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Neurological Surgery No Shinkei Geka Volume 50, Issue 1 （January 2022）

Neurological Surgery 脳神経外科 50巻1号（2022年1月発行）

Japanese English

特集 Precision Medicine—個別化医療を目指した遺伝子診断と新治療の知見

Ⅲ脳血管障害

脳動脈瘤—遺伝子解析と治療薬開発の現状 Current Knowledge on the Genetic Analysis and Development of Medical Therapy for Intracranial Aneurysms 青木友浩 ¹ , 栢原智道 ^1,2 , 小野功朗 ^1,3 , 岡田明大 ^1,3 Tomohiro AOKI ¹ , Tomomichi KAYAHARA ^1,2 , Isao ONO ^1,3 , Akihiro OKADA ^1,3 ¹国立循環器病研究センター研究所分子薬理部 ²埼玉医科大学国際医療センター脳卒中外科 ³京都大学大学院医学研究科脳神経外科学 ¹Department of Molecular Pharmacology, Research Institute, National Cerebral and Cardiovascular Center ²Department of Cerebrovascular Surgery, Saitama Medical University International Medical Center ³Department of Neurosurgery, Kyoto University Graduate School of Medicine キーワード：脳動脈瘤 , 家族性脳動脈瘤 , ゲノムワイド関連解析 , 体細胞変異 , スタチン製剤 , intracranial aneurysm , familial intracranial aneurysm , genome-wide association study , somatic mutation , statin Keyword: 脳動脈瘤 , 家族性脳動脈瘤 , ゲノムワイド関連解析 , 体細胞変異 , スタチン製剤 , intracranial aneurysm , familial intracranial aneurysm , genome-wide association study , somatic mutation , statin pp.179-195

発行日 2022年1月10日 Published Date 2022/1/10

DOI https://doi.org/10.11477/mf.1436204543

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Point

・一塩基多型の解析では，複数の多型で脳動脈瘤との関連が示されている．そのため，脳動脈瘤は多因子疾患であると考えられる．

・脳動脈瘤多発家系や遺伝病において，細胞外基質や内皮細胞に関連する遺伝子などが原因遺伝子として同定されている．

・スタチン製剤やアスピリンの服用による脳動脈瘤破裂に起因するくも膜下出血発症抑制効果が臨床研究により示されている．

　Genetic studies on intracranial aneurysms（IAs）, like genome-wide association studies, or studies analyzing familial intracranial aneurysms, have successfully revealed the potential contribution of a set of genes to the pathology of IAs. Some of the genes may promote the formation of IAs or the process leading to rupture of the lesions through exacerbating inflammatory responses or facilitating the degenerative changes of arterial walls. Many genes or single-nucleotide polymorphisms have been identified through extensive analyses, but they can only explain one-fifth of the IA pathology; therefore, the pathogenesis of IAs is influenced by many factors, including environmental factors, and not only genetic ones. Intriguingly, a somatic mutation in the PDGFRB gene has recently been identified in more than half of the cases with fusiform aneurysms, making the development of medical therapy targeting PDGFRβ signaling realistic. Nowadays, following a series of recent experimental studies, IA is considered a chronic inflammatory disease affecting intracranial arteries, indicating the potential of anti-inflammatory drugs as therapeutic drugs for the treatment of IAs. No wonder, recently published observational studies have revealed the preventive effect of statins and aspirin, with potent anti-inflammatory effects on the rupture of IAs.