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Fuchs' dystrophy

March 12, 2023

Fuchs dystrophy, also referred to as Fuchs endothelial corneal dystrophy (FECD) and Fuchs endothelial dystrophy (FED), is a slowly progressing corneal dystrophy that usually affects both eyes and is slightly more common in women than in men. Although early signs of Fuchs dystrophy are sometimes seen in people in their 30s and 40s, the disease rarely affects vision until people reach their 50s and 60s.

Fuchs' dystrophy
Other namesFuchs endothelial corneal dystrophy (FECD)
Fuchs corneal dystrophy. Light microscopic appearance of the cornea showing numerous excrescences (guttae) on the posterior surface of Descemet's membrane and the presence of cysts in the corneal epithelium beneath ectopically placed intraepithelial basement membrane. Periodic acid-Schiff stain. From a review by Klintworth, 2009.[1]
Pronunciation
SpecialtyOphthalmology 

Signs and symptoms

As a progressive, chronic condition, signs and symptoms of Fuchs dystrophy gradually progress over decades of life, starting in middle age. Early symptoms include blurry vision upon wakening which improves during the morning,[2] as fluid retained in the cornea is unable to evaporate through the surface of the eye when the lids are closed overnight. As the disease worsens, the interval of blurry morning vision extends from minutes to hours.[citation needed]

In moderate stages of the disease, an increase in guttae and swelling in the cornea can contribute to changes in vision and decreased sharpness throughout the day. Contrast sensitivity may be affected. The change in the refractive index of the cornea may result in subtle refractive shifts, which affected individuals may experience as a small change in their eyeglass prescription.

In the late stages of the disease, the cornea is unable to maintain its fluid content and blisters, known as bullae, form on the surface of the cornea. These cause foreign body sensations and can be painful. The cornea may not heal from such epithelial defects, until corneal transplantation is able to restore the endothelial pump function.

Cause

FECD is a degenerative disease of the corneal endothelium with accumulation of focal outgrowths called guttae (drops) and thickening of Descemet's membrane, leading to corneal edema and loss of vision. The corneal endothelial cell layer and its basement membrane (Descemet's membrane) act as a barrier to hydration of the corneal stroma by aqueous humor and are "pump" cells of the cornea that function to maintain hydration of the cornea at a specific level that maintains corneal stromal clarity through precise spatial arrangement of collagen fibers. In FED, Descemet's membrane is grossly thickened with accumulation of abnormal wide-spaced collagen and numerous guttae. Corneal endothelial cells in end-stage FED are reduced in number and appear attenuated, causing progressive stromal edema (swelling). Progressive endothelial cell loss causes relative influx of aqueous humor into the cornea, leading to swelling (corneal stromal edema), which results in blurred vision. Eventually, the epithelium also becomes edematous, resulting in more severe visual impairment. Focal blisters of epithelial edema ("bullae") may be particularly painful when they burst.[citation needed]

The inheritance of FECD is complex and polymorphic such that although inheritance is autosomal dominant there are genetic and environmental modifiers that determine the degree to which members of the same family express the disease. There is reasonable evidence of associations between transcription factor 4 (TCF4) genetic polymorphisms and risk of Fuchs' endothelial dystrophy (FED).[3] Endothelial cell loss may be aggravated or accelerated by intraocular trauma or surgery. A common scenario involves prolonged corneal swelling or edema following cataract surgery or other types of ocular surgery. Hence, patients with a history of Fuchs' dystrophy may be at a greater risk of corneal edema after ocular surgery as they have fewer functioning endothelial cells.[citation needed]

FECD is classified into 4 stages, from early signs of guttae formation to end-stage subepithelial scarring. Diagnosis is made by biomicroscopic examination in the clinic. Other modalities, such as corneal thickness measurement (pachymetry), in-vivo confocal biomicroscopy, and specular microscopy can be used in conjunction.[citation needed]

The exact pathogenesis is unknown but factors include endothelial cell apoptosis, sex hormones, inflammation, and aqueous humor flow and composition. Mutations in collagen VIII, a major component of Descemet's membrane secreted by endothelial cells, have been linked to the early-onset FECD.[4]

As a genetically heterogeneous disease, the phenotype, or clinical experience of patients with Fuchs dystrophy may reflect the combination of genetic contributors to the disease. Some genetic lesions correlate with more severe disease and earlier onset.[5][6][7] Therefore, some individuals may experience symptoms of the disease at a much earlier age, while others may not experience symptoms until late in life.[citation needed]

