過飽和の解消による蛋白質の異常凝集体の形成に関する研究

2014 Fiscal Year Annual Research Report

• Project/Area Number: 14J04433
• Research Institution: Osaka University
• Principal Investigator: 林 雨曦 大阪大学, 理学研究科, 特別研究員(DC1)
• Project Period (FY): 2014-04-25 – 2017-03-31
• Keywords: protein aggregation / supersaturation / solubility / phase diagram

Outline of Annual Research Achievements

Aberrant Protein aggregation is essential for more than 30 serious diseases, such as Alzheimer's disease and type Ⅱ diabetes. A better understanding of the mechanism leading to protein aggregation is very important for the treatment and prevention of these diseases. In my previous study, I constructed phase diagrams of lysozyme to explain the role of solubility and supersaturation in alcohol-induced lysozyme aggregation. Cytochrome c aggregation was investigated in the same system this year for deepening the understanding of protein aggregation.
Apocytochrome c and Ag-apocytchrome c were prepared from holocytochrome c using silver sulfate method. Then, the aggregation behavior of three types of cytochrome c were examined in water/alcohol mixtures. Based on the results, phase diagrams of three types of cytochrome c were contrasted. By comparing the phase diagrams, we found that cytochrome c might be inherently low amyloidogenic, and removing heme group decreased cytochrome c solubility, widening the amoprphous region. My results further suggested that protein aggregation was not correlated with protein secondary structure content.

Current Status of Research Progress

2: Research has progressed on the whole more than it was originally planned.

Reason

The aggregation behavior of three types of cytochrome c was examined as the plan, and phase diagrams of them were successfully constructed at the same time. Paper of this study is in preparation now.

Strategy for Future Research Activity

I examined the aggregation behavior of two model globular proteins, lysozyme and cyotchrome c, in water/alcohol mixtures, and constructed their phase diagrams depending on the results. I will study the aggregation of intrinsically disordered proteins in the next. Amyloid β(1-40) and α-synuclein will be employed because of their close association with Alzheimer's disease and Parkinson's disease.

Research Products

• [Journal Article] Supersaturation-limited Amyloid Fibrillation of Insulin Revealed by Ultrasonication (2014)
  • Author(s): Hiroya Muta, Young-Ho Lee, Jozsef Kardos, Yuxi Lin, Hisashi Yagi, Yuji Goto
  • Journal Title: The Journal of Biological Chemistry Volume: 289 Pages: 18228-18238
  • DOI: 10.1074/jbc.M114.566950.
  • Peer Reviewed
• [Presentation] Context-dependent Amyloid Fibrillation of Amyloid beta 1-40 (2015)
  • Author(s): Yuxi Lin
  • Organizer: The POSTECH EPB-Department of Chemistry & Osaka University Institute for Protein Research Symposium
  • Place of Presentation: 大阪
  • Year and Date: 2015-01-11 – 2015-01-11
• [Presentation] Distinct mechanisms of amyloid fibrillation of amyloid beta 1-40 in alcohol/water mixtures (2014)
  • Author(s): Yuxi Lin, Young-Ho Lee, Mayu S. Terakawa, Tatsuya Ikenoue, Yuji Goto
  • Organizer: Institute of Protein Research retreat
  • Place of Presentation: 淡路島
  • Year and Date: 2014-12-01 – 2014-12-02
• [Presentation] Solubility and Supersaturation-dependent Protein Misfolding Revealed by Ultrasonication (2014)
  • Author(s): Yuxi Lin, Young-Ho Lee, Yuichi Yoshimura, Hisashi Yagi, Yuji Goto
  • Organizer: The 4th Asia Pacific Protein Association Conference
  • Place of Presentation: Jeju island, Korea
  • Year and Date: 2014-05-17 – 2014-05-20