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'''Leber’s hereditary optic neuropathy (LHON)''' or '''Leber optic atrophy''' is a [[Human mitochondrial genetics|mitochondrially inherited]] (transmitted from mother to offspring) degeneration of [[retina]]l [[ganglion cell]]s (RGCs) and their [[axon]]s that leads to an acute or subacute loss of central vision; this affects predominantly young adult males. However, LHON is only transmitted through the mother as it is primarily due to [[mutation]]s in the mitochondrial (not nuclear) [[genome]] and only the [[ovum|egg]] contributes [[mitochondria]] to the [[embryo]]. LHON is usually due to one of three pathogenic mitochondrial [[DNA]] (mtDNA) [[point mutation]]s. These mutations are at [[nucleotide]] positions 11778 [[guanine|G]] to [[adenine|A]], 3460 [[guanine|G]] to [[adenine|A]] and 14484 [[thymine|T]] to [[cytosine|C]], respectively in the ND4, ND1 and ND6 subunit [[gene]]s of [[electron transfer chain|complex I]] of the [[oxidative phosphorylation]] chain in mitochondria. Men cannot pass on the disease to their offspring.<ref>{{cite journal |author=Bandelt HJ, Kong QP, Parson W, Salas A |title=More evidence for non-maternal inheritance of mitochondrial DNA? |journal=J. Med. Genet. |volume=42 |issue=12 |pages=957–60 |year=2005 |month=December |pmid=15923271 |doi=10.1136/jmg.2005.033589 |url= |pmc=1735965}}</ref>
'''Leber’s hereditary optic neuropathy (LHON)''' or '''Leber optic atrophy''' is a [[Human mitochondrial genetics|mitochondrially inherited]] (transmitted from mother to offspring) degeneration of [[retina]]l [[ganglion cell]]s (RGCs) and their [[axon]]s that leads to an acute or subacute loss of central vision; this affects predominantly young adult males. However, LHON is only transmitted through the mother as it is primarily due to [[mutation]]s in the mitochondrial (not nuclear) [[genome]] and only the [[ovum|egg]] contributes [[mitochondria]] to the [[embryo]]. LHON is usually due to one of three pathogenic mitochondrial [[DNA]] (mtDNA) [[point mutation]]s. These mutations are at [[nucleotide]] positions 11778 [[guanine|G]] to [[adenine|A]], 3460 [[guanine|G]] to [[adenine|A]] and 14484 [[thymine|T]] to [[cytosine|C]], respectively in the ND4, ND1 and ND6 subunit [[gene]]s of [[electron transfer chain|complex I]] of the [[oxidative phosphorylation]] chain in mitochondria. Men cannot pass on the disease to their offspring.<ref>{{cite journal |author=Bandelt HJ, Kong QP, Parson W, Salas A |title=More evidence for non-maternal inheritance of mitochondrial DNA? |journal=J. Med. Genet. |volume=42 |issue=12 |pages=957–60 |year=2005 |month=December |pmid=15923271 |doi=10.1136/jmg.2005.033589 |url= |pmc=1735965}}</ref>


