Human Gene FLNA (ENST00000369850.10_12) from GENCODE V47lift37
  Description: filamin A, transcript variant 2 (from RefSeq NM_001110556.2)
Gencode Transcript: ENST00000369850.10_12
Gencode Gene: ENSG00000196924.19_19
Transcript (Including UTRs)
   Position: hg19 chrX:153,576,899-153,603,002 Size: 26,104 Total Exon Count: 48 Strand: -
Coding Region
   Position: hg19 chrX:153,577,217-153,599,613 Size: 22,397 Coding Exon Count: 47 

Page IndexSequence and LinksUniProtKB CommentsPrimersMalaCardsCTD
Gene AllelesRNA-Seq ExpressionMicroarray ExpressionRNA StructureProtein StructureOther Species
GO AnnotationsmRNA DescriptionsPathwaysOther NamesGeneReviewsModel Information
Methods
Data last updated at UCSC: 2024-08-22 23:36:26

-  Sequence and Links to Tools and Databases
 
Genomic Sequence (chrX:153,576,899-153,603,002)mRNA (may differ from genome)Protein (2647 aa)
Gene SorterGenome BrowserOther Species FASTAVisiGeneGene interactionsTable Schema
AlphaFoldBioGPSEnsemblEntrez GeneExonPrimerGeneCards
HGNCMalacardsMGIOMIMPubMedReactome
UniProtKBWikipediaBioGrid CRISPR DB

