대한한의학회지 (The Journal of Korean Medicine)

  • 제29권2호
  • /
  • Pages.151-164
  • /
  • 2008
  • /
  • 1010-0695(pISSN)
  • /
  • 2288-3339(eISSN)
대한한의학회 (The Society of Korean Medicine)
권호 표지

($A{\beta}-oligomer$로 유도된 Neuro2A 세포주에서 용담사간탕(龍膽瀉肝湯)의 치매 억제 효과

A Study on the Inhibitory Effect of Yeongdamsagantang on Alzheimer in $A{\beta}-oligomer-induced$ Neuro 2A Cell Lines

  • 김해수 (대구한의대 심계내과학교실) ;
  • 신유정 (대구한의대 심계내과학교실) ;
  • 박종혁 (대구한의대 심계내과학교실) ;
  • 김승모 (대구한의대 내과학교실) ;
  • 백경민 (대구한의대 심계내과학교실) ;
  • 박치상 (대구한의대 심계내과학교실)
  • Kim, Hae-Su (Dept. of Cardiovascular and Neurologic Disease, College of Oriental Medicine, Daegu-Haany University) ;
  • Shin, Yoo-Jeong (Dept. of Cardiovascular and Neurologic Disease, College of Oriental Medicine, Daegu-Haany University) ;
  • Park, Jong-Hyuk (Dept. of Cardiovascular and Neurologic Disease, College of Oriental Medicine, Daegu-Haany University) ;
  • Kim, Seung-Mo (Dept. of Internal Medicine, College of Oriental Medicine, Daegu-Haany University) ;
  • Paek, Kyung-Min (Dept. of Cardiovascular and Neurologic Disease, College of Oriental Medicine, Daegu-Haany University) ;
  • Park, Chi-Sang (Dept. of Cardiovascular and Neurologic Disease, College of Oriental Medicine, Daegu-Haany University)
  • 발행 : 2008.06.30
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초록

Objective: To investigate the effects of Yeongdamsagantang (YDGT) on apoptosis of neuronal cells that can result in dementia. Method: The water extract of the YDGT was tested in vitro for its beneficial effects on neuronal survival and neuroprotective functions, particularly in connection with $A{\beta}$ oligomer-related dementias. $A{\beta}$ oligomers derived from proteolytic processing of the ${\beta}-amyloid$ precursor protein (APP), including the $amyloid-{\beta}$ peptide $(A{\beta})$, play a critical role in the pathogenesis of Alzheimer's disease. A neuroblastoma cell line stably expressing an $A{\beta}$ oligomerassociated neuronal degeneration was used to investigate if YDGT inhibits formation of $A{\beta}$ oligomer. To measure the ATP generating level in mitochondrial membrane, luciferin/luciferase luminescence kit (Promega) and luminator was used, and to survey the protein's apparition, confocal microscopy was used. Result: $A{\beta}oligomer$ had a profound attenuation in the increase in CT105 expressing neuro2A cells from YDGT. Experimental evidence indicates that YDGT protected against neuronal damage from cells, but its cellular and molecular mechanisms remain unknown. We demonstrated that YDGT inhibited formation of $amyloid-{\beta}$ $(A{\beta})$ oligomers, which were the behavior, and possibly causative, features of AD. The decreased $A{\beta}$ oligomer in the presence of YDGT was observed in the conditioned medium of this $A{\beta}oligomer-secreting$ cell line under in vitro. In the cells, YDGT significantly attenuated mitochondrion-initiated apoptosis. Conclusion: (i) a direct $A{\beta}$ oligomer toxicity and the apoptosis initiated by the mitochondria; and (ii) multiple cellular and molecular neuroprotective mechanisms, including attenuation of apoptosis and direct inhibition of $A{\beta}$ oligomer aggregation, underlie the neuroprotective effects of YDGT.

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