FGF21 is a biomarker for mitochondrial translation and mtDNA maintenance disorders

Lehtonen, Jenni M.; Forsström, Saara; Bottani, Emanuela; Viscomi, Carlo; Baris, Olivier; Isoniemi, Helena; Höckerstedt, Krister; Österlund, Pia; Hurme, Mikko; Jylhävä, Juulia; Leppä, Sirpa; Markkula, Ritva; Heliö, Tiina; Mombelli, Giuliana; Uusimaa, Johanna; Laaksonen, Reijo; Laaksovirta, Hannu; Auranen, Mari; Zeviani, Massimo; Smeitink, Jan A.M.; Wiesner, Rudolf J.; Nakada, Kazuto; Isohanni, Pirjo; Suomalainen, Anu

doi:10.1212/wnl.0000000000003374

Cited by 168 publications

(155 citation statements)

References 38 publications

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“…The significant correlation between abnormal MRC activities and plasma FGF21 confirms that this protein is a good marker for MRC dysfunction in accord with previously reported findings [19]. Moreover, the finding that elevated FGF21 was prevalent in the combined group and suspected of mitochondrial translation or maintenance defects is certainly consistent with the recent report by Lehtonen et al [20]. Nevertheless, as some discrepancies were observed between plasma FGF21 and urine organic acids, it seems that the combination of these two tests would be more informative than each one alone.…”

Section: Discussionsupporting

confidence: 92%

“…Among these are growth differentiation factor 15, amino acids, liver function tests, pyruvate, muscle pathology, etc. [5,20,21]. Nevertheless, according to our findings, testing patients suspected of a mitochondrial diseases, for organic acids in urine and FGF21 in plasma is informative and the results facilitate the decision whether to perform a biopsy or not.…”

Section: Discussionmentioning

confidence: 66%

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The Relationship between Mitochondrial Respiratory Chain Activities in Muscle and Metabolites in Plasma and Urine: A Retrospective Study

Alban

Fatale

Joulani

et al. 2017

JCM

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The relationship between 114 cases with decreased enzymatic activities of mitochondrial respiratory chain (MRC) complexes I-V (C I-V) in muscle and metabolites in urine and plasma was retrospectively examined. Less than 35% disclosed abnormal plasma amino acids and acylcarnitines, with elevated alanine and low free carnitine or elevated C4-OH-carnitine as the most common findings, respectively. Abnormal urine organic acids (OA) were detected in 82% of all cases. In CI and CII defects, lactic acid (LA) in combination with other metabolites was the most common finding. 3-Methylglutaconic (3MGA) acid was more frequent in CIV and CV, while Tyrosine metabolites, mainly 4-hydroxyphenyllactate, were common in CI and IV defects. Ketones were present in all groups but more prominent in combined deficiencies. There was a significant strong correlation between elevated urinary LA and plasma lactate but none between urine Tyrosine metabolites and plasma Tyrosine or urinary LA and plasma Alanine. All except one of 14 cases showed elevated FGF21, but correlation with urine OA was weak. Although this study is limited, we conclude that urine organic acid test in combination with plasma FGF21 determination are valuable tools in the diagnosis of mitochondrial diseases.

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Section: Discussionsupporting

confidence: 92%

Section: Discussionmentioning

confidence: 66%

The Relationship between Mitochondrial Respiratory Chain Activities in Muscle and Metabolites in Plasma and Urine: A Retrospective Study

Alban

Fatale

Joulani

et al. 2017

JCM

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“…We therefore consider IBM a secondary mitochondrial disease. As “non‐mitochondrial disease controls”, we analysed serum metabolomes from 15 patients with different neuromuscular diseases (NMDs; Suomalainen et al , ; Lehtonen et al , ): Becker's muscle dystrophy ( DMD ), myotonic dystrophy type I ( DMPK ) and II ( ZNF9 ), motoneuron disease (unknown), muscle weakness ( CAPN3 ), oculopharyngeal muscular dystrophy ( PABPN1 ), late‐onset Pompe's disease ( GAA ), spinal muscular atrophy type II ( SMN1 ) and III (unknown), and Welander's muscular dystrophy ( TIA1 ; Table ). To compare the parallel disease‐specific signatures of all available genetically defined mitochondrial disease groups, we also re‐analyse metabolomic data from blood and muscle of patients with progressive external ophthalmoplegia (PEO) and infantile‐onset spinocerebellar ataxia (IOSCA; Nikkanen et al , ).…”

