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¡¶ÐÄÔàÔÓÖ¾¡·[ISSN:1009-7236/CN:61-1268/R]

ÆÚÊý:

2007ÄêµÚ1ÆÚ

Ò³Âë:

24-27

À¸Ä¿:

»ù´¡Ñо¿

³ö°æÈÕÆÚ:

2007-01-01

ÎÄÕÂÐÅÏ¢/Info

Title:

Electrophysiology of volume sensitive chloride channel in Clcn3-/- mouse cardiomyocytes

×÷Õß:

¹¨ÎÀÇÙ¹; ÀîÔ´¹; ÍõÏþÃ÷¹; ÕÅɺºì¹; ê°ÒæÃñ²

µÚËľüÒ½´óѧ£º1.Î÷¾©Ò½ÔºÀÏÄ겡¿Æ£¬2.»ù´¡²¿ÉúÀíѧ½ÌÑÐÊÒ£¬ÉÂÎ÷ Î÷°² 710032

Author(s):

GONG Weiª²qin¹;  LI Yuan¹;  WANG Xiaoª²ming¹;  ZHANG Shanª²hong¹;  ZANG Yiª²min²

1.Department of Geriatrics, Xijing Hospital, 2.Department of Physiology, Fourth Military Medical University, Xi¡äan 710032, Shaanxi, China

¹Ø¼ü´Ê:

ClCª²3; »ùÒòÇóý; Ðļ¡Ï¸°û; ÈÝ»ýÃô¸ÐÐÔÂȵçÁ÷

Keywords:

ClCª²3;  gene knockª²out;  cardiomyocytes;  volume sensitive chloride current

·ÖÀàºÅ:

R329.25

DOI:

-

ÎÄÏ×±êʶÂë:

A

ÕªÒª:

Ä¿µÄ Ñо¿ClCª²3»ùÒòÇóý£¨Clcn3-/-£©ÊóÐļ¡Ï¸°ûÈÝ»ýÃô¸ÐÐÔÂÈͨµÀµÄµçÉúÀíѧÌص㡣·½·¨ ÖƱ¸Clcn3-/-ÊóÄ£ÐÍ£¬²ÉÓÃĤƬǯȫϸ°û¼Ç¼¼¼Êõ¹Û²ìСÊóÐļ¡Ï¸°û±©Â¶ÓÚµÍÉøÈÜÒº¼¤»îµÄÈÝ»ýÃô¸ÐÐÔÂȵçÁ÷¼°Æäµ°°×¼¤Ã¸C£¨PKC£©Ãô¸ÐÐÔ¡£½á¹û Clcn3-/-ÊóÐļ¡Ï¸°ûÔÚµÈÉø״̬ϵı³¾°µçÁ÷ºÜС£¬µÍÉø´Ì¼¤ºóµÄ2.3¡À1.0 minĤµçµ¼¸Ä±ä²»Ã÷ÏÔ£¬ËæºóÔö´óµÄµçÁ÷³ÊÍâÏòÕûÁ÷ÐÔ¡¢µçѹºÍʱ¼äÒÀÀµÐÔ²¿·Öʧ»î£¬µçÁ÷-µçѹÇúÏßÉϵķ´×ªµçλ½Ó½üÂÈƽºâµçλµÄÀíÂÛÖµ£¬·´×ªµçλËæϸ°ûÍâÂÈŨ¶È(£ÛCl-£Ýo)½µµÍÏòÈ¥¼«»¯µçλ·½ÏòÆ«ÒÆ¡£ÂÈͨµÀ×è¶Ï¼ÁDIDSºÍNPPB¿ÉÄæÐÔÒÖÖƸÃͨµÀµÄÍâÏòÐÔĤµçµ¼£¬ÒÖÖÆÇ¿¶È·Ö±ðΪ88.8%¡À2.6%ºÍ76.3%¡À2.1%¡£PKC¼¤»î¼ÁPMAÃ÷ÏÔÔö´ó¸ÃµçÁ÷£¬+100 mVºÍ-100 mVÔöÇ¿·ù¶È·Ö±ðΪ110%¡À7%ºÍ110%¡À6%£¬¶øPKCÒÖÖƼÁchelerythrineÔ¤´¦ÀíÄÜÍêÈ«Ïû³ýPMAµÄµçÁ÷·Å´ó×÷Ó᣽áÂÛ Clcn3-/-ÊóÐļ¡Ï¸°û´æÔÚµäÐ͵ÄÈÝ»ýÃô¸ÐÐÔÂÈͨµÀ£¬PKC¼¤»î²ÎÓëÉϵ÷¸ÃͨµÀµÄ¹¦ÄÜÐÔ±í´ï¡£

