Reciprocal Feedback Regulation of PI3K and Androgen Receptor Signaling in PTEN-Deficient Prostate Cancer

Kim²,

et al. 2018

Cancer Medicine

BackgroundWe evaluated the association between serum levels of insulin‐like growth factor‐1 (IGF‐1), bioavailable testosterone, and surgical Gleason score (GS).MethodsWe analyzed 793 patients who underwent radical prostatectomy and 272 men with negative prostate biopsy. Serum levels of IGF‐1 and testosterone were measured before surgery or biopsy.ResultsThe mean IGF‐1 levels of prostate cancer patients and men with a negative biopsy were 143.8 and 118.9 ng/mL, respectively (P < 0.001). Men with high serum IGF‐1 were more likely to have prostate cancer (highest vs lowest quartile, odds ratio [OR] = 3.35; P trend < 0.001). However, among men with prostate cancer, the mean IGF‐1 levels of those with low (GS ≤ 6), intermediate (GS = 7), and high surgical GS (GS ≥8) were 151.7, 144.1, and 132.9 ng/mL, respectively (P < 0.001). Using quartile analysis, high serum IGF‐1 levels were shown to be associated with a low risk of high surgical GS (OR = 0.464; P trend = 0.006). Serum bioavailable testosterone concentration was positively correlated with serum IGF‐1 level (r = 0.157, P < 0.001). High bioavailable testosterone level was also associated with a low risk of high surgical GS in patients without diabetes mellitus (OR = 0.569; P trend = 0.040). Among men with biopsy GS ≤ 3 + 4 (n = 460), upgrading to high surgical GS was more frequent in patients with low IGF‐1 level (≤116.0 ng/mL; 9.9%) or low bioavailable testosterone level (≤0.85 ng/mL; 9.3%) than in patients with normal IGF‐1 and bioavailable testosterone levels (2.6%; P = 0.004).ConclusionsSerum levels of IGF‐1 and bioavailable testosterone show inverse associations with high surgical GS. This suggests that high‐grade prostate cancer develops independently of these two substances.

Section: Discussionmentioning

confidence: 99%

Association between serum levels of insulin‐like growth factor‐1, bioavailable testosterone, and pathologic Gleason score

Kim²,

et al. 2018

Cancer Medicine

“…In some cases the biomarker rationale for AKT inhibitor synergy with RTK or MAPK inhibition was less direct and indicative of crosstalk and feedback signaling previously reported 31 . Interestingly antagonism was observed in cell lines harboring activating mutations of AR [32][33][34][35] . Feedback signaling resulting from AKT inhibition has been seen to drive AR activity which in turn can lead to the activation of the MAPK cascade 35,36 , attenuating respectively targeting drug activity.…”

Section: Discussionmentioning

confidence: 99%

A cancer pharmacogenomic screen powering crowd-sourced advancement of drug combination prediction

Wang

Guan

et al. 2017

Preprint

In the last decade advances in genomics, uptake of targeted therapies, and the advent of personalized treatments have fueled a dramatic change in cancer care. However, the effectiveness of most targeted therapies is short lived, as tumors evolve and develop resistance. Combinations of drugs offer the potential to overcome resistance. The space of possible combinations is vast, and significant advances are required to effectively find optimal treatment regimens tailored to a patient's tumor. DREAM and AstraZeneca hosted a Challenge open to the scientific community aimed at computational prediction of synergistic drug combinations and predictive biomarkers associated to these combinations. We released a data set comprising ~11,500 experimentally tested drug combinations, coupled to deep molecular characterization of the respective 85 cancer cell lines. Among 150 submitted approaches, those that incorporated prior knowledge of putative drug targets showed superior performance predicting drug synergy across independent data. Genomic features of best-performing models revealed putative mechanisms of drug synergy for multiple drugs in combination with PI3K/AKT pathway inhibitors.All rights reserved. No reuse allowed without permission.(which was not peer-reviewed) is the author/funder, who has granted bioRxiv a license to display the preprint in perpetuity.

Molecular Cancer Research

“…The thermal cycling conditions were as follows: 95 C for 20 seconds followed by 40 cycles of 95 C for one second and 60 C for 20 seconds. To quantify the miRNA expression in the tumor tissues, we used the relative quantification (DDCt) method (13) with RNU6b serving as an internal control. RNA from PNF or LNCaP cells was always analyzed in parallel on the same reaction plate, and the expression of examined miRNAs in PNF or LNCaP cells was arbitrarily set to one.…”

Section: Mirna Qrt-pcrmentioning

confidence: 99%

“…The Pleckstrin homology domain and leucine rich repeat protein phosphatase (PHLPP) enzymes dephosphorylate the AKT kinase, which, in the phosphorylated state, induces cell growth. Loss of, or reduction of, PHLPP1 or PHLPP2 and the ensuing increase in phosphorylation of AKT is an established cause for induction and/or progression of prostate carcinoma (11)(12)(13). MiR-15a and miR-375, therefore, play important roles in prostate carcinoma and may represent potential therapeutic targets.…”

Section: Introductionmentioning

confidence: 99%

Comparative microRNA Profiling of Prostate Carcinomas with Increasing Tumor Stage by Deep Sequencing

Hart

Nolte

Wach

et al. 2014

MicroRNAs (miRNA) posttranscriptionally regulate gene expression and are important in tumorigenesis. Previous deep sequencing identified the miRNA profile of prostate carcinoma versus nonmalignant prostate tissue. Here, we generated miRNA expression profiles of prostate carcinoma by deep sequencing, with increasing tumor stage relative to corresponding nonmalignant and healthy prostate tissue, and detected clearly changed miRNA expression patterns. The miRNA profiles of the healthy and nonmalignant tissues were consistent with our previous findings, indicating a high fidelity of the method employed. In the tumors, quantitative real-time PCR (qRT-PCR) analysis of 40 paired samples of prostate carcinoma versus normal tissue revealed significant upregulation of miR-20a, miR-148a, miR-200b, and miR-375 and downregulation of miR-143 and miR-145. Hereby, miR-375 increased from normal to organ-confined tumors (pT2 pN0), slightly decreased in tumors with extracapsular growth (pT3 pN0), but was then expressed again at higher levels in lymph node metastasizing (pN1) tumors. The sequencing data for miR-375 were confirmed by Northern blotting and qRT-PCR. The regulation for other selected miRNAs could, however, not be confirmed by qRT-PCR in individual tumor stages. MiR-200b, in addition to miR-200c and miR-375 reduced the expression of SEC23A. Interestingly, miR-375, found by sequencing in pT2 upregulated by us and others in tumor versus normal tissue, and miR-15a, found by sequencing in pT2 and pT3 and in the metastasizing tumors, target the phosphatases PHLPP1 and PHLPP2, respectively. PHLPP1 and PHLPP2 dephosphorylate members of the AKT family of signal transducers, thereby inhibiting cell growth. Coexpression of miR-15a and miR-375 resulted in downregulation of PHLPP1/2 and strongly increased prostate carcinoma cell growth.Implications: These genomic data reveal relevant miRNAs in prostate cancer that may have biomarker and therapeutic potential. Mol Cancer Res; 12(2); 250-63. Ó2013 AACR. IntroductionProstate carcinoma is the second most frequently diagnosed malignancy and a leading cause of cancer-related death in men worldwide (1). The underlying mechanisms resulting in invasive growth after dissemination of the primary tumor from the initial site in the prostate are not completely understood. MicroRNAs (miRNAs) are now recognized as contributing factors to the induction, growth, and metastasis