Section: Methodsmentioning

confidence: 99%

“…MIRAS is an autosomal recessive disorder affecting mainly the central nervous system (CNS). The MIRAS patients in this study manifested typically with progressive gait disturbance, polyneuropathy, ataxia, and some with epilepsy, but signs of muscle pathology were absent or mild (respiratory chain-deficient muscle fibres, mtDNA deletions and blood FGF21 concentration; Table 1; Hakonen et al, 2005;Lehtonen et al, 2016). We also collected plasma from 16 non-manifesting MIRAS family members heterozygous for the MIRAS allele ("MIRAS carriers", Dataset EV1).…”

Section: Methodsmentioning

confidence: 99%

Metabolomes of mitochondrial diseases and inclusion body myositis patients: treatment targets and biomarkers

et al. 2018

Self Cite

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Mitochondrial disorders (MDs) are inherited multi‐organ diseases with variable phenotypes. Inclusion body myositis (IBM), a sporadic inflammatory muscle disease, also shows mitochondrial dysfunction. We investigated whether primary and secondary MDs modify metabolism to reveal pathogenic pathways and biomarkers. We investigated metabolomes of 25 mitochondrial myopathy or ataxias patients, 16 unaffected carriers, six IBM and 15 non‐mitochondrial neuromuscular disease (NMD) patients and 30 matched controls. MD and IBM metabolomes clustered separately from controls and NMDs. MDs and IBM showed transsulfuration pathway changes; creatine and niacinamide depletion marked NMDs, IBM and infantile‐onset spinocerebellar ataxia (IOSCA). Low blood and muscle arginine was specific for patients with m.3243A>G mutation. A four‐metabolite blood multi‐biomarker (sorbitol, alanine, myoinositol, cystathionine) distinguished primary MDs from others (76% sensitivity, 95% specificity). Our omics approach identified pathways currently used to treat NMDs and mitochondrial stroke‐like episodes and proposes nicotinamide riboside in MDs and IBM, and creatine in IOSCA and IBM as novel treatment targets. The disease‐specific metabolic fingerprints are valuable “multi‐biomarkers” for diagnosis and promising tools for follow‐up of disease progression and treatment effect.

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“…Mitochondrial myopathy, encephalopathy, lactic acidosis, and stroke‐like episodes (MELAS) represents the most common subtype of mitochondrial myopathy, with affected patients characterized by stroke‐like episodes (SLEs) . Recently, new biomarkers for diagnosis and severity were reported, including FGF21, shown to be a useful indicator of a muscle manifesting mitochondrial disorder, and GDF15, which was found to be a genetic indicator of mitochondrial disorders regardless of clinical phenotype.…”

Section: Introductionmentioning

confidence: 99%

Biomarker changes associated with clinical symptoms in MELAS patient

Matsui

Yamadera

Saitô

et al. 2019

Neurology & Clinical Neurosc

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FGF21 and GDF15 are known as useful biomarkers for diagnosis of mitochondrial disorders, though their efficacy for evaluating disease severity is not well established. We determined their levels in a patient with a mitochondrial disorder and report our findings. Both biomarkers were elevated at the initial disease stage and then greatly increased with progression. Furthermore, those levels decreased along with improved clinical symptoms in response to pyruvate therapy.

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FGF21 is a biomarker for mitochondrial translation and mtDNA maintenance disorders

Cited by 168 publications

References 38 publications

The Relationship between Mitochondrial Respiratory Chain Activities in Muscle and Metabolites in Plasma and Urine: A Retrospective Study

The Relationship between Mitochondrial Respiratory Chain Activities in Muscle and Metabolites in Plasma and Urine: A Retrospective Study

Metabolomes of mitochondrial diseases and inclusion body myositis patients: treatment targets and biomarkers

Biomarker changes associated with clinical symptoms in MELAS patient

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