==History==
==Bunghole==


This disease was first described by the German ophthalmologist [[Theodor Leber]] (1840–1917) in 1871.<ref name=Leber1871>Leber T. Ueber hereditaere und congenital angelegte sehnervenleiden (1871) Graefes Arch Clin Exp Ophthalmol. 17:249–291</ref> In this paper Leber described four families in which a number of young men suffered abrupt loss of vision in both eyes either simultaneously or sequentially. This disease was initially thought to be X linked but was subsequently shown to be mitochondrial.<ref name=Erickson1972>{{cite journal | author = Erickson RP | year = 1972 | title = Leber's optic atrophy, a possible example of maternal inheritance | url = | journal = Am J Hum Genet | volume = 24 | issue = 3| pages = 348–349 }}</ref> The nature of the causative mutation was first identified in 1988 by Wallace ''et al.'' who discovered the [[guanine]] (G) to [[adenosine]] (A) mutation at nucleotide position 11778 in nine families.<ref name=Wallace1988>{{cite journal | author = Wallace DC, Singh G, Lott MT, Hodge JA, Schurr TG, Lezza AM, Elsas LJ 2nd, Nikoskelainen EK | year = 1988 | title = Mitochondrial DNA mutation associated with Leber's hereditary optic neuropathy | url = | journal = Science | volume = 242 | issue = 4884| pages = 1427–1430 }}</ref> This mutation converts a highly conserved [[arginine]] to [[histidine]] at [[codon]] 340 in the [[NADH dehydrogenase]] subunit 4 of [[complex I]] of the [[mitochondria]]l respiratory chain. The other two mutations known to cause this condition were identified in 1991 (G to A point mutation at nucleotide position 3460)<ref name=Huoponen1991>{{cite journal | author = Huoponen K, Vilkki J, Aula P, Nikoskelainen EK, Savontaus ML | year = 1991 | title = A new mtDNA mutation associated with Leber hereditary optic neuroretinopathy | url = | journal = Am J Hum Genet | volume = 48 | issue = 6| pages = 1147–1153 }}</ref> and 1992 ([[thymidine]] (T) to [[cytosine]] (C) mutation at nucleotide 14484).<ref name=Johns1992>{{cite journal | author = Johns DR, Neufeld MJ, Park RD | year = 1992 | title = An ND-6 mitochondrial DNA mutation associated with Leber hereditary optic neuropathy | url = | journal = Biochem Biophys Res Commun | volume = 187 | issue = 3| pages = 1551–1557 }}</ref> These three mutations account for over 95% of cases: the 11778 mutation accounts for 50-70% of cases, the 14484 mutation for 10-15% and the 3460 mutation for 8-25%.
This disease was first described by the German ophthalmologist [[Theodor Leber]] (1840–1917) in 1871.<ref name=Leber1871>Leber T. Ueber hereditaere und congenital angelegte sehnervenleiden (1871) Graefes Arch Clin Exp Ophthalmol. 17:249–291</ref> In this paper Leber described four families in which a number of young men suffered abrupt loss of vision in both eyes either simultaneously or sequentially. This disease was initially thought to be X linked but was subsequently shown to be mitochondrial.<ref name=Erickson1972>{{cite journal | author = Erickson RP | year = 1972 | title = Leber's optic atrophy, a possible example of maternal inheritance | url = | journal = Am J Hum Genet | volume = 24 | issue = 3| pages = 348–349 }}</ref> The nature of the causative mutation was first identified in 1988 by Wallace ''et al.'' who discovered the [[guanine]] (G) to [[adenosine]] (A) mutation at nucleotide position 11778 in nine families.<ref name=Wallace1988>{{cite journal | author = Wallace DC, Singh G, Lott MT, Hodge JA, Schurr TG, Lezza AM, Elsas LJ 2nd, Nikoskelainen EK | year = 1988 | title = Mitochondrial DNA mutation associated with Leber's hereditary optic neuropathy | url = | journal = Science | volume = 242 | issue = 4884| pages = 1427–1430 }}</ref> This mutation converts a highly conserved [[arginine]] to [[histidine]] at [[codon]] 340 in the [[NADH dehydrogenase]] subunit 4 of [[complex I]] of the [[mitochondria]]l respiratory chain. The other two mutations known to cause this condition were identified in 1991 (G to A point mutation at nucleotide position 3460)<ref name=Huoponen1991>{{cite journal | author = Huoponen K, Vilkki J, Aula P, Nikoskelainen EK, Savontaus ML | year = 1991 | title = A new mtDNA mutation associated with Leber hereditary optic neuroretinopathy | url = | journal = Am J Hum Genet | volume = 48 | issue = 6| pages = 1147–1153 }}</ref> and 1992 ([[thymidine]] (T) to [[cytosine]] (C) mutation at nucleotide 14484).<ref name=Johns1992>{{cite journal | author = Johns DR, Neufeld MJ, Park RD | year = 1992 | title = An ND-6 mitochondrial DNA mutation associated with Leber hereditary optic neuropathy | url = | journal = Biochem Biophys Res Commun | volume = 187 | issue = 3| pages = 1551–1557 }}</ref> These three mutations account for over 95% of cases: the 11778 mutation accounts for 50-70% of cases, the 14484 mutation for 10-15% and the 3460 mutation for 8-25%.

