Phosphoinositide 3-Kinase-independent Non-genomic Signals Transit from the Androgen Receptor to Akt1 in Membrane Raft Microdomains

Cinar, Bekir; Mukhopadhyay, Nishit K.; Meng, Guowang; Freeman, Michael R.

doi:10.1074/jbc.m703310200

Cited by 85 publications

(63 citation statements)

References 42 publications

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“…These studies suggest a mechanism of signal downregulation of IRS-1 that is mediated by monomeric p85 through the formation of a sequestration complex between p85 and IRS-1 ( 187 ). Modulation of PI3K-Akt signaling components in the membrane raft microdomains have been reported (188)(189)(190). Consistent with these reports, we have also demonstrated the localization of the IR and PI3K in detergentresistant membrane rafts of rod photoreceptor outer segments ( 191 ).…”

Section: Pi3k Knockout Phenotypessupporting

confidence: 90%

Phosphoinositide 3-kinase signaling in the vertebrate retina

Rajala

2010

Journal of Lipid Research

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This article is available online at http://www.jlr.org was established by Streb et al. ( 3 ) in their classic paper that showed elevations in IP 3 caused intracellular release of bound calcium. Subsequently, 1,2-DG was found to stimulate protein kinase C (PKC), a serine/threonine kinase that phosphorylates a number of cellular proteins ( 4 ). Activation of the PLC/PKC cascade affects a variety of cellular events, including secretion, phagocytosis, smooth muscle contraction, proliferation, neurotransmission, and metabolism [see reviews by Rhee ( 5 ), Rhee and Choi ( 6 ), and Berridge ( 7 ) THE PI CYCLEIn the early 1950s, Hokin and Hokin ( 1, 2 ) discovered that addition of acetylcholine to brain slices stimulated the incorporation of phosphate and inositol but not glycerol into lipids; the major products of this incorporation were phosphatidylinositol (PI) and phosphatidic acid. Subsequent studies defi ned the reactions of the PI cycle and showed that the initial event was receptor-meditated activation of a phospholipase C (PLC), which hydrolyzes phosphatidylinositol 4,5-bisphosphate (PI-4,5-P 2 ) to 1,2-diacylglycerol (DG) and inositol 1,4,5-trisphosphate (IP 3 ). This increase in lipid synthesis reported by the Hokins was a recovery reaction that rapidly replenished PI separate from de novo PI synthesis. The role of 1,4, This work was supported by grants

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Section: Pi3k Knockout Phenotypessupporting

confidence: 90%

Phosphoinositide 3-kinase signaling in the vertebrate retina

Rajala

2010

Journal of Lipid Research

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“…In this study, we showed that ␤2M mAb inhibited a large number of cell signaling networks, including MAPK, SREBP-1, AR, and PI3K/Akt. It is conceivable that these signaling networks are interconnected through lipid raft complexes (47,48). The inhibitory action exerted by ␤2M mAb could affect the lipid composition of the raft structures, hence altering domain interactions and how downstream cell signal networks can be assembled and interact in a coordinated manner (45,49).…”

Section: Discussionmentioning

confidence: 99%

Androgen Receptor Survival Signaling Is Blocked by Anti-β2-microglobulin Monoclonal Antibody via a MAPK/Lipogenic Pathway in Human Prostate Cancer Cells

