Complex formation between calmodulin and a peptide from the intracellular loop of the gap junction protein connexin43: Molecular conformation and energetics of binding

Myllykoski, Matti; Kuczera, Krzysztof; Kursula, Petri

doi:10.1016/j.bpc.2009.08.001

Cited by 15 publications

(21 citation statements)

References 36 publications

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“…The Cx36 binding motif is highly conserved across species from humans to lower vertebrates, like lamprey and zebrafish, and overlapping with a CaMKII binding site (Alev et al, 2008). In contrast, the CaM binding sites of Cx35/Cx36 are distinct from other connexins including Cx32, Cx43, Cx44, Cx46, and Cx50 in terms of ligand class (1–8 versus 1–5–10), location of the ligand binding sites, and resemble to date the only connexins activated by CaM (Zhou et al, 2007, 2009; Dodd et al, 2008; Myllykoski et al, 2009; Chen et al, 2011; Xu et al, 2012; Mruk et al, 2014). …”

Section: Discussionmentioning

confidence: 84%

“…In more general terms, connexins bind CaM with dissociation kinetics and thermodynamic characteristics covering more than a 100-fold range (Dodd et al, 2008; Myllykoski et al, 2009; Zhou et al, 2009; Chen et al, 2011). Together, the specific localization of binding motifs, distinct subclasses and different dissociation kinetics suggest functional adaptations specific for each connexins protein.…”

Section: Discussionmentioning

confidence: 99%

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Structural and Functional Consequences of Connexin 36 (Cx36) Interaction with Calmodulin

Siu

Smirnova

Brown

et al. 2016

Front. Mol. Neurosci.

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Functional plasticity of neuronal gap junctions involves the interaction of the neuronal connexin36 with calcium/calmodulin-dependent kinase II (CaMKII). The important relationship between Cx36 and CaMKII must also be considered in the context of another protein partner, Ca2+ loaded calmodulin, binding an overlapping site in the carboxy-terminus of Cx36. We demonstrate that CaM and CaMKII binding to Cx36 is calcium-dependent, with Cx36 able to engage with CaM outside of the gap junction plaque. Furthermore, Ca2+ loaded calmodulin activates Cx36 channels, which is different to other connexins. The NMR solution structure demonstrates that CaM binds Cx36 in its characteristic compact state with major hydrophobic contributions arising from W277 at anchor position 1 and V284 at position 8 of Cx36. Our results establish Cx36 as a hub binding Ca2+ loaded CaM and they identify this interaction as a critical step with implications for functions preceding the initiation of CaMKII mediated plasticity at electrical synapses.

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Section: Discussionmentioning

confidence: 84%

Section: Discussionmentioning

confidence: 99%

Structural and Functional Consequences of Connexin 36 (Cx36) Interaction with Calmodulin

Siu

Smirnova

Brown

et al. 2016

Front. Mol. Neurosci.

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“…Synchrotron small-angle X-ray scattering (SAXS) data for rmMBP were collected on beamline I711 [25] at MAX-Lab, Lund, Sweden, and analyzed as previously described [7], [8], [26]. An exposure time of 10 min was used for all samples.…”

Section: Methodsmentioning

confidence: 99%

“…The final model was obtained in each case from 10 independent ab initio models by averaging by DAMAVER [30]. CaM was used as a molecular weight standard due to its similar size to MBP and previously observed good behaviour in our SAXS experiments [7], [26].…”

Section: Methodsmentioning

confidence: 99%

Charge Isomers of Myelin Basic Protein: Structure and Interactions with Membranes, Nucleotide Analogues, and Calmodulin

