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Dentatorubral–pallidoluysian atrophy

April 12, 2024

Dentatorubral–pallidoluysian atrophy (DRPLA) is an autosomal dominant spinocerebellar degeneration caused by an expansion of a CAG repeat encoding a polyglutamine tract in the atrophin-1 protein.[1] It is also known as Haw River Syndrome and Naito–Oyanagi disease. Although this condition was perhaps first described by Smith et al. in 1958, and several sporadic cases have been reported from Western countries, this disorder seems to be very rare except in Japan.[citation needed]

Dentatorubral–pallidoluysian atrophy
Dentatorubral–pallidoluysian atrophy is inherited in an autosomal dominant manner.
SpecialtyNeurology 

There are at least eight neurodegenerative diseases that are caused by expanded CAG repeats encoding polyglutamine (polyQ) stretches (see: Trinucleotide repeat disorder). The expanded CAG repeats create an adverse gain-of-function mutation in the gene products. Of these diseases, DRPLA is most similar to Huntington's disease.[citation needed]

Signs and symptoms edit

DRPLA can be juvenile-onset (<20 years), early adult-onset (20–40 years), or late adult-onset (>40 years). Late adult-onset DRPLA is characterized by ataxia, choreoathetosis and dementia. Early adult-onset DRPLA also includes seizures and myoclonus. Juvenile-onset DRPLA presents with ataxia and symptoms consistent with progressive myoclonus epilepsy[2] (myoclonus, multiple seizure types and dementia). Other symptoms that have been described include cervical dystonia,[3] corneal endothelial degeneration[4] autism, and surgery-resistant obstructive sleep apnea.[5]

Genetics edit

The human genome contains two atrophin genes; DRPLA has been correlated to the expansion of the polyglutamine region of the atrophin-1 gene on chromosome 12p13.3.[6] A normal number of CAG repeats in the atrophin-1 gene is 7–34, affected individuals display 49–93 repeats. DRPLA displays anticipation (earlier age of onset for subsequent generations) and an inverse correlation between the size of the expanded CAG repeat and the age of symptom onset. Paternal transmission results in more prominent anticipation (26–29 years) than maternal transmission (14–15 years).[2]

Atrophin-1 edit

Atrophin-1 (ATN1) encodes a hydrophilic 1184 amino acid protein with several repetitive motifs including a serine-rich region, a variable length polyglutamine tract, a polyproline tract, and a region of alternating acidic and basic residues. It contains a putative nuclear localization signal in the N-terminus of the protein and a putative nuclear export signal in the C-terminus.[7] ATN1 is ubiquitously expressed in all tissues, but proteolytically cleaved in neuronal cells. The function of ATN1 is not clear, however it is believed to be a transcriptional co-repressor. ATN1 and atrophin-2 can be co-immunoprecipitated, indicating that they may carry out some functions together in a molecular complex.[8] Atrophin-1 may be a dispensable or redundant protein as mice bred with a null allele for atrophin-1 produce viable and fertile offspring and show no compensatory upregulation of atrophin-2.[9]

Transgenic mouse models edit

Mouse models of DRPLA have been successfully generated, which demonstrate the same intergenerational instability and severe phenotype as human DRPLA.[10][11][12] The Schilling mice express full-length human atrophin-1 with 65 CAG repeats under transcriptional control of the mouse prion protein promoter. The mice demonstrated progressive ataxia, tremors, abnormal movements, seizures and premature death. Like in human brains, nuclear accumulation was demonstrated and occasional NIIs were visualised, but the NIIs did not stain for ubiquitin and no neuronal loss was seen.[13] The Sato mice harbored a single copy of full-length human atrophin-1 with 76 or 129 CAG repeats. The hemizygous transgenic offspring of the Q129 mice exhibited symptoms similar to juvenile-type DRPLA, such as myoclonus and seizures. Again, neuronal atrophy was noted, but no neuronal loss (until death). Diffuse accumulation in the nuclei began on post-natal day 4 and ubiquitinated NII formation was detectable at 9 weeks of age. No PML bodies were found to be associated with the NIIs, which were morphologically mildly altered from those seen in human neural cells.[13][14]

Pathology edit

DRPLA is characterized by marked, generalized brain atrophy and the accumulation of atrophin-1 with expanded glutamine stretches. Mutant atrophin-1 proteins have been found in neuronal intranuclear inclusions (NII) and diffusely accumulated in the neuronal nuclei. While the role of NIIs (pathologic or protective) is unclear, the diffuse accumulation of mutant protein is regarded as toxic.[citation needed]

