594  |  ORPHANET;GHR;UniProtKB-KW
ARL6  |  84100  |  ORPHANET;UniProtKB-KW
OFD1  |  8481  |  ORPHANET
PNPLA6  |  10908  |  UniProtKB-KW
RPE65  |  6121  |  CLINVAR;CTD_human;ORPHANET;GHR;UniProtKB-KW
SLC7A14  |  57709  |  ORPHANET;UniProtKB-KW
MFRP  |  83552  |  UniProtKB-KW
RPGRIP1  |  57096  |  CTD_human;ORPHANET;UniProtKB-KW
SNRNP200  |  23020  |  CLINVAR;ORPHANET;GHR;UniProtKB-KW
C2orf71  |  388939  |  CLINVAR;CTD_human;UniProtKB-KW;GHR
TULP1  |  7287  |  CLINVAR;ORPHANET;GHR;UniProtKB-KW
ABHD12  |  26090  |  UniProtKB-KW
NRL  |  4901  |  CLINVAR;CTD_human;ORPHANET;GHR;UniProtKB-KW
LRAT  |  9227  |  CLINVAR;ORPHANET;GHR
RHO  |  6010  |  CLINVAR;CTD_human;ORPHANET;GHR;UniProtKB-KW
PDZD7  |  79955  |  UniProtKB-KW
PRPH2  |  5961  |  CLINVAR;ORPHANET;GHR;UniProtKB-KW
ZNF513  |  130557  |  ORPHANET;GHR;UniProtKB-KW
AGBL5  |  60509  |  ORPHANET;UniProtKB-KW
PEX7  |  5191  |  UniProtKB-KW
CERKL  |  375298  |  ORPHANET;GHR
RBP3  |  5949  |  CTD_human;ORPHANET;GHR;UniProtKB-KW
HARS  |  3035  |  UniProtKB-KW
TTPA  |  7274  |  CTD_human
RGR  |  5995  |  CTD_human;ORPHANET;GHR;UniProtKB-KW
POMGNT1  |  55624  |  ORPHANET;UniProtKB-KW
USH2A  |  7399  |  CLINVAR;CTD_human;ORPHANET;GHR;UniProtKB-KW
FAM161A  |  84140  |  CTD_human;ORPHANET;GHR;UniProtKB-KW
IMPDH1  |  3614  |  CTD_human;ORPHANET;GHR;UniProtKB-KW
TTC8  |  123016  |  ORPHANET;GHR;UniProtKB-KW
DHDDS  |  79947  |  ORPHANET;UniProtKB-KW
IFT140  |  9742  |  CLINVAR;ORPHANET
CNGA3  |  1261  |  ORPHANET
CNGA1  |  1259  |  CTD_human;ORPHANET;GHR;UniProtKB-KW
ZNF408  |  79797  |  ORPHANET;UniProtKB-KW
GUCA1B  |  2979  |  CTD_human;ORPHANET;GHR;UniProtKB-KW
PITPNM3  |  83394  |  ORPHANET;UniProtKB-KW
ADAM9  |  8754  |  ORPHANET;UniProtKB-KW
MERTK  |  10461  |  CLINVAR;CTD_human;ORPHANET;GHR;UniProtKB-KW
C8orf37  |  157657  |  UniProtKB-KW
EYS  |  346007  |  CLINVAR;CTD_human;ORPHANET;GHR;UniProtKB-KW
SAG  |  6295  |  CTD_human;ORPHANET;GHR;UniProtKB-KW
TTLL5  |  23093  |  ORPHANET;UniProtKB-KW
KCNV2  |  169522  |  UniProtKB-KW
GUCA1A  |  2978  |  ORPHANET
RP9  |  6100  |  ORPHANET;GHR;UniProtKB-KW
RP1  |  6101  |  CLINVAR;ORPHANET;GHR;UniProtKB-KW
IMPG2  |  50939  |  CLINVAR;ORPHANET;GHR;UniProtKB-KW
PRPF31  |  26121  |  CLINVAR;ORPHANET;GHR;UniProtKB-KW
RLBP1  |  6017  |  CTD_human;UNIPROT;ORPHANET;GHR
SPATA7  |  55812  |  CTD_human;ORPHANET;GHR;UniProtKB-KW
PANK2  |  80025  |  CLINVAR
CEP78  |  84131  |  UniProtKB-KW
BEST1  |  7439  |  CLINVAR;ORPHANET;GHR;UniProtKB-KW
SLC4A4  |  8671  |  UniProtKB-KW
RAB28  |  9364  |  ORPHANET;UniProtKB-KW
TOPORS  |  10210  |  CLINVAR;ORPHANET;GHR;UniProtKB-KW
CLRN1  |  7401  |  ORPHANET;UniProtKB-KW
HGSNAT  |  138050  |  ORPHANET;UniProtKB-KW
PHYH  |  5264  |  UniProtKB-KW
RAX2  |  84839  |  ORPHANET;UniProtKB-KW
DRAM2  |  128338  |  ORPHANET;UniProtKB-KW
TUB  |  7275  |  ORPHANET
CRB1  |  23418  |  CLINVAR;CTD_human;ORPHANET;GHR;UniProtKB-KW
FLVCR1  |  28982  |  UniProtKB-KW
REEP6  |  92840  |  UniProtKB-KW
ATF6  |  22926  |  CTD_human
CRX  |  1406  |  CLINVAR;GHR;ORPHANET;UniProtKB-KW;UNIPROT;CTD_human
CIB2  |  10518  |  UniProtKB-KW
IFT172  |  26160  |  ORPHANET;UniProtKB-KW
UNC119  |  9094  |  CTD_human;ORPHANET;UniProtKB-KW
CDHR1  |  92211  |  ORPHANET;UniProtKB-KW
KLHL7  |  55975  |  ORPHANET;GHR;UniProtKB-KW
ROM1  |  6094  |  CLINVAR;ORPHANET;GHR;UniProtKB-KW
AIPL1  |  23746  |  CTD_human;ORPHANET
FSCN2  |  25794  |  ORPHANET;GHR
PCYT1A  |  5130  |  UniProtKB-KW
ABCA4  |  24  |  CLINVAR;CTD_human;ORPHANET;GHR;UniProtKB-KW
RDH12  |  145226  |  CLINVAR;CTD_human;ORPHANET;GHR;UniProtKB-KW
ARL2BP  |  23568  |  ORPHANET
TRNT1  |  51095  |  UniProtKB-KW
CNGB1  |  1258  |  CLINVAR;CTD_human;ORPHANET;GHR;UniProtKB-KW
RP1L1  |  94137  |  CLINVAR
IDH3B  |  3420  |  CTD_human;ORPHANET;GHR;UniProtKB-KW
OPN1MW  |  2652  |  ORPHANET
RP22  |  6114  |  CTD_human
RP24  |  6116  |  CTD_human
NR2E3  |  10002  |  CLINVAR;ORPHANET
CACNA2D4  |  93589  |  ORPHANET
SEMA4A  |  64218  |  ORPHANET;GHR;UniProtKB-KW
OPN1LW  |  5956  |  ORPHANET
Inferring Gene
Entrez_id | Symbol | Resource(Total Genes:32)
24  |  ABCA4  |  infer
375298  |  CERKL  |  infer
1258  |  CNGB1  |  infer
23418  |  CRB1  |  infer
1406  |  CRX  |  infer
346007  |  EYS  |  infer
25794  |  FSCN2  |  infer
2782  |  GNB1  |  infer
2792  |  GNGT1  |  infer
2979  |  GUCA1B  |  infer
3614  |  IMPDH1  |  infer
9227  |  LRAT  |  infer
10461  |  MERTK  |  infer
10002  |  NR2E3  |  infer
4901  |  NRL  |  infer
5132  |  PDC  |  infer
5145  |  PDE6A  |  infer
5158  |  PDE6B  |  infer
26121  |  PRPF31  |  infer
5961  |  PRPH2  |  infer
145226  |  RDH12  |  infer
5995  |  RGR  |  infer
8787  |  RGS9  |  infer
6010  |  RHO  |  infer
6017  |  RLBP1  |  infer
6101  |  RP1  |  infer
6102  |  RP2  |  infer
6121  |  RPE65  |  infer
6103  |  RPGR  |  infer
10210  |  TOPORS  |  infer
7287  |  TULP1  |  infer
7399  |  USH2A  |  infer
Text Mined Gene
Entrez_id | Symbol | Score | Resource(Total Genes:954)
253962  |  CACNA1G-AS1  |  DISEASES
1595  |  CYP51A1  |  DISEASES
10083  |  USH1C  |  DISEASES
79657  |  RPAP3  |  DISEASES
57414  |  RHBDD2  |  DISEASES
1407  |  CRY1  |  DISEASES
55200  |  PLEKHG6  |  DISEASES
1015  |  CDH17  |  DISEASES
5009  |  OTC  |  DISEASES
2978  |  GUCA1A  |  DISEASES
2978  |  GUCA1A  |  DISEASES
2046  |  EPHA8  |  DISEASES
6694  |  SPP2  |  DISEASES
50700  |  RDH8  |  DISEASES
50939  |  IMPG2  |  DISEASES
5019  |  OXCT1  |  DISEASES
6193  |  RPS5  |  DISEASES
51314  |  NME8  |  DISEASES
10081  |  PDCD7  |  DISEASES
84572  |  GNPTG  |  DISEASES
2802  |  GOLGA3  |  DISEASES
9942  |  XYLB  |  DISEASES
7494  |  XBP1  |  DISEASES
23551  |  RASD2  |  DISEASES
64781  |  CERK  |  DISEASES
64781  |  CERK  |  DISEASES
328  |  APEX1  |  DISEASES
328  |  APEX1  |  DISEASES
1591  |  CYP24A1  |  DISEASES
1917  |  EEF1A2  |  DISEASES
6880  |  TAF9  |  DISEASES
2986  |  GUCY2F  |  DISEASES
2986  |  GUCY2F  |  DISEASES
282808  |  RAB40AL  |  DISEASES
6102  |  RP2  |  DISEASES
8237  |  USP11  |  DISEASES
7076  |  TIMP1  |  DISEASES
84560  |  MT4  |  DISEASES
10204  |  NUTF2  |  DISEASES
869  |  CBLN1  |  DISEASES
23568  |  ARL2BP  |  DISEASES
79650  |  USB1  |  DISEASES
64714  |  PDIA2  |  DISEASES
9028  |  RHBDL1  |  DISEASES
1428  |  CRYM  |  DISEASES
3163  |  HMOX2  |  DISEASES
55192  |  DNAJC17  |  DISEASES
2137  |  EXTL3  |  DISEASES
6101  |  RP1  |  DISEASES
4849  |  CNOT3  |  DISEASES
7288  |  TULP2  |  DISEASES
64130  |  LIN7B  |  DISEASES
57030  |  SLC17A7  |  DISEASES
84922  |  FIZ1  |  DISEASES
1406  |  CRX  |  DISEASES
1406  |  CRX  |  DISEASES
10567  |  RABAC1  |  DISEASES
5864  |  RAB3A  |  DISEASES
6671  |  SP4  |  DISEASES
51678  |  MPP6  |  DISEASES
6119  |  RPA3  |  DISEASES