Revision as of 15:37, 9 December 2013

Leber's hereditary optic neuropathy
SpecialtyOphthalmology Edit this on Wikidata

Leber’s hereditary optic neuropathy (LHON) or Leber optic atrophy is a mitochondrially inherited (transmitted from mother to offspring) degeneration of retinal ganglion cells (RGCs) and their axons that leads to an acute or subacute loss of central vision; this affects predominantly young adult males. However, LHON is only transmitted through the mother as it is primarily due to mutations in the mitochondrial (not nuclear) genome and only the egg contributes mitochondria to the embryo. LHON is usually due to one of three pathogenic mitochondrial DNA (mtDNA) point mutations. These mutations are at nucleotide positions 11778 G to A, 3460 G to A and 14484 T to C, respectively in the ND4, ND1 and ND6 subunit genes of complex I of the oxidative phosphorylation chain in mitochondria. Men cannot pass on the disease to their offspring.[1]

Bunghole

This disease was first described by the German ophthalmologist Theodor Leber (1840–1917) in 1871.[2] In this paper Leber described four families in which a number of young men suffered abrupt loss of vision in both eyes either simultaneously or sequentially. This disease was initially thought to be X linked but was subsequently shown to be mitochondrial.[3] The nature of the causative mutation was first identified in 1988 by Wallace et al. who discovered the guanine (G) to adenosine (A) mutation at nucleotide position 11778 in nine families.[4] This mutation converts a highly conserved arginine to histidine at codon 340 in the NADH dehydrogenase subunit 4 of complex I of the mitochondrial respiratory chain. The other two mutations known to cause this condition were identified in 1991 (G to A point mutation at nucleotide position 3460)[5] and 1992 (thymidine (T) to cytosine (C) mutation at nucleotide 14484).[6] These three mutations account for over 95% of cases: the 11778 mutation accounts for 50-70% of cases, the 14484 mutation for 10-15% and the 3460 mutation for 8-25%.

Signs & symptoms

Clinically, there is an acute onset of visual loss, first in one eye, and then a few weeks to months later in the other. Onset is usually young adulthood, but age range at onset from 7-75 is reported. The age of onset is slightly higher in females (range 19–55 years: mean 31.3 years) than males (range 15–53 years: mean 24.3). The male to female ratio varies between mutations: 3:1 for 3460 G>A, 6:1 for 11778 G>A and 8:1 for 14484 T>C.

This typically evolves to very severe optic atrophy and permanent decrease of visual acuity. Both eyes become affected either simultaneously (25% of cases) or sequentially (75% of cases) with a median inter-eye delay of 8 weeks. Rarely only one eye may be affected. In the acute stage, lasting a few weeks, the affected eye demonstrates an edematous appearance of the nerve fiber layer especially in the arcuate bundles and enlarged or telangectatic and tortuous peripapillary vessels (microangiopathy). The main features are seen on fundus examination, just before or subsequent to the onset of visual loss. A pupillary defect may be visible in the acute stage as well. Examination reveals decreased visual acuity, loss of color vision and a cecocentral scotoma on visual field examination.

LHON Plus

"LHON Plus" is a name given to rare strains of the disorder with eye disease together with other conditions.[7] The symptoms of this higher form of the disease include loss of the brain's ability to control the movement of muscles, tremors, and cardiac arrhythmia.[8] Many cases of LHON plus have been comparable to multiple sclerosis because of the lack of muscular control.[9]

Genetics

Leber’s hereditary optic neuropathy has a mitochondrial inheritance pattern.

Leber hereditary optic neuropathy is a condition related to changes in mitochondrial DNA. Although most DNA is packaged in chromosomes within the nucleus, mitochondria have a distinct mitochondrial genome composed of mtDNA.

