Subunits of the translation initiation factor eIF2B are mutant in leukoencephalopathy with vanishing white matter

Leegwater, P.A.J.; Vermeulen, Gerre; Könst, Andrea A.M.; Naidu, Sakkubai; Mulders, Joyce; Visser, Allerdien; Kersbergen, Paula; Mobach, Dragosh; Fonds, Dafna; Berkel, Carola G.M. van; Lemmers, Richard J.L.F.; Frants, Rune R.; Oudejans, Cees B.M.; Schutgens, R. B. H.; Pronk, Jan C.; Knaap, Marjo S. van der

doi:10.1038/ng764

Cited by 372 publications

(305 citation statements)

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“…VWM is caused by mutations in the genes encoding the five subunits of the eukaryotic translation initiation factor 2B (eIF2B), EIF2B1 through EIF2B5 7, 8. eIF2B is an enzyme complex essential for translation of mRNAs into proteins and central in downregulating the rate of translation under different stress conditions 9.…”

Section: Introductionmentioning

confidence: 99%

Axonal abnormalities in vanishing white matter

Klok

Bugiani

Vries

et al. 2018

Ann Clin Transl Neurol

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ObjectiveWe aimed to study the occurrence and development of axonal pathology and the influence of astrocytes in vanishing white matter.MethodsAxons and myelin were analyzed using electron microscopy and immunohistochemistry on Eif2b4 and Eif2b5 single‐ and double‐mutant mice and patient brain tissue. In addition, astrocyte‐forebrain co‐culture studies were performed.ResultsIn the corpus callosum of Eif2b5‐mutant mice, myelin sheath thickness, axonal diameter, and G‐ratio developed normally up to 4 months. At 7 months, however, axons had become thinner, while in control mice axonal diameters had increased further. Myelin sheath thickness remained close to normal, resulting in an abnormally low G‐ratio in Eif2b5‐mutant mice. In more severely affected Eif2b4‐Eif2b5 double‐mutants, similar abnormalities were already present at 4 months, while in milder affected Eif2b4 mutants, few abnormalities were observed at 7 months. Additionally, from 2 months onward an increased percentage of thin, unmyelinated axons and increased axonal density were present in Eif2b5‐mutant mice. Co‐cultures showed that Eif2b5 mutant astrocytes induced increased axonal density, also in control forebrain tissue, and that control astrocytes induced normal axonal density, also in mutant forebrain tissue. In vanishing white matter patient brains, axons and myelin sheaths were thinner than normal in moderately and severely affected white matter. In mutant mice and patients, signs of axonal transport defects and cytoskeletal abnormalities were minimal.InterpretationIn vanishing white matter, axons are initially normal and atrophy later. Astrocytes are central in this process. If therapy becomes available, axonal pathology may be prevented with early intervention.

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Section: Introductionmentioning

confidence: 99%

Axonal abnormalities in vanishing white matter

Klok

Bugiani

Vries

et al. 2018

Ann Clin Transl Neurol

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“…It is caused by recessive mutations in any of the genes EIF2B1–5. 5, 6 Patients typically have normal early development, followed by chronic neurological deterioration and additionally stress‐provoked episodes of rapid decline 2. No curative treatment is available 7.…”

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confidence: 99%

Natural History of Vanishing White Matter

Hamilton

Lei

Vermeulen

et al. 2018

Annals of Neurology

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173

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ObjectiveTo comprehensively describe the natural history of vanishing white matter (VWM), aiming at improving counseling of patients/families and providing natural history data for future therapeutic trials.MethodsWe performed a longitudinal multicenter study among 296 genetically confirmed VWM patients. Clinical information was obtained via disease‐specific clinical questionnaire, Health Utilities Index and Guy's Neurological Disability Scale assessments, and chart review.ResultsFirst disease signs occurred at a median age of 3 years (mode = 2 years, range = before birth to 54 years); 60% of patients were symptomatic before the age of 4 years. The nature of the first signs varied for different ages of onset. Overall, motor problems were the most common presenting sign, especially in children. Adolescent and adult onset patients were more likely to exhibit cognitive problems early after disease onset. One hundred two patients were deceased. Multivariate Cox regression analysis revealed a positive relation between age at onset and both preservation of ambulation and survival. Absence of stress‐provoked episodes and absence of seizures predicted more favorable outcome. In patients with onset before 4 years, earlier onset was associated with more severe disability and higher mortality. For onset from 4 years on, disease course was generally milder, with a wide variation in severity. There were no significant differences for sex or for the 5 eIF2B gene groups. The results confirm the presence of a genotype–phenotype correlation.InterpretationThe VWM disease spectrum consists of a continuum with extremely wide variability. Age at onset is a strong predictor for disease course. Ann Neurol 2018;84:274–288

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“…To initiate the next round of translations, eIF2-bound GDP must be replaced by GTP; in this process, eIF2B subunits catalyze the exchange of GDP with GTP. 16 The pathogenic mechanisms of VWM due to eIF2B gene defects are far from well understood; the aberrant translation of some protein with upstream open reading frames in mRNA, such as activating transcription factor (ATF) 4, and activation of unfolded-protein response (UPR) in ER are believed to be involved. [12][13][14][15] eIF2B is a complex of five subunits.…”

Section: Discussionmentioning

confidence: 99%

“…Mutations in EIF2B1-5, encoding the five subunits of eukaryotic translation initiation factor (eIF2B a, b, g, d and e), respectively, were found in VWM patients. 4,5 eIF2B, along with some other eIFs, plays key roles in the initiation of protein translation in all eukaryotic cells. Since 2001, more than 120 mutations in EIF2B1-5 have been identified.…”

Section: Introductionmentioning

confidence: 99%

Identification of novel EIF2B mutations in Chinese patients with vanishing white matter disease

Pan

et al. 2009

J Hum Genet

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Subunits of the translation initiation factor eIF2B are mutant in leukoencephalopathy with vanishing white matter

Cited by 372 publications

References 20 publications

Axonal abnormalities in vanishing white matter

Axonal abnormalities in vanishing white matter

Natural History of Vanishing White Matter

Identification of novel EIF2B mutations in Chinese patients with vanishing white matter disease

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