Brain atrophy edit

There is significant reduction in CNS tissue throughout the brain and spinal cord, with brain weights of DRPLA patients often becoming less than 1000g.[15] In regions lacking obvious neuronal depletion, atrophy of the neuropil is noted. The globus pallidus (lateral greater than medial segment) and subthalamic nucleus demonstrate consistent neuronal loss and astrocytic gliosis. The dentate nucleus shows neuronal loss with the remaining atrophic neurons exhibiting grumose degeneration. In general, the pallidoluysian degeneration is more severe than the dentatorubral degeneration in juvenile-onset and the reverse is true for the late adult-onset.[13]

Transgenic DRPLA mice demonstrated several neuronal abnormalities including a reduction in the number and size of dendritic spines as well as in the area of perikarya and diameter of dendrites.[14] Spine morphology and density have been linked to learning and memory functions as well as epilepsy. The stubby-type spines seen in DRPLA mice are morphologically different from the thin and mushroom-type spines seen in Huntington's mice.[citation needed]

Morphometric analysis of DRPLA mouse brains has shown a loss of normal inter-microtubule spacing in neuronal axons. The microtubules were relatively compacted, suggesting abnormalities in protein transport may play a role in neuronal degeneration.[14] In humans, atrophin-1 interacts with IRSp53, which interacts with Rho GTPases to regulate the organization of the actin cytoskeleton and the pathways that regulate lamellipodia and filopodia.[16]

Neuronal intranuclear inclusions edit

NIIs are not exclusive to DRPLA; they have been found in a variety of neurodegenerative disorders. In DRPLA, NIIs have been demonstrated in both neurons and glial cells in the striatum, pontine nuclei, inferior olive, cerebellar cortex and dentate nucleus,[17] though the incidence of neurons with NIIs is low, roughly 1-3%.[13]

In DRPLA, the NIIs are spherical, eosinophilic structures of various sizes. They are non-membrane-bound and are composed of both granular and filamentous structures. They are ubiquitinated and may be paired or in doublet form within the nucleus.[18]

NIIs are immunopositive for several transcription factors such as TATA binding protein (TBP), TBP-associated factor (TAFII130), Sp1, camp-responsive element-binding protein (CREB) and CREB-binding protein (CBP).[19][20] It has been proposed that recruitment of transcription factors into NIIs may induce transcriptional abnormalities that contribute to progressive neuronal degeneration.[13] Other polyQ disorders, such as Huntington's and spinocerebellar ataxia (types 3 and 7), have been demonstrated to sequester some of the same transcriptions factors. That different gene products sequester the same transcription factors may contribute to the overlapping symptoms of genetically different diseases.[21]

NIIs have also been demonstrated to alter the distribution of the intranuclear structures, such as promyelocytic leukemia protein (PML) nuclear bodies. Although the role of PML bodies is unclear, they are believed to be involved in apoptosis. In neurons with NII, PML bodies in DRPLA patients form a shell or ring around the ubiquitinated core.[13][21] In similar polyQ diseases, the association of this PML shell has been shown to be size-dependent with larger NIIs being PML negative.[22][23] This has led to two models, one in which PML bodies represent sites for NII formation and a second in which PML bodies are involved in degradation and proteolysis of NIIs.[21]

Filementous, atrophin-1 positive, inclusions are also observed exclusively in the cytoplasm of the dentate nucleus, which are extremely similar to the inclusions observed in the motor neurons in amyotrophic lateral sclerosis.[24]

Diffuse accumulation in the nuclei edit

In DRPLA, diffuse accumulation of mutant ATN1 occurs far more extensively than NII formation. The extent and frequency of neurons showing the diffuse nuclear accumulations changes depending on CAG repeat length. It is believed that the diffuse nuclear accumulations contribute to the clinical features such as dementia and epilepsy.[citation needed]

ATN1 contains both a nuclear localization sequence and a nuclear export sequence. Cleavage of ATN1 to an N terminal fragment relieves ATN1 of its nuclear export signal and concentrates it in the nucleus. Increased nuclear concentrations have been demonstrated via transfection assay to enhance cellular toxicity.[7]

In both the juvenile and adult forms, regions in which more than 40% of neurons became immunoreactive to 1C2 (a monoclonal antibody against expanded polyglutamine stretches) included: the nucleus basalis of Meynert, large striatal neurons, globus pallidus, subthalamic nucleus, thalamic intralaminar nucleus, lateral geniculate body, oculomotor nucleus, red nucleus, substantia nigra, trigeminal motor nucleus, nucleus raphes pontis, pontine nuclei, vestibular nucleus, inferior olive and the cerebellar dentate nucleus. The juvenile type also shows reactivity in the cerebral cortex, hippocampal CA1 area, and the reticular formation of the brainstem.[13] Nuclei containing accumulations of mutant atrophin-1 are deformed with nuclear membrane indentations.[25]

