High frequency of the TARDBP p.M337 V mutation among south-eastern Chinese patients with familial amyotrophic lateral sclerosis

Amyotrophic lateral sclerosis (ALS) is a typical form of motor neuron disease characterized by selective degeneration of both the upper motor neurons (UMNs) and the lower motor neurons (LMNs) in the cerebral cortex, brain stem, and spinal cord, with an incidence of approximately 1-2 per 100,000 people [1]. Typically, ALS patients initially present with symptoms in the upper limbs later in life (40-60 years old). The disease then spreads to the trunk and bulbar muscles, and patients ultimately die from respiratory failure, with a mean survival of 3-5 years [2]. ALS is a progressive and incurable disease with no effective treatment available.

Currently, the complete aetiology of ALS is unclear. Approximately 5-10% of ALS patients have a family history of ALS (defined as familial ALS), and the remainder of patients have sporadic ALS. ALS is a neurodegenerative disorder with substantial genetic heterogeneity, and more than 30 genes are associated with familial ALS. In the Caucasian population, chromosome 9 open reading frame 72 (C9ORF72, MIM: 614260) repeat expansions are the most common genetic cause of ALS; in China, Cu/Zn superoxide dismutase 1 (SOD1, MIM: 147450), fused in sarcoma/translated in liposarcoma (FUS/TLS, MIM: 137070), and TAR DNA-binding protein (TARDBP, MIM: 605078) are the main causative genes among ALS patients [2, 3]. However, the frequencies of gene mutations are diverse between different populations, and this diversity has been linked to different genetic backgrounds. Thus far, only a few TARDBP-ALS families have been reported in China, and no mutation analysis has been reported in south-eastern China [4‐7].

In this study, 7 SOD1- and FUS-negative ALS families and 215 sporadic ALS patients were enrolled to screen the TARDBP mutation. Two TARDBP mutations in exon 6 (c.1009A > G, p.M337 V and c.1042G > T, p.G348 C) were identified in 5 families (family 1II3, family 2II6, family 3II4, family 4II4, and family 5II5). Interestingly, 4 unrelated ALS families (families 1-4) carried the same p.M337 V mutation. No disease-causing mutations were identified in the sporadic ALS patients. TARDBP-linked familial ALS patients often showed upper limb and bulbar onset and had a benign disease course.

In this study, among the 7 unrelated SOD1- and FUS-negative ALS families, we detected 2 TARDBP mutations (c.1009A > G, p.M337 V and c.1042G > T, p.G348C) in 5 families. Importantly, 4 families carried the same TARDBP mutation, c.1009A > G, p.M337 V. Hou L et al. screened SOD1, TARDBP, and FUS gene mutations in ALS patients from central-southern China and revealed that SOD1 (20%) and FUS (13.3%) mutations were the main causal mutations in familial ALS, but they did not detect any TARDBP-linked ALS families [9]. In a Brazilian research centre, Chadi G et al. reported that the most common gene mutations in familial ALS were VAPB (43.6%), C9orf72 (12.8%), and SOD1 (7.7%), whereas no FUS or TARDBP mutations were detected in any familial ALS subjects [10]. In Australia, McCann EP et al. also reported that the main gene mutations in familial ALS were SOD1 (13.7%), FUS (2.4%), and TARDBP (1.9%) [11]. Our study indicated a high frequency of the TARDBP gene mutation in familial ALS in the south-eastern region of China.

Among the 5 ALS families with the TARDBP gene mutation in the present study, 12 symptomatic ALS patients and 1 asymptomatic patient were identified (Table 1). For the 12 symptomatic patients, including 8 males and 4 females, the average age of onset was 57.0 ± 4.7 years. In addition, the TARDBP-linked familial ALS patients presented a trend towards higher rates of bulbar (50.0%, 6/12) onset and upper limb (41.7%, 5/12) onset than lower rates of limb onset (8.3%, 1/12); this finding is consistent with a predominance of upper limb onset in TARDBP-linked ALS reported in a previous study [12]. Furthermore, similar to previous reports, ALS patients with TARDBP mutations showed a benign disease course and an average survival of 106.5 ± 41.8 months (n = 8) [13].

Furthermore, TARDBP p.M337 V ALS patients showed substantial clinical heterogeneity between and among families carrying the same mutation. These patients could exhibit a LMN-dominant presentation, an UMN-dominant presentation, or the typical presentation with both LMN and UMN involvement, which is similar to the cases that we reported in family 2 and family 3. In addition, in family 3, compared with affected members II4 and II5, II2 first showed symptoms at the age of 50 years and died from respiratory failure 36 months later, reflecting a relatively short disease duration, which may suggest intrafamilial clinical heterogeneity. We also found a p.M337 V carrier without any neurological symptoms in family 4, which may be explained by incomplete penetrance; no similar patient has been previously reported. In addition, Ju X et al. reported a pedigree with the p.M337 V mutation that showed cognitive impairment. In this study, none of the 4 families with the p.M337 V mutation developed cognitive impairment; this result is similar to the results from a Taiwanese cohort. The substantial clinical heterogeneity between p.M337 V mutation pedigrees indicated the potential presence of other underlying phenotype-modifying factors [14, 15]. Kühnlein P et al. described the first ALS patient with the p.G348C mutation who presented with early spinal onset (31 years) without cognitive impairment [16]. Del Bo R et al. also reported a 5-generation p.G348C mutation ALS family with 9 affected members, and the affected members showed highly variable clinical features, including the age at onset (36 to 67 years) and disease duration (36 to 60 months) [17]. In this study, p.G348C mutation ALS patients (family 5, I1 and II5) had an age of onset of 50 to 55 years and spinal onset, which are similar to the features of previously reported patients [16, 17]. Among different ethnic groups, due to different genetic backgrounds, patients with TARDBP gene mutations also show substantial clinical heterogeneity. According to Corcia P et al., approximately 51.3% of Caucasian ALS patients have upper limb onset, while 58.8% of Asian patients have bulbar onset [18]. Similarly, bulbar-onset patients accounted for 50% of the patients in this study.

In this study, only a single nucleotide polymorphism (c.1098C > G, p.A366A) was identified in 5 sporadic patients. However, no mutation was detected in exon 6 of the TARDBP gene in the 215 sporadic patients. Similarly, in southern China, Ye CH et al. detected no TARDBP exon 6 mutations in 207 sporadic ALS patients [19]. Huang R and Zou ZY demonstrated that the frequency of TARDBP gene mutations in Chinese sporadic ALS patients was approximately 0.61% to 0.73% [5, 20]. The c.1098C > G, p.A366A polymorphism, which may increase susceptibility to ALS, was also previously reported [5].

TARDBP gene mutations are the common causal mutations in this cohort of familial ALS patients from south-eastern China, with a high frequency of the p.M337 V mutation. The TARDBP-linked ALS patients showed substantial clinical heterogeneity and a more benign disease phenotype with a longer disease duration.