2001 Fiscal Year Final Research Report Summary

Molecular mechanism ofapoptosis in target organs of sex steroid hormones

Research Project

Project/Area Number	12670220
Research Category	Grant-in-Aid for Scientific Research (C)
Allocation Type	Single-year Grants
Section	一般
Research Field	Experimental pathology
Research Institution	HYOGO COLLEGE OF MEDICINE
Principal Investigator	TERADA Nobuyuki Hyogo College of Medicine, Professor, 医学部, 教授 (50150339)
Co-Investigator(Kenkyū-buntansha)	YAMADA Naoko Hyogo College of Medicine, Research Associate, 医学部, 助手 (10319858) TSUJIMURA Tohru Hyogo College of Medicine, Associate Professor, 医学部, 助教授 (20227408)
Project Period (FY)	2000 – 2001
Keywords	apoptosis / androgen / estrogen / Fas / Fas ligand / VDAC / mouse / cytochrome C
Research Abstract	1.We examined the effect of castration on apoptosis in the epithelia of the mouse seminal vesicle and epididymis, and found the followings. (1) Castration induces apoptosis in the epithelia of these organs from birth to adulthood. (2) The extent of apoptosis is lower at the slowly growing stage of these organs than at their rapidly growing stage thereafter. 2.By the experiments with mutant mice deficient in Fas or Fas ligand, we have shown that the Fas- Fas ligand system plays little role in castration-induced apoptosis in the mouse seminal vesicle, epididymis, prostate and coagulating gland. 3.We have shown that apoptosis in the mouse uterine epithelium after estrogen deprivation correlates to release of cytochrome C in mitochondria into cytoplasm, activation of caspase-3, the ratio of Bak or Bax/Bcl-2 or Bcl-xL and the amount of voltage dependent anion channel (VDAC) in the mitochondria. These results suggest the followings. (1) Mitochondria play an important role in estrogen deprivation-induced apoptosis in the uterine epithelium. (2) This apoptotic process is regulated by proteins of the Bcl-2 family. (3) The increase in VDAC enhances the sensitivity of cells to apoptosis since VDAC is thought to be a channel, through which cytochrome C moves from mitochondria to cytoplasm.

Research Products
(4 results)

All Other

All Publications (4 results)

[Publications] Sugihara A., Terada N., et al.: "Castration induces apoptosis in the male accessory sex organs of Fas-deficient Ipr and Fas ligand-deficient gid mutant mice"In Vivo. 15・5. 385-390 (2001)
- Description
  「研究成果報告書概要(和文)」より
[Publications] Takagi-Morishita Y., Terada N., et al.: "Castration induces apoptosis in the mouse epididymis during postnatal development"Endocrine Journal. 49・1. 75-84 (2002)
- Description
  「研究成果報告書概要(和文)」より
[Publications] SugiharaA.,: "Castration induces apoptosis in the male accessory sex organs of Fas-deficient Ipr and Fas ligand-deficient gld mutant mice"InVivo. 15-5. 385-390 (2001)
- Description
  「研究成果報告書概要(欧文)」より
[Publications] Takagi-Morishita Y,: "Castration induces apoptosis in the mouse epididymis during postnatal development"Endocrine Journal. 49-1. 75-84 (2002)
- Description
  「研究成果報告書概要(欧文)」より

2001 Fiscal Year Final Research Report Summary

Molecular mechanism ofapoptosis in target organs of sex steroid hormones

Principal Investigator

TERADA Nobuyuki Hyogo College of Medicine, Professor, 医学部, 教授 (50150339)

Research Products

[Publications] Sugihara A., Terada N., et al.: "Castration induces apoptosis in the male accessory sex organs of Fas-deficient Ipr and Fas ligand-deficient gid mutant mice"In Vivo. 15・5. 385-390 (2001)

Description

[Publications] Takagi-Morishita Y., Terada N., et al.: "Castration induces apoptosis in the mouse epididymis during postnatal development"Endocrine Journal. 49・1. 75-84 (2002)

Description

[Publications] SugiharaA.,: "Castration induces apoptosis in the male accessory sex organs of Fas-deficient Ipr and Fas ligand-deficient gld mutant mice"InVivo. 15-5. 385-390 (2001)

Description

[Publications] Takagi-Morishita Y,: "Castration induces apoptosis in the mouse epididymis during postnatal development"Endocrine Journal. 49-1. 75-84 (2002)

Description