4232  |  MEST  |  DISEASES
5949  |  RBP3  |  DISEASES
5949  |  RBP3  |  DISEASES
2584  |  GALK1  |  DISEASES
6347  |  CCL2  |  DISEASES
2648  |  KAT2A  |  DISEASES
1845  |  DUSP3  |  DISEASES
5957  |  RCVRN  |  DISEASES
5957  |  RCVRN  |  DISEASES
3381  |  IBSP  |  DISEASES
27339  |  PRPF19  |  DISEASES
4598  |  MVK  |  DISEASES
81566  |  CSRNP2  |  DISEASES
2597  |  GAPDH  |  DISEASES
2784  |  GNB3  |  DISEASES
7287  |  TULP1  |  DISEASES
7287  |  TULP1  |  DISEASES
6206  |  RPS12  |  DISEASES
2979  |  GUCA1B  |  DISEASES
2979  |  GUCA1B  |  DISEASES
5961  |  PRPH2  |  DISEASES
5961  |  PRPH2  |  DISEASES
2916  |  GRM6  |  DISEASES
57709  |  SLC7A14  |  DISEASES
2779  |  GNAT1  |  DISEASES
6787  |  NEK4  |  DISEASES
338  |  APOB  |  DISEASES
83444  |  INO80B  |  DISEASES
150465  |  TTL  |  DISEASES
92840  |  REEP6  |  DISEASES
10560  |  SLC19A2  |  DISEASES
10560  |  SLC19A2  |  DISEASES
5311  |  PKD2  |  DISEASES
9540  |  TP53I3  |  DISEASES
54812  |  AFTPH  |  DISEASES
29094  |  LGALSL  |  DISEASES
4488  |  MSX2  |  DISEASES
84918  |  LRP11  |  DISEASES
157506  |  RDH10  |  DISEASES
27241  |  BBS9  |  DISEASES
27019  |  DNAI1  |  DISEASES
28981  |  IFT81  |  DISEASES
29095  |  ORMDL2  |  DISEASES
1300  |  COL10A1  |  DISEASES
6903  |  TBCC  |  DISEASES
10930  |  APOBEC2  |  DISEASES
4201  |  MEA1  |  DISEASES
583  |  BBS2  |  DISEASES
57409  |  MIF4GD  |  DISEASES
10045  |  SH2D3A  |  DISEASES
6253  |  RTN2  |  DISEASES
8195  |  MKKS  |  DISEASES
8195  |  MKKS  |  DISEASES
6939  |  TCF15  |  DISEASES
402  |  ARL2  |  DISEASES
402  |  ARL2  |  DISEASES
3346  |  HTN1  |  DISEASES
6945  |  MLX  |  DISEASES
387332  |  TBPL2  |  DISEASES
821  |  CANX  |  DISEASES
50832  |  TAS2R4  |  DISEASES
57576  |  KIF17  |  DISEASES
7277  |  TUBA4A  |  DISEASES
2792  |  GNGT1  |  DISEASES
25775  |  C22orf24  |  DISEASES
2781  |  GNAZ  |  DISEASES
5880  |  RAC2  |  DISEASES
84316  |  NAA38  |  DISEASES
1258  |  CNGB1  |  DISEASES
2780  |  GNAT2  |  DISEASES
51095  |  TRNT1  |  DISEASES
8735  |  MYH13  |  DISEASES
25873  |  RPL36  |  DISEASES
81  |  ACTN4  |  DISEASES
55422  |  ZNF331  |  DISEASES
10343  |  PKDREJ  |  DISEASES
9104  |  RGN  |  DISEASES
2670  |  GFAP  |  DISEASES
83639  |  TEX101  |  DISEASES
23335  |  WDR7  |  DISEASES
5176  |  SERPINF1  |  DISEASES
3000  |  GUCY2D  |  DISEASES
3000  |  GUCY2D  |  DISEASES
5145  |  PDE6A  |  DISEASES
5145  |  PDE6A  |  DISEASES
78986  |  DUSP26  |  DISEASES
8739  |  HRK  |  DISEASES
5959  |  RDH5  |  DISEASES
5959  |  RDH5  |  DISEASES
9038  |  TAAR5  |  DISEASES
10200  |  MPHOSPH6  |  DISEASES
55213  |  RCBTB1  |  DISEASES
3569  |  IL6  |  DISEASES
10518  |  CIB2  |  DISEASES
27177  |  IL36B  |  DISEASES
55363  |  HEMGN  |  DISEASES
4856  |  NOV  |  DISEASES
11258  |  DCTN3  |  DISEASES
7274  |  TTPA  |  DISEASES
403  |  ARL3  |  DISEASES
403  |  ARL3  |  DISEASES
6857  |  SYT1  |  DISEASES
5700  |  PSMC1  |  DISEASES
3843  |  IPO5  |  DISEASES
64398  |  MPP5  |  DISEASES
7782  |  SLC30A4  |  DISEASES
8766  |  RAB11A  |  DISEASES
9187  |  SLC24A1  |  DISEASES
338917  |  VSX2  |  DISEASES
338917  |  VSX2  |  DISEASES
4591  |  TRIM37  |  DISEASES
6121  |  RPE65  |  DISEASES
6121  |  RPE65  |  DISEASES
8787  |  RGS9  |  DISEASES
27130  |  INVS  |  DISEASES
9837  |  GINS1  |  DISEASES
83394  |  PITPNM3  |  DISEASES
10325  |  RRAGB  |  DISEASES
7089  |  TLE2  |  DISEASES
10133  |  OPTN  |  DISEASES
5264  |  PHYH  |  DISEASES
7290  |  HIRA  |  DISEASES
3553  |  IL1B  |  DISEASES
5582  |  PRKCG  |  DISEASES
10714  |  POLD3  |  DISEASES
8850  |  KAT2B  |  DISEASES
7301  |  TYRO3  |  DISEASES
84708  |  LNX1  |  DISEASES
23301  |  EHBP1  |  DISEASES
11181  |  TREH  |  DISEASES
54431  |  DNAJC10  |  DISEASES
79644  |  SRD5A3  |  DISEASES
9486  |  CHST10  |  DISEASES
51602  |  NOP58  |  DISEASES
8916  |  HERC3  |  DISEASES
8452  |  CUL3  |  DISEASES
7840  |  ALMS1  |  DISEASES
2247  |  FGF2  |  DISEASES
55212  |  BBS7  |  DISEASES
55081  |  IFT57  |  DISEASES
10686  |  CLDN16  |  DISEASES
131890  |  GRK7  |  DISEASES
131890  |  GRK7  |  DISEASES
1767  |  DNAH5  |  DISEASES
1950  |  EGF  |  DISEASES
11112  |  HIBADH  |  DISEASES
793  |  CALB1  |  DISEASES
4547  |  MTTP  |  DISEASES
4986  |  OPRK1  |  DISEASES
54806  |  AHI1  |  DISEASES
54806  |  AHI1  |  DISEASES
4885  |  NPTX2  |  DISEASES
4885  |  NPTX2  |  DISEASES
399979  |  SNX19  |  DISEASES
53904  |  MYO3A  |  DISEASES
53904  |  MYO3A  |  DISEASES
9044  |  BTAF1  |  DISEASES
9044  |  BTAF1  |  DISEASES
24148  |  PRPF6  |  DISEASES
7078  |  TIMP3  |  DISEASES
7078  |  TIMP3  |  DISEASES
5149  |  PDE6H  |  DISEASES
5149  |  PDE6H  |  DISEASES
6895  |  TARBP2  |  DISEASES
145226  |  RDH12  |  DISEASES
145226  |  RDH12  |  DISEASES
9321  |  TRIP11  |  DISEASES
10099  |  TSPAN3  |  DISEASES
585  |  BBS4  |  DISEASES
6017  |  RLBP1  |  DISEASES
6017  |  RLBP1  |  DISEASES
5373  |  PMM2  |  DISEASES
9785  |  DHX38  |  DISEASES
5636  |  PRPSAP2  |  DISEASES
114799  |  ESCO1  |  DISEASES
396  |  ARHGDIA  |  DISEASES
1762  |  DMWD  |  DISEASES
6205  |  RPS11  |  DISEASES
4209  |  MEF2D  |  DISEASES
10899  |  JTB  |  DISEASES
51542  |  VPS54  |  DISEASES
9381  |  OTOF  |  DISEASES
1261  |  CNGA3  |  DISEASES
1261  |  CNGA3  |  DISEASES
151230  |  KLHL23  |  DISEASES
151230  |  KLHL23  |  DISEASES
6508  |  SLC4A3  |  DISEASES
10550  |  ARL6IP5  |  DISEASES
9515  |  STXBP5L  |  DISEASES
6167  |  RPL37  |  DISEASES
142685  |  ASB15  |  DISEASES
5127  |  CDK16  |  DISEASES
56548  |  CHST7  |  DISEASES
9258  |  MFHAS1  |  DISEASES
123  |  PLIN2  |  DISEASES
123  |  PLIN2  |  DISEASES
55327  |  LIN7C  |  DISEASES
726  |  CAPN5  |  DISEASES
6094  |  ROM1  |  DISEASES
6094  |  ROM1  |  DISEASES
22897  |  CEP164  |  DISEASES
219854  |  TMEM218  |  DISEASES
196463  |  PLBD2  |  DISEASES
7069  |  THRSP  |  DISEASES
202559  |  KHDRBS2  |  DISEASES
7082  |  TJP1  |  DISEASES
60558  |  GUF1  |  DISEASES
60558  |  GUF1  |  DISEASES
57724  |  EPG5  |  DISEASES
5495  |  PPM1B  |  DISEASES
651  |  BMP3  |  DISEASES
170692  |  ADAMTS18  |  DISEASES
170692  |  ADAMTS18  |  DISEASES
1070  |  CETN3  |  DISEASES
22934  |  RPIA  |  DISEASES
22934  |  RPIA  |  DISEASES
8526  |  DGKE  |  DISEASES
7070  |  THY1  |  DISEASES
1525  |  CXADR  |  DISEASES
4645  |  MYO5B  |  DISEASES
760  |  CA2  |  DISEASES
5018  |  OXA1L  |  DISEASES
145483  |  FAM161B  |  DISEASES
157657  |  C8orf37  |  DISEASES
157657  |  C8orf37  |  DISEASES
6156  |  RPL30  |  DISEASES
5147  |  PDE6D  |  DISEASES
5147  |  PDE6D  |  DISEASES
26060  |  APPL1  |  DISEASES
9162  |  DGKI  |  DISEASES
6781  |  STC1  |  DISEASES
873  |  CBR1  |  DISEASES
57369  |  GJD2  |  DISEASES
7307  |  U2AF1  |  DISEASES
