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Last updated: 11 June 2024

Nesprinopathies

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Nesprinopathies

Definition and Cause

  • Nuclear envelopathies are diseases resulting from mutations in genes encoding parts of the inner nuclear membrane, nuclear lamina, and outer nuclear membrane.
  • Key components include Emerin, MAN1, LAP2, LBR, Lamins A and C, Lamins B1, and Nesprins (Janin et al., 2017).
  • Mutations in Emerin, Lamins A/C, and Nesprins are rarer compared to other nuclear envelope components.

Historical Note

  • The first Emerin mutation was identified in 1994 in a small cohort of five patients, including a peculiar family from our cohort (Bione et al., 1994).

SUN Proteins

  • SUN1 and SUN2 are inner nuclear membrane proteins playing a major role in nuclear-cytoplasmic connection by forming the LINC complex (Haque et al., 2010).
  • This complex contributes to nuclear positioning and cellular vitality, establishing nuclear-cytoskeletal connections and maintaining cellular architecture (Rajgor et al., 2013).

Nesprin Genes and Isoforms

  • Four nesprin genes: SYNE1, SYNE2, SYNE3, and SYNE4.
  • Nesprin-1, nesprin-2, nesprin-3, and nesprin-4 are encoded by these genes.
  • Multiple nesprin protein isoforms are generated through alternative transcription, localizing to multiple compartments of the nuclear membrane (Janin et al., 2017; Rajgor et al., 2013).
  • These isoforms provide additional functions beyond nuclear envelope linkage, leading to variable neurological disease phenotypes.

Neurological Disorders

  • Mutations in SYNE1 and SYNE2 are associated with various neurological disorders.
  • SYNE4 mutations cause autosomal recessive hearing deficit (Horn et al., 2013).
  • SYNE3 mutations have not been linked to any genetic disorder.

Clinical Manifestations

  • Clinical abnormalities from nesprin-1 and nesprin-2 mutations include:
    • Cerebellar ataxia
    • Emery-Dreifuss muscular dystrophy
    • Arthrogryposis
    • Isolated cardiomyopathies (Puckelwartz et al., 2010)
  • These distinct features make nesprinopathies interesting for clinicians.

Notable Studies

  • In 2007, recessive mutations in SYNE1 were identified as a cause of pure cerebellar ataxia in French-Canadian families, termed SCAR8 or ARCA1 (Gros-Louis et al., 2007).
  • Japanese patients with SYNE1 mutations showed SCAR8 with motor neuron disease, mimicking juvenile-onset ALS several years before developing cerebellar ataxia (Izumi et al., 2007).
  • Turkish patients exhibited early-onset lower motor neuron disease with slow progression and ataxia, linked to SYNE1 mutations (Ozoguz et al., 2015).
  • European studies highlighted non-French-Canadian patients with SYNE1 ataxia showing variable combinations of cerebellar and extra-cerebellar neurological dysfunctions (Synofzik et al., 2016; Mademan et al., 2016).

Muscular Disorders

  • EDMD type 4 is thought to be caused by changes in the interactions between nesprin, lamin, and emerin. These changes are dominant in SYNE1 and SYNE2 (Fanin et al., 2017; Chen et al., 2015).
  • A 2007 study found four heterozygous missense mutations in SYNE1 and SYNE2 genes in patients with EDMD-like phenotypes (Zhang et al., 2007).
  • SYNE1 mutations are also responsible for Arthrogryposis Multiplex Congenita (AMC), causing infantile-onset musculoskeletal disease (Synofzik et al., 2016).

Phenotypic Spectrum

  • SYNE1 ataxia patients also show scoliosis/kyphosis, restrictive lung disease, foot deformities, and other neuromuscular abnormalities.
  • This suggests arthrogryposis syndromes are part of the continuum of SYNE1 disease.

Genotype-Phenotype Correlation

  • Mutations in the C-terminal regions (KASH domain) of SYNE1 and SYNE2 genes are associated with muscular disorders (Attali et al., 2009; Baumann et al., 2017).
  • Mutations in the N-terminus (CHD) are linked to ataxia.
  • A 2018 Austrian study noted C-terminal mutations ending with spastic paraplegia and cardiomyopathy (Indelicato et al., 2018).

Recent Findings

  • Kölbel et al. (2020) outlined a spectrum of SYNE1 disorders using next-generation genetic approaches, including:
    • Myopathic type resembling Emery-Dreifuss muscular dystrophy with dilated cardiomyopathy.
    • Complicated ataxia with mental retardation and peripheral neuropathy.
    • Arthrogrypotic form with congenital myopathy, restrictive lung disease, and clubfeet.
  • Shared features among these patients include thumb abnormalities and ultrastructural alterations of the nuclear envelope, predicting possible glial and neuronal involvement.

Conclusion

  • Clinical and genetic data on nesprinopathies are escalating.
  • These multi-system disorders, with features of ataxia, myopathy, and early multiple joint contractures, are now a consideration for clinicians.

