研究者業績

嶋田 誠

Shimada Makoto

基本情報

所属
藤田医科大学 医科学研究センター 講師
中京学院大学 看護学部 非常勤講師
学位
博士(理学)(京都大学)

研究者番号
00528044
ORCID ID
 https://orcid.org/0000-0003-0067-0082
J-GLOBAL ID
200901081274695690
Researcher ID
K-4613-2015
researchmap会員ID
6000009803

外部リンク

Bioinformaticsのアプローチを中心にスプライシングについて研究しています。
以前は、野生の霊長類の集団遺伝研究のため、のべ1年くらいアフリカでフィールド・ワークをしたこともあります。
その後、進化遺伝学、ゲノム進化、生物情報(転写物や多型データベースの研究)と幅を広げてきました。

受賞

 1

論文

 31
  • Shimada, Makoto K.
    International Journal of Molecular Sciences 24(11) 9622 2023年6月1日  査読有り筆頭著者最終著者責任著者
  • Makoto K. Shimada, Tsunetoshi Nishida
    MOLECULAR PHYLOGENETICS AND EVOLUTION 109 409-414 2017年4月  査読有り筆頭著者責任著者
    Felsenstein's PHYLIP package of molecular phylogeny tools has been used globally since 1980. The programs are receiving renewed attention because of their character-based user interface, which has the advantage of being scriptable for use with large-scale data studies based on super-computers or massively parallel computing clusters. However, occasionally we found, the PHYLIP Consense program output text file displays two or more divided bootstrap values for the same cluster in its result table, and when this happens the output Newick tree file incorrectly assigns only the last value to that cluster that disturbs correct estimation of a consensus tree. We ascertained the cause of this aberrant behavior in the bootstrapping calculation. Our rewrite of the Consense program source code outputs bootstrap values, without redundancy, in its result table, and a Newick tree file with appropriate, corresponding bootstrap values. Furthermore, we developed an add-on program and shell script, add_bootstrap.pl and fasta2tre_bs.bsh, to generate a Newick tree containing the topology and branch lengths inferred from the original data along with valid bootstrap values, and to actualize the automated inference of a phylogenetic tree containing the originally inferred topology and branch lengths with bootstrap values, from multiple unaligned sequences, respectively. These programs can be downloaded at: https://github.com/ShimadaMK/PHYLIP_enhance/. (C) 2017 Elsevier Inc. All rights reserved.
  • Makoto K. Shimada, Ryoko Sanbonmatsu, Yumi Yamaguchi-Kabata, Chisato Yamasaki, Yoshiyuki Suzuki, Ranajit Chakraborty, Takashi Gojobori, Tadashi Imanishi
    MOLECULAR GENETICS AND GENOMICS 291(5) 1851-1869 2016年10月  査読有り筆頭著者責任著者
    Short Tandem Repeats (STRs) comprise repeats of one to several base pairs. Because of the high mutability due to strand slippage during DNA synthesis, rapid evolutionary change in the number of repeating units directly shapes the range of repeat-number variation according to selection pressure. However, the remaining questions include: Why are STRs causing repeat expansion diseases maintained in the human population; and why are these limited to neurodegenerative diseases? By evaluating the genome-wide selection pressure on STRs using the database we constructed, we identified two different patterns of relationship in repeat-number polymorphisms between DNA and amino-acid sequences, although both patterns are evolutionary consequences of avoiding the formation of harmful long STRs. First, a mixture of degenerate codons is represented in poly-proline (poly-P) repeats. Second, long poly-glutamine (poly-Q) repeats are favored at the protein level; however, at the DNA level, STRs encoding long poly-Qs are frequently divided by synonymous SNPs. Furthermore, significant enrichments of apoptosis and neurodevelopment were biological processes found specifically in genes encoding poly-Qs with repeat polymorphism. This suggests the existence of a specific molecular function for polymorphic and/or long poly-Q stretches. Given that the poly-Qs causing expansion diseases were longer than other poly-Qs, even in healthy subjects, our results indicate that the evolutionary benefits of long and/or polymorphic poly-Q stretches outweigh the risks of long CAG repeats predisposing to pathological hyper-expansions. Molecular pathways in neurodevelopment requiring long and polymorphic poly-Q stretches may provide a clue to understanding why poly-Q expansion diseases are limited to neurodegenerative diseases.
  • Makoto K. Shimada, Noriko Sasaki-Haraguchi, Akila Mayeda
    INTERNATIONAL JOURNAL OF MOLECULAR SCIENCES 16(5) 10376-10388 2015年5月  査読有り筆頭著者
    According to the length distribution of human introns, there is a large population of short introns with a threshold of 65 nucleotides (nt) and a peak at 85 nt. Using human genome and transcriptome databases, we investigated the introns shorter than 66 nt, termed ultra-short introns, the identities of which are scarcely known. Here, we provide for the first time a list of bona fide human ultra-short introns, which have never been characterized elsewhere. By conducting BLAST searches of the databases, we screened 22 introns (37-65 nt) with conserved lengths and sequences among closely related species. We then provide experimental and bioinformatic evidence for the splicing of 15 introns, of which 12 introns were remarkably G-rich and 9 introns contained completely inefficient splice sites and/or branch sites. These unorthodox characteristics of ultra-short introns suggest that there are unknown splicing mechanisms that differ from the well-established mechanism.
  • 嶋田誠
    Research Bulletin, Saito Ho-on Kai Museum 78 77-85 2014年3月  招待有り筆頭著者責任著者

