A Single RET Mutation in Hirschsprung Disease Induces Intestinal Aganglionosis Via a Dominant-Negative Mechanism

Sunardi, Mukhamad; Ito, Keisuke; Sato, Yuya; Uesaka, Toshihiro; Iwasaki, Mitsuhiro; Enomoto, Hideki

https://hdl.handle.net/20.500.14094/0100482164

このアイテムのアクセス数:73件（2025-08-02 19:46 集計）

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メタデータID	0100482164
アクセス権	open access
出版タイプ	Version of Record
タイトル	A Single RET Mutation in Hirschsprung Disease Induces Intestinal Aganglionosis Via a Dominant-Negative Mechanism
著者	Sunardi, Mukhamad ; Ito, Keisuke ; Sato, Yuya ; Uesaka, Toshihiro ; Iwasaki, Mitsuhiro ; Enomoto, Hideki
著者名 Sunardi, Mukhamad
著者ID A0837 研究者ID 1000010575468 KUID https://kuid-rm-web.ofc.kobe-u.ac.jp/search/detail?systemId=2666849c070eb3a6520e17560c007669 著者名 Ito, Keisuke 伊藤, 圭祐イトウ, ケイスケ所属機関名医学研究科
著者ID A2587 研究者ID 1000000866353 著者名 Sato, Yuya 佐藤, 祐哉サトウ, ユウヤ所属機関名医学研究科
著者ID A1669 研究者ID 1000090304451 KUID https://kuid-rm-web.ofc.kobe-u.ac.jp/search/detail?systemId=c5669b2d190545f4520e17560c007669 著者名 Uesaka, Toshihiro 上坂, 敏弘ウエサカ, トシヒロ所属機関名医学研究科
著者名 Iwasaki, Mitsuhiro
著者ID A0835 研究者ID 1000000360511 KUID https://kuid-rm-web.ofc.kobe-u.ac.jp/search/detail?systemId=52429d8e75d81a3d520e17560c007669 著者名 Enomoto, Hideki 榎本, 秀樹エノモト, ヒデキ所属機関名医学研究科
言語	English (英語)
収録物名	Cellular and Molecular Gastroenterology and Hepatology
巻(号)	15(6)
ページ	1505-1524
出版者	Elsevier
刊行日	2023
公開日	2023-06-13
抄録	Background & Aims: Hirschsprung disease (HSCR) is a congenital disorder characterized by the absence of the enteric nervous system (ENS). HSCR potentially involves multiple gene aberrations and displays complex patterns of inheritance. Mutations of the RET gene, encoding the RET receptor tyrosine kinase, play a central role in the pathogenesis of HSCR. Although a wide variety of coding RET mutations have been identified, their pathogenetic significance in vivo has remained largely unclear. Methods: We introduced a HSCR-associated RET missense mutation, RET(S811F), into the corresponding region (S812) of the mouse Ret gene. Pathogenetic impact of Ret(S812F) was assessed by histologic and functional analyses of the ENS and by biochemical analyses. Interactions of the Ret(S812F) allele with HSCR susceptibility genes, the RET9 allele and the Ednrb gene, were examined by genetic crossing in mice. Results: RetS812F/+ mice displayed intestinal aganglionosis (incidence, 50%) or hypoganglionosis (50%), impaired differentiation of enteric neurons, defecation deficits, and increased lethality. Biochemical analyses revealed that Ret(S811F) protein was not only kinase-deficient but also abrogated function of wild-type RET in trans. Moreover, the Ret(S812F) allele interacted with other HSCR susceptibility genes and caused intestinal aganglionosis with full penetrance. Conclusions: This study demonstrates that a single RET missense mutation alone induces intestinal aganglionosis via a dominant-negative mechanism. The RetS812F/+ mice model HSCR displays dominant inheritance with incomplete penetrance and serves as a valuable platform for better understanding of the pathogenetic mechanism of HSCR caused by coding RET mutations.
キーワード	RET
	Hirschsprung Disease
	Genetic Interactions
	Missense Mutation
カテゴリ	医学研究科
カテゴリ	学術雑誌論文
権利	© 2023 The Authors.
権利	This is an open access article under the Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International license
関連情報	DOI https://doi.org/10.1016/j.jcmgh.2022.12.003

資源タイプ	journal article
eISSN	2352-345X　OPACで所蔵を検索　 CiNiiで学外所蔵を検索

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