-
Views
-
Cite
Cite
Rina Takai, Eriko Tanaka, Toshiaki Miyazaki, Mikiya Suda, Fumio Tashiro, Function of RNH-l/14–3–3β Gene in Cellular Differentiation and Proliferation, The Journal of Biochemistry, Volume 118, Issue 5, October 1995, Pages 1045–1053, https://doi.org/10.1093/jb/118.5.1045
Close - Share Icon Share
Abstract
It has recently been reported that the members of 14–3–3 protein family participate in cell cycle control and associate with Raf, Bcr, Bcr-Abl, and polyomavirus middle tumor antigen (MT) as modulators of signal transduction. During cDNA cloning for the 17-kDa neuronal differentiation factor (K2 factor) secreted from rat hepatoma Kagura-2 (K2) cells from a K2 cDNA library using rat prepronerve growth factor (prepro NGF) cDNA as a probe, we obtained RNH-1 (rat NGF homologue) clone, which was identified as 14–3–3β cDNA, but not K2 factor, although no significant homology is present between 14–3–3β and prepro NGF cDNAs. RNH-1/14–3–3β gene was markedly expressed as a 2.9-kb mRNA in K2 cells and in newborn rat brain tissue. In PC12 cells the expression of this gene was down-regulated during the neuronal differentiation primed by NGF. The enforced expression of RNH-1/14–3–3β in PC12 and K2 cells conferred on them a higher sensitivity to NGF for neuronal differentiation and an intense growth ability in low serum medium, respectively. These results provide additional evidence that RNH-l/14–3–3β protein participates in cellular differentiation, proliferation and transformation through the signal transduction pathways of various growth factors.
- signal transduction
- cloning
- liver neoplasms
- carcinoma, hepatocellular
- clone cells
- dna, complementary
- genes
- growth factor
- newborn
- libraries
- pc12 cells
- polyomavirus
- rna, messenger
- rats
- liver cancer
- tumor antigens
- signal transduction pathways
- cell cycle control
- bcr-abl tyrosine kinase
- brain tissue
- neuron differentiation
- synthetic cannabinoids