-  Comments and Description Text from UniProtKB
  ID: FLNA_HUMAN
DESCRIPTION: RecName: Full=Filamin-A; Short=FLN-A; AltName: Full=Actin-binding protein 280; Short=ABP-280; AltName: Full=Alpha-filamin; AltName: Full=Endothelial actin-binding protein; AltName: Full=Filamin-1; AltName: Full=Non-muscle filamin;
FUNCTION: Promotes orthogonal branching of actin filaments and links actin filaments to membrane glycoproteins. Anchors various transmembrane proteins to the actin cytoskeleton and serves as a scaffold for a wide range of cytoplasmic signaling proteins. Interaction with FLNA may allow neuroblast migration from the ventricular zone into the cortical plate. Tethers cell surface- localized furin, modulates its rate of internalization and directs its intracellular trafficking (By similarity). Involved in ciliogenesis.
SUBUNIT: Interacts with PDLIM2 (By similarity). Homodimer. Interacts with FCGR1A, FLNB, FURIN, HSPB7, INPPL1, KCND2, MYOT, MYOZ1, ARHGAP24, PSEN1, PSEN2 and ECSCR. Interacts also with various other binding partners in addition to filamentous actin. Interacts (via N-terminus) with MIS18BP1 (via N-terminus). Interacts (via N-terminus) with TAF1B. Interacts with TMEM67 (via C-terminus) and MKS1.
INTERACTION: Q8N264:ARHGAP24; NbExp=6; IntAct=EBI-350432, EBI-988764; P46108:CRK; NbExp=2; IntAct=EBI-350432, EBI-886; O75369:FLNB; NbExp=5; IntAct=EBI-350432, EBI-352089; P62993:GRB2; NbExp=2; IntAct=EBI-350432, EBI-401755; P07228:ITGB1 (xeno); NbExp=2; IntAct=EBI-350432, EBI-5606437; P35372:OPRM1; NbExp=5; IntAct=EBI-350432, EBI-2624570;
SUBCELLULAR LOCATION: Cytoplasm, cell cortex. Cytoplasm, cytoskeleton.
TISSUE SPECIFICITY: Ubiquitous.
DOMAIN: Comprised of a NH2-terminal actin-binding domain, 24 immunoglobulin-like internally homologous repeats and two hinge regions. Repeat 24 and the second hinge domain are important for dimer formation.
PTM: Phosphorylated upon DNA damage, probably by ATM or ATR (By similarity). Phosphorylation extent changes in response to cell activation.
DISEASE: Defects in FLNA are the cause of periventricular nodular heterotopia type 1 (PVNH1) [MIM:300049]; also called nodular heterotopia, bilateral periventricular (NHBP or BPNH). PVNH is a developmental disorder characterized by the presence of periventricular nodules of cerebral gray matter, resulting from a failure of neurons to migrate normally from the lateral ventricular proliferative zone, where they are formed, to the cerebral cortex. PVNH1 is an X-linked dominant form. Heterozygous females have normal intelligence but suffer from seizures and various manifestations outside the central nervous system, especially related to the vascular system. Hemizygous affected males die in the prenatal or perinatal period.
DISEASE: Defects in FLNA are the cause of periventricular nodular heterotopia type 4 (PVNH4) [MIM:300537]; also known as periventricular heterotopia Ehlers-Danlos variant. PVNH4 is characterized by nodular brain heterotopia, joint hypermobility and development of aortic dilation in early adulthood.
DISEASE: Defects in FLNA are the cause of otopalatodigital syndrome type 1 (OPD1) [MIM:311300]. OPD1 is an X-linked dominant multiple congenital anomalies disease mainly characterized by a generalized skeletal dysplasia, mild mental retardation, hearing loss, cleft palate, and typical facial anomalies. OPD1 belongs to a group of X-linked skeletal dysplasias known as oto-palato- digital syndrome spectrum disorders that also include OPD2, Melnick-Needles syndrome (MNS), and frontometaphyseal dysplasia (FMD). Remodeling of the cytoskeleton is central to the modulation of cell shape and migration. FLNA is a widely expressed protein that regulates re-organization of the actin cytoskeleton by interacting with integrins, transmembrane receptor complexes and second messengers. Males with OPD1 have cleft palate, malformations of the ossicles causing deafness and milder bone and limb defects than those associated with OPD2. Obligate female carriers of mutations causing both OPD1 and OPD2 have variable (often milder) expression of a similar phenotypic spectrum.
DISEASE: Defects in FLNA are the cause of otopalatodigital syndrome type 2 (OPD2) [MIM:304120]; also known as cranioorodigital syndrome. OPD2 is a congenital bone disorder that is characterized by abnormally modeled, bowed bones, small or absent first digits and, more variably, cleft palate, posterior fossa brain anomalies, omphalocele and cardiac defects.
DISEASE: Defects in FLNA are the cause of frontometaphyseal dysplasia (FMD) [MIM:305620]. FMD is a congenital bone disease characterized by supraorbital hyperostosis, deafness and digital anomalies.
DISEASE: Defects in FLNA are the cause of Melnick-Needles syndrome (MNS) [MIM:309350]. MNS is a severe congenital bone disorder characterized by typical facies (exophthalmos, full cheeks, micrognathia and malalignment of teeth), flaring of the metaphyses of long bones, s-like curvature of bones of legs, irregular constrictions in the ribs, and sclerosis of base of skull.
DISEASE: Defects in FLNA are the cause of X-linked congenital idiopathic intestinal pseudoobstruction (CIIPX) [MIM:300048]. CIIPX is characterized by a severe abnormality of gastrointestinal motility due to primary qualitative defects of enteric ganglia and nerve fibers. Affected individuals manifest recurrent signs of intestinal obstruction in the absence of any mechanical lesion.
DISEASE: Defects in FLNA are the cause of FG syndrome type 2 (FGS2) [MIM:300321]. FG syndrome (FGS) is an X-linked disorder characterized by mental retardation, relative macrocephaly, hypotonia and constipation.
DISEASE: Defects in FLNA are the cause of terminal osseous dysplasia (TOD) [MIM:300244]. A rare X-linked dominant male-lethal disease characterized by skeletal dysplasia of the limbs, pigmentary defects of the skin and recurrent digital fibroma during infancy. A significant phenotypic variability is observed in affected females.
DISEASE: Defects in FLNA are the cause of cardiac valvular dysplasia X-linked (CVDX) [MIM:314400]. A rare X-linked heart disease characterized by mitral and/or aortic valve regurgitation. The histologic features include fragmentation of collagenous bundles within the valve fibrosa and accumulation of proteoglycans, which produces excessive valve tissue leading to billowing of the valve leaflets.
DISEASE: Note=Defects in FLNA may be a cause of macrothrombocytopenia, a disorder characterized by subnormal levels of blood platelets. Blood platelets are abonormally enlarged.
SIMILARITY: Belongs to the filamin family.
SIMILARITY: Contains 1 actin-binding domain.
SIMILARITY: Contains 2 CH (calponin-homology) domains.
SIMILARITY: Contains 24 filamin repeats.
SEQUENCE CAUTION: Sequence=BAC03408.2; Type=Erroneous initiation; Note=Translation N-terminally shortened;
WEB RESOURCE: Name=GeneReviews; URL="http://www.ncbi.nlm.nih.gov/sites/GeneTests/lab/gene/FLNA";