Genes include:

Type OMIM Gene Locus
FECD1 136800 COL8A2 1p34.3-p32.3
FECD4 610206 SLC4A11 20p13-p12
FECD6 189909 ZEB1 10p11.2

Diagnosis

The diagnosis of Fuchs dystrophy is often made with slit lamp biomicroscopy. With direct illumination, the clinician can visualize guttae, the characteristic pathological changes in disease.[citation needed]

Scheimpflug imaging, anterior segment optical coherence tomography, confocal microscopy, and specular microscopy are additional imaging techniques that can identify the presence of guttae and quantify the thickness of the cornea. While corneal thickness can be a valuable indicator of how the cornea is changing over time, it is affected by multiple factors and is not adequate itself as a screening tool to diagnose Fuchs dystrophy.[citation needed]

Treatment

Non-surgical treatments of FECD may be used to treat symptoms of early disease. Medical management includes topical hypertonic saline, the use of a hairdryer to dehydrate the precorneal tear film, and therapeutic soft contact lenses. Hypertonic saline draws water out of the cornea through osmosis. When using a hairdryer, the patient is instructed to hold it at an arm's length or directed across the face in a cold setting, to dry out the epithelial blisters. This can be done two or three times a day. Scleral lenses can improve vision when it is affected by irregularities on the surface of the cornea,[8] but may stress the corneal endothelium.

Corneal transplantation is the definitive treatment for FECD. The most common types of surgery for FECD are Descemet's stripping automated endothelial keratoplasty (DSAEK) and Descemet's membrane endothelial keratoplasty (DMEK), which account for over half of corneal transplants in the United States.[9] Injection of cultured endothelial cells is under investigation and in a series of 11 patients in Japan with bullous keratopathy, was able to clear corneal edema.[10]

In the United Kingdom, DMEK was pioneered by Dr Fayyaz Musa.[11][12] Dr Musa is the current course instructor for DMEK at the European Society of Cataract and Refractive Surgery Conference and won a 'best in category' award by the American Academy for his work on the procedure[13]

Epidemiology

Few studies have examined the prevalence of FECD on a large scale. First assessed in a clinical setting, Fuchs himself estimated the occurrence of dystrophia epithelialis corneae to be one in every 2000 patients; a rate that is likely reflective of those who progress to advanced disease. Cross-sectional studies suggest a relatively higher prevalence of disease in European countries relative to other areas of the world. Fuchs dystrophy rarely affects individuals under 50 years of age.[2]

History

The condition was first described by Austrian ophthalmologist Ernst Fuchs (1851–1930), after whom it is named. In 1910, Fuchs first reported 13 cases of central corneal clouding, loss of corneal sensation and the formation of epithelial bullae, or blisters, which he labeled 'dystrophia epithelialis corneae'. It was characterized by late onset, slow progression, decreased visual acuity in the morning, lack of inflammation, diffuse corneal opacity, intense centrally, and roughened epithelium with vesicle-like features.[14]

A shift to the understanding of FECD as primarily a disease of the corneal endothelium resulted after a number of observations in the 1920s. Crystal-like features of the endothelium were noted by Kraupa in 1920, who suggested that the epithelial changes were dependent on the endothelium. Using a slit lamp, Vogt described the excrescences associated with FCD as drop-like in appearance in 1921. In 1924, Graves then provided an extremely detailed explanation of the endothelial elevations visible with slit lamp biomicroscopy. A patient with unilateral epithelial dystrophy and bilateral endothelial changes was described by the Friedenwalds in 1925; subsequent involvement of the second eye led them to emphasize that endothelial changes preceded epithelial changes. As only a subset of patients with endothelial changes proceeded to epithelial involvement, Graves stated on 19 October 1925 to the New York Academy of Medicine that "Fuchs' epithelial dystrophy may be a very late sequel to severer cases of the deeper affection".[15]