MISC

 27
  • 嶋田 誠
    霊長類研究 40(1) 2024年6月20日  招待有り筆頭著者責任著者
  • 嶋田 誠
    岩波『科学』 91(2) 178-181 2021年2月  招待有り筆頭著者責任著者
  • 杉山 幸丸, 松林 清明, 庄武 孝義, 川本 芳, 嶋田 誠
    霊長類研究 36(2) 67-72 2020年12月20日  
  • Makoto K. Shimada, Tsunetoshi Nishida
    bioRxiv 2020年3月29日  
    <title>Abstract</title>The application of current genome-wide sequencing techniques on human populations helps elucidate the considerable gene flow among genus<italic>Homo</italic>, which includes modern and archaic humans. Gene flow among current human populations has been studied using frequencies of single nucleotide polymorphisms. Unlike single nucleotide polymorphism frequency data, haplotype data are suitable for identifying and tracing rare evolutionary events. Haplotype data can also conveniently detect genomic location and estimate molecular function that may be a target of selection. We analyzed eight loci of the human genome using the same procedure for each locus to infer human haplotype diversity and reevaluate past explanations of the evolutionary mechanisms that affected these loci. These loci have been recognized by separate studies because of their unusual gene genealogy and geographic distributions that are inconsistent with the recent out-of-Africa model. For each locus, we constructed genealogies for haplotypes using sequence data of the 1000 Genomes Project. Then, we performed S* analysis to estimate distinct gene flow events other than out-of-Africa events. Furthermore, we also estimated unevenness of selective pressure between haplotypes by Extended Haplotype Homozygosity analysis. Based on the patterns of results obtained by this combination of analyses, we classified the examined loci without using a specific population model. This simple method helped clarify evolutionary events for each locus, including rare evolutionary events such as introgression, incomplete lineage sorting, selection, and haplotype recombination that may be hard to discriminate from each other.
  • Makoto K. Shimada
    GENES & GENETIC SYSTEMS 91(6) 343-343 2016年12月  

書籍等出版物

 2
  • (担当:分担執筆, 範囲:2章 霊長類の分類・系統・進化, グエノン類(オナガザル科), ヒヒ類(オナガザル科))
    丸善出版 2023年7月 (ISBN: 9784621308042)
    日本霊長類学会が総力をあげて編集した、霊長類を総合理解するために編まれた事典。霊長類学の歴史をたどった上で、霊長類の分類・系統・進化、形態、遺伝、脳や生理・医科学、心理・認知、行動、社会と生態などの側面から霊長類研究にアプローチし、ひいては野生霊長類の保全や飼育霊長類の福祉の向上にも活かせる話題豊富な内容。また、ヒトも霊長類の一種であるため、ヒトのもつ形質の起源とその進化の研究にも活用でき、人類学的関心の追求にも役立つ中項目事典。
  • Shimada, Makoto (Ediotrs, Matsuzawa, Tetsuro, Humle, Tatyana, Sugiyama, Yukimaru, Tetsuro Matsuzawa, Tatyana Humle, Yukimaru Sugiyama (担当:共著, 範囲:Chap. 34, pp339-345, Genetic variation in the chimpanzees of Bossou and Nimba.; Append. E, DNA sequencing data, pp416-419)
    Springer 2011年6月 (ISBN: 4431539204)

講演・口頭発表等

 12

担当経験のある科目(授業)

 10

共同研究・競争的資金等の研究課題

 13

学術貢献活動

 29

社会貢献活動

 7

メディア報道

 2
  • 中日新聞社 中日新聞 夕刊 2014年1月11日 新聞・雑誌
    文部科学省科研費 新学術領域(新学術領域「交代劇」・公募研究)研究紹介
  • AAAS Science誌News欄 Science 308: 490-491, 22 April 2005 2005年4月22日 会誌・広報誌
    Shimada et al. (2007) 論文の内容を学会発表(The 74th Annual Meeting of American Association of Physical Anthropologists)した際の、Scienceの記者による報告。

その他

 14

教育内容・方法の工夫(授業評価等を含む)

 2
  • 件名
    藤田保健衛生大学内Faculty Development講習受講
    開始年月日
    2012/08/07
    終了年月日
    2012/08/07
    概要
    「ティーチング・ポートフォリオTPの導入・活用の実際と課題」
    外部講師: 土持ゲーリー法一
    (帝京大学高等教育開発センター長 ファカルティ・ディベロッパー
  • 件名
    第1回藤田保健衛生大学医学部医学情報教育ワークショップ「eラーニングシステムを体験する―Moodleの基礎―」修了
    開始年月日
    2014/06/24
    終了年月日
    2014/07/08

作成した教科書、教材、参考書

 1
  • 件名
    大学院特別講義資料(Web公開)
    開始年月日
    2012/10/09
    概要
    名古屋大学医学研究科での大学院特別講義資料を以下にて公開している。
    http://tinyurl.com/shimada-mk/

その他教育活動上特記すべき事項

 3
  • 件名
    学内アセンブリ教育・サイエンスカフェ参加(アセンブリII)
    開始年月日
    2017/04/01
    概要
    総合医科学研究所主催第2回メディカル・サイエンス・カフェの実行委員として学内アセンブリII(プロジェクト代表:倉橋総医研所長)活動を指導した。
  • 件名
    学内アセンブリ教育サッカー班(アセンブリI)
    開始年月日
    2009/05/11
    概要
    学内アセンブリ教育(各学部・学校1年時)サッカー班
  • 件名
    卒論指導
    開始年月日
    2018/04/02
    終了年月日
    2018/10/15