84988  |  PPP1R16A  |  DISEASES
1173  |  AP2M1  |  DISEASES
5130  |  PCYT1A  |  DISEASES
1742  |  DLG4  |  DISEASES
30812  |  SOX8  |  DISEASES
4760  |  NEUROD1  |  DISEASES
4760  |  NEUROD1  |  DISEASES
129880  |  BBS5  |  DISEASES
129880  |  BBS5  |  DISEASES
10461  |  MERTK  |  DISEASES
10461  |  MERTK  |  DISEASES
56983  |  POGLUT1  |  DISEASES
3490  |  IGFBP7  |  DISEASES
9497  |  SLC4A7  |  DISEASES
166336  |  PRICKLE2  |  DISEASES
8820  |  HESX1  |  DISEASES
51304  |  ZDHHC3  |  DISEASES
54585  |  LZTFL1  |  DISEASES
55764  |  IFT122  |  DISEASES
6010  |  RHO  |  DISEASES
6010  |  RHO  |  DISEASES
149461  |  CLDN19  |  DISEASES
8927  |  BSN  |  DISEASES
80155  |  NAA15  |  DISEASES
11157  |  LSM6  |  DISEASES
9265  |  CYTH3  |  DISEASES
6100  |  RP9  |  DISEASES
168667  |  BMPER  |  DISEASES
222962  |  SLC29A4  |  DISEASES
25798  |  BRI3  |  DISEASES
25962  |  KIAA1429  |  DISEASES
79937  |  CNTNAP3  |  DISEASES
55172  |  DNAAF2  |  DISEASES
23093  |  TTLL5  |  DISEASES
9317  |  PTER  |  DISEASES
121643  |  FOXN4  |  DISEASES
3419  |  IDH3A  |  DISEASES
6866  |  TAC3  |  DISEASES
4130  |  MAP1A  |  DISEASES
2793  |  GNGT2  |  DISEASES
2793  |  GNGT2  |  DISEASES
51117  |  COQ4  |  DISEASES
93210  |  PGAP3  |  DISEASES
762  |  CA4  |  DISEASES
4218  |  RAB8A  |  DISEASES
10476  |  ATP5H  |  DISEASES
284110  |  GSDMA  |  DISEASES
3960  |  LGALS4  |  DISEASES
56890  |  MDM1  |  DISEASES
7343  |  UBTF  |  DISEASES
253959  |  RALGAPA1  |  DISEASES
116984  |  ARAP2  |  DISEASES
6203  |  RPS9  |  DISEASES
3308  |  HSPA4  |  DISEASES
6870  |  TACR3  |  DISEASES
2339  |  FNTA  |  DISEASES
6869  |  TACR1  |  DISEASES
165215  |  FAM171B  |  DISEASES
10114  |  HIPK3  |  DISEASES
10594  |  PRPF8  |  DISEASES
51362  |  CDC40  |  DISEASES
440533  |  PSG8  |  DISEASES
7275  |  TUB  |  DISEASES
7275  |  TUB  |  DISEASES
115861  |  NXNL1  |  DISEASES
7399  |  USH2A  |  DISEASES
7399  |  USH2A  |  DISEASES
378  |  ARF4  |  DISEASES
2353  |  FOS  |  DISEASES
7569  |  ZNF182  |  DISEASES
7386  |  UQCRFS1  |  DISEASES
54910  |  SEMA4C  |  DISEASES
1501  |  CTNND2  |  DISEASES
4632  |  MYL1  |  DISEASES
10474  |  TADA3  |  DISEASES
6137  |  RPL13  |  DISEASES
2752  |  GLUL  |  DISEASES
389524  |  GTF2IRD2B  |  DISEASES
57124  |  CD248  |  DISEASES
64446  |  DNAI2  |  DISEASES
89866  |  SEC16B  |  DISEASES
2147  |  F2  |  DISEASES
741  |  ZNHIT2  |  DISEASES
29984  |  RHOD  |  DISEASES
29766  |  TMOD3  |  DISEASES
54715  |  RBFOX1  |  DISEASES
6138  |  RPL15  |  DISEASES
79797  |  ZNF408  |  DISEASES
55320  |  MIS18BP1  |  DISEASES
8815  |  BANF1  |  DISEASES
6670  |  SP3  |  DISEASES
79884  |  MAP9  |  DISEASES
79884  |  MAP9  |  DISEASES
27235  |  COQ2  |  DISEASES
6208  |  RPS14  |  DISEASES
836  |  CASP3  |  DISEASES
9657  |  IQCB1  |  DISEASES
9657  |  IQCB1  |  DISEASES
407  |  ARR3  |  DISEASES
407  |  ARR3  |  DISEASES
1488  |  CTBP2  |  DISEASES
5771  |  PTPN2  |  DISEASES
26986  |  PABPC1  |  DISEASES
4117  |  MAK  |  DISEASES
4867  |  NPHP1  |  DISEASES
4867  |  NPHP1  |  DISEASES
80025  |  PANK2  |  DISEASES
54862  |  CC2D1A  |  DISEASES
25980  |  AAR2  |  DISEASES
51130  |  ASB3  |  DISEASES
10294  |  DNAJA2  |  DISEASES
57539  |  WDR35  |  DISEASES
283150  |  FOXR1  |  DISEASES
64837  |  KLC2  |  DISEASES
10692  |  RRH  |  DISEASES
1191  |  CLU  |  DISEASES
7592  |  ZNF41  |  DISEASES
9129  |  PRPF3  |  DISEASES
7566  |  ZNF18  |  DISEASES
5191  |  PEX7  |  DISEASES
1310  |  COL19A1  |  DISEASES
9229  |  DLGAP1  |  DISEASES
54714  |  CNGB3  |  DISEASES
54714  |  CNGB3  |  DISEASES
23020  |  SNRNP200  |  DISEASES
23020  |  SNRNP200  |  DISEASES
10464  |  PIBF1  |  DISEASES
63973  |  NEUROG2  |  DISEASES
120103  |  SLC36A4  |  DISEASES
582  |  BBS1  |  DISEASES
26155  |  NOC2L  |  DISEASES
8939  |  FUBP3  |  DISEASES
55603  |  FAM46A  |  DISEASES
130557  |  ZNF513  |  DISEASES
23621  |  BACE1  |  DISEASES
23621  |  BACE1  |  DISEASES
166379  |  BBS12  |  DISEASES
26526  |  TSPAN16  |  DISEASES
124590  |  USH1G  |  DISEASES
84179  |  MFSD7  |  DISEASES
54943  |  DNAJC28  |  DISEASES
6863  |  TAC1  |  DISEASES
149830  |  PRNT  |  DISEASES
3615  |  IMPDH2  |  DISEASES
134957  |  STXBP5  |  DISEASES
23350  |  U2SURP  |  DISEASES
10160  |  FARP1  |  DISEASES
51010  |  EXOSC3  |  DISEASES
10615  |  SPAG5  |  DISEASES
282809  |  POC1B  |  DISEASES
282809  |  POC1B  |  DISEASES
148109  |  FAM187B  |  DISEASES
8100  |  IFT88  |  DISEASES
9282  |  MED14  |  DISEASES
26061  |  HACL1  |  DISEASES
26121  |  PRPF31  |  DISEASES
283518  |  KCNRG  |  DISEASES
4642  |  MYO1D  |  DISEASES
2932  |  GSK3B  |  DISEASES
80031  |  SEMA6D  |  DISEASES
57010  |  CABP4  |  DISEASES
55892  |  MYNN  |  DISEASES
3590  |  IL11RA  |  DISEASES
161882  |  ZFPM1  |  DISEASES
94101  |  ORMDL1  |  DISEASES
9792  |  SERTAD2  |  DISEASES
80821  |  DDHD1  |  DISEASES
56478  |  EIF4ENIF1  |  DISEASES
5148  |  PDE6G  |  DISEASES
5148  |  PDE6G  |  DISEASES
9364  |  RAB28  |  DISEASES
9364  |  RAB28  |  DISEASES
147719  |  LYPD4  |  DISEASES
83733  |  SLC25A18  |  DISEASES
7401  |  CLRN1  |  DISEASES
1915  |  EEF1A1  |  DISEASES
283869  |  NPW  |  DISEASES
277  |  AMY1B  |  DISEASES
8701  |  DNAH11  |  DISEASES
201475  |  RAB12  |  DISEASES
5727  |  PTCH1  |  DISEASES
25901  |  CCDC28A  |  DISEASES
80311  |  KLHL15  |  DISEASES
388939  |  C2orf71  |  DISEASES
388939  |  C2orf71  |  DISEASES
2689  |  GH2  |  DISEASES
113612  |  CYP2U1  |  DISEASES
1769  |  DNAH8  |  DISEASES
340075  |  ARSI  |  DISEASES
51004  |  COQ6  |  DISEASES
388531  |  RGS9BP  |  DISEASES
5204  |  PFDN5  |  DISEASES
84068  |  SLC10A7  |  DISEASES
25794  |  FSCN2  |  DISEASES
25794  |  FSCN2  |  DISEASES
344658  |  SAMD7  |  DISEASES
55589  |  BMP2K  |  DISEASES
6011  |  GRK1  |  DISEASES
6011  |  GRK1  |  DISEASES
283149  |  BCL9L  |  DISEASES
1174  |  AP1S1  |  DISEASES
3842  |  TNPO1  |  DISEASES
468  |  ATF4  |  DISEASES
5357  |  PLS1  |  DISEASES
1058  |  CENPA  |  DISEASES
9094  |  UNC119  |  DISEASES
9094  |  UNC119  |  DISEASES
9227  |  LRAT  |  DISEASES
9227  |  LRAT  |  DISEASES
8409  |  UXT  |  DISEASES
64359  |  NXN  |  DISEASES
1641  |  DCX  |  DISEASES
139212  |  PIH1D3  |  DISEASES
143098  |  MPP7  |  DISEASES
57701  |  NCKAP5L  |  DISEASES
51263  |  MRPL30  |  DISEASES
55205  |  ZNF532  |  DISEASES
6622  |  SNCA  |  DISEASES
6809  |  STX3  |  DISEASES
28968  |  SLC6A16  |  DISEASES
27031  |  NPHP3  |  DISEASES
64682  |  ANAPC1  |  DISEASES
23275  |  POFUT2  |  DISEASES
6129  |  RPL7  |  DISEASES
51315  |  KRCC1  |  DISEASES
60506  |  NYX  |  DISEASES
5493  |  PPL  |  DISEASES
4128  |  MAOA  |  DISEASES
2709  |  GJB5  |  DISEASES
347344  |  ZNF81  |  DISEASES
375298  |  CERKL  |  DISEASES
