Involvement of Shc in the signaling response of human prostate tumor cell lines to epidermal growth factor

Abstract: Autocrine growth factors for the epidermal growth factor receptor (EGFR) have been identified in prostate tumors, implicating a role for EGFR in the progression of prostate cancer. To investigate early signaling mechanisms used by the EGFR in prostate tumor cells, we have characterized the involvement of the Shc (src homology 2/x‐collagen related) adapter protein in EGFR signaling in several human prostate tumor cell lines. In androgen‐responsive lymph node‐prostate cancer (LNCaP) cells and androgen‐insensitiv… Show more

“…For example, Shc has been identi®ed as one of the important molecules involved in BCR ± Abl mediated transformation (Goga et al, 1995). Moreover, Shc has been found to be hyperphosphorylated in several breast cancer lines and prostate cancer cells, and in some cases the proliferation of these transformed cells could be inhibited by overexpression of dominant negative proteins (Agarwal, 2000;Biscardi et al, 1998;Dankort et al, 2001;Gresham et al, 1998;Qiu et al, 1998;Rauh et al, 1999;Stevenson and Frackelton, 1998;Stevenson et al, 1999). Whether Shc provides a proliferative or survival signal under these conditions is not known, but it was suggestive that enhanced Shcmediated signaling was bene®cial in the growth or maintenance of the tumorigenic state.…”

Signaling via Shc family adapter proteins

“…For example, Shc has been identi®ed as one of the important molecules involved in BCR ± Abl mediated transformation (Goga et al, 1995). Moreover, Shc has been found to be hyperphosphorylated in several breast cancer lines and prostate cancer cells, and in some cases the proliferation of these transformed cells could be inhibited by overexpression of dominant negative proteins (Agarwal, 2000;Biscardi et al, 1998;Dankort et al, 2001;Gresham et al, 1998;Qiu et al, 1998;Rauh et al, 1999;Stevenson and Frackelton, 1998;Stevenson et al, 1999). Whether Shc provides a proliferative or survival signal under these conditions is not known, but it was suggestive that enhanced Shcmediated signaling was bene®cial in the growth or maintenance of the tumorigenic state.…”

Signaling via Shc family adapter proteins

“…Alternatively, sex hormones may stabilize p66 Shc protein by altering its metabolic pathway including protein biosynthesis and/or degradation rate, resulting in an increased level of p66 Shc protein. Although the mechanism by which sex hormones raise p66 Shc protein level and cell growth rate remains to be elucidated, it is of interest that in androgen‐independent DU 145 cells, high basal level of p66 Shc protein is also correlated with rapid growth rate (unpublished observations) 29, 30. The same parallel can be drawn between our observation of a coordinated increase in p66 Shc levels and growth rate and the observation that the p66 Shc protein levels in human breast cancer correlate with increased metastatic potential 31…”

p66^Shc protein is upregulated by steroid hormones in hormone‐sensitive cancer cells and in primary prostate carcinomas

“…The Shc gene is related to cell proliferation and carcinogenesis (16,48). In fact the p52 Shc and p46 Shc isoforms of Shc were found to be overexpressed (5,8,56,58) or hyperphosphorylated (28,49) in many tumor types.…”

“…Indeed different levels of p66 Shc were found in some tumors but the results seem contradictory. For example, in breast cancer cells and primary tumors, p66 Shc was described to be both overexpressed (16,22,29) and downregulated (49,59). Indeed the ablation of p66 Shc does not increase spontaneous or induced tumor incidence in mice (32,51).…”

Apoptosis and Aging: Role of p66^ShcRedox Protein