et al. 2011

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As an essential structural protein required for tight compaction of the central nervous system myelin sheath, myelin basic protein (MBP) is one of the candidate autoantigens of the human inflammatory demyelinating disease multiple sclerosis, which is characterized by the active degradation of the myelin sheath. In this work, recombinant murine analogues of the natural C1 and C8 charge components (rmC1 and rmC8), two isoforms of the classic 18.5-kDa MBP, were used as model proteins to get insights into the structure and function of the charge isomers. Various biochemical and biophysical methods such as size exclusion chromatography, calorimetry, surface plasmon resonance, small angle X-ray and neutron scattering, Raman and fluorescence spectroscopy, and conventional as well as synchrotron radiation circular dichroism were used to investigate differences between these two isoforms, both from the structural point of view, and regarding interactions with ligands, including calmodulin (CaM), various detergents, nucleotide analogues, and lipids. Overall, our results provide further proof that rmC8 is deficient both in structure and especially in function, when compared to rmC1. While the CaM binding properties of the two forms are very similar, their interactions with membrane mimics are different. CaM can be used to remove MBP from immobilized lipid monolayers made of synthetic lipids - a phenomenon, which may be of relevance for MBP function and its regulation. Furthermore, using fluorescently labelled nucleotides, we observed binding of ATP and GTP, but not AMP, by MBP; the binding of nucleoside triphosphates was inhibited by the presence of CaM. Together, our results provide important further data on the interactions between MBP and its ligands, and on the differences in the structure and function between MBP charge isomers.

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“…It has for instance been shown to contain the preferred interaction site for calmodulin (CaM; region 136–158) and as such, to mediate the closure of GJ channels in response to increasing [Ca 2+ ] i (Zhou et al, 2007; Myllykoski et al, 2009). Indeed, Ca 2+ -induced closure of GJs is likely to be mediated by intracellular effector proteins since the uncoupled state may persist long after [Ca 2+ ] i has been restored (Cotrina et al, 1998; Lurtz and Louis, 2003, 2007).…”

Section: Oddd-linked Mutations and Cx43 Channel Functionmentioning

confidence: 99%

Neurological manifestations of oculodentodigital dysplasia: a Cx43 channelopathy of the central nervous system?

et al. 2013

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The coordination of tissue function is mediated by gap junctions (GJs) that enable direct cell–cell transfer of metabolic and electric signals. GJs are formed by connexins of which Cx43 is most widespread in the human body. In the brain, Cx43 GJs are mostly found in astroglia where they coordinate the propagation of Ca2+ waves, spatial K+ buffering, and distribution of glucose. Beyond its role in direct intercellular communication, Cx43 also forms unapposed, non-junctional hemichannels in the plasma membrane of glial cells. These allow the passage of several neuro- and gliotransmitters that may, combined with downstream paracrine signaling, complement direct GJ communication among glial cells and sustain glial-neuronal signaling. Mutations in the GJA1 gene encoding Cx43 have been identified in a rare, mostly autosomal dominant syndrome called oculodentodigital dysplasia (ODDD). ODDD patients display a pleiotropic phenotype reflected by eye, hand, teeth, and foot abnormalities, as well as craniofacial and bone malformations. Remarkably, neurological symptoms such as dysarthria, neurogenic bladder (manifested as urinary incontinence), spasticity or muscle weakness, ataxia, and epilepsy are other prominent features observed in ODDD patients. Over 10 mutations detected in patients diagnosed with neurological disorders are associated with altered functionality of Cx43 GJs/hemichannels, but the link between ODDD-related abnormal channel activities and neurologic phenotype is still elusive. Here, we present an overview on the nature of the mutants conveying structural and functional changes of Cx43 channels and discuss available evidence for aberrant Cx43 GJ and hemichannel function. In a final step, we examine the possibilities of how channel dysfunction may lead to some of the neurological manifestations of ODDD.

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Complex formation between calmodulin and a peptide from the intracellular loop of the gap junction protein connexin43: Molecular conformation and energetics of binding

Cited by 15 publications

References 36 publications

Structural and Functional Consequences of Connexin 36 (Cx36) Interaction with Calmodulin

Structural and Functional Consequences of Connexin 36 (Cx36) Interaction with Calmodulin

Charge Isomers of Myelin Basic Protein: Structure and Interactions with Membranes, Nucleotide Analogues, and Calmodulin

Neurological manifestations of oculodentodigital dysplasia: a Cx43 channelopathy of the central nervous system?

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