par Nakahara, Masanori;Isozaki, K;Vanderwinden, Jean-Marie 
;Shinomura, Yasuhisa;Kitamura, Yukihiko;Hirota, S;Matsuzawa, Yuji
Référence Life sciences, 70, 20, page (2367-2376)
Publication Publié, 2002-04
;Shinomura, Yasuhisa;Kitamura, Yukihiko;Hirota, S;Matsuzawa, YujiRéférence Life sciences, 70, 20, page (2367-2376)
Publication Publié, 2002-04
Article révisé par les pairs
| Résumé : | Interstitial cells of Cajal (ICCs) play a role as pacemakers for gastrointestinal movement. Although some in vivo experiments showed that the c-kit receptor tyrosine kinase (KIT) and its ligand, stem cell factor (SCF), might be required for the development of murine ICCs near birth, in vitro experiments would be useful to clarify the role of SCF-KIT system for the development of ICCs. We attempted to establish a culture system in order to investigate the proliferation of ICCs. Murine gastrointestinal cells from embryos or neonates were cultured with SCF and stained with anti-KIT antibody and/or alcian-blue. The numbers of KIT+ cells a n d alcian-blue+ cells we re counted, and the number of KIT+.alcian-blue- cells, which represent ICCs was calculated. Clusters containing KIT+ cells were formed in culture. The number of KIT+.alcian-blue- cells from day-18 post coitum embryos increased in response to SCF up to a concentration of 50 ng/ml or for 8 days. The number of cells from day-2 post-partum neonates increased for 4 days, and then remained constant in the presence of SCF. In contrast, the number of cells from day-6 post-partum neonates did not increase and remained constant, even in the presence of SCF. ICCs showed a dose-dependent and time-limited proliferation in response to SCF in the in vitro culture system used here in. |