Diagnosis edit

Diagnosis of DRPLA rests on positive family history, clinical findings, and genetic testing. Family history can be difficult to obtain if a relative was misdiagnosed, died young, or experiences late onset of symptoms.[citation needed]

Other diseases in the differential diagnosis of adult-onset DRPLA include Huntington's and the spinocerebellar ataxias. For juvenile-onset disease, familial essential myoclonus and epilepsy (FEME), Lafora, Unverricht-Lundborg, Neuroaxonal dystrophy, Gaucher's disease, Sialidosis, and Galactosialidosis should be considered.[citation needed]

Management edit

To quantify the extent of the disease, an MRI, EEG and neuropsychological testing are recommended. Seizures are treated with anticonvulsants and psychiatric disturbances with psychotropic medications. Physical therapy has also been recommended to maintain function as the condition progresses and occupational therapy to focus on activities of daily living, advice for careers and adaptation to the environment.[citation needed]

Epidemiology edit

The prevalence of DRPLA in the Japanese population is believed to be 2–7 in 1,000,000. DRPLA is observed relatively less frequently in other ethnic populations and an analysis of normal ATN1 alleles has demonstrated that CAG repeat lengths greater than 17 are significantly more frequent in the Japanese population.[26][27]

References edit

  1. ^ Kanazawa I (June 1999). "Molecular pathology of dentatorubral–pallidoluysian atrophy". Philos. Trans. R. Soc. Lond. B Biol. Sci. 354 (1386): 1069–74. doi:10.1098/rstb.1999.0460. PMC 1692599. PMID 10434307.
  2. ^ a b Tsuji, S. (1999). "Dentatorubral–pallidoluysian atrophy: Clinical features and molecular genetics". Adv Neurol. 79: 399–409. PMID 10514829.
  3. ^ Hatano, T.; et al. (2003). "Cervical dystonia in dentatorubral–pallidoluysian atrophy". Acta Neurol Scand. 108 (4): 287–9. doi:10.1034/j.1600-0404.2003.00150.x. PMID 12956864. S2CID 8681273.
  4. ^ Ito, D.; et al. (2002). "Corneal endothelial degeneration in dentatorubral–pallidoluysian atrophy". Arch Neurol. 59 (2): 289–91. doi:10.1001/archneur.59.2.289. PMID 11843701.
  5. ^ Licht D, Lynch D (2002). "Juvenile Dentatorubral–Pallidoluysian Atrophy: New Clinical Features". Pediatr Neurol. 26 (1): 51–4. doi:10.1016/S0887-8994(01)00346-0. PMID 11814736.
  6. ^ Yazawa, I; et al. (1995). "Abnormal Gene Product Identified in Hereditary DRPLA Brain". Nat Genet. 10 (1): 99–103. doi:10.1038/ng0595-99. PMID 7647802. S2CID 5850726.
  7. ^ a b Nucifora, F; et al. (2003). "Nuclear localization of a Non-caspase Truncation Product of Atrophin-1, with an Expanded Polyglutamine Repeat, Increases Cellular Toxicity". J Biol Chem. 278 (15): 13047–55. doi:10.1074/jbc.M211224200. PMID 12464607.
  8. ^ Zoltewicz, J; et al. (2004). "Atrophin-2 recruits histone deacetylase and is required for the function of multiple signaling centers during mouse embryogenesis". Development. 131 (1): 3–14. doi:10.1242/dev.00908. PMID 14645126.
  9. ^ Shen, Y; et al. (2007). "Functional Architecture of Atrophins". J Biol Chem. 282 (7): 5037–44. doi:10.1074/jbc.M610274200. PMID 17150957.
  10. ^ Sato, T; et al. (1999). "Transgenic mice harboring a full-length human mutant DRPLA gene exhibit age-dependent intergenerational and somatic instabilities of CAG repeats comparable with those in DRPLA patients". Hum Mol Genet. 8 (1): 99–106. doi:10.1093/hmg/8.1.99. PMID 9887337.
  11. ^ Sato, T; et al. (1999). "Transgenic mice harboring a full-length human DRPLA gene with highly expanded CAG repeats exhibit severe disease phenotype". Am J Hum Genet. 65 (suppl): A30.
  12. ^ Schilling, G; et al. (1999). "Nuclear accumulation of truncated atrophin-1 fragments in a transgenic mouse model of DRPLA". Neuron. 24 (1): 275–86. doi:10.1016/S0896-6273(00)80839-9. PMID 10677044.
