Keppen-Lubinsky Syndrome Is Caused by Mutations in the Inwardly Rectifying K+ Channel Encoded by KCNJ6

Masotti, Andrea; Uva, Paolo; Davis‐Keppen, Laura; Basel‐Vanagaite, Lina; Cohen, Lior; Pisaneschi, Elisa; Celluzzi, Antonella; Bencivenga, Paola; Fang, Mingyan; Tian, Mingyu; Xu, Xun; Cappa, Marco; Dallapiccola, Bruno

doi:10.1016/j.ajhg.2014.12.011

Cited by 95 publications

(78 citation statements)

References 25 publications

(31 reference statements)

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“…[12][13][14][15] By contrast, the other types of lipodystrophy-mandibuloacral dysplasia, autoinflammatory lipodystrophy, progeroid syndromes associated lipodystrophy, SHORT syndrome associated lipodystrophy and Keppen-Lubinsky syndrome associ ated lipodystrophy-are extremely rare and in total each subtype has been reported in no more than 30 patients (Box 1). 10,11,[16][17][18][19][20][21][22][23][24][25][26][27][28][29][30] However, FPLD has autosomal dominant inheritance and some patients with subtle loss of fat from the extremities might not receive an accurate diagnosis; therefore, the prevalence of this lipodystrophy might be higher than is reported. CGL has the most extreme pheno type with loss of nearly all the body fat at birth ( Figure 1) and early development of metabolic complications in childhood.…”

Section: Introductionmentioning

confidence: 59%

Congenital generalized lipodystrophies—new insights into metabolic dysfunction

2015

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Congenital generalized lipodystrophy (CGL) is a heterogeneous autosomal recessive disorder characterized by a near complete lack of adipose tissue from birth and, later in life, the development of metabolic complications, such as diabetes mellitus, hypertriglyceridaemia and hepatic steatosis. Four distinct subtypes of CGL exist: type 1 is associated with AGPAT2 mutations; type 2 is associated with BSCL2 mutations; type 3 is associated with CAV1 mutations; and type 4 is associated with PTRF mutations. The products of these genes have crucial roles in phospholipid and triglyceride synthesis, as well as in the formation of lipid droplets and caveolae within adipocytes. The predominant cause of metabolic complications in CGL is excess triglyceride accumulation in the liver and skeletal muscle owing to the inability to store triglycerides in adipose tissue. Profound hypoleptinaemia further exacerbates metabolic derangements by inducing a voracious appetite. Patients require psychological support, a low-fat diet, increased physical activity and cosmetic surgery. Aside from conventional therapy for hyperlipidaemia and diabetes mellitus, metreleptin replacement therapy can dramatically improve metabolic complications in patients with CGL. In this Review, we discuss the molecular genetic basis of CGL, the pathogenesis of the disease's metabolic complications and therapeutic options for patients with CGL.

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Section: Introductionmentioning

confidence: 59%

Congenital generalized lipodystrophies—new insights into metabolic dysfunction

2015

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“…Consistent with this view, a missense mutation of Kcnj6 altering the pore-forming domain of the potassium channel is responsible for the ‘ weaver’ phenotype, characterized by abnormal development of the cerebellum (Patil et al, 1995). In addition, a heterozygous deletion of three nucleotides or a missense mutation introducing a single amino acid change from glycine to serine in Kir3.2 subunit causes the Keppen-Lubinsky syndrome, a rare genetic disorder characterized by severe developmental delay, intellectual disability, and microcephaly (Basel-Vanagaite et al, 2009; Masotti et al, 2015). …”

Section: Discussionmentioning

confidence: 99%

Evidence that increased Kcnj6 gene dose is necessary for deficits in behavior and dentate gyrus synaptic plasticity in the Ts65Dn mouse model of Down syndrome

