MEIS1 intronic risk haplotype associated with restless legs syndrome affects its mRNA and protein expression levels

Xiong, Lan; Catoire, Hélène; Dion, Patrick A.; Gaspar, Cláudia; Lafrenière, Ronald G.; Girard, Simon L.; Levchenko, Аnastasia; Rivière, Jean Baptiste; Fiori, Laura M.; St‐Onge, Judith; Bachand, Isabelle; Thibodeau, Pascale; Allen, Richard P.; Earley, Christopher J.; Turecki, Gustavo; Montplaisir, Jacques; Rouleau, Guy A.

doi:10.1093/hmg/ddn443

Cited by 83 publications

(96 citation statements)

References 56 publications

(47 reference statements)

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“…The extracted RNA was reverse-transcribed (RT) using a classic protocol (7). Different primers were design to flank the mutation site as follows: primers "4" hybridized at the beginning of exon 4 (5Ј-GAAATGGACACCAGACCGAA-3Ј); primers "4/5" hybridized at the junction of exons 4 and 5 (5Ј-GCCCAC-CAAGACCCCCCAAA-3Ј); primers "5/6" hybridized at the junction of exons 5 and 6 (5Ј-TCAACATTGTACAGCAG-CAG-3Ј), and primers "6" hybridized at the end of exon 6 (5Ј-TGGCACCACTCCATTAGTGG-3Ј).…”

Section: Methodsmentioning

confidence: 99%

Transit Defect of Potassium-Chloride Co-transporter 3 Is a Major Pathogenic Mechanism in Hereditary Motor and Sensory Neuropathy with Agenesis of the Corpus Callosum

Salin-Cantegrel

Rivière

Shekarabi

et al. 2011

Journal of Biological Chemistry

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Missense and protein-truncating mutations of the human potassium-chloride co-transporter 3 gene (KCC3) cause hereditary motor and sensory neuropathy with agenesis of the corpus callosum (HMSN/ACC), which is a severe neurodegenerative disease characterized by axonal dysfunction and neurodevelopmental defects. We previously reported that KCC3-truncating mutations disrupt brain-type creatine kinase-dependent activation of the co-transporter through the loss of its last 140 amino acids. Here, we report a novel and more distal HMSN/ACCtruncating mutation (3402C3 T; R1134X) that eliminates only the last 17 residues of the protein. This small truncation disrupts the interaction with brain-type creatine kinase in mammalian cells but also affects plasma membrane localization of the mutant transporter. Although it is not truncated, the previously reported HMSN/ACC-causing 619C3 T (R207C) missense mutation also leads to KCC3 loss of function in Xenopus oocyte flux assay. Immunodetection in Xenopus oocytes and in mammalian cultured cells revealed a decreased amount of R207C at the plasma membrane, with significant retention of the mutant proteins in the endoplasmic reticulum. In mammalian cells, curcumin partially corrected these mutant protein mislocalizations, with more protein reaching the plasma membrane. These findings suggest that mis-trafficking of mutant protein is an important pathophysiological feature of HMSN/ACC causative KCC3 mutations.

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Section: Methodsmentioning

confidence: 99%

Transit Defect of Potassium-Chloride Co-transporter 3 Is a Major Pathogenic Mechanism in Hereditary Motor and Sensory Neuropathy with Agenesis of the Corpus Callosum

Salin-Cantegrel

Rivière

Shekarabi

et al. 2011

Journal of Biological Chemistry

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“…Key roles of this transcription factor are now documented both in normal development and disease formation (1)(2)(3)(4). Decreased MEIS1 levels are associated with Restless leg syndrome (RLS) (5,6). Overexpression of MEIS1, on the other hand, has been linked to leukemia (3,4).…”

Section: Introductionmentioning

confidence: 99%

Identification of E74-like factor 1 (ELF1) as a transcriptional regulator of the Hox cofactor MEIS1

Xiang

Argiropoulos

et al. 2010

Experimental Hematology

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Objective-MEIS1 is a Hox cofactor known for its role in development and strongly linked to normal and leukemic hematopoiesis. Although previous studies have focused on identifying protein partners of MEIS1 and its transcriptionaly regulated targets, little is known about the upstream transcriptional regulators of this tightly regulated gene. Understanding the regulation of MEIS1 is important toward the understanding of normal hematopoiesis and leukemogenesis.Materials and Methods-Here we describe our studies focusing on the evolutionary conserved putative MEIS1 promoter region. Phylogenetic sequence analysis followed and reporter assays in MEIS1 expressing (K562) and non-expressing (HL60) leukemic cell line models were used to identify key regulatory regions and potential transcription factor binding sites within the candidate promoter region followed by functional and expression studies of one identified regulator in both cell lines and primary human cord blood and leukemia samples. Results-The chromatin status of MEIS1 promoter region is associated with MEIS1 expression.Truncation and mutation studies coupled with reporter assays revealed that a conserved ETS family member binding site located 289bp upstream of the annotated human MEIS1 transcription start site (AHTSS) is required for promoter activity. Of the three ETS family members tested, only ELF1 was enriched on the MEIS1 promoter as assessed by both electrophoretic mobility shift assay (EMSA) and chromatin immunoprecipitation (ChIP) experiments in K562. This finding was confirmed in MEIS1 expressing primary human samples. Moreover, siRNA -mediated knockdown of ELF1 in K562 cells was associated with a decreased MEIS1 expression.Conclusions-We conclude that the ETS transcription factor ELF1 is an important positive regulator of MEIS1 expression.

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“…A minor allele in MEIS1 nearly doubles a person's risk and is in a suspected cis-regulatory element potentially associated with reductions in MEIS1 messenger RNA (mRNA) and protein expression. 24,25 RLS susceptibility variants associated with PTPRD, MAP2K5, SKOR1, and TOX3 confer more modest risks. Almost nothing is known about how factors generally acknowledged to influence RLS expressivity (eg, female sex, advanced age, and iron decrements) 3 interact with these at-risk variants.…”

Section: Genome-wide Association Studiesmentioning

confidence: 98%

“…Similarly, informative cis (local) or trans (distant) regulatory effects on gene and protein expression and splice variants associated with the at-risk alleles have not been reported. 12,19,20,24 The coding regions and exon-intron boundaries of BTBD9 4,26 and MEIS1 24,26,27 also lack any common functional polymorphisms. Several rare exonic variants in MEIS1 have been reported, but they do not segregate faithfully with the RLS phenotype.…”

Section: Genome-wide Association Studiesmentioning

confidence: 99%

The Molecular Genetics of Restless Legs Syndrome

Rye

2015

Sleep Medicine Clinics

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MEIS1 intronic risk haplotype associated with restless legs syndrome affects its mRNA and protein expression levels

Cited by 83 publications

References 56 publications

Transit Defect of Potassium-Chloride Co-transporter 3 Is a Major Pathogenic Mechanism in Hereditary Motor and Sensory Neuropathy with Agenesis of the Corpus Callosum

Transit Defect of Potassium-Chloride Co-transporter 3 Is a Major Pathogenic Mechanism in Hereditary Motor and Sensory Neuropathy with Agenesis of the Corpus Callosum

Identification of E74-like factor 1 (ELF1) as a transcriptional regulator of the Hox cofactor MEIS1

The Molecular Genetics of Restless Legs Syndrome

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