About the Authors:
Marka van Blitterswijk
* E-mail: [email protected]
Affiliation: Department of Neurology, Rudolf Magnus Institute of Neuroscience, University Medical Center Utrecht, Utrecht, The Netherlands
Lotte Vlam
Affiliation: Department of Neurology, Rudolf Magnus Institute of Neuroscience, University Medical Center Utrecht, Utrecht, The Netherlands
Michael A. van Es
Affiliation: Department of Neurology, Rudolf Magnus Institute of Neuroscience, University Medical Center Utrecht, Utrecht, The Netherlands
W-Ludo van der Pol
Affiliation: Department of Neurology, Rudolf Magnus Institute of Neuroscience, University Medical Center Utrecht, Utrecht, The Netherlands
Eric A. M. Hennekam
Affiliation: Department of Medical Genetics, University Medical Center Utrecht, Utrecht, The Netherlands
Dennis Dooijes
Affiliation: Department of Medical Genetics, University Medical Center Utrecht, Utrecht, The Netherlands
Helenius J. Schelhaas
Affiliation: Department of Neurology, Donders Institute for Brain, Cognition and Behavior, Radboud University Nijmegen Medical Center, Nijmegen, The Netherlands
Anneke J. van der Kooi
Affiliation: Department of Neurology, Academic Medical Center, University of Amsterdam, Amsterdam, The Netherlands
Marianne de Visser
Affiliation: Department of Neurology, Academic Medical Center, University of Amsterdam, Amsterdam, The Netherlands
Jan H. Veldink
Contributed equally to this work with: Jan H. Veldink, Leonard H. van den Berg
Affiliation: Department of Neurology, Rudolf Magnus Institute of Neuroscience, University Medical Center Utrecht, Utrecht, The Netherlands
Leonard H. van den Berg
Contributed equally to this work with: Jan H. Veldink, Leonard H. van den Berg
Affiliation: Department of Neurology, Rudolf Magnus Institute of Neuroscience, University Medical Center Utrecht, Utrecht, The Netherlands
Introduction
Motor neuron diseases (MNDs) are a heterogeneous group of disorders characterized by muscle weakness and/or spasticity due to degeneration of motor neurons. Progressive muscular atrophy (PMA) refers to a subgroup of the MND patients with rapidly or gradually developing muscle weakness. PMA accounts for 5–10% of adult-onset MNDs, and is caused by a progressive loss of lower motor neurons (LMNs) [1], [2]. Differentiation of PMA from amyotrophic lateral sclerosis (ALS) is important, since the median survival of patients with PMA is significantly longer than that of patients with ALS [3].
The etiology of MNDs is complex. Most of the ALS cases, for instance, are sporadic in nature and thought to be caused by an interaction of genetic and environmental factors [4]. Currently, many genes appear to be involved in the pathogenesis of ALS, including chromosome 9 open reading frame 72 (C9orf72), superoxide dismutase-1 (SOD1), angiogenin (ANG), fused in sarcoma/translated in liposarcoma (FUS/TLS), TAR DNA-binding protein 43 (TARDBP/TDP-43), vesicle-associated membrane protein B (VAPB), optineurin (OPTN), valosin-containing protein (VCP), ubiquilin-2 (UBQLN2), sequestosome-1 (SQSTM1), and profilin-1 (PFN1) [5], [6], [7], [8], [9], [10], [11]. We have recently shown that C9orf72 repeat expansions can also be detected in apparently sporadic PMA, but at a lower frequency (1.6%) than in apparently sporadic ALS (6.1%) [12]. Moreover, we have demonstrated that mutations in four major MND-associated genes, SOD1, ANG, FUS/TLS and TARDBP, account for less than two percent of the sporadic ALS cases [13]. The combined mutation frequency of these four MND-associated genes is unknown for sporadic PMA patients. Mutations in charged multivesicular body protein 2B (CHMP2B) have, however, been reported in sporadic PMA patients [14], [15].
The objective of this study is to determine the mutation frequency of major MND-associated genes in patients with apparently sporadic PMA. We compared their mutation frequencies to those in a large cohort of patients with apparently sporadic ALS, revealing a genetic overlap.
