Activating PIK3CA mutations coexist with BRAF or NRAS mutations in a limited fraction of melanomas

BackgroundActivated PI3K-AKT pathway may contribute to decrease sensitivity to inhibitors of key pathogenetic effectors (mutated BRAF, active NRAS or MEK) in melanoma. Functional alterations are deeply involved in PI3K-AKT activation, with a minimal role reported for mutations in PIK3CA, the catalytic subunit of the PI3K gene. We here assessed the prevalence of the coexistence of BRAF/NRAS and PIK3CA mutations in a series of melanoma samples.MethodsA total of 245 tumor specimens (212 primary melanomas and 33 melanoma cell lines) was screened for mutations in BRAF, NRAS, and PIK3CA genes by automated direct sequencing.ResultsOverall, 110 (44.9%) samples carried mutations in BRAF, 26 (10.6%) in NRAS, and 24 (9.8%) in PIK3CA. All identified PIK3CA mutations have been reported to induce PI3K activation; those detected in cultured melanomas were investigated for their interference with the antiproliferative activity of the BRAF-mutant inhibitor vemurafenib. A reduced suppression in cell growth was observed in treated cells carrying both BRAF and PIK3CA mutations as compared with those presenting a mutated BRAF only. Among the analysed melanomas, 12/245 (4.9%) samples presented the coexistence of PIK3CA and BRAF/NRAS mutations.ConclusionsOur study further suggests that PIK3CA mutations account for a small fraction of PI3K pathway activation and have a limited impact in interfering with the BRAF/NRAS-driven growth in melanoma.

• Publication year

  2015

• Venue

  Journal of Translational Medicine

• Publication date

  2015-01-28

• Fields of study

  Biology, Medicine

• Identifiers
  DOI 10.1186/s12967-015-0401-8PMID 25627962PMCID 4312444
• External record

  Open on Semantic Scholar

• Source metadata

  Semantic Scholar, PubMed

• No claims are published for this paper.

• No concepts are published for this paper.

• The role of melanogenesis in regulation of melanoma behavior: melanogenesis leads to stimulation of HIF-1α expression and HIF-dependent attendant pathways.

  2014cited by this paper
• Beyond BRAFV600: clinical mutation panel testing by next-generation sequencing in advanced melanoma

  2014cited by this paper
• Melanoma resistance: a bright future for academicians and a challenge for patient advocates.

  2014cited by this paper
• Future perspectives in melanoma research: meeting report from the “Melanoma Bridge”, Napoli, December 5th-8th 2013

  2014cited by this paper
• The genetic landscape of clinical resistance to RAF inhibition in metastatic melanoma.

  2014cited by this paper
• Overcoming resistance to BRAF inhibition in BRAF-mutated metastatic melanoma

  2014cited by this paper
• Whole-genome sequencing reveals complex mechanisms of intrinsic resistance to BRAF inhibition

  2014cited by this paper
• Heterogeneous distribution of BRAF/NRAS mutations among Italian patients with advanced melanoma

  2013cited by this paper
• Future perspectives in melanoma research. Meeting report from the “Melanoma Bridge. Napoli, December 2nd-4th 2012”

  2013cited by this paper
• Future perspectives in melanoma research: meeting report from the “Melanoma Bridge”: Napoli, December 3rd–6th 2014

  2013cited by this paper
• Resistance to RAF inhibitors revisited

  2013cited by this paper
• Resistance to BRAF Inhibition in BRAF-Mutant Colon Cancer Can Be Overcome with PI3K Inhibition or Demethylating Agents

  2012cited by this paper
• The Clinical Effect of the Dual-Targeting Strategy Involving PI3K/AKT/mTOR and RAS/MEK/ERK Pathways in Patients with Advanced Cancer

  2012cited by this paper
• Abrogation of BRAFV600E-induced senescence by PI3K pathway activation contributes to melanomagenesis.

  2012cited by this paper
• Novel Somatic Mutations to PI3K Pathway Genes in Metastatic Melanoma

  2012cited by this paper
• Sensitivity to the MEK inhibitor E6201 in melanoma cells is associated with mutant BRAF and wildtype PTEN status

  2012influential reference
• Prevalence of KRAS, BRAF, and PIK3CA somatic mutations in patients with colorectal carcinoma may vary in the same population: clues from Sardinia

  2012cited by this paper
• Exome sequencing identifies recurrent somatic RAC1 mutations in melanoma

  2012cited by this paper
• BRAF/NRAS mutation frequencies among primary tumors and metastases in patients with melanoma.

  2012cited by this paper
• L‐tyrosine and L‐dihydroxyphenylalanine as hormone‐like regulators of melanocyte functions

  2012cited by this paper
• Concurrent loss of the PTEN and RB1 tumor suppressors attenuates RAF dependence in melanomas harboring V600EBRAF

  2012cited by this paper
• Role and therapeutic potential of PI3K‐mTOR signaling in de novo resistance to BRAF inhibition

  2012influential reference
• Combinations of BRAF, MEK, and PI3K/mTOR Inhibitors Overcome Acquired Resistance to the BRAF Inhibitor GSK2118436 Dabrafenib, Mediated by NRAS or MEK Mutations

  2012cited by this paper
• A landscape of driver mutations in melanoma.