  13. ^ a b c d e f g Yamada, M; et al. (2008). "CAG repeat disorder models and human neuropathology: similarities and differences". Acta Neuropathol. 115 (1): 71–86. doi:10.1007/s00401-007-0287-5. PMID 17786457. S2CID 25796375.
  14. ^ a b c Sakai, K; et al. (2006). "Neuronal Atrophy and Synaptic Alteration in a Mouse Model of Dentatorubral–pallidoluysian Atrophy". Brain. 129 (Pt 9): 2353–62. doi:10.1093/brain/awl182. hdl:2297/19183. PMID 16891319.
  15. ^ Naito H, Oyanagi S (1982). "Familial myoclonus epilepsy and choreoathetosis: hereditary dentatorubral–pallidoluysian atrophy". Neurology. 32 (8): 798–807. doi:10.1212/wnl.32.8.798. PMID 6808417. S2CID 37169746.
  16. ^ Mackie S, Aitken A (2005). "Novel brain 14-3-3 interacting proteins involved in neurodegenerative disease". FEBS. 272 (16): 4202–10. doi:10.1111/j.1742-4658.2005.04832.x. PMID 16098201. S2CID 27027519.
  17. ^ Hayashi, Y; et al. (1998). "Hereditary dentatorubral–pallidoluysian atrophy: Detection of widespread ubiquitinated neuronal and glial intranuclear inclusions in the brain". Acta Neuropathol. 96 (6): 547–52. doi:10.1007/s004010050933. PMID 9845282. S2CID 12861680.
  18. ^ Yamada, M; et al. (2001). "Interaction between Neuronal Intranuclear Inclusions and Promyelocytic Leukemia Protein Nuclear and Coiled Bodies in CAG Repeat Diseases". Am J Pathol. 159 (5): 1785–95. doi:10.1016/S0002-9440(10)63025-8. PMC 1867069. PMID 11696439.
  19. ^ Yamada, M; et al. (2001). "Widespread occurrence of intranuclear atrophin-1 accumulation in the central nervous system neurons of patients with dentatorubral–pallidoluysian atrophy". Ann Neurol. 49 (1): 14–23. doi:10.1002/1531-8249(200101)49:1<14::AID-ANA5>3.0.CO;2-X. PMID 11198291. S2CID 37415413.
  20. ^ Shimohata, T; et al. (2000). "Expanded polyglutamine stretches interact with TAFII130, interfering with CREB-dependent transcription". Nat Genet. 26 (1): 29–36. doi:10.1038/79139. PMID 10973244. S2CID 22949605.
  21. ^ a b c Woulfe, JM (2007). "Abnormalities of the nucleus and nuclear inclusions in neurodegenerative disease: a work in progress". Neuropathol Appl Neurobiol. 33 (1): 2–42. doi:10.1111/j.1365-2990.2006.00819.x. PMID 17239006. S2CID 43663416.
  22. ^ Takahashi-Fujigasaki, J; et al. (2006). "SUMOylation substrates in neuronal intranuclear inclusion disease". Neuropathol Appl Neurobiol. 32 (1): 92–100. doi:10.1111/j.1365-2990.2005.00705.x. PMID 16409557. S2CID 36501485.
  23. ^ Takahashi, J; et al. (2002). "Two populations of neuronal intranuclear inclusions in SCA7 differ in size and promyelocytic leukaemia protein content". Brain. 125 (7): 1534–43. doi:10.1093/brain/awf154. PMID 12077003.
  24. ^ Yamada, M; et al. (2000). "Ubiquitinated filamentous inclusions in cerebellar dentate nucleus neurons in dentatorubral–pallidoluysian atrophy contain expanded polyglutamine stretches". Acta Neuropathol. 99 (6): 615–8. doi:10.1007/s004010051171. PMID 10867794. S2CID 19300464.
  25. ^ Takahashi, J; et al. (2001). "Neuronal nuclear alterations in dentatorubral–pallidoluysian atrophy: ultrastructural and morphometric studies of the cerebellar granule cells". Brain Res. 919 (1): 12–9. doi:10.1016/S0006-8993(01)02986-9. PMID 11689158. S2CID 30439704.
  26. ^ Burke, JR; et al. (1994). "Dentatorubral–pallidoluysian atrophy and Haw River Syndrome". Lancet. 344 (8938): 1711–2. doi:10.1016/S0140-6736(94)90497-9. PMID 7996992. S2CID 43014713.
  27. ^ Takano, H; et al. (1998). "Close associations between prevalences of dominantly inherited spinocerebellar ataxias with CAG-repeat expansions and frequencies of large normal CAG alleles in Japanese and Caucasian populations". Am J Hum Genet. 63 (4): 1060–6. doi:10.1086/302067. PMC 1377499. PMID 9758625.