Mutations in the MT-ND1, MT-ND4, MT-ND4L, and MT-ND6 genes cause Leber hereditary optic neuropathy.[10] These genes code for the NADH dehydrogenase protein involved in the normal mitochondrial function of oxidative phosphorylation. Oxidative phosphorylation uses a series of four large multienzyme complexes, which are all embedded in the inner mitochondrial membrane to convert oxygen and simple sugars to energy. Mutations in any of the genes disrupt this process to cause a variety of syndromes depending on the type of mutation and other factors. It remains unclear how these genetic changes cause the death of cells in the optic nerve and lead to the specific features of Leber hereditary optic neuropathy.

Epidemiology

In Northern European populations about one in 9000 people carry one of the three primary LHON mutations.[11] [12] There is a prevalence of between 1:30,000 to 1:50,000 in Europe.

The LHON ND4 G11778A mutation dominates as the primary mutation in most of the world with 70% of European cases and 90% of Asian cases. Due to a Founder effect, the LHON ND6 T14484C mutation accounts for 86% of LHON cases in Quebec, Canada.[13]

More than 50 percent of males with a mutation and more than 85 percent of females with a mutation never experience vision loss or related medical problems. The particular mutation type may predict likelihood of penetrance, severity of illness and probability of vision recovery in the affected. As a rule of thumb, a woman who harbors a homoplasmic primary LHON mutation has a ~40% risk of having an affected son and a ~10% risk of having an affected daughter.

Additional factors may determine whether a person develops the signs and symptoms of this disorder. Environmental factors such as smoking and alcohol use may be involved, although studies of these factors have produced conflicting results. Researchers are also investigating whether changes in additional genes, particularly genes on the X chromosome,[14] [15] contribute to the development of signs and symptoms. The degree of heteroplasmy, the percentage of mitochondria which have mutant alleles, may play a role.[16] Patterns of mitochondrial alleles called haplogroup may also affect expression of mutations.[17]

Pathophysiology

The eye pathology is limited to the retinal ganglion cell layer especially the maculopapillary bundle. Degeneration is evident from the retinal ganglion cell bodies to the axonal pathways leading to the lateral geniculate nucleii. Experimental evidence reveals impaired glutamate transport and increased reactive oxygen species (ROS) causing apoptosis of retinal ganglion cells. Also, experiments suggest that normal non LHON affected retinal ganglion cells produce less of the potent superoxide radical than other normal central nervous system neurons.[18] Viral vector experiments which augment superoxide dismutase 2 in LHON cybrids[19] or LHON animal models or use of exogenous glutathione in LHON cybrids[20] have been shown to rescue LHON affected retinal ganglion cells from apoptotic death. These experiments may in part explain the death of LHON affected retinal ganglion cells in preference to other central nervous system neurons which also carry LHON affected mitochondria.

Diagnosis and management

Without a known family history of LHON the diagnosis usually requires a neuro-ophthalmological evaluation and blood testing for mitochondrial DNA assessment.[21] It is important to exclude other possible causes of vision loss and important associated syndromes such as heart electrical conduction system abnormalities. The prognosis for those affected left untreated is almost always that of continued significant visual loss in both eyes. Regular corrected visual acuity and perimetry checks are advised for follow up of affected individuals. There is beneficial treatment available for some cases of this disease especially for early onset disease.[22] Also, experimental treatment protocols are in progress.[23] Genetic counselling should be offered. Health and lifestyle choices should be reassessed particularly in light of toxic and nutritional theories of gene expression. Vision aides assistance and work rehabilitation should be used to assist in maintaining employment.

For those who are carriers of a LHON mutation, preclinical markers may be used to monitor progress.[24] For example fundus photography can monitor nerve fiber layer swelling. Optical coherence tomography can be used for more detailed study of retinal nerve fiber layer thickness. Red green color vision testing may detect losses. Contrast sensitivity may be diminished. There could be an abnormal electroretinogram or visual evoked potentials. Neuron-specific enolase and axonal heavy chain neurofilament blood markers may predict conversion to affected status.

Cyanocobalamin (a form of B12) should be avoided as it may lead to blindness in Leber's disease patients.

