Pam and Its Ortholog Highwire Interact with and May Negatively Regulate the TSC1·TSC2 Complex

Murthy, Vanishree; Han, Sungwon; Beauchamp, Roberta L.; Smith, Nicole; Haddad, Luciana A.; Ito, Naoto; Ramesh, Vijaya

doi:10.1074/jbc.m310208200

Cited by 76 publications

(77 citation statements)

References 43 publications

(54 reference statements)

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“…Complete loss of function of fsn-1 in C. elegans results in defects that are characterized by the simultaneous presence of overdeveloped and underdeveloped neuromuscular junctions (NMJs) and which are similar to, but not as pronounced as, those observed in rpm-1 Ϫ/Ϫ mutants. These genetic findings support the notion that the functions of FSN-1 and RPM-1 are partially overlapping (21).Although PHR family members interact with many potential targets (11,24,26,31), genetic data have shown that one key substrate of RPM-1 and HIW is the mitogen-activated protein kinase kinase kinase known as DLK (dual leucine zipper kinase) in C. elegans and known as Wallenda in D. melanogaster, respectively. The abundance of this kinase is increased in rpm-1 or hiw mutants, and synaptic defects in the mutant worms and flies are suppressed by a loss of DLK or Wallenda.…”

supporting

confidence: 69%

Fbxo45 Forms a Novel Ubiquitin Ligase Complex and Is Required for Neuronal Development

Saiga

Fukuda

Matsumoto

et al. 2009

Molecular and Cellular Biology

108

131

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Fbxo45 is an F-box protein that is restricted to the nervous system. Unlike other F-box proteins, Fbxo45 was found not to form an SCF complex as a result of an amino acid substitution in the consensus sequence for Cul1 binding. Proteomics analysis revealed that Fbxo45 specifically associates with PAM (protein associated with Myc), a RING finger-type ubiquitin ligase. Mice deficient in Fbxo45 were generated and found to die soon after birth as a result of respiratory distress. Fbxo45؊/؊ embryos show abnormal innervation of the diaphragm, impaired synapse formation at neuromuscular junctions, and aberrant development of axon fiber tracts in the brain. Similar defects are also observed in mice lacking Phr1 (mouse ortholog of PAM), suggesting that Fbxo45 and Phr1 function in the same pathway. In addition, neuronal migration was impaired in Fbxo45 ؊/؊ mice. These results suggest that Fbxo45 forms a novel Fbxo45-PAM ubiquitin ligase complex that plays an important role in neural development.Ubiquitin-dependent proteolysis is indispensable for various biological processes (3,40). Protein ubiquitylation is mediated by several enzymes that act in concert, with a ubiquitin ligase (E3) playing a key role in substrate recognition (14). E3 enzymes contain specific structural motifs that mediate recruitment of a ubiquitin-conjugating enzyme (E2), with these motifs including HECT, RING finger, U-box, and PHD finger domains (30). The SCF complex consists of Skp1 (adaptor subunit), Cul1 (scaffold subunit), an F-box protein (substrate recognition subunit), and Rbx1 (also known as Roc1 or Hrt1; RING finger-containing subunit). Whereas Skp1, Cul1, and Rbx1 are common to all SCF complexes, the F-box protein is variable (with ϳ70 such proteins having been identified in humans) and confers substrate specificity.Fbxo45 is an F-box protein that was originally isolated as an estrogen-induced protein (47). Human and mouse Fbxo45 genes comprise three exons and possess several consensus binding sequences for the estrogen receptor in the promoter region. Fbxo45 mRNA is rapidly induced on exposure of MCF-7 cells to 17␤-estradiol (47). FSN-1, the Caenorhabditis elegans ortholog of Fbxo45, binds to RPM-1 (regulator of presynaptic morphology 1) together with CUL-1 and SKR-1, the C. elegans orthologs of mammalian Cul1 and Skp1, respectively (21, 46). RPM-1 belongs to an evolutionarily conserved family of proteins (the PHR family) that include Highwire (HIW) (Drosophila melanogaster), Esrom (Danio rerio), Phr1 (Mus musculus), and protein associated with Myc (PAM) (Homo sapiens), each of which contains a RING-finger domain that is required for its E3 activity (7,20,21,27,44). Complete loss of function of fsn-1 in C. elegans results in defects that are characterized by the simultaneous presence of overdeveloped and underdeveloped neuromuscular junctions (NMJs) and which are similar to, but not as pronounced as, those observed in rpm-1 Ϫ/Ϫ mutants. These genetic findings support the notion that the functions of FSN-1 and RPM-1 are partially overlappi...

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supporting

confidence: 69%

Fbxo45 Forms a Novel Ubiquitin Ligase Complex and Is Required for Neuronal Development

Saiga

Fukuda

Matsumoto

et al. 2009

Molecular and Cellular Biology

108

131

View full text Add to dashboard Cite

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“…The partial innervation of the diaphragm and the thinner phrenic nerve that we have observed in mice also raises the possibility that PHR1 regulates factors critical for proper axonal outgrowth (14). Thus, PHR1 activity would be important not only for the proper function of neuronal connections but also for their formation.…”

Section: Discussionmentioning

confidence: 82%

Evidence for a Conserved Function in Synapse Formation Reveals Phr1 as a Candidate Gene for Respiratory Failure in Newborn Mice