Materials and Methods
Patient Selection
We included 261 patients with apparently sporadic PMA and screened their DNA for mutations in SOD1, ANG, FUS/TLS, TARDBP, and CHMP2B. PMA patients had already been screened for mutations in transient receptor potential vanilloid 4 (TRPV4) and repeat expansions in C9orf72 [12], [16]. Their diagnosis was based on LMN involvement on clinical and electrophysiological examination at time of referral. We excluded patients with a family history of PMA, a history of acute poliomyelitis, spinal radiculopathy, diabetic amyotrophy, thyrotoxicosis, or hyperparathyroidism, clinical signs of upper motor neuron (UMN) involvement, sensory signs on neurological examination, structural lesions on magnetic resonance imaging or computed tomography of head and spine, and motor conduction block on extensive standardized nerve conduction studies [2].
Cohorts of sporadic ALS patients had already been screened for mutations in SOD1 (N = 451), ANG (N = 941), FUS/TLS (N = 1,192), TARDBP (N = 1,192), and C9orf72 (N = 1,422) [12], [13], [17], [18], [19]. We screened 1,002 sporadic ALS patients for mutations in CHMP2B. ALS patients were recruited through the Dutch Prospective Population-based ALS registry; they were diagnosed according to the El Escorial Criteria at national referral centers for neuromuscular diseases (University Medical Center Utrecht, Academic Medical Center Amsterdam, or Radboud University Nijmegen Medical Center) [20], [21].
Mutations in SOD1 (N = 1,894), ANG (N = 1,582), FUS/TLS (N = 970), and TARDBP (N = 1,415) had previously been reported in Dutch control subjects [13], [18], [19]. We screened a total of 750 control subjects of Dutch descent for mutations in CHMP2B.
Ethics Statement
All material was obtained with approval of the medical ethics committee for research in humans of the University Medical Center Utrecht, The Netherlands, and all participants gave written informed consent.
Genetic Analysis
Coding regions of SOD1 (NM_000454.4), ANG (NM_001145.4), FUS/TLS (NM_004960.3, exon 5, 6, 14, 15), TARDBP (NM_007375.3, exon 6), and CHMP2B (NM_014043.3) were screened for mutations using touchdown PCR, as described previously [13], [22]. Sanger sequencing and data analysis were performed with BigDye Terminator 3.1 sequencing kit (Applied Biosystems, Foster City, California), DNA Analyzer 3730XL (Applied Biosystems) and PolyPhred [23]. Each mutation was confirmed on genomic DNA and its impact on the structure, and function of the protein was predicted with PolyPhen-2 (PolyPhen-2 version 2.1.0; http://genetics.bwh.harvard.edu/pph2/) and PMut (http://mmb.pcb.ub.es/PMut/PMut.jsp).
Genealogical Analysis
Lists of descendants were compiled for index patients. Based on these lists, civil records/registers, and church records of the Dutch population, pedigrees were generated (containing two parents, four grandparents, eight great-grandparents, etc.). This information was then used to determine whether index patients were related, and detailed family trees were constructed.
Haplotype Analysis
Extended haplotype analysis, using six extragenic polymorphic markers flanking TARDBP (D1S1612, D1S503, D1S244 proximal of TARDBP, and D1S2667, D1S2740 and D1S1597 distal of TARDBP), was performed to construct a haplotype segregating with the identified p.N352S mutation in TARDBP. Validity of the constructed haplotype was determined by segregation analysis in families and patients whose DNA was available for testing.
Statistical Analysis
A Fisher’s exact test or Chi-square test was used to compare mutation frequencies, gender, site of onset, and current status (alive/deceased) between PMA and ALS patients; a Mann-Whitney test was used to compare age at onset and disease duration (GraphPad Prism version 5; http://www.graphpad.com). P-values below 0.05 were considered significant.
Results
Study Population
Baseline characteristics of the 261 sporadic PMA patients and 1,002 sporadic ALS patients are shown in Table 1. Patients with PMA were more likely to be male (72% versus 59%); furthermore, they lived longer (7.6 year versus 3.8 year), and had a lower age at onset (58.0 year versus 60.6 year) than patients with ALS.
[Figure omitted. See PDF.]
Table 1. Baseline characteristics of study population.