Avoiding optic nerve toxins is generally advised, especially tobacco and alcohol. Certain prescription drugs are known to be a potential risk, so all drugs should be treated with suspicion and checked before use by those at risk. Ethambutol, in particular, has been implicated as triggering visual loss in carriers of LHON. In fact, toxic and nutritional optic neuropathies may have overlaps with LHON in symptoms, mitochondrial mechanisms of disease and management.[25] Of note, when a patient carrying or suffering from LHON or toxic/nutritional optic neuropathy suffers a hypertensive crisis as a possible complication of the disease process, nitroprusside (trade name: Nipride) should not be used due to increased risk of optic nerve ischemia in response to this anti-hypertensive in particular.[26]

Idebenone[22][27][28] has been shown in a small placebo controlled trial to have modest benefit in about half of patients. People most likely to respond best were those treated early in onset.

α-Tocotrienol-quinone, a vitamin E metabolite, has had some success in small open label trials in reversing early onset vision loss.[23][29]

There are various treatment approaches which have had early trials or are proposed, none yet with convincing evidence of usefulness or safety for treatment or prevention including brimonidine,[30] minocycline,[31] curcumin,[32] glutathione,[20] near infrared light treatment,[33] and viral vector techniques.[19]

"Three person in vitro fertilisation" is a proof of concept research technique for preventing mitochondrial disease in developing human fetuses. So far, viable macaque monkeys have been produced. But ethical and knowledge hurdles remain before use of the technique in humans is established.[34]