375298  |  CERKL  |  DISEASES
84419  |  C15orf48  |  DISEASES
55171  |  TBCCD1  |  DISEASES
51513  |  ETV7  |  DISEASES
6187  |  RPS2  |  DISEASES
5132  |  PDC  |  DISEASES
148398  |  SAMD11  |  DISEASES
55975  |  KLHL7  |  DISEASES
284415  |  VSTM1  |  DISEASES
390259  |  BSX  |  DISEASES
8481  |  OFD1  |  DISEASES
8481  |  OFD1  |  DISEASES
755  |  C21orf2  |  DISEASES
755  |  C21orf2  |  DISEASES
55972  |  SLC25A40  |  DISEASES
84747  |  UNC119B  |  DISEASES
56479  |  KCNQ5  |  DISEASES
3614  |  IMPDH1  |  DISEASES
89790  |  SIGLEC10  |  DISEASES
347148  |  QRFP  |  DISEASES
54788  |  DNAJB12  |  DISEASES
6122  |  RPL3  |  DISEASES
6050  |  RNH1  |  DISEASES
7267  |  TTC3  |  DISEASES
133584  |  EGFLAM  |  DISEASES
4635  |  MYL4  |  DISEASES
64218  |  SEMA4A  |  DISEASES
64218  |  SEMA4A  |  DISEASES
8650  |  NUMB  |  DISEASES
3792  |  KEL  |  DISEASES
55750  |  AGK  |  DISEASES
2202  |  EFEMP1  |  DISEASES
5979  |  RET  |  DISEASES
54766  |  BTG4  |  DISEASES
4649  |  MYO9A  |  DISEASES
200734  |  SPRED2  |  DISEASES
9600  |  PITPNM1  |  DISEASES
9600  |  PITPNM1  |  DISEASES
26507  |  CNNM1  |  DISEASES
92359  |  CRB3  |  DISEASES
2980  |  GUCA2A  |  DISEASES
7323  |  UBE2D3  |  DISEASES
60  |  ACTB  |  DISEASES
51125  |  GOLGA7  |  DISEASES
1121  |  CHM  |  DISEASES
10987  |  COPS5  |  DISEASES
90410  |  IFT20  |  DISEASES
1524  |  CX3CR1  |  DISEASES
131873  |  COL6A6  |  DISEASES
157680  |  VPS13B  |  DISEASES
84735  |  CNDP1  |  DISEASES
56980  |  PRDM10  |  DISEASES
5980  |  REV3L  |  DISEASES
7415  |  VCP  |  DISEASES
57162  |  PELI1  |  DISEASES
5995  |  RGR  |  DISEASES
126014  |  OSCAR  |  DISEASES
171392  |  ZNF675  |  DISEASES
1201  |  CLN3  |  DISEASES
6427  |  SRSF2  |  DISEASES
79947  |  DHDDS  |  DISEASES
60509  |  AGBL5  |  DISEASES
343171  |  OR2W3  |  DISEASES
10210  |  TOPORS  |  DISEASES
8662  |  EIF3B  |  DISEASES
8662  |  EIF3B  |  DISEASES
8532  |  CPZ  |  DISEASES
4519  |  MT-CYB  |  DISEASES
2475  |  MTOR  |  DISEASES
676  |  BRDT  |  DISEASES
4508  |  MT-ATP6  |  DISEASES
4508  |  MT-ATP6  |  DISEASES
4541  |  MT-ND6  |  DISEASES
23139  |  MAST2  |  DISEASES
4976  |  OPA1  |  DISEASES
9760  |  TOX  |  DISEASES
1756  |  DMD  |  DISEASES
65217  |  PCDH15  |  DISEASES
4538  |  MT-ND4  |  DISEASES
779  |  CACNA1S  |  DISEASES
23038  |  WDTC1  |  DISEASES
1270  |  CNTF  |  DISEASES
10806  |  SDCCAG8  |  DISEASES
23596  |  OPN3  |  DISEASES
6905  |  TBCE  |  DISEASES
7257  |  TSNAX  |  DISEASES
142  |  PARP1  |  DISEASES
28982  |  FLVCR1  |  DISEASES
4751  |  NEK2  |  DISEASES
343035  |  RD3  |  DISEASES
343035  |  RD3  |  DISEASES
5362  |  PLXNA2  |  DISEASES
722  |  C4BPA  |  DISEASES
6993  |  DYNLT1  |  DISEASES
56995  |  TULP4  |  DISEASES
84947  |  SERAC1  |  DISEASES
163486  |  DENND1B  |  DISEASES
23418  |  CRB1  |  DISEASES
23418  |  CRB1  |  DISEASES
2165  |  F13B  |  DISEASES
6004  |  RGS16  |  DISEASES
10767  |  HBS1L  |  DISEASES
22926  |  ATF6  |  DISEASES
84134  |  TOMM40L  |  DISEASES
3766  |  KCNJ10  |  DISEASES
3766  |  KCNJ10  |  DISEASES
1382  |  CRABP2  |  DISEASES
10763  |  NES  |  DISEASES
4942  |  OAT  |  DISEASES
246269  |  LACE1  |  DISEASES
11231  |  SEC63  |  DISEASES
56957  |  OTUD7B  |  DISEASES
25957  |  PNISR  |  DISEASES
9659  |  PDE4DIP  |  DISEASES
4803  |  NGF  |  DISEASES
4354  |  MPP1  |  DISEASES
6785  |  ELOVL4  |  DISEASES
6785  |  ELOVL4  |  DISEASES
167691  |  LCA5  |  DISEASES
167691  |  LCA5  |  DISEASES
2773  |  GNAI3  |  DISEASES
54805  |  CNNM2  |  DISEASES
2652  |  OPN1MW  |  DISEASES
3617  |  IMPG1  |  DISEASES
3617  |  IMPG1  |  DISEASES
5956  |  OPN1LW  |  DISEASES
5956  |  OPN1LW  |  DISEASES
278  |  AMY1C  |  DISEASES
276  |  AMY1A  |  DISEASES
118427  |  OLFM3  |  DISEASES
81621  |  KAZALD1  |  DISEASES
79955  |  PDZD7  |  DISEASES
24  |  ABCA4  |  DISEASES
24  |  ABCA4  |  DISEASES
79627  |  OGFRL1  |  DISEASES
60682  |  SMAP1  |  DISEASES
2258  |  FGF13  |  DISEASES
51557  |  LGSN  |  DISEASES
401265  |  KLHL31  |  DISEASES
29929  |  ALG6  |  DISEASES
1791  |  DNTT  |  DISEASES
221391  |  OPN5  |  DISEASES
5146  |  PDE6C  |  DISEASES
5146  |  PDE6C  |  DISEASES
202500  |  TCTE1  |  DISEASES
6342  |  SCP2  |  DISEASES
55624  |  POMGNT1  |  DISEASES
6130  |  RPL7A  |  DISEASES
94233  |  OPN4  |  DISEASES
92211  |  CDHR1  |  DISEASES
92211  |  CDHR1  |  DISEASES
23404  |  EXOSC2  |  DISEASES
9533  |  POLR1C  |  DISEASES
79717  |  PPCS  |  DISEASES
80712  |  ESX1  |  DISEASES
1759  |  DNM1  |  DISEASES
27095  |  TRAPPC3  |  DISEASES
6865  |  TACR2  |  DISEASES
8565  |  YARS  |  DISEASES
79140  |  CCDC28B  |  DISEASES
286204  |  CRB2  |  DISEASES
222658  |  KCTD20  |  DISEASES
1104  |  RCC1  |  DISEASES
1104  |  RCC1  |  DISEASES
474354  |  LRRC18  |  DISEASES
9128  |  PRPF4  |  DISEASES
7295  |  TXN  |  DISEASES
6015  |  RING1  |  DISEASES
19  |  ABCA1  |  DISEASES
494513  |  DFNB59  |  DISEASES
494513  |  DFNB59  |  DISEASES
8859  |  STK19  |  DISEASES
6499  |  SKIV2L  |  DISEASES
4958  |  OMD  |  DISEASES
158046  |  NXNL2  |  DISEASES
199  |  AIF1  |  DISEASES
778  |  CACNA1F  |  DISEASES
778  |  CACNA1F  |  DISEASES
4007  |  PRICKLE3  |  DISEASES
7546  |  ZIC2  |  DISEASES
7088  |  TLE1  |  DISEASES
26090  |  ABHD12  |  DISEASES
26090  |  ABHD12  |  DISEASES
84131  |  CEP78  |  DISEASES
84131  |  CEP78  |  DISEASES
955  |  ENTPD6  |  DISEASES
6668  |  SP2  |  DISEASES
4943  |  TBC1D25  |  DISEASES
5611  |  DNAJC3  |  DISEASES
11166  |  SOX21  |  DISEASES
26504  |  CNNM4  |  DISEASES
10529  |  NEBL  |  DISEASES
64802  |  NMNAT1  |  DISEASES
64802  |  NMNAT1  |  DISEASES
8340  |  HIST1H2BL  |  DISEASES
728577  |  CNTNAP3B  |  DISEASES
285641  |  SLC36A3  |  DISEASES
23177  |  CEP68  |  DISEASES
4129  |  MAOB  |  DISEASES
8516  |  ITGA8  |  DISEASES
8514  |  KCNAB2  |  DISEASES
261734  |  NPHP4  |  DISEASES
261734  |  NPHP4  |  DISEASES
10159  |  ATP6AP2  |  DISEASES
6103  |  RPGR  |  DISEASES
6103  |  RPGR  |  DISEASES
84912  |  SLC35B4  |  DISEASES
8406  |  SRPX  |  DISEASES
6990  |  DYNLT3  |  DISEASES
1536  |  CYBB  |  DISEASES
2782  |  GNB1  |  DISEASES
2782  |  GNB1  |  DISEASES
7504  |  XK  |  DISEASES
2098  |  ESD  |  DISEASES
11127  |  KIF3A  |  DISEASES
285440  |  CYP4V2  |  DISEASES
5422  |  POLA1  |  DISEASES
5080  |  PAX6  |  DISEASES
254158  |  CXorf58  |  DISEASES
254173  |  TTLL10  |  DISEASES
1906  |  EDN1  |  DISEASES
22944  |  KIN  |  DISEASES
138050  |  HGSNAT  |  DISEASES
3801  |  KIFC3  |  DISEASES
1059  |  CENPB  |  DISEASES
23322  |  RPGRIP1L  |  DISEASES
6247  |  RS1  |  DISEASES
54875  |  CNTLN  |  DISEASES
123016  |  TTC8  |  DISEASES
265  |  AMELX  |  DISEASES
11168  |  PSIP1  |  DISEASES
3420  |  IDH3B  |  DISEASES