External links edit

April 12, 2024
dentatorubral, pallidoluysian, atrophy, drpla, autosomal, dominant, spinocerebellar, degeneration, caused, expansion, repeat, encoding, polyglutamine, tract, atrophin, protein, also, known, river, syndrome, naito, oyanagi, disease, although, this, condition, p. Dentatorubral pallidoluysian atrophy DRPLA is an autosomal dominant spinocerebellar degeneration caused by an expansion of a CAG repeat encoding a polyglutamine tract in the atrophin 1 protein 1 It is also known as Haw River Syndrome and Naito Oyanagi disease Although this condition was perhaps first described by Smith et al in 1958 and several sporadic cases have been reported from Western countries this disorder seems to be very rare except in Japan citation needed Dentatorubral pallidoluysian atrophyDentatorubral pallidoluysian atrophy is inherited in an autosomal dominant manner SpecialtyNeurology There are at least eight neurodegenerative diseases that are caused by expanded CAG repeats encoding polyglutamine polyQ stretches see Trinucleotide repeat disorder The expanded CAG repeats create an adverse gain of function mutation in the gene products Of these diseases DRPLA is most similar to Huntington s disease citation needed Contents 1 Signs and symptoms 2 Genetics 2 1 Atrophin 1 2 2 Transgenic mouse models 3 Pathology 3 1 Brain atrophy 3 2 Neuronal intranuclear inclusions 3 3 Diffuse accumulation in the nuclei 4 Diagnosis 5 Management 6 Epidemiology 7 References 8 External linksSigns and symptoms editDRPLA can be juvenile onset lt 20 years early adult onset 20 40 years or late adult onset gt 40 years Late adult onset DRPLA is characterized by ataxia choreoathetosis and dementia Early adult onset DRPLA also includes seizures and myoclonus Juvenile onset DRPLA presents with ataxia and symptoms consistent with progressive myoclonus epilepsy 2 myoclonus multiple seizure types and dementia Other symptoms that have been described include cervical dystonia 3 corneal endothelial degeneration 4 autism and surgery resistant obstructive sleep apnea 5 Genetics editThe human genome contains two atrophin genes DRPLA has been correlated to the expansion of the polyglutamine region of the atrophin 1 gene on chromosome 12p13 3 6 A normal number of CAG repeats in the atrophin 1 gene is 7 34 affected individuals display 49 93 repeats DRPLA displays anticipation earlier age of onset for subsequent generations and an inverse correlation between the size of the expanded CAG repeat and the age of symptom onset Paternal transmission results in more prominent anticipation 26 29 years than maternal transmission 14 15 years 2 Atrophin 1 edit Atrophin 1 ATN1 encodes a hydrophilic 1184 amino acid protein with several repetitive motifs including a serine rich region a variable length polyglutamine tract a polyproline tract and a region of alternating acidic and basic residues It contains a putative nuclear localization signal in the N terminus of the protein and a putative nuclear export signal in the C terminus 7 ATN1 is ubiquitously expressed in all tissues but proteolytically cleaved in neuronal cells The function of ATN1 is not clear however it is believed to be a transcriptional co repressor ATN1 and atrophin 2 can be co immunoprecipitated indicating that they may carry out some functions together in a molecular complex 8 Atrophin 1 may be a dispensable or redundant protein as mice bred with a null allele for atrophin 1 produce viable and fertile offspring and show no compensatory upregulation of atrophin 2 9 Transgenic mouse models edit Mouse models of DRPLA have been successfully generated which demonstrate the same intergenerational instability and severe phenotype as human DRPLA 10 11 12 The Schilling mice express full length human atrophin 1 with 65 CAG repeats under transcriptional control of the mouse prion protein promoter The mice demonstrated progressive ataxia tremors abnormal movements seizures and premature death Like in human brains nuclear accumulation was demonstrated and occasional NIIs were visualised but the NIIs did not stain for ubiquitin and no neuronal loss was seen 13 The Sato mice harbored a single copy of full length human atrophin 1 with 76 or 129 CAG repeats The hemizygous transgenic offspring of the Q129 mice exhibited symptoms similar to juvenile