Expression and function of TRK-B and BDNF in human neuroblastomas.

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Mol Cell Biol. 1994 January; 14(1): 759-767

Expression and function of TRK-B and BDNF in human neuroblastomas.

A Nakagawara, C G Azar, N J Scavarda and G M Brodeur

Department of Pediatrics, Washington University School of Medicine, St. Louis, Missouri 63110.

ABSTRACT

There is considerable interest in the role of the TRK familyof neuotrophin receptors in regulating growth and differentiationin normal and neoplastic nerve cells. A neuroblastoma is a commonpediatric tumor derived from the neural crest, and the majorityof favorable neuroblastomas express a high level of TRK-A mRNA.However, little is known about the expression or function ofTRK-B in these tumors. TRK-B encodes a tyrosine kinase thatbinds to brain-derived neuotrophic factor (BDNF), as well asneurotrophin-3 (NT-3) and NT-4/5. We have studied the N-myc-amplifiedhuman neuroblastoma cell line, SMS-KCN, which expresses bothTRK-B and BDNF. Exogenous BDNF induces tyrosine phosphorylationof TRK-B as well as phosphorylation of phospholipase C-gamma1, the extracellular signal-regulated kinases 1 and 2, and phosphatidylinositol-3kinase. BDNF also induces expression of the immediate-earlygenes c-FOS and NGFI-A but not NGFI-B or NGFI-C. In addition,BDNF appears to promote cell survival and neurite outgrowth.SMS-KCN cells also express TRK-A, which is phosphorylated inresponse to nerve growth factor. However, the downstream TRK-Asignaling is apparently defective. Finally, we determined thatin a series of 74 primary neuroblastomas, 36% express TRK-BmRNA, 68% express BDNF mRNA, and 31% express both. TruncatedTRK-B appears to be preferentially expressed in more-differentiatedtumors (ganglioneuromas and ganglioneuroblastomas), whereasfull-length TRK-B is expressed almost exclusively in immatureneuroblastomas with N-myc amplification. Our findings suggestthat in TRK-B-expressing human neuroblastomas, BDNF promotessurvival and induces neurite outgrowth in an autocrine or paracrinemanner. The BDNF/TRK-B pathway may be particularly importantfor growth and differentiation of neuroblastomas with N-mycamplification.

Mol Cell Biol. 1994 January; 14(1): 759-767

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