Abstract:

AIM To study the electrophysiologic characteristics of volume sensitive chloride channel in Clcn3-/- mouse cardiomyocytes. METHODS Mice with homozygous disruption of Clcn3 gene (Clcn3-/-) were produced by techniques of gene targeting. The cardiomyocytes were isolated from adult Clcn3-/- mice and exposed to hypotonic solution. Whole cell patch clamp recording technique was used. RESULTS Small basal current was recorded under isotonic conditions. No significant alteration of the membrane conductance was observed during initial several minutes (2.3 ¡À1.0) min when the cells were exposed to hypotonic solution. The swelling-activated current exhibited moderate outward rectification and time-dependent inactivation at large positive potentials. The reversal potential of the current was close to the calculated equilibrium potential for £ÛCl-£Ýo. A rightward shift of the reversal potential was also observed upon reduction of £ÛCl-£Ýo. The chloride channel blockers DIDS and NPPB inhibited reversibly the outward conductance of the channel (by 88.8%¡À2.6% and 76.3%¡À2.1% suppression at +100 mV). PKC activator PMA significantly increased the swelling-activated current (by 110%¡À7% and 110%¡À6% amplitude respectively at +100 mV and -100 mV). Chelerythrine, a PKC inhibitor, eliminated completely the PMA effect on the chloride current. CONCLUSION The ClCª²3-deficient cardiomyocytes express the volume sensitive chloride channel. PKC activation upª²regulates the functional expression of the chloride channel.

²Î¿¼ÎÄÏ×/References

£Û1£ÝDuan D, Winter C, Cowley S, et al. Molecular identification of a volume-regulated chloride channel£ÛJ£Ý. Nature, 1997, 390(6658):417-421.

£Û2£ÝFriedrich T, Breiderhoff T, Jentsch TJ. Mutational analysis demonstrates that ClCª²4 and ClCª²5 directly mediate plasma membrane currents£ÛJ£Ý. J Biol Chem, 1999, 274(2):896-902.

£Û3£ÝWeylandt KH, Valverde MA, Nobles M, et al. Human ClCª²3 is not the swellingª²activated chloride channel involved in cell volume regulation£ÛJ£Ý. J Biol Chem, 2001, 276(20):17461-17467.

£Û4£ÝStobrawa SM, Breiderhoff T, Takamori S, et al. Disruption of ClCª²3, a chloride channel expressed on synaptic vesicles, leads to a loss of the hippocampus£ÛJ£Ý. Neuron, 2001, 29(1):185-196.

£Û5£ÝArreola J, Begenisich T, Nehrke K, et al. Secretion and cell volume regulation by salivary acinar cells from mice lacking expression of the Clcn3 Cl- channel gene£ÛJ£Ý. J Physiol, 2002, 545(pt 1):207-216.

£Û6£ÝWang GX, Hatton WJ, Wang GL, et al. Functional effects of novel anti-ClCª²3 antibodies on native volumeª²sensitive osmolyte and anion channels in cardiac and smooth muscle cells£ÛJ£Ý. Am J Physiol Heart Circ Physiol, 2003, 285(4):H1453-H1463.

£Û7£ÝYoshikawa M, Uchida S, Ezaki J, et al. ClCª²3 deficiency leads to phenotypes similar to human neuronal ceroid lipofuscinosis£ÛJ£Ý. Genes Cells, 2002, 7(6):597-605.

£Û8£ÝGong WQ, Xu HT,Shimizu T, et al. ClCª²3ª²independent, PKC-dependent activity of volumeª²sensitive Cl- channel in mouse ventricular cardiomyocytes£ÛJ£Ý. Cell Physiol Biochem, 2004, 14(4-6):213-224.

£Û9£ÝOkada Y, Oiki S, Hazama A, et al. Criteria for the molecular identification of the volumeª²sensitive outwardly rectifying Cl- channel£ÛJ£Ý. J Gen Physiol, 1998, 112(3):365-367.

£Û10£ÝHermoso M, Satterwhite CM, Andrade YN, et al. ClCª²3 is a fundamental molecular component of volumeª²sensitive outwardly rectifying Cl- channels and volume regulation in HeLa cells and Xenopus laevis oocytes£ÛJ£Ý. J Biol Chem, 2002, 277(42):40066-40074.

±¸×¢/Memo

±¸×¢/Memo:

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