-  Primer design for this transcript
 

Primer3Plus can design qPCR Primers that straddle exon-exon-junctions, which amplify only cDNA, not genomic DNA.
Click here to load the transcript sequence and exon structure into Primer3Plus

Exonprimer can design one pair of Sanger sequencing primers around every exon, located in non-genic sequence.
Click here to open Exonprimer with this transcript

To design primers for a non-coding sequence, zoom to a region of interest and select from the drop-down menu: View > In External Tools > Primer3


-  MalaCards Disease Associations
  MalaCards Gene Search: FLNA
Diseases sorted by gene-association score: melnick-needles syndrome* (1713), heterotopia, periventricular* (1681), otopalatodigital syndrome, type i* (1650), otopalatodigital syndrome, type ii* (1650), cardiac valvular dysplasia, x-linked* (1580), terminal osseous dysplasia* (1378), intestinal pseudoobstruction, neuronal* (1369), fg syndrome 2* (1329), frontometaphyseal dysplasia 1* (1230), frontometaphyseal dysplasia* (912), moved to 300049* (750), otopalatodigital spectrum disorders* (619), flna-related periventricular nodular heterotopia* (519), cleft palate, isolated* (405), congenital short bowel syndrome* (267), ehlers-danlos syndrome, cardiac valvular form* (247), flna-related disorders* (100), flna-related x-linked cardiac valvular dysplasia* (100), otopalatodigital syndrome (41), constipation (18), keloid formation (17), foster-kennedy syndrome (16), pulmonary plasma cell granuloma (16), omphalocele (16), discharging ear (15), skeletal dysplasias (14), x-linked disease (13), short bowel syndrome (12), senile entropion (11), exophthalmos (10), mite infestation (9), vaginal discharge (9), primary optic atrophy (9), intestinal pseudo-obstruction (9), urethral calculus (9), skeletal tuberculosis (9), paraphimosis (9), intestinal obstruction (8), leech infestation (8), postmenopausal atrophic vaginitis (8), myopathy, myofibrillar, 5 (8), neuroretinitis (8), aicardi syndrome (8), parasitic ectoparasitic infectious disease (8), mongolian spot (7), skeletal dysplasia (7), taylor's syndrome (7), lichen nitidus (7), miliaria (7), chronic purulent otitis media (7), lower urinary tract calculus (6), schizotypal personality disorder (6), otomycosis (6), punctate palmoplantar keratoderma (6), hydrocephalus (6), cervix disease (6), atelosteogenesis (6), boomerang dysplasia (6), regular astigmatism (6), mental retardation, x-linked syndromic, lubs type (5), narcissistic personality disorder (5), glomangioma (5), breast abscess (5), spinal cord astrocytoma (5), cardiovascular organ benign neoplasm (5), benign perivascular tumor (5), vaginal disease (5), chronic dacryocystitis (5), shoulder impingement syndrome (5), hyperostosis (5), chronic inflammation of lacrimal passage (5), cervicitis (5), avoidant personality disorder (5), osteochondrodysplasia (5), subdural empyema (5), neuronal migration disorders (5), diphyllobothriasis (4), congenital nervous system abnormality (4), leukocoria (4), west syndrome (4), tricuspid valve stenosis (4), sed congenita (4), borjeson-forssman-lehmann syndrome (3), hajdu-cheney syndrome (3), physical disorder (1)
* = Manually curated disease association

-  Comparative Toxicogenomics Database (CTD)
  The following chemicals interact with this gene

+  Common Gene Haplotype Alleles
  Press "+" in the title bar above to open this section.

-  RNA-Seq Expression Data from GTEx (53 Tissues, 570 Donors)
  Highest median expression: 1712.88 RPKM in Artery - Tibial
Total median expression: 16613.47 RPKM



View in GTEx track of Genome Browser    View at GTEx portal     View GTEx Body Map

+  Microarray Expression Data
  Press "+" in the title bar above to open this section.

-  mRNA Secondary Structure of 3' and 5' UTRs
 
RegionFold EnergyBasesEnergy/Base
Display As
5' UTR -111.90245-0.457 Picture PostScript Text
3' UTR -116.60318-0.367 Picture PostScript Text

The RNAfold program from the Vienna RNA Package is used to perform the secondary structure predictions and folding calculations. The estimated folding energy is in kcal/mol. The more negative the energy, the more secondary structure the RNA is likely to have.