https://doi.org/10.1371/journal.pone.0048983.t001
Mutation Frequencies
Table 2 summarizes the mutations found in patients and control subjects. In individual PMA patients we detected heterozygous mutations in SOD1 (p.D90A [c.1078A>C], p.I113T [c.1147T>C]), ANG (p.K17I [c.122A>T]), FUS/TLS (p.R521H [c.1562G>A]) and TARDBP (p.N352S [c.1055A>G]), accounting for 2.3% of the patients. Previously, we showed that missense mutations in SOD1, ANG, FUS/TLS and TARDBP were present in 1.7% of the ALS patients, and 0.4% of the control subjects [13], [17], [18], [19]. In our current study, we also identified four novel CHMP2B mutations, one of which was present in a PMA patient (p.R69Q [c.206G>A]), and three in ALS patients (p.R22Q [c.65G>A], p.N54T [c.161A>C], p.T83I [c.248C>T]). All four CHMP2B mutations are located in a domain that is important for the formation of multivesicular bodies (MVBs), involved in sorting of cargo proteins to intraluminal vesicles [24]. These mutations are located in well conserved areas (Figure S1) and predicted to be pathological (Table 2). They account for 0.38% of the sporadic PMA patients and 0.30% of the sporadic ALS patients. None of these CHMP2B mutations was present in our control subjects; however, in one control subject (0.13%) we did detect a mutation (p.S194L [c.581C>T]) that had previously been reported in a patient with frontotemporal dementia (FTD) [25].
[Figure omitted. See PDF.]
Table 2. Missense mutations found in SOD1, ANG, FUS/TLS, TARDBP, and CHMP2B.
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Clinical Characteristics
The average age at onset of PMA patients with missense mutations was 48 years, and five of them were male (71%). Although only one of these patients had died, their average disease duration already exceeded 114 months (range 37–316). These clinical characteristics of sporadic PMA patients with missense mutations were consistent with the characteristics of our entire PMA cohort. More detailed signs and symptoms are provided in Table 3.
[Figure omitted. See PDF.]
Table 3. Clinical characteristics of newly identified patients with missense mutations.
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Genealogical- and Haplotype Analyses
Previously, we have shown that the p.N352S mutation in TARDBP is a founder mutation in the Dutch ALS population [13]. Hence, we performed a thorough genealogical analysis and demonstrated that our PMA patients with p.N352S mutations had common ancestors, dating back to the 17th century in the north of France (Figure S2). Haplotype analysis revealed that these patients also shared the haplotype that was reported in Dutch ALS patients [13].
Discussion
Patients with isolated LMN signs represent a subgroup of the patients with MND. To assess the mutation frequency of MND-associated genes in this subgroup, we compared 261 apparently sporadic PMA patients to apparently sporadic ALS patients. Our PMA patients were more likely to be male and lived significantly longer than ALS patients, as reported previously [3]. We detected two SOD1 mutations (p.D90A, p.I113T), one ANG mutation (p.K17I), one FUS/TLS mutation (p.R521H), one TARDBP mutation (p.N352S), and one novel CHMP2B mutation (p.R69Q) in individual PMA patients. For each of these genes we compared mutation frequencies between our PMA patients and ALS patients, and did not detect significant differences.
Clinical and pathological similarities between PMA and ALS have already been reported: more than twenty percent of the patients with isolated LMN signs will develop UMN signs within six years, especially in the first years after symptom onset [1], [3], [26]. Nonetheless, it can be difficult to diagnose these UMN signs due to LMN wasting and pathophysiological abnormalities caused by damaged motor pathways, motor neurons and interneurons [27]. Pathological studies have also revealed ubiquitinated inclusions and involvement of the corticospinal tract in PMA patients, which are typical for ALS patients and emphasize similarities between these diseases [28], [29].
Previously, mutations in SOD1, ANG, FUS/TLS, TARDBP and CHMP2B have been identified in patients with a range of clinical phenotypes, including combinations of FTD, Parkinson’s disease, and ALS [14], [18], [22], [30], [31], [32], [33], [34], [35], [36], [37], [38], [39], [40], [41], [42], [43], [44], [45]. CHMP2B mutations have also been described in sporadic PMA patients, while mutations in MND-associated genes have been detected in familial ALS patients with predominantly LMN signs [15], [19], [28], [46], [47], [48], [49], [50]. In addition, we have recently shown that C9orf72 repeat expansions are present in sporadic PMA patients, but at a lower frequency than in sporadic ALS patients (1.6% versus 6.1%) [12]; other studies have shown that C9orf72 repeat expansions were present in approximately 7% of white sporadic ALS patients from the USA, Europe and Australia, and that bulbar onset ALS is frequently encountered in patients with these expansions [51], [52], [53], [54]. Our current findings demonstrate that mutations in SOD1, ANG, FUS/TLS, TARDBP and CHMP2B are also associated with apparently sporadic PMA, thus expanding the wide range of clinical phenotypes reported to date. Furthermore, the comparable mutation frequencies between PMA and ALS patients show that, apart from clinical and pathological similarities, these diseases demonstrate a genetic overlap as well, suggesting that PMA is a subtype of ALS.
