Mutations in FLVCR1 Cause Posterior Column Ataxia and Retinitis Pigmentosa

Rajadhyaksha, Anjali M.; Elemento, Olivier; Puffenberger, Erik G.; Schierberl, Kathryn C.; Xiang, Jenny; Putorti, Maria Lisa; Berciano, José; Poulin, Chantal; Brais, Bernard; Michaelides, Michel; Weleber, Richard G.; Higgins, Joseph

doi:10.1016/j.ajhg.2010.10.013

Cited by 94 publications

(118 citation statements)

References 27 publications

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“…FLVCR1 mutations in DBA patients have not been found as of yet (19); however, if they were to exist, one would predict that they would occur in the FLVCR1b isoform. Interestingly, missense mutations in FLVCR1 have recently been described in patients with the rare autosomal recessive disease posterior column ataxia and retinitis pigmentosa (PCARP) (20,21). Three of the four reported disease-associated FLVCR1 variants, all of which are present in the homozygous state in PCARP patients, occur in exon 1 of the gene -the part of the gene that is omitted in the FLVCR1b transcript and protein.…”

Section: Flvcr1 and Human Diseasementioning

confidence: 99%

Mitochondrial heme: an exit strategy at last

Fleming¹,

Hamza²

2012

J. Clin. Invest.

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Section: Flvcr1 and Human Diseasementioning

confidence: 99%

Mitochondrial heme: an exit strategy at last

Fleming¹,

Hamza²

2012

J. Clin. Invest.

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“…We achieved 65 ± 17X sequencing depth on average and at least 20X depth on 81.7 ± 7.8% of the region targeted. We performed single nucleotide variants (SNVs) calling using a previously published procedure [14][15][16]. We directly compared each relapse sample to its matched diagnosis tumor to identify gained or lost coding region nonsynonynmous SNVs at relapse (SNVs within copy number alteration (CNA) regions were excluded; Figure 2A; Additional file 4).…”

Section: Distinctive Genetic Evolution Patterns Of the Two Relapse Scmentioning

confidence: 99%

“…Duplicated paired reads were filtered and variant detection was performed as previously described [14][15][16]. Novel coding region SNVs (not present in SNP132) were further filtered according to sequencing depth (≥20X) and variant percentage (≥25%).…”

Section: Exome Analysis Pipeline Snv Discoverymentioning

confidence: 99%

Deep-sequencing reveals clonal evolution patterns and mutation events associated with relapse in B-cell lymphomas

Jiang¹,

Redmond²,

Nie³

et al. 2014

Genome Biol

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Background: Molecular mechanisms associated with frequent relapse of diffuse large B-cell lymphoma (DLBCL) are poorly defined. It is especially unclear how primary tumor clonal heterogeneity contributes to relapse. Here, we explore unique features of B-cell lymphomas -VDJ recombination and somatic hypermutation -to address this question. Results: We performed high-throughput sequencing of rearranged VDJ junctions in 14 pairs of matched diagnosis-relapse tumors, among which 7 pairs were further characterized by exome sequencing. We identify two distinctive modes of clonal evolution of DLBCL relapse: an early-divergent mode in which clonally related diagnosis and relapse tumors diverged early and developed in parallel; and a late-divergent mode in which relapse tumors developed directly from diagnosis tumors with minor divergence. By examining mutation patterns in the context of phylogenetic information provided by VDJ junctions, we identified mutations in epigenetic modifiers such as KMT2D as potential early driving events in lymphomagenesis and immune escape alterations as relapse-associated events. Conclusions: Altogether, our study for the first time provides important evidence that DLBCL relapse may result from multiple, distinct tumor evolutionary mechanisms, providing rationale for therapies for each mechanism. Moreover, this study highlights the urgent need to understand the driving roles of epigenetic modifier mutations in lymphomagenesis, and immune surveillance factor genetic lesions in relapse.

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“…To see this illustration in color, the reader is referred to the web version of this article at www .liebertpub.com/ars mitochondrial FLVCR1 expression, given that specific deletion of the Flvcr1a gene variant is dispensable for erythropoiesis, although necessary to prevent edema and hemorrhage (35). FLVCR1 mutations in humans are associated with the development of posterior column ataxia and retinitis pigmentosa (136), whereas FLVCR2 mutations have been associated to proliferative brain vasculopathy, such as observed in the Fowler syndrome (47). Conversely, mutations in ABCG2 and ABCB6 do not impair erythroid differentiation, suggesting a redundant role for these transporters in erythropoiesis (75,144,189).…”

Section: Fig 2 Bioavailable Fementioning

confidence: 99%

Coupling Heme and Iron MetabolismviaFerritin H Chain

Gozzelino

Soares

2014

Antioxidants & Redox Signaling

126

139

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Significance: Inflammation and immunity can be associated with varying degrees of heme release from hemoproteins, eventually leading to cellular and tissue iron (Fe) overload, oxidative stress, and tissue damage. Presumably, these deleterious effects contribute to the pathogenesis of systemic infections. Recent Advances: Heme release from hemoglobin sensitizes parenchyma cells to undergo programmed cell death in response to proinflammatory cytokines, such as tumor necrosis factor. This cytotoxic effect is driven by a mechanism involving intracellular accumulation of free radicals, which sustain the activation of the c-Jun N-terminal kinase ( JNK) signaling transduction pathway. While heme catabolism by heme oxygenase-1 (HO-1) prevents programmed cell death, this cytoprotective effect requires the co-expression of ferritin H (heart/heavy) chain (FTH), which controls the pro-oxidant effect of labile Fe released from the protoporphyrin IX ring of heme. This antioxidant effect of FTH restrains JNK activation, whereas JNK activation inhibits FTH expression, a cross talk that controls metabolic adaptation to cellular Fe overload associated with systemic infections. Critical Issues and Future Directions: Identification and characterization of the mechanisms via which FTH provides metabolic adaptation to tissue Fe overload should provide valuable information to our current understanding of the pathogenesis of systemic infections as well as other immune-mediated inflammatory diseases.

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Mutations in FLVCR1 Cause Posterior Column Ataxia and Retinitis Pigmentosa

Cited by 94 publications

References 27 publications

Mitochondrial heme: an exit strategy at last

Mitochondrial heme: an exit strategy at last

Deep-sequencing reveals clonal evolution patterns and mutation events associated with relapse in B-cell lymphomas

Coupling Heme and Iron MetabolismviaFerritin H Chain

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