8777  |  MPDZ  |  DISEASES
10283  |  CWC27  |  DISEASES
23746  |  AIPL1  |  DISEASES
23746  |  AIPL1  |  DISEASES
8908  |  GYG2  |  DISEASES
9946  |  CRYZL1  |  DISEASES
137868  |  SGCZ  |  DISEASES
169522  |  KCNV2  |  DISEASES
94137  |  RP1L1  |  DISEASES
94137  |  RP1L1  |  DISEASES
27201  |  GPR78  |  DISEASES
5888  |  RAD51  |  DISEASES
93589  |  CACNA2D4  |  DISEASES
93589  |  CACNA2D4  |  DISEASES
2706  |  GJB2  |  DISEASES
6545  |  SLC7A4  |  DISEASES
91050  |  CCDC149  |  DISEASES
91050  |  CCDC149  |  DISEASES
11340  |  EXOSC8  |  DISEASES
29844  |  TFPT  |  DISEASES
23521  |  RPL13A  |  DISEASES
147700  |  KLC3  |  DISEASES
83636  |  C19orf12  |  DISEASES
6397  |  SEC14L1  |  DISEASES
3993  |  LLGL2  |  DISEASES
51559  |  NT5DC3  |  DISEASES
143187  |  VTI1A  |  DISEASES
54903  |  MKS1  |  DISEASES
79738  |  BBS10  |  DISEASES
338699  |  ANKRD42  |  DISEASES
55812  |  SPATA7  |  DISEASES
55812  |  SPATA7  |  DISEASES
116985  |  ARAP1  |  DISEASES
64333  |  ARHGAP9  |  DISEASES
9801  |  MRPL19  |  DISEASES
285331  |  CCDC66  |  DISEASES
285331  |  CCDC66  |  DISEASES
7784  |  ZP3  |  DISEASES
11158  |  RABL2B  |  DISEASES
79924  |  ADM2  |  DISEASES
831  |  CAST  |  DISEASES
7920  |  ABHD16A  |  DISEASES
10117  |  ENAM  |  DISEASES
6161  |  RPL32  |  DISEASES
4901  |  NRL  |  DISEASES
4901  |  NRL  |  DISEASES
7289  |  TULP3  |  DISEASES
23259  |  DDHD2  |  DISEASES
11190  |  CEP250  |  DISEASES
55174  |  INTS10  |  DISEASES
23426  |  GRIP1  |  DISEASES
594857  |  NPS  |  DISEASES
4905  |  NSF  |  DISEASES
4356  |  MPP3  |  DISEASES
6314  |  ATXN7  |  DISEASES
6314  |  ATXN7  |  DISEASES
56099  |  PCDHGB7  |  DISEASES
64072  |  CDH23  |  DISEASES
54890  |  ALKBH5  |  DISEASES
57728  |  WDR19  |  DISEASES
57728  |  WDR19  |  DISEASES
57096  |  RPGRIP1  |  DISEASES
57096  |  RPGRIP1  |  DISEASES
100287898  |  TTC34  |  DISEASES
9612  |  NCOR2  |  DISEASES
1259  |  CNGA1  |  DISEASES
1120  |  CHKB  |  DISEASES
3098  |  HK1  |  DISEASES
9699  |  RIMS2  |  DISEASES
60489  |  APOBEC3G  |  DISEASES
60489  |  APOBEC3G  |  DISEASES
84140  |  FAM161A  |  DISEASES
84140  |  FAM161A  |  DISEASES
84163  |  GTF2IRD2  |  DISEASES
3238  |  HOXD12  |  DISEASES
5670  |  PSG2  |  DISEASES
3778  |  KCNMA1  |  DISEASES
7018  |  TF  |  DISEASES
2570  |  GABRR2  |  DISEASES
4647  |  MYO7A  |  DISEASES
4647  |  MYO7A  |  DISEASES
6295  |  SAG  |  DISEASES
152789  |  JAKMIP1  |  DISEASES
501  |  ALDH7A1  |  DISEASES
501  |  ALDH7A1  |  DISEASES
3267  |  AGFG1  |  DISEASES
54619  |  CCNJ  |  DISEASES
9805  |  SCRN1  |  DISEASES
388336  |  SHISA6  |  DISEASES
6336  |  SCN10A  |  DISEASES
136371  |  ASB10  |  DISEASES
83552  |  MFRP  |  DISEASES
83552  |  MFRP  |  DISEASES
10903  |  MTMR11  |  DISEASES
9343  |  EFTUD2  |  DISEASES
11020  |  IFT27  |  DISEASES
11020  |  IFT27  |  DISEASES
85458  |  DIXDC1  |  DISEASES
643376  |  BTBD18  |  DISEASES
8031  |  NCOA4  |  DISEASES
734  |  OSGIN2  |  DISEASES
57511  |  COG6  |  DISEASES
57511  |  COG6  |  DISEASES
757  |  TMEM50B  |  DISEASES
4696  |  NDUFA3  |  DISEASES
57545  |  CC2D2A  |  DISEASES
7124  |  TNF  |  DISEASES
3491  |  CYR61  |  DISEASES
3109  |  HLA-DMB  |  DISEASES
7439  |  BEST1  |  DISEASES
55611  |  OTUB1  |  DISEASES
266727  |  MDGA1  |  DISEASES
5923  |  RASGRF1  |  DISEASES
9742  |  IFT140  |  DISEASES
5830  |  PEX5  |  DISEASES
10908  |  PNPLA6  |  DISEASES
10540  |  DCTN2  |  DISEASES
2668  |  GDNF  |  DISEASES
834  |  CASP1  |  DISEASES
55591  |  VEZT  |  DISEASES
57579  |  FAM135A  |  DISEASES
3586  |  IL10  |  DISEASES
2569  |  GABRR1  |  DISEASES
2569  |  GABRR1  |  DISEASES
627  |  BDNF  |  DISEASES
5635  |  PRPSAP1  |  DISEASES
3831  |  KLC1  |  DISEASES
8842  |  PROM1  |  DISEASES
8842  |  PROM1  |  DISEASES
55652  |  SLC48A1  |  DISEASES
407738  |  FAM19A1  |  DISEASES
374308  |  PTCHD3  |  DISEASES
5528  |  PPP2R5D  |  DISEASES
8754  |  ADAM9  |  DISEASES
30816  |  ERVW-1  |  DISEASES
5158  |  PDE6B  |  DISEASES
150590  |  C2orf15  |  DISEASES
6949  |  TCOF1  |  DISEASES
80745  |  THUMPD2  |  DISEASES
100506742  |  CASP12  |  DISEASES
346007  |  EYS  |  DISEASES
346007  |  EYS  |  DISEASES
139628  |  FOXR2  |  DISEASES
22999  |  RIMS1  |  DISEASES
22999  |  RIMS1  |  DISEASES
10424  |  PGRMC2  |  DISEASES
157848  |  NKX6-3  |  DISEASES
55819  |  RNF130  |  DISEASES
79776  |  ZFHX4  |  DISEASES
9791  |  PTDSS1  |  DISEASES
92482  |  BBIP1  |  DISEASES
6188  |  RPS3  |  DISEASES
4190  |  MDH1  |  DISEASES
401505  |  TOMM5  |  DISEASES
9414  |  TJP2  |  DISEASES
441864  |  TARM1  |  DISEASES
6141  |  RPL18  |  DISEASES
8972  |  MGAM  |  DISEASES
8825  |  LIN7A  |  DISEASES
1649  |  DDIT3  |  DISEASES
80184  |  CEP290  |  DISEASES
80184  |  CEP290  |  DISEASES
10490  |  VTI1B  |  DISEASES
29957  |  SLC25A24  |  DISEASES
10896  |  OCLM  |  DISEASES
29115  |  SAP30BP  |  DISEASES
4946  |  OAZ1  |  DISEASES
768206  |  PRCD  |  DISEASES
8153  |  RND2  |  DISEASES
6223  |  RPS19  |  DISEASES
200959  |  GABRR3  |  DISEASES
728558  |  ENTPD1-AS1  |  DISEASES
100506343  |  FAM212B-AS1  |  DISEASES
104326057  |  GACAT1  |  DISEASES
104797537  |  GACAT3  |  DISEASES
594842  |  HAS2-AS1  |  DISEASES
283902  |  HCCAT5  |  DISEASES
101927813  |  HMMR-AS1  |  DISEASES
221883  |  HOXA11-AS  |  DISEASES
100287569  |  LINC00173  |  DISEASES
29931  |  LINC00312  |  DISEASES
414243  |  LINC00595  |  DISEASES
100506930  |  LINC00665  |  DISEASES
151877  |  MAGI1-IT1  |  DISEASES
4566  |  MT-TK  |  DISEASES
4567  |  MT-TL1  |  DISEASES
4575  |  MT-TS2  |  DISEASES
4578  |  MT-TW  |  DISEASES
25859  |  PART1  |  DISEASES
283104  |  SBF2-AS1  |  DISEASES
286002  |  SLC26A4-AS1  |  DISEASES
677833  |  SNORA54  |  DISEASES
400128  |  TUSC8  |  DISEASES
101929665  |  UBE2R2-AS1  |  DISEASES
652995  |  UCA1  |  DISEASES
51352  |  WT1-AS  |  DISEASES
Locus(Waiting for update.)
Disease ID 629
Disease cone-rod dystrophy
Integrated Phenotype
HPO | Name(Total Integrated Phenotypes:3)
HP:0001133  |  Depressed visual field
HP:0000662  |  Poor night vision
HP:0000510  |  Retinitis pigmentosa
Text Mined Phenotype
HPO | Name | Sentences' Count(Total Phenotypes:9)
HP:0100255  |  Metaphyseal dysplasia  |  6
HP:0002657  |  Spondylometaphyseal dysplasia  |  6
HP:0000705  |  Amelogenesis imperfecta  |  3
HP:0000618  |  Blindness  |  2
HP:0000545  |  Near sightedness  |  2
HP:0011003  |  High myopia  |  1
HP:0000572  |  Visual loss  |  1
HP:0010834  |  Trophic changes  |  1
HP:0001513  |  Obesity  |  1
Disease ID 629
Disease cone-rod dystrophy
Manually Symptom(Waiting for update.)
Text Mined Symptom(Waiting for update.)
Manually Genotype(Total Text Mining Genotypes:0)
(Waiting for update.)