We detected a SOD1 mutation (p.D90A) in a patient with sporadic PMA, a patient with classical sporadic ALS, and control subjects. This is the most common SOD1 mutation, and causes both autosomal dominant and recessive ALS [55], [56]. Although it behaves dominantly in many families, it is a polymorphism in the Swedish population, primarily causing ALS when in the homozygous state [57]. Another SOD1 mutation (p.I113T) was also present in a PMA patient; it is known for its clinical heterogeneity, including asymptomatic subjects, patients with mild fasciculations, patients with typical ALS, and patients with ALS-FTD and chorea [41], [58]. Both these SOD1 mutations appear to result in ALS through aggregation of mutant SOD1 protein [59].
In addition, we identified an ANG mutation (p.K17I) in one PMA patient, and in two out of 1,582 Dutch control subjects. The p.K17I mutation has already been reported in ALS patients and in control subjects [18]. Despite its presence in control subjects, it does affect the neuroprotective-, angiogenic- and ribonucleolytic activity of ANG [50], [60], [61]. It seems likely that this mutation raises ALS susceptibility and/or acts as a genetic modifier, a hypothesis supported by recent reports of families that harbor a p.K17I mutation in combination with TARDBP- or FUS/TLS mutations, and a large international collaborative study, which demonstrates that ANG mutations confer a substantial risk for ALS [13], [18], [62].
In one PMA patient, we identified a FUS/TLS mutation (p.R521H); one of the most common FUS/TLS mutations with a disease duration of approximately four years [63], [64]. In two other PMA patients we detected a TARDBP mutation (p.N352S), which has been described in German and Japanese ALS patients [65], [66], [67]. We have recently reported that p.N352S is a founder mutation in the Dutch ALS population [13]. In the present study, we revealed that our PMA patients had common ancestors and shared a haplotype also detected in Dutch ALS patients.
The four CHMP2B mutations we detected (p.R69Q, p.R22Q, p.N54T, p.T83I) are novel, absent in control subjects, located in well conserved areas, and predicted to be pathogenic. One of these was identified in a patient with sporadic PMA (0.38%), three in patients with sporadic ALS (0.30%). These mutation frequencies demonstrate that CHMP2B mutations are not specific for PMA, but are present in patients with PMA, FTD, ALS-FTD, and ALS. We also detected one previously reported mutation (p.S194L) in a control subject [25]. Since this variant is located within an area of low complexity and predicted to have neutral effects, it probably represents a rare benign polymorphism.
Recently, we have provided evidence for an oligogenic etiology of familial ALS [13]. We reported five families with mutations in multiple MND-associated genes: ANG mutations were detected in combination with FUS/TLS and TARDBP mutations, and C9orf72 repeat expansions in combination with TARDBP, SOD1, and FUS/TLS mutations (p-value 1.57×10−7). In our present study, we did not identify mutations in multiple MND-associated genes in a single patient; however, the high phenotypic variability that is seen amongst patients with mutations in these genes (ranging from FTD to Parkinson’s disease and MNDs) does suggest that other genetic and/or environmental factors influence disease characteristics of sporadic MNDs.
To summarize, we have detected comparable mutation frequencies in patients with apparently sporadic PMA and ALS, indicating a genetic overlap between these two diseases. Thus, our findings favor the hypothesis that PMA is a subtype of ALS and not a distinct entity, broadening the disease spectrum of ALS.
Supporting Information
[Figure omitted. See PDF.]
Figure S1.
CHMP2B mutations and conservation. Conservation of amino-acid residues across species was generated using ClustalW2 online tool, http://www.ebi.ac.uk/Tools/msa/clustalw2/.
https://doi.org/10.1371/journal.pone.0048983.s001
(DOC)
Figure S2.
Pedigree of two PMA patients with p.N352S mutations in TARDBP .
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(DOC)
Author Contributions
Conceived and designed the experiments: MvB LV MAvE WLvdP JHV LHvdB. Performed the experiments: MvB LV EAMH DD HJS AJvdK MdV JHV LHvdB. Analyzed the data: MvB LV MAvE WLvdP EAMH DD JHV LHvdB. Contributed reagents/materials/analysis tools: MvB LV MAvE WLvdP EAMH DD HJS AJvdK MdV JHV LHvdB. Wrote the paper: MvB. Revising manuscript for content: MvB LV MAvE WLvdP EAMH DD HJS AJvdK MdV JHV LHvdB. Statistical analysis: MvB LV JHV. Study supervision or coordination: JHV LHvdB.
