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Literature DB >> 17640933

Low-affinity spermine block mediating outward currents through Kir2.1 and Kir2.2 inward rectifier potassium channels.

Abstract

The outward component of the strong inward rectifier K(+) current (I(Kir)) plays a pivotal role in polarizing the membranes of excitable and non-excitable cells and is regulated by voltage-dependent channel block by internal cations. Using the Kir2.1 channel, we previously showed that a small fraction of the conductance susceptible only to a low-affinity mode of block likely carries a large portion of the outward current. To further examine the relevance of the low-affinity block to outward I(Kir) and to explore its molecular mechanism, we studied the block of the Kir2.1 and Kir2.2 channels by spermine, which is the principal Kir2 channel blocker. Current-voltage relations of outward Kir2.2 currents showed a peak, a plateau and two peaks in the presence of 10, 1 and 0.1 microm spermine, respectively, which was explained by the presence of two conductances that differ in their susceptibility to spermine block. When the current-voltage relations showed one peak, like those of native I(Kir), outward Kir2.2 currents were mediated mostly by the conductance susceptible to the low-affinity block. They also flowed in a narrower range than the corresponding Kir2.1 currents, because of 3- to 4-fold greater susceptibility to the low-affinity block than in Kir2.1. Reducing external [K(+)] shifted the voltage dependences of both the high- and low-affinity block of Kir2.1 in parallel with the shift in the reversal potential, confirming the importance of the low-affinity block in mediating outward I(Kir). When Kir2.1 mutants known to have reduced sensitivity to internal blockers were examined, the D172N mutation in the transmembrane pore region made almost all of the conductance susceptible only to low-affinity block, while the E224G mutation in the cytoplasmic pore region reduced the sensitivity to low-affinity block without markedly altering that to the high-affinity block or the high/low conductance ratio. The effects of these mutations support the hypothesis that Kir2 channels exist in two states having different susceptibilities to internal cationic blockers.

Entities: Chemical Gene Mutation

Mesh：

Substances：

Year: 2007 PMID： 17640933 PMCID： PMC2277198 DOI： 10.1113/jphysiol.2007.136028

Source DB: PubMed Journal: J Physiol ISSN： 0022-3751 Impact factor: 5.182

56 in total

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2. Mechanism of IRK1 channel block by intracellular polyamines.

Authors: D Guo; Z Lu
Journal: J Gen Physiol Date: 2000-06 Impact factor: 4.086

3. The anomalous rectification and cation selectivity of the membrane of a starfish egg cell.

Authors: S Hagiwara; K Takahashi
Journal: J Membr Biol Date: 1974 Impact factor: 1.843

4. Calculator programs for computing the composition of the solutions containing multiple metals and ligands used for experiments in skinned muscle cells.

Authors: A Fabiato; F Fabiato
Journal: J Physiol (Paris) Date: 1979

5. Mutations in Kir2.1 cause the developmental and episodic electrical phenotypes of Andersen's syndrome.

Authors: N M Plaster; R Tawil; M Tristani-Firouzi; S Canún; S Bendahhou; A Tsunoda; M R Donaldson; S T Iannaccone; E Brunt; R Barohn; J Clark; F Deymeer; A L George; F A Fish; A Hahn; A Nitu; C Ozdemir; P Serdaroglu; S H Subramony; G Wolfe; Y H Fu; L J Ptácek
Journal: Cell Date: 2001-05-18 Impact factor: 41.582

6. Control of rectification and permeation by two distinct sites after the second transmembrane region in Kir2.1 K+ channel.

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Journal: J Physiol Date: 2001-03-15 Impact factor: 5.182

7. Influence of potassium ions and osmolality on the resting membrane potential of rabbit ventricular papillary muscle with estimation of the activity and the activity coefficient of internal potassium.

Authors: T Akiyama; H A Fozzard
Journal: Circ Res Date: 1975-11 Impact factor: 17.367

8. Comparison of cloned Kir2 channels with native inward rectifier K+ channels from guinea-pig cardiomyocytes.

Authors: G X Liu; C Derst; G Schlichthörl; S Heinen; G Seebohm; A Brüggemann; W Kummer; R W Veh; J Daut; R Preisig-Müller
Journal: J Physiol Date: 2001-04-01 Impact factor: 5.182

9. Ionic blockage of sodium channels in nerve.

Authors: A M Woodhull
Journal: J Gen Physiol Date: 1973-06 Impact factor: 4.086

10. Molecular basis of inward rectification: polyamine interaction sites located by combined channel and ligand mutagenesis.

Authors: Harley T Kurata; L Revell Phillips; Thierry Rose; Gildas Loussouarn; Stefan Herlitze; Hariolf Fritzenschaft; Decha Enkvetchakul; Colin G Nichols; Thomas Baukrowitz
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2. The bundle crossing region is responsible for the inwardly rectifying internal spermine block of the Kir2.1 channel.

Authors: Chiung-Wei Huang; Chung-Chin Kuo
Journal: Pflugers Arch Date: 2013-07-20 Impact factor: 3.657

Review 3. Mammalian polyamine metabolism and function.

Authors: Anthony E Pegg
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Journal: Nat Chem Date: 2013-06-30 Impact factor: 24.427

6. The anti-protozoal drug pentamidine blocks KIR2.x-mediated inward rectifier current by entering the cytoplasmic pore region of the channel.

Authors: T P de Boer; L Nalos; A Stary; B Kok; M J C Houtman; G Antoons; T A B van Veen; J D M Beekman; B L de Groot; T Opthof; M B Rook; M A Vos; M A G van der Heyden
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8. Inward-rectifying potassium (Kir) channels regulate pacemaker activity in spinal nociceptive circuits during early life.

Authors: Jie Li; Meredith L Blankenship; Mark L Baccei
Journal: J Neurosci Date: 2013-02-20 Impact factor: 6.167

9. Neonatal tissue injury reduces the intrinsic excitability of adult mouse superficial dorsal horn neurons.

Authors: J Li; M L Baccei
Journal: Neuroscience Date: 2013-11-01 Impact factor: 3.590

10. Revisiting inward rectification: K ions permeate through Kir2.1 channels during high-affinity block by spermidine.

Authors: Tai-An Liu; Hsueh-Kai Chang; Ru-Chi Shieh
Journal: J Gen Physiol Date: 2012-03 Impact factor: 4.086