All Snps(Total Genotypes:178)
snpId pubmedId geneId geneSymbol diseaseId sourceId sentence score Year geneSymbol_dbSNP CHROMOSOME POS REF ALT
rs104893768256975366010RHOumls:C0035334BeFreeTo find an optimal pharmacological treatment for rhodopsin-associated retinitis pigmentosa, we performed two cell-based HTSs with mammalian cells expressing the P23H rod opsin mutant and identified two sets of novel compounds for further validation and characterization.0.4645570812015RHO3129528801CA
rs10489376814189976010RHOumls:C0035334BeFreeWe inserted into the germline of mice either a mutant or wild-type allele from a patient with retinitis pigmentosa and a missense mutation (P23H) in the rhodopsin gene.0.4645570811992RHO3129528801CA
rs104893768177153416010RHOumls:C0035334BeFreeTo elucidate the molecular mechanisms underlying the light-sensitive retinal degeneration caused by the rhodopsin mutation P23H, which causes retinitis pigmentosa (RP) in humans, we expressed Xenopus laevis, bovine, human, and murine forms of P23H rhodopsin in transgenic X. laevis rod photoreceptors.0.4645570812007RHO3129528801CA
rs104893768193259386010RHOumls:C0035334BeFreeSearch for a correlation between telomere length and severity of retinitis pigmentosa due to the dominant rhodopsin Pro23His mutation.0.4645570812009RHO3129528801CA
rs104893768208050326010RHOumls:C0035334BeFreeRetinobenzaldehydes as proper-trafficking inducers of folding-defective P23H rhodopsin mutant responsible for retinitis pigmentosa.0.4645570812010RHO3129528801CA
rs1048937681512616810594PRPF8umls:C0035334BeFreeHistologic study of retinitis pigmentosa due to a mutation in the RP13 gene (PRPC8): comparison with rhodopsin Pro23His, Cys110Arg, and Glu181Lys.0.1327974942004RHO3129528801CA
rs104893768151261686010RHOumls:C0035334BeFreeHistologic study of retinitis pigmentosa due to a mutation in the RP13 gene (PRPC8): comparison with rhodopsin Pro23His, Cys110Arg, and Glu181Lys.0.4645570812004RHO3129528801CA
rs104893768121400486010RHOumls:C0035334BeFreeHistopathologic study of variation in severity of retinitis pigmentosa due to the dominant rhodopsin mutation Pro23His.0.4645570812002RHO3129528801CA
rs10489376876016416010RHOumls:C0035334BeFreePatients with retinitis pigmentosa and the pro-23-his rhodopsin mutation had a decrease in the gain of activation.0.4645570811995RHO3129528801CA
rs104893769256375226010RHOumls:C0035334BeFreeWe observed similar vacuolization in outer segments of transgenic mice expressing human rhodopsin with a T17M mutation (hT17M), suggesting that the mechanism responsible for the degenerative process in mice expressing the non-glycosylated rhodopsin and the RHO(hT17M) mice is likely the cause of phenotype observed in retinitis pigmentosa patients carrying T17M mutation.0.4645570812015RHO3129528783CT
rs104893769252748136010RHOumls:C0035334BeFreePhotoactivation-induced instability of rhodopsin mutants T4K and T17M in rod outer segments underlies retinal degeneration in X. laevis transgenic models of retinitis pigmentosa.0.4645570812015RHO3129528783CT
rs104893769245733206010RHOumls:C0035334BeFreeRetinitis pigmentosa‑associated rhodopsin mutant T17M induces endoplasmic reticulum (ER) stress and sensitizes cells to ER stress-induced cell death.0.4645570812014RHO3129528783CT
rs104893773110941746010RHOumls:C0035334BeFreeThe Gly106Arg mutation of the rhodopsin gene has been found in Japanese patients with sectorial retinitis pigmentosa.0.4645570812000RHO3129529049GA,T
rs104893774155488066010RHOumls:C0035334BeFreeGenotype-phenotype correlation in a family with Arg135Leu rhodopsin retinitis pigmentosa.0.4645570812004RHO3129530918GA,T
rs104893775NA6010RHOumls:C0035334CLINVARNA0.464557081NARHO3129530917CT
rs104893779190853856010RHOumls:C0035334BeFreeTo phenotype a family with RHO (Asp190Asn or D190N) dominantly inherited retinitis pigmentosa (RP) and to describe an approach to surveying affected families.0.4645570812008RHO3129532288GA,T
rs104893779236259266010RHOumls:C0035334BeFreeThermal stability of rhodopsin and progression of retinitis pigmentosa: comparison of S186W and D190N rhodopsin mutants.0.4645570812013RHO3129532288GA,T
rs10489378192282426010RHOumls:C0035334BeFreeOur results suggest that the Pro-267-Leu rhodopsin mutation is associated with a very mild phenotype of retinitis pigmentosa.0.4645570811997RHO3129532636CT
rs104893786NA6010RHOumls:C0035334CLINVARNA0.464557081NARHO3129528777AG
rs104894082128828126101RP1umls:C0035334BeFreeDe novo mutation in the RP1 gene (Arg677ter) associated with retinitis pigmentosa.0.2713626192003RP1854625911CT
rs104894373110788525959RDH5umls:C0035334BeFreeHis mother had the Arg280His mutation and his father had the Val177Gly mutation, but his father's aunt who has typical retinitis pigmentosa had the wild type RDH5 gene.0.0038101182000RDH5;BLOC1S1-RDH51255721908TG
rs104894459127962494901NRLumls:C0035334BeFreePhenotype of retinitis pigmentosa associated with the Ser50Thr mutation in the NRL gene.0.3690870652003NRL1424082701AT
rs10489447017389517145226RDH12umls:C0035334BeFreeThe retinal disease in persons with RDH12 mutations in the homozygous (p.G127X, p.Q189X, p.Y226C, p.A269GfsX1, and p.L274P) or compound heterozygous state (p.R65X/p.A269GfsX1, p.H151D/p.T155I, p.H151D/p.A269GfsX1) was diagnosed initially as Leber congenital amaurosis (LCA) or early-onset retinitis pigmentosa.0.366177152007RDH121467727097CT
rs10489447417389517145226RDH12umls:C0035334BeFreeThe retinal disease in persons with RDH12 mutations in the homozygous (p.G127X, p.Q189X, p.Y226C, p.A269GfsX1, and p.L274P) or compound heterozygous state (p.R65X/p.A269GfsX1, p.H151D/p.T155I, p.H151D/p.A269GfsX1) was diagnosed initially as Leber congenital amaurosis (LCA) or early-onset retinitis pigmentosa.0.366177152007RDH121467726086GT
rs10489447517389517145226RDH12umls:C0035334BeFreeThe retinal disease in persons with RDH12 mutations in the homozygous (p.G127X, p.Q189X, p.Y226C, p.A269GfsX1, and p.L274P) or compound heterozygous state (p.R65X/p.A269GfsX1, p.H151D/p.T155I, p.H151D/p.A269GfsX1) was diagnosed initially as Leber congenital amaurosis (LCA) or early-onset retinitis pigmentosa.0.366177152007RDH121467726983CA,G
rs10489455915295099762CA4umls:C0035334BeFreeIn collaboration with scientists at the University of Cape Town (Rondebosch, South Africa), we recently showed that the R14W mutation in the signal sequence of CA IV, which they identified in patients with the retinitis pigmentosa (RP) 17 form of autosomal dominant RP, results in accumulation of unfolded protein in the endoplasmic reticulum (ER), leading to ER stress, the unfolded protein response, and apoptosis in a large fraction of transfected COS-7 cells expressing mutant, but not wild-type, CA IV.0.1270773522004CA41760150074CT
rs104894671109670371406CRXumls:C0035334BeFreeTwo point mutations of Crx, R41W and E80A, that cause cone-rod dystrophy in humans and lie within the homeodomain but outside the NLS did not disrupt the nuclear localization of Crx protein, but a R90W mutation of Crx that causes human Leber congenital amaurosis (LCA) and resides within the NLS resulted in the fusion protein localized in both nuclei and cytoplasm in majority (51% to 69%) of the transfected cells.0.4891530792000CRX1947836381AC
rs104894672128199821406CRXumls:C0035334BeFreeA heterozygous Arg41Trp mutation in the CRX gene can produce cone-rod dystrophy in Japanese patients.0.4891530792003CRX1947836263CT
rs104894672109670371406CRXumls:C0035334BeFreeTwo point mutations of Crx, R41W and E80A, that cause cone-rod dystrophy in humans and lie within the homeodomain but outside the NLS did not disrupt the nuclear localization of Crx protein, but a R90W mutation of Crx that causes human Leber congenital amaurosis (LCA) and resides within the NLS resulted in the fusion protein localized in both nuclei and cytoplasm in majority (51% to 69%) of the transfected cells.0.4891530792000CRX1947836263CT
rs104894673109670371406CRXumls:C0035334BeFreeTwo point mutations of Crx, R41W and E80A, that cause cone-rod dystrophy in humans and lie within the homeodomain but outside the NLS did not disrupt the nuclear localization of Crx protein, but a R90W mutation of Crx that causes human Leber congenital amaurosis (LCA) and resides within the NLS resulted in the fusion protein localized in both nuclei and cytoplasm in majority (51% to 69%) of the transfected cells.0.4891530792000CRX1947839335CT
rs104894673245164011406CRXumls:C0035334BeFreeR90W mice carry a substitution mutation in the CRX homeodomain, Arg90Trp, which is associated with dominant mild late-onset CoRD and recessive LCA.0.4891530792013CRX1947839335CT
rs118031911NA6101RP1umls:C0035334CLINVARNA0.271362619NARP1854629679CT
rs121434241203094039129PRPF3umls:C0035334BeFreeTo characterize the clinical, psychophysical, and electrophysiological phenotypes in a five-generation Swiss family with dominantly inherited retinitis pigmentosa caused by a T494M mutation in the Precursor mRNA-Processing factor 3 (PRPF3) gene, and to relate the phenotype to the underlying genetic mutation.0.1259915842010PRPF31150344216CT
rs12143433717389517145226RDH12umls:C0035334BeFreeThe retinal disease in persons with RDH12 mutations in the homozygous (p.G127X, p.Q189X, p.Y226C, p.A269GfsX1, and p.L274P) or compound heterozygous state (p.R65X/p.A269GfsX1, p.H151D/p.T155I, p.H151D/p.A269GfsX1) was diagnosed initially as Leber congenital amaurosis (LCA) or early-onset retinitis pigmentosa.0.366177152007RDH121467726996CT
rs121434631234720982978GUCA1Aumls:C0035334BeFreeRNAi-mediated gene suppression in a GCAP1(L151F) cone-rod dystrophy mouse model.0.0032573022013GUCA1A642179248CG,T
rs121909076NA7287TULP1umls:C0035334CLINVARNA0.247805801NATULP1635503816AG
rs12190939815708351375298CERKLumls:C0035334BeFreeFurthermore, we propose that the cause for retinitis pigmentosa in patients bearing the CERKL R257X mutation might be the accumulation of a truncated CERKL protein in the nucleus.0.1264485922005CERKL2181558617GC,A
rs121912550158515763614IMPDH1umls:C0035334BeFreeScreen of the IMPDH1 gene among patients with dominant retinitis pigmentosa and clinical features associated with the most common mutation, Asp226Asn.0.2623514982005IMPDH17128398557CT
