Mutations and Deregulation of Ras/Raf/MEK/ERK and PI3K/PTEN/Akt/mTOR Cascades Which Alter Therapy Response.

MicroRNAs (miRs) regulate a variety of cellular processes, and their impaired expression is involved in cancer. Silencing of tumorsuppressive miRs in cancer can occur through epigenetic modifications, including DNA methylation and histone deacetylation. We performed comparative miR profiling on cultured lung cancer cells before and after treatment with 5′aza-deoxycytidine plus Trichostatin A to reverse DNA methylation and histone deacetylation, respectively. Several tens of miRs were strongly induced by such 'epigenetic therapy'. Two representatives, miR-512-5p (miR-512) and miR-373, were selected for further analysis. Both miRs were secreted in exosomes. Re-expression of both miRs augmented cisplatin-induced apoptosis and inhibited cell migration; miR-512 also reduced cell proliferation. TEAD4 mRNA was confirmed as a direct target of miR-512; likewise, miR-373 was found to target RelA and PIK3CA mRNA directly. Our results imply that miR-512 and miR-373 exert cell-autonomous and non-autonomous tumor-suppressive effects in lung cancer cells, where their re-expression may benefit epigenetic cancer therapy.

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“…35 In agreement, miR-373 overexpression reduced Akt phosphorylation without affecting the overall amount of Akt (Figure 6e). Figure 5e.…”

Section: Mir-373supporting

confidence: 72%

“…Cells were harvested and subjected to western blot analysis of total Akt1, phosphorylated Akt (pAkt) and GAPDH, n = 2 Activation of the PI3K/Akt pathway confers chemotherapy resistance. 35 Therefore, inhibition of PIK3CA may contribute to the enhanced death of A549 cells upon combined treatment with miR-373 and cisplatin.…”

Section: Mir-373mentioning

confidence: 99%

Reactivation of epigenetically silenced miR-512 and miR-373 sensitizes lung cancer cells to cisplatin and restricts tumor growth

et al. 2015

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“…Furthermore, PI3K activation via activating mutations of RAS contributes to RASmediated cellular transformation (9,10). In addition to promoting cancer cell proliferation and survival, activation of the PI3K pathway mediates resistance to both RTK inhibitors and genotoxic agents (11,12), such that PI3K inhibition increases cancer cell sensitivity to targeted agents, as well as platinum-based drugs and taxanes (13)(14)(15). Selective inhibition of key nodes of the PI3K pathway represents an attractive therapeutic intervention for the treatment of solid and hematologic cancers, and both pan-class I and isoform-selective PI3K inhibitors have entered clinical testing (3,16).…”

Section: Introductionmentioning

confidence: 99%

Phase I Safety, Pharmacokinetic, and Pharmacodynamic Study of SAR245408 (XL147), an Oral Pan-Class I PI3K Inhibitor, in Patients with Advanced Solid Tumors

Shapiro

Rodón

Bedell

et al. 2014

Clinical Cancer Research

140

101

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Purpose: SAR245408 is a pan-class I phosphoinositide 3-kinase (PI3K) inhibitor. This phase I study determined the maximum tolerated dose (MTD) of two dosing schedules [first 21 days of a 28-day period (21/7) and continuous once-daily dosing (CDD)], pharmacokinetic and pharmacodynamic profiles, and preliminary efficacy.Experimental Design: Patients with refractory advanced solid malignancies were treated with SAR245408 using a 3 þ 3 design. Pharmacokinetic parameters were determined after single and repeated doses. Pharmacodynamic effects were evaluated in plasma, hair sheath cells, and skin and tumor biopsies.Results: Sixty-nine patients were enrolled. The MTD of both schedules was 600 mg; dose-limiting toxicities were maculopapular rash and hypersensitivity reaction. The most frequent drug-related adverse events included dermatologic toxicities, diarrhea, nausea, and decreased appetite. Plasma pharmacokinetics showed a median time to maximum concentration of 8 to 22 hours, mean terminal elimination half-life of 70 to 88 hours, and 5-to 13-fold accumulation after daily dosing (first cycle). Steady-state concentration was reached between days 15 and 21, and exposure was dose-proportional with doses up to 400 mg. SAR245408 inhibited the PI3K pathway ($40%-80% reduction in phosphorylation of AKT, PRAS40, 4EBP1, and S6 in tumor and surrogate tissues) and, unexpectedly, also inhibited the MEK/ERK pathway. A partial response was seen in one patient with advanced non-small cell lung cancer. Eight patients were progression-free at 6 months. Pharmacodynamic and clinical activity were observed irrespective of tumor PI3K pathway molecular alterations.Conclusions: SAR245408 was tolerable at doses associated with PI3K pathway inhibition. The recommended phase II dose of the capsule formulation is 600 mg administered orally with CDD. Clin Cancer Res; 20(1); 233-45. Ó2013 AACR.

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“…Since p53 is the "guardian of the genome," then successful treatment with these drugs would hinge on the presence of functional p53 within the cancer itself. 4,41,42 The genomic TP53 status of the 22Rv-1, LNCaP and DU145 prostate cancer cell lines have been reported ( Table 1). 43 Retroviral constructs expressing the full-length wild-type p53 protein (p53WT) and the truncated dominant-negative form of the p53 protein (p53DD) were stably introduced into the 22Rv-1 and LNCaP cell lines.…”

Section: Resultsmentioning

confidence: 99%

p53 expression controls prostate cancer sensitivity to chemotherapy and the MDM2 inhibitor Nutlin-3

et al. 2012

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Mutations and Deregulation of Ras/Raf/MEK/ERK and PI3K/PTEN/Akt/mTOR Cascades Which Alter Therapy Response.

Cited by 242 publications

References 384 publications

Reactivation of epigenetically silenced miR-512 and miR-373 sensitizes lung cancer cells to cisplatin and restricts tumor growth

Reactivation of epigenetically silenced miR-512 and miR-373 sensitizes lung cancer cells to cisplatin and restricts tumor growth

Phase I Safety, Pharmacokinetic, and Pharmacodynamic Study of SAR245408 (XL147), an Oral Pan-Class I PI3K Inhibitor, in Patients with Advanced Solid Tumors

p53 expression controls prostate cancer sensitivity to chemotherapy and the MDM2 inhibitor Nutlin-3

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