Steroids and growth factors control neuronal development through their receptors under physiological and pathological conditions. We show that PC12 cells harbor endogenous androgen receptor (AR), whose inhibition or silencing strongly interferes with neuritogenesis stimulated by the nonaromatizable synthetic androgen R1881 or NGF. This implies a role for AR not only in androgen signaling, but also in NGF signaling. In turn, a pharmacological TrkA inhibitor interferes with NGF- or androgen-induced neuritogenesis. In addition, androgen or NGF triggers AR association with TrkA, TrkA interaction with PI3-K delta, and downstream activation of PI3-K delta and Rac in PC12 cells. Once associated with AR, filamin A (FlnA) contributes to androgen or NGF neuritogenesis, likely through its interaction with signaling effectors, such as Rac. This study thus identifies a previously unrecognized reciprocal crosstalk between AR and TrkA, which is controlled by beta 1 integrin. The contribution of FlnA/AR complex and PI3-K d to neuronal differentiation by androgens and NGF is also novel. This is the first description of AR function in PC12 cells.
Cross-talk between androgen receptor/filamin A and TrkA regulates neurite outgrowth in PC12 cells / Di Donato, Marzia; Bilancio, Antonio; D'Amato, Loredana; Claudiani, Pamela; Oliviero, Maria Antoniett; Barone, Maria Vittoria; Auricchio, Alberto; Appella, Ettore; Migliaccio, Antimo; Auricchio, Ferdinando; Castoria, Gabriella. - In: MOLECULAR BIOLOGY OF THE CELL. - ISSN 1059-1524. - 26:15(2015), pp. 2858-2872. [10.1091/mbc.E14-09-1352]
Cross-talk between androgen receptor/filamin A and TrkA regulates neurite outgrowth in PC12 cells
Barone, Maria Vittoria;AURICCHIO, ALBERTO;
2015
Abstract
Steroids and growth factors control neuronal development through their receptors under physiological and pathological conditions. We show that PC12 cells harbor endogenous androgen receptor (AR), whose inhibition or silencing strongly interferes with neuritogenesis stimulated by the nonaromatizable synthetic androgen R1881 or NGF. This implies a role for AR not only in androgen signaling, but also in NGF signaling. In turn, a pharmacological TrkA inhibitor interferes with NGF- or androgen-induced neuritogenesis. In addition, androgen or NGF triggers AR association with TrkA, TrkA interaction with PI3-K delta, and downstream activation of PI3-K delta and Rac in PC12 cells. Once associated with AR, filamin A (FlnA) contributes to androgen or NGF neuritogenesis, likely through its interaction with signaling effectors, such as Rac. This study thus identifies a previously unrecognized reciprocal crosstalk between AR and TrkA, which is controlled by beta 1 integrin. The contribution of FlnA/AR complex and PI3-K d to neuronal differentiation by androgens and NGF is also novel. This is the first description of AR function in PC12 cells.I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.