See also

References

  1. ^ Bandelt HJ, Kong QP, Parson W, Salas A (2005). "More evidence for non-maternal inheritance of mitochondrial DNA?". J. Med. Genet. 42 (12): 957–60. doi:10.1136/jmg.2005.033589. PMC 1735965. PMID 15923271. {{cite journal}}: Unknown parameter |month= ignored (help)CS1 maint: multiple names: authors list (link)
  2. ^ Leber T. Ueber hereditaere und congenital angelegte sehnervenleiden (1871) Graefes Arch Clin Exp Ophthalmol. 17:249–291
  3. ^ Erickson RP (1972). "Leber's optic atrophy, a possible example of maternal inheritance". Am J Hum Genet. 24 (3): 348–349.
  4. ^ Wallace DC, Singh G, Lott MT, Hodge JA, Schurr TG, Lezza AM, Elsas LJ 2nd, Nikoskelainen EK (1988). "Mitochondrial DNA mutation associated with Leber's hereditary optic neuropathy". Science. 242 (4884): 1427–1430.{{cite journal}}: CS1 maint: multiple names: authors list (link) CS1 maint: numeric names: authors list (link)
  5. ^ Huoponen K, Vilkki J, Aula P, Nikoskelainen EK, Savontaus ML (1991). "A new mtDNA mutation associated with Leber hereditary optic neuroretinopathy". Am J Hum Genet. 48 (6): 1147–1153.{{cite journal}}: CS1 maint: multiple names: authors list (link)
  6. ^ Johns DR, Neufeld MJ, Park RD (1992). "An ND-6 mitochondrial DNA mutation associated with Leber hereditary optic neuropathy". Biochem Biophys Res Commun. 187 (3): 1551–1557.{{cite journal}}: CS1 maint: multiple names: authors list (link)
  7. ^ Nikoskelainen EK, Marttila RJ, Huoponen K; et al. (1995). "Leber's "plus": neurological abnormalities in patients with Leber's hereditary optic neuropathy". J. Neurol. Neurosurg. Psychiatr. 59 (2): 160–4. doi:10.1136/jnnp.59.2.160. PMC 485991. PMID 7629530. {{cite journal}}: Explicit use of et al. in: |author= (help); Unknown parameter |month= ignored (help)CS1 maint: multiple names: authors list (link)
  8. ^ cardiac arrythmia
  9. ^ Mayo Clinic: Multiple Sclerosis
  10. ^ Online Mendelian Inheritance in Man (OMIM): LEBER OPTIC ATROPHY - 535000
  11. ^ Man PY, Griffiths PG, Brown DT, Howell N, Turnbull DM, Chinnery PF (2003). "The Epidemiology of Leber Hereditary Optic Neuropathy in the North East of England". Am. J. Hum. Genet. 72 (2): 333–9. doi:10.1086/346066. PMC 379226. PMID 12518276. {{cite journal}}: Unknown parameter |month= ignored (help)CS1 maint: multiple names: authors list (link)
  12. ^ Puomila A, Hämäläinen P, Kivioja S; et al. (2007). "Epidemiology and penetrance of Leber hereditary optic neuropathy in Finland". Eur. J. Hum. Genet. 15 (10): 1079–89. doi:10.1038/sj.ejhg.5201828. PMID 17406640. {{cite journal}}: Explicit use of et al. in: |author= (help); Unknown parameter |month= ignored (help)CS1 maint: multiple names: authors list (link)
  13. ^ Laberge AM, Jomphe M, Houde L; et al. (2005). "A "Fille du Roy" Introduced the T14484C Leber Hereditary Optic Neuropathy Mutation in French Canadians". Am. J. Hum. Genet. 77 (2): 313–7. doi:10.1086/432491. PMC 1224533. PMID 15954041. {{cite journal}}: Explicit use of et al. in: |author= (help)CS1 maint: multiple names: authors list (link)
  14. ^ Hudson G, Carelli V, Horvath R, Zeviani M, Smeets HJ, Chinnery PF (2007). "X-Inactivation patterns in females harboring mtDNA mutations that cause Leber hereditary optic neuropathy". Mol. Vis. 13: 2339–43. PMID 18199976.{{cite journal}}: CS1 maint: multiple names: authors list (link)
  15. ^ Hudson G, Keers S, Yu Wai Man P; et al. (2005). "Identification of an X-Chromosomal Locus and Haplotype Modulating the Phenotype of a Mitochondrial DNA Disorder". Am. J. Hum. Genet. 77 (6): 1086–91. doi:10.1086/498176. PMC 1285165. PMID 16380918. {{cite journal}}: Explicit use of et al. in: |author= (help); Unknown parameter |month= ignored (help)CS1 maint: multiple names: authors list (link)
  16. ^ Chinnery PF, Andrews RM, Turnbull DM, Howell NN (2001). "Leber hereditary optic neuropathy: Does heteroplasmy influence the inheritance and expression of the G11778A mitochondrial DNA mutation?". Am. J. Med. Genet. 98 (3): 235–43. doi:10.1002/1096-8628(20010122)98:3<235::AID-AJMG1086>3.0.CO;2-O. PMID 11169561. {{cite journal}}: Unknown parameter |month= ignored (help)CS1 maint: multiple names: authors list (link)
  17. ^ Hudson G, Carelli V, Spruijt L; et al. (2007). "Clinical Expression of Leber Hereditary Optic Neuropathy Is Affected by the Mitochondrial DNA–Haplogroup Background". Am. J. Hum. Genet. 81 (2): 228–33. doi:10.1086/519394. PMC 1950812. PMID 17668373. {{cite journal}}: Explicit use of et al. in: |author= (help); Unknown parameter |month= ignored (help)CS1 maint: multiple names: authors list (link)