-  Protein Domain and Structure Information
  InterPro Domains: Graphical view of domain structure
IPR001589 - Actinin_actin-bd_CS
IPR001715 - CH-domain
IPR001298 - Filamin
IPR017868 - Filamin/ABP280_repeat-like
IPR013783 - Ig-like_fold
IPR014756 - Ig_E-set

Pfam Domains:
PF00307 - Calponin homology (CH) domain
PF00630 - Filamin/ABP280 repeat

SCOP Domains:
47576 - Calponin-homology domain, CH-domain
49373 - Invasin/intimin cell-adhesion fragments
81296 - E set domains
49309 - Transglutaminase, two C-terminal domains
141729 - FimD N-terminal domain-like
49785 - Galactose-binding domain-like
49863 - Hyaluronate lyase-like, C-terminal domain
55550 - SH2 domain

Protein Data Bank (PDB) 3-D Structure
MuPIT help
2AAV - NMR MuPIT 2BP3 - X-ray MuPIT 2BRQ - X-ray MuPIT 2J3S - X-ray MuPIT 2JF1 - X-ray MuPIT 2K3T - NMR MuPIT 2K7P - NMR MuPIT 2K7Q - NMR MuPIT 2W0P - X-ray MuPIT 2WFN - X-ray MuPIT 3CNK - X-ray MuPIT 3HOC - X-ray MuPIT 3HOP - X-ray MuPIT 3HOR - X-ray MuPIT 3ISW - X-ray MuPIT 3RGH - X-ray MuPIT


ModBase Predicted Comparative 3D Structure on P21333
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The pictures above may be empty if there is no ModBase structure for the protein. The ModBase structure frequently covers just a fragment of the protein. You may be asked to log onto ModBase the first time you click on the pictures. It is simplest after logging in to just click on the picture again to get to the specific info on that model.

-  Orthologous Genes in Other Species
  Orthologies between human, mouse, and rat are computed by taking the best BLASTP hit, and filtering out non-syntenic hits. For more distant species reciprocal-best BLASTP hits are used. Note that the absence of an ortholog in the table below may reflect incomplete annotations in the other species rather than a true absence of the orthologous gene.
MouseRatZebrafishD. melanogasterC. elegansS. cerevisiae
No orthologNo orthologNo orthologNo orthologNo orthologNo ortholog
Gene DetailsGene Details    
Gene SorterGene Sorter    
 RGD    
      
      

-  Gene Ontology (GO) Annotations with Structured Vocabulary
  Molecular Function:
GO:0001664 G-protein coupled receptor binding
GO:0003723 RNA binding
GO:0003779 actin binding
GO:0005515 protein binding
GO:0008134 transcription factor binding
GO:0015459 potassium channel regulator activity
GO:0017048 Rho GTPase binding
GO:0017160 Ral GTPase binding
GO:0019900 kinase binding
GO:0031267 small GTPase binding
GO:0031852 mu-type opioid receptor binding
GO:0034988 Fc-gamma receptor I complex binding
GO:0042803 protein homodimerization activity
GO:0044325 ion channel binding
GO:0044877 macromolecular complex binding
GO:0045296 cadherin binding
GO:0046332 SMAD binding
GO:0048365 Rac GTPase binding
GO:0051015 actin filament binding
GO:0051020 GTPase binding

