Epigenetic regulation of autism-susceptibility gene, NLGN4X.

• Project/Area Number: 26460483
• Research Category: Grant-in-Aid for Scientific Research (C)
• Allocation Type: Multi-year Fund
• Section: 一般
• Research Field: Experimental pathology
• Research Institution: Institute for Developmental Research, Aichi Human Service Center
• Principal Investigator: Iio Akio 愛知県心身障害者コロニー発達障害研究所, 発生障害学部, リサーチレジデント (80344349)
• Co-Investigator(Renkei-kenkyūsha): NAKAYAMA Atsuo 愛知県心身障害者コロニー発達障害研究所, 発生障害学部, 部長 (50227964)
• Project Period (FY): 2014-04-01 – 2017-03-31
• Project Status: Completed (Fiscal Year 2016)
• Budget Amount: ¥4,940,000 (Direct Cost: ¥3,800,000、Indirect Cost: ¥1,140,000); Fiscal Year 2016: ¥910,000 (Direct Cost: ¥700,000、Indirect Cost: ¥210,000); Fiscal Year 2015: ¥1,430,000 (Direct Cost: ¥1,100,000、Indirect Cost: ¥330,000); Fiscal Year 2014: ¥2,600,000 (Direct Cost: ¥2,000,000、Indirect Cost: ¥600,000)
• Keywords: NLGN4X / CpG methylation / MeCP2 / miR-23a / exosome / lncRNA / epigenetic / iPSC / 自閉症 / メチル化 / microRNA / AVP / TOP1 / エピジェネティックス / CpGメチル化 / mTOR / Topoisomerase I

Outline of Final Research Achievements

Some types of genetic mutation in NLGN4X, including point mutations and copy number variants, are considered responsible for rare autism spectrum disorders. However, it is unclear about the transcriptional and post-transcriptional regulation of NLGN4X expression. Thus, we focus on elucidating how the NLGN4X expression is epigenetically regulated in the neural cell. Firstly, we showed that NLGN4X promoters were silenced by CpG methylation in association with MeCP2. Next, we clarified that NLGN4X was down-regulated by exosomal miR-23a, which secreted by heat-stressed microglia. Finally, we identified a novel natural antisense transcript (AS-NLGN4X), which was partially complementary to NLGN4X exon 1s. Its expression pattern was similar with NLGN4X. Interestingly, forced expression of AS-NLGN4X down-regulated NLGN4X expression, and AS-NLGN4X knockdown up-regulated it. These results suggest that NLGN4X is transcriptionally and/or post-transcriptionally under control by non-coding RNAs.

Research Products

• [Journal Article] 統合失調症と発達障害の関連 (2016)
  • Author(s): 椎野智子、 宍戸恵美子、 飯尾明生、 尾崎紀夫
  • Journal Title: 臨床精神医学 Volume: 45 Pages: 1169-1175
• [Presentation] 神経極性を制御するLKB1-Stk25シグナルが自閉症発症機構に果たす役割の解明 (2016)
  • Author(s): 松木亨、飯尾明生、中山敦雄
  • Organizer: 第119回日本小児科学学会学術集会
  • Place of Presentation: 札幌
• [Presentation] 神経極性制御に関わるStk25-LKB1シグナルが神経系の発達と機能に果す役割 (2016)
  • Author(s): 松木亨、飯尾明生、中山敦雄
  • Organizer: 日本組織培養学会第89回大会
  • Place of Presentation: 豊中
• [Presentation] Multiple regulatory mechanisms of autism susceptibility gene, NLGN4X, expression by non-coding RNAs. (2015)
  • Author(s): A. Iio, T. Matsuki, E. Aoki, A. Nakayama.
  • Organizer: 第38回日本分子生物学会年会
  • Place of Presentation: 兵庫県神戸市
  • Year and Date: 2015-12-03
• [Presentation] ニューロリギン4Xのエピジェネティックスによる発現制御機構の解析 (2015)
  • Author(s): 飯尾明生
  • Organizer: 第二回 霊長類への展開に向けた幹細胞・発生・エピゲノム研究
  • Place of Presentation: 愛知県犬山市
  • Year and Date: 2015-09-02
  • Invited
• [Presentation] 自閉症感受性遺伝子NLGN4Xの発現解析とその制御機構 (2015)
  • Author(s): 中山敦雄、深田斉秀、飯尾明生、青木英子、正木茂夫
  • Organizer: 第104回日本病理学会総会
  • Place of Presentation: 愛知県名古屋市
  • Year and Date: 2015-05-02
• [Presentation] The expression of autism-susceptibility gene NLGN4X is regulated by miR-23a. (2014)
  • Author(s): A. Iio, T. Matsuki, E. Aoki, A. Nakayama.
  • Organizer: 第37回日本分子生物学会年会
  • Place of Presentation: 神奈川県横浜市
  • Year and Date: 2014-11-27
• [Remarks] 発生障害学部トップページ
  • URL: http://www.inst-hsc.jp/d-embryology/index.html
• [Remarks] 愛知県心身障害者コロニー発達障害研究所発生障害学部トップページ
  • URL: http://www.inst-hsc.jp/d-embryology/index.html
• [Remarks] 発達障害研究所発生障害学部
  • URL: http://www.inst-hsc.jp/d-embryology/index.html