Burgess

Peterson

Johnson

et al. 2004

Molecular and Cellular Biology

101

105

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Genetic studies using a set of overlapping deletions centered at the piebald locus on distal mouse chromosome 14 have defined a genomic region associated with respiratory distress and lethality at birth. We have isolated and characterized the candidate gene Phr1 that is located within the respiratory distress critical genomic interval. Phr1 is the ortholog of the human Protein Associated with Myc as well as Drosophila highwire and Caenorhabditis elegans regulator of presynaptic morphology 1. Phr1 is expressed in the embryonic and postnatal nervous system. In mice lacking Phr1, the phrenic nerve failed to completely innervate the diaphragm. In addition, nerve terminal morphology was severely disrupted, comparable with the synaptic defects seen in the Drosophila hiw and C. elegans rpm-1 mutants. Although intercostal muscles were completely innervated, they also showed dysmorphic nerve terminals. In addition, sensory neuron terminals in the diaphragm were abnormal. The neuromuscular junctions showed excessive sprouting of nerve terminals, consistent with inadequate presynaptic stimulation of the muscle. On the basis of the abnormal neuronal morphology seen in mice, Drosophila, and C. elegans, we propose that Phr1 plays a conserved role in synaptic development and is a candidate gene for respiratory distress and ventilatory disorders that arise from defective neuronal control of breathing.

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“…One group comprised proteins representing different signaling pathways. The second group included proteins involved in transcriptional regulation, which was not unexpected, because the involvement of MYCBP2 in the regulation of transcriptional and translational regulation through Myc and mTOR signaling pathways has been demonstrated previously by different groups (1,21,41). The largest group comprised cytoskeletal associated proteins involved in growth regulation and receptor or vesicle trafficking, such as ROCK2, myosin Va, and myosin VI (31,33,42).…”

Section: Discussionmentioning

confidence: 99%

The Ubiquitin Ligase MYCBP2 Regulates Transient Receptor Potential Vanilloid Receptor 1 (TRPV1) Internalization through Inhibition of p38 MAPK Signaling

Holland

Coste

Zhang

et al. 2011

Journal of Biological Chemistry

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The E3 ubiquitin ligase MYCBP2 negatively regulates neuronal growth, synaptogenesis, and synaptic strength. More recently it was shown that MYCBP2 is also involved in receptor and ion channel internalization. We found that mice with a MYCBP2-deficiency in peripheral sensory neurons show prolonged thermal hyperalgesia. Loss of MYCBP2 constitutively activated p38 MAPK and increased expression of several proteins involved in receptor trafficking. Surprisingly, loss of MYCBP2 inhibited internalization of transient receptor potential vanilloid receptor 1 (TRPV1) and prevented desensitization of capsaicin-induced calcium increases. Lack of desensitization, TRPV internalization and prolonged hyperalgesia were reversed by inhibition of p38 MAPK. The effects were TRPVspecific, since neither mustard oil-induced desensitization nor behavioral responses to mechanical stimuli were affected. In summary, we show here for the first time that p38 MAPK activation can inhibit activity-induced ion channel internalization and that MYCBP2 regulates internalization of TRPV1 in peripheral sensory neurons as well as duration of thermal hyperalgesia through p38 MAPK.The E3-ubiquitin ligase MYCBP2 (Myc-binding protein 2; also known as protein associated with Myc (PAM)) 2 is an unusual large protein with a predicted size of 510 kDa. MYCBP2 orthologs have been described in mouse as Phr1, in zebrafish as Esrom, in drosophila as Highwire and in Caenorhabditis elegans as RPM-1. While MYCBP2 mRNA is found in nearly all human tissues, its expression is exceptionally high in peripheral and central neurons (1-3). MYCBP2 has been shown to act as negative regulators of synaptic growth, synaptogenesis, and neurite growth in C. elegans (4), Drosophila (5), zebrafish (6), and mice (7,8). In C. elegans and Drosophila MYCBP2-dependent growth inhibition is largely mediated by the p38 MAPK pathway (9, 10) whereas in mice the role of p38 MAPK in MYCBP2-regulated axonal growth is less clear.Whereas growth regulation of cortical axons by MYCBP2 does not involve p38 MAPK (8), MYCBP2-dependent axonal overgrowth of spinal cord motor neurons and sensory dorsal root ganglion (DRG) neurons was regulated by p38 MAPKmediated alterations in microtubule stability (11).Besides its role in the regulation of neuronal growth, also a function of MYCBP2 in neuronal transmission has been demonstrated. In C. elegans and drosophila loss-of-function mutations in the MYCBP2 orthologs decreased the number of synaptic vesicles at cholinergic and GABAergic synapses in a p38 MAPK-dependent manner (9) and reduced strength of synaptic transmission at neuromuscular junctions (5, 12, 13). More recently, it was shown that the MYCBP2 ortholog in C. elegans, RPM-1, prevents in central neurons activity-dependent internalization of AMPA receptors by inhibiting p38 MAPK signaling through ubiquitylation of MAPK kinase kinase 12 (MAPKKK12), (14). Loss of RPM-1 caused constitutive activation of p38MAPK leading to an increased internalization of the AMPA receptor ortholog GLR1.Interestingly, in ma...

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Pam and Its Ortholog Highwire Interact with and May Negatively Regulate the TSC1·TSC2 Complex

Cited by 76 publications

References 43 publications

Fbxo45 Forms a Novel Ubiquitin Ligase Complex and Is Required for Neuronal Development

Fbxo45 Forms a Novel Ubiquitin Ligase Complex and Is Required for Neuronal Development

Evidence for a Conserved Function in Synapse Formation Reveals Phr1 as a Candidate Gene for Respiratory Failure in Newborn Mice

The Ubiquitin Ligase MYCBP2 Regulates Transient Receptor Potential Vanilloid Receptor 1 (TRPV1) Internalization through Inhibition of p38 MAPK Signaling

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