Biological Process:
GO:0002576 platelet degranulation
GO:0007195 adenylate cyclase-inhibiting dopamine receptor signaling pathway
GO:0016479 negative regulation of transcription from RNA polymerase I promoter
GO:0021943 formation of radial glial scaffolds
GO:0021987 cerebral cortex development
GO:0030030 cell projection organization
GO:0030168 platelet activation
GO:0030334 regulation of cell migration
GO:0031532 actin cytoskeleton reorganization
GO:0032233 positive regulation of actin filament bundle assembly
GO:0034329 cell junction assembly
GO:0034394 protein localization to cell surface
GO:0042177 negative regulation of protein catabolic process
GO:0042789 mRNA transcription from RNA polymerase II promoter
GO:0043066 negative regulation of apoptotic process
GO:0043113 receptor clustering
GO:0043123 positive regulation of I-kappaB kinase/NF-kappaB signaling
GO:0043433 negative regulation of sequence-specific DNA binding transcription factor activity
GO:0044319 wound healing, spreading of cells
GO:0045184 establishment of protein localization
GO:0050821 protein stabilization
GO:0051220 cytoplasmic sequestering of protein
GO:0051764 actin crosslink formation
GO:0060271 cilium assembly
GO:0070527 platelet aggregation
GO:0071526 semaphorin-plexin signaling pathway
GO:0072659 protein localization to plasma membrane
GO:0090307 mitotic spindle assembly
GO:0097368 establishment of Sertoli cell barrier
GO:1900026 positive regulation of substrate adhesion-dependent cell spreading
GO:1901381 positive regulation of potassium ion transmembrane transport
GO:1902396 protein localization to bicellular tight junction
GO:1905000 regulation of membrane repolarization during atrial cardiac muscle cell action potential
GO:1905031 regulation of membrane repolarization during cardiac muscle cell action potential
GO:2000179 positive regulation of neural precursor cell proliferation
GO:2001046 positive regulation of integrin-mediated signaling pathway
GO:2001224 positive regulation of neuron migration

Cellular Component:
GO:0005576 extracellular region
GO:0005634 nucleus
GO:0005730 nucleolus
GO:0005737 cytoplasm
GO:0005829 cytosol
GO:0005856 cytoskeleton
GO:0005884 actin filament
GO:0005886 plasma membrane
GO:0005911 cell-cell junction
GO:0005925 focal adhesion
GO:0005938 cell cortex
GO:0015629 actin cytoskeleton
GO:0016020 membrane
GO:0030018 Z disc
GO:0030863 cortical cytoskeleton
GO:0031523 Myb complex
GO:0043025 neuronal cell body
GO:0043198 dendritic shaft
GO:0048471 perinuclear region of cytoplasm
GO:0070062 extracellular exosome
GO:0097440 apical dendrite
GO:0031941 filamentous actin


-  Descriptions from all associated GenBank mRNAs
  LF214070 - JP 2014500723-A/21573: Polycomb-Associated Non-Coding RNAs.
LF211538 - JP 2014500723-A/19041: Polycomb-Associated Non-Coding RNAs.
BC041179 - Homo sapiens, Similar to filamin C, gamma (actin binding protein 280), clone IMAGE:4152096, mRNA, partial cds.
AL050396 - Homo sapiens mRNA; cDNA DKFZp586K1720 (from clone DKFZp586K1720).
AK074048 - Homo sapiens mRNA for FLJ00119 protein.
GQ891316 - Homo sapiens clone HEL-S-39a epididymis secretory sperm binding protein mRNA, partial cds.
AB371579 - Homo sapiens FLNA mRNA for filamin A, splicing variant, complete cds, clone: HP00079-ARiS088J13.
AB371576 - Homo sapiens FLNA mRNA for filamin A, splicing variant, complete cds, clone: HP00079-ARi47G07.
AK090427 - Homo sapiens FLJ00343 mRNA for FLJ00343 protein.
BC014654 - Homo sapiens filamin A, alpha (actin binding protein 280), mRNA (cDNA clone IMAGE:4559790), complete cds.
AB371574 - Homo sapiens FLNA mRNA for filamin A, splicing variant, complete cds, clone: HP00079-ARi13C12.
BC028089 - Homo sapiens filamin A, alpha (actin binding protein 280), mRNA (cDNA clone IMAGE:4156935), with apparent retained intron.
AK300165 - Homo sapiens cDNA FLJ57890 complete cds, highly similar to Filamin-A.
AB191259 - Homo sapiens FLNA mRNA for filamin A, complete cds, clone: ARe06F05.
AB371575 - Homo sapiens FLNA mRNA for filamin A, splicing variant, complete cds, clone: HP00079-ARi37B09.
AB371577 - Homo sapiens FLNA mRNA for filamin A, splicing variant, complete cds, clone: HP00079-ARi50A09.
AB371578 - Homo sapiens FLNA mRNA for filamin A, splicing variant, complete cds, clone: HP00079-ARi66B08.
AB191260 - Homo sapiens FLNA mRNA for filamin A, complete cds, clone: ARe27E03.
AB593010 - Homo sapiens FLNA mRNA for filamin A, complete cds, clone: HP00079-RBdS070P22.
BC067111 - Homo sapiens filamin A, alpha (actin binding protein 280), mRNA (cDNA clone IMAGE:4800733), partial cds.
AL157419 - Homo sapiens mRNA; cDNA DKFZp434P031 (from clone DKFZp434P031).
GU727643 - Homo sapiens epididymis secretory sperm binding protein Li 190P mRNA, complete cds.
LF380839 - JP 2014500723-A/188342: Polycomb-Associated Non-Coding RNAs.
JD295148 - Sequence 276172 from Patent EP1572962.
X53416 - Human mRNA for actin-binding protein (filamin) (ABP-280).
AK304255 - Homo sapiens cDNA FLJ57038 complete cds, highly similar to Filamin-A.
JD338751 - Sequence 319775 from Patent EP1572962.
JD161044 - Sequence 142068 from Patent EP1572962.
JD129343 - Sequence 110367 from Patent EP1572962.
LF380840 - JP 2014500723-A/188343: Polycomb-Associated Non-Coding RNAs.
JD142045 - Sequence 123069 from Patent EP1572962.
JD120956 - Sequence 101980 from Patent EP1572962.
AB463042 - Synthetic construct DNA, clone: pF1KF0343, Homo sapiens FLNA gene for filamin A alpha, without stop codon, in Flexi system.
BC109289 - Homo sapiens filamin A, alpha (actin binding protein 280), mRNA (cDNA clone IMAGE:40034073), partial cds.
CU677081 - Synthetic construct Homo sapiens gateway clone IMAGE:100023476 5' read FLNA mRNA.
JD389256 - Sequence 370280 from Patent EP1572962.
JD389255 - Sequence 370279 from Patent EP1572962.
JD095332 - Sequence 76356 from Patent EP1572962.
JD040005 - Sequence 21029 from Patent EP1572962.
AK125630 - Homo sapiens cDNA FLJ43642 fis, clone STOMA2004925.
JD461232 - Sequence 442256 from Patent EP1572962.
MA449647 - JP 2018138019-A/21573: Polycomb-Associated Non-Coding RNAs.
MA447115 - JP 2018138019-A/19041: Polycomb-Associated Non-Coding RNAs.
MA616416 - JP 2018138019-A/188342: Polycomb-Associated Non-Coding RNAs.
MA616417 - JP 2018138019-A/188343: Polycomb-Associated Non-Coding RNAs.