See also

References

  1. ^ Klintworth GK (2009). "Corneal dystrophies". Orphanet J Rare Dis. 4 (1): 7. doi:10.1186/1750-1172-4-7. PMC 2695576. PMID 19236704.
  2. ^ a b Kunimoto, Derek; Kunal Kanitkar; Mary Makar (2004). The Wills eye manual: office and emergency room diagnosis and treatment of eye disease (4th ed.). Philadelphia: Lippincott Williams & Wilkins. p. 80. ISBN 978-0781742078.
  3. ^ Li, Dan; Peng, XiaoYan; Sun, HuiYu (2015-01-01). "Association of TCF4 polymorphisms and Fuchs' endothelial dystrophy: a meta-analysis". BMC Ophthalmology. 15: 61. doi:10.1186/s12886-015-0055-6. ISSN 1471-2415. PMC 4474332. PMID 26087656.
  4. ^ Gottsch JD, Sundin OH, Liu SH, et al. (June 2005). "Inheritance of a novel COL8A2 mutation defines a distinct early-onset subtype of Fuchs corneal dystrophy". Invest. Ophthalmol. Vis. Sci. 46 (6): 1934–9. doi:10.1167/iovs.04-0937. PMID 15914606.
  5. ^ Eghrari, AO; McGlumphy, EJ; Iliff, BW; Wang, J; Emmert, D; Riazuddin, SA; Katsanis, N; Gottsch, JD (June 2012). "Prevalence and severity of fuchs corneal dystrophy in Tangier Island". American Journal of Ophthalmology. 153 (6): 1067–72. doi:10.1016/j.ajo.2011.11.033. PMC 4154491. PMID 22321803.
  6. ^ Meadows, DN; Eghrari, AO; Riazuddin, SA; Emmert, DG; Katsanis, N; Gottsch, JD (December 2009). "Progression of Fuchs corneal dystrophy in a family linked to the FCD1 locus". Investigative Ophthalmology & Visual Science. 50 (12): 5662–6. doi:10.1167/iovs.09-3568. PMID 19608546.
  7. ^ McGlumphy, EJ; Yeo, WS; Riazuddin, SA; Al-Saif, A; Wang, J; Eghrari, AO; Meadows, DN; Emmert, DG; Katsanis, N; Gottsch, JD (December 2010). "Age-severity relationships in families linked to FCD2 with retroillumination photography". Investigative Ophthalmology & Visual Science. 51 (12): 6298–302. doi:10.1167/iovs.10-5187. PMC 3055756. PMID 20811064.
  8. ^ Jedlicka, Jason, OD, Scleral Contact Lenses, https://www.allaboutvision.com/contacts/scleral-lenses.htm
  9. ^ Stuart AJ, Virgili G, Shortt AJ (2016). "Descemet's membrane endothelial keratoplasty versus Descemet's stripping automated endothelial keratoplasty for corneal endothelial failure". Cochrane Database Syst Rev (3): CD012097. doi:10.1002/14651858.CD012097.
  10. ^ Kinoshita, Shigeru; Koizumi, Noriko; Ueno, Morio; Okumura, Naoki; Imai, Kojiro; Tanaka, Hiroshi; Yamamoto, Yuji; Nakamura, Takahiro; Inatomi, Tsutomu; Bush, John; Toda, Munetoyo (2018-03-15). "Injection of Cultured Cells with a ROCK Inhibitor for Bullous Keratopathy". New England Journal of Medicine. 378 (11): 995–1003. doi:10.1056/NEJMoa1712770. ISSN 0028-4793. PMID 29539291.
  11. ^ Baydoun, Lamis; van Dijk, Korine; Dapena, Isabel; Musa, Fayyaz U.; Liarakos, Vasilis S.; Ham, Lisanne; Melles, Gerrit R.J. (December 2014). "Repeat Descemet Membrane Endothelial Keratoplasty after Complicated Primary Descemet Membrane Endothelial Keratoplasty". Ophthalmology. 122 (1): 8–16. doi:10.1016/j.ophtha.2014.07.024.
  12. ^ "DMEK for Fuchs Dystrophy".
  13. ^ "Dr Fayyaz Musa - Ophthalmologist | Specialist Private Consultant in Corneal and External Eye Disease & Glaucoma Treatment | Elland, West Yorkshire (Near Huddersfield & Halifax) | Spire Elland Hospital".
  14. ^ Fuchs, Ernst (1910). "Dystrophia epithelialis corneae" (PDF). Graefes Archiv für Ophthalmologie. Springer. 76 (3): 478–508.
  15. ^ Eghrari, Allen O; John D Gottsch (April 2010). "Fuchs' corneal dystrophy". Expert Rev Ophthalmol. 5 (2): 147–159. doi:10.1586/eop.10.8. PMC 2897712. PMID 20625449.

