스테로이드 합성을 교란하는 내분비계장애물질 검색을 위한 라이디히 세포 분리 및 배양조건 확립

Establishment of Purification and Incubation Conditions of Leydig Cells for Screen Endocrine Disruptors Altering Steroidogenesis

  • 강일현 (식약청 국립독성연구원 독성연구부 내분비장애물질팀) ;
  • 강태석 (식약청 국립독성연구원 독성연구부 내분비장애물질팀) ;
  • 강호일 (식약청 국립독성연구원 독성연구부 내분비장애물질팀) ;
  • 문현주 (식약청 국립독성연구원 독성연구부 내분비장애물질팀) ;
  • 김태성 (식약청 국립독성연구원 독성연구부 내분비장애물질팀) ;
  • 기호연 (식약청 국립독성연구원 독성연구부 내분비장애물질팀) ;
  • 류혜원 (식약청 국립독성연구원 독성연구부 내분비장애물질팀) ;
  • 신재호 (식약청 국립독성연구원 독성연구부 내분비장애물질팀) ;
  • 동미숙 (고려대학교 생명공학부) ;
  • 한순영 (식약청 국립독성연구원 독성연구부 내분비장애물질팀) ;
  • 김승희 (식약청 국립독성연구원 독성연구부 내분비장애물질팀) ;
  • 홍진환 (식약청 국립독성연구원 독성연구부 내분비장애물질팀)
  • Kang Il-Hyun (Endocrine Toxicology Team, Department of Toxicological Research, NITR, KFDA) ;
  • Kang Tae-Seok (Endocrine Toxicology Team, Department of Toxicological Research, NITR, KFDA) ;
  • Kang Ho-Il (Endocrine Toxicology Team, Department of Toxicological Research, NITR, KFDA) ;
  • Moon Hyun-Ju (Endocrine Toxicology Team, Department of Toxicological Research, NITR, KFDA) ;
  • Kim Tae-Sung (Endocrine Toxicology Team, Department of Toxicological Research, NITR, KFDA) ;
  • Ki Ho-Hyun (Endocrine Toxicology Team, Department of Toxicological Research, NITR, KFDA) ;
  • Ryu Hye-Won (Endocrine Toxicology Team, Department of Toxicological Research, NITR, KFDA) ;
  • Sin Jae-Ho (Endocrine Toxicology Team, Department of Toxicological Research, NITR, KFDA) ;
  • Dong Mi-Sook (School of Life Sciences and Biotechnology, Korea University) ;
  • Han Soon-Young (Endocrine Toxicology Team, Department of Toxicological Research, NITR, KFDA) ;
  • Kim Seung-Hee (Endocrine Toxicology Team, Department of Toxicological Research, NITR, KFDA) ;
  • Hong Jin-Hwan (Endocrine Toxicology Team, Department of Toxicological Research, NITR, KFDA)
  • 발행 : 2006.06.01

초록

Normally, environmental toxicants are classified as endocrine disruptors if they interfere with regulation of cellular function by endogeneous steroids through inhibition of receptor binding and/or transcriptional activation. So, many studies have been performed about agonist/antagonist of hormone receptor to study mechanisms of endocrine disruptors. If toxicants affect steroid biosynthesis and/or degradation and alter hormone homeostasis, these also are classified as endocrine disruptors. But there are not many studies of the mechanisms of endocrine disruptors on the basis of alteration of steroid biosynthesis and/or degradation. Isolation and culture of Leydig cells from testis is one of methods for the steroidogenesis screening assays to evaluate a substance for altering steroidogenesis. Leydig cells were harvested using the method described by Klinefelter with modifications. Leydig cells were purified by perfusion of testis and incubation ($34^{\circ}C$, 80cycles/minute, 20 minutes) with collagenase (0.25 mg/kg), centrifugal elutriation, percoll gradient centrifugation and BSA multidensity gradient centrifugation. To confirm if this method is one of appropriate tools to evaluate a substance for altering steroidogenesis, ketoconazole, positive control was administered to purified Leydig cells. Ketoconazole ($10^{-8}M$ and above) significantly reduced testosterone production in purified Leydig cells. From above results, we suggest that this method for steroidogenesis screening assay appears to be a appropriate tool to detect suspected compounds for altering steroidogenesis.

키워드

참고문헌

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