Citation: van Blitterswijk M, Vlam L, van Es MA, van der Pol W-L, Hennekam EAM, Dooijes D, et al. (2012) Genetic Overlap between Apparently Sporadic Motor Neuron Diseases. PLoS ONE 7(11): e48983. https://doi.org/10.1371/journal.pone.0048983
1. Visser J, van den Berg-Vos RM, Franssen H, van den Berg LH, Wokke JH, et al. (2007) Disease course and prognostic factors of progressive muscular atrophy. Arch Neurol 64: 522–528.
2. Van den Berg-Vos RM, Visser J, Kalmijn S, Fischer K, de Visser M, et al. (2009) A long-term prospective study of the natural course of sporadic adult-onset lower motor neuron syndromes. Arch Neurol 66: 751–757.
3. Kim WK, Liu X, Sandner J, Pasmantier M, Andrews J, et al. (2009) Study of 962 patients indicates progressive muscular atrophy is a form of ALS. Neurology 73: 1686–1692.
4. Wingo TS, Cutler DJ, Yarab N, Kelly CM, Glass JD (2011) The heritability of amyotrophic lateral sclerosis in a clinically ascertained United States research registry. PLoS One 6: e27985.
5. DeJesus-Hernandez M, Mackenzie IR, Boeve BF, Boxer AL, Baker M, et al. (2011) Expanded GGGGCC hexanucleotide repeat in noncoding region of C9ORF72 causes chromosome 9p-linked FTD and ALS. Neuron 72: 245–256.
6. Renton AE, Majounie E, Waite A, Simon-Sanchez J, Rollinson S, et al. (2011) A hexanucleotide repeat expansion in C9ORF72 is the cause of chromosome 9p21-linked ALS-FTD. Neuron 72: 257–268.
7. Andersen PM, Al-Chalabi A (2011) Clinical genetics of amyotrophic lateral sclerosis: what do we really know? Nat Rev Neurol 7: 603–615.
8. Johnson JO, Mandrioli J, Benatar M, Abramzon Y, Van Deerlin VM, et al. (2010) Exome sequencing reveals VCP mutations as a cause of familial ALS. Neuron 68: 857–864.
9. Deng HX, Chen W, Hong ST, Boycott KM, Gorrie GH, et al. (2011) Mutations in UBQLN2 cause dominant X-linked juvenile and adult-onset ALS and ALS/dementia. Nature 477: 211–215.
10. Fecto F, Yan J, Vemula SP, Liu E, Yang Y, et al. (2011) SQSTM1 mutations in familial and sporadic amyotrophic lateral sclerosis. Arch Neurol 68: 1440–1446.
11. Wu CH, Fallini C, Ticozzi N, Keagle PJ, Sapp PC, et al. (2012) Mutations in the profilin 1 gene cause familial amyotrophic lateral sclerosis. Nature 488: 499–503.
12. van Rheenen W, van Blitterswijk M, Huisman MH, Vlam L, van Doormaal PT, et al. (2012) Hexanucleotide repeat expansions in C9ORF72 in the spectrum of motor neuron diseases. Neurology 79: 878–882.
13. van Blitterswijk M, van Es MA, Hennekam EA, Dooijes D, van Rheenen W, et al. (2012) Evidence for an oligogenic basis of amyotrophic lateral sclerosis. Hum Mol Genet 21: 3776–3784.
14. Parkinson N, Ince PG, Smith MO, Highley R, Skibinski G, et al. (2006) ALS phenotypes with mutations in CHMP2B (charged multivesicular body protein 2B). Neurology 67: 1074–1077.
15. Cox LE, Ferraiuolo L, Goodall EF, Heath PR, Higginbottom A, et al. (2010) Mutations in CHMP2B in lower motor neuron predominant amyotrophic lateral sclerosis (ALS). PLoS One 5: e9872.
16. Vlam L, Schelhaas HJ, van Blitterswijk M, van Vught PW, de Visser M, et al. (2012) Mutations in the TRPV4 Gene Are Not Associated With Sporadic Progressive Muscular Atrophy. Arch Neurol 69: 790–791.
17. van Es MA, Dahlberg C, Birve A, Veldink JH, van den Berg LH, et al. (2010) Large-scale SOD1 mutation screening provides evidence for genetic heterogeneity in amyotrophic lateral sclerosis. J Neurol Neurosurg Psychiatry 81: 562–566.
18. van Es MA, Schelhaas HJ, van Vught PW, Ticozzi N, Andersen PM, et al. (2011) Angiogenin variants in Parkinson disease and amyotrophic lateral sclerosis. Ann Neurol 70: 964–973.