type DRPLA such as myoclonus and seizures Again neuronal atrophy was noted but no neuronal loss until death Diffuse accumulation in the nuclei began on post natal day 4 and ubiquitinated NII formation was detectable at 9 weeks of age No PML bodies were found to be associated with the NIIs which were morphologically mildly altered from those seen in human neural cells 13 14 Pathology editDRPLA is characterized by marked generalized brain atrophy and the accumulation of atrophin 1 with expanded glutamine stretches Mutant atrophin 1 proteins have been found in neuronal intranuclear inclusions NII and diffusely accumulated in the neuronal nuclei While the role of NIIs pathologic or protective is unclear the diffuse accumulation of mutant protein is regarded as toxic citation needed Brain atrophy edit There is significant reduction in CNS tissue throughout the brain and spinal cord with brain weights of DRPLA patients often becoming less than 1000g 15 In regions lacking obvious neuronal depletion atrophy of the neuropil is noted The globus pallidus lateral greater than medial segment and subthalamic nucleus demonstrate consistent neuronal loss and astrocytic gliosis The dentate nucleus shows neuronal loss with the remaining atrophic neurons exhibiting grumose degeneration In general the pallidoluysian degeneration is more severe than the dentatorubral degeneration in juvenile onset and the reverse is true for the late adult onset 13 Transgenic DRPLA mice demonstrated several neuronal abnormalities including a reduction in the number and size of dendritic spines as well as in the area of perikarya and diameter of dendrites 14 Spine morphology and density have been linked to learning and memory functions as well as epilepsy The stubby type spines seen in DRPLA mice are morphologically different from the thin and mushroom type spines seen in Huntington s mice citation needed Morphometric analysis of DRPLA mouse brains has shown a loss of normal inter microtubule spacing in neuronal axons The microtubules were relatively compacted suggesting abnormalities in protein transport may play a role in neuronal degeneration 14 In humans atrophin 1 interacts with IRSp53 which interacts with Rho GTPases to regulate the organization of the actin cytoskeleton and the pathways that regulate lamellipodia and filopodia 16 Neuronal intranuclear inclusions edit NIIs are not exclusive to DRPLA they have been found in a variety of neurodegenerative disorders In DRPLA NIIs have been demonstrated in both neurons and glial cells in the striatum pontine nuclei inferior olive cerebellar cortex and dentate nucleus 17 though the incidence of neurons with NIIs is low roughly 1 3 13 In DRPLA the NIIs are spherical eosinophilic structures of various sizes They are non membrane bound and are composed of both granular and filamentous structures They are ubiquitinated and may be paired or in doublet form within the nucleus 18 NIIs are immunopositive for several transcription factors such as TATA binding protein TBP TBP associated factor TAFII130 Sp1 camp responsive element binding protein CREB and CREB binding protein CBP 19 20 It has been proposed that recruitment of transcription factors into NIIs may induce transcriptional abnormalities that contribute to progressive neuronal degeneration 13 Other polyQ disorders such as Huntington s and spinocerebellar ataxia types 3 and 7 have been demonstrated to sequester some of the same transcriptions factors That different gene products sequester the same transcription factors may contribute to the overlapping symptoms of genetically different diseases 21 NIIs have also been demonstrated to alter the distribution of the intranuclear structures such as promyelocytic leukemia protein PML nuclear bodies Although the role of PML bodies is unclear they are believed to be involved in apoptosis In neurons with NII PML bodies in DRPLA patients form a shell or ring around the ubiquitinated core 13 21 In similar polyQ diseases the association of this PML shell has been shown to be size dependent with larger NIIs being PML negative 22 23 This has led to two models one in which PML bodies represent sites for NII formation and a second in which PML bodies are involved in degradation and proteolysis of NIIs 21 Filementous atrophin 1 positive inclusions