Huang

Zhau

Chung

2010

Journal of Biological Chemistry

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A new cis-acting element, sterol regulatory element-binding protein-1 (SREBP-1) binding site, within the 5-flanking human androgen receptor (AR) promoter region and its binding transcription factor, SREBP-1, was identified to regulate AR transcription in AR-positive human prostate cancer cells. We further characterized the molecular mechanism by which a novel anti-␤2-microglobulin monoclonal antibody (␤2M mAb), shown to induce massive cell death in a number of human and mouse cancer cell lines, interrupted multiple cell signaling pathways in human prostate cancer cells. ␤2M mAb decreased AR expression through inactivation of MAPK and SREBP-1. By inactivation of MAPK, ␤2M mAb decreased prostate cancer cell proliferation and survival. By inhibition of SREBP-1, ␤2M mAb reduced fatty acid and lipid levels, an integral component of cell membrane, cell signaling mediators, and energy metabolism. These results provide for the first time a molecular link between the ␤2M intracellular signaling axis mediated by MAPK and SREBP-1 and involving lipid signaling, which collectively regulates AR expression and function. Antagonizing ␤2M by ␤2M mAb may be an effective therapeutic approach simultaneously targeting multiple downstream signaling pathways converging with MAPK, SREBP-1, and AR, important for controlling prostate cancer cell growth, survival, and progression. ␤2-Microglobulin (␤2M)3 is a co-receptor of a major histocompatibility complex class I antigen. ␤2M has been implicated in the regulation of the host immune mechanism and is essential for the recognition of foreign antigens by T-lymphocytes (1). Recent reports from our laboratory and others assigned additional biological functions to ␤2M as a diagnostic and prognostic indicator for multiple myeloma, prostate, and breast cancers (2-5); a growth factor and a signaling molecule (6, 7); a new androgen and androgen receptor (AR) target gene (8); and an attractive new therapeutic target for both liquid (9) and solid (10, 11) tumor malignancies. Blockade of ␤2M and its related signaling pathways by sequence-specific siRNA or antibody resulted in the inhibition of AR expression and activity and the induction of extensive prostate cancer cell death in vitro as well as prostate tumor regression in immune-compromised mice (7, 10). In addition, anti-␤2M monoclonal antibody (␤2M mAb) has been shown not to significantly affect the growth of normal cells, consistent with experimental observations where transgenic mice with a ␤2M deficit had normal organ function and life expectancy (9, 10, 12). Therefore, ␤2M and its signaling axis may offer an opportunity for improving the clinical targeting of prostate cancer.AR is a key growth and survival regulatory transcription factor for androgen target organs during normal development and neoplastic progression. Recognition of the importance of the AR signaling axis, particularly in castration-resistant prostate cancer, has prompted discoveries targeting androgen biosynthetic pathways using abiraterone as an agent for a Phase III trial...

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“…However, we (Liao et al, 2004) and other (Mellinghoff et al, 2004) found that Src kinase inhibitor did not suppress androgen-induced gene expression, indicating that Src kinase is not involved in androgen-induced PI3K activation or AR genomic effect. In addition, recent studies showed that after androgen stimulation the AR was transiently translocated to the lipid rafts on the plasma membrane (Lu et al, 2001;Cinar et al, 2007), where multiple signaling molecules such as G proteins are located (reviewed in Chini and Parenti, 2004). In fact, G protein a-subunit has been shown to activate the AR in the absence or presence of androgens (Kasbohm et al, 2005).…”

Section: Discussionmentioning

confidence: 99%

Phosphoinositide 3-OH kinase p85α and p110β are essential for androgen receptor transactivation and tumor progression in prostate cancers

et al. 2008

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Phosphoinositide 3-OH kinases (PI3Ks) are a group of major intracellular signaling molecules. In our previous study, we found that inhibition of PI3K activity suppressed the androgen receptor (AR)-mediated gene expression in prostate cancer cells. The AR has been considered as a critical determinant for the development and progression of human prostate cancers. In this study, we sought to identify the PI3K isoforms involved in AR transactivation. Using a gene-specific small interference RNA (siRNA) approach, we determined that the regulatory isoform p85a and the catalytic isoform p110b, but not p110a, were required for androgen-stimulated AR transactivation and cell proliferation in prostate cancer cells. Consistently, overexpression of wild-type p110b but not p110a gene led to androgen-independent AR transactivation. Silencing p110b gene in prostate cancer cells abolished tumor growth in nude mice. Of the dual (lipid and protein) kinase activities, p110b's lipid kinase activity was required for AR transactivation. Further analysis by a chromatin immunoprecipitation assay showed that p110b is indispensable for androgen-induced AR-DNA interaction. Finally, gene expression analysis of clinical specimens showed that both p85a and p110b were highly expressed in malignant prostate tissues compared to the nonmalignant compartments, and their expression levels correlated significantly with disease progression. Taken together, our data demonstrated that p85a and p110b are essential for androgen-stimulated AR transactivation, and their aberrant expression or activation might play an important role in prostate cancer progression.

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Phosphoinositide 3-Kinase-independent Non-genomic Signals Transit from the Androgen Receptor to Akt1 in Membrane Raft Microdomains

Cited by 85 publications

References 42 publications

Phosphoinositide 3-kinase signaling in the vertebrate retina

Phosphoinositide 3-kinase signaling in the vertebrate retina

Androgen Receptor Survival Signaling Is Blocked by Anti-β2-microglobulin Monoclonal Antibody via a MAPK/Lipogenic Pathway in Human Prostate Cancer Cells

Phosphoinositide 3-OH kinase p85α and p110β are essential for androgen receptor transactivation and tumor progression in prostate cancers

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