19. Groen EJ, van Es MA, van Vught PW, Spliet WG, van Engelen-Lee J, et al. (2010) FUS mutations in familial amyotrophic lateral sclerosis in the Netherlands. Arch Neurol 67: 224–230.
20. Huisman MH, de Jong SW, van Doormaal PT, Weinreich SS, Schelhaas HJ, et al. (2011) Population based epidemiology of amyotrophic lateral sclerosis using capture-recapture methodology. J Neurol Neurosurg Psychiatry 82: 1165–1170.
21. Brooks BR, Miller RG, Swash M, Munsat TL (2000) El Escorial revisited: revised criteria for the diagnosis of amyotrophic lateral sclerosis. Amyotroph Lateral Scler Other Motor Neuron Disord 1: 293–299.
22. Skibinski G, Parkinson NJ, Brown JM, Chakrabarti L, Lloyd SL, et al. (2005) Mutations in the endosomal ESCRTIII-complex subunit CHMP2B in frontotemporal dementia. Nat Genet 37: 806–808.
23. Nickerson DA, Tobe VO, Taylor SL (1997) PolyPhred: automating the detection and genotyping of single nucleotide substitutions using fluorescence-based resequencing. Nucleic Acids Res 25: 2745–2751.
24. Horii M, Shibata H, Kobayashi R, Katoh K, Yorikawa C, et al. (2006) CHMP7, a novel ESCRT-III-related protein, associates with CHMP4b and functions in the endosomal sorting pathway. Biochem J 400: 23–32.
25. Ghanim M, Guillot-Noel L, Pasquier F, Jornea L, Deramecourt V, et al. (2010) CHMP2B mutations are rare in French families with frontotemporal lobar degeneration. J Neurol 257: 2032–2036.
26. Traynor BJ, Codd MB, Corr B, Forde C, Frost E, et al. (2000) Clinical features of amyotrophic lateral sclerosis according to the El Escorial and Airlie House diagnostic criteria: A population-based study. Arch Neurol 57: 1171–1176.
27. Swash M (2012) Why are upper motor neuron signs difficult to elicit in amyotrophic lateral sclerosis? J Neurol Neurosurg Psychiatry 83: 659–662.
28. Cudkowicz ME, McKenna-Yasek D, Chen C, Hedley-Whyte ET, Brown RH Jr (1998) Limited corticospinal tract involvement in amyotrophic lateral sclerosis subjects with the A4V mutation in the copper/zinc superoxide dismutase gene. Ann Neurol 43: 703–710.
29. Ince PG, Evans J, Knopp M, Forster G, Hamdalla HH, et al. (2003) Corticospinal tract degeneration in the progressive muscular atrophy variant of ALS. Neurology 60: 1252–1258.
30. Van Langenhove T, van der Zee J, Sleegers K, Engelborghs S, Vandenberghe R, et al. (2010) Genetic contribution of FUS to frontotemporal lobar degeneration. Neurology 74: 366–371.
31. Blair IP, Williams KL, Warraich ST, Durnall JC, Thoeng AD, et al. (2010) FUS mutations in amyotrophic lateral sclerosis: clinical, pathological, neurophysiological and genetic analysis. J Neurol Neurosurg Psychiatry 81: 639–645.
32. Borroni B, Archetti S, Del Bo R, Papetti A, Buratti E, et al. (2010) TARDBP mutations in frontotemporal lobar degeneration: frequency, clinical features, and disease course. Rejuvenation Res 13: 509–517.
33. Borroni B, Bonvicini C, Alberici A, Buratti E, Agosti C, et al. (2009) Mutation within TARDBP leads to frontotemporal dementia without motor neuron disease. Hum Mutat 30: E974–983.
34. Ticozzi N, Silani V, LeClerc AL, Keagle P, Gellera C, et al. (2009) Analysis of FUS gene mutation in familial amyotrophic lateral sclerosis within an Italian cohort. Neurology 73: 1180–1185.
35. Benajiba L, Le Ber I, Camuzat A, Lacoste M, Thomas-Anterion C, et al. (2009) TARDBP mutations in motoneuron disease with frontotemporal lobar degeneration. Ann Neurol 65: 470–473.
36. Broustal O, Camuzat A, Guillot-Noel L, Guy N, Millecamps S, et al. (2010) FUS mutations in frontotemporal lobar degeneration with amyotrophic lateral sclerosis. J Alzheimers Dis 22: 765–769.