are also observed exclusively in the cytoplasm of the dentate nucleus which are extremely similar to the inclusions observed in the motor neurons in amyotrophic lateral sclerosis 24 Diffuse accumulation in the nuclei edit In DRPLA diffuse accumulation of mutant ATN1 occurs far more extensively than NII formation The extent and frequency of neurons showing the diffuse nuclear accumulations changes depending on CAG repeat length It is believed that the diffuse nuclear accumulations contribute to the clinical features such as dementia and epilepsy citation needed ATN1 contains both a nuclear localization sequence and a nuclear export sequence Cleavage of ATN1 to an N terminal fragment relieves ATN1 of its nuclear export signal and concentrates it in the nucleus Increased nuclear concentrations have been demonstrated via transfection assay to enhance cellular toxicity 7 In both the juvenile and adult forms regions in which more than 40 of neurons became immunoreactive to 1C2 a monoclonal antibody against expanded polyglutamine stretches included the nucleus basalis of Meynert large striatal neurons globus pallidus subthalamic nucleus thalamic intralaminar nucleus lateral geniculate body oculomotor nucleus red nucleus substantia nigra trigeminal motor nucleus nucleus raphes pontis pontine nuclei vestibular nucleus inferior olive and the cerebellar dentate nucleus The juvenile type also shows reactivity in the cerebral cortex hippocampal CA1 area and the reticular formation of the brainstem 13 Nuclei containing accumulations of mutant atrophin 1 are deformed with nuclear membrane indentations 25 Diagnosis editDiagnosis of DRPLA rests on positive family history clinical findings and genetic testing Family history can be difficult to obtain if a relative was misdiagnosed died young or experiences late onset of symptoms citation needed Other diseases in the differential diagnosis of adult onset DRPLA include Huntington s and the spinocerebellar ataxias For juvenile onset disease familial essential myoclonus and epilepsy FEME Lafora Unverricht Lundborg Neuroaxonal dystrophy Gaucher s disease Sialidosis and Galactosialidosis should be considered citation needed Management editTo quantify the extent of the disease an MRI EEG and neuropsychological testing are recommended Seizures are treated with anticonvulsants and psychiatric disturbances with psychotropic medications Physical therapy has also been recommended to maintain function as the condition progresses and occupational therapy to focus on activities of daily living advice for careers and adaptation to the environment citation needed Epidemiology editThe prevalence of DRPLA in the Japanese population is believed to be 2 7 in 1 000 000 DRPLA is observed relatively less frequently in other ethnic populations and an analysis of normal ATN1 alleles has demonstrated that CAG repeat lengths greater than 17 are significantly more frequent in the Japanese population 26 27 References edit Kanazawa I June 1999 Molecular pathology of dentatorubral pallidoluysian atrophy Philos Trans R Soc Lond B Biol Sci 354 1386 1069 74 doi 10 1098 rstb 1999 0460 PMC 1692599 PMID 10434307 a b Tsuji S 1999 Dentatorubral pallidoluysian atrophy Clinical features and molecular genetics Adv Neurol 79 399 409 PMID 10514829 Hatano T et al 2003 Cervical dystonia in dentatorubral pallidoluysian atrophy Acta Neurol Scand 108 4 287 9 doi 10 1034 j 1600 0404 2003 00150 x PMID 12956864 S2CID 8681273 Ito D et al 2002 Corneal endothelial degeneration in dentatorubral pallidoluysian atrophy Arch Neurol 59 2 289 91 doi 10 1001 archneur 59 2 289 PMID 11843701 Licht D Lynch D 2002 Juvenile Dentatorubral Pallidoluysian Atrophy New Clinical Features Pediatr Neurol 26 1 51 4 doi 10 1016 S0887 8994 01 00346 0 PMID 11814736 Yazawa I et al 1995 Abnormal Gene Product Identified in Hereditary DRPLA Brain Nat Genet 10 1 99 103 doi 10 1038 ng0595 99 PMID 7647802 S2CID 5850726 a b Nucifora F et al 2003 Nuclear localization of a Non caspase Truncation Product of Atrophin 1 with an Expanded Polyglutamine Repeat Increases Cellular Toxicity J Biol Chem 278 15 13047 55 doi 10 1074 jbc M211224200 PMID 12464607 Zoltewicz J et al 2004 Atrophin 2 recruits histone deacetylase and is required for the function of multiple signaling centers during mouse embryogenesis