Kleschevnikov

Kim

et al. 2017

Neurobiology of Disease

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Down syndrome (DS), trisomy 21, is caused by increased dose of genes present on human chromosome 21 (HSA21). The gene-dose hypothesis argues that a change in the dose of individual genes or regulatory sequences on HSA21 is necessary for creating DS-related phenotypes, including cognitive impairment. We focused on a possible role for Kcnj6, the gene encoding Kir3.2 (Girk2) subunits of a G-protein-coupled inwardly-rectifying potassium channel. This gene resides on a segment of mouse Chromosome 16 that is present in one extra copy in the genome of the Ts65Dn mouse, a well-studied genetic model of DS. Kir3.2 subunit-containing potassium channels serve as effectors for a number of postsynaptic metabotropic receptors including GABAB receptors. Several studies raise the possibility that increased Kcnj6 dose contributes to synaptic and cognitive abnormalities in DS. To assess directly a role for Kcnj6 gene dose in cognitive deficits in DS, we produced Ts65Dn mice that harbor only 2 copies of Kcnj6 (Ts65Dn:Kcnj6++− mice). The reduction in Kcnj6 gene dose restored to normal the hippocampal level of Kir3.2. Long-term memory, examined in the novel object recognition test with the retention period of 24h, was improved to the level observed in the normosomic littermate control mice (2N:Kcnj6++). Significantly, both short-term and long-term potentiation (STP and LTP) was improved to control levels in the dentate gyrus (DG) of the Ts65Dn:Kcnj6++− mouse. In view of the ability of fluoxetine to suppress Kir3.2 channels, we asked if fluoxetine-treated DG slices of Ts65Dn:Kcnj6+++ mice would rescue synaptic plasticity. Fluoxetine increased STP and LTP to control levels. These results are evidence that increased Kcnj6 gene dose is necessary for synaptic and cognitive dysfunction in the Ts65Dn mouse model of DS. Strategies aimed at pharmacologically reducing channel function should be explored for enhancing cognition in DS.

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“…), as well as being responsible for several classes of developmental malformation in humans (Galanopoulou ; Tristani‐Firouzi & Etheridge ; Masotti et al. ). Bioelectric signals can trigger the formation of whole ectopic organs, such as in the case of eye development (Pai et al.…”

Section: Introductionmentioning

confidence: 99%

Genome‐wide analysis reveals conserved transcriptional responses downstream of resting potential change in Xenopus embryos, axolotl regeneration, and human mesenchymal cell differentiation

et al. 2015

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Endogenous bioelectric signaling via changes in cellular resting potential (V mem ) is a key regulator of patterning during regeneration and embryogenesis in numerous model systems. Depolarization of V mem has been functionally implicated in dedifferentiation, tumorigenesis, anatomical re-specification, and appendage regeneration. However, no unbiased analyses have been performed to understand genome-wide transcriptional responses to V mem change in vivo. Moreover, it is unknown which genes or gene networks represent conserved targets of bioelectrical signaling across different patterning contexts and species. Here, we use microarray analysis to comparatively analyze transcriptional responses to V mem depolarization. We compare the response of the transcriptome during embryogenesis (Xenopus development), regeneration (axolotl regeneration), and stem cell differentiation (human mesenchymal stem cells in culture) to identify common networks across model species that are associated with depolarization. Both subnetwork enrichment and PANTHER analyses identified a number of key genetic modules as targets of V mem change, and also revealed important (well-conserved) commonalities in bioelectric signal transduction, despite highly diverse experimental contexts and species. Depolarization regulates specific transcriptional networks across all three germ layers (ectoderm, mesoderm, and endoderm) such as cell differentiation and apoptosis, and this information will be used for developing mechanistic models of bioelectric regulation of patterning. Moreover, our analysis reveals that V mem change regulates transcripts related to important disease pathways such as cancer and neurodegeneration, which may represent novel targets for emerging electroceutical therapies.

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Keppen-Lubinsky Syndrome Is Caused by Mutations in the Inwardly Rectifying K+ Channel Encoded by KCNJ6

Cited by 95 publications

References 25 publications

Congenital generalized lipodystrophies—new insights into metabolic dysfunction

Congenital generalized lipodystrophies—new insights into metabolic dysfunction

Evidence that increased Kcnj6 gene dose is necessary for deficits in behavior and dentate gyrus synaptic plasticity in the Ts65Dn mouse model of Down syndrome

Genome‐wide analysis reveals conserved transcriptional responses downstream of resting potential change in Xenopus embryos, axolotl regeneration, and human mesenchymal cell differentiation

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