37. Mackenzie IR, Rademakers R, Neumann M (2010) TDP-43 and FUS in amyotrophic lateral sclerosis and frontotemporal dementia. Lancet Neurol 9: 995–1007.
38. Yan J, Deng HX, Siddique N, Fecto F, Chen W, et al. (2010) Frameshift and novel mutations in FUS in familial amyotrophic lateral sclerosis and ALS/dementia. Neurology 75: 807–814.
39. van Es MA, Diekstra FP, Veldink JH, Baas F, Bourque PR, et al. (2009) A case of ALS-FTD in a large FALS pedigree with a K17I ANG mutation. Neurology 72: 287–288.
40. Quadri M, Cossu G, Saddi V, Simons EJ, Murgia D, et al. (2011) Broadening the phenotype of TARDBP mutations: the TARDBP Ala382Thr mutation and Parkinson’s disease in Sardinia. Neurogenetics 12: 203–209.
41. Lopate G, Baloh RH, Al-Lozi MT, Miller TM, Fernandes Filho JA, et al. (2010) Familial ALS with extreme phenotypic variability due to the I113T SOD1 mutation. Amyotroph Lateral Scler 11: 232–236.
42. Borghero G, Floris G, Cannas A, Marrosu MG, Murru MR, et al.. (2011) A patient carrying a homozygous p.A382T TARDBP missense mutation shows a syndrome including ALS, extrapyramidal symptoms, and FTD. Neurobiol Aging 32: 2327 e2321–2325.
43. Kovacs GG, Murrell JR, Horvath S, Haraszti L, Majtenyi K, et al. (2009) TARDBP variation associated with frontotemporal dementia, supranuclear gaze palsy, and chorea. Mov Disord 24: 1843–1847.
44. Praline J, Vourc’h P, Guennoc AM, Veyrat-Durebex C, Corcia P (2012) Co-occurrence of progressive anarthria with an S393L TARDBP mutation and ALS within a family. Amyotroph Lateral Scler 13: 155–157.
45. Camdessanche JP, Belzil VV, Jousserand G, Rouleau GA, Creac’h C, et al. (2011) Sensory and motor neuronopathy in a patient with the A382P TDP-43 mutation. Orphanet J Rare Dis 6: 4.
46. Suzuki M, Irie T, Watanabe T, Mikami H, Yamazaki T, et al. (2008) Familial amyotrophic lateral sclerosis with Gly93Ser mutation in Cu/Zn superoxide dismutase: a clinical and neuropathological study. J Neurol Sci 268: 140–144.
47. Cervenakova L, Protas, II, Hirano A, Votiakov VI, Nedzved MK, et al. (2000) Progressive muscular atrophy variant of familial amyotrophic lateral sclerosis (PMA/ALS). J Neurol Sci 177: 124–130.
48. Restagno G, Lombardo F, Sbaiz L, Mari C, Gellera C, et al. (2008) The rare G93D mutation causes a slowly progressing lower motor neuron disease. Amyotroph Lateral Scler 9: 35–39.
49. Gellera C, Colombrita C, Ticozzi N, Castellotti B, Bragato C, et al. (2008) Identification of new ANG gene mutations in a large cohort of Italian patients with amyotrophic lateral sclerosis. Neurogenetics 9: 33–40.
50. Wu D, Yu W, Kishikawa H, Folkerth RD, Iafrate AJ, et al. (2007) Angiogenin loss-of-function mutations in amyotrophic lateral sclerosis. Ann Neurol 62: 609–617.
51. Millecamps S, Boillee S, Le Ber I, Seilhean D, Teyssou E, et al. (2012) Phenotype difference between ALS patients with expanded repeats in C9ORF72 and patients with mutations in other ALS-related genes. J Med Genet 49: 258–263.
52. Stewart H, Rutherford NJ, Briemberg H, Krieger C, Cashman N, et al. (2012) Clinical and pathological features of amyotrophic lateral sclerosis caused by mutation in the C9ORF72 gene on chromosome 9p. Acta Neuropathol 123: 409–417.
53. Brettschneider J, Van Deerlin VM, Robinson JL, Kwong L, Lee EB, et al. (2012) Pattern of ubiquilin pathology in ALS and FTLD indicates presence of C9ORF72 hexanucleotide expansion. Acta Neuropathol 123: 825–839.
54. Majounie E, Renton AE, Mok K, Dopper EG, Waite A, et al. (2012) Frequency of the C9orf72 hexanucleotide repeat expansion in patients with amyotrophic lateral sclerosis and frontotemporal dementia: a cross-sectional study. Lancet Neurol 11: 323–330.