Development 131 1 3 14 doi 10 1242 dev 00908 PMID 14645126 Shen Y et al 2007 Functional Architecture of Atrophins J Biol Chem 282 7 5037 44 doi 10 1074 jbc M610274200 PMID 17150957 Sato T et al 1999 Transgenic mice harboring a full length human mutant DRPLA gene exhibit age dependent intergenerational and somatic instabilities of CAG repeats comparable with those in DRPLA patients Hum Mol Genet 8 1 99 106 doi 10 1093 hmg 8 1 99 PMID 9887337 Sato T et al 1999 Transgenic mice harboring a full length human DRPLA gene with highly expanded CAG repeats exhibit severe disease phenotype Am J Hum Genet 65 suppl A30 Schilling G et al 1999 Nuclear accumulation of truncated atrophin 1 fragments in a transgenic mouse model of DRPLA Neuron 24 1 275 86 doi 10 1016 S0896 6273 00 80839 9 PMID 10677044 a b c d e f g Yamada M et al 2008 CAG repeat disorder models and human neuropathology similarities and differences Acta Neuropathol 115 1 71 86 doi 10 1007 s00401 007 0287 5 PMID 17786457 S2CID 25796375 a b c Sakai K et al 2006 Neuronal Atrophy and Synaptic Alteration in a Mouse Model of Dentatorubral pallidoluysian Atrophy Brain 129 Pt 9 2353 62 doi 10 1093 brain awl182 hdl 2297 19183 PMID 16891319 Naito H Oyanagi S 1982 Familial myoclonus epilepsy and choreoathetosis hereditary dentatorubral pallidoluysian atrophy Neurology 32 8 798 807 doi 10 1212 wnl 32 8 798 PMID 6808417 S2CID 37169746 Mackie S Aitken A 2005 Novel brain 14 3 3 interacting proteins involved in neurodegenerative disease FEBS 272 16 4202 10 doi 10 1111 j 1742 4658 2005 04832 x PMID 16098201 S2CID 27027519 Hayashi Y et al 1998 Hereditary dentatorubral pallidoluysian atrophy Detection of widespread ubiquitinated neuronal and glial intranuclear inclusions in the brain Acta Neuropathol 96 6 547 52 doi 10 1007 s004010050933 PMID 9845282 S2CID 12861680 Yamada M et al 2001 Interaction between Neuronal Intranuclear Inclusions and Promyelocytic Leukemia Protein Nuclear and Coiled Bodies in CAG Repeat Diseases Am J Pathol 159 5 1785 95 doi 10 1016 S0002 9440 10 63025 8 PMC 1867069 PMID 11696439 Yamada M et al 2001 Widespread occurrence of intranuclear atrophin 1 accumulation in the central nervous system neurons of patients with dentatorubral pallidoluysian atrophy Ann Neurol 49 1 14 23 doi 10 1002 1531 8249 200101 49 1 lt 14 AID ANA5 gt 3 0 CO 2 X PMID 11198291 S2CID 37415413 Shimohata T et al 2000 Expanded polyglutamine stretches interact with TAFII130 interfering with CREB dependent transcription Nat Genet 26 1 29 36 doi 10 1038 79139 PMID 10973244 S2CID 22949605 a b c Woulfe JM 2007 Abnormalities of the nucleus and nuclear inclusions in neurodegenerative disease a work in progress Neuropathol Appl Neurobiol 33 1 2 42 doi 10 1111 j 1365 2990 2006 00819 x PMID 17239006 S2CID 43663416 Takahashi Fujigasaki J et al 2006 SUMOylation substrates in neuronal intranuclear inclusion disease Neuropathol Appl Neurobiol 32 1 92 100 doi 10 1111 j 1365 2990 2005 00705 x PMID 16409557 S2CID 36501485 Takahashi J et al 2002 Two populations of neuronal intranuclear inclusions in SCA7 differ in size and promyelocytic leukaemia protein content Brain 125 7 1534 43 doi 10 1093 brain awf154 PMID 12077003 Yamada M et al 2000 Ubiquitinated filamentous inclusions in cerebellar dentate nucleus neurons in dentatorubral pallidoluysian atrophy contain expanded polyglutamine stretches Acta Neuropathol 99 6 615 8 doi 10 1007 s004010051171 PMID 10867794 S2CID 19300464 Takahashi J et al 2001 Neuronal nuclear alterations in dentatorubral pallidoluysian atrophy ultrastructural and morphometric studies of the cerebellar granule cells Brain Res 919 1 12 9 doi 10 1016 S0006 8993 01 02986 9 PMID 11689158 S2CID 30439704 Burke JR et al 1994 Dentatorubral pallidoluysian atrophy and Haw River Syndrome Lancet 344 8938 1711 2 doi 10 1016 S0140 6736 94 90497 9 PMID 7996992 S2CID 43014713 Takano H et al 1998 Close associations between prevalences of dominantly inherited spinocerebellar ataxias with CAG repeat expansions and frequencies of large normal CAG alleles in Japanese and Caucasian populations Am J Hum Genet 63 4 1060 6 doi 10 1086 302067 PMC 1377499 PMID 9758625 External links edit Retrieved from https en wikipedia org w index php title Dentatorubral pallidoluysian atrophy amp oldid 1216632889, 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