-  Biochemical and Signaling Pathways
  Reactome (by CSHL, EBI, and GO)

Protein P21333 (Reactome details) participates in the following event(s):

R-HSA-430096 GP1b-IX-V binds filamin
R-HSA-5669240 FLNA binds PAK1
R-HSA-430347 MigFilin associates with Filamin and F-actin
R-HSA-482772 Release of platelet cytosolic components
R-HSA-5669250 PAK1 phosphorylates FLNA
R-HSA-430116 GP1b-IX-V activation signalling
R-HSA-5627123 RHO GTPases activate PAKs
R-HSA-446353 Cell-extracellular matrix interactions
R-HSA-114608 Platelet degranulation
R-HSA-76002 Platelet activation, signaling and aggregation
R-HSA-195258 RHO GTPase Effectors
R-HSA-446728 Cell junction organization
R-HSA-76005 Response to elevated platelet cytosolic Ca2+
R-HSA-109582 Hemostasis
R-HSA-194315 Signaling by Rho GTPases
R-HSA-1500931 Cell-Cell communication
R-HSA-162582 Signal Transduction

-  Other Names for This Gene
  Alternate Gene Symbols: E9KL45, ENST00000369850.1, ENST00000369850.2, ENST00000369850.3, ENST00000369850.4, ENST00000369850.5, ENST00000369850.6, ENST00000369850.7, ENST00000369850.8, ENST00000369850.9, FLN, FLN1, FLNA_HUMAN, NM_001110556, P21333, Q5HY53, Q5HY55, Q8NF52, uc318hxh.1, uc318hxh.2
UCSC ID: ENST00000369850.10_12
RefSeq Accession: NM_001110556.2
Protein: P21333 (aka FLNA_HUMAN)

-  GeneReviews for This Gene
  GeneReviews article(s) related to gene FLNA:
opd (X-Linked Otopalatodigital Spectrum Disorders)
taa (Heritable Thoracic Aortic Disease Overview)
x-pvh (FLNA Deficiency)

-  Gene Model Information
  Click here for a detailed description of the fields of the table above.

-  Methods, Credits, and Use Restrictions
  Click here for details on how this gene model was made and data restrictions if any.