rs121917745NA6121RPE65umls:C0035334CLINVARNA0.372711618NARPE65168429835GA
rs121917849117549177274TTPAumls:C0035334BeFreeTo discuss the clinicopathological findings in a patient with retinitis pigmentosa (RP) accompanied by a vitamin E deficiency caused by an H101Q mutation in the alpha-tocopherol transfer protein (alpha-TTP) gene.0.1216286512001TTPA863072990AC
rs121917849120396607274TTPAumls:C0035334BeFreeAVED caused by the 744 del A could be distinguished by head titubation, lower frequency of the neuropathy and slower disease progression, decreased visual activity and retinitis pigmentosa, which has also been associated with a His(101) Gln missense mutation in the alpha-TTP gene.0.1216286512002TTPA863072990AC
rs121918581NA5158PDE6Bumls:C0035334CLINVARNA0.451096779NAPDE6B;LOC1027252004662188CT
rs121918582170440145158PDE6Bumls:C0035334BeFreeIndividuals with CSNB in the Rambusch pedigree were found to carry the H258N allele of PDE6B (MIM
180072); a similar mutation was not found in RP patients.0.4510967792007PDE6B;LOC1019285214653912CA
rs137853903155050302979GUCA1Bumls:C0035334BeFreeIndividual patients with atypical or recessive retinitis pigmentosa (RP) had additional heterozygous GCAP1-T114I and GCAP2 gene changes (V85M and F150C) of unknown pathogenicity.0.2434527992004GUCA1B642188686CT
rs137853903155050302978GUCA1Aumls:C0035334BeFreeIndividual patients with atypical or recessive retinitis pigmentosa (RP) had additional heterozygous GCAP1-T114I and GCAP2 gene changes (V85M and F150C) of unknown pathogenicity.0.0032573022004GUCA1B642188686CT
rs139185976106271335961PRPH2umls:C0035334BeFreeWe found three different unreported mutations 689delT, 857del17, corresponding to two macular dystrophy families and G208D in a retinitis pigmentosa (RP) family giving us a proportion of about 20% of RDS mutations in autosomal dominant Spanish macular dystrophies and 3% in ADRP.0.2601501691998PRPH2642704570CT
rs13918597610627133123PLIN2umls:C0035334BeFreeWe found three different unreported mutations 689delT, 857del17, corresponding to two macular dystrophy families and G208D in a retinitis pigmentosa (RP) family giving us a proportion of about 20% of RDS mutations in autosomal dominant Spanish macular dystrophies and 3% in ADRP.0.0029957921998PRPH2642704570CT
rs144738703NA26121PRPF31umls:C0035334CLINVARNA0.279773436NAPRPF311954123836CA,G,T
rs147394623252553644117MAKumls:C0035334BeFreeWe screened 275 North American patients with recessive/isolate retinitis pigmentosa for two mutations: an Alu insertion in the MAK gene and the p.Lys42Glu missense in the DHDDS gene.0.2413572092014DHDDS126438228AG
rs1473946232525536457538ALPK3umls:C0035334BeFreeWe screened 275 North American patients with recessive/isolate retinitis pigmentosa for two mutations: an Alu insertion in the MAK gene and the p.Lys42Glu missense in the DHDDS gene.0.0008143262014DHDDS126438228AG
rs1473946232407870979947DHDDSumls:C0035334BeFreeWe observed a characteristic shortening of plasma and urinary dolichols in retinitis pigmentosa (RP) patients carrying K42E and T206A mutations in the dehydrodolichol diphosphate synthase (DHDDS) gene, using liquid chromatography-mass spectrometry.0.1205428842014DHDDS126438228AG
rs1473946232525536479947DHDDSumls:C0035334BeFreeWe screened 275 North American patients with recessive/isolate retinitis pigmentosa for two mutations: an Alu insertion in the MAK gene and the p.Lys42Glu missense in the DHDDS gene.0.1205428842014DHDDS126438228AG
rs147620225173350014901NRLumls:C0035334BeFreeThe p.P67S (c.199C>T) and p.L235F (c.703C>T) variations in NRL do not appear to directly cause retinitis pigmentosa, while p.E63K (c.187G>A), p.A76V (c.227C>T), p.G122E (c.365G>A), and p.H125Q (c.375C>G) are of uncertain significance.0.3690870652007NRL1424082662CT
rs149921817173350014901NRLumls:C0035334BeFreeThe p.P67S (c.199C>T) and p.L235F (c.703C>T) variations in NRL do not appear to directly cause retinitis pigmentosa, while p.E63K (c.187G>A), p.A76V (c.227C>T), p.G122E (c.365G>A), and p.H125Q (c.375C>G) are of uncertain significance.0.3690870652007NRL1424082622GA
rs183589498NA346007EYSumls:C0035334CLINVARNA0.369987267NAEYS663720822AG
rs18999326125783483343171OR2W3umls:C0035334BeFreeAfter a pipeline of database filtering, including public databases and in-house databases, a novel missense mutation, c. 424 C > T transition (p.R142W) in OR2W3 gene, was identified as a potentially causative mutation for autosomal dominant RP.0.0002714422015OR2W31247896010CT
rs199691910173350014901NRLumls:C0035334BeFreeThe p.P67S (c.199C>T) and p.L235F (c.703C>T) variations in NRL do not appear to directly cause retinitis pigmentosa, while p.E63K (c.187G>A), p.A76V (c.227C>T), p.G122E (c.365G>A), and p.H125Q (c.375C>G) are of uncertain significance.0.3690870652007NRL1424082650GA
rs199867882NA50939IMPG2umls:C0035334CLINVARNA0.240271442NAIMPG23101231117GA
rs201358563173350014901NRLumls:C0035334BeFreeThe p.P67S (c.199C>T) and p.L235F (c.703C>T) variations in NRL do not appear to directly cause retinitis pigmentosa, while p.E63K (c.187G>A), p.A76V (c.227C>T), p.G122E (c.365G>A), and p.H125Q (c.375C>G) are of uncertain significance.0.3690870652007NRL1424081247GA
rs201493928NA6101RP1umls:C0035334CLINVARNA0.271362619NARP1854625068CT
rs201527662NA7399USH2Aumls:C0035334CLINVARNA0.381527241NAUSH2A1216246592AC
rs201970559173350014901NRLumls:C0035334BeFreeThe p.P67S (c.199C>T) and p.L235F (c.703C>T) variations in NRL do not appear to directly cause retinitis pigmentosa, while p.E63K (c.187G>A), p.A76V (c.227C>T), p.G122E (c.365G>A), and p.H125Q (c.375C>G) are of uncertain significance.0.3690870652007NRL1424082474GC
rs202126574NA145226RDH12umls:C0035334CLINVARNA0.36617715NARDH121467726084CT
rs26760669020398886388939C2orf71umls:C0035334BeFreeTwo mutations were found in C2ORF71 in human RP patients: A nonsense mutation (p.W253X) in the first exon is likely to be a null allele; the second, a missense mutation (p.I201F) within a highly conserved region of the protein, leads to proteosomal degradation.0.2408143262010C2orf71;LOC105374385229073661TA
rs2893398993269426017RLBP1umls:C0035334UNIPROTMutation of the gene encoding cellular retinaldehyde-binding protein in autosomal recessive retinitis pigmentosa.0.366177151997NANANANANA
rs2893968293905631406CRXumls:C0035334UNIPROTCone-rod dystrophy due to mutations in a novel photoreceptor-specific homeobox gene (CRX) essential for maintenance of the photoreceptor.0.4891530791997NANANANANA
rs2894031317389517145226RDH12umls:C0035334BeFreeThe retinal disease in persons with RDH12 mutations in the homozygous (p.G127X, p.Q189X, p.Y226C, p.A269GfsX1, and p.L274P) or compound heterozygous state (p.R65X/p.A269GfsX1, p.H151D/p.T155I, p.H151D/p.A269GfsX1) was diagnosed initially as Leber congenital amaurosis (LCA) or early-onset retinitis pigmentosa.0.366177152007ZFYVE26;RDH121467729209AG
rs29001566222170316010RHOumls:C0035334BeFreeAssociation of p.P347L in the rhodopsin gene with early-onset cystoid macular edema in patients with retinitis pigmentosa.0.4645570812012RHO3129533711CA,G,T
rs2900156620211726010RHOumls:C0035334BeFreeThis mutation, detected in leukocyte DNA, corresponds to a substitution of leucine for proline in amino acid 347 of the rhodopsin protein, and, therefore, we designated this form of retinitis pigmentosa as rhodopsin, proline-347-leucine.0.4645570811991RHO3129533711CA,G,T
rs2900163789430806010RHOumls:C0035334BeFreeTo explore the pathogenic mechanism of dominant mutations affecting the carboxyl terminus of rhodopsin that cause retinitis pigmentosa, we generated five lines of transgenic mice carrying the proline-347 to serine (P347S) mutation.0.4645570811996RHO3129533710CT
rs369588426150072395959RDH5umls:C0035334BeFreeA novel homozygous Gly107Arg mutation in the RDH5 gene in a Japanese patient with fundus albipunctatus with sectorial retinitis pigmentosa.0.0038101182004BLOC1S1;RDH5;BLOC1S1-RDH51255719191GA
rs372989281NA7439BEST1umls:C0035334CLINVARNA0.240542884NABEST11161958194CT
rs377269054NA94137RP1L1umls:C0035334CLINVARNA0.120271442NARP1L1810622967GA
rs3879069802504474557728WDR19umls:C0035334BeFreeThe phenotype associated with homozygous p.Arg106ProPOC1B may thus be highly variable, analogous to homozygous p.Leu710Ser in WDR19 causing either isolated retinitis pigmentosa or Jeune syndrome.0.0005428842014WDR19439231943TC
rs390659161806995630PRPHumls:C0035334BeFreePeripherin/RDS gene polymorphisms (Glu304Gln and Gly338Asp) were found in Indonesian patients with retinitis pigmentosa.0.0038001862005PRPH2642698426GC
rs397518039NA7399USH2Aumls:C0035334CLINVARNA0.381527241NAUSH2A1215877882TC
rs434102161806995630PRPHumls:C0035334BeFreePeripherin/RDS gene polymorphisms (Glu304Gln and Gly338Asp) were found in Indonesian patients with retinitis pigmentosa.0.0038001862005PRPH2642698323TA,C,G
rs527236055NA388939C2orf71umls:C0035334CLINVARNA0.240814326NAC2orf71;LOC105374385229072136C-
rs527236056NA388939C2orf71umls:C0035334CLINVARNA0.240814326NAC2orf71;LOC105374385229071273-G
rs527236060NA1258CNGB1umls:C0035334CLINVARNA0.362638474NACNGB11657964482CT,G
rs527236061NA1258CNGB1umls:C0035334CLINVARNA0.362638474NACNGB11657904843-T
rs527236062NA1406CRXumls:C0035334CLINVARNA0.489153079NACRX1947836335GC
rs527236063NA1406CRXumls:C0035334CLINVARNA0.489153079NACRX1947839964GC
rs527236064NA346007EYSumls:C0035334CLINVARNA0.369987267NAEYS663778111CT
rs527236065NA346007EYSumls:C0035334CLINVARNA0.369987267NAEYS664590909-T
rs527236066NA346007EYSumls:C0035334CLINVARNA0.369987267NAEYS663762613CT
rs527236067NA346007EYSumls:C0035334CLINVARNA0.369987267NAEYS663721226GT
rs527236068NA346007EYSumls:C0035334CLINVARNA0.369987267NAEYS664081870CT,G
rs527236069NA346007EYSumls:C0035334CLINVARNA0.369987267NAEYS663984390A-
rs527236070NA346007EYSumls:C0035334CLINVARNA0.369987267NAEYS663721651-TGCA
rs527236071NA346007EYSumls:C0035334CLINVARNA0.369987267NAEYS664590664AC-
rs527236072NA346007EYSumls:C0035334CLINVARNA0.369987267NAEYS665334996CT,A
rs527236073NA346007EYSumls:C0035334CLINVARNA0.369987267NAEYS664591464-CCTCTTGA
rs527236074NA346007EYSumls:C0035334CLINVARNA0.369987267NAEYS664590853GA
rs527236075NA346007EYSumls:C0035334CLINVARNA0.369987267NAEYS664591480T-
rs527236076NA346007EYSumls:C0035334CLINVARNA0.369987267NAEYS663762520AT