External links

March 12, 2023
fuchs, dystrophy, fuchs, dystrophy, also, referred, fuchs, endothelial, corneal, dystrophy, fecd, fuchs, endothelial, dystrophy, slowly, progressing, corneal, dystrophy, that, usually, affects, both, eyes, slightly, more, common, women, than, although, early, . Fuchs dystrophy also referred to as Fuchs endothelial corneal dystrophy FECD and Fuchs endothelial dystrophy FED is a slowly progressing corneal dystrophy that usually affects both eyes and is slightly more common in women than in men Although early signs of Fuchs dystrophy are sometimes seen in people in their 30s and 40s the disease rarely affects vision until people reach their 50s and 60s Fuchs dystrophyOther namesFuchs endothelial corneal dystrophy FECD Fuchs corneal dystrophy Light microscopic appearance of the cornea showing numerous excrescences guttae on the posterior surface of Descemet s membrane and the presence of cysts in the corneal epithelium beneath ectopically placed intraepithelial basement membrane Periodic acid Schiff stain From a review by Klintworth 2009 1 Pronunciation f uː k s ˈ d ɪ s t r e f i fooks DIS tre feeSpecialtyOphthalmology Contents 1 Signs and symptoms 2 Cause 3 Diagnosis 4 Treatment 5 Epidemiology 6 History 7 See also 8 References 9 External linksSigns and symptoms EditAs a progressive chronic condition signs and symptoms of Fuchs dystrophy gradually progress over decades of life starting in middle age Early symptoms include blurry vision upon wakening which improves during the morning 2 as fluid retained in the cornea is unable to evaporate through the surface of the eye when the lids are closed overnight As the disease worsens the interval of blurry morning vision extends from minutes to hours citation needed In moderate stages of the disease an increase in guttae and swelling in the cornea can contribute to changes in vision and decreased sharpness throughout the day Contrast sensitivity may be affected The change in the refractive index of the cornea may result in subtle refractive shifts which affected individuals may experience as a small change in their eyeglass prescription In the late stages of the disease the cornea is unable to maintain its fluid content and blisters known as bullae form on the surface of the cornea These cause foreign body sensations and can be painful The cornea may not heal from such epithelial defects until corneal transplantation is able to restore the endothelial pump function Cause EditFECD is a degenerative disease of the corneal endothelium with accumulation of focal outgrowths called guttae drops and thickening of Descemet s membrane leading to corneal edema and loss of vision The corneal endothelial cell layer and its basement membrane Descemet s membrane act as a barrier to hydration of the corneal stroma by aqueous humor and are pump cells of the cornea that function to maintain hydration of the cornea at a specific level that maintains corneal stromal clarity through precise spatial arrangement of collagen fibers In FED Descemet s membrane is grossly thickened with accumulation of abnormal wide spaced collagen and numerous guttae Corneal endothelial cells in end stage FED are reduced in number and appear attenuated causing progressive stromal edema swelling Progressive endothelial cell loss causes relative influx of aqueous humor into the cornea leading to swelling corneal stromal edema which results in blurred vision Eventually the epithelium also becomes edematous resulting in more severe visual impairment Focal blisters of epithelial edema bullae may be particularly painful when they burst citation needed The inheritance of FECD is complex and polymorphic such that although inheritance is autosomal dominant there are genetic and environmental modifiers that determine the degree to which members of the same family express the disease There is reasonable evidence of associations between transcription factor 4 TCF4 genetic polymorphisms and risk of Fuchs endothelial dystrophy FED 3 Endothelial cell loss may be aggravated or accelerated by intraocular trauma or surgery A common scenario involves prolonged corneal swelling or edema following cataract surgery or other types of ocular surgery Hence patients with a history of Fuchs dystrophy may be at a greater risk of corneal edema after ocular surgery as they have fewer functioning endothelial