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  • Nuclear GRP75 binds retinoic acid receptors to promote neuronal differentiation of neuroblastoma.

Nuclear GRP75 binds retinoic acid receptors to promote neuronal differentiation of neuroblastoma.

PloS one (2011-10-25)
Yu-Yin Shih, Hsinyu Lee, Akira Nakagawara, Hseuh-Fen Juan, Yung-Ming Jeng, Yeou-Guang Tsay, Dong-Tsamn Lin, Fon-Jou Hsieh, Chien-Yuan Pan, Wen-Ming Hsu, Yung-Feng Liao
ANOTACE

Retinoic acid (RA) has been approved for the differentiation therapy of neuroblastoma (NB). Previous work revealed a correlation between glucose-regulated protein 75 (GRP75) and the RA-elicited neuronal differentiation of NB cells. The present study further demonstrated that GRP75 translocates into the nucleus and physically interacts with retinoid receptors (RARα and RXRα) to augment RA-elicited neuronal differentiation. GRP75 was required for RARα/RXRα-mediated transcriptional regulation and was shown to reduce the proteasome-mediated degradation of RARα/RXRαin a RA-dependent manner. More intriguingly, the level of GRP75/RARα/RXRα tripartite complexes was tightly associated with the RA-induced suppression of tumor growth in animals and the histological grade of differentiation in human NB tumors. The formation of GRP75/RARα/RXRα complexes was intimately correlated with a normal MYCN copy number of NB tumors, possibly implicating a favorable prognosis of NB tumors. The present findings reveal a novel function of nucleus-localized GRP75 in actively promoting neuronal differentiation, delineating the mode of action for the differentiation therapy of NB by RA.

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Sigma-Aldrich
Nuclei Isolation Kit: Nuclei EZ Prep, sufficient for 25 nuclei preparations (~1-10×107 cells/preparation)