rs527236077NA346007EYSumls:C0035334CLINVARNA0.369987267NAEYS665353572TA
rs527236078NA346007EYSumls:C0035334CLINVARNA0.369987267NAEYS663788134T-
rs527236079NA9227LRATumls:C0035334CLINVARNA0.242367032NALRAT4154744489CT
rs527236080NA4117MAKumls:C0035334CLINVARNA0.241357209NAMAK610803830CT
rs527236081NA4117MAKumls:C0035334CLINVARNA0.241357209NAMAK610803887GA
rs527236082NA4117MAKumls:C0035334CLINVARNA0.241357209NAMAK610813661-C
rs527236083NA10461MERTKumls:C0035334CLINVARNA0.367262917NAMERTK2111929283A-
rs527236084NA10461MERTKumls:C0035334CLINVARNA0.367262917NAMERTK2111994404GA
rs527236085NA4647MYO7Aumls:C0035334CLINVARNA0.122171535NAMYO7A1177162965GT
rs527236086NA10002NR2E3umls:C0035334CLINVARNA0.253907006NANR2E31571811969CT
rs527236087NA4901NRLumls:C0035334CLINVARNA0.369087065NANRL1424082826A-
rs527236088NA5158PDE6Bumls:C0035334CLINVARNA0.451096779NAPDE6B4660603TA
rs527236089NA5158PDE6Bumls:C0035334CLINVARNA0.451096779NAPDE6B4659018GC
rs527236090NA5158PDE6Bumls:C0035334CLINVARNA0.451096779NAPDE6B;LOC1019285214655939GC
rs527236091NA5158PDE6Bumls:C0035334CLINVARNA0.451096779NAPDE6B4660575GA
rs527236094NA26121PRPF31umls:C0035334CLINVARNA0.279773436NAPRPF311954123783GT
rs527236095NA26121PRPF31umls:C0035334CLINVARNA0.279773436NAPRPF311954124565AT
rs527236096NA24148PRPF6umls:C0035334CLINVARNA0.240271442NAPRPF62063995027GC
rs527236097NA5961PRPH2umls:C0035334CLINVARNA0.260150169NAPRPH2642721925CT
rs527236098NA5961PRPH2umls:C0035334CLINVARNA0.260150169NAPRPH2642721836CT
rs527236099NA145226RDH12umls:C0035334CLINVARNA0.36617715NAZFYVE26;RDH121467729308G-
rs527236100NA6010RHOumls:C0035334CLINVARNA0.464557081NARHO3129532282GA
rs527236101NA6010RHOumls:C0035334CLINVARNA0.464557081NARHO3129528913CA
rs527236102NA6010RHOumls:C0035334CLINVARNA0.464557081NARHO3129533648ACCC-
rs527236103NA6010RHOumls:C0035334CLINVARNA0.464557081NARHO3129531034GA
rs527236104NA6094ROM1umls:C0035334CLINVARNA0.244267125NAROM1;EML31162613612-G
rs527236105NA6101RP1umls:C0035334CLINVARNA0.271362619NARP1854622150G-
rs527236106NA6101RP1umls:C0035334CLINVARNA0.271362619NARP1854628758GA
rs527236107NA94137RP1L1umls:C0035334CLINVARNA0.120271442NARP1L1810612126GA
rs527236108NA6103RPGRumls:C0035334CLINVARNA0.418185333NARPGRX38287018CA
rs527236109NA6103RPGRumls:C0035334CLINVARNA0.418185333NARPGRX38299113-CTAC
rs527236111NA6103RPGRumls:C0035334CLINVARNA0.418185333NARPGRX38304674AA-
rs527236112NA6103RPGRumls:C0035334CLINVARNA0.418185333NARPGRX38304647CG
rs527236113NA23020SNRNP200umls:C0035334CLINVARNA0.241085767NASNRNP200296293090CT
rs527236114NA23020SNRNP200umls:C0035334CLINVARNA0.241085767NASNRNP200296293085CA
rs527236115NA23020SNRNP200umls:C0035334CLINVARNA0.241085767NASNRNP200296293481CT
rs527236116NA10210TOPORSumls:C0035334CLINVARNA0.247815732NATOPORS932541968TCTC-
rs527236117NA7287TULP1umls:C0035334CLINVARNA0.247805801NATULP1635511648CT
rs527236118NA7399USH2Aumls:C0035334CLINVARNA0.381527241NAUSH2A1215799114AG
rs527236119NA7399USH2Aumls:C0035334CLINVARNA0.381527241NAUSH2A1215782779TG,C
rs527236120NA7399USH2Aumls:C0035334CLINVARNA0.381527241NAUSH2A1215867170C-
rs527236121NA7399USH2Aumls:C0035334CLINVARNA0.381527241NAUSH2A1216292292-TC
rs527236122NA7399USH2Aumls:C0035334CLINVARNA0.381527241NAUSH2A1215634523GC
rs527236123NA7399USH2Aumls:C0035334CLINVARNA0.381527241NAUSH2A1216418675CA
rs527236124NA7399USH2Aumls:C0035334CLINVARNA0.381527241NAUSH2A1215671258CA
rs527236125NA7399USH2Aumls:C0035334CLINVARNA0.381527241NAUSH2A1215648660CT
rs527236126NA7399USH2Aumls:C0035334CLINVARNA0.381527241NAUSH2A1215650692GA
rs527236127NA7399USH2Aumls:C0035334CLINVARNA0.381527241NAUSH2A1215674445CT
rs55958016NA7399USH2Aumls:C0035334CLINVARNA0.381527241NAUSH2A1216000489CA,G,T
rs61748441NA1406CRXumls:C0035334UNIPROTNA0.489153079NACRX1947839432GA
rs61748459126687631406CRXumls:C0035334BeFreeAs an example, we discover an unannotated Tf_Otx Pfam domain on the cone rod homeobox protein, which suggests a possible mechanism for how the V242M mutation on this protein causes cone-rod dystrophy.0.4891530792003CRX1947839791GA
rs6174845994272551406CRXumls:C0035334UNIPROTMutations in the cone-rod homeobox gene are associated with the cone-rod dystrophy photoreceptor degeneration.0.4891530791997CRX1947839791GA
rs61750172111354903000GUCY2Dumls:C0035334BeFreeAutosomal dominant cone-rod dystrophy due to a missense mutation (R838C) in the guanylate cyclase 2D gene (GUCY2D) with preserved rod function in one branch of the family.0.1308676062000GUCY2D178014700CA,T
rs61750172151759143000GUCY2Dumls:C0035334BeFreeAutosomal dominant cone-rod dystrophy with R838H and R838C mutations in the GUCY2D gene in Japanese patients.0.1308676062004GUCY2D178014700CA,T
rs61750172170415763000GUCY2Dumls:C0035334BeFreePhenotype of autosomal dominant cone-rod dystrophy due to the R838C mutation of the GUCY2D gene encoding retinal guanylate cyclase-1.0.1308676062007GUCY2D178014700CA,T
rs61750173250828855961PRPH2umls:C0035334BeFreePatients with pattern dystrophy (PD) were screened for mutations in PRPH2, BEST1, ELOVL4, CTRP5, and ABCA4; patients with cone-rod dystrophy (CRD) were screened for mutations in CRX, ABCA4, PRPH2, ELOVL4, and the c.2513G>A p.Arg838His variant in GUCY2D.0.2601501692014GUCY2D178014701GA
rs61750173250828856785ELOVL4umls:C0035334BeFreePatients with pattern dystrophy (PD) were screened for mutations in PRPH2, BEST1, ELOVL4, CTRP5, and ABCA4; patients with cone-rod dystrophy (CRD) were screened for mutations in CRX, ABCA4, PRPH2, ELOVL4, and the c.2513G>A p.Arg838His variant in GUCY2D.0.0035386762014GUCY2D178014701GA
rs6175017325082885114902C1QTNF5umls:C0035334BeFreePatients with pattern dystrophy (PD) were screened for mutations in PRPH2, BEST1, ELOVL4, CTRP5, and ABCA4; patients with cone-rod dystrophy (CRD) were screened for mutations in CRX, ABCA4, PRPH2, ELOVL4, and the c.2513G>A p.Arg838His variant in GUCY2D.0.0002714422014GUCY2D178014701GA
rs61750173151759143000GUCY2Dumls:C0035334BeFreeAutosomal dominant cone-rod dystrophy with R838H and R838C mutations in the GUCY2D gene in Japanese patients.0.1308676062004GUCY2D178014701GA
rs61750173250828853000GUCY2Dumls:C0035334BeFreeTIMP3 novel variants were found in two SFD patients, PRPH2 variants in 14 PD patients, ABCA4 variants in four PD patients, and p.Arg838His GUCY2D mutation in six patients diagnosed with dominant CRD; one patient additionally had a CRX VUS.0.1308676062014GUCY2D178014701GA
rs61750173250828851406CRXumls:C0035334BeFreeTIMP3 novel variants were found in two SFD patients, PRPH2 variants in 14 PD patients, ABCA4 variants in four PD patients, and p.Arg838His GUCY2D mutation in six patients diagnosed with dominant CRD; one patient additionally had a CRX VUS.0.4891530792014GUCY2D178014701GA
rs61751281NA6121RPE65umls:C0035334CLINVARNA0.372711618NARPE65168446837CT
rs6175577178256925961PRPH2umls:C0035334BeFreeA 46-year-old man with retinitis pigmentosa was found to have a heterozygous mutation in the peripherin/RDS gene (arginine-46-stop).0.2601501691995PRPH2642722199GA
rs61755798114857655630PRPHumls:C0035334BeFreeA novel mutation (Pro210Leu) of the peripherin/RDS gene has been found in one Japanese patient with retinitis pigmentosa.0.0038001862001PRPH2642704564GC,A
rs61755798114857655961PRPH2umls:C0035334BeFreeA novel mutation (Pro210Leu) of the peripherin/RDS gene has been found in one Japanese patient with retinitis pigmentosa.0.2601501692001PRPH2642704564GC,A
rs61755800180501335961PRPH2umls:C0035334BeFreeTo describe an Italian family in which two separate phenotypes (retinitis pigmentosa and adult onset vitelliform macular dystrophy) are associated with an identical mutation (S212G) in the peripherin/RDS gene.0.2601501692007PRPH2642704559TG,C
rs61755800180501335630PRPHumls:C0035334BeFreeTo describe an Italian family in which two separate phenotypes (retinitis pigmentosa and adult onset vitelliform macular dystrophy) are associated with an identical mutation (S212G) in the peripherin/RDS gene.0.0038001862007PRPH2642704559TG,C
rs6175581585408545630PRPHumls:C0035334BeFreeAutosomal dominant cone-rod dystrophy associated with mutations in codon 244 (Asn244His) and codon 184 (Tyr184Ser) of the peripherin/RDS gene.0.0038001861996PRPH2642704463TG
rs6175581585408545961PRPH2umls:C0035334BeFreeAutosomal dominant cone-rod dystrophy associated with mutations in codon 244 (Asn244His) and codon 184 (Tyr184Ser) of the peripherin/RDS gene.0.2601501691996PRPH2642704463TG
rs61755817NA5961PRPH2umls:C0035334CLINVARNA0.260150169NAPRPH2642704457AG
rs62638193110788525959RDH5umls:C0035334BeFreeHis mother had the Arg280His mutation and his father had the Val177Gly mutation, but his father's aunt who has typical retinitis pigmentosa had the wild type RDH5 gene.0.0038101182000RDH5;BLOC1S1-RDH51255724427GA,T
rs62638646NA6103RPGRumls:C0035334CLINVARNA0.418185333NARPGRX38318828CT
rs6264592685408545630PRPHumls:C0035334BeFreeAutosomal dominant cone-rod dystrophy associated with mutations in codon 244 (Asn244His) and codon 184 (Tyr184Ser) of the peripherin/RDS gene.0.0038001861996PRPH2642721784TG
rs6264592685408545961PRPH2umls:C0035334BeFreeAutosomal dominant cone-rod dystrophy associated with mutations in codon 244 (Asn244His) and codon 184 (Tyr184Ser) of the peripherin/RDS gene.0.2601501691996PRPH2642721784TG
rs6264593289129675961PRPH2umls:C0035334BeFreeAutosomal dominant cone-rod dystrophy associated with a Val200Glu mutation of the peripherin/RDS gene.0.2601501691996PRPH2642704594AT
rs6264593289129675630PRPHumls:C0035334BeFreeAutosomal dominant cone-rod dystrophy associated with a Val200Glu mutation of the peripherin/RDS gene.0.0038001861996PRPH2642704594AT
rs62645935249631625961PRPH2umls:C0035334BeFreeFinally, we demonstrate that the p.G266D retinitis pigmentosa mutation found within TM4 selectively abolishes the binding of peripherin-2 to rhodopsin.0.2601501692015PRPH2642704396CT
rs730882261NA6103RPGRumls:C0035334CLINVARNA0.418185333NARPGRX38286572CT-
rs779007169NA9742IFT140umls:C0035334CLINVARNA0.240271442NAIFT140161520177CG,T
rs80338902NA7399USH2Aumls:C0035334CLINVARNA0.381527241NAUSH2A1216247118CA
rs80338903NA7399USH2Aumls:C0035334CLINVARNA0.381527241NAUSH2A1216247095C-
rs80338904NA7399USH2Aumls:C0035334CLINVARNA0.381527241NAUSH2A1215671085TC
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