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A new horizon of moyamoya disease and associated health risks explored through RNF213
Authors:Akio Koizumi  Hatasu Kobayashi  Toshiaki Hitomi  Kouji H. Harada  Toshiyuki Habu  Shohab Youssefian
Affiliation:1.Department of Health and Environmental Sciences, Graduate School of Medicine,Kyoto University,Kyoto,Japan;2.Department of Preventive Medicine,St. Marianna University School of Medicine,Kawasaki,Japan;3.Laboratory of Nutritional Sciences, Department of Food Science and Nutrition,Mukogawa Women’s University,Nishinomiya,Japan;4.Laboratory of Molecular Biosciences, Graduate School of Medicine,Kyoto University,Kyoto,Japan
Abstract:The cerebrovascular disorder moyamoya disease (MMD) was first described in 1957 in Japan, and is typically considered to be an Asian-specific disease. However, it is globally recognized as one of the major causes of childhood stroke. Although several monogenic diseases are known to be complicated by Moyamoya angiopathy, the ring finger protein 213 gene (RNF213) was identified as a susceptibility gene for MMD. RNF213 is unusual, because (1) it induces MMD with no other recognizable phenotypes, (2) the RNF213 p.R4810K variant is an Asian founder mutation common to Japanese, Korean and Chinese with carrier rates of 0.5–2 % of the general population but a low penetrance, and (3) it encodes a relatively largest proteins with a dual AAA+ ATPase and E3 Ligase activities. In this review, we focus on the genetics and genetic epidemiology of RNF213, the pathology of RNF213 R4810K, and the molecular functions of RNF213, and also address the public health contributions to current unresolved issues of MMD. We also emphasize the importance of a more updated definition for MMD, of qualified cohort studies based on genetic epidemiology and an awareness of the ethical issues associated with genetic testing of carriers.
Keywords:Moyamoya disease   RNF213 R4810K   Asian founder mutation   Angiogenesis   Hypoxia
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