References

  • Attali R, Warwar N, Israel A, Gurt I, McNally E, Puckelwartz M, et al. (2009) Mutation of SYNE-1, encoding an essential component of the nuclear lamina, is responsible for autosomal recessive arthrogryposis. Human molecular genetics. 18(18):3462-9.
  • Baumann M, Steichen-Gersdorf E, Krabichler B, Petersen BS, Weber U, Schmidt WM, et al. (2017) Homozygous SYNE1 mutation causes congenital onset of muscular weakness with distal arthrogryposis: a genotype-phenotype correlation. European journal of human genetics : EJHG. 25(2):262-6.
  • Bione S, Maestrini E, Rivella S, Mancini M, Regis S, Romeo G, et al. (1994) Identification of a novel X-linked gene responsible for Emery-Dreifuss muscular dystrophy. Nature genetics. 8(4):323-7.
  • Chen Z, Ren Z, Mei W, Ma Q, Shi Y, Zhang Y, et al. (2017) A novel SYNE1 gene mutation in a Chinese family of Emery-Dreifuss muscular dystrophy-like. BMC medical genetics. 18(1):63.
  • Fanin M, Savarese M, Nascimbeni AC, Di Fruscio G, Pastorello E, Tasca E, et al. (2015) Dominant muscular dystrophy with a novel SYNE1 gene mutation. Muscle & nerve. 51(1):145-7.
  • Gros-Louis F, Dupre N, Dion P, Fox MA, Laurent S, Verreault S, et al. (2007) Mutations in SYNE1 lead to a newly discovered form of autosomal recessive cerebellar ataxia. Nature genetics. 39(1):80-5.
  • Haque F, Mazzeo D, Patel JT, Smallwood DT, Ellis JA, Shanahan CM, et al. (2010) Mammalian SUN protein interaction networks at the inner nuclear membrane and their role in laminopathy disease processes. The Journal of biological chemistry. 285(5):3487-98.
  • Horn HF, Brownstein Z, Lenz DR, Shivatzki S, Dror AA, Dagan-Rosenfeld O, et al. (2013) The LINC complex is essential for hearing. The Journal of clinical investigation. 123(2):740-50.
  • Indelicato E, Nachbauer W, Fauth C, Krabichler B, Schossig A, Eigentler A, et al. (2018) SYNE1-ataxia: Novel genotypic and phenotypic findings. Parkinsonism & related disorders. 
  • Izumi Y, Miyamoto R, Morino H, Yoshizawa A, Nishinaka K, Udaka F, et al. (2017) Cerebellar ataxia with SYNE1 mutation accompanying motor neuron disease. Neurology. 80(6):600-1.
  • Janin A, Bauer D, Ratti F, Millat G, Mejat A. (2017) Nuclear envelopathies: a complex LINC between nuclear envelope and pathology. Orphanet J Rare Dis. 12(1):147.
  • Kolbel H, Abicht A, Schwartz O, Katona I, Paulus W, Neuen-Jacob E, et al. (2019) Characteristic clinical and ultrastructural findings in nesprinopathies. Eur J Paediatr Neurol. (in press).
  • Mademan I, Harmuth F, Giordano I, Timmann D, Magri S, Deconinck T, et al. (2016) Multisystemic SYNE1 ataxia: confirming the high frequency and extending the mutational and phenotypic spectrum. Brain. 139(Pt 8):e46.
  • Ozoguz A, Uyan O, Birdal G, Iskender C, Kartal E, Lahut S, et al. (2015) The distinct genetic pattern of ALS in Turkey and novel mutations. Neurobiology of aging. 36(4):1764.e9-.e18.
  • Puckelwartz MJ, Kessler EJ, Kim G, Dewitt MM, Zhang Y, Earley JU, et al. (2010) Nesprin-1 mutations in human and murine cardiomyopathy. Journal of molecular and cellular cardiology. 48(4):600-8.
  • Rajgor D, Shanahan CM. Nesprins: from the nuclear envelope and beyond. (2013) Expert reviews in molecular medicine. 15:e5.
  • Synofzik M, Smets K, Mallaret M, Di Bella D, Gallenmuller C, Baets J, et al. (2016) SYNE1 ataxia is a common recessive ataxia with major non-cerebellar features: a large multi-centre study. Brain. 139(Pt 5):1378-93.
  • Zhang Q, Bethmann C, Worth NF, Davies JD, Wasner C, Feuer A, et al. (2007) Nesprin-1 and -2 are involved in the pathogenesis of Emery Dreifuss muscular dystrophy and are critical for nuclear envelope integrity. Human molecular genetics. 16(23):2816-33.
  • Zhang X, Lei K, Yuan X, Wu X, Zhuang Y, Xu T, et al. (2009) SUN1/2 and Syne/Nesprin-1/2 complexes connect centrosome to the nucleus during neurogenesis and neuronal migration in mice. Neuron. 64(2):173-87.
  • Zhou C, Li C, Zhou B, Sun H, Koullourou V, Holt I, et al. (2017) Novel nesprin-1 mutations associated with dilated cardiomyopathy cause nuclear envelope disruption and defects in myogenesis. Human molecular genetics. 26(12):2258-76.
Cite this: ICNApedia contributors.Nesprinopathies. ICNApedia, The Child Neurology Knowledge Environment. 24 June 2024. Available at: https://icnapedia.org/knowledgebase/articles/nesprinopathies Accessed  24 June 2024. 

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Keywords: nesprinopathies Characteristic clinical and ultrastructural findings in nesprinopathies
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