Molecular dissection of ALS-associated toxicity of SOD1 in transgenic mice using an exon-fusion approach

Deng, Han Xiang; Jiang, Hujun; Fu, Rui; Zhai, Hong; Shi, Yong; Liu, Erdong; Hirano, Minoru; Mauro, Ceroni; Siddique, Teepu

doi:10.1093/hmg/ddn131

Cited by 30 publications

(20 citation statements)

References 35 publications

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“…In our previous studies of SOD1 inclusions in spinal cord of SOD1-linked FALS patients and SOD1 transgenic mice, we observed that antigen retrieval methodology played an essential role in detection of SOD1 inclusions in lower motor neurons 21, 22 , especially in some human cases (unpublished data). We compared three antigen retrieval protocols: boiling and microwave that are most commonly used, and high pressure decloaking chamber.…”

Section: Resultsmentioning

confidence: 87%

“…2 and supplementary figure 1), but not in the four FALS cases with SOD1 mutations. Previous studies have demonstrated that SOD1/ubiqutin-positive inclusions in spinal motor neurons are a pathological hallmark in ALS patients with SOD1 mutations and in the transgenic mice overexpressing mutant SOD1 18, 22 . Supporting the notion that the FUS-positive inclusions are absent in SOD1-linked ALS, we found that the ubiquitin-positive inclusions in spinal neurons were FUS-negative in patients with SOD1 G85R or SOD1 A4V mutation and in the transgenic mice overexpressing SOD1 G93A and SOD1 L126Z 21, 23 (Supplementary figure 2).…”

Section: Resultsmentioning

confidence: 99%

“…We compared three antigen retrieval protocols: boiling and microwave that are most commonly used, and high pressure decloaking chamber. We found that antigen retrieval using the high pressure decloaking chamber was the most efficient in detection of SOD1 inclusions, and have therefore adopted this protocol as the routine method for antigen retrieval 21, 22 . Because other studies failed to show FUS pathology in SALS using microwave protocol for antigen retrieval 8, 25, 26 , we assumed that in addition to the sensitivity of the antibodies, antigen retrieval methodology may be an important factor for influencing the detestability of FUS-positive inclusions.…”

Section: Resultsmentioning

confidence: 99%

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FUS‐immunoreactive inclusions are a common feature in sporadic and non‐SOD1 familial amyotrophic lateral sclerosis

Deng

Zhai

Bigio

et al. 2010

Annals of Neurology

290

177

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Objective Amyotrophic lateral sclerosis (ALS) is a fatal disorder of motor neuron degeneration. Most cases of ALS are sporadic (SALS), but about 5-10% of ALS cases are familial (FALS). Recent studies have shown that mutations in FUS are causal in approximately 4-5% of FALS and some apparent SALS cases. The pathogenic mechanism of the mutant FUS-mediated ALS and potential roles of FUS in non-FUS ALS remain to be investigated. Methods Immunostaining was performed on postmortem spinal cords from 78 ALS cases, including SALS (n=52), ALS with dementia (ALS/dementia, n=10) and FALS (n=16). In addition, postmortem brains or spinal cords from 22 cases with or without frontotemporal lobar degeneration (FTLD) were also studied. In total, 100 cases were studied. Results FUS-immunoreactive inclusions were observed in spinal anterior horn neurons in all sporadic and familial ALS cases, except for those with SOD1 mutations. The FUS-containing inclusions were also immunoreactive with antibodies to TDP43, p62 and ubiquitin. A fraction of tested FUS antibodies recognized FUS inclusions and an unusual antigen retrieval appeared to be important for detection of the skein-like FUS inclusions. Interpretation Although mutations in FUS account for only a small fraction of FALS and SALS, our data suggest that FUS protein may be a common component of the cellular inclusions in non-SOD1 ALS and some other neurodegenerative conditions, implying a shared pathogenic pathway underlying SALS, non-SOD1 FALS, ALS/dementia and related disorders. Our data also indicate that SOD1-linked ALS may have a distinct pathogenic pathway from SALS and other types of FALS.

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Section: Resultsmentioning

confidence: 87%

Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

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FUS‐immunoreactive inclusions are a common feature in sporadic and non‐SOD1 familial amyotrophic lateral sclerosis

Deng

Zhai

Bigio

et al. 2010

Annals of Neurology

290

177

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“…It was reported that nonsense-mediated mRNA decay underlies the clearance of SOD1 mRNA with a premature termination codon in exons 1-4, but not in exon 5. 16 This is why among the reported SOD1 ALS mutations, stop codon mutations exclusively occur in exon 5. It is possible that nonsense-mediated decay could be involved in the degradation of the alternatively spliced SOD1 mRNA, which could be more efficient in spinal cord tissue than in blood cells, since the level of SOD1 transcript without exon 2 was lower in the spinal cord (figure 3).…”

mentioning

confidence: 99%

A mechanism for low penetrance in an ALS family with a novel SOD1 deletion

Zinman¹,

N.²,

Sato³

et al. 2009

Neurology

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“…Some transition metals such as iron, cobalt, zinc, selenium, molybdenum, magnesium, chromium, manganese and copper are essential for life. Others, such as mercury, lead, nickel, cadmium, palladium, and arsenic are widely used in industry and in various implants but are toxic at certain levels in humans [7][8][9].…”

Section: Heavy Metals Intoxicationmentioning

confidence: 99%

Atypical Levels of Heavy Metals, Creatinine, Haptoglobin, and Ferritin Found in Amyotrophic Lateral Sclerosis Outpatients vs. Healthy Controls: Possible Utility as a Diagnostic Biomarker

Steenblock¹,

Ikrar²

2019

Int J Pathol Clin Res

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Heavy metal toxicity has been conjectured as a possible risk factor for and player in amyotrophic lateral sclerosis (ALS) and other neurodegenerative disorders. To test for a correlational relationship or linkage, we conducted a retrospective study of 54 sALS and 26 healthy volunteers who agreed to serve as controls, all of whom were seen at the Personalized Regenerative Medicine Clinic (San Clemente, California USA) between 2011 and 2016. We evaluated clinical laboratory findings including heavy metal content in blood and urine samples, along with serum creatinine, ferritin and haptoglobin levels, by means of inductively coupled plasma optical spectrometry and instrumental activation analysis. Disease progression, assessed using the Revised ALS Functional Rating Scale (ALS-FRS-R), was generally associated with mercury, lead, cadmium, arsenic and nickel burden. In our analysis, we found evidence of an association between ALS morbidity risk and elevated levels of mercury, lead, cadmium, arsenic, and nickel. Our findings implicate and support a linkage between relatively high levels of heavy metals, elevated serum ferritin and haptoglobin levels, and reduced urine creatinine level and sporadic amyotrophic lateral sclerosis. By virtue of this the authors argue that these may serve as a biomarker to help distinguish clinically ALS from other, symptom similar neurogenerative conditions.

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Molecular dissection of ALS-associated toxicity of SOD1 in transgenic mice using an exon-fusion approach

Cited by 30 publications

References 35 publications

FUS‐immunoreactive inclusions are a common feature in sporadic and non‐SOD1 familial amyotrophic lateral sclerosis

FUS‐immunoreactive inclusions are a common feature in sporadic and non‐SOD1 familial amyotrophic lateral sclerosis

A mechanism for low penetrance in an ALS family with a novel SOD1 deletion

Atypical Levels of Heavy Metals, Creatinine, Haptoglobin, and Ferritin Found in Amyotrophic Lateral Sclerosis Outpatients vs. Healthy Controls: Possible Utility as a Diagnostic Biomarker

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