  2012cited by this paper
• PIK3CA Mutations Frequently Coexist with RAS and BRAF Mutations in Patients with Advanced Cancers

  2011cited by this paper
• Protein kinase D3 sensitizes RAF inhibitor RAF265 in melanoma cells by preventing reactivation of MAPK signaling.

  2011cited by this paper
• Induction of arginosuccinate synthetase (ASS) expression affects the antiproliferative activity of arginine deiminase (ADI) in melanoma cells.

  2011cited by this paper
• Abstract 5370: PTEN loss confers BRAF inhibitor resistance to melanoma cells through the suppression of BIM expression

  2011influential reference
• Basal and treatment-induced activation of AKT mediates resistance to cell death by AZD6244 (ARRY-142886) in Braf-mutant human cutaneous melanoma cells.

  2010influential reference
• Cooperative interactions of PTEN deficiency and RAS activation in melanoma metastasis

  2010cited by this paper
• Role of key-regulator genes in melanoma susceptibility and pathogenesis among patients from South Italy

  2009cited by this paper
• Inhibition of mTORC1 leads to MAPK pathway activation through a PI3K-dependent feedback loop in human cancer.

  2008cited by this paper
• Targeting V600EB-Raf and Akt3 using nanoliposomal-small interfering RNA inhibits cutaneous melanocytic lesion development.

  2008cited by this paper
• Akt3 and mutant V600E B-Raf cooperate to promote early melanoma development.

  2008cited by this paper
• A novel AKT3 mutation in melanoma tumours and cell lines

  2008cited by this paper
• PI3-kinase subunits are infrequent somatic targets in melanoma.

  2006cited by this paper
• Mutations of PIK3CA are rare in cutaneous melanoma

  2006cited by this paper
• Journal of Translational Medicine BioMed Central Review

  2005cited by this paper
• Distinct sets of genetic alterations in melanoma.

  2005cited by this paper
• Akt-dependent transformation: there is more to growth than just surviving

  2005cited by this paper
• BRAF gene is somatically mutated but does not make a major contribution to malignant melanoma susceptibility: the Italian Melanoma Intergroup Study.

  2004cited by this paper
• Multiple synchronous cutaneous melanomas: implications for prevention

  2002cited by this paper
• Mutations of the BRAF gene in human cancer

  2002cited by this paper
• The phosphatidylinositol 3-Kinase–AKT pathway in human cancer

  2002cited by this paper

• Identification of SLC22A17 DNA methylation hotspot as a potential biomarker in cutaneous melanoma

  2024cites this paper
• Genetic silencing of AKT induces melanoma cell death via mTOR suppression.

  2023cites this paper
• Genetic silencing of AKT induces melanoma cell death

  2022cites this paper
• Actionable Mutation Profile of Sun-Protected Melanomas in South America

  2022cites this paper
• Resistance to Molecularly Targeted Therapies in Melanoma

  2021cites this paper
• The role of PI3'‐lipid signalling in melanoma initiation, progression and maintenance

  2021cites this paper
• In Vitro Biophysical and Biological Characterization of Lipid Nanoparticles Co-Encapsulating Oncosuppressors miR-199b-5p and miR-204-5p as Potentiators of Target Therapy in Metastatic Melanoma

  2020cites this paper
• A Melanoma-Tailored Next-Generation Sequencing Panel Coupled with a Comprehensive Analysis to Improve Routine Melanoma Genotyping

  2020cites this paper
• A pre-existing rare PIK 3 CA E 545 K subpopulation confers clinical resistance to MEK plus CDK 4 / 6 inhibition in NRAS melanoma and is dependent on S 6 K 1 signaling

  2018cites this paper
• Naturally Occurring Canine Melanoma as a Predictive Comparative Oncology Model for Human Mucosal and Other Triple Wild-Type Melanomas

  2018cites this paper
• A Preexisting Rare PIK3CAE545K Subpopulation Confers Clinical Resistance to MEK plus CDK4/6 Inhibition in NRAS Melanoma and Is Dependent on S6K1 Signaling.

  2018cites this paper
• Autophagy: In the cROSshairs of cancer.

  2017cites this paper
• Impact of phosphoinositide-3-kinase and vitamin D3 nuclear receptor single-nucleotide polymorphisms on the outcome of malignant melanoma patients

  2017cites this paper
• Melanoma: Genetic Abnormalities, Tumor Progression, Clonal Evolution and Tumor Initiating Cells

  2017cites this paper
• Copy number changes of clinically actionable genes in melanoma, non‐small cell lung cancer and colorectal cancer—A survey across 822 routine diagnostic cases

  2016cites this paper
• Melanoma Brain Metastasis: Mechanisms, Models, and Medicine

  2016cites this paper
• The next generation of metastatic melanoma: uncovering the genetic variants for anti-BRAF therapy response

  2016cites this paper