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Differential Expression of Four $Ca_v$3.1 Splice Variants in the Repeat III-IV Loop
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  • Differential Expression of Four $Ca_v$3.1 Splice Variants in the Repeat III-IV Loop
  • Differential Expression of Four $Ca_v$3.1 Splice Variants in the Repeat III-IV Loop
저자명
Lee. Sang-Soo,Park. You-Mi,Kang. Ho-Won,Bang. Hyo-Weon,Jeong. Seong-Woo,Lee. Jung-Ha
간행물명
Animal cells and systems
권/호정보
2008년|12권 3호|pp.137-141 (5 pages)
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한국통합생물학회
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정기간행물|ENG|
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이 논문은 한국과학기술정보연구원과 논문 연계를 통해 무료로 제공되는 원문입니다.
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기타언어초록

Molecular cloning revealed the three isoforms($Ca_v3.1,;Ca_v3.2,;and;Ca_v3.3$) of the T-type calcium channel subfamily. Expression studies exhibited their distinctive electrophysiological and pharmacological properties, accounting for diverse properties of T-type calcium channel currents previously characterized from isolated cells. However, electrophysiological properties of ion channels have shown to be more diversified by their splice variants. We here searched splice variants of rat $Ca_v3.1$ T-type channel by reverse-transcription-polymerase chain reaction(RT-PCR) to further explore diversity of $Ca_v3.1$. Interestingly, analyses of cloned RT-PCR products displayed that there were at least four splicing variants of rat $Ca_v3.1$ in the loop connecting repeats III and IV. Southern blot analyses indicated that the predominantly detected variant in brain was $Ca_v3.1a$(492 bp), which were rarely detected in most of peripheral tissues. Other two variants($Ca_v3.1c$, 546 bp; $Ca_v3.1d$, 525 bp) were detected in most of the tissues examined. The smallest isoform($Ca_v3.1b$, 471 bp) was rarely detected all the tissues. Electrophysiological characterization of the splicing variants indicated that the splice variants differ in inactivation kinetics and the voltage dependence of activation and inactivation as well.