  18. ^ Hoegger MJ, Lieven CJ, Levin LA (2008). "Differential production of superoxide by neuronal mitochondria". BMC Neurosci. 9: 4. doi:10.1186/1471-2202-9-4. PMC 2266764. PMID 18182110.{{cite journal}}: CS1 maint: multiple names: authors list (link) CS1 maint: unflagged free DOI (link)
  19. ^ a b Qi X, Sun L, Hauswirth WW, Lewin AS, Guy J (2007). "Use of mitochondrial antioxidant defenses for rescue of cells with a Leber hereditary optic neuropathy-causing mutation". Arch. Ophthalmol. 125 (2): 268–72. doi:10.1001/archopht.125.2.268. PMID 17296905. {{cite journal}}: Unknown parameter |month= ignored (help)CS1 maint: multiple names: authors list (link)
  20. ^ a b Ghelli A, Porcelli AM, Zanna C, Martinuzzi A, Carelli V, Rugolo M (2008). "Protection against oxidant-induced apoptosis by exogenous glutathione in Leber hereditary optic neuropathy cybrids". Invest. Ophthalmol. Vis. Sci. 49 (2): 671–6. doi:10.1167/iovs.07-0880. PMID 18235013. {{cite journal}}: Unknown parameter |month= ignored (help)CS1 maint: multiple names: authors list (link)
  21. ^ GeneTests LHON search
  22. ^ a b Klopstock, T. (25 July 2011). "A randomized placebo-controlled trial of idebenone in Leber's hereditary optic neuropathy". Brain. 134 (9): 2677. doi:10.1093/brain/awr170. {{cite journal}}: Unknown parameter |coauthors= ignored (|author= suggested) (help)
  23. ^ a b Attention: This template ({{cite pmid}}) is deprecated. To cite the publication identified by PMID 21600768, please use {{cite journal}} with |pmid=21600768 instead.
  24. ^ Sadun AA, Salomao SR, Berezovsky A; et al. (2006). "SUBCLINICAL CARRIERS AND CONVERSIONS IN LEBER HEREDITARY OPTIC NEUROPATHY: A PROSPECTIVE PSYCHOPHYSICAL STUDY". Trans Am Ophthalmol Soc. 104: 51–61. PMC 1809912. PMID 17471325. {{cite journal}}: Explicit use of et al. in: |author= (help)CS1 maint: multiple names: authors list (link)
  25. ^ Carelli V, Ross-Cisneros FN, Sadun AA (2004). "Mitochondrial dysfunction as a cause of optic neuropathies". Prog Retin Eye Res. 23 (1): 53–89. doi:10.1016/j.preteyeres.2003.10.003. PMID 14766317. {{cite journal}}: Unknown parameter |month= ignored (help)CS1 maint: multiple names: authors list (link)
  26. ^ Katz, Jason (2006). Parkland Manual of Inpatient Medicine. Dallas, TX: FA Davis. p. 903. {{cite book}}: Unknown parameter |coauthors= ignored (|author= suggested) (help)
  27. ^ Clinical Idebenone trial recruiting at Newcastle University UK http://lhon.ncl.ac.uk
  28. ^ Mashima Y, Kigasawa K, Wakakura M, Oguchi Y (2000). "Do idebenone and vitamin therapy shorten the time to achieve visual recovery in Leber hereditary optic neuropathy?". J Neuroophthalmol. 20 (3): 166–70. doi:10.1097/00041327-200020030-00006. PMID 11001192. {{cite journal}}: Unknown parameter |month= ignored (help)CS1 maint: multiple names: authors list (link)
  29. ^ Sadun,A et al. "EPI-743 alters the natural history of progression of Leber hereditary optic neuropathy". AOS meeting. May 2011
  30. ^ Newman NJ, Biousse V, David R; et al. (2005). "Prophylaxis for second eye involvement in leber hereditary optic neuropathy: an open-labeled, nonrandomized multicenter trial of topical brimonidine purite". Am. J. Ophthalmol. 140 (3): 407–15. doi:10.1016/j.ajo.2005.03.058. PMID 16083844. {{cite journal}}: Explicit use of et al. in: |author= (help); Unknown parameter |month= ignored (help)CS1 maint: multiple names: authors list (link)
  31. ^ Haroon MF, Fatima A, Schöler S; et al. (2007). "Minocycline, a possible neuroprotective agent in Leber's hereditary optic neuropathy (LHON): Studies of cybrid cells bearing 11778 mutation". Neurobiol Dis. 28 (3): 237–50. doi:10.1016/j.nbd.2007.07.021. PMID 17822909. {{cite journal}}: Explicit use of et al. in: |author= (help)CS1 maint: multiple names: authors list (link)
  32. ^ Clinical Curcurmin trial recruiting at ClinicalTrials.nlm.nih.gov
  33. ^ Wisconsin near infrared trial
  34. ^ Craven L, Tuppen HA, Greggains GD, Harbottle SJ, Murphy JL, Cree LM, Murdoch AP, Chinnery PF, Taylor RW, Lightowlers RN, Herbert M, Turnbull DM (2010). "Pronuclear transfer in human embryos to prevent transmission of mitochondrial DNA disease". Nature. 465 (7294): 82–85. doi:10.1038/nature08958. PMC 2875160. PMID 20393463. {{cite journal}}: Unknown parameter |month= ignored (help)CS1 maint: multiple names: authors list (link)
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