55. Robberecht W, Aguirre T, Van den Bosch L, Tilkin P, Cassiman JJ, et al. (1996) D90A heterozygosity in the SOD1 gene is associated with familial and apparently sporadic amyotrophic lateral sclerosis. Neurology 47: 1336–1339.
56. Andersen PM, Nilsson P, Ala-Hurula V, Keranen ML, Tarvainen I, et al. (1995) Amyotrophic lateral sclerosis associated with homozygosity for an Asp90Ala mutation in CuZn-superoxide dismutase. Nat Genet 10: 61–66.
57. Valdmanis PN, Rouleau GA (2008) Genetics of familial amyotrophic lateral sclerosis. Neurology 70: 144–152.
58. Eisen A, Mezei MM, Stewart HG, Fabros M, Gibson G, et al. (2008) SOD1 gene mutations in ALS patients from British Columbia, Canada: clinical features, neurophysiology and ethical issues in management. Amyotroph Lateral Scler 9: 108–119.
59. Banci L, Bertini I, Boca M, Girotto S, Martinelli M, et al. (2008) SOD1 and amyotrophic lateral sclerosis: mutations and oligomerization. PLoS One 3: e1677.
60. Sebastia J, Kieran D, Breen B, King MA, Netteland DF, et al. (2009) Angiogenin protects motoneurons against hypoxic injury. Cell Death Differ 16: 1238–1247.
61. Padhi AK, Kumar H, Vasaikar SV, Jayaram B, Gomes J (2012) Mechanisms of loss of functions of human angiogenin variants implicated in amyotrophic lateral sclerosis. PLoS One 7: e32479.
62. Millecamps S, Salachas F, Cazeneuve C, Gordon P, Bricka B, et al. (2010) SOD1, ANG, VAPB, TARDBP, and FUS mutations in familial amyotrophic lateral sclerosis: genotype-phenotype correlations. J Med Genet 47: 554–560.
63. Kwiatkowski TJ Jr, Bosco DA, Leclerc AL, Tamrazian E, Vanderburg CR, et al. (2009) Mutations in the FUS/TLS gene on chromosome 16 cause familial amyotrophic lateral sclerosis. Science 323: 1205–1208.
64. Vance C, Rogelj B, Hortobagyi T, De Vos KJ, Nishimura AL, et al. (2009) Mutations in FUS, an RNA processing protein, cause familial amyotrophic lateral sclerosis type 6. Science 323: 1208–1211.
65. Kuhnlein P, Sperfeld AD, Vanmassenhove B, Van Deerlin V, Lee VM, et al. (2008) Two German kindreds with familial amyotrophic lateral sclerosis due to TARDBP mutations. Arch Neurol 65: 1185–1189.
66. Kamada M, Maruyama H, Tanaka E, Morino H, Wate R, et al. (2009) Screening for TARDBP mutations in Japanese familial amyotrophic lateral sclerosis. J Neurol Sci 284: 69–71.
67. Iida A, Kamei T, Sano M, Oshima S, Tokuda T, et al. (2012) Large-scale screening of TARDBP mutation in amyotrophic lateral sclerosis in Japanese. Neurobiol Aging 33: 786–790.
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Abstract
Progressive muscular atrophy (PMA) and amyotrophic lateral sclerosis (ALS) are devastating motor neuron diseases (MNDs), which result in muscle weakness and/or spasticity. We compared mutation frequencies in genes known to be associated with MNDs between patients with apparently sporadic PMA and ALS. A total of 261 patients with adult-onset sporadic PMA, patients with sporadic ALS, and control subjects of Dutch descent were obtained at national referral centers for neuromuscular diseases in The Netherlands. Sanger sequencing was used to screen these subjects for mutations in the coding regions of superoxide dismutase-1 (SOD1), angiogenin (ANG), fused in sarcoma/translated in liposarcoma (FUS/TLS), TAR DNA-binding protein 43 (TARDBP), and multivesicular body protein 2B (CHMP2B). In our cohort of PMA patients we identified two SOD1 mutations (p.D90A, p.I113T), one ANG mutation (p.K17I), one FUS/TLS mutation (p.R521H), one TARDBP mutation (p.N352S), and one novel CHMP2B mutation (p.R69Q). The mutation frequency of these genes was similar in sporadic PMA (2.7%) and ALS (2.0%) patients, and therefore, our findings demonstrate a genetic overlap between apparently sporadic PMA and ALS.
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