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Higher Expression of TRPM7 Channels in Murine Mature B Lymphocytes than Immature Cells
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  • Higher Expression of TRPM7 Channels in Murine Mature B Lymphocytes than Immature Cells
저자명
JinKyoungKim,JaeHongKo,JooHyunNam,Ji-EunWoo,KyeongMinMin,YungEEarm,SungJoonKim
간행물명
The Korean Journal of Physiology & PharmacologyKCI
권/호정보
2005년|9권 2호(통권50호)|pp.69-76 (8 pages)
발행정보
대한생리학회-대한약리학회|한국
파일정보
정기간행물|ENG|
PDF텍스트(0.31MB)
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영문초록

TRPM7, a cation channel protein permeable to various metal ions such as Mg2⁢, is ubiquitously expressed in variety of cells including lymphocytes. The activity of TRPM7 is tightly regulated by intracellular Mg2⁢, thus named Mg2⁢-inhibited cation (MIC) current, and its expression is known to be critical for the viability and proliferation of B lymphocytes. In this study, the level of MIC current was compared between immature (WEHI-231) and mature (Bal-17) B lymphocytes. In both cell types, an intracellular dialysis with Mg2⁢-free solution (140 mM CsCl) induced an outwardly-rectifying MIC current. The peak amplitude of MIC current and the permeability to divalent cation (Mn2⁢) were several fold higher in Bal-17 than WEHI-231. Also, the level of mRNAs for TRPM7, a molecular correspondence of the MIC channel, was significantly higher in Bal-17 cells. The amplitude of MIC was further increased, and the relation between current and voltage became linear under divalent cation-free conditions, demonstrating typical properties of the TRPM7. The stimulation of B cell receptors (BCR) by ligation with antibodies did not change the amplitude of MIC current. Also, increase of extracellular [Mg2⁢]c to enhance the Mg2⁢ influx did not affect the BCR ligation-induced death of WEHI-231 cells. Although the level of TRPM7 was not directly related with the cell death of immature B cells, the remarkable difference of TRPM7 might indicate a fundamental change in the permeability to divalent cations during the development of B cells.

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