cells citation needed FECD is classified into 4 stages from early signs of guttae formation to end stage subepithelial scarring Diagnosis is made by biomicroscopic examination in the clinic Other modalities such as corneal thickness measurement pachymetry in vivo confocal biomicroscopy and specular microscopy can be used in conjunction citation needed The exact pathogenesis is unknown but factors include endothelial cell apoptosis sex hormones inflammation and aqueous humor flow and composition Mutations in collagen VIII a major component of Descemet s membrane secreted by endothelial cells have been linked to the early onset FECD 4 As a genetically heterogeneous disease the phenotype or clinical experience of patients with Fuchs dystrophy may reflect the combination of genetic contributors to the disease Some genetic lesions correlate with more severe disease and earlier onset 5 6 7 Therefore some individuals may experience symptoms of the disease at a much earlier age while others may not experience symptoms until late in life citation needed Genes include Type OMIM Gene LocusFECD1 136800 COL8A2 1p34 3 p32 3FECD4 610206 SLC4A11 20p13 p12FECD6 189909 ZEB1 10p11 2Diagnosis EditThe diagnosis of Fuchs dystrophy is often made with slit lamp biomicroscopy With direct illumination the clinician can visualize guttae the characteristic pathological changes in disease citation needed Scheimpflug imaging anterior segment optical coherence tomography confocal microscopy and specular microscopy are additional imaging techniques that can identify the presence of guttae and quantify the thickness of the cornea While corneal thickness can be a valuable indicator of how the cornea is changing over time it is affected by multiple factors and is not adequate itself as a screening tool to diagnose Fuchs dystrophy citation needed Treatment EditNon surgical treatments of FECD may be used to treat symptoms of early disease Medical management includes topical hypertonic saline the use of a hairdryer to dehydrate the precorneal tear film and therapeutic soft contact lenses Hypertonic saline draws water out of the cornea through osmosis When using a hairdryer the patient is instructed to hold it at an arm s length or directed across the face in a cold setting to dry out the epithelial blisters This can be done two or three times a day Scleral lenses can improve vision when it is affected by irregularities on the surface of the cornea 8 but may stress the corneal endothelium Corneal transplantation is the definitive treatment for FECD The most common types of surgery for FECD are Descemet s stripping automated endothelial keratoplasty DSAEK and Descemet s membrane endothelial keratoplasty DMEK which account for over half of corneal transplants in the United States 9 Injection of cultured endothelial cells is under investigation and in a series of 11 patients in Japan with bullous keratopathy was able to clear corneal edema 10 In the United Kingdom DMEK was pioneered by Dr Fayyaz Musa 11 12 Dr Musa is the current course instructor for DMEK at the European Society of Cataract and Refractive Surgery Conference and won a best in category award by the American Academy for his work on the procedure 13 Epidemiology EditFew studies have examined the prevalence of FECD on a large scale First assessed in a clinical setting Fuchs himself estimated the occurrence of dystrophia epithelialis corneae to be one in every 2000 patients a rate that is likely reflective of those who progress to advanced disease Cross sectional studies suggest a relatively higher prevalence of disease in European countries relative to other areas of the world Fuchs dystrophy rarely affects individuals under 50 years of age 2 History EditThe condition was first described by Austrian ophthalmologist Ernst Fuchs 1851 1930 after whom it is named In 1910 Fuchs first reported 13 cases of central corneal clouding loss of corneal sensation and the formation of epithelial bullae or blisters which he labeled dystrophia epithelialis corneae It was characterized by late onset slow progression decreased visual acuity in the morning lack of inflammation diffuse corneal opacity intense centrally and roughened epithelium with vesicle like features 14 A shift to the understanding of FECD as primarily a disease of the corneal endothelium resulted after a number of observations in the 1920s Crystal like features of the endothelium were noted by Kraupa in 1920 who suggested that the epithelial changes were dependent on the endothelium Using a slit lamp Vogt described the excrescences associated with FCD as drop like in appearance in 1921 In 1924 Graves then provided an extremely detailed explanation of the endothelial elevations visible with slit lamp biomicroscopy A patient with unilateral epithelial dystrophy and bilateral endothelial changes was described by the Friedenwalds in 1925 subsequent involvement of the second eye led them to emphasize that endothelial changes preceded epithelial changes As only a subset of patients with endothelial changes proceeded to epithelial involvement Graves stated on 19 October 1925 to the New York Academy of Medicine that Fuchs epithelial dystrophy may be a very late sequel to severer cases of the deeper affection 15 See also EditFuchs heterochromic iridocyclitis a disease of the iris Ocular straylightReferences Edit Klintworth GK 2009 Corneal dystrophies Orphanet J Rare Dis 4 1 7 doi 10 1186 1750 1172 4 7 PMC 2695576 PMID 19236704 a b Kunimoto Derek Kunal Kanitkar Mary Makar 2004 The Wills eye manual office and emergency room diagnosis and treatment of eye disease 4th ed Philadelphia Lippincott Williams amp Wilkins p 80 ISBN 978 0781742078 Li Dan Peng XiaoYan Sun HuiYu 2015 01 01 Association of TCF4 polymorphisms and Fuchs endothelial dystrophy a meta analysis BMC Ophthalmology 15 61 doi 10 1186 s12886 015 0055 6 ISSN 1471 2415 PMC 4474332 PMID 26087656 Gottsch JD Sundin OH Liu SH et al June 2005 Inheritance of a novel COL8A2 mutation defines a distinct early onset subtype of Fuchs corneal dystrophy Invest Ophthalmol Vis Sci 46 6 1934 9 doi 10 1167 iovs 04 0937 PMID 15914606 Eghrari AO McGlumphy EJ Iliff BW Wang J Emmert D Riazuddin SA Katsanis N Gottsch JD June 2012 Prevalence and severity of fuchs corneal dystrophy in Tangier Island American Journal of Ophthalmology 153 6 1067 72 doi 10 1016 j ajo 2011 11 033 PMC 4154491 PMID 22321803 Meadows DN Eghrari AO Riazuddin SA Emmert DG Katsanis N Gottsch JD December 2009 Progression of Fuchs corneal dystrophy in a family linked to the FCD1 locus Investigative Ophthalmology amp Visual Science 50 12 5662 6 doi 10 1167 iovs 09 3568 PMID 19608546 McGlumphy EJ Yeo WS Riazuddin SA Al Saif A Wang J Eghrari AO Meadows DN Emmert DG Katsanis N Gottsch JD December 2010 Age severity relationships in families linked to FCD2 with retroillumination photography Investigative Ophthalmology amp Visual Science 51 12 6298 302 doi 10 1167 iovs 10 5187 PMC 3055756 PMID 20811064 Jedlicka Jason OD Scleral Contact Lenses https www allaboutvision com contacts scleral lenses htm Stuart AJ Virgili G Shortt AJ 2016 Descemet s membrane endothelial keratoplasty versus Descemet s stripping automated endothelial keratoplasty for corneal endothelial failure Cochrane Database Syst Rev 3 CD012097 doi 10 1002 14651858 CD012097 Kinoshita Shigeru Koizumi Noriko Ueno Morio Okumura Naoki Imai Kojiro Tanaka Hiroshi Yamamoto Yuji Nakamura Takahiro Inatomi Tsutomu Bush John Toda Munetoyo 2018 03 15 Injection of Cultured Cells with a ROCK Inhibitor for Bullous Keratopathy New England Journal of Medicine 378 11 995 1003 doi 10 1056 NEJMoa1712770 ISSN 0028 4793 PMID 29539291 Baydoun Lamis van Dijk Korine Dapena Isabel Musa Fayyaz U Liarakos Vasilis S Ham Lisanne Melles Gerrit R J December 2014 Repeat Descemet Membrane Endothelial Keratoplasty after Complicated Primary Descemet Membrane Endothelial Keratoplasty Ophthalmology 122 1 8 16 doi 10 1016 j ophtha 2014 07 024 DMEK for Fuchs Dystrophy Dr Fayyaz Musa Ophthalmologist Specialist Private Consultant in Corneal and External Eye Disease amp Glaucoma Treatment Elland West Yorkshire Near Huddersfield amp Halifax Spire Elland Hospital Fuchs Ernst 1910 Dystrophia epithelialis corneae PDF Graefes Archiv fur Ophthalmologie Springer 76 3 478 508 Eghrari Allen O John D Gottsch April 2010 Fuchs corneal dystrophy Expert Rev Ophthalmol 5 2 147 159 doi 10 1586 eop 10 8 PMC 2897712 PMID 20625449 External links EditFacts About the Cornea and Corneal Disease The National Eye Institute United States Fuchs dystrophy at Curlie Retrieved from https en wikipedia org w index php title Fuchs 27 dystrophy amp oldid 1130148320, wikipedia, wiki, book, books, library,

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