2001 Fiscal Year Final Research Report Summary

Effect of disturbing endocrine drug, DEHP, on microcyst formation in the epithelial cells.

Research Project

Project/Area Number	11680571
Research Category	Grant-in-Aid for Scientific Research (C)
Allocation Type	Single-year Grants
Section	一般
Research Field	環境保全
Research Institution	Hamamatsu University School of Medicine
Principal Investigator	UEZATO Tadayoshi Hamamatsu Univ. School of Med., Associate professor, 医学部, 助教授 (40115465)
Co-Investigator(Kenkyū-buntansha)	WU Yi-xin Hamamatsu Univ. School of Med., Associate professor, 医学部, 助手 (60283363) SATO Eiji Hamamatsu Univ. School of Med., Assistant professor, 医学部, 助手 (70118751)
Project Period (FY)	1999 – 2001
Keywords	Endocrine disrupter / Lysosome / V-ATPase / DEHP / Peroxvsome
Research Abstract	Vacuolar H^+-ATPase(V-ATPase) is localized in organelles of the central vacuolar system such as lysosomes, coated vesicles, and the Golgi apparatus, and it plays an important role in maintaining the acidic enviroment in these compartments. We investigated the effects of di(2-ethylhexyl) phthalate (DEHP) on mouse liver lysosomes. After 2-3 weeks of oral administration in mice, a reduction in vacuolar H^+-ATPase, as determined by immunocytochemical analysis. When the mice were subsequently fed a normal diet for 1 week, V-ATPase, levels recovered to normal values. According to Northern blot analysis, V-ATPase subunit A mRNA decreased gradually with DEHP treatment. Enzyme cytochemical staining showed acid phosphatase to be present in lysosomes and late autophagosomes in normal animals as well as in DEHP-treated animals. But the number of late autophagosomes containing acid phosphatase increased clearly after DEHP treatment. These results suggest that, DEHP causes marked V-ATPase reduction in the liver lysosomal compartment and the effect to DEHP is reversible, and the effect of DEHP on protein expression is likely to be exerted at the transcriptional level. Thus in this study, we report that DEHP treatment causes a reduction in V-ATPase subunit A in the liver lysosomal compartment, which may accent for the inability to degrade excess cell organelles.

Research Products
(4 results)

All Other

All Publications (4 results)

[Publications] Wu Y.-X.: "Tyrosine phosphorylation and cellular redistribution of ezrin in MDCK cells treated with pervanadate"J. Cellular Biochemistry. 79. 311-321 (2000)
- Description
  「研究成果報告書概要(和文)」より
[Publications] Wan T.: "Inhibition effect of DEHP on mouse liver lysosomal vacuolar H^+-ATPase"J. Cellular Biochemistry. 81. 295-303 (2001)
- Description
  「研究成果報告書概要(和文)」より
[Publications] Wu Y.-X., Uezato T., Fujita M.: "Tyrosine phosphorylation and cellular redistribution of ezrin In MDCK cells treated with pervanadate"J. Cellular Biochemistry. 79. 311-321 (2000)
- Description
  「研究成果報告書概要(欧文)」より
[Publications] Wan T., Uezato T., Miura N.: "Inhibition effect of DEHP on mouse liver lysosomal Vacuolar H^+-ATPase"J. Cellular Biochemistry. 81. 295-303 (2001)
- Description
  「研究成果報告書概要(欧文)」より

2001 Fiscal Year Final Research Report Summary

Effect of disturbing endocrine drug, DEHP, on microcyst formation in the epithelial cells.

Principal Investigator

UEZATO Tadayoshi Hamamatsu Univ. School of Med., Associate professor, 医学部, 助教授 (40115465)

Research Products

[Publications] Wu Y.-X.: "Tyrosine phosphorylation and cellular redistribution of ezrin in MDCK cells treated with pervanadate"J. Cellular Biochemistry. 79. 311-321 (2000)

Description

[Publications] Wan T.: "Inhibition effect of DEHP on mouse liver lysosomal vacuolar H^+-ATPase"J. Cellular Biochemistry. 81. 295-303 (2001)

Description

[Publications] Wu Y.-X., Uezato T., Fujita M.: "Tyrosine phosphorylation and cellular redistribution of ezrin In MDCK cells treated with pervanadate"J. Cellular Biochemistry. 79. 311-321 (2000)

Description

[Publications] Wan T., Uezato T., Miura N.: "Inhibition effect of DEHP on mouse liver lysosomal Vacuolar H^+-ATPase"J. Cellular Biochemistry. 81. 295-303 (2001)

Description