Analysis of the mouse transcriptome based on functional annotation of 60,770 full-length cDNAs

Y. Okazaki; M. Furuno; T. Kasukawa; J. Adachi; H. Bono; S. Kondo; I. Nikaido; N. Osato; R. Saito; H. Suzuki; I. Yamanaka; H. Kiyosawa; K. Yagi; Y. Tomaru; Y. Hasegawa; A. Nogami; C. Schönbach; T. Gojobori; R. Baldarelli; D. P. Hill; C. Bult; D. A. Hume; J. Quackenbush; L. M. Schriml; A. Kanapin; H. Matsuda; S. Batalov; K. W. Beisel; J. A. Blake; D. Bradt; V. Brusic; C. Chothia; L. E. Corbani; S. Cousins; E. Dalla; T. A. Dragani; C. F. Fletcher; A. Forrest; K. S. Frazer; T. Gaasterland; M. Gariboldi; C. Gissi; A. Godzik; J. Gough; S. Grimmond; S. Gustincich; N. Hirokawa; I. J. Jackson; E. D. Jarvis; A. Kanai; H. Kawaji; Y. Kawasawa; R. M. Kedzierski; B. L. King; A. Konagaya; I. V. Kurochkin; Y. Lee; B. Lenhard; P. A. Lyons; D. R. Maglott; L. Maltais; L. Marchionni; L. McKenzie; H. Miki; T. Nagashima; K. Numata; T. Okido; W. J. Pavan; G. Pertea; G. Pesole; N. Petrovsky; R. Pillai; J. U. Pontius; D. Qi; S. Ramachandran; T. Ravasi; J. C. Reed; D. J. Reed; J. Reid; B. Z. Ring; M. Ringwald; A. Sandelin; C. Schneider; C. A.M. Semple; M. Setou; K. Shimada; R. Sultana; Y. Takenaka; M. S. Taylor; R. D. Teasdale; M. Tomita; R. Verardo; L. Wagner; C. Wahlestedt; Y. Wang; Y. Watanabe; C. Wells; L. G. Wilming; A. Wynshaw-Boris; M. Yanagisawa; I. Yang; L. Yang; Z. Yuan; M. Zavolan; Y. Zhu; A. Zimmer; P. Carninci; N. Hayatsu; T. Hirozane-Kishikawa; H. Konno; M. Nakamura; N. Sakazume; K. Sato; T. Shiraki; K. Waki; J. Kawai; K. Aizawa; T. Arakawa; S. Fukuda; A. Hara; W. Hashizume; K. Imotani; Y. Ishii; M. Itoh; I. Kagawa; A. Miyazaki; K. Sakai; D. Sasaki; K. Shibata; A. Shinagawa; A. Yasunishi; M. Yoshino; R. Waterston; E. S. Lander; J. Rogers; E. Birney; Y. Hayashizaki

Journal ArticleOPEN ACCESS

Analysis of the mouse transcriptome based on functional annotation of 60,770 full-length cDNAs

Nature (2002) 420(6915) 563-573

DOI: 10.1038/nature01266

1.5kCitations

723Readers

Abstract

Only a small proportion of the mouse genome is transcribed into mature messenger RNA transcripts. There is an international collaborative effort to identify all full-length mRNA transcripts from the mouse, and to ensure that each is represented in a physical collection of clones. Here we report the manual annotation of 60,770 full-length mouse complementary DNA sequences. These are clustered into 33,409 'transcriptional units', contributing 90.1% of a newly established mouse transcriptome database. Of these transcriptional units, 4,258 are new protein-coding and 11,665 are new non-coding messages, indicating that non-coding RNA is a major component of the transcriptome. 41% of all transcriptional units showed evidence of alternative splicing. In protein-coding transcripts, 79% of splice variations altered the protein product. Whole-transcriptome analyses resulted in the identification of 2,431 sense-antisense pairs. The present work, completely supported by physical clones, provides the most comprehensive survey of a mammalian transcriptome so far, and is a valuable resource for functional genomics.

Cite

CITATION STYLE

APA

Okazaki, Y., Furuno, M., Kasukawa, T., Adachi, J., Bono, H., Kondo, S., … Hayashizaki, Y. (2002). Analysis of the mouse transcriptome based on functional annotation of 60,770 full-length cDNAs. Nature, 420(6915), 563–573. https://doi.org/10.1038/nature01266

Analysis of the mouse transcriptome based on functional annotation of 60,770 full-